Abstract

Aberrant labor is a major clinical problem resulting in significant infant morbidity in spite of recent advances in obstetrical and neonatal care. The mechanisms that control labor onset and its progression, term or preterm, are not well understood. Rupture of the fetal membranes (ROM) is an integral event to the onset and development of the labor process. ROM usually follows the onset of uterine contractions. However, in 10% of term and 40% of preterm births, ROM is the sentinel event leading to uterine contractions and delivery. Thus, the mechanism of ROM has both physiological and clinical importance. Previous thinking that ROM results exclusively from physical stretch forces produced by uterine contractions has evolved to theories that ROM, at term, is a maturational event culminating from a gene controlled program of membrane weakening, including collagen modification and apoptosis. Preterm ROM, initiated in some cases by infection inflammation, and by as yet unknown causes in others, may involve premature activation of the same developmental program. Considerable work has been reported by us and other researchers documenting the ability of various agents to cause apoptosis in cultured cells derived from fetal membranes. However, there has been no direct demonstration that apoptosis and/or remodeling lead to membrane weakening, or to changes in membrane viscoelastic properties which make rupture more likely. We hypothesize that human fetal membranes weaken during gestation as a result of a combination of two processes: programmed biochemical changes leading to collagen remodeling and apoptosis, and superimposed physical stretch forces leading to tissue damage. Further, we suggest that stretch also initiates biochemical changes, which modify membrane viscoelastic properties. We propose a study documenting the one-to-one correspondence of the biochemical changes - apoptosis and membrane remodeling - and the physical weakening of the membranes. Initially we will determine the biochemical/histological characteristics over the topological surface of the fetal membranes and compare them with strength, and other physical properties. Second, we will prospectively inflict precise membrane damage with apoptotic agents or with physical forces and determine the resulting changes in histology and membrane strength. Finally, we will determine the requirements for membrane self repair after physical or biochemically mediated damage. Understanding the relationship between biochemical changes and physical properties of the fetal membranes may allow monitoring of, and/or intervention in, pregnancies at risk for premature delivery due to premature ROM.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Research Project (R01)
Project #
5R01HD048476-05
Application #
7540912
Study Section
Pregnancy and Neonatology Study Section (PN)
Program Officer
Ilekis, John V
Project Start
2005-01-01
Project End
2011-12-31
Budget Start
2009-01-01
Budget End
2011-12-31
Support Year
5
Fiscal Year
2009
Total Cost
$316,747
Indirect Cost

  Institution

Name
Case Western Reserve University
Department
Pediatrics
Type
Schools of Medicine
DUNS #
077758407
City
Cleveland
State
OH
Country
United States
Zip Code
44106

  Publications

Joyce, E M; Diaz, P; Tamarkin, S et al. (2016) In-vivo stretch of term human fetal membranes. Placenta 38:57-66
Rangaswamy, N; Abdelrahim, A; Moore, R M et al. (2011) [Biomechanical characteristics of human fetal membranes. Preterm fetal membranes are stronger than term fetal membranes]. Gynecol Obstet Fertil 39:373-7
Kumar, D; Schatz, F; Moore, R M et al. (2011) The effects of thrombin and cytokines upon the biomechanics and remodeling of isolated amnion membrane, in vitro. Placenta 32:206-13
Strohl, A; Kumar, D; Novince, R et al. (2010) Decreased adherence and spontaneous separation of fetal membrane layers--amnion and choriodecidua--a possible part of the normal weakening process. Placenta 31:18-24
Moore, R M; Schatz, F; Kumar, D et al. (2010) Alpha-lipoic acid inhibits thrombin-induced fetal membrane weakening in vitro. Placenta 31:886-92
Mercer, Brian M; Abdelrahim, Adli; Moore, Robert M et al. (2010) The impact of vitamin C supplementation in pregnancy and in vitro upon fetal membrane strength and remodeling. Reprod Sci 17:685-95
Joyce, Erinn M; Moore, John J; Sacks, Michael S (2009) Biomechanics of the fetal membrane prior to mechanical failure: review and implications. Eur J Obstet Gynecol Reprod Biol 144 Suppl 1:S121-7
Kumar, D; Novince, R; Strohl, A et al. (2009) A new methodology to measure strength of adherence of the fetal membrane components, amnion and the choriodecidua. Placenta 30:560-3
Moore, Robert M; Novak, Jillian B; Kumar, Deepak et al. (2009) Alpha-lipoic acid inhibits tumor necrosis factor-induced remodeling and weakening of human fetal membranes. Biol Reprod 80:781-7
Moore, R M; Redline, R W; Kumar, D et al. (2009) Differential expression of fibulin family proteins in the para-cervical weak zone and other areas of human fetal membranes. Placenta 30:335-41

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