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Could Mycobacterium avium subspecies paratuberculosis cause Crohn’s disease ulcerative colitis…and colorectal cancer?

机译:禽分枝杆菌亚种副结核病会导致克罗恩病溃疡性结肠炎...和结直肠癌吗?

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摘要

Infectious agents are known causes of human cancers. Schistosoma japonicum and Schistosoma mansoni cause a percentage of colorectal cancers in countries where the respective Schistosoma species are prevalent. Colorectal cancer is a complication of ulcerative colitis and colonic Crohn’s disease, the two main forms of idiopathic inflammatory bowel disease (IIBD). Mycobacterium avium subspecies paratuberculosis (MAP), the cause of a chronic intestinal disease in domestic and wild ruminants, is one suspected cause of IIBD. MAP may therefore be involved in the pathogenesis of IIBD-associated colorectal cancer as well as colorectal cancer in individuals without IIBD (sporadic colorectal cancer) in countries where MAP infection of domestic livestock is prevalent and MAP’s presence in soil and water is extensive. MAP organisms have been identified in the intestines of patients with sporadic colorectal cancer and IIBD when high magnification, oil immersion light microscopy (×1000 total magnification rather than the usual ×400 total magnification) is used. Research has demonstrated MAP’s ability to invade intestinal goblet cells and cause acute and chronic goblet cell hyperplasia. Goblet cell hyperplasia is the little-recognized initial pathologic lesion of sporadic colorectal cancer, referred to as transitional mucosa, aberrant crypt foci, goblet cell hyperplastic polyps or transitional polyps. It is the even lesser-recognized initial pathologic feature of IIBD, referred to as hypermucinous mucosa, hyperplastic-like mucosal change, serrated epithelial changes, flat serrated changes, goblet cell rich mucosa or epithelial hyperplasia. Goblet cell hyperplasia is the precursor lesion of adenomas and dysplasia in the classical colorectal cancer pathway, of sessile serrated adenomas and serrated dysplasia in the serrated colorectal cancer pathway, and of flat and elevated dysplasia and dysplasia-associated lesions or masses in IIBD-associated intestinal cancers. MAP’s invasion of intestinal goblet cells may result in the initial pathologic lesion of IIBD and sporadic colorectal cancer. MAP’s persistence in infected intestines may result in the eventual development of both IIBD-associated and sporadic colorectal cancer.Electronic supplementary materialThe online version of this article (10.1186/s13027-017-0172-3) contains supplementary material, which is available to authorized users.
机译:感染因子是已知的人类癌症原因。日本血吸虫和曼氏血吸虫在各个血吸虫物种流行的国家中引起一定比例的结直肠癌。大肠癌是溃疡性结肠炎和结肠克罗恩氏病(一种特发性炎症性肠病(IIBD)的两种主要形式)的并发症。禽分枝杆菌亚种副结核病(MAP)是引起家庭和野生反刍动物慢性肠道疾病的原因,是IIBD的一种可疑原因。因此,MAP可能参与了IIBD相关的结直肠癌的发病机理,以及在家畜受到MAP感染的国家以及MAP在土壤和水中广泛存在的国家中,没有IIBD的个体(零星结直肠癌)的结肠直肠癌。当使用高放大倍率,油浸式光学显微镜(×1000总放大倍率而不是通常的×400总放大倍率)时,在散发性结直肠癌和IIBD患者的肠中已发现MAP微生物。研究表明,MAP具有入侵肠道杯状细胞并引起急性和慢性杯状细胞增生的能力。杯状细胞增生是散发性结直肠癌的鲜为人知的初始病理病变,称为过渡黏膜,隐窝异常灶,杯状细胞增生性息肉或过渡性息肉。它是IIBD的较不为人所知的初始病理特征,称为高粘液性粘膜,增生样粘膜变化,锯齿状上皮变化,锯齿状扁平变化,杯状细胞富含粘膜或上皮增生。杯状细胞增生是典型结直肠癌途径中腺瘤和发育不良的前体病变,是锯齿状结肠直肠癌途径中的无柄锯齿状腺瘤和锯齿状发育异常,以及IIBD相关的肠道中与发育异常和不典型增生相关的病变或肿块。癌症。 MAP侵袭肠杯状细胞可能导致IIBD和散发性结直肠癌的初始病理病变。 MAP在受感染肠道中的持久性可能导致IIBD相关性和散发性结直肠癌的最终发展电子补充材料本文的在线版本(10.1186 / s13027-017-0172-3)包含补充材料,授权用户可以使用。 。

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