首页> 美国卫生研究院文献>Clinical Molecular Pathology >The novel human MOST-1 (C8orf17) gene exhibits tissue specific expression maps to chromosome 8q24.2 and is overexpressed/amplified in high grade cancers of the breast and prostate
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The novel human MOST-1 (C8orf17) gene exhibits tissue specific expression maps to chromosome 8q24.2 and is overexpressed/amplified in high grade cancers of the breast and prostate

机译:新型人类MOST-1(C8orf17)基因表现出组织特异性表达定位于8q24.2染色体在乳腺癌和前列腺癌中过表达/扩增

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摘要

>Aims: To elucidate genes that participate in the process of oncogenesis, primers based on the E6 genes of genital human papillomaviruses (HPVs) were used to amplify potential expressed sequence tags (ESTs) from the MOLT-4 T lymphoblastic leukaemia cell line.>Methods: Using the polymerase chain reaction (PCR) with human papillomavirus E6 gene primers, an EST from the MOLT-4 T lymphoblastic leukaemia cell line was amplified. Via rapid amplification of cDNA ends (RACE) and cycle sequencing from MOLT-4 and fetal lung cDNA libraries, overlapping cDNAs of 2786 bp and 2054 bp of the corresponding novel human intronless gene designated MOST-1 (for MOLT-4 sequence tag-1) were characterised and assigned the symbol C8orf17 by the HUGO Nomenclature Committee.>Results: Both cDNAs contained a potential open reading frame (ORF) of 297 bp incorporating a methionine codon with an ideal Kozak consensus sequence for translation initiation, and encoding a putative hydrophilic polypeptide of 99 amino acids. Although reverse transcription PCR (RT-PCR) demonstrated MOST-1 expression in all 19 cancer and two normal cell lines tested, differential expression was seen in only nine of 16 normal tissues tested (heart, kidney, liver, pancreas, small intestine, ovary, testis, prostate, and thymus). A 388 bp fragment was amplified from the NS-1 mouse myeloma cell line, the sequence of which was identical to that within the MOST-1 ORF. The MOST-1 gene was mapped by fluorescent in situ hybridisation to chromosome 8q24.2, a region amplified in many breast cancers and prostate cancers, which is also the candidate site of potential oncogene(s) other than c-myc located at 8q24.1. Analysis of paired biopsies of invasive ductal breast cancer and adjacent normal tissue by semiquantitative and real time RT-PCR revealed average tumour to normal ratios of MOST-1 expression that were two times greater in grade 3 cancers than in grade 1 and 2 cancers. Quantitative real time PCR of archival prostatic biopsies displayed MOST-1 DNA values that were 9.9, 7.5, 4.2, and 1.4 times higher in high grade carcinomas, intermediate grade carcinomas, low grade carcinomas, and benign hyperplasias, respectively, than in normal samples.>Conclusions: These data suggest a role for MOST-1 in cellular differentiation, proliferation, and carcinogenesis.
机译:>目的:为了阐明参与肿瘤发生过程的基因,使用了基于生殖器人乳头瘤病毒(HPV)E6基因的引物,从MOLT-4 T扩增潜在的表达序列标签(EST)。 >方法:使用人乳头瘤病毒E6基因引物的聚合酶链反应(PCR),扩增了MOLT-4 T淋巴细胞白血病细胞系的EST。通过快速扩增cDNA末端(RACE)并从MOLT-4和胎儿肺cDNA文库中进行循环测序,将相应的新型人类无内含子基因命名为MOST-1的2786 bp和2054 bp的重叠cDNA(用于MOLT-4序列标签1) >结果:这两个cDNA都含有一个297 bp的潜在开放阅读框(ORF),其中包含一个蛋氨酸密码子和一个理想的Kozak共有序列,可用于翻译起始。 ,并编码一个推测的99个氨基酸的亲水性多肽。尽管逆转录PCR(RT-PCR)在所有19种癌症和两种正常细胞系中均显示MOST-1表达,但在16种正常组织(心脏,肾脏,肝脏,胰腺,小肠,卵巢)中只有9种表达差异,睾丸,前列腺和胸腺)。从NS-1小鼠骨髓瘤细胞系中扩增了388 bp的片段,其序列与MOST-1 ORF中的序列相同。通过荧光原位杂交将MOST-1基因定位到染色体8q24.2,该染色体在许多乳腺癌和前列腺癌中都有扩增,该区域也是位于8q24处的c-myc以外的潜在致癌基因的候选位点。 1。通过半定量和实时RT-PCR对浸润性导管癌和邻近正常组织的配对活检进行分析,发现平均肿瘤与正常MOST-1表达的比率在3级癌症中是1级和2级癌症的两倍。存档前列腺活检的定量实时PCR显示,与正常样品相比,高等级癌,中等级癌,低等级癌和良性增生的MOST-1 DNA值分别高9.9、7.5、4.2和1.4倍。 >结论:这些数据表明MOST-1在细胞分化,增殖和致癌性中的作用。

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