Low dose aspirin in hypertensive pregnant women: effect on pregnancy outcome and prostacyclin‐thromboxane balance in mother and newborn

Viinikka, Lasse; Hartikainen‐Sorri, Anna‐Liisa; Lumme, Riitta; Hiilesmaa, Vilho; Ylikorkala, Olavi

doi:10.1111/j.1471-0528.1993.tb14304.x

Cited by 84 publications

(15 citation statements)

References 24 publications

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“…In this study, aspirin and dipyridamole did not prolong the bleeding time. Previous studies of patients receiving low-dose aspirin have reported prolonged bleeding time, which was not associated with clinical bleeding [15,16]. The explanation of this discrepancy is not clear, but it may be related to the lower dose of aspirin used in our study compared with other studies (40 mg vs 50-60 mg), different methods of measurement, and the small number of subjects in our study.…”

Section: Discussioncontrasting

confidence: 66%

Platelet function in pregnant women receiving aspirin and dipyridamole

Kinouchi¹,

Fujita

Narahara

et al. 2000

Journal of Anesthesia

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Section: Discussioncontrasting

confidence: 66%

Platelet function in pregnant women receiving aspirin and dipyridamole

Kinouchi¹,

Fujita

Narahara

et al. 2000

Journal of Anesthesia

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“…Low-dose aspirin has been proven to reduce the risk of pregnancy-induced hypertension (PIH) complicated with proteinuria (preeclampsia), and/or of intrauterine growth retardation, and to a lesser extent the risk of noncomplicated PIH, only in selected multiparous or mixed popula tions with a high risk of developing these complications [1][2][3][4][5][6] but not in nonselected populations with moderate risk as in the recent Italian study [7], In the pioneering study ofBeaufils et al [1] in multipa ras the selection criteria were severe vascular complica tions during the previous pregnancies (early precclampsia, in utero fetal death, abruptio placentae, pregnancy-in duced hypertension with small for gestational age (SGA) babies. The same type of criteria were used in the study of Benigni et al [2] and Uzan et al [3].…”

Section: P-human Chorionic Gonadotrophinmentioning

confidence: 99%

Validity in Nulliparas of Increased b-Human Chorionic Gonadotrophin at Mid-Term for Predicting Pregnancy-Induced Hypertension Complicated with Proteinuria and Intrauterine Growth Retardation

Vaillant

David

Constant

et al. 1996

Nephron

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The objective of the present study was to investigate whether increased β-human chorionic gonadotrophin (βHCG) plasma concentrations in an unselected population of nulliparas could predict the occurrence of complicated pregnancy-induced hypertension (PIH). The design was that of a prospective population study. It was conducted at the obstetric departments of Amiens University Hospital and Creil General Hospital on 434 consecutive nulliparas with singleton pregnancies after natural fertilization who accepted the systematic offer of trisomy 21 screening but for whom this disorder was finally eliminated. Measurement of plasma concentration of βHCG (ELISA method) was carried out between 14 and 20 weeks (mean: 17 weeks) of amenorrhea, and measurement of blood pressure and proteinuria ( > 300 mg/24 h or Albustix ++) during the first, second and third term and 2-3 months after the delivery, as well as measurement of birth weight for determination of small for gestational age (SGA) babies. 37 women developed PIH, 10 without other complication, 16 with proteinuria (5 of which with SGA babies) and 11 with SGA babies. Furthermore 2 patients presented abruptio placentae without PIH. 395 women did not develop PIH including 389 normotensive women and 6 chronic hypertensive patients without superimposed toxemia. Only 1 was diabetic. None had chronic renal disease. Mean ( ± SD) levels of βHCG were higher in PIH than in controls: 46,805 ± 19,068 versus 23,479 ± 13,463 IU. A pathological threshold was chosen as the mean for the whole population + 1 SD: 25,613 + 15,479 = 41,082 IU. Elevated levels (above this value) were significantly associated with isolated PIH or PIH complicated with proteinuria and/or with SGA babies. The positive predictive value of this criterion was respectively 11, 15 and 12% for each of these complications. The relative risk (and 95% confidence limit) of women with elevated βHCG for each of these complications was 20 (6-79), 11 (4-43) and 22 (7-93). Elevated plasma βHCG found around 17 weeks of amenorrhea predicts PIH complicated with either proteinuria or SGA babies with a positive predictive value comparable to that of the best and earliest test proposed up to now to select nulliparas at high risk of preeclampsia, namely the abnormalities of the Doppler waveforms of the uterine arteries. Since this test is simpler to perform, it represents the most convenient method to screen a population of nulliparas for evaluation of the benefits of low-dose aspirin.

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“…[28][29][30][31] A avaliação da redução do risco de restrição de crescimento fetal com o uso de aspirina foi definida como objetivo principal num estudo multicêntrico, publicado em 1991, o estudo EPREDA. 30 Concluiu que com a utilização entre as 15 -18 semanas de aspirina na dose de 150 mg, associada a dipiridamol (225 mg/dia) houve prevenção do risco de restrição de crescimento fetal, em grávidas com este antecedente.…”

Section: Methodsunclassified

“…Vinikka et al, 31 utilizando uma baixa dose (50 mg) de ácido acetilsalicílico iniciado em média às 15 semanas em mulheres com hipertensão arterial prévia à gravidez ou pré--eclâmpsia grave em gestação anterior, verificou que, em comparação com os controles, os agentes anti-plaquetá-rios não impediram a subida da pressão arterial materna, mas melhoraram os resultados fetais, com melhor resposta hemodinâmica fetal, redução de restrição de crescimento fetal e menor necessidade de internamento em unidades de cuidados intensivos neonatais. Verificaram uma forte inibição do tromboxano A2 materno, sem redução da produção de prostaciclina, preponderando portanto a dominância da ação vasodilatadora e de anti-agregação plaquetária.…”

Section: Methodsunclassified

O Papel da Aspirina na Prevenção da Pré-Eclâmpsia: Estado da Arte

Campos

2015

Acta Med Port

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Acta Med Port 2015 Jul-Aug;28(4):517-524 RESUMOIntrodução: O papel do ácido acetilsalicílico (AAS ou aspirina) na prevenção das complicações associadas à pré-eclâmpsia tem sido objeto de estudos e de controvérsias ao longo de 30 anos. Os primeiros trabalhos de investigação acerca do papel da placenta na gé-nese da pré-eclâmpsia surgiram em finais dos anos 70 e assinalavam um aumento da atividade plaquetária e alteração da síntese das prostaglandinas, como consequência da deficiente adaptação da placenta. Ao longo dos últimos 20 anos do século XX, sucederam-se estudos de investigação acerca do papel profilático da aspirina na redução do risco de pré-eclâmpsia. Material e Métodos: Para analisar os trabalhos publicados sobre o uso da aspirina na prevenção da pré-eclâmpsia, bem como sobre a dose mais adequada e momento de administração, foram consultados apenas estudos prospetivos, revisões sistemáticas e meta-análises através das seguintes fontes pesquisa (PubMed, Cochrane, Embase). Os artigos citados foram considerados os mais relevantes. Os trabalhos foram divididos em dois grupos: no primeiro foram incluídos os trabalhos em que a aspirina era administrada até às 16 semanas e o segundo, com início de administração por um período mais alargado. Resultados e Discussão:No primeiro grupo, com menor número de casos, mas com início mais precoce de administração do fár-maco, até às 16 semanas, concluiu-se que a aspirina poderia ter um papel positivo na redução de risco de gravidade da pré-eclâmpsia; o segundo grupo, com maior número de casos nos estudos, mas com condições menos restritas de entrada e de tempo de início do fármaco, teve resultados mais controversos. As meta-análises destes estudos concluíram que os resultados favoráveis estavam associados às condições de e momento da administração. Conclusão: Não existindo ainda alternativas ou fármacos que lhe possam ser associados, a aspirina em baixas doses (80 a 150 mg/ dia) ao deitar, iniciada no 1º trimestre e até às 16 semanas mantém-se um fármaco seguro, que tem contribuído para redução do risco de pré-eclâmpsia precoce, com as consequências que lhe estão associadas. Palavras-chave: Aspirina; Pré-eclâmpsia/prevenção e controlo. ABSTRACT Introduction:The role of acetyl salicylic acid (ASA or aspirin) in preeclampsia prevention and in other complications has been subject to studies and controversies for the last 30 years. The first research results concerning the role of placenta in preeclampsia have been published by the end of seventies and they showed an increase in the platelet activity and a prostaglandin synthesis disturbance, as a consequence of a deficient placentation. In the last twenty years of the XX century important studies were published on the aspirin prophylactic role in preeclampsia risk reduction. Material and Methods:To analyze published studies about Aspirin use for preeclampsia prevention and about the more adequate dosage to be administered, Medline was used for searching the most relevant prospective research papers on this subject in order ...

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Low dose aspirin in hypertensive pregnant women: effect on pregnancy outcome and prostacyclin‐thromboxane balance in mother and newborn

Cited by 84 publications

References 24 publications

Platelet function in pregnant women receiving aspirin and dipyridamole

Platelet function in pregnant women receiving aspirin and dipyridamole

Validity in Nulliparas of Increased b-Human Chorionic Gonadotrophin at Mid-Term for Predicting Pregnancy-Induced Hypertension Complicated with Proteinuria and Intrauterine Growth Retardation

O Papel da Aspirina na Prevenção da Pré-Eclâmpsia: Estado da Arte

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