首页> 外文期刊>Journal of Cancer Research and Clinical Oncology >Deletion in chromosome 11 and Bcl-1/Cyclin D1 alterations are independently associated with the development of uterine cervical carcinoma.
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Deletion in chromosome 11 and Bcl-1/Cyclin D1 alterations are independently associated with the development of uterine cervical carcinoma.

机译:11号染色体的缺失和Bcl-1 / Cyclin D1的改变与子宫宫颈癌的发生独立相关。

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PURPOSE: The aim of this study was to understand whether there is any association between specific deleted regions in chromosome 11 (chr.11) and alteration (amplification/rearrangement) of Bcl-1/Cyclin D1 locus, located at 11q13, in uterine cervical carcinoma (CA-CX).METHODS: The deletion mapping of chr.11 was studied using 17 highly polymorphic microsatellite markers in 65 primary uterine cervical lesions. The Bcl-1/Cyclin D1 alterations were analyzed by Southern blot and/or polymerase chain reaction (PCR) method in respective cervical lesions.RESULTS: Chr.11 deletion was found to be significantly associated with progression of CA-CX. High frequency (48-65%) of deletion was found in 11p15.5 (D1), 11q22.3-23.1(D2), and 11q23.3-24.1(D3) regions and significant association was seen among deletions in D2 and D3 regions. Bcl-1/Cyclin D1 locus alteration was observed in overall 27% cervical lesions. Co-amplification of Bcl-1/Cyclin D1 locus was seen in 10% samples. However, no association was found between the deleted regions and Bcl-1/Cyclin D1 locus alterations.CONCLUSIONS: Our study suggests that there is no co-operativity between the deleted regions (D1- D3) in chr.11 and Bcl-1/Cyclin D1 alterations, but these alterations may provide cumulative effect in progression of the tumor. The D1-D3 regions may harbor candidate tumor suppressor gene(s) (TSGs) associated with the development of CA-CX.
机译:目的:本研究的目的是了解11号染色体13号染色体上特定缺失区域(chr.11)与子宫宫颈Bcl-1 / Cyclin D1基因座11q13位点的改变(扩增/重排)之间是否存在任何关联。方法:使用17个高度多态性微卫星标记在65例原发性宫颈癌病变中研究了chr.11的缺失作图。通过Southern blot和/或聚合酶链反应(PCR)方法分析相应宫颈病变中Bcl-1 / Cyclin D1的变化。结果:Chr.11缺失与CA-CX的进展密切相关。在11p15.5(D1),11q22.3-23.1(D2)和11q23.3-24.1(D3)地区发现了较高的删除频率(48-65%),并且在D2和D3中发现了明显的关联地区。在全部27%的宫颈病变中观察到Bcl-1 / Cyclin D1基因座改变。在10%的样品中发现Bcl-1 / Cyclin D1基因座的共扩增。然而,在缺失的区域与Bcl-1 / Cyclin D1基因座变化之间未发现任何关联。结论:我们的研究表明在chr.11和Bcl-1 /的缺失区域(D1-D3)之间没有协同作用。细胞周期蛋白D1改变,但是这些改变可以在肿瘤的进展中提供累积作用。 D1-D3区可能包含与CA-CX发育相关的候选肿瘤抑制基因(TSG)。

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