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构建发育缺陷的生物剂量反应模型的过程。

Process of building biologically based dose-response models for developmental defects.

作者信息

Gaylor D W, Razzaghi M

机构信息

National Center for Toxicological Research, U.S. Food and Drug Administration, Jefferson, Arkansas 72079.

出版信息

Teratology. 1992 Dec;46(6):573-81. doi: 10.1002/tera.1420460607.

Abstract

The problem of developing biologically-based dose-response models is addressed for predicting the prevalence of birth defects at low doses of toxic chemicals administered during pregnancy. To illustrate the process of incorporating biological information, a model is postulated to predict the prevalence of cleft palate for a chemical that reduces embryonic/fetal growth, which results in inadequate palatal cells for closure. Experimental bioassay data examining the prevalence of cleft palate in mice exposed to the herbicide 2,4,5-T are used to illustrate the process. With the limited data available, it is necessary to assume a model for cell growth and the relationship between the cell growth rate parameter and dose of 2,4,5-T. Also, a relationship between cleft palate prevalence and growth is assumed and then checked with experimental data. The purpose of the paper is not to provide a universal biologically based dose-response model for cleft palate, but rather to demonstrate the extent, and type of information and data required. It remains to be seen if the form of the model is appropriate for chemicals that primarily produce embryo/fetal malformations or death via reduced or delayed cellular growth.

摘要

针对预测孕期接触低剂量有毒化学物质时出生缺陷的发生率这一问题,探讨了基于生物学的剂量反应模型的开发。为说明纳入生物学信息的过程,假定了一个模型来预测一种会降低胚胎/胎儿生长的化学物质导致腭裂的发生率,这种化学物质会导致用于腭部闭合的细胞数量不足。通过检测接触除草剂2,4,5-T的小鼠中腭裂发生率的实验生物测定数据来说明这一过程。鉴于可用数据有限,有必要假定一个细胞生长模型以及细胞生长速率参数与2,4,5-T剂量之间的关系。此外,假定腭裂发生率与生长之间的关系,然后用实验数据进行检验。本文的目的不是为腭裂提供一个通用的基于生物学的剂量反应模型,而是展示所需信息和数据的范围及类型。该模型的形式是否适用于主要通过细胞生长减少或延迟而导致胚胎/胎儿畸形或死亡的化学物质,还有待观察。

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