TY - JOUR
T1 - Blood pressure thresholds in pregnancy for identifying maternal and infant risk
T2 - a secondary analysis of Community-Level Interventions for Pre-eclampsia (CLIP) trial data
AU - CLIP Study Group
AU - Bone, Jeffrey N.
AU - Magee, Laura A.
AU - Singer, Joel
AU - Nathan, Hannah
AU - Qureshi, Rahat N.
AU - Sacoor, Charfudin
AU - Sevene, Esperança
AU - Shennan, Andrew
AU - Bellad, Mrutyunjaya B.
AU - Goudar, Shivaprasad S.
AU - Mallapur, Ashalata A.
AU - Munguambe, Khátia
AU - Vidler, Marianne
AU - Bhutta, Zulfiqar A.
AU - von Dadelszen, Peter
AU - Woo Kinshella, Mai Lei
AU - Wong, Hubert
AU - Vilanculo, Faustino
AU - Vala, Anifa
AU - Ukah, Ugochi V.
AU - Tu, Domena K.
AU - Thabane, Lehana
AU - Tchavana, Corsino
AU - Thornton, Jim
AU - Sotunsa, John O.
AU - Sheikh, Sana
AU - Sharma, Sumedha
AU - Schuurman, Nadine
AU - Sawchuck, Diane
AU - Revankar, Amit P.
AU - Raza, Farrukh
AU - Ramdurg, Umesh Y.
AU - Pires, Rosa
AU - Payne, Beth A.
AU - Nobela, Vivalde
AU - Nkumbula, Cláudio
AU - Nhancolo, Ariel
AU - Nhamirre, Zefanias
AU - Mungarwadi, Geetanjali I.
AU - Mulungo, Dulce
AU - Mocumbi, Sibone
AU - Mitton, Craig
AU - Merialdi, Mario
AU - Memon, Javed
AU - Matavele, Analisa
AU - Mastiholi, Sphoorthi S.
AU - Mandlate, Ernesto
AU - Maculuve, Sónia
AU - Macuacua, Salésio
AU - Macete, Eusébio
N1 - Funding Information:
The CLIP trials were funded by the University of British Columbia, a grantee of the Gates Foundation (PRE-EMPT initiative, OPP1017337). We thank the Government of Mozambique, Province of Sindh, and Government of India for permission to integrate the CLIP trials into their health systems with in-kind support.
Funding Information:
The CLIP trials were funded by the University of British Columbia, a grantee of the Gates Foundation (PRE-EMPT initiative, OPP1017337). We thank the Government of Mozambique, Province of Sindh, and Government of India for permission to integrate the CLIP trials into their health systems with in-kind support.
Publisher Copyright:
© 2021 The Author(s). Published by Elsevier Ltd. This is an Open Access article under the CC BY 4.0 license
Copyright:
Copyright 2021 Elsevier B.V., All rights reserved.
PY - 2021/8
Y1 - 2021/8
N2 - Background: Blood pressure measurement is a marker of antenatal care quality. In well resourced settings, lower blood pressure cutoffs for hypertension are associated with adverse pregnancy outcomes. We aimed to study the associations between blood pressure thresholds and adverse outcomes and the diagnostic test properties of these blood pressure cutoffs in low-resource settings. Methods: We did a secondary analysis of data from 22 intervention clusters in the Community-Level Interventions for Pre-eclampsia (CLIP) cluster randomised trials (NCT01911494) in India (n=6), Mozambique (n=6), and Pakistan (n=10). We included pregnant women aged 15–49 years (12–49 years in Mozambique), identified in their community by trained community health workers, who had data on blood pressure measurements and outcomes. The trial was unmasked. Maximum blood pressure was categorised as: normal blood pressure (systolic blood pressure [sBP] <120 mm Hg and diastolic blood pressure [dBP] <80 mm Hg), elevated blood pressure (sBP 120–129 mm Hg and dBP <80 mm Hg), stage 1 hypertension (sBP 130–139 mm Hg or dBP 80–89 mm Hg, or both), non-severe stage 2 hypertension (sBP 140–159 mm Hg or dBP 90–109 mm Hg, or both), or severe stage 2 hypertension (sBP ≥160 mm Hg or dBP ≥110 mm Hg, or both). We classified women according to the maximum blood pressure category reached across all visits for the primary analyses. The primary outcome was a maternal, fetal, or neonatal mortality or morbidity composite. We estimated dose-response relationships between blood pressure category and adverse outcomes, as well as diagnostic test properties. Findings: Between Nov 1, 2014, and Feb 28, 2017, 21 069 women (6067 in India, 4163 in Mozambique, and 10 839 in Pakistan) contributed 103 679 blood pressure measurements across the three CLIP trials. Only women with non-severe or severe stage 2 hypertension, as discrete diagnostic categories, experienced more adverse outcomes than women with normal blood pressure (risk ratios 1·29–5·88). Using blood pressure categories as diagnostic thresholds (women with blood pressure within the category or any higher category vs those with blood pressure in any lower category), dose-response relationships were observed between increasing thresholds and adverse outcomes, but likelihood ratios were informative only for severe stage 2 hypertension and maternal CNS events (likelihood ratio 6·36 [95% CI 3·65–11·07]) and perinatal death (5·07 [3·64–7·07]), particularly stillbirth (8·53 [5·63–12·92]). Interpretation: In low-resource settings, neither elevated blood pressure nor stage 1 hypertension were associated with maternal, fetal, or neonatal mortality or morbidity adverse composite outcomes. Only the threshold for severe stage 2 hypertension met diagnostic test performance standards. Current diagnostic thresholds for hypertension in pregnancy should be retained. Funding: University of British Columbia, the Bill & Melinda Gates Foundation.
AB - Background: Blood pressure measurement is a marker of antenatal care quality. In well resourced settings, lower blood pressure cutoffs for hypertension are associated with adverse pregnancy outcomes. We aimed to study the associations between blood pressure thresholds and adverse outcomes and the diagnostic test properties of these blood pressure cutoffs in low-resource settings. Methods: We did a secondary analysis of data from 22 intervention clusters in the Community-Level Interventions for Pre-eclampsia (CLIP) cluster randomised trials (NCT01911494) in India (n=6), Mozambique (n=6), and Pakistan (n=10). We included pregnant women aged 15–49 years (12–49 years in Mozambique), identified in their community by trained community health workers, who had data on blood pressure measurements and outcomes. The trial was unmasked. Maximum blood pressure was categorised as: normal blood pressure (systolic blood pressure [sBP] <120 mm Hg and diastolic blood pressure [dBP] <80 mm Hg), elevated blood pressure (sBP 120–129 mm Hg and dBP <80 mm Hg), stage 1 hypertension (sBP 130–139 mm Hg or dBP 80–89 mm Hg, or both), non-severe stage 2 hypertension (sBP 140–159 mm Hg or dBP 90–109 mm Hg, or both), or severe stage 2 hypertension (sBP ≥160 mm Hg or dBP ≥110 mm Hg, or both). We classified women according to the maximum blood pressure category reached across all visits for the primary analyses. The primary outcome was a maternal, fetal, or neonatal mortality or morbidity composite. We estimated dose-response relationships between blood pressure category and adverse outcomes, as well as diagnostic test properties. Findings: Between Nov 1, 2014, and Feb 28, 2017, 21 069 women (6067 in India, 4163 in Mozambique, and 10 839 in Pakistan) contributed 103 679 blood pressure measurements across the three CLIP trials. Only women with non-severe or severe stage 2 hypertension, as discrete diagnostic categories, experienced more adverse outcomes than women with normal blood pressure (risk ratios 1·29–5·88). Using blood pressure categories as diagnostic thresholds (women with blood pressure within the category or any higher category vs those with blood pressure in any lower category), dose-response relationships were observed between increasing thresholds and adverse outcomes, but likelihood ratios were informative only for severe stage 2 hypertension and maternal CNS events (likelihood ratio 6·36 [95% CI 3·65–11·07]) and perinatal death (5·07 [3·64–7·07]), particularly stillbirth (8·53 [5·63–12·92]). Interpretation: In low-resource settings, neither elevated blood pressure nor stage 1 hypertension were associated with maternal, fetal, or neonatal mortality or morbidity adverse composite outcomes. Only the threshold for severe stage 2 hypertension met diagnostic test performance standards. Current diagnostic thresholds for hypertension in pregnancy should be retained. Funding: University of British Columbia, the Bill & Melinda Gates Foundation.
UR - http://www.scopus.com/inward/record.url?scp=85110700357&partnerID=8YFLogxK
U2 - 10.1016/S2214-109X(21)00219-9
DO - 10.1016/S2214-109X(21)00219-9
M3 - Article
AN - SCOPUS:85110700357
SN - 2214-109X
VL - 9
SP - e1119-e1128
JO - The Lancet Global Health
JF - The Lancet Global Health
IS - 8
ER -