Cross-Reactions between the Cytotoxic T-Lymphocyte Responses of Human Immunodeficiency Virus-Infected African and European Patients

Author:

Durali Deniz1,Morvan Jacques2,Letourneur Franck3,Schmitt Doris4,Guegan Nelly1,Dalod Marc1,Saragosti Sentob3,Sicard Didier5,Levy Jean-Paul3,Gomard Elisabeth1

Affiliation:

1. Laboratoire d’Immunologie des Pathologies Infectieuses et Tumorales, Unité INSERM 445, UniversitéRené Descartes,1

2. Institut Pasteur, Bangui, Central African Republic2

3. Institut Cochin de Génétique Moléculaire,3 and

4. Transgène, Strasbourg,4 France, and

5. Département de Médecine Interne,5 Hôpital Cochin, Paris, and

Abstract

ABSTRACT The great variability of protein sequences from human immunodeficiency virus (HIV) type 1 (HIV-1) isolates represents a major obstacle to the development of an effective vaccine against this virus. The surface protein (Env), which is the predominant target of neutralizing antibodies, is particularly variable. Here we examine the impact of variability among different HIV-1 subtypes (clades) on cytotoxic T-lymphocyte (CTL) activities, the other major component of the antiviral immune response. CTLs are produced not only against Env but also against other structural proteins, as well as some regulatory proteins. The genetic subtypes of HIV-1 were determined for Env and Gag from several patients infected either in France or in Africa. The cross-reactivities of the CTLs were tested with target cells expressing selected proteins from HIV-1 isolates of clade A or B or from HIV type 2 isolates. All African patients were infected with viruses belonging to clade A for Env and for Gag, except for one patient who was infected with a clade A Env-clade G Gag recombinant virus. All patients infected in France were infected with clade B viruses. The CTL responses obtained from all the African and all the French individuals tested showed frequent cross-reactions with proteins of the heterologous clade. Epitopes conserved between the viruses of clades A and B appeared especially frequent in Gag p24, Gag p18, integrase, and the central region of Nef. Cross-reactivity also existed among Gag epitopes of clades A, B, and G, as shown by the results for the patient infected with the clade A Env-clade G Gag recombinant virus. These results show that CTLs raised against viral antigens from different clades are able to cross-react, emphasizing the possibility of obtaining cross-immunizations for this part of the immune response in vaccinated individuals.

Publisher

American Society for Microbiology

Subject

Virology,Insect Science,Immunology,Microbiology

Reference43 articles.

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2. HIV antibodies and vaccine design;Bolognesi D.;AIDS,1989

3. Brander C. Walker B. D. The HLA-class I-restricted CTL response in HIV-1 infection; identification of optimal epitopes. HIV Molecular Immunology Database 1995 Los Alamos National Laboratory Los Alamos N.Mex IV-1 to IV-8.

4. Characterization of an HIV-1 p24gag epitope recognized by a CD8+ cytotoxic T-cell clone;Buseyne F.;Immunol. Lett.,1997

5. Analysis of the human env-specific cytotoxic T-lymphocyte (CTL) response in natural human immunodeficiency virus type 1 infection: low prevalence of broadly cross-reactive env-specific CTL

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