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重组 SV40 在严重遗传性高胆红素血症 Ugt1a1-/- 小鼠中疗效低。

Low efficacy of recombinant SV40 in Ugt1a1-/- mice with severe inherited hyperbilirubinemia.

机构信息

Amsterdam UMC, Tytgat Institute for Liver and Intestinal Research, AGEM, University of Amsterdam, Amsterdam, The Netherlands.

International Centre for Genetic Engineering and Biotechnology, Trieste, Italy.

出版信息

PLoS One. 2021 Apr 23;16(4):e0250605. doi: 10.1371/journal.pone.0250605. eCollection 2021.

Abstract

In contrast to AAV, Simian Virus 40 (rSV40) not inducing neutralizing antibodies (NAbs) allowing re-treatment seems a promising vector for neonatal treatment of inherited liver disorders. Several studies have reported efficacy of rSV40 in animal models for inherited liver diseases. In all studies the ubiquitous endogenous early promoter controlled transgene expression establishing expression in all transduced tissues. Restricting this expression to the target tissues reduces the risk of immune response to the therapeutic gene. In this study a liver specific rSV40 vector was generated by inserting a hepatocyte specific promoter. This increased the specificity of the expression of hUGT1A1 in vitro. However, in vivo the efficacy of rSV40 appeared too low to demonstrate tissue specificity while increasing the vector dose was not possible because of toxicity. In contrast to earlier studies, neutralizing antibodies were induced. Overall, the lack of a platform to produce high titered and pure rSV40 particles and the induction of NAbs, renders it a poor candidate for in vivo gene therapy.

摘要

与 AAV 相反,猴病毒 40(rSV40)不会诱导中和抗体(NAb),似乎允许重新治疗,是治疗新生儿遗传性肝脏疾病的有前途的载体。几项研究报道了 rSV40 在遗传性肝脏疾病动物模型中的疗效。在所有研究中,普遍存在的内源性早期启动子控制转基因表达,在所有转导的组织中建立表达。将这种表达限制在靶组织中可以降低对治疗基因的免疫反应的风险。在这项研究中,通过插入肝细胞特异性启动子,生成了一种肝脏特异性 rSV40 载体。这增加了 hUGT1A1 在体外表达的特异性。然而,体内 rSV40 的疗效似乎太低,无法证明组织特异性,而增加载体剂量由于毒性而不可能。与早期研究不同,诱导了中和抗体。总的来说,缺乏生产高滴度和纯 rSV40 颗粒的平台以及中和抗体的诱导,使得它成为体内基因治疗的不良候选者。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/730a/8064607/6bed1802343f/pone.0250605.g001.jpg

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