Abstract

The proper development and growth of the fetal heart is essential to the health of the growing fetus. Eventhough we have some understanding of the development and subsequent growth of the mammalian heart,the mechanisms underlying fetal cardiac growth are not well understood. Our laboratory has a long-standingnterest in fetal cardiac growth. We have found that fetal cardiac function is different during pressureoverload or volume overload. We have also found that fetal cardiac myocytes undergo different rates ofterminal differentiation when exposed to increased pressure or to increased volume load. We havediscovered that hyperplasia and hypertrophy are not directly temporally linked in the growing fetal heart.These discoveries are important because these growth mechanisms are different from those of the adult andbecause the heart uses the anatomic configuration it develops as a fetus for life. Project II will furtherexplore the relationship between cardiac function and growth by pursuing the following Specific Aims:
Specific Aim 1 (Cardiac Function): to assess fetal cardiovascular function during systolic load modulatedgrowth. Functional adaptation of the fetal heart to systolic load likely allows the fetus to maintain adequateblood flow to the fetal systemic and fetal placental circulations maintaining the well being of the fetus.
Specific Aim 2 (Cardiac Growth): to determine the relative contribution and timing of hyperplasia andhypertrophy in conditions of increased systolic pressure load and reduced systolic pressure load. Growth ofthe fetal heart is likely dependent on a load driven balance of myocyte hyperplasia, hypertrophy and terminaldifferentiation.
Specific Aim 3 (In Vivo Cardiac Myocyte Signaling): to determine the role of the MAP Kinase signalingcascade in hyperplasia and hypertrophy in response to increased or decreased cardiac load. Myocardialtissue from hearts exposed to normal, increased or decreased systolic load will be studied. Mechanical loadinduced fetal cardiac growth is likely mediated by the MAP kinase signaling cascade.Superimposed on the genetic instructions for developing cardiac chamber form are hemodynamic clues,which determine the rate of growth and function of the fetal heart. Understanding the mechanisms of cardiacgrowth and terminal differentiation during the fetal period will provide important insight into thepathophysiological processes affecting the adult heart in later life.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Research Program Projects (P01)
Project #
2P01HD034430-11
Application #
7298842
Study Section
Special Emphasis Panel (ZHD1-MCHG-B (KT))
Project Start
2007-06-01
Project End
2012-05-31
Budget Start
2007-06-01
Budget End
2008-05-31
Support Year
11
Fiscal Year
2007
Total Cost
$187,313
Indirect Cost

  Institution

Name
Oregon Health and Science University
Department
Type
DUNS #
096997515
City
Portland
State
OR
Country
United States
Zip Code
97239

  Publications

Kolahi, Kevin S; Valent, Amy M; Thornburg, Kent L (2017) Cytotrophoblast, Not Syncytiotrophoblast, Dominates Glycolysis and Oxidative Phosphorylation in Human Term Placenta. Sci Rep 7:42941
Midgett, Madeline; Thornburg, Kent; Rugonyi, Sandra (2017) Blood flow patterns underlie developmental heart defects. Am J Physiol Heart Circ Physiol 312:H632-H642
Wallace, Alexandra H; Dalziel, Stuart R; Cowan, Brett R et al. (2017) Long-term cardiovascular outcome following fetal anaemia and intrauterine transfusion: a cohort study. Arch Dis Child 102:40-45
Kolahi, Kevin; Louey, Samantha; Varlamov, Oleg et al. (2016) Real-Time Tracking of BODIPY-C12 Long-Chain Fatty Acid in Human Term Placenta Reveals Unique Lipid Dynamics in Cytotrophoblast Cells. PLoS One 11:e0153522
Jonker, Sonnet S; Davis, Lowell; Soman, Divya et al. (2016) Functional adaptations of the coronary microcirculation to anaemia in fetal sheep. J Physiol 594:6165-6174
Jonker, S S; Louey, S (2016) Endocrine and other physiologic modulators of perinatal cardiomyocyte endowment. J Endocrinol 228:R1-18
Burton, Graham J; Fowden, Abigail L; Thornburg, Kent L (2016) Placental Origins of Chronic Disease. Physiol Rev 96:1509-65
Barry, James S; Rozance, Paul J; Brown, Laura D et al. (2016) Increased fetal myocardial sensitivity to insulin-stimulated glucose metabolism during ovine fetal growth restriction. Exp Biol Med (Maywood) 241:839-47
Thornburg, Kent L; Kolahi, Kevin; Pierce, Melinda et al. (2016) Biological features of placental programming. Placenta 48 Suppl 1:S47-S53
Chadderdon, Scott M; Belcik, J Todd; Bader, Lindsay et al. (2016) Temporal Changes in Skeletal Muscle Capillary Responses and Endothelial-Derived Vasodilators in Obesity-Related Insulin Resistance. Diabetes 65:2249-57

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