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N-Myc下游调控基因1b是早期肌肉发育过程中细胞黏附的调节因子。

N-Myc downstream regulated gene 1b is a regulator of cell adhesion during early muscle development.

作者信息

Chowdhary P K, Brewster R M

机构信息

University of Maryland, Baltimore County.

出版信息

bioRxiv. 2025 May 13:2025.05.08.652902. doi: 10.1101/2025.05.08.652902.

Abstract

The complexity of cellular functions necessitates intricate pathways that govern protein synthesis, transport, and degradation; yet the mechanisms governing the trafficking of key developmental proteins remain incompletely understood. N-Myc downstream-regulated genes (NDRGs) have recently emerged as stress-responsive proteins with roles in protein trafficking, but their functions during normal embryogenesis are largely unknown. Here, we identify N-Myc downstream-regulated gene 1b (Ndrg1b) as a novel regulator of N-cadherin (N-cad, ) trafficking during zebrafish muscle development. We show that is broadly expressed during embryonic and larval stages and is required for proper skeletal muscle morphogenesis. Loss of Ndrg1b disrupts N-cad localization and impairs cell adhesion , highlighting a key role in maintaining tissue integrity. Mechanistically, Ndrg1b promotes the recycling of N-cad to the plasma membrane, identifying it as a novel component of the endocytic trafficking machinery . Given N-cad's central role in development and disease, these findings provide new insight into how its localization is fine-tuned during morphogenesis. This work also expands the functional repertoire of NDRGs beyond stress response, suggesting that Ndrg1b - and potentially other NDRG family members - may broadly regulate transmembrane protein trafficking in a context-dependent manner. Furthermore, these findings may shed greater light on the etiology of Charcot-Marie-Tooth Disease type 4D, which has been linked to mutations in NDRG1.

摘要

细胞功能的复杂性需要复杂的途径来调控蛋白质的合成、运输和降解;然而,调控关键发育蛋白运输的机制仍未完全了解。N-Myc下游调控基因(NDRGs)最近作为应激反应蛋白出现,在蛋白质运输中发挥作用,但其在正常胚胎发育过程中的功能很大程度上尚不清楚。在这里,我们确定N-Myc下游调控基因1b(Ndrg1b)是斑马鱼肌肉发育过程中N-钙黏蛋白(N-cad)运输的一种新型调节因子。我们发现Ndrg1b在胚胎和幼体阶段广泛表达,是正常骨骼肌形态发生所必需的。Ndrg1b的缺失会破坏N-cad的定位并损害细胞黏附,突出了其在维持组织完整性中的关键作用。从机制上讲,Ndrg1b促进N-cad循环回到质膜,将其确定为内吞运输机制的一个新成分。鉴于N-cad在发育和疾病中的核心作用,这些发现为其在形态发生过程中如何进行精细定位提供了新的见解。这项工作还将NDRGs的功能范围扩展到应激反应之外,表明Ndrg1b以及潜在的其他NDRG家族成员可能以上下文依赖的方式广泛调节跨膜蛋白运输。此外,这些发现可能会为与NDRG1突变相关的4D型夏科-马里-图斯病的病因提供更多线索。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a028/12132217/567303bfa42b/nihpp-2025.05.08.652902v1-f0002.jpg

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