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Haptoglobin phenotype and abnormal uterine artery Doppler in a racially diverse cohort.
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- Author(s): Weissgerber, Tracey L.1 (AUTHOR) ; McGee, Paula L.2 (AUTHOR); Myatt, Leslie3 (AUTHOR); Hauth, John C.4 (AUTHOR); Varner, Michael W.5 (AUTHOR); Wapner, Ronald J.6 (AUTHOR); Thorp, John M.7 (AUTHOR); Mercer, Brian M.8 (AUTHOR); Peaceman, Alan M.9 (AUTHOR); Ramin, Susan M.10 (AUTHOR); Samuels, Philip11 (AUTHOR); Sciscione, Anthony C.12 (AUTHOR); Harper, Margaret13 (AUTHOR); Saade, George14 (AUTHOR); Sorokin, Yoram15 (AUTHOR)
- Source:
Journal of Maternal-Fetal & Neonatal Medicine. Nov2014, Vol. 27 Issue 17, p1728-1733. 6p.
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- Abstract:
Objective: The anti-oxidant and proangiogenic protein haptoglobin (Hp) is believed to be important for implantation and pregnancy, although its specific role is not known. The three phenotypes (1-1, 2-1 and 2-2) differ in structure and function. Hp 2-2 is associated with increased vascular stiffness in other populations. We examined whether Hp phenotype is associated with abnormal uterine artery Doppler (UAD) in pregnancy. Methods: We conducted a secondary analysis of a preeclampsia prediction cohort nested within a larger placebo-controlled randomized clinical trial of antioxidants for prevention of preeclampsia. We determined Hp phenotype in 2184 women who completed UAD assessments at 17 weeks gestation. Women with notching were re-evaluated for persistent notching at 24 weeks' gestation. Logistic regression was used to assess differences in UAD indices between phenotype groups. Results: Hp phenotype did not significantly influence the odds of having any notch ( p = 0.32), bilateral notches ( p = 0.72), or a resistance index ( p = 0.28) or pulsatility index ( p = 0.67) above the 90th percentile at 17 weeks' gestation. Hp phenotype also did not influence the odds of persistent notching at 24 weeks ( p = 0.25). Conclusions: Hp phenotype is not associated with abnormal UAD at 17 weeks' gestation or with persistent notching at 24 weeks. [ABSTRACT FROM AUTHOR]
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