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Distinguishing and Biochemical Phenotype Analysis of Epilepsy Patients Using a Novel Serum Profiling Platform

Diagnosis of non-symptomatic epilepsy includes a history of two or more seizures and brain imaging to rule out structural changes like trauma, tumor, infection. Such analysis can be problematic. It is important to develop capabilities to help identify non-symptomatic epilepsy in order to better moni...

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Autores principales: Hanas, Jay S., Hocker, James R. S., Vannarath, Christian, Evangeline, Betcy, Prabhakaran, Vasudevan, Oommen, Anna, Couch, James, Anderson, Michael, Rajshekhar, Vedantam, Carabin, Hélène, Drevets, Douglas
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7464346/
https://www.ncbi.nlm.nih.gov/pubmed/32751954
http://dx.doi.org/10.3390/brainsci10080504
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author Hanas, Jay S.
Hocker, James R. S.
Vannarath, Christian
Evangeline, Betcy
Prabhakaran, Vasudevan
Oommen, Anna
Couch, James
Anderson, Michael
Rajshekhar, Vedantam
Carabin, Hélène
Drevets, Douglas
author_facet Hanas, Jay S.
Hocker, James R. S.
Vannarath, Christian
Evangeline, Betcy
Prabhakaran, Vasudevan
Oommen, Anna
Couch, James
Anderson, Michael
Rajshekhar, Vedantam
Carabin, Hélène
Drevets, Douglas
author_sort Hanas, Jay S.
collection PubMed
description Diagnosis of non-symptomatic epilepsy includes a history of two or more seizures and brain imaging to rule out structural changes like trauma, tumor, infection. Such analysis can be problematic. It is important to develop capabilities to help identify non-symptomatic epilepsy in order to better monitor and understand the condition. This understanding could lead to improved diagnostics and therapeutics. Serum mass peak profiling was performed using electrospray ionization mass spectrometry (ESI-MS). A comparison of sera mass peaks between epilepsy and control groups was performed via leave one [serum sample] out cross-validation (LOOCV). MS/MS peptide analysis was performed on serum mass peaks to compare epilepsy patient and control groups. LOOCV identified significant differences between the epilepsy patient group and control group (p = 10(−22)). This value became non-significant (p = 0.10) when the samples were randomly allocated between the groups and reanalyzed by LOOCV. LOOCV was thus able to distinguish a non-symptomatic epilepsy patient group from a control group based on physiological differences and underlying phenotype. MS/MS was able to identify potential peptide/protein changes involved in this epilepsy versus control comparison, with 70% of the top 100 proteins indicating overall neurologic function. Specifically, peptide/protein sera changes suggested neuro-inflammatory, seizure, ion-channel, synapse, and autoimmune pathways changing between epilepsy patients and controls.
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spelling pubmed-74643462020-09-04 Distinguishing and Biochemical Phenotype Analysis of Epilepsy Patients Using a Novel Serum Profiling Platform Hanas, Jay S. Hocker, James R. S. Vannarath, Christian Evangeline, Betcy Prabhakaran, Vasudevan Oommen, Anna Couch, James Anderson, Michael Rajshekhar, Vedantam Carabin, Hélène Drevets, Douglas Brain Sci Article Diagnosis of non-symptomatic epilepsy includes a history of two or more seizures and brain imaging to rule out structural changes like trauma, tumor, infection. Such analysis can be problematic. It is important to develop capabilities to help identify non-symptomatic epilepsy in order to better monitor and understand the condition. This understanding could lead to improved diagnostics and therapeutics. Serum mass peak profiling was performed using electrospray ionization mass spectrometry (ESI-MS). A comparison of sera mass peaks between epilepsy and control groups was performed via leave one [serum sample] out cross-validation (LOOCV). MS/MS peptide analysis was performed on serum mass peaks to compare epilepsy patient and control groups. LOOCV identified significant differences between the epilepsy patient group and control group (p = 10(−22)). This value became non-significant (p = 0.10) when the samples were randomly allocated between the groups and reanalyzed by LOOCV. LOOCV was thus able to distinguish a non-symptomatic epilepsy patient group from a control group based on physiological differences and underlying phenotype. MS/MS was able to identify potential peptide/protein changes involved in this epilepsy versus control comparison, with 70% of the top 100 proteins indicating overall neurologic function. Specifically, peptide/protein sera changes suggested neuro-inflammatory, seizure, ion-channel, synapse, and autoimmune pathways changing between epilepsy patients and controls. MDPI 2020-07-31 /pmc/articles/PMC7464346/ /pubmed/32751954 http://dx.doi.org/10.3390/brainsci10080504 Text en © 2020 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Hanas, Jay S.
Hocker, James R. S.
Vannarath, Christian
Evangeline, Betcy
Prabhakaran, Vasudevan
Oommen, Anna
Couch, James
Anderson, Michael
Rajshekhar, Vedantam
Carabin, Hélène
Drevets, Douglas
Distinguishing and Biochemical Phenotype Analysis of Epilepsy Patients Using a Novel Serum Profiling Platform
title Distinguishing and Biochemical Phenotype Analysis of Epilepsy Patients Using a Novel Serum Profiling Platform
title_full Distinguishing and Biochemical Phenotype Analysis of Epilepsy Patients Using a Novel Serum Profiling Platform
title_fullStr Distinguishing and Biochemical Phenotype Analysis of Epilepsy Patients Using a Novel Serum Profiling Platform
title_full_unstemmed Distinguishing and Biochemical Phenotype Analysis of Epilepsy Patients Using a Novel Serum Profiling Platform
title_short Distinguishing and Biochemical Phenotype Analysis of Epilepsy Patients Using a Novel Serum Profiling Platform
title_sort distinguishing and biochemical phenotype analysis of epilepsy patients using a novel serum profiling platform
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7464346/
https://www.ncbi.nlm.nih.gov/pubmed/32751954
http://dx.doi.org/10.3390/brainsci10080504
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