全反式和13顺式RAs在胎鼠次级腭中维甲酸(RA)受体mrna表达的改变:对RA诱导的致畸的影响。

H Naitoh, C Mori, Y Nishimura, K Shiota
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引用次数: 0

摘要

视黄酸(RA)是各种生物过程和正常胚胎发育的必需物质,但高浓度时具有致畸性。在啮齿动物中,RA引起的主要畸形之一是腭裂(CP)。RA通过RA受体(RARs)介导其作用,但RARs在发育中的腭中的表达模式尚不清楚。采用Northern blot方法研究了RAR α、β和γ信使rna (mrna)在胎鼠次级腭裂组织中的正常表达,以及全反式和13顺式RAs对RAR mrna表达的影响。RAR α(2.8、3.8 kb)、RAR β (3.3 kb)和RAR γ (3.7 kb) mrna在妊娠期(GD) 12.5-14.5时在胎儿腭部检测到。RAR α和γ mRNA的表达没有明显的顺序变化,但RAR β mRNA的表达在GD 13.5时增加。用100 mg/kg全反式RA治疗妊娠小鼠,94%的胎儿产生CP,胎儿上颚RAR β和γ mrna水平升高。全反式RA对RAR β mRNA的上调比对RAR γ mRNA的上调更为明显。用100 mg/kg 13-cis RA治疗仅19%的胎儿产生CP。13-顺式RA虽然提高了胎儿腭RAR β和γ mRNA水平,但其上调速度较全反式RA慢且不明显。这些研究结果表明,RAR β mRNA在胎儿上颚的诱导与RA治疗后全反式RA的组织浓度密切相关,RAR β可能是RA诱导致畸最具影响力的候选分子之一。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Altered expression of retinoic acid (RA) receptor mRNAs in the fetal mouse secondary palate by all-trans and 13-cis RAs: implications for RA-induced teratogenesis.

Retinoic acid (RA) is mandatory for various biological processes and normal embryonic development but is teratogenic at high concentrations. In rodents, one of the major malformations induced by RA is cleft palate (CP). RA mediates its effects by RA receptors (RARs), but the expression patterns of RARs in the developing palate are still unclear. We investigated the normal expression of RAR alpha, beta, and gamma messenger RNAs (mRNAs) in the fetal mouse secondary palate and the effects of all-trans and 13-cis RAs on the expression of RAR mRNAs by Northern blot analysis. RAR alpha (2.8, 3.8 kb), RAR beta (3.3 kb), and RAR gamma (3.7 kb) mRNAs were detected in the fetal palate on gestational days (GD) 12.5-14.5. The expression of RAR alpha and gamma mRNAs did not show apparent sequential changes, but that of RAR beta mRNA increased at GD 13.5. Treatment of pregnant mice with 100 mg/kg all-trans RA induced CP in 94% of the fetuses and elevated the levels of RAR beta and gamma mRNAs in the fetal palate. The up-regulation of RAR beta mRNA by all-trans RA was more marked than that of RAR gamma mRNA. Treatment with 100 mg/kg 13-cis RA induced CP in only 19% of the fetuses. Although 13-cis RA elevated the RAR beta and gamma mRNA levels in fetal palates, its up-regulation was slower and less marked than that induced by all-trans RA. These findings indicate that the induction of RAR beta mRNA in the fetal palate correlates well with the tissue concentration of all-trans RA after RA treatment, and RAR beta may be one of the most influential candidate molecules for RA-induced teratogenesis.

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