AAV gene replacement therapy for treating MPS IIIC: Facilitating bystander effects via EV-mRNA cargo

IF 15.5 1区 医学 Q1 CELL BIOLOGY
Tierra A. Bobo, Michael Robinson, Christopher Tofade, Marina Sokolski-Papkov, Peter Nichols, Stephen Vorobiov, Haiyan Fu
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Abstract

MPS IIIC is a lysosomal storage disease caused by mutations in heparan-α-glucosaminide N-acetyltransferase (HGSNAT), for which no treatment is available. Because HGSNAT is a trans-lysosomal-membrane protein, gene therapy for MPS IIIC needs to transduce as many cells as possible for maximal benefits. All cells continuously release extracellular vesicles (EVs) and communicate by exchanging biomolecules via EV trafficking. To address the unmet need, we developed a rAAV-hHGSNATEV vector with an EV-mRNA-packaging signal in the 3′UTR to facilitate bystander effects, and tested it in an in vitro MPS IIIC model. In human MPS IIIC cells, rAAV-hHGSNATEV enhanced HGSNAT mRNA and protein expression, EV-hHGSNAT-mRNA packaging, and cleared GAG storage. Importantly, incubation with EVs led to hHGSNAT protein expression and GAG contents clearance in recipient MPS IIIC cells. Further, rAAV-hHGSNATEV transduction led to the reduction of pathological EVs in MPS IIIC cells to normal levels, suggesting broader therapeutic benefits. These data demonstrate that incorporating the EV-mRNA-packaging signal into a rAAV-hHGSNAT vector enhances EV packaging of hHGSNAT-mRNA, which can be transported to non-transduced cells and translated into functional rHGSNAT protein, facilitating cross-correction of disease pathology. This study supports the therapeutic potential of rAAVEV for MPS IIIC, and broad diseases, without having to transduce every cell.

Abstract Image

用于治疗 MPS IIIC 的 AAV 基因替代疗法:通过 EV-mRNA 货物促进旁观者效应。
MPS IIIC 是一种溶酶体贮积病,由肝素-α-氨基葡萄糖 N-乙酰转移酶(HGSNAT)突变引起,目前尚无治疗方法。由于 HGSNAT 是一种跨溶酶体膜蛋白,因此 MPS IIIC 的基因疗法需要转导尽可能多的细胞才能获得最大疗效。所有细胞都会不断释放细胞外囊泡 (EV),并通过 EV 转运交换生物分子进行交流。为了满足这一需求,我们开发了一种 rAAV-hHGSNATEV 载体,其 3'UTR 中含有 EV-mRNA 包装信号,以促进旁观者效应,并在体外 MPS IIIC 模型中进行了测试。在人类 MPS IIIC 细胞中,rAAV-hHGSNATEV 增强了 HGSNAT mRNA 和蛋白质的表达、EV-hHGSNAT-mRNA 包装,并清除了 GAG 储存。重要的是,与 EVs 一起孵育可导致受体 MPS IIIC 细胞中 hHGSNAT 蛋白表达和 GAG 含量清除。此外,rAAV-hHGSNATEV 转导还能将 MPS IIIC 细胞中的病理性 EVs 降低到正常水平,从而带来更广泛的治疗效果。这些数据表明,在 rAAV-hHGSNAT 载体中加入 EV-mRNA 包装信号可增强 EV 对 hHGSNAT-mRNA 的包装,而 hHGSNAT-mRNA 可被转运到非转导细胞并翻译成功能性 rHGSNAT 蛋白,从而促进疾病病理的交叉矫正。这项研究证明了 rAAVEV 治疗 MPS IIIC 和其他疾病的潜力,而无需转导每个细胞。
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来源期刊
Journal of Extracellular Vesicles
Journal of Extracellular Vesicles Biochemistry, Genetics and Molecular Biology-Cell Biology
CiteScore
27.30
自引率
4.40%
发文量
115
审稿时长
12 weeks
期刊介绍: The Journal of Extracellular Vesicles is an open access research publication that focuses on extracellular vesicles, including microvesicles, exosomes, ectosomes, and apoptotic bodies. It serves as the official journal of the International Society for Extracellular Vesicles and aims to facilitate the exchange of data, ideas, and information pertaining to the chemistry, biology, and applications of extracellular vesicles. The journal covers various aspects such as the cellular and molecular mechanisms of extracellular vesicles biogenesis, technological advancements in their isolation, quantification, and characterization, the role and function of extracellular vesicles in biology, stem cell-derived extracellular vesicles and their biology, as well as the application of extracellular vesicles for pharmacological, immunological, or genetic therapies. The Journal of Extracellular Vesicles is widely recognized and indexed by numerous services, including Biological Abstracts, BIOSIS Previews, Chemical Abstracts Service (CAS), Current Contents/Life Sciences, Directory of Open Access Journals (DOAJ), Journal Citation Reports/Science Edition, Google Scholar, ProQuest Natural Science Collection, ProQuest SciTech Collection, SciTech Premium Collection, PubMed Central/PubMed, Science Citation Index Expanded, ScienceOpen, and Scopus.
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