Fragile X Syndrome Patient-Derived Neurons Developing in the Mouse Brain Show FMR1-Dependent Phenotypes

脆性 X 综合征患者衍生的小鼠脑内发育的神经元表现出 FMR1 依赖性表型

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

Background

Fragile X syndrome (FXS) is characterized by physical abnormalities, anxiety, intellectual disability, hyperactivity, autistic behaviors, and seizures. Abnormal neuronal development in FXS is poorly understood. Data on patients with FXS 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.

Conclusions

This transplantation approach provides new insights into the alterations of neuronal development in FXS by facilitating physiological development of cells in a 3-dimensional context.

Methods

To mimic human neuron development in vivo, we coinjected neural precursor cells derived from FXS patient-derived induced pluripotent stem cells and neural precursor cells derived from corrected isogenic control induced pluripotent stem cells into the brain of neonatal immune-deprived mice.

Results

The transplanted cells populated the brain and a proportion differentiated into neurons and glial cells. Immunofluorescence and single and bulk RNA sequencing analyses showed accelerated maturation of FXS neurons after an initial delay. Additionally, we found increased percentages of Arc- and Egr-1-positive FXS neurons and wider dendritic protrusions of mature FXS striatal medium spiny neurons. Conclusions: This transplantation approach provides new insights into the alterations of neuronal development in FXS by facilitating physiological development of cells in a 3-dimensional context.

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