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头颈部癌前病变中的线粒体C序列改变:进展和克隆增殖的标志物

Mitochondrial C-tract alteration in premalignant lesions of the head and neck: a marker for progression and clonal proliferation.

作者信息

Ha Patrick K, Tong Betty C, Westra William H, Sanchez-Cespedes Montserrat, Parrella Paola, Zahurak Marianna, Sidransky David, Califano Joseph A

机构信息

Departments of Otolaryngology, Head and Neck Cancer Research Division, Johns Hopkins Medical Institution, Baltimore, Maryland 21205, USA.

出版信息

Clin Cancer Res. 2002 Jul;8(7):2260-5.

Abstract

PURPOSE

Although mitochondrial DNA mutations have been described recently in many different tumor types, the nature and timing of such alterations remain unclear. In an effort to further examine the role of mitochondrial DNA mutations in carcinogenesis, we examined 137 premalignant lesions of the head and neck from 93 patients for DNA alterations in the poly-cytosine tract (C-tract) of the displacement loop, discovered recently to be a hot spot of mitochondrial DNA alteration. EXPERIMENTAL DESING: All premalignant lesions were tested using a length-based PCR assay, which amplified the C-tract region of mitochondrial DNA. Somatic microsatellites at six loci were also tested on a subset of patients with metachronous or synchronous lesions found to possess a mitochondrial C-tract alteration.

RESULTS

Thirty-four of 93 (37%) patients harbored lesions that displayed a C-tract alteration. There was a clear increase in incidence from histologically benign hyperplasia (22%) to squamous carcinoma in situ (62%: P < 0.01). We also tested synchronous dysplastic lesions, metachronous dysplastic lesions, and normal epithelium adjacent to dysplastic epithelium with this assay. In most cases, the mitochondrial C-tract status identified a clonal relationship between these lesions. Genomic microsatellites also confirmed that a clonal relationship was present in many of these cases.

CONCLUSIONS

Mitochondrial DNA alterations in the head and neck occur in the earliest premalignant lesions and demonstrate a rising incidence that parallels histological severity. These alterations are valuable as additional markers of histopathological progression.

摘要

目的

尽管线粒体DNA突变最近在许多不同肿瘤类型中都有报道,但这些改变的性质和时间仍不清楚。为了进一步研究线粒体DNA突变在致癌过程中的作用,我们检测了93例患者的137个头颈部癌前病变,以检测位移环多聚胞嘧啶序列(C序列)中的DNA改变,该序列最近被发现是线粒体DNA改变的一个热点。实验设计:所有癌前病变均采用基于长度的PCR检测方法进行检测,该方法可扩增线粒体DNA的C序列区域。对一部分发现有线粒体C序列改变的异时性或同时性病变患者的六个位点的体细胞微卫星也进行了检测。

结果

93例患者中有34例(37%)的病变显示C序列改变。从组织学良性增生(22%)到原位鳞状癌(62%:P < 0.01),发病率明显增加。我们还用该检测方法检测了同时性发育异常病变、异时性发育异常病变以及发育异常上皮相邻的正常上皮。在大多数情况下,线粒体C序列状态确定了这些病变之间的克隆关系。基因组微卫星也证实了许多病例中存在克隆关系。

结论

头颈部线粒体DNA改变发生于最早的癌前病变中,且发病率呈上升趋势,与组织学严重程度平行。这些改变作为组织病理学进展的额外标志物具有重要价值。

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