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胸腺激素对DBA/2J淋巴细胞诱导移植物抗宿主病中年龄诱导变化的调节作用。

Thymic hormone modulation of age-induced changes in the induction of graft-versus-host disease by DBA/2J lymphocytes.

作者信息

Fast L D, Kouttab N M, Badamchian M, Goldstein A L

机构信息

Department of Medicine, Rhode Island Hospital, Providence.

出版信息

Cell Immunol. 1990 Nov;131(1):232-41. doi: 10.1016/0008-8749(90)90249-q.

Abstract

Aging induces a number of changes in the immune system, including the involution of the thymus which results in the loss of thymic hormone production and alteration in T cell function. One age-dependent change in immune response is the increasing risk of developing acute or chronic form of graft-versus-host disease (GVHD) following bone marrow transplantation as the age of the recipient increases. A murine model of GVHD that has been extensively studied is one in which injection of C57BL/6 spleen cells into unirradiated B6D2F1 mice results in an acute form of GVHD characterized by cytolytic T lymphocytes (CTL), suppressor cells, runting, and occasionally death. In contrast, injection of DBA/2J spleen cells results in a chronic form of GVHD characterized by a lack of CTL and hyperproduction of immunoglobulin and autoantibodies. This study shows that the GVHD response of DBA/2J spleen cells is dependent on the age of the donor DBA/2J mice. If spleen cells from DBA/2J mice older than 3 months are injected into B6D2F1 recipients, CTL and lack of immunoglobulin production indicative of acute GVHD result. Administration of thymosin fraction 5, a collection of thymic hormones, to DBA/2J mice older than 3 months caused spleen cells from these treated mice to give a GVHD response characteristic of the chronic form of GVHD in B6D2F1 recipients. Thus, thymic hormones were able to modulate the changes in GVHD responses of DBA/2 lymphocytes that occur as the mice age. Preliminary fractionation of TF5 has indicated that there are at least two active thymic peptides present in TF5.

摘要

衰老会引发免疫系统的一系列变化,包括胸腺退化,这会导致胸腺激素分泌丧失以及T细胞功能改变。免疫反应中一个与年龄相关的变化是,随着骨髓移植受体年龄的增加,发生急性或慢性移植物抗宿主病(GVHD)的风险也在增加。一种被广泛研究的GVHD小鼠模型是,将C57BL/6脾细胞注射到未受照射的B6D2F1小鼠体内,会导致以细胞溶解性T淋巴细胞(CTL)、抑制细胞、发育迟缓以及偶尔死亡为特征的急性GVHD。相比之下,注射DBA/2J脾细胞会导致以缺乏CTL以及免疫球蛋白和自身抗体过度产生为特征的慢性GVHD。这项研究表明,DBA/2J脾细胞的GVHD反应取决于供体DBA/2J小鼠的年龄。如果将3个月以上DBA/2J小鼠的脾细胞注射到B6D2F1受体小鼠体内,就会产生CTL以及缺乏免疫球蛋白产生的情况,这表明出现了急性GVHD。给3个月以上的DBA/2J小鼠注射胸腺素组分5(一种胸腺激素混合物),会使这些经处理小鼠的脾细胞在B6D2F1受体小鼠中产生慢性GVHD形式的GVHD反应特征。因此,胸腺激素能够调节随着小鼠年龄增长而发生的DBA/2淋巴细胞GVHD反应的变化。TF5的初步分级分离表明,TF5中至少存在两种活性胸腺肽。

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