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D-青霉胺诱导小鼠腭裂

D-penicillamine-induced cleft palate in mice.

作者信息

Myint B

出版信息

Teratology. 1984 Dec;30(3):333-40. doi: 10.1002/tera.1420300305.

Abstract

The teratogenic potential of the lathyrogen, D-penicillamine (DP), was assessed in pregnant mice, especially with respect to its ability to produce cleft palate. The dosage and the duration of treatment as they relate to the induction of cleft palate were also studied. Two different doses of DP were administered orally for either 5 or 4 consecutive days during the critical period of palatal closure. D-penicillamine (DP) at a dose level which does not have any apparent maternal toxic effects produced cleft palate in the offspring, and this teratogenic effect depended more upon the duration of treatment than the dosage administered. Inhibitory effects on the formation of bone matrix were observed at the base of the palatal shelf. It is suggested that DP is potentially an osteolathyrogenic agent. The mechanism of induction of cleft palate in DP-treated mice was explored by histological studies using light microscopy. Delayed elevation of the palatal shelves was observed and is considered to be the cause of the induction of cleft palate. No other external malformations could be detected in DP-treated fetuses.

摘要

致畸物质D-青霉胺(DP)对怀孕小鼠的致畸潜力进行了评估,尤其关注其导致腭裂的能力。还研究了与腭裂诱导相关的治疗剂量和持续时间。在腭部闭合的关键时期,连续5天或4天口服两种不同剂量的DP。剂量水平的D-青霉胺(DP)对母体没有任何明显的毒性作用,但却导致了后代腭裂,而且这种致畸作用更多地取决于治疗持续时间而非给药剂量。在腭架底部观察到对骨基质形成的抑制作用。提示DP可能是一种致骨畸形剂。通过光学显微镜组织学研究探索了DP处理小鼠中腭裂诱导的机制。观察到腭架延迟抬高,这被认为是腭裂诱导的原因。在DP处理的胎儿中未检测到其他外部畸形。

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