Transcriptional dysregulation and impaired neuronal activity in<i>FMR1</i>knock-out and Fragile X patients’ iPSC-derived models

Maussion, Gilles; Rocha, Cecilia; Abdian, Narges; Yang, Dimitri; Turk, Julien; Valenzuela, Dulce Carrillo; Pimentel, Luisa; You, Zhipeng; Morquette, Barbara; Nicouleau, Michael; Deneault, Eric; Higgins, Samuel; Chen, Carol X.-Q.; Reintsch, Wolfgang; Stanley, Ho; Soubannier, Vincent; Lépine, Sarah; Modrusan, Zora; Lund, Jessica; Stephenson, William; Schubert, Rajib; Durcan, Thomas M.

doi:10.1101/2023.08.30.554628

2023

DOI: 10.1101/2023.08.30.554628

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Transcriptional dysregulation and impaired neuronal activity inFMR1knock-out and Fragile X patients’ iPSC-derived models

Gilles Maussion,

Cecilia Rocha,

Narges Abdian

et al.

Abstract: The lack of fragile X mental retardation protein (FMRP) protein, due to a repression of the FMR1 gene, causes Fragile X syndrome (FXS), one of the most prevalent forms of syndromic autisms. The FMR1 gene codes for a RNA binding protein involved in the regulation of gene expression through RNA processing, control of local translation and protein-protein interactions; processes that are crucial for proper brain development. Taking advantage of induced pluripotent stem cells (iPSCs) and CRISPR-Cas9 genome editing… Show more

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2024

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Recent Therapeutic Gene Editing Applications to Genetic Disorders

Deneault

2024

CIMB

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Recent years have witnessed unprecedented progress in therapeutic gene editing, revolutionizing the approach to treating genetic disorders. In this comprehensive review, we discuss the progression of milestones leading to the emergence of the clustered regularly interspaced short palindromic repeats (CRISPR)-based technology as a powerful tool for precise and targeted modifications of the human genome. CRISPR-Cas9 nuclease, base editing, and prime editing have taken center stage, demonstrating remarkable precision and efficacy in targeted ex vivo and in vivo genomic modifications. Enhanced delivery systems, including viral vectors and nanoparticles, have further improved the efficiency and safety of therapeutic gene editing, advancing their clinical translatability. The exploration of CRISPR-Cas systems beyond the commonly used Cas9, such as the development of Cas12 and Cas13 variants, has expanded the repertoire of gene editing tools, enabling more intricate modifications and therapeutic interventions. Outstandingly, prime editing represents a significant leap forward, given its unparalleled versatility and minimization of off-target effects. These innovations have paved the way for therapeutic gene editing in a multitude of previously incurable genetic disorders, ranging from monogenic diseases to complex polygenic conditions. This review highlights the latest innovative studies in the field, emphasizing breakthrough technologies in preclinical and clinical trials, and their applications in the realm of precision medicine. However, challenges such as off-target effects and ethical considerations remain, necessitating continued research to refine safety profiles and ethical frameworks.

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Recent Therapeutic Gene Editing Applications to Genetic Disorders

Deneault

2024

CIMB

Self Cite

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Transcriptional dysregulation and impaired neuronal activity inFMR1knock-out and Fragile X patients’ iPSC-derived models

Cited by 1 publication

References 55 publications

Recent Therapeutic Gene Editing Applications to Genetic Disorders

Recent Therapeutic Gene Editing Applications to Genetic Disorders

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