| Literature DB >> 27212239 |
Qiao-Chu Wang1, Qiaoxia Zheng1, Haiyan Tan2, Bing Zhang3, Xiaoling Li1, Yuxiu Yang3, Jie Yu4, Yang Liu5, Hao Chai3, Xi Wang1, Zhongshuai Sun5, Jiu-Qiang Wang1, Shu Zhu1, Fengli Wang1, Maojun Yang4, Caixia Guo5, Heng Wang6, Qingyin Zheng7, Yang Li3, Quan Chen1, Aimin Zhou8, Tie-Shan Tang9.
Abstract
Maintaining homeostasis of Ca(2+) stores in the endoplasmic reticulum (ER) is crucial for proper Ca(2+) signaling and key cellular functions. The Ca(2+)-release-activated Ca(2+) (CRAC) channel is responsible for Ca(2+) influx and refilling after store depletion, but how cells cope with excess Ca(2+) when ER stores are overloaded is unclear. We show that TMCO1 is an ER transmembrane protein that actively prevents Ca(2+) stores from overfilling, acting as what we term a "Ca(2+) load-activated Ca(2+) channel" or "CLAC" channel. TMCO1 undergoes reversible homotetramerization in response to ER Ca(2+) overloading and disassembly upon Ca(2+) depletion and forms a Ca(2+)-selective ion channel on giant liposomes. TMCO1 knockout mice reproduce the main clinical features of human cerebrofaciothoracic (CFT) dysplasia spectrum, a developmental disorder linked to TMCO1 dysfunction, and exhibit severe mishandling of ER Ca(2+) in cells. Our findings indicate that TMCO1 provides a protective mechanism to prevent overfilling of ER stores with Ca(2+) ions.Entities:
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Year: 2016 PMID: 27212239 DOI: 10.1016/j.cell.2016.04.051
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 41.582