TY - JOUR
T1 - Glymphatic distribution of CSF-derived apoE into brain is isoform specific and suppressed during sleep deprivation
AU - Achariyar, Thiyagaragan M.
AU - Li, Baoman
AU - Peng, Weiguo
AU - Verghese, Philip B.
AU - Shi, Yang
AU - McConnell, Evan
AU - Benraiss, Abdellatif
AU - Kasper, Tristan
AU - Song, Wei
AU - Takana, Takahiro
AU - Holtzman, David M.
AU - Nedergaard, Maiken
AU - Deane, Rashid
N1 - Funding Information:
This work was supported by the National Institutes of Health-(1R56NS086924 and R21AG050212 to RD; R01 NS090934, R01AG047644 and NS034467 to DMH; R01NS078167 and R01NS078304 to MN).
Funding Information:
This work was supported by the National Institutes of Health-(1R56NS086924 and R21AG050212 to RD; R01 NS090934, R01AG047644 and NS034467 to DMH; R01NS078167 and R01NS078304 to MN). We thank Sheng Gong for culturing the mouse primary astrocytes. We also thank Dr. Lulu Xie for generating the 2-photon images.
Publisher Copyright:
© 2016 The Author(s).
PY - 2016/12/8
Y1 - 2016/12/8
N2 - Background: Apolipoprotein E (apoE) is a major carrier of cholesterol and essential for synaptic plasticity. In brain, it's expressed by many cells but highly expressed by the choroid plexus and the predominant apolipoprotein in cerebrospinal fluid (CSF). The role of apoE in the CSF is unclear. Recently, the glymphatic system was described as a clearance system whereby CSF and ISF (interstitial fluid) is exchanged via the peri-arterial space and convective flow of ISF clearance is mediated by aquaporin 4 (AQP4), a water channel. We reasoned that this system also serves to distribute essential molecules in CSF into brain. The aim was to establish whether apoE in CSF, secreted by the choroid plexus, is distributed into brain, and whether this distribution pattern was altered by sleep deprivation. Methods: We used fluorescently labeled lipidated apoE isoforms, lenti-apoE3 delivered to the choroid plexus, immunohistochemistry to map apoE brain distribution, immunolabeled cells and proteins in brain, Western blot analysis and ELISA to determine apoE levels and radiolabeled molecules to quantify CSF inflow into brain and brain clearance in mice. Data were statistically analyzed using ANOVA or Student's t- test. Results: We show that the glymphatic fluid transporting system contributes to the delivery of choroid plexus/CSF-derived human apoE to neurons. CSF-delivered human apoE entered brain via the perivascular space of penetrating arteries and flows radially around arteries, but not veins, in an isoform specific manner (apoE2 > apoE3 > apoE4). Flow of apoE around arteries was facilitated by AQP4, a characteristic feature of the glymphatic system. ApoE3, delivered by lentivirus to the choroid plexus and ependymal layer but not to the parenchymal cells, was present in the CSF, penetrating arteries and neurons. The inflow of CSF, which contains apoE, into brain and its clearance from the interstitium were severely suppressed by sleep deprivation compared to the sleep state. Conclusions: Thus, choroid plexus/CSF provides an additional source of apoE and the glymphatic fluid transporting system delivers it to brain via the periarterial space. By implication, failure in this essential physiological role of the glymphatic fluid flow and ISF clearance may also contribute to apoE isoform-specific disorders in the long term.
AB - Background: Apolipoprotein E (apoE) is a major carrier of cholesterol and essential for synaptic plasticity. In brain, it's expressed by many cells but highly expressed by the choroid plexus and the predominant apolipoprotein in cerebrospinal fluid (CSF). The role of apoE in the CSF is unclear. Recently, the glymphatic system was described as a clearance system whereby CSF and ISF (interstitial fluid) is exchanged via the peri-arterial space and convective flow of ISF clearance is mediated by aquaporin 4 (AQP4), a water channel. We reasoned that this system also serves to distribute essential molecules in CSF into brain. The aim was to establish whether apoE in CSF, secreted by the choroid plexus, is distributed into brain, and whether this distribution pattern was altered by sleep deprivation. Methods: We used fluorescently labeled lipidated apoE isoforms, lenti-apoE3 delivered to the choroid plexus, immunohistochemistry to map apoE brain distribution, immunolabeled cells and proteins in brain, Western blot analysis and ELISA to determine apoE levels and radiolabeled molecules to quantify CSF inflow into brain and brain clearance in mice. Data were statistically analyzed using ANOVA or Student's t- test. Results: We show that the glymphatic fluid transporting system contributes to the delivery of choroid plexus/CSF-derived human apoE to neurons. CSF-delivered human apoE entered brain via the perivascular space of penetrating arteries and flows radially around arteries, but not veins, in an isoform specific manner (apoE2 > apoE3 > apoE4). Flow of apoE around arteries was facilitated by AQP4, a characteristic feature of the glymphatic system. ApoE3, delivered by lentivirus to the choroid plexus and ependymal layer but not to the parenchymal cells, was present in the CSF, penetrating arteries and neurons. The inflow of CSF, which contains apoE, into brain and its clearance from the interstitium were severely suppressed by sleep deprivation compared to the sleep state. Conclusions: Thus, choroid plexus/CSF provides an additional source of apoE and the glymphatic fluid transporting system delivers it to brain via the periarterial space. By implication, failure in this essential physiological role of the glymphatic fluid flow and ISF clearance may also contribute to apoE isoform-specific disorders in the long term.
KW - AQP4
KW - Alzheimer's disease
KW - Brain clearance
KW - Glymphatic pathways
KW - Lymphatic system
KW - Sleep/wake
UR - http://www.scopus.com/inward/record.url?scp=85008429122&partnerID=8YFLogxK
U2 - 10.1186/s13024-016-0138-8
DO - 10.1186/s13024-016-0138-8
M3 - Article
C2 - 27931262
AN - SCOPUS:85008429122
SN - 1750-1326
VL - 11
JO - Molecular Neurodegeneration
JF - Molecular Neurodegeneration
IS - 1
M1 - 74
ER -