Laurent David scite author profile

A fascinating but uncharacterized action of antimitotic chemotherapy is to collectively prime cancer cells to apoptotic mitochondrial outer membrane permeabilization (MOMP), while impacting only on cycling cell subsets. Here, we show that a proapoptotic secretory phenotype is induced by activation of cGAS/STING in cancer cells that are hit by antimitotic treatment, accumulate micronuclei and maintain mitochondrial integrity despite intrinsic apoptotic pressure. Organotypic cultures of primary human breast tumors and patientderived xenografts sensitive to paclitaxel exhibit gene expression signatures typical of type I IFN and TNFα exposure. These cytokines induced by cGAS/STING activation trigger NOXA expression in neighboring cells and render them acutely sensitive to BCL-xL inhibition. cGAS/STING-dependent apoptotic effects are required for paclitaxel response in vivo, and they are amplified by sequential, but not synchronous, administration of BH3 mimetics. Thus anti-mitotic agents propagate apoptotic priming across heterogeneously sensitive cancer cells through cytosolic DNA sensing pathway-dependent extracellular signals, exploitable by delayed MOMP targeting.

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Hyaluronan hydrogel: An appropriate three-dimensional model for evaluation of anticancer drug sensitivity

David

Dulong

Cerf

et al. 2008

Acta Biomaterialia

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Reticulated hyaluronan hydrogels: a model for examining cancer cell invasion in 3D

et al. 2004

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Collagens, stromal cell‐derived factor‐1α and basic fibroblast growth factor increase cancer cell invasiveness in a hyaluronan hydrogel

David¹,

Dulong²,

Coquerel³

et al. 2008

Cell Proliferation

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Laurent David

STING-dependent paracriny shapes apoptotic priming of breast tumors in response to anti-mitotic treatment

Hyaluronan hydrogel: An appropriate three-dimensional model for evaluation of anticancer drug sensitivity

Reticulated hyaluronan hydrogels: a model for examining cancer cell invasion in 3D

Collagens, stromal cell‐derived factor‐1α and basic fibroblast growth factor increase cancer cell invasiveness in a hyaluronan hydrogel

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