首页> 外文期刊>Applied immunohistochemistry and molecular morphology: AIMM >Immunohistologic parameters in minimal morphologic change duodenal biopsies from patients with clinically suspected gluten-sensitive enteropathy.
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Immunohistologic parameters in minimal morphologic change duodenal biopsies from patients with clinically suspected gluten-sensitive enteropathy.

机译:临床怀疑的麸质敏感型肠病患者的最小形态学十二指肠活检中的免疫组织学参数。

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Subclinical or latent cases of gluten-sensitive enteropathy (GSE) are difficult to diagnose, and serology-positive, histology-negative (minimal morphologic change) and serology-negative, histology-positive patients have been identified. Both, particularly the histology-negative group, require the correct diagnosis for proper management, especially because the concept of minimal histologic change GSE has escaped attention in standard textbooks. We assessed the numbers and distribution of intraepithelial T cells and their subsets with CD3, CD8, and CD4 immunostaining and examined for crypt hyperplasia with mitotic and Ki-67 proliferative indices with the aim of refining the criteria for the diagnosis of minimal change GSE. Duodenal biopsies from 46 clinically suspected cases of GSE tested for antigliadin, antiendomysium, and antitissue transglutaminase antibodies were divided into four groups: serology-positive, histology-positive (S+H+, n = 20); serology-positive, histology-negative (S+H-, n = 22), representing the minimal morphologic change group; serology-negative, histology-positive (S-H+, n = 4); and serology-negative, histology-negative (S-H-, n = 28), controls with histologically normal duodenal biopsies obtained for unrelated reasons. The numbers of CD3+ and CD8+ intraepithelial T cells (IETCs) were significantly higher in histology-positive biopsies with (mean, 40.3/100 and 39.3/100 enterocytes, respectively) and without positive serology (mean, 33.3/100 and 35/100 enterocytes, respectively) compared with all other groups (S+H-, mean, 26.5/100 and 24.3/100 enterocytes, respectively; S-H-, mean, 23.3/100 and 17.9/100 enterocytes, respectively). Values for Ki-67 index in crypt enterocytes were also significantly different between histology-positive and histology-negative groups (P = 0.000). The distribution of CD3+ and CD8+ IETCs was mostly even along the surface enterocytes in histology-positive cases compared with the controls, which showed an uneven distribution. The 2 parameters that significantly discriminated between minimal morphologic change GSE (S+H-) and controls (S-H-) were Ki-67 index (P = 0.007) and the distribution pattern of CD8+ IETCs (P = 0.049). CD4 IETC counts were generally low, with no significant difference between all groups. The few S-H+ cases seen most likely represented false-negative serology, because the assessed parameters of this group and S+H+ cases were indistinguishable.
机译:面筋敏感型肠病(GSE)的亚临床或潜伏病例难以诊断,并且已经鉴定出血清学阳性,组织学阴性(最小形态学改变)和血清学阴性,组织学阳性的患者。两者,特别是组织学阴性的人,都需要对正确的诊断进行正确的处理,特别是因为最小化组织学改变的概念GSE在标准教科书中已引起关注。我们评估了CD3,CD8和CD4免疫染色的上皮内T细胞及其亚群的数量和分布,并检查了有丝分裂和Ki-67增生指数的隐窝增生症,旨在完善诊断微小变化GSE的标准。将来自46例临床怀疑的GSE的十二指肠活检检测为抗麦胶蛋白,抗内胚层和抗组织转谷氨酰胺酶抗体,分为四组:血清学阳性,组织学阳性(S + H +,n = 20);血清学阳性,组织学阴性(S + H-,n = 22),代表最小形态变化组;血清学阴性,组织学阳性(S-H +,n = 4);血清学阴性,组织学阴性(S-H-,n = 28),是由于无关原因而获得的组织学正常的十二指肠活检的对照。在组织学阳性活检中,CD3 +和CD8 +上皮内T细胞(IETC)的数量显着高于(平均分别为40.3 / 100和39.3 / 100肠细胞)和没有阳性血清学(平均为33.3 / 100和35/100肠细胞)与所有其他组(分别为S + H-,平均26.5 / 100和24.3 / 100肠上皮细胞; SH-分别为23.3 / 100和17.9 / 100肠上皮细胞)进行比较。在组织学阳性组和组织学阴性组之间,隐窝肠上皮细胞的Ki-67指数值也显着不同(P = 0.000)。与对照组相比,在组织学阳性的病例中,CD3 +和CD8 + IETC的分布大部分沿着表面肠上皮细胞均匀分布,这表明分布不均。显着区分最小形态变化GSE(S + H-)和对照(S-H-)的2个参数是Ki-67指数(P = 0.007)和CD8 + IETC的分布模式(P = 0.049)。 CD4 IETC计数通常较低,所有组之间无显着差异。很少见到的S-H +病例代表假阴性血清学,因为该组与S + H +病例的评估参数无法区分。

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