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Old game, new players: Linking classical theories to new trends in transplant immunology

机译:老游戏,新玩家:将经典理论与移植免疫学的新趋势联系起来

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摘要

The evolutionary emergence of an efficient immune system has a fundamental role in our survival against pathogenic attacks. Nevertheless, this same protective mechanism may also establish a negative consequence in the setting of disorders such as autoimmunity and transplant rejection. In light of the latter, although research has long uncovered main concepts of allogeneic recognition, immune rejection is still the main obstacle to long-term graft survival. Therefore, in order to define effective therapies that prolong graft viability, it is essential that we understand the underlying mediators and mechanisms that participate in transplant rejection. This multifaceted process is characterized by diverse cellular and humoral participants with innate and adaptive functions that can determine the type of rejection or promote graft acceptance. Although a number of mediators of graft recognition have been described in traditional immunology, recent studies indicate that defining rigid roles for certain immune cells and factors may be more complicated than originally conceived. Current research has also targeted specific cells and drugs that regulate immune activation and induce tolerance. This review will give a broad view of the most recent understanding of the allogeneic inflammatory/tolerogenic response and current insights into cellular and drug therapies that modulate immune activation that may prove to be useful in the induction of tolerance in the clinical setting.
机译:有效免疫系统的进化出现在我们抵抗病原体侵袭的生存中具有根本作用。然而,这种相同的保护机制也可能在自身免疫和移植排斥等疾病的发生中产生负面影响。鉴于后者,尽管长期以来研究一直未发现同种异体识别的主要概念,但免疫排斥仍然是移植物长期存活的主要障碍。因此,为了定义延长移植物存活力的有效疗法,必须了解参与移植排斥的潜在介质和机制。这种多方面的过程的特点是具有固有和适应性功能的各种细胞和体液参与者可以确定排斥的类型或促进移植物的接受。尽管在传统的免疫学中已经描述了移植识别的许多介体,但是最近的研究表明,为某些免疫细胞和因子定义刚性作用可能比最初设想的要复杂。当前的研究还针对调节免疫激活并诱导耐受性的特定细胞和药物。这篇综述将广泛地了解同种异体炎症/耐受性应答的最新理解,以及对调节免疫激活的细胞和药物疗法的最新见解,这可能在临床环境中可诱导耐受性。

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