Litcius/Paper detail

Mitochondrial ClpX activates an essential biosynthetic enzyme through partial unfolding

Julia R. Kardon, Jamie A. Moroco, John R. Engen, Tania A. Baker

2020eLife38 citationsDOIOpen Access PDF

Abstract

Mitochondria control the activity, quality, and lifetime of their proteins with an autonomous system of chaperones, but the signals that direct substrate-chaperone interactions and outcomes are poorly understood. We previously discovered that the mitochondrial AAA+ protein unfoldase ClpX (mtClpX) activates the initiating enzyme for heme biosynthesis, 5-aminolevulinic acid synthase (ALAS), by promoting cofactor incorporation. Here, we ask how mtClpX accomplishes this activation. Using S. cerevisiae proteins, we identified sequence and structural features within ALAS that position mtClpX and provide it with a grip for acting on ALAS. Observation of ALAS undergoing remodeling by mtClpX revealed that unfolding is limited to a region extending from the mtClpX-binding site to the active site. Unfolding along this path is required for mtClpX to gate cofactor binding to ALAS. This targeted unfolding contrasts with the global unfolding canonically executed by ClpX homologs and provides insight into how substrate-chaperone interactions direct the outcome of remodeling.

Topics & Concepts

Chaperone (clinical)EnzymeCofactorHemeATP synthaseCell biologyBiologyMitochondrionPlasma protein bindingBiochemistryChemistryBiophysicsMedicinePathologyPorphyrin Metabolism and DisordersPhotosynthetic Processes and MechanismsEnzyme Structure and Function