Embryonic lethality in mice lacking Trim59 due to impaired gastrulation development

Xiaomin Su; Chenglei Wu; Xiaoying Ye; Ming Zeng; Zhujun Zhang; Yongzhe Che; Yuan Zhang; Lin Liu; Yushuang Lin; Rongcun Yang

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Embryonic lethality in mice lacking Trim59 due to impaired gastrulation development

机译：缺乏Trim59的小鼠的胚芽致死性，因为它们的胃排卵发育受到损害

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TRIM family members have been implicated in a variety of biological processes such as differentiation and development. We here found that Trim59 plays a critical role in early embryo development from blastocyst stage to gastrula. There existed delayed development and empty yolk sacs from embryonic day (E) 8.5 in Trim59?/? embryos. No viable Trim59?/? embryos were observed beyond E9.5. Trim59 deficiency affected primary germ layer formation at the beginning of gastrulation. At E6.5 and E7.5, the expression of primary germ layer formation-associated genes including Brachyury, lefty2, Cer1, Otx2, Wnt3, and BMP4 was reduced in Trim59?/? embryos. Homozygous mutant embryonic epiblasts were contracted and the mesoderm was absent. Trim59 could interact with actin- and myosin-associated proteins. Its deficiency disturbed F-actin polymerization during inner cell mass differentiation. Trim59-mediated polymerization of F-actin was via WASH K63-linked ubiquitination. Thus, Trim59 may be a critical regulator for early embryo development from blastocyst stage to gastrula through modulating F-actin assembly.

机译：TRIM家族成员已经牵涉到多种生物学过程，例如分化和发育。我们在这里发现，Trim59在从胚泡期到胃胚的早期胚胎发育中起着至关重要的作用。从Trim59？/？的胚胎天（E）8.5开始，卵子囊发育迟缓，卵黄囊变空。胚胎。没有可行的Trim59？/？观察到胚胎超过E9.5。 Trim59缺乏症影响了开始胃泌乳时初级细菌层的形成。在E6.5和E7.5，在Trim59α/β中初级胚层形成相关基因包括Brachyury，lefty2，Cer1，Otx2，Wnt3和BMP4的表达降低。胚胎。纯合突变体胚胎胚成骨细胞收缩，中胚层不存在。 Trim59可以与肌动蛋白和肌球蛋白相关蛋白相互作用。它的缺乏干扰了内细胞团分化过程中的F-肌动蛋白聚合。 Trim59介导的F-肌动蛋白的聚合反应是通过WASH K63连接的泛素化作用完成的。因此，Trim59可能是通过调节F-肌动蛋白装配从胚泡阶段到胃胚的早期胚胎发育的关键调控因子。

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《Cell death & disease.》 |2018年第3期|共页
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Xiaomin Su; Chenglei Wu; Xiaoying Ye; Ming Zeng; Zhujun Zhang; Yongzhe Che; Yuan Zhang; Lin Liu; Yushuang Lin; Rongcun Yang;
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1. Embryonic Lethality Caused by Apoptosis during Gastrulation in Mice Lacking the Gene of the ADP-Ribosylation Factor-Related Protein 1 [J] . A. G. Mueller, M. Moser, R. Kluge, Molecular and Cellular Biology . 2002,第5期

机译：缺少ADP核糖基化因子相关蛋白1基因的小鼠排卵过程中凋亡引起的胚胎致死率。
2. Embryonic Lethality Caused by Apoptosis during Gastrulation in Mice Lacking the Gene of the ADP-Ribosylation Factor-Related Protein 1 [J] . A. G. Mueller, M. Moser, R. Kluge, Molecular and Cellular Biology . 2002,第5期

机译：缺少ADP核糖基化因子相关蛋白1基因的小鼠排卵过程中凋亡引起的胚胎致死率。
3. Late embryonic lethality and impaired V(D)J recombination in mice lacking DNA ligase IV. [J] . FrankKM, SekiguchiJM, SeidlKJ, Nature . 1998,第6707期

机译：缺乏DNA连接酶IV的小鼠的晚期胚胎致死率和V（D）J重组受损。
4. Impaired Chronotropic Response to Exercisein Mice Lacking Catecholaminesin Adrenergic Cells [C] . Xuping Sao, Fujun Liu, Yusu Gu, International Symposium on Catecholamines and Other Neurotransmitters in Stress . 2008

机译：在缺乏儿茶酚胺和肾上腺素能细胞的小鼠中对锻炼的时程度反应受损
5. Mid- and late-gestation lethality in mice lacking the N terminus of TATA -binding protein [D] . Hobbs, Nicole Kay 2004

机译：缺乏TATA结合蛋白N末端的小鼠的妊娠中期和晚期致死率
6. Embryonic lethality in mice lacking Trim59 due to impaired gastrulation development [O] . Xiaomin Su, Chenglei Wu, Xiaoying Ye, 2018

机译：缺乏Trim59的小鼠的胚芽致死性因为它们的生殖器官发育受损
7. Embryonic lethality in mice lacking Trim59 due to impaired gastrulation development [O] . Xiaomin Su, Chenglei Wu, Xiaoying Ye, 2017

机译：由于腐蚀性发育损害，缺乏TRIM59缺乏TRIM59的胚胎致死性

Embryonic lethality in mice lacking Trim59 due to impaired gastrulation development

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