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LC3A 沉默抑制原发性脉络丛癌中聚集物微管相关蛋白 vimentin 笼的清除。

LC3A Silencing Hinders Aggresome Vimentin Cage Clearance in Primary Choroid Plexus Carcinoma.

机构信息

Tumor Biology Research Program, Basic Research Unit, Department of Research, Children's Cancer Hospital Egypt 57357, P.O Box 11441, 1 Seket Al-Emam Street, Cairo, Egypt.

Biotechnology Graduate Program, American University in Cairo. New Cairo Campus, AUC Avenue, P.O Box 74, New Cairo, 11835, Egypt.

出版信息

Sci Rep. 2017 Aug 14;7(1):8022. doi: 10.1038/s41598-017-07403-5.

Abstract

Aggresomes are transient microtubule-dependent inclusion bodies that sequester misfolded proteins and are ultimately removed by autophagy. Here we report the generation of a choroid plexus carcinoma cell line; Children's Cancer Hospital Egypt (CCHE)-45, which is characterized by the constitutive formation of aggresomes. When examining the autophagy pathway as the main route for aggresomes clearance, CCHE-45 cells displayed increased autophagy flux mediated by MAP1LC3B. MAP1LC3A-Variant1 gene expression was silenced by promoter methylation. Restoring MAP1LC3A-Variant1 expression resulted in the formation of MAP1LC3A positive autophagosmes and the disruption of the aggresomes' vimentin cage independent of MAP1LC3B positive autophagosomes. Our data supports the notion that basal quality control autophagy and vimentin cage clearance in CCHE-45 are mediated by MAP1LC3A. Hence we propose that absence of MAP1LC3A disrupts the autophagic pathway and leads to the failure of aggresome vimentin cage degradation. Consequently, this could represent a targetable pathway in autophagy-dependent cancers.

摘要

聚集物是瞬时的微管依赖性包含体,可隔离错误折叠的蛋白质,并最终通过自噬清除。在这里,我们报告了一种脉络丛癌细胞系的产生;埃及儿童癌症医院(CCHE)-45,其特征是聚集物的组成型形成。在研究自噬途径作为聚集物清除的主要途径时,CCHE-45 细胞显示出由 MAP1LC3B 介导的增加的自噬通量。MAP1LC3A-Variant1 基因表达被启动子甲基化沉默。恢复 MAP1LC3A-Variant1 表达导致 MAP1LC3A 阳性自噬体的形成和聚集物的微管相关蛋白 1A/1B 轻链 3B (MAP1LC3B) 阳性自噬体的形成,而不依赖于微管相关蛋白 1A/1B 阳性自噬体。我们的数据支持这样一种观点,即 CCHE-45 中的基础质量控制自噬和微管相关蛋白 1A 笼清除是由 MAP1LC3A 介导的。因此,我们提出缺乏 MAP1LC3A 会破坏自噬途径,并导致聚集物微管相关蛋白 1A 笼降解失败。因此,这可能代表了自噬依赖性癌症中一个可靶向的途径。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b3c5/5556083/8ebb08872e1e/41598_2017_7403_Fig1_HTML.jpg

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