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PubMed articles by:
Rozera, G.
Abbate, I.
Bruselles, A.
Capobianchi, M.
Retrovirology. 2009; 6: 15.
Published online 2009 February 12. doi: 10.1186/1742-4690-6-15.
PMCID: PMC2660291
Copyright © 2009 Rozera et al; licensee BioMed Central Ltd.
Massively parallel pyrosequencing highlights minority variants in the HIV-1 env quasispecies deriving from lymphomonocyte sub-populations
Gabriella Rozera,1 Isabella Abbate,corresponding author1 Alessandro Bruselles,1 Crhysoula Vlassi,2 Gianpiero D'Offizi,2 Pasquale Narciso,2 Giovanni Chillemi,3 Mattia Prosperi,1 Giuseppe Ippolito,4 and Maria R Capobianchi1
1Laboratory of Virology, INMI L. Spallanzani, Rome, Italy
2Clinical Department, INMI L. Spallanzani, Rome, Italy
3Consorzio Interuniversitario per le Applicazioni di Supercalcolo per l'Università e la Ricerca (CASPUR), Rome, Italy
4Scientific Direction, INMI L. Spallanzani, Rome, Italy
corresponding authorCorresponding author.
Gabriella Rozera: rozera/at/inmi.it; Isabella Abbate: abbate/at/inmi.it; Alessandro Bruselles: a.bruselles/at/gmail.com; Crhysoula Vlassi: vlassi/at/inmi.it; Gianpiero D'Offizi: gdoffizi/at/inmi.it; Pasquale Narciso: narciso/at/inmi.it; Giovanni Chillemi: giovanni.chillemi/at/caspur.it; Mattia Prosperi: ahnven/at/yahoo.it; Giuseppe Ippolito: ippolito/at/inmi.it; Maria R Capobianchi: capobianchi/at/inmi.it
Received November 10, 2008; Accepted February 12, 2009.
This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
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Abstract
Background
Virus-associated cell membrane proteins acquired by HIV-1 during budding may give information on the cellular source of circulating virions. In the present study, by applying immunosorting of the virus and of the cells with antibodies targeting monocyte (CD36) and lymphocyte (CD26) markers, it was possible to directly compare HIV-1 quasispecies archived in circulating monocytes and T lymphocytes with that present in plasma virions originated from the same cell types. Five chronically HIV-1 infected patients who underwent therapy interruption after prolonged HAART were enrolled in the study. The analysis was performed by the powerful technology of ultra-deep pyrosequencing after PCR amplification of part of the env gene, coding for the viral glycoprotein (gp) 120, encompassing the tropism-related V3 loop region. V3 amino acid sequences were used to establish heterogeneity parameters, to build phylogenetic trees and to predict co-receptor usage.
Results
The heterogeneity of proviral and viral genomes derived from monocytes was higher than that of T-lymphocyte origin. Both monocytes and T lymphocytes might contribute to virus rebounding in the circulation after therapy interruptions, but other virus sources might also be involved. In addition, both proviral and circulating viral sequences from monocytes and T lymphocytes were predictive of a predominant R5 coreceptor usage. However, minor variants, segregating from the most frequent quasispecies variants, were present. In particular, in proviral genomes harboured by monocytes, minority variant clusters with a predicted X4 phenotype were found.
Conclusion
This study provided the first direct comparison between the HIV-1 quasispecies archived as provirus in circulating monocytes and T lymphocytes with that of plasma virions replicating in the same cell types. Ultra-deep pyrosequencing generated data with some order of magnitude higher than any previously obtained with conventional approaches. Next generation sequencing allowed the analysis of previously inaccessible aspects of HIV-1 quasispecies, such as co-receptor usage of minority variants present in archived proviral sequences and in actually replicating virions, which may have clinical and therapeutic relevance.
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