A Pseudoautosomal Glycosylation Disorder Prompts the Revision of Dolichol Biosynthesis

Overview

Journal Cell

Publisher Cell Press

Specialty Cell Biology

Date 2024 May 31

PMID 38821050

Authors

Matthew P Wilson

Takfarinas Kentache

Charlotte R Althoff

Celine Schulz

Geoffroy de Bettignies

Gisele Mateu Cabrera

Loreta Cimbalistiene

Birute Burnyte

Grace Yoon

Gregory Costain

Sandrine Vuillaumier-Barrot

David Cheillan

Daisy Rymen

Lucie Rychtarova

Hana Hansikova

Marina Bury

Joseph P Dewulf

Francesco Caligiore

Jaak Jaeken

Vincent Cantagrel

Emile Van Schaftingen

Gert Matthijs

Francois Foulquier

Guido T Bommer

Affiliations

Soon will be listed here.

Abstract

Dolichol is a lipid critical for N-glycosylation as a carrier for activated sugars and nascent oligosaccharides. It is commonly thought to be directly produced from polyprenol by the enzyme SRD5A3. Instead, we found that dolichol synthesis requires a three-step detour involving additional metabolites, where SRD5A3 catalyzes only the second reaction. The first and third steps are performed by DHRSX, whose gene resides on the pseudoautosomal regions of the X and Y chromosomes. Accordingly, we report a pseudoautosomal-recessive disease presenting as a congenital disorder of glycosylation in patients with missense variants in DHRSX (DHRSX-CDG). Of note, DHRSX has a unique dual substrate and cofactor specificity, allowing it to act as a NAD-dependent dehydrogenase and as a NADPH-dependent reductase in two non-consecutive steps. Thus, our work reveals unexpected complexity in the terminal steps of dolichol biosynthesis. Furthermore, we provide insights into the mechanism by which dolichol metabolism defects contribute to disease.

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