Hamiltonian energy as an efficient approach to identify the significant key regulators in biological networks.
The topological characteristics of biological networks enable us to identify the key nodes in terms of modularity. However, due to a large size of the biological networks with many hubs and functional modules across intertwined layers within the network, it often becomes difficult to accomplish the...
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doaj-e17460ddc3f2455294ac79808d8697f92021-03-03T19:51:11ZengPublic Library of Science (PLoS)PLoS ONE1932-62032019-01-01148e022146310.1371/journal.pone.0221463Hamiltonian energy as an efficient approach to identify the significant key regulators in biological networks.Shazia HaiderKalaiarasan PonnusamyR K Brojen SinghAnirban ChakrabortiRameshwar N K BamezaiThe topological characteristics of biological networks enable us to identify the key nodes in terms of modularity. However, due to a large size of the biological networks with many hubs and functional modules across intertwined layers within the network, it often becomes difficult to accomplish the task of identifying potential key regulators. We use for the first time a generalized formalism of Hamiltonian Energy (HE) with a recursive approach. The concept, when applied to the Apoptosis Regulatory Gene Network (ARGN), helped us identify 11 Motif hubs (MHs), which influenced the network up to motif levels. The approach adopted allowed to classify MHs into 5 significant motif hubs (S-MHs) and 6 non-significant motif hubs (NS-MHs). The significant motif hubs had a higher HE value and were considered as high-active key regulators; while the non-significant motif hubs had a relatively lower HE value and were considered as low-active key regulators, in network control mechanism. Further, we compared the results of the HE analyses with the topological characterization, after subjecting to the three conditions independently: (i) removing all MHs, (ii) removing only S-MHs, and (iii) removing only NS-MHs from the ARGN. This procedure allowed us to cross-validate the role of 5 S-MHs, NFk-B1, BRCA1, CEBPB, AR, and POU2F1 as the potential key regulators. The changes in HE calculations further showed that the removal of 5 S-MHs could cause perturbation at all levels of the network, a feature not discernible by topological analysis alone.https://doi.org/10.1371/journal.pone.0221463 |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Shazia Haider Kalaiarasan Ponnusamy R K Brojen Singh Anirban Chakraborti Rameshwar N K Bamezai |
spellingShingle |
Shazia Haider Kalaiarasan Ponnusamy R K Brojen Singh Anirban Chakraborti Rameshwar N K Bamezai Hamiltonian energy as an efficient approach to identify the significant key regulators in biological networks. PLoS ONE |
author_facet |
Shazia Haider Kalaiarasan Ponnusamy R K Brojen Singh Anirban Chakraborti Rameshwar N K Bamezai |
author_sort |
Shazia Haider |
title |
Hamiltonian energy as an efficient approach to identify the significant key regulators in biological networks. |
title_short |
Hamiltonian energy as an efficient approach to identify the significant key regulators in biological networks. |
title_full |
Hamiltonian energy as an efficient approach to identify the significant key regulators in biological networks. |
title_fullStr |
Hamiltonian energy as an efficient approach to identify the significant key regulators in biological networks. |
title_full_unstemmed |
Hamiltonian energy as an efficient approach to identify the significant key regulators in biological networks. |
title_sort |
hamiltonian energy as an efficient approach to identify the significant key regulators in biological networks. |
publisher |
Public Library of Science (PLoS) |
series |
PLoS ONE |
issn |
1932-6203 |
publishDate |
2019-01-01 |
description |
The topological characteristics of biological networks enable us to identify the key nodes in terms of modularity. However, due to a large size of the biological networks with many hubs and functional modules across intertwined layers within the network, it often becomes difficult to accomplish the task of identifying potential key regulators. We use for the first time a generalized formalism of Hamiltonian Energy (HE) with a recursive approach. The concept, when applied to the Apoptosis Regulatory Gene Network (ARGN), helped us identify 11 Motif hubs (MHs), which influenced the network up to motif levels. The approach adopted allowed to classify MHs into 5 significant motif hubs (S-MHs) and 6 non-significant motif hubs (NS-MHs). The significant motif hubs had a higher HE value and were considered as high-active key regulators; while the non-significant motif hubs had a relatively lower HE value and were considered as low-active key regulators, in network control mechanism. Further, we compared the results of the HE analyses with the topological characterization, after subjecting to the three conditions independently: (i) removing all MHs, (ii) removing only S-MHs, and (iii) removing only NS-MHs from the ARGN. This procedure allowed us to cross-validate the role of 5 S-MHs, NFk-B1, BRCA1, CEBPB, AR, and POU2F1 as the potential key regulators. The changes in HE calculations further showed that the removal of 5 S-MHs could cause perturbation at all levels of the network, a feature not discernible by topological analysis alone. |
url |
https://doi.org/10.1371/journal.pone.0221463 |
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