The HIV and AIDS epidemic has remained one of the leading causes of death in the world and
has been destructive in Africa with Sub-Saharan Africa remaining the epidemiological locus of
the epidemic. HIV and AIDS hinders development by erasing decades of health, economic and
social progress, reducing life expectancy by years and deepening poverty [57].The most urgent
public-health problem globally is to devise effective strategies to minimize the destruction caused
by the HIV and AIDS epidemic. Due to the problems caused by HIV and AIDS, well defined
endpoints to evaluate treatment benefits are needed. The surrogate and true endpoints for a
disease need to be specified. The purpose of a surrogate endpoint is to draw conclusions about
the effect of intervention on true endpoint without having to observe the true endpoint. It is
of great importance to understand the surrogate validation methods. At present the question
remains as to whether CD4 count and viral load are good surrogate markers for death in HIV or
there are some better surrogate markers. This dissertation was undertaken to obtain some clarity
on this question by adopting a mathematical model for HIV at immune system level and the
impact of treatment in the form of reverse transcriptase inhibitors (RTIs). For an understanding
of HIV, the dissertation begins with the description of the human immune system, HIV virion
structure, HIV disease progression and HIV drugs. Then a review of an existing mathematical
model follows, analyses and simulations of this model are done. These gave an insight into the
dynamics of the CD4 count, viral load and HIV therapy. Thereafter surrogate marker validation
methods followed. Finally generalized estimating equations (GEEs) approach was used to analyse
real data for HIV positive individuals, from the Centre for the AIDS Programme of Research
in South Africa (CAPRISA). Numerical simulations for the HIV dynamic model with treatment
suggest that the higher the treatment efficacy, the lower the infected cells are left in the body.
The infected cells are suppressed to a lower threshold value but they do not completely disappear,
as long as the treatment is not 100% efficacious. Further numerical simulations suggest that it
is advantageous to have a low proportion of infectious virions (ω) at an individual level because
the individual would produce few infectious virions to infect healthy cells. Statistical analysis
model using GEEs suggest that CD4 count< 200 and viral load are highly associated with death,
meaning that they are good surrogate markers for death. An interesting finding from the analysis
of this particular data from CAPRISA was that low CD4 count and high viral loads as surrogates
for HIV survival act independently/additively. The interaction effect was found to be insignificant.
Individual characteristics or factors that were found to be significantly associated with HIV related
death are weight, CD4 count< 200 and viral load. / Thesis (M.Sc.)-University of KwaZulu-Natal, Pietermaritzburg, 2010.
| Identifer | oai:union.ndltd.org:netd.ac.za/oai:union.ndltd.org:ukzn/oai:http://researchspace.ukzn.ac.za:10413/10365 |
| Date | 29 January 2014 |
| Creators | Ngwenya, Olina. |
| Contributors | Mwambi, Henry G. |
| Source Sets | South African National ETD Portal |
| Language | en_ZA |
| Detected Language | English |
| Type | Thesis |
Page generated in 0.002 seconds