首页> 外文期刊>Revista do Colégio Brasileiro de Cirurgies >Es?fago de Barrett: aspectos fisiopatológicos e moleculares da seqüência metaplasia-displasia-adenocarcinoma - artigo de revis?o
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Es?fago de Barrett: aspectos fisiopatológicos e moleculares da seqüência metaplasia-displasia-adenocarcinoma - artigo de revis?o

机译:巴雷特食管:化生-异型增生-腺癌序列的病理生理和分子方面-评论文章

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The Barrett's esophagus (BE) is defined as endoscopically visible columnar mucosa at the distal esophagus, of any extension, proved to harbor intestinal metaplasia on biopsy, highlighted by the presence of goblet cells. BE denotes long-standing gastroesophageal reflux disease (GERD) and is an important risk factor for the development of esophageal adenocarcinoma (EAC). Therefore, these patients must be on follow-up, in order to diagnose cancer early. BE patients have frequent alterations in esophageal physiologyc studies. Alkaline duodenogastroesophageal reflux seems to have important role. The development BE occurs in steps, initially with formation of cardiac type mucosa subsequent intestinalization. Futher progression can follow a sequence, from low grade dysplasia, to high grade dysplasia and esophageal adenocarcinoma. Current follow-up is based on the presence of dysplasia. It has limitations, grouping patients heterogeneously. Different steps of carcinogenesis have been studied looking for an ideal prognostic marker. Uncontrolled proliferative activity, apoptosis inhibition, angiogenesis, tissue invasion and metastases formation are all implicated in cancer origin. Some cycle cell molecules have been studied in BE, such as retinoblastoma protein, ciclins, kinase dependent ciclins and cell cycle inhibitors. The P53 protein is one of the most investigated in the metaplasia-adenocarcinoma progression. Growth Factors, apoptotic proteins, telomers and DNA ploidy have also been searched. Increased proliferative activity has been implicated in Barrett's carcinogenesis and the Ki-67 antigen, through imunohistochemical analysis, has become the the method of choice. Present in the nucleus, it is found in proliferative cells only. Some studies suport association between Ki-67 activity and the metaplasia-dysplasia-adenocarcinoma sequence.The results, however, are inconclusive and research should follow this way.
机译:Barrett食管(BE)的定义是在食管远端可见内镜可见的柱状粘膜,且有任何延伸,经活检证实具有肠化生特征,其特征在于杯状细胞的存在。 BE代表长期的胃食管反流病(GERD),并且是发展食管腺癌(EAC)的重要危险因素。因此,这些患者必须接受随访,以便及早诊断出癌症。 BE患者在食管生理学研究中经常发生改变。碱性十二指肠胃食管反流似乎具有重要作用。 BE的发生是逐步发生的,最初是随着心脏类型粘膜的形成,随后是肠道的形成。从低度不典型增生到高度不典型增生和食道腺癌,可以进一步发展。当前的随访是基于发育异常的情况。它有局限性,将患者异类分组。已经研究了癌变的不同步骤,以寻找理想的预后指标。不受控制的增殖活性,细胞凋亡抑制,血管生成,组织侵袭和转移形成均与癌症起源有关。在BE中已经研究了一些循环细胞分子,例如成视网膜细胞瘤蛋白,ciclins,激酶依赖性ciclins和细胞周期抑制剂。 P53蛋白是在化生腺癌进展中研究最多的蛋白之一。还已经研究了生长因子,凋亡蛋白,端粒和DNA倍性。已通过Barunt的致癌作用增加了增殖活性,通过免疫组织化学分析,Ki-67抗原已成为一种选择的方法。它存在于细胞核中,仅在增殖细胞中发现。一些研究支持Ki-67活性与化生-异型增生-腺癌序列之间的关联,但结果尚无定论,应遵循这种方法进行研究。

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