Litcius/Paper detail

A systemic cell stress signal confers neuronal resilience toward oxidative stress in a Hedgehog-dependent manner

Kyung Min Chung, Hyunha Kim, Cláudio Gouveia Roque, Ethan P. McCurdy, Trang Nguyen, Markus D. Siegelin, Jee-Yeon Hwang, Ulrich Hengst

2022Cell Reports21 citationsDOIOpen Access PDF

Abstract

Cells possess several conserved adaptive mechanisms to respond to stress. Stress signaling is initiated to reestablish cellular homeostasis, but its effects on the tissue or systemic levels are far less understood. We report that the secreted luminal domain of the endoplasmic reticulum (ER) stress transducer CREB3L2 (which we name TAILS [transmissible activator of increased cell livability under stress]) is an endogenous, cell non-autonomous activator of neuronal resilience. In response to oxidative insults, neurons secrete TAILS, which potentiates hedgehog signaling through direct interaction with Sonic hedgehog (SHH) and its receptor PTCH1, leading to improved antioxidant signaling and mitochondrial function in neighboring neurons. In an in vivo model of ischemic brain injury, administration of TAILS enables survival of CNS neurons and fully preserves cognitive function in behavioral tests. Our findings reveal an SHH-mediated, cell non-autonomous branch of cellular stress signaling that confers resilience to oxidative stress in the mature brain, providing protection from ischemic neurodegeneration.

Topics & Concepts

Cell biologyOxidative stressBiologyHedgehogSonic hedgehogEndoplasmic reticulumNeurodegenerationSignal transductionNeuroscienceHedgehog signaling pathwaySTAT proteinSTAT3EndocrinologyInternal medicineMedicineDiseaseEndoplasmic Reticulum Stress and DiseaseHedgehog Signaling Pathway StudiesMitochondrial Function and Pathology