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罗马哈沙蛋白和克林特1蛋白的功能表征再次证实了斑马鱼发育中表皮的质膜稳态、细胞大小维持和组织稳态之间的联系。

Functional characterisation of romeharsha and clint1 reaffirms the link between plasma membrane homeostasis, cell size maintenance and tissue homeostasis in developing zebrafish epidermis.

作者信息

Phatak Mandar, Sonawane Mahendra

机构信息

Department of Biological Sciences, Tata Institute of Fundamental Research, Colaba, Mumbai 400 005, India.

出版信息

J Biosci. 2018 Sep;43(4):605-619.

Abstract

In vertebrates, early developing epidermis is a bilayered epithelium consisting of an outer periderm and the underlying basal epidermis. It eventually develops into a multi-layered epithelium. The mechanisms that control the architecture and homeostasis of early developing bilayered epidermis have remained poorly understood. Recently, we have shown that the function of Myosin Vb, an actin based molecular motor, is essential in peridermal cells for maintenance of plasma membrane homeostasis. Furthermore, our analyses of the goosepimples/myosin Vb mutant unravelled a direct link between plasma membrane homeostasis, cell size maintenance and tissue homeostasis in the developing epidermis. However, it remained unclear whether this link is specific to myosin Vb mutant or this is a general principle. Here we have identified two more genetic conditions, romeharsha mutant and clint1 knockdown, in which membrane homeostasis is perturbed, as evident by increased endocytosis and accumulation of lysosomes. As a consequence, peridermal cells exhibit smaller size and increased proliferation. We further show that decreasing endocytosis in romeharsha mutant and clint1 morphants rescues or mitigates the effect on cell size, cell proliferation and morphological phenotype. Our data confirms generality of the principle by reaffirming the causal link between plasma membrane homeostasis, cell size maintenance and tissue homeostasis.

摘要

在脊椎动物中,早期发育的表皮是一种双层上皮组织,由外层的周皮和下方的基底表皮组成。它最终发育成多层上皮组织。控制早期发育的双层表皮的结构和稳态的机制一直未得到充分理解。最近,我们发现肌球蛋白Vb(一种基于肌动蛋白的分子马达)的功能对于周皮细胞维持质膜稳态至关重要。此外,我们对“鸡皮疙瘩”/肌球蛋白Vb突变体的分析揭示了发育中的表皮中质膜稳态、细胞大小维持和组织稳态之间的直接联系。然而,尚不清楚这种联系是肌球蛋白Vb突变体所特有的,还是一个普遍原则。在这里,我们又确定了另外两种遗传条件,即romeharsha突变体和CLINT1基因敲低,在这两种情况下,膜稳态受到干扰,这可通过内吞作用增加和溶酶体积累表现出来。结果,周皮细胞表现出较小的尺寸和增加的增殖。我们进一步表明,降低romeharsha突变体和CLINT1基因敲降胚胎中的内吞作用可挽救或减轻对细胞大小、细胞增殖和形态表型的影响。我们的数据通过再次确认质膜稳态、细胞大小维持和组织稳态之间的因果联系,证实了这一原则的普遍性。

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