Chronic immune activation is a characteristic of HIV disease progression. Immune-activation-driven apoptosis of CD4+ cells, more than a direct virological pathogenic effect, is responsible for the decline in CD4+ T-lymphocytes seen in HIV infection 27. HIV triggers polyclonal B cell activation, increased T cell turnover, production of proinflammatory cytokines and increased numbers of activated T cells 28. CD4+ T cells that express activation markers such as CD69, CD25, and MHC class II are a prime target for HIV infection and a source of active HIV replication. Increased numbers of these activated T cells correlate with HIV disease progression 293031. Another important surface marker of cell activation is CD38. In HIV negative individuals, CD38 is expressed in relatively greater numbers by naïve lymphocytes, while in HIV infection, memory T-cells, particularly CD8+ memory T-cells, express the largest quantities of CD38 3233. CD8+CD38+T-cell levels correlate strongly with HIV-RNA levels, decreasing with ART-induced virological suppression and increasing with transient viremia, suggesting that continuously high levels of CD38+ cells may be an indicator of ongoing viral replication 32333435. Indeed, HIV replication has been nominated the main driving force behind CD8+ T-cell activation 3233. Similar to the stabilization of HIV-RNA levels following initial infection, an immune activation "set point" has also been described and shown to have prognostic value 36.

Despite the strength of the relationship with HIV-RNA, the search for a clear association between CD8+ T-cell activation and CD4 count has resulted in conflicting findings 32333537. In contrast, CD4+ T-cell activation has a considerable influence on CD4+ T-cell decline 273435. One prospective study of 102 seroconverters has found that CD8+CD38+ proportions lose their prognostic significance over time and only elevated CD4+CD38+ percentage is associated with clinical deterioration at 5 years follow up 27. The clinical value of monitoring CD38 expression is yet to be clarified, however, there is no doubt that disease progression is related to both CD4+ and CD8+ T-cell activation as indicated by expression of CD38.

A switch from T-Helper Type 1 (TH1) to T-Helper Type 2 (TH2) cytokine response is seen in HIV-related immune dysfunction and is associated with HIV disease progression. TH1 cytokines such as interleukin (IL)-2, IL-12, IL-18 and interferon-γ promote strong cellular responses and early HIV viremic control while TH2 cytokines, predominantly modulated by IL-1β, IL-4, IL-6, IL-10 and tumor necrosis factor-α (TNF-α), promote HIV viral replication and dampen cellular response to HIV 838. HIV-positive individuals have high plasma IL-10 levels, reduced production of IL-12 and poor proliferation of IL-2 producing CD4+ central memory T-cells 303940. Levels of pro-inflammatory cytokines such as TNF-α are also increased, causing CD8+ T-cell apoptosis 140.

Soluble markers of immunological activity have been the focus of many studies over the years in the hope that they will show utility as prognostic indicators. Unfortunately, the product of these endeavours is a large number of studies with apparently conflicting results, some studies linking elevated levels of these markers with more rapid disease progression 414243444546, and others finding no correlation 464748. Factors investigated include neopterin 414243454648, β₂-microglobulin 42464748, tumour necrosis factor type II receptor 4146, tumour necrosis factor receptor 75 45, endogenous interferon 43 and tumour necrosis factor-α 25. The lack of specificity of these markers for HIV infection appears to curtail their utility. Current treatment guidelines make no mention of their use for either disease or therapeutic monitoring 64950. As the immune response to HIV is clarified with further research, the utility of monitoring these immune modulators may become more apparent.

The value of HIV-RNA quantification as a prognostic marker has long been established 65152. An approximately inverse relationship to the CD4+ T-cell count and survival time has been observed in around 80% of patients 5354. Higher HIV-RNA levels are associated with more rapid decline of CD4+ T-cells, assisting prediction of the rate of CD4 count decline and disease progression. However, once the CD4 count is very low (<50–100 cells/mm³), the disease progression risk is so great that HIV-RNA levels add little prognostic information 25545556. The correlation between CD4 count and disease progression seen clearly in Table 1 has already been described 10. Further highlighting the risk of AIDS in those with CD4 counts of 200–350 cell/mm³ (the current threshold for ART initiation), a four-fold risk increase can be seen between those with a HIV-RNA of 3000 copies/mL and those with ≥300 000 copies/mL, even within the same age bracket. Additionally, there is a considerable increase in risk of disease progression in those with HIV-RNA >100 000 copies/mL across all age and CD4 strata.

Higher baseline HIV-RNA levels in early infection have been associated with faster CD4+ T-cell decline over the first two years of infection 1557. Research has suggested that HIV-RNA levels at later time points are better indicators of long term disease progression than levels at seroconversion, with the viral load reaching a stable mean or 'set point' around one year after infection 412525859. Indicative of the efficiency of immunological control of viral replication, this set point is strongly associated with the rate of disease progression as can be inferred from Figure 115259606162. Desquilbet et al. 63 studied the effect of early ART on the virological set point by starting treatment during Primary HIV Infection (PHI) and then ceasing it soon after. They found the virological set point was mainly determined by pre-treatment viral load, early treatment having minimal reducing effect.

Treatment response has been strongly linked to the baseline HIV-RNA level; Van Leth et al. 19 finding that patients with a HIV-RNA >100 000 copies/mL were almost 1.5 times more likely to experience virological failure (HIV-RNA >50 copies/mL) after 48 weeks of treatment than those with HIV-RNA <100 000 copies/mL.

An analysis of a subgroup (6814 participants) of the EuroSIDA study cohort verified that clinical outcome correlates strongly with most recent CD4+ T-cell or HIV RNA level, regardless of ART regimen used. In particular, it is worth noting that those with CD4 count ≤350 cells/mm³ were at increased risk of AIDS or death than higher CD4 counts (rate ratio ≥3.39 vs ≤1.57), while the risk of these outcomes was substantially lower at HIV-RNA <500 copies/mL compared to >50 000 copies/mL (rate ratio 0.22 vs 0.61) 64. These findings support the continued use of HIV-RNA and CD4 count as markers of disease progression on any HAART regimen 65165.

There is no doubt that monitoring viral load is critical to assessing the efficacy of ART 65666768. Findings from multiple studies reinforce the association between greater virological suppression and sustained virological response to ART 650. Guidelines define virological failure as either a failure to achieve an undetectable HIV-RNA (<50 copies/mL) after 6 months or a sustained HIV-RNA >50 copies/mL or >400 copies/mL following suppression below this level 6. A greater than threefold increase in viral load has been associated with increased risk of clinical deterioration and so this value is recommended to guide therapeutic regimen change in the developed world 6970. Several studies have shown a significant correlation between HIV-RNA >10 000 copies/mL and increased mortality and morbidity, and therapeutic switching should occur prior to this point 49. The World Health Organisation recommends that this level be considered the definition of virological failure in resource limited settings 49.

Some patients experience intermittent episodes of low-level viremia followed by re-suppression below detectable levels, known as "blips". A very detailed study by Nettles et al. 71 defined a typical blip as lasting about 2.5 days, of low magnitude (79 copies/ml) and requiring no change in therapy to return to <50 copies/ml. Havlir et al. 72 and Martinez et al. 73 demonstrated that there was no association between intermittent low-level viremia and virological failure. Intermittent viremia does not appear to be a significant risk factor for disease progression. Nevertheless, it must be distinguished from true virological failure, which is consistently elevated HIV-RNA, as defined above. Continued follow up is essential.

Even in patients achieving apparently undetectable HIV-RNA levels, the HIV virus persists through the infection of memory T-cells 7475. This 'viral reservoir' has an extremely long half life and remains remarkably stable even in prolonged virological suppression 747677. Responsible for the failure of ART to eradicate infection, regardless of therapy efficacy, it may also contribute to the 'blips' described above 76. Like intermittent viremia, its effect on disease progression appears trivial, being mainly of therapeutic importance 7879. However, as the long-term clinical outcomes of viral resistance and sub-detection viral replication become clearer, its significance may increase 15.

Drug resistance is a strong predictor of virological failure after HAART, with a clear relationship seen between the number of mutations and virological outcome 568081828384. Hence maximal suppression of viral replication, with the parallel effect of preventing the development of resistance, is essential to optimise both response to treatment and improvement in disease progression 8586.

The transmission of resistant virus is a serious reality, with implications for the efficacy of initial regimens in ART naïve patients. Prevalence of resistance mutations amongst seroconverters varies according to geographic location, with inter-country prevalence varying from 3–26%. This reinforces the need to gain local data, especially as resistance increases with increasing HAART use 87. In the USA, the prevalence of primary (transmitted) resistance was 24.1% in 2003–2004, an almost two-fold increase from the 13.2% prevalence recorded in 1995–1998 88. European prevalence for 2001–2002 was 10.4%, which, although lower than the US figures, remains quite high 8687. Pre-treatment resistance testing has been shown to reduce the risk of virological failure in patients with primary drug resistance 650. The DHHS guidelines suggest that pre-treatment resistance testing in ART naïve patients may be considered if the risk of resistance is high (ie: population prevalence ≥5%) while the British HIV Association (BHIVA) recommends testing for transmitted resistance in all newly diagnosed patients and prior to initiating ART in chronically infected patients 49. In resource-limited settings, resistance testing may not be readily available; however, in such locations, primary resistance is likely to be rare, and need for pre-treatment resistance testing is lower 89. An exception to this rule is the case of child-bearing women who have received intrapartum nevirapine, in whom poorer virological responses to post-partum nevirapine based regimens have been seen (49% vs 68% achieved HIV-RNA <50 copies/mL at 6 months) 4989. Regardless of the setting, there is a need for surveillance of local drug resistance prevalence 1290.

CCR5 and CXCR4 chemokine receptors act as co-receptors for HIV virions. Proportionately greater tropism for one or the other of these receptors has been associated with different rates of disease progression. Slowly progressing phases of infection are associated with predominance of the "R5 virus strains" that ligate the CCR5 receptor, mainly present on activated immune cell surfaces (including macrophages). "X4 strains" showing tropism for CXCR4, expressed by naïve or resting T-cells, and dual-tropic R5X4 strains, increase proportionately in the later stages of disease and are associated with more rapid clinical and immunological deterioration 1290. 'X4' strains have been associated with greater immune activation, suggesting a possible mechanism for their effects on disease progression 27. Patients with predominantly X4 strains have been found to have lower CD4 counts, but correlations with viral load have been inconsistent 909192. Some host genetic phenotypes namely CCR5-Δ32 and SDF-1'A, affect R5 strain binding and are associated with delayed disease progression 939495.

It is evident that even under effective HAART suppression 96, the predominant viral strain can change from R5 to X4 909297. Additionally, about 50% of triple therapy experienced patients have been found to harbour X4 strains, a far greater proportion than the 18.2% seen in an ART naïve population 98. The evidence for a difference in survival between those on HAART with X4 strains and those with R5 strains is difficult to interpret. Brumme et al. 98 suggested that a group of patients with the 11/25 envelope sequence (a highly specific predictor of the presence of X4 strains) had higher mortality and poorer immunological response to HAART despite similar virological responses to those without the 11/25 sequence. In contrast, a later study indicated that after adjustment for baseline characteristics, X4 strains were not associated with a difference in survival or response to HAART 99. As can be seen, the effects of chemokine receptor tropism remain controversial and as yet, there is no clear evidence that monitoring or measuring these parameters will be useful clinically.

Complicating the assessment of the effect of viral subtype on disease progression are the potential confounders such as race, prevalence of various opportunistic infections and access to health care. Subtype C affects 50% of people with HIV and is seen mostly in Southern and Eastern Africa, India and China. Subtype D is found in East Africa and Subtype CRF_01 AE is seen mainly in Thailand. Caucasians are predominantly infected by subtype B, seen in 12% of the global HIV infected population 99. The majority of research on all aspects of HIV has been performed amongst subtype B-affected individuals. The implications for treatment practice are obvious should differences in viral pathogenicity or disease progression exist between subtypes 99100.

Rangsin et al. 100 noted median survival times in young Thai men (Type E 97%) of only 7.4 years, significantly shorter than the 11.0 years reported by the mainly Caucasian CASCADE cohort (Type B ≥50%). Hu et al. 101 found differences in early viral load between those with Type E (n = 103) when compared to Type B (n = 27) in Thai injecting drug users. Kaleebu et al. 102 studied a large cohort in Uganda, providing the strongest evidence for a difference in survival between A and D subtypes. However, analysis of a small cohort in Sweden reported no difference in survival rates between subtypes A-D 103. Only Rangsin et al. 100 and Hu et al. 101 studied cohorts with estimable seroconversion dates.

It is difficult to control for the multiple potential confounding factors in research measuring the influence of subtype on disease progression. Geretti 99 remarked that the evidence for survival and disease progression rate differences between subtypes is currently inadequate to draw any definitive conclusions. Ongoing research is essential not only to determine the effect of subtype on disease progression but also to evaluate response to therapy.

Many of the confounding factors affecting subtype investigation also confound research into the effect of race on disease progression. Studies with clinical endpoints have found no significant relationship between race and disease progression 104105, while another study of clinical response to HAART suggested disease progression appears to correlate more strongly with other factors (eg: depression, drug toxicity) than with race per se 106. In support of this, data from the TAHOD databaseⁱⁱ (see Appendix 1 for details) suggests that responses to HAART among Asians are comparable to those seen in other races 11. Evidence for racial variation in viral loads and CD4 counts has not been consistent and confounders have been difficult to exclude 107108109. Morgan et al. 110 reported a median survival time of 9.8 years amongst HIV infected Ugandans which does not differ greatly from the 11.0 years reported by the mainly Caucasian CASCADE cohort. Race as an independent factor does not appear to play a part in the rate of disease progression independently of confounders such as psychosocial factors, access to care and genetically driven response to therapy.

An understanding of the effect of host genetics on disease susceptibility and progression has significant implications for the development of therapies and vaccines 95. Host genetics impact HIV infection at two main points: (i) cell-virion fusion, mediated primarily by the chemokine receptors CXCR4 and CCR5 and their natural ligands, and (ii) the host immune response, mediated by Human Leukocyte Antigen (HLA) molecules 95111.

Polymorphisms of the genes controlling these two pathways have been extensively studied and multiple genetic alleles that have been found to correlate with either delayed or accelerated disease progression 95111112.

HLA molecules provide the mechanism by which the immune system generates a specific response to a pathogen. As has been described earlier, the diversity of HIV-specific immune responses plays a crucial role in containment of the virus and it is HLA molecules that control that diversity. Thus, HLA polymorphisms should affect disease progression. Investigation of the effect of specific alleles has found that heterozygosity of any MHC Class I HLA alleles appears to delay progression, while rapid progression has been associated with some alleles in particular, for example, HLA-B35 and Cω495. The HLA-B57 allele, present in 11% of the US population and around 10% of HIV-positive individuals, has been linked to long-term non-progression, a lower viral set-point and fewer symptoms of primary HIV infection 95112.

In addition to the effect of genetic polymorphisms on the natural history of infection, host genetic profile can influence the response to HAART 113. In Australia, the presence of the HLA-B5701 allele accounts for nearly 90% of patients with abacavir hypersensitivity. Drug clearance also varies significantly between racial groups due to genetic variations in CYP enzyme isoforms 114. For example, polymorphisms of CYP2B6 occurring more frequently in people of African origin are associated with three-fold greater plasma efavirenz concentrations, leading to a greater incidence of central nervous system toxicity amongst this group 115. Potential outcomes of such phenomena include treatment discontinuation in the case of toxicity or hypersensitivity and drug resistance when medications are ceased simultaneously causing monotherapy of the drug with the prolonged half life 114. Genetic screening in order to guide choice of therapy is already underway in Australia for HLA-B57 alleles related to abacavir hypersensitivity 114. Studies of host genetics appear likely to significantly influence the clinical management of HIV in the future.

Age at seroconversion has repeatedly been found to have considerable impact on the future progression of disease. Concurring with earlier studies, the CASCADE collaboration 62 found a considerable age effect correlating with CD4 count and HIV-RNA, across all exposure categories, CD4 count and HIV-RNA strata in an analysis of multiple international seroconversion cohorts, reinforcing these findings again recently 10117118. Table 1 clearly demonstrates the importance of stratification by age, CD4 count and HIV-RNA as predictive of the short term risk of AIDS. There is a clear relationship between increasing risk with increasing age. For example, a 25 year old with a CD4 count of 200 and HIV-RNA level of 3000 has one third the risk of disease progression when compared to a 55 year old. This raises the issue of whether or not older patients should be treated at higher CD4+ T-cell counts 10.

Older age is associated with lower CD4 counts at similar time from seroconversion which may explain the relationship between age and disease progression 57119. However, age disparities seem to diminish with HAART treatment; CD4 counts and HIV-RNA levels becoming more useful prognostic indicators 119. It appears that the age effect seen on HAART treatment is closer to the natural effect of aging rather than the pre-treatment, HIV-related increase in mortality, suggesting that HAART attenuates the effect of age at seroconversion on HIV disease progression 120.

Mean HIV-RNA has been found to vary between men and women for given CD4 count strata 107121122123. Low levels of CD4+ T-cells (<50 cells/mm³) are associated with higher mean HIV-RNA in women (of the order of 1.3 log₁₀copies/mL) than in men within the same CD4 count stratum. Conversely, at higher CD4+ T-cell levels (>350 cells/mm³), mean HIV-RNA has been noted to be 0.2–0.5 log₁₀copies/mL lower in women 124. Despite HIV-RNA variation, disease progression has not been seen to differ between the genders for given CD4 counts 121124125. On this basis, the current DHHS Guidelines for the use of Antiretroviral Drugs in HIV-1 Infected Adults and Adolescents state that there is no need for sex-specific treatment guidelines for the initiation of treatment given that antiretroviral therapy initiation is guided primarily by CD4 count 6.

Comparing disease progression rates between transmission risk groups has led to conflicting findings. An early study found significantly faster progression amongst homosexuals than heterosexuals 126. However, more recent studies analysing much larger cohorts reported no difference in disease progression rates following adjustment for age and exclusion of Kaposi's sarcoma as an AIDS defining illness 62127128. Prins et al. 127 noted that injecting drug users have a very high other-cause mortality rate that could confound results failing to take this into account.

The CASCADE collaboration 120 examined the change in morbidity and mortality between the pre- and post-HAART periods. They found a reduction in mortality in the post-HAART era amongst homosexual and heterosexual risk groups but no such change in injecting drug users. This apparently higher risk of death than other groups may be related to poor therapy adherence, less access to HAART and the higher rate of co-morbid illnesses such as Hepatitis C. Other factors may have a larger role to play in clinical deterioration than the mode of transmission.

Understanding the interaction between physical and psychosocial factors in disease progression is important to maximise holistic care for the patient. Several studies have found significant relationships between poorer clinical outcome and lack of satisfaction with social support, stressful life events, depression and denial-based coping strategies 129130131132. Other studies have found strong correlations between poorer adherence to therapy and depression, singleness and homelessness 106133. Patient management should include consideration of the psychosocial context and aim to provide assistance in problem areas.

Mediated by CD4+ T-lymphocytes, DTH-type responses give an indication of CD4+ T-cell function in vivo. It has been shown that DTH responses decline in parallel with CD4+ T-cells resulting in a corresponding increase in mortality 134135. Failure to respond to a given number of antigens has been suggested as a marker for the initiation of ART in resource-limited settings 135136.

Improved DTH responses have been noted with ART, although the degree of improvement appears dependent on the CD4+ nadir prior to HAART initiation 137138139. This holds implications for the timing of initiation of treatment, as delayed treatment and hence low nadir CD4 counts may cause long-term immune deficits 139. There is a need for further research in resource-limited settings to determine the utility of DTH testing as both a marker for HAART initiation and a means of monitoring its efficacy.

Another marker available in resource-limited countries, total lymphocyte count (TLC), has been investigated as an alternative to CD4+ T-cell count. Current WHO guidelines recommend using 1200 cells/mm³ or below as a substitute marker for ART initiation in symptomatic patients 140. Evidence for the predictive worth of this TLC level is encouraging, with several large studies confirming the significant association between a TLC of <1200 cells/mm³ and subsequent disease progression or mortality 135141142. Others propose that rate of TLC decline should be used in disease monitoring as a rapid decline (33% per year) precedes the onset of AIDS by 1–2 years 142143. Disappointingly, there is generally a poor correlation between TLC and CD4 count at specific given values.

While TLC measurement has been validated as a means of monitoring disease progression in ART-naïve patients, its use for therapeutic monitoring is questionable and not recommended 49144145146.

The body mass index (BMI) is a simple and commonly used measure of nutritional status. Its relationship to survival in HIV infection is important for two main reasons. Firstly, 'wasting syndrome' (>10% involuntary weight loss in conjunction with chronic diarrhoea and weakness, +/- fever) is considered an AIDS defining illness according to the CDC classification of disease 1. Secondly, the ease of measurement of this parameter makes it potentially highly useful as a marker for the initiation of ART in resource limited countries.

Like TLC, long-term monitoring of BMI is predictive of disease progression. A rapid decline has been noted in the 6 months preceding AIDS although the sensitivity of this measure was only 33% 145146. A baseline BMI of <20.3 kg/m² for men and <18.5 kg/m² for women is predictive of increased mortality, even in racially diverse cohorts, with a BMI of 17–18 kg/m² and <16 kg/m² being associated with a 2-fold and 5-fold risk of AIDS respectively 147148149.

In combination with other simple markers such as haemoglobin, clinical staging and TLC, a BMI <18.5 kg/m² shows similar utility to CD4 count and HIV-RNA based guidelines for the initiation of HAART 150151. A sustained BMI <17 kg/m² 6 months after HAART initiation has been associated with a two-fold increase in risk of death 152.

As can be seen, measurement of the body mass index is a simple and useful predictor of disease progression. A BMI of <18.5 kg/m² was consistently strongly associated with increased risk of disease progression and may prove to be a valuable indicator of the need for HAART.

Haemoglobin levels reflect rapidity of disease progression rates and independently predict prognosis across demographically diverse cohorts 151153. Rates of haemoglobin decrease also correlate with falling CD4 counts 135141.

There have been suggestions that increases in haemoglobin are predictive of treatment success when combined with a TLC increase 143. While racial variation in normal haemoglobin ranges and the side effects of antiretroviral agents such as zidovudine on the HIV infected bone marrow must be taken into account 144, monitoring haemoglobin levels shows utility in predicting disease progression both before and following HAART initiation.