Immunochemical and flow cytometric analysis of androgen receptor expression in thymocytes

Susan M. Viselli; Nancy J. Olsen; Keith Shults; Greg Steizer; William J. Kovacs

doi:10.1016/0303-7207(95)03479-Q

Immunochemical and flow cytometric analysis of androgen receptor expression in thymocytes

Susan M. Viselli, Nancy J. Olsen, Keith Shults, Greg Steizer, William J. Kovacs

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Abstract

A variety of evidence suggests that the cells of the immune system are targets for the actions of gonadal steroids. Experiments in both normal animals and in autoimmune disease models have established that androgens exert immunomodulatory effects at the level of the thymus. We have attempted to define precisely the potential target cells for androgen action in the thymus using recently developed antibodies to the androgen receptor. We report here that these antibodies reveal AR expression in all classes of thymocytes defined by surface markers CD4 and CD8. The highest levels of AR expression were observed in the CD4^-CD8⁺ and CD4^-CD8^- subsets that include the most immature cells. These experiments establish that thymocytes are potential targets for direct actions of androgens. The data further suggest AR expression in thymocytes may be developmentally regulated in these cells, and that androgen effects early in the process of thymocyte selection may contribute to the sexual dimorphism of immune responsiveness.

Original language	English (US)
Pages (from-to)	19-26
Number of pages	8
Journal	Molecular and Cellular Endocrinology
Volume	109
Issue number	1
DOIs	https://doi.org/10.1016/0303-7207(95)03479-Q
State	Published - Mar 1995

All Science Journal Classification (ASJC) codes

Biochemistry
Molecular Biology
Endocrinology

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10.1016/0303-7207(95)03479-Q

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title = "Immunochemical and flow cytometric analysis of androgen receptor expression in thymocytes",

abstract = "A variety of evidence suggests that the cells of the immune system are targets for the actions of gonadal steroids. Experiments in both normal animals and in autoimmune disease models have established that androgens exert immunomodulatory effects at the level of the thymus. We have attempted to define precisely the potential target cells for androgen action in the thymus using recently developed antibodies to the androgen receptor. We report here that these antibodies reveal AR expression in all classes of thymocytes defined by surface markers CD4 and CD8. The highest levels of AR expression were observed in the CD4-CD8+ and CD4-CD8- subsets that include the most immature cells. These experiments establish that thymocytes are potential targets for direct actions of androgens. The data further suggest AR expression in thymocytes may be developmentally regulated in these cells, and that androgen effects early in the process of thymocyte selection may contribute to the sexual dimorphism of immune responsiveness.",

author = "Viselli, {Susan M.} and Olsen, {Nancy J.} and Keith Shults and Greg Steizer and Kovacs, {William J.}",

note = "Funding Information: We appreciatteh e expertt echnicaal ssistancoef Max-ine Turneya ndK athrynR eese.D r. Gail Prins (University of Illinois) and Drs. ShutsungL iao and RichardH ipaaka (University of Chicago) generouslyp rovided anti-AR antibodiesD. r. Michael McPhaul providedC HO cells stablye xpressingth e humanA R. This work was sup-portedi n part by grantsf rom the NationalI nstituteso f Health( DK 41053t o N.J.O.), the Lupus Foundationo f America( to W.J.K) andt he UnitedS tatesD epartmenotf VeteransA ffairs (to W.J.K.). S.M.V. wast her ecipiento f an NIH postdoctorafl ellowship under training grant HD07043.",

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doi = "10.1016/0303-7207(95)03479-Q",

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AU - Viselli, Susan M.

AU - Olsen, Nancy J.

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AU - Steizer, Greg

AU - Kovacs, William J.

N1 - Funding Information: We appreciatteh e expertt echnicaal ssistancoef Max-ine Turneya ndK athrynR eese.D r. Gail Prins (University of Illinois) and Drs. ShutsungL iao and RichardH ipaaka (University of Chicago) generouslyp rovided anti-AR antibodiesD. r. Michael McPhaul providedC HO cells stablye xpressingth e humanA R. This work was sup-portedi n part by grantsf rom the NationalI nstituteso f Health( DK 41053t o N.J.O.), the Lupus Foundationo f America( to W.J.K) andt he UnitedS tatesD epartmenotf VeteransA ffairs (to W.J.K.). S.M.V. wast her ecipiento f an NIH postdoctorafl ellowship under training grant HD07043.

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N2 - A variety of evidence suggests that the cells of the immune system are targets for the actions of gonadal steroids. Experiments in both normal animals and in autoimmune disease models have established that androgens exert immunomodulatory effects at the level of the thymus. We have attempted to define precisely the potential target cells for androgen action in the thymus using recently developed antibodies to the androgen receptor. We report here that these antibodies reveal AR expression in all classes of thymocytes defined by surface markers CD4 and CD8. The highest levels of AR expression were observed in the CD4-CD8+ and CD4-CD8- subsets that include the most immature cells. These experiments establish that thymocytes are potential targets for direct actions of androgens. The data further suggest AR expression in thymocytes may be developmentally regulated in these cells, and that androgen effects early in the process of thymocyte selection may contribute to the sexual dimorphism of immune responsiveness.

AB - A variety of evidence suggests that the cells of the immune system are targets for the actions of gonadal steroids. Experiments in both normal animals and in autoimmune disease models have established that androgens exert immunomodulatory effects at the level of the thymus. We have attempted to define precisely the potential target cells for androgen action in the thymus using recently developed antibodies to the androgen receptor. We report here that these antibodies reveal AR expression in all classes of thymocytes defined by surface markers CD4 and CD8. The highest levels of AR expression were observed in the CD4-CD8+ and CD4-CD8- subsets that include the most immature cells. These experiments establish that thymocytes are potential targets for direct actions of androgens. The data further suggest AR expression in thymocytes may be developmentally regulated in these cells, and that androgen effects early in the process of thymocyte selection may contribute to the sexual dimorphism of immune responsiveness.

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Immunochemical and flow cytometric analysis of androgen receptor expression in thymocytes

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