Department of Molecular Medicine and Surgery, Karolinska Institutet and University Hospital, Stockholm, Sweden.
Blood. 2012 Nov 22;120(22):4296-303. doi: 10.1182/blood-2012-07-292094. Epub 2012 Sep 19.
Coagulation factor XII (FXII, Hageman factor, EC = 3.4.21.38) is the zymogen of the serine protease, factor XIIa (FXIIa). FXII is converted to FXIIa through autoactivation induced by "contact" to charged surfaces. FXIIa is of crucial importance for fibrin formation in vitro, but deficiency in the protease is not associated with excessive bleeding. For decades, FXII was considered to have no function for coagulation in vivo. Our laboratory developed the first murine knockout model of FXII. Consistent with their human counterparts, FXII(-/-) mice have a normal hemostatic capacity. However, thrombus formation in FXII(-/-) mice is largely defective, and the animals are protected from experimental cerebral ischemia and pulmonary embolism. This murine model has created new interest in FXII because it raises the possibility for safe anticoagulation, which targets thrombosis without influence on hemostasis. We recently have identified platelet polyphosphate (an inorganic polymer) and mast cell heparin as in vivo FXII activators with implications on the initiation of thrombosis and edema during hypersensitivity reactions. Independent of its protease activity, FXII exerts mitogenic activity with implications for angiogenesis. The goal of this review is to summarize the in vivo functions of FXII, with special focus to its functions in thrombosis and vascular biology.
凝血因子 XII(FXII, Hageman 因子,EC = 3.4.21.38)是丝氨酸蛋白酶因子 XIIa(FXIIa)的酶原。FXII 通过与带电表面的“接触”诱导自动激活转化为 FXIIa。FXIIa 对于体外纤维蛋白形成至关重要,但蛋白酶缺乏与过度出血无关。数十年来,FXII 被认为在体内凝血中没有功能。我们的实验室开发了第一个 FXII 基因敲除的小鼠模型。与人类 FXII 相似,FXII(-/-) 小鼠具有正常的止血能力。然而,FXII(-/-) 小鼠的血栓形成缺陷很大,动物免受实验性脑缺血和肺栓塞的影响。这种小鼠模型引起了对 FXII 的新兴趣,因为它有可能进行安全的抗凝治疗,针对血栓形成而不影响止血。我们最近发现血小板多聚磷酸盐(一种无机聚合物)和肥大细胞肝素是体内 FXII 的激活剂,对过敏反应期间的血栓形成和水肿的发生有影响。FXII 发挥有丝分裂活性,具有血管生成的意义,而不依赖其蛋白酶活性。本综述的目的是总结 FXII 的体内功能,特别关注其在血栓形成和血管生物学中的功能。
