AMPD1 polymorphism and response to regadenoson

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2015-11
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American English
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Future Medicine
Abstract

AIMS: AMPD1 c.34C > T (rs17602729) polymorphism results in AMPD1 deficiency. We examined the association of AMPD1 deficiency and variability of hemodynamic response to regadenoson. SUBJECTS & METHODS: Genotyping for c.34C>T was performed in 267 patients undergoing regadenoson cardiac stress testing. RESULTS: Carriers of c.34C >T variant exhibited higher relative changes in systolic blood pressure (SBP) compared with wild-type subjects ([%] SBP change to peak: 12 ± 25 vs 5 ± 13%; p = 0.01) ([%] SBP change to nadir: -3 ± 15 vs -7 ± 11%; p = 0.04). Change in heart rate was similar between groups, but side effects were more common in carriers of the variant (+LR = 4.2; p = 0.04). CONCLUSION: AMPD1 deficiency may be involved in the modulation of regadenoson's systemic effects.

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Saab, R., Zouk, A. N., Mastouri, R., Skaar, T. C., Philips, S., & Kreutz, R. P. (2015). AMPD1 polymorphism and response to regadenoson. Pharmacogenomics, 16(16), 1807–1815. http://doi.org/10.2217/pgs.15.116
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1744-8042
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Pharmacogenomics
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PMC
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Article
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