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膀胱癌,一种分两个阶段的疾病?

Bladder cancer, a two phased disease?

作者信息

Höglund Mattias

机构信息

Department of Clinical Genetics, Lund University Hospital, Lund SE-221 81, Sweden.

出版信息

Semin Cancer Biol. 2007 Jun;17(3):225-32. doi: 10.1016/j.semcancer.2006.02.002. Epub 2006 Feb 28.

Abstract

The processes of intraepithelial migration, intraluminal seeding, and field cancerization as models for initiation, spread, and recurrences of urothelial cell carcinoma (UCC) are reviewed in light of recent molecular investigations. The accumulated molecular data on synchronous and metachronous tumors indicate that the majority of recurrent and multiple tumors are monoclonal. Molecular data has also shown the presence of chromosomal and genetic changes in precursor lesions as well as in normal urothelial cells. Genetic-histological mapping of cystectomized bladders has shown that overt tumors occur as local events in areas of genetically altered urothelium. A model is put forward in which the tumor process is initiated by genetically altered but histologically normal cells that produce fields of altered cells by intraepithelial displacement. By the accumulation of further genetic changes the fields of altered urothelium reaches a state of criticality, which locally may produce frank tumors.

摘要

根据最近的分子研究,对上皮内迁移、管腔内播散和场癌化等作为尿路上皮细胞癌(UCC)起始、扩散和复发模型的过程进行了综述。关于同步性和异时性肿瘤积累的分子数据表明,大多数复发性和多发性肿瘤是单克隆性的。分子数据还显示,在前体病变以及正常尿路上皮细胞中存在染色体和基因变化。膀胱切除标本的基因-组织学图谱显示,明显的肿瘤作为基因改变的尿路上皮区域的局部事件出现。提出了一个模型,其中肿瘤过程由基因改变但组织学正常的细胞启动,这些细胞通过上皮内移位产生改变细胞的区域。通过进一步基因变化的积累,改变的尿路上皮区域达到临界状态,局部可能产生明显的肿瘤。

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