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来自启动子诱导型逆转录病毒的MHC II类基因的调控表达。

Regulated expression of an MHC class II gene from a promoter-inducible retrovirus.

作者信息

Sonntag K C, Haller G W, Giauffret D, Germana S, Reeves S A, Levy J, Sachs D H, LeGuern C

机构信息

Biology Research Center, Massachusetts General Hospital/Harvard Medical School, Boston, MA 02129, USA.

出版信息

Hum Gene Ther. 2000 Sep 20;11(14):1961-9. doi: 10.1089/10430340050143390.

Abstract

Specific immune tolerance to fully allogeneic kidney grafts can be achieved in a miniature swine transplantation model by retrovirus-mediated transfer of allogeneic MHC class II genes into bone marrow cells (BMCs) of recipient animals. Graft survival correlated with transient expression of the somatic transgene (Tg) in the induction phase of tolerance. With the aim of investigating the effects of timing and threshold levels of Tg expression on induction of hyporesponsiveness to the grafted tissues, two recombinant retrovirus constructs containing the tetracycline binary regulatory system were used to achieve conditional expression of either the green fluorescent protein (tetGFP) as a control, or the porcine MHC class II DRbeta chain (tetDRB). Effective downregulation of GFP gene transcription was demonstrated in transduced murine fibroblasts after doxycycline treatment, leading to a > 90% reduction of GFP fluorescence. Similar diminution of the DRB gene transcription was achieved in transduced pig endothelial cells (ECs). Drug-dependent downregulation of DRBc gene expression in SLAd pig ECs coincided with complete inhibition of allogeneic activation of anti-class IIc-primed SLAd T cells. These in vitro results suggest that the binary tetracycline retrovirus system may also be adequate to regulate MHC class II Tg expression in vivo.

摘要

在小型猪移植模型中,通过逆转录病毒介导将同种异体MHC II类基因转移至受体动物的骨髓细胞(BMC),可实现对完全同种异体肾移植的特异性免疫耐受。移植物存活与耐受诱导期体细胞转基因(Tg)的短暂表达相关。为了研究Tg表达的时间和阈值水平对诱导对移植组织低反应性的影响,使用了两种含有四环素二元调控系统的重组逆转录病毒构建体,以实现绿色荧光蛋白(tetGFP)作为对照或猪MHC II类DRβ链(tetDRB)的条件性表达。强力霉素处理后,在转导的小鼠成纤维细胞中证明了GFP基因转录的有效下调,导致GFP荧光减少>90%。在转导的猪内皮细胞(EC)中也实现了DRB基因转录的类似减少。SLAd猪EC中DRBc基因表达的药物依赖性下调与抗IIc致敏的SLAd T细胞的同种异体激活的完全抑制相吻合。这些体外结果表明,二元四环素逆转录病毒系统也可能足以在体内调节MHC II类Tg表达。

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