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直击播散性转移瘤:溶瘤病毒的全身递送

Striking out at disseminated metastases: the systemic delivery of oncolytic viruses.

作者信息

Fisher Kerry

机构信息

Department of Clinical Pharmacology, University of Oxford, Woodstock Road, Oxford OX2 6HE, UK.

出版信息

Curr Opin Mol Ther. 2006 Aug;8(4):301-13.

Abstract

Oncolytic viruses are capable of selective replication in malignant cells and therefore offer levels of potency and specificity that are potentially far higher than conventional treatments for cancer. New developments in vector design and administration regimes are gradually moving toward systemic applications, with the ultimate aim of treating common cancer indications that present with multiple disseminated metastases. Nevertheless, the delivery of therapeutic quantities of viruses via the blood stream to target cells in humans or stringent animal models remains a challenging task: the relatively large size of virus particles restricts their penetration into tissues, and defines their biodistribution and clearance kinetics. In addition, multiple interactions with blood cells and serum proteins can impact on vector bioavailability. Finally, the immunological response to virus administration can vary considerably from patient to patient and even more so between species, making it difficult to draw accurate clinical predictions from model systems. Unfortunately, the extensive experience gained from the application of low-molecular-weight therapeutic drugs provides little insight into the behavior of viral therapeutics administered into the blood stream. In this review, the fate of virus particles following intravenous delivery is described, followed by an assessment of the latest approaches to control and improve vector delivery.

摘要

溶瘤病毒能够在恶性细胞中进行选择性复制,因此其效力和特异性水平可能远高于传统癌症治疗方法。载体设计和给药方案的新进展正逐渐朝着全身应用发展,最终目标是治疗出现多处播散性转移的常见癌症适应症。然而,通过血流将治疗量的病毒递送至人类或严格的动物模型中的靶细胞仍然是一项具有挑战性的任务:病毒颗粒相对较大的尺寸限制了它们渗透到组织中,并决定了它们的生物分布和清除动力学。此外,与血细胞和血清蛋白的多种相互作用会影响载体的生物利用度。最后,对病毒给药的免疫反应在患者之间可能有很大差异,在不同物种之间差异更大,这使得很难从模型系统中得出准确的临床预测。不幸的是,从应用低分子量治疗药物中获得的丰富经验对注入血流的病毒治疗剂的行为几乎没有提供什么见解。在这篇综述中,描述了静脉给药后病毒颗粒的命运,随后评估了控制和改善载体递送的最新方法。

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