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Functional Immune Anatomy of the Liver-As an Allograft

机译:作为同种异体移植肝的功能性免疫解剖

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摘要

The liver is an immunoregulatory organ in which a tolerogenic microenvironment mitigates the relative "strength" of local immune responses. Paradoxically, necro-inflammatory diseases create the need for most liver transplants. Treatment of hepatitis B virus, hepatitis C virus, and acute T cell-mediated rejection have redirected focus on long-term allograft structural integrity. Understanding of insults should enable decades of morbidity-free survival after liver replacement because of these tolerogenic properties. Studies of long-term survivors show low-grade chronic inflammatory, fibrotic, and microvascular lesions, likely related to some combination of environment insults (i.e. abnormal physiology), donor-specific antibodies, and T cell-mediated immunity. The resultant conundrum is familiar in transplantation: adequate immunosuppression produces chronic toxicities, while lightened immunosuppression leads to sensitization, immunological injury, and structural deterioration. The "balance" is more favorable for liver than other solid organ allografts. This occurs because of unique hepatic immune physiology and provides unintended benefits for allografts by modulating various afferent and efferent limbs of allogenic immune responses. This review is intended to provide a better understanding of liver immune microanatomy and physiology and thereby (a) the potential structural consequences of low-level, including allo-antibody-mediated injury; and (b) how liver allografts modulate immune reactions. Special attention is given to the microvasculature and hepatic mononuclear phagocytic system.
机译:肝脏是一种免疫调节器官,其中耐受性微环境减轻了局部免疫反应的相对“强度”。矛盾的是,坏死性炎症疾病导致大多数肝移植的需求。乙型肝炎病毒,丙型肝炎病毒和急性T细胞介导的排斥反应的治疗已将重点转向长期同种异体移植物结构完整性。由于这些致耐受性的特性,对侮辱的理解应使肝脏置换后数十年无病生存。长期幸存者的研究表明,低度慢性炎症,纤维化和微血管病变可能与环境侵害(即生理异常),供体特异性抗体和T细胞介导的免疫力的某些组合有关。由此产生的难题在移植中是很熟悉的:充分的免疫抑制会产生慢性毒性,而轻度的免疫抑制则会导致过敏,免疫损伤和结构恶化。与其他实体器官同种异体移植相比,“平衡”对肝脏更有利。发生这种情况是由于独特的肝脏免疫生理学,并且通过调节同种异体免疫反应的各种传入和传出肢体,为同种异体移植提供了意想不到的好处。这篇综述旨在更好地了解肝脏免疫显微解剖学和生理学,从而(a)低水平的潜在结构后果,包括同种抗体介导的损伤; (b)肝脏同种异体移植物如何调节免疫反应。特别注意微脉管系统和肝单核吞噬系统。

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