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接触长春瑞滨可抑制膀胱移行细胞癌的体外增殖和侵袭能力。

Exposure to vinorelbine inhibits in vitro proliferation and invasiveness of transitional cell bladder carcinoma.

作者信息

Bonfil R D, Russo D M, Schmilovich A J

机构信息

Laboratory of Fundación de Investigación del Cáncer at CEFYBO, Buenos Aires, Argentina.

出版信息

J Urol. 1996 Aug;156(2 Pt 1):517-21. doi: 10.1097/00005392-199608000-00074.

DOI:10.1097/00005392-199608000-00074
PMID:8683728
Abstract

PURPOSE

To study the effect of vinorelbine (VNR) on in vitro cell proliferation, invasiveness, cell adhesion to substrate, cell motility and metalloproteinase secretion of MB-49, a murine transitional cell carcinoma of the bladder (TCC).

MATERIALS AND METHODS

The colorimetric MTS assay, which depends upon viable versus nonviable mitochondria, was used to evaluate the effect of graded concentrations of VNR on in vitro MB-49 cell growth. Chemoinvasion and cell motility were studied in TCC cells exposed for 24 hours to a noncytotoxic dose of VNR, through their ability to migrate across Matrigel-coated or Type IV collagen-coated 8-microns. pore filters. Zymographic studies in gelatin-embedded polyacrylamide gels were done to investigate gelatinolytic activity in conditioned media from treated and untreated MB-49 cells.

RESULTS

Vinorelbine inhibited MB-49 cell growth in a dose-dependent manner (IC(50)40 ng./ml.). In vitro cell invasive capacity of MB-49 cells pretreated for 24 hours with VNR at noncytotoxic doses (1 and 10 ng./ml.) was significantly lower than that of untreated cells. The decreased invasion of VNR-treated cells was not accompanied by a diminished adhesion to Matrigel or type IV collagen nor by a significant reduced secretion of gelatinolytic metalloproteinases. Instead, motility of MB-49 cells exposed to noncytotoxic concentrations of VNR was inhibited in a dose-response fashion similar to that of invasion.

CONCLUSION

Vinorelbine proved to be an effective drug to inhibit tumor cell growth and invasion in a transitional cell bladder carcinoma model. The results obtained would justify preclinical studies to evaluate the effectiveness of VNR as a potential treatment of TCC.

摘要

目的

研究长春瑞滨(VNR)对小鼠膀胱移行细胞癌(TCC)MB - 49细胞体外增殖、侵袭、细胞与底物黏附、细胞运动及金属蛋白酶分泌的影响。

材料与方法

采用依赖于活细胞与死细胞线粒体的比色MTS法,评估不同浓度VNR对体外MB - 49细胞生长的影响。通过将TCC细胞暴露于非细胞毒性剂量的VNR 24小时后,研究其穿过基质胶包被或IV型胶原包被的8微米孔径滤膜的迁移能力,以此来研究化学侵袭和细胞运动。在明胶包埋的聚丙烯酰胺凝胶中进行酶谱分析,以研究处理和未处理的MB - 49细胞条件培养基中的明胶酶活性。

结果

长春瑞滨以剂量依赖性方式抑制MB - 49细胞生长(IC50为40 ng/ml)。在非细胞毒性剂量(1和10 ng/ml)下用VNR预处理24小时的MB - 49细胞的体外细胞侵袭能力显著低于未处理细胞。VNR处理细胞侵袭能力的降低并非伴随着对基质胶或IV型胶原黏附的减少,也不是明胶酶解金属蛋白酶分泌的显著减少。相反,暴露于非细胞毒性浓度VNR的MB - 49细胞的运动能力以与侵袭相似的剂量反应方式受到抑制。

结论

在膀胱移行细胞癌模型中,长春瑞滨被证明是一种抑制肿瘤细胞生长和侵袭的有效药物。所获得的结果可为评估VNR作为TCC潜在治疗方法的有效性的临床前研究提供依据。

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