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过度表达诱导自噬细胞死亡。

overexpression induces autophagic cell death.

机构信息

Department of Biological Sciences, San José State University, San José, CA 95112.

出版信息

Mol Biol Cell. 2024 Jul 1;35(7):br13. doi: 10.1091/mbc.E24-02-0058. Epub 2024 May 2.

Abstract

Autophagy is a conserved catabolic process where double membrane-bound structures form around macromolecules or organelles targeted for degradation. Autophagosomes fuse with lysosomes to facilitate degradation and macromolecule recycling for homeostasis or growth in a cell autonomous manner. In cancer cells, autophagy is often up-regulated and helps cancer cells survive nutrient deprivation and stressful growth conditions. Here, we propose that the increased intracellular pH (pHi) common to cancer cells is sufficient to induce autophagic cell death. We previously developed tools to increase pHi in the eye via overexpression of resulting in aberrant patterning and reduced tissue size. We examined fly eyes at earlier stages of development and found fewer interommatidial cells. We next tested whether this decrease in cell number was due to increased cell death. We found that the -induced cell death was caspase independent, which is inconsistent with apoptosis. However, this cell death required autophagy genes, which supports autophagy as the mode of cell death. We also found that expression of molecular markers supports increased autophagy. Together, our findings suggest new roles for ion transport proteins in regulating conserved, critical developmental processes and provide evidence for new paradigms in growth control.

摘要

自噬是一种保守的分解代谢过程,其中双层膜结构围绕着大分子或细胞器形成,这些大分子或细胞器是降解的目标。自噬体与溶酶体融合,以促进降解和大分子的回收,从而实现细胞自主的稳态或生长。在癌细胞中,自噬通常被上调,有助于癌细胞在营养缺乏和应激生长条件下存活。在这里,我们提出,癌细胞中常见的细胞内 pH 值(pHi)升高足以诱导自噬性细胞死亡。我们之前开发了通过过表达来增加眼睛内 pHi 的工具,导致异常的图案形成和组织大小减少。我们在发育的早期阶段检查了果蝇的眼睛,发现了更少的小眼间细胞。我们接下来测试了细胞数量的减少是否是由于细胞死亡增加所致。我们发现这种细胞死亡不依赖于半胱天冬酶,这与细胞凋亡不一致。然而,这种细胞死亡需要自噬基因,这支持自噬是细胞死亡的模式。我们还发现,分子标记的表达支持自噬的增加。总之,我们的研究结果表明,离子转运蛋白在调节保守的、关键的发育过程中发挥新的作用,并为生长控制的新范式提供了证据。

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