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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT00163020
Other study ID # OBX0003
Secondary ID OBX 0012
Status Completed
Phase Phase 2/Phase 3
First received September 9, 2005
Last updated November 4, 2015
Start date November 2004
Est. completion date August 2009

Study information

Verified date October 2012
Source Mednax Center for Research, Education and Quality
Contact n/a
Is FDA regulated No
Health authority United States: Food and Drug Administration
Study type Interventional

Clinical Trial Summary

Hypothesis: Among women with twin or triplet pregnancies, weekly injections of 17-alpha-hydroxyprogesterone caproate (17OHP), started before 24 weeks of gestation, will reduce neonatal morbidity by reducing the rate of preterm delivery.

This study involves two concurrent double-blinded randomized clinical trials of 17OHP versus placebo. Each trial will test the efficacy and safety of 17OHP in women with a specific risk factor for preterm birth. The two risk factors to be studied are:

1. Twin pregnancy

2. Triplet pregnancy


Description:

Prematurity is a leading cause of neonatal morbidity and mortality in the USA. Nationally, 12% of all babies deliver before term and 3% deliver before 32 wks gestational age (GA). Recent studies suggest that 17OHP and other progesterone derivatives may reduce the rate of preterm birth among women with a history of prior preterm birth. However, it has not been demonstrated that this reduction in preterm birth is accompanied by a clinically significant reduction in neonatal complications. Further, most women who deliver preterm have no history of a prior preterm birth. Little is known about whether progesterone treatment is effective in women with other risk factors for preterm birth such as multiple gestation. The proposed study will assess the role of 17OHP in women with twin or triplet pregnancies and will assess the impact on neonatal health, not merely the impact on gestational age at delivery. Prior studies were not designed to be large enough to have statistical power to assess effects on neonatal morbidity.

In the 6 trials combined in the Goldstein meta-analysis, only 279 women were treated with 17OHP and only 73 women had a preterm delivery. The NICHD study presented by Meis approximately doubles the world-wide experience, with 306 women under treatment, of whom 73 delivered prior to 35 wks. Yet, this study was not designed to have power to show a reduction in neonatal complications but only a reduction in preterm birth rates.

The present study is the first to be specifically designed to have adequate power to test whether 17OHP reduces neonatal morbidity among women with one of two specific risk factors for preterm birth.


Recruitment information / eligibility

Status Completed
Enrollment 321
Est. completion date August 2009
Est. primary completion date August 2009
Accepts healthy volunteers No
Gender Female
Age group 18 Years to 65 Years
Eligibility Inclusion Criteria:

1. Gestational age (GA) 15-23w0d gestational age at the time of recruitment

2. GA 16w0dk to 23w6d at the time of randomization and initiation of injections

3. Maternal age 18 years or older

4. One of these risk factors for spontaneous preterm birth:

1. Twins in current pregnancy, dichorionic placentation

2. Triplets in current pregnancy, trichorionic placentation

5. Intact membranes

6. Patient has had at least one detailed 2nd-trimester ultrasound examination documenting placentation, chorionicity, fetal number, fetal size, amniotic fluid volumes, and fetal anatomy. (This examination must comply with minimum standards such as those published by the American Institute of Ultrasound in Medicine, American College of Radiology, or American College of Obstetricians & Gynecologists It is NOT mandatory that this examination be performed at the research-study center.)

7. Investigator believes patient will be reliable with follow-up visits and believes that delivery data and neonatal data are likely to be available.

Exclusion Criteria:

1. Symptomatic uterine contractions in current pregnancy

2. Contraindication to interventions intended to prolong the pregnancy (including lethal fetal anomalies, amnionitis, preeclampsia, severe oligohydramnios, severe growth delay, fetal death appears imminent or inevitable)

3. Risk factors for major neonatal morbidity unrelated to preterm delivery (such as monochorionic placentation in multiple gestation, major malformations, certain medication exposures)

4. Preexisting maternal medical condition that might be worsened by progesterone therapy, including: asthma requiring medications, renal insufficiency, seizure disorder, ischemic heart disease, active cholecystitis, impaired liver function, history of thromboembolic disorder, history of breast cancer, history of major depression requiring hospitalization.

5. Preexisting maternal medical condition associated with a high risk of preterm delivery including: refractory hypertension, diabetes with nephropathy or retinopathy, renal insufficiency, active systemic lupus erythematosus. Note that a history of prior preterm birth is NOT an exclusion.

6. Use of progesterone or progesterone-derivative medication after 15 weeks gestation in current pregnancy.

7. Allergy to 17OHP or oil vehicle.

8. Placement of emergent cerclage (defined as one placed after the occurrence of cervical change such as dilation, funneling, or effacement) with this pregnancy. Prophylactic cerclage is NOT an exclusion (defined as one placed before any cervical change, for example, because of a history of cervical incompetence, or because of a prior cervical procedure such as LEEP or cone biopsy).

Study Design

Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment


Related Conditions & MeSH terms


Intervention

Drug:
17-alpha-hydroxyprogesterone caproate injectable
250mg of 17-alpha-hydroxyprogesterone caproate (+ preservatives) injectable weekly starting as early as 19wks gestation until 34.0wks gestation of delivery which ever comes first.
Placebo
Weekly doses of placebo (NS + preservatives) via injection as early as 19weeks until 34.0weeks gestation or delivery which ever comes first.

Locations

Country Name City State
United States Erlanger Medical Center Chattanooga Tennessee
United States Baylor University Medical Center Dallas Texas
United States Presbyterian/St Luke's Hospital Denver Colorado
United States Rose Medical Center Denver Colorado
United States Swedish Medical Center Denver Colorado
United States Mercy Medical Center Des Moines Iowa
United States Harris Methodist Fort Worth Hospital Fort Worth Texas
United States Saint Luke's Hospital, Kansas City Kansas City Missouri
United States Evergreen Hospital Kirkland Washington
United States Saddleback Memorial Medical Center Laguna Hills California
United States Skyridge Medical Center Lonetree Colorado
United States Long Beach Memorial Medical Center Long Beach California
United States University of Southern California-Irvine Medical Center Orange California
United States Banner Good Samaritan Hospital Phoenix Arizona
United States Good Samaritan Hospital San Jose California
United States Swedish Medical Center Seattle Washington
United States Tacoma General Hospital Tacoma Washington
United States Tucson Medical Center Tucson Arizona

Sponsors (1)

Lead Sponsor Collaborator
Obstetrix Medical Group

Country where clinical trial is conducted

United States, 

References & Publications (4)

American College of Obstetricians & Gynecologists. Special problems of multiple gestation. Educational Bulletin 253, 1998.

da Fonseca EB, Bittar RE, Carvalho MH, Zugaib M. Prophylactic administration of progesterone by vaginal suppository to reduce the incidence of spontaneous preterm birth in women at increased risk: a randomized placebo-controlled double-blind study. Am J Obstet Gynecol. 2003 Feb;188(2):419-24. — View Citation

Goldstein P, Berrier J, Rosen S, Sacks HS, Chalmers TC. A meta-analysis of randomized control trials of progestational agents in pregnancy. Br J Obstet Gynaecol. 1989 Mar;96(3):265-74. — View Citation

Meis PJ, Klebanoff M, Thom E, Dombrowski MP, Sibai B, Moawad AH, Spong CY, Hauth JC, Miodovnik M, Varner MW, Leveno KJ, Caritis SN, Iams JD, Wapner RJ, Conway D, O'Sullivan MJ, Carpenter M, Mercer B, Ramin SM, Thorp JM, Peaceman AM, Gabbe S; National Institute of Child Health and Human Development Maternal-Fetal Medicine Units Network. Prevention of recurrent preterm delivery by 17 alpha-hydroxyprogesterone caproate. N Engl J Med. 2003 Jun 12;348(24):2379-85. Erratum in: N Engl J Med. 2003 Sep 25;349(13):1299. — View Citation

Outcome

Type Measure Description Time frame Safety issue
Primary Newborn Respiratory Distress Syndrome (RDS) Newborn RDS in the twin arm is defined as compatible symptoms with radiographically confirmed hyaline membrane disease or with respiratory insufficiency of prematurity requiring ventilator support.
Data expressed as mean n(%),Odds ratio, CI, and P-value were determined using repeated measures model wherein each twin/triplet within a given pregnancy is considered a repeated measure. Exceptions are comparison with 0 outcomes in one or both groups, so Fisher's Exact Test was used.
Morbidity measures were based on live births with data available for the outcomes.
Measured from delivery until 30 days after baby was discharged from the hospital Yes
Primary Use of Oxygen Therapy at 28 Days of Newborn Life Supplemental oxygen use by the baby measured at the point that the baby reaches 28 days old (after birth)within the twin group. Measured at 28 days after birth. Yes
Primary Newborn Sepsis Newborn Sepsis in the twin group was defined as the presence of positive blood culture obtained in the first week of life in association with clinical findings suggesting illness for which the neonate received antibiotics. measured during the first week following birth Yes
Primary Newborn Pneumonia Newborn Pneumonia in the twin group is described as compatible symptoms with diagnostic radiograph findings and positive results on blood cultures, persistent leukopenia measure during the first 28 days after birth. Yes
Primary Newborn Intraventricular Hemorrhage Grade 3 or 4 Newborn Intraventricular hemorrhage (IVH) Stage III in the twin group is described as - IVH with ventricular dilatation.
Neonatal Intraventricular hemorrhage (IVH)Stage IV in the twin group is described as - IVH with parenchymal extension.
measured during the first 28 days after birth Yes
Primary Newborn Periventricular Leukomalacia (PVL) Newborn Periventricular leukomalacia (PVL) in the twin group is described as the presence of more than 1 obvious hypo echoic cyst in the periventricular white matter. measured in the first 28 days after birth. Yes
Primary Newborn Necrotizing Enterocolitis (NEC)Requiring Surgery Newborn NEC in the twin group is described as the presence of any of the following: (1)unequivocal intramural air in abdominal radiograph; (2) perforation abdominal radiograph; (3) clinical evidence of perforation (erythema and induration of the abdominal wall or intrabdominal abscess formation); (4) characteristic findings observed at surgery or autopsy; (5) Stricture formation after an episode of suspected necrotizing enterocolitis. measured in the first 28 days after birth Yes
Primary Newborn Retinopathy of Prematurity (ROP) Newborn ROP within the twin group is described as retinopathy confirmed on fundoscopic examination, felt to be due to prematurity and subsequent oxygen therapy. measured during the first 28 day after birth Yes
Primary Newborn Asphyxia With Ischemic Injury of Brain, Heart, Kidneys, or Liver Newborn Asphyxia or Hypoxic-ischemic encephalopathy (HEI) within the twin group is characterized by clinical and laboratory evidence of acute or subacute brain injury due to asphyxia (ie, hypoxia, acidosis). measured during the first 28 days after delivery Yes
Primary Perinatal Death Perinatal death within the twin group is described as a stillbirth, neonatal death, or miscarriage after randomization. measured from randomization to 28 days after birth. Yes
Secondary Individual Components of Neonatal Morbidity (RDS, IVH-III/IV, Bronchopulmonary Dysplasia(BPD), PVL, Sepsis, NEC, ROP-Stage 3/4, Perinatal Death) Composite Neonatal Morbidity within the twin group is described as the presence of any one or more of the following neonatal morbidities (RDS, IVH-III/IV, BPD, PVL, sepsis, NEC, ROP-Stage 3/4, Perinatal Death). measured as any event noted in the first 28 day following birth. Yes
Secondary Twins: Delivery Prior to 28 Weeks (Wks), 32 Wks, 34wks, and 37 Wks Gestational age was noted at time of delivery and stratified into three categories (Twins: Delivery prior to 28 weeks (wks), 32 wks, 34 wks, and 37 wks) Gestational age noted at time of birth Yes
Secondary Triplets: Delivery Prior to 28 Wks, 32 Wks, 35 Wks Gestational age was noted at time of delivery and stratified into three categories (Triplets: Delivery prior to 28 wks, 32 wks, 35 wks) noted at delivery Yes
Secondary Newborn Gestational Age (GA) at Delivery Newborn Gestational age at delivery within the twin group is described as the gestational age of the baby on the day of birth. determined at the time of birth Yes
Secondary Newborn Birthweight Newborn Birthweight within the twins group was measure following delivery and noted in grams. measure following delivery Yes
Secondary Participant Drop-out Rates Drop-out rates in the twin group are described as any randomized participant who is withdrawn from the trial between randomization (as early at 16 weeks of pregnancy) and completion of the final dose of study medication (as late as 34 weeks of pregnancy). any time from randomization to completion of final dose of study medication No
Secondary Participant Side Effects Requiring Cessation of Therapy Describe as the cessation of study related therapy for the participant within the twin group at anytime from initial study related injection until the final injection at 34 weeks of pregnancy. anytime from initial injection to final injection at 34 weeks. Yes
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