1.Therapeautic effect of hepatic arterial infusion of cisplatin in primary hepatocelluar carcinoma.
Jae Yong CHO ; Jin Hyuk CHOI ; Nae Choon YOO ; Ho Young LIM ; Joo Hang KIM ; Jae Kyung ROH ; Jong Tae LEE ; Byung Soo KIM
Journal of the Korean Cancer Association 1993;25(6):865-872
No abstract available.
Cisplatin*
2.Study on acute and subchronic toxicity of cisplatin synthesized in Vietnam on the hemopoietic system
Pharmaceutical Journal 2005;0(5):16-19
Experimentation of using Cisplatin produced by Vietnam with dose of LD50=26.00 (23.21-29.12) mg/kg on injection line on peritoneum of white house-mice was monitored for a week, and the 100% mice died. Before the death, the mice often had some kinds of epilepsy. It was proved that this medicine affected on central nervous system. In terms of semi-chronic toxicity, Cisplatin with dose of 0.2mg/kg/24 hours of intravenous injections 5 days per course, with dose of 0.3mg/kg/24 hours of intravenous injection in 5 days, using two courses after 10 days changed some indexes of hematology and microscopic findings of bone marrow. After 15 days to 30 days of discontinuous injection, injuries gradually recovered
Cisplatin
;
Cisplatin/toxicity
4.The effect of moderate dose cisplatin infusion on hearing.
Jung Ho KIM ; Kang Pyo HONG ; Kwon Hyung LEE ; Yun Joon KIM ; Byung Don LEE ; Hyuck Soon CHAGN ; Ju Won KANG
Korean Journal of Otolaryngology - Head and Neck Surgery 1993;36(6):1186-1193
No abstract available.
Cisplatin*
;
Hearing*
5.Study on semi-chronic toxicity of cisplatin DLTW 1 on liver and kineys
Pharmaceutical Journal 2005;0(7):23-26
Cisplatin was intravenously injected at the dose of 0.2 mg/kg (equivalent to 1/10 of the maximum non-toxicating dose in mice) four 5-day episodes with the interval of 5 days caused a slight increase in the serum creatinine and urea levels. Similar effects were also observed when cisplatin was IV administered at 0.3 mg/kg/24h for two 5-day episodes with the interval of 10 days. Other mild side effects towards liver and some organs were also observed in about 50% of the mice population. Most of the side effects significantly subdued in both groups 15 days after stopping drug, except damages in hepatic histology, which recovered more slowly
Cisplatin
;
Cisplatin/toxicity
;
Liver
;
Kidney
6.Efficacy of ONDANSETRON(GR38032F) for the control of cisplatin induced nausea and vomiting in patients with advanced malignancies.
Jae Kyung ROH ; Nae Chun YOO ; Jin Hyuk CHOI ; Hyun Cheol CHUNG ; Ho Young LIM ; Eun Hee KOH ; Joo Hang KIM ; Byung Soo KIM
Journal of the Korean Cancer Association 1991;23(4):814-820
No abstract available.
Cisplatin*
;
Humans
;
Nausea*
;
Vomiting*
7.A Case of Capecitabine and Cisplatin-induced Cutaneous Hyperpigmentation.
Sang Hyeon HWANG ; Ji Hye PARK ; Chong Won CHOI ; Ga Young LEE ; Won Serk KIM
Korean Journal of Dermatology 2014;52(3):210-212
No abstract available.
Cisplatin
;
Hyperpigmentation*
;
Capecitabine
8.Phase II trial of VP-16 plus cisplatin for advanced epithelial ovarian cancer.
Young Iee PARK ; Tae Yoo KIM ; Kyung Hae JUNG ; Sung Hyun YANG ; Jung Ae LEE ; Dae Suk HUH ; Young Joo BANG ; No Kyung KIM
Journal of the Korean Cancer Association 1993;25(4):539-547
No abstract available.
Cisplatin*
;
Etoposide*
;
Ovarian Neoplasms*
9.Radiation Recall Dermatitis after Treatment with Paclitaxel and Cisplatin.
Seung Woo BAEK ; Young Joon SEO ; Jun Sang KIM ; Hyo Jin LEE
Annals of Dermatology 2012;24(2):223-224
No abstract available.
Cisplatin
;
Paclitaxel
;
Radiodermatitis
10.The Effects of Glutathione on Human Cancer Cells before and after the Application of Cisplatin.
Young Shin CHO ; Hyoung Gyun ROH ; Tae Gyu AHN ; Sei Jun HAN
Korean Journal of Obstetrics and Gynecology 2004;47(1):161-165
OBJECTIVE: The purpose of this study is to determine the time-dependant effects of Glutathione on the Cisplatin-induced cytotoxicity of human cervical carcinoma cells. METHODS: Two human cervical carcinoma cells, SiHa (squamous cell carcinoma cell), and CaSki (epidermoid metastatic carcinoma cell) were cultivated with RPMI1640 media. Reduced glutathione (GSH) and 2-oxo 4-thiazolidine carboxylic acid (OTC) were added one hour before and after Cisplatin (2-50 micro M/ml) was applied. The cells were incubated an additional 24 hours and viable cells were examined using a 3-[4,5- dimethylthiazol-2-yl]-2,5-diphenyl tetrazolium bromide (MTT) assay. RESULTS: The MTT reduction rate of cisplatin-treated cervical carcinoma cells was increased significantly by the addition of glutathione (5 mM) or OTC (5 mM) both one hour before and after Cisplatin. A difference between MTT reduction rates one hour before and after cisplatin were not observed in either GSH or OTC. CONCLUSION: These results suggest that GSH and OTC have a protective effect on cisplatin-induced toxicity, and that this effect is about the same whether the agents were applied before or after the Cisplatin.
Cisplatin*
;
Glutathione*
;
Humans*
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