The amniotic fluid proteome changes with gestational age in normal pregnancy: a cross-sectional study

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作者
Gaurav Bhatti
Roberto Romero
Nardhy Gomez-Lopez
Tinnakorn Chaiworapongsa
Eunjung Jung
Francesca Gotsch
Roger Pique-Regi
Percy Pacora
Chaur-Dong Hsu
Mahendra Kavdia
Adi L. Tarca
机构
[1] National Institutes of Health,Perinatology Research Branch, US Department of Health and Human Services, Eunice Kennedy Shriver National Institute of Child Health and Human Development
[2] Wayne State University School of Medicine,Department of Obstetrics and Gynecology
[3] Wayne State University College of Engineering,Department of Biomedical Engineering
[4] University of Michigan,Department of Obstetrics and Gynecology
[5] Michigan State University,Department of Epidemiology and Biostatistics
[6] Wayne State University,Center for Molecular Medicine and Genetics
[7] Detroit Medical Center,Department of Biochemistry, Microbiology and Immunology
[8] Wayne State University School of Medicine,Office of Women’s Health, Integrative Biosciences Center
[9] Wayne State University,Department of Physiology
[10] Wayne State University School of Medicine,Department of Computer Science
[11] Wayne State University College of Engineering,Department of Obstetrics, Gynecology & Reproductive Sciences
[12] The University of Texas Health Sciences Center at Houston,Department of Obstetrics & Gynecology
[13] University of Arizona College of Medicine -Tucson,undefined
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The cell-free transcriptome in amniotic fluid (AF) has been shown to be informative of physiologic and pathologic processes in pregnancy; however, the change in AF proteome with gestational age has mostly been studied by targeted approaches. The objective of this study was to describe the gestational age-dependent changes in the AF proteome during normal pregnancy by using an omics platform. The abundance of 1310 proteins was measured on a high-throughput aptamer-based proteomics platform in AF samples collected from women during midtrimester (16–24 weeks of gestation, n = 15) and at term without labor (37–42 weeks of gestation, n = 13). Only pregnancies without obstetrical complications were included in the study. Almost 25% (320) of AF proteins significantly changed in abundance between the midtrimester and term gestation. Of these, 154 (48.1%) proteins increased, and 166 (51.9%) decreased in abundance at term compared to midtrimester. Tissue-specific signatures of the trachea, salivary glands, brain regions, and immune system were increased while those of the gestational tissues (uterus, placenta, and ovary), cardiac myocytes, and fetal liver were decreased at term compared to midtrimester. The changes in AF protein abundance were correlated with those previously reported in the cell-free AF transcriptome. Intersecting gestational age-modulated AF proteins and their corresponding mRNAs previously reported in the maternal blood identified neutrophil-related protein/mRNA pairs that were modulated in the same direction. The first study to utilize an aptamer-based assay to profile the AF proteome modulation with gestational age, it reveals that almost one-quarter of the proteins are modulated as gestation advances, which is more than twice the fraction of altered plasma proteins (~ 10%). The results reported herein have implications for future studies focused on discovering biomarkers to predict, monitor, and diagnose obstetrical diseases.
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