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Clinical Trial Summary

Preterm delivery (PTD) is a leading cause of neonatal mortality and continues to be a major public health concern, reaching 12.9% in 2006, despite intense research to reverse this trend. Currently, fetal fibronectin (fFN) screening and cervical length determined by ultrasound are two tests which are proven to have benefit in the identification of those at greatest risk for preterm delivery. However the benefit of these tests is limited to situations where a negative result can avoid unnecessary interventions. Currently, maternal fetal monitoring is limited, as it is difficult to "see" what is going on in the placenta (maternal-fetal interface) without invasive measures such as placental biopsy or amniocentesis. Our goal for this study is to identify a group of biomarkers in non-invasive compartments (such as saliva, blood, urine, and/or cervical and vaginal secretions) that are associated with preterm labor and birth. We hypothesize that preterm labor will display an inflammatory profile, which consists of unique inflammatory biomarkers from different non-invasive bodily fluid compartments (such as Il-10 in urine, VEGF in cervical secretions, and IP-10 in saliva), that correlates with a high incidence of preterm birth.


Clinical Trial Description

Preterm delivery (PTD) is a leading cause of neonatal mortality and continues to be a major public health concern, reaching 12.9% in 2006, despite intense research to reverse this trend. Currently, fetal fibronectin (fFN) screening and cervical length determined by ultrasound are two tests which are proven to have benefit in the identification of those at greatest risk for preterm delivery. However the benefit of these tests is limited to situations where a negative result can avoid unnecessary interventions. The first goal of this study is to identify non-invasive predictor(s) that will increase the clinician's ability to identify patients who present with second trimester preterm labor (PTL) at risk for preterm delivery (PTD) ≤ 32 weeks gestation.

Currently, maternal fetal monitoring is limited, as it is difficult to "see" what is going on in the placenta (maternal-fetal interface) without invasive measures such as placental biopsy or amniocentesis. Our preliminary study from term pregnancies has shown that a specific correlation of an intrauterine cytokine may be reflected in one noninvasive site but not another, depending upon the type of cytokine and the compartment from which it is secreted. Therefore, our second goal for this study is to identify inflammatory markers in non-invasive maternal compartments (such as saliva, blood, urine, and/or cervical and vaginal secretions) that have a strong association with placenta/fetal membranes at the time of preterm birth ≤ 32 weeks gestation.

Pregnant women, under 32 weeks gestation, who are admitted to Winthrop University Hospital for evaluation of preterm labor will be eligible for this study. Women with indicated preterm births (i.e. pre-eclampsia), multiple pregnancies, known major fetal abnormality (ex. those that are known to be incompatible with life) and premature rupture of membranes will be excluded from this study. After consent is obtained, samples (blood, urine, saliva, vaginal, and cervical secretions) will be obtained and biomarkers will be identified using a Bio-Plex cytokine concentration assay. These women will than be followed until they deliver. Women who deliver after 32 weeks gestation will form our control group and women who deliver before 32 weeks gestation will form our preterm birth group. Concentration of the biomarkers in the various maternal-fetal compartments will be analyzed and compared between the two groups. For all women who delivery ≤ 32 weeks gestation, non-invasive samples will also be collected around delivery and these cytokine levels will be compared to placenta/fetal membranes to access how well non-invasive fluids reflect the intrauterine environment.

We hypothesize that preterm labor will display an inflammatory profile, which consists of unique inflammatory biomarkers from different non-invasive bodily fluid compartments (such as Il-10 in urine, VEGF in cervical secretions, and IP-10 in saliva), that correlates with a high incidence of preterm birth. ;


Study Design


Related Conditions & MeSH terms


NCT number NCT02317315
Study type Observational
Source Winthrop University Hospital
Contact
Status Completed
Phase N/A
Start date January 2013
Completion date September 7, 2017

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