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环磷酰胺和4-酮环磷酰胺对小鼠肢体发育的影响。

Influence of cyclophosphamide and 4-ketocyclophosphamide on mouse limb development.

作者信息

Manson J M, Smith C C

出版信息

Teratology. 1977 Jun;15(3):291-9. doi: 10.1002/tera.1420150311.

Abstract

Many studies have been performed on the in vivo teratogenicity of cyclophosphamide, and there is uncertainty whether the parent compound or P-450 generated alkylating metabolite(s) is the proximal teratogen(s). We have examined the influence of cyclophosphamide and a metabolite, 4-ketocyclophosphamide, on mouse limb development. Pregnant mice were injected with 10, 15 or 20 mg/kg of cyclophosphamide on days 9 to 11 of gestation. Hindlimb buds were maximally sensitive to 20 mg/kg of cyclophosphamide at 9 A.M. on day 11, and the predominant malformations formed were preaxial ectrodactyly and hemimelia. Hindlimb buds of the same gestational age exposed to cyclophosphamide in vitro responded identically to controls in morphology and uptake of 3H-thymidine and 35SO4. Exposure to 4-ketocyclophosphamide in culture, however, resulted in the formation of limbs with a "hemimelic" appearance and distal limb reduction, and with reduced uptake of 3H-thymidine and 35SO4. These findings support the position that the P-450 generated metabolite(s), and not the parent compound, is the proximal teratogen(s).

摘要

已经对环磷酰胺的体内致畸性进行了许多研究,对于母体化合物或细胞色素P-450生成的烷基化代谢物是否是近端致畸原存在不确定性。我们研究了环磷酰胺及其代谢物4-酮环磷酰胺对小鼠肢体发育的影响。在妊娠第9至11天,给怀孕小鼠注射10、15或20mg/kg的环磷酰胺。后肢芽在妊娠第11天上午9点对20mg/kg的环磷酰胺最为敏感,形成的主要畸形是轴前缺指(趾)畸形和半肢畸形。在体外暴露于环磷酰胺的相同胎龄的后肢芽在形态以及3H-胸腺嘧啶核苷和35SO4的摄取方面与对照的反应相同。然而,在培养物中暴露于4-酮环磷酰胺会导致形成具有“半肢”外观和远端肢体发育不全的肢体,并且3H-胸腺嘧啶核苷和35SO4的摄取减少。这些发现支持了细胞色素P-450生成的代谢物而非母体化合物是近端致畸原的观点。

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