Journal
ADVANCED MATERIALS
Volume 33, Issue 41, Pages -Publisher
WILEY-V C H VERLAG GMBH
DOI: 10.1002/adma.202103307
Keywords
fluorination; Idebenone; in situ mitochondrial gene therapy; Leber's hereditary optic neuropathy; pathologically responsive polymers
Categories
Funding
- National Natural Science Foundation of China [82020108029, 81773667, 82073398, 82003670]
- Priority Academic Program Development of Jiangsu Higher Education Institutions
- Project of State Key Laboratory of Natural Medicines, China Pharmaceutical University [SKLNMZZ202021]
- 111 Project from the Ministry of Education of China
- State Administration of Foreign Experts Affairs of China [B16046]
- Project of State Key Laboratory of Pathogenesis, Double First-class University Projects [CPU2018GY06]
- Natural Science Foundation of Jiangsu Province [BK20190566]
- Key Research and Development Program of Jiangsu Province [BE2018742]
- Jiangsu Postgraduate Research and Innovation Program [KYCX20_0625]
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Leber's hereditary optic neuropathy (LHON) is a rare inherited blindness caused by mutations in mitochondrial DNA. The traditional chemotherapeutic agent Idebenone only alleviates symptoms, and in situ mitochondrial gene therapy is challenging. A novel pathologically responsive mitochondrial gene delivery vector named TISUH has been developed, showing promising potential for LHON treatment by targeting diseased mitochondria and releasing functional genes for correcting genetic abnormalities.
Leber's hereditary optic neuropathy (LHON) is a rare inherited blindness caused by mutations in the mitochondrial DNA (mtDNA). The disorder is untreatable and tricky, as the existing chemotherapeutic agent Idebenone alleviates symptoms rather than overcoming the underlying cause. Although some studies have made progress on allotopic expression for LHON, in situ mitochondrial gene therapy remains challenging, which may simplify delivery procedures to be a promising therapeutic for LHON. LHON becomes more difficult to manage in the changed mitochondrial microenvironment, including increasing reactive oxygen species (ROS) and decreasing mitochondrial membrane potential (MMP). Herein, a pathologically responsive mitochondrial gene delivery vector named [triphenylphosphine-terminated poly(sulfur-containing thioketal undecafluorohexylamine histamine) and Ide-terminated poly(sulfur-containing thioketal undecafluorohexylamine histamine)] (TISUH) is reported to facilitate commendable in situ mitochondrial gene therapy for LHON. TISUH directly targets diseased mitochondria via triphenylphosphine and fluorination addressing the decreasing MMP. In addition, TISUH can be disassembled by high mitochondrial ROS levels to release functional genes for enhancing gene transfection efficiency and fundamentally correcting genetic abnormalities. In both traditional and gene-mutation-induced LHON mouse models, TISUH-mediated gene therapy shows satisfactory curative effect through the sustained therapeutic protein expression in vivo. This work proposes a novel pathologically responsive in situ mitochondrial delivery platform and provides a promising approach for refractory LHON as well as other mtDNA mutated diseases treatments.
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