全结肠区域的缺陷可通过 CGH 在患有异型增生/癌症的 UC 患者的结肠中检测到。
Pan-colonic field defects are detected by CGH in the colons of UC patients with dysplasia/cancer.
机构信息
Department of Medicine, University of Washington, Seattle, WA, United States.
出版信息
Cancer Lett. 2012 Jul 28;320(2):180-8. doi: 10.1016/j.canlet.2012.02.031. Epub 2012 Mar 2.
Abstract
BAC arrays were used to evaluate genomic instability along the colon of patients with ulcerative colitis (UC). Genomic instability increases with disease progression and biopsies more proximal to dysplasia showed increased instability. Pan-colonic field copy number gain or loss involving small (<1Mb) regions were detected in most patients and were particularly apparent in the UC progressor patients who had dysplasia or cancer. Chromosomal copy gains or losses affecting large regions were mainly restricted to dysplastic biopsies. Areas of significant chromosomal losses were detected in the UC progressors on chromosomes 2q36, 3q25, 3p21, 4q34, 4p16.2, 15q22, and 16p13 (p-value⩽0.04). These results extend our understanding of the dynamic nature of pan-colonic genomic instability in this disease.
摘要
BAC 阵列用于评估溃疡性结肠炎(UC)患者结肠的基因组不稳定性。随着疾病的进展,基因组不稳定性增加,并且与发育不良更接近的活检显示出增加的不稳定性。在大多数患者中检测到涉及小(<1Mb)区域的全结肠区域的拷贝数增益或缺失,并且在患有发育不良或癌症的 UC 进展患者中尤为明显。影响大区域的染色体拷贝数增益或缺失主要限于发育不良的活检。在 UC 进展者中,在染色体 2q36、3q25、3p21、4q34、4p16.2、15q22 和 16p13 上检测到显著的染色体缺失区域(p 值 ⩽0.04)。这些结果扩展了我们对该疾病中全结肠基因组不稳定性动态性质的理解。
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