Extent of Antigenic Diversity in the V3 Region of the Surface Glycoprotein, gp120, of Human Immunodeficiency Virus Type 1 Group M and Consequences for Serotyping

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J Virol, January 1998, p. 677-683, Vol. 72, No. 1
0022-538X/98/$04.00+0
Copyright © 1998, American Society for Microbiology. All rights reserved.

Extent of Antigenic Diversity in the V3 Region of the Surface Glycoprotein, gp120, of Human Immunodeficiency Virus Type 1 Group M and Consequences for Serotyping

Jean-Christophe Plantier,¹ Sophie Le Pogam,¹ Francis Poisson,¹ Laurence Buzelay,¹ Bernard Lejeune,² and Francis Barin¹^,^*

Laboratoire de Virologie, EP CNRS 117,¹ and Laboratoire de Biophysique Pharmaceutique et Biomathématiques,² Université François Rabelais, Tours, France

Received 20 February 1997/Accepted 24 September 1997

Human immunodeficiency virus type 1 (HIV-1) may be studied by molecular or immunological approaches. Most analyses have beenperformed by genetic comparison of isolates and have led to thedefinition of clades or subtypes within the major (M) group ofHIV-1. Five subtypes (A to E) were initially identified by comparisonof genomic sequences. Four new subtypes (F to I) were identifiedmore recently. Amino acid differences in the immunogenic V3 loopbetween isolates have also been studied, leading to a pheneticclassification of at least 14 clusters (1 to 14) of sequences(B. T. M. Korber, K. McInnes, R. F. Smith, and G. Myers, J. Virol.68:6730-6744, 1994). In this study, we compared the antigenicityof the V3 consensus sequences defined by phylogenetic analysisto the antigenicity of those defined by phenetic analysis. Weused a recently developed subtype-specific enzyme immunoassay(SSEIA) that uses the principle of blocking with an excess ofpeptide in the liquid phase. Two SSEIAs were performed, the firstwith five V3 sequences defined by phylogenetic analysis and thesecond with 14 V3 sequences defined by phenetic analysis. A totalof 168 HIV-1 sera taken from seropositive individuals from sevendifferent countries or regions were studied. Experimental andstatistical data, including correlation matrix and cluster analyses,demonstrated associations between the genetic subtypes and pheneticallyassociated groups. Most of these were predicted by Korber et al.(J. Virol. 68:6730-6744, 1994) by theoretical analysis. We alsofound that V3 sequences can be grouped into between three andfive antigenically unrelated categories. Residues that may beresponsible for major antigenic differences were identified atthe apex of the V3 loop, within the octapeptide xIGPGxxx, wherex represents the critical positions. Our study provides evidencethat there is a limited number of V3 serotypes which could beeasily monitored by serological assays to study the diversityand dynamics of HIV-1 strains.

^* Corresponding author. Mailing address: Laboratoire de Virologie, EP CNRS 117, CHRU Bretonneau, 37044 Tours Cedex, France.Phone: (33) 2 47 47 80 58. Fax: (33) 2 47 47 36 10.

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