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[使用胶原凝胶基质支持培养系统进行泌尿生殖系统肿瘤化学敏感性试验的疗效]

[Efficacy of the chemosensitivity test using collagen gel matrix-supported culture system for urogenital tumors].

作者信息

Ogihara M, Aikawa K, Ishibashi K, Irisawa C, Shiraiwa Y, Koseki K, Ishiwata H

机构信息

Department of Urology, Fukuishima Medical College, Japan.

出版信息

Nihon Hinyokika Gakkai Zasshi. 1996 Apr;87(4):740-7. doi: 10.5980/jpnjurol1989.87.740.

Abstract

BACKGROUND

We evaluated the usefulness of in vitro tumor culture system using a specialized collagen gel matrix (CGM assay) as a chemosensitivity test.

PATIENTS AND METHODS

Chemosensitivity results of CGM assay were compared with other in vivo and in vitro assays on an implantable murine bladder tumor cell line (MBT-2). In addition we investigated the possibility of the clinical use of CGM assay using clinical specimens obtained from urogenital malignant tumor patients by comparing the result with that of the other chemosensitivity test, SDI testing using single cells (conventional SDI test). Methods of CGM assay were as follows. Tumor tissues on the collagen gel matrices were incubated under the existence of anticancer drugs following 4 days preculture. Drug sensitivities were evaluated by counting the number of viable cells adjusted to the tumor weight.

RESULTS

Inhibition rates in MBT-2 were high in the order of mitomycin C, cisdiamminedichloroplatinum (II), (2"R)-4'-0-tetrahydropyranyl adriamycin. Four of 6 anticancer drugs were decided as chemosensitive drugs. These results corresponded to the results of the antitumor effects on subcutaneously transplanted MBT-2 in vivo, moreover was correlated well with those of the conventional SDI test. Twenty of 22 cases, including 11 of 13 bladder cancer cases, 1 of 3 renal cancer cases, 2 of 3 testicular cancer cases and 1 of 1 adrenal cortical cancer cases, were evaluable in the clinical study of the CGM assay. Corresponding rates between the results of the CGM assay and those of the conventional SDI test performed simultaneously in 12 cases were excellent for each anticancer drug.

CONCLUSION

This CGM assay can serve as an effective tool for chemosensitivity testing because of its convenience and high evaluable rate.

摘要

背景

我们评估了使用特殊胶原凝胶基质的体外肿瘤培养系统(CGM检测)作为化疗敏感性检测的实用性。

患者与方法

将CGM检测的化疗敏感性结果与针对可植入小鼠膀胱肿瘤细胞系(MBT - 2)的其他体内和体外检测方法进行比较。此外,我们通过将结果与另一种化疗敏感性检测方法(单细胞SDI检测,传统SDI检测)进行比较,研究了使用从泌尿生殖系统恶性肿瘤患者获得的临床标本进行CGM检测的临床应用可能性。CGM检测方法如下。胶原凝胶基质上的肿瘤组织在预培养4天后,于抗癌药物存在的情况下进行孵育。通过计算根据肿瘤重量调整后的活细胞数量来评估药物敏感性。

结果

在MBT - 2中,丝裂霉素C、顺二氨二氯铂(II)、(2“R)-4'-O - 四氢吡喃阿霉素的抑制率较高。6种抗癌药物中有4种被判定为化疗敏感药物。这些结果与对皮下移植的MBT - 2的体内抗肿瘤作用结果相符,而且与传统SDI检测结果相关性良好。在CGM检测的临床研究中,22例中有20例可评估,包括13例膀胱癌患者中的11例、3例肾癌患者中的1例、3例睾丸癌患者中的2例和1例肾上腺皮质癌患者。在12例中同时进行的CGM检测结果与传统SDI检测结果之间,每种抗癌药物的对应率都非常好。

结论

这种CGM检测因其便利性和高可评估率,可作为化疗敏感性检测的有效工具。

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