Mutations in GFAP Disrupt the Distribution and Function of Organelles in Human Astrocytes.

Authors :: Jones JR
Kong L
Hanna MG 4th
Hoffman B
Krencik R
Bradley R
Hagemann T
Choi J
Doers M
Dubovis M
Sherafat MA
Bhattacharyya A
Kendziorski C
Audhya A
Messing A
Zhang SC
Source :: Cell reports [Cell Rep] 2018 Oct 23; Vol. 25 (4), pp. 947-958.e4.
Publication Year :: 2018
Abstract: How mutations in glial fibrillary acidic protein (GFAP) cause Alexander disease (AxD) remains elusive. We generated iPSCs from two AxD patients and corrected the GFAP mutations to examine the effects of mutant GFAP on human astrocytes. AxD astrocytes displayed GFAP aggregates, recapitulating the pathological hallmark of AxD. RNA sequencing implicated the endoplasmic reticulum, vesicle regulation, and cellular metabolism. Corroborating this analysis, we observed enlarged and heterogeneous morphology coupled with perinuclear localization of endoplasmic reticulum and lysosomes in AxD astrocytes. Functionally, AxD astrocytes showed impaired extracellular ATP release, which is responsible for attenuated calcium wave propagation. These results reveal that AxD-causing mutations in GFAP disrupt intracellular vesicle regulation and impair astrocyte secretion, resulting in astrocyte dysfunction and AxD pathogenesis.<br /> (Copyright © 2018 The Authors. Published by Elsevier Inc. All rights reserved.)

Subjects :: Adenosine Triphosphate metabolism
Alexander Disease metabolism
Alexander Disease pathology
Animals
Astrocytes cytology
Calcium Signaling
Cell Differentiation
Endoplasmic Reticulum metabolism
Humans
Lysosomes metabolism
Mice
Protein Aggregates
RNA, Messenger genetics
RNA, Messenger metabolism
Astrocytes metabolism
Glial Fibrillary Acidic Protein genetics
Mutation genetics
Organelles metabolism

Full Text Access

Tools