Haematological safety of perinatal Zidovudine in pregnant HIV-1-infected women in Thailand secondary analysis of a randomized trial

Haematological safety of perinatal Zidovudine in pregnant HIV-1-infected women in Thailand secondary analysis of a randomized trial

Objectives: To respond to the primary safety objective of the Perinatal HIV Prevention Trial 1 (PHPT-1) by studying the evolution of haematological parameters according to zidovudine exposure duration in HIV-1-infected pregnant women. Design: Multicenter, randomized, double-blind, controlled trial o...

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Main Authors: Nelly Briand, Marc Lallemant, Gonzague Jourdain, Somnuek Techapalokul, Preecha Tunthanathip, Surachet Suphanich, Truengta Chanpoo, Patrinee Traisathit, Kenneth McIntosh, Sophie Le Cour
Format: Journal
Published: 2018
Subjects:
Medicine
Online Access:https://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=34249798728&origin=inward
http://cmuir.cmu.ac.th/jspui/handle/6653943832/61313
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Institution: Chiang Mai University
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spelling th-cmuir.6653943832-613132018-09-10T04:08:29Z Haematological safety of perinatal Zidovudine in pregnant HIV-1-infected women in Thailand secondary analysis of a randomized trial Nelly Briand Marc Lallemant Gonzague Jourdain Somnuek Techapalokul Preecha Tunthanathip Surachet Suphanich Truengta Chanpoo Patrinee Traisathit Kenneth McIntosh Sophie Le Cour Medicine Objectives: To respond to the primary safety objective of the Perinatal HIV Prevention Trial 1 (PHPT-1) by studying the evolution of haematological parameters according to zidovudine exposure duration in HIV-1-infected pregnant women. Design: Multicenter, randomized, double-blind, controlled trial of different durations of zidovudine prophylaxis. Setting: 27 hospitals in Thailand. Participants: 1,436 HIV-infected pregnant women in PHPT-1. Intervention: Zidovudine prophylaxis initiation at 28 or 35 wk gestation. Outcome measures: Haemoglobin level, leucocytes, total lymphocyte counts, and absolute neutrophil counts were measured at 26, 32, and 35 wk and at delivery. The evolution of haematological parameters was estimated between 26 and 35 wk (zidovudine/placebo) and between 35 wk and delivery to compare a long versus short zidovudine exposure. For each parameter, linear mixed models were adjusted on baseline sociodemographic variables, HIV clinical stage, CD4 count, and viral load. Results: Between 26 and 35 wk, haemoglobin, leucocytes, and absolute neutrophil counts decreased in zidovudine-exposed compared to unexposed women (mean difference [95% Cl] -0.4 [-0.5 to-0.3],-423 [-703 to-142],-485 [-757 to-213], respectively). However, between 35 wk and delivery, the haematological parameters increased faster in women exposed to long rather than short durations of zidovudine (0.1 [0.0 to 0.1]; 105 [18 to 191]; 147 [59 to 234], respectively). At delivery, the differences were not statistically significant, except for mean haemoglobin level, which remained slightly lower in the long zidovudine treatment group (difference: 0.2 g/dl). Zidovudine had no negative impact on the absolute lymphocyte counts. Conclusion: Zidovudine initiated at 28 wk gestation rather than 35 wk had a transient negative impact on the evolution of haematological parameters, which was largely reversed by delivery despite continuation of zidovudine. This result provides reassurance about the safety of early initiation of zidovudine prophylaxis during pregnancy to maximize prevention of perinatal HIV. 2018-09-10T04:08:29Z 2018-09-10T04:08:29Z 2007-04-27 Journal 15555887 2-s2.0-34249798728 10.1371/journal.pctr.0020011 https://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=34249798728&origin=inward http://cmuir.cmu.ac.th/jspui/handle/6653943832/61313
institution Chiang Mai University
building Chiang Mai University Library
country Thailand
collection CMU Intellectual Repository
topic Medicine
spellingShingle Medicine
Nelly Briand
Marc Lallemant
Gonzague Jourdain
Somnuek Techapalokul
Preecha Tunthanathip
Surachet Suphanich
Truengta Chanpoo
Patrinee Traisathit
Kenneth McIntosh
Sophie Le Cour
Haematological safety of perinatal Zidovudine in pregnant HIV-1-infected women in Thailand secondary analysis of a randomized trial
description Objectives: To respond to the primary safety objective of the Perinatal HIV Prevention Trial 1 (PHPT-1) by studying the evolution of haematological parameters according to zidovudine exposure duration in HIV-1-infected pregnant women. Design: Multicenter, randomized, double-blind, controlled trial of different durations of zidovudine prophylaxis. Setting: 27 hospitals in Thailand. Participants: 1,436 HIV-infected pregnant women in PHPT-1. Intervention: Zidovudine prophylaxis initiation at 28 or 35 wk gestation. Outcome measures: Haemoglobin level, leucocytes, total lymphocyte counts, and absolute neutrophil counts were measured at 26, 32, and 35 wk and at delivery. The evolution of haematological parameters was estimated between 26 and 35 wk (zidovudine/placebo) and between 35 wk and delivery to compare a long versus short zidovudine exposure. For each parameter, linear mixed models were adjusted on baseline sociodemographic variables, HIV clinical stage, CD4 count, and viral load. Results: Between 26 and 35 wk, haemoglobin, leucocytes, and absolute neutrophil counts decreased in zidovudine-exposed compared to unexposed women (mean difference [95% Cl] -0.4 [-0.5 to-0.3],-423 [-703 to-142],-485 [-757 to-213], respectively). However, between 35 wk and delivery, the haematological parameters increased faster in women exposed to long rather than short durations of zidovudine (0.1 [0.0 to 0.1]; 105 [18 to 191]; 147 [59 to 234], respectively). At delivery, the differences were not statistically significant, except for mean haemoglobin level, which remained slightly lower in the long zidovudine treatment group (difference: 0.2 g/dl). Zidovudine had no negative impact on the absolute lymphocyte counts. Conclusion: Zidovudine initiated at 28 wk gestation rather than 35 wk had a transient negative impact on the evolution of haematological parameters, which was largely reversed by delivery despite continuation of zidovudine. This result provides reassurance about the safety of early initiation of zidovudine prophylaxis during pregnancy to maximize prevention of perinatal HIV.
format Journal
author Nelly Briand
Marc Lallemant
Gonzague Jourdain
Somnuek Techapalokul
Preecha Tunthanathip
Surachet Suphanich
Truengta Chanpoo
Patrinee Traisathit
Kenneth McIntosh
Sophie Le Cour
author_facet Nelly Briand
Marc Lallemant
Gonzague Jourdain
Somnuek Techapalokul
Preecha Tunthanathip
Surachet Suphanich
Truengta Chanpoo
Patrinee Traisathit
Kenneth McIntosh
Sophie Le Cour
author_sort Nelly Briand
title Haematological safety of perinatal Zidovudine in pregnant HIV-1-infected women in Thailand secondary analysis of a randomized trial
title_short Haematological safety of perinatal Zidovudine in pregnant HIV-1-infected women in Thailand secondary analysis of a randomized trial
title_full Haematological safety of perinatal Zidovudine in pregnant HIV-1-infected women in Thailand secondary analysis of a randomized trial
title_fullStr Haematological safety of perinatal Zidovudine in pregnant HIV-1-infected women in Thailand secondary analysis of a randomized trial
title_full_unstemmed Haematological safety of perinatal Zidovudine in pregnant HIV-1-infected women in Thailand secondary analysis of a randomized trial
title_sort haematological safety of perinatal zidovudine in pregnant hiv-1-infected women in thailand secondary analysis of a randomized trial
publishDate 2018
url https://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=34249798728&origin=inward
http://cmuir.cmu.ac.th/jspui/handle/6653943832/61313
_version_ 1681425597481353216

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