A description of the methods of the aspirin supplementation for pregnancy indicated risk reduction in nulliparas (ASPIRIN) study

A description of the methods of the aspirin supplementation for pregnancy indicated risk reduction in nulliparas (ASPIRIN) study

Abstract Background Preterm birth (PTB) remains the leading cause of neonatal mortality and long term disability throughout the world. Though complex in its origins, a growing body of evidence suggests that first trimester administration of low dose aspirin (LDA) may substantially reduce the rate of...

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Main Authors: Matthew K. Hoffman, Shivaprasad S. Goudar, Bhalachandra S. Kodkany, Norman Goco, Marion Koso-Thomas, Menachem Miodovnik, Elizabeth M. McClure, Dennis D. Wallace, Jennifer J. Hemingway-Foday, Antoinette Tshefu, Adrien Lokangaka, Carl L. Bose, Elwyn Chomba, Musaku Mwenechanya, Waldemar A. Carlo, Ana Garces, Nancy F. Krebs, K. Michael Hambidge, Sarah Saleem, Robert L. Goldenberg, Archana Patel, Patricia L. Hibberd, Fabian Esamai, Edward A. Liechty, Robert Silver, Richard J. Derman
Format: Article
Language:English
Published: BMC 2017-05-01
Series:BMC Pregnancy and Childbirth
Subjects:
Prematurity
Preterm birth
Low dose Aspirin
Online Access:http://link.springer.com/article/10.1186/s12884-017-1312-x
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spelling doaj-b04749230cc347f89a09567a7270db3a2020-11-25T00:53:08ZengBMCBMC Pregnancy and Childbirth1471-23932017-05-0117111510.1186/s12884-017-1312-xA description of the methods of the aspirin supplementation for pregnancy indicated risk reduction in nulliparas (ASPIRIN) studyMatthew K. Hoffman0Shivaprasad S. Goudar1Bhalachandra S. Kodkany2Norman Goco3Marion Koso-Thomas4Menachem Miodovnik5Elizabeth M. McClure6Dennis D. Wallace7Jennifer J. Hemingway-Foday8Antoinette Tshefu9Adrien Lokangaka10Carl L. Bose11Elwyn Chomba12Musaku Mwenechanya13Waldemar A. Carlo14Ana Garces15Nancy F. Krebs16K. Michael Hambidge17Sarah Saleem18Robert L. Goldenberg19Archana Patel20Patricia L. Hibberd21Fabian Esamai22Edward A. Liechty23Robert Silver24Richard J. Derman25Christiana CareKLE’s JN Medical CollegeKLE’s JN Medical CollegeRTI InternationalEunice Kennedy Shriver National Institute of Child Health and Human DevelopmentEunice Kennedy Shriver National Institute of Child Health and Human DevelopmentRTI InternationalRTI InternationalRTI InternationalKinshasa School of Public HealthKinshasa School of Public HealthUniversity of North CarolinaUniversity Teaching HospitalUniversity Teaching HospitalUniversity of Alabama at BirminghamInstituto de Nutrición de Centroamérica y Panamá (INCAP)University of Colorado School of MedicineUniversity of Colorado School of MedicineAga Khan UniversityColumbia UniversityLata Medical Research FoundationBoston University School of Public HealthDepartment of Child Health and Paediatrics, Moi University School of MedicineSchool of Medicine, Indiana UniversityUniversity of UtahThomas Jefferson UniversityAbstract Background Preterm birth (PTB) remains the leading cause of neonatal mortality and long term disability throughout the world. Though complex in its origins, a growing body of evidence suggests that first trimester administration of low dose aspirin (LDA) may substantially reduce the rate of PTB. Methods Hypothesis: LDA initiated in the first trimester reduces the risk of preterm birth. Study Design Type: Prospective randomized, placebo-controlled, double-blinded multi-national clinical trial conducted in seven low and middle income countries. Trial will be individually randomized with one-to-one ratio (intervention/control) Population: Nulliparous women between the ages of 14 and 40, with a singleton pregnancy between 6 0/7 weeks and 13 6/7 weeks gestational age (GA) confirmed by ultrasound prior to enrollment, no more than two previous first trimester pregnancy losses, and no contraindications to aspirin. Intervention: Daily administration of low dose (81 mg) aspirin, initiated between 6 0/7 weeks and 13 6/7 weeks GA and continued to 36 0/7 weeks GA, compared to an identical appearing placebo. Compliance and outcomes will be assessed biweekly. Outcomes Primary outcome: Incidence of PTB (birth prior to 37 0/7 weeks GA). Secondary outcomes Incidence of preeclampsia/eclampsia, small for gestational age and perinatal mortality. Discussion This study is unique as it will examine the impact of LDA early in pregnancy in low-middle income countries with preterm birth as a primary outcome. The importance of developing low-cost, high impact interventions in low-middle income countries is magnified as they are often unable to bear the financial costs of treating illness. Trial registration ClinicalTrials.gov identifier: NCT02409680 Date: March 30, 2015http://link.springer.com/article/10.1186/s12884-017-1312-xPrematurityPreterm birthLow dose Aspirin
collection DOAJ
language English
format Article
sources DOAJ
author Matthew K. Hoffman
Shivaprasad S. Goudar
Bhalachandra S. Kodkany
Norman Goco
Marion Koso-Thomas
Menachem Miodovnik
Elizabeth M. McClure
Dennis D. Wallace
Jennifer J. Hemingway-Foday
Antoinette Tshefu
Adrien Lokangaka
Carl L. Bose
Elwyn Chomba
Musaku Mwenechanya
Waldemar A. Carlo
Ana Garces
Nancy F. Krebs
K. Michael Hambidge
Sarah Saleem
Robert L. Goldenberg
Archana Patel
Patricia L. Hibberd
Fabian Esamai
Edward A. Liechty
Robert Silver
Richard J. Derman
spellingShingle Matthew K. Hoffman
Shivaprasad S. Goudar
Bhalachandra S. Kodkany
Norman Goco
Marion Koso-Thomas
Menachem Miodovnik
Elizabeth M. McClure
Dennis D. Wallace
Jennifer J. Hemingway-Foday
Antoinette Tshefu
Adrien Lokangaka
Carl L. Bose
Elwyn Chomba
Musaku Mwenechanya
Waldemar A. Carlo
Ana Garces
Nancy F. Krebs
K. Michael Hambidge
Sarah Saleem
Robert L. Goldenberg
Archana Patel
Patricia L. Hibberd
Fabian Esamai
Edward A. Liechty
Robert Silver
Richard J. Derman
A description of the methods of the aspirin supplementation for pregnancy indicated risk reduction in nulliparas (ASPIRIN) study
BMC Pregnancy and Childbirth
Prematurity
Preterm birth
Low dose Aspirin
author_facet Matthew K. Hoffman
Shivaprasad S. Goudar
Bhalachandra S. Kodkany
Norman Goco
Marion Koso-Thomas
Menachem Miodovnik
Elizabeth M. McClure
Dennis D. Wallace
Jennifer J. Hemingway-Foday
Antoinette Tshefu
Adrien Lokangaka
Carl L. Bose
Elwyn Chomba
Musaku Mwenechanya
Waldemar A. Carlo
Ana Garces
Nancy F. Krebs
K. Michael Hambidge
Sarah Saleem
Robert L. Goldenberg
Archana Patel
Patricia L. Hibberd
Fabian Esamai
Edward A. Liechty
Robert Silver
Richard J. Derman
author_sort Matthew K. Hoffman
title A description of the methods of the aspirin supplementation for pregnancy indicated risk reduction in nulliparas (ASPIRIN) study
title_short A description of the methods of the aspirin supplementation for pregnancy indicated risk reduction in nulliparas (ASPIRIN) study
title_full A description of the methods of the aspirin supplementation for pregnancy indicated risk reduction in nulliparas (ASPIRIN) study
title_fullStr A description of the methods of the aspirin supplementation for pregnancy indicated risk reduction in nulliparas (ASPIRIN) study
title_full_unstemmed A description of the methods of the aspirin supplementation for pregnancy indicated risk reduction in nulliparas (ASPIRIN) study
title_sort description of the methods of the aspirin supplementation for pregnancy indicated risk reduction in nulliparas (aspirin) study
publisher BMC
series BMC Pregnancy and Childbirth
issn 1471-2393
publishDate 2017-05-01
description Abstract Background Preterm birth (PTB) remains the leading cause of neonatal mortality and long term disability throughout the world. Though complex in its origins, a growing body of evidence suggests that first trimester administration of low dose aspirin (LDA) may substantially reduce the rate of PTB. Methods Hypothesis: LDA initiated in the first trimester reduces the risk of preterm birth. Study Design Type: Prospective randomized, placebo-controlled, double-blinded multi-national clinical trial conducted in seven low and middle income countries. Trial will be individually randomized with one-to-one ratio (intervention/control) Population: Nulliparous women between the ages of 14 and 40, with a singleton pregnancy between 6 0/7 weeks and 13 6/7 weeks gestational age (GA) confirmed by ultrasound prior to enrollment, no more than two previous first trimester pregnancy losses, and no contraindications to aspirin. Intervention: Daily administration of low dose (81 mg) aspirin, initiated between 6 0/7 weeks and 13 6/7 weeks GA and continued to 36 0/7 weeks GA, compared to an identical appearing placebo. Compliance and outcomes will be assessed biweekly. Outcomes Primary outcome: Incidence of PTB (birth prior to 37 0/7 weeks GA). Secondary outcomes Incidence of preeclampsia/eclampsia, small for gestational age and perinatal mortality. Discussion This study is unique as it will examine the impact of LDA early in pregnancy in low-middle income countries with preterm birth as a primary outcome. The importance of developing low-cost, high impact interventions in low-middle income countries is magnified as they are often unable to bear the financial costs of treating illness. Trial registration ClinicalTrials.gov identifier: NCT02409680 Date: March 30, 2015
topic Prematurity
Preterm birth
Low dose Aspirin
url http://link.springer.com/article/10.1186/s12884-017-1312-x
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