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细胞与细胞外基质黏附的精确协调对于黑素细胞在发育过程中的有效迁移至关重要。

Precise coordination of cell-ECM adhesion is essential for efficient melanoblast migration during development.

机构信息

Department of Biomedical Sciences, University of North Dakota, 1301 N Columbia Rd, Grand Forks, ND 58202, ND, USA.

Department of Cellular and Physiological Sciences, 2350 Health Sciences Mall, University of British Columbia, Vancouver, BC, Canada.

出版信息

Development. 2020 Jul 17;147(14):dev184234. doi: 10.1242/dev.184234.

Abstract

Melanoblasts disperse throughout the skin and populate hair follicles through long-range cell migration. During migration, cells undergo cycles of coordinated attachment and detachment from the extracellular matrix (ECM). Embryonic migration processes that require cell-ECM attachment are dependent on the integrin family of adhesion receptors. Precise regulation of integrin-mediated adhesion is important for many developmental migration events. However, the mechanisms that regulate integrin-mediated adhesion in melanoblasts are not well understood. Here, we show that autoinhibitory regulation of the integrin-associated adapter protein talin coordinates cell-ECM adhesion during melanoblast migration Specifically, an autoinhibition-defective talin mutant strengthens and stabilizes integrin-based adhesions in melanocytes, which impinges on their ability to migrate. Mice with defective talin autoinhibition exhibit delays in melanoblast migration and pigmentation defects. Our results show that coordinated integrin-mediated cell-ECM attachment is essential for melanoblast migration and that talin autoinhibition is an important mechanism for fine-tuning cell-ECM adhesion during cell migration in development.

摘要

黑素细胞通过长距离细胞迁移散布在皮肤中,并定植在毛囊中。在迁移过程中,细胞经历与细胞外基质(ECM)附着和脱离的协调循环。需要细胞-ECM 附着的胚胎迁移过程依赖于整合素家族的粘附受体。整合素介导的粘附的精确调节对于许多发育性迁移事件很重要。然而,调节黑素细胞中整合素介导的粘附的机制尚不清楚。在这里,我们表明整合素相关衔接蛋白塔林的自动抑制调节在黑素细胞迁移过程中协调细胞-ECM 粘附。具体而言,一种自动抑制缺陷的塔林突变体增强并稳定黑素细胞中的整合素基附着,这影响了它们的迁移能力。具有缺陷的塔林自动抑制的小鼠表现出黑素细胞迁移延迟和色素沉着缺陷。我们的结果表明,协调的整合素介导的细胞-ECM 附着对于黑素细胞迁移是必不可少的,并且塔林自动抑制是在发育过程中细胞迁移期间精细调节细胞-ECM 粘附的重要机制。

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