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用降脂过氧化物酶体增殖剂萘酚平治疗的无过氧化氢酶小鼠中的肝细胞癌。

Hepatocellular carcinomas in acatalasemic mice treated with nafenopin, a hypolipidemic peroxisome proliferator.

作者信息

Reddy J K, Rao S, Moody D E

出版信息

Cancer Res. 1976 Apr;36(4):1211-7.

PMID:177202
Abstract

The effects of long-term administration of nafenopin, a potent hypolipidemic drug with marked hepatomegalic and peroxisome-proliferative properties, were studied in wild-type (Csa strain) and acatalasemic (Csb strain) mice. Nafenopin was administered in the diet at a concentration of 0.1% during the first 12 months and then at 0.05% until the termination of the experiment at 20 months. By 56 weeks, 100% mortality occurred in both male and female wild-type mice, whereas the mortality rate in acatalasemic mice was approximately 50%. Between 18 and 20 months of the experiment, 9 of 9 male and 12 of 12 female acatalasemic mice that survived chronic nafenopin treatment developed hepatocellular carcinomas, some of which metastasized to the lungs. None of the 15 male and 15 female acatalasemic controls developed liver cancers. Numerous peroxisomes were seen in the lung metastases of these hepatocellular carcinomas on electron microscopic examination; in contrast the number of peroxisomes in primary liver tumor cells varied considerably. The hepatocarcinogenicity of nafenopin strongly suggests the need for long-term studies with other hypolipidemic drugs that cause hepatomegaly and peroxisome proliferation to clarify the role, if any, of peroxisome proliferation in liver carcinogenesis.

摘要

在野生型(Csa品系)和无过氧化氢酶血症型(Csb品系)小鼠中研究了强效降血脂药物萘苯丁酸的长期给药效果。萘苯丁酸以0.1%的浓度添加到饲料中,在实验的前12个月给药,然后以0.05%的浓度给药至20个月实验结束。到56周时,雄性和雌性野生型小鼠的死亡率均为100%,而无过氧化氢酶血症型小鼠的死亡率约为50%。在实验的18至20个月期间,9只雄性和12只雌性经萘苯丁酸长期治疗存活下来的无过氧化氢酶血症型小鼠发生了肝细胞癌,其中一些转移到了肺部。15只雄性和15只雌性无过氧化氢酶血症型对照小鼠均未发生肝癌。电子显微镜检查发现,这些肝细胞癌的肺转移灶中有大量过氧化物酶体;相比之下,原发性肝肿瘤细胞中的过氧化物酶体数量差异很大。萘苯丁酸的致癌性强烈表明,有必要对其他导致肝肿大和过氧化物酶体增殖的降血脂药物进行长期研究,以阐明过氧化物酶体增殖在肝癌发生中的作用(如果有作用的话)。

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