POGLUT2/3介导的EGF o糖基化通过影响原纤维蛋白网络重组、信号传导和细胞动力学促进数字2和3的分离。

IF 2.1 3区 生物学 Q2 DEVELOPMENTAL BIOLOGY
Sanjiv Neupane , Isabella A. Janowicz , Alan R.F. Godwin , Kaitlyn E. Donnelly , Richard C. Grady , Robert S. Haltiwanger , Clair Baldock , Bernadette C. Holdener
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引用次数: 0

摘要

单个指的分离依赖于指间周期的建立、指间间质的重塑和指间上皮舌的内陷。在蛋白o -葡萄糖基转移酶2和3双敲除(Poglut2/3 DKO)小鼠中,2和3趾融合,表明在一个或多个过程中存在缺陷。POGLUT2/3向表皮生长因子样(EGF)重复序列添加o -连接葡萄糖。当编码POGLUT2/3底物原纤维蛋白2 (FBN2)或Nidogen 1和2 (NID1/2)的基因被敲除时,也观察到并指现象,这表明o -糖基化对它们的功能或定位很重要。在这项研究中,我们评估了这些底物在手指分离过程中的分布,以及Poglut2/3 DKO对其定位和细胞行为的影响。在手指分离期间,fbn经历了戏剧性的重组。在Poglut2/3 DKO中观察到异常的FBNs水平和分布,从Poglut2/3 DKO皮肤中分离的微原纤维显示出纤维蛋白微原纤维的周期性改变。相比之下,Poglut2/3 DKO对NID1的水平或定位没有影响。在Poglut2/3 dko中,骨形态发生蛋白(BMP)信号在手指发育过程中减少,尤其是在前自足。早期前路BMP信号减少可能会影响趾2和趾3的间距。而随后2-3趾区Poglut2/3 DKO中BMP信号的减少可能是指间间质清除和指间舌形态发生缺陷的原因。这些结果强调了POGLUT2/3介导的o -葡萄糖化对FBN微纤维组织的重要性,并提出了o -葡萄糖调节FBN微纤维网络的生物学或物理特性的可能性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

POGLUT2/3 mediated EGF O-glucosylation promotes separation of digits 2 and 3 by influencing fibrillin network reorganization, signaling, and cell dynamics

POGLUT2/3 mediated EGF O-glucosylation promotes separation of digits 2 and 3 by influencing fibrillin network reorganization, signaling, and cell dynamics
The separation of individual digits is dependent on establishment of digit-interdigit periodicity, remodeling of the interdigital mesenchyme, and invagination of interdigital epithelial tongues. In Protein O-glucosyltransferase 2 and 3 double knockout (Poglut2/3 DKO) mice, digits 2 and 3 are fused, suggesting a defect in one or more processes. POGLUT2/3 add O-linked glucose to epidermal growth factor-like (EGF) repeats. Syndactyly is also observed when genes encoding the POGLUT2/3 substrates fibrillin 2 (FBN2) or both Nidogen 1 and 2 (NID1/2) are knocked out, suggesting that O-glucosylation is important for their function or localization. In this study, we evaluated the distribution of these substrates during digit separation and the effects of the Poglut2/3 DKO on their localization and cell behavior. During digit separation, the FBNs underwent a dramatic reorganization. Aberrant levels and distribution of the FBNs were observed in the Poglut2/3 DKO and microfibrils isolated from Poglut2/3 DKO skin showed altered periodicity in Fibrillin microfibrils. In contrast, the Poglut2/3 DKO had no effect on the levels or localization of NID1. In Poglut2/3 DKOs, bone morphogenetic protein (BMP) signaling was reduced during digit development, especially in the anterior autopod. Early anterior reduction of BMP signaling could potentially affect spacing of digits 2 & 3. While later reduction of BMP signaling in the Poglut2/3 DKO in the digit 2–3 region was likely responsible for defects in clearance of interdigital mesenchyme and interdigital tongue morphogenesis. These results highlight the importance of POGLUT2/3 mediated O-glucosylation for FBN microfibril organization and raise the possibility that O-glucose modulates the biological or physical properties of the FBN microfibril network.
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来源期刊
Developmental biology
Developmental biology 生物-发育生物学
CiteScore
5.30
自引率
3.70%
发文量
182
审稿时长
1.5 months
期刊介绍: Developmental Biology (DB) publishes original research on mechanisms of development, differentiation, and growth in animals and plants at the molecular, cellular, genetic and evolutionary levels. Areas of particular emphasis include transcriptional control mechanisms, embryonic patterning, cell-cell interactions, growth factors and signal transduction, and regulatory hierarchies in developing plants and animals.
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