Abstract Body: Introduction
GJA1-20k, an N-terminus truncated isoform of the gap junction protein Connexin 43, is stress responsive and mimics ischemia preconditioning, reducing ischemia-reperfusion (IR) injury. GJA1-20k localizes to the outer membrane of mitochondria, stabilizes actin, and mediates an actin mediated mitochondrial protection. The mechanism is not known how GJA1-20k and actin work towards mitochondrial protection.

Methods
Cell-free TIRF imaging was performed to study direct interactions between actin and purified GJA1-20k. High-resolution confocal microscopy was applied to visualize GJA1-20k and actin organization around mitochondria in intact HEK cells and cell-free suspensions wherein rhodamine-labeled actin, purified GJA1-20k, and isolated mitochondria were incubated together.

Results
Cell-free TIRF imaging establishes that GJA1-20k directly binds to actin, forming both actin clusters and stabilized actin filaments. As expected, live-cell imaging reveals that GJA1-20k is enriched at the mitochondrial outer membrane. The direct binding of GJA1-20k and actin results in a rich collection of actin around mitochondria, as evidenced in both live-cell imaging and cell-free suspensions containing only purified actin, GJA1-20k, and isolated mitochondria. 3D reconstruction reveals that mitochondrial localization of GJA1-20k causes formation of dense actin sheets enveloping mitochondria, which we call “mitochondrial actin cages” which appear to limit the ability of mitochondria to swell under stress conditions.

Conclusions
GJA1-20k induced actin cages could be critical to GJA1-20k mediated protection against IR injury. The observed actin around mitochondria could prevent pathological mitochondrial swelling, preserving mitochondrial integrity and function in oxidative stress conditions.