Ferluga Janez, Kouser Lubna, Murugaiah Valarmathy, Sim Robert B, Kishore Uday
Biosciences, College of Health and Life Sciences, Brunel University London, Uxbridge, UB8 3PH, United Kingdom.
Department of Pharmacology, University of Oxford, Mansfield Road, Oxford OX1 3QT, United Kingdom.
Mol Immunol. 2017 Apr;84:84-106. doi: 10.1016/j.molimm.2017.01.015. Epub 2017 Feb 16.
Complement system homeostasis is important for host self-protection and anti-microbial immune surveillance, and recent research indicates roles in tissue development and remodelling. Complement also appears to have several points of interaction with the blood coagulation system. Deficiency and altered function due to gene mutations and polymorphisms in complement effectors and regulators, including Factor H, have been associated with familial and sporadic autoimmune inflammatory - thrombotic disorders, in which autoantibodies play a part. These include systemic lupus erythematosus, rheumatoid arthritis, atypical haemolytic uremic syndrome, anti-phospholipid syndrome and age-related macular degeneration. Such diseases are generally complex - multigenic and heterogeneous in their symptoms and predisposition/susceptibility. They usually need to be triggered by vascular trauma, drugs or infection and non-complement genetic factors also play a part. Underlying events seem to include decline in peripheral regulatory T cells, dendritic cell, and B cell tolerance, associated with alterations in lymphoid organ microenvironment. Factor H is an abundant protein, synthesised in many cell types, and its reported binding to many different ligands, even if not of high affinity, may influence a large number of molecular interactions, together with the accepted role of Factor H within the complement system. Factor H is involved in mesenchymal stem cell mediated tolerance and also contributes to self-tolerance by augmenting iC3b production and opsonisation of apoptotic cells for their silent dendritic cell engulfment via complement receptor CR3, which mediates anti-inflammatory-tolerogenic effects in the apoptotic cell context. There may be co-operation with other phagocytic receptors, such as complement C1q receptors, and the Tim glycoprotein family, which specifically bind phosphatidylserine expressed on the apoptotic cell surface. Factor H is able to discriminate between self and nonself surfaces for self-protection and anti-microbe defence. Factor H, particularly as an abundant platelet protein, may also modulate blood coagulation, having an anti-thrombotic role. Here, we review a number of interaction pathways in coagulation and in immunity, together with associated diseases, and indicate where Factor H may be expected to exert an influence, based on reports of the diversity of ligands for Factor H.
补体系统的稳态对于宿主自身保护和抗微生物免疫监视很重要,最近的研究表明其在组织发育和重塑中也发挥作用。补体似乎还与凝血系统有多个相互作用点。由于补体效应器和调节因子(包括H因子)的基因突变和多态性导致的功能缺陷和改变,与家族性和散发性自身免疫性炎症 - 血栓形成疾病有关,其中自身抗体也起一定作用。这些疾病包括系统性红斑狼疮、类风湿性关节炎、非典型溶血尿毒综合征、抗磷脂综合征和年龄相关性黄斑变性。此类疾病通常很复杂——症状和易感性/易患性具有多基因和异质性。它们通常需要由血管创伤、药物或感染引发,非补体遗传因素也起作用。潜在事件似乎包括外周调节性T细胞、树突状细胞和B细胞耐受性下降,这与淋巴器官微环境的改变有关。H因子是一种在多种细胞类型中合成的丰富蛋白质,其与许多不同配体的结合(即使亲和力不高)可能会影响大量分子相互作用,同时H因子在补体系统中也有公认的作用。H因子参与间充质干细胞介导的耐受性,还通过增强iC3b的产生以及凋亡细胞通过补体受体CR3被沉默树突状细胞吞噬的调理作用来促进自身耐受性,这在凋亡细胞环境中介导抗炎耐受性效应。可能与其他吞噬受体(如补体C1q受体)以及Tim糖蛋白家族存在协同作用,Tim糖蛋白家族特异性结合凋亡细胞表面表达的磷脂酰丝氨酸。H因子能够区分自身和非自身表面以实现自我保护和抗微生物防御。H因子,特别是作为一种丰富的血小板蛋白,也可能调节凝血,具有抗血栓形成作用。在此,我们综述了凝血和免疫中的一些相互作用途径以及相关疾病,并根据H因子配体多样性的报道指出H因子可能发挥影响的地方。
