Screening of Missense SNPs in Coding Regions of COX-2 as a Key Enzyme Involved in Cancer
Background & Objectives: Non-synonymous single nucleotide polymorphism (nsSNPs) which results in disruption of protein function are used as markers in linkage and association of human proteins that might be involved in diseases and cancers . Methods: To study the functional effect of nsSNP in...
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Ardabil University of Medical Sciences
2013-09-01
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doaj-188767ae207f4de285e97f19e239f1422020-11-25T03:40:15ZfasArdabil University of Medical SciencesJournal of Ardabil University of Medical Sciences2228-72802228-72992013-09-01133305316Screening of Missense SNPs in Coding Regions of COX-2 as a Key Enzyme Involved in CancerSodabeh Jahanbakhsh-Godehkahriz0Elnaz Naderi1Ashraf Mohamadkhani2 Background & Objectives: Non-synonymous single nucleotide polymorphism (nsSNPs) which results in disruption of protein function are used as markers in linkage and association of human proteins that might be involved in diseases and cancers . Methods: To study the functional effect of nsSNP in cyclooxygenase-2 (COX2 ) amino acids, the nucleotide sequences encoding COX-2 gene in cancers were extracted from the NCBI (gi|223941909) data bank (283 cases) and analyzed by SIFT, I-Mutant 2.0, SNP and GO, PANTHER and FASTSNP servers. These servers involve programs that predict the effects of amino acid substitution on protein function, stability and missense . Results: COX-2 is an essential enzyme for the production of pro-inflammatory prostaglandins which are relevant to cancer development and progression. The substitutions in some positions such as R228H and S428A of COX-2 in most of cancers linked to reformed protein function through disruption in enzyme active site. Conclusion: Amino acid substitutions as a consequence of COX-2 nsSNPs have important role in human disease. Substitutions which are located in catalytic domain are important for the enzymatic function of COX-2 and associated with higher expression of COX-2.http://jarums.arums.ac.ir/browse.php?a_code=A-10-27-83&slc_lang=en&sid=1Cancer; Cyclooxygenase-2; Protein Coding Regions; SNP |
collection |
DOAJ |
language |
fas |
format |
Article |
sources |
DOAJ |
author |
Sodabeh Jahanbakhsh-Godehkahriz Elnaz Naderi Ashraf Mohamadkhani |
spellingShingle |
Sodabeh Jahanbakhsh-Godehkahriz Elnaz Naderi Ashraf Mohamadkhani Screening of Missense SNPs in Coding Regions of COX-2 as a Key Enzyme Involved in Cancer Journal of Ardabil University of Medical Sciences Cancer; Cyclooxygenase-2; Protein Coding Regions; SNP |
author_facet |
Sodabeh Jahanbakhsh-Godehkahriz Elnaz Naderi Ashraf Mohamadkhani |
author_sort |
Sodabeh Jahanbakhsh-Godehkahriz |
title |
Screening of Missense SNPs in Coding Regions of COX-2 as a Key Enzyme Involved in Cancer |
title_short |
Screening of Missense SNPs in Coding Regions of COX-2 as a Key Enzyme Involved in Cancer |
title_full |
Screening of Missense SNPs in Coding Regions of COX-2 as a Key Enzyme Involved in Cancer |
title_fullStr |
Screening of Missense SNPs in Coding Regions of COX-2 as a Key Enzyme Involved in Cancer |
title_full_unstemmed |
Screening of Missense SNPs in Coding Regions of COX-2 as a Key Enzyme Involved in Cancer |
title_sort |
screening of missense snps in coding regions of cox-2 as a key enzyme involved in cancer |
publisher |
Ardabil University of Medical Sciences |
series |
Journal of Ardabil University of Medical Sciences |
issn |
2228-7280 2228-7299 |
publishDate |
2013-09-01 |
description |
Background & Objectives: Non-synonymous single nucleotide polymorphism (nsSNPs) which results in disruption of protein function are used as markers in linkage and association of human proteins that might be involved in diseases and cancers . Methods: To study the functional effect of nsSNP in cyclooxygenase-2 (COX2 ) amino acids, the nucleotide sequences encoding COX-2 gene in cancers were extracted from the NCBI (gi|223941909) data bank (283 cases) and analyzed by SIFT, I-Mutant 2.0, SNP and GO, PANTHER and FASTSNP servers. These servers involve programs that predict the effects of amino acid substitution on protein function, stability and missense . Results: COX-2 is an essential enzyme for the production of pro-inflammatory prostaglandins which are relevant to cancer development and progression. The substitutions in some positions such as R228H and S428A of COX-2 in most of cancers linked to reformed protein function through disruption in enzyme active site. Conclusion: Amino acid substitutions as a consequence of COX-2 nsSNPs have important role in human disease. Substitutions which are located in catalytic domain are important for the enzymatic function of COX-2 and associated with higher expression of COX-2. |
topic |
Cancer; Cyclooxygenase-2; Protein Coding Regions; SNP |
url |
http://jarums.arums.ac.ir/browse.php?a_code=A-10-27-83&slc_lang=en&sid=1 |
work_keys_str_mv |
AT sodabehjahanbakhshgodehkahriz screeningofmissensesnpsincodingregionsofcox2asakeyenzymeinvolvedincancer AT elnaznaderi screeningofmissensesnpsincodingregionsofcox2asakeyenzymeinvolvedincancer AT ashrafmohamadkhani screeningofmissensesnpsincodingregionsofcox2asakeyenzymeinvolvedincancer |
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