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Heme oxygenase-1 system in organ transplantation.

机译:血红素加氧酶-1系统在器官移植中。

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摘要

The heme oxygenase-1 (HO-1) system, the rate-limiting step in the conversion of heme, is among the most critical of cytoprotective mechanisms activated during cellular stress. The cytoprotection may result from the elimination of heme and the function of HO-1 downstream mediators, that is, biliverdin, carbon monoxide, and free iron. HO-1 overexpression exerts beneficial effects in a number of transplantation models, including antigen-independent ischemia/reperfusion injury, acute and chronic allograft rejection, and xenotransplantation. The HO-1 system is thought to exert four major functions: (1) antioxidant function; (2) maintenance of microcirculation; (3) modulatory function upon the cell cycle; and (4) anti-inflammatory function. The antioxidant function depends on heme degradation, oxygen consumption, biliverdin, and production of ferritin via iron accumulation. The production of carbon monoxide, which has vasodilation and antiplatelet aggregation properties, maintains tissue microcirculation and may be instrumental in antiapoptotic and cell arrest mechanisms. Heme catabolism and HO-1 overexpression exert profound direct and indirect inhibitory effects on the cascade of host inflammatory responses mediated by neutrophils, macrophages, and lymphocytes. These anti-inflammatory properties result in cytoprotection in a broad spectrum of graft injury experimental models, including ischemia/reperfusion, acute and chronic allograft, and xenotransplant rejection. Further, the multifaceted targets of HO-1-mediated cytoprotection may simultaneously benefit both local graft function and host systemic immune responses. Thus, the HO-1 system serves as a novel therapeutic concept in organ transplantation.
机译:血红素加氧酶-1(HO-1)系统是血红素转化过程中的限速步骤,是细胞应激期间激活的最重要的细胞保护机制之一。细胞保护作用可能归因于血红素的消除和HO-1下游介体(即胆绿素,一氧化碳和游离铁)的功能。 HO-1的过表达在许多移植模型中发挥有益作用,包括不依赖抗原的局部缺血/再灌注损伤,急性和慢性同种异体移植排斥以及异种移植。 HO-1系统被认为具有四个主要功能:(1)抗氧化功能; (2)维持微循环; (3)对细胞周期的调节功能; (4)抗炎功能。抗氧化剂的功能取决于血红素的降解,耗氧量,胆绿素和通过铁积累产生的铁蛋白。一氧化碳的产生具有血管舒张和抗血小板凝集特性,可以维持组织的微循环,并可能在抗凋亡和细胞停滞机制中发挥作用。血红素分解代谢和HO-1过表达对嗜中性粒细胞,巨噬细胞和淋巴细胞介导的宿主炎症反应的级联产生深远的直接和间接抑制作用。这些抗炎特性在广泛的移植物损伤实验模型中导致细胞保护,包括缺血/再灌注,急性和慢性同种异体移植以及异种移植排斥。此外,HO-1介导的细胞保护的多方面靶标可同时有益于局部移植物功能和宿主全身免疫应答。因此,HO-1系统在器官移植中作为一种新颖的治疗概念。

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