Peptide therapy for anti-CD4 autoimmunity in HIV-1 infection: Toward the development of an autoimmune animal model

R. Abulafia-Lapid; M. Afentoulis; A. A. Vandenbark

doi:10.1016/j.vaccine.2009.01.049

Peptide therapy for anti-CD4 autoimmunity in HIV-1 infection: Toward the development of an autoimmune animal model

R. Abulafia-Lapid, M. Afentoulis, A. A. Vandenbark

Neurology

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

Abstract

Aiming to develop an animal model for anti-CD4 autoimmunity reflective of that observed in HIV-1 patients, we injected the selected peptides p1, p28 and p29 as the major immunogenic epitopes into HLA-DR4 and human CD4 transgenic DBA/16J mice, as well as into C57BL/6 and DBA mice. We document a decrease of CD4+ cells in peripheral blood and spleen after immunization with the human CD4-p28 immunogenic peptide of transgenic mice expressing human CD4, human HLA class II and mouse class II I-A^q (HLA-DR4-huCD4-I-A^q+); however, no decrease of CD4 cells was found in transgenic HLA-DR4-huCD4-I-A^q- mice or in control C57BL/6 and DBA immunized mice. Overall, the consistency of CD4 reduction and immunological recognition of p28 peptide favors the HLA-DR4-huCD4-I-A^q+ mouse as the most promising autoimmune mouse model.

Original language	English (US)
Pages (from-to)	3475-3480
Number of pages	6
Journal	Vaccine
Volume	27
Issue number	25-26
DOIs	https://doi.org/10.1016/j.vaccine.2009.01.049
State	Published - May 26 2009

Keywords

Anti-CD4 autoimmunity
HIV-1
Transgenic mice

ASJC Scopus subject areas

Molecular Medicine
Immunology and Microbiology(all)
veterinary(all)
Public Health, Environmental and Occupational Health
Infectious Diseases

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10.1016/j.vaccine.2009.01.049

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title = "Peptide therapy for anti-CD4 autoimmunity in HIV-1 infection: Toward the development of an autoimmune animal model",

abstract = "Aiming to develop an animal model for anti-CD4 autoimmunity reflective of that observed in HIV-1 patients, we injected the selected peptides p1, p28 and p29 as the major immunogenic epitopes into HLA-DR4 and human CD4 transgenic DBA/16J mice, as well as into C57BL/6 and DBA mice. We document a decrease of CD4+ cells in peripheral blood and spleen after immunization with the human CD4-p28 immunogenic peptide of transgenic mice expressing human CD4, human HLA class II and mouse class II I-Aq (HLA-DR4-huCD4-I-Aq+); however, no decrease of CD4 cells was found in transgenic HLA-DR4-huCD4-I-Aq- mice or in control C57BL/6 and DBA immunized mice. Overall, the consistency of CD4 reduction and immunological recognition of p28 peptide favors the HLA-DR4-huCD4-I-Aq+ mouse as the most promising autoimmune mouse model.",

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author = "R. Abulafia-Lapid and M. Afentoulis and Vandenbark, {A. A.}",

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AU - Afentoulis, M.

AU - Vandenbark, A. A.

PY - 2009/5/26

Y1 - 2009/5/26

N2 - Aiming to develop an animal model for anti-CD4 autoimmunity reflective of that observed in HIV-1 patients, we injected the selected peptides p1, p28 and p29 as the major immunogenic epitopes into HLA-DR4 and human CD4 transgenic DBA/16J mice, as well as into C57BL/6 and DBA mice. We document a decrease of CD4+ cells in peripheral blood and spleen after immunization with the human CD4-p28 immunogenic peptide of transgenic mice expressing human CD4, human HLA class II and mouse class II I-Aq (HLA-DR4-huCD4-I-Aq+); however, no decrease of CD4 cells was found in transgenic HLA-DR4-huCD4-I-Aq- mice or in control C57BL/6 and DBA immunized mice. Overall, the consistency of CD4 reduction and immunological recognition of p28 peptide favors the HLA-DR4-huCD4-I-Aq+ mouse as the most promising autoimmune mouse model.

AB - Aiming to develop an animal model for anti-CD4 autoimmunity reflective of that observed in HIV-1 patients, we injected the selected peptides p1, p28 and p29 as the major immunogenic epitopes into HLA-DR4 and human CD4 transgenic DBA/16J mice, as well as into C57BL/6 and DBA mice. We document a decrease of CD4+ cells in peripheral blood and spleen after immunization with the human CD4-p28 immunogenic peptide of transgenic mice expressing human CD4, human HLA class II and mouse class II I-Aq (HLA-DR4-huCD4-I-Aq+); however, no decrease of CD4 cells was found in transgenic HLA-DR4-huCD4-I-Aq- mice or in control C57BL/6 and DBA immunized mice. Overall, the consistency of CD4 reduction and immunological recognition of p28 peptide favors the HLA-DR4-huCD4-I-Aq+ mouse as the most promising autoimmune mouse model.

KW - Anti-CD4 autoimmunity

KW - HIV-1

KW - Transgenic mice

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Peptide therapy for anti-CD4 autoimmunity in HIV-1 infection: Toward the development of an autoimmune animal model

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Keywords

ASJC Scopus subject areas

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