AMPD1 polymorphism and response to regadenoson

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.

Keywords

adenosine, genetic, myocardial perfusion imaging, regadenoson

Cite As

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

ISSN

1744-8042

Journal

Pharmacogenomics

Rights

Publisher Policy

Source

PMC

Type

Article

Permanent Link

https://hdl.handle.net/1805/10839

DOI

https://doi.org/10.2217/pgs.15.116

Version

Author's manuscript

Collections

Open Access Policy Articles
Department of Medicine Works
Todd Skaar

Full item page