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1
Role of hemostatic factors in hepatic injury and disease: animal models de-liver.止血因子在肝损伤和疾病中的作用:动物模型研究。 (你提供的原文似乎不太完整或有拼写错误,推测可能是“Role of hemostatic factors in hepatic injury and disease: animal models deliver.”这样更通顺些,但我按照你给的原文进行了翻译)
J Thromb Haemost. 2016 Jul;14(7):1337-49. doi: 10.1111/jth.13327. Epub 2016 May 10.
2
Fibrin deposition following bile duct injury limits fibrosis through an αMβ2-dependent mechanism.胆管损伤后纤维蛋白沉积通过αMβ2依赖性机制限制纤维化。
Blood. 2016 Jun 2;127(22):2751-62. doi: 10.1182/blood-2015-09-670703. Epub 2016 Feb 26.
3
Platelets and fibrin in progression of liver disease: friends or foes?血小板和纤维蛋白在肝病进展中的作用:是友还是敌?
J Thromb Haemost. 2015 Jan;13(1):54-6. doi: 10.1111/jth.12783. Epub 2014 Dec 6.
4
Coagulation-driven platelet activation reduces cholestatic liver injury and fibrosis in mice.凝血驱动的血小板活化可减轻小鼠胆汁淤积性肝损伤和纤维化。
J Thromb Haemost. 2015 Jan;13(1):57-71. doi: 10.1111/jth.12770. Epub 2014 Dec 11.
5
Extrahepatic platelet-derived growth factor-β, delivered by platelets, promotes activation of hepatic stellate cells and biliary fibrosis in mice.血小板衍生的肝外血小板衍生生长因子-β通过血小板促进肝星状细胞激活和小鼠胆管纤维化。
Gastroenterology. 2014 Dec;147(6):1378-92. doi: 10.1053/j.gastro.2014.08.038. Epub 2014 Aug 28.
6
The antifibrinolytic drug tranexamic acid reduces liver injury and fibrosis in a mouse model of chronic bile duct injury.抗纤维蛋白溶解药物氨甲环酸可减少慢性胆管损伤小鼠模型的肝损伤和纤维化。
J Pharmacol Exp Ther. 2014 Jun;349(3):383-92. doi: 10.1124/jpet.113.210880. Epub 2014 Mar 14.
7
Platelet signaling.血小板信号传导
Handb Exp Pharmacol. 2012(210):59-85. doi: 10.1007/978-3-642-29423-5_3.
8
The coagulation system contributes to alphaVbeta6 integrin expression and liver fibrosis induced by cholestasis.凝血系统有助于胆汁淤积诱导的α Vβ 6 整合素表达和肝纤维化。
Am J Pathol. 2010 Dec;177(6):2837-49. doi: 10.2353/ajpath.2010.100425. Epub 2010 Oct 29.
9
Thrombocytopenia exacerbates cholestasis-induced liver fibrosis in mice.血小板减少症加剧了小鼠胆汁淤积性肝纤维化。
Gastroenterology. 2010 Jun;138(7):2487-98, 2498.e1-7. doi: 10.1053/j.gastro.2010.02.054. Epub 2010 Mar 2.
10
Protective and damaging effects of platelets in acute cholestatic liver injury revealed by depletion and inhibition strategies.通过耗竭和抑制策略揭示血小板在急性胆汁淤积性肝损伤中的保护和损伤作用。
Toxicol Sci. 2010 May;115(1):286-94. doi: 10.1093/toxsci/kfq042. Epub 2010 Feb 4.

抑制PAR-4和P2Y12受体介导的血小板活化在实验性外源化学物诱导的胆汁淤积性肝病中产生不同的肝脏病理变化。

Inhibition of PAR-4 and P2Y12 receptor-mediated platelet activation produces distinct hepatic pathologies in experimental xenobiotic-induced cholestatic liver disease.

作者信息

Joshi Nikita, Kopec Anna K, Ray Jessica L, Luyendyk James P

机构信息

Department of Pharmacology & Toxicology, Michigan State University, East Lansing, MI 48824, United States; Institute for Integrative Toxicology, Michigan State University, East Lansing, MI 48824, United States.

Department of Pathobiology & Diagnostic Investigation, Michigan State University, East Lansing, MI 48824, United States; Institute for Integrative Toxicology, Michigan State University, East Lansing, MI 48824, United States.

出版信息

Toxicology. 2016 Jul 15;365:9-16. doi: 10.1016/j.tox.2016.07.021. Epub 2016 Jul 27.

DOI:10.1016/j.tox.2016.07.021
PMID:27475285
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5091088/
Abstract

Emerging evidence supports a protective effect of platelets in experimental cholestatic liver injury and cholangiofibrosis. Coagulation-mediated platelet activation has been shown to inhibit experimental chronic cholestatic liver necrosis and biliary fibrosis. This occurs through thrombin-mediated activation of protease activated receptor-4 (PAR-4) in mice. However, it is not known whether other pathways of platelet activation, such as adenosine diphosphate (ADP)-mediated receptor P2Y12 activation is also protective. We tested the hypothesis that inhibition of P2Y12-mediated platelet activation exacerbates hepatic injury and cholangiofibrosis, and examined the impact of P2Y12 inhibition in both the presence and absence of PAR-4. Treatment of wild-type mice with the P2Y12 receptor antagonist clopidogrel increased biliary hyperplasia and cholangiofibrosis in wild-type mice exposed to the xenobiotic alpha-naphthylisothiocyanate (ANIT) for 4 weeks compared to vehicle-treated mice exposed to ANIT. Interestingly, this effect of clopidogrel occurred without a corresponding increase in hepatocellular necrosis. Whereas biliary hyperplasia and cholangiofibrosis were increased in PAR-4(-/-) mice, clopidogrel treatment failed to further increase these pathologies in PAR-4(-/-) mice. The results indicate that inhibition of receptor P2Y12-mediated platelet activation exacerbates bile duct fibrosis in ANIT-exposed mice, independent of hepatocellular necrosis. Moreover, the lack of an added effect of clopidogrel administration on the exaggerated pathology in ANIT-exposed PAR-4(-/-) mice reinforces the prevailing importance of coagulation-mediated platelet activation in limiting this unique liver pathology.

摘要

新出现的证据支持血小板在实验性胆汁淤积性肝损伤和胆管纤维化中具有保护作用。凝血介导的血小板活化已被证明可抑制实验性慢性胆汁淤积性肝坏死和胆管纤维化。这一过程通过凝血酶介导的小鼠蛋白酶激活受体-4(PAR-4)活化来实现。然而,尚不清楚血小板活化的其他途径,如二磷酸腺苷(ADP)介导的受体P2Y12活化是否也具有保护作用。我们检验了以下假设:抑制P2Y12介导的血小板活化会加剧肝损伤和胆管纤维化,并研究了在存在和不存在PAR-4的情况下抑制P2Y12的影响。与接受α-萘基异硫氰酸酯(ANIT)处理4周的野生型小鼠相比,用P2Y12受体拮抗剂氯吡格雷处理野生型小鼠,增加了胆管增生和胆管纤维化。有趣的是,氯吡格雷的这种作用并未伴随着肝细胞坏死的相应增加。虽然PAR-4基因敲除(-/-)小鼠的胆管增生和胆管纤维化增加,但氯吡格雷处理未能进一步加重PAR-4基因敲除(-/-)小鼠的这些病理变化。结果表明,抑制受体P2Y12介导的血小板活化会加剧ANIT暴露小鼠的胆管纤维化,且与肝细胞坏死无关。此外,氯吡格雷给药对ANIT暴露的PAR-4基因敲除(-/-)小鼠中过度病理变化缺乏额外影响,这进一步强调了凝血介导的血小板活化在限制这种独特肝脏病理变化中的重要性。