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骨髓移植后T细胞库的改变:过度表达亚群的特征分析。

Alterations of T cell repertoire after bone marrow transplantation: characterization of over-represented subsets.

作者信息

Gaschet J, Denis C, Milpied N, Hallet M M, Romagné F, Necker A, Vivien R, David-Ameline J, Davodeau F, Bonneville M

机构信息

INSERM U211, Institut de Biologie, Nantes, France.

出版信息

Bone Marrow Transplant. 1995 Sep;16(3):427-35.

PMID:8535316
Abstract

We recently demonstrated that frequencies of T cell receptor-V (TcR-V)-specific subsets are frequently altered after both allogeneic and autologous BMT. The data reported here describe several characteristics of altered T cell subsets: (i) their capacity to endure peripherally, (ii) their correspondence to clonal donor T cell subsets, (iii) the origin of the clone (in one case amenable to analysis) from a mature T cell and not from new lymphopoiesis, and (iv) the presence of such a clone throughout a year of follow-up in a patient with chronic graft-versus-host disease (GVHD) in whom it represented up to 1/10th of CD3+ peripheral blood lymphocytes (PBL) and was found to be host-reactive. Taken together, these findings provide direct evidence for the oligoclonality of a large proportion of the peripheral T cell repertoire in patients subsequent to bone marrow transplantation, possibly accounting for their frequent depressed immune status. Moreover, the anti-host reactivity demonstrated in a clone from the patient with chronic GVHD strongly suggests that an oligoclonal response can be linked to a pathological process.

摘要

我们最近证明,在同种异体和自体骨髓移植后,T细胞受体-V(TcR-V)特异性亚群的频率经常发生改变。此处报告的数据描述了T细胞亚群改变的几个特征:(i)它们在外周持续存在的能力;(ii)它们与克隆性供体T细胞亚群的对应关系;(iii)克隆(在一个可进行分析的病例中)起源于成熟T细胞而非新的淋巴细胞生成;(iv)在一名慢性移植物抗宿主病(GVHD)患者的一年随访中存在这样一个克隆,在该患者中它占CD3⁺外周血淋巴细胞(PBL)的1/10,并且被发现具有宿主反应性。综上所述,这些发现为骨髓移植后患者外周T细胞库中很大一部分的寡克隆性提供了直接证据,这可能是他们免疫状态频繁低下的原因。此外,在慢性GVHD患者的一个克隆中表现出的抗宿主反应强烈表明,寡克隆反应可能与病理过程有关。

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