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Article Abstract

Certain genotypes are linked to a lower efficacy of tamoxifen therapy. This study aimed to observe polymorphisms and examine the impact of genotyping among tamoxifen-treated breast cancer patients in Indonesia. 150 breast cancer participants were recruited. Buccal swab samples were collected; gDNA was extracted and genotyped using the qPCR method. Blood samples were collected, and measurement of tamoxifen metabolite levels was performed using UPLC-MS/MS. 43.3% (n = 65) of participants were IMs. *10 was the most common haplotype (n = 89, 29.7%), followed by *36 (n = 73, 29.7%), making *10/*36 the most common diplotype (n = 34, 22.7%) in this study. The difference in endoxifen levels between the NM and IM-PM groups at baseline was statistically significant ( ≤ 0.001). A dose increase in tamoxifen to 40 mg daily successfully increased endoxifen levels in IMs to a similar level with NMs at baseline ( > 0.05) without exposing IMs to serious side effects. No statistically significant differences were observed between the 20mg group and the 40 mg group on the adjusted OS ( > 0.05) and the adjusted PFS ( > 0.05). Our study observed a considerably high proportion of IMs. The dose adjustment of tamoxifen was proven to significantly and safely improve the level of endoxifen and survival.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11943653PMC
http://dx.doi.org/10.3390/jpm15030093DOI Listing

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