ER Stress-Induced Aggresome Trafficking of HtrA1 Protects Against 1! Proteotoxicity

Maximilian Gerhardt, Joseph Marsh, Margaux A Morrison, Andrius Kazlauskas, Arogya Khadka, Stephan Rosenkranz, Margaret M Deangelis, Magali Saint-Geniez, Sarah Melissa Jacobo

Research output: Contribution to journalArticlepeer-review

Abstract

High temperature requirement A1 (HtrA1) belongs to an ancient protein family that is linked to various human disorders. The precise role of exon 1-encoded N-terminal domains and how these influence the biological functions of human HtrA1 remain elusive. In this study, we traced the evolutionary origins of these N-terminal domains to a single gene fusion event in the most recent common ancestor of vertebrates. We hypothesized that human HtrA1 is implicated in unfolded protein response. In highly secretory cells of the retinal pigmented epithelia, endoplasmic reticulum (ER) stress upregulated HtrA1. HtrA1 co-localized with vimentin intermediate filaments in highly arborized fashion. Upon ER stress, HtrA1 tracked along intermediate filaments, which collapsed and bundled in an aggresome at the microtubule organizing center. Gene silencing of HtrA1 altered the schedule and amplitude of adaptive signaling and concomitantly resulted in apoptosis. Restoration of wild-type HtrA1, but not its protease inactive mutant, was necessary and sufficient to protect from apoptosis. A variant of HtrA1 that harbored exon 1 substitutions displayed reduced efficacy in rescuing cells from proteotoxicity. Our results illuminate the integration of HtrA1 in the toolkit of mammalian cells against protein misfolding and the implications of defects in HtrA1 in proteostasis.
Original languageEnglish
JournalJournal of Molecular Cell Biology
Early online date20 Jul 2017
DOIs
Publication statusPublished - 10 Aug 2017

Fingerprint

Dive into the research topics of 'ER Stress-Induced Aggresome Trafficking of HtrA1 Protects Against 1! Proteotoxicity'. Together they form a unique fingerprint.

Cite this