T-cell progenitor function during progressive human immunodeficiency virus-1 infection and after antiretroviral therapy

Author:

Clark Dawn R.1,Repping Sjoerd1,Pakker Nadine G.1,Prins Jan M.1,Notermans Daan W.1,Wit Ferdinand W. N. M.1,Reiss Peter1,Danner Sven A.1,Coutinho Roel A.1,Lange Joep M. A.1,Miedema Frank1

Affiliation:

1. From the Department of Clinical Viro-Immunology, Laboratory for Experimental and Clinical Immunology, CLB, Sanquin Blood Supply Foundation, the National AIDS Therapy Evaluation Center, the Division of Infectious Diseases, Tropical Medicine and AIDS, and the Department of Internal Medicine, Academic Medical Centre, and the Department of Public Health, Municipal Health Service, Amsterdam, The Netherlands.

Abstract

Abstract Impairment of T-cell renewal has been proposed as contributing to CD4+ T-cell depletion in persons infected with human immunodeficiency virus-1. We analyzed the T-cell development capacity of progenitors using fetal thymus organ culture. Those who progressed to AIDS had a dramatic loss in T-cell development capacity shortly after seroconversion. In contrast, long-term nonprogressors retained progenitor capacity 8 years after seroconversion. Approximately 70% of patients experienced an improvement in T-cell development capacity after receiving 6 months of potent antiretroviral therapy. Improvement in T-cell development in fetal thymus organ culture correlated with an increase in the number of naive CD4+ T cells in peripheral blood. Numbers of progenitors in blood and bone marrow after seroconversion or during therapy did not correlate with the change observed in T-cell development capacity. These data provide evidence that HIV-1 infection can interfere with T-cell renewal at the level of the progenitor cell. Interference with T-cell renewal may contribute to CD4+ T-cell depletion.

Publisher

American Society of Hematology

Subject

Cell Biology,Hematology,Immunology,Biochemistry

Reference44 articles.

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