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转移性结肠癌中与异质性相关的抗癌治疗反应差异:基于肿瘤部位的个性化癌症治疗新线索。

Heterogeneity-related anticancer therapy response differences in metastatic colon carcinoma: new hints to tumor-site-based personalized cancer therapy.

作者信息

Pan Weihuo, Huang Shuru, Zhang Jianwei, Zhao Bo, Wang Haohao, Liu Fanlong, Jin Ketao, Mou Xiaozhou

出版信息

Hepatogastroenterology. 2013 Nov-Dec;60(128):1927-34.

Abstract

BACKGROUND/AIMS: Heterogeneity in primary tumor and related metastases may result in different response to anticancer therapy. Previous work revealed that there were heterogeneity in primary colon carcinoma and matched lymphatic and hepatic metastases. Whether such heterogeneity in primary colon carcinoma and corresponding lymphatic and hepatic metastases would result in different response to anticancer therapy is unknown.

METHODOLOGY

To investigate whether the heterogeneity in primary colon carcinoma and matched lymphatic and hepatic metastases would result in different response to anticancer therapy, patient-derived tumor tissue (PDTT) xenograft models of colon carcinoma with lymphatic and hepatic metastases were used to evaluate the response to VEGF-targeted therapy (bevacizumab) in combination with chemotherapy (capecitabine).

RESULTS

All xenografts of primary colon carcinoma and corresponding lymphatic and hepatic metastases in nude mice responded to VEGF-targeted therapy in combination with chemotherapy. However, chemotherapy alone resulted in significantly higher tumor growth inhibition rate in xenogfafts of primary colon carcinoma than that of corresponding lymphatic and hepatic metastasis (p < 0.01). VEGF-targeted therapy in combination with chemotherapy resulted in significantly higher tumor growth inhibition rate in xenogfafts of colon carcinoma lymphatic metastasis than that of corresponding primary colon carcinoma and hepatic metastasis (p < 0.001).

CONCLUSIONS

Our results demonstrate that primary colon carcinoma and its corresponding lymphatic and hepatic metastases have different response rate to chemotherapy and to VEGF-targeted therapy in combination with chemotherapy. This study provides us new hints to tumor-site-based personalized cancer therapy in metastatic colon carcinoma.

摘要

背景/目的:原发性肿瘤及其相关转移灶的异质性可能导致对抗癌治疗产生不同反应。先前的研究表明,原发性结肠癌及其匹配的淋巴和肝转移灶存在异质性。原发性结肠癌及其相应的淋巴和肝转移灶的这种异质性是否会导致对抗癌治疗产生不同反应尚不清楚。

方法

为了研究原发性结肠癌及其匹配的淋巴和肝转移灶的异质性是否会导致对抗癌治疗产生不同反应,使用具有淋巴和肝转移的结肠癌患者来源的肿瘤组织(PDTT)异种移植模型来评估抗血管生成因子靶向治疗(贝伐单抗)联合化疗(卡培他滨)的反应。

结果

裸鼠体内原发性结肠癌及其相应的淋巴和肝转移灶的所有异种移植瘤均对血管生成因子靶向治疗联合化疗有反应。然而,单独化疗导致原发性结肠癌异种移植瘤的肿瘤生长抑制率显著高于相应的淋巴和肝转移灶(p<0.01)。血管生成因子靶向治疗联合化疗导致结肠癌淋巴转移异种移植瘤的肿瘤生长抑制率显著高于相应的原发性结肠癌和肝转移灶(p<0.001)。

结论

我们的结果表明,原发性结肠癌及其相应的淋巴和肝转移灶对化疗以及对血管生成因子靶向治疗联合化疗有不同的反应率。本研究为转移性结肠癌基于肿瘤部位的个性化癌症治疗提供了新的线索。

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