Structure of a human intramembrane ceramidase explains enzymatic dysfunction found in leukodystrophy

Author:

Vasiliauskaité-Brooks Ieva,Healey Robert D.,Rochaix Pascal,Sounier Rémy,Grison Claire,Waltrich-Augusto Thierry,Fortier Mathieu,Hoh François,Saied Essa M.,Arenz Christoph,Basu Shibom,Leyrat CédricORCID,Granier Sébastien

Abstract

AbstractAlkaline ceramidases (ACERs) are a class of poorly understood transmembrane enzymes controlling the homeostasis of ceramides. They are implicated in human pathophysiology, including progressive leukodystrophy, colon cancer as well as acute myeloid leukemia. We report here the crystal structure of the human ACER type 3 (ACER3). Together with computational studies, the structure reveals that ACER3 is an intramembrane enzyme with a seven transmembrane domain architecture and a catalytic Zn2+ binding site in its core, similar to adiponectin receptors. Interestingly, we uncover a Ca2+ binding site physically and functionally connected to the Zn2+ providing a structural explanation for the known regulatory role of Ca2+ on ACER3 enzymatic activity and for the loss of function in E33G-ACER3 mutant found in leukodystrophic patients.

Publisher

Cold Spring Harbor Laboratory

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