Structure and Functionality of a Multimeric Human COQ7:COQ9 Complex

Overview

Journal Mol Cell

Publisher Cell Press

Specialty Cell Biology

Date 2022 Oct 28

PMID 36306796

Authors

Mateusz Manicki

Halil Aydin

Luciano A Abriata

Katherine A Overmyer

Rachel M Guerra

Joshua J Coon

Matteo Dal Peraro

Adam Frost

David J Pagliarini

Affiliations

Soon will be listed here.

Abstract

Coenzyme Q (CoQ) is a redox-active lipid essential for core metabolic pathways and antioxidant defense. CoQ is synthesized upon the mitochondrial inner membrane by an ill-defined "complex Q" metabolon. Here, we present structure-function analyses of a lipid-, substrate-, and NADH-bound complex comprising two complex Q subunits: the hydroxylase COQ7 and the lipid-binding protein COQ9. We reveal that COQ7 adopts a ferritin-like fold with a hydrophobic channel whose substrate-binding capacity is enhanced by COQ9. Using molecular dynamics, we further show that two COQ7:COQ9 heterodimers form a curved tetramer that deforms the membrane, potentially opening a pathway for the CoQ intermediates to translocate from the bilayer to the proteins' lipid-binding sites. Two such tetramers assemble into a soluble octamer with a pseudo-bilayer of lipids captured within. Together, these observations indicate that COQ7 and COQ9 cooperate to access hydrophobic precursors within the membrane and coordinate subsequent synthesis steps toward producing CoQ.

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