以肝脏内皮细胞为靶点的 GP64 伪型慢病毒载体可矫正 A 型血友病小鼠。

IF 9 1区 医学 Q1 MEDICINE, RESEARCH & EXPERIMENTAL EMBO Molecular Medicine Pub Date : 2024-06-01 Epub Date: 2024-04-29 DOI:10.1038/s44321-024-00072-8
Michela Milani, Cesare Canepari, Simone Assanelli, Simone Merlin, Ester Borroni, Francesco Starinieri, Mauro Biffi, Fabio Russo, Anna Fabiano, Desirèe Zambroni, Andrea Annoni, Luigi Naldini, Antonia Follenzi, Alessio Cantore
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引用次数: 0

摘要

慢病毒载体(LV)是向肝脏体内传递基因的高效载体。LV 整合到靶细胞的染色质中,可确保其在增殖过程中传输,因此一次给药后就可能实现终身基因治疗,即使是年轻人也不例外。水泡性口炎病毒(VSV.G)的糖蛋白被广泛用于伪造 LV,因为它具有广泛的滋养性和高稳定性。有人建议将来源于杆状病毒的 GP64 包膜蛋白作为体内肝脏定向基因治疗的替代品。在这里,我们对 VSV.G 型和 GP64 伪型 LV 在体外和体内进行了详细比较。我们发现 VSV.G-LV 对肝细胞的转导效果优于 GP64-LV,但后者对肝窦状内皮细胞(LSEC)的转导效果更好。将 GP64 伪分型与表面高含量的吞噬抑制剂 CD47 相结合,可进一步增强 LSEC 的转导能力。凝血因子 VIII(FVIII)是 A 型血友病的变异基因,可在 LSEC 中自然表达,因此我们利用 GP64-LV 在内源性 FVIII 启动子的控制下递送 FVIII 转基因,获得了治疗量的 FVIII 并矫正了 A 型血友病小鼠。
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GP64-pseudotyped lentiviral vectors target liver endothelial cells and correct hemophilia A mice.

Lentiviral vectors (LV) are efficient vehicles for in vivo gene delivery to the liver. LV integration into the chromatin of target cells ensures their transmission upon proliferation, thus allowing potentially life-long gene therapy following a single administration, even to young individuals. The glycoprotein of the vesicular stomatitis virus (VSV.G) is widely used to pseudotype LV, as it confers broad tropism and high stability. The baculovirus-derived GP64 envelope protein has been proposed as an alternative for in vivo liver-directed gene therapy. Here, we perform a detailed comparison of VSV.G- and GP64-pseudotyped LV in vitro and in vivo. We report that VSV.G-LV transduced hepatocytes better than GP64-LV, however the latter showed improved transduction of liver sinusoidal endothelial cells (LSEC). Combining GP64-pseudotyping with the high surface content of the phagocytosis inhibitor CD47 further enhanced LSEC transduction. Coagulation factor VIII (FVIII), the gene mutated in hemophilia A, is naturally expressed by LSEC, thus we exploited GP64-LV to deliver a FVIII transgene under the control of the endogenous FVIII promoter and achieved therapeutic amounts of FVIII and correction of hemophilia A mice.

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来源期刊
EMBO Molecular Medicine
EMBO Molecular Medicine 医学-医学:研究与实验
CiteScore
17.70
自引率
0.90%
发文量
105
审稿时长
4-8 weeks
期刊介绍: EMBO Molecular Medicine is an open access journal in the field of experimental medicine, dedicated to science at the interface between clinical research and basic life sciences. In addition to human data, we welcome original studies performed in cells and/or animals provided they demonstrate human disease relevance. To enhance and better specify our commitment to precision medicine, we have expanded the scope of EMM and call for contributions in the following fields: Environmental health and medicine, in particular studies in the field of environmental medicine in its functional and mechanistic aspects (exposome studies, toxicology, biomarkers, modeling, and intervention). Clinical studies and case reports - Human clinical studies providing decisive clues how to control a given disease (epidemiological, pathophysiological, therapeutic, and vaccine studies). Case reports supporting hypothesis-driven research on the disease. Biomedical technologies - Studies that present innovative materials, tools, devices, and technologies with direct translational potential and applicability (imaging technologies, drug delivery systems, tissue engineering, and AI)
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