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Qualitative De Novo Analysis of Full Length cDNA and Quantitative Analysis of Gene Expression for Common Marmoset (Callithrix jacchus) Transcriptomes Using Parallel Long-Read Technology and Short-Read Sequencing

机译:使用平行长读和短读测序技术对普通Mar猴(Callithrix jacchus)转录组进行全长cDNA的定性从头分析和基因表达的定量分析

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摘要

The common marmoset (Callithrix jacchus) is a non-human primate that could prove useful as human pharmacokinetic and biomedical research models. The cytochromes P450 (P450s) are a superfamily of enzymes that have critical roles in drug metabolism and disposition via monooxygenation of a broad range of xenobiotics; however, information on some marmoset P450s is currently limited. Therefore, identification and quantitative analysis of tissue-specific mRNA transcripts, including those of P450s and flavin-containing monooxygenases (FMO, another monooxygenase family), need to be carried out in detail before the marmoset can be used as an animal model in drug development. De novo assembly and expression analysis of marmoset transcripts were conducted with pooled liver, intestine, kidney, and brain samples from three male and three female marmosets. After unique sequences were automatically aligned by assembling software, the mean contig length was 718 bp (with a standard deviation of 457 bp) among a total of 47,883 transcripts. Approximately 30% of the total transcripts were matched to known marmoset sequences. Gene expression in 18 marmoset P450- and 4 FMO-like genes displayed some tissue-specific patterns. Of these, the three most highly expressed in marmoset liver were P450 2D-, 2E-, and 3A-like genes. In extrahepatic tissues, including brain, gene expressions of these monooxygenases were lower than those in liver, although P450 3A4 (previously P450 3A21) in intestine and P450 4A11- and FMO1-like genes in kidney were relatively highly expressed. By means of massive parallel long-read sequencing and short-read technology applied to marmoset liver, intestine, kidney, and brain, the combined next-generation sequencing analyses reported here were able to identify novel marmoset drug-metabolizing P450 transcripts that have until now been little reported. These results provide a foundation for mechanistic studies and pave the way for the use of marmosets as model animals for drug development in the future.
机译:普通mar猴(Callithrix jacchus)是一种非人类的灵长类动物,可被证明可作为人类药代动力学和生物医学研究模型。细胞色素P450(P450s)是酶的超家族,其通过广泛的异种生物素的单加氧作用在药物代谢和处置中起关键作用;但是,有关mar猴P450的信息目前有限。因此,在将mar猴用作药物开发的动物模型之前,需要详细进行组织特异性mRNA转录物的鉴定和定量分析,包括P450和含黄素的单加氧酶(FMO,另一个单加氧酶家族)的转录物。 。从头到尾组装和mar猴转录本的表达分析是用来自三个雄性和三个雌性mos猴的肝脏,肠,肾和脑的集合样本进行的。通过组装软件自动比对独特序列后,在总共47,883个转录物中,平均重叠群长度为718 bp(标准差为457 bp)。总转录本中约30%与已知的mar猴序列匹配。在18个mar猴P450和4个FMO样基因中的基因表达表现出一些组织特异性模式。其中,在mar猴肝脏中表达最高的三个是P450 2D,2E和3A样基因。尽管包括肠中的P450 3A4(以前称为P450 3A21)和肾脏中的P450 4A11和FMO1样基因相对较高,但在包括脑在内的肝外组织中,这些单加氧酶的基因表达均低于肝脏。通过将大规模并行的长读测序和短读技术应用于mar猴的肝,肠,肾和脑,本文报道的下一代测序综合分析能够鉴定到目前为止,新颖的mar猴药物代谢的P450转录本鲜有报道。这些结果为机理研究提供了基础,并为将of猴用作未来药物开发的模型动物铺平了道路。

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