• Applied Biological Chemistry
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• 제34권2호
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• pp.86-93
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• 1991

CDDP는 $100\;{\mu}M$ 이하의 농도에서 BTV 캡시드 단백질에 crosslink를 형성하지 않는다. 밀도구배초원심분리 결과에 의하면 캡시드 단백질과 RNA사이의 crosslink도 일어나지 않는다. CDDP를 처리한 BTV RNA를 폴리아크릴아마이드 겔에 전기연동하면 RNA이동 패턴이 변한다. 이 결과는 BTV core에 없는 RNA중합효소의 불활성화가 CDDP에 의한 BNA RNA의 구조변화에 의함을 가리킨다.

• 대한간호학회지
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• 제44권4호
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• pp.371-380
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• 2014

Purpose: The purpose of this study was to examine the effects of Cu/Zn SOD on reduction of hindlimb muscular atrophy induced by cisplatin in rats. Methods: Forty-two rats were assigned to three groups; control group, Cisplatin (CDDP) group and cisplatin with Cu/Zn SOD (CDDP-SOD) group. At day 35 hindlimb muscles were dissected. Food intake, activity, withdrawal threshold, muscle weight, and Type I, II fiber cross-sectional area (CSA) of dissected muscles were measured. Relative SOD activity and expression of MHC and phosphorylated Akt, ERK were measured after dissection. Results: Muscle weight and Type I, II fiber CSA of hindlimb muscles in the CDDP group were significantly less than the control group. Muscle weight and Type I, II fiber CSA of hindlimb muscles, food intake, activity, and withdrawal thresholds of the CDDP-SOD group were significantly greater than the CDDP group. There were no significant differences in relative SOD activities of hindlimb muscles between the CDDP-SOD and CDDP groups. MHC expression and phosphorylated Akt, ERK of hindlimb muscles in the CDDP-SOD group were significantly greater than the CDDP group. Conclusion: Cu/Zn SOD attenuates hindlimb muscular atrophy induced by cisplatin through increased food intake and activity. Increment of phosphorylated Akt, ERK may relate to attenuation of hindlimb muscular atrophy.

• BMB Reports
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• 제39권6호
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• pp.656-661
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• 2006

Cisplatin (CDDP) is a widely used anticancer drug, but at high dose, it can produce undesirable side effects such as hepatotoxicity. Because silymrin has been used to treat liver disorders, the protective effect of silymarin on CDDP -induced hepatotoxicity was evaluated in rats. Hepatotoxicity was determined by changes in serum alanine aminotransferase [ALT] and aspartate aminotransferase [AST], nitric oxide [NO] levels, albumin and calcium levels, and superoxide dismutase [SOD], glutathione peroxidase [GSHPx] activities, glutathione content, malondialdehyde [MDA] and nitric oxide [NO] levels in liver tissue of rats. Male albino rats were divided into four groups, 10 rats in each. In the control group, rats were injected i.p. with 0.2 ml of propylene glycol in saline 75/25 (v/v) for 5 consecutive days [Silymarin was dissolved in 0.2 ml of propylene glycol in saline 75/25 v/v]. The second group were injected with CDDP (7.5 mg /kg, I.P.), whereas animals in the third group were i.p. injected with silymarin at a dose of 100 mg/kg/day for 5 consecutive days. The Fourth group received a daily i.p. injection of silymarin (100 mg/kg/day for 5 days) 1 hr before a single i.p. injection of CDDP (7.5 mg/kg). CDDP hepatotoxicity was manifested biochemically by an increase in serum ALT and AST, elevation of MDA and NO in liver tissues as well as a decrease in GSH and the activities of antioxidant enzymes, including SOD, GSHPx in liver tissues. In addition, marked decrease in serum NO, albumin and calcium levels were observed. Serum ALT, AST, liver NO level, MDA was found to decreased in the combination group in comparison with the CDDP group. The activities of SOD, GSHPx, GSH and serum NO were lower in CDDP group than both the control and CDDP pretreated with silymarin groups. The results obtained suggested that silymarin significantly attenuated the hepatotoxicity as an indirect target of CDDP in an animal model of CDDP-induced nephrotoxicity.

• 미생물학회지
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• 제29권1호
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• pp.34-39
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• 1991

The BTV core associated transcriptase activity, assayed by acid precipitable counts, was reduced to an undetectable level after treat the core with .$100{\mu}{\M}$ CDDP. When the RNA transcripts prepared from the CDDP treated BTV core were analysed on agaroseurea gel, it was observed that the band intensity of the large size RNA was reduced while the band intensity of the small size RNA was enhanced. Northern blot analysis showed that much of the small size RNAs appeared to be prematurely terminated transcripts. These results suggest that CDDP adduction to the template RNA blocks chain elongation process of the virion bound transcriptase that is ultimately responsible for the inactivation of BTV infectivity.

• Molecules and Cells
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• 제37권9호
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• pp.699-704
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• 2014

Themetastasis-associated gene 1 (MTA1) oncogene hasbeen suggested to be involved in the regulation of cancer progression. However, there is still no direct evidence that MTA1 regulates cisplatin (CDDP) resistance, as well as cancer stem cell properties. In this study, we found that MTA1 was enriched in CNE1/CDDP cells. Knock down of MTA1 in CNE1/CDDP cells reversed CSCs properties and CDDP resistance. However, ectopic expression of MTA1 in CNE1 cells induced CSCs phenotypes and CDDP insensitivity. Interestingly, ectopic overexpression of MTA1-induced CSCs properties and CDDP resistance were reversed in CNE1 cells after inhibition of PI3K/Akt by LY294002. In addition, MTA1 expression and Akt activity in CNE1/CDDP cells was much higher than that in CNE1 cells. These results suggested that MTA1 may play a critical role in promoting CDDP resistance in NPC cells by regulatingcancer stem cell properties via thePI3K/Akt signaling pathway. Our findings suggested that MTA1 may be a potential target for overcoming CDDP resistance in NPC therapy.

• Journal of Gastric Cancer
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• 제6권3호
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• pp.139-145
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• 2006

목적: 진행성 위암환자에게 여러 종류의 항암요법이 시행되고 있으나 심각한 부작용 발현 없이 예후증진을 이룰 수 있는 약제는 아직 개발되지 않고 있다. 이처럼 표준요법의 개발이 시급한 시점에서 TS-1이 한국인 위암환자에서 어떤 항암효과 및 안정성을 보이는지 알고자 하였다. 대상 및 방법: 진행성 위암으로 진단된 78명을 대상으로 TS-1 단독 또는 TS-1/CDDP 병용요법을 시행하였다. TS-1은 $80\;mg/m^{2}/day$을 단독요법의 경우 4주 복용 및 2주 휴약을, 병용요법인 경우엔 3주 복용 및 2주 휴약을 1 cycle로 하였다. CDDP은 $60\;mg/m^{2}$ 용량으로 제8일째에 정맥 주사하였다. 결과: 수술 전 요법군과 재발 및 비근치적 수술군에서의 종양 반응률은 각각 87.5%, 및 32.4%였고, 단독요법군 28.6%, 병용요법군 48.4%였다. 재발 및 비근치적 수술군의 경우 종양의 반응률에 따른 생존율 차이는 의미 있는 차이(P=0.0016)를 보였고, 1년 생존율은 단독요법 56.1%, 병용요법 58.5%였으며 두 군간의 차이는 의미가 없었다. 전체 환자에서 치료관련 부작용 발현빈도(grade 3 이상)는 단독 및 병용요법의 경우 14.3% 및 36.8%였다. 결론: 한국인 진행성 위암환자를 대상으로 시행한 TS-1 단독 또는 CDDP와의 병용요법은 높지 않은 부작용 발현빈도와 높은 종양 반응률을 보였으며, 향후 용량 조절과 스케줄 조절을 통해 표준항암요법의 하나가 될 수 있는 가능성을 보여주었다.

• Applied Microscopy
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• 제40권3호
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• pp.133-138
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• 2010

인체 자궁암 세포 HeLa에 항암제 cisplatin (CDDP)과 산삼배양근 추출물(ETCMG)을 투여하여 세포 성장률, 형태, 전기영동에 의한 DNA fragmentation, 세포주기 분석을 통하여 apoptosis 유도를 확인하였다. ETCMG 2, 4, 6mg/mL, CDDP $4{\mu}g/mL$의 농도로 24시간 투여한 후 세포의 성장에 미치는 영향을 분석하고, ETCMG를 항암제로서 효과가 입증되어있는 CDDP와 복합투여하여 비교한 결과 apoptosis비율은 대조군에 비하여 ETCMG의 농도가 증가할수록 농도에 비례하여 현저히 증가하였고 (p<0.05), CDDP와 ETCMG를 복합투여한 경우에 ETCMG를 단독으로 투여한 경우 보다 apoptosis비율이 매우 높은것으로 나타났다(p<0.05). 세포의 형태를 도립현미경과 투과전자현미경으로 관찰한 결과, 대조군은 세포의 정상적인 형태를 유지하고 있는 반면에 CDDP와 ETCMG를 각각 처리한 암세포는 세포의 성장이 현저히 억제되었고, 염색질의 응축과 apoptotic body가 관찰되었다. 세포의 성장억제가 apoptosis에 의한 것인지를 확인하고자 DNA를 분리하여 전기영동한 결과, HeLa 세포에서 ETCMG의 농도가 증가할수록 ladder가 뚜렷이 관찰되었고, CDDP를 복합 처리한 것 역시 ETCMG의 농도에 비례하여 ladder가 선명하게 나타났다. Flow cytometry (FC)에 의한 세포주기 분석 결과, ETCMG를 농도별로 처리한 경우에 apoptosis를 나타내는 Sub-$G_1$기의 양이 농도에 비례하여 증가하였고, 항암제인 CDDP와 복합 투여한 경우에 Sub-$G_1$기 DNA양이 눈에 띠게 증가한 것으로 나타났다. 이상의 실험 결과를 종합하면, ETCMG는 인체 자궁암에서 항암효과를 가지고 있으며, 항암제 CDDP의 단독 투여보다는 ETCMG와 함께 사용하는 경우에 암 치료제로서의 상승효과가 있는 것으로 사료된다.

• Applied Biological Chemistry
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• 제33권4호
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• pp.343-348
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• 1990

CDDP를 처리한 pBR322 DNA로 형질변환된 대장균 LE392를 ampicillin이 포함된 한천평판배지위에 도말시켰다. Ampicillin을 함유하고 있는 평판배지위에 형성된 집락수는 13.3 ${\mu}M$의 CDDP를 처리한 뒤에는 검출되지 않을 정도로 감소하였다. CDDP를 처리한 pBR322 DNA는 외가닥 DNA에 특이성이 있는 S1 핵산분해호소에 의해 전달되었고 아가로즈 겔 전기영동상에서 이동 유형이 변했다. 이러한 결과에 의하면 CDDP가 pBR322 DNA에 반응하여 이증나선의 변성과 궁극적으로는 ampicillin 저항성 유전자를 불활성화시키는 구조변화를 일으키는 것 같다.

• Journal of Korean Biological Nursing Science
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• 제14권1호
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• pp.49-56
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• 2012

Purpose: The purpose of this study was to compare the effects of anorexia induced by consecutive low-dose and high-dose of cisplatin (CDDP) on the hindlimb muscles of rats. Methods: Male Sprague-Dawley rats were assigned to three groups: Control group (C) received a saline (the same dose and duration as the low CDDP group), the high-dose cisplatin (High CDDP) group received a single 5 mg/kg dose of cisplatin, the consecutive low-dose cisplatin (Low CDDP) group had 1 mg/kg of cisplatin administered for five consecutive days. On the 8th day the soleus and gastrocnemius muscles were dissected. Body weight, food intake, activity, muscle weight, Type I, II fiber cross-sectional area (CSA) of the dissected muscles were measured. Results: Body weight, food intake, muscle weight and Type I, II fiber CSA of the High CDDP and Low CDDP groups were significantly less than the C group. The High CDDP group showed significant decreases, compared to the Low CDDP group, in body weight, food intake, activity score, muscle weight and Type I, II fiber CSA. Conclusion: Hindlimb muscle atrophy occurs due to anorexia induced by both consecutive low-dose and high-dose cisplatin. The muscle atrophy induced by consecutive low-dose cisplatin is less apparent than high-dose cisplatin.

• BMB Reports
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• 제36권4호
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• pp.373-378
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• 2003

Effects of L-arginine and NG-nitro-L-arginine methyl ester (L-NAME) on the renal dysfunction that is induced by cisplatin (CDDP) were investigated. A single dose of CDDP (7.5 mg/kg i.p.) induced renotoxicity, which was manifested by increasing the sensitivity of isolated urinary bladder rings to acetylcholine (ACh), together with a significant elevation of serum urea and creatinine, and a severe decrease in serum albumin. Moreover, renal dysfunction was further confirmed by a significant decrease of enzyme activities, such as glutathione peroxidase, GSH-Px (E.C 1.11.1.9), catalase (E.C 1.11.1.6), as well as a significant increase in lipid peroxides that were measured as malondialdhyde (MDA) in kidney tissue homogenates. The administration of L-arginine (70 mg/kg/d p.o in drinking water 5 d before and 5 d after the CDDP injection) significantly ameliorated the renotoxic effects of CDDP, as judged by restoring the normal responses of isolated bladder rings to Ach, and also by an improvement in a range of renal function indices, which included serum urea and creatinine concentrations and kidney weight. In addition, L-arginine prevents the rise of MDA, as well as a reduction of GSH-Px and catalase activities in kidney tissues homogenates. On the other hand, the administration of L-NAME (4 mg/kg/d p.o) resulted in no protection against renal dysfunction that was induced by CDDP treatment. The findings of this study suggest that L-arginine can attenuate kidney injury that is produced by CDDP treatment. In addition, L-arginine may be a beneficial remedy for CDDP-induced renal toxicity, and could be used to improve the therapeutic index of CDDP.