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Comorbidity network analyses of global rheumatoid arthritis and Type 2 diabetes reveal IL2 & IL6 as common role players

Comorbidities are associated with harder clinical management, worse health outcomes and an overall increase in healthcare expenditure. Here, we present a novel method of finding the common key genes and pathways via comorbidity network analyses. Essentially, we deployed data from the RAvariome datab...

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Main Authors: Liew, Tuck Onn *, Mishra, Rohit, Lahiri, Chandrajit *
Other Authors: Rojas, I.
Format: Book Section
Published: Springer 2020
Subjects:
QH301 Biology
Online Access:http://eprints.sunway.edu.my/1433/
http://doi.org/10.1007/978-3-030-45385-5_21
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spelling my.sunway.eprints.14332020-09-30T07:42:45Z http://eprints.sunway.edu.my/1433/ Comorbidity network analyses of global rheumatoid arthritis and Type 2 diabetes reveal IL2 & IL6 as common role players Liew, Tuck Onn * Mishra, Rohit Lahiri, Chandrajit * QH301 Biology Comorbidities are associated with harder clinical management, worse health outcomes and an overall increase in healthcare expenditure. Here, we present a novel method of finding the common key genes and pathways via comorbidity network analyses. Essentially, we deployed data from the RAvariome database and Type 2 Diabetes Knowledge Portal for mutually exclusive interpopulation RA and T2D susceptibility genes, respectively. Protein interactomes (PIN) are built by mapping direct interactions between the above gene products and their interacting partners, along with a comorbid network combining both RA and T2D PIN. Network centrality analyses of all PIN projected 18 overlapping proteins with IL-6 and IL-2 being the common key role players found in the comorbid PIN, despite being exclusive to our curated RA susceptible gene list. Subsequent pathway analyses revealed the involvement of cellular senescence, MAPK and AGE-RAGE signalling in diabetic complications. We conclude that RA and T2D susceptible genes do not necessarily translate into indispensable proteins in their induced individual or comorbid diseased networks, but those of RA can outcompete T2D susceptible genes despite the much larger T2D component in the comorbid network. Our method is a unique approach to find key genes/proteins and implicated pathways in disease comorbidities. Springer Rojas, I. Valenzuela, O. Rojas, F. Herrera, L. Ortuno, F. 2020-04-30 Book Section PeerReviewed Liew, Tuck Onn * and Mishra, Rohit and Lahiri, Chandrajit * (2020) Comorbidity network analyses of global rheumatoid arthritis and Type 2 diabetes reveal IL2 & IL6 as common role players. In: Bioinformatics and Biomedical Engineering. IWBBIO 2020. Lecture Notes in Computer Science, vol 12108. Springer, Cham, pp. 227-236. ISBN 978-3-030-45385-5 http://doi.org/10.1007/978-3-030-45385-5_21 doi:10.1007/978-3-030-45385-5_21
institution Sunway University
building Sunway Campus Library
collection Institutional Repository
continent Asia
country Malaysia
content_provider Sunway University
content_source Sunway Institutional Repository
url_provider http://eprints.sunway.edu.my/
topic QH301 Biology
spellingShingle QH301 Biology
Liew, Tuck Onn *
Mishra, Rohit
Lahiri, Chandrajit *
Comorbidity network analyses of global rheumatoid arthritis and Type 2 diabetes reveal IL2 & IL6 as common role players
description Comorbidities are associated with harder clinical management, worse health outcomes and an overall increase in healthcare expenditure. Here, we present a novel method of finding the common key genes and pathways via comorbidity network analyses. Essentially, we deployed data from the RAvariome database and Type 2 Diabetes Knowledge Portal for mutually exclusive interpopulation RA and T2D susceptibility genes, respectively. Protein interactomes (PIN) are built by mapping direct interactions between the above gene products and their interacting partners, along with a comorbid network combining both RA and T2D PIN. Network centrality analyses of all PIN projected 18 overlapping proteins with IL-6 and IL-2 being the common key role players found in the comorbid PIN, despite being exclusive to our curated RA susceptible gene list. Subsequent pathway analyses revealed the involvement of cellular senescence, MAPK and AGE-RAGE signalling in diabetic complications. We conclude that RA and T2D susceptible genes do not necessarily translate into indispensable proteins in their induced individual or comorbid diseased networks, but those of RA can outcompete T2D susceptible genes despite the much larger T2D component in the comorbid network. Our method is a unique approach to find key genes/proteins and implicated pathways in disease comorbidities.
author2 Rojas, I.
author_facet Rojas, I.
Liew, Tuck Onn *
Mishra, Rohit
Lahiri, Chandrajit *
format Book Section
author Liew, Tuck Onn *
Mishra, Rohit
Lahiri, Chandrajit *
author_sort Liew, Tuck Onn *
title Comorbidity network analyses of global rheumatoid arthritis and Type 2 diabetes reveal IL2 & IL6 as common role players
title_short Comorbidity network analyses of global rheumatoid arthritis and Type 2 diabetes reveal IL2 & IL6 as common role players
title_full Comorbidity network analyses of global rheumatoid arthritis and Type 2 diabetes reveal IL2 & IL6 as common role players
title_fullStr Comorbidity network analyses of global rheumatoid arthritis and Type 2 diabetes reveal IL2 & IL6 as common role players
title_full_unstemmed Comorbidity network analyses of global rheumatoid arthritis and Type 2 diabetes reveal IL2 & IL6 as common role players
title_sort comorbidity network analyses of global rheumatoid arthritis and type 2 diabetes reveal il2 & il6 as common role players
publisher Springer
publishDate 2020
url http://eprints.sunway.edu.my/1433/
http://doi.org/10.1007/978-3-030-45385-5_21
_version_ 1680323437499777024
score 13.211869

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