Repetitive deformation activates Src-independent FAK-dependent ERK motogenic signals in human Caco-2 intestinal epithelial cells

机译：重复变形激活人Caco-2肠上皮细胞中Src依赖性FAK依赖性ERK致病信号

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Repetitive deformation due to villous motility or peristalsis may support the intestinal mucosa, stimulating intestinal epithelial proliferation under normal circumstances and restitution in injured and inflamed mucosa rich in tissue fibronectin. Cyclic strain enhances Caco-2 and IEC-6 intestinal epithelial cell migration across fibronectin via ERK. However, the upstream mediators of ERK activation are unknown. We investigated whether Src and FAK mediate strain-induced ERK phosphorylation and migration in human Caco-2 intestinal epithelial cells on fibronectin. Monolayers on tissue fibronectin-precoated membranes were subjected to an average 10% repetitive deformation at 10 cycles/min. Phosphorylation of Src-Tyr⁴¹⁸, FAK-Tyr³⁹⁷-Tyr⁵⁷⁶-Tyr⁹²⁵, and ERK were significantly increased by deformation. The stimulation of wound closure by strain was prevented by Src blockade with PP2 (10 (µmol/l) or specific short interfering (si)RNA. Src inhibition also prevented strain-induced FAK phosphorylation at Tyr³⁹⁷ and Tyr⁵⁷⁶ but not FAK-Tyr⁹²⁵ or ERK phosphorylation. Reducing FAK by siRNA inhibited strain-induced ERK phosphorylation. Transfection of NH2-terminal tyrosine phosphorylation-deficient FAK mutants Y397F, Y576F–Y577F, and Y397F–Y576F–Y577F did not prevent the activation of ERK2 by cyclic strain, but a FAK mutant at the COOH terminal (Y925F) prevented the strain-induced activation of ERK2. Although the Y397F–Y576F–Y577F FAK construct exhibited less basal FAK-Tyr⁹²⁵ phosphorylation under static conditions, it nevertheless exhibited increased FAK-Tyr⁹²⁵ phosphorylation in response to strain. These results suggest that repetitive deformation stimulates intestinal epithelial motility across fibronectin in a manner that requires both Src activation and a novel Src-independent FAK-Tyr⁹²⁵-dependent pathway that activates ERK. This pathway may be an important target for interventions to promote mucosal healing in settings of intestinal ileus or fasting.

机译：绒毛运动或蠕动引起的反复变形可支持肠粘膜，在正常情况下可刺激肠上皮增殖，并在富含组织纤连蛋白的受伤和发炎的粘膜中恢复原状。循环应变通过ERK增强了Caco-2和IEC-6肠上皮细胞跨纤连蛋白的迁移。但是，ERK激活的上游介质是未知的。我们调查了Src和FAK是否在纤连蛋白上的人Caco-2肠上皮细胞中介导了菌株诱导的ERK磷酸化和迁移。组织纤连蛋白包被的膜上的单层膜以10个循环/分钟的速度平均发生10％的重复变形。 Src-Tyr ^{418 ，FAK-Tyr ^{397 -Tyr ^{576 -Tyr ^{925 和ERK的磷酸化显着因变形而增加。通过PP2（10（μmol/ l）或特定的短干扰（si）RNA阻断Src，防止了菌株刺激伤口闭合，抑制Src也阻止了菌株诱导的Tyr ^{397 和FAK磷酸化。 Tyr ^{576 ，而不是FAK-Tyr ^{925 或ERK磷酸化；通过siRNA还原FAK可抑制菌株诱导的ERK磷酸化；转染NH2-末端酪氨酸磷酸化缺陷的FAK突变体Y397F， Y576F–Y577F和Y397F–Y576F–Y577F不能阻止环状菌株激活ERK2，但是COOH末端的FAK突变体（Y925F）可以阻止菌株诱导的ERK2激活。尽管Y397F–Y576F–Y577F FAK构建体在静态条件下显示出较少的基础FAK-Tyr ^{925 磷酸化，但响应于应变显示出增加的FAK-Tyr ^{925 磷酸化，这些结果表明重复变形刺激了肠上皮运动需要bot的方式跨纤连蛋白h Src激活和一种新的非Src依赖性FAK-Tyr ^{925 依赖性途径激活ERK。该途径可能是在肠肠梗阻或禁食时促进粘膜愈合的干预措施的重要目标。}}}}}}}}}}

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期刊名称 American Journal of Physiology - Cell Physiology
作者
Lakshmi S. Chaturvedi; Christopher P. Gayer; Harold M. Marsh; Marc D. Basson;
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作者单位

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年(卷),期 -1(294),6
年度 -1
页码 C1350–C1361
总页数 27
原文格式 PDF
正文语种
中图分类细胞生物学;人体生理学;
关键词
migration cyclic strain intestine mechanotransduction signaling;

机译：迁移;循环应变;肠;机械转导;信号;
入库时间 2022-08-21 10:50:26

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专利

1. Repetitive deformation activates Src-independent FAK-dependent ERK motogenic signals in human Caco-2 intestinal epithelial cells [J] . Lakshmi S. Chaturvedi, Christopher P. Gayer, Harold M. Marsh, American Journal of Physiology . 2008,第6aPta1期

机译：重复变形在人Caco-2肠上皮细胞中激活SRC无关的FAK依赖性ERK春季血糖信号
2. Repetitive deformation activates Src-independent FAK-dependent ERK motogenic signals in human Caco-2 intestinal epithelial cells [J] . Lakshmi S. Chaturvedi, Christopher P. Gayer, Harold M. Marsh, American Journal of Physiology . 2008,第6aPta1期

机译：重复变形激活人Caco-2肠上皮细胞中Src依赖性FAK依赖性ERK致病信号
3. Role of RhoA and its effectors ROCK and mDia1 in the modulation of deformation-induced FAK, ERK, p38, and MLC motogenic signals in human Caco-2 intestinal epithelial cells. [J] . Chaturvedi LS, Marsh HM, Basson MD American Journal of Physiology . 2011,第5Parta1期

机译：rhOA及其作用岩体的作用和MDIA1在人Caco-2肠上皮细胞中变形诱导的FAK，ERK，P38和MLC春季春季血泡信号调节中的作用。
4. Regulation of interleukin-8 secretion in human intestinal epithelial Caco-2 cells by alpha-humulene [C] . Hideo Satsu, Tomoko Matsuda, Takayuki Toshimitsu, International Conference on Food Factors . 2004

机译：α-humulene的人肠上皮Caco-2细胞中白细胞介素-8分泌的调节
5. Tuning of interleukin-13 signaling in intestinal epithelial cells via IL-13Ralpha2-induced MAP kinase activation and induction of reactive oxygen species. [D] . Mandal, Debasmita. 2010

机译：通过IL-13Ralpha2诱导的MAP激酶激活和活性氧的诱导，肠上皮细胞中白介素13信号的调节。
6. Cytoskeletal Signaling via α-Actinin-1 Mediates ERK1/2 Activation by Repetitive Deformation in Human Caco-2 Intestinal Epithelial Cells [O] . David H. Craig, Jianhu Zhang, Marc D. Basson -1

机译：通过α-肌动蛋白-1的细胞骨架信号通过人类Caco-2肠上皮细胞的重复变形介导ERK1 / 2激活。
7. Cytoskeletal signaling by way of α-actinin-1 mediates ERK1/2 activation by repetitive deformation in human Caco2 intestinal epithelial cells [O] . David H. Craig, Jianhu Zhang, Marc D. Basson 2007

机译：通过α-Actinin-1的细胞骨架信号传导通过人CaCO 2肠上皮细胞中的重复变形介导ERK1 / 2活化

Repetitive deformation activates Src-independent FAK-dependent ERK motogenic signals in human Caco-2 intestinal epithelial cells

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