Genesis of Progressive T‐Cell Deficiency Owing to a Single Missense Mutation in the Common Gamma Chain Gene

Patients with a moderate X‐linked combined immunodeficiency (XCID) owing to a single missense mutation in the common gamma chain (γc) gene (L→Q271) were found to have a progressive T‐cell deficiency. Blood T cells from four older subjects with XCIDL→Q271 were studied to ascertain the basis of that p...

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Published in	Scandinavian journal of immunology Vol. 54; no. 6; pp. 582 - 591
Main Authors	Goldman, A. S., Palkowetz, K. H., Rudloff, H. E., Dallas, D. V., Schmalstieg, F. C.
Format	Journal Article
Language	English
Published	Oxford, UK Blackwell Science Ltd 01.12.2001 Wiley Subscription Services, Inc
Subjects	Adolescent Adult Annexin A5 - metabolism Apoptosis Base Sequence Case-Control Studies Child DNA - genetics Female Genetic Linkage Humans Immunologic Deficiency Syndromes - genetics Immunologic Deficiency Syndromes - immunology Immunologic Deficiency Syndromes - metabolism Immunologic Deficiency Syndromes - pathology In Vitro Techniques Interleukin Receptor Common gamma Subunit Lymphocyte Activation Lymphocyte Count Male Mutation, Missense Necrosis Pedigree Propidium - metabolism propidium iodide Receptors, Interleukin-7 - genetics T-Lymphocytes - immunology T-Lymphocytes - metabolism T-Lymphocytes - ultrastructure Telomere - ultrastructure X Chromosome - genetics
Online Access	Get full text
ISSN	0300-9475 1365-3083
DOI	10.1046/j.1365-3083.2001.01006.x

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Abstract	Patients with a moderate X‐linked combined immunodeficiency (XCID) owing to a single missense mutation in the common gamma chain (γc) gene (L→Q271) were found to have a progressive T‐cell deficiency. Blood T cells from four older subjects with XCIDL→Q271 were studied to ascertain the basis of that progression. Few CD4+ T cells displayed the phenotype (CD45RA+ CD62L+) or deletion circles from T‐cell receptor (TCR) Vβ‐gene rearrangements found in recent thymic emigrants. These deficiencies were more severe in older males with XCIDL→Q271. Relative frequencies of fresh CD4+ and CD8+ T cells that bound annexin V, an early indicator of programmed cell death, or propidium iodide, an indicator of cell necrosis, were greater in XCIDL→Q271 T cells than in normal fresh T cells. The binding of annexin V and propidium iodide to XCIDL→Q271 T cells increased marginally after stimulation with anti‐CD3, but binding by fresh or stimulated XCIDL→Q271 T cells exceeded that found in normal stimulated T cells. Also, telomeres from XCIDL→Q271 CD4+ T cells were shortened in these patients compared to normal young adults. It therefore appears that the thymus is dysfunctional and that mature T cells are not effectively rescued from apoptosis or replication senescence via γc‐mediated pathways in XCIDL→Q271.
AbstractList	Patients with a moderate X-linked combined immunodeficiency (XCID) owing to a single missense mutation in the common gamma chain ( gamma c) gene (LQ271) were found to have a progressive T-cell deficiency. Blood T cells from four older subjects with XCID super(LQ271) were studied to ascertain the basis of that progression. Few CD4+ T cells displayed the phenotype (CD45RA+ CD62L+) or deletion circles from T-cell receptor (TCR) V beta -gene rearrangements found in recent thymic emigrants. These deficiencies were more severe in older males with XCID super(LQ271). Relative frequencies of fresh CD4+ and CD8+ T cells that bound annexin V, an early indicator of programmed cell death, or propidium iodide, an indicator of cell necrosis, were greater in XCID super(LQ271) T cells than in normal fresh T cells. The binding of annexin V and propidium iodide to XCID super(LQ271) T cells increased marginally after stimulation with anti-CD3, but binding by fresh or stimulated XCID super(LQ271) T cells exceeded that found in normal stimulated T cells. Also, telomeres from XCID super(LQ271) CD4+ T cells were shortened in these patients compared to normal young adults. It therefore appears that the thymus is dysfunctional and that mature T cells are not effectively rescued from apoptosis or replication senescence via gamma c-mediated pathways in XCID super(LQ271). Patients with a moderate X‐linked combined immunodeficiency (XCID) owing to a single missense mutation in the common gamma chain (γ c ) gene (L→Q271) were found to have a progressive T‐cell deficiency. Blood T cells from four older subjects with XCID L→Q271 were studied to ascertain the basis of that progression. Few CD4 + T cells displayed the phenotype (CD45RA + CD62L + ) or deletion circles from T‐cell receptor (TCR) Vβ‐gene rearrangements found in recent thymic emigrants. These deficiencies were more severe in older males with XCID L→Q271 . Relative frequencies of fresh CD4 + and CD8 + T cells that bound annexin V, an early indicator of programmed cell death, or propidium iodide, an indicator of cell necrosis, were greater in XCID L→Q271 T cells than in normal fresh T cells. The binding of annexin V and propidium iodide to XCID L→Q271 T cells increased marginally after stimulation with anti‐CD3, but binding by fresh or stimulated XCID L→Q271 T cells exceeded that found in normal stimulated T cells. Also, telomeres from XCID L→Q271 CD4 + T cells were shortened in these patients compared to normal young adults. It therefore appears that the thymus is dysfunctional and that mature T cells are not effectively rescued from apoptosis or replication senescence via γ c ‐mediated pathways in XCID L→Q271 . Patients with a moderate X-linked combined immunodeficiency (XCID) owing to a single missense mutation in the common gamma chain (gammac) gene (L-->Q271) were found to have a progressive T-cell deficiency. Blood T cells from four older subjects with XCIDL-->Q271 were studied to ascertain the basis of that progression. Few CD4+ T cells displayed the phenotype (CD45RA+ CD62L+) or deletion circles from T-cell receptor (TCR) Vbeta-gene rearrangements found in recent thymic emigrants. These deficiencies were more severe in older males with XCIDL-->Q271. Relative frequencies of fresh CD4+ and CD8+ T cells that bound annexin V, an early indicator of programmed cell death, or propidium iodide, an indicator of cell necrosis, were greater in XCIDL-->Q271 T cells than in normal fresh T cells. The binding of annexin V and propidium iodide to XCIDL-Q271 T cells increased marginally after stimulation with anti-CD3, but binding by fresh or stimulated XCIDL-Q271 T cells exceeded that found in normal stimulated T cells. Also, telomeres from XCIDL-->Q271 CD4+ T cells were shortened in these patients compared to normal young adults. It therefore appears that the thymus is dysfunctional and that mature T cells are not effectively rescued from apoptosis or replication senescence via gamma-mediated pathways in XCIDL-->Q271.Patients with a moderate X-linked combined immunodeficiency (XCID) owing to a single missense mutation in the common gamma chain (gammac) gene (L-->Q271) were found to have a progressive T-cell deficiency. Blood T cells from four older subjects with XCIDL-->Q271 were studied to ascertain the basis of that progression. Few CD4+ T cells displayed the phenotype (CD45RA+ CD62L+) or deletion circles from T-cell receptor (TCR) Vbeta-gene rearrangements found in recent thymic emigrants. These deficiencies were more severe in older males with XCIDL-->Q271. Relative frequencies of fresh CD4+ and CD8+ T cells that bound annexin V, an early indicator of programmed cell death, or propidium iodide, an indicator of cell necrosis, were greater in XCIDL-->Q271 T cells than in normal fresh T cells. The binding of annexin V and propidium iodide to XCIDL-Q271 T cells increased marginally after stimulation with anti-CD3, but binding by fresh or stimulated XCIDL-Q271 T cells exceeded that found in normal stimulated T cells. Also, telomeres from XCIDL-->Q271 CD4+ T cells were shortened in these patients compared to normal young adults. It therefore appears that the thymus is dysfunctional and that mature T cells are not effectively rescued from apoptosis or replication senescence via gamma-mediated pathways in XCIDL-->Q271. Patients with a moderate X‐linked combined immunodeficiency (XCID) owing to a single missense mutation in the common gamma chain (γc) gene (L→Q271) were found to have a progressive T‐cell deficiency. Blood T cells from four older subjects with XCIDL→Q271 were studied to ascertain the basis of that progression. Few CD4+ T cells displayed the phenotype (CD45RA+ CD62L+) or deletion circles from T‐cell receptor (TCR) Vβ‐gene rearrangements found in recent thymic emigrants. These deficiencies were more severe in older males with XCIDL→Q271. Relative frequencies of fresh CD4+ and CD8+ T cells that bound annexin V, an early indicator of programmed cell death, or propidium iodide, an indicator of cell necrosis, were greater in XCIDL→Q271 T cells than in normal fresh T cells. The binding of annexin V and propidium iodide to XCIDL→Q271 T cells increased marginally after stimulation with anti‐CD3, but binding by fresh or stimulated XCIDL→Q271 T cells exceeded that found in normal stimulated T cells. Also, telomeres from XCIDL→Q271 CD4+ T cells were shortened in these patients compared to normal young adults. It therefore appears that the thymus is dysfunctional and that mature T cells are not effectively rescued from apoptosis or replication senescence via γc‐mediated pathways in XCIDL→Q271. Patients with a moderate X-linked combined immunodeficiency (XCID) owing to a single missense mutation in the common gamma chain (gammac) gene (L-->Q271) were found to have a progressive T-cell deficiency. Blood T cells from four older subjects with XCIDL-->Q271 were studied to ascertain the basis of that progression. Few CD4+ T cells displayed the phenotype (CD45RA+ CD62L+) or deletion circles from T-cell receptor (TCR) Vbeta-gene rearrangements found in recent thymic emigrants. These deficiencies were more severe in older males with XCIDL-->Q271. Relative frequencies of fresh CD4+ and CD8+ T cells that bound annexin V, an early indicator of programmed cell death, or propidium iodide, an indicator of cell necrosis, were greater in XCIDL-->Q271 T cells than in normal fresh T cells. The binding of annexin V and propidium iodide to XCIDL-Q271 T cells increased marginally after stimulation with anti-CD3, but binding by fresh or stimulated XCIDL-Q271 T cells exceeded that found in normal stimulated T cells. Also, telomeres from XCIDL-->Q271 CD4+ T cells were shortened in these patients compared to normal young adults. It therefore appears that the thymus is dysfunctional and that mature T cells are not effectively rescued from apoptosis or replication senescence via gamma-mediated pathways in XCIDL-->Q271.
Author	Rudloff, H. E. Dallas, D. V. Schmalstieg, F. C. Goldman, A. S. Palkowetz, K. H.
Author_xml	– sequence: 1 givenname: A. S. surname: Goldman fullname: Goldman, A. S. – sequence: 2 givenname: K. H. surname: Palkowetz fullname: Palkowetz, K. H. – sequence: 3 givenname: H. E. surname: Rudloff fullname: Rudloff, H. E. – sequence: 4 givenname: D. V. surname: Dallas fullname: Dallas, D. V. – sequence: 5 givenname: F. C. surname: Schmalstieg fullname: Schmalstieg, F. C.
BackLink	https://www.ncbi.nlm.nih.gov/pubmed/11902333$$D View this record in MEDLINE/PubMed
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Snippet	Patients with a moderate X‐linked combined immunodeficiency (XCID) owing to a single missense mutation in the common gamma chain (γc) gene (L→Q271) were found... Patients with a moderate X‐linked combined immunodeficiency (XCID) owing to a single missense mutation in the common gamma chain (γ c ) gene (L→Q271) were... Patients with a moderate X-linked combined immunodeficiency (XCID) owing to a single missense mutation in the common gamma chain (gammac) gene (L-->Q271) were... Patients with a moderate X-linked combined immunodeficiency (XCID) owing to a single missense mutation in the common gamma chain ( gamma c) gene (LQ271) were...
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SubjectTerms	Adolescent Adult Annexin A5 - metabolism Apoptosis Base Sequence Case-Control Studies Child DNA - genetics Female Genetic Linkage Humans Immunologic Deficiency Syndromes - genetics Immunologic Deficiency Syndromes - immunology Immunologic Deficiency Syndromes - metabolism Immunologic Deficiency Syndromes - pathology In Vitro Techniques Interleukin Receptor Common gamma Subunit Lymphocyte Activation Lymphocyte Count Male Mutation, Missense Necrosis Pedigree Propidium - metabolism propidium iodide Receptors, Interleukin-7 - genetics T-Lymphocytes - immunology T-Lymphocytes - metabolism T-Lymphocytes - ultrastructure Telomere - ultrastructure X Chromosome - genetics
Title	Genesis of Progressive T‐Cell Deficiency Owing to a Single Missense Mutation in the Common Gamma Chain Gene
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