Genetic and acute CPEB1 depletion ameliorate fragile X pathophysiology

Udagawa, Tsuyoshi ; Farny, Natalie G ; Jakovcevski, Mira ; Kaphzan, Hanoch ; Alarcon, Juan Marcos ; Anilkumar, Shobha ; Ivshina, Maria ; Hurt, Jessica A ; Nagaoka, Kentaro ; Nalavadi, Vijayalaxmi C ; Lorenz, Lori J ; Bassell, Gary J ; Akbarian, Schahram ; Chattarji, Sumantra ; Klann, Eric ; Richter, Joel D (2013) Genetic and acute CPEB1 depletion ameliorate fragile X pathophysiology Nature Medicine, 19 (11). pp. 1473-1477. ISSN 1078-8956

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Official URL: http://doi.org/10.1038/nm.3353

Related URL: http://dx.doi.org/10.1038/nm.3353

Abstract

Fragile X syndrome (FXS), the most common cause of inherited mental retardation and autism, is caused by transcriptional silencing of FMR1, which encodes the translational repressor fragile X mental retardation protein (FMRP). FMRP and cytoplasmic polyadenylation element–binding protein (CPEB), an activator of translation, are present in neuronal dendrites, are predicted to bind many of the same mRNAs and may mediate a translational homeostasis that, when imbalanced, results in FXS. Consistent with this possibility, Fmr1−/y; Cpeb1−/− double-knockout mice displayed amelioration of biochemical, morphological, electrophysiological and behavioral phenotypes associated with FXS. Acute depletion of CPEB1 in the hippocampus of adult Fmr1−/y mice rescued working memory deficits, demonstrating reversal of this FXS phenotype. Finally, we find that FMRP and CPEB1 balance translation at the level of polypeptide elongation. Our results suggest that disruption of translational homeostasis is causal for FXS and that the maintenance of this homeostasis by FMRP and CPEB1 is necessary for normal neurologic function.

Item Type:Article
Source:Copyright of this article belongs to Springer Nature Limited
ID Code:130557
Deposited On:28 Nov 2022 05:18
Last Modified:28 Nov 2022 05:18

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