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十二指肠胃化生的发病机制:局部杯状细胞转化的作用。

The pathogenesis of duodenal gastric metaplasia: the role of local goblet cell transformation.

作者信息

Shaoul R, Marcon P, Okada Y, Cutz E, Forstner G

机构信息

Department of Pediatrics, B'nai Zion Medical Center, Haifa, Israel.

出版信息

Gut. 2000 May;46(5):632-8. doi: 10.1136/gut.46.5.632.

Abstract

BACKGROUND AND AIMS

Gastric metaplasia is frequently seen in biopsies of the duodenal cap, particularly when inflamed or ulcerated. In its initial manifestation small patches of gastric foveolar cells appear near the tip of a villus. These cells contain periodic acid-Schiff (PAS) positive neutral mucins in contrast with the alcian blue (AB) positive acidic mucins within duodenal goblet cells. Previous investigations have suggested that these PAS positive cells originate either in Brunner's gland ducts or at the base of duodenal crypts and migrate in distinct streams to the upper villus. To investigate the origin of gastric metaplasia in superficial patches, we used the PAS/AB stain to distinguish between neutral and acidic mucins and in addition specific antibodies to immunolocalise foveolar cell mucin MUC5AC, the foveolar cell secretory product, gastric trefoil factor (TFF1), the mature goblet cell mucin MUC2, and MUC2 core antigen.

RESULTS

Cells in focal patches of gastric metaplasia contained secretory granules of both gastric and goblet cell phenotypes. MUC5AC and TFF1 were present as expected in gastric foveolar cells but in addition, MUC2 core antigen, normally present only in the Golgi of intestinal goblet cells, was expressed in secretory granules. Goblet cells in the vicinity of metaplastic patches also expressed both gastric and intestinal antigens. MUC5AC/MUC2 containing goblet cells were most common near the villus tip but were also seen at the base of crypts. Where crypts and Brunner's gland ducts merged they were always seen on the crypt side of the junction. Goblet cells were the only cells to express gastric antigens in these areas. In advanced metaplastic lesions, dual phenotype goblet cells were less evident and fewer cells expressed intestinal mucin antigens.

CONCLUSIONS

We suggest that goblet cells that express both intestinal and gastric antigens may represent local precursors of gastric metaplasia undergoing a transition to foveolar-like cells of mixed phenotype at the site of early metaplastic patches. As metaplasia becomes more widespread, a more pure gastric phenotype emerges. This progression is likely to be controlled by local inflammatory signals.

摘要

背景与目的

胃化生在十二指肠球部活检中较为常见,尤其是在发炎或溃疡时。在其初始表现中,绒毛顶端附近会出现小片状胃小凹细胞。这些细胞含有过碘酸希夫(PAS)阳性中性黏液,与十二指肠杯状细胞内的阿尔辛蓝(AB)阳性酸性黏液形成对比。先前的研究表明,这些PAS阳性细胞要么起源于Brunner腺导管,要么起源于十二指肠隐窝底部,并以不同的流向上迁移至绒毛上部。为了研究浅表片状胃化生的起源,我们使用PAS/AB染色来区分中性和酸性黏液,此外还使用特异性抗体对胃小凹细胞黏蛋白MUC5AC、胃小凹细胞分泌产物胃三叶因子(TFF1)、成熟杯状细胞黏蛋白MUC2以及MUC2核心抗原进行免疫定位。

结果

胃化生灶中的细胞含有胃和杯状细胞两种表型的分泌颗粒。MUC5AC和TFF1如预期出现在胃小凹细胞中,但此外,通常仅存在于肠道杯状细胞高尔基体中的MUC2核心抗原也在分泌颗粒中表达。化生灶附近的杯状细胞也表达胃和肠道抗原。含有MUC5AC/MUC2的杯状细胞在绒毛顶端附近最为常见,但在隐窝底部也可见到。在隐窝和Brunner腺导管汇合处,它们总是出现在连接处的隐窝一侧。杯状细胞是这些区域中唯一表达胃抗原的细胞。在晚期化生病变中,双表型杯状细胞不太明显,表达肠道黏蛋白抗原的细胞也较少。

结论

我们认为,表达肠道和胃抗原 的杯状细胞可能代表胃化生的局部前体细胞,它们在早期化生灶部位正经历向混合表型的小凹样细胞的转变。随着化生变得更加广泛,会出现更纯的胃表型。这种进展可能受局部炎症信号控制。

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本文引用的文献

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