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Bioinformatics of non small cell lung cancer and the ras proto-oncogene

Cancer is initiated by activation of oncogenes or inactivation of tumor suppressor genes. Mutations in the K-ras proto-oncogene are responsible for 10–30% of adenocarcinomas. Clinical Findings point to a wide variety of other cancers contributing to lung cancer incidence. Such a scenario makes ident...

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Detalles Bibliográficos
Autores principales: Kashyap, Amita, Bujamma, D, Babu M, Naresh
Lenguaje:eng
Publicado: Springer 2015
Materias:
Acceso en línea:https://dx.doi.org/10.1007/978-981-4585-08-8
http://cds.cern.ch/record/1968750
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author Kashyap, Amita
Bujamma, D
Babu M, Naresh
author_facet Kashyap, Amita
Bujamma, D
Babu M, Naresh
author_sort Kashyap, Amita
collection CERN
description Cancer is initiated by activation of oncogenes or inactivation of tumor suppressor genes. Mutations in the K-ras proto-oncogene are responsible for 10–30% of adenocarcinomas. Clinical Findings point to a wide variety of other cancers contributing to lung cancer incidence. Such a scenario makes identification of lung cancer difficult and thus identifying its mechanisms can contribute to the society. Identifying unique conserved patterns common to contributing proto-oncogenes may further be a boon to Pharmacogenomics and pharmacoinformatics. This calls for ab initio/de novo drug discovery that in turn will require a comprehensive in silico approach of Sequence, Domain, Phylogenetic and Structural analysis of the receptors, ligand screening and optimization and detailed Docking studies. This brief involves extensive role of the RAS subfamily that includes a set of proteins, which cause an over expression of cancer-causing genes like M-ras and initiate tumour formation in lungs. SNP Studies and Structure based drug discovery will also be undertaken.
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publishDate 2015
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spelling cern-19687502021-04-21T20:49:53Zdoi:10.1007/978-981-4585-08-8http://cds.cern.ch/record/1968750engKashyap, AmitaBujamma, DBabu M, NareshBioinformatics of non small cell lung cancer and the ras proto-oncogeneEngineeringCancer is initiated by activation of oncogenes or inactivation of tumor suppressor genes. Mutations in the K-ras proto-oncogene are responsible for 10–30% of adenocarcinomas. Clinical Findings point to a wide variety of other cancers contributing to lung cancer incidence. Such a scenario makes identification of lung cancer difficult and thus identifying its mechanisms can contribute to the society. Identifying unique conserved patterns common to contributing proto-oncogenes may further be a boon to Pharmacogenomics and pharmacoinformatics. This calls for ab initio/de novo drug discovery that in turn will require a comprehensive in silico approach of Sequence, Domain, Phylogenetic and Structural analysis of the receptors, ligand screening and optimization and detailed Docking studies. This brief involves extensive role of the RAS subfamily that includes a set of proteins, which cause an over expression of cancer-causing genes like M-ras and initiate tumour formation in lungs. SNP Studies and Structure based drug discovery will also be undertaken.Springeroai:cds.cern.ch:19687502015
spellingShingle Engineering
Kashyap, Amita
Bujamma, D
Babu M, Naresh
Bioinformatics of non small cell lung cancer and the ras proto-oncogene
title Bioinformatics of non small cell lung cancer and the ras proto-oncogene
title_full Bioinformatics of non small cell lung cancer and the ras proto-oncogene
title_fullStr Bioinformatics of non small cell lung cancer and the ras proto-oncogene
title_full_unstemmed Bioinformatics of non small cell lung cancer and the ras proto-oncogene
title_short Bioinformatics of non small cell lung cancer and the ras proto-oncogene
title_sort bioinformatics of non small cell lung cancer and the ras proto-oncogene
topic Engineering
url https://dx.doi.org/10.1007/978-981-4585-08-8
http://cds.cern.ch/record/1968750
work_keys_str_mv AT kashyapamita bioinformaticsofnonsmallcelllungcancerandtherasprotooncogene
AT bujammad bioinformaticsofnonsmallcelllungcancerandtherasprotooncogene
AT babumnaresh bioinformaticsofnonsmallcelllungcancerandtherasprotooncogene