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  • The stress granule protein G3BP1 promotes pre-condensation of cGAS to allow rapid responses to DNA.

The stress granule protein G3BP1 promotes pre-condensation of cGAS to allow rapid responses to DNA.

EMBO reports (2021-11-16)
Ming Zhao, Tian Xia, Jia-Qing Xing, Le-Hua Yin, Xiao-Wei Li, Jie Pan, Jia-Yu Liu, Li-Ming Sun, Miao Wang, Tingting Li, Jie Mao, Qiu-Ying Han, Wen Xue, Hong Cai, Kai Wang, Xin Xu, Teng Li, Kun He, Na Wang, Ai-Ling Li, Tao Zhou, Xue-Min Zhang, Wei-Hua Li, Tao Li
ABSTRACT

Cyclic GMP-AMP synthase (cGAS) functions as a key sensor for microbial invasion and cellular damage by detecting emerging cytosolic DNA. Here, we report that GTPase-activating protein-(SH3 domain)-binding protein 1 (G3BP1) primes cGAS for its prompt activation by engaging cGAS in a primary liquid-phase condensation state. Using high-resolution microscopy, we show that in resting cells, cGAS exhibits particle-like morphological characteristics, which are markedly weakened when G3BP1 is deleted. Upon DNA challenge, the pre-condensed cGAS undergoes liquid-liquid phase separation (LLPS) more efficiently. Importantly, G3BP1 deficiency or its inhibition dramatically diminishes DNA-induced LLPS and the subsequent activation of cGAS. Interestingly, RNA, previously reported to form condensates with cGAS, does not activate cGAS. Accordingly, we find that DNA - but not RNA - treatment leads to the dissociation of G3BP1 from cGAS. Taken together, our study shows that the primary condensation state of cGAS is critical for its rapid response to DNA.

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