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重症联合免疫缺陷中T淋巴细胞的体外分化。干细胞缺陷。

T-lymphocyte differentiation in vitro in severe combined immunodeficiency. Defects of stem cells.

作者信息

Pahwa R N, Pahwa S G, Good R A

出版信息

J Clin Invest. 1979 Dec;64(6):1632-41. doi: 10.1172/JCI109625.

Abstract

A study of T-lymphocyte differentiation was made on fractionated bone marrow cells from normal volunteers and from 11 patients with severe combined immunodeficiency (SCID) using normal thymic epithelial monolayers and their culture supernates as inducing agents. Normal marrow cells could regularly be induced to bear the human T-lymphocyte antigen (HTLA), to form rosettes with sheep erythrocytes (E rosettes), and to respond to the mitogen concanavalin A (Con A) after coculture with the thymic epithelial monolayers or their culture supernates. In contrast, studies of T-cell differentiation on the marrow cells of patients with SCID revealed varying defects, ranging from a complete "absence" of definable T-cell precursors to partial differentiation resulting in acquisition of one (HTLA) or two (HTLA and E rosettes) markers for T lymphocytes. Only in one patient was there induction of all three T-cell markers, namely, HTLA, E rosettes, and responsiveness to Con A. These observations indicate that SCID is a heterogeneous disorder in which defects of differentiation can occur at one or more multiple sites of differentiation leading the the clinical expression of T- and B-cell dysfunction. Further, our studies indicate that in T-cell differentiation, HTLA probably appears before the capacity to form E-rosettes, and development of the latter capacity is followed by a state of responsiveness to mitogens. A scheme of normal differentiation along with the defects of precursor T cells seen in SCID is presented.

摘要

利用正常胸腺上皮单层细胞及其培养上清液作为诱导剂,对正常志愿者和11例严重联合免疫缺陷(SCID)患者的分离骨髓细胞进行了T淋巴细胞分化研究。正常骨髓细胞与胸腺上皮单层细胞或其培养上清液共培养后,可被定期诱导产生人类T淋巴细胞抗原(HTLA),与绵羊红细胞形成花环(E花环),并对促有丝分裂原刀豆球蛋白A(Con A)作出反应。相比之下,对SCID患者骨髓细胞的T细胞分化研究显示出不同程度的缺陷,从完全“缺乏”可定义的T细胞前体到部分分化,导致获得一种(HTLA)或两种(HTLA和E花环)T淋巴细胞标志物。只有一名患者诱导出了所有三种T细胞标志物,即HTLA、E花环和对Con A的反应性。这些观察结果表明,SCID是一种异质性疾病,其中分化缺陷可发生在一个或多个分化位点,导致T细胞和B细胞功能障碍的临床表现。此外,我们的研究表明,在T细胞分化过程中,HTLA可能在形成E花环的能力之前出现,而后者能力的发展之后是对促有丝分裂原的反应状态。本文给出了正常分化的示意图以及SCID中所见前体T细胞的缺陷。

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