Parameters influencing measurement of the Gag antigen-specific T-proliferative response to HIV-1 infection

D.S. Schiller; J.M. Binley; K Roux; Catherine Sarah Adamson; I.M. Jones; H-G Krausslich; A Hurley; M Markowitz; J.P. Moore

doi:doi:10.1089/088922200309359

Parameters influencing measurement of the Gag antigen-specific T-proliferative response to HIV-1 infection

D.S. Schiller, J.M. Binley, K Roux, Catherine Sarah Adamson, I.M. Jones, H-G Krausslich, A Hurley, M Markowitz, J.P. Moore

Research output: Contribution to journal › Article › peer-review

Abstract

We have analyzed factors that might influence the in vitro quantitation of the T-proliferative response to HIV-1 Gag antigens, a common and increasingly used clinical measurement of helper T cell function in the context of HIV-1 infection. We have compared the rate and extent of T cell proliferation in freshly prepared and previously frozen PBMC samples, and have concluded that frozen cells can be used successfully; we have assessed whether the suppression of any HIV-1 replication in the PBMC cultures affects the extent of T cell proliferation; we have studied which forms of the Gag antigens are the most efficient at inducing T cell proliferation. From the latter experiments, we conclude that Gag proteins that include p17, and perhaps also p7, sequences flanking the central p24 capsid protein, are better stimulants than proteins that comprise only p24 sequences.

Original language	English
Pages (from-to)	259-271
Journal	AIDS Research and Human Retroviruses
Volume	16
Issue number	3
DOIs	https://doi.org/doi:10.1089/088922200309359
Publication status	Published - Jul 2000

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doi:10.1089/088922200309359

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title = "Parameters influencing measurement of the Gag antigen-specific T-proliferative response to HIV-1 infection",

abstract = "We have analyzed factors that might influence the in vitro quantitation of the T-proliferative response to HIV-1 Gag antigens, a common and increasingly used clinical measurement of helper T cell function in the context of HIV-1 infection. We have compared the rate and extent of T cell proliferation in freshly prepared and previously frozen PBMC samples, and have concluded that frozen cells can be used successfully; we have assessed whether the suppression of any HIV-1 replication in the PBMC cultures affects the extent of T cell proliferation; we have studied which forms of the Gag antigens are the most efficient at inducing T cell proliferation. From the latter experiments, we conclude that Gag proteins that include p17, and perhaps also p7, sequences flanking the central p24 capsid protein, are better stimulants than proteins that comprise only p24 sequences.",

author = "D.S. Schiller and J.M. Binley and K Roux and Adamson, {Catherine Sarah} and I.M. Jones and H-G Krausslich and A Hurley and M Markowitz and J.P. Moore",

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T1 - Parameters influencing measurement of the Gag antigen-specific T-proliferative response to HIV-1 infection

AU - Schiller, D.S.

AU - Binley, J.M.

AU - Roux, K

AU - Adamson, Catherine Sarah

AU - Jones, I.M.

AU - Krausslich, H-G

AU - Hurley, A

AU - Markowitz, M

AU - Moore, J.P.

PY - 2000/7

Y1 - 2000/7

N2 - We have analyzed factors that might influence the in vitro quantitation of the T-proliferative response to HIV-1 Gag antigens, a common and increasingly used clinical measurement of helper T cell function in the context of HIV-1 infection. We have compared the rate and extent of T cell proliferation in freshly prepared and previously frozen PBMC samples, and have concluded that frozen cells can be used successfully; we have assessed whether the suppression of any HIV-1 replication in the PBMC cultures affects the extent of T cell proliferation; we have studied which forms of the Gag antigens are the most efficient at inducing T cell proliferation. From the latter experiments, we conclude that Gag proteins that include p17, and perhaps also p7, sequences flanking the central p24 capsid protein, are better stimulants than proteins that comprise only p24 sequences.

AB - We have analyzed factors that might influence the in vitro quantitation of the T-proliferative response to HIV-1 Gag antigens, a common and increasingly used clinical measurement of helper T cell function in the context of HIV-1 infection. We have compared the rate and extent of T cell proliferation in freshly prepared and previously frozen PBMC samples, and have concluded that frozen cells can be used successfully; we have assessed whether the suppression of any HIV-1 replication in the PBMC cultures affects the extent of T cell proliferation; we have studied which forms of the Gag antigens are the most efficient at inducing T cell proliferation. From the latter experiments, we conclude that Gag proteins that include p17, and perhaps also p7, sequences flanking the central p24 capsid protein, are better stimulants than proteins that comprise only p24 sequences.

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DO - doi:10.1089/088922200309359

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EP - 271

JO - AIDS Research and Human Retroviruses

JF - AIDS Research and Human Retroviruses

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ER -

Parameters influencing measurement of the Gag antigen-specific T-proliferative response to HIV-1 infection

Abstract

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