HLA DRB1 shared epitope alleles and non HLA gene polymorphisms as risk factors for rheumatoid arthritis

dc.contributor.guideNalini Ganesan
dc.coverage.spatialorthopedics
dc.creator.researcherVasanth K.M.
dc.date.accessioned2018-03-23T05:29:07Z
dc.date.available2018-03-23T05:29:07Z
dc.date.awarded16/03/2018
dc.date.completed16/03/2018
dc.date.registered01/07/2010
dc.description.abstractA significant elevation in laboratory measures was observed in rheumatoid arthritis patients compared to controlsand#61472;The frequency of HLA DRB1 01 04 10 and 14 is found to be more with autoantibodies positive RA patientsand#61472;The HLA DRB1 07 08 11 13 and 15 alleles were less frequent in rheumatoid arthritis patients and found to be significantly increased in control group as compared to patients indicating a possible protective effect and#61472;The frequency of CTLA4 CT60 A allele and padi 4 90T carriers was significantly higher in rheumatoid arthritis patients and also it is preferentially observed in SE positive rheumatoid arthritis patients and#61472;The frequency of CD244 T allele carriers was significantly higher in RA patients and it is independent of SE positive RA patients We found significant association of the susceptible AT haplotype and RA patients The AC haplotype is found to be significantly increased in control group compared to rheumatoid arthritis patients and#61472;The AT haplotype of PADI4 gene was significantly associated with 1 2 copies and the AC haplotype was significantly associated with 2 copies of HLA DRB1 SE alleles in RA patientsand#61472;and#61472;The combination of non HLA allele frequency ATCAGC is found to be associated with increased RA susceptibility while ACCGGC is significantly reduced and confer protection against RA disease and#61472;In RA patients the ATCAGC frequencies of non HLA gene was increased with 1 and 2 copies of HLA DRB1 SE alleles when compared to 0 copy of HLA DRB1 SE alleles and#61472;The combined allele frequency of non HLA risk variants ATCAGC showed an increased frequency in the autoantibodies RF and anti CCP positive RA patients newline
dc.description.noteIntroduction p.26 Review of literature p.27-40 Need and Scope of the Study p.41 Materials and methods p.43-86 Results p.87-127 Discussion p.128-144 Summary p.145-146
dc.format.accompanyingmaterialDVD
dc.format.dimensions15cms
dc.format.extent1-267
dc.identifier.urihttp://hdl.handle.net/10603/197943
dc.languageEnglish
dc.publisher.institutionMedical College
dc.publisher.placeChennai
dc.publisher.universitySri Ramachandra University
dc.relation
dc.rightsself
dc.source.universityUniversity
dc.subject.keywordAutoimmune diseases
dc.subject.keywordBone erosion
dc.subject.keywordMultiple sclerosis
dc.subject.keywordRheumatoid arthritis
dc.subject.keywordSynovial fluid
dc.titleHLA DRB1 shared epitope alleles and non HLA gene polymorphisms as risk factors for rheumatoid arthritis
dc.title.alternative
dc.type.degreePh.D.

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