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包膜靶向逆转录病毒载体可转导黑色素瘤异种移植物,但不能转导脾脏或肝脏。

Envelope-targeted retrovirus vectors transduce melanoma xenografts but not spleen or liver.

作者信息

Martín Francisco, Chowdhury Simon, Neil Stuart, Phillipps Neil, Collins Mary K

机构信息

Department of Immunology and Molecular Pathology, Windeyer Institute of Medical Science, University College London, 46 Cleveland Street, London W1P 6DB, UK.

出版信息

Mol Ther. 2002 Mar;5(3):269-74. doi: 10.1006/mthe.2002.0550.

Abstract

Many cancer gene therapy applications would benefit from the development of targeted vectors that could deliver genes in vivo. We have previously achieved efficient in vitro targeting of retrovirus vectors to melanoma cells by fusion of a single chain antibody recognizing the high-molecular-weight melanoma-associated antigen (HMWMAA), followed by a blocking peptide and a matrix metalloprotease cleavage site, to the amino terminus of the murine leukemia virus amphotropic strain envelope. Here we report that up to 3% of cells within an HMWMAA-positive tumor xenograft were infected following a single injection of targeted vector into the tumor and up to 10% of tumor cells became infected when they were co-injected with viral producer cells. No infected cells were detected after delivery of targeted vectors to HMWMAA-negative tumor xenografts. Intraperitoneal injection of amphotropic vectors or producer cells resulted in transduction in spleen and liver, which was not detected when targeted vectors or producer cells were used. Our results demonstrate the feasibility of using targeted retroviral vectors for in vivo gene delivery to tumors and highlight the safety benefits of targeted vectors that do not infect other host tissues.

摘要

许多癌症基因治疗应用将受益于能够在体内递送基因的靶向载体的开发。我们之前通过将识别高分子量黑色素瘤相关抗原(HMWMAA)的单链抗体与一个阻断肽和一个基质金属蛋白酶切割位点融合到鼠白血病病毒嗜异性株包膜的氨基末端,实现了逆转录病毒载体在体外对黑色素瘤细胞的高效靶向。在此我们报告,在将靶向载体单次注射到肿瘤内后,HMWMAA阳性肿瘤异种移植物中高达3%的细胞被感染,当它们与病毒生产细胞共同注射时,高达10%的肿瘤细胞被感染。将靶向载体递送至HMWMAA阴性肿瘤异种移植物后未检测到感染细胞。腹腔注射嗜异性载体或生产细胞会导致脾脏和肝脏中的转导,而使用靶向载体或生产细胞时未检测到这种情况。我们的结果证明了使用靶向逆转录病毒载体在体内向肿瘤递送基因的可行性,并突出了不感染其他宿主组织的靶向载体的安全性优势。

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