Mathematical assessment of the impact of different microclimate conditions on malaria transmission dynamics

Ann Nwankwo; Daniel Okuonghae; Ann Nwankwo; Daniel Okuonghae

doi:10.3934/mbe.2019069

Mathematical Biosciences and Engineering

2019, Volume 16, Issue 3: 1414-1444. doi: 10.3934/mbe.2019069

Previous Article Next Article

Research article Special Issues

Mathematical assessment of the impact of different microclimate conditions on malaria transmission dynamics

Ann Nwankwo ,
Daniel Okuonghae ^,

Department of Mathematics, University of Benin, Benin City, Nigeria

Received: 20 November 2018 Accepted: 24 January 2019 Published: 21 February 2019

A new non-autonomous model incorporating diurnal temperature fluctuation is designed to study the transmission dynamics of malaria. In particular, the model is used to assess the impact of different microclimate condition on the population dynamics of malaria. The disease free state of the model is seen to be globally asymptotically stable in the absence of disease induced mortality when the associated reproduction number is less than unity. Also when the associated reproduction number of the model is greater than unity, the disease persist in the population. Numerical simulations of the time-averaged basic reproduction number show that neglecting the variation of indoor and outdoor temperature will under-estimate the value of this threshold parameter. Numerical simulations of the model show that the higher indoor temperature influences the efficacy of control measures as a higher prevalence level is obtained when indoor and outdoor temperature variation is considered. It is further shown that both where the mosquitoes rest and how long they rest there may determine the transmission intensity.

Keywords:

Citation: Ann Nwankwo, Daniel Okuonghae. Mathematical assessment of the impact of different microclimate conditions on malaria transmission dynamics[J]. Mathematical Biosciences and Engineering, 2019, 16(3): 1414-1444. doi: 10.3934/mbe.2019069

Related Papers:

[1]	Jinliang Wang, Jingmei Pang, Toshikazu Kuniya . A note on global stability for malaria infections model with latencies. Mathematical Biosciences and Engineering, 2014, 11(4): 995-1001. doi: 10.3934/mbe.2014.11.995
[2]	Peter Witbooi, Gbenga Abiodun, Mozart Nsuami . A model of malaria population dynamics with migrants. Mathematical Biosciences and Engineering, 2021, 18(6): 7301-7317. doi: 10.3934/mbe.2021361
[3]	Jia Li . Malaria model with stage-structured mosquitoes. Mathematical Biosciences and Engineering, 2011, 8(3): 753-768. doi: 10.3934/mbe.2011.8.753
[4]	Eunha Shim, Zhilan Feng, Carlos Castillo-Chavez . Differential impact of sickle cell trait on symptomatic and asymptomatic malaria. Mathematical Biosciences and Engineering, 2012, 9(4): 877-898. doi: 10.3934/mbe.2012.9.877
[5]	Yilong Li, Shigui Ruan, Dongmei Xiao . The Within-Host dynamics of malaria infection with immune response. Mathematical Biosciences and Engineering, 2011, 8(4): 999-1018. doi: 10.3934/mbe.2011.8.999
[6]	Bassidy Dembele, Abdul-Aziz Yakubu . Controlling imported malaria cases in the United States of America. Mathematical Biosciences and Engineering, 2017, 14(1): 95-109. doi: 10.3934/mbe.2017007
[7]	Manuela M. Nimpa, Hyacinthe N. Teytsa, Joseph Mbang, Charles S. Wondji, Ramsès Djidjou-Demasse . Optimizing MDA and antimalarial treatment in the presence of drug resistance for effective malaria control. Mathematical Biosciences and Engineering, 2025, 22(8): 1898-1930. doi: 10.3934/mbe.2025069
[8]	Qian Ding, Jian Liu, Zhiming Guo . Dynamics of a malaria infection model with time delay. Mathematical Biosciences and Engineering, 2019, 16(5): 4885-4907. doi: 10.3934/mbe.2019246
[9]	Cruz Vargas-De-León . Global analysis of a delayed vector-bias model for malaria transmission with incubation period in mosquitoes. Mathematical Biosciences and Engineering, 2012, 9(1): 165-174. doi: 10.3934/mbe.2012.9.165
[10]	Jia Li . A malaria model with partial immunity in humans. Mathematical Biosciences and Engineering, 2008, 5(4): 789-801. doi: 10.3934/mbe.2008.5.789

Abstract

1. Introduction

Malaria is an infectious vector-borne disease caused by female Anopheles mosquitoes infected with the Plasmodium parasite. It remains a major cause of mortality and morbidity in many tropical and subtropical regions of the world ^[38]. Even with resolute disease control efforts advocated by several health authorities, government and non-governmental organizations, the World Health Organization (WHO) estimated that there were 216 million cases of malaria in 2016 in 91 countries globally, where as there were 211 million cases in 2015 ^[39]. Also, there were roughly 445 thousand malaria deaths in 2016 ^[39]. Nigeria accounted for 27% of this global incidence and 24% of this global malaria deaths ^[39].

The dynamics and distribution of malaria have been shown to be strongly influenced by environmental factors such as temperature, rainfall, relative humidity and their daily fluctuations ^[5,30]. These factors have been shown to have significant impact on a range of mosquito life history traits such as the life cycle of mosquitoes as well as the development of sporogonic stages of the parasite within the body of the mosquito and hence, malaria transmission ^[38,21]. Since mosquitoes are highly sensitive to environmental conditions, which can trigger their dynamics and as well affect disease spread ^[7], there has been predictions that climate change will altar the transmission dynamics of malaria and also put at risk previously unexposed populations ^[5,7]. Thus, the understanding of the relationship between the malaria vector and its environment is necessary for effective control of mosquito population and disease prevention ^[7].

Particularly, the study by Paaijmans et al. ^[24] showed that fluctuations in temperature can substantially alter the length of parasite incubation in mosquitoes and that temperature fluctuation can reduce the impact of increases in mean temperature. In other words, fluctuations in temperature can make possible malaria transmission at lower mean temperatures than currently predicted and can potentially prevent transmission at higher mean temperatures than currently predicted ^[25]. The study in ^[25] thus highlighted the need to incorporate the effects of daily temperature variation into predictive models. Also, Blanford et al. ^[6] compared the effect of three measures of temperature; mean monthly temperature, mean daily temperature, and hourly temperatures on estimates of the extrinsic incubation period (EIP). They showed that under low temperature, using mean monthly temperature underestimates the EIP and overestimates it under high temperature. Recently, Shapiro et al. ^[32] used the Asian mosquito, Anopheles stephensi and the malaria parasite, Plasmodium falciparum to show how temperature affects a range of mosquito and parasite traits relevant to transmission.

In addition to daily temperature fluctuations, studies have shown the use of outdoor air temperature in malaria risk models will fail to capture the important features of the actual microclimate experienced by mosquitoes ^[28]. In particular, water temperature influences development rates of immature mosquitoes whereas outdoor and indoor air temperature (as studies have reported the tendency of mosquito species to be endophilic or exophilic or both) determines adult longevity as well as the rate of parasite development within the adult mosquito ^[27]. Therefore, the need for incorporating the variations of indoor and outdoor temperatures in the dynamics of malaria transmission is important as endophilic mosquitoes, and parasites within them, will be exposed more to indoor temperatures than the outdoor air temperature ^[27]. Hence, estimating malaria transmission intensity requires both indoor as well as outdoor temperatures. This is so because indoor temperatures differ from outdoor temperature ^[2,27] and parasite development rate (extrinsic incubation period (EIP)) in endophilic mosquitoes will be faster than predicted from ambient conditions. Also, this difference tend to become larger at higher altitudes as indoor and outdoor temperatures become more divergent with increase in altitude ^[27].

Many studies have explored the impact of climatic variables on the transmission dynamics of malaria. A study by Mondzozo et al. ^[11], showed that a marginal change in temperature and precipitation could lead to a significant change in malaria incidence in African countries. The study in ^[11] made use of a semi-parametric econometric model that investigated the relationship between malaria cases and climatic factors. Mordecai et al. ^[18], using a model which includes empirically derived nonlinear thermal responses, showed that the optimal malaria transmission occurs at 25℃ and decreases for temperature greater than 28℃. Agusto et al. ^[3] showed that for cities across different regions in Sub-Saharan Africa, the malaria burden increases with increasing temperature in the range (16℃–28℃). The work by Christiansen-Jucht et al. ^[8] showed that including age dependence in the vector component of the mosquito-borne disease model may be important to predict (more reliably) disease transmission dynamics. Ngarakana-Gwasira et al. ^[19] showed that as a result of climate change, malaria burden is likely to increase in the tropics, the highland regions and East Africa. Okuneye and Gumel ^[23] developed and analyzed a temperature and rainfall dependent mechanistic malaria model and incorporated features such as host age structure, dynamics of immature mosquitoes (with the egg, larva and pupa stages fused into one class) and reduced susceptibility to malaria infection due to prior malaria infection. Beck-Johnson et al. ^[5] explored the effects of temperature fluctuations on mosquito population dynamics in a stage-structured, delay-differential equation (DDE) model using diurnal, annual, and a combined annual and diurnal sinusoidal temperature fluctuations.

The purpose of this current study is to design, and analyze, a non-autonomous model for assessing the impact of the actual microclimates experienced by mosquitoes on the transmission dynamics of malaria and its control. Specifically, the model will be used to study the impact of the differences in indoor vs outdoor environments on the efficacy of control strategies. To the best of our knowledge, there is no study that has used mathematical models to quantify the differential effects of indoor and outdoor temperatures (explicitly) on the dynamics of malaria in a population. The model is formulated in Section 2. The autonomous version of the model is analyzed in Section 3, while the non-autonomous model will be analyzed in Section 4. Numerical simulations are considered in Section 5. The main conclusions from this study are summarized in Section 6.

2. Materials and method

2.1. Model formulation

The total human population at time t, denoted by $N_h(t)$ , is split into sub-populations of susceptible humans $(S_h(t))$ , exposed humans $(E_h(t))$ , infectious humans $(I_h(t))$ and recovered humans $(R_h(t))$ . Thus, $N_h(t) = S_h(t)+E_h(t)+I_h(t)+R_h(t)$ .

The total vector population, denoted by $N_v(t)$ , is divided into sub-populations of aquatic and adult mosquitoes. The aquatic mosquito sub-population is denoted by $A_m(t)$ . While the adult mosquito population $N_m(t)$ , include outdoor susceptible mosquitoes ( $(S_{vo}(t))$ ), indoor susceptible mosquitoes ( $(S_{vi}(t))$ ), outdoor exposed mosquitoes ( $(E_{vo}(t))$ ), indoor exposed mosquitoes ( $(E_{vi}(t))$ ), outdoor infectious mosquitoes ( $(I_{vo}(t))$ ) and indoor infectious mosquitoes ( $(I_{vi}(t))$ ), so that $N_m(t) = S_{vo}(t)+S_{vi}(t)+E_{vo}(t)+E_{vi}(t)+I_{vo}(t)+I_{vi}(t)$ . Thus, $N_v(t) = A_m(t)+N_m(t)$ .

The non-autonomous model for malaria transmission dynamics in a population is given by the following system of deterministic non-linear differential equations ( describes the associated state variables and parameters in the model (2.1) while gives the flow diagram of model (2.1). $b$ and $\epsilon$ accounts for the efficacy of the bed-nets and door and window nets respectively.):

$\begin{equation} \begin{split} \frac{dS_h}{dt}& = \Lambda_h - (\lambda_{ho}(T_o)+\lambda_{hi}(T_i)(1-b))S_h - \mu_h S_h+\sigma_h R_h,\\ \frac{dE_h}{dt}& = (\lambda_{ho}(T_o)+\lambda_{hi}(T_i)(1-b)) S_h-(\gamma_h+\mu_h)E_h,\\ \frac{dI_h}{dt}& = \gamma_h E_h-(\tau_h+\mu_h+\delta_h)I_h,\quad \frac{dR_h}{dt} = \tau_h I_h-(\mu_h+\sigma_h)R_h,\\ \frac{dA_m}{dt}& = \phi_v(T_o)\left(1-\frac{A_m}{k_v(T_o)}\right)N_m-(\gamma_a(T_w)+\mu_a(T_w))A_m,\\ \frac{dS_{vo}}{dt}& = \gamma_a(T_w)A_m-\lambda_{vo}(T_o) S_{vo}+\rho(T_d)(1-\epsilon)S_{vi}-(\mu_v(T_o)+\alpha(T_d)(1-\epsilon))S_{vo},\\ \frac{dS_{vi}}{dt}& = \alpha(T_d)(1-\epsilon)S_{vo}-\lambda_{vi}(T_i)(1-b) S_{vi}-(\mu_v(T_i)(1+b)+\rho(T_d)(1-\epsilon))S_{vi},\\ \frac{dE_{vo}}{dt}& = \lambda_{vo}(T_o) S_{vo}+\rho(T_d)(1-\epsilon)E_{vi}-(\mu_v(T_o)+\gamma_{vo}(T_o)+\alpha(T_d)(1-\epsilon))E_{vo},\\ \frac{dE_{vi}}{dt}& = \lambda_{vi}(T_i,b)S_{vi}+\alpha(T_d)(1-\epsilon)E_{vo}-(\mu_v(T_i)(1+b)+\gamma_{vi}(T_i)+\rho(T_d)(1-\epsilon))E_{vi},\\ \frac{dI_{vo}}{dt}& = \gamma_{vo}(T_o)E_{vo}+\rho(T_d)(1-\epsilon)I_{vi}-(\mu_v(T_o)+\alpha(T_d)(1-\epsilon))I_{vo},\\ \frac{dI_{vi}}{dt}& = \gamma_{vi}(T_i)E_{vi}+\alpha(T_d)(1-\epsilon)I_{vo}-(\mu_v(T_i)(1+b)+\rho(T_d)(1-\epsilon))I_{vi},\\ \end{split} \end{equation}$

(2.1)

Table 1. Description of variables and parameters in the model (2.1).

Variable	Description
$S_h$	Population of susceptible humans
$E_h$	Population of exposed humans
$I_h$	Population of infectious humans
$R_h$	Population of recovered humans
$A_m$	Immature mosquito population
$S_{vo}$	Susceptible mosquitoes outdoor
$S_{vi}$	Susceptible mosquitoes indoor
$E_{vo}$	Exposed mosquitoes outdoor
$E_{vi}$	Exposed mosquitoes indoor
$I_{vo}$	Infectious mosquitoes outdoor
$I_{vi}$	Infectious mosquitoes indoor
Parameter	Interpretation
$\Lambda_h$	Recruitment rate for humans
$\mu_h$	Natural mortality rate for humans
$\beta_o(T_o)$	Outdoor biting rate of mosquitoes
$\beta_i(T_i)$	Indoor biting rate of mosquitoes
$\rho_{hv}$	Probability of malaria transmission from infectious humans to susceptible mosquitoes
$\rho_{vh}$	Probability of malaria transmission from infectious mosquitoes to susceptible humans
$\sigma_h$	Rate of loss of immunity
$\gamma_h$	Progression rate of exposed humans
$\tau_h$	Recovery rate for humans
$\delta_h$	Disease induced death rate for humans
$b$	Efficacy of insecticide treated net
$\epsilon$	Efficacy of door and window nets
$\phi_v(T_o)$	Egg deposition rate
$k_v(T_o)$	Mosquito carrying capacity
$\gamma_a(T_w)$	Maturation rate of immature mosquito
$\mu_a(T_w)$	Mortality rate of immature mosquito
$\alpha(T_d)$	Outdoor to indoor movement rate of adult mosquitoes
$\rho(T_d)$	Indoor to outdoor movement rate of adult mosquitoes
$\mu_v(T_o)$	Outdoor mortality rate of adult mosquitoes
$\mu_v(T_i)$	Indoor mortality rate of adult mosquitoes
$\gamma_{vo}(T_o)$	Outdoor progression rate of exposed mosquitoes
$\gamma_{vi}(T_i)$	Indoor progression rate of exposed mosquitoes

| Show Table

DownLoad: CSV

Figure 1. Schematic diagram of the model (2.1), where

$\lambda_{ho}$ ,

$\lambda_{hi}$ ,

$\lambda_{vo}$ , and

$\lambda_{vi}$ are given in (2.2).

DownLoad: Full-Size Img PowerPoint

where the forces of infection for humans (outdoor and indoor) and vectors (outdoor and indoor) are given, respectively, by

$\begin{equation} \begin{split} \lambda_{ho}& = \rho_{vh}\beta_o(T_o)\frac{I_{vo}}{N_h},\quad \lambda_{hi} = \rho_{vh}\beta_i(T_i)\frac{I_{vi}}{N_h},\\ \lambda_{vo}& = \rho_{hv}\beta_o(T_o)\frac{I_{h}}{N_h},\quad \lambda_{vi} = \rho_{hv}\beta_i(T_i)\frac{I_{h}}{N_h}.\\ \end{split} \end{equation}$

(2.2)

2.1.1. Temperature-dependent parameters

The temperature-dependent parameters for mosquito egg deposition rate, the per-capita death rate of the immature mosquitoes, maturation rate of immature mosquitoes, mosquito biting rate, natural mortality rate for adult vectors and progression rate of exposed vectors of the model (2.1), (defined using the functions in ^[3,23] where $T_w$ , $T_o$ , $T_i$ denote water, outdoor and indoor temperature, respectively, at time t), are given below:

$\begin{equation} \begin{split} \phi_v(T_o)& = -0.153T_o^2+8.61T_o-97.7,\quad \mu_a(T_w) = \frac{1}{8.560+20.654(1+(\frac{T_w}{19.759})^{6.827})^{-1}},\\ \gamma_a(T_w)& = (-0.153T_w^2+8.61T_w-97.7)(-0.00924T_w^2+0.453T_w-4.77)\\ &\quad(-0.00094T_w^2+0.049T_w-0.552)\left(\frac{1}{-\ln(-0.000828T_w^2+0.0367T_w+0.522)}\right),\\ \beta_o(T_o)& = -0.00014T_o^2+0.027T_o-0.322, \quad \beta_i(T_i,b) = (-0.00014T_i^2+0.027T_i-0.322)(1-b),\\ \mu_{vo}(T_o)& = -\ln(-0.000828T_o^2+0.0367T_o+0.522), \mu_{vi}(T_i) = -\ln(-0.000828T_i^2+0.0367T_i+0.522),\\ \gamma_{vo}(T_o)& = -0.00083T_o^2+0.044T_o-0.487, \quad \gamma_{vi}(T_i) = -0.00083T_i^2+0.044T_i-0.487. \\ \end{split} \end{equation}$

(2.3)

We used a temperature-dependent carrying capacity ( $k_v(T_o)$ ) modeled following ^[40] which assumed that the carrying capacity increases for temperature values in the range $(15^oC to 26.6^oC)$ and begins to decrease for temperature values above $26.6^oC$ due to evaporation and low rainfall. To model mosquito movement rates, it was shown in ^[21] that mosquitoes shift location from indoors to outdoors relative to differences in indoor and outdoor temperature conditions. Therefore, the carrying capacity ( $k_v(T_o)$ ), the outdoor to indoor ( $\alpha(T_d)$ ) and indoor to outdoor ( $\rho(T_d)$ ) movements of mosquitoes are given as follows

$\begin{equation} \begin{split} k_v(T_o)& = -64.36To^2+3298To-34193,\\ \alpha(T_d)& = -0.0583T_d+0.55,\quad \rho(T_d) = 0.0583T_d+0.55\quad \text{where}\quad T_d = T_i-T_o. \end{split} \end{equation}$

(2.4)

Studies have shown that indoor temperatures are warmer than outdoors but show less variation ^[27] (and other references therein). Water temperature has also been shown to be $4-6^oC$ higher than the mean air temperature through out most part of the day ^[26]. Therefore, the following sinusoidal functions given below are used to explore in detail the dynamic consequences of variable temperatures (where $T_w$ , $T_o$ and $T_i$ denote water, outdoor and indoor temperature, respectively, at time t).

$\begin{equation} \begin{split} T_w(t)& = 27+5\cos\left(\frac{2\pi(t-15)}{24}\right),\quad T_o(t) = 24+7\cos\left(\frac{2\pi(t-15)}{24}\right),\\ T_i(t)& = 25+4\cos\left(\frac{2\pi(t-15)}{24}\right). \end{split} \end{equation}$

(2.5)

The model (2.1) is an extension of numerous published malaria transmission models that investigated the impact of climatic variables such as temperature on the population dynamics of malaria. (e.g., ^[3,19,23,29]) inter alia:

(ⅰ) Including the role of indoor and outdoor temperature variations on the dynamics of malaria. None of the works in ^[3,19,23,29] or any other (to the best of our knowledge) considered the impact of such variations.

(ⅱ) Including control measures such as door and window nets as well as bed-net usage. The models in ^[3,19,23,29] did not include all such control measures put together.

(ⅲ) Including outdoor and indoor movement of mature mosquitoes.

2.1.2. Basic properties

The basic properties of the non-autonomous model (2.1) will now be explored. Consider the rate of change of the total human population $N_h'(t)$ and vector population $N_v'(t)$

$\begin{equation} \begin{split} N_h'(t)& = \Lambda_h-\mu_h S_h-\mu_h E_h-\mu_h I_h-\mu_h R_h-\delta_h I_h\leq\Lambda_h-\mu_h N_h,\quad \text{and}\\ \end{split} \end{equation}$

(2.6)

$\begin{equation} \begin{split} N_v'(t)& = \phi_v(t)\left(1-\frac{A_m(t)}{k_v(t)}\right)N_m(t)-\mu_V(t)N_v(t),\\ \end{split} \end{equation}$

(2.7)

where $\mu_V(t) = min\{\mu_a(t), \mu_v(t), \mu_v(t)(1+b)\}$ and $N_m(t) = S_{vo}(t)+S_{vi}(t)+E_{vo}(t)+E_{vi}(t)+I_{vo}(t)+I_{vi}(t)$ is the total population of adult mosquitoes.

In a periodic environment, it is often assumed that the mosquito population stabilizes at a periodic steady state ^[16]. It is then assumed that there exists a positive number $n_o$ ^[16] such that

$\begin{equation} \begin{split} N_v'(t)& = \phi_v(t)\left(1-\frac{A_m(t)}{k_v(t)}\right)N_m(t)-\mu_V(t)L \lt 0 \quad \text{for all}\quad L\geq n_o.\\ \end{split} \end{equation}$

(2.8)

Lemma 2.1. Consider the model (2.1) with non-negative initial conditions satisfying $N_h(t) > 0$ for all $t > 0$ . Then, the model has a unique non-negative solution in $C([0], \mathbb{R}^{11}_+)$ and all solutions are ultimately and uniformly-bounded.

Proof. Following ^[10], the non-autonomous model (2.1) can be written in the form

$\begin{equation} \frac{dY}{dt} = \mathcal{E}(Y)Y+G, \end{equation}$

(2.9)

with $Y = (S_h, E_h, I_h, R_h, A_m, S_{vo}, S_{vi}, E_{vo}, E_{vi}, I_{vo}, I_{vi})$ , $G = (\Lambda_h, 0, 0, 0, 0, 0, 0, 0, 0, 0, 0)^T$ and $\mathcal{E}(Y)$ is a $11\times11$ matrix given as

$\begin{eqnarray*} \mathcal{E}(Y) = \left( \begin{array}{*{11}c} E_1&0&0&\sigma_h&0&0&0&0&0&0&0\\ E_2&-k_1&0&0&0&0&0&0&0&0&0\\ 0&\gamma_h&-k_2&0&0&0&0&0&0&0&0\\ 0&0&\tau_h&-k_3&0&0&0&0&0&0&0\\ 0&0&0&0&-E_3-k_4&0&0&0&0&0&0\\ 0&0&0&0&\gamma_a(t)&-E_4-k_5&\rho(t)(1-\epsilon)&0&0&0&0\\ 0&0&0&0&0&\alpha(t)(1-\epsilon)&-E_5-k_6&0&0&0&0\\ 0&0&0&0&0&E_4&0&-k_7&\rho(t)(1-\epsilon)&0&0\\ 0&0&0&0&0&0&E_5&\alpha(t)(1-\epsilon)&-k_8&0&0\\ 0&0&0&0&0&0&0&\gamma_{vo}(t)&0&-k_5&\rho(t)(1-\epsilon)\\ 0&0&0&0&0&0&0&0&\gamma_{vi}(t)&\alpha(t)(1-\epsilon)&-k_6\\ \end{array} \right), \end{eqnarray*}$

where

$\begin{split} E_1& = -\rho_{vh}\frac{\beta_o(t)Y_{10}+\beta_i(t,b)Y_{11}}{N_h}-\mu_h, \quad E_2 = \rho_{vh}\frac{\beta_o(t)Y_{10}+\beta_i(t,b)Y_{11}}{N_h},\\ E_3& = \frac{\phi_v(t)(Y_{6}+Y_{7}+Y_{8}+Y_{9}+Y_{10}+Y_{11})}{k_v(t)},\quad E_4 = \rho_{hv}\frac{\beta_o(t)Y_3}{N_h}, \quad E_5 = \rho_{hv}\frac{\beta_i(t,b)Y_3}{N_h},\\ k_1 = &\gamma_h+\mu_h, \quad k_2 = \tau_h+\mu_h+\delta_h, \quad k_3 = \mu_h+\sigma_h, \quad k_4 = \gamma_a(t)+\mu_a(t)\quad k_5 = \mu_v(t)+\alpha(1-\epsilon),\\ k_6 = &\mu_v(t)(1+b)+\rho(1-\epsilon),\quad k_7 = \mu_v(t)+\alpha(1-\epsilon)+\gamma_{vo}(t),\quad k_8 = \mu_v(t)(1+b)+\rho(1-\epsilon)+\gamma_{vi}(t).\\ \end{split}$

Now, using the fact that $G\geq0$ and that the matrix $\mathcal{E}(Y)$ is quasi-positive, it follows that the model (2.9) is positively-invariant in $C([0], \mathbb{R}^{11}_+)$ . Furthermore, by the comparison theorem ^[14], the solutions of (2.6) and (2.7) exist for all $t\geq0$ . Moreover, from (2.6), we see that

$N_h(t)\leq N_h(0)\exp(-\mu_h(t))+\frac{\Lambda_h}{\mu_h}[1-\exp(-\mu_h(t))], \quad \text{so that} \quad \limsup\limits_{t\rightarrow\infty} N_h(t)\leq\frac{\Lambda_h}{\mu_h}.$

The unique $\tau$ -periodic solution of (2.7) in $C([0], \mathbb{R}_+)\backslash\{0\}$ $N_v^*(t)$ is given by

$\begin{equation} \begin{split} N_v^*(t)& = \exp\left(-\int^t_0\mu_V(s)\mathrm{d}s\right)\times\int^t_0\left[\phi_v(s)\left(1-\frac{A_m(s)}{k_v(s)}\right)N_m(s)\exp\left(\int^s_0\mu_V(\zeta)d\zeta\right)\right]\mathrm{d}s \\ &\quad+\exp\left(-\int^t_0\mu_V(s)\mathrm{d}s\right)\times\frac{\int^{\tau}_0\phi_v(s)\left(1-\frac{A_m(s)}{k_v(s)}\right)N_m(s)\exp\left(\int^s_0(\mu_V(\omega)\mathrm{d}\omega)\right)\mathrm{d}s}{\left(\exp\left(\int^\tau_0\mu_V(s)\mathrm{d}s\right)-1\right)}, \end{split} \end{equation}$

(2.10)

so that

$\limsup\limits_{t\rightarrow\infty}(A_m(t)+S_{vo}(t)+S_{vi}(t)+E_{vo}(t)+E_{vi}(t)+I_{vo}(t)+I_{vi}(t)-N_v^*(t))\leq0.$

Hence all solutions of the model (2.1) are ultimately bounded. Moreover, it follows from (2.6) and (2.8) that $N'_h(t) < 0$ and $N'_v(t) < 0$ whenever $N_h(t) > \frac{\Lambda_h}{\mu_h}$ and $N_v(t) > n_o$ , respectively. Thus all solutions of the model (2.1) are uniformly bounded.

2.2. Analysis of the autonomous model

It is important to analyze the dynamics of the autonomous version of the non-autonomous model (2.1). Consider the case of the non-autonomous model (2.1) where all the temperature-dependent parameters are constants, then the reduced model is denoted as the autonomous model. We define the threshold quantity

$\begin{equation} \mathcal{R}_v = \frac{\phi_v\gamma_a(g_6+\alpha(1-\epsilon))}{g_4(g_5g_6-\alpha\rho(1-\epsilon)^2)}, \end{equation}$

(2.11)

to be the production rate of mosquitoes offsprings. It is a product of the egg deposition rate $\phi_v$ , probability that an egg becomes an adult $\frac{\gamma_a}{g_4}$ and the duration spent in the adult stage $\frac{\mu_v(1+b)+(1-\epsilon)(\alpha+\rho)}{\mu_v(\mu_v(1+b)+(1-\epsilon)(\alpha+\rho))}.$

The autonomous model has two disease-free equilibria. We shall call them the trivial disease free equilibrium (TDFE) and the realistic disease free equilibrium (RDFE), explained thus:

(ⅰ) If $\mathcal{R}_v\leq1$ , the autonomous model has a TDFE (where there are no mosquitoes). This is given as

$\mathcal{T}_o = (S_h^o, E_h^o, I_h^o, R_h^o, A_m^o,S_{vo}^o, S_{vi}^o, E_{vo}^o, E_{vi}^o, I_{vo}^o, I_{vi}^o) = \left(\frac{\Lambda_h}{\mu_h}, 0, 0, 0, 0, 0, 0, 0, 0, 0, 0\right)$

(ⅱ) If $\mathcal{R}_v > 1$ , the autonomous model has a RDFE (where we have mosquitoes present) given as

$\mathcal{E}_o = (S_h^*, E_h^*, I_h^*, R_h^*, A_m^*, S_{vo}^*, S_{vi}^*, E_{vo}^*, E_{vi}^*, I_{vo}^*, I_{vi}^*) = \left(\frac{\Lambda_h}{\mu_h}, 0, 0, 0, \bar{A_m}, \bar{S}_{vo}, \bar{S}_{vi}, 0, 0, 0, 0\right),$

where

$\begin{split} \bar{A_m}& = k_v\left(1-\frac{1}{\mathcal{R}_v}\right), \quad \bar{S}_{vo} = \frac{g_6\gamma_a k_v}{g_5 g_6-\alpha\rho(1-\epsilon)^2}\left(1-\frac{1}{\mathcal{R}_v}\right),\quad \text{and} \\ \bar{S}_{vi}& = \frac{\alpha(1-\epsilon) \gamma_a k_v}{g_5 g_6-\alpha\rho(1-\epsilon)^2}\left(1-\frac{1}{\mathcal{R}_v}\right).\\ \end{split}$

2.2.1. Asymptotic stability of disease-free equilibria

Global asymptotic stability of the trivial disease free equilibrium (TDFE)

Theorem 2.1. The TDFE of the autonomous version of the model (2.1), denoted by $\mathcal{T}_o$ , is globally asymptotically stable (GAS) in $C([0], \mathbb{R}^{11}_+)$ whenever $\mathcal{R}_v\leq1$ .

Proof. Following the approach in ^[10,23], let $\mathcal{R}_v\leq1$ , so that only the TDFE $(\mathcal{T}_o)$ exist. Also, let $Y = X-TDFE$ . So that, $\frac{\mathrm{d}Y}{\mathrm{d}t} = \mathcal{B}(Y)Y$ , where $S_h = Y_1, \quad E_h = Y_2, \quad I_h = Y_3, \quad R_h = Y_4, \quad A_m = Y_5, \quad S_{vo} = Y_6, \quad S_{vi} = Y_7, \quad E_{vo} = Y_{8}, \quad E_{vi} = Y_{8}, \quad I_{vo} = Y_{10}, \quad I_{vi} = Y_{11} \quad \text{and}\quad \mathcal{B}(Y)\quad \text{is given as}$

$\begin{eqnarray*} \mathcal{B}(Y) = \left( \begin{array}{*{13}c} B_1&0&0&\sigma_h&0&0&0&0&0&-\rho_{vh}\beta_o&-\rho_{vh}\beta_i(b)\\ B_2&-g_1&0&0&0&0&0&0&0&\rho_{vh}\beta_o&\rho_{vh}\beta_i(b)\\ 0&\gamma_h&-g_2&0&0&0&0&0&0&0&0\\ 0&0&\tau_h&-g_3&0&0&0&0&0&0&0\\ 0&0&0&0&B_3-g_4&\phi_v&\phi_v&\phi_v&\phi_v&\phi_v&\phi_v\\ 0&0&0&0&\gamma_a&-B4-g_5&\rho(1-\epsilon)&0&0&0&0\\ 0&0&0&0&0&\alpha(1-\epsilon)&-B_5-g_6&0&0&0&0\\ 0&0&0&0&0&B_4&0&-g_7&\rho(1-\epsilon)&0&0\\ 0&0&0&0&0&0&B_5&\alpha(1-\epsilon)&-g_{8}&0&0\\ 0&0&0&0&0&0&0&\gamma_{vo}&0&-g_5&\rho(1-\epsilon)\\ 0&0&0&0&0&0&0&0&\gamma_{vi}&\alpha(1-\epsilon)&-g_6\\ \end{array} \right), \end{eqnarray*}$

with

$\begin{split} B_1& = -\rho_{vh}\frac{\beta_{o}Y_{10}+\beta_{i}Y_{11}}{N_h}-\mu_h, \quad B_2 = \rho_{vh}\frac{\beta_{o}Y_{10}+\beta_{i}Y_{11}}{N_h},\\ B_3& = -\frac{\phi_v(Y_{6}+Y_{7}+Y_{8}(t)+Y_{9}+Y_{10}+Y_{11})}{k_v},\quad B_4 = \rho_{hv}\frac{\beta_{o}Y_3}{N_h}\quad B_5 = \rho_{hv}\frac{\beta_{i}(1-b)Y_3(t)}{N_h},\\ g_1& = \gamma_h+\mu_h, \quad g_2 = \tau_h+\mu_h+\delta_h, \quad g_3 = \mu_h+\sigma_h, \quad g_4 = \gamma_a+\mu_a,\quad g_5 = \mu_v+\alpha(1-\epsilon),\\ g_6& = \mu_v(1+b)+\rho(1-\epsilon),\quad g_7 = \mu_v+\alpha(1-\epsilon)+\gamma_{vo},\quad g_{8} = \mu_v(1+b)+\rho(1-\epsilon)+\gamma_{vi}.\\ \end{split}$

Consider the Lyapunov function

$\mathcal{V}(Y) = \langle\mathcal{W},Y\rangle, \quad \text{with} \quad \mathcal{W} = (1, 1, 1, 1,\frac{\mu_v}{\phi_v},1,1,1,1,1,1). \quad \text{We then have that} \\ \dot{\mathcal{V}}(Y) = \langle\mathcal{W},\mathcal{B}(Y)Y\rangle = -\mu_h(Y_1+Y_2+Y_3+Y_4)-\delta_h Y_3-\frac{\mu_v}{k_v}Y_5(Y_6+Y_7+Y_8+Y_9+Y_{10}+Y_{11})\\-b\mu_v(Y_7+Y_9+Y_{11})-\quad\frac{g_4\mu_v Y_5}{\phi_v}\left[1-\frac{\mu_v(1+b)+\rho(1-\epsilon)+\alpha(1-\epsilon)(1+b)}{\mu_v(1+b)+\rho(1-\epsilon)+\alpha(1-\epsilon)}\mathcal{R}_v\right].$

It then follows that

$\dot{\mathcal{V}}(Y)\leq0 \quad \text{if} \quad\frac{\mu_v(1+b)+\rho(1-\epsilon)+\alpha(1-\epsilon)(1+b)}{\mu_v(1+b)+\rho(1-\epsilon)+\alpha(1-\epsilon)}\mathcal{R}_v\leq1,\quad \text{which implies that}$

$\mathcal{R}_v\leq\frac{\mu_v(1+b)+\rho(1-\epsilon)+\alpha(1-\epsilon)}{\mu_v(1+b)+\rho(1-\epsilon)+\alpha(1-\epsilon)(1+b)}.$

It is easy to see that for $0\leq b\leq 1$ , $\frac{\mu_v(1+b)+\rho(1-\epsilon)+\alpha(1-\epsilon)}{\mu_v(1+b)+\rho(1-\epsilon)+\alpha(1-\epsilon)(1+b)}\leq1$ .

Hence, $\mathcal{\dot{V}}\leq0$ . Furthermore, it follow from LaSalle's Invariance Principle (Theorem 6.4 of ^[15]) that the maximal invariant set contained in $\{\mathcal{V}|\dot{\mathcal{V}}(Y)\}$ is the $TDFE_Y$ . Thus, the transformed equilibrium $TDFE_Y$ is GAS in $C([0], \mathbb{R}^{11}_+)$ if $\mathcal{R}_v\leq1$ . Hence, $\mathcal{T}_o$ is also GAS in $C([0], \mathbb{R}^{11}_+)$ whenever $\mathcal{R}_v\leq1$ .

Local asymptotic stability of the realistic disease free equilibrium (RDFE)

Let $\mathcal{R}_v > 1$ so that the RDFE $(\mathcal{E}_o)$ exist. The local stability of $\mathcal{E}_o$ in $C([0], \mathbb{R}^{11}_+)\setminus{\mathcal{T}_o}$ can be established using the next generation operator method on the autonomous version of the model (2.1) ^[9,36]. Using closely related notations in ^[36], the matrices $F$ and $V$ , for the new infection terms and the remaining transfer terms are, respectively, given by

$\begin{eqnarray*} F = \begin{pmatrix} 0&0&0&0&\rho_{vh}\beta_{o}&\rho_{vh}\beta_{i}(b)\\ 0&0&0&0&0&0\\ 0&\frac{\rho_{hv}\beta_{o}S_{vo}^*}{N_h^*}&0&0&0&0\\ 0&\frac{\rho_{hv}\beta_{i}(b)S_{vi}^*}{N_h^*}&0&0&0&0\\ 0&0&0&0&0&0\\ 0&0&0&0&0&0\\ \end{pmatrix},\quad \text{and} \end{eqnarray*}$

$\begin{eqnarray*} V = \begin{pmatrix} g_1&0&0&0&0&0\\ -\gamma_h&g_2&0&0&0&0\\ 0&0&g_7&-\rho(1-\epsilon)&0&0\\ 0&0&-\alpha(1-\epsilon)&g_{8}&0&0\\ 0&0&-\gamma_{vo}&0&g_5&-\rho(1-\epsilon)\\ 0&0&0&-\gamma_{vi}&-\alpha(1-\epsilon)&g_6\\ \end{pmatrix}. \end{eqnarray*}$

Hence it follows from ^[36] that the reproduction number of the autonomous version of the model (2.1) is given by

$\begin{equation} \begin{split} \mathcal{R}_T& = \sqrt{{\rho_{vh}\rho_{hv}\gamma_a\gamma_h\mu_hk_v\left(1-\frac{1}{\mathcal{R}_v}\right)(\beta_o^2g_6(\gamma_{vi}\alpha\rho(1-\epsilon)^2+\gamma_{vo}g_6g_8)+\atop\beta_o\beta_i(b)\alpha(1-\epsilon)(g_5g_6\gamma_{vi}+g_6g_8\gamma_{vo}+g_6\gamma_{vo}\rho(1-\epsilon)+g_7\gamma_{vi}\rho(1-\epsilon))+\beta_i(b)^2\alpha(1-\epsilon)(\gamma_{vo}\alpha\rho(1-\epsilon)^2+g_5g_7\gamma_{vi}))}\over g_1g_2\Lambda_h(g_5g_6-\alpha\rho(1-\epsilon)^2)^2(g_7g_8-\alpha\rho(1-\epsilon)^2)},\quad \text{where}\\ g_1& = \gamma_h+\mu_h, \quad g_2 = \tau_h+\mu_h+\delta_h, \quad g_3 = \mu_h+\sigma_h, \quad g_4 = \gamma_a+\mu_a,\quad g_5 = \mu_v+\alpha(1-\epsilon),\\ g_6& = \mu_v(1+b)+\rho(1-\epsilon),\quad g_7 = \mu_v+\alpha(1-\epsilon)+\gamma_{vo},\quad g_{8} = \mu_v(1+b)+\rho(1-\epsilon)+\gamma_{vi},\\ \end{split} \end{equation}$

(2.12)

and $\mathcal{R}_v$ is defined as

$\mathcal{R}_v = \frac{\phi_v\gamma_a(g_6+\alpha(1-\epsilon))}{g_4(g_5g_6-\alpha\rho(1-\epsilon)^2)}.$

It should be noted from (2.12) that $\mathcal{R}_T$ is positive if and only if $\mathcal{R}_v > 1$ (so that $\mathcal{E}_o$ exist). The result below follows from Theorem 2 of ^[36].

Theorem 2.2. The RDFE, $\mathcal{E}_o$ , of the autonomous version of the model (2.1) is locally asymptotically stable (LAS) in $C([0], \mathbb{R}^{11}_+)\setminus{\mathcal{T}_o}$ if $\mathcal{R}_T < 1$ , and unstable if $\mathcal{R}_T > 1$ .

The threshold quantity $\mathcal{R}_{T}$ is the effective or control reproduction number for the autonomous version of the model (2.1). It represents the average number of secondary malaria infections generated by a typical infected individual in a completely susceptible population where there are control measures are present ^[36]. By Theorem 2.2, biologically speaking, malaria can be eliminated from the population when $\mathcal{R}_{T} < 1$ if the initial sizes of the population of the model are in the region of attraction $\mathcal{E}_o$ .

2.2.2. Global Asymptotic Stability of the RDFE: special case

We now prove the global asymptotic stability of the RDFE of the autonomous version of the model (2.1) for the special case when $\delta_h = 0$ , since it has been repeatedly shown in literature that the presence of disease-induced mortality in humans can cause a backward bifurcation in vector-borne diseases ^[12,13,22]. We claim the following result.

Theorem 2.3. The RDFE of the special case of the autonomous version of the model (2.1) with $\delta_h = 0$ is globally asymptotically stable in $C([0], \mathbb{R}^{11}_+)\setminus{\mathcal{T}_o}$ if $\mathcal{R}_T^m\leq1$ (with $\mathcal{R}_T^m$ given as)

$\begin{equation} \begin{split} \mathcal{R}_T^m& = \sqrt{{\rho_{vh}\rho_{hv}\gamma_a\gamma_h\Lambda_hk_v\left(1-\frac{1}{\mathcal{R}_v}\right)(\beta_o^2g_6(\gamma_{vi}\alpha\rho(1-\epsilon)^2+\gamma_{vo}g_6g_8)+\atop\beta_o\beta_i(b)\alpha(1-\epsilon)(g_5g_6\gamma_{vi}+g_6g_8\gamma_{vo}+g_6\gamma_{vo}\rho(1-\epsilon)+g_7\gamma_{vi}\rho(1-\epsilon))+\beta_i(b)^2\alpha(1-\epsilon)(\gamma_{vo}\alpha\rho(1-\epsilon)^2+g_5g_7\gamma_{vi}))}\over g_1g_2\mu_h(g_5g_6-\alpha\rho(1-\epsilon)^2)^2(g_7g_8-\alpha\rho(1-\epsilon)^2)}, \end{split} \end{equation}$

(2.13)

Proof. Consider the following Lyapunov function:

$\begin{split} \mathcal{L}& = L_1\frac{\gamma_h E_h}{g_1g_2}+L_1\frac{I_h}{g_2}+L_2E_{vo}+L_3E_{vi}+\mathcal{R}_T^m\frac{\beta_o g_6+\alpha(1-\epsilon)\beta_i(b)}{g_5g_6-\alpha\rho(1-\epsilon)^2}I_{vo}+\mathcal{R}_T^m\frac{\beta_o\rho(1-\epsilon)+g_5\beta_i(b)}{g_5g_6-\alpha\rho(1-\epsilon)^2}I_{vi},\\ L_1& = {{\rho_{hv}(\beta_o^2S_{vo}^*(\alpha\rho(1-\epsilon)^2\gamma_{vi}+g_6g_8\gamma_{vo})+\beta_i(b)\beta_o(\alpha(1-\epsilon)S_{vo}^*(g_5\gamma_{vi}+g_8\gamma_{vo})+\atop\rho(1-\epsilon)S_{vi}^*(g_7\gamma_{vi}+g_6\gamma_{vo}))+\beta_i^2(b)S_{vi}^*(g_5g_7\gamma_{vi}+\alpha\rho(1-\epsilon)^2\gamma_{vo}))}\over(g_5g_6-\alpha\rho(1-\epsilon)^2)(g_7g_8-\alpha\rho(1-\epsilon)^2)}\\ L_2& = \frac{\beta_o(\alpha\rho(1-\epsilon)^2\gamma_{vi}+g_6g_8\gamma_{vo})+\alpha(1-\epsilon)\beta_i(b)(g_5\gamma_{vi}+g_8\gamma_{vo})}{(g_5g_6-\alpha\rho(1-\epsilon)^2)(g_7g_8-\alpha\rho(1-\epsilon)^2)}\mathcal{R}_T^m\quad \text{and} \\ L_3& = \frac{\rho(1-\epsilon)\beta_o(g_7\gamma_{vi}+g_6\gamma_{vo})+\beta_i(b)(g_5g_7\gamma_{vi}+\alpha\rho(1-\epsilon)^2\gamma_{vo})}{(g_5g_6-\alpha\rho(1-\epsilon)^2)(g_7g_8-\alpha\rho(1-\epsilon)^2)}\mathcal{R}_T^m. \end{split}$

with a Lyapunov derivative given by,

$\begin{equation} \begin{split} \mathcal{\dot{L}}& = L_1\frac{\gamma_h \dot{E}_h}{g_1g_2}+L_1\frac{\dot{I}_h}{g_2}+L_2\dot{E}_{vo}+L_3\dot{E}_{vi}+\mathcal{R}_T^m\frac{\beta_o g_6+\alpha(1-\epsilon)\beta_i(b)}{g_5g_6-\alpha\rho(1-\epsilon)^2}\dot{I}_{vo}+\mathcal{R}_T^m\frac{\beta_o\rho(1-\epsilon)+g_5\beta_i(b)}{g_5g_6-\alpha\rho(1-\epsilon)^2}\dot{I}_{vi},\\ \end{split} \end{equation}$

(2.14)

Substituting the expressions of the derivatives of $\dot{E}_h \quad \dot{I}_h \quad \dot{E}_{vo}\quad \dot{E}_{vi}\quad \dot{I}_{vo}\quad \text{and} \quad \dot{I}_{vi}$ , from the autonomous version of the model (2.1) with $\delta_h = 0$ , into (2.14) (and after some algebraic calculations) leads to

$\mathcal{\dot{L}}\leq(L_1I_h+\mathcal{R}_T^m\beta_o I_{vo}+\mathcal{R}_T^m\beta_i I_{vi})(\mathcal{R}_T^m-1).$

Since all the parameters and variables of the mass action model of the autonomous version of the model (2.1) are non-negative, it follows that $\mathcal{\dot{L}}\leq 0$ for $\mathcal{R}_T^m\leq1$ . Furthermore, $\mathcal{\dot{L}} = 0$ if and only if $E_h = I_h = E_{vo} = E_{vi} = I_{vo} = I_{vi} = 0$ . Hence, $\mathcal{L}$ is a Lyapunov function. Thus, it follows, by LaSalle's Invariance Principle ^[15], that every solution to the equations in the autonomous version of the model (2.1) with initial conditions in $C([0], \mathbb{R}^{11}_+)\setminus{\mathcal{T}_o}$ converges to the RDFE $\mathcal{E}_{o}$ as $t\rightarrow\infty$ . That is,

$(E_h (t), I_h (t), E_{vo} (t), E_{vi} (t), I_{vo} (t), I_{vi} (t))\rightarrow(0, 0, 0, 0, 0, 0)$ as $t\rightarrow\infty$ . Substituting $E_h = I_h = E_{vo} = E_{vi} = I_{vo} = I_{vi} = 0$ into the first, fifth, sixth, seventh eighth and ninth equations of the autonomous version of the model (2.1) gives the following as $t\rightarrow\infty$

$(S_h(t), A_m(t), S_{vo}(t), S_{vi}(t))\rightarrow (S_h(t)^*, A_m(t)^*, S_{vo}(t)^*, S_{vi}(t)^*).$

Thus the RDFE of the special case of the autonomous version of the model (2.1) with $\delta_h = 0$ is globally asymptotically stable in $C([0], \mathbb{R}^{11}_+)\setminus{\mathcal{T}_o}$ if $\mathcal{R}_T^m\leq1$ .

2.3. Analysis of the non-autonomous model

Just like the autonomous version, the non-autonomous version has two disease free equilibria, namely, the trivial disease free equilibrium and the realistic disease free equilibrium. We will however analyze only the realistic disease free equilibrium as the former is ecologically unrealistic. We define the threshold quantity $\mathcal{R}_v(t)$ (the production rate of mosquitoes offsprings), given as

$\mathcal{R}_v(t) = \frac{\phi_v(t)\gamma_a(t)(k_6+\alpha(t)(1-\epsilon))}{k_4(t)(k_5(t) k_6(t)-\alpha(t)\rho(t)(1-\epsilon)^2)}.$

The realistic disease free equilibrium (RDFE) is obtained by setting $E_h = I_h = R_h = E_{vo} = E_{vi} = I_{vo} = I_{vi} = 0$ in the model (2.1),

$\mathcal{E}_{0N} = (S_h^a,0,0,0,A_m^a,S_{vo}^a,S_{vi}^a,0,0,0,0) \quad \text{where} \quad S_h^a = \frac{\Lambda_h}{\mu_h},$

with ( $A_m^a, S_{vo}^a, S_{vi}^a$ ) being the unique periodic solution (for $\mathcal{R}_v(t) > 1 \quad for\quad all\quad t\geq0$ ), satisfying:

$\begin{split} \frac{d A_m^a(t)}{dt}& = \phi_v(t)\left(1-\frac{A_m^a(t)}{k_v(t)}\right)(S_{vo}^a(t)+S_{vi}^a(t))-(\gamma_a(t)+\mu_a(t))A_m^a(t),\\ \frac{d S_{vo}^a(t)}{dt}& = \gamma_a(t)A_m^a(t)-\lambda_{vo}(t) S_{vo}^a(t)+\rho(t)(1-\epsilon)S_{vi}^a(t)-(\mu_v(t)+\alpha(t)(1-\epsilon))S_{vo}^a(t),\\ \frac{d S_{vi}^a(t)}{dt}& = \alpha(t)(1-\epsilon)S_{vo}^a(t)-\lambda_{vi}(t,b) S_{vi}^a(t)-(\mu_v(t,b)+\rho(t)(1-\epsilon))S_{vi}^a(t).\\ \end{split}$

2.3.1. Local asymptotic stability of RDFE ( $\mathcal{E}_{0N}$ )

The basic reproduction ratio associated with the non-autonomous model (2.1) will now be computed using the the approach in ^[37]. The next generation matrix $F_N(t)$ (of the new infection terms) and the M-Matrix $V_N(t)$ (of the remaining transfer terms), associated with non-autonomous model (2.1), are given respectively by

$\begin{eqnarray*} F_N(t) = \begin{pmatrix} 0&0&0&0&\rho_{vh}\beta_{o}(t)&\rho_{vh}\beta_{i}(t,b)\\ 0&0&0&0&0&0\\ 0&\frac{\rho_{hv}\beta_{o}(t)S_{vo}^a(t)}{N_h^a}&0&0&0&0\\ 0&\frac{\rho_{hv}\beta_{i}(t,b)S_{vi}^a(t)}{N_h^a}&0&0&0&0\\ 0&0&0&0&0&0\\ 0&0&0&0&0&0\\ \end{pmatrix},\quad \text{and} \end{eqnarray*}$

$V_N(t) = \begin{pmatrix} k_1&0&0&0&0&0\\ -\gamma_h&k_2&0&0&0&0\\ 0&0&k_7&-\rho(t)(1-\epsilon)&0&0\\ 0&0&-\alpha(t)(1-\epsilon)&k_{8}&0&0\\ 0&0&-\gamma_{vo}(t)&0&k_5&-\rho(t)(1-\epsilon)\\ 0&0&0&-\gamma_{vi}(t)&-\alpha(t)(1-\epsilon)&k_6\\ \end{pmatrix}.$

Following ^[23,37], let $\Phi_M$ be the monodromy matrix of the linear $\tau$ -periodic system

$\frac{dZ}{dt} = M(t)Z.$

Also, let $\rho(\Phi_M(\tau))$ be the spectral radius of $\Phi_M(\tau)$ and $Y(s, t), \quad t = s$ , be the evolution operator of the linear $\tau$ -periodic system $\frac{dy}{dt} = -V_N(t)y$ . So that for each $s\in\mathbb{R}$ , the associated $6\times6$ matrix $Y(t, s)$ satisfies ^[37]

$\frac{dY(t,s)}{dt} = -V_N(t)Y(t,s)\forall t\geq s, Y(s,s) = I.$

Furthermore, let $\phi(s)\quad (\tau-periodic\quad in \quad s)$ be the initial distribution of infectious individuals. Thus, $F_N(s)\phi(s)$ is the rate at which new infections are produced by infected individuals who were introduced into the population at time $s$ ^[37]. Since $t = s$ , it follows that $Y(t, s)F_N(s)\phi(s)$ represents the distribution of those infected individuals who were newly infected at time $s$ , and remain infected at time $t$ . Hence, the cumulative distribution of new infections at time $t$ , produced by all infected individuals $(\phi(s))$ introduced at a prior time $s = t$ , is given by

$\Psi(t) = \int^t_{-\infty} Y(t,s)F_N(s)\phi(s)ds = \int^\infty_0 Y(t,t-a)F_N(t-a)\phi(t-a)da.$

Let $\mathbb{C}_\tau$ be the ordered Banach space of all $\tau-periodic$ functions from $\mathbb{R}$ to $\mathbb{R}^6$ , equipped with a maximum norm $\parallel.\parallel$ and positive cone

$\mathbb{C}^+_\tau\{\phi\in\mathbb{C}_\tau:\phi(t)\geq0,\forall t\in \mathbb{R}\}.$

Define a linear-operator $L:\mathbb{C}_\tau\rightarrow\mathbb{C}_\tau$ ^[37]

$(L\phi)(t) = \int^\infty_0 Y(t,t-a)F_N(t-a)\phi(t-a)da \forall t\in \mathbb{R}, \phi \in \mathbb{C}_l$

The basic reproduction number $\mathcal{R}_T(t)$ is then given as the spectral radius of $L$ , denoted by $\rho(L)$ . The proof that the model (2.1) satisfies the conditions A1-A7 in ^[37,4] is given in Appendix A. The result below follows from Theorem 2.2 in ^[37].

Theorem 2.4. The RDFE of the non-autonomous model (2.1) is locally asymptotically stable if $\mathcal{R}_T(t) < 1$ (given that $\mathcal{R}_v(t) > 1$ ) and unstable if $\mathcal{R}_T(t) > 1$ .

2.3.2. Global asymptotic stability of RDFE ( $\mathcal{E}_{0N}$ )

The global stability of the realistic disease free equilibrium of the non-autonomous model (2.1) will now be explored for the special case where $\delta_h = 0$ . We claim the following result, with the proof in Appendix B.

Theorem 2.5. Consider the special case of the non-autonomous model (2.1) with $\delta_h = 0$ so that $N_h^*(t)\rightarrow\frac{\Lambda_h}{\mu_h}$ as $t\rightarrow\infty$ . The RDFE of the resulting model is GAS in $C([0], \mathbb{R}^{11}_+)\setminus{\mathcal{T}_o}$ if $\mathcal{R}_T^m(t) = \mathcal{R}_T(t)|_{\delta_h = 0} < 1$

The proof of Theorem 2.5, based on using comparison theorem ^[34], is given in Appendix B. The epidemiological implication of Theorem 2.5 is that malaria can be effectively controlled(if not eliminated) if the reproduction threshold $\mathcal{R}_T^m(t)$ can be brought to as well as maintained at a value less than unity.

2.3.3. Uniform persistence of the disease

We now explore the possibility of the existence of a positive periodic equilibrium for the model (2.1) using the uniform persistence theory. Let $\mathcal{E}_N(t)$ be any arbitrary positive periodic equilibrium of the model (2.1). Following ^[16,17,23], it is convenient to define the following sets:

We claim the following result, with the proof in Appendix C.

Theorem 2.6. Consider the non-autonomous model (2.1). Suppose that $\mathcal{R}_T(t) > 1$ and $\mathcal{R}_v(t) > 1$ for all $t\geq0$ . Then the model has at least one positive periodic equilibrium, and there exists a $q > 0$ such that any equilibrium $\Phi_t(\phi)$ of the model with initial value $\phi\in X_0$ satisfies

$\liminf\limits_{t\rightarrow\infty}(E_h(t),I_h(t),R_h(t),E_{vo}(t),E_{vi}(t),I_{vo}(t),I_{vi}(t))\geq(q,q,q,q,q,q,q)$

The proof of Theorem 2.6, based on using the approach in ^[16,23], is given in Appendix C. The epidemiological implication of Theorem 2.6 is that malaria will persist in the population whenever $\mathcal{R}_T(t) > 1$ and $\mathcal{R}_v(t) > 1$ , for all $t\geq0$ .

3. Results: Numerical simulations of the model (2.1)

The model (2.1) is simulated numerically to investigate the impact of the variation in indoor and outdoor conditions on the transmission of malaria using parameter values given in Table 2.

Table 2. Parameter value of temperature independent parameters in the model (2.1).

Parameter	Baseline value	Range	Reference
$\Lambda_h$	$62.3979$ /day	$(41.8066-82.9892)$ /day	Estimated
$\mu_h$	$5.1752\times10^{-5}$ /day	$(3.4674\times10^{-5}-6.8830\times10^{-5})$ /day	Estimated
$\rho_{hv}$	$0.25$ /day	$(0.072-0.64)$ /day	[23]
$\rho_{vh}$	$0.013$ /day	$(0.027-0.64)$ /day	[23]
$b$	$0.4$	$(0-1)$	variable
$\sigma_h$	$0.000017$ /day	$(5.5\times10^{-5}-1.1\times10^{-2})$ /day	[3]
$\gamma_h$	$0.083$ /day	$(0.0067-0.2)$ /day	[20]
$\tau_h$	$0.00032338$ /day	$(0.0001-0.023)$ /day	[16]
$\epsilon$	$0.5$	$(0-1)$	variable
$\delta_h$	$0.0003233$ /day	$(0.00001-0.0004)$ /day	[23,22]

| Show Table

DownLoad: CSV

3.1. Numerical simulation of the reproduction number

The time-averaged basic reproduction number ( $[\mathcal{R}_T(t)]$ ) of the model (2.1) is simulated for two different scenarios namely $T_i\neq T_o$ and $T_i = T_o$ . In , it is seen that the reproduction threshold is under-estimated when $T_i = T_o$ (i.e when the variation between indoor and outdoor conditions are not incorporated). This is may be due to the higher progression rate experienced by indoor vectors (see Figure 4) as studies have shown that the extrinsic incubation period (EIP) is highly temperature dependent and affects the basic reproduction number in an exponential manner (as it influences the number of infected mosquitoes that become infections) ^[6,24] (and other references therein).

Figure 3. Simulation of the time-averaged basic reproduction number of the model (2.1) to assess the impact indoor and outdoor temperature variation.

DownLoad: Full-Size Img PowerPoint

Figure 4. Simulations of the progression rate of exposed mosquitoes. Parameters and ranges used are as in Table 2.

DownLoad: Full-Size Img PowerPoint

3.2. Numerical Investigation of the impact of indoor and outdoor temperature variation

We now investigate the effect of variability in outdoor and indoor microclimates on the transmission dynamics of malaria. Figure 5 shows the impact of the difference between indoor and outdoor temperature on the number of infectious humans as well as the cumulative incidence. Results from Figure 5(a) show that the model under-estimates the number of infectious humans when indoor temperature is assumed to be equal to outdoor temperature. In the same vein, this finding is supported by results from Figure 5(b) when the cumulative incidence (outdoor and indoor) is used instead of the number of infectious humans.

Figure 5. Simulations of the model (2.1) to assess the impact of variation in indoor and outdoor conditions. Parameters and ranges used are as in Table 2.

DownLoad: Full-Size Img PowerPoint

3.3. Numerical Investigation of the impact of indoor and outdoor temperature variation on efficacy of controls

Investigating the effect of the differences in indoor and outdoor temperature on the efficacy $(b)$ of bed-net, it is seen from that the cumulative incidence are higher when $T_i\neq T_o$ (, and ) for the different values of $b$ than when indoor temperature is assumed to be equal to outdoor temperature i.e $T_i = T_o$ (Figures 6(b), 6(d) and 6(f)). These results therefore indicate that differences in the micro habitats where mosquitoes rest can impact on the transmission dynamics of malaria as well as efficacy of control measures.

Figure 6. Simulations of the model (2.1) to assess the impact the variation in indoor and outdoor conditions on the efficacy of control measure

$b$ . Parameters and ranges used are as in Table 2.

DownLoad: Full-Size Img PowerPoint

Again, clearly shows that the differences in indoor and outdoor environment impacts on the efficacy $(\epsilon)$ of the door and window nets. It is seen that the cumulative incidences that occur both outside and inside a human dwelling for various values of $\epsilon$ when $T_i = 25+4\cos(2\pi(t-15)/24)$ and $T_o = 24+7\cos(2\pi(t-15)/24)$ (, and ) are higher than in the case when $T_i = T_o = 24+7\cos(2\pi(t-15)/24)$ (Figures 7(b), 7(d) and 7(f)).

Figure 7. Simulation of model (2.1) to assess the impact the variation in indoor and outdoor conditions on the efficacy of control measure

$\epsilon$ . Parameters and ranges used are as in Table 2.

DownLoad: Full-Size Img PowerPoint

Additionally, we can see from Figures 6(c) and 6(d) that the use of indoor bed-nets significantly affects the outdoor dynamics. This is a pointer to how much malaria transmission intensity can be affected by indoor conditions.

Furthermore, we can observe from and that increasing $\epsilon$ leads to a decrease in the indoor cumulative incidence as well as the cumulative incidence comprising both outdoor and indoor incidences. However, there is an increase in the outdoor cumulative incidence when $\epsilon$ is increased (). This leaves us with a very interesting finding of how much the indoor environment affects the transmission intensity. So, although an increase in $\epsilon$ (a situation that does not just prevent indoor entry of mosquitoes and allow for increase in outdoor transmission intensity but also prevents the exit of indoor mosquitoes) led to an increase in the outdoor cumulative incidence, there is however a far more significant reduction in the indoor incidence that results in a decrease in total cumulative incidence (indoor and outdoor). This reduction in the total cumulative incidence may be due to the efficacy of the indoor bed nets which repel or kill indoor mosquitoes and so reduces the population of infectious vectors. It might also be as a result of the outdoor conditions which makes for a longer extrinsic incubation period (see Figure 4) and further reduces the number of infectious vectors.

Considering the cases above, we set $b = 0$ and investigate how $\epsilon$ effects the dynamics of the vector population. From and we observe that when $\epsilon = 0.9$ results in a larger vector population oudoor. However, we observe that though we have more vectors outdoor, the number of infectious vectors indoor is grater than the number of infectious vectors outdoor (Figures 8(c) and 8(d)). The faster progression rate experienced by vectors indoor (due to the different indoor microclimate) may account for this rise in the number of infectious vectors in the absence of an indoor control while the slower progression rate of the outdoor vectors account for the lower number of infectious vectors outdoor though we had more mosquitoes outdoor. Both cases are shown to be true as seen from Figures 8(e) and 8(f). Therefore, the use of the bed-net reduces though more significantly the number of infectious vectors indoors, it also reduces the number of infectious mosquitoes outdoor (Figures 8(e) and 8(f)) and thereby decreases the total population of infectious vectors. Generally, we see that if there is no indoor control, the transmission intensity would significantly increase.

Figure 8. Simulations of the model (2.1) to assess the impact the variation in indoor and outdoor conditions and the efficacy of bed-nets on the vector population. Parameters and ranges used are as in Table 2.

DownLoad: Full-Size Img PowerPoint

3.4. Numerical Investigation of the interaction between the controls

Numerical results from show the interaction between the controls. If there is an indoor control, putting more mosquitoes outdoor will result in a decrease in the number of infectious humans this is so because the a higher percentage of infectious vectors which are indoor will have contact with the bed-nets as seen in . On the other hand, if there is no indoor control, having $\epsilon = 0.1$ will result in less disease prevalence. In summary, we can say that the impact of the indoor environment on the transmission intensity is felt most in the absence of any form of indoor control.

Figure 9. Simulation of model (2.1) to assess the impact of the efficacy of control measures

$b$ and

$\epsilon$ . Parameters and ranges used are as in Table 2.

DownLoad: Full-Size Img PowerPoint

4. Discussion

A new mathematical model for the transmission dynamics of malaria in a community is designed (and rigorously analyzed) and used to assess the impact of indoor and outdoor temperature variations in a population where control measures are in place (like indoor bed-nets and door and window nets). Some of the theoretical findings are given below.

$(1)$ The autonomous version of the model (2.1) has a trivial disease free equilibrium (TDFE)(when there are no mosquitoes in the population) as well as a realistic disease free equilibrium (RDFE)(when mosquitoes are present). The trivial disease free equilibrium is globally asymptotically stable whenever the threshold $\mathcal{R}_v$ is less than unity while the realistic disease free equilibrium is locally asymptotically stable whenever the associated reproduction number is less than unity. Also, the RDFE is globally asymptotically stable in the absence of disease induced mortality for humans whenever the associated reproduction number is less than unity.

$(2)$ The model (2.1) has a globally asymptotically stable realistic disease free equilibrium in the absence of disease induced mortality for humans whenever the associated reproduction number is less than unity ( $\mathcal{R}_T(t) < 1$ ). The model (2.1) has at least a periodic solution whenever the associated reproduction number is greater than unity ( $\mathcal{R}_T(t) > 1$ ). In this case, the disease persist.

Results from the numerical simulations of the model (2.1) are given below.

$(1)$ When the variation of the indoor and outdoor temperatures are taken into consideration, i.e. $T_o = 24+6\cos(2\pi(t-15)/24)$ and $T_i = 23+3\cos(2\pi(t-15)/24)$ , the bed-net efficacy needed to bring the time averaged basic reproduction number $[\mathcal{R}_T(t)]$ below unity is greater than when $T_i = T_o = 24+6\cos(2\pi(t-15)/24)$ . Also, having a 100% bed-net efficacy $(b)$ results in 58.69% reduction in the time averaged basic reproduction number $[\mathcal{R}_T(t)]$ when the variation of the indoor and outdoor temperatures are taken into consideration. However, if indoor and outdoor temperatures are assumed to be the same, having a 100% bed-net efficacy results in 61.93% reduction. This shows that the differences in indoor and outdoor conditions impacts on the efficacy of the bed-nets and hence on malaria transmission.

It is interesting to state that Paaijmans and Thomas ^[27], reported that small differences in indoor and outdoor temperatures can have significant impact on the length of the (EIP) and consequently on the basic reproduction number as the EIP is one of the most influential parameters that determines disease reproduction threshold. Clearly our results support this finding reported in ^[27] as seen from Figures 3 and 4. Therefore, Thomas et al. ^[35] concluded that since the actual microclimates experienced by mosquitoes in different microhabitants play a significant role in most mosquito and parasite life history traits, appropriate characterization of the local microclimate conditions is important in understanding transmission intensity.

$(2)$ When indoor temperature is assumed to be the same as outdoor temperature, the model underestimates the number of infectious humans as well the cumulative incidence of the disease. This again strongly agrees with the results in ^[27] which reported that better knowledge of endophilic and exophilic behaviours of mosquitoes (resting behaviour) and the associated microclimate is needed to fully understand malaria transmission intensity. This study (^[27]) stated that differences in microclimate of places where mosquitoes rest translate to increases in transmission risk. Furthermore, it was reported in ^[28] that models that use outdoor air temperatures only will underestimate the speed of processes such as parasite development, blood meal digestion and egg-production of endophilic mosquitoes.

$(3)$ In the absence of an indoor control measure having $\epsilon = 0.1$ (a conditions that allows for higher movement rate of mosquitoes in and out of a human dwelling) may be more helpful. However, when we an indoor control measure restricting vector movement (i.e. having $\epsilon = 0.9$ ) may be of a better advantage. This may be as a result of the different temperature conditions experienced by the vectors in the different micro niches as they move in and out of a human dwelling since temperature has been shown to altar the length of the extrinsic incubation period (EIP). This study may be pointing to the fact that both the mosquito resting behaviour and how long it rest there may determine the transmission intensity. This may be due to the fact that having $\epsilon = 0.9$ does not just prevent indoor entry but also prevents exit of indoor vectors so vectors are confined to a particular microclimate for a longer period. When $\epsilon = 0.1$ the movement rate ( $\alpha$ and $\rho$ ) are higher and so vectors are exposed to variable microclimate from time to time as they move in and out of a human dwelling. Therefore, if mosquitoes spend a greater parts of their adult life resting indoors (in a population without any form of indoor control measures), this may lead to a considerable increase in transmission risk as ^[27] reported that that mosquitoes that rest indoor could transmit malaria between 0.3 and 22.5 days earlier than outdoor-resting counterparts.

5. Conclusion

This study has shown the significance of including the variation between outdoor and indoor temperatures on the dynamics of malaria in a given population as the difference between indoor and outdoor temperatures is expected to alter temperature-related estimates of transmission intensity. This agrees with the findings in ^[28] where indoor and outdoor temperature data from a study carried out in Tanzania were used to assess the effects of these different microclimate on the extrinsic incubation period of the parasite as well as the gonotrophic cycle length of mosquitoes. This study has confirmed that warmer indoor temperatures result in faster parasite development as well as leads to an increase in the transmission intensity. Also, both where the mosquitoes rest and how long they rest there may determine the the population of the infectious vectors and thus the transmission intensity.

In this work, the variations in indoor temperature due to house design and construction materials and relative humidity were not considered. However, since indoor temperature has been shown to vary considerably depending on house design, construction materials, housing density, adjacent vegetation cover and altitude as noted in ^[27,35], it would be interesting to study the impact of this on malaria dynamics. Moreover, it would be interesting to study the combined impact of microclimate variables like temperature and relative humidity on the transmission dynamics of malaria.

Acknowledgments

We would like to thank the anonymous reviewers for their constructive comments.

Conflict of interest

There are no conflict of interests.

Appendix A:. Verification of assumptions $A1-A7$ in ^[37]

Verification of the Assumptions A1-A7 in ^[37,4]. Following ^[31] and using the notation in ^[37], the model (2.1) can be written as:

$\frac{d}{dt}x(t) = \mathcal{F}(t,x(t))-\mathcal{V}(t,x(t)) = f(t,x(t)),$

where,

$\begin{eqnarray*} x = \left( \begin{array}{c} S_h(t) \\ E_h(t) \\ I_h(t) \\ R_h(t) \\ A_m(t) \\ S_{vo}(t) \\ S_{vi}(t) \\ E_{vo}(t) \\ E_{vi}(t) \\ I_{vo}(t) \\ I_{vi}(t) \\ \end{array} \right),\qquad\mathcal{F} = \left( \begin{array}{c} 0 \\ (\lambda_{ho}(t)+\lambda_{hi}(t))S_h(t) \\ \gamma_h E_h(t) \\ 0 \\ 0 \\ 0 \\ 0 \\ \lambda_{vo}(t)S_{vo}(t) \\ \lambda_{vi}(t)S_{vi}(t)\\ \gamma_{vo} E_{vo}(t) \\ \gamma_{vi} E_{vi}(t) \\ \end{array} \right), \end{eqnarray*}$

and

$\begin{eqnarray*} \mathcal{V} = \mathcal{V}^–\mathcal{V}^+ = \left( \begin{array}{c} -\Lambda_h+\lambda_{ho}S_h+\lambda_{hi}S_h+\mu_h S_h-\sigma_h R_h \\ k_1 E_h(t) \\ k_2 I_h(t) \\ -\tau_h I_h(t)+k_3 R_h(t) \\ -\phi_v(t)(1-\frac{A_m(t)}{k_v(t)})(S_{vo}+S_{vi}+E_{vo}+E_{vi}+I_{vo}+I_{vi})+k_4 A_m(t) \\ -\gamma_a A_m(t)+\lambda_{vo}(t)S_{vo}(t)-\rho(t)(1-\epsilon)S_{vi}(t)+k_5 S_{vo}(t) \\ -\alpha(t)(1-\epsilon)S_{vo}(t)+\lambda_{vi}(t)S_{vi}(t)+k_6 S_{vi}(t) \\ -\rho(t)(1-\epsilon)E_{vi}(t)+k_7 E_{vo}(t) \\ -\alpha(t)(1-\epsilon)E_{vo}(t)+k_{8} E_{vi}(t) \\ -\rho(t)(1-\epsilon)I_{vi}(t)+k_5 I_{vo}(t) \\ -\alpha(t)(1-\epsilon)I_{vo}(t)+k_6 I_{vi}(t) \\ \end{array} \right). \end{eqnarray*}$

The functions $\mathcal{F}$ , $\mathcal{V}^-$ and $\mathcal{V}^+$ satisfy the following conditions in ^[37].

(A1) For each $1\leq i\leq11$ , $\mathcal{F}_i(t, x)$ , $\mathcal{V}_i^+(t, x)$ and $\mathcal{V}_i^-(t, x)$ are non-negative, continuous on $\mathbb{R}\times\mathbb{R}^{11}_+$ and continuously differentiable with respect to $x$ .

(A2) There is a real number $\omega > 0$ such that for each $1\leq i\leq = 11$ , the functions $\mathcal{F}_i(t, x)$ , $\mathcal{V}^+_i(t, x)$ and $\mathcal{V}_i^-(t, x)$ are $\tau$ -periodic in $t$ .

(A3) If $x_i = 0$ , then $\mathcal{V}_i^- = 0$ for $i = 2, 3, 4, 8, 9, 10, 11$

(A4) $\mathcal{F}_i = 0$ for $i = 1, 5, 6, 7.$

(A5) Define $X_s = {x\geq0:x_i = 0\quad for\quad i = 2, 3, 4, 8, 9, 10, 11}$ . It is clear that if $x\in X_s$ , then $\mathcal{F}_i = \mathcal{V}_i^+ = 0$ for $i = 2, 3, 4, 8, 9, 10, 11$ . The model (2.1) has RDFE given by $\mathcal{E}_{0N} = (S_h^*, 0, 0, 0, A_m^*, S_{vo}^*, S_{vi}^*, 0, 0, 0, 0)$ . Define a $5\times5$ matrix

$M(t) = \left( \begin{array}{*{1}c} \frac{\partial f_i(t,x^*)}{\partial x_j}\\ \end{array} \right)_{i,j = 1,4,5,6,7}.$

It follows from ^[31], and the definitions of the matrices $\mathcal{F}$ and $\mathcal{V}$ , that

$\begin{eqnarray*} M(t) = \left( \begin{array}{*{7}c} -\mu_h&\sigma_h&0&0&0\\ 0&-k_3&0&0&0\\ 0&0&-\phi_v(t)\frac{1}{k_v(t)}(S^*_{vo}+S^*_{vi})-k_4&\phi_v(t)(1-\frac{A_m^*(t)}{k_v(t)})&\phi_v(t)(1-\frac{A_m^*(t)}{k_v(t)})\\ 0&0&\gamma_a(t)&-k_5&\rho(t)(1-\epsilon)\\ 0&0&0&\alpha(t)(1-\epsilon)&-k_6\\ \end{array} \right) \end{eqnarray*}$

(A6) Since $M(t)$ is a diagonalize matrix with negative eigenvalues, then $\rho(\Phi_M(\tau)) < 1$ .

(A7) Similarly, $-\mathcal{V}(t)$ is a diagonalize matrix with negative eigenvalues. Hence, $\rho(\Phi_{-v}(\tau)) < 1$ .

Therefore, the model (2.1) satisfies the conditions $A1-A7$ in ^[37].

Appendix B:. Proof of Theorem 2.5

Consider the model (2.1) where $\delta_h = 0$ with $\mathcal{R}_v(t) > 1$ for all $t\geq0$ . Let $\mathcal{R}_T^m(t) < 1$ . The proof is based on the comparison theorem ^[34]. Using the fact that $S_h(t)\leq\frac{\Lambda_h}{\mu_h}$ , $A_m(t)\leq k_v(t)(1-\frac{1}{\mathcal{R}_v(t)})$ , $S_{vo}(t)\leq \frac{k_v(t)\gamma_a(t)k_6}{k_5 k_6-\alpha\rho(1-\epsilon)^2)}(1-\frac{1}{\mathcal{R}_v(t)})$ and $S_{vi}(t)\leq \frac{k_v(t)\gamma_a(t)\alpha(t)(1-\epsilon)}{k_5 k_6-\alpha\rho(1-\epsilon)^2)}(1-\frac{1}{\mathcal{R}_v(t)})$ , for all $t\geq0$ in $C([0], \mathbb{R}^{11}_+)\setminus{\mathcal{T}_o}$ . We can then re-write the non-autonomous model (2.1) as

$\begin{split} \frac{d E_h}{dt}&\leq \rho_{vh}\beta_{o}(t)I_{vo}+\rho_{vh}\beta_{i}(t,b)I_{vi}-(\gamma_h+\mu_h)E_h,\\ \frac{d I_h}{d t}& = \gamma_h E_h-(\tau_h+\mu_h)I_h,\quad \frac{d R_h}{d t} = \tau_h I_h-(\sigma_h+\mu_h)R_h,\\ \frac{d E_{vo}}{d t}&\leq\frac{\rho_{hv}\beta_o(t)\mu_h I_h}{\Lambda_h}\frac{k_v(t)\gamma_a(t)k_6}{k_5 k_6-\alpha\rho(1-\epsilon)^2)}(1-\frac{1}{\mathcal{R}_v(t)})+\rho(t)(1-\epsilon)E_{vi}-k_7 E_{vo},\\ \frac{d E_{vi}}{d t}&\leq\frac{\rho_{hv}\beta_i(t,b)\mu_h I_h}{\Lambda_h}\frac{k_v(t)\gamma_a(t)\alpha(t)(1-\epsilon)}{k_5 k_6-\alpha\rho(1-\epsilon)^2)}(1-\frac{1}{\mathcal{R}_v(t)})+\alpha(t)(1-\epsilon)E_{vo}-k_8 E_{vi},\\ \frac{d I_{vo}}{d t}& = \gamma_{vo}(t)E_{vo}+\rho(t)(1-\epsilon)I_{vi}-k_5 I_{vo},\quad \frac{d I_{vi}}{d t} = \gamma_{vi}(t)E_{vi}+\alpha(t)(1-\epsilon)I_{vo}-k_6 I_{vi}.\\ \end{split}$

The equations with equalities used in place of inequalities can be written in terms of the next generation matrices $\mathcal{F}(t)$ and $\mathcal{V}(t)$ following ^[37]

$\begin{equation} \frac{d W(t)}{d t} = [\mathcal{F}(t)-\mathcal{V}(t)]W(t) \end{equation}$

(5.1)

There exist a positive $\tau$ -periodic function $w(t) = (E_h(t), I_h(t), E_{vo}(t), E_{vi}(t), I_{vo}(t), I_{vi}(t))$ , (following lemma 2.1 in ^[41]) such that $W(t) = \exp^{\theta t}w(t)$ with $\theta = \frac{1}{\tau}\ln\rho[\phi_{\mathcal{F}-\mathcal{V}}(\tau)]$ is a solution of the linearized system (5.1). Furthermore, the assumption that $\mathcal{R}_T^m(t) < 1$ implies that $\rho[\phi_{\mathcal{F}-\mathcal{V}}(\tau)] < 1$ . Hence, $\theta$ is a negative constant. Thus, $W(t)\rightarrow0$ as $t\rightarrow\infty$ .

The unique realistic disease free solution of the linear system (9.1) given by $W(t) = 0$ , is GAS. For any non-negative initial condition $(E_h(0), I_h(0), E_{vo}(0), E_{vi}(0), I_{vo}(0), I_{vi}(0))$ of the system (9.1) there exists a sufficiently large $M^* > 0$ such that

$((E_h, I_h, E_{vo}, E_{vi}, I_{vo}, I_{vi})(0))^T\leq M^*((E_h, I_h, E_{vo}, E_{vi}, I_{vo}, I_{vi})(0))$

Thus, it follows by comparison theorem that $(E_h(t), I_h(t), E_{vo}(t), E_{vi}(t), I_{vo}(t), I_{vi}(t))\leq M^*W(t)$ for all $t > 0$ where $M^*W(t)$ is also a solution of the model (5.1). Hence,

$((E_h(t), I_h(t), E_{vo}(t), E_{vi}(t), I_{vo}(t), I_{vi}(t)))\rightarrow(0, 0, 0, 0, 0, 0)$ as $t\rightarrow\infty$ .

It also follows that $S_h(t)\rightarrow\frac{\Lambda_h}{\mu_h}$ as $t\rightarrow\infty$ and $(A_m(t), S_{vo}(t), S_{vi}(t))$ satisfy for ( $\mathcal{R}_v(t) > 1$ for all $t$ )

$\begin{split} \dot{A}_m(t)& = \phi_v(t)(1-\frac{A_m(t)}{k_v})(S_{vo}(t)+S_{vi}(t))-k_4 A_m(t),\\ \dot{S}_{vo}(t)& = \gamma_a(t)A_m(t)+\rho(t)(1-\epsilon)S_{vi}(t)-k_5 S_{vo}(t)\\ \dot{S}_{vi}(t)& = \alpha(t)(1-\epsilon)S_{vo}(t)-k_6S_{vi}(t).\\ \end{split}$

Thus for $\mathcal{R}_T^m(t) < 1$ , $(S_h, E_h, I_h, R_h, A_m, S_{vo}, S_{vi}, E_{vo}, E_{vi}, I_{vo}, I_{vi})\rightarrow \mathcal{E}_{0N}$ as $t\rightarrow\infty$

Appendix C:. Proof of Theorem 2.6

Consider the non-autonomous model (2.1) with $\mathcal{R}_v(t) > 1$ and $\mathcal{R}_T(t) > 1$ for all $t\geq0$ . Both conditions are needed to ensure that mosquitoes are present in the population and that the realistic disease free solution is unstable. The proof of Theorem 2.6 is based on using the technique of in ^[16]. Define the sets

$\begin{split} X& = C([0],\mathbb{R}^{11}_+),\\ X_0& = \{\phi = (\phi_1,\phi_2,\phi_3,\phi_4,\phi_5,\phi_6,\phi_7,\phi_8,\phi_9,\phi_{10},\phi_{11})\in X:\phi_i(0) \gt 0\\ &\quad \forall i\in\{2,3,4,8,9,10,11\}\}.\\ \partial X_0& = X\backslash X_0 = \{\phi\in X:\phi_i(0) = 0\quad for\quad some\quad i\in \{2,3,4,8,9,10,11\}\}\\ \end{split}$

Let $u(t, \phi)$ be the unique solution of the model (2.1) (through the initial condition $u(0, \phi) = \phi$ ). Define $\Phi(t)\varphi = u(t, \varphi)$ , the flow generated by the model (2.1) with respect to $\varphi$ .

Let $P:X\rightarrow X$ be the poincar $\acute{e}$ map associated with the model (2.1). That is $P(\phi) = u(\tau, \phi)$ for all $\phi\in X$ . Then using the approach in the proof of lemma 2.1 in ^[16], it can be shown that $X_0$ is a positively invariant and compact set with respect to the model (2.1). Since the model's solutions are uniformly bounded, it follows that $P$ is point-dissipative. ^[16,23]. Furthermore, it follows from theorem 1.1.2 in ^[42] that in $X$ , $P$ admits a global attractor.

Next, we show that $P$ is uniformly persistent with respect to ( $X_0$ , $\partial X_0$ ). It is convenient to define where $P^n(\phi), n\geq0$ , are the periodic points of the poincar $\acute{e}$ map ^[16]:

$\begin{equation} \begin{split} K_\partial& = \{\phi\in\partial X_0:P^n(\phi)\in\partial X_0, n\geq 0\},\\ D_1& = \{\phi\in X:\phi_i(0) = 0 \quad \text{for all} i\in\{5,6,7,8,9,10,11\}\},\\ D_2& = \{\phi\in X:\phi_i(0) = 0 \quad \text{for all} i\in\{2,3,4,8,9,10,11\}\}.\\ \end{split} \end{equation}$

(5.2)

It follows from (5.2) that

$\begin{equation} \begin{split} D_1\cup D_2& = \{\phi\in X:\phi_i(0) = 0 \quad \text{for all}\quad i\in\{5,6,7,8,9,10,11\}\}\quad or \quad\phi_i(0) = 0 \quad \text{for all}\\&\quad i = \{2,3,4,8,9,10,11\}\},\\ \partial X_0\setminus (D_1\cup D_2)& = \{\phi\in X:\phi_i(0)\geq0 \quad \text{for some} \quad i\in\{2,3,4,8,9,10,11\}\}.\\ \end{split} \end{equation}$

(5.3)

In the case where $0$ is a solution, of the equation (2.10) for the total mosquito population $N_v^*(t)$ . We claim the following

Lemma 5.1. $K_\partial = D_1\cup D_2$ .

Proof. We can define the set $K_\partial$ and $D_1\cup D_2$ as given below

$\begin{equation} \begin{split} K_\partial = \{(&S_h(0), E_h(0), I_h(0), R_h(0), A_m(0) S_{vo}(0), S_{vi}(0), E_{vo}(0), E_{vi}(0), I_{vo}(0), I_{vi}(0))\in\partial X_0:\\ P^n(S_h(0),&\quad E_h(0), I_h(0), R_h(0), A_m(0) S_{vo}(0), S_{vi}(0), E_{vo}(0), E_{vi}(0), I_{vo}(0), I_{vi}(0))\in\partial X_0, n\geq 0\}\\ D_1\cup D_2& = \{(\frac{\Lambda_h}{\mu_h}, 0,0,0,A_m^*, S_{vo}^*, S_{vi}^*, 0, 0, 0, 0) :\frac{\Lambda_h}{\mu_h} \gt 0,A_m^* \gt 0, S_{vo}^* \gt 0, S_{vi}^* \gt 0\} \end{split} \end{equation}$

(5.4)

By the definition of $\partial X_0$ , $\{(\frac{\Lambda_h}{\mu_h}, 0, 0, 0, A_m^*, S_{vo}^*, S_{vi}^*, 0, 0, 0, 0):\frac{\Lambda_h}{\mu_h} > 0, S_{vs} > 0, S_{vr} > 0\}\subset K_\partial$ . Therefore, $D_1\cup D_2\subset K_\partial$ .

Let $(S_h(0), E_h(0), I_h(0), R_h(0), A_m(0), S_{vo}(0), S_{vi}(0), E_{vo}(0), E_{vi}(0), I_{vo}(0), I_{vi}(0))\in \partial X_0\backslash D_1\cup D_2$ .

If $E_h(0) = 0$ , $I_h(0) = 0$ , $R_h(0) = 0$ , $E_{vo}(0) = 0$ , $E_{vi}(0) = 0$ , $I_{vo}(0) > 0$ and $I_{vi}(0) > 0$ , then $S_h(0) > 0$ , $S_{vo}(0) > 0$ , $S_{vi}(0) > 0$ , $I_{vo}(0) > 0$ and $I_{vi}(0) > 0$ .

It follows from the second equation in (2.1) that

$\begin{split} E_h^\prime(0)& \gt \rho_{vh}(\beta_{o}(t)I_{vo}(0)+\beta_{i}(t,b)I_{vi}(0))\frac{S_h(0)}{N_h(0)} \gt 0,\quad I_h^\prime(0) \gt \gamma_h E_h(0) \gt 0,\\ R_h^\prime(0)& \gt \tau_h I_h(0) \gt 0, \quad E_{vo}^\prime(0) \gt \rho_{hv}\beta_{o}(t)I_h(0)S_{vo}(0)+\rho(t)(1-\epsilon)E_{vi}(0) \gt 0,\\ E_{vi}^\prime(0)& \gt \rho_{hv}\beta_{i}(t,b)I_h(0)S_{vi}(0)+\alpha(t)(1-\epsilon)E_{vo} \gt 0,\\ I_{vo}^\prime(0)& \gt \gamma_{vo} E_{vo}(0)+\rho(t)(1-\epsilon)I_{vi}(0) \gt 0\quad \text{and} \quad I_{vi}^\prime(0) \gt \gamma_{vi} E_{vi}(0)+\alpha(t)(1-\epsilon)I_{vo} \gt 0.\\ \end{split}$

Similarly, the above result holds for other cases such as $E_h(0) > 0$ , $I_h(0) = 0$ , $R_h(0) = 0$ , $E_{vo}(0) > 0$ , $E_{vi}(0) > 0$ , $I_{vo}(0) = 0$ and $I_{vi}(0) = 0$ , then $S_h(0) > 0$ , $A_m(0)$ , $S_{vo}(0) > 0$ , $S_{vi}(0) > 0$ , $E_h(0) > 0$ , $E_{vo}(0) > 0$ and $E_{vi}(0) > 0$ .

Therefore, $(S_h(0), E_h(0), I_h(0), R_h(0), A_m(0), S_{vo}(0), S_{vi}(0), E_{vo}(0), E_{vi}(0), I_{vo}(0), I_{vi}(0))\not \in \partial X_0$ for all $0 < t\ll1$ .

Hence, $K_\partial\subset D_1\cup D_2$ . Thus, it then follows that $K_\partial = D_1\cup D_2$ .

From 5.3, it can be verified that $P^n(\phi)$ , $n\geq0$ contains two disease free states namely $\mathcal{T}_{0}$ and $\mathcal{E}_{0N}$ . The sets $\mathcal{T}_{0}$ and $\mathcal{E}_{0N}$ disjoint, compact, and isolated invariant sets for the poincar $\acute{e}$ map $P$ in $K_\partial$ and $\bigcup_{\phi\in K_\partial}\omega(\phi) = \{\mathcal{T}_{0}, \mathcal{E}_{0N}\}$ ^[16]. No subset of { $\mathcal{T}_{0}$ , $\mathcal{E}_{0N}$ } forms a cycle of in $K_\partial$ and hence in $\partial X_0$ ^[16]. In addition, it follows from the proof of Theorem 3.2 in ^[16] that since $N_v^*(t)$ is a positive periodic solution with respect to $X_0$ then, there exist a $\delta > 0$ and an $\epsilon > 0$ such that $\lim_{t\rightarrow\infty}\sup|\Phi(n\tau)\phi-\mathcal{T}_{0}|\geq\delta$ and $\lim_{t\rightarrow\infty}\sup|\Phi(n\tau)\phi-\mathcal{E}_{0N}|\geq\epsilon$ for all $\phi\in X_0$ .

Define the sets $A_1: = \mathcal{T}_{0}$ and $A_2: = \mathcal{E}_{0N}$ . In view of the claims above, it follows that $A_1$ and $A_2$ are isolated invariant sets for $P$ in $X$ , and $W^s(A_i)\cap X_0 = \varnothing$ , for all $i = 1, 2$ where $W^s(A_i)$ is the stable set of $A_i$ for $P$ ^[16]. In the case where $0$ is not a solution of the equation (2.10), we can show that $K_\partial = D_2$ in a similar manner. It then follows that ${A_2}$ is the only compact invariant set for $P$ in $K_\partial$ ^[16].

Hence, every solution in $K_\partial$ converges to either $A_1$ or $A_2$ and ${A_1}$ or ${A_2}$ are acyclic in $K_\partial$ ^[42]. It then follows from Theorem 1.3.1 in ^[42] that $P$ is uniformly persistent with respect to $X_0$ . Thus, from Theorem 3.1.1 in ^[42] the periodic semiflow $\Phi(t):X\rightarrow X$ is also uniformly-persistent to $X$ ^[16] where $\Phi(t)\varphi = u(t, \varphi)$ . It then follows from Theorem 4.5 in ^[17] that the non-autonomous model (2.1) has a positive periodic solution denoted by $\mathcal{E}^*_N(t) = \Phi(t)\phi$ with $\phi\in X_0$ .

It again follows from Theorem 4.5 in ^[17] that $P:X_0\rightarrow X_0$ has a compact global attractor, denoted by $\mathcal{A}_0$ . Hence, $\mathcal{A}_0$ is invariant for $P$ (that is $\mathcal{A}_0 = P(\mathcal{A}_0) = \Phi(\tau)\mathcal{A}_0$ ). Also, using the notation in ^[43], let $\mathcal{A}^*_0: = \bigcup_{t\in [0, \tau]}\Phi(t)\mathcal{A}_0$ . Then, $\psi_i(0) > 0$ for all $\psi\in \mathcal{A}^*_0, \quad i\in[1, 11]$ ^[16]. Since $\Phi(t)\phi\in X_0$ , for all $t\geq0$ and $\phi\in X_0$ (as $X_0$ is invariant), it follows that $\Phi(t)X_0\subset X_0$ . Thus, $\mathcal{A}^*_0\subset X_0$ and $\limsup_{t\rightarrow\infty}d(\Phi(t)\phi, \mathcal{A}^*_0) = 0$ for all $\phi\in X_0$ ^[16,43]. Also, it follows from the continuity of $\Phi(t)\phi$ for all $(t, \phi)\in [0, \infty)\times X_0$ and the compactness of $[0, \tau]\times\mathcal{A}_0$ ^[43], that $\mathcal{A}^*_0$ is compact in $X_0$ ^[16,43]. Thus, $\inf_{\phi\in\mathcal{A}^*_0}d(\phi, \partial X_0) > 0$ ^[16,43]. Consequently, there exist $q > 0$ such that

$\begin{split} \liminf\limits_{t\rightarrow\infty}\min(S_h(t,\phi),E_h(t,\phi),I_h(t,\phi),R_h(t,\phi), A_m(t,\phi), S_{vo}(t,\phi), S_{vi}(t,\phi),\\ E_{vo}(t,\phi), E_{vi}(t,\phi), I_{vo}(t,\phi), I_{vi}(t,\phi)) = \liminf\limits_{t\rightarrow\infty}d(\phi,\partial X_0)\geq q, \quad \text{for all} \quad \phi\in X_0\\ \end{split}$

In particular, $\liminf_{t\rightarrow\infty}\min(\Phi(t)\phi^*)\geq q$ , and hence, $u_i(t, \phi) > 0$ , $1\leq i\leq11$ for all $t\geq0$ .

References

[1]	G. J. Abiodun, R. Maharaj, P. Witbooi, et al., Modelling the influence of temperature and rainfall on the population dynamics of anopheles arabiensis, Malaria J., 15 (2016), 364.
[2]	Y. A. Afrane, B.W. Lawson, A. K. Githeko, et al., Effects of microclimatic changes caused by land use and land cover on duration of gonotrophic cycles of anopheles gambiae (Diptera: Culicidae) in western Kenya highlands, J. Med. Entomol., 42 (2005), 974–980.
[3]	F. B. Agusto, A. B. Gumel and P. E. Parham, Qualitative assessment of the role of temperature variation on malaria transmission dynamics, J. Biol. Syst., 24 (2015), 1–34.
[4]	N. Bacaer, Approximation of the basic reproduction number Ro for vector-borne diseases with a periodic vector population, B. Math. Biol., 69 (2007), 1067–1091.
[5]	L. M. Beck-Johnson, W. A. Nelson, K. P. Paaijmans, et al., The importance of temperature fluctuations in understanding mosquito population dynamics and malaria risk, Roy. Soc. Open Sci., 4 (2017). Available from :http://dx.doi.org/10.1098/rsos.160969.
[6]	J. I. Blanford, S. Blanford, R. G. Crane, et al., Implications of temperature variation for malaria parasite development across Africa, Sci. Rep., 3 (2013), 1300.
[7]	P. Cailly, A. Tran, T. Balenghien, et al., A climate-driven abundance model to assess mosquito control strategies, Ecol. Model., 227 (2012), 7–17.
[8]	C. Christiansen-Jucht, K. Erguler, C. Y. Shek, et al., Modelling anopheles gambiae s.s. population dynamics with temperature and age-dependent survival, Int. J. Env. Res. Pub. He., 12 (2015), 5975–6005.
[9]	O. Diekmann, J. Heesterbeek and J. Metz, On the definition and the computation of the basic reproduction ratio R0 in models for infectious diseases in heterogeneous populations, J. Math. Biol., 28 (1990), 365–382.
[10]	Y. Dumont and F. Chiroleu, Vector control for the chikungunya disease, Math. Biosci. Eng., 7 (2010), 105–111.
[11]	A. Egbendewe-Mondzozo, M. Musumba, B. A. McCarl, et al., Climate change and vector-borne diseases: an economic impact analysis of malaria in Africa, Int. J. Env. Res. Pub. He., 8 (2011), 913–930.
[12]	S. M. Garba, A. B. Gumel and M. R. A. Bakar, Backward bifurcations in dengue transmission dynamics, Math. Biosci., 215 (2008), 11–25.
[13]	A. B. Gumel, Causes of backward bifurcation in some epidemiological models, J. Math. Anal. Appl., 395 (2012), 355–365.
[14]	V. Lakshmikantham and S. Leela, Differential and Integral Inequalities: Theory and Applications, Academic Press, New York, 1969.
[15]	J. La Salle and S. Lefschetz, The stability of dynamical systems, SIAM, Philadephia, 1976.
[16]	Y. Lou and X. Q. Zhao, A climate-based malaria transmission model with structured vector population, SIAM J. Appl. Math., 70 (2010), 2023–2044.
[17]	P. Magal and X. Q. Zhao, Global attractors and steady states for uniformly persistent dynamical systems, SIAM J. Math. Anal., 37 (2005), 251–275.
[18]	E. A. Mordecai, Optimal temperature for malaria transmission is dramatically lower than previously predicted, Ecol. Lett., 16 (2013), 22–30.
[19]	E. T. Ngarakana-Gwasira, C. P. Bhunu, M. Masocha, et al., Assessing the role of climate change in malaria transmission in Africa, Malaria Res. Treat., 1 (2016), 1–7.
[20]	C. N. Ngonghala, S. Y. Del Valle, R. Zhao, et al., Quantifying the impact of decay in bed-net efficacy on malaria transmission, J. Theor. Biol., 363 (2014), 247–261.
[21]	H. S. Ngowo, E. W. Kaindoa, J. Matthiopoulos, et al., Variations in household microclimate affect outdoor-biting behaviour of malaria vectors, Wellcome Open Research, 2 (2017).
[22]	A. M. Niger and A. B. Gumel, Mathematical analysis of the role of repeated exposure on malaria transmission dynamics, Diff. Equa. Dyn. Syst., 16 (2008), 251–287.
[23]	K. Okuneye and A. B. Gumel, Analysis of a temperature- and rainfall-dependent model for malaria transmission dynamics, Math. Biosci., 287 (2017), 72–92.
[24]	K. P. Paaijmans, A. F. Read and M. B. Thomas, Understanding the link between malaria risk and climate, P. Natl. Acad. Sci. USA, 106 (2009), 13844–13849.
[25]	K. P. Paaijmans, S. Blanford, A. S. Bell, et al., Influence of climate on malaria transmission depends on daily temperature variation, P. Natl. Acad. Sci. USA, 107 (2010), 15135–15139.
[26]	K. P. Paaijmans, S. S. Imbahale, M. B. Thomas, et al., Relevant microclimate for determining thedevelopment rate of malaria mosquitoes and possible implications of climate change, Malaria J., 9 (2010), 196.
[27]	K. P. Paaijmans and M. B. Thomas, The influence of mosquito resting behaviour and associated microclimate for malaria risk, Malaria J., 10 (2011), 183.
[28]	K. P. Paaijmans and M. B. Thomas, Relevant temperatures in mosquito and malaria biology, In: Ecology of parasite-vector interactions, Wageningen Academic Publishers, 2013.
[29]	P. E. Parham and E. Michael, Modeling the effects of weather and climate change on malaria transmission, Environ. Health Persp., 118 (2010), 620–626.
[30]	D. J. Rogers and S. E. Randolph, Advances in Parasitology, Elsevier Academic Inc, San Diego, 2006.
[31]	M. A. Safi, M. Imran and A. B. Gumel, Threshold dynamics of a non-autonomous SEIRS model with quarantine and isolation, Theor. Biosci., 131 (2012), 19–30.
[32]	L. L. M. Shapiro, S. A. Whitehead and M. B. Thomas, Quantifying the effects of temperature on mosquito and parasite traits that determine the transmission potential of human malaria, PLoS Biol., 15 (2017), e2003489.
[33]	P. Singh, Y. Yadav, S. Saraswat, et al., Intricacies of using temperature of different niches for assessing impact on malaria transmission, Indian J. Med. Res., 144 (2016), 67–75.
[34]	H. L. Smith, Monotone dynamical systems: an introduction to the theory of competitive and cooperative systems, Am. Math. Soc., 41, 1995.
[35]	S. Thomas, S. Ravishankaran, N. A. J. Amala Justin, et al., Microclimate variables of the ambient environment deliver the actual estimates of the extrinsic incubation period of plasmodium vivax and plasmodium falciparum: a study from a malaria endemic urban setting, Chennai in India, Malaria J., 17 (2018), 201.
[36]	P. Van den Driessche and J. Watmough, Reproduction numbers and sub-threshold endemic equilibria for compartmental models of disease transmission, Math. Biosci., 180 (2002), 29–48.
[37]	W. Wang and X. Q. Zhao, Threshold dynamics for compartmental epidemic models in periodic environments, J. Dyn. Differ. Equations, 20 (2008), 699–717.
[38]	Malaria Report, from World Health Organization, 2010. Available from: www.who.int/ mediacenter/factsheets/fs094/en/.
[39]	World Malaria Day, Report of the World Health Organisation (WHO), 2018. Available from: www.who.int/malaria/media/world-malaria-day-2018/en/.
[40]	H. Zhang, P. Georgescu and A. S. Hassan, Mathematical insights and integrated strategies for the control of Aedes aegypti mosquito, Appl. Math. Comput., 273 (2016), 1059–1089.
[41]	F. Zhang and X. Q. Zhao, A periodic epidemic model in a patchy environment, J. Math. Anal. Appl., 325 (2007), 496–516.
[42]	X. Q. Zhao, Dynamical systems in population biology, Springer, New York, 2003.
[43]	X. Q. Zhao, Uniform persistence and periodic co-existence states in infinite-dimensional periodic semiflows with applications, Can. Appl. Math. Q., 3 (1995), 473–495.

This article has been cited by:

1.	A. Nwankwo, Quantifying the impact of insecticide resistance in the transmission dynamics of malaria, 2021, 142, 09600779, 110481, 10.1016/j.chaos.2020.110481
2.	Mahmoud A. Ibrahim, Attila Dénes, Threshold and stability results in a periodic model for malaria transmission with partial immunity in humans, 2021, 392, 00963003, 125711, 10.1016/j.amc.2020.125711
3.	Ramsés Djidjou‐Demasse, Gbenga J. Abiodun, Abiodun M. Adeola, Joel O. Botai, Development and analysis of a malaria transmission mathematical model with seasonal mosquito life‐history traits, 2020, 144, 0022-2526, 389, 10.1111/sapm.12296
4.	Temidayo Oluwafemi, Emmanuel Azuaba, Impact of Hygiene on Malaria Transmission Dynamics: A Mathematical Model, 2022, 2, 2774-3047, 1, 10.47352/jmans.2774-3047.97
5.	Temesgen Duressa Keno, Legesse Lemecha Obsu, Oluwole Daniel Makinde, Modeling and optimal control analysis of malaria epidemic in the presence of temperature variability, 2022, 15, 1793-5571, 10.1142/S179355712250005X
6.	Temesgen Duressa Keno, Lemesa Bedjisa Dano, Gamachu Adugna Ganati, Kenan Yildirim, Optimal Control and Cost-Effectiveness Strategies of Malaria Transmission with Impact of Climate Variability, 2022, 2022, 2314-4785, 1, 10.1155/2022/5924549
7.	Temesgen Duressa Keno, Lemessa Bedjisa Dano, Oluwole Daniel Makinde, Suresh Rasappan, Modeling and Optimal Control Analysis for Malaria Transmission with Role of Climate Variability, 2022, 2022, 2577-7408, 1, 10.1155/2022/9667396
8.	Emmanuel Chidiebere Duru, Godwin C.E. Mbah, Approximate solution for a malaria model using the homotopy analysis method, 2025, 2199-577X, 10.2478/bile-2025-0001
9.	Emmanuel Chidiebere Duru, Michael C. Anyanwu, Mbah Godwin Christopher Ezike, A mathematical model to investigate the effect of misdiagnosis and wrong treatment in the co-circulation and co-infection of Malaria and Zika virus disease, 2025, 3, 2980-1869, 79, 10.59292/bulletinbiomath.1711811

Reader Comments

Your name:*

Email:*
© 2019 the Author(s), licensee AIMS Press. This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0)

通讯作者: 陈斌, bchen63@163.com

1.
沈阳化工大学材料科学与工程学院沈阳 110142

Mathematical Biosciences and Engineering

4.4

Metrics

Article views(5359) PDF downloads(729) Cited by(9)

Preview PDF

Download XML

Export Citation

Article outline

Show full outline

Figures and Tables

Figures(8) / Tables(2)

Mathematical Biosciences and Engineering

Mathematical assessment of the impact of different microclimate conditions on malaria transmission dynamics

Related Papers:

Abstract

1. Introduction

2. Materials and method

2.1. Model formulation

2.1.1. Temperature-dependent parameters

2.1.2. Basic properties

2.2. Analysis of the autonomous model

2.2.1. Asymptotic stability of disease-free equilibria

2.2.2. Global Asymptotic Stability of the RDFE: special case

2.3. Analysis of the non-autonomous model

2.3.1. Local asymptotic stability of RDFE (E0N \mathcal{E}_{0N} )

2.3.2. Global asymptotic stability of RDFE (E0N \mathcal{E}_{0N} )

2.3.3. Uniform persistence of the disease

3. Results: Numerical simulations of the model (2.1)

3.1. Numerical simulation of the reproduction number

3.2. Numerical Investigation of the impact of indoor and outdoor temperature variation

3.3. Numerical Investigation of the impact of indoor and outdoor temperature variation on efficacy of controls

3.4. Numerical Investigation of the interaction between the controls

4. Discussion

5. Conclusion

Acknowledgments

Conflict of interest

Appendix A:. Verification of assumptions A1−A7 A1-A7 in [37]

Appendix B:. Proof of Theorem 2.5

Appendix C:. Proof of Theorem 2.6

References

This article has been cited by:

Reader Comments

通讯作者: 陈斌, bchen63@163.com

Metrics

Figures and Tables

Other Articles By Authors

Related pages

Tools

Export File

Citation

Format

Content

Catalog

Abstract

1. Introduction

2. Materials and method

2.1. Model formulation

2.1.1. Temperature-dependent parameters

2.1.2. Basic properties

2.2. Analysis of the autonomous model

2.2.1. Asymptotic stability of disease-free equilibria

2.2.2. Global Asymptotic Stability of the RDFE: special case

2.3. Analysis of the non-autonomous model

2.3.1. Local asymptotic stability of RDFE (E0N \mathcal{E}_{0N} )

2.3.2. Global asymptotic stability of RDFE (E0N \mathcal{E}_{0N} )

2.3.3. Uniform persistence of the disease

3. Results: Numerical simulations of the model (2.1)

3.1. Numerical simulation of the reproduction number

3.2. Numerical Investigation of the impact of indoor and outdoor temperature variation

3.3. Numerical Investigation of the impact of indoor and outdoor temperature variation on efficacy of controls

3.4. Numerical Investigation of the interaction between the controls

4. Discussion

5. Conclusion

Acknowledgments

Conflict of interest

Appendix A:. Verification of assumptions A1−A7 A1-A7 in [37]

Appendix B:. Proof of Theorem 2.5

Appendix C:. Proof of Theorem 2.6

References

2.3.1. Local asymptotic stability of RDFE ( $\mathcal{E}_{0N}$ )

2.3.2. Global asymptotic stability of RDFE ( $\mathcal{E}_{0N}$ )

Appendix A:. Verification of assumptions $A1-A7$ in ^[37]

2.3.1. Local asymptotic stability of RDFE ( $\mathcal{E}_{0N}$ )

2.3.2. Global asymptotic stability of RDFE ( $\mathcal{E}_{0N}$ )

Appendix A:. Verification of assumptions $A1-A7$ in ^[37]