在临床前研究中，伊马替尼在临床相关浓度下不会引起心脏毒性。

Imatinib does not induce cardiotoxicity at clinically relevant concentrations in preclinical studies.

机构信息

Preclinical Safety, Novartis Institutes for Biomedical Research, CH-4009 Basel, Switzerland.

出版信息

Leuk Res. 2010 Sep;34(9):1180-8. doi: 10.1016/j.leukres.2010.01.004. Epub 2010 Jan 31.

DOI:10.1016/j.leukres.2010.01.004

PMID:20122731

Abstract

Cytotoxic concentrations of imatinib mesylate (10-50 microM) were required to trigger markers of apoptosis and endoplasmic reticulum stress response in neonatal rat ventricular myocytes and fibroblasts, with no significant differences observed between c-Abl silenced and nonsilenced cells. In mice, oral or intraperitoneal imatinib treatment did not induce cardiovascular pathology or heart failure. In rats, high doses of oral imatinib did result in some cardiac hypertrophy. Multi-organ toxicities may have increased the cardiac workload and contributed to the cardiac hypertrophy observed in rats only. These data suggest that imatinib is not cardiotoxic at clinically relevant concentrations (5 microM).

摘要

甲磺酸伊马替尼的细胞毒性浓度（10-50μM）需要在新生大鼠心室肌细胞和成纤维细胞中引发细胞凋亡和内质网应激反应的标志物，而在沉默和非沉默细胞之间未观察到显著差异。在小鼠中，口服或腹腔内给予伊马替尼治疗不会引起心血管病理或心力衰竭。在大鼠中，高剂量的口服伊马替尼确实导致一些心脏肥大。多器官毒性可能增加了心脏的工作量，并导致仅在大鼠中观察到的心脏肥大。这些数据表明，在临床相关浓度（5μM）下，伊马替尼无心脏毒性。

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在临床前研究中，伊马替尼在临床相关浓度下不会引起心脏毒性。

Imatinib does not induce cardiotoxicity at clinically relevant concentrations in preclinical studies.

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