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Evaluation of toxicity from high-dose systemic administration of recombinant adenovirus vector in vector-naive and pre-immunized mice.

机译:大剂量全身给药重组腺病毒载体对初免载体和预免疫小鼠的毒性评估。

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摘要

Toxicity associated with in vivo administration of adenovirus (Ad) vectors has been linked to activation of both innate and adaptive immune responses. Pre-existing immunity to the prevalent Ad serotypes, acquired by the majority of the human population as a result of natural infections, has the potential to modulate vector efficacy and safety. Previously, we evaluated some aspects of toxicity from systemic Ad vector in vector-naive and pre-immunized rhesus monkeys. In this report, we summarize data from several studies analyzing toxic effects from systemically administered E1/E3-deleted Ad vector in vector-naive and pre-immunized C57BL/6 mice. Our results indicate that pre-immunization can be associated with increased mortality shortly after systemic administration of Ad. Transient leukopenia and thrombocytopenia were observed early post vector infusion in both vector-naive and pre-immunized animals. Pre-exposure to the vector did not prevent induction of pro-inflammatory cytokines; however, pre-immunized mice showed less tissue toxicity. Growth of bone marrow myeloid and erythroid progenitors was transiently inhibited in pre-immunized animals, but only the myeloid progenitors were affected in vector-naive animals. In summary, pre-existing immunity to Ad vector substantially modifies host immune responses to systemic Ad vector.
机译:与体内施用腺病毒(Ad)载体相关的毒性已经与先天免疫和适应性免疫应答的激活相关。大多数人由于自然感染而获得的对流行的Ad血清型的已有免疫力有可能调节载体的功效和安全性。以前,我们评估了在纯载体和预先免疫的恒河猴中全身性Ad载体毒性的某些方面。在本报告中,我们总结了几项研究的数据,这些研究分析了从系统给药的E1 / E3缺失的Ad载体在纯载体和预先免疫的C57BL / 6小鼠中的毒性作用。我们的结果表明,免疫接种可能与全身性施用Ad后不久的死亡率增加有关。在初次接种载体和免疫前的动物中,在载体输注后早期观察到短暂性白细胞减少症和血小板减少症。预先暴露于载体不能阻止促炎细胞因子的诱导。但是,预先免疫的小鼠组织毒性较小。在免疫前的动物中,骨髓髓样和红系祖细胞的生长被短暂抑制,但在单纯载体的动物中仅骨髓祖细胞受到影响。总之,预先存在的对Ad载体的免疫力实质上改变了宿主对全身性Ad载体的免疫反应。

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