Setting.

The INTERGROWTH-21st Project was carried out from 2009 to 2016 across 8 diverse geographically delimited urban areas: Pelotas (Brazil), Turin (Italy), Muscat (Oman), Oxford (United Kingdom), Seattle (United States of America), Shunyi County in Beijing (China), central Nagpur (India), and the Parklands suburb of Nairobi (Kenya). Area and hospital selection has been previously described [13]. Women receiving antenatal care had to plan to deliver in these institutions or in a similar hospital located in the same geographical area.

Participants.

Participants were selected based upon WHO criteria for optimal health, nutrition, education, and socioeconomic status needed to construct international standards [13]. Women aged ≥18 and <35 years old with a body mass index (BMI) <30 kg/m² and height ≥153 cm, at low risk of adverse maternal and perinatal outcomes, who commenced antenatal care before 14 weeks’ gestation with reliable menstrual dates, and a confirmatory ultrasound dating scan and provided written informed consent are the FGLS population. Exclusion criteria included hypertension (defined as systolic ≥140 mmHg or diastolic ≥90 mmHg) in a previous pregnancy or the first trimester of the present pregnancy; chronic hypertension on treatment; and a past history of preeclampsia, eclampsia, or haemolysis, elevated liver enzymes and low platelets (HELLP) syndrome.

FGLS also excluded women whose pregnancies became complicated by a priori specified criteria including fetal death, congenital abnormality, severe or catastrophic medical morbidity not evident at enrolment (such as cancer or HIV), severe unanticipated conditions related to the pregnancy that required admission to hospital (such as severe preeclampsia or eclampsia), and those identified during the study who no longer fulfilled entry criteria (such as women who started smoking or had a malaria episode) [13].

Bias.

Entry criteria for FGLS were chosen to balance the strict WHO-recommended criteria for selecting a healthy population with external validity of the results [13].

Variables, data sources, and measurement.

Gestational age was calculated from the last menstrual period (LMP) date, provided it was certain; the woman had a regular 24- to 32-day menstrual cycle; she had not been using hormonal contraception or breastfeeding in the preceding 2 months; and any discrepancy between the gestational ages based on LMP and crown rump length (CRL), measured by ultrasound between 9 and 13⁺⁶ weeks’ gestation, was ≤7 days. The ultrasound dating scan was undertaken using standard study criteria for measuring CRL [13].

The instruction manual for measurement techniques, methods for multicentre standardisation of measures, and procedures for equipment calibration and maintenance is published [17]. All documentation, protocols, data collection forms, and electronic transfer strategies are available at www.intergrowth21.org. Trained research personnel measured systolic and diastolic blood pressure using an automated machine validated in pregnancy (Microlife Blood Pressure Monitor for Pregnant Women, Microlife USA, Florida, USA) with an appropriately sized cuff on study entry between 9 and 13⁺⁶ weeks’ gestation and every 5 ± 1 weeks until delivery (i.e., from enrolment, blood pressure was measured in the gestational age windows 14 to 18, 19 to 23, 24 to 28, 29 to 33, 34 to 38, and 39 to 42 weeks).

Study size.

The sample size for FGLS was based on practical and statistical considerations [18]. FGLS established an average sample of 500 pregnant women per study site, after exclusion of complicated pregnancies (approximately 3%) and those lost to follow-up (estimated to be 3%, S1 Text). This sample size was adequate to explore site-specific differences [18].

Quantitative variables.

We included all recorded blood pressures from all participants in the main analysis and constructed smoothed centiles for systolic and diastolic blood pressure by gestational age. We modelled blood pressure at fortnightly gestational age windows from 12 to 40 weeks. We constructed international, gestational age-specific, smoothed centiles for blood pressure following WHO recommendations [19].

Statistical methods.

We included a statistical analysis plan in our application to use data from the INTERGROWTH-21st Project (S2 Text). We assessed variation in systolic and diastolic blood pressure between sites [18] to explore whether we could pool data. We used analysis of variance (ANOVA) to calculate the percentage of variance in the longitudinal blood pressure measures from variance between sites adjusted for gestational age (fixed effects). We treated sites and individuals as random effects. We calculated a standardised site difference (SSD, similar to a z score) as the difference between the mean of 1 site and the mean of all sites. We expressed differences as a proportion of the all sites’ standard deviation (SD) at each corresponding gestational age. The SSD allows direct comparisons across gestational age windows. A priori, we specified an overall value of £ 0.5 SSD as adequate for combining data from all sites [18], as described previously for the construction of international standards in WHO MGRS and INTERGROWTH-21st studies [14]. We undertook a post hoc analysis of the effect of removing outlying sites (with SSDs >0.5).

We estimated blood pressure centiles from generalised additive models for location, scale, and shape (GAMLSS) framework. We assessed different distributions for both systolic and diastolic blood pressure within the GAMLSS framework. This included Box-Cox Cole and Green, Box-Cox Power Exponential, Box-Cox-t, Skew Power Exponential type 3, Skew t type 3, and Power Exponential. We used penalised splines and fractional polynomials to create smooth centiles across the gestational age range. We chose the best fitting distribution based on model fit (Akaike information criterion and Bayesian information criterion) and a comparison of fitted versus empirical centiles. We chose the same distribution for all subgroups within any given blood pressure.

We estimated the precision of the centiles via bootstrapping, by repeatedly sampling and analysing the dataset 50 times. We used the SD of those bootstrapped estimates to calculate the 95% confidence interval for each centile at 2-week intervals. We used the R (version 3·4; R Foundation, Vienna, Austria, www.r-project.org) and GAMLSS (version 4·3–3; R Foundation, www.gamlss.com) packages for all analyses.

We conducted a post hoc sensitivity analysis to assess the effect of excluding women who developed hypertension (defined as systolic ≥140 mmHg or diastolic ≥90 mmHg at any antenatal visit), constructing gestational age-specific centiles for blood pressure in women who remained normotensive (blood pressure <140/90 mmHg).

Finally, we performed post hoc analyses to explore changes in systolic and diastolic blood pressure by baseline for all women and by blood pressure quartile. Our statistical analysis plan included further subgroup analyses (booking BMI, booking BP, and maternal age), which will be considered in future publications.

Loss to follow-up and missing data.

Where a woman did not contribute blood pressure measures within one of the possible gestational age windows (14 to 18, 19 to 23, 24 to 28, 29 to 33, 34 to 38, and 39 to 42 weeks), we included all those available. Where women did not complete the study but we knew the final outcome, we included all the data available unless consent for data use was withdrawn.

Blood pressure.

Our findings are contrary to much published literature upholding a clinically significant mid-second trimester drop. Data underlying this view are often dated [9,10], routinely collected [21,22], single centre [9,10], and based on non-standardised measurement of blood pressure [9,10] or devices not ratified for use in pregnancy [10,21–23]. Larger, routinely acquired birth cohorts from single geographical regions show smaller drops [12,24]. More recent, prospective, standardised studies refute this dogma [25,26]. Our systematic review, including over 36,000 women, found an almost identical progressive rise in systolic blood pressure and approximately 1 mmHg mid-second trimester drop in diastolic blood pressure [27]. Taken together, clinically significant drops in population blood pressure from booking to delivery clearly do not occur in modern practice.

Confusion may have arisen because studies use different definitions of baseline blood pressure. Where prepregnancy blood pressure (rather than the first blood pressure taken in pregnancy) is used as the baseline, a small drop is generally seen mid-second trimester [11,23]. Although physiologically interesting, recent prepregnancy blood pressures are not usually available. Blood pressure patterns during pregnancy, as revealed in our study, are probably more important clinically.

Women in the lowest quartile of booking blood pressure demonstrated the largest rise in blood pressure, while the highest quartile had the greatest range of likely decreases, showing regression to the mean. These prospective findings add to previous work from routinely acquired data [12].

Limitations.

The study has limitations. The lack of prepregnancy blood pressure data may disguise a relative drop in blood pressure in early pregnancy. However, as a prepregnancy measure is rarely available in routine clinical practice, comparison with blood pressure in early pregnancy contributes to clinical applicability.

We did not exclude the few women who developed gestational hypertension (3%) or preeclampsia (<1%), rather, we chose to demonstrate that excluding these women did not affect our findings (Fig C in S3 Text). The large size of the study made it impractical to define the time of day at which blood pressure was measured to allow exploration of circadian effects. In our study, blood pressure was not measured in duplicate; however, this mirrors clinical practice. The INTERGROWTH-21st Project recruited women with a BMI <30 kg/m²; therefore, the applicability of the findings to women with a BMI ³30 kg/m² is uncertain. Further work is needed to determine how knowledge of these centiles affects the detection of deteriorating health in pregnant women.