Cross-Platform Synaptic Network Analysis of Human Entorhinal Cortex Identifies TWF2 as a Modulator of Dendritic Spine Length

Proteomic studies using postmortem human brain tissue samples have yielded robust assessments of the aging and neurodegenerative disease(s) proteomes. While these analyses provide lists of molecular alterations in human conditions, like Alzheimer's disease (AD), identifying individual proteins...

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Autores principales: Walker, Courtney K., Greathouse, Kelsey M., Tuscher, Jennifer J., Dammer, Eric B., Weber, Audrey J., Liu, Evan, Curtis, Kendall A., Boros, Benjamin D., Freeman, Cameron D., Seo, Jung Vin, Ramdas, Raksha, Hurst, Cheyenne, Duong, Duc M., Gearing, Marla, Murchison, Charles F., Day, Jeremy J., Seyfried, Nicholas T., Herskowitz, Jeremy H.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Society for Neuroscience 2023
Materias:
Research Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10198456/
https://www.ncbi.nlm.nih.gov/pubmed/37055180
http://dx.doi.org/10.1523/JNEUROSCI.2102-22.2023
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author Walker, Courtney K.
Greathouse, Kelsey M.
Tuscher, Jennifer J.
Dammer, Eric B.
Weber, Audrey J.
Liu, Evan
Curtis, Kendall A.
Boros, Benjamin D.
Freeman, Cameron D.
Seo, Jung Vin
Ramdas, Raksha
Hurst, Cheyenne
Duong, Duc M.
Gearing, Marla
Murchison, Charles F.
Day, Jeremy J.
Seyfried, Nicholas T.
Herskowitz, Jeremy H.
author_facet Walker, Courtney K.
Greathouse, Kelsey M.
Tuscher, Jennifer J.
Dammer, Eric B.
Weber, Audrey J.
Liu, Evan
Curtis, Kendall A.
Boros, Benjamin D.
Freeman, Cameron D.
Seo, Jung Vin
Ramdas, Raksha
Hurst, Cheyenne
Duong, Duc M.
Gearing, Marla
Murchison, Charles F.
Day, Jeremy J.
Seyfried, Nicholas T.
Herskowitz, Jeremy H.
author_sort Walker, Courtney K.
collection PubMed
description Proteomic studies using postmortem human brain tissue samples have yielded robust assessments of the aging and neurodegenerative disease(s) proteomes. While these analyses provide lists of molecular alterations in human conditions, like Alzheimer's disease (AD), identifying individual proteins that affect biological processes remains a challenge. To complicate matters, protein targets may be highly understudied and have limited information on their function. To address these hurdles, we sought to establish a blueprint to aid selection and functional validation of targets from proteomic datasets. A cross-platform pipeline was engineered to focus on synaptic processes in the entorhinal cortex (EC) of human patients, including controls, preclinical AD, and AD cases. Label-free quantification mass spectrometry (MS) data (n = 2260 proteins) was generated on synaptosome fractionated tissue from Brodmann area 28 (BA28; n = 58 samples). In parallel, dendritic spine density and morphology was measured in the same individuals. Weighted gene co-expression network analysis was used to construct a network of protein co-expression modules that were correlated with dendritic spine metrics. Module-trait correlations were used to guide unbiased selection of Twinfilin-2 (TWF2), which was the top hub protein of a module that positively correlated with thin spine length. Using CRISPR-dCas9 activation strategies, we demonstrated that boosting endogenous TWF2 protein levels in primary hippocampal neurons increased thin spine length, thus providing experimental validation for the human network analysis. Collectively, this study describes alterations in dendritic spine density and morphology as well as synaptic proteins and phosphorylated tau from the entorhinal cortex of preclinical and advanced stage AD patients. SIGNIFICANCE STATEMENT Proteomic studies can yield vast lists of molecules that are altered under various experimental or disease conditions. Here, we provide a blueprint to facilitate mechanistic validation of protein targets from human brain proteomic datasets. We conducted a proteomic analysis of human entorhinal cortex (EC) samples spanning cognitively normal and Alzheimer's disease (AD) cases with a comparison of dendritic spine morphology in the same samples. Network integration of proteomics with dendritic spine measurements allowed for unbiased discovery of Twinfilin-2 (TWF2) as a regulator of dendritic spine length. A proof-of-concept experiment in cultured neurons demonstrated that altering Twinfilin-2 protein level induced corresponding changes in dendritic spine length, thus providing experimental validation for the computational framework.
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spelling pubmed-101984562023-05-20 Cross-Platform Synaptic Network Analysis of Human Entorhinal Cortex Identifies TWF2 as a Modulator of Dendritic Spine Length Walker, Courtney K. Greathouse, Kelsey M. Tuscher, Jennifer J. Dammer, Eric B. Weber, Audrey J. Liu, Evan Curtis, Kendall A. Boros, Benjamin D. Freeman, Cameron D. Seo, Jung Vin Ramdas, Raksha Hurst, Cheyenne Duong, Duc M. Gearing, Marla Murchison, Charles F. Day, Jeremy J. Seyfried, Nicholas T. Herskowitz, Jeremy H. J Neurosci Research Articles Proteomic studies using postmortem human brain tissue samples have yielded robust assessments of the aging and neurodegenerative disease(s) proteomes. While these analyses provide lists of molecular alterations in human conditions, like Alzheimer's disease (AD), identifying individual proteins that affect biological processes remains a challenge. To complicate matters, protein targets may be highly understudied and have limited information on their function. To address these hurdles, we sought to establish a blueprint to aid selection and functional validation of targets from proteomic datasets. A cross-platform pipeline was engineered to focus on synaptic processes in the entorhinal cortex (EC) of human patients, including controls, preclinical AD, and AD cases. Label-free quantification mass spectrometry (MS) data (n = 2260 proteins) was generated on synaptosome fractionated tissue from Brodmann area 28 (BA28; n = 58 samples). In parallel, dendritic spine density and morphology was measured in the same individuals. Weighted gene co-expression network analysis was used to construct a network of protein co-expression modules that were correlated with dendritic spine metrics. Module-trait correlations were used to guide unbiased selection of Twinfilin-2 (TWF2), which was the top hub protein of a module that positively correlated with thin spine length. Using CRISPR-dCas9 activation strategies, we demonstrated that boosting endogenous TWF2 protein levels in primary hippocampal neurons increased thin spine length, thus providing experimental validation for the human network analysis. Collectively, this study describes alterations in dendritic spine density and morphology as well as synaptic proteins and phosphorylated tau from the entorhinal cortex of preclinical and advanced stage AD patients. SIGNIFICANCE STATEMENT Proteomic studies can yield vast lists of molecules that are altered under various experimental or disease conditions. Here, we provide a blueprint to facilitate mechanistic validation of protein targets from human brain proteomic datasets. We conducted a proteomic analysis of human entorhinal cortex (EC) samples spanning cognitively normal and Alzheimer's disease (AD) cases with a comparison of dendritic spine morphology in the same samples. Network integration of proteomics with dendritic spine measurements allowed for unbiased discovery of Twinfilin-2 (TWF2) as a regulator of dendritic spine length. A proof-of-concept experiment in cultured neurons demonstrated that altering Twinfilin-2 protein level induced corresponding changes in dendritic spine length, thus providing experimental validation for the computational framework. Society for Neuroscience 2023-05-17 /pmc/articles/PMC10198456/ /pubmed/37055180 http://dx.doi.org/10.1523/JNEUROSCI.2102-22.2023 Text en Copyright © 2023 Walker et al. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution 4.0 International license (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution and reproduction in any medium provided that the original work is properly attributed.
spellingShingle Research Articles
Walker, Courtney K.
Greathouse, Kelsey M.
Tuscher, Jennifer J.
Dammer, Eric B.
Weber, Audrey J.
Liu, Evan
Curtis, Kendall A.
Boros, Benjamin D.
Freeman, Cameron D.
Seo, Jung Vin
Ramdas, Raksha
Hurst, Cheyenne
Duong, Duc M.
Gearing, Marla
Murchison, Charles F.
Day, Jeremy J.
Seyfried, Nicholas T.
Herskowitz, Jeremy H.
Cross-Platform Synaptic Network Analysis of Human Entorhinal Cortex Identifies TWF2 as a Modulator of Dendritic Spine Length
title Cross-Platform Synaptic Network Analysis of Human Entorhinal Cortex Identifies TWF2 as a Modulator of Dendritic Spine Length
title_full Cross-Platform Synaptic Network Analysis of Human Entorhinal Cortex Identifies TWF2 as a Modulator of Dendritic Spine Length
title_fullStr Cross-Platform Synaptic Network Analysis of Human Entorhinal Cortex Identifies TWF2 as a Modulator of Dendritic Spine Length
title_full_unstemmed Cross-Platform Synaptic Network Analysis of Human Entorhinal Cortex Identifies TWF2 as a Modulator of Dendritic Spine Length
title_short Cross-Platform Synaptic Network Analysis of Human Entorhinal Cortex Identifies TWF2 as a Modulator of Dendritic Spine Length
title_sort cross-platform synaptic network analysis of human entorhinal cortex identifies twf2 as a modulator of dendritic spine length
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10198456/
https://www.ncbi.nlm.nih.gov/pubmed/37055180
http://dx.doi.org/10.1523/JNEUROSCI.2102-22.2023
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