Atazanavir and lopinavir with ritonavir alone or in combination: analysis of pharmacokinetic interaction and predictors of drug exposure

Objectives Studies on the pharmacokinetic interaction between atazanavir and lopinavir with ritonavir (lopinavir/ritonavir) report contradictory results. We aimed to establish the in vivo interaction between these two protease inhibitors as well as the variables influencing drug exposure. Methods Pharmacokinetic parameters were investigated in HIV‐infected patients treated with atazanavir 300 mg with ritonavir 100 mg q24h (group A) or lopinavir/ritonavir 400/100 mg q12h (group B) or atazanavir 300 mg q24h with lopinavir/ritonavir 400/100 mg q12h (group C). Patients receiving other concomitant protease inhibitors or non‐nucleoside reverse transcriptase inhibitors were excluded. Results In group A ( n =10), mean ± standard deviation atazanavir C min was 390 ± 460 ng/mL, C max 3051 ± 1996 ng/mL and AUC 24 29 913 ± 17 686 ng/mL/h. In group B ( n =9), lopinavir C min was 7562 ± 4292 ng/mL, C max 12 944 ± 4838 ng/mL and AUC 0–12 122 313 ± 38 225 ng/mL/h. In group C ( n =7), atazanavir C min was 876 ± 460 ng/mL ( P =0.039 vs. group A), C max 3421 ± 3399 ng/mL and AUC 0–24 65 055 ± 49 843 ng/mL/h (two‐sided P >0.05 for each comparison with group A), lopinavir C min was 7471 ± 3745 ng/mL, C max 10 143 ± 5217 ng/mL and AUC 0–12 104 501 ± 43 565 ng/mL/h ( P >0.05 for each comparison with group B). When analysing all the groups, including controls from routine clinical practice, higher body mass index was associated with lower atazanavir C min and with lower lopinavir C max . Atazanavir C min showed a correlation with total bilirubin levels. Conclusions Combination with lopinavir/ritonavir provides higher atazanavir C min than combination with ritonavir alone, possibly because of an effect of the additional ritonavir dose. Low BMI may be associated with higher drug exposure.