• Asian Pacific Journal of Cancer Prevention
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• 제15권8호
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• pp.3651-3657
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• 2014

Hepatocellular carcinoma (HCC) has a relatively higher incidence in many countries of Asia. Globally, HCC has a high fatality rate and short survival. Epirubicin, a doxorubicin analogue, may be administered alone or in combination with other agents to treat primary liver cancer and metastatic diseases. However, the toxic effects of epirubicin to normal tissues and cells have been one of the major obstacles to successful cancer chemotherapy. Here, we investigated the effects of epirubicin in combination with kappa-selenocarrageenan on mice with H22 implanted tumors and HepG-2 cell proliferation, immune organ index, morphology, cell cycle and related protein expressions in vivo and in vitro with sequential drug exposure. The inhibitory rate of tumor growth in vivo was calculated. Drug sensitivity was measured by MTT assay, and the King's principle was used to evaluate the interaction of drug combination. Morphological changes were observed by fluorescent microscopy. Cell cycle changes were analyzed by flow cytometry. Expression of cyclin A, Cdc25A and Cdk2 were detected by Western blotting. In vivo results demonstrated that the inhibitory rate of EPI combined with KSC was higher than that of KSC or EPI alone, and the Q value indicated an additive effect. In addition, KSC could significantly raise the thymus and spleen indices of mice with H22 implanted tumors. In the drug sensitivity assay in vitro, exposure to KSC and EPI simultaneously was more effective than exposure sequentially in HepG-2 cells, while exposure to KSC prior to EPI was more effective than exposure to EPI prior to KSC. Q values showed an additive effect in the simultaneous group and antagonistic effects in the sequential groups. Morphological analysis showed similar results to the drug sensitivity assay. Cell cycle analysis revealed that exposure to KSC or EPI alone arrested the cells in S phase in HepG-2 cells, exposure to KSC and EPI simultaneously caused accumulation in the S phase, an effect caused by either KSC or EPI. Expression of cyclin A, Cdc25A and Cdk2 protein was down-regulated following exposure to KSC and EPI alone or in combination, exposure to KSC and EPI simultaneously resulting in the lowest values. Taken together, our findings suggest that KSC in combination with EPI might have potential as a new therapeutic regimen against HCC.

• Radiation Oncology Journal
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• 제11권2호
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• pp.311-319
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• 1993

본 국립의료원 치료 방사선과 에서는 1986년 1월부터 1990년 12월까지 5년간 방사선 치료를 받은 III병기 비소세포성 폐암 37예를 대상으로 후향성 조사를 통하여 임상적 특징과 생존율을 분석하여 보고하는 바이다. 이중 29예가 사망시 또는 1991년 8월까지 추적 관찰이 가능하였으며 치료후 추적 조사기간은 최소10개월, 최고60개월 이었고, 추적율은 $78.4\%$이었다. Kaplan-Meier법에 따른 전체 환자 37예의 2, 5년 생존율은 각각 $20.6\%,\;6.9\%$이었으며 중앙생존 기간은 10개월 이었다. Performance status에 의하면 KPS가 $80\%$ 이상인 I군의 2,5년 생존율과 중앙생존기간은 각각 $29.2\%,\;9.7\%,$ 13개월 이었고, KPS가 $80\%$ 이하인 II군의 2년 생존율과 중앙 생존기간은 $13.7\%$와 7개월 로서, 통계학적으로 유의 한 차이를 보였다(p<0.05). AJCC 병기에 따른 생존율 및 중앙 생존기 간을 보면 $III_a$ 병기의 2, 5년 생존율 및 중앙 생존기간이 $29.2\%,9.7\%$및 12개월 이었고 $III_b$ 병기의 2년 생존율과 중앙 생존기간은 $8.6\%$와 10개월로 생존율의 유의한 차이를 보이지 않았다(p>0.1). 그외 조직 병리학적 유형별, 방사선 선량별, 방사선 반응군별, 항암화학요법 유무에 따른 생존율은 유의한 차이를 보이지 않았다. 결론적으로 overall 5년 생존율 및 중앙 생존기간은 $6.7\%$와 10개월 이었고 performance status 만이 통계적으로유의한 예후인자였으며, 병리조직학적 유형, 병기, 방사선 치료선량, 방사선 반응유무와 항암화학요법 등의 예후인자들은 통계학적으로 유의하지 않았다.