Diarrhoea continues to affect the quality of life of people with HIV in the modern treatment era

Roger Pebody
Published: 07 August 2018

A meta-analysis of 38 clinical trials of antiretroviral therapies (ART) conducted in the past decade found that an average of 17% of study participants suffered from diarrhoea, with no improvement in more recent studies. Diarrhoea has multiple causes and only some of these cases are likely to be due to the drugs used in the studies, but it remains a significant co-morbidity that affects people’s quality of life. The analysis was presented at the 22nd International AIDS Conference (AIDS 2018) in Amsterdam last month.

Diarrhoea in people with well-treated HIV usually has a non-infectious cause, such as ART side-effects or the effects of HIV on the gastrointestinal tract. The virus can infect the cells in the gastrointestinal tract and cause damage, especially to gut-associated immune system tissue. Such damage may not be repaired with ART and there is evidence that HIV continues to replicate in gut tissue despite virologically suppressive ART. Another possible explanation is damage to autonomic nerves in the gastrointestinal tract.

The investigators identified efficacy trials of anti-HIV drugs, conducted in the United States (including multinational trials), between 2008 and 2016, that were listed on www.clinicaltrials.gov. The incidence of diarrhoea reported in each trial was examined for both intervention and control groups.

Over 21,000 people took part in the 38 trials that were identified. In 21 trials, people took ART for the first time, with the rest being studies of people changing treatment. The drugs being taken included dolutegravir, raltegravir, elvitegravir, efavirenz, rilpivirine, atazanavir, darunavir, cobicistat, emtricitabine and tenofovir.

It is important to note that the incidence of diarrhoea reported does not reflect only new cases of diarrhoea or cases that could be attributed to a person’s HIV treatment. A trial participant might simply continue to have the diarrhoea that they already had.

The median incidence of diarrhoea was virtually identical in intervention and control arms of studies, at 17.5% and 17.9% respectively. Comparing trials conducted a decade ago with those conducted more recently, there was no change over time even though the drugs studied had changed.

The rate of diarrhoea reported amongst trial participants tended to be much higher than the rate of diarrhoea reported as an adverse event in the US Food and Drug Administration-approved package insert. For example, the label for the single-tablet regimen Stribild (elvitegravir/cobicistat/emtricitabine/tenofovir) reports 12.0% as side-effect, whereas 20.6% of those taking the tablet in studies experienced diarrhoea.

Diarrhoea was more commonly reported by people taking HIV treatment for the first time (19.7%) than for people who had previously taken treatment (13.7%). This difference, which was statistically significant, could reflect a higher incidence of drug side-effects in people first encountering ART, but could equally well be due to persistent gut damage in treatment-naive people with hitherto untreated HIV infection.

“The incidence of diarrhea as an adverse event in HIV clinical trials has not declined significantly in the modern cART era,” conclude David Asmuth and colleagues. “These findings emphasize the need for more targeted epidemiologic and interventional studies to characterise the residual morbidity of gastrointestinal complaints in people living with HIV.”

Reference

Asmuth DM et al. Prevalence of diarrhea in HIV clinical trials in the recent post-combined antiretroviral therapy (cART) era: Analysis of data from 39 clinical trials from 2008-2017 in over 20,000 patients. 22nd International AIDS Conference (AIDS 2018), Amsterdam, abstract TUPEB145, 2018.

View the abstract on the conference website. 

Download the e-poster from the conference website.

NAM's news coverage of the 22nd International AIDS Conference has been supported by Gilead Sciences Europe Ltd. and ViiV Healthcare.



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