Identification of Germinal Center B Cells in Blood from HIV-infected Drug-naive Individuals in Central Africa

Author:

Béniguel Lydie1,Bégaud Evelyne2,Cognasse Fabrice1,Gabrié Philippe3,Mbolidi Christophe D.3,Sabido Odile4,Marovich Mary A.5,deFontaine Christiane6,Frésard Anne6,Lucht Frédéric6,Genin Christian1,Garraud Olivier1

Affiliation:

1. GIMAP EA3064, Faculté de Médecine, Université Jean Monnet, 15 Rue A. Paré, Saint Etienne cédex 2 42023, France

2. Institut Pasteur de Bangui, Bangui, Central African Republic

3. Hôpital Communautaire, Bangui, Central African Republic

4. Centre Commun de Cytométrie en Flux, Faculté de Médecine, Université Jean Monnet, 15 Rue A. Paré, Saint Etienne cédex 2 42023, France

5. Combined US Military HIV research Program, Rockville, MD, USA

6. Service des Maladies Infectieuses, University Hospital, Saint Etienne, France

Abstract

To better understand the pathophysiology of B cell populations—the precursors of antibody secreting cells—during chronic human immunodeficiency virus (HIV) infection, we examined the phenotype of circulating B cells in newly diagnosed Africans. We found that all African individuals displayed low levels of naive B cells and of memory-type CD27+B cells, and high levels of differentiated B cells. On the other hand, HIV-infected African patients had a population of germinal center B cells (i.e. CD20+, sIgM-, sIgD+, CD77+, CD138±), which are generally restricted to lymph nodes and do not circulate unless the lymph node architecture is altered. The first observations could be linked to the tropical environment whereas the presence of germinal center B cells may be attributable to chronic exposure to HIV as it is not observed in HIV-negative African controls and HAART treated HIV-infected Europeans. It may impact the management of HIV infection in countries with limited access to HIV drugs and urges consideration for implementation of therapeutic vaccines.

Publisher

Hindawi Limited

Subject

General Medicine,Immunology,Immunology and Allergy

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