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In vivo gene editing via homology-independent targeted integration for adrenoleukodystrophy treatment.


ABSTRACT: Adrenoleukodystrophy (ALD) is caused by various pathogenic mutations in the X-linked ABCD1 gene, which lead to metabolically abnormal accumulations of very long-chain fatty acids in many organs. However, curative treatment of ALD has not yet been achieved. To treat ALD, we applied two different gene-editing strategies, base editing and homology-independent targeted integration (HITI), in ALD patient-derived fibroblasts. Next, we performed in vivo HITI-mediated gene editing using AAV9 vectors delivered via intravenous administration in the ALD model mice. We found that the ABCD1 mRNA level was significantly increased in HITI-treated mice, and the plasma levels of C24:0-LysoPC (lysophosphatidylcholine) and C26:0-LysoPC, sensitive diagnostic markers for ALD, were significantly reduced. These results suggest that HITI-mediated mutant gene rescue could be a promising therapeutic strategy for human ALD treatment.

SUBMITTER: Hong SA 

PROVIDER: S-EPMC8753287 | biostudies-literature | 2022 Jan

REPOSITORIES: biostudies-literature

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In vivo gene editing via homology-independent targeted integration for adrenoleukodystrophy treatment.

Hong Sung-Ah SA   Seo Jung Hwa JH   Wi Soohyun S   Jung Eul Sik ES   Yu Jihyeon J   Hwang Gue-Ho GH   Yu Ji Hea JH   Baek Ahreum A   Park Soeon S   Bae Sangsu S   Cho Sung-Rae SR  

Molecular therapy : the journal of the American Society of Gene Therapy 20210529 1


Adrenoleukodystrophy (ALD) is caused by various pathogenic mutations in the X-linked ABCD1 gene, which lead to metabolically abnormal accumulations of very long-chain fatty acids in many organs. However, curative treatment of ALD has not yet been achieved. To treat ALD, we applied two different gene-editing strategies, base editing and homology-independent targeted integration (HITI), in ALD patient-derived fibroblasts. Next, we performed in vivo HITI-mediated gene editing using AAV9 vectors del  ...[more]

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