Fc gamma RII/III and CD2 expression mark distinct subpopulations of immature CD4-CD8- murine thymocytes: in vivo developmental kinetics and T cell receptor beta chain rearrangement status.

H R Rodewald; K Awad; P Moingeon; L DAdamio; D Rabinowitz; Y Shinkai; F W Alt; E L Reinherz

首页> 外文期刊>The Journal of Experomental Medicine >Fc gamma RII/III and CD2 expression mark distinct subpopulations of immature CD4-CD8- murine thymocytes: in vivo developmental kinetics and T cell receptor beta chain rearrangement status.

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Fc gamma RII/III and CD2 expression mark distinct subpopulations of immature CD4-CD8- murine thymocytes: in vivo developmental kinetics and T cell receptor beta chain rearrangement status.

机译：FcγRII / III和CD2表达标记未成熟CD4-CD8-鼠胸腺细胞的不同亚群：体内发育动力学和T细胞受体β链重排状态。

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We have recently identified a dominant wave of CD4-CD8- (double-negative [DN]) thymocytes in early murine fetal development that express low affinity Fc gamma receptors (Fc gamma RII/III) and contain precursors for Ti alpha/beta lineage T cells. Here we show that Fc gamma RII/III is expressed in very immature CD4low single-positive (SP) thymocytes and that Fc gamma RII/III expression is downregulated within the DN subpopulation and before the CD3-CD8low SP stage in T cell receptor (TCR)-alpha/beta lineage-committed thymocytes. DN Fc gamma RII/III+ thymocytes also contain a small fraction of TCR-gamma/delta lineage cells in addition to TCR-alpha/beta progenitors. Fetal day 15.5 DN TCR-alpha/beta lineage progenitors can be subdivided into three major subpopulations as characterized by cell surface expression of Fc gamma RII/III vs. CD2 (Fc gamma RII/III+CD2-, Fc gamma RII/III+CD2+, Fc gamma RII/III-CD2+). Phenotypic analysis during fetal development as well as adoptive transfer of isolated fetal thymocyte subpopulations derived from C57B1/6 (Ly5.1) mice into normal, nonirradiated Ly5.2 congenic recipient mice identifies one early differentiation sequence (Fc gamma RII/III+CD2(-)--Fc gamma RII/III+CD2(+)--Fc gamma RII/III-CD2+) that precedes the entry of DN thymocytes into the CD4+CD8+ double-positive (DP) TCRlow/- stage. Unseparated day 15.5 fetal thymocytes develop into DP thymocytes within 2.5 d and remain at the DP stage for 48 h before being selected into either CD4+ or CD8+ SP thymocytes. In contrast, Fc gamma RII/III+CD2- DN thymocytes follow this same developmental pathway but are delayed by approximately 24 h before entering the DP compartment, while Fc gamma RII/III-CD2+ display accelerated development by approximately 24 h compared with total day 15.5 thymocytes. Fc gamma RII/III-CD2+ are also more developmentally advanced than Fc gamma RII/III+CD2- fetal thymocytes with respect to their TCR beta chain V(D)J rearrangement. At day 15.5 in gestation, beta chain V(D)J rearrangement is mostly, if not entirely, restricted to the Fc gamma RII/III-CD2+ subset of DN fetal thymocytes. Consistent with this analysis in fetal thymocytes, 90% of adult thymocytes derived from mice carrying a disrupting mutation at the recombination-activating gene 2 locus (RAG-2-/-) on both alleles are developmentally arrested at the DN CD2- stage. In addition, there is a fivefold increase in the relative percentage of thymocytes expressing Fc gamma RII/III in TCR and immunoglobulin gene rearrangement-incompetent homozygous RAG-2-/- mice (15% Fc gamma RII/III+) versus rearrangement-competent heterozygous RAG-2+/- mice ( 3% Fc gamma RII/III+). Thus, Fc gamma RII/III expression defines an early DN stage preceding V beta(D beta)I beta rearrangement, which in turn is followed by surface expression of CD2. Loss of Fc gamma RII/III and acquisition of CD2 expression characterize a late DN stage immediately before the conversion into DP thymocytes.

机译：我们最近在早期小鼠胎儿发育中发现了CD4-CD8-（双阴性[DN]）胸腺细胞的主导波，这些胸腺细胞表达低亲和力Fcγ受体（FcγRII / III），并含有Ti alpha /β谱系T的前体细胞。在这里，我们显示FcγRII / III在非常不成熟的CD4low单阳性（SP）胸腺细胞中表达，并且FcγRII / III的表达在DN亚群内以及在T细胞受体（TCR）的CD3-CD8low SP阶段之前被下调。）-α/β谱系定型的胸腺细胞。 DN FcγRII / III +胸腺细胞除TCR-α/β祖细胞外，还包含一小部分TCR-γ/δ谱系细胞。胎儿15.5 DNTCR-α/β世系祖细胞可分为三个主要亚群，其特征为FcγRII / III与CD2（FcγRII / III + CD2-，FcγRII/ III + CD2 + ，FcγRII / III-CD2 +）。胎儿发育过程中的表型分析以及源自C57B1 / 6（Ly5.1）小鼠的分离的胎儿胸腺细胞亚群过继转移至正常的，未经辐照的Ly5.2同系受体小鼠中，鉴定出一种早期分化序列（FcγRII / III + CD2（ -）-> FcγRII / III + CD2（+）-> FcγRII / III-CD2 +）在DN胸腺细胞进入CD4 + CD8 +双阳性（DP）TCRlow /-阶段之前。在分离后的第15.5天，胎儿胸腺细胞在2.5 d内发育为DP胸腺细胞，并在进入DP阶段的时间大于48小时，然后被选为CD4 +或CD8 + SP胸腺细胞。相比之下，FcγRII / III + CD2- DN胸腺细胞遵循相同的发育途径，但在进入DP隔室之前被延迟了约24 h，而FcγRII / III-CD2 +与全天相比显示出了约24 h的加速发育。 15.5胸腺细胞。就其TCRβ链V（D）J重排而言，FcγRII / III-CD2 +也比FcγRII / III + CD2-胎儿胸腺细胞发育更先进。在妊娠的第15.5天，β链V（D）J重排大部分（如果不是全部）局限于DN胎儿胸腺细胞的FcγRII / III-CD2 +亚群。与胎儿胸腺细胞中的该分析一致，在两个等位基因上在重组激活基因2位点（RAG-2-/-）携带破坏突变的小鼠中，有超过90％的成年胸腺细胞在DN CD2-阶段发育停滞。此外，与具有重排能力的杂合子相比，TCR和免疫球蛋白基因不能重排的纯合子RAG-2-/-小鼠（15％FcγRII / III +）中表达FcγRII / III的胸腺细胞的相对百分比增加了五倍RAG-2 +/-小鼠（<3％FcγRII / III +）。因此，FcγRII / III表达定义了在V beta（D beta）I beta重排之前的早期DN阶段，依次是CD2的表面表达。 FcγRII / III的丢失和CD2表达的获得是DN晚期的一个特征，即即将转化为DP胸腺细胞之前。

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《The Journal of Experomental Medicine》 |1993年第4期|共14页
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H R Rodewald; K Awad; P Moingeon; L DAdamio; D Rabinowitz; Y Shinkai; F W Alt; E L Reinherz;
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1. Signal transduction by the CD2 antigen in T cells and natural killer cells: requirement for expression of a functional T cell receptor or binding of antibody Fc to the Fc receptor, Fc gamma RIIIA (CD16). [J] . L L Spruyt, M J Glennie, A D Beyers, The Journal of Experomental Medicine . 1991,第6期

机译：T细胞和自然杀伤细胞中CD2抗原的信号转导：表达功能性T细胞受体或抗体Fc与Fc受体FcγRIIIA（CD16）结合的要求。
2. Lipopolysaccharide-induced suppression of erythrocyte binding and phagocytosis via Fc gamma RI, Fc gamma RII, Fc gamma RIII, and CR3 receptors in murine macrophages. [J] . A Ghaffar, E P Mayer, J D Gangemi, Journal of Leukocyte Biology: An Official Publication of the Reticuloendothelial Society . 1993,第1期

机译：脂多糖诱导的巨噬细胞中通过FcγRI，FcγRII，FcγRIII和CR3受体抑制红细胞结合和吞噬作用。
3. Developmentally regulated expression of T cell receptor beta chain variable domains in immature thymocytes. [J] . R C Budd, G C Miescher, R C Howe, The Journal of Experomental Medicine . 1987,第2期

机译：T细胞受体β链可变域在未成熟胸腺细胞中的发育调控表达。
4. T cell development and gamma/delta T cell antigen receptor: I. Structure and rearrangement of murine T cell antigen receptor delta chain gene. II. Expression of fetal type gamma/delta T cell receptor in adult transgenic mice and its effects on T cell development. [D] . Iwashima, Makio. 1990

机译：T细胞发育和γ/δT细胞抗原受体：I.鼠T细胞抗原受体δ链基因的结构和重排。二。胎儿型γ/δT细胞受体在成年转基因小鼠中的表达及其对T细胞发育的影响。
5. Fc gamma RII/III and CD2 expression mark distinct subpopulations of immature CD4-CD8- murine thymocytes: in vivo developmental kinetics and T cell receptor beta chain rearrangement status [O] . 1993

机译：FcγRII / III和CD2表达标记未成熟CD4-CD8-鼠胸腺细胞的不同亚群：体内发育动力学和T细胞受体β链重排状态
6. Fc gamma RII/III and CD2 expression mark distinct subpopulations of immature CD4-CD8- murine thymocytes: in vivo developmental kinetics and T cell receptor beta chain rearrangement status [O] . 1993

机译：FcγRII / III和CD2表达标记未成熟CD4-CD8-鼠胸腺细胞的不同亚群：体内发育动力学和T细胞受体β链重排状态

Fc gamma RII/III and CD2 expression mark distinct subpopulations of immature CD4-CD8- murine thymocytes: in vivo developmental kinetics and T cell receptor beta chain rearrangement status.

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