Post-translational Modification Crosstalk and Hotspots in Sirtuin Interactors Implicated in Cardiovascular Diseases

Sirtuins are protein deacetylases that play a protective role in cardiovascular diseases (CVDs), as well as many other diseases. Absence of sirtuins can lead to hyperacetylation of both nuclear and mitochondrial proteins leading to metabolic dysregulation. The protein post-translational modification...

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Main Authors: Suruchi Aggarwal, Sanjay K. Banerjee, Narayan Chandra Talukdar, Amit Kumar Yadav
Format: Article
Language:English
Published: Frontiers Media S.A. 2020-04-01
Series:Frontiers in Genetics
Subjects:
Online Access:https://www.frontiersin.org/article/10.3389/fgene.2020.00356/full
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spelling doaj-14ac19dca72c4b08af816a28d49089c42020-11-25T02:54:38ZengFrontiers Media S.A.Frontiers in Genetics1664-80212020-04-011110.3389/fgene.2020.00356519883Post-translational Modification Crosstalk and Hotspots in Sirtuin Interactors Implicated in Cardiovascular DiseasesSuruchi Aggarwal0Suruchi Aggarwal1Suruchi Aggarwal2Sanjay K. Banerjee3Narayan Chandra Talukdar4Narayan Chandra Talukdar5Amit Kumar Yadav6Translational Health Science and Technology Institute, NCR Biotech Science Cluster, Faridabad, IndiaDivision of Life Sciences, Institute of Advanced Study in Science and Technology, Guwahati, IndiaDepartment of Molecular Biology and Biotechnology, Cotton University, Guwahati, IndiaTranslational Health Science and Technology Institute, NCR Biotech Science Cluster, Faridabad, IndiaDivision of Life Sciences, Institute of Advanced Study in Science and Technology, Guwahati, IndiaDepartment of Molecular Biology and Biotechnology, Cotton University, Guwahati, IndiaTranslational Health Science and Technology Institute, NCR Biotech Science Cluster, Faridabad, IndiaSirtuins are protein deacetylases that play a protective role in cardiovascular diseases (CVDs), as well as many other diseases. Absence of sirtuins can lead to hyperacetylation of both nuclear and mitochondrial proteins leading to metabolic dysregulation. The protein post-translational modifications (PTMs) are known to crosstalk among each other to bring about complex phenotypic outcomes. Various PTM types such as acetylation, ubiquitination, and phosphorylation, and so on, drive transcriptional regulation and metabolism, but such crosstalks are poorly understood. We integrated protein–protein interactions (PPI) and PTMs from several databases to integrate information on 1,251 sirtuin-interacting proteins, of which 544 are associated with cardiac diseases. Based on the ∼100,000 PTM sites obtained for sirtuin interactors, we observed that the frequency of PTM sites (83 per protein), as well as PTM types (five per protein), is higher than the global average for human proteome. We found that ∼60–70% PTM sites fall into ordered regions. Approximately 83% of the sirtuin interactors contained at least one competitive crosstalk (in situ) site, with half of the sites occurring in CVD-associated proteins. A large proportion of identified crosstalk sites were observed for acetylation and ubiquitination competition. We identified 614 proteins containing PTM hotspots (≥5 PTM sites) and 133 proteins containing crosstalk hotspots (≥3 crosstalk sites). We observed that a large proportion of disease-associated sequence variants were found in PTM motifs of CVD proteins. We identified seven proteins (TP53, LMNA, MAPT, ATP2A2, NCL, APEX1, and HIST1H3A) containing disease-associated variants in PTM and crosstalk hotspots. This is the first comprehensive bioinformatics analysis on sirtuin interactors with respect to PTMs and their crosstalks. This study forms a platform for generating interesting hypotheses that can be tested for a deeper mechanistic understanding gained or derived from big-data analytics.https://www.frontiersin.org/article/10.3389/fgene.2020.00356/fullcardiovascular diseaseshotspotcancerprotein–protein interactionsneurodegenerativemodifications
collection DOAJ
language English
format Article
sources DOAJ
author Suruchi Aggarwal
Suruchi Aggarwal
Suruchi Aggarwal
Sanjay K. Banerjee
Narayan Chandra Talukdar
Narayan Chandra Talukdar
Amit Kumar Yadav
spellingShingle Suruchi Aggarwal
Suruchi Aggarwal
Suruchi Aggarwal
Sanjay K. Banerjee
Narayan Chandra Talukdar
Narayan Chandra Talukdar
Amit Kumar Yadav
Post-translational Modification Crosstalk and Hotspots in Sirtuin Interactors Implicated in Cardiovascular Diseases
Frontiers in Genetics
cardiovascular diseases
hotspot
cancer
protein–protein interactions
neurodegenerative
modifications
author_facet Suruchi Aggarwal
Suruchi Aggarwal
Suruchi Aggarwal
Sanjay K. Banerjee
Narayan Chandra Talukdar
Narayan Chandra Talukdar
Amit Kumar Yadav
author_sort Suruchi Aggarwal
title Post-translational Modification Crosstalk and Hotspots in Sirtuin Interactors Implicated in Cardiovascular Diseases
title_short Post-translational Modification Crosstalk and Hotspots in Sirtuin Interactors Implicated in Cardiovascular Diseases
title_full Post-translational Modification Crosstalk and Hotspots in Sirtuin Interactors Implicated in Cardiovascular Diseases
title_fullStr Post-translational Modification Crosstalk and Hotspots in Sirtuin Interactors Implicated in Cardiovascular Diseases
title_full_unstemmed Post-translational Modification Crosstalk and Hotspots in Sirtuin Interactors Implicated in Cardiovascular Diseases
title_sort post-translational modification crosstalk and hotspots in sirtuin interactors implicated in cardiovascular diseases
publisher Frontiers Media S.A.
series Frontiers in Genetics
issn 1664-8021
publishDate 2020-04-01
description Sirtuins are protein deacetylases that play a protective role in cardiovascular diseases (CVDs), as well as many other diseases. Absence of sirtuins can lead to hyperacetylation of both nuclear and mitochondrial proteins leading to metabolic dysregulation. The protein post-translational modifications (PTMs) are known to crosstalk among each other to bring about complex phenotypic outcomes. Various PTM types such as acetylation, ubiquitination, and phosphorylation, and so on, drive transcriptional regulation and metabolism, but such crosstalks are poorly understood. We integrated protein–protein interactions (PPI) and PTMs from several databases to integrate information on 1,251 sirtuin-interacting proteins, of which 544 are associated with cardiac diseases. Based on the ∼100,000 PTM sites obtained for sirtuin interactors, we observed that the frequency of PTM sites (83 per protein), as well as PTM types (five per protein), is higher than the global average for human proteome. We found that ∼60–70% PTM sites fall into ordered regions. Approximately 83% of the sirtuin interactors contained at least one competitive crosstalk (in situ) site, with half of the sites occurring in CVD-associated proteins. A large proportion of identified crosstalk sites were observed for acetylation and ubiquitination competition. We identified 614 proteins containing PTM hotspots (≥5 PTM sites) and 133 proteins containing crosstalk hotspots (≥3 crosstalk sites). We observed that a large proportion of disease-associated sequence variants were found in PTM motifs of CVD proteins. We identified seven proteins (TP53, LMNA, MAPT, ATP2A2, NCL, APEX1, and HIST1H3A) containing disease-associated variants in PTM and crosstalk hotspots. This is the first comprehensive bioinformatics analysis on sirtuin interactors with respect to PTMs and their crosstalks. This study forms a platform for generating interesting hypotheses that can be tested for a deeper mechanistic understanding gained or derived from big-data analytics.
topic cardiovascular diseases
hotspot
cancer
protein–protein interactions
neurodegenerative
modifications
url https://www.frontiersin.org/article/10.3389/fgene.2020.00356/full
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