Incorporation of [ 3H]Valproic Acid into Lipids in GT1–7 Neurons
Valproic acid (2-propylpentanoic acid, valproate, VPA), an 8-carbon, branched chain fatty acid, is effectively used in the treatment of mania and epilepsy. The biochemical mechanisms by which this drug has its therapeutic effects are not yet established. The purpose of this study was to partially ch...
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Published in | Biochemical pharmacology Vol. 56; no. 2; pp. 207 - 212 |
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Main Authors | , , , |
Format | Journal Article |
Language | English |
Published |
New York, NY
Elsevier Inc
15.07.1998
Elsevier Science |
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Abstract | Valproic acid (2-propylpentanoic acid, valproate, VPA), an 8-carbon, branched chain fatty acid, is effectively used in the treatment of mania and epilepsy. The biochemical mechanisms by which this drug has its therapeutic effects are not yet established. The purpose of this study was to partially characterize the incorporation of [
3H]VPA into phospholipids of GT1–7 neurons, an immortalized hypothalamic cell line. GT1–7 neurons were grown to confluence in culture dishes, and then were incubated with various concentrations of [
3H]VPA between 10 and 400 μg/mL for various times up to 20 hr. Total lipids were extracted and phospholipids were separated from neutral lipids using TLC. Our results indicate that [
3H]VPA (10 μg/mL) was incorporated into phospholipids of GT1–7 neurons in a time-dependent and saturable manner over 300 min. Subsequent separation of the lipid fraction by TLC indicated that 44.4% of the radioactivity taken up by the cells was incorporated into phospholipids and neutral lipids. One of the phospholipids migrated with a slightly lower
R
f
value than authentic phosphatidylcholine. Our results show that the incorporation of VPA into phospholipids and glycerides was linear with VPA concentrations from 10 to 400 μg/mL. Finally, we synthesized 1-acyl-2-valproyl-
sn-glycero-3-phosphocholine and validated its structure with nuclear magnetic resonance and electrospray mass spectrometry to verify the structure of this compound, confirming that this compound is structurally possible. We conclude that VPA is incorporated into lipids in GT1–7 neurons and discuss the possible effects of valproyl phospholipids on neuronal functional properties. |
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AbstractList | Valproic acid (2-propylpentanoic acid, valproate, VPA), an 8-carbon, branched chain fatty acid, is effectively used in the treatment of mania and epilepsy. The biochemical mechanisms by which this drug has its therapeutic effects are not yet established. The purpose of this study was to partially characterize the incorporation of [3H]VPA into phospholipids of GT1-7 neurons, an immortalized hypothalamic cell line. GT1-7 neurons were grown to confluence in culture dishes, and then were incubated with various concentrations of [3H]VPA between 10 and 400 microg/mL for various times up to 20 hr. Total lipids were extracted and phospholipids were separated from neutral lipids using TLC. Our results indicate that [3H]VPA (10 microg/mL) was incorporated into phospholipids of GT1-7 neurons in a time-dependent and saturable manner over 300 min. Subsequent separation of the lipid fraction by TLC indicated that 44.4% of the radioactivity taken up by the cells was incorporated into phospholipids and neutral lipids. One of the phospholipids migrated with a slightly lower Rf value than authentic phosphatidylcholine. Our results show that the incorporation of VPA into phospholipids and glycerides was linear with VPA concentrations from 10 to 400 microg/mL. Finally, we synthesized 1-acyl-2-valproyl-sn-glycero-3-phosphocholine and validated its structure with nuclear magnetic resonance and electrospray mass spectrometry to verify the structure of this compound, confirming that this compound is structurally possible. We conclude that VPA is incorporated into lipids in GT1-7 neurons and discuss the possible effects of valproyl phospholipids on neuronal functional properties. Valproic acid (2-propylpentanoic acid, valproate, VPA), an 8-carbon, branched chain fatty acid, is effectively used in the treatment of mania and epilepsy. The biochemical mechanisms by which this drug has its therapeutic effects are not yet established. The purpose of this study was to partially characterize the incorporation of [ 3H]VPA into phospholipids of GT1–7 neurons, an immortalized hypothalamic cell line. GT1–7 neurons were grown to confluence in culture dishes, and then were incubated with various concentrations of [ 3H]VPA between 10 and 400 μg/mL for various times up to 20 hr. Total lipids were extracted and phospholipids were separated from neutral lipids using TLC. Our results indicate that [ 3H]VPA (10 μg/mL) was incorporated into phospholipids of GT1–7 neurons in a time-dependent and saturable manner over 300 min. Subsequent separation of the lipid fraction by TLC indicated that 44.4% of the radioactivity taken up by the cells was incorporated into phospholipids and neutral lipids. One of the phospholipids migrated with a slightly lower R f value than authentic phosphatidylcholine. Our results show that the incorporation of VPA into phospholipids and glycerides was linear with VPA concentrations from 10 to 400 μg/mL. Finally, we synthesized 1-acyl-2-valproyl- sn-glycero-3-phosphocholine and validated its structure with nuclear magnetic resonance and electrospray mass spectrometry to verify the structure of this compound, confirming that this compound is structurally possible. We conclude that VPA is incorporated into lipids in GT1–7 neurons and discuss the possible effects of valproyl phospholipids on neuronal functional properties. |
Author | Patiris, Marinis Javors, Martin Siafaka-Kapadai, Athanassia Bowden, Charles |
Author_xml | – sequence: 1 givenname: Athanassia surname: Siafaka-Kapadai fullname: Siafaka-Kapadai, Athanassia organization: Department of Chemistry, University of Athens, Athens, Greece – sequence: 2 givenname: Marinis surname: Patiris fullname: Patiris, Marinis organization: Department of Chemistry, University of Athens, Athens, Greece – sequence: 3 givenname: Charles surname: Bowden fullname: Bowden, Charles organization: Departments of Psychiatry and Pharmacology, The University of Texas Health Science Center, San Antonio, TX 78284, U.S.A – sequence: 4 givenname: Martin surname: Javors fullname: Javors, Martin organization: Departments of Psychiatry and Pharmacology, The University of Texas Health Science Center, San Antonio, TX 78284, U.S.A |
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Keywords | epilepsy neuron valproic acid GT1–7 phospholipid lipid hypothalamus mania Nervous system diseases Neuron Epilepsy Central nervous system disease Established cell line Phospholipid Lipids Hypothalamus Valproic acid In vitro Cerebral disorder |
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Snippet | Valproic acid (2-propylpentanoic acid, valproate, VPA), an 8-carbon, branched chain fatty acid, is effectively used in the treatment of mania and epilepsy. The... |
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SubjectTerms | Anticonvulsants - metabolism Anticonvulsants. Antiepileptics. Antiparkinson agents Biological and medical sciences Cell Line, Transformed Chromatography, Thin Layer epilepsy GT1–7 hypothalamus lipid mania Medical sciences neuron Neurons - metabolism Neuropharmacology Pharmacology. Drug treatments phospholipid Phospholipids - metabolism Tritium valproic acid Valproic Acid - metabolism |
Title | Incorporation of [ 3H]Valproic Acid into Lipids in GT1–7 Neurons |
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