Flow blockage disrupts cilia-driven fluid transport in the epileptic brain

被引:0
|
作者
Regina J. Faubel
Veronica S. Santos Canellas
Jenna Gaesser
Nancy H. Beluk
Tim N. Feinstein
Yong Wang
Maya Yankova
Kalyani B. Karunakaran
Stephen M. King
Madhavi K. Ganapathiraju
Cecilia W. Lo
机构
[1] University of Pittsburgh School of Medicine,Department of Developmental Biology
[2] University of Pittsburgh School of Medicine,Division of Child Neurology, Department of Pediatrics
[3] University of Pittsburgh,Division of Radiology
[4] Pattern Formation and Biocomplexity,Laboratory for Fluid Physics
[5] Max Planck Institute for Dynamics and Self-Organization,Department of Molecular Biology and Biophysics, And Electron Microscopy Facility
[6] University of Connecticut Health Center,Supercomputer Education and Research Centre
[7] Indian Institute of Science,Department of Biomedical Informatics
[8] University of Pittsburgh School of Medicine,undefined
来源
Acta Neuropathologica | 2022年 / 144卷
关键词
Cerebrospinal fluid; Seizure; Cilia; Epilepsy; Transport; Homeostasis;
D O I
暂无
中图分类号
学科分类号
摘要
A carpet of ependymal motile cilia lines the brain ventricular system, forming a network of flow channels and barriers that pattern cerebrospinal fluid (CSF) flow at the surface. This CSF transport system is evolutionary conserved, but its physiological function remains unknown. Here we investigated its potential role in epilepsy with studies focused on CDKL5 deficiency disorder (CDD), a neurodevelopmental disorder with early-onset epilepsy refractory to seizure medications and the most common cause of infant epilepsy. CDKL5 is a highly conserved X-linked gene suggesting its function in regulating cilia length and motion in the green alga Chlamydomonas might have implication in the etiology of CDD. Examination of the structure and function of airway motile cilia revealed both the CDD patients and the Cdkl5 knockout mice exhibit cilia lengthening and abnormal cilia motion. Similar defects were observed for brain ventricular cilia in the Cdkl5 knockout mice. Mapping ependymal cilia generated flow in the ventral third ventricle (v3V), a brain region with important physiological functions showed altered patterning of flow. Tracing of cilia-mediated inflow into v3V with fluorescent dye revealed the appearance of a flow barrier at the inlet of v3V in Cdkl5 knockout mice. Analysis of mice with a mutation in another epilepsy-associated kinase, Yes1, showed the same disturbance of cilia motion and flow patterning. The flow barrier was also observed in the Foxj1± and FOXJ1CreERT:Cdkl5y/fl mice, confirming the contribution of ventricular cilia to the flow disturbances. Importantly, mice exhibiting altered cilia-driven flow also showed increased susceptibility to anesthesia-induced seizure-like activity. The cilia-driven flow disturbance arises from altered cilia beating orientation with the disrupted polarity of the cilia anchoring rootlet meshwork. Together these findings indicate motile cilia disturbances have an essential role in CDD-associated seizures and beyond, suggesting cilia regulating kinases may be a therapeutic target for medication-resistant epilepsy.
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页码:691 / 706
页数:15
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