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在持续输注甲氨蝶呤期间,药物浓度和暴露持续时间对小鼠骨髓毒性的相对贡献。

The relative contribution of drug concentration and duration of exposure to mouse bone marrow toxicity during continuous methotrexate infusion.

作者信息

Pinedo H M, Zaharko D S, Bull J, Chabner B A

出版信息

Cancer Res. 1977 Feb;37(2):445-50.

PMID:832268
Abstract

The effects of exposure of bone marrow to specific methotrexate (MTX) concentrations were studied by constant infusion of the drug into C57BL mice. The residual marrow nucleated cell count was determined in 168 mice at specific intervals. In vitro culture of colony-forming cells (CFU-C) was also performed in 69 of these mice. Duration of exposure varied from 12 to 72 hr. Plateau plasma MTX concentrations were studied in the range from 10(-8) to 10(-5) M. The total number of nucleated cells per femur fell to a nadir of 30% of control for all drug concentrations studied. The nadir was reached earliest with the highest drug concentrations. The percentage of CFU-C per 7.5 X 10(4) nucleated cells plated increased after 48-hr infusions compared to the percentage after 24-hr infusions. This increase was seen at all plasma concentrations studied. The total number of CFU-C per femur at plasma MTX concentrations above 10(-6) M decreased in the first 24 hr to 40% of control, but then the number significantly increased to 66% of control between 24 and 48 hr. In contrast, no change was observed in CFU-C per femur between 24 and 48 hr during constant infusion at plasma concentrations below 10(-6) M. Wright's-stained smears showed no change in the differential count of marrow specimens at 24 and 48 hr that might account for the increased percentage of CFU-C at 48 hr. The increase in CFU-C per femur during high-dose infusions is probably the result of recruitment of CFU-C. The increased percentage of CFU-C suggests recruitment at the lower concentrations as well, but selective elimination of non-CFU-C cells cannot be excluded. Marrow [6-3]deoxyrudine incorporation studies in vivo during exposure to 10(-7) M MTX showed that the phenomenon of recruitment observed in vitro was initiated during the absence of DNA synthesis in vivo.

摘要

通过向C57BL小鼠持续输注甲氨蝶呤(MTX),研究了骨髓暴露于特定浓度MTX的影响。在特定时间间隔测定了168只小鼠的残余骨髓有核细胞计数。还对其中69只小鼠进行了集落形成细胞(CFU-C)的体外培养。暴露时间从12小时到72小时不等。研究了血浆MTX浓度在10^(-8)至10^(-5) M范围内的平台期血浆MTX浓度。对于所有研究的药物浓度,每根股骨的有核细胞总数降至对照值的30%的最低点。药物浓度越高,最低点出现得越早。与24小时输注后的百分比相比,48小时输注后每7.5×10^4个接种有核细胞中CFU-C的百分比增加。在所有研究的血浆浓度下均观察到这种增加。血浆MTX浓度高于10^(-6) M时,每根股骨的CFU-C总数在最初24小时内降至对照值的40%,但在24至48小时之间显著增加至对照值的66%。相比之下,在血浆浓度低于10^(-6) M的持续输注过程中,24至48小时内每根股骨的CFU-C未观察到变化。瑞氏染色涂片显示,在24小时和48小时时骨髓标本的分类计数没有变化,这可能解释了48小时时CFU-C百分比的增加。高剂量输注期间每根股骨CFU-C的增加可能是CFU-C募集的结果。CFU-C百分比的增加也表明在较低浓度下存在募集,但不能排除非CFU-C细胞的选择性消除。在暴露于10^(-7) M MTX期间进行的体内骨髓[6-3]脱氧核苷掺入研究表明,体外观察到的募集现象是在体内无DNA合成期间开始的。

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