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ORIGINAL ARTICLE: Age dependency and mutual relations in T and B lymphocyte abnormalities in common variable immunodeficiency patients
Common variable immunodeficiency (CVID) is primary hypogammaglobulinaemia with an unknown aetiopathogenesis. Although various abnormalities of T and B cells have been described, their pathogenetic roles are unclear. We determined T and B lymphocyte subsets known to be abnormal in CVID in order to di...
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| Published in: | Clinical and experimental immunology 2006-02, Vol.143 (2), p.373-379 |
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| container_end_page | 379 |
| container_issue | 2 |
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| container_title | Clinical and experimental immunology |
| container_volume | 143 |
| creator | Vlkova, M Thon, V Sarfyova, M Blaha, L Svobodnik, A Lokaj, J Litzman, J |
| description | Common variable immunodeficiency (CVID) is primary hypogammaglobulinaemia with an unknown aetiopathogenesis. Although various abnormalities of T and B cells have been described, their pathogenetic roles are unclear. We determined T and B lymphocyte subsets known to be abnormal in CVID in order to disclose possible relations between numerical abnormalities in those cells. Markers associated with B cell development (CD21, CD27, IgM, IgD) were determined on B lymphocytes (CD19 super(+)); T lymphocyte development (CD45RA, CD45RO, CD62L) and activation markers (CD25, CD27, CD28, CD29, CD38, CD57, HLA-DR) were determined on CD4 super(+) and CD8 super(+) T lymphocytes in 42 CVID patients and in 33 healthy controls. Abnormalities in CD4 super(+) T lymphocyte activation markers (increase in CD29, HLA-DR, CD45RO, decrease in CD27, CD62L, CD45RA) were observed particularly in patients with a decreased number of memory (CD27 super(+)) and mature (CD21 super(+)) B cells (group Ia according to the Freiburg group's classification), while abnormalities observed in CD8 super(+) cells (increase in CD27 and CD28 and decrease in HLA-DR, CD57 and CD38) did not depend upon grouping patients together according to B lymphocyte developmental subpopulations. We observed correlations between immature B cells (IgM super(+) CD21 super(-)) and expression of CD27, CD62L, CD45RA, CD45RO and HLA-DR on CD4 super(+) T cells in CVID patients but not in the control group. The expression of CD27 and CD45RA on CD4 super(+) T lymphocytes, such as the percentage of IgD super(+) CD27 super(-) and IgD super(+) CD27 super(+) cells in B lymphocytes, showed age dependency to be more significant than in the control group. Our study demonstrates that T and B lymphocyte abnormalities in CVID are partially related to each other. Some of those abnormalities are not definite, but may evolve with age of the patient. |
| doi_str_mv | 10.1111/j.1365-2249.2006.02999.x |
| format | article |
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Although various abnormalities of T and B cells have been described, their pathogenetic roles are unclear. We determined T and B lymphocyte subsets known to be abnormal in CVID in order to disclose possible relations between numerical abnormalities in those cells. Markers associated with B cell development (CD21, CD27, IgM, IgD) were determined on B lymphocytes (CD19 super(+)); T lymphocyte development (CD45RA, CD45RO, CD62L) and activation markers (CD25, CD27, CD28, CD29, CD38, CD57, HLA-DR) were determined on CD4 super(+) and CD8 super(+) T lymphocytes in 42 CVID patients and in 33 healthy controls. Abnormalities in CD4 super(+) T lymphocyte activation markers (increase in CD29, HLA-DR, CD45RO, decrease in CD27, CD62L, CD45RA) were observed particularly in patients with a decreased number of memory (CD27 super(+)) and mature (CD21 super(+)) B cells (group Ia according to the Freiburg group's classification), while abnormalities observed in CD8 super(+) cells (increase in CD27 and CD28 and decrease in HLA-DR, CD57 and CD38) did not depend upon grouping patients together according to B lymphocyte developmental subpopulations. We observed correlations between immature B cells (IgM super(+) CD21 super(-)) and expression of CD27, CD62L, CD45RA, CD45RO and HLA-DR on CD4 super(+) T cells in CVID patients but not in the control group. The expression of CD27 and CD45RA on CD4 super(+) T lymphocytes, such as the percentage of IgD super(+) CD27 super(-) and IgD super(+) CD27 super(+) cells in B lymphocytes, showed age dependency to be more significant than in the control group. Our study demonstrates that T and B lymphocyte abnormalities in CVID are partially related to each other. 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Although various abnormalities of T and B cells have been described, their pathogenetic roles are unclear. We determined T and B lymphocyte subsets known to be abnormal in CVID in order to disclose possible relations between numerical abnormalities in those cells. Markers associated with B cell development (CD21, CD27, IgM, IgD) were determined on B lymphocytes (CD19 super(+)); T lymphocyte development (CD45RA, CD45RO, CD62L) and activation markers (CD25, CD27, CD28, CD29, CD38, CD57, HLA-DR) were determined on CD4 super(+) and CD8 super(+) T lymphocytes in 42 CVID patients and in 33 healthy controls. Abnormalities in CD4 super(+) T lymphocyte activation markers (increase in CD29, HLA-DR, CD45RO, decrease in CD27, CD62L, CD45RA) were observed particularly in patients with a decreased number of memory (CD27 super(+)) and mature (CD21 super(+)) B cells (group Ia according to the Freiburg group's classification), while abnormalities observed in CD8 super(+) cells (increase in CD27 and CD28 and decrease in HLA-DR, CD57 and CD38) did not depend upon grouping patients together according to B lymphocyte developmental subpopulations. We observed correlations between immature B cells (IgM super(+) CD21 super(-)) and expression of CD27, CD62L, CD45RA, CD45RO and HLA-DR on CD4 super(+) T cells in CVID patients but not in the control group. The expression of CD27 and CD45RA on CD4 super(+) T lymphocytes, such as the percentage of IgD super(+) CD27 super(-) and IgD super(+) CD27 super(+) cells in B lymphocytes, showed age dependency to be more significant than in the control group. Our study demonstrates that T and B lymphocyte abnormalities in CVID are partially related to each other. 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Although various abnormalities of T and B cells have been described, their pathogenetic roles are unclear. We determined T and B lymphocyte subsets known to be abnormal in CVID in order to disclose possible relations between numerical abnormalities in those cells. Markers associated with B cell development (CD21, CD27, IgM, IgD) were determined on B lymphocytes (CD19 super(+)); T lymphocyte development (CD45RA, CD45RO, CD62L) and activation markers (CD25, CD27, CD28, CD29, CD38, CD57, HLA-DR) were determined on CD4 super(+) and CD8 super(+) T lymphocytes in 42 CVID patients and in 33 healthy controls. Abnormalities in CD4 super(+) T lymphocyte activation markers (increase in CD29, HLA-DR, CD45RO, decrease in CD27, CD62L, CD45RA) were observed particularly in patients with a decreased number of memory (CD27 super(+)) and mature (CD21 super(+)) B cells (group Ia according to the Freiburg group's classification), while abnormalities observed in CD8 super(+) cells (increase in CD27 and CD28 and decrease in HLA-DR, CD57 and CD38) did not depend upon grouping patients together according to B lymphocyte developmental subpopulations. We observed correlations between immature B cells (IgM super(+) CD21 super(-)) and expression of CD27, CD62L, CD45RA, CD45RO and HLA-DR on CD4 super(+) T cells in CVID patients but not in the control group. The expression of CD27 and CD45RA on CD4 super(+) T lymphocytes, such as the percentage of IgD super(+) CD27 super(-) and IgD super(+) CD27 super(+) cells in B lymphocytes, showed age dependency to be more significant than in the control group. Our study demonstrates that T and B lymphocyte abnormalities in CVID are partially related to each other. Some of those abnormalities are not definite, but may evolve with age of the patient.</abstract><doi>10.1111/j.1365-2249.2006.02999.x</doi></addata></record> |
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| source | PubMed Central |
| title | ORIGINAL ARTICLE: Age dependency and mutual relations in T and B lymphocyte abnormalities in common variable immunodeficiency patients |
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