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使用阳离子化明胶偶联的HVJ包膜载体对腹腔播散性结肠癌进行靶向化疗。

Targeted chemotherapy against intraperitoneally disseminated colon carcinoma using a cationized gelatin-conjugated HVJ envelope vector.

作者信息

Mima Hidetoshi, Yamamoto Seiji, Ito Makoto, Tomoshige Ryuji, Tabata Yasuhiko, Tamai Katsuto, Kaneda Yasufumi

机构信息

Division of Gene Therapy Science, Graduate School of Medicine, Osaka University, 2-2 Yamada-oka, Suita, Osaka 565-0871, Japan.

出版信息

Mol Cancer Ther. 2006 Apr;5(4):1021-8. doi: 10.1158/1535-7163.MCT-05-0352.

Abstract

The hemagglutinating virus of Japan envelope (HVJ-E; Sendai virus) vector derived from inactivated HVJ particles can be used to deliver DNA, proteins, and drugs into cells both in vitro and in vivo. HVJ-E is capable of delivering bleomycin, an anticancer drug, to various cancer cell lines, thereby producing 300-fold greater cytotoxicity than administration of bleomycin alone. In a mouse model of peritoneally disseminated colon cancer, we injected HVJ-E containing the luciferase gene into the peritoneum. Unexpectedly, luciferase gene expression was not observed within the tumor deposits or any organs. However, when combined with cationized gelatin (CG), CG-HVJ-E produced a high level of luciferase gene expression primarily within the tumor deposits. Forty-eight hours after introducing colon cancer cells into the peritoneum of experimental mice, CG-HVJ-E with or without bleomycin was injected into the abdominal cavity. Following six injections of bleomycin-incorporated CG-HVJ-E, complete responses were observed in 40% of the mice examined. All of the mice that received either empty CG-HVJ-E or bleomycin alone died within 40 days of having cancer cells introduced into the peritoneum. When the mice with complete responses were rechallenged with colon cancer cells from the same cell line, no tumors developed. Thus, CG-HVJ-E may suppress peritoneal dissemination of cancer.

摘要

源自灭活日本血凝病毒颗粒的日本血凝病毒包膜(HVJ-E;仙台病毒)载体可用于在体外和体内将DNA、蛋白质和药物递送至细胞。HVJ-E能够将抗癌药物博来霉素递送至各种癌细胞系,从而产生比单独施用博来霉素大300倍的细胞毒性。在腹膜播散性结肠癌小鼠模型中,我们将含有荧光素酶基因的HVJ-E注入腹膜。出乎意料的是,在肿瘤沉积物或任何器官内均未观察到荧光素酶基因表达。然而,当与阳离子化明胶(CG)结合时,CG-HVJ-E主要在肿瘤沉积物内产生高水平的荧光素酶基因表达。将结肠癌细胞引入实验小鼠腹膜48小时后,将含或不含博来霉素的CG-HVJ-E注入腹腔。在六次注射掺入博来霉素的CG-HVJ-E后,在40%接受检查的小鼠中观察到完全缓解。所有接受空CG-HVJ-E或单独博来霉素治疗的小鼠在将癌细胞引入腹膜后40天内死亡。当对具有完全缓解的小鼠用来自同一细胞系的结肠癌细胞进行再次攻击时,未出现肿瘤。因此,CG-HVJ-E可能抑制癌症的腹膜播散。

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