Preferential expression of T-cell receptor Vβ-chains in atopic eczema

Karsten Neuber; Cornelius Löliger; Ingrid Köhler; Johannes Ring

Preferential expression of T-cell receptor Vβ-chains in atopic eczema

Karsten Neuber, Cornelius Löliger, Ingrid Köhler, Johannes Ring

University Medical Center Hamburg-Eppendorf

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

38 Scopus citations

Abstract

Chronic skin colonization with Staphylococcus aureus is a characteristic feature of atopic eczema, and about 60% of S. aureus strains isolated from the skin of patients with atopic eczema secrete enterotoxins. T-cell stimulation by staphylococcal enterotoxins is restricted to the Vβ-chain of the T-cell receptor. Therefore, the expression of different Vβ-chains (Vβ3, 5 a,b,c, 6, 8, 12) on peripheral blood T-cells (CD4+) from patients with atopic eczema was measured by flowcytometry before and after stimulation with staphylococcal enterotoxin B. Lymphocytes from healthy donors served as controls. Additionally, the expression of Vβ-chains in normal skin and in lesional skin of patients with atopic eczema was determined by immunofluorescence histology. In atopic eczema, higher numbers of CD4+ T- cells expressed Vβ3, Vβ8 and Vβ12 compared to the control group. No correlation between S. aureus enterotoxin B-stimulated Vβ-expression and HLA-haplotypes was found. In lesional skin of patients with atopic eczema most of the infiltrating T-cells were Vβ3+, whereas in normal skin only very few T-cell receptor-expressing cells were detected. To evaluate the significance of these T-cell clones for allergic inflammation, T-cells from patients with atopic eczema and normal donors were stimulated with monoclonal antibodies against Vβ3, 5(c) and 8. Afterwards, the proliferative response of lymphocytes as well as IL-5 and IFNγ synthesis were measured. T-cells from patients with atopic eczema showed a significantly higher proliferation and IL-5 secretion than normal donors after stimulation with monoclonal antibodies against Vβ3 and Vβ8. In contrast, the monoclonal antibodies directed to Vβ5(c) induced a markedly elevated proliferation and IFNγ production of normal lymphocytes compared to patients with atopic eczema. Our results suggest a preferential expression of certain Vβ-subgroups during inflammation in atopic eczema; this may be explained by a selective stimulation of T(H)2-cells via S. aureus-derived enterotoxins.

Original language	English
Pages (from-to)	214-218
Number of pages	5
Journal	Acta Dermato-Venereologica
Volume	76
Issue number	3
State	Published - 1996
Externally published	Yes

Cite this

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title = "Preferential expression of T-cell receptor Vβ-chains in atopic eczema",

abstract = "Chronic skin colonization with Staphylococcus aureus is a characteristic feature of atopic eczema, and about 60% of S. aureus strains isolated from the skin of patients with atopic eczema secrete enterotoxins. T-cell stimulation by staphylococcal enterotoxins is restricted to the Vβ-chain of the T-cell receptor. Therefore, the expression of different Vβ-chains (Vβ3, 5 a,b,c, 6, 8, 12) on peripheral blood T-cells (CD4+) from patients with atopic eczema was measured by flowcytometry before and after stimulation with staphylococcal enterotoxin B. Lymphocytes from healthy donors served as controls. Additionally, the expression of Vβ-chains in normal skin and in lesional skin of patients with atopic eczema was determined by immunofluorescence histology. In atopic eczema, higher numbers of CD4+ T- cells expressed Vβ3, Vβ8 and Vβ12 compared to the control group. No correlation between S. aureus enterotoxin B-stimulated Vβ-expression and HLA-haplotypes was found. In lesional skin of patients with atopic eczema most of the infiltrating T-cells were Vβ3+, whereas in normal skin only very few T-cell receptor-expressing cells were detected. To evaluate the significance of these T-cell clones for allergic inflammation, T-cells from patients with atopic eczema and normal donors were stimulated with monoclonal antibodies against Vβ3, 5(c) and 8. Afterwards, the proliferative response of lymphocytes as well as IL-5 and IFNγ synthesis were measured. T-cells from patients with atopic eczema showed a significantly higher proliferation and IL-5 secretion than normal donors after stimulation with monoclonal antibodies against Vβ3 and Vβ8. In contrast, the monoclonal antibodies directed to Vβ5(c) induced a markedly elevated proliferation and IFNγ production of normal lymphocytes compared to patients with atopic eczema. Our results suggest a preferential expression of certain Vβ-subgroups during inflammation in atopic eczema; this may be explained by a selective stimulation of T(H)2-cells via S. aureus-derived enterotoxins.",

author = "Karsten Neuber and Cornelius L{\"o}liger and Ingrid K{\"o}hler and Johannes Ring",

year = "1996",

language = "English",

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TY - JOUR

T1 - Preferential expression of T-cell receptor Vβ-chains in atopic eczema

AU - Neuber, Karsten

AU - Löliger, Cornelius

AU - Köhler, Ingrid

AU - Ring, Johannes

PY - 1996

Y1 - 1996

N2 - Chronic skin colonization with Staphylococcus aureus is a characteristic feature of atopic eczema, and about 60% of S. aureus strains isolated from the skin of patients with atopic eczema secrete enterotoxins. T-cell stimulation by staphylococcal enterotoxins is restricted to the Vβ-chain of the T-cell receptor. Therefore, the expression of different Vβ-chains (Vβ3, 5 a,b,c, 6, 8, 12) on peripheral blood T-cells (CD4+) from patients with atopic eczema was measured by flowcytometry before and after stimulation with staphylococcal enterotoxin B. Lymphocytes from healthy donors served as controls. Additionally, the expression of Vβ-chains in normal skin and in lesional skin of patients with atopic eczema was determined by immunofluorescence histology. In atopic eczema, higher numbers of CD4+ T- cells expressed Vβ3, Vβ8 and Vβ12 compared to the control group. No correlation between S. aureus enterotoxin B-stimulated Vβ-expression and HLA-haplotypes was found. In lesional skin of patients with atopic eczema most of the infiltrating T-cells were Vβ3+, whereas in normal skin only very few T-cell receptor-expressing cells were detected. To evaluate the significance of these T-cell clones for allergic inflammation, T-cells from patients with atopic eczema and normal donors were stimulated with monoclonal antibodies against Vβ3, 5(c) and 8. Afterwards, the proliferative response of lymphocytes as well as IL-5 and IFNγ synthesis were measured. T-cells from patients with atopic eczema showed a significantly higher proliferation and IL-5 secretion than normal donors after stimulation with monoclonal antibodies against Vβ3 and Vβ8. In contrast, the monoclonal antibodies directed to Vβ5(c) induced a markedly elevated proliferation and IFNγ production of normal lymphocytes compared to patients with atopic eczema. Our results suggest a preferential expression of certain Vβ-subgroups during inflammation in atopic eczema; this may be explained by a selective stimulation of T(H)2-cells via S. aureus-derived enterotoxins.

AB - Chronic skin colonization with Staphylococcus aureus is a characteristic feature of atopic eczema, and about 60% of S. aureus strains isolated from the skin of patients with atopic eczema secrete enterotoxins. T-cell stimulation by staphylococcal enterotoxins is restricted to the Vβ-chain of the T-cell receptor. Therefore, the expression of different Vβ-chains (Vβ3, 5 a,b,c, 6, 8, 12) on peripheral blood T-cells (CD4+) from patients with atopic eczema was measured by flowcytometry before and after stimulation with staphylococcal enterotoxin B. Lymphocytes from healthy donors served as controls. Additionally, the expression of Vβ-chains in normal skin and in lesional skin of patients with atopic eczema was determined by immunofluorescence histology. In atopic eczema, higher numbers of CD4+ T- cells expressed Vβ3, Vβ8 and Vβ12 compared to the control group. No correlation between S. aureus enterotoxin B-stimulated Vβ-expression and HLA-haplotypes was found. In lesional skin of patients with atopic eczema most of the infiltrating T-cells were Vβ3+, whereas in normal skin only very few T-cell receptor-expressing cells were detected. To evaluate the significance of these T-cell clones for allergic inflammation, T-cells from patients with atopic eczema and normal donors were stimulated with monoclonal antibodies against Vβ3, 5(c) and 8. Afterwards, the proliferative response of lymphocytes as well as IL-5 and IFNγ synthesis were measured. T-cells from patients with atopic eczema showed a significantly higher proliferation and IL-5 secretion than normal donors after stimulation with monoclonal antibodies against Vβ3 and Vβ8. In contrast, the monoclonal antibodies directed to Vβ5(c) induced a markedly elevated proliferation and IFNγ production of normal lymphocytes compared to patients with atopic eczema. Our results suggest a preferential expression of certain Vβ-subgroups during inflammation in atopic eczema; this may be explained by a selective stimulation of T(H)2-cells via S. aureus-derived enterotoxins.

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AN - SCOPUS:0029997929

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Preferential expression of T-cell receptor Vβ-chains in atopic eczema

Abstract

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