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静脉注射RMP-7可增加更昔洛韦向大鼠脑肿瘤的递送,并增强单纯疱疹病毒胸苷激酶基因治疗的效果。

Intravenous RMP-7 increases delivery of ganciclovir into rat brain tumors and enhances the effects of herpes simplex virus thymidine kinase gene therapy.

作者信息

LeMay D R, Kittaka M, Gordon E M, Gray B, Stins M F, McComb J G, Jovanovic S, Tabrizi P, Weiss M H, Bartus R, Anderson W F, Zlokovic B V

机构信息

Department of Neurological Surgery, Childrens Hospital of Los Angeles, The University of Southern California School of Medicine, 90033, USA.

出版信息

Hum Gene Ther. 1998 May 1;9(7):989-95. doi: 10.1089/hum.1998.9.7-989.

DOI:10.1089/hum.1998.9.7-989
PMID:9607410
Abstract

Herpes simplex virus thymidine kinase (HSV-tk) gene therapy for brain tumors depends on ganciclovir (GCV) and its transport across the blood-brain tumor barrier (BBTB). We examined whether RMP-7, the bradykinin analog and potent BBTB permeabilizer, could enhance the efficacy of GCV treatment of brain tumors by increasing the BBTB delivery of GCV. In vitro, a significant bystander cytocidal effect of GCV was shown in mixed HSV-tk-transduced (HSV-tk+) and control vector-transduced (HSV-tk-) C6 glioma cultures. A dose-dependent cytotoxic effect of GCV on untransformed C6 cells was also shown. In vivo, rats with 100% HSV-tk+ or 100% HSV-tk- intracerebral C6 gliomas were treated for 7 days with intravenous infusions of GCV alone or with GCV and RMP-7 (2.5 microg/kg/day). The growth of HSV-tk+ and HSV-tk- gliomas decreased with increasing doses of GCV. A high dosage (100 mg of GCV/kg/day) eradicated all HSV-tk- and HSV-tk+ tumors. An intermediate dosage (5 mg of GCV/kg/day) reduced the growth of HSV-tk- gliomas by 42% if given alone, and by 88% in combination with RMP-7. A low dosage (0.5 mg of GCV/kg/day) in combination with RMP-7 enhanced the regression of HSV-tk+ gliomas by 87% compared with GCV alone. Low-dose GCV was ineffective in HSV-tk- tumors. RMP-7 increased [3H] GCV tumoral uptake by 2.6- and 1.7-fold in the tumor center and periphery, respectively. We conclude that RMP-7 could be an important adjunctive treatment for suicide gene therapy of brain tumors, while an RMP-7/GCV combination may also have a significant antitumor effect in untransfected gliomas.

摘要

单纯疱疹病毒胸苷激酶(HSV - tk)基因疗法治疗脑肿瘤依赖于更昔洛韦(GCV)及其穿越血脑肿瘤屏障(BBTB)的转运。我们研究了缓激肽类似物且强效的BBTB通透剂RMP - 7是否能通过增加GCV向BBTB的递送,来增强GCV治疗脑肿瘤的疗效。在体外,在混合的经HSV - tk转导(HSV - tk +)和对照载体转导(HSV - tk -)的C6胶质瘤培养物中,显示出GCV显著的旁观者杀细胞效应。还显示出GCV对未转化的C6细胞有剂量依赖性细胞毒性作用。在体内,对患有100% HSV - tk +或100% HSV - tk -脑内C6胶质瘤的大鼠,单独静脉输注GCV或联合GCV和RMP - 7(2.5微克/千克/天)治疗7天。随着GCV剂量增加,HSV - tk +和HSV - tk -胶质瘤的生长均减缓。高剂量(100毫克GCV/千克/天)可根除所有HSV - tk -和HSV - tk +肿瘤。中等剂量(5毫克GCV/千克/天)单独使用时可使HSV - tk -胶质瘤的生长减少42%,与RMP - 7联合使用时减少88%。低剂量(0.5毫克GCV/千克/天)与RMP - 7联合使用时,与单独使用GCV相比,HSV - tk +胶质瘤的消退增强了87%。低剂量GCV对HSV - tk -肿瘤无效。RMP - 7使肿瘤中心和周边的[3H] GCV肿瘤摄取分别增加2.6倍和1.7倍。我们得出结论,RMP - 7可能是脑肿瘤自杀基因疗法的重要辅助治疗手段,而RMP - 7/GCV联合疗法在未转染的胶质瘤中可能也有显著的抗肿瘤作用。

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