Fragile X syndrome patient-derived neurons developing in the mouse brain show FMR1 -dependent phenotypes

Author:

Krzisch Marine A.,Wu Hao,Yuan Bingbing,Whitfield Troy W.,Shawn Liu X.,Fu Dongdong,Shih Jennifer,Garrett-Engele Carrie M.,Chang Aaron N.,Warren Stephen,Cacace Angela,Andrykovich Kristin R.,Rietjens Rosalie G. J.,Jain Bhav,Wallace Owen,Sur Mriganka,Jaenisch Rudolf

Abstract

AbstractAbnormal neuronal development in Fragile X syndrome (FXS) is poorly understood. Data on FXS patients remain scarce and FXS animal models have failed to yield successful therapies. In vitro models do not fully recapitulate the morphology and function of human neurons. Here, we co-injected neural precursor cells (NPCs) from FXS patient-derived and corrected isogenic control induced pluripotent stem cells into the brain of neonatal immune-deprived mice. The transplanted cells populated the brain and a proportion differentiated into neurons and glial cells. Single-cell RNA sequencing of transplanted cells revealed upregulated excitatory synaptic transmission and neuronal differentiation pathways in FXS neurons. Immunofluorescence analyses showed accelerated maturation of FXS neurons after an initial delay. Additionally, increased percentages of Arc- and Egr1-positive FXS neurons and wider dendritic protrusions of mature FXS striatal medium spiny neurons pointed to an increase in synaptic activity and synaptic strength as compared to control. This transplantation approach provides new insights into the alterations of neuronal development in FXS by facilitating physiological development of cells in a 3D context, and could be used to test new therapeutic compounds correcting neuronal development defects in FXS.

Publisher

Cold Spring Harbor Laboratory

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