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Review
. 2020;20(2):100-108.
doi: 10.2174/1566523220666200806111451.

NF1, Neurofibromin and Gene Therapy: Prospects of Next-Generation Therapy

Affiliations
Review

NF1, Neurofibromin and Gene Therapy: Prospects of Next-Generation Therapy

Xi-Wei Cui et al. Curr Gene Ther. 2020.

Abstract

Neurofibromatosis type 1 [NF1] is an autosomal dominant genetic disorder affecting multiple organs. NF1 is well known for its various clinical manifestations, including café-au-late macules, Lisch nodules, bone deformity and neurofibromas. However, there is no effective therapy for NF1. Current therapies are aimed at alleviating NF1 clinical symptoms but not curing the disease. By altering pathogenic genes, gene therapy regulates cell activities at the nucleotide level. In this review, we described the structure and functions of neurofibromin domains, including GAP-related domain [GRD], cysteine-serine rich domain [CSRD], leucine-rich domain [LRD] and C-terminal domain [CTD], which respectively alter downstream pathways. By transfecting isolated sequences of these domains, researchers can partially restore normal cell functions in neurofibroma cell lines. Furthermore, recombinant transgene sequences may be designed to encode truncated proteins, which is functional and easy to be packaged into viral vectors. In addition, the treatment effect of gene therapy is also determined by various factors such as the vectors selection, transgene packaging strategies and drug administration. We summarized multiple NF1 gene therapy strategies and discussed their feasibility from multiple angles. Different protein domains alter the function and downstream pathways of neurofibromin.

Keywords: Gene therapy; adeno associated virus vector; malignant peripheral nerve sheath tumor; neurofibromatosis type 1; neurofibromin; plexiform neurofibroma.

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