fullPIERS for When Laboratory Tests Are Readily Available

The fullPIERS model includes demographics, symptoms, signs, and laboratory tests [18]. The fullPIERS was developed and internally validated in Australia, Canada, New Zealand and the United Kingdom [19, 20]. Following the same model development procedures as miniPIERS, independently informative predictors of adverse maternal outcomes include gestational age, chest pain or dyspnoea, oxygen saturation, platelet count and creatinine and aspartate transaminase (AST) concentrations (in the United Kingdom, alanine transaminase [ALT] can be substituted for AST). The fullPIERS model predicts adverse maternal outcomes within 48 hours of admission with preeclampsia (AUROC 0.88 [95% confidence interval [CI] 0.84–0.92], and performed well (AUROC >0.7) up to 7 days after admission [19, 20]. The fullPIERS model has been externally and temporally validated in both less and more developed country settings, is superior to the PREP (Prediction models for Risks of complications in Early-onset Pre-eclampsia) model for predicting adverse outcomes in women with early-onset preeclampsia [21] and is recommended by the 2019 update of the UK National Institute for Health and Care Excellence guidelines for pregnancy hypertension. The open-access online fullPIERS calculator is available at: https://pre-empt.bcchr.ca/monitoring/fullpiers.

CIPHER for Women Receiving Critical Care

The aim of the CIPHER (Collaborative Integrated Pregnancy High-dependency Estimate of Risk) model is to provide an internally validated multivariable prognostic model calibrated specifically for pregnant or recently delivered women admitted for critical care [22]. Predictors included in the final CIPHER model are maternal age, surgery in the preceding 24 hours, systolic blood pressure, Glasgow Coma Scale score, serum sodium, serum potassium, activated partial thromboplastin time, arterial blood gas (ABG) pH, serum creatinine and serum bilirubin. The CIPHER model is a pragmatic risk prediction tool, as it identifies critically ill pregnant women at highest risk for adverse outcomes, informs counselling of patients and their families about risk and facilitates benchmarking of outcomes between centres by adjusting for baseline risk. The open-access online CIPHER calculator is available at https://pre-empt.bcchr.ca/monitoring/cipher.

Fetal Assessment

Severe preeclampsia is often associated with significant fetal growth restriction (FGR). The computerised cardiotocograph/non-stress test (cCTG) reflects changes in fetal autonomic and chemoreceptor activity, as placental oxygenation deteriorates in women with FGR [23, 24]. Progression of the ductus venosus (DV) waveform to absent and reverse a-wave (atrial contraction) patterns is generally limited to severe and early-onset FGR [25, 26]. At ≥32 weeks, late decelerations and reduced variability noted on CTG almost invariably precede DV abnormalities [27], while fetal hypoxaemia and acidaemia result in autonomic system–mediated decreased fetal heart rate variation (i.e., lower cCTG short-term variability [cCTG-STV]). Shallow late decelerations are indicative of both fetal acidaemia and its effect on myocardial tissue [28].

Timing of Delivery

Delivery is the only intervention that initiates resolution of preeclampsia; however, it should be remembered that it initiates and does not cure the condition. In women with severe preeclampsia, the woman’s clinical and laboratory state may well deteriorate for 24–72 hours before resolution of the condition begins. Using our definition of severe preeclampsia, all women with severe preeclampsia should be delivered immediately (either vaginally or by caesarean section), regardless of gestational age.

The phrase ‘planned delivery on the best day in the best way’ reflects the myriad of considerations regarding timing (and mode) of delivery [26]. Timing of delivery will reflect evolving complications (Table 4.1). Consensus-derived indications for delivery are (1) term gestation, (2) development of severe maternal complication(s) (Table 4.1) (3) stillbirth or (4) fetal monitoring results that indicate delivery (see the section ‘Fetal Assessment’).

Table 4.1 Definition of severe preeclampsia

Organ system affected	Adverse conditions (that increase the risk of severe preeclampsia)	Severe preeclampsia(complications that warrant delivery irrespective of gestational age)
CNS	Headache/visual symptoms	Eclampsia PRES Cortical blindness or retinal detachment Glasgow Coma Scale <13 Stroke, TIA or RIND
Cardiorespiratory	Chest pain/dyspnoea Oxygen saturation <97%	Uncontrolled severe hypertension (over a period of 12 hours despite use of three antihypertensive agents) Oxygen saturation <90%, need for ≥50% oxygen for >1 hour, intubation (other than for caesarean section), pulmonary oedema Positive inotropic support Myocardial ischemia or infarction
Haematological	Elevated WBC count Elevated INR or aPTT Low platelet count	Platelet count <50 × 109/L Transfusion of any blood product
Renal	Elevated serum creatinine Elevated serum uric acid	Acute kidney injury (creatinine >150 µM with no prior renal disease) New indication for dialysis
Hepatic	Nausea or vomiting RUQ or epigastric pain Elevated serum AST, ALT, LDH or bilirubin Low plasma albumin	Hepatic dysfunction (INR >2 in absence of DIC or warfarin) Hepatic haematoma or rupture
Feto-placental	Non-reassuring FHR FGR Oligohydramnios Absent or reversed end-diastolic flow by Doppler velocimetry	Abruption with evidence of maternal or fetal compromise Reverse ductus venosus A wave Stillbirth

Modified from Magee et al. [5].

ALT, alanine transaminase; aPTT, activated partial thromboplastin time; AST, aspartate transaminase; DIC, disseminated intravascular coagulation; FGR, fetal growth restriction; FHR, fetal heart rate; INR, international normalised ratio; LDH, lactate dehydrogenase; PRES, posterior reversible encephalopathy syndrome; RIND, reversible ischaemic neurological deficit; RUQ, right upper quadrant; TIA, transient ischaemic attack; WBC, white blood cell.

Currently, no tool exists to guide balancing risks, benefits and the preferences of the woman and her family.

The best treatment for the mother is always delivery, limiting her exposure to preeclampsia; therefore, expectant management is best considered when potential perinatal benefits are substantial, usually at early gestational ages. For women with non-severe preeclampsia complicated by HELLP (haemolysis, elevated liver enzymes, low platelet count) syndrome at 24⁺⁰–34⁺⁶ weeks gestation, it may be reasonable to delay delivery long enough to administer antenatal corticosteroids for acceleration of fetal pulmonary maturity, especially as there is often temporary improvement in maternal laboratory testing.

Expectant management of preeclampsia refers to attempted pregnancy prolongation following a period of maternal and fetal observation and assessment and maternal stabilisation. Expectant management should occur only in an experienced unit where neonates can be cared for at the woman’s current gestational age (as delivery cannot be accurately anticipated).

Expectant management at <24⁺⁰ weeks is associated with perinatal mortality >80% and maternal complications of 27%–71% (including one maternal death). Consequently, termination of pregnancy should be discussed.

Expectant management at 24⁺⁰–33⁺⁶ weeks may decrease neonatal respiratory distress syndrome, necrotising enterocolitis and neonatal intensive care, despite poor fetal growth velocity during the time gained [29, 30]. Rates of serious maternal complications appear very low (median < 5%) [31]; however, these low levels of maternal risk are predicated on obsessive maternal and fetal surveillance. Timing of delivery should be individualised, recognising that, on average, pregnancy prolongation is 2 weeks. If preeclampsia is complicated by HELLP syndrome, fewer days will be gained (median: 5 days) and serious maternal morbidity will be higher (median: 15%); >50% have temporary improvement of HELLP which may enable regional anaesthesia or vaginal delivery.

For late preterm preeclampsia (34⁺⁰–36⁺⁶ weeks), delaying delivery facilitates cervical ripening and vaginal delivery and reduces the risks of neonatal respiratory morbidity, but at a modest risk to mothers [32].

With term preeclampsia (37⁺⁰–42⁺⁰ weeks), labour induction is indicated to reduce poor maternal outcome (relative risk [RR] 0.61; 95% CI 0.45–0.82) [33].

Route of Delivery

All women with preeclampsia should be considered for labour induction. Choosing the mode of delivery should take into consideration both gestational age and fetal status. In severe early-onset preeclampsia with clinical evidence of fetal compromise, caesarean delivery may be preferable.

For labour induction, cervical ripening (even with an unfavourable cervix), increases the chance of vaginal delivery. With severe preeclampsia, this will take more time and be less successful compared with normotensive pregnancy. Neither FGR nor oligohydramnios are contraindications to induction.

Rates of vaginal delivery after induction are 6.7%–10% at 24–28 weeks (suggesting advisability of caesarean delivery with viable fetuses), 47.5% at 28–32 weeks, 68.8% at 32–34 weeks and 30% with birthweights <1500 g [34]. Vaginal delivery likelihood is reduced (but still exceeds 50%) when there is increased umbilical artery resistance [35].

Severe Hypertension

National and international guidance consistently recommends that severe pregnancy hypertension (systolic BP ≥160 mm Hg or diastolic BP ≥110 mm Hg) requires antihypertensive therapy to avoid acute cerebrovascular complications, particularly stroke. As in non-pregnancy, severe hypertension not associated with end-organ complications is usually a medical ‘urgency’ and BP can be lowered over hours. In contrast, women with end-organ complications (e.g., pulmonary oedema or acute kidney injury) should have their BP lowered over a shorter time frame; to be conservative, women with headache and visual symptoms should be regarded as having end-organ complications.

As for nonpregnancy, the goal should be to lower BP to non-severe levels (i.e., <160/110 mm Hg) over hours without reducing it by more than 25% initially, with gradual lowering over hours thereafter.

The intravascular volume depletion of preeclampsia can precipitate hypotension after the administration of antihypertensive drugs.

Hydralazine may be a less effective antihypertensive and associated with more maternal adverse effects as compared with calcium channel blockers. Hydralazine may be a more effective antihypertensive but associated with more maternal hypotension and adverse effects as compared with parenteral labetalol.

Oral nifedipine and parenteral nicardipine appear to be similarly effective for BP control as parenteral labetalol. The 10 mg nifedipine tablet may be associated with less maternal hypotension compared with the 10 mg capsule when it is bitten/punctured [38]. The 5 mg capsule may reduce the risk of a precipitous fall in BP.

In women with severe hypertension in pregnancy, single agents, nifedipine (10 mg, repeated hourly up to 30 mg) and labetalol (200 mg, repeated hourly up to 600 mg) were found to be superior to methyldopa (1000 mg as a single dose). However, while superior for maternal BP control, nifedipine use was associated with more frequent adverse neonatal events.

In summary, oral nifedipine, parenteral hydralazine and parenteral labetalol are the most commonly studied antihypertensive agents for severe hypertension. As none is clearly superior, each is a reasonable choice, in doses listed in Table 4.2.

Table 4.2 Commonly used antihypertensives for severe and non-severe pregnancy hypertension

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Related posts:

1. Chapter 8 – Uterine Rupture
2. Chapter 9 – Breech Delivery
3. Chapter 29 – Convulsions and Epilepsy
4. Chapter 45 – Risk Management

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