Division of Cell Biology, Biocenter Innsbruck, Medical University Innsbruck, Innsbruck, Austria; Division of Pathology, Department of Pediatric Laboratory Medicine, Hospital for Sick Children, Toronto, Canada.
Traffic. 2014 Jan;15(1):22-42. doi: 10.1111/tra.12131. Epub 2013 Nov 19.
Microvillus inclusion disease (MVID) is a congenital enteropathy characterized by loss of apical microvilli and formation of cytoplasmic inclusions lined by microvilli in enterocytes. MVID is caused by mutations in the MYO5B gene, coding for the myosin Vb motor protein. Although myosin Vb is implicated in the organization of intracellular transport and cell surface polarity in epithelial cells, its precise role in the pathogenesis of MVID is unknown. We performed correlative immunohistochemistry analyses of sections from duodenal biopsies of a MVID patient, compound heterozygous for two novel MYO5B mutations, predicting loss of function of myosin Vb in duodenal enterocytes together with a stable MYO5B CaCo2 RNAi cell system. Our findings show that myosin Vb-deficient enterocytes display disruption of cell polarity as reflected by mislocalized apical and basolateral transporter proteins, altered distribution of certain endosomal/lysosomal constituents including Rab GTPases. Together, this severe disturbance of epithelial cell function could shed light on the pathology and symptoms of MVID.
微绒毛包涵体病(MVID)是一种先天性肠病,其特征是肠细胞中顶膜微绒毛缺失和微绒毛衬里的细胞质包涵体形成。MVID 是由编码肌球蛋白 Vb 运动蛋白的 MYO5B 基因突变引起的。尽管肌球蛋白 Vb 参与了上皮细胞内细胞运输和细胞表面极性的组织,但它在 MVID 发病机制中的精确作用尚不清楚。我们对 MVID 患者十二指肠活检切片进行了相关免疫组织化学分析,该患者为两种新型 MYO5B 突变的复合杂合子,预测肌球蛋白 Vb 在十二指肠肠细胞中的功能丧失,同时还建立了稳定的 MYO5B CaCo2 RNAi 细胞系统。我们的研究结果表明,肌球蛋白 Vb 缺陷的肠细胞表现出细胞极性的破坏,表现为顶膜和基底外侧转运蛋白的位置改变,某些内体/溶酶体成分(包括 Rab GTPases)的分布改变。综上所述,这种严重的上皮细胞功能障碍可能阐明了 MVID 的病理学和症状。
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