Inner ear pathologies impair sodium-regulated ion transport in Meniere’s disease

被引:0
|
作者
Andreas H. Eckhard
MengYu Zhu
Jennifer T. O’Malley
Gordon H. Williams
Johannes Loffing
Steven D. Rauch
Joe B. Nadol
M. Charles Liberman
Joe C. Adams
机构
[1] Massachusetts Eye and Ear Infirmary,Otopathology Laboratory
[2] Brigham and Women’s Hospital,Division of Endocrinology, Diabetes, and Hypertension, Department of Medicine
[3] Harvard Medical School,Institute of Anatomy
[4] University of Zurich,Eaton
[5] Massachusetts Eye and Ear Infirmary,Peabody Laboratories
[6] Harvard Medical School,Department of Otolaryngology
[7] Massachusetts Eye and Ear Infirmary,Vestibular Division, Department of Otolaryngology
[8] Massachusetts General Hospital,Department of Otorhinolaryngology
[9] University Hospital Zurich,undefined
来源
Acta Neuropathologica | 2019年 / 137卷
关键词
Meniere’s disease; Endolymphatic sac; Endolymphatic hydrops; Sodium; Aldosterone;
D O I
暂无
中图分类号
学科分类号
摘要
Meniere’s disease (MD), a syndromal inner ear disease, is commonly associated with a pathological accumulation of endolymphatic fluid in the inner ear, termed “idiopathic” endolymphatic hydrops (iEH). Although numerous precipitating/exacerbating factors have been proposed for MD, its etiology remains elusive. Here, using immunohistochemistry and in situ protein–protein interaction detection assays, we demonstrate mineralocorticoid-controlled sodium transport mechanisms in the epithelium of the extraosseous portion of the endolymphatic sac (eES) in the murine and human inner ears. Histological analysis of the eES in an extensive series of human temporal bones consistently revealed pathological changes in the eES in cases with iEH and a clinical history of MD, but no such changes were found in cases with “secondary” EH due to other otological diseases or in healthy controls. Notably, two etiologically different pathologies—degeneration and developmental hypoplasia—that selectively affect the eES in MD were distinguished. Clinical records from MD cases with degenerative and hypoplastic eES pathology revealed distinct intergroup differences in clinical disease presentation. Overall, we have identified for the first time two inner ear pathologies that are consistently present in MD and can be directly linked to the pathogenesis of EH, and which potentially affect the phenotypical presentation of MD.
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页码:343 / 357
页数:14
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