Open-access Glymphatic system waste clearance and Alzheimer’s disease

The clearance of extracellular material from the brain has been a topic of great interest in the scientific community. Illif et al. recently described the role of the glymphatic system in this clearence,1 which consists of a peri-arterial flow of cerebral spinal fluid (CSF) driven by the pulsatility of the arterial wall (Figure 1). The fluid exchange occurring in the glymphatic system ultimately helps maintain homeostasis in the central nervous system by removing toxic components and excessive proteins, such as amyloid-beta (Aβ), α-synuclein, and tau.2 It has been shown that glymphatic fluid leaves the brain through peri-venous spaces and ultimately leaves the central nervous system into the deep cervical lymph node through lymphatic vessels surrounding the skull.3 It has been speculated that through the excretion of excessive proteins, the glymphatic system may prevent proteins from aggregating in the brain’s interstitial spaces.

Figure 1
The glymphatic system and waste clearance. The glymphatic system is considered a waste clearance system that removes soluble proteins and metabolites from the central nervous system by utilizing a system of perivascular channels generated by astrocytes. AQP4 channels are found in the endfeet of astrocytes and facilitate fluid flow, leading to waste clearance and distribution of macromolecules within the brain parenchyma. AQP4 = aquaporin-4 water channels.

Alzheimer’s disease (AD) is typically characterized by brain accumulation of Aβ protein in the form of plaques and tau protein in the form of neurofibrillary tangles, which leads to brain degeneration and eventually cognitive decline.4,5 AD patients are known to have altered CSF flow, and impaired brain clearance is postulated as one cause of AD-related protein aggregation.6 In addition, Aβ accumulation may occur in the vascular space, leading to cerebral amyloid angiopathy, which may reduce arterial pulsation, the driving force of the glymphatic system.1,2,7 Recent studies have identified that as the brain ages, the efficiency of perivascular fluid exchange within the glymphatic system significantly reduces, leading to a reduction in Aβ clearance while production remains constant.6 Taken together, these observations suggest that glymphatic system waste management dysfunction has a role in the pathogenesis of AD. In preclinical observations of the glymphatic system, CSF intermixes with the interstitial, spinal fluid through a process that utilizes aquaporin-4 water channels (AQP4). AQP4 is a water channel protein found in the endfeet of astrocytes covering the cerebral vasculature and perivascular spaces of the brain that is believed to be driven by cerebral arterial pulsation. AQP4 channels contribute to brain homeostasis by acting as selectively permeable water channels that facilitate water transport across the plasma membrane and manage the exchange of brain-specific extracellular fluid, such as through the influx of CSF and the efflux of interstitial and spinal fluid.8 Human studies have shown reduced polarization and modified expression of AQP4 in AD patients.9 Reduced perivascular AQP4 levels were found in the frontal cortex of AD patients in a post-mortem study, while preserved AQP4 levels were found in those who remained cognitively intact.9 In addition, single nucleotide polymorphisms of the AQP4 gene have been associated with Aβ production and cognitive decline.10 These results suggest AQP4 as a potential target to rectify glymphatic system impairment in AD patients.

To conclude, the link between the glymphatic system and protein aggregation in AD still has many unresolved issues, including the need for a better understanding of fluid dynamics and artifacts when analyzing histological data. Currently, the waste clearance role that the glymphatic system plays via AQP4 seems associated with central nervous system homeostasis and balanced protein accumulation, including Aβ, a hallmark of AD. Targeting the brain’s waste removal system is an attractive option because it has the potential to decrease aggregation of different proteins in bulk without the need for specific transporters. If successful, this could alleviate the brain burden of multiple proteinopathies. This approach aligns with the notion that AD is a multifactorial condition in which multiple brain processes play a role in dementia symptoms.11

References

  • 1 Iliff JJ, Wang M, Liao Y, Plogg BA, Peng W, Gundersen GA, et al. A paravascular pathway facilitates CSF flow through the brain parenchyma and the clearance of interstitial solutes, including amyloid β. Sci Transl Med. 2012;4:147ra111.
  • 2 Iliff JJ, Wang M, Zeppenfeld DM, Venkataraman A, Plog BA, Liao Y, et al. Cerebral arterial pulsation drives paravascular CSF-interstitial fluid exchange in the murine brain. J Neurosci. 2013;33:18190-9.
  • 3 Mestre H, Mori Y, Nedergaard M. The brain’s glymphatic system: current controversies. Trends Neurosci. 2020;43:458-66.
  • 4 Knopman DS, Amieva H, Petersen RC, Chételat G, Holtzman DM, Hyman BT, et al. Alzheimer disease. Nat Rev Dis Primers. 2021;7:33.
  • 5 Hablitz LM, Plá V, Giannetto M, Vinitsky HS, Stæger FF, Metcalfe T, et al. Circadian control of brain glymphatic and lymphatic fluid flow. Nat Commun. 2020;11:4411.
  • 6 Hampel H, Hardy J, Blennow K, Chen C, Perry G, Kim SH, et al. The amyloid-β pathway in Alzheimer’s disease. Mol Psychiatry. 2021;26:5481-503.
  • 7 Reeves BC, Karimy JK, Kundishora AJ, Mestre H, Cerci HM, Matouk C, et al. Glymphatic system impairment in Alzheimer’s disease and idiopathic normal pressure hydrocephalus. Trends Mol Med. 2020;26:285-95.
  • 8 Mestre H, Hablitz LM, Xavier AL, Feng W, Zou W, Pu T, et al. Aquaporin-4-dependent glymphatic solute transport in the rodent brain. Elife. 2018;7:e40070.
  • 9 Zeppenfeld DM, Simon M, Haswell JD, D’Abreo D, Murchison C, Quinn JF, et al. Association of perivascular localization of aquaporin-4 with cognition and Alzheimer disease in aging brains. JAMA. 2017;74:91-9.
  • 10 Salman MM, Kitchen P, Halsey A, Wang MX, Törnroth-Horsefield S, Conner AC, et al. Emerging roles for dynamic aquaporin-4 subcellular relocalization in CNS water homeostasis. Brain. 2022;145:64-75.
  • 11 Schneider JA, Arvanitakis Z, Bang W, Bennett DA. Mixed brain pathologies account for most dementia cases in community-dwelling older persons. Neurology. 2007;69:2197-204.

Publication Dates

  • Publication in this collection
    17 Nov 2023
  • Date of issue
    Sep-Oct 2023

History

  • Received
    12 Apr 2023
  • Accepted
    12 Apr 2023
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