Cloning and characterization of hamster fetal retinoic acid receptor isoforms

Raghubir P. Sharma, Royal A. McGraw, Raviprakash R. Dugyala
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Abstract

Hamsters are routinely employed in toxicology evaluation, particularly for investigating the teratologic potential of chemicals. We have employed Syrian golden hamsters in retinoid-induced teratogenesis, mechanisms of which involve various retinoic acid receptor (RAR) isoforms. The purpose of this study was to clone and characterize different full-length hamster RAR isoforms. A 12-day old fetal hamster cDNA library was constructed and screened for RAR isoforms using human or mouse probes. Three full-length clones representing RARα, β, and γ were isolated, amplified and sequenced, and based on their homology to known mammalian isoforms were termed as hamster RARα variant, RARβ2 and RARγ2, respectively. The respective translated products for these clones were 430, 448 and 406 amino acids long. The clones were homologous to their human or mouse counterparts, although differences, particularly in the N-terminal region, were observed. These differences may represent differential splicing of exons controlled by two promoters for each isoform.

仓鼠胎儿维甲酸受体异构体的克隆与鉴定
仓鼠通常用于毒理学评估,特别是用于调查化学品的致畸潜力。我们使用叙利亚金仓鼠进行类视黄酸诱导的致畸,其机制涉及多种视黄酸受体(RAR)亚型。本研究的目的是克隆和表征不同的全长仓鼠RAR亚型。构建12日龄胎鼠cDNA文库,利用人或小鼠探针筛选RAR异构体。对代表RARα、β和γ的3个全长克隆进行分离、扩增和测序,根据其与已知哺乳动物同种型的同源性,分别命名为仓鼠RARα变体、RARβ2和RARγ2。这些克隆的翻译产物长度分别为430、448和406个氨基酸。这些克隆与人类或小鼠的克隆是同源的,尽管存在差异,特别是在n端区域。这些差异可能代表每个异构体由两个启动子控制的外显子的不同剪接。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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