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三叶肽pS2和人解痉多肽在十二指肠溃疡边缘胃化生中的表达

Expression of trefoil peptides pS2 and human spasmolytic polypeptide in gastric metaplasia at the margin of duodenal ulcers.

作者信息

Khulusi S, Hanby A M, Marrero J M, Patel P, Mendall M A, Badve S, Poulsom R, Elia G, Wright N A, Northfield T C

机构信息

Department of Medicine, St George's Hospital Medical School, London.

出版信息

Gut. 1995 Aug;37(2):205-9. doi: 10.1136/gut.37.2.205.

Abstract

Duodenal ulcers are associated with gastric metaplasia in the duodenum, both at the ulcer margin and at more distant sites in the duodenal bulb. pS2 and human spasmolytic polypeptide (hSP) are secretory peptides expressed in gastric epithelial cells and in gastric metaplasia. As these peptides may be important in ulcer healing, this study investigated the possibility that the expression of pS2 and hSP is increased in gastric metaplasia at the margin of duodenal ulcers. Duodenal bulb biopsy specimens from 12 duodenal ulcer patients were assessed. Sections were immunostained with monoclonal antibodies for pS2 and hSP. Cytoplasmic stain intensities were measured by an image analysis system and expressed as integrated optical density (IOD) units, In situ hybridisation for pS2 and hSP mRNA was carried out on parallel sections. Duodenal sections were also stained with diatase periodic acid Schiff/alcian blue to localise areas of gastric metaplasia. pS2 antigen staining in the duodenum was restricted to surface epithelial cells, and hSP to acinar and ductular components of Brunner's gland. mRNA localisation corresponded to immunostaining cells. In gastric metaplasia, pS2 expression was greater at the ulcer margin than away from the ulcer, as judged by the intensity of antibody staining (mean IOD units (SEM), 20.6 (3.3) v 9.5 (3.0); p < 0.001). There was a trend towards greater hSP staining at the ulcer margin but this did not achieve statistical significance. These findings support the putative role of pS2 and possible hSP in mucosal healing and providy further evidence for an autocrine 'ulcer-gastric metaplasia-repair' loop involving these trefoil peptides.

摘要

十二指肠溃疡与十二指肠的胃化生有关,在溃疡边缘以及十二指肠球部更远的部位均如此。pS2和人解痉多肽(hSP)是在胃上皮细胞和胃化生中表达的分泌性肽。由于这些肽可能在溃疡愈合中起重要作用,本研究调查了十二指肠溃疡边缘胃化生中pS2和hSP表达增加的可能性。对12例十二指肠溃疡患者的十二指肠球部活检标本进行了评估。切片用pS2和hSP的单克隆抗体进行免疫染色。通过图像分析系统测量细胞质染色强度,并表示为积分光密度(IOD)单位。在平行切片上进行pS2和hSP mRNA的原位杂交。十二指肠切片还用淀粉酶过碘酸希夫/阿尔辛蓝染色以定位胃化生区域。十二指肠中的pS2抗原染色仅限于表面上皮细胞,而hSP仅限于布伦纳腺的腺泡和导管成分。mRNA定位与免疫染色细胞相对应。在胃化生中,根据抗体染色强度判断,溃疡边缘的pS2表达高于远离溃疡处(平均IOD单位(SEM),20.6(3.3)对9.5(3.0);p<0.001)。溃疡边缘hSP染色有增加的趋势,但未达到统计学意义。这些发现支持了pS2和可能的hSP在黏膜愈合中的假定作用,并为涉及这些三叶肽的自分泌“溃疡-胃化生-修复”环提供了进一步的证据。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b243/1382719/aa344150c34c/gut00527-0059-a.jpg

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