Evaluate Azithromycin Plus Chloroquine And Sulfadoxine Plus Pyrimethamine Combinations For Intermittent Preventive Treatment Of Falciparum Malaria Infection In Pregnant Women In Africa

Phase 3

Terminated

• Conditions: Intermittent Preventive Treatment In Pregnancy (IPTp)
• Interventions: Drug: Azithromycin plus chloroquine; Drug: sulfadoxine-pyrimethamine

• Registration Number: NCT01103063
• Lead Sponsor: Pfizer

Brief Summary

The primary objective is to establish superiority of AZCQ over SP in protective efficacy for IPTp as measured by the proportion of subjects with sub-optimal pregnancy outcome.

Detailed Description

After interim analysis of efficacy data by an External Data Monitoring Committee, this study was terminated. Investigators were notified on 22 Aug 2013. There were no safety concerns that led to this termination.

Study Timeline

• Study First Submitted: 2010-04-07
• Study First Submitted QC: 2010-04-12
• Study First Posted: 2010-04-13
• Study Start: 2010-10
• Primary Completion: 2013-10
• Study Completion: 2013-11
• Results First Submitted: 2014-08-25
• Results First Submitted QC: 2014-08-25
• Results First Posted: 2014-09-05
• Status Verified: 2015-05
• Last Update Submitted: 2015-05-14
• Last Update Posted: 2015-06-16

Recruitment & Eligibility

• Status: TERMINATED
• Sex: Female
• Target Recruitment: 2891

Inclusion Criteria

• Pregnant women (all gravidae) with ≥14 and ≤26 weeks of gestational age (by ultrasound).
• Evidence of a personally signed and dated informed consent/assent document. Assent will be obtained from subjects <18 years of age.
• Subjects who are willing to and able to comply with scheduled visits, treatment plan, laboratory tests, and other study procedures.
• Subjects who are available for follow up at delivery and on 28 days post delivery.

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Exclusion Criteria

• Age <16 years old or >35 years old.
• Multiple gestations as per the ultrasound at screening.
• Clinical symptoms of malaria.
• Hemoglobin < 8 g/dL (at enrollment).
• Any condition requiring hospitalization at enrollment.
• History of convulsions, hypertension, diabetes or any other chronic illness that may adversely affect fetal growth and viability.
• Inability to tolerate oral treatment in tablet form.
• Known allergy to the study drugs (azithromycin, chloroquine, and sulfadoxine-pyrimethamine) or to any macrolides or sulphonamides.
• Requirement to use medication during the study that might interfere with the evaluation of the study drug eg, trimethoprim-sulfamethoxazole use in subjects positive for HIV infection.
• Other severe acute or chronic medical or psychiatric condition or laboratory abnormality that may increase the risk associated with study participation.
• Evidence of current obstetric complications that may adversely impact the pregnancy and/or fetal outcomes, including presence of congenital anomalies, placenta previa or abruption.
• Known severe Sickle Cell (SS) disease or Sickle Hemoglobin C (SC) anemia.
• Known family history of prolonged QT Syndrome, serious ventricular arrhythmia, or sudden cardiac death.

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Study & Design

• Study Type: INTERVENTIONAL
• Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
AZCQ	Azithromycin plus chloroquine	Azithromycin/chloroquine
SP	sulfadoxine-pyrimethamine	sulfadoxine-pyrimethamine (Fansidar)

Primary Outcome Measures

Name	Time	Method
Percentage Participants With Sub-optimal Pregnancy Outcome in Intent-to-Treat (IIT) Population	Approximately 40 weeks of gestational age	Adverse pregnancy outcomes were defined as live-borne neonate (singleton) with low birth weight (LBW) (\<2,500 g), premature births (\<37 weeks as confirmed by the Ballard score), abortion (≤28 weeks), still birth (\>28 weeks), lost to follow-up prior to termination of pregnancy or delivery, or missing birth weight of the neonates.

Secondary Outcome Measures

Name	Time	Method
Percentage of Participants With Sub-optimal Pregnancy Outcome in Efficacy Analyzable Per Protocol (PP) Population	Approximately 40 weeks of gestational age	Adverse pregnancy outcomes were defined as live-borne neonate (singleton) with LBW (\<2,500g), premature births (\<37 weeks as confirmed by the Ballard score), abortion (≤28 weeks), still birth (\>28 weeks), lost to follow-up prior to termination of pregnancy or delivery, or missing birth weight of the neonates.
Percentage of Neonates With LBW (<2500 g) in ITT Population	Approximately 40 weeks of gestational age	LBW was defined as live birth weight \<2500 g (up to and including 2499 g).
Percentage of Neonates With LBW (<2500 g) in Efficacy Analyzable PP Population	Approximately 40 weeks of gestational age	LBW was defined as live birth weight \<2500 g (up to and including 2499 g).
Percentage of Participants With Severe Maternal Anemia (Hemoglobin [Hb] <8 g/dL) at 36-38 Weeks of Gestation	At 36-38 weeks of gestation.	Severe maternal anemia was defined as Hb \<8 g/dL.
Percentage of Participants With Maternal Anemia (Hb <11 g/dL) at 36-38 Weeks of Gestation	At 36-38 weeks of gestation.	Anemia was defined as Hb \<11 g/dL.
Percentage of Participants With Placental Parasitemia at Delivery	Approximately 40 weeks of gestational age	Participants with placental parasitemia at delivery were diagnosed using Placental blood smear at birth from participants who deliver at hospital.
Percentage of Participants With Placental Malaria at Delivery Based on Histology	Approximately 40 weeks of gestational age	Participants positive for placental malaria at delivery were evaluated based on placental histology.
Sexually Transmitted Infection (STI) Episodes Per Participant	Approximately 40 weeks of gestational age .	Number of episodes of sexually transmitted infection episodes per participant were noted. The STI's including Treponema pallidum, Neisseria gonorrhoeae, Chlamydia trachomatis, from first dose to delivery (diagnosis was based on clinical presentation and lab results).
Percentage of Participants With Sub-optimal Pregnancy Outcome Including Neonatal Death and Congenital Malformation	Approximately 40 weeks of gestational age.	Sub-optimal pregnancy outcome including neonatal deaths and congenital malformations, defined as any of the following: live-borne neonate (singleton) with low birth-weight (or LBW for short, defined as live birth weight \<2,500g), premature birth (\<37 weeks), abortion (≤28 weeks), still birth (\>28 weeks), neonatal death, congenital malformation, lost to follow-up prior to termination of pregnancy or delivery, or missing birth weight of the neonates.
Change From Baseline to 36-38 Weeks of Gestation in Hb Concentration.	Baseline, at 36-38 weeks of gestation.	Change from Baseline to 36-38 weeks of gestation in Hb concentration was noted.
Percentage of Perinatal or Neonatal Deaths	Day 28 after delivery.	Percentage of perinatal or neonatal deaths were noted.
Birth Weight of Live Borne Neonate	Approximately 40 weeks of gestational age.	Birth weight of live borne neonates were calculated in grams.
Percentage of Participants With Peripheral Parasitemia at 36-38 Weeks of Gestation	At 36-38 weeks of gestation	This outcome measure evaluated the percentage of participants positive for peripheral parasitemia at 36-38 weeks of gestation. A participant was positive for parasitemia if the number of asexual parasites per μL was \>0.
Percentage of Participants With Peripheral Parasitemia at Delivery	Approximately 40 weeks of gestational age	This outcome measure evaluated the percentage of participants positive for peripheral parasitemia at delivery. A participant was positive for parasitemia if the number of asexual parasites per μL was \>0.
Percentage of Participants With Cord Blood Parasitemia at Delivery	Approximately 40 weeks of gestational age	This outcome measure evaluated the percentage of participants positive for cord blood parasitemia at delivery. A participant was positive for parasitemia if the number of asexual parasites per μL was \>0.
Percentage of Neonates With Congenital Abnormalities at Birth	Approximately 40 weeks of gestational age.	Neonates with congenital abnormalities at birth were noted.
Number of Episodes of Symptomatic Malaria Per Participant From First Intermittent Preventive Treatment of Falciparum Dose to Delivery	Approximately 40 weeks of gestational age	This outcome measure determined if an episode of malaria started within the time period of first dose to delivery. Clinical episode of malaria was determined if the participant presented with clinical symptoms of malaria (fever \>37.5°C, oral) and diagnosed (either by rapid diagnostic tests or microscopy) with malaria.
Percentage of Participants With Neisseria Gonorrhoeae Infection at 36-38 Weeks of Gestation	At 36-38 weeks of gestation	Participants positive for Neisseria gonorrhoeae infection was diagnosed based on laboratory result at 36-38 weeks of gestation. A vaginal swab was collected and PCR assay was used for analysis.
Percentage of Participants With Trichomonas Vaginalis Infection at 36-38 Weeks of Gestation	At 36-38 weeks of gestation	Participants positive for Trichomonas vaginalis infection was diagnosed based on laboratory result at 36-38 weeks of gestation. A vaginal swab was collected for the laboratory test.
Percentage of Participants Requiring Additional Treatment for Symptomatic Malaria From First Dose to Delivery	Approximately 40 weeks of gestational age	This outcome measure evaluated the participants requiring additional treatments for malaria during the study period following the first dose (diagnosed based on clinical presentation and/or lab test results).
Percentage of Participants With Sexually Transmitted Infections From First Dose to 36-38 Weeks of Gestation	Upto 36-38 weeks of gestation	Sexual transmitted disease included Treponema pallidum, Neisseria gonorrhoeae, and Chlamydia trachomatis infections. This was diagnosed based on clinical presentation prior to Week 36-38 and/or lab test results between Week 36-38.
Percentage of Participants With Chlamydia Trachomatis Infection at 36-38 Weeks of Gestation	At 36-38 weeks of gestation	Participants positive for Chlamydia trachomatis infection was diagnosed based on laboratory result at 36-38 weeks of gestation. A vaginal swab was collected and PCR assay was used for analysis.
Percentage of Participants With Bacterial Vaginosis Infection at 36-38 Weeks of Gestation.	At 36-38 weeks of gestation	Bacterial vaginosis was diagnosed based on laboratory result at 36-38 weeks of gestation. A vaginal swab was collected for the Gram staining.
Percentage of Neonates With Ophthalmia Neonatorum at Birth Period	Approximately 40 weeks of gestational age	Ophthalmia neonatorum was diagnosed at birth. The laboratory diagnosis was performed among neonates with purulent discharge.
Percentage of Participants With Bacterial Infections Including Pneumonia and Other Lower Respiratory Tract Infections From First Dose to Delivery	Up to approximately 40 weeks of gestational age	Participants positive for bacterial infections including other lower respiratory tract infections were measured anytime from first dose administration to delivery.
Percentage of Participants With Pre-eclampsia From Week 20 to Delivery	From Week 20 to approximately 40 weeks of gestational age	Pre-eclampsia was diagnosed as systolic blood pressure of at least 140 mmHg and/or diastolic blood pressure of at least 90 mmHg on two separate readings taken at least 4 hours apart and proteinuria at least 300 mg protein in a 24 hour urine collection.
Nasopharyngeal Swabs Positive for Macrolide Resistant Streptococcus Pneumoniae	Visits 6 and 7	This outcome measure evaluated the Streptococcus pneumoniae sensitivity against macrolide antibiotics.
Nasopharyngeal Swabs Positive for Penicillin Resistant Streptococcus Pneumoniae	Visits 6 and 7	This outcome measure evaluated the Streptococcus pneumoniae sensitivity against penicillin antibiotics.
Percentage of Participants With Treponema Pallidum Infection at 36-38 Weeks of Gestation	At 36-38 weeks of gestation	Participants positive for Treponema pallidum infection was diagnosed based on laboratory result at 36-38 weeks of gestation. Treponema Pallidum particle Agglutination Assay was used.

Trial Locations

Locations (9)

Bugando Medical Centre; 🇹🇿 Mwanza, Tanzania

Zomba Central Hospital; 🇲🇼 Zomba, Malawi

Nyamagana District Hospital; 🇹🇿 Mwanza, Tanzania

Nyamagana District Hospital, c/o National Institute for Medical Research, Mwanza Centre; 🇹🇿 Mwanza, Tanzania

Centre de Santé d'AHOUANSORI-AGUE; 🇧🇯 Cotonou, Benin

Hôpital Bethesda; 🇧🇯 Cotonou, Benin

Siaya District Hospital; 🇰🇪 Siaya, Kenya

Mulago Hospital Complex; 🇺🇬 Kampala, Uganda

Teule Hospital; 🇹🇿 Muheza, Tanga, Tanzania