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本文引用的文献

1
Liver regeneration after partial hepatectomy: critical analysis of mechanistic dilemmas.部分肝切除术后的肝脏再生:对机制难题的批判性分析。
Am J Pathol. 2010 Jan;176(1):2-13. doi: 10.2353/ajpath.2010.090675. Epub 2009 Dec 17.
2
Liver-specific ablation of integrin-linked kinase in mice results in enhanced and prolonged cell proliferation and hepatomegaly after phenobarbital administration.在小鼠中特异性敲除整合素连接激酶可导致苯巴比妥给药后细胞增殖增强和持续时间延长,并导致肝肿大。
Toxicol Sci. 2010 Feb;113(2):358-66. doi: 10.1093/toxsci/kfp281. Epub 2009 Nov 17.
3
Migfilin interacts with Src and contributes to cell-matrix adhesion-mediated survival signaling.Migfilin与Src相互作用,并参与细胞-基质黏附介导的生存信号传导。
J Biol Chem. 2009 Dec 4;284(49):34308-20. doi: 10.1074/jbc.M109.045021. Epub 2009 Oct 15.
4
Enhanced liver regeneration following changes induced by hepatocyte-specific genetic ablation of integrin-linked kinase.整合素连接激酶肝细胞特异性基因敲除诱导的变化后肝脏再生增强。
Hepatology. 2009 Sep;50(3):844-51. doi: 10.1002/hep.23059.
5
Investigation of the role of glypican 3 in liver regeneration and hepatocyte proliferation.磷脂酰肌醇蛋白聚糖3在肝脏再生和肝细胞增殖中的作用研究。
Am J Pathol. 2009 Aug;175(2):717-24. doi: 10.2353/ajpath.2009.081129. Epub 2009 Jul 2.
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Focal adhesion kinase and cancer.粘着斑激酶与癌症
Histol Histopathol. 2009 Apr;24(4):503-10. doi: 10.14670/HH-24.503.
7
FAK expression regulation and therapeutic potential.粘着斑激酶(FAK)的表达调控及治疗潜力
Adv Cancer Res. 2008;101:45-61. doi: 10.1016/S0065-230X(08)00403-X.
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The Hippo-YAP pathway: new connections between regulation of organ size and cancer.河马 - YAP信号通路:器官大小调控与癌症之间的新联系
Curr Opin Cell Biol. 2008 Dec;20(6):638-46. doi: 10.1016/j.ceb.2008.10.001. Epub 2008 Nov 18.
9
Liver-specific ablation of integrin-linked kinase in mice results in abnormal histology, enhanced cell proliferation, and hepatomegaly.小鼠中整合素连接激酶的肝脏特异性消融导致组织学异常、细胞增殖增强和肝肿大。
Hepatology. 2008 Dec;48(6):1932-41. doi: 10.1002/hep.22537.
10
Integrin-linked kinase--essential roles in physiology and cancer biology.整合素连接激酶——在生理学和癌症生物学中的重要作用。
J Cell Sci. 2008 Oct 1;121(Pt 19):3121-32. doi: 10.1242/jcs.017996.

1,4-双[2-(3,5-二氯吡啶氧基)]苯处理后,整合素连接激酶在肝细胞中靶向消除导致小鼠肝肿大过度。

Excessive hepatomegaly of mice with hepatocyte-targeted elimination of integrin linked kinase following treatment with 1,4-bis [2-(3,5-dichaloropyridyloxy)] benzene.

机构信息

Department of Pathology, University of Pittsburgh School of Medicine, Pittsburgh, PA 15261, USA.

出版信息

Hepatology. 2011 Feb;53(2):587-95. doi: 10.1002/hep.24040. Epub 2011 Jan 6.

DOI:10.1002/hep.24040
PMID:21274879
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3062106/
Abstract

UNLABELLED

TCBOPOP (1,4-bis [2-(3,5-dichaloropyridyloxy)] benzene) an agonist of the constitutive androstane receptor (CAR), produces rapid hepatocyte hyperplasia and hepatomegaly in the absence of hepatic injury. In this study we demonstrate that integrin-linked kinase (ILK), which is involved in transmission of the extracellular matrix (ECM) signaling by way of integrin receptors, plays an important role in regulating TCPOBOP-induced proliferation of hepatocytes and hepatomegaly. Hepatocyte-specific ILK knockout mice (ILK/liver-/- mice) and wildtype mice (WT) were given a single dose of TCPOBOP (3 mg/kg) by oral gavage. Mice were sacrificed at days 1, 2, 5, and 7 after TCPOBOP administration. WT mice showed maximum proliferation on days 1 and 2, which came back to baseline levels by days 5 and 7 after TCPOBOP administration. The ILK/liver-/- mice, on the other hand, showed a prolonged and a sustained proliferative response as evident by an increased number of proliferative cell nuclear antigen assay (PCNA)-positive cells even at days 5 and 7 after TCPOBOP administration. At day 7 the WT mice showed close to a 2.5-fold increase in liver weight, whereas the ILK/liver-/- mice showed a 3.7-fold increase in liver weight. The prolonged proliferative response in the ILK/liver-/- mice seems to be due to sustained induction of CAR leading to sustained induction of c-Myc, which is known to be a key mediator of TCPOPOP-CAR induced direct liver hyperplasia.

CONCLUSION

The data indicate that ECM-mediated signaling by way of ILK is essential for adjustment of final liver size and proper termination of TCPOBOP-induced proliferation of hepatocytes.

摘要

未加标签

TCBOPOP(1,4-双[2-(3,5-二氯吡啶氧基)]苯)是一种组成型雄烷受体(CAR)激动剂,在没有肝损伤的情况下会导致肝细胞快速增生和肝肿大。在这项研究中,我们证明整合素连接激酶(ILK)在通过整合素受体传递细胞外基质(ECM)信号中发挥重要作用,调节 TCPOBOP 诱导的肝细胞增殖和肝肿大。肝细胞特异性 ILK 敲除小鼠(ILK/肝-/-小鼠)和野生型小鼠(WT)通过口服灌胃给予 TCPOBOP(3mg/kg)单次剂量。在 TCPOBOP 给药后第 1、2、5 和 7 天处死小鼠。WT 小鼠在第 1 和第 2 天显示出最大的增殖,在 TCPOBOP 给药后第 5 和第 7 天恢复到基线水平。另一方面,ILK/肝-/-小鼠表现出延长和持续的增殖反应,增殖细胞核抗原检测(PCNA)阳性细胞的数量增加,甚至在 TCPOBOP 给药后第 5 和第 7 天也是如此。在第 7 天,WT 小鼠的肝重增加了近 2.5 倍,而 ILK/肝-/-小鼠的肝重增加了 3.7 倍。ILK/肝-/-小鼠中延长的增殖反应似乎是由于 CAR 的持续诱导,导致 c-Myc 的持续诱导,c-Myc 是 TCPOPOP-CAR 诱导的直接肝增生的关键介质。

结论

数据表明,通过 ILK 的细胞外基质介导的信号对于调整最终肝大小和适当终止 TCPOBOP 诱导的肝细胞增殖是必不可少的。