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胎儿存活:胎儿 B 和 T 细胞受体库发育。

Survival of the fetus: fetal B and T cell receptor repertoire development.

机构信息

Pediatric Department A and Immunology Service, Jeffrey Modell Foundation Center, "Edmond and Lily Safra" Children's Hospital, Sheba Medical Center, Tel Hashomer, Sackler School of Medicine, Tel Aviv University, 6997801, Tel Aviv, Israel.

出版信息

Semin Immunopathol. 2017 Nov;39(6):577-583. doi: 10.1007/s00281-017-0626-0. Epub 2017 May 2.

DOI:10.1007/s00281-017-0626-0
PMID:28466095
Abstract

A mature and diverse T and B cell receptor repertoire is a prerequisite for immunocompetence. In light of its increased susceptibility to infection, the human fetus has long been considered deficient in this regard. However, data accumulated since the 1990s and in earnest in the past couple of years paints a more complicated picture. As we describe in this review, mechanisms responsible for generating a diverse receptor repertoire, such as somatic recombination, class switch recombination, and somatic hypermutation, are all operational to surprising extents in the growing fetus. The composition of the fetal repertoire differs from that of adults, with preferential usage of certain variable (V), diversity (D), and joining (J) gene segments and a shorter complementarity determining (CDR3) region, primarily due to decreased terminal deoxynucleotidyl transferase (TdT) expression. Both T and B cell receptor repertoires are extremely diverse by the end of the second trimester, and in the case of T cells, are capable of responding to an invading pathogen with in utero clonal expansion. Thus, it would appear as though the T and B cell receptor repertoires are not a hindrance towards immunocompetence of the newborn. Our improved understanding of fetal receptor repertoire development is already bearing fruit in the early diagnosis of primary immunodeficiencies (PID) and may help clarify the pathogenesis of congenital infections, recurrent abortions, and autoimmune disorders in the near future.

摘要

成熟且多样化的 T 细胞和 B 细胞受体库是免疫能力的前提。鉴于其对感染的易感性增加,人类胎儿在这方面长期以来一直被认为存在缺陷。然而,自 20 世纪 90 年代以来积累的数据,以及近年来的认真研究,描绘出了一幅更为复杂的图景。正如我们在这篇综述中所描述的,负责产生多样化受体库的机制,如体细胞重组、类别转换重组和体细胞超突变,在不断发育的胎儿中都以惊人的程度运作着。胎儿受体库的组成与成人不同,主要是由于末端脱氧核苷酸转移酶 (TdT) 表达减少,因此存在某些特定的可变 (V)、多样性 (D) 和连接 (J) 基因片段的优先使用,以及较短的互补决定区 (CDR3) 区域。到第二个妊娠期末,T 细胞和 B 细胞受体库都变得极其多样化,而在 T 细胞中,能够通过宫内克隆扩增对入侵病原体产生反应。因此,似乎 T 和 B 细胞受体库并不会阻碍新生儿的免疫能力。我们对胎儿受体库发育的理解的提高,已经在原发性免疫缺陷 (PID) 的早期诊断中取得了成果,并可能有助于在不久的将来阐明先天性感染、反复流产和自身免疫性疾病的发病机制。

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History and current status of newborn screening for severe combined immunodeficiency.
组织中巨细胞病毒的免疫监视。
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Making inroads to precision medicine for the treatment of autoimmune diseases: Harnessing genomic studies to better diagnose and treat complex disorders.在自身免疫性疾病治疗中迈向精准医学:利用基因组研究更好地诊断和治疗复杂疾病。
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