作者
Ayodeji Sanusi,Justin M. Leach,Kim Boggess,Lorraine Dugoff,Baha M. Sibai,Kirsten Lawrence,Brenna L. Hughes,Joseph Bell,Kjersti M. Aagaard,Rodney K. Edwards,Kelly S. Gibson,David M. Haas,Lauren Plante,Torri D. Metz,Brian M. Casey,Sean Esplin,Sherri Longo,Matthew Hoffman,George R Saade,Kara K. Hoppe,Janelle Foroutan,Methodius G. Tuuli,Michelle Owens,Hyagriv N. Simhan,Heather A. Frey,Todd Rosen,Anna Palatnik,Susan Baker,Phyllis August,Uma M. Reddy,Emily Su,Iris Krishna,Nguyet A Nguyen,Mary E. Norton,Daniel Skupski,Yasser Y El-Sayed,Dotun Ogunyemi,Zorina S. Galis,Lorie Harper,Namasivayam Ambalavanan,Nancy L Geller,Hui-Chien Kuo,Rachel G Sinkey,R. Librizzi,Leonardo Pereira,Everett F. Magann,Mounira Habli,Shauna Williams,Giancarlo Mari,Gabriella Pridjian,David S. McKenna,Marc Parrish,Eugene Chang,Sarah S. Osmundson,Joanne N. Quiñones,Jeff M. Szychowski,Alan T N Tita
摘要
OBJECTIVE: To evaluate maternal and neonatal outcomes by type of antihypertensive used in participants of the CHAP (Chronic Hypertension in Pregnancy) trial. METHODS: We conducted a planned secondary analysis of CHAP, an open-label, multicenter, randomized trial of antihypertensive treatment compared with standard care (no treatment unless severe hypertension developed) in pregnant patients with mild chronic hypertension (blood pressure 140–159/90–104 mm Hg before 20 weeks of gestation) and singleton pregnancies. We performed three comparisons based on medications prescribed at enrollment: labetalol compared with standard care, nifedipine compared with standard care, and labetalol compared with nifedipine. Although active compared with standard care groups were randomized, medication assignment within the active treatment group was not random but based on clinician or patient preference. The primary outcome was the occurrence of superimposed preeclampsia with severe features, preterm birth before 35 weeks of gestation, placental abruption, or fetal or neonatal death. The key secondary outcome was small for gestational age (SGA) neonates. We also compared medication adverse effects between groups. Relative risks (RRs) and 95% CIs were estimated with log binomial regression to adjust for confounding. RESULTS: Of 2,292 participants analyzed, 720 (31.4%) received labetalol, 417 (18.2%) received nifedipine, and 1,155 (50.4%) received no treatment. The mean gestational age at enrollment was 10.5±3.7 weeks; nearly half of participants (47.5%) identified as non-Hispanic Black; and 44.5% used aspirin. The primary outcome occurred in 217 (30.1%), 130 (31.2%), and 427 (37.0%) in the labetalol, nifedipine, and standard care groups, respectively. Risk of the primary outcome was lower among those receiving treatment (labetalol use vs standard adjusted RR 0.82, 95% CI, 0.72–0.94; nifedipine use vs standard adjusted RR 0.84, 95% CI, 0.71–0.99), but there was no significant difference in risk when labetalol was compared with nifedipine (adjusted RR 0.98, 95% CI, 0.82–1.18). There were no significant differences in SGA or serious adverse events between participants receiving labetalol and those receiving nifedipine. CONCLUSION: No significant differences in predetermined maternal or neonatal outcomes were detected on the basis of the use of labetalol or nifedipine for treatment of chronic hypertension in pregnancy. CLINICAL TRIAL REGISTRATION: ClinicalTrials.gov, NCT02299414.