Antiretroviral (ARV) therapy during pregnancy is recommended to reduce the risk of mother‐to‐child transmission (MTCT). Physiologic changes during pregnancy can affect PK. We present the PK of total and unbound (pharmacologically active) DRV in HIV‐1‐infected pregnant women receiving twice‐daily (bid) DRV/ritonavir (rtv). This Phase IIIb study enrolled HIV‐1‐infected pregnant women≥18 years old in the 2nd trimester of pregnancy receiving DRV/rtv 600/100 mg bid and other ARVs. DRV (total and unbound) and rtv (total) plasma concentrations were obtained predose and 1, 2, 3, 4, 6, 9 and 12 hours postdose during the 2nd and 3rd trimesters and postpartum. Total DRV and rtv plasma concentrations were determined using a previously validated HPLC‐MS/MS assay (lower limit of quantification 5.00 ng/mL). Unbound DRV was determined by fortifying plasma samples with 14‐C DRV and separating total and unbound DRV using ultrafiltration. Total and unbound 14‐C DRV were measured using liquid scintillation counting. Total and unbound PK parameters were derived using a noncompartmental analysis. Safety and efficacy were investigated at each visit and summarized using descriptive statistics. Sixteen women (10 black, 4 Hispanic, 2 white) were enrolled; 11 had evaluable PK data. Total DRV AUC12h was 24% and 17% lower during 2nd and 3rd trimesters, respectively, vs postpartum (Table). Unbound DRV AUC12h was unchanged during 2nd and 3rd trimesters vs postpartum. Total and unbound DRV Cmin increased by 43% and 10%, respectively, during 2nd trimester and by 86% and 14%, respectively, during 3rd trimester vs postpartum. Unbound DRV was above the EC50 (27.5 ng/mL) for PI‐resistant HIV in all patients. Albumin and α1‐acid glycoprotein (AAG) concentrations were 22%–29% lower during pregnancy vs postpartum. Viral load decreased and CD4+ count increased over time. One serious adverse event was reported (increased transaminase). Three of 12 infants were born prior to 37 weeks (30, 36 and 36 weeks), and all 12 infants were HIV‐1‐negative by standard PCR testing. Total DRV and rtv PK decreased during pregnancy likely due to pregnancy‐related dilution of albumin and/or AAG. No clinically relevant change in unbound DRV AUC12h and Cmin occurred during pregnancy, and there was no MTCT; therefore no dose adjustment is required for DRV/rtv 600/100mg bid in pregnant women. This ongoing trial will further evaluate the effects of pregnancy on DRV/rtv once daily, etravirine and rilpivirine PK. Pharmacokinetic parameters a LS mean ratio, (90% CI) 2nd trimester vs postpartum 3rd trimester vs postpartum Darunavir (total) N 11b vs 11 11 vs 11 Cmin 1.43 (0.39, 5.22) 1.86 (0.49, 7.04) Cmax 0.72 (0.61, 0.86) 0.81 (0.69, 0.96) AUC12h 0.76 (0.63, 0.90) 0.83 (0.72, 0.97) Darunavir (unbound) N 6d vs 11 7e vs 11 Cmin c 1.10 (0.59, 2.06) 1.14 (0.59, 2.20) Cmax 0.78 (0.52, 1.18) 0.82 (0.57, 1.16) AUC12h 0.92 (0.66, 1.30) 0.93 (0.69, 1.24) Ritonavir (total) N 11f vs 11 11g vs 11 Cmin 1.08 (0.31, 3.81) 1.22 (0.41, 3.59) Cmax 0.66 (0.41, 1.08) 0.63 (0.40, 0.98) AUC12h 0.72 (0.44, 1.17) 0.67 (0.43, 1.04) Efficacy parameters Parameter Baseline, n=15 h 2 nd trimester, n=14 3 rd trimester, n=11 Log10 viral load, mean (SD) 2.17 (0.770) 1.99 (0.514) 1.88 (0.598) CD4+ cell count, cells/mm3, median (range) 419 (104, 793) 429 (81, 933) 470 (103, 960) Virologic response (HIV RNA <50 copies/mL), n (%) 5 (33.3) 9 (64.3) 9i (81.8) aOne patient was excluded from the PK analysis due to low adherence; bn=10 for AUC12h; cn=10 for postpartum; dn=9 for Cmin and n=7 for Cmax; en=8 for Cmin and Cmax; fn=12 for Cmax; gn=10 for Cmin; hn=14 for CD4+ cell count; i1 patient had VL 50–<400 copies/mL and 1 patient had VL≥1000 copies/mL; LS, least squares; CI, confidence interval; Cmin, minimum plasma concentration; Cmax, maximum plasma concentration; AUC12h, area under the plasma concentration‐time curve over 12 hours; SD, standard deviation; PK, pharmacokinetic.