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致死性照射和骨髓移植后,辐射抗性造血细胞重建 T 细胞区室。

Auto-reconstitution of the T-cell compartment by radioresistant hematopoietic cells following lethal irradiation and bone marrow transplantation.

机构信息

Department of Biomedicine, Group of Developmental and Molecular Immunology, University of Basel, Basel, Switzerland.

出版信息

Exp Hematol. 2010 Mar;38(3):222-232.e2. doi: 10.1016/j.exphem.2009.12.006. Epub 2010 Jan 4.

Abstract

OBJECTIVE

In lethally irradiated bone marrow chimeras, part of the reconstituted T-cell compartment is derived from the irradiated host, but the detailed origin and functional activity of host-derived T cells has not been thoroughly analyzed. Herein, we determine the origin and function of radioresistant host-derived T cells.

MATERIALS AND METHODS

Lethally irradiated thymectomized or nonthymectomized C57BL/6 host mice were reconstituted with syngeneic bone marrow, itself incapable of generating T cells. Using fetal thymic organ cultures, bulk and limiting dilution assays on OP9-DL1 stromal cells, unambiguous cohorts of thymus-derived and peripheral T-cell-derived T cells were phenotypically characterized by flow cytometry and functionally characterized by their ability to participate in a T-cell-dependent antibody response.

RESULTS

Both thymus-derived and peripheral T-cell-derived host T cells are functional and can reconstitute 35% of the normal T-cell pool. By comparing thymectomized vs nonthymectomized hosts, host-derived T cells were shown to comprise a major (70%) subpopulation of de novo generated, thymus-derived, polyclonal, naïve cells, and a minor subpopulation of surviving, peripheral, oligoclonal, memory-like cells. Unlike euthymic recipients, mice whose T cells were derived from surviving peripheral T cells were frequently incapable of mounting a T-cell-dependent antibody response. Host-derived thymocytes regenerated in an interleukin-7-dependent fashion from conventional DN2 thymocytes and their differentiation recapitulated normal thymic ontogeny.

CONCLUSION

We characterized, for the first time, functional radioresistant DN2-phenotype thymic T-cell precursors, the T-cell progeny of which might provide a first line of defense against infections during the lymphopenic phase post-bone marrow transplantation.

摘要

目的

在致死剂量照射的骨髓嵌合体中,部分重建的 T 细胞群来源于受照射的宿主,但宿主来源的 T 细胞的详细起源和功能活性尚未得到彻底分析。在此,我们确定了耐辐射宿主来源 T 细胞的起源和功能。

材料和方法

用本身不能产生 T 细胞的同基因骨髓重建致死剂量照射的胸腺切除或非胸腺切除 C57BL/6 宿主小鼠。使用胎胸腺器官培养物、在 OP9-DL1 基质细胞上进行的批量和有限稀释测定,通过流式细胞术对胸腺来源和外周 T 细胞来源的 T 细胞进行明确的表型特征分析,并通过参与 T 细胞依赖性抗体反应的能力对其功能进行特征分析。

结果

胸腺来源和外周 T 细胞来源的宿主 T 细胞均具有功能,可以重建正常 T 细胞池的 35%。通过比较胸腺切除和非胸腺切除的宿主,宿主来源的 T 细胞包含由新生成的、胸腺来源的、多克隆、幼稚细胞组成的主要(70%)亚群,以及存活的、外周的、寡克隆、记忆样细胞组成的次要亚群。与正常宿主相比,其 T 细胞来源于存活的外周 T 细胞的宿主,常常无法产生 T 细胞依赖性抗体反应。宿主来源的胸腺细胞以依赖白细胞介素-7 的方式从常规 DN2 胸腺细胞中再生,其分化过程再现了正常的胸腺发生。

结论

我们首次对功能性耐辐射的 DN2 表型胸腺 T 细胞前体进行了特征描述,其 T 细胞后代可能为骨髓移植后淋巴细胞减少期的感染提供第一道防线。

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