Cdc42/Par6/aPKC 极性复合物调节上皮细胞凋亡诱导的代偿性增殖。

The Cdc42/Par6/aPKC polarity complex regulates apoptosis-induced compensatory proliferation in epithelia.

机构信息

Department of Medicine, BRIGHT Institute, Washington University School of Medicine, St. Louis, MO 63110, USA.

出版信息

Curr Biol. 2010 Apr 27;20(8):677-86. doi: 10.1016/j.cub.2010.03.025. Epub 2010 Apr 8.

DOI:10.1016/j.cub.2010.03.025

PMID:20381350

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2910247/

Abstract

BACKGROUND

In response to stress- or tissue-damage-induced apoptosis, unaffected epithelial cells undergo compensatory proliferation to maintain the integrity of the epithelium. Proximal signals regulating this response are not fully understood, but c-Jun N-terminal kinase (JNK) activity appears to be critical for both apoptosis and compensatory proliferation. Disruption of epithelial cell apical-basal polarity occurs in early cancer development and is often correlated with increased proliferation by means not fully characterized. We considered whether disruption of the various polarity complexes could provide signals identifying damaged epithelial cells and thus lead to apoptosis-induced compensatory proliferation.

RESULTS

We identify the Cdc42/Par6/atypical protein kinase C (aPKC) Par polarity complex as uniquely and specifically regulating apoptosis-induced compensatory proliferation in Drosophila epithelia. Genetic depletion of individual components or disruption of formation and localization of this complex, but not other polarity complexes, induces JNK-dependent apoptosis and JNK-dependent compensatory proliferation following radiation injury. When apoptosis execution is blocked, by p35 expression, Cdc42/Par6/aPKC-depleted tissues uniquely hyperproliferate, leading to tissue and organ overgrowth. Disruption of Cdc42/Par6/aPKC leads to activation of JNK through increased Rho1 and Rok activity and Rok's capacity to activate myosin but not F-actin.

CONCLUSIONS

We show that the Cdc42/Par6/aPKC polarity complex influences both a physiologic compensatory proliferation response after irradiation injury and a contrived compensatory non-cell-autonomous hyperproliferation response when cell-autonomous apoptosis, resulting from Cdc42/Par6/aPKC disruption, is inhibited. These results suggest the possibility that in cancer where apoptotic regulation is disrupted, loss of Cdc42/Par6/aPKC polarity complex organization or localization could contribute to tumor hyperproliferation and explain how polarity disruption contributes to tumor development.

摘要

背景

在应对应激或组织损伤诱导的细胞凋亡时，未受影响的上皮细胞会进行代偿性增殖，以维持上皮组织的完整性。目前尚不完全清楚调节这种反应的近端信号，但 c-Jun N 端激酶（JNK）的活性似乎对细胞凋亡和代偿性增殖都至关重要。上皮细胞顶端-基底极性的破坏发生在癌症早期发展过程中，并且常常与增殖增加有关，但具体机制尚未完全阐明。我们考虑是否破坏各种极性复合物可以提供识别受损上皮细胞的信号，从而导致凋亡诱导的代偿性增殖。

结果

我们发现 Cdc42/Par6/非典型蛋白激酶 C（aPKC）Par 极性复合物可特异性调节果蝇上皮细胞中的凋亡诱导性代偿性增殖。单独耗尽单个成分或破坏该复合物的形成和定位，但不破坏其他极性复合物，会导致辐射损伤后 JNK 依赖性细胞凋亡和 JNK 依赖性代偿性增殖。当通过表达 p35 阻止细胞凋亡执行时，Cdc42/Par6/aPKC 耗尽的组织会独特地过度增殖，导致组织和器官过度生长。Cdc42/Par6/aPKC 的破坏会通过增加 Rho1 和 Rok 的活性以及 Rok 激活肌球蛋白但不激活 F- 肌动蛋白来激活 JNK。

结论

我们表明，Cdc42/Par6/aPKC 极性复合物既影响辐射损伤后生理性代偿性增殖反应，又影响因 Cdc42/Par6/aPKC 破坏导致的细胞自主凋亡被抑制时的非细胞自主代偿性过度增殖反应。这些结果表明，在凋亡调节失调的癌症中，Cdc42/Par6/aPKC 极性复合物组织或定位的丧失可能导致肿瘤过度增殖，并解释了极性破坏如何促进肿瘤的发展。

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Cdc42/Par6/aPKC 极性复合物调节上皮细胞凋亡诱导的代偿性增殖。

The Cdc42/Par6/aPKC polarity complex regulates apoptosis-induced compensatory proliferation in epithelia.

机构信息

Department of Medicine, BRIGHT Institute, Washington University School of Medicine, St. Louis, MO 63110, USA.

出版信息

Curr Biol. 2010 Apr 27;20(8):677-86. doi: 10.1016/j.cub.2010.03.025. Epub 2010 Apr 8.

DOI:10.1016/j.cub.2010.03.025

PMID:20381350

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2910247/

Abstract

BACKGROUND

RESULTS

CONCLUSIONS

摘要

Cdc42/Par6/aPKC 极性复合物调节上皮细胞凋亡诱导的代偿性增殖。

The Cdc42/Par6/aPKC polarity complex regulates apoptosis-induced compensatory proliferation in epithelia.

机构信息

出版信息

BACKGROUND

RESULTS

CONCLUSIONS

背景

结果

结论

相似文献

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Cdc42/Par6/aPKC 极性复合物调节上皮细胞凋亡诱导的代偿性增殖。

The Cdc42/Par6/aPKC polarity complex regulates apoptosis-induced compensatory proliferation in epithelia.

机构信息

出版信息

BACKGROUND

RESULTS

CONCLUSIONS

背景

结果

结论