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血红素衍生的抗凝剂。体内外生成。

Hematin-derived anticoagulant. Generation in vitro and in vivo.

作者信息

Jones R L

出版信息

J Exp Med. 1986 Mar 1;163(3):724-39. doi: 10.1084/jem.163.3.724.

DOI:10.1084/jem.163.3.724
PMID:3950544
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2188044/
Abstract

Prolongation of clotting times produced by hematin was investigated both in vitro and in vivo. Hematin-derived anticoagulant (HDA) was found to be due to a degradative product or derivative of hematin, and was generated in vitro in standing (aging) aqueous solutions of the parent compound. Generation of HDA in vitro was inhibited by antioxidants. The anticoagulant effect of HDA was inhibited by freshly prepared hematin, fresh Sn-protoporphyrin, imidazole, or the iron chelator desferrioxamine. Ferrioxamine did not inhibit HDA, and inhibition by imidazole was reversed with ferric citrate, suggesting a role for iron in the mechanism of HDA activity. HDA activity was dissociated from hematin in plasma by clotting with thrombin. HDA segregated into the clot fraction, whereas hematin remained largely in the serum fraction, suggesting that HDA may preferentially bind to fibrinogen. TLC and HPLC showed a single peak of HDA activity that was not associated with the parent compound. Evidence for HDA generation in vivo was found when rats were injected with fresh (no HDA) hematin. Prolongation of clotting times appeared after hematin appeared in the plasma, and anticoagulant activity persisted after a fall in plasma hematin concentration. Thus, there was a temporal dissociation between hematin and HDA, suggesting that a modification of hematin must occur in vivo before an anticoagulant effect is produced. Generation of HDA in vitro has implications for hematin preparation and administration. Generation of HDA in vivo suggests that similar modifications of endogenous heme or other porphyrins may occur to produce HDA under physiologic or pathophysiologic conditions.

摘要

研究了血晶素在体外和体内对凝血时间的延长作用。发现血晶素衍生的抗凝剂(HDA)是血晶素的一种降解产物或衍生物,在母体化合物的静置(老化)水溶液中可在体外产生。抗氧化剂可抑制体外HDA的生成。新鲜制备的血晶素、新鲜的锡原卟啉、咪唑或铁螯合剂去铁胺可抑制HDA的抗凝作用。铁胺不抑制HDA,咪唑的抑制作用可被柠檬酸铁逆转,提示铁在HDA活性机制中起作用。通过凝血酶凝血可使血浆中的HDA活性与血晶素分离。HDA分离到凝块部分,而血晶素大部分保留在血清部分,提示HDA可能优先与纤维蛋白原结合。薄层层析(TLC)和高效液相色谱(HPLC)显示HDA活性为单一峰,与母体化合物无关。给大鼠注射新鲜(无HDA)血晶素时,发现体内有HDA生成的证据。血浆中出现血晶素后凝血时间延长,血浆血晶素浓度下降后抗凝活性仍持续存在。因此,血晶素与HDA之间存在时间上的分离,提示在产生抗凝作用之前,血晶素必须在体内发生修饰。体外HDA的生成对血晶素的制备和给药有影响。体内HDA的生成提示,在生理或病理生理条件下,内源性血红素或其他卟啉可能发生类似修饰以产生HDA。

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本文引用的文献

1
A comparison of the binding of imidazole to valence hybrid and methemoglobin: an assignment of individual heme reactivity.咪唑与价态杂化血红蛋白和高铁血红蛋白结合的比较:单个血红素反应性的归属
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Proc Natl Acad Sci U S A. 1981 Oct;78(10):6466-70. doi: 10.1073/pnas.78.10.6466.
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