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干扰素和嘌呤霉素对烷化剂磷嘌呤所致人淋巴细胞细胞遗传学损伤的修饰作用。

Modifying effects of interferon and puromycin on cytogenetic damage induced by alkylating drug phopurine in human lymphocytes.

作者信息

Lazutka J R, Jarmalaitè S, Lekevicius R

机构信息

Ecological Genetics Laboratory, Vilnius University, Lithuania, USSR.

出版信息

Acta Biol Hung. 1990;41(1-3):137-48.

PMID:1709768
Abstract

The induction of sister chromatid exchanges (SCEs) by the bifunctional alkylating antineoplastic drug phopurine (2-dimethyl-amino-6-diethyleneiminophosphamido-7-methylpurine) and its modification by human recombinant interferons alpha 2, beta and gamma (HuIFN alpha 2, HuIFN beta and HuIFN gamma) and puromycin (PM) were studied in human lymphocytes. Results demonstrated a striking similarity in the modifying action of HuIFN alpha 2 and PM: 1) both modifiers reduced SCE values induced by phopurine, 2) at high and low doses of phopurine the effect of both modifiers was minimal, and 3) both agents were able to convert DNA lesions from short-term to long-term.

摘要

在人淋巴细胞中研究了双功能烷化抗肿瘤药物磷嘌呤(2-二甲基氨基-6-二乙烯亚氨基磷酰胺基-7-甲基嘌呤)诱导的姐妹染色单体交换(SCEs),以及人重组干扰素α2、β和γ(HuIFNα2、HuIFNβ和HuIFNγ)和嘌呤霉素(PM)对其的修饰作用。结果表明,HuIFNα2和PM的修饰作用具有显著相似性:1)两种修饰剂均降低了磷嘌呤诱导的SCE值;2)在高剂量和低剂量磷嘌呤条件下,两种修饰剂的作用最小;3)两种药物均能够将DNA损伤从短期转变为长期。

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