
Antimalarial drugs are critical for controlling malaria, but the emergence of drug resistance poses a significant challenge to global eradication efforts. This study explores strategies to minimize resistance prevalence and improve malaria control, particularly through the use of mass drug administration (MDA) in combination with antimalarial drugs. We develop a compartmental mathematical model that incorporates asymptomatic, paucisymptomatic, and clinical states of infection and evaluates the impact of resistance mutations on transmission dynamics. The model includes both treated and untreated states among infected and recovered individuals, with a focus on optimizing control strategies through MDA and antimalarial treatment. A global sensitivity analysis identifies the critical factors that influence malaria dynamics, including MDA coverage, treatment access for different infection states, the probability of mutation from treated sensitive human infections, to treated resistant human infections and the initial prevalence of resistance. The model is extended to include optimal control strategies that provide time-dependent control interventions for treatment and MDA. Intuitively, when the mutation rate is relatively low, the optimal strategy combines the use of antimalarial drugs and MDA, with a gradual decrease in antimalarial drug use over time, ensuring sustainable malaria control. In contrast, at higher mutation rates, the strategy prioritizes broader deployment of MDA while significantly reducing reliance on antimalarial to minimize the risk of resistance developing. Numerical simulations of the optimal control problem reinforce the importance of strategic intervention in mitigating drug resistance. This study contributes to understanding the role of MDA and treatment strategies in the control of malaria, with implications for optimizing malaria control programs in endemic regions.
Citation: 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[J]. Mathematical Biosciences and Engineering, 2025, 22(8): 1898-1930. doi: 10.3934/mbe.2025069
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Antimalarial drugs are critical for controlling malaria, but the emergence of drug resistance poses a significant challenge to global eradication efforts. This study explores strategies to minimize resistance prevalence and improve malaria control, particularly through the use of mass drug administration (MDA) in combination with antimalarial drugs. We develop a compartmental mathematical model that incorporates asymptomatic, paucisymptomatic, and clinical states of infection and evaluates the impact of resistance mutations on transmission dynamics. The model includes both treated and untreated states among infected and recovered individuals, with a focus on optimizing control strategies through MDA and antimalarial treatment. A global sensitivity analysis identifies the critical factors that influence malaria dynamics, including MDA coverage, treatment access for different infection states, the probability of mutation from treated sensitive human infections, to treated resistant human infections and the initial prevalence of resistance. The model is extended to include optimal control strategies that provide time-dependent control interventions for treatment and MDA. Intuitively, when the mutation rate is relatively low, the optimal strategy combines the use of antimalarial drugs and MDA, with a gradual decrease in antimalarial drug use over time, ensuring sustainable malaria control. In contrast, at higher mutation rates, the strategy prioritizes broader deployment of MDA while significantly reducing reliance on antimalarial to minimize the risk of resistance developing. Numerical simulations of the optimal control problem reinforce the importance of strategic intervention in mitigating drug resistance. This study contributes to understanding the role of MDA and treatment strategies in the control of malaria, with implications for optimizing malaria control programs in endemic regions.
Antimalarial drugs are crucial for controlling and eliminating malaria worldwide. However, the emergence of resistance in malaria parasites has significantly reduced their effectiveness, posing a critical challenge to global malaria control efforts [1]. Resistance often arises from genetic mutations in Plasmodium falciparum, enabling the parasite to withstand specific treatments. The spread and impact of these mutations on malaria endemicity have been extensively documented [1,2,3,4,5,6]. These developments raise concerns about the continued efficacy of key interventions, such as intermittent preventive treatment in pregnancy with sulfadoxine-pyrimethamine and seasonal malaria chemoprevention (SMC), particularly in affected regions. Consequently, it is essential to explore strategies to minimize the prevalence of resistance and reduce malaria-related mortality. One promising approach endorsed by the World Health Organization (WHO) is the mass drug administration (MDA) [7].
MDA involves administering antimalarial drugs to all individuals in a defined geographic area, regardless of the presence of symptoms or infection [7]. When implemented effectively, MDA can eliminate both drug-resistant and drug-sensitive parasites, providing the long-term benefit of prolonging the therapeutic efficacy of first-line treatments across entire populations, not just within the targeted region [8]. Given these advantages, incorporating MDA into models of malaria transmission dynamics is essential for understanding its role in controlling drug resistance and optimizing intervention strategies.
Malaria's pathogenesis involves multiple interacting factors, and significant research on malaria's transmission dynamics in the presence of drug resistance has been carried out over the past few decades. These studies include models with and without the MDA strategy, as well as models that incorporate genetic mutations in both the mosquito and human populations (e.g., [3,9,10,11]). In [9], an epidemiological model for the spread of antimalarial resistance, excluding mutations, was developed, considering the treated and untreated statuses of individuals. In [11], a mathematical model for malaria was formulated with treatment and three levels of resistance in humans, where the results showed the limited benefits of treatments in a population with resistant strains, especially in high-transmission areas. The prevalence of mutations related to antimalarial resistance in Plasmodium falciparum was studied using a Bayesian malaria model in [3]. A simple compartmental malaria model including MDA was developed in [10] to compute the probability of extinction. The model analytically calculated the expected time to extinction in small populations following MDA for various scenarios.
While some human malaria infections initially progress through an asymptomatic phase before developing into symptomatic or clinical cases, others remain paucisymptomatic throughout the entire duration of the infection, meaning they never advance to symptomatic or clinical stages, (e.g., [12,13]). Despite their mild symptoms, paucisymptomatic infections contribute to malaria transmission similarly to asymptomatic cases. Due to the overlap between malaria symptoms and those of other diseases, paucisymptomatic individuals often fail to realize they are infected. As a result, the parasites can persist in their bodies for extended periods, facilitating the spread of the disease [12,13]. However, the aforementioned studies do not incorporate the paucisymptomatic characteristic as addressed in the current work. In addition, we examine the combined effects of antimalarial drugs and the implementation of MDA within the host population for effective malaria control. Using a compartmental modeling approach, we assess the impact of resistance-associated mutations on malaria dynamics; we optimize control strategies, including MDA and the treatment proportions for individuals in asymptomatic, paucisymptomatic, and clinical states; and, finally, we investigate how the proportion of paucisymptomatic individuals affects the control strategies.
We begin by considering a model without optimal control that accounts for both the treated and untreated states among infected and recovered individuals. This approach is motivated by the challenges in accessing treatment in certain endemic regions. An in-depth asymptotic analysis of the model's steady states is performed using various threshold parameters, including the basic reproduction number, T0. Key findings include the local stability of the disease-free equilibrium and conditions under which the malaria model exhibits bistability through a backward bifurcation. Our findings suggest that increasing the proportion of infected individuals receiving treatment and the coverage of MDA significantly reduces the spread of resistance and malaria-related mortality. Additionally, a global sensitivity analysis is conducted to identify the key parameters influencing the prevalence of resistance and mortality. Four critical factors are identified: (ⅰ) The proportion of individuals covered by MDA, reflecting the strategy's acceptability in endemic areas; (ⅱ) the proportion of asymptomatic individuals receiving antimalarial treatment, highlighting access to treatment for this group; (ⅲ) the proportion of clinical cases receiving treatment; and (ⅳ) the initial prevalence of resistance and the mutation rate.
Next, we extend the model to include optimal control, where the MDA rate and the proportions of infectious individuals receiving treatment serve as time-dependent control strategies. We analyze the impact of these control measures on the transmission dynamics of malaria associated with resistance mutations. Pontryagin's maximum principle [14] is applied to characterize the optimal control strategies. Numerical simulations of the optimal control problem reinforce the findings of the global sensitivity analysis.
The remainder of the manuscript is organized as follows: Section 2 presents the model's description and associated parameters. In Section 3, we establish some fundamental properties of the model, including the existence of a globally defined semiflow, the asymptotic stability of the model's stationary states, and an analysis of the backward bifurcation. Baseline model simulations and sensitivity analysis results are detailed in Section 4. Section 5 introduces the optimal control problem, including the derivation of the necessary optimality conditions and numerical simulations of the control strategies. The overall findings of the manuscript are discussed in Section 6. Finally, Section 7 provides the detailed proofs of the manuscript's main results.
We examine the interconnected dynamics of humans and mosquitoes in malaria transmission. We use the variable k∈{r,s} to denote the type of infection, where r represents a resistant infection and s represents a sensitive infection. Furthermore, the variable ℓ∈{U,T} indicates the treatment status of the human host, with U representing an untreated infection and T representing a treated infection. The human population is classified into five states, namely susceptible (Sh), asymptomatic infected (Ak,ℓh), paucisymptomatic infected (Pk,ℓh), clinical cases (Ik,ℓh), and recovered (Rk,ℓh), while the mosquito population is divided into susceptible (Sm) and infectious mosquitoes (Ikm). The disease is transmitted from infectious mosquitoes to humans at time t through the force of infection, denoted as
λkm(t)=βkmNh(t)Ikm(t),k∈{s,r}, |
where βkm represents the transmission probability, and Nh denotes the total human population, given by
Nh(t)=Sh(t)+∑k∈{r,s}∑ℓ∈{T,U}(Ak,ℓh(t)+Pk,ℓh(t)+Ik,ℓh(t)+Rk,ℓh(t)). |
The force of infections from infected humans, either with sensitive infection (λsh) or with resistant infection (λrh), to mosquitoes is given by
λsh(t)=βshNh(t)[As,Uh(t)+Ps,Uh(t)+Is,Uh(t)+εr(Ar,Th(t)+Pr,Th(t)+Ir,Th(t))]+βshNh(t)[(1−εs)(As,Th(t)+Ps,Th(t)+Is,Th(t))],λrh(t)=βrhNh(t)[Ar,Uh(t)+Pr,Uh(t)+Ir,Uh(t)+εs(As,Th+Ps,Th(t)+Is,Th(t))]+βrhNh(t)[(1−εr)(Ar,Th(t)+Pr,Th(t)+Ir,Th(t))]. |
Here, εr represents the probability of mutation from treated resistant human infections to treated sensitive human infections, while εs represents the probability of mutation from treated sensitive human infections to treated resistant human infections.
The model we shall consider then reads
{˙Sh=Λh−μhSh−(λsm+λrm)Sh+ρh∑k∈{r,s}∑ℓ∈{U,T}Rk,ℓh,˙Ak,Th=−μhAk,Th+(1−p)ϕ(t)λkmSh−νhAk,Th−g(t)Ak,Th,k∈{s,r},˙Ak,Uh=−μhAk,Uh+(1−p)(1−ϕ(t))λkmSh−νhAk,Uh−g(t)Ak,Uh,k∈{s,r},˙Pk,Th=−μhPk,Th+pϕ(t)λkmSh−g(t)Pk,Th,k∈{s,r},˙Pk,Uh=−μhPk,Uh+p(1−ϕ(t))λkmSh−g(t)Pk,Uh,k∈{s,r},˙Ik,Th=−μhIk,Th+θ(t)νhAk,Th+θ(t)νhAk,Uh−γk,ThIk,Th−δk,ThIk,Th,k∈{s,r},˙Ik,Uh=−μhIk,Uh+(1−θ(t))νhAk,Th+(1−θ(t))νhAk,Uh−γk,UhIk,Uh−δk,UhIk,Uh,k∈{s,r},˙Rk,ℓh=−(μh+ρh)Rk,ℓh+γk,ℓhIk,ℓh+g(t)Ak,ℓh+g(t)Pk,ℓh,k∈{s,r}, ℓ∈{U,T}, | (2.1) |
and
{˙Sm=Λm−μmSm−(λsh+λrh)Sm,˙Ikm=λkhSm−δkmIkm,k∈{s,r}. | (2.2) |
The dynamic of the total number of disease-induced deaths is defined by
˙Dh=∑k∈{s,r},ℓ∈{T,U}δk,ℓhIk,ℓh. |
In System (2.1), the variable ϕ(t) denotes the rate of exposure of asymptomatic infections to antimalarial treatment without a curative intention at time t, whereas θ(t) represents the rate of exposure of clinical cases to antimalarial treatment with a curative intention. In addition, g(t) describes the implementation of MDA efforts. Note that
g(t)=qmda(t)Dmda, |
where qmda(t) denotes the proportion of the target population participating in MDA, and Dmda represents the delay required for an individual to be considered no longer a carrier after taking MDA treatment. Systems (2.1) and (2.2) will be considered under the following natural assumptions:
νh≥0;ρh≥0;g≥0;p,θ,ϕ∈(0,1);Λk≥0(for k=h,m);δkm≥0;δk,ℓh≥0;γk,ℓh≥0;(for k=s,r; and ℓ=T,U). |
The model is shown in Figure 1, and the remaining parameters of Models (2.1) and (2.2) are summarized in Tables 1 and 2.
Parameters | Description (unit) | Value [Ref] |
ϕ | Rate of exposure of asymptomatic and paucisymptomatic infections to antimalarial treatment without a curative intention | (0;1) |
θ | Rate of exposure of clinical cases to antimalarial treatment with a curative intention | (0;1) |
qmda | Proportion of humans under MDA | (0;1) |
εs | Probability of mutation from treated sensitive human infections to treated resistant human infections | 10−1−10−3(assumed) |
ˉγh | Ratio of the recovered rate | (0;1) |
ˉδh | Ratio of the additional mortality rate of humans due to disease | (0;1) |
ˉε | Ratio of the mutation rate | (0;1) |
ˉβm | Ratio of the infection rate of human by infectious mosquitoes | (0;1) |
ˉδm | Ratio of the mortality rate of infectious mosquitoes | (0;1) |
InitPrevR | Initial prevalence of drug resistance within the host population | {10−1,10−3} (assumed) |
εr | Probability of mutation from treated resistant human infections to treated sensitive human infections (day−1) | ˉεεs |
δr,Th | Additional death rate of treated infectious humans to resistant infection (day−1) | ˉδhδs,Uh |
βrm | Resistant infection rate of human by infectious mosquitoes (day−1 bites−1) | ˉβmβsm |
δrm | Mortality rate of mosquitoes with resistant infection (day−1) | ˉδmδsm |
γr,Th | Recovery rate of treated humans to resistant infection (day−1) | ˉγhγs,Th |
Parameters | Description (unit) | Value [Ref] |
T0,0 | Basic reproduction number for ϕ=0,θ=0,andg=0 | 5 (assumed) |
γs,Th | Recovery rate of treated humans to sensitive infection (day−1) | 0.0035 [15] |
γs,Uh | Recovery rate of untreated humans to sensitive infection (day−1) | 0 (assumed) |
γr,Uh | Recovery rate of untreated humans to resistant infection (day−1) | 0 (assumed) |
βsh | Sensitive infection rate of mosquitoes by infected humans (day−1 bites−1) | βh defined by (4.1) |
βrh | Resistant infection rate of mosquitoes by infected humans (day−1 bites−1) | βh defined by (4.1) |
βsm | Sensitive infection rate of humans by infectious mosquitoes (day−1 bites−1) | 0.022 [15] |
δs,Th | Additional death rate of treated infectious humans from sensitive infection (day−1) | 0 (assumed) |
δs,Uh | Additional death rate of untreated infectious humans from sensitive infection (day−1) | 1/5 [15] |
δr,Uh | Additional death rate of untreated infectious humans from resistant infection (day−1) | 9×10−5 [15] |
Λh | Recruitment rate of susceptible humans (day−1 humans) | 102 (assumed) |
μh | Natural mortality rate of humans (day−1) | 0.00224 (assumed) |
μm | Natural mortality rate of mosquitoes (day−1) | 1/20 (assumed) |
Λm | Recruitment rate of susceptible mosquitoes (day−1 mosquitoes) | 100 (assumed) |
δsm | Mortality rate of mosquitoes with sensitive infection (day−1) | 0.033 [15] |
ρh | Loss of immunity rate of recovered humans (day−1) | 5.5×10−4[15] |
νh | The rate at which asymptomatic humans become infectious (day−1) | 0.1 [15] |
p | The proportion of paucisymptomatic infections (day−1) | 0.7 (assumed) |
Dmda | Delay to being no longer a carrier after MDA (days) | 1 [16] |
ch | Balancing coefficients in the objective function ($ per person) | 1 (assumed) |
bh | Balancing coefficients in the objective function ($ per person) | 1 (assumed) |
Tf | End time of controls (year) | 10 (assumed) |
Cost of control | ||
cϕ | Cost of ϕ ($ per person) | 10 [17,18,19] |
cθ | Cost of θ ($ per person) | 3−20 [17,18,19] |
cg | Cost of MDA ($ per person) | 3−20 [17,18,19] |
Newborn humans and mosquitoes appear with the flux Λh and Λm, respectively. Susceptible humans (Sh) become infected with a force of infection denoted by λsm for sensitive infections and λrm for resistant infections. Similarly, susceptible mosquitoes (Sm) become infected with a force of infection denoted by λsh for sensitive infections and λrh for resistant infections. A fraction p of infected individuals will never develop clinical symptoms and will enter the group of paucisymptomatic infections (Ph). The rest will initially progress through an asymptomatic phase (Ah) before developing into symptomatic or clinical cases (Ih). Paucisymptomatic and asymptomatic infections are treated with antimalarial drugs without a curative intention at a rate ϕ, leading to the partitioning of compartments Ph and Ah into untreated (U) and treated (T) sub compartments. Similarly, symptomatic infections are treated with a curative intention at a rate θ, resulting in the partitioning of the symptomatic compartment into untreated (U) and treated (T) sub compartments. The implementation of MDA efforts is represented by g. Ah infections progress to Ih infections at a rate νh, while Ih infections recover at a rate γh. Recovered individuals lose their temporary immunity at a rate ρh. The death rates are either natural μk (for k=h,m) or due to infections for humans δh. Infectious mosquitoes die at a rate δkm (for k=s,r). The Notation is shown in Tables 1 and 2.
The aim of this section is to provide some preliminary remarks to Systems (2.1) and (2.2). Let us introduce the following vector notations:
Ah=(As,Th,Ar,Th,As,Uh,Ar,Uh)′,Ph=(Ps,Th,Pr,Th,Ps,Uh,Pr,Uh)′,Ih=(Is,Th,Ir,Th,Is,Uh,Ir,Uh)′,Rh=(Rs,Th,Rr,Th,Rs,Uh,Rr,Uh)′,Im=(Ism,Irm)′, |
as well as the matrices βh=diag(βkh)k∈{s,r}, βm=diag(βkm)k∈{s,r}, γh=diag(γk,ℓh)k∈{s,r},ℓ∈{T,U}, δh=diag(δk,ℓh)k∈{s,r},ℓ∈{T,U}, δm=diag(δkm)k∈{s,r},
Θ=(θ00θ1−θ001−θ),Φ=(ϕ00ϕ1−ϕ001−ϕ),e=(10100101),andε=(1−εsεr10εs1−εr01). |
Then Models (2.1) and (2.2) are rewritten as
{˙Sh=Λh−μhSh−12λmSh+ρh14Rh,˙Ah=(1−p)Φ(t)λmSh−(νh+μh+g(t))Ah,˙Ph=−μhPh+pΦ(t)λmSh−g(t)Ph,˙Ih=−μhIh+Θ(t)eνhAh−γhIh−δhIh,˙Rh=γhIh+g(t)Ah+g(t)Ph−(μh+ρh)Rh,˙Sm=Λm−μmSm−12λhSm,˙Im=λhSm−δmIm, | (3.1) |
with 12=(1,1), 14=(1,1,1,1), and
λh=λh(Sh,Ah,Ph,Ih,Rh)=βhNhε(Ah+Ph+Ih),λm=λm(Sh,Ah,Ph,Ih,Rh,Im)=1NhβmIm. |
Let us introduce the matrix B=−diag(μh,(μh+g(t)+νh)Id,(μh+g(t))Id,(μh+γh+δh)Id,(μh+ρh)Id,μm,δm), where Id is the identity matrix, as well as the nonlinear map
M[t](Sh,Ah,Ph,Ih,Rh,Sm,Im)=(Λh−12λmSh+ρh14Rh(1−p)Φ(t)λmShpΦ(t)λmShΘ(t)eνhAhg(t)(Ah+Ph)+γhIhΛm−12λhSmλhSm). |
By identifying v together with (Sh,Ah,Ph,Ih,Rh,Sm,Im) and by setting v0=(Sh(0),Ah(0),Ph(0),Ih(0),Rh(0),Sm(0),Im(0)), Systems (2.1) and (2.2) are rewritten as the following Cauchy problem:
{dv(t)dt=Bv(t)+M[t](v(t)),v(0)=v0. | (3.2) |
The existence and uniqueness of the bounded solutions of (3.2) reads as follows:
Theorem 3.1. Let v0∈R20+. Assume that θ, ϕ, and g are constant functions. Then the following hold.
(1) A unique global solution V(⋅,v0):[0,∞)→R20 exists such that V(t,v0)=v(t) and V(0,v0)=v0. Furthermore,
V(t,v0)=eBtv0+∫t0eB(t−η)M(v(η))dη. |
(2) The semiflow defined by {V(t,v0)}t is bounded, dissipative, and asymptotically smooth, and hence it admits a global attractor in R20+.
We recall the following definition.
Bounded dissipative : A bounded set Ω⊂R20 exists such that for any bounded set U⊂R20, τ=τ(U,Ω)≥0 exists such that V(t,U)⊂Ω for t≥τ.
Asymptotically smooth : For any nonempty, closed, bounded set U⊂R20, a nonempty compact set J=J(U) exists such that J attracts {φ∈U:V(t,φ)∈U,∀t≥0}.
Furthermore, we also recall that a nonempty set J⊂R20 is said to attract a nonempty set U⊂R20 if δ(V(t,U),J))→0 as t→+∞, where δ(U,J)=supu∈Uinfv∈J‖u−v‖.
Note that the term "asymptotically smooth" is used here following the terminology of Hale, LaSalle, and Slemrod [20]. However, this is strictly equivalent to the notion of asymptotically compact as defined by Ladyzhenskaya [21]. Finally, refer to Section 7.1 for the detailed proof of Theorem 3.1.
To determine the threshold of System (3.2), which govern the invasion dynamics of the disease in a host population that is completely free of infections, we linearize (3.2) around the disease-free equilibrium (DFE) E0. Specifically, the DFE is written as
E0=(S0h,0R4,0R4,0R4,0R4,S0m,0R2),S0h=Λhμh,S0m=Λmμm, |
and we linearize the infective compartments of (3.2) at the disease-free equilibrium E0 to obtain the following system:
dw(t)dt=ˆBw(t)+ˆMw(t), |
where w(t)=(Ah(t),Ph(t),Ih(t),Im(t)), and
ˆB=(−(μh+νh+g)Id04×404×404×204×4−(μh+g)Id04×404×2Θeνh04×4−(μhId+γh+δh)04×202×402×402×4−δm),ˆM=(04×404×404×4(1−p)Φβm04×404×404×4pΦβm04×404×404×404×2βhεS0mS0hβhεS0mS0hβhεS0mS0h02×2). |
Lemma 3.2. Assume that θ, ϕ, and g are constant functions. The following then hold.
(1) The square matrix ˆM is positive, i.e., ˆM is not the zero matrix, and all entries of ˆM are non-negative.
(2) The spectral bound s(ˆB), i.e., s(ˆB)=sup{ℜ(λ):λ∈σ(ˆB)}, satisfies s(ˆB)<0.
The proof of Lemma 3.2 is straightforward and thus the details are omitted.
We now define
T0:=r(ˆM(−ˆB)−1), |
where r(ˆM(−ˆB)−1) represents the spectral radius of the square matrix ˆM(−ˆB)−1.
The subsequent lemma provides a connection between the sign of T0−1 and the growth bound of the C0-semigroup generated by (ˆB+ˆM).
Lemma 3.3. Assume that θ, ϕ, and g are constant functions. In this case
sgn(s(ˆB+ˆM))=sgn(T0−1). |
Furthermore, we have
T0=√S0mS0hr(ThTm). |
Here, the 2×2 matrices Th and Tm describe the infectiousness of humans and mosquitoes, respectively, and are defined by
Th=βhε{((νh+μh+g)−1Id(1−p)+(g+μh)−1Idp+(μhId+γh+δh)−1Θeνh((νh+μh+g)−1Id(1−p)}Φ,Tm=βmδ−1m=diag(βsmδs−1m,βrmδr−1m). | (3.3) |
Through a straightforward computation, an explicit formula of T0 is given by
T20=(Ts0+Tr0)+√(Ts0−Tr0)2+4Qsr2, | (3.4) |
where
Ts0=S0mS0hβsmδsmβshKsh,Tr0=S0mS0hβrmδrmβrhKrh, |
Ksh=(1−εs)((1−p)θνh(νh+μh+g)(μh+γs,Th+δs,Th)+(1−p)ϕ1(νh+μh+g)+pϕ1(g+μh))⏟lifespan of s-infections exposed to antimalarial drugs+(1−p)(1−θ)νh(νh+μh+g)(μh+γs,Uh+δs,Uh)+(1−p)(1−ϕ)1(νh+μh+g)+p(1−ϕ)1(g+μh)⏟lifespan of s-infections unexposed to antimalarial drugs, |
Krh=(1−εr)((1−p)θνh(νh+μh+g)(μh+γr,Th+δr,Th)+(1−p)ϕ1(νh+μh+g)+pϕ1(g+μh))⏟lifespan of r-infections exposed to antimalarial drugs+(1−p)(1−θ)νh(νh+μh+g)(μh+γr,Uh+δr,Uh)+(1−p)(1−ϕ)1(νh+μh+g)+p(1−ϕ)1(g+μh)⏟lifespan of r-infections unexposed to antimalarial drugs, |
and
Qsr=εrβrhβrmδrm(S0mS0h)(θ(1−p)νh(μh+γr,Th+δr,Th)(νh+μh+g)+(1−p)ϕ1(νh+μh+g)+pϕ1g+μh)⏟{average rate of new s-infection from resistant infections due to mutation}×εsβshβsmδsm(S0mS0h)(θ(1−p)νh(μh+γs,Th+δs,Th)(νh+μh+g)+(1−p)ϕ1(νh+μh+g)+pϕ1g+μh)⏟{average rate of new r-infection from sensitive infections due to mutation}. |
Furthermore, employing the next-generation matrix approach introduced in Lemma 6.12 of [22], we can determine that T0 represents the basic reproduction number of the entire system, while Ts0 and Tr0 denote the basic reproduction numbers induced only by s- and r-infections, respectively. Consequently, by Lemma 3.3 and the results on the asymptotic stability of equilibria for the vector fields given in Theorem 3.16 of [22], we find that the DFE E0 is locally asymptotically stable if and only if T0<1.
The proof of Lemma 3.3 is appended in Section 7.2.
Remark 1. Parameters Ksh and Krh can be interpreted as lifespans of s- and r-infections, respectively. For instance, Ksh is rewritten as
Ksh=(1−εs)(1−p)θνh(νh+μh+g)Ds,T+(1−εs)(1−p)ϕDA+(1−εs)pϕDP+(1−p)(1−θ)νh(νh+μh+g)Ds,U+(1−p)(1−ϕ)DA+p(1−ϕ)DP, |
where DP=(μh+g)−1, DA=(μh+νh+g)−1, Ds,ℓ=(μh+γs,ℓh+δs,ℓh)−1, and ℓ=T,U are the lifespans of paucisymptomatic, asymptomatic, and clinical infections, respectively. From this, since (1−εs)(1−p)θνh(νh+μh+g), (1−εs)(1−p)ϕ, and (1−εs)pϕ represent the proportions of s-clinical, s-asymptomatic, and s-paucisymptomatic infections exposed to antimalarial drugs, respectively, we can easily interpret the term
(1−εs)(1−p)θνh(νh+μh+g)Ds,T+(1−εs)(1−p)ϕDA+(1−εs)pϕDP, |
as the lifespan of s-infections exposed to antimalarial drugs. By the same way, the term
(1−p)(1−θ)νh(νh+μh+g)Ds,U+(1−p)(1−ϕ)DA+p(1−ϕ)DP, |
represents the lifespan of s-infections unexposed to antimalarial drugs. Consequently, Ksh is then the lifespan of the overall s-infections.
A similar interpretation applies to Krh. As for Qsr, it can be understood as the product of the average rate of new s-infections arising from resistant infections and the average rate of new r-infections emerging from sensitive infections due to mutations.
Assume that θ, ϕ, and g are constant functions. Let
E∗h=(S∗h,A∗h,P∗h,I∗h,R∗h,S∗m,I∗m)′∈R20+, |
be an endemic equilibrium of System (3.1), and
λs∗h=βshN∗h[As,U∗h+Ps,U∗h+Is,U∗h+εr(Ar,T∗h+Pr,T∗h+Ir,T∗h)+(1−εs)(As,T∗h+Ps,T∗h+Is,T∗h)],λr∗h=βrhN∗h[Ar,U∗h+Pr,U∗h+Ir,U∗h+(1−εr)(Ar,T∗h+Pr,T∗h+Ir,T∗h)+εs(As,T∗h+Ps,T∗h+Is,T∗h)]. |
The next theorem provides the necessary conditions on which we have the existence of a unique endemic equilibrium and the demonstration of a backward bifurcation. We examine the occurrence of a bifurcation of the endemic equilibrium in Model (3.1) at T0=1. We find that an endemic equilibrium of (3.1) exists if and only if a positive constant κ exists such that
L(T20,κ)=1, |
where L is defined by
L(T20,κ)=ΛmS0hS0mT20(μh+χ1κ)(1+χ2κ)(Λhμm+(χ2+Λhμmωs+χ3)κ), |
where χ1=ωr(1−as)+ωs(1−ar), χ2=ωr(bs+as)+ωs(br+ar), and χ3=ωs(cs+ds)+ωr(cr+dr), with ω=(ωs,ωr) being the principal eigenvector of the matrix TmTh, and with ‖ω‖=1; aj, bj, cj, and dj, s are positive constants given later.
Next, we introduce the following bifurcation constant:
K=Λhμmχ1−(2χ2+Λhμmωs+χ3)μh. |
We then obtain the following result on the existence and bifurcation of the endemic equilibrium.
Theorem 3.4. Assume that θ, ϕ, and g are constant functions. We then have the following.
(1) If K>0, then a backward bifurcation occurs at T0=1, meaning that for T0 values slightly less than 1, two endemic equilibria exist for Model (3.1).
(2) If K<0, then a forward bifurcation occurs at T0=1, meaning that for T0 values slightly greater than 1, a unique endemic equilibrium exists, while for T0 values slightly less than 1, no endemic equilibrium exists.
(3) If T0>1, then at least one endemic equilibrium exists for (3.1). Moreover, if K>0, then when T0=1, an endemic equilibrium also exists.
(4) Assume that the map κ⟼L(T20,κ) is strictly decreasing on R+. Thus, an endemic equilibrium exists if and only if T0>1; in this case, the equilibrium is unique.
We refer to Section 7.3 for the proof of Theorem 3.4.
For the illustrative dynamics in this section, we assume that θ, ϕ, and g are constant functions.
The parameter values used in the model are summarized in Tables 1 and 2. In general, we assume that the parameters for sensitive infections are well-established for both humans and vectors. To estimate parameters for resistant infections, we introduce variable scaling parameters. For example, the mutation probability εs for transitions from sensitive to resistant infections is a known value. The mutation probability εr for transitions from resistant to sensitive infections is then estimated as εr=ˉεεs, where ˉε∈(0,1) is a scaling parameter that represents the ratio of the mutation rates. This approach ensures a consistent framework for parameter estimation across sensitive and resistant infections.
The transmission rate βh, which represents the rate of transmission from infected humans to mosquitoes and is assumed to be identical for both sensitive and resistant infections, is determined using the basic reproduction number T0 as given by (3.4). Specifically, βh is calibrated on the basis of the value of T0,0 under the baseline scenario where ϕ=0, θ=0, and g=0. This ensures that the transmission dynamics align with the expected epidemiological behavior under the given conditions. More precisely, we have
βh=T20,0S0hS0mmax{Cs0,Cr0}, | (4.1) |
with
Cs0=βsmδsm((1−p)νh(νh+μh)(μh+γs,Uh+δs,Uh)+(1−p)1(νh+μh)+p1μh),Cr0=βrmδrm((1−p)νh(νh+μh)(μh+γr,Uh+δr,Uh)+(1−p)1(νh+μh)+p1μh). |
The initial conditions are specified using parameters such as the initial prevalence of drug resistance (InitPrevR) within the host population. We assume an initial infection prevalence of Prev=50% with PrevI=10% of these infections being clinical cases. In addition, we suppose that a proportion (p=0.7) of infected humans will develop paucisymptomatic infections. The initial susceptible human population, asymptomatic infected, paucisymptomatic infected, and infectious case are, respectively, given by Sh(0)=(1−Prev)S0h; Ah(0)=(1−p)S0h(1−PrevI)Prev(1−InitPrevR,InitPrevR,0,0); Ph(0)=pS0hPrev(1−InitPrevR,InitPrevR,0,0); Ih(0)=(1−p)S0hPrevPrevI(1−InitPrevR,InitPrevR,0,0); and Rh(0)=(0,0,0,0). For mosquitoes, we assume that Sm(0)=0.9S0m and Im(0)=0.1S0m(1−InitPrevR,InitPrevR).
Model (3.1) is employed to characterize the malaria infection burden within the human host population and to capture the dynamics of resistant clinical cases.
When the probability of mutation from treated sensitive human infections to treated resistant human infections (εs) is relatively low (Figure 2), the exposure rate ϕ of asymptomatic and paucisymptomatic infections to antimalarial treatment has a marginal impact on both mortality and the number of resistant clinical cases (Figure 2, Column 1 vs. Column 2 vs. Column 3). However, while increasing the antimalarial treatment rate θ for clinical cases has a relatively marginal effect on the cumulative number of deaths due to infection when qmda is moderate (Figure 2A–C), such an increase significantly reduces infection-related mortality when qmda is relatively high (Figure 2D–I). Likewise, increasing the proportion of humans covered under MDA has a pronounced effect in reducing both mortality and resistant clinical cases, with a particularly strong impact on the latter (Figure 2). Importantly, increasing the treatment rate for clinical cases is associated with a rise in the number of resistant clinical cases (Figure 2A–F), except in the scenario where the proportion qmda is sufficiently strong (Figure 2G–I). These contrasting behaviors highlight the beneficial effect of combining antimalarial treatment and MDA to simultaneously reduce infection-related mortality and the number of resistant clinical cases.
The configuration above remains similar under high mutation rates (εs) (Figure 3). However, a high mutation rate εs leads to a higher number of deaths within the host population (Figure 3) compared with the case of a moderate mutation rate (Figure 2). Furthermore, high values of εs accelerate the emergence of antimalarial resistance within the host population (Figure 3A–F) compared with scenarios with low mutation rates (Figure 2A–F). Although extensive use of MDA helps reduce both deaths and resistant cases, the reduction in resistant cases occurs more slowly under high mutation rates (Figure 3G–I) than in the case of low mutation rates (Figure 2G–I).
Finally, for Figures 2D–I and 3D–I, one may observe a peak in resistant clinical cases at the initial time t=0. This peak is due to our chosen initial data. However, in Figure 3G–I, we observe an increase in resistant clinical cases during the first year before they start to decline. This initial increase can be explained by the high mutation rate εs. Indeed, although the proportion of humans covered under MDA (qmda) is sufficiently high, the strong mutation capability initially leads to an increase in the number of resistant clinical cases before they begin to decline (Figure 3G–I). In contrast, this pattern is not observed when the mutation rate is low (Figure 2G–I).
We analyze the sensitivity of cumulative deaths and resistant cases (including paucisymptomatic, asymptomatic, and clinical cases) to five key parameters: the initial prevalence of drug resistance within the host population (InitPrevR), the probability of mutation from treated sensitive human infections to treated resistant human infections (εs), the rate of exposure of asymptomatic and paucisymptomatic infections to antimalarial treatment without a curative intention (ϕ), the rate of exposure of clinical cases to antimalarial treatment with a curative intention (θ), and the proportion of humans covered under MDA (qmda). The variation range for these parameters is specified in Table 1. Sensitivity indices are calculated by fitting an analysis of variance (ANOVA) linear model, including up to third-order interactions, to simulation-generated data. This ANOVA model demonstrates a high level of accuracy, explaining more than 99% of the variance.
Overall, the sensitivity analysis identifies qmda as the primary parameter influencing both the number of deaths and the prevalence of resistant cases (Figure A1). It accounts for 89% of the variance in the number of deaths (Figure A1, left) and 53% in the prevalence of resistant cases (Figure A1, right). When interactions with other parameters are included, these indices increase to 94% and 83%, respectively. The second most influential parameter is θ, which explains 5% of the variance in the number of deaths (rising to 10% when accounting for interactions with other parameters) and 14% of the variance in the prevalence of resistance (rising to 44% with interactions). The parameters InitPrevR and εs have a comparable and modest impact, each contributing 0.2%–0.4% to the variance in both outcomes. Finally, ϕ has a negligible effect on both the number of deaths and the prevalence of resistance, explaining less than 0.09% of the variance, even when accounting for interactions.
Although previous analyses were performed under the assumption of constant parameter values for the rate of exposure of asymptomatic and paucisymptomatic infections to antimalarial treatment without curative intent (ϕ), the rate of exposure of clinical cases to antimalarial treatment with curative intent (θ), and the proportion of humans covered under MDA (g). This section considers these parameters as time-dependent functions and assigns reasonable upper and lower bounds to account for potential temporal variations.
The control scheme (θ,ϕ,g) lies on the set
Ω={(θ,ϕ,g)∈(L∞(0,Tf))3:0≤θ≤1;0≤ϕ≤1;0≤g≤gmax}, |
with gmax being a positive constant.
Although our objective is not to provide a detailed analysis of the controlled system, i.e., System (3.1) where the control scheme (θ,ϕ,g) is considered as a time-dependent function, we present the following well-posedness result.
Theorem 5.1. Assume that the time-dependent functions θ, ϕ, and g are continuous. Then the controlled system, that is, the System (3.1), where the control scheme (θ(t),ϕ(t),g(t)) is considered as a time-dependent function, generating a unique, globally defined, positive, and bounded non autonomous semiflow.
The proof of this result relies on a standard methodology (e.g., [23,24]).
We assume that a successful control scheme is one that effectively reduces both the total number of deaths and the total number of resistant cases. Consequently, the control scheme is considered optimal if it minimizes the following objective functional:
J(θ,ϕ,g)=∫Tf0(chDh(t)+bh∑ℓ∈{T,U}(Ar,ℓh(t)+Pr,ℓh(t)+Ir,ℓh(t))+cθ2θ2(t)+cϕ2ϕ2(t)+cg2g2(t))dt. | (5.1) |
Here, bh and ch are balancing coefficients that transform the integral into the cost expended over a finite period of Tf years (see Table 2). The first integral, weighted by bh and ch, captures the economic losses associated with deaths and resistant infections, respectively. The second integral represents the costs of implementing the three control measures, with quadratic terms for the controls included to account for the nonlinear costs.
We find that (θ∗,ϕ∗,g∗) satisfies
J(θ∗,ϕ∗,g∗)=min(θ,ϕ,g)∈ΩJ(θ,ϕ,g). | (5.2) |
To address the necessary optimality conditions, we follow the framework provided by [25,26,27]. Given a solution v=(Sh,Ah,Ph,Ih,Rh,Sm,Im) of System (3.1), where the control scheme (θ(t),ϕ(t),g(t)) is considered as a time-dependent function, we define the corresponding adjoint functions as ϑ=(ϑSh,ϑAh,ϑPh,ϑIh,ϑRh,ϑSm,ϑIm,ϑDh). Theorem 5.1 gives the existence and boundedness of the solutions of System (3.1) with time-dependent control functions. According to the results in [25,27], the set of controls Ω is nonempty, convex, and closed. Moreover, the right-hand side of System (3.1) is continuous and can be expressed as a linear function of the controls θ, ϕ, and g, with coefficients that depend on both time and the state variables.
If we choose a1∈R∗+, a2=min{cθ2,cϕ2,cg2}, and α=2, the integrant h(v,θ,ϕ,g)(t) of J verifies
h(v,θ,ϕ,g)(t)=chDh(t)+bh∑ℓ∈{T,U}(Ar,ℓh(t)+Pr,ℓh(t)+Ir,ℓh(t))+cθ2θ2+cϕ2ϕ2+cg2g2≥cθ2θ2+cϕ2ϕ2+cg2g2≥−a1+min{cθ2,cϕ2,cg2}(θ2+ϕ2+g2). |
Therefore, the existence of the optimal control is given by the following result.
Theorem 5.2. Assume that the time-dependent functions θ, ϕ, and g are continuous. Let v=(Sh,Ah,Ph,Ih,Rh,Sm,Im) be the solution of System (3.1) where the control scheme (θ,ϕ,g) is considered as a time-dependent function. Here, (θ∗,ϕ∗,g∗)∈Ω exists such that
min(θ,ϕ,g)∈ΩJ(θ,ϕ,g)=J(θ∗,ϕ∗,g∗). |
The existence of such a control is well-established using standard techniques, as detailed in [25,27].
Pontryagin's maximum principle [14] allows us to reformulate the problem (5.2) to the problem of minimizing the Hamiltonian defined as follows:
H=chDh+bh∑ℓ∈{T,U}(Ar,ℓh+Pr,ℓh+Ir,ℓh)+cθ2θ2+cϕ2ϕ2+cg2g2+∑z∈Zϑzfz, |
where Z={Sh,Ah,Ph,Ih,Rh,Dh,Sm,Im}, (ϑz)z∈Z are adjoint functions and fz is given by the right-hand side of Models (2.1) and (2.2) for the z-compartment.
The necessary conditions for the existence of the solution to the problem (5.2) are
˙ϑz=−∇zH,for z∈Z, | (5.3) |
and
∂H∂w=0,for w∈{θ,ϕ,g}. | (5.4) |
From (5.3), we find that the adjoint system (ϑk)z∈Z verifies:
{˙ϑSh=(μh+12λm(1−ShNh))ϑSh−(1−ShNh)(1−p)(Φλm)tϑAh−(1−ShNh)p(Φλm)tϑPh−12λhSmNhϑSm+SmNh⟨λh,ϑIm⟩,˙ϑAh=b−ShNh(12λm)1t4ϑSh+(μh+νh+g(t))ϑAh+ShNh(1−p)(14(Φλm)tϑAh)t+ShNhp(14(Φλm)tϑPh)t−(Θeνh)tϑIh−g(t)ϑRh+SmNh((12βhε)t−(12λh)1t4)ϑSm−SmNh((βhε)tϑIm−⟨λh,ϑIm⟩1t4),˙ϑPh=b−ShNh(12λm)1t4ϑSh+(μh+g(t))ϑPh+ShNhp(14(Φλm)tϑPh)t+ShNh(1−p)(14(Φλm)tϑAh)t−g(t)ϑRh+SmNh((12βhε)t−(12λh)1t4)ϑSm−SmNh((βhε)tϑIm−⟨λh,ϑIm⟩1t4),˙ϑIh=b−ShNh(12λm)1t4ϑSh+ShNh(1−p)(14(Φλm)tϑAh)t+ShNhp(14(Φλm)tϑPh)t−γhϑRh+(μhId+γh+δh)ϑIh+δh1t4ϑDh+SmNh((12βhε)t−(12λh)1t4)ϑSm−SmNh((βhε)tϑIm−⟨λh,ϑIm⟩1t4),˙ϑRh=−ShNh(12λm)1t4ϑSh+ShNh(1−p)(14(Φλm)tϑAh)t+ShNhp(14(Φλm)tϑPh)t−ρh1t4ϑSh+(μh+ρh)ϑRh+SmNh((12λh)1t4ϑSm−⟨λh,ϑIm⟩1t4),˙ϑDh=−ch, | (5.5) |
and
{˙ϑSm=(μm+12λh)ϑSm−⟨λh,ϑIm⟩,˙ϑIm=δmϑIm+ShNh(12βm)tϑSh−ShNh(Φβm)t((1−p)ϑAh+pϑPh), | (5.6) |
with b=(0,−bh,0,−bh). Systems (5.5) and (5.6) are associated with the boundary conditions or transversality conditions, ϑz(Tf)=0, for all z∈Z.
Furthermore, by (5.4), we have:
∂H∂θ=cθθ−νh∑kAk,Th(ϑk,TIh−ϑk,UIh)−νh∑kAk,Uh(ϑk,TIh−ϑk,UIh)=0,∂H∂ϕ=cϕϕ−∑k(1−p)λkmShϑk,UAh−∑kpλkmShϑPhPk,U+∑k(1−p)λkmShϑk,TAh+∑kpλkmShϑk,TPh=0,∂H∂g=cgg−bh((Ar,Th+Ar,Uh)+(Pr,Th+Pr,Uh))−∑k,ℓ(Ak,ℓh)t(ϑk,ℓAh−ϑk,ℓRh)−∑k,ℓ(Pk,ℓh)t(ϑk,ℓPh−ϑk,ℓRh)=0. | (5.7) |
Therefore, if (θ∗,ϕ∗,g∗)∈Ω is a solution of (5.2), then by (5.7), it is characterized by:
θ=max{0,min{1;νh∑k(Ak,Th+Ak,Uh)(ϑk,TIh−ϑk,UIh)cθ}},ϕ=max{0,min{1;Sh∑kλkm[(1−p)(ϑk,UAh−ϑk,TAh)+p(ϑk,UPh−ϑk,TPh)]cϕ}},g=max{0,min{gmax;bh((Ar,Th+Ar,Uh)+(Pr,Th+Pr,Uh))+∑k,ℓ[(Ak,ℓh)t(ϑk,ℓAh−ϑk,ℓRh)+(Pk,ℓh)t(ϑk,ℓPh−ϑk,ℓRh)]cg}}. | (5.8) |
The state system (3.1), the adjoint systems (5.5) and (5.6), and the control characterization system (5.8) together form the optimality system that must be solved numerically. These systems operate as a feedback system in the following sense.
(1) State system input: A given controller serves as the input for the state system.
(2) Adjoint system input: The controller, along with the output of the state system, becomes the input for the adjoint system.
(3) Control update: The outputs of the state and adjoint systems are then used to update the controller via the control characterization system.
(4) Loop closure: The updated controller is fed back as the input for the state system, forming a "closed loop" system.
Since the state equations are governed by the initial conditions and the adjoint equations rely on the final-time conditions, the optimality system cannot be solved straightforwardly by sweeping forward in time alone. Instead, an iterative approach known as the forward−backward sweep method is applied (see [26]). This method alternates between solving the state equations forward in time and the adjoint equations backward in time, iteratively updating the control until convergence is achieved.
Figure 4 demonstrates the impact of an optimal intervention strategy on the number of deaths and clinical cases. The optimal control strategy strongly discourages the exposure of asymptomatic and paucisymptomatic infections to antimalarial treatment without curative intent (Figure 4A). This aligns with the findings of the global sensitivity analysis, which indicates that this parameter has a minimal impact on both mortality and the prevalence of resistant strains. Antimalarial treatment with curative intention is employed at relatively high levels during the initial years, followed by a gradual reduction toward the end of the control period. In contrast, the use of MDA is strongly recommended at a consistently high rate throughout the control period (Figure 4A). Furthermore, the reduction in antimalarial treatment is effectively offset by the increased use of MDA within the host population. This approach is likely driven by the assumption that the costs of both control strategies are equivalent in this scenario. The optimal intervention strategies markedly diminish the severity of the projected outbreaks, reducing both the total number of deaths (Figure 4B) and the prevalence of clinical cases (Figure 4C).
Antimalarial treatments and mass drug administration (MDA) are key strategies to alleviate the burden of malaria. However, the rise of parasite resistance to antimalarial drugs presents a significant challenge to effective malaria control and treatment. To assess the impact of combining antimalarial treatments and MDA for effective disease control, the human population is categorized into five distinct states: susceptible, asymptomatic infected (individuals with very mild or no symptoms who may later develop symptomatic infections), paucisymptomatic infected (individuals with very mild or no symptoms who do not progress to symptomatic infections), clinical cases, and recovered individuals. An infected human, whether symptomatic, paucisymptomatic, or asymptomatic, can be treated with antimalarial drugs either with curative intent or without. Meanwhile, the mosquito population is divided into two states: susceptible and infectious mosquitoes.
We use optimal control theory [26] to characterize an optimal strategy that significantly reduces the number of deaths and resistant clinical cases. Our formulation assumes a quadratic cost for the control effort. Overall, for a relatively low mutation rate from treated sensitive human infections to treated resistant human infections ( \varepsilon_s = 10^{-3} ), the optimal strategy strongly limits antimalarial treatments for asymptomatic and paucisymptomatic infections without curative intent. Curative treatments are applied heavily in the initial years, then taper off while MDA is consistently maintained at high levels throughout the control period (Figure 4).
In the scenario of a relatively high mutation rate ( \varepsilon_s = 10^{-1} ) (see Figure 5), the configuration closely resembles that of a low mutation rate (Figure 4). However, a higher mutation rate leads to a reduced deployment of antimalarial drugs, which is compensated by an increased reliance on MDA within the host population for effective control (Figures 4A and 5A). Intuitively, when the mutation rate is relatively low, the optimal strategy combines the use of both antimalarial treatment with curative intent and MDA, with a gradual decrease in antimalarial use over time, ensuring sustainable malaria control. In contrast, at higher mutation rates, the strategy prioritizes broader deployment of MDA while significantly reducing reliance on antimalarial drugs to minimize the risk of resistance developing. Figure 6 assesses the impact of control costs on the model's dynamics. For a high cost of curative treatment and a low cost of MDA (as shown in Figure 6A–C), the control strategies favor higher reliance on MDA and reduced use of antimalarial treatments. This pattern is evident in society, where high treatment costs often prevent individuals from seeking care until they are already ill. As a result, implementing MDA on a large scale is crucial to effectively reduce both deaths and clinical cases over time.
In contrast, when the cost of curative treatments is lower than that of MDA (see Figure 6D–F), the control strategy advocates for a combination of both approaches: treating clinical cases with curative intent while also implementing a significant level of MDA to more effectively reduce deaths and clinical cases. However, the use of MDA is less extensive in this scenario compared with the previous one (see Figure 6A–C), likely due to the higher cost of MDA. It is also clear that the number of deaths and clinical cases is lower when MDA is more affordable (Figure A2). It is essential to note that treating infected individuals without curative intent in both scenarios is strongly discouraged to prevent the emergence of resistance over time.
Human malaria infections are characterized by the actual presence of parasites within an individual, but with the absence or very mild malaria-related symptoms, this remains a challenge for malaria control programs due to their significant influence on transmission dynamics [12,13]. While some infected individuals never develop clinical symptoms and transit to the group of paucisymptomatic infections, others initially progress through an asymptomatic phase (i.e., without symptoms) before developing into symptomatic or clinical cases. Treating the infectious parasite reservoir in paucisymptomatic and asymptomatic individuals is a critical intervention strategy with a positive impact on reducing the malaria burden (Figures 4 and 5). The proportion of paucisymptomatic infections ( p ) within the host population significantly affects control strategies that combine MDA and antimalarial treatments (Figure 7). Specifically, a low proportion of paucisymptomatic infections results in a greater reliance on MDA for effective control (Figure 7, Row 1). This is because a lower prevalence of paucisymptomatic infections corresponds to a higher proportion of asymptomatic infections that eventually progress to symptomatic cases. Consequently, antimalarial use remains relatively high during the initial years of the control period and continues, albeit at a lower rate, over the duration of the control period (Figure 7A). In contrast, when the proportion of paucisymptomatic infections is moderate (Figure 7, Row 2) or high (Figure 7, Row 3), the deployment of MDA is less intense compared with scenarios with low paucisymptomatic prevalence. Additionally, the use of antimalarials is robust during the initial years of the control period but decreases substantially afterward (Figure 7D, G).
The proposed model assumes heterogeneity within both the human and mosquito populations. However, this presents a potential limitation, as incorporating factors such as the chronological age of human and mosquito populations and the time since infection can have significant epidemiological implications for malaria control strategies [13,28,29,30]. According to previous studies, e.g., [28,29], an age-structured model formulation within this context may indeed be interesting to investigate in detail but would deserve a dedicated study.
Another potential limitation of this study is the arbitrary choice of the balancing coefficients in the objective function. Specifically, the value of the balancing cost lacks precise justification, introducing an element of uncertainty into the outcome of the optimal control function. Although we have deliberately chosen its value, we acknowledge that this parameter can significantly influence the resulting optimal control function.
Note that the linear operator \mathcal{B} is the infinitesimal generator of a strongly continuous semigroup \{e^{\mathcal{B}t}\}_t which preserves \mathbb{R}^{20}_+ . Furthermore, the map \mathcal{M}: \mathbb{R}^{20} \to \mathbb{R}^{20} is locally Lipschitz; therefore, classical results (e.g., [24,31]) shows that for any v_0 \in \mathbb{R}^{20} , we can find a time T = T(v_0) > 0 such that (3.2) has a unique solution v \in C\left([0, T) \right) \cap C^1\left((0, T) \right) such that
\mathcal{V}(t,v_0): = v(t) = e^{\mathcal{B}t}v_0+ \displaystyle {\int}_0^t e^{\mathcal{B}(t-\eta)} \mathcal{M}(v(\eta)) {{\rm{d}}} \eta, \forall t\in [0,T). |
Moreover, statements below are valid.
(ⅰ) If T < +\infty , then \lim_{t \to T^-}\| \mathcal{V}(t, v_0) \|_{ \mathbb{R}^{20}} = +\infty .
(ⅱ) Let t\in (0, T) . If a sequence \{u_n\}_n \subset \mathbb{R}^{20} such that u_n \to v_0 in \mathbb{R}^{20} as n\to \infty , then \mathcal{V}(\eta, u_n) exists for all \eta \in [0, t] , where n is sufficiently large and \sup_{\eta \in [0, t]} \| \mathcal{V}(\eta, u_n)- \mathcal{V}(\eta, v_0)\|_{ \mathbb{R}^{20}} \to 0 , as n \to \infty .
We are now interested in the positiveness of the solutions. Note that \mathcal{B} is resolvent positive, i.e., for all \zeta , with \zeta > -\omega: = \min \{\mu_h, \mu_m, \delta_m\} > 0 , (\zeta{\rm{I_d}}- \mathcal{B}) is invertible and (\zeta{\rm{I_d}}- \mathcal{B})^{-1} \mathbb{R}^{20}_+ \subset \mathbb{R}^{20}_+ . Moreover, for all \eta > 0 , we can find \zeta_\eta > 0 such that
\begin{equation} \mathcal{M}(v(t))+ \zeta_\eta v(t) \ge 0_{ \mathbb{R}^{20}}, \quad \forall v \in \mathbb{R}^{20}_+ \cap \overline{B}(0,\eta), \forall t \in [0,T), \end{equation} | (7.1) |
with B(0, \eta) being the open ball in \mathbb{R}^{20} centered at 0 with a radius \eta . Therefore, for all v_0 \in \mathbb{R}^{20}_+ , \mathcal{V}(t, v_0) \in \mathbb{R}^{20}_+ for all t\in [0, T) , i.e.,
\mathcal{V}(t, \mathbb{R}^{20}_+) \subset \mathbb{R}^{20}_+, \quad \forall t\in [0,T). |
The statement above follows from well-known results, e.g., [34, Theorem 5.2.7,p. 226]. Inequality (7.1) should be understood in the following sense. We recall that the mapping \mathcal{M}: \mathbb{R}^{20} \to \mathbb{R}^{20} is such that \mathcal{M} = \left(\mathcal{M}_\ell \right)_{\ell = 1, \cdots, 20} . Thus, (7.1) expresses that, for all, \ell = 1, \cdots, 20 , \mathcal{M}_\ell (v)+ \zeta_\eta v_\ell\ge 0 , where v = (v_\ell)_{\ell = 1, \cdots, 20} \in \mathbb{R}^{20} .
Next, for v_0 \in \mathbb{R}^{20}_+ , let \mathcal{V}(t, v_0) \in \mathbb{R}^{20}_+ , for all t\in [0, T(v_0)) , be the solution of (3.2). Then
\begin{align*} \dot N_h(t)\leq&\Lambda_h-\mu_h N_h(t), \quad \dot N_m(t)\leq \Lambda_m - \min(\mu_m,\delta_m^*) N_m(t),\quad \mbox{with}\quad \delta_m^* = \min(\delta_m^s,\delta_m^r), \end{align*} |
i.e.,
\begin{align*} & N_h(t)\leq N_h(0)e^{-\mu_h t} + \dfrac{\Lambda_h}{\mu_h}(1-e^{-\mu_h t}),\\ & N_m(t)\leq N_m(0)e^{-\min(\mu_m,\delta_m^*) t}+\dfrac{\Lambda_m}{\min(\mu_m,\delta_m^*)}(1-e^{-\min(\mu_m,\delta_m^*) t}). \end{align*} |
From the case where \forall t \in [0, T) ,
\begin{align*} N_h(t) \le \max \left(N_h(0), \dfrac{\Lambda_h}{\mu_h} \right), \quad N_m(t) \le \max \left(N_m(0), \dfrac{\Lambda_h}{\min(\mu_m,\delta_m^*)} \right). \end{align*} |
Consequently
\sup\limits_{t \in [0,T(v_0))} \| \mathcal{V}(t,v_0)\| < \infty, |
which ends the global well-posedness in \mathbb{R}^{20}_+ .
It remains to show the bounded dissipativity, that is, a bounded subset \mathcal{Q} \subset \mathbb{R}^{20}_+ exists such that, for each bounded subset Q \subset \mathbb{R}^{20}_+ , t_0 = t_0(Q) > 0 exists such that \mathcal{V}(t, Q) \subset \mathcal{Q} , for all t\ge t_0 . Let v_0 \in \mathbb{R}^{20}_+ , and let \mathcal{V}(t, v_0) = (S(t), A_h(t), P_h(t), I_h(t), R_h(t), S_m(t), I_m(t)) be the corresponding semiflow. Setting
\mathcal{Q} = \left\{\begin{array}{ll}(S_h,A_h,P_h,I_h,R_h,S_m,I_m) \in \mathbb{R}^{20}_+: &\\S_h+ S_m +\|A_h\|+\|P_h\|+\|I_h\|+\|R_h\|+\|I_m\| \leq \dfrac{\Lambda_h}{\mu_h}+ \dfrac{\Lambda_m}{\min(\mu_m,\delta_m^*)}\end{array}\right\}, |
we easily find the bounded dissipativity of the semiflow.
To end with the proof of Theorem 3.1, it remains to show that the semiflow \{\mathcal{V}(t, \cdot)\}_t is asymptotically smooth, i.e., for any closed, bounded, and positively invariant set Q \subset \mathbb{R}^{20}_+ , a compact set K \subset \mathbb{R}^{20}_+ exists such that d\left(\mathcal{V}(t, Q), K)\right) \to 0 , as t \to \infty , where d is the Hausdorff semi distance, see e.g., [32]. Note that
\mathcal{V}(t,v_0) = e^{\mathcal{B}t}v_0+ \displaystyle {\int}_0^t e^{\mathcal{B}(t-\eta)} \mathcal{M} \left( \mathcal{V}(\eta,v_0) \right) {{\rm{d}}} \eta. |
Since \{e^{\mathcal{B}t}\}_t is strictly contractive and \mathcal{M} is compact, the lemma follows from the results established in [33].
By Lemma 3.2, we can employ the results in [22] to establish the first part of the lemma.
For the second part of the lemma, note that
(-\hat{B})^{-1} = \begin{pmatrix} (\mu_{h}+g +\nu_{h})^{-1}{\rm{I_d}}& 0_{4 \times 4}& 0_{4 \times 4} & 0_{4 \times 2}\\ 0_{4 \times 4}&(\mu_{h}+g )^{-1}{\rm{I_d}}&0_{4 \times 4}& 0_{4 \times 2}\\ \nu_{h}(\mu_{h}+g +\nu_{h})^{-1}(\mu_{h}{\rm{I_d}}+\gamma_{h}+\delta_{h})^{-1}\Theta\textbf{e} & 0_{4 \times 4} & (\mu_{h}{\rm{I_d}}+\gamma_{h}+\delta_{h})^{-1} & 0_{4 \times 2}\\ 0_{2 \times 4} & 0_{4 \times 4} & 0_{4 \times 4} & \delta_{m}^{-1} \end{pmatrix} |
From this, \hat{M}(-\hat{B})^{-1} can be written as
\hat{M}(-\hat{B})^{-1} = \begin{pmatrix} 0_{12\times 12} & V \\ U & 0_{2\times 2} \end{pmatrix}, |
where U and V are, respectively, 2\times 12 and 12\times 2 matrices such that
\begin{align*} & U = \frac{ S^0_{m}}{S^0_{h}}\begin{pmatrix} (\mu_{h}+g +\nu_{h})^{-1}\beta_{h}\varepsilon \left[{\rm{I_d}}+\nu_{h} (\mu_{h}{\rm{I_d}}+\gamma_{h}+\delta_{h})^{-1}\Theta\textbf{e}\right]& \beta_{h}\varepsilon (\mu_{h}+g_{h})^{-1}{\rm{I_d}} & \beta_{h}\varepsilon (\mu_{h}{\rm{I_d}}+\gamma_{h}+\delta_{h})^{-1} \end{pmatrix} , \\ & V = \begin{pmatrix} (1-p) \Phi\beta_{m}\delta_{m}^{-1}\\ p\Phi\beta_{m}\delta_{m}^{-1}\\ 0_{4\times 2} \end{pmatrix}. \end{align*} |
Therefore,
\left(\hat{M}(-\hat{B})^{-1}\right)^2 = \text{diag} \left(UV, VU\right), |
where
\left(\mathsf{r}(\hat{M}(-\hat{B})^{-1}) \right)^2 = \mathsf{r}(\hat{M}(-\hat{B})^{-1})^2 = \max \left\{ \mathsf{r}(UV), \mathsf{r}(VU) \right\}. |
Finally, we have
\mathsf{r}(UV) = \mathsf{r}(VU) = \frac{ S^0_{m}}{S^0_{h} } \mathsf{r} \left( \mathcal{T}_{h} \mathcal{T}_{m} \right), |
with \mathcal{T}_{h} and \mathcal{T}_{m} introduced by (3.3).
The different composants of E_h^* are given by
\begin{align*} \begin{pmatrix} S^*_h \\ R^*_h \end{pmatrix} = &\begin{pmatrix} \mu_h+ \mathbf{1_2}\lambda^*_m & - \rho_h \mathbf{1_4} \\\\ -[\gamma_h (\mu_h{\rm{I_d}} +\gamma_h+\delta_h)^{-1} \Theta\boldsymbol{e} \nu_h (\nu_h+\mu_h+g )^{-1}(1-p)+g (g +\mu_h)^{-1} {\rm{I_d}}p\\+g (\nu_h+\mu_h+g )^{-1}(1-p)]\Phi \lambda^*_m & (\mu_h+\rho_h) {\rm{I_d}} \end{pmatrix}^{-1} \begin{pmatrix} \Lambda_h\\ 0_4 \end{pmatrix}\\ : = &f(\lambda^*_m). \end{align*} |
Set
Z = [\gamma_h(\mu_h {\rm{I_d}}+\gamma_h+\delta_h )^{-1}\Theta\boldsymbol{e} \nu_h (\nu_h+\mu_h+g )^{-1}(1-p)+g (g +\mu_h {\rm{I_d}})^{-1}p+g (\nu_h+\mu_h+g )^{-1}(1-p)]\Phi, |
then
\begin{pmatrix} S^*_h \\ R^*_h \end{pmatrix}: = f(\lambda^*_m) = \begin{pmatrix} \Lambda_h[\mu_h+(\mathbf{1_2}-\rho_h \mathbf{1_4} (\mu_h+\rho_h)^{-1} {\rm{I_d}}Z)\lambda^*_m]^{-1}\\ \Lambda_h(\mu_h+\rho_h)^{-1} {\rm{I_d}}Z[\mu_h+(\mathbf{1_2}-\rho_h \mathbf{1_4} (\mu_h+\rho_h)^{-1} {\rm{I_d}}Z)\lambda^*_m]^{-1}\lambda^*_m \end{pmatrix}. |
Consequently
\begin{pmatrix} A^*_h \\ P^*_h\\I^*_h \end{pmatrix} = \begin{pmatrix} (\nu_h+\mu_h+g )^{-1}{\rm{I_d}} (1-p)\Phi \lambda^*_m & 0_{4\times4}\\ (g +\mu_h)^{-1} {\rm{I_d}}p\Phi \lambda^*_m & 0_{4\times4}\\ (\mu_h{\rm{I_d}}+\gamma_h+\delta_h)^{-1} \Theta\boldsymbol{e} \nu_h(\nu_h+\mu_h+g )^{-1}{\rm{I_d}} (1-p)\Phi \lambda_m & 0_{4\times4} \end{pmatrix} f(\lambda^*_m). |
i.e.,
\begin{align*} \begin{pmatrix} A_h^* \\ P_h^*\\ I_h^* \end{pmatrix} = &\begin{pmatrix} (\nu_h+\mu_h+g )^{-1} (1-p)\Phi\Lambda_h[\mu_h+(\mathbf{1_2}-\rho_h \mathbf{1_4} (\mu_h+\rho_h)^{-1} {\rm{I_d}}Z)\lambda^*_m]^{-1} \lambda^*_m\\ (g +\mu_h)^{-1} {\rm{I_d}}p\Phi\Lambda_h[\mu_h+(\mathbf{1_2}-\rho_h \mathbf{1_4} (\mu_h+\rho_h)^{-1} {\rm{I_d}}Z)\lambda^*_m]^{-1} \lambda^*_m \\ (\mu_h{\rm{I_d}}+\gamma_h+\delta_h)^{-1} \Theta\boldsymbol{e} \nu_h(\nu_h+\mu_h+g )^{-1}{\rm{I_d}} (1-p)\Phi \Lambda_h[\mu_h+(\mathbf{1_2}-\rho_h \mathbf{1_4} (\mu_h+\rho_h)^{-1} {\rm{I_d}}Z)\lambda^*_m]^{-1} \lambda^*_m \end{pmatrix}. \end{align*} |
At the equilibrium, the total population of human is written as
N^*_h = \begin{pmatrix} 1 & 1_4 \end{pmatrix} \begin{pmatrix} S^*_h \\ R^*_h \end{pmatrix}+ \begin{pmatrix} 1_4 & 1_4&1_4 \end{pmatrix} \begin{pmatrix} A^*_h \\ P^*_h\\ I^*_h \end{pmatrix}. |
We have
\begin{align*} N^*_h = & \begin{pmatrix} 1 & 1_4 \end{pmatrix} f(\lambda^*_m)+ \begin{pmatrix} 1_4 & 1_4&1_4 \end{pmatrix} \begin{pmatrix} (\nu_h+\mu_h+g )^{-1}{\rm{I_d}} (1-p)\Phi \lambda^*_m & 0_{4\times4}\\ (g +\mu_h)^{-1} {\rm{I_d}}p\Phi \lambda^*_m & 0_{4\times4}\\ (\mu_h{\rm{I_d}}+\gamma_h+\delta_h)^{-1} \Theta\boldsymbol{e} \nu_h(\nu_h+\mu_h+g )^{-1}{\rm{I_d}} (1-p)\Phi \lambda^*_m & 0_{4\times4} \end{pmatrix} f(\lambda^*_m)\\ : = & g(\lambda^*_m) f(\lambda^*_m). \end{align*} |
With this, the two forces of infection are written as follows
\begin{align*} \lambda^*_h = & \dfrac{\beta_h}{g(\lambda^*_m) f(\lambda^*_m)}\varepsilon \begin{pmatrix} 1 & 1&1 \end{pmatrix} \begin{pmatrix} (\nu_h+\mu_h+g )^{-1}{\rm{I_d}} (1-p)\Phi \lambda^*_m & 0_{4\times4}\\ (g +\mu_h)^{-1} {\rm{I_d}}p\Phi \lambda^*_m & 0_{4\times4}\\ (\mu_h{\rm{I_d}}+\gamma_h+\delta_h)^{-1} \Theta\boldsymbol{e} \nu_h(\nu_h+\mu_h+g )^{-1}{\rm{I_d}} (1-p)\Phi \lambda^*_m & 0_{4\times4} \end{pmatrix} f(\lambda^*_m)\\ : = & J (\lambda^*_m) ,\\ \lambda^*_m = & \dfrac{1}{g(\lambda^*_m) f(\lambda^*_m)} \beta_m I^*_m. \end{align*} |
\begin{align*} J (\lambda^*_m) = & \dfrac{\beta_h}{g(\lambda^*_m) f(\lambda^*_m)}\varepsilon \begin{pmatrix} 1 & 1 & 1 \end{pmatrix} \\ &\begin{pmatrix} (\nu_h+\mu_h+g )^{-1} (1-p)\Phi\Lambda_h[\mu_h+(\mathbf{1_2}-\rho_h \mathbf{1_4} (\mu_h+\rho_h)^{-1} {\rm{I_d}}Z)\lambda^*_m]^{-1} \lambda^*_m\\ (g +\mu_h)^{-1} {\rm{I_d}}p\Phi\Lambda_h[\mu_h+(\mathbf{1_2}-\rho_h \mathbf{1_4} (\mu_h+\rho_h)^{-1} {\rm{I_d}}Z)\lambda^*_m]^{-1} \lambda^*_m \\ (\mu_h{\rm{I_d}}+\gamma_h+\delta_h)^{-1} \Theta\boldsymbol{e} \nu_h(\nu_h+\mu_h+g )^{-1}{\rm{I_d}} (1-p)\Phi \Lambda_h[\mu_h+(\mathbf{1_2}-\rho_h \mathbf{1_4} (\mu_h+\rho_h)^{-1} {\rm{I_d}}Z)\lambda^*_m]^{-1} \lambda^*_m. \end{pmatrix}. \end{align*} |
Furthermore, replacing \lambda^*_h in the two last equations of System (3.1) yields
\begin{cases} & S_m^* = (\mu_m + \mathbf{1_2} \lambda^*_h)^{-1} \Lambda_m = \left (\mu_m + \mathbf{1_2} J (\lambda^*_m) \right)^{-1} \Lambda_m ,\\ & I_m^* = \delta_m^{-1} \lambda^*_h S_m = \delta_m^{-1} J(\lambda^*_m) \left (\mu_m + \mathbf{1_2} J(\lambda^*_m) \right)^{-1} \Lambda_m. \end{cases} |
Consequently, the existence of an endemic equilibrium is given by the solution of the following fixed-point equation
\begin{equation*} \mathbb{R}^2 \ni \lambda^*_m = \dfrac{1}{g(\lambda^*_m) f(\lambda^*_m)} \beta_m \delta_m^{-1} J(\lambda^*_m) \left (\mu_m + \mathbf{1_2} J(\lambda^*_m) \right)^{-1} \Lambda^*_m: = F(\lambda^*_m) \in \mathbb{R}^2, \end{equation*} |
The system above is then rewritten as
\begin{equation*} \lambda^*_m = G(\lambda^*_m)\beta_m \delta_m^{-1} \beta_h\varepsilon \{(\nu_h+\mu_h+g )^{-1}(1-p)+(g +\mu_h)^{-1}p+(\mu_h {\rm{I_d}}+\gamma_h+\delta_h )^{-1}\Theta\boldsymbol{e} \nu_h (\nu_h+\mu_h+g )^{-1}(1-p)\}\Phi\lambda^*_m, \end{equation*} |
that is,
\begin{align} \mathcal{T}_{m}\mathcal{T}_{h}\lambda^*_m = \frac{1}{G(\lambda^*_m)} \lambda^*_m, \end{align} | (7.2) |
where
\begin{equation*} G: \lambda^*_m \in \mathbb{R}^2 \mapsto G(\lambda^*_m) = \frac{\Lambda_mG_1(\lambda^*_m)}{G_2(\lambda^*_m)G_3(\lambda^*_m)} \in \mathbb{R}, \end{equation*} |
with
\begin{align*} G_1(\lambda^*_m) = &\mu_h+(\mathbf{1_2}-\rho_h \mathbf{1_4} (\mu_h+\rho_h)^{-1} {\rm{I_d}}Z)\lambda^*_m, \\ G_2(\lambda^*_m) = & 1+\left\{\mathbf{1_4}[(\nu_h+\mu_h+g )^{-1} (1-p)+(g +\mu_h)^{-1}{\rm{I_d}}p]\Phi\right\}\lambda^*_m \\ +&\left\{\mathbf{1_4}(\mu_h{\rm{I_d}}+\gamma_h+\delta_h)^{-1} \Theta\boldsymbol{e} \nu_h(\nu_h+\mu_h+g )^{-1}{\rm{I_d}} (1-p)\Phi +\mathbf{1_4}(\mu_h+\rho_h)^{-1} {\rm{I_d}}Z\right\}\lambda^*_m,\\ G_3(\lambda^*_m) = &\Lambda_h\mu_mG_2(\lambda^*_m)+\mathbf{1_2}\beta_h\varepsilon \{(\nu_h+\mu_h+g )^{-1}(1-p)+(g +\mu_h)^{-1}p+(\mu_h {\rm{I_d}}\\ +&\gamma_h+\delta_h )^{-1}\Theta\boldsymbol{e} \nu_h (\nu_h+\mu_h+g )^{-1}(1-p)\}\Phi\lambda^*_m. \end{align*} |
Since \mathcal{T}_{m}\mathcal{T}_{h} is a positive and irreducible matrix, by the Perron–Frobenius theorem, we have
\begin{align*} &\frac{1}{G(\lambda^*_m)} = r\left(\mathcal{T}_{m}\mathcal{T}_{h}\right), \\ &\lambda^*_m = \kappa \omega, \end{align*} |
where \omega = (\omega^s, \omega^r) is the eigenvector, with \|\omega\| = 1 , associated with the principal eigenvalue r\left(\mathcal{T}_{m}\mathcal{T}_{h}\right) of the matrix \mathcal{T}_{m}\mathcal{T}_{h} , and \kappa is a positive constant to be determined.
The constant \kappa is then the solution of the equation \frac{1}{G(\lambda^*_m)} = r\left(\mathcal{T}_{m}\mathcal{T}_{h}\right) , i.e., \frac{1}{G(\kappa \omega)} = r\left(\mathcal{T}_{m}\mathcal{T}_{h}\right) , which is rewritten as
\Lambda_m r\left(\mathcal{T}_{m}\mathcal{T}_{h}\right) \frac{ G_1(\kappa\omega)}{G_2(\kappa\omega) G_3(\kappa\omega)} = 1. |
The equality above is equivalent to
\begin{equation} L(\kappa): = \Lambda_m r\left(\mathcal{T}_{m}\mathcal{T}_{h}\right) \frac{\left(\mu_h+\chi_1 \kappa\right)}{\left(1+\chi_2 \kappa \right)\left(\Lambda_h\mu_m+(\chi_2+\Lambda_h\mu_m\omega^s+\chi_3) \kappa\right)} = 1, \end{equation} | (7.3) |
with
\begin{align*} &\chi_1 = \omega^r\left( 1-a_s\right) +\omega^s\left(1-a_r\right),\\ &\chi_2 = \omega^r(b_s+a_s)+\omega^s(b_r+a_r),\\ &\chi_3 = \omega^s( c_s+d_s)+\omega^r(c_r+d_r), \end{align*} |
and
\begin{align*} a_j = & \frac{\nu_h\theta\gamma_h^{j,T}\rho_h}{(\mu_h+\gamma_h^{j,T}+\delta_h^{j,T})(\nu_h+\mu_h)(\mu_h+\rho_h) }+\frac{\nu_h\gamma_h^{j,U}\rho_h(1-\theta)}{(\mu_h+\gamma_h^{j,U}+\delta_h^{j,U})(\nu_h+\mu_h)(\mu_h+\rho_h)},\\ b_j = & \frac{\theta\nu_h(1-p)}{(\mu_h+\gamma^{j,T}_h+\delta^{j,T}_h)(\nu_h+\mu_h+g )}+\frac{(1-\theta)\nu_h(1-p)}{(\mu_h+\gamma^{j,U}_h+\delta^{j,U}_h)(\nu_h+\mu_h+g )}+\frac{(1-p)}{(\nu_h+\mu_h+g )} +\frac{p}{(g +\mu_h)},\\ c_j = &\left(\frac{(1-p)\phi}{(\nu_h+\mu_h+g )}+\frac{p\phi}{(g +\mu_h)}+\frac{\theta(1-p)\nu_h}{(\mu_h +\gamma^{j,T}_h+\delta^{j,T}_h )(\nu_h+\mu_h+g )}\right)((1-\varepsilon_j)\beta_h^s+\varepsilon_j\beta_h^r),\\ d_j = & \beta_h^j\left( \frac{(1-p)\nu_h(1-\theta)}{(\mu_h +\gamma^{j,U}_h+\delta^{j,U}_h )(\nu_h+\mu_h+g )}+\frac{(1-p)(1-\phi)}{(\nu_h+\mu_h+g )}+\frac{p(1-\phi)}{(g +\mu_h)}\right). \end{align*} |
Since L(0) = \Lambda_m r\left(\mathcal{T}_{m}\mathcal{T}_{h}\right) \frac{\mu_h}{\Lambda_h \mu_m} = \frac{S_m^0}{S_h^0}r\left(\mathcal{T}_{m}\mathcal{T}_{h}\right) = \mathcal{T}_0^2 , equality (7.3) is rewritten as \mathcal{T}_0^2 -parametric equation
\begin{equation} L(\mathcal{T}_0^2,\kappa) = 1, \end{equation} | (7.4) |
such that L(1, 0) = 1 .
Then, using the implicit function theorem, we get
\left. {\frac{ {{\rm{d}}} \kappa}{ {{\rm{d}}} \mathcal{T}_0^2}} \right|_{(\mathcal{T}_0^2 = 1,\kappa = 0)} = -\frac{\partial_{\mathcal{T}_0^2} L(1,0)}{\partial_{\kappa} L(1,0)}. |
We have
\partial_{\mathcal{T}_0^2} L(1,0) = 1, |
and
\partial_{\kappa} L(1,0) = \frac{\Lambda_mS_h^0}{S_m^0(\Lambda_h\mu_m)^2} K, |
with
K = \Lambda_h\mu_m \chi_1- \left(2\chi_2 +\Lambda_h\mu_m\omega^s+ \chi_3 \right)\mu_h. |
A backward bifurcation occurs at \mathcal{T}_0^2 = 1 if and only if
\left. {\frac{ {{\rm{d}}} \kappa}{ {{\rm{d}}} \mathcal{T}_0^2}} \right|_{(\mathcal{T}_0^2 = 1,\kappa = 0)} < 0 |
which is equivalent to \partial_{\kappa} L(1, 0) > 0 , that is, K > 0 .
Similarly, a forward bifurcation occurs at \mathcal{T}_0^2 = 1 if and only if
\left. {\frac{ {{\rm{d}}} \kappa}{ {{\rm{d}}} \mathcal{T}_0^2}} \right|_{(\mathcal{T}_0^2 = 1,\kappa = 0)} > 0 |
which is equivalent to \partial_{\kappa} L(1, 0) < 0 , that is, K < 0 .
Furthermore, for all \mathcal{T}_0 , we find that L(\mathcal{T}_0^2, 0) = \mathcal{T}_0^2 and \lim_{\kappa\to \infty} L(\mathcal{T}_0^2, \kappa) = 0 . Therefore, if \mathcal{T}_0^2 > 1 , then at least one solution \kappa to the equation L(\mathcal{T}_0^2, \kappa) = 1 exists. Next, assume that \mathcal{T}_0^2 = 1 and K > 0 . Then, on one hand, we have L(1, 0) = 1 and \partial_{\kappa} L(1, 0) > 0 . Hence, we obtain L(1, \kappa_0) > 1 for any \kappa_0 > 0 that is sufficiently small. Consequently, at least one \kappa > 0 exists such that L(1, \kappa) = 1 .
Finally, the uniqueness of a positive \kappa satisfying L(k) = 1 is obtain if the function \kappa\longmapsto L(\mathcal{T}_0^2, \kappa) is strictly decreasing on \mathbb{R}_+ . Indeed, since L(\mathcal{T}_0^2, 0) = \mathcal{T}_0^2 , we readily see that a unique \kappa > 0 exists such that L(\mathcal{T}_0^2, \kappa) = 1 . We also note that a forward bifurcation occurs in this configuration since here, we have K < 0 .
The authors declare they have not used artificial intelligence (AI) tools in the creation of this article.
This work received support from the African Consortium in Modeling for Effective Vector Control (ACoMVeC) project INV-047049. The sponsors had no role in study design, data collection and analysis, decision to publish or manuscript preparation.
The authors would like to thank the anonymous referees for the valuable comments which helped to improve the overall quality of the manuscript.
The authors of this article declare that they have no financial conflict of interest with the content of this article.
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Parameters | Description (unit) | Value [Ref] |
\phi | Rate of exposure of asymptomatic and paucisymptomatic infections to antimalarial treatment without a curative intention | (0;1) |
\theta | Rate of exposure of clinical cases to antimalarial treatment with a curative intention | (0;1) |
q_{\rm{mda}} | Proportion of humans under MDA | (0;1) |
\varepsilon_s | Probability of mutation from treated sensitive human infections to treated resistant human infections | 10^{-1}-10^{-3} (assumed) |
\bar{\gamma}_h | Ratio of the recovered rate | (0;1) |
\bar{\delta}_h | Ratio of the additional mortality rate of humans due to disease | (0;1) |
\bar{\varepsilon} | Ratio of the mutation rate | (0;1) |
\bar{\beta}_m | Ratio of the infection rate of human by infectious mosquitoes | (0;1) |
\bar{\delta}_m | Ratio of the mortality rate of infectious mosquitoes | (0;1) |
{\rm{InitPrevR}} | Initial prevalence of drug resistance within the host population | \{10^{-1}, 10^{-3}\} (assumed) |
\varepsilon_r | Probability of mutation from treated resistant human infections to treated sensitive human infections (day ^{-1} ) | \bar{\varepsilon}\varepsilon_s |
\delta_h^{r, T} | Additional death rate of treated infectious humans to resistant infection (day ^{-1} ) | \bar{\delta}_h \delta_h^{s, U} |
\beta_m^r | Resistant infection rate of human by infectious mosquitoes (day ^{-1} bites ^{-1} ) | \bar{\beta}_m\beta_m^s |
\delta_m^r | Mortality rate of mosquitoes with resistant infection (day ^{-1} ) | \bar{\delta}_m\delta_m^s |
\gamma_{h}^{r, T} | Recovery rate of treated humans to resistant infection (day ^{-1} ) | \bar{\gamma}_h\gamma_h^{s, T} |
Parameters | Description (unit) | Value [Ref] |
\mathcal{T}_{0, 0} | Basic reproduction number for \phi=0, \; \theta=0, \; \text{and}\; g=0 | 5 (assumed) |
\gamma_{h}^{s, T} | Recovery rate of treated humans to sensitive infection (day ^{-1} ) | 0.0035 [15] |
\gamma_{h}^{s, U} | Recovery rate of untreated humans to sensitive infection (day ^{-1} ) | 0 (assumed) |
\gamma_{h}^{r, U} | Recovery rate of untreated humans to resistant infection (day ^{-1} ) | 0 (assumed) |
\beta_{h}^s | Sensitive infection rate of mosquitoes by infected humans (day ^{-1} bites ^{-1} ) | \beta_h defined by (4.1) |
\beta_{h}^r | Resistant infection rate of mosquitoes by infected humans (day ^{-1} bites ^{-1} ) | \beta_h defined by (4.1) |
\beta_{m}^s | Sensitive infection rate of humans by infectious mosquitoes (day ^{-1} bites ^{-1} ) | 0.022 [15] |
\delta_{h}^{s, T} | Additional death rate of treated infectious humans from sensitive infection (day ^{-1} ) | 0 (assumed) |
\delta_{h}^{s, U} | Additional death rate of untreated infectious humans from sensitive infection (day ^{-1} ) | 1/5 [15] |
\delta_{h}^{r, U} | Additional death rate of untreated infectious humans from resistant infection (day ^{-1} ) | 9\times 10^{-5} [15] |
\Lambda_{h} | Recruitment rate of susceptible humans (day ^{-1} humans) | 102 (assumed) |
\mu_{h} | Natural mortality rate of humans (day ^{-1} ) | 0.00224 (assumed) |
\mu_{m} | Natural mortality rate of mosquitoes (day ^{-1} ) | 1/20 (assumed) |
\Lambda_{m} | Recruitment rate of susceptible mosquitoes (day ^{-1} mosquitoes) | 100 (assumed) |
\delta_m^s | Mortality rate of mosquitoes with sensitive infection (day ^{-1} ) | 0.033 [15] |
\rho_{h} | Loss of immunity rate of recovered humans (day ^{-1} ) | 5.5\times 10^{-4} [15] |
\nu_{h} | The rate at which asymptomatic humans become infectious (day ^{-1} ) | 0.1 [15] |
p | The proportion of paucisymptomatic infections (day ^{-1} ) | 0.7 (assumed) |
D_{\rm{mda}} | Delay to being no longer a carrier after MDA (days) | 1 [16] |
c_h | Balancing coefficients in the objective function ($ per person) | 1 (assumed) |
b_h | Balancing coefficients in the objective function ($ per person) | 1 (assumed) |
T_f | End time of controls (year) | 10 (assumed) |
Cost of control | ||
c_\phi | Cost of \phi ($ per person) | 10 [17,18,19] |
c_\theta | Cost of \theta ($ per person) | 3-20 [17,18,19] |
c_g | Cost of MDA ($ per person) | 3-20 [17,18,19] |
Parameters | Description (unit) | Value [Ref] |
\phi | Rate of exposure of asymptomatic and paucisymptomatic infections to antimalarial treatment without a curative intention | (0;1) |
\theta | Rate of exposure of clinical cases to antimalarial treatment with a curative intention | (0;1) |
q_{\rm{mda}} | Proportion of humans under MDA | (0;1) |
\varepsilon_s | Probability of mutation from treated sensitive human infections to treated resistant human infections | 10^{-1}-10^{-3} (assumed) |
\bar{\gamma}_h | Ratio of the recovered rate | (0;1) |
\bar{\delta}_h | Ratio of the additional mortality rate of humans due to disease | (0;1) |
\bar{\varepsilon} | Ratio of the mutation rate | (0;1) |
\bar{\beta}_m | Ratio of the infection rate of human by infectious mosquitoes | (0;1) |
\bar{\delta}_m | Ratio of the mortality rate of infectious mosquitoes | (0;1) |
{\rm{InitPrevR}} | Initial prevalence of drug resistance within the host population | \{10^{-1}, 10^{-3}\} (assumed) |
\varepsilon_r | Probability of mutation from treated resistant human infections to treated sensitive human infections (day ^{-1} ) | \bar{\varepsilon}\varepsilon_s |
\delta_h^{r, T} | Additional death rate of treated infectious humans to resistant infection (day ^{-1} ) | \bar{\delta}_h \delta_h^{s, U} |
\beta_m^r | Resistant infection rate of human by infectious mosquitoes (day ^{-1} bites ^{-1} ) | \bar{\beta}_m\beta_m^s |
\delta_m^r | Mortality rate of mosquitoes with resistant infection (day ^{-1} ) | \bar{\delta}_m\delta_m^s |
\gamma_{h}^{r, T} | Recovery rate of treated humans to resistant infection (day ^{-1} ) | \bar{\gamma}_h\gamma_h^{s, T} |
Parameters | Description (unit) | Value [Ref] |
\mathcal{T}_{0, 0} | Basic reproduction number for \phi=0, \; \theta=0, \; \text{and}\; g=0 | 5 (assumed) |
\gamma_{h}^{s, T} | Recovery rate of treated humans to sensitive infection (day ^{-1} ) | 0.0035 [15] |
\gamma_{h}^{s, U} | Recovery rate of untreated humans to sensitive infection (day ^{-1} ) | 0 (assumed) |
\gamma_{h}^{r, U} | Recovery rate of untreated humans to resistant infection (day ^{-1} ) | 0 (assumed) |
\beta_{h}^s | Sensitive infection rate of mosquitoes by infected humans (day ^{-1} bites ^{-1} ) | \beta_h defined by (4.1) |
\beta_{h}^r | Resistant infection rate of mosquitoes by infected humans (day ^{-1} bites ^{-1} ) | \beta_h defined by (4.1) |
\beta_{m}^s | Sensitive infection rate of humans by infectious mosquitoes (day ^{-1} bites ^{-1} ) | 0.022 [15] |
\delta_{h}^{s, T} | Additional death rate of treated infectious humans from sensitive infection (day ^{-1} ) | 0 (assumed) |
\delta_{h}^{s, U} | Additional death rate of untreated infectious humans from sensitive infection (day ^{-1} ) | 1/5 [15] |
\delta_{h}^{r, U} | Additional death rate of untreated infectious humans from resistant infection (day ^{-1} ) | 9\times 10^{-5} [15] |
\Lambda_{h} | Recruitment rate of susceptible humans (day ^{-1} humans) | 102 (assumed) |
\mu_{h} | Natural mortality rate of humans (day ^{-1} ) | 0.00224 (assumed) |
\mu_{m} | Natural mortality rate of mosquitoes (day ^{-1} ) | 1/20 (assumed) |
\Lambda_{m} | Recruitment rate of susceptible mosquitoes (day ^{-1} mosquitoes) | 100 (assumed) |
\delta_m^s | Mortality rate of mosquitoes with sensitive infection (day ^{-1} ) | 0.033 [15] |
\rho_{h} | Loss of immunity rate of recovered humans (day ^{-1} ) | 5.5\times 10^{-4} [15] |
\nu_{h} | The rate at which asymptomatic humans become infectious (day ^{-1} ) | 0.1 [15] |
p | The proportion of paucisymptomatic infections (day ^{-1} ) | 0.7 (assumed) |
D_{\rm{mda}} | Delay to being no longer a carrier after MDA (days) | 1 [16] |
c_h | Balancing coefficients in the objective function ($ per person) | 1 (assumed) |
b_h | Balancing coefficients in the objective function ($ per person) | 1 (assumed) |
T_f | End time of controls (year) | 10 (assumed) |
Cost of control | ||
c_\phi | Cost of \phi ($ per person) | 10 [17,18,19] |
c_\theta | Cost of \theta ($ per person) | 3-20 [17,18,19] |
c_g | Cost of MDA ($ per person) | 3-20 [17,18,19] |