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Supplementary Thesis data.

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Research Data Australia2024-12-14 收录
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This is the supplementary data for Mullan et al. Monash thesis (2018-2022).  Abstract The unpredictable Type IV drug hypersensitivity reactions (DHRs) are T cell mediated reactions that range in severity from the mild maculopapular exanthema (MPE) to severe Stevens-Johnson syndrome/toxic epidermal necrolysis (SJS/TEN). Unlike mild MPE reactions, SJS/TEN has associated morbidities and mortality in both acute and resolved disease. Anti-seizure medications (ASM), especially carbamazepine (CBZ), are among the most common causes of DHRs. The HLA-B*15:02 allele is strongly associated with increased risk of CBZ-SJS/TEN in East Asians but not in other populations (Odds ratio[OR]>2000), while another HLA allele, HLA-A*31:01, confers increased risk of CBZ-DHRs in European (OR: 25.9) and Japanese (OR: 33.9) populations. However, neither of these risk HLA allotypes are sufficient to cause CBZ-DHRs, which suggests other factors contribute to the DHR. To identify other risk factors, I used a multi-omics approach that involved two investigative modalities. The first was genomics, where I identified common variants from the whole genome of 116 ASM-SJS/TEN cases and 84 ASM tolerant controls. This analysis identified nine genome wide variants significantly associated with ASM-SJS/TEN. Using an interaction analysis to qualify the relative risk of the novel risk variant by HLA-B*15:02 carrier status, I identified two variants predicted to lower the relative risk of ASM-SJS/TEN, providing a potential explanation for ASM tolerance in some HLA-B*15:02 carriers. Additionally, the analysis suggested ASM-SJS/TEN had complex inheritance and indicated that many variants were contributing a small fraction of risk, and that some of these variants may not have reached genome wide significance (p-value
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