Homozygous Expression of Mutant ELOVL4 Leads to Seizures and Death in a Novel Animal Model of Very Long-Chain Fatty Acid Deficiency

Blake R. Hopiavuori; Ferenc Deák; Joseph L. Wilkerson; Richard S. Brush; Nicole A. Rocha-Hopiavuori; Austin R. Hopiavuori; Kathryn G. Ozan; Michael T. Sullivan; Jonathan D. Wren; Constantin Georgescu; Luke Szweda; Vibhudutta Awasthi; Rheal Towner; David M. Sherry; Robert E. Anderson; Martin Paul Agbaga

doi:10.1007/s12035-017-0824-8

Homozygous Expression of Mutant ELOVL4 Leads to Seizures and Death in a Novel Animal Model of Very Long-Chain Fatty Acid Deficiency

Blake R. Hopiavuori
, Ferenc Deák
, Joseph L. Wilkerson
, Richard S. Brush
, Nicole A. Rocha-Hopiavuori
, Austin R. Hopiavuori
, Kathryn G. Ozan
, Michael T. Sullivan
, Jonathan D. Wren
, Constantin Georgescu
, Luke Szweda
, Vibhudutta Awasthi
, Rheal Towner
, David M. Sherry
, Robert E. Anderson
, Martin Paul Agbaga

Research output: Contribution to journal › Article › peer-review

36 Scopus citations

Abstract

Lipids are essential components of the nervous system. However, the functions of very long-chain fatty acids (VLC-FA; ≥ 28 carbons) in the brain are unknown. The enzyme ELOngation of Very Long-chain fatty acids-4 (ELOVL4) catalyzes the rate-limiting step in the biosynthesis of VLC-FA (Agbaga et al., Proc Natl Acad Sci USA 105(35): 12843–12848, 2008; Logan et al., J Lipid Res 55(4): 698–708, 2014), which we identified in the brain as saturated fatty acids (VLC-SFA). Homozygous mutations in ELOVL4 cause severe neuropathology in humans (Ozaki et al., JAMA Neurol 72(7): 797–805, 2015; Mir et al., BMC Med Genet 15: 25, 2014; Cadieux-Dion et al., JAMA Neurol 71(4): 470–475, 2014; Bourassa et al., JAMA Neurol 72(8): 942–943, 2015; Aldahmesh et al., Am J Hum Genet 89(6): 745–750, 2011) and are post-natal lethal in mice (Cameron et al., Int J Biol Sci 3(2): 111–119, 2007; Li et al., Int J Biol Sci 3(2): 120–128, 2007; McMahon et al., Molecular Vision 13: 258–272, 2007; Vasireddy et al., Hum Mol Genet 16(5): 471–482, 2007) from dehydration due to loss of VLC-SFA that comprise the skin permeability barrier. Double transgenic mice with homozygous knock-in of the Stargardt-like macular dystrophy (STDG3; 797-801_AACTT) mutation of Elovl4 with skin-specific rescue of wild-type Elovl4 expression (S⁺Elovl4^mut/mut mice) develop seizures by P19 and die by P21. Electrophysiological analyses of hippocampal slices showed aberrant epileptogenic activity in S⁺Elovl4^mut/mut mice. FM1-43 dye release studies showed that synapses made by cultured hippocampal neurons from S⁺Elovl4^mut/mut mice exhibited accelerated synaptic release kinetics. Supplementation of VLC-SFA to cultured hippocampal neurons from mutant mice rescued defective synaptic release to wild-type rates. Together, these studies establish a critical, novel role for ELOVL4 and its VLC-SFA products in regulating synaptic release kinetics and epileptogenesis. Future studies aimed at understanding the molecular mechanisms by which VLC-SFA regulate synaptic function may provide new targets for improved seizure therapies.

Original language	English (US)
Pages (from-to)	1795-1813
Number of pages	19
Journal	Molecular Neurobiology
Volume	55
Issue number	2
DOIs	https://doi.org/10.1007/s12035-017-0824-8
State	Published - Feb 1 2018
Externally published	Yes

Keywords

Brain lipids
ELOVL4
Seizure
Synaptic dysregulation
Synaptic vesicle fusion kinetics
Very long-chain saturated fatty acids

ASJC Scopus subject areas

Neuroscience (miscellaneous)
Neurology
Cellular and Molecular Neuroscience

Access to Document

10.1007/s12035-017-0824-8

Cite this

Hopiavuori, B. R., Deák, F., Wilkerson, J. L., Brush, R. S., Rocha-Hopiavuori, N. A., Hopiavuori, A. R., Ozan, K. G., Sullivan, M. T., Wren, J. D., Georgescu, C., Szweda, L., Awasthi, V., Towner, R., Sherry, D. M., Anderson, R. E., & Agbaga, M. P. (2018). Homozygous Expression of Mutant ELOVL4 Leads to Seizures and Death in a Novel Animal Model of Very Long-Chain Fatty Acid Deficiency. Molecular Neurobiology, 55(2), 1795-1813. https://doi.org/10.1007/s12035-017-0824-8

Hopiavuori, BR, Deák, F, Wilkerson, JL, Brush, RS, Rocha-Hopiavuori, NA, Hopiavuori, AR, Ozan, KG, Sullivan, MT, Wren, JD, Georgescu, C, Szweda, L, Awasthi, V, Towner, R, Sherry, DM, Anderson, RE & Agbaga, MP 2018, 'Homozygous Expression of Mutant ELOVL4 Leads to Seizures and Death in a Novel Animal Model of Very Long-Chain Fatty Acid Deficiency', Molecular Neurobiology, vol. 55, no. 2, pp. 1795-1813. https://doi.org/10.1007/s12035-017-0824-8

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title = "Homozygous Expression of Mutant ELOVL4 Leads to Seizures and Death in a Novel Animal Model of Very Long-Chain Fatty Acid Deficiency",

abstract = "Lipids are essential components of the nervous system. However, the functions of very long-chain fatty acids (VLC-FA; ≥ 28 carbons) in the brain are unknown. The enzyme ELOngation of Very Long-chain fatty acids-4 (ELOVL4) catalyzes the rate-limiting step in the biosynthesis of VLC-FA (Agbaga et al., Proc Natl Acad Sci USA 105(35): 12843–12848, 2008; Logan et al., J Lipid Res 55(4): 698–708, 2014), which we identified in the brain as saturated fatty acids (VLC-SFA). Homozygous mutations in ELOVL4 cause severe neuropathology in humans (Ozaki et al., JAMA Neurol 72(7): 797–805, 2015; Mir et al., BMC Med Genet 15: 25, 2014; Cadieux-Dion et al., JAMA Neurol 71(4): 470–475, 2014; Bourassa et al., JAMA Neurol 72(8): 942–943, 2015; Aldahmesh et al., Am J Hum Genet 89(6): 745–750, 2011) and are post-natal lethal in mice (Cameron et al., Int J Biol Sci 3(2): 111–119, 2007; Li et al., Int J Biol Sci 3(2): 120–128, 2007; McMahon et al., Molecular Vision 13: 258–272, 2007; Vasireddy et al., Hum Mol Genet 16(5): 471–482, 2007) from dehydration due to loss of VLC-SFA that comprise the skin permeability barrier. Double transgenic mice with homozygous knock-in of the Stargardt-like macular dystrophy (STDG3; 797-801\_AACTT) mutation of Elovl4 with skin-specific rescue of wild-type Elovl4 expression (S+Elovl4mut/mut mice) develop seizures by P19 and die by P21. Electrophysiological analyses of hippocampal slices showed aberrant epileptogenic activity in S+Elovl4mut/mut mice. FM1-43 dye release studies showed that synapses made by cultured hippocampal neurons from S+Elovl4mut/mut mice exhibited accelerated synaptic release kinetics. Supplementation of VLC-SFA to cultured hippocampal neurons from mutant mice rescued defective synaptic release to wild-type rates. Together, these studies establish a critical, novel role for ELOVL4 and its VLC-SFA products in regulating synaptic release kinetics and epileptogenesis. Future studies aimed at understanding the molecular mechanisms by which VLC-SFA regulate synaptic function may provide new targets for improved seizure therapies.",

keywords = "Brain lipids, ELOVL4, Seizure, Synaptic dysregulation, Synaptic vesicle fusion kinetics, Very long-chain saturated fatty acids",

author = "Hopiavuori, \{Blake R.\} and Ferenc De{\'a}k and Wilkerson, \{Joseph L.\} and Brush, \{Richard S.\} and Rocha-Hopiavuori, \{Nicole A.\} and Hopiavuori, \{Austin R.\} and Ozan, \{Kathryn G.\} and Sullivan, \{Michael T.\} and Wren, \{Jonathan D.\} and Constantin Georgescu and Luke Szweda and Vibhudutta Awasthi and Rheal Towner and Sherry, \{David M.\} and Anderson, \{Robert E.\} and Agbaga, \{Martin Paul\}",

note = "Publisher Copyright: {\textcopyright} 2017, The Author(s).",

year = "2018",

month = feb,

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doi = "10.1007/s12035-017-0824-8",

language = "English (US)",

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pages = "1795--1813",

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T1 - Homozygous Expression of Mutant ELOVL4 Leads to Seizures and Death in a Novel Animal Model of Very Long-Chain Fatty Acid Deficiency

AU - Hopiavuori, Blake R.

AU - Deák, Ferenc

AU - Wilkerson, Joseph L.

AU - Brush, Richard S.

AU - Rocha-Hopiavuori, Nicole A.

AU - Hopiavuori, Austin R.

AU - Ozan, Kathryn G.

AU - Sullivan, Michael T.

AU - Wren, Jonathan D.

AU - Georgescu, Constantin

AU - Szweda, Luke

AU - Awasthi, Vibhudutta

AU - Towner, Rheal

AU - Sherry, David M.

AU - Anderson, Robert E.

AU - Agbaga, Martin Paul

PY - 2018/2/1

Y1 - 2018/2/1

N2 - Lipids are essential components of the nervous system. However, the functions of very long-chain fatty acids (VLC-FA; ≥ 28 carbons) in the brain are unknown. The enzyme ELOngation of Very Long-chain fatty acids-4 (ELOVL4) catalyzes the rate-limiting step in the biosynthesis of VLC-FA (Agbaga et al., Proc Natl Acad Sci USA 105(35): 12843–12848, 2008; Logan et al., J Lipid Res 55(4): 698–708, 2014), which we identified in the brain as saturated fatty acids (VLC-SFA). Homozygous mutations in ELOVL4 cause severe neuropathology in humans (Ozaki et al., JAMA Neurol 72(7): 797–805, 2015; Mir et al., BMC Med Genet 15: 25, 2014; Cadieux-Dion et al., JAMA Neurol 71(4): 470–475, 2014; Bourassa et al., JAMA Neurol 72(8): 942–943, 2015; Aldahmesh et al., Am J Hum Genet 89(6): 745–750, 2011) and are post-natal lethal in mice (Cameron et al., Int J Biol Sci 3(2): 111–119, 2007; Li et al., Int J Biol Sci 3(2): 120–128, 2007; McMahon et al., Molecular Vision 13: 258–272, 2007; Vasireddy et al., Hum Mol Genet 16(5): 471–482, 2007) from dehydration due to loss of VLC-SFA that comprise the skin permeability barrier. Double transgenic mice with homozygous knock-in of the Stargardt-like macular dystrophy (STDG3; 797-801_AACTT) mutation of Elovl4 with skin-specific rescue of wild-type Elovl4 expression (S+Elovl4mut/mut mice) develop seizures by P19 and die by P21. Electrophysiological analyses of hippocampal slices showed aberrant epileptogenic activity in S+Elovl4mut/mut mice. FM1-43 dye release studies showed that synapses made by cultured hippocampal neurons from S+Elovl4mut/mut mice exhibited accelerated synaptic release kinetics. Supplementation of VLC-SFA to cultured hippocampal neurons from mutant mice rescued defective synaptic release to wild-type rates. Together, these studies establish a critical, novel role for ELOVL4 and its VLC-SFA products in regulating synaptic release kinetics and epileptogenesis. Future studies aimed at understanding the molecular mechanisms by which VLC-SFA regulate synaptic function may provide new targets for improved seizure therapies.

AB - Lipids are essential components of the nervous system. However, the functions of very long-chain fatty acids (VLC-FA; ≥ 28 carbons) in the brain are unknown. The enzyme ELOngation of Very Long-chain fatty acids-4 (ELOVL4) catalyzes the rate-limiting step in the biosynthesis of VLC-FA (Agbaga et al., Proc Natl Acad Sci USA 105(35): 12843–12848, 2008; Logan et al., J Lipid Res 55(4): 698–708, 2014), which we identified in the brain as saturated fatty acids (VLC-SFA). Homozygous mutations in ELOVL4 cause severe neuropathology in humans (Ozaki et al., JAMA Neurol 72(7): 797–805, 2015; Mir et al., BMC Med Genet 15: 25, 2014; Cadieux-Dion et al., JAMA Neurol 71(4): 470–475, 2014; Bourassa et al., JAMA Neurol 72(8): 942–943, 2015; Aldahmesh et al., Am J Hum Genet 89(6): 745–750, 2011) and are post-natal lethal in mice (Cameron et al., Int J Biol Sci 3(2): 111–119, 2007; Li et al., Int J Biol Sci 3(2): 120–128, 2007; McMahon et al., Molecular Vision 13: 258–272, 2007; Vasireddy et al., Hum Mol Genet 16(5): 471–482, 2007) from dehydration due to loss of VLC-SFA that comprise the skin permeability barrier. Double transgenic mice with homozygous knock-in of the Stargardt-like macular dystrophy (STDG3; 797-801_AACTT) mutation of Elovl4 with skin-specific rescue of wild-type Elovl4 expression (S+Elovl4mut/mut mice) develop seizures by P19 and die by P21. Electrophysiological analyses of hippocampal slices showed aberrant epileptogenic activity in S+Elovl4mut/mut mice. FM1-43 dye release studies showed that synapses made by cultured hippocampal neurons from S+Elovl4mut/mut mice exhibited accelerated synaptic release kinetics. Supplementation of VLC-SFA to cultured hippocampal neurons from mutant mice rescued defective synaptic release to wild-type rates. Together, these studies establish a critical, novel role for ELOVL4 and its VLC-SFA products in regulating synaptic release kinetics and epileptogenesis. Future studies aimed at understanding the molecular mechanisms by which VLC-SFA regulate synaptic function may provide new targets for improved seizure therapies.

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KW - ELOVL4

KW - Seizure

KW - Synaptic dysregulation

KW - Synaptic vesicle fusion kinetics

KW - Very long-chain saturated fatty acids

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U2 - 10.1007/s12035-017-0824-8

DO - 10.1007/s12035-017-0824-8

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Homozygous Expression of Mutant ELOVL4 Leads to Seizures and Death in a Novel Animal Model of Very Long-Chain Fatty Acid Deficiency

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