Microbial Translocation Does Not Drive Immune Activation in Ugandan Children Infected With HIV.

Felicity Fitzgerald ,Gabriel Chipili ,Isaac Sebuliba ,Shadreck Chanshi ,Steven Malama ,Helen Mcilleron ,Bernard Bainomuhwezi ,Sylvia Mulambo ,Julianne R Brown ,Chifumbe Chintu ,Charles O Okello ,Paul Oronon ,Lincoln Mugarura ,Constance Lukowe ,Desiree Kabamba ,Geoffrey Amone ,Chama Chama ,Julia Kenny ,Dorothy Kavindele ,Winnie Namala ,Peter Elyanu ,Immaculate Nagawa ,J Vicent Tukei ,Zainab Akol ,Margaret J Thomason ,Angela Colbers ,E Bagurukira ,Matthew Odera ,Justine Komunyena ,Elias Chambula ,Nigel Klein ,Emmanuel Achol ,Dorothy Zangata ,Innocent Mwape ,Dorica Masuka ,A Sarah Walker ,Joshua Zulu ,Kathryn Harris ,Chishala Chabala ,Marjory N Liusha ,Elizabeth Kaudha ,James Abach ,Daniel Chola ,Veronica Mulenga ,George Abongomera ,Phyllis Mwesigwa ,Dick Isabirye ,Violet Korutaro ,Terence Chipoya ,Gladys Namutebi ,Philliam Aleti ,Ronan Doyle ,Daniel Sseremba ,Edward Otim ,Elwyn Chomba ,I Aciro ,David Baptiste ,Immaculate Nankya ,Harriet Nakimuli ,Peter Okello ,Emmanuel Ndashimyeeva ,Édouard Lhomme ,Carolyn Nansubuga ,N Justine Mpanga ,Monica Kapasa ,Philip Apugulu ,Liam P Shaw ,Victor Musiime ,Cissy Kityo ,D Odoch ,Mpala Mwanza ,Fred Sunday ,Moses Matovu ,Brendan Murphy ,R Alice Asiimwe ,Sharon Kesande ,Patrick Kidega ,Joyce Lungu ,Priscilla Wavamunno ,David M Burger ,Geoffrey Onen ,Amos Drasiku ,E Glorius Tumuheirirwe ,W Odong ,Joshua Kayiwa ,E Williams ,Florence Odongo ,Caroline C Zulu ,Linda Chibesa ,Alex Ferrier ,Joseph Omongin ,Fatuma Kabasita ,Semy Zulu ,Adrian Cook ,Diana M Gibb ,Beatrice Arach ,Rodolphe Thiébaut ,Andrew J Prendergast ,Mox Kalumbi ,Muzamil Kisekka ,Charlotte Male ,Betty Chanda ,Ellen Owen-Powell ,A Brooks ,Sarah Nakimera ,Alison Balaba ,Musaku Mwenechanya ,Alice Kwaga ,Eva Nabulime ,Moira Spyer ,Quirine Fillekes ,Jose Luis Ramos ,Grace Mirembe

doi:10.1093/infdis/jiy495

Abstract

ObjectiveImmune activation is associated with morbidity and mortality during human immunodeficiency virus (HIV) infection, despite receipt of antiretroviral therapy (ART). We investigated whether microbial translocation drives immune activation in HIV-infected Ugandan children.MethodsNineteen markers of immune activation and inflammation were measured over 96 weeks in HIV-infected Ugandan children in the CHAPAS-3 Trial and HIV-uninfected age-matched controls. Microbial translocation was assessed using molecular techniques, including next-generation sequencing.ResultsOf 249 children included, 142 were infected with HIV; of these, 120 were ART naive, with a median age of 2.8 years (interquartile range [IQR], 1.7–4.0 years) and a median baseline CD4+ T-cell percentage of 20% (IQR, 14%–24%), and 22 were ART experienced, with a median age of 6.5 years (IQR, 5.9–9.2 years) and a median baseline CD4+ T-cell percentage of 35% (IQR, 31%–39%). The control group comprised 107 children without HIV infection. The median increase in the CD4+ T-cell percentage was 17 percentage points (IQR, 12–22 percentage points) at week 96 among ART-naive children, and the viral load was <100 copies/mL in 76% of ART-naive children and 91% of ART-experienced children. Immune activation decreased with ART use. Children could be divided on the basis of immune activation markers into the following 3 clusters: in cluster 1, the majority of children were HIV uninfected; cluster 2 comprised a mix of HIV-uninfected children and HIV-infected ART-naive or ART-experienced children; and in cluster 3, the majority were ART naive. Immune activation was low in cluster 1, decreased in cluster 3, and persisted in cluster 2. Blood microbial DNA levels were negative or very low across groups, with no difference between clusters except for Enterobacteriaceae organisms (the level was higher in cluster 1; P < .0001).ConclusionImmune activation decreased with ART use, with marker clustering indicating different activation patterns according to HIV and ART status. Levels of bacterial DNA in blood were low regardless of HIV status, ART status, and immune activation status. Microbial translocation did not drive immune activation in this setting.Clinical Trials RegistrationISRCTN69078957.

Highlights

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Children could be divided on the basis of immune activation markers into the following 3 clusters: in cluster 1, the majority of children were human immunodeficiency virus (HIV) uninfected; cluster 2 comprised a mix of HIV-uninfected children and HIV-infected antiretroviral therapy (ART)-naive or ART-experienced children; and in cluster 3, the majority were ART naive
Immune activation decreased with ART use, with marker clustering indicating different activation patterns according to HIV and ART status

Summary

Introduction

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