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Gelsolin 的突变谱及其下调与乳腺癌相关。

Mutational spectrum of Gelsolin and its down regulation is associated with breast cancer.

机构信息

Cancer Genetics Lab, Department of Biosciences, COMSATS Institute of Information Technology, Chak shazad, Islamabad, Pakistan.

出版信息

Dis Markers. 2013;34(2):71-80. doi: 10.3233/DMA-120952.

DOI:10.3233/DMA-120952
PMID:23324580
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3809971/
Abstract

Cytoskeletal rearrangement occurs in variety of cellular processes and involves a wide spectrum of proteins. Gelsolin super family proteins control actin organization by severing and capping filament ends and nucleating actin assembly. Gelsolin is the founding member of this family and plays important role in pathogenesis of human neoplasia. This study aimed to investigate the germline mutations and expressional profile of Gelsolin in human breast cancer tissues. For germ line screening PCR-SSCP technique was used while expression was analyzed through quantitative real time PCR. Different types of mutations were observed in Gelsolin coding regions on exons 4, 10, 11, 14 and 15. These mutations include 3 missense nonsynonymous substitution mutations, 2 deletions, 1 insertion and 1 synonymous substitution mutation. Gelsolin transcript level was found significantly lower in breast tumor tissues compared to control samples (p=0.03). Low level of Gelsolin was found in metastatic patients (p=0.002) and patients who died from breast cancer (P=0.03) compared to disease free patients at final follow up. This study shows that level of Gelsolin is down regulated in breast cancer tissues and is linked with metastasis development and death in patients. It is concluded that genetic changes in coding regions of Gelsolin can potentially contribute to genetic instability. These genetic variations and expressional correlation with patient survival may prove to be of significant importance.

摘要

细胞骨架重排发生在多种细胞过程中,涉及广泛的蛋白质。凝胶蛋白超家族蛋白通过切断和封闭纤维末端以及引发肌动蛋白组装来控制肌动蛋白的组织。凝胶蛋白是该家族的创始成员,在人类肿瘤的发病机制中发挥重要作用。本研究旨在研究人类乳腺癌组织中凝胶蛋白的种系突变和表达谱。对于种系筛选,使用了 PCR-SSCP 技术,而表达则通过定量实时 PCR 进行分析。在第 4、10、11、14 和 15 外显子的凝胶蛋白编码区观察到不同类型的突变。这些突变包括 3 种错义非同义取代突变、2 种缺失、1 种插入和 1 种同义取代突变。与对照样本相比,乳腺癌组织中的凝胶蛋白转录水平明显降低(p=0.03)。与无病患者相比,转移性患者(p=0.002)和死于乳腺癌的患者(P=0.03)的凝胶蛋白水平较低。本研究表明,凝胶蛋白水平在乳腺癌组织中下调,并与转移发展和患者死亡相关。结论是,凝胶蛋白编码区的遗传变化可能导致遗传不稳定性。这些遗传变异与患者生存的表达相关性可能具有重要意义。