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抗肿瘤铂化合物对范可尼贫血的细胞遗传学毒性。

Cytogenetic toxicity of antitumor platinum compounds in Fanconi's anemia.

作者信息

Poll E H, Arwert F, Joenje H, Eriksson A W

出版信息

Hum Genet. 1982;61(3):228-30. doi: 10.1007/BF00296447.

Abstract

Peripheral blood lymphocytes of patients with Fanconi's anemia (FA) were tested for their susceptibility to chromosome breakage by cis-platinum(II)-diamminedichloride [cis-Pt(II)], cis-platinum(IV)diamminetetrachloride [cis-Pt(IV)], and trans-platinum(IV)diamminetetrachloride [trans-Pt(IV)]. Low doses (0.1 microgram/ml) of the DNA-DNA cross-linking agents cis-Pt(II) and cis-Pt(IV) dramatically increased the chromosome breakage level in FA cultures without affecting the controls. The predominantly DNA-protein cross-linking compound trans-Pt(IV), however, was much less effective in producing chromosomal damage in FA. The differential response of FA cells to cis-Pt(IV) and trans-Pt(IV) suggests that the high susceptibility of FA to bifunctional cross-linking agents is due to an impairment of the cells to tolerate DNA-DNA cross-links, rather than DNA-protein cross-links.

摘要

对范科尼贫血(FA)患者的外周血淋巴细胞进行检测,以评估其对顺铂(II)-二氨二氯铂[顺铂(II)]、顺铂(IV)-二氨四氯铂[顺铂(IV)]和反铂(IV)-二氨四氯铂[反铂(IV)]诱导染色体断裂的敏感性。低剂量(0.1微克/毫升)的DNA-DNA交联剂顺铂(II)和顺铂(IV)显著提高了FA培养物中的染色体断裂水平,而对对照无影响。然而,主要为DNA-蛋白质交联化合物的反铂(IV)在FA中产生染色体损伤的效果要差得多。FA细胞对顺铂(IV)和反铂(IV)的不同反应表明,FA对双功能交联剂的高敏感性是由于细胞耐受DNA-DNA交联而非DNA-蛋白质交联的能力受损。

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