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Thymic Involution in Viable Motheaten (me(υ)) Mice is Associated with a Loss of Intrathymic Precursor Activity
Mice homozygous for the viable motheaten (me(υ)) allele manifest abnormalities in thymocytopoiesis, are severely immunodeficient, and develop autoimmune disorders early in life. Premature thymic involution occurs in me(υ)/me(υ) mice, and their bone marrow prothymocytes are unable to repopulate the t...
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Formato: | Texto |
Lenguaje: | English |
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Hindawi Publishing Corporation
1992
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Materias: | |
Acceso en línea: | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2275861/ https://www.ncbi.nlm.nih.gov/pubmed/1627951 http://dx.doi.org/10.1155/1992/68954 |
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author | Hayes, Sandra M. Shultz, Leonard D. Greiner, Dale L. |
author_facet | Hayes, Sandra M. Shultz, Leonard D. Greiner, Dale L. |
author_sort | Hayes, Sandra M. |
collection | PubMed |
description | Mice homozygous for the viable motheaten (me(υ)) allele manifest abnormalities in thymocytopoiesis, are severely immunodeficient, and develop autoimmune disorders early in life. Premature thymic involution occurs in me(υ)/me(υ) mice, and their bone marrow prothymocytes are unable to repopulate the thymus of adoptive recipients following intravenous (i.v.) transfer. However, analysis of thymocytopoiesis following intrathymic (i.t.) adoptive transfer of bone marrow from me(υ)/me(υ) mice demonstrates the presence of normal numbers of prothymocytes. To investigate intrathymic development in me(υ)/me(υ) mice, we determined intrathymic precursor cell number and activity. Dual labeling analyses showed that an involuted me(υ)/me(υ) thymus is relatively enriched (fivefold) in CD4(–) CD8(–) thymocytes (intrathymic precursor phenotype) compared with wild-type (+/+) thymus. However, thymocytes from me(υ)/me(υ) mice were deficient in precursor activity when adoptively transferred i.t. into irradiated recipients. Thymocytes recovered from the involuted thymus of aged or steroid-treated normal mice also displayed reduced precursor activity. However, the phenotypic profile of thymocyte subsets from steroid-treated mice was enriched in single positive cells (mature phenotype) and was distinctly different from the subset distribution of thymocytes in me(υ)/me(υ) and aged mice. These results suggest that intrathymic precursor activity in me(υ)/me(υ) mice is decreased, and may be reflective of decreased prothymocyte seeding to the thymus in vivo, In addition, the results suggest that the thymic involution in me(υ)/me(υ) mice is not due solely to effects of corticosteroids. |
format | Text |
id | pubmed-2275861 |
institution | National Center for Biotechnology Information |
language | English |
publishDate | 1992 |
publisher | Hindawi Publishing Corporation |
record_format | MEDLINE/PubMed |
spelling | pubmed-22758612008-03-31 Thymic Involution in Viable Motheaten (me(υ)) Mice is Associated with a Loss of Intrathymic Precursor Activity Hayes, Sandra M. Shultz, Leonard D. Greiner, Dale L. Dev Immunol Research Article Mice homozygous for the viable motheaten (me(υ)) allele manifest abnormalities in thymocytopoiesis, are severely immunodeficient, and develop autoimmune disorders early in life. Premature thymic involution occurs in me(υ)/me(υ) mice, and their bone marrow prothymocytes are unable to repopulate the thymus of adoptive recipients following intravenous (i.v.) transfer. However, analysis of thymocytopoiesis following intrathymic (i.t.) adoptive transfer of bone marrow from me(υ)/me(υ) mice demonstrates the presence of normal numbers of prothymocytes. To investigate intrathymic development in me(υ)/me(υ) mice, we determined intrathymic precursor cell number and activity. Dual labeling analyses showed that an involuted me(υ)/me(υ) thymus is relatively enriched (fivefold) in CD4(–) CD8(–) thymocytes (intrathymic precursor phenotype) compared with wild-type (+/+) thymus. However, thymocytes from me(υ)/me(υ) mice were deficient in precursor activity when adoptively transferred i.t. into irradiated recipients. Thymocytes recovered from the involuted thymus of aged or steroid-treated normal mice also displayed reduced precursor activity. However, the phenotypic profile of thymocyte subsets from steroid-treated mice was enriched in single positive cells (mature phenotype) and was distinctly different from the subset distribution of thymocytes in me(υ)/me(υ) and aged mice. These results suggest that intrathymic precursor activity in me(υ)/me(υ) mice is decreased, and may be reflective of decreased prothymocyte seeding to the thymus in vivo, In addition, the results suggest that the thymic involution in me(υ)/me(υ) mice is not due solely to effects of corticosteroids. Hindawi Publishing Corporation 1992 /pmc/articles/PMC2275861/ /pubmed/1627951 http://dx.doi.org/10.1155/1992/68954 Text en Copyright © 1992 Hindawi Publishing Corporation. http://creativecommons.org/licenses/by/ This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited. |
spellingShingle | Research Article Hayes, Sandra M. Shultz, Leonard D. Greiner, Dale L. Thymic Involution in Viable Motheaten (me(υ)) Mice is Associated with a Loss of Intrathymic Precursor Activity |
title | Thymic Involution in Viable Motheaten (me(υ)) Mice is
Associated with a Loss of Intrathymic Precursor Activity |
title_full | Thymic Involution in Viable Motheaten (me(υ)) Mice is
Associated with a Loss of Intrathymic Precursor Activity |
title_fullStr | Thymic Involution in Viable Motheaten (me(υ)) Mice is
Associated with a Loss of Intrathymic Precursor Activity |
title_full_unstemmed | Thymic Involution in Viable Motheaten (me(υ)) Mice is
Associated with a Loss of Intrathymic Precursor Activity |
title_short | Thymic Involution in Viable Motheaten (me(υ)) Mice is
Associated with a Loss of Intrathymic Precursor Activity |
title_sort | thymic involution in viable motheaten (me(υ)) mice is
associated with a loss of intrathymic precursor activity |
topic | Research Article |
url | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2275861/ https://www.ncbi.nlm.nih.gov/pubmed/1627951 http://dx.doi.org/10.1155/1992/68954 |
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