Transforming growth factor beta 1 (TGF-beta 1) controls expression of major histocompatibility genes in the postnatal mouse: aberrant histocompatibility antigen expression in the pathogenesis of the TGF-beta 1 null mouse phenotype.

机译：转化生长因子beta 1（TGF-beta 1）控制出生后小鼠中主要组织相容性基因的表达：在TGF-beta 1空小鼠表型的发病机理中异常的组织相容性抗原表达。

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The phenotype of the transforming growth factor beta 1 (TGF-beta 1) null mouse has been previously described and is characterized by inflammatory infiltrates in multiple organs leading to a wasting syndrome and death as early as 3 weeks after birth. Since this phenotype occurs in the absence of any detectable pathogen, potential autoimmune disease mechanisms were investigated. We examined major histocompatibility complex (MHC) mRNA expression in tissues of the TGF-beta 1 null mouse and found levels of both the class I and class II MHC mRNA elevated compared to normal or TGF-beta 1 heterozygous littermates. This elevated expression was seen prior to any evidence of inflammatory infiltrates, suggesting a causal relationship between increased MHC expression and activation of immune cell populations. Cell surface expression of MHC molecules was detected by immunohistochemistry and correlated well with mRNA levels. Expression of mRNA for interferon gamma and its receptor was unchanged at the ages when increased MHC expression became apparent. Down-regulation of class I MHC expression by TGF-beta 1 was also demonstrated in vitro in fibroblasts isolated from TGF-beta 1 null mice. These findings suggest that one natural function of TGF-beta 1 is to control expression of both MHC classes. Altered regulation of MHC expression may be a critical step leading to the multifocal inflammation and wasting syndrome seen in the TGF-beta 1 null mouse. These results suggest potential applications for TGF-beta in the management of autoimmune disease, allograft rejection, and other problems associated with altered MHC expression.

机译：先前已经描述了转化生长因子beta 1（TGF-beta 1）无效小鼠的表型，其特征是早在出生后3周就在多个器官中引起炎症浸润，导致消耗综合征和死亡。由于这种表型是在没有任何可检测病原体的情况下发生的，因此研究了潜在的自身免疫疾病机制。我们检查了主要组织相容性复合体（MHC）mRNA在TGF-β1无效小鼠组织中的表达，发现与正常或TGF-β1杂合子同窝相比，I类和II类MHC mRNA的水平均升高。在炎症浸润的任何证据之前就已经观察到这种升高的表达，表明增加的MHC表达与免疫细胞群的活化之间存在因果关系。通过免疫组织化学检测MHC分子的细胞表面表达，并与mRNA水平很好地相关。当MHC表达增加变得明显的年龄，干扰素γ及其受体的mRNA表达没有变化。在从TGF-β1无效小鼠中分离的成纤维细胞中，还证实了TGF-β1对I类MHC表达的下调。这些发现表明，TGF-beta 1的一项自然功能是控制两种MHC类型的表达。 MHC表达的调节改变可能是导致多灶性炎症和TGF-beta 1 null小鼠中所见的虚弱综合征的关键步骤。这些结果表明，TGF-β在自身免疫性疾病，同种异体移植排斥反应以及与MHC表达改变有关的其他问题中的潜在应用。

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期刊名称 Proceedings of the National Academy of Sciences of the United States of America
作者
A G Geiser; J J Letterio; A B Kulkarni; S Karlsson; A B Roberts; M B Sporn;
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年(卷),期 1993(90),21
年度 1993
页码 9944–9948
总页数 5
原文格式 PDF
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6. Transforming growth factor-beta down-regulates major histocompatibility complex class I antigen expression and increases the susceptibility of uveal melanoma cells to natural killer cell-mediated cytolysis. [O] . D Ma, J Y Niederkorn 1995

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7. Transforming growth factor beta 1 (TGF-beta 1) controls expression of major histocompatibility genes in the postnatal mouse: aberrant histocompatibility antigen expression in the pathogenesis of the TGF-beta 1 null mouse phenotype. [O] . Geiser, A G, Letterio, J J, Kulkarni, A B, 1993

机译：转化生长因子beta 1（TGF-beta 1）控制出生后小鼠中主要组织相容性基因的表达：在TGF-beta 1空小鼠表型的发病机理中异常的组织相容性抗原表达。
8. Expression of Transforming Growth Factor-Beta (TGF-Beta) in Prostate Cancer Progression [R] . Lee, C. 2003

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Transforming growth factor beta 1 (TGF-beta 1) controls expression of major histocompatibility genes in the postnatal mouse: aberrant histocompatibility antigen expression in the pathogenesis of the TGF-beta 1 null mouse phenotype.

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