Abstract

The high probability of breakdown in the functioning of the central nervous system (CNS) during late stages of aging, as in Alzheimer?s disease and various dementias is a major concern for the elderly. Triggers that initiate age-associated diseases and neurological conditions are for the most part unknown. A key to these associations could be the population of ependymal cells in the brain. Ependymal cells form a monolayer that functions as a barrier between the cerebrospinal fluid (CSF) and the overlying cellular compartments of the brain. As such, they regulate CSF production, circulation, and filtering, and thus ependymal cells are a key component of the newly described ?glymphtic-lymphatic? system. This system is purported to control CSF- vascular interactions in the brain parenchyma and thus contribute to the overall clearance of the brain of toxicants and metabolic byproducts and allow entry of immune cells into the brain. The ependymal layer appears damaged in the aged brain, yet whether the damage is caused by malfunctioning signals in the overlying CNS tissue, or if ependymal damage causes defects in neurons and glia in the CNS remain unknown. We have developed several genetic mouse models which suggest the ependymal layer may be the root of many problems in the brain interstitium related to various neurodegenerative diseases and during normal aging in the CNS. We will use these models to study this novel concept. Studies in our mouse models have revealed a previously unknown expression and clearance of mucins by ependymal cells in the CNS. Since mucins function to protect against inflammation and infectious diseases in other tissues, our results have led to the central hypothesis that mucin secretion by ependymal cells is required for maintenance and functional integrity of homeostasis in the forebrain during aging, and that disruption of mucin secretion can lead to aberrant function and disease in the CNS. Our project uses a variety of genetic mice, together with cellular, molecular, and biochemical approaches to test our hypothesis. Potential for Broader Impact: Our approaches to understand how aging affects the brain through its monolayer of ependymal cells have wide implications. Disruption of filtration and protective functions of ependymal cells may be the root of a range of pathological conditions that emerge during late stages of aging. Therefore, undertaking the basic cellular mechanisms that control aging of the brain is critical to understanding not only how healthy aging may be controlled by ependymal cells, but also how abnormalities in ependymal aging may lead to devastating diseases such as Alzheimer?s. Moreover, the mechanisms we study can be harnessed to develop novel aging therapeutics by targeting ependymal functions selectively.

Public Health Relevance

This research proposal explores the role of ependymal cells, a monolayer of epithelium in the brain that is thought to help protect the brain by regulation of its homeostasis during various stages of life. We have discovered that protective and supportive functions of ependymal cells can be manipulated through genetic perturbation of these cells, which can result in insult to the overlying brain interstitium including the emergence of markers of stress, inflammation, and neuroimmune responses. Understanding and identifying novel regulators of ependymal functions, therefore is critical for understanding normal brain aging, as well as the paradigm-shifting notion that damage to the monolayer of ependymal cells may be the root of multiple age- associated diseases in the brain, such as Alzheimer?s disease and various forms of dementias. Our studies may result in new targeted therapies for age-associated neurodegenerative diseases that underlie cognitive decline during aging.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
5R01NS098370-05
Application #
9899335
Study Section
Cellular and Molecular Biology of Glia Study Section (CMBG)
Program Officer
Mcgavern, Linda
Project Start
2016-07-01
Project End
2021-03-31
Budget Start
2020-04-01
Budget End
2021-03-31
Support Year
5
Fiscal Year
2020
Total Cost
Indirect Cost

  Institution

Name
North Carolina State University Raleigh
Department
Veterinary Sciences
Type
Schools of Veterinary Medicine
DUNS #
042092122
City
Raleigh
State
NC
Country
United States
Zip Code
27695

  Publications

Muthusamy, Nagendran; Brumm, Andrew; Zhang, Xuying et al. (2018) Foxj1 expressing ependymal cells do not contribute new cells to sites of injury or stroke in the mouse forebrain. Sci Rep 8:1766
Brudvig, J J; Cain, J T; Sears, R M et al. (2018) MARCKS regulates neuritogenesis and interacts with a CDC42 signaling network. Sci Rep 8:13278
Ren, Yilong; Ao, Yan; O'Shea, Timothy M et al. (2017) Ependymal cell contribution to scar formation after spinal cord injury is minimal, local and dependent on direct ependymal injury. Sci Rep 7:41122
Muthusamy, Nagendran; Zhang, Xuying; Johnson, Caroline A et al. (2017) Developmentally defined forebrain circuits regulate appetitive and aversive olfactory learning. Nat Neurosci 20:20-23
Dwyer, Noelle D; Chen, Bin; Chou, Shen-Ju et al. (2016) Neural Stem Cells to Cerebral Cortex: Emerging Mechanisms Regulating Progenitor Behavior and Productivity. J Neurosci 36:11394-11401