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Cell. 2012 Jun 22;149(7):1622-34. doi: 10.1016/j.cell.2012.04.041.
2
Downregulation of gastrokine-1 in gastric cancer tissues and restoration of its expression induced gastric cancer cells to apoptosis.胃癌组织中 gastrokine-1 的下调及其表达的恢复诱导胃癌细胞凋亡。
J Exp Clin Cancer Res. 2012 May 23;31(1):49. doi: 10.1186/1756-9966-31-49.
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OSA: a fast and accurate alignment tool for RNA-Seq.OSA:用于 RNA-Seq 的快速准确比对工具。
Bioinformatics. 2012 Jul 15;28(14):1933-4. doi: 10.1093/bioinformatics/bts294. Epub 2012 May 15.
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The evolution of pepsinogen C genes in vertebrates: duplication, loss and functional diversification.脊椎动物胃蛋白酶原 C 基因的进化:复制、丢失和功能多样化。
PLoS One. 2012;7(3):e32852. doi: 10.1371/journal.pone.0032852. Epub 2012 Mar 9.
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Tamoxifen induces rapid, reversible atrophy, and metaplasia in mouse stomach.他莫昔芬诱导小鼠胃快速、可逆性萎缩和化生。
Gastroenterology. 2012 Jan;142(1):21-24.e7. doi: 10.1053/j.gastro.2011.09.050. Epub 2011 Oct 14.
6
Gastrokine 1 functions as a tumor suppressor by inhibition of epithelial-mesenchymal transition in gastric cancers.胃泌素 1 通过抑制胃癌中的上皮-间充质转化发挥肿瘤抑制作用。
J Cancer Res Clin Oncol. 2011 Nov;137(11):1697-704. doi: 10.1007/s00432-011-1051-8. Epub 2011 Sep 7.
7
Gastrointestinal tract specific gene GDDR inhibits the progression of gastric cancer in a TFF1 dependent manner.胃肠道特异性基因 GDDR 通过 TFF1 依赖性方式抑制胃癌进展。
Mol Cell Biochem. 2012 Jan;359(1-2):369-74. doi: 10.1007/s11010-011-1030-z. Epub 2011 Aug 26.
8
Overexpression of gastrokine 1 in gastric cancer cells induces Fas-mediated apoptosis.胃癌细胞中 gastrokine 1 的过表达诱导 Fas 介导的细胞凋亡。
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9
BRICHOS domain associated with lung fibrosis, dementia and cancer--a chaperone that prevents amyloid fibril formation?BRICHOS 结构域与肺纤维化、痴呆和癌症相关——一种防止淀粉样纤维形成的伴侣蛋白?
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10
MEGA5: molecular evolutionary genetics analysis using maximum likelihood, evolutionary distance, and maximum parsimony methods.MEGA5:用于最大似然法、进化距离法和最大简约法的分子进化遗传学分析。
Mol Biol Evol. 2011 Oct;28(10):2731-9. doi: 10.1093/molbev/msr121. Epub 2011 May 4.

人类胃动蛋白基因座的进化和 GKN3 假基因性的混杂因素。

Evolution of the human gastrokine locus and confounding factors regarding the pseudogenicity of GKN3.

机构信息

Division of Gastroenterology, Department of Medicine, School of Medicine, Washington University, St. Louis, Missouri 63110, USA.

出版信息

Physiol Genomics. 2013 Aug 1;45(15):667-83. doi: 10.1152/physiolgenomics.00169.2012. Epub 2013 May 28.

DOI:10.1152/physiolgenomics.00169.2012
PMID:23715263
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3742967/
Abstract

In a screen for genes expressed specifically in gastric mucous neck cells, we identified GKN3, the recently discovered third member of the gastrokine family. We present confirmatory mouse data and novel porcine data showing that mouse GKN3 expression is confined to mucous cells of the corpus neck and antrum base and is prominently expressed in metaplastic lesions. GKN3 was proposed originally to be expressed in some human populations and a pseudogene in others. To investigate that hypothesis, we studied human GKN3 evolution in the context of its paralogous genomic neighbors, GKN1 and GKN2. Haplotype analysis revealed that GKN3 mimics GKN2 in patterns of exonic SNP allocation, whereas GKN1 appeared to be more stringently selected. GKN3 showed signatures of both directional selection and population based selective sweeps in humans. One such selective sweep includes SNP rs10187256, originally identified as an ancestral tryptophan to premature STOP codon mutation. The derived (nonancestral) allele went to fixation in Asia. We show that another SNP, rs75578132, identified 5 bp downstream of rs10187256, exhibits a second selective sweep in almost all Europeans, some Latinos, and some Africans, possibly resulting from a reintroduction of European genes during African colonization. Finally, we identify a mutation that would destroy the splice donor site in the putative exon3-intron3 boundary, which occurs in all human genomes examined to date. Our results highlight a stomach-specific human genetic locus, which has undergone various selective sweeps across European, Asian, and African populations and thus reflects geographic and ethnic patterns in genome evolution.

摘要

在一项专门针对胃黏膜颈细胞表达基因的筛选中,我们发现了 GKN3,这是最近发现的 gastrokine 家族的第三个成员。我们提供了确认的小鼠数据和新的猪数据,表明小鼠 GKN3 表达仅限于胃体颈部和胃窦基部的黏液细胞,并在化生病变中表达明显。GKN3 最初被提议在一些人群中表达,而在另一些人群中则是假基因。为了验证这一假说,我们研究了人类 GKN3 在其同源基因基因组邻居 GKN1 和 GKN2 背景下的进化。单倍型分析表明,GKN3 在外显子 SNP 分配模式上与 GKN2 相似,而 GKN1 似乎受到更严格的选择。GKN3 在人类中表现出定向选择和基于群体的选择清除的特征。其中一个选择清除包括 SNP rs10187256,最初被鉴定为一个祖先色氨酸到提前终止密码子的突变。衍生(非祖先)等位基因在亚洲固定下来。我们表明,另一个 SNP rs75578132,位于 rs10187256 下游 5 个碱基处,在几乎所有欧洲人、一些拉丁美洲人和一些非洲人中出现了第二个选择清除,这可能是由于非洲殖民时期欧洲基因的重新引入。最后,我们确定了一个突变,该突变会破坏假定的exon3-intron3 边界的剪接供体位点,该突变发生在迄今为止检查的所有人类基因组中。我们的研究结果突出了一个胃特异性的人类遗传基因座,该基因座在欧洲、亚洲和非洲人群中经历了各种选择清除,因此反映了基因组进化中的地理和种族模式。