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尽管小鼠胸腺中末端脱氧核苷酸转移酶表达水平较低,但出生时T细胞受体α基因仍产生了大量的N多样性。

Substantial N diversity is generated in T cell receptor alpha genes at birth despite low levels of terminal deoxynucleotidyl transferase expression in mouse thymus.

作者信息

Cherrier Marie, Cardona Ana, Rosinski-Chupin Isabelle, Rougeon François, Doyen Noëlle

机构信息

Genetics and Developmental Biochemistry Unit CNRS, URA 1960, Department of Immunology, Pasteur Institute, Paris, France.

出版信息

Eur J Immunol. 2002 Dec;32(12):3651-6. doi: 10.1002/1521-4141(200212)32:12<3651::AID-IMMU3651>3.0.CO;2-D.

Abstract

N region diversity in antigen receptors is a developmentally regulated process in B and T lymphocytes, which correlates with the differential expression of terminal deoxynucleotidyl transferase (TdT). To precisely determine the onset of TdT gene activation during T cell differentiation and thymic ontogeny, TdT expression was directly detected at the cellular level by in situ hybridization and TdT function was assessed by analyzing the distribution of N additions in alpha and beta TCR genes at early stages of development. Even though TdT transcripts were undetectable at birth, substantial N additions were observed in ValphaJalpha junctions and 3 days later in VbetaDbetaJbeta junctions, indicating that TdT expression could be induced in immature thymocytes much earlier than expected. Indeed low TdT expression level was found in TN3/4 and DP from fetal day 17, suggesting that the onset of TdT expression occurs simultaneously in both populations and may depend on microenvironmental cues. Moreover significant increase in the proportion of thymocytes expressing high levels of TdT mRNA during the first week after birth without a similar increase in the level of N diversity suggests that TdT expression and TdT function in the generation of N diversity are not strictly correlated.

摘要

抗原受体中的N区多样性是B淋巴细胞和T淋巴细胞中一个受发育调控的过程,它与末端脱氧核苷酸转移酶(TdT)的差异表达相关。为了精确确定T细胞分化和胸腺发育过程中TdT基因激活的起始时间,通过原位杂交在细胞水平直接检测TdT表达,并通过分析发育早期α和β TCR基因中N添加的分布来评估TdT功能。尽管出生时检测不到TdT转录本,但在VαJα连接处观察到大量N添加,3天后在VβDβJβ连接处也观察到大量N添加,这表明TdT表达可在未成熟胸腺细胞中比预期更早地被诱导。事实上,从胚胎第17天起,在TN3/4和双阳性(DP)细胞中发现了低水平的TdT表达,这表明TdT表达的起始在这两个群体中同时发生,并且可能依赖于微环境信号。此外,出生后第一周内,表达高水平TdT mRNA的胸腺细胞比例显著增加,而N多样性水平没有类似增加,这表明TdT表达与N多样性产生过程中的TdT功能并不严格相关。

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