The relevance of HLA-B*5801 pharmacogenotyping in personalising allopurinol therapy / Norleen Mohamed Ali
Allopurinol is one of the drug reported to cause cutaneous ADR. From previous studies, Allopurinol causing SCAR was strongly associated with HLA-B*58:01 in Han Chinese population. The allele was present in all patients with allopurinol induced SCAR (51 out 51) but only 15% (20 of 135) in allopurinol...
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my.uitm.ir.991402024-09-17T04:36:53Z https://ir.uitm.edu.my/id/eprint/99140/ The relevance of HLA-B*5801 pharmacogenotyping in personalising allopurinol therapy / Norleen Mohamed Ali Mohamed Ali, Norleen Allopurinol is one of the drug reported to cause cutaneous ADR. From previous studies, Allopurinol causing SCAR was strongly associated with HLA-B*58:01 in Han Chinese population. The allele was present in all patients with allopurinol induced SCAR (51 out 51) but only 15% (20 of 135) in allopurinol tolerant patient and 20% (19 out 93) in the general population. The odds ratio (OR) to a patient with allopurinol induced SCAR was significantly high, 580.0 with a p value of 4.7x10'24 (Hung et al, 2005). This association was also observed in Thai population (Tassaneeyakul et al, 2009) and Korean population ( Kang et al, 2011). This study to determine the association between HLA-B*58:01 and clinical association of Allopurinol induced cutaneous adverse drug reaction in Malaysian population. As a conclusion, AS-PCR for the simultaneous detection of HLAB* 5 8:01 allele was successfully developed. This method provided a more rapid and convenient way in detection of single nucleotide polymorphism. We also have successfully genotyped our patients. The interesting finding in this study would be able to provide a preliminary data of HLA-B*58:01 allele and genotype in patients who experienced SCAR after allopurinol initiation. Based on the results, HLAB*58:01 allele is significantly associated with the increased risk of SCAR in patients using allopurinol. Therefore, this study recommended the pharmacogenetic test of HLA-B*58:01 may provide personalized medicine in clinical application and a valid marker to prevent allopurinol induced serious cutaneous reactions. 2016 Thesis NonPeerReviewed text en https://ir.uitm.edu.my/id/eprint/99140/2/99140.pdf The relevance of HLA-B*5801 pharmacogenotyping in personalising allopurinol therapy / Norleen Mohamed Ali. (2016) Masters thesis, thesis, Universiti Teknologi MARA (UiTM). <http://terminalib.uitm.edu.my/99140.pdf> |
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Allopurinol is one of the drug reported to cause cutaneous ADR. From previous studies, Allopurinol causing SCAR was strongly associated with HLA-B*58:01 in Han Chinese population. The allele was present in all patients with allopurinol induced SCAR (51 out 51) but only 15% (20 of 135) in allopurinol tolerant patient and 20% (19 out 93) in the general population. The odds ratio (OR) to a patient with allopurinol induced SCAR was significantly high, 580.0 with a p value of 4.7x10'24 (Hung et al, 2005). This association was also observed in Thai population (Tassaneeyakul et al, 2009) and Korean population ( Kang et al, 2011). This study to determine the association between HLA-B*58:01 and clinical association of Allopurinol induced cutaneous adverse drug reaction in Malaysian population. As a conclusion, AS-PCR for the simultaneous detection of HLAB* 5 8:01 allele was successfully developed. This method provided a more rapid and convenient way in detection of single nucleotide polymorphism. We also have successfully genotyped our patients. The interesting finding in this study would be able to provide a preliminary data of HLA-B*58:01 allele and genotype in patients who experienced SCAR after allopurinol initiation. Based on the results, HLAB*58:01 allele is significantly associated with the increased risk of SCAR in patients using allopurinol. Therefore, this study recommended the pharmacogenetic test of HLA-B*58:01 may provide personalized medicine in clinical application and a valid marker to prevent allopurinol induced serious cutaneous reactions. |
| format |
Thesis |
| author |
Mohamed Ali, Norleen |
| spellingShingle |
Mohamed Ali, Norleen The relevance of HLA-B*5801 pharmacogenotyping in personalising allopurinol therapy / Norleen Mohamed Ali |
| author_facet |
Mohamed Ali, Norleen |
| author_sort |
Mohamed Ali, Norleen |
| title |
The relevance of HLA-B*5801 pharmacogenotyping in personalising allopurinol therapy / Norleen Mohamed Ali |
| title_short |
The relevance of HLA-B*5801 pharmacogenotyping in personalising allopurinol therapy / Norleen Mohamed Ali |
| title_full |
The relevance of HLA-B*5801 pharmacogenotyping in personalising allopurinol therapy / Norleen Mohamed Ali |
| title_fullStr |
The relevance of HLA-B*5801 pharmacogenotyping in personalising allopurinol therapy / Norleen Mohamed Ali |
| title_full_unstemmed |
The relevance of HLA-B*5801 pharmacogenotyping in personalising allopurinol therapy / Norleen Mohamed Ali |
| title_sort |
relevance of hla-b*5801 pharmacogenotyping in personalising allopurinol therapy / norleen mohamed ali |
| publishDate |
2016 |
| url |
https://ir.uitm.edu.my/id/eprint/99140/2/99140.pdf https://ir.uitm.edu.my/id/eprint/99140/ |
| _version_ |
1811598108766765056 |
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13.214268 |