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Species-specific FMRP regulation of RACK1 is critical for prenatal cortical development

Fragile X Syndrome
DOI: 10.1016/j.neuron.2023.09.014 Publication Date: 2023-10-10T14:30:08Z
Abstract Supplemental Material References Cited by
AUTHORS (25)
Minjie Shen
Carissa L. Sirois
Yu Guo
Meng Li
Qiping Dong
Natasha M. Méndez...
Yu Gao
Saniya Khullar
Lee Kissel
Soraya O. Sandoval
Natalie E. Wolkoff
Sabrina X. Huang
Zhiyan Xu
Jonathan E. Bryan
Amaya M. Contractor
Tomer Korabelnikov
Ian A. Glass
Dan Doherty
Jon E. Levine
André M.M. Sousa
Qiang Chang
Anita Bhattacharyya
Daifeng Wang
Donna M. Werling
Xinyu Zhao
ABSTRACT
Fragile X messenger ribonucleoprotein 1 protein (FMRP) deficiency leads to fragile X syndrome (FXS), an autism spectrum disorder. The role of FMRP in prenatal human brain development remains unclear. Here, we show that FMRP is important for human and macaque prenatal brain development. Both FMRP-deficient neurons in human fetal cortical slices and FXS patient stem cell-derived neurons exhibit mitochondrial dysfunctions and hyperexcitability. Using multiomics analyses, we have identified both FMRP-bound mRNAs and FMRP-interacting proteins in human neurons and unveiled a previously unknown role of FMRP in regulating essential genes during human prenatal development. We demonstrate that FMRP interaction with CNOT1 maintains the levels of receptor for activated C kinase 1 (RACK1), a species-specific FMRP target. Genetic reduction of RACK1 leads to both mitochondrial dysfunctions and hyperexcitability, resembling FXS neurons. Finally, enhancing mitochondrial functions rescues deficits of FMRP-deficient cortical neurons during prenatal development, demonstrating targeting mitochondrial dysfunction as a potential treatment.
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