Table 1.

Genes and variant alleles interrogated by the pharmacogenetic panel

Gene	Variant allelesa
ABCB1	c.3435T>C (rs1045642), c.2677T>A/G (rs2032582)
ABCG2	c.421C>A (rs2231142)
ADRA2A	c.‐1252G>C (rs1800544)
COMT	c.472G>A (rs4680)
CYP1A2	*1A, *1C, *1D, *1F, *1K, *1L, *1V
CYP2B6	*6 (*9), *29, *30
CYP2C cluster	rs12777823
CYP2C19	*2, *3, *4, *5, *6, *7, *8, *9, *10, *16, *17, *19, *22, *24, *25, *26, *35, *36, *37
CYP2C8	*2, *3, *4
CYP2C9	*2, *3 (*18), *4, *5, *6, *8, *11, *12, *13, *15, *25, *27, *31
CYP2D6	*2, *3, *4, *5, *6, *7, *8, *9, *10, *11, *12, *13, *14, *15, *17, *18, *19, *20, *29, *30 (*40), *31, *36, *38, *41, *42, *44, *47, *49, *50, *51, *54, *55, *56, *57, *62, *64, *68, *69, *72, *100, *101, *107, *114
CYP3A4	*1B, *2, *3, *12, *17, *22
CYP3A5	*3, *6, *7
CYP4F2	*3
DPYD	*2, *13, c.2846A>T (rs67376798)
DRD2	c.811‐83G>T (rs1076560), c.‐585A>G (rs1799978)
F2	c.*97G>A (rs1799963)
F5	c.1601G>A (rs6025)
G6PD	Mediterranean, A+, A‐202, A‐968, A‐680, Chatam, Canton, Cosenza, Kerala‐Kalyan, Orissa
GRIK4	c.83‐10039T>C (rs1954787)
HTR2A	c.614‐2211T>C (rs7997012), c.102C>T (rs6313), c.102C>T (rs6311)
HTR2C	c.‐759C>T (rs3813929), c.551‐3008C>G (rs1414334)
NUDT15	*2 (*3), *4, *5
OPRM1	c.118A>G (rs1799971)
SLCO1B1	c.521T>C (rs4149056; *5, *15, *17)
TPMT	*2, *3A, *3B, *3C, *4
UGT1A1	*6, *27, *80,b rs8175347 (*28, *36, *37) b
UGT2B15	c.253T>G (rs1902023; *2)
VKORC1	c.‐1639G>A (rs9923231), c.106G>T (rs61742245), c.196G>A (rs72547529)

^aBrackets indicate star (*) allele haplotypes with shared variants that cannot be distinguished by genotyping.

^bThe UGT1A1*80 variant (rs887829) is in linkage disequilibrium with the dinucleotide repeat *28 allele (rs8175347) and is used as an internal control for the independent UGT1A1*28 capillary electrophoresis test (see Methods and Results).