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在摄入谷蛋白的乳糜泻患者中,与黏膜扁平相关的隐窝凋亡小体。

An association between crypt apoptotic bodies and mucosal flattening in celiac disease patients exposed to dietary gluten.

机构信息

Department of Pathology and Cell Biology, Columbia University Medical Center, 630 West 168th Street, VC14-240A, New York, NY, 10032, USA.

Internal Medicine, Columbia University Medical Center, New York, NY, USA.

出版信息

Diagn Pathol. 2019 Aug 31;14(1):98. doi: 10.1186/s13000-019-0878-1.

Abstract

BACKGROUND

Celiac disease (CD) is characterized histologically by inflammation and villous atrophy. Villous atrophy is thought to result from a disruption of epithelial cellular proliferation and death. Epithelial cells in intestinal mucosa normally proliferate in the crypts and migrate towards the lumen, eventually dying. Apoptotic bodies in crypts are usually abnormal and are associated with certain disease states. The presence of crypt apoptosis in celiac disease has not been thoroughly examined by routine histologic assessment of crypt apoptotic body count (ABC).

METHODS

We quantified the ABC in duodenal biopsies from celiac patients before and after initiation of a gluten-free diet (GFD). We examined twenty-three duodenal biopsies from adult patients with celiac disease at diagnosis and following GFD and determined the maximum ABC in 10 consecutive crypts. Fourteen biopsies from heartburn patients served as controls.

RESULTS

Mean duration between paired biopsies was 2.9 (0.5-8.5) years. Mean maximum ABC in active celiac disease was 5.44 per crypt and decreased to 2.60 with GFD (p = <.0001). The mean maximum ABC in controls was 1.79, lower than both active celiac disease and GFD (p = <.0001 and p = .019 respectively). Flat lesions with total villous atrophy (mean: 6.44) showed a higher ABC compared to non-flat lesions (mean: 4.87); p = .04.

CONCLUSIONS

Crypt ABC is markedly elevated in active celiac disease and decreases significantly with GFD, however it does not achieve normalcy. Total villous atrophy is associated with a higher ABC than all other lesions. Crypt apoptosis is likely a significant contributor to villous atrophy in celiac disease and can be appreciated by routine histologic examination.

摘要

背景

乳糜泻(CD)的组织学特征为炎症和绒毛萎缩。绒毛萎缩被认为是由于上皮细胞增殖和死亡的破坏所致。肠黏膜上皮细胞通常在隐窝中增殖并向腔迁移,最终死亡。隐窝中的凋亡体通常是异常的,并与某些疾病状态有关。乳糜泻中隐窝凋亡的存在尚未通过常规组织学评估隐窝凋亡体计数(ABC)进行彻底检查。

方法

我们在开始无麸质饮食(GFD)之前和之后量化了乳糜泻患者的十二指肠活检中的 ABC。我们检查了 23 例乳糜泻患者的十二指肠活检,这些患者在诊断时和 GFD 后进行了检查,并确定了 10 个连续隐窝中的最大 ABC。 14 例烧心患者的活检作为对照。

结果

配对活检之间的平均时间为 2.9(0.5-8.5)年。活动期乳糜泻的平均最大 ABC 为每个隐窝 5.44,GFD 后降至 2.60(p<.0001)。对照组的平均最大 ABC 为 1.79,低于活动期乳糜泻和 GFD(p<.0001 和 p=.019)。总绒毛萎缩的平坦病变(平均:6.44)的 ABC 高于非平坦病变(平均:4.87);p=.04。

结论

活跃的乳糜泻中 ABC 明显升高,并且在用 GFD 治疗后显着降低,但并未恢复正常。总绒毛萎缩与其他所有病变相比,ABC 更高。隐窝凋亡可能是乳糜泻中绒毛萎缩的重要原因,可以通过常规组织学检查来评估。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/27a1/6717634/22f1a69fdc0d/13000_2019_878_Fig1_HTML.jpg

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