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通过单通道cDNA测序构建人胎儿肝脏的基因表达谱。

Construction of a gene expression profile of a human fetal liver by single-pass cDNA sequencing.

作者信息

Choi S S, Yun J W, Choi E K, Cho Y G, Sung Y C, Shin H S

机构信息

Department of Life Science, Pohang University of Science and Technology, Kyungbuk, Republic of Korea.

出版信息

Mamm Genome. 1995 Sep;6(9):653-7. doi: 10.1007/BF00352374.

DOI:10.1007/BF00352374
PMID:8535075
Abstract

We have obtained an overall gene expression profile of a human fetal liver by sequencing the 5' ends of random cDNA clones from an unbiased cDNA library. As a result, many novel genes that might be related to liver growth and hemopoiesis have been identified. Poly (A)+ RNA was purified from the liver of a human fetus obtained at the 22nd week of gestation, and a directional library was constructed with oligo d(T)-primed cDNAs synthesized without any normalizing procedures. The 5' end of each randomly chosen clone was sequenced by the dideoxy-chain termination methods, and each sequence was used for homology search in the public databases such as GenBank, SWISS-PROT, and PIR. Of 1231 random cDNA clones analyzed, 697 clones representing 204 different transcripts (57%), were identical to previously known human genes. The spectrum of the genes in this category reflected well the physiological characteristics of the fetal liver, a combination of hepatic and hemopoietic functions. About 4% of the clones represented novel gene transcripts with significant homologies to known genes of human or other organisms. These included several genes that are known to be involved in cellular differentiation and/or proliferation. About 25% of the clones had no statistically significant match to any known genes. In summary, we have identified 546 different gene transcripts consisting of 204 known human genes, 42 homologous genes, and 300 unknown genes. Thus, this approach appears to be a highly efficient way to identify novel genes of biological interest.

摘要

我们通过对一个无偏向性cDNA文库中随机cDNA克隆的5'末端进行测序,获得了人类胎儿肝脏的整体基因表达谱。结果,鉴定出了许多可能与肝脏生长和造血相关的新基因。从妊娠第22周获得的人类胎儿肝脏中纯化出聚腺苷酸(Poly(A)+)RNA,并使用寡聚d(T)引物合成的cDNA构建了一个定向文库,且未进行任何标准化程序。通过双脱氧链终止法对每个随机选择的克隆的5'末端进行测序,并将每个序列用于在公共数据库如GenBank、SWISS-PROT和PIR中进行同源性搜索。在分析的1231个随机cDNA克隆中,697个克隆(代表204种不同转录本,占57%)与先前已知的人类基因相同。这一类基因的谱很好地反映了胎儿肝脏的生理特征,即肝脏和造血功能的结合。约4%的克隆代表与人类或其他生物体已知基因具有显著同源性的新基因转录本。这些包括几个已知参与细胞分化和/或增殖的基因。约25%的克隆与任何已知基因没有统计学上的显著匹配。总之,我们鉴定出了546种不同的基因转录本,包括204种已知人类基因、42种同源基因和300种未知基因。因此,这种方法似乎是鉴定具有生物学意义的新基因的一种高效方法。

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