SBIR-STTR Award

A Noninvasive Platform to Assess Maternal Risk for Perinatal Complications in the First Trimester
Award last edited on: 3/4/19

Sponsored Program
SBIR
Awarding Agency
NIH : NICHD
Total Award Amount
$299,992
Award Phase
1
Solicitation Topic Code
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Principal Investigator
Leena Kadam

Company Information

Advanced Reproductive Testing LLC (AKA: ART~cradle Genomics Inc)

5718 Tequesta Drive
West Bloomfield, MI 48323
   (313) 577-1748
   N/A
   www.papseek.com
Location: Single
Congr. District: 11
County: Oakland

Phase I

Contract Number: 1R43HD097904-01
Start Date: 9/26/18    Completed: 8/31/19
Phase I year
2018
Phase I Amount
$299,992
Limited information is available about early human placentation when many pregnancy pathologies originate. To address this knowledge gap and begin development of robust diagnostic tool to manage pregnancy complica- tions, we propose a pilot study based on a highly sensitive immune assay and our company’s base technology, Trophoblast Retrieval and Isolation from the Cervix (TRIC). TRIC uses a Pap smear, considered safe during pregnancy, to non-invasively capture hundreds of homogeneous, HLA-G-expressing, fetal cells during ongoing pregnancies at 5 to 20 weeks of gestational age (GA). We propose that these fetal cells are useful for assessing pregnancy status and assessing risk of perinatal disease in vivo. Our premise is based on data demonstrating that cells obtained by TRIC express trophoblast extravillous lineage markers (e.g., hCG, HLA-G), and have mo- lecular profiles affected by pathology. Specifically, immunocytochemical protein expression analysis of the cells demonstrates altered levels of several key proteins in pregnancies that later develop miscarriage, fetal growth restriction (FGR) or preeclampsia. We hypothesize that, based on robust data obtained in our published studies, that AFP and PGF levels are significantly altered in EVT cells from pregnancies linked to FGR, a key indicator of placenta-based perinatal disorders. Therefore, we will rigorously determine if expression of two proteins iden- tified in our preliminary studies in fetal cells obtained by TRIC correlate with fetal growth rates, considering fetal sex and other relevant factors. The specific aim of this application is to establish the relationship of cervical extravillous trophoblast biomarker levels to pregnancy outcomes. We will quantify AFP and PGF in EVT cells obtained by TRIC in the first trimester, comparing cohorts of subjects with normal term pregnancies to those with adverse outcomes associated with low birth weight for GA at birth. This goal will be accomplished in four milestones. Milestone 1, we will develop a high-sensitivity immune assay to quantify AFP and PGF levels in trophoblast cells. Milestone 2, we will build a biobank of 100 specimens of trophoblast cells isolated by TRIC from pregnant patients in the first trimester, along with de-identified medical records to determine pregnancy outcomes. Milestone 3, the immune assay will be optimized with patient trophoblast samples. Milestone 4, the remaining patient trophoblast samples will be assayed for AFP and PGF levels and compared to patient out- comes, particularly reduced birth weight for gestational age. These experiments will validate the testing platform and provide preliminary data for a larger clinical study to establish a perinatal test for maternal-fetal disorders. Our long-term goal is to develop and commercialize products for early diagnosis of perinatal pathologies using EVT cells obtained safely during ongoing pregnancies through TRIC.

Public Health Relevance Statement:
This research provides major public health benefits by leveraging a safe, noninvasive method to capture human fetal cells with placental cell properties to develop a method to quantify biomarkers of obstetrical disease during the first trimester of pregnancy. These assays will enable monitoring of pregnancy, analogous to using ultrasound charts to monitor fetal growth, but at a much earlier stage when intervention strategies can be developed. Our company will develop a perinatal test that can be commercialized for maternal-fetal health management, and that will generate clinical and experimental breakthroughs beneficial to the well-being of mothers and their babies.

Project Terms:
2 year old; Address; adverse outcome; adverse pregnancy outcome; Affect; alpha-Fetoproteins; Archives; base; biobank; Biological Assay; Biological Markers; Birth; Birth Weight; Cell Count; Cell Line; Cells; Cervical; Cervix Uteri; Characteristics; Clinical; Clinical Research; cohort; cost; Data; design; Development; Diagnosis; Diagnostic; Diagnostic tests; disability; Discipline of obstetrics; Disease; Early Diagnosis; experimental study; Expression Profiling; fetal; Fetal Diseases; Fetal Growth; Fetal Growth Retardation; Fetal health; Fetal Monitoring; Fetus; fetus cell; First Pregnancy Trimester; Future; Gases; Gestational Age; Goals; Growth; Health Benefit; health management; Health Personnel; healthy pregnancy; HLA G antigen; Human; Human Chorionic Gonadotropin; Immunology procedure; in vivo; indexing; Intervention; keratin CK7; Knowledge; Link; Low Birth Weight Infant; Maternal-Fetal Exchange; Medical; Medical Records; Methods; Molecular Profiling; Monitor; Morbidity - disease rate; mortality; Mothers; Nutrient; Pap smear; Pathology; Patient-Focused Outcomes; Patients; Perinatal; perinatal complications; Perinatal Disorder; Personal Satisfaction; Phase; Pilot Projects; Placenta; Placental Growth Factor; Placentation; Plant Roots; Population; Positioning Attribute; Pre-Eclampsia; Pregnancy; Pregnancy Complications; pregnancy disorder; Pregnancy Outcome; pregnant; prenatal; Prevention strategy; Preventive Intervention; Property; protein complex; protein expression; Proteins; Public Health; Publishing; reproductive; Research; Retrieval; Risk; Sampling; sex; Small for Gestational Age Infant; Specimen; Spontaneous abortion; Technology; Testing; tool; trophoblast; Ultrasonography; Woma

Phase II

Contract Number: ----------
Start Date: 00/00/00    Completed: 00/00/00
Phase II year
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Phase II Amount
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