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Nef protein of HIV-1 has B-cell stimulatory activity.

作者信息

Chirmule N, Oyaizu N, Saxinger C, Pahwa S

机构信息

Department of Pediatrics, North Shore University Hospital-Cornell University Medical College, Manhasset, New York 11030.

出版信息

AIDS. 1994 Jun;8(6):733-4. doi: 10.1097/00002030-199406000-00002.

Abstract

OBJECTIVE

To examine the B-cell stimulatory properties of the regulatory Nef protein of HIV-1.

METHODS

The effect of the HIV-1 regulatory proteins Nef, Tat and Vif, were analyzed for their ability to induce differentiation of normal B lymphocytes into immunoglobulin secreting cells (ISC).

RESULTS

A recombinant Nef protein, but neither Tat or Vif, was able to induce ISC in peripheral blood lymphocyte (PBL) cultures of HIV-1-seronegative donors. Another recombinant Nef protein, d-Nef, with a truncated amino terminal (deletion of 34 amino acids) failed to induce B-cell differentiation. Pretreatment of the Nef protein with a polyclonal anti-Nef-antibody abrogated its B-cell stimulatory activity. The Nef-induced B-cell differentiation was dependent on cell-to-cell contact. Cell surface molecules leukocyte function-associated molecule (LFA)-1, intracellular adhesion molecule (ICAM)-1, human lymphocyte antigen-DR and B7 were involved in the T-B-cell interaction because monoclonal antibodies to these molecules abrogated the Nef-induced B-cell differentiation response. The Nef protein was able to induce interleukin (IL)-6 messenger (m)RNA and IL-6 protein secretion in PBL, with monocytes as the primary source.

CONCLUSIONS

These findings indicate that regulatory (Nef) proteins of HIV-1 contribute to the intense B-cell activation that occurs in association with HIV-1 infection. T-B-cell contact-dependent interaction and induction of IL-6 by these proteins appear to play major roles in this process.

摘要

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