Defective post-transcriptional processing of MUC2 mucin in ulcerative colitis and in Crohn's disease increases detectability of the MUC2 protein core.

Hanski C; Born M; Foss HD; Marowski B; Mansmann U; Arasteh K; Bachler B; Papenfuss M; Niedobitek F

首页> 外文期刊>Journal of Pathology: Journal of the Pathological Society of Great Britain and Ireland >Defective post-transcriptional processing of MUC2 mucin in ulcerative colitis and in Crohn's disease increases detectability of the MUC2 protein core.

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Defective post-transcriptional processing of MUC2 mucin in ulcerative colitis and in Crohn's disease increases detectability of the MUC2 protein core.

机译：在溃疡性结肠炎和克罗恩氏病中，MUC2粘蛋白的转录后加工有缺陷，从而增加了MUC2蛋白核心的可检测性。

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Ulcerative colitis (UC) and, to a lesser extent, Crohn's disease (CD) are associated with a reduction of the protective mucus layer in the large intestine; the role of this alteration in the pathogenesis of either disease is, however, not clear. To learn more about the molecular mechanism of the alteration of the mucus layer, the expression of the main intestinal mucin, MUC2, was investigated in relation to inflammation and dysplasia. Formalin-fixed, paraffin-embedded biopsies from 70 patients with UC and 16 patients with CD, and 13 biopsies from normal colonic mucosa, were used for detection of MUC2 mRNA by in situ hybridization with the SMUC41 probe, and MUC2 protein by immunohistochemistry with the antibody CCP58. The steady-state concentration of MUC2 mRNA was not affected by UC or CD. By contrast, the amount of the detectable MUC2 protein, assessed as the immunoreactive score (IRS), was significantly (p<0. 0001) increased in UC (IRS=8.0+/-3.8) and CD (8.0+/-3.7), compared with the normal colonic mucosa (IRS=2.0+/-1.5). This alteration occurred in the inactive phase of inflammation and persisted in the active phase of the disease. It was also observed during bacterial or protozoal inflammation (n=7). The IRS values did not correlate with the grade of inflammation or dysplasia. Simultaneous histochemistry with high iron diamine and immunohistochemistry indicated that the increase of detectable MUC2 is concomitant with low mucin sulphation in the same cells. These data indicate that the strong MUC2 protein staining in colonic mucosa of patients with UC or CD is due to a long-term alteration of the post-transcriptional modification of the MUC2 molecule, leading to its better detectability by the anti-MUC2 antibody CCP58. This alteration, induced by the inflammatory process, may affect the gel thickness and may contribute to a protracted autoimmune response. Copyright 1999 John Wiley & Sons, Ltd.

机译：溃疡性结肠炎（UC）和克罗恩氏病（CD）在较小程度上与大肠中保护性粘液层的减少有关。然而，这种改变在两种疾病的发病机理中的作用尚不清楚。为了更多地了解改变粘液层的分子机制，研究了主要的肠粘蛋白MUC2的表达与炎症和不典型增生的关系。用SMUC41探针与MUC2蛋白原位杂交，通过70例UC患者和16例CD患者的福尔马林固定，石蜡包埋的活检以及13例正常结肠粘膜的活检来检测MUC2 mRNA和MUC2蛋白的免疫组化。抗体CCP58。 MUC2 mRNA的稳态浓度不受UC或CD的影响。相比之下，评估为免疫反应评分（IRS）的可检测MUC2蛋白量在UC（IRS = 8.0 +/- 3.8）和CD（8.0 +/- 3.7）中显着（p <0.0001）增加与正常结肠粘膜相比（IRS = 2.0 +/- 1.5）。这种改变发生在炎症的非活动期，并持续在疾病的活动期。在细菌或原生动物发炎期间也观察到了这一现象（n = 7）。 IRS值与炎症或不典型增生无关。同时用高铁二胺和免疫组织化学进行组织化学分析表明，在同一细胞中可检测到的MUC2的增加伴随着粘蛋白硫酸化的降低。这些数据表明，患有UC或CD的患者结肠黏膜中强烈的MUC2蛋白染色是由于MUC2分子转录后修饰的长期改变所致，从而导致其被抗MUC2抗体CCP58更好地检测。由炎症过程引起的这种改变可能影响凝胶厚度，并可能导致长期的自身免疫反应。版权所有1999 John Wiley＆Sons，Ltd.

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《Journal of Pathology: Journal of the Pathological Society of Great Britain and Ireland》 |1999年第3期|共8页
作者
Hanski C; Born M; Foss HD; Marowski B; Mansmann U; Arasteh K; Bachler B; Papenfuss M; Niedobitek F;
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正文语种 eng
中图分类病理学;
关键词
Colitis; Ulcerative; Crohn Disease; Mucins; Muc-2-protein; RNA; Messenger; 结肠炎; 溃疡性; Crohn病; 粘蛋白类;

机译：Colitis;Ulcerative;Crohn Disease;Mucins;Muc-2-protein;RNA;Messenger;结肠炎;溃疡性;Crohn病;粘蛋白类;

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1. Defective post-transcriptional processing of MUC2 mucin in ulcerative colitis and in Crohn's disease increases detectability of the MUC2 protein core. [J] . Hanski C, Born M, Foss HD, Journal of Pathology: Journal of the Pathological Society of Great Britain and Ireland . 1999,第3期

机译：在溃疡性结肠炎和克罗恩氏病中，MUC2粘蛋白的转录后加工有缺陷，从而增加了MUC2蛋白核心的可检测性。
2. Ulcerative colitis is not associated with differences in MUC2 mucin allele length (letter) [J] . Swallow DM, Vinall LE, Gum JR, Journal of Medical Genetics . 1999,第11期

机译：溃疡性结肠炎与MUC2粘蛋白等位基因长度的差异无关（字母）
3. TGFalpha-associated MUC2 and MUC3 expression of the gastric epithelium in Menetrier's disease during remission of ulcerative colitis. [J] . Zimmer KP, Heine M, Weissen Plenz G, Gut: Journal of the British Society of Gastroenterology . 2011,第11期

机译：溃疡性结肠炎缓解期间Menetrier病中TGFalpha相关的胃上皮MUC2和MUC3表达。
4. Modulation of Intestinal Epithelial Permeability and Mucin mRNA (MUC2, MUC5AC,and MUC5B) Expression and Protein Secretion in Caco-2/HT29-MTX Co-cultures Exposed to Aflatoxin M1, Ochratoxin A, and Zearalenone Individually or Collectively [C] . ChenQing Wu, SongLi Li, Xin Huang, The 6th International Symposium on Dairy Cow Nutrition and Milk Quality（第六届“奶牛营养与牛奶质量”国际研讨会）论文集 . -1

机译：调制肠上皮渗透性和粘液mRNA（MUC2，MUC5Ac和MUC5B）的表达和蛋白质分泌在暴露于黄曲霉毒素M1，OCHRATOXIN A和Zearalenone的CaCo-2 / HT29-MTX共培养物中，或分别或共同
5. Epigenetics of Crohn's Disease, Ulcerative Colitis, and Phenotypically Normal Individuals [D] . Phillips, Delisa L. 2017

机译：克罗恩病，溃疡性结肠炎和表型正常个体的表观遗传
6. Immunohistochemical detection of MUC2 mucin core protein in ulcerative colitis [O] . Yuji Hinoda, Hirofumi Akashi, Takamaro Suwa, 1998

机译：溃疡性结肠炎中MUC2粘蛋白核心蛋白的免疫组织化学检测
7. P185 Mucin 16 (MUC16) and mucin 20 (MUC20) over-expression in colonic mucosa is associated with histological remission in patients with ulcerative colitis [O] . J. Yamamoto-Furusho, I. Ascaño-Gutiérrez, J. Furuzawa-Carballeda, 2014

机译：结肠粘膜中的P185粘蛋白16（MUC16）和粘蛋白20（MUC20）过表达与溃疡性结肠炎患者的组织学缓解有关

Defective post-transcriptional processing of MUC2 mucin in ulcerative colitis and in Crohn's disease increases detectability of the MUC2 protein core.

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