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The Preventive Effect of Dexrazoxane and Pentoxifylline on Adriamycin Induced Cardiomyopathy

Korean Journal of Pediatrics 2005;48(12):1378-1384.
Published online December 15, 2005.
The Preventive Effect of Dexrazoxane and Pentoxifylline on Adriamycin Induced Cardiomyopathy
Ling Zhu1, Eun-Jung Bae1, Il-Soo Ha1, Jung-Wook Seo2, Chung-Il Noh1, Jung-Yun Choi1, Yong-Soo Yun1
1Department of Pediatrics, Seoul National University College of Medicine, Seoul, Korea
2Department of Pathology, Seoul National University College of Medicine, Seoul, Korea
Dexrazoxane과 Pentoxifylline의 Adriamycin 유발성심근증에 대한 예방 효과
주령1, 배은정1, 하일수1, 서정욱2, 노정일1, 최정연1, 윤용수1
1서울대학교 의과대학 소아과학교실
2서울대학교 의과대학 병리학교실
Correspondence: 
Eun-Jung Bae, Email: eunjbae@plaza.snu.ac.kr
Abstract
Purpose
: We hypothesized dexrazoxane(DXR) and pentoxifylline(PTX) may prevent myocardial damage in adriamycin(ADR)-induced cardiomyopathic rat model. We also investigated their effects on the myocardial apoptosis and fibrosis in ADR induced cardiomyopathy.
Methods
: The six-week old female Spregue-Dawley rats were divided into control group(CNT, n= 4), ADR group(n=6), ADR+DXR group(DXR, n=5), ADR+PTX group(PTX, n=6), ADR+DXR+PTX group(DXPT, n=5). ADR(5 mg/week, twice) was administrated intravenously to rats except CNT group to induce cardiomyopathy. The PTX(50 mg/kg/day) was administered daily from day-0 to Day-21. The DXR(100 mg/kg) was administered 30 minutes before each ADR injection. On day 21, the rats were sacrificed and the degree of histopathologic changes of hypercontraction band necrosis, cytoplasmic vacuolar change and fibrosis were scored. Immunohistochemical staining for Bcl-2 expression and RT-PCR for TNF-α and CTGF were performed.
Results
: Histopathological scores of myocardial damage were significantly higher in ADR rats than CNT rats(P<0.05), and significantly lower in DXPT rats than ADR rats(P<0.01). Myocardial fibrosis was prevented in both PTX rats and DXPT rats. The expression of Bcl-2 was weaker in ADR rats than that in CNT rats(P<0.05), and stronger in both DXR and DXPT rats than that in ADR rats (P<0.05). TNF-α concentration of ADR rats was not different from that of treated groups.
Conclusion
: DXR prevented myocyte apoptosis with increased Bcl-2 expression, and PTX prevented myocardial fibrosis in ADR induced cardiomyopathic rats. The combination therapy of DXR and PTX showed prevention of cardiomyopathy in ADR induced cardiomyopathy rat model.
Key Words: Adriamycin , Cardiomyopathy , Dexrazoxane , Pentoxifylline , Fibrosis


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