4.2 Article

Specificity of the autologous neutralizing antibody response

期刊

CURRENT OPINION IN HIV AND AIDS
卷 4, 期 5, 页码 358-363

出版社

LIPPINCOTT WILLIAMS & WILKINS
DOI: 10.1097/COH.0b013e32832ea7e8

关键词

autologous neutralization; C3; escape; strain-specific; variable loops

资金

  1. CAPRISA
  2. NIAID Center for HIV/AIDS Vaccine Immunology (CHAVI) [AI067854]
  3. South African Vaccine Initiative (SAAVI)
  4. South African Medical Research Council
  5. Poliomyelitis Research Foundation of South Africa
  6. National Institute of Allergy and infectious Disease (NIAID)
  7. National Institutes of Health (NIH) [AI51794]
  8. National Research Foundation [67385]
  9. Columbia University-Southern African Fogarty AIDS International Training and Research Programme (AITRP)
  10. Fogarty International Center, NIH [D43TW00231]
  11. LifeLab
  12. biotechnology center of the South African Government Department of Science and Technology

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Purpose of review It has long been known that autologous neutralizing antibodies (AnAbs) exert pressure on the envelope of HIV, resulting in neutralization escape. However, recently, progress has been made in uncovering the precise targets of these potent early antibodies. Recent findings AnAbs primarily target variable regions of the HIV-1 envelope, explaining the strain-specificity of these antibodies. Despite high neutralizing potential and cross-reactivity, anti-V3 antibodies do not contribute to autologous neutralization. The V1V2 is commonly immunogenic in early HIV-1 and simian human immunodeficiency virus infections, though the nature of these epitopes remains to be determined. In subtype C viruses, the C3 region is a neutralization target, possibly as a result of its more exposed and amphipathic structure. Autologous neutralization appears to be mediated by very few AnAb specificities that develop sequentially suggesting the possibility of immunological hierarchies for both binding and neutralizing antibodies. The role of AnAbs in preventing superinfection and in restricting virus replication is reexamined in the context of recent data. Summary New studies have greatly contributed toward our understanding of the specificities mediating autologous neutralization and highlighted potential vulnerabilities on transmitted viruses. However, the contribution of AnAbs to the development of neutralization breadth remains to be characterized.

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