High frequency of circulating ¿d T cells with dominance of the vd1 subset in a healthy population

L Hviid; B D Akanmori; S Loizon; J A Kurtzhals; C H Ricke; A Lim; K A Koram; F K Nkrumah; O Mercereau-Puijalon; C Behr

High frequency of circulating ¿d T cells with dominance of the vd1 subset in a healthy population

L Hviid, B D Akanmori, S Loizon, J A Kurtzhals, C H Ricke, A Lim, K A Koram, F K Nkrumah, O Mercereau-Puijalon, C Behr

54 Citationer (Scopus)

Abstract

Udgivelsesdato: 2000-Jun

Originalsprog	Engelsk
Tidsskrift	International Immunology
Vol/bind	12
Udgave nummer	6
Sider (fra-til)	797-805
Antal sider	8
ISSN	0953-8178
Status	Udgivet - 2000

Citationsformater

@article{93b09200a03b11dd86a6000ea68e967b,

title = "High frequency of circulating ¿d T cells with dominance of the vd1 subset in a healthy population",

abstract = "TCR gamma delta(+) cells constitute <5% of all circulating T cells in healthy, adult Caucasians, and V(delta)1(+) cells constitute a minority of these cells. In contrast to TCR alpha beta(+) cells, their repertoire is selected extrathymically by environmental antigens. Although increased frequencies of V(delta)1(+) cells are found in several diseases, their function remains obscure. Here we show that the frequency of peripheral blood gamma delta T cells in healthy West Africans is about twice that of Caucasians, mainly due to a 5-fold increase in V(delta)1(+) cells, which is consequently the dominant subset. No age dependency of V(delta)1 frequencies was identified and the V(delta)1(+) cells in the African donors did not show preferential V(gamma) chain usage. Analysis of the CDR3 region size did not reveal any particular skewing of the V(delta)1 repertoire, although oligoclonality was more pronounced in adults compared to children. The proportions of CD8(+), CD38(+) and CD45RA(hi)CD45RO(-) cells within the V(delta)1(+) subset were higher in the African than in the European donors, without obvious differences in expression of activation markers. No significant correlations between levels of V(delta)1(+) cells and environmental antigens or immunological parameters were identified. Taken together, the evidence argues against a CDR3-restricted, antigen-driven expansion of V(delta)1(+) cells in the African study population. Our study shows that high frequencies of TCR gamma delta(+) cells with dominance of the V(delta)1(+) subset can occur at the population level in healthy people, raising questions about the physiological role of V(delta)1(+) T cells in the function and regulation of the immune system.",

author = "L Hviid and Akanmori, {B D} and S Loizon and Kurtzhals, {J A} and Ricke, {C H} and A Lim and Koram, {K A} and Nkrumah, {F K} and O Mercereau-Puijalon and C Behr",

note = "Keywords: Adult; African Continental Ancestry Group; Age Factors; Child; European Continental Ancestry Group; Humans; Immunoglobulin G; Immunophenotyping; Malaria; Parasitemia; Receptors, Antigen, T-Cell, gamma-delta; T-Lymphocyte Subsets",

year = "2000",

language = "English",

volume = "12",

pages = "797--805",

journal = "International Immunology",

issn = "0953-8178",

publisher = "Oxford University Press",

number = "6",

}

TY - JOUR

T1 - High frequency of circulating ¿d T cells with dominance of the vd1 subset in a healthy population

AU - Hviid, L

AU - Akanmori, B D

AU - Loizon, S

AU - Kurtzhals, J A

AU - Ricke, C H

AU - Lim, A

AU - Koram, K A

AU - Nkrumah, F K

AU - Mercereau-Puijalon, O

AU - Behr, C

N1 - Keywords: Adult; African Continental Ancestry Group; Age Factors; Child; European Continental Ancestry Group; Humans; Immunoglobulin G; Immunophenotyping; Malaria; Parasitemia; Receptors, Antigen, T-Cell, gamma-delta; T-Lymphocyte Subsets

PY - 2000

Y1 - 2000

N2 - TCR gamma delta(+) cells constitute <5% of all circulating T cells in healthy, adult Caucasians, and V(delta)1(+) cells constitute a minority of these cells. In contrast to TCR alpha beta(+) cells, their repertoire is selected extrathymically by environmental antigens. Although increased frequencies of V(delta)1(+) cells are found in several diseases, their function remains obscure. Here we show that the frequency of peripheral blood gamma delta T cells in healthy West Africans is about twice that of Caucasians, mainly due to a 5-fold increase in V(delta)1(+) cells, which is consequently the dominant subset. No age dependency of V(delta)1 frequencies was identified and the V(delta)1(+) cells in the African donors did not show preferential V(gamma) chain usage. Analysis of the CDR3 region size did not reveal any particular skewing of the V(delta)1 repertoire, although oligoclonality was more pronounced in adults compared to children. The proportions of CD8(+), CD38(+) and CD45RA(hi)CD45RO(-) cells within the V(delta)1(+) subset were higher in the African than in the European donors, without obvious differences in expression of activation markers. No significant correlations between levels of V(delta)1(+) cells and environmental antigens or immunological parameters were identified. Taken together, the evidence argues against a CDR3-restricted, antigen-driven expansion of V(delta)1(+) cells in the African study population. Our study shows that high frequencies of TCR gamma delta(+) cells with dominance of the V(delta)1(+) subset can occur at the population level in healthy people, raising questions about the physiological role of V(delta)1(+) T cells in the function and regulation of the immune system.

AB - TCR gamma delta(+) cells constitute <5% of all circulating T cells in healthy, adult Caucasians, and V(delta)1(+) cells constitute a minority of these cells. In contrast to TCR alpha beta(+) cells, their repertoire is selected extrathymically by environmental antigens. Although increased frequencies of V(delta)1(+) cells are found in several diseases, their function remains obscure. Here we show that the frequency of peripheral blood gamma delta T cells in healthy West Africans is about twice that of Caucasians, mainly due to a 5-fold increase in V(delta)1(+) cells, which is consequently the dominant subset. No age dependency of V(delta)1 frequencies was identified and the V(delta)1(+) cells in the African donors did not show preferential V(gamma) chain usage. Analysis of the CDR3 region size did not reveal any particular skewing of the V(delta)1 repertoire, although oligoclonality was more pronounced in adults compared to children. The proportions of CD8(+), CD38(+) and CD45RA(hi)CD45RO(-) cells within the V(delta)1(+) subset were higher in the African than in the European donors, without obvious differences in expression of activation markers. No significant correlations between levels of V(delta)1(+) cells and environmental antigens or immunological parameters were identified. Taken together, the evidence argues against a CDR3-restricted, antigen-driven expansion of V(delta)1(+) cells in the African study population. Our study shows that high frequencies of TCR gamma delta(+) cells with dominance of the V(delta)1(+) subset can occur at the population level in healthy people, raising questions about the physiological role of V(delta)1(+) T cells in the function and regulation of the immune system.

M3 - Journal article

C2 - 10837407

SN - 0953-8178

VL - 12

SP - 797

EP - 805

JO - International Immunology

JF - International Immunology

IS - 6

ER -

High frequency of circulating ¿d T cells with dominance of the vd1 subset in a healthy population

Abstract

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