Reduction of Mortality Rate Due to AIDS When Treatment Is Considered

AIDS is one of the most threatening diseases for human being that is caused by a virus named HIV. Here the reduction of the death rate after infected by AIDS has been discussed. A mathematical model of HIV has been formulated. Then its positivity and boundedness has been investigated. It has been shown that it is possible to minimize the mortality rate by providing the treatment to the HIV infected people. Moreover, the control of the transfer rate from the infected class to the AIDS class reduces the disease rate. The increasing of the transfer rate from the infected class to the treated class also reduces the mortality rate.


Introduction
In the last decades or so mathematical models in epidemiology are playing a very important role in analyzing the spread and control of the infectious disease that are causing a lot of human death every year. In the past, human being have been threatened by many infectious disease, most of them are caused by viruses [1]. Among them HIV is responsible for a lot of human death. Till now people are dying by this virus.
Human Immunodeficiency Virus (HIV) is a member of Lent Virus sub member family of retrovirus that produces chronic infections in the host and gradually damages the host`s immune system [2]. There are two types of HIV viruses: HIV-1 and HIV-2. Among them, HIV-1 is more dangerous. It easily transmits among the people and causes a lot of HIV infections globally every year [3]. Immediately after HIV infection, people cannot determine his/her infection. In this time, HIV infection may not show up on an HIV test, but people who have it are highly infectious and can spread the infection to others. People with chronic HIV infection may not have any HIV-related symptoms or only mild ones [4].
After being infected, people who aren't taking medicine to treat HIV, this period can last a decade or longer, but some may progress through this phase faster. People who are taking medicine to treat HIV the right way, every day may be in this stage for several decades because treatment helps keep the virus in check.
HIV is treated using a combination of medicines to fight HIV infection. This is called antiretroviral therapy (ART). ART isn't a cure, but it can control the virus so that one can live a longer, healthier life and reduce the risk of transmitting HIV to others. ART is recommended for all people with HIV, regardless of how long they've had the virus or how healthy they are. If left untreated, HIV will attack the immune system and eventually progress to AIDS.

Formulation of the Model
The total sexually-active population at time t, denoted by , is subdivided into mutually-exclusive compartments, namely susceptible Here β is the transmission rate for HIV and ! " 1 are known as the modification parameter. These modification parameters indicate that the infected individuals are more infectious than the treated class. Among these class, AIDS class is assumed to spread more infection than other two classes. In the HIV exposed class , individuals entering into this class from susceptible class at a rate λ. In the HIV exposed class individuals progress to infected class at a rate $. Individual also progresses to the treatment class ) at a rate τ ! . And Individual also progresses to the AIDS class ) at a rate δ ! . In the treatment class, individuals progress to AIDS class at a rate % . Also individuals progress to the AIDS and HIV treatment class at a rate % & . In this class, let µ + ' denotes the death rate due to the disease and ( be the natural mortality rate.
Combining all the aforementioned assumption and definitions, the model becomes: Where, " ! 1. Schematically this can be shown as follows:

Boundedness Region
Here we have used some parameters (explained in the table 2) to described the model (1). These variables are nonnegative. Also the state variables (described in table 1) are non-negative for all time 0. The total population is denoted by . Total population can be written as: The equation written above, is changing at a rate In absence of disease, i.e. for = = = = 0, we have , ,-1 ) * ( By the separation of variables we can write After integration we have Here 3 is the integrating constant which is to be determined. Let at 0, 7 . From the Eq.

Positivity of Solution
Now we need to check the positivity of the solution of the model (1). Let the initial data be < 0 , 0 , 0 , 0 , 0 = ΨA. Now we have to show that the solution set

Disease-Free Equilibrium Point
Disease free equilibrium point is denoted by 7 . To obtain the disease-free equilibrium points on Ψ ∩ ℜ ? , we need to put = = = = 0 (since in the disease-free equilibrium there is no disease). The positive DFE for this model is =

Local Stability of the Disease-Free Equilibrium
The basic reproduction number which is denoted by K 7 plays a vital role in the stability of the model. The number of new infections generated by an infected individual is known as the basic reproduction number. The associated nonnegative matrix L for the new infection terms and the non-singular M-matrix, N for the remaining transfer terms are given respectively by And N has the following expression The basic reproduction number K 7 is the spectral radius of the matrix LN 5! . The eigenvalues of the matrix LN 5! are Lemma [5]. Local stability of the disease-free equilibrium depends on the basic reproduction number. If the basic reproduction number is bigger than one, then disease-free equilibrium point locally asymptotically unstable and if the basic reproduction number is less than one, then it is locally asymptotically unstable.

Global Stability of the Disease-Free Equilibrium
Here we have used a technique established by Castillo-Chavez [6] to investigate the global stability of the diseasefree equilibrium point. We rewrite the model as: Where U = and W = ( , , , , ). Here the components of W ∈ ℝ & denotes the infected population. The disease free equilibrium is now denoted as: The condition must be met to guarantee a local asymptotic stability: Here, U * is globally asymptotically stable (GAS). Where \ = a X Y(U * , 0), is an M -matrix (the off-diagonal elements of \ are non-negative) and Ω is the region where the model makes biological sense. If the system satisfies the conditions of then the theorem below holds: Theorem [5]. The fixed point 7 = (U * , 0) is a globally asymptotically stable equilibrium of the system (6) provided that K 7 < 1 and the assumptions in (4) are satisfied.

Endemic Equilibrium of the Model
We have used a well-known technique known as the Central Manifold Theorem [6] to check the stability of the endemic equilibrium point of the model. To apply this theorem we make the following change of variables. Let S x ! , E = x " , I = x , T = x & , A = x ? = p ! + p " + p + p & + p ?
The model (1) can be rewritten in the form: The Jacobean of the system (8) is To analyze the dynamics of (8), we compute the eigenvalues of the Jacobian of (8) at the disease free equilibrium (DFE). It can be shown that this Jacobian has a right eigenvector given by: Thus we have established the following theorem: Theorem. Thus we have the following results: the endemic equilibrium point is locally stable when the basic reproduction number is bigger than one and unstable when basic reproduction number is less than one.

Numerical Simulations and Discussions
The description of the variable is shown in the    Figure 2 shows that the total infected population is increasing when the basic reproduction number K 7 1 and figure 3 shows that the infected population is decreasing when K 7 E 1. Here the value of the basic reproduction number K 7 depends on the transfer rate % ! from the infected class to treated class . The values of the reproduction number K 7 decreases with the transfer rate % ! . Thus we can minimize the mortality rate by increasing the number of the treated population. Figure 4 shows that, the prevalence is decreasing when the basic reproduction number K 7 E 1 and figure 5 shows that it is increasing when K 7 1.

Conclusions
AIDS is one of the devastating diseases for human being. Mathematical models are used to estimate the dynamics of the diseases. Here we have formulated a model describing the HIV with treatment. The findings of the study are listed below: We can minimize the mortality rate by providing the treatment to the HIV infected people. The basic reproduction number highly depends on . ! , which is the transfer rate from to class. Thus the reduction in the transfer rate from the infected rate to the AIDS class will reduce the mortality rate. The increasing of the transfer rate % ! from the infected class to the treated class also reduces the disease burden.