Infancy‐onset diabetes caused by de‐regulated
AMPylation
of the human endoplasmic reticulum chaperone
BiP
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Peer-reviewed
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Abstract
Abstract
Dysfunction of the endoplasmic reticulum (ER) in insulin‐producing beta cells results in cell loss and diabetes mellitus. Here we report on five individuals from three different consanguineous families with infancy‐onset diabetes mellitus and severe neurodevelopmental delay caused by a homozygous p.(Arg371Ser) mutation in
FICD
. The
FICD
gene encodes a bifunctional Fic domain‐containing enzyme that regulates the ER Hsp70 chaperone, BiP, via catalysis of two antagonistic reactions: inhibitory AMPylation and stimulatory deAMPylation of BiP. Arg371 is a conserved residue in the Fic domain active site. The FICD
R371S
mutation partially compromises BiP AMPylation
in vitro
but eliminates all detectable deAMPylation activity. Overexpression of FICD
R371S
or knock‐in of the mutation at the
FICD
locus of stressed CHO cells results in inappropriately elevated levels of AMPylated BiP and compromised secretion. These findings, guided by human genetics, highlight the destructive consequences of de‐regulated BiP AMPylation and raise the prospect of tuning FICD's antagonistic activities towards therapeutic ends.
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Journal Title
EMBO Molecular Medicine
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1757-4676
1757-4684
1757-4684
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Publisher
Springer Science and Business Media LLC
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Except where otherwised noted, this item's license is described as http://creativecommons.org/licenses/by/4.0/
Sponsorship
Diabetes UK (19_0005971)
Research England, Expanding Excellence in England (E3) Fund (N/A)
Wellcome Trust (WT) (224407/Z/21Z, 105636/Z/14/Z)
Research England, Expanding Excellence in England (E3) Fund (N/A)
Wellcome Trust (WT) (224407/Z/21Z, 105636/Z/14/Z)