首页> 外文期刊>Toxicological sciences: An official journal of the Society of Toxicology >Assessment of the safety and biodistribution of a regulated AAV2 gene transfer vector after delivery to murine submandibular glands.
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Assessment of the safety and biodistribution of a regulated AAV2 gene transfer vector after delivery to murine submandibular glands.

机译:评估后的AAV2基因转移载体的安全性和生物分布到鼠下颌下腺。

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摘要

Clinical gene transfer holds promise for the treatment of many inherited and acquired disorders. A key consideration for all clinical gene transfer applications is the tight control of transgene expression. We have examined the safety and biodistribution of a serotype 2, recombinant adeno-associated viral (AAV2) vector that encodes a rapamycin-responsive chimeric transcription factor, which regulates the expression of a therapeutic transgene (human erythropoietin [hEpo]). The vector, AAV2-TF2.3w-hEpo (2.5 x 10(7)-2.5 x 10(10) particles), was administered once to a single submandibular gland of male and female mice and mediated hEpo expression in vivo following a rapamycin injection but not in its absence. Control (saline treated) and vector-treated animals maintained their weight, and consumed food and water, similarly. Vector delivery led to no significant toxicological effects as judged by hematology, clinical chemistry, and gross and microscopic pathology evaluations. On day 3 after vector delivery, vector copies were not only abundant in the targeted right submandibular gland but also detected in multiple other tissues. Vector was cleared from the targeted gland much more rapidly in female mice than in male mice. Overall, our results are consistent with the notion that administration of the AAV2-TF2.3w-hEpo vector to salivary glands posed no significant risk in mice.
机译:临床基因转移有望用于治疗许多遗传性和后天性疾病。所有临床基因转移应用的关键考虑因素是转基因表达的严格控制。我们已经检查了血清型2,重组腺相关病毒(AAV2)载体的安全性和生物分布,该载体编码雷帕霉素响应性嵌合转录因子,该因子调节治疗性转基因(人促红细胞生成素[hEpo])的表达。将载体AAV2-TF2.3w-hEpo(2.5 x 10(7)-2.5 x 10(10)颗粒)一次给予雄性和雌性小鼠的单个下颌下腺,并在雷帕霉素注射后体内介导hEpo表达但不是在没有它的情况下。对照(经盐水处理)和经载体处理的动物保持体重,并消耗食物和水。如通过血液学,临床化学以及总体和微观病理学评估所判断的,载体的递送不会导致明显的毒理作用。在载体递送后的第3天,载体拷贝不仅在靶向的右下颌下腺中丰富,而且在多个其他组织中也检测到。与雄性小鼠相比,雌性小鼠从靶腺中清除载体的速度要快得多。总体而言,我们的结果与以下观点一致:将AAV2-TF2.3w-hEpo载体施用至唾液腺不会对小鼠造成明显的风险。

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