First trimester INCB024360 datasheet inhibitors uterine artery Doppler, shows promise but needs further ‘real life’ evaluation [200]. Markers of preeclampsia risk that become available in the second and third trimesters include measures of: placental
perfusion, vascular resistance, and morphology (e.g., mean maternal second trimester BP, 24-h ABPM, Doppler); maternal cardiac output and systemic vascular resistance; fetoplacental unit endocrinology [e.g., pregnancy-associated plasma protein-A (PAPP-A) in the first trimester, and alpha-fetoprotein, hCG, and inhibin-A in the early second trimester]; maternal renal function (e.g., serum uric acid or microalbuminuria); maternal endothelial function and endothelial–platelet interaction (e.g., platelet count, antiphospholipid antibodies, or homocysteine); oxidative stress (e.g., serum lipids); and circulating angiogenic factors [201], [202] and [203]. Systematic reviews of primary studies have evaluated clinically available Gefitinib mw biomarkers [163], [164] and [204] and no single clinical test reaches the ideal of ⩾90% sensitivity for preeclampsia prediction. Only uterine artery Doppler
at 20–24 weeks has sensitivity >60% for detection of preeclampsia, particularly when testing is performed: (i) in women at increased risk of preeclampsia; (ii) during the second trimester, and/or (iii) when predicting severe and early preeclampsia. Women with abnormal velocimetry could be considered for increased surveillance to detect preeclampsia or other adverse placental outcomes. Uterine artery Doppler should not be used in low risk women [162] and [205]. It is unclear whether markers used for Down syndrome screening are useful in isolation (or with uterine artery Doppler) for preeclampsia prediction
[206]. Thrombophilia screening is not recommended for investigation of prior preeclampsia or other placental complications, except if the woman satisfies the clinical Sitaxentan criteria for the antiphospholipid antibody syndrome [207] and [208]. As no single test predicts preeclampsia with sufficient accuracy to be clinically useful [209], interest has grown in researching multivariable models that include clinical and laboratory predictors available at booking and thereafter [166], [209] and [210]. Clinicians should support clinics conducting relevant prospective longitudinal studies. We have based our recommendations on both prevention of preeclampsia and/or its associated complications. Pregnant women have been classified as being at ‘low’ or ‘increased’ risk of preeclampsia, usually by the presence of one or more risk markers as shown in Table 5 [see Prediction].