Early HIV treatment reduces risk of serious illness and death by 44%

Starting HIV treatment at CD4 count above 500 reduces the risk of serious illness and death by 44%, African Temprano trial shows


First published on http://www.aidsmap.com/ on 26 Feb 2015


Keith Alcorn

Christine Danel presenting at CROI 2015. Photo by Liz Highleyman, hivandhepatitis.com

Starting HIV treatment at a CD4 cell count above 500 reduced the risk of serious illness including tuberculosis (TB), and death, by 44% when compared to starting treatment according to World Health Organization (WHO) guidelines, results from the seven-year Temprano study show. The findings were presented on Wednesday at the Conference on Retroviruses and Opportunistic Infections (CROI 2015) in Seattle, USA.

The study also found that a six-month course of isoniazid preventive treatment reduced the risk of developing TB by 35%.

Temprano was designed to test the safety and efficacy of early HIV treatment initiation compared to standard treatment initiation in a lower-income setting with a high prevalence of TB and bacterial infections. The study was conducted in Ivory Coast by the French AIDS research institute ANRS.

The study was also designed to test whether isoniazid preventive therapy (IPT) offered additional benefit in preventing TB for people living with HIV, over and above taking antiretroviral therapy. Despite evidence that it is effective in preventing TB in people living with HIV, IPT is not implemented in many settings, due in part to difficulties in ruling out active TB, but also because of concerns that it will lead to resistance to isoniazid in people who turn out to have active TB after starting IPT.

The study recruited previously untreated people with HIV with CD4 cell counts below 800 cells/mm3without active tuberculosis, and randomised them into four groups, taking antiretroviral therapy (ART) and isoniazid according to the following multifactorial scheme:

WHO ARTCD4 threshold for starting:March 2008-Dec 2009: <200Dec 2009-July 2012: <350July 2012-Dec 2014: <500 Arm 1 HIV treatment initiation according to CD4 count. N = 518
Arm 2 HIV treatment initiation according to CD4 count and daily isoniazid for six months. N = 517
EARLY ART Arm 3 Immediate HIV treatment initiation on study entry. N = 520
Arm 4 Immediate HIV treatment initiation on study entry and daily isoniazid for six months. N = 521

The study went through a number of protocol revisions to reflect changes in treatment guidelines.

Participants received either: tenofovir, emtricitabine and efavirenz; tenofovir, emtricitabine and lopinavir/ritonavir – for pregnant women, those with prior nevirapine exposure for PMTCT (prevention of mother-to-child transmission) and for those not using hormonal contraception; or tenofovir, emtricitabine and zidovudine for those co-infected with HIV-2.

The primary study endpoint was a composite endpoint of severe HIV morbidity, defined as all-cause mortality, any AIDS-defining event, severe bacterial disease and non-AIDS-related cancer.

The median CD4 count at study entry was 465 cells/mm3; 41% had a CD4 count above 500, 38% in the range 350 to 500 and 21% below 350. Seventy-eight per cent of study participants were women, with a median age of 35 years. Participants were followed for a median of 29 months; during this period, 58% of those randomised to the WHO arm became eligible for antiretroviral therapy and started treatment, after a median of 14.8 months in the study. Ninety per cent of those randomised to receive IPT started taking it, and of these, 94% completed the 6-month course.

The study found that early antiretroviral treatment reduced the risk of severe HIV-related illness or death by 44%, and that IPT independently reduced the risk of severe HIV-related illness or death by 35%. Both reductions in risk were statistically significant.

Severe HIV morbidity endpoints (n = 2056)

No. of events Rate per 100 person years Adjusted hazard ratio P value
WHO ART 111 4.9
EARLY ART 64 2.8 0.56 P=0.0002
NO IPT 104 4.7
IPT 71 3.0 0.65 P=0.005

The most frequent severe events were tuberculosis and bacterial infections. As in the HPTN 052 study, a large proportion of the reduction in TB cases was in disseminated rather than pulmonary TB. Whereas there were 24 pulmonary TB cases in the WHO arm and 19 in the early ART arm, there were 33 disseminated TB cases in the WHO arm and only 9 in the early ART arm.

When severe events were analysed only for those with CD4 counts above 500, in order to rule out any possible bias of changes in treatment guidelines over time, the effect of IPT ceased to be significant, but the effect of early treatment remained exactly the same as in the full trial analysis. It reduced the risk of severe events by 44%

Severe HIV morbidity endpoints in participants with baseline CD4 counts >500 cells/mm3

No. of events Rate per 100 person years Adjusted hazard ratio P value
WHO ART 38 4.1
EARLY ART 23 2.4 0.56 P=0.003
NO IPT 37 4.0
IPT 24 2.5 0.61 P=0.056 (ns)

Grade 3 and 4 adverse events were significantly more frequent in the early ART group during the first six months of treatment but thereafter they declined so that they were significantly less frequent (aHR 0.74, p = 0.003). This finding suggests that long-term drug side-effects do not cause significant morbidity in people who start treatment early.

Further analyses will be carried out to look at responses to treatment according to different CD4 counts at baseline.

The results of Temprano will lend support to the view that CD4 criteria for starting treatment should be dropped, and that the threshold for starting treatment should shift from a CD4 count of 500 to whenever the patient is ready to start, at least in lower-income settings where tuberculosis and bacterial infections are major causes of illness in people living with HIV. The START study of early treatment initiation will provide information about the risks and benefits of early treatment in developed world settings, where TB and bacterial infections do not cause substantial morbidity in people living with HIV. Results of the START study are expected in late 2016 or early 2017.


 

Reference

Danel C et al. Early ART and IPT in HV-infected African adults with high CD4 count (Temprano trial).2015 Conference on Retroviruses and Opportunistic Infections (CROI), Seattle, USA, abstract 115LB, 2015.

View a webcast of this presentation.

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