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. 2011 Feb 3;3:1–13. doi: 10.4137/BIC.S6111

Table SA.

Effect modification of NAT1 and NAT2 in relation to PCa susceptibility.

#NAT1*10 alleles #Slow NAT2 alleles Cases (%)|| controls (%) Estimated OR (95% CI)a Estimated OR (95% CI)b P-value for Interaction
0 or 1 0 NAT2 Slow 12 (7.1) || 43 (9.4) 1.00 (Referent) 1.00 (Referent) 0.2897
0 or 1 1 NAT2 Slow 58 (34.3) || 158 (34.8) 1.32 (0.65–2.67) 1.01 (0.46–2.22)
0 or 1 2 NAT2 Slow 63 (37.3) || 132 (29.1) 1.71 (0.84–3.47) 1.63 (0.74–3.58)
2 0 NAT2 Slow 3 (1.8) || 18 (4.0) 0.60 (0.15–2.37) 0.73 (0.17–3.13)
2 1 NAT2 Slow 22 (13.0) || 54 (11.9) 1.46 (0.65–3.28) 1.18 (0.48–2.90)
2 2 NAT2 Slow 11 (6.5) || 49 (10.8) 0.80 (0.32–2.01) 0.75 (0.28–2.04)
0 or 1 0 NAT2 Rapid 63 (37.3) || 132 (29.1) 1.00 (Referent) 1.00 (Referent) 0.2156
0 or 1 1 NAT2 Rapid 58 (34.3) || 158 (34.8) 0.77 (0.50–1.18) 0.62 (0.38–1.02)
0 or 1 2 NAT2 Rapid 12 (7.1) || 43 (9.4) 0.58 (0.29–1.18) 0.61 (0.28–1.34)
2 0 NAT2 Rapid 11 (6.5) || 49 (10.8) 0.47 (0.23–0.97) 0.46 (0.21–1.01)
2 1 NAT2 Rapid 22 (13.0) || 54 (11.9) 0.85 (0.48–1.52) 0.72 (0.38–1.40)
2 2 NAT2 Rapid 3 (1.8) || 18 (4.0) 0.35 (0.10–1.23) 0.45 (0.12–1.68)

Notes:

a

Associations were determined using univariate logistic regression models to estimate the risk of developing PCa. 151 subjects had missing genotype data for NAT1 and/or NAT2;

b

Risk estimates adjusted for age (continuous variable) and West African Ancestry (WAA; continuous variable).