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Departments of Pediatrics and Physiology, University of Texas Southwestern Medical Center at Dallas, Dallas, Texas 75235
In fetal sheep, umbilical responsiveness
to ANG II exceeds systemic vascular responsiveness. Fetal systemic
vascular smooth muscle (VSM) exhibits an immature phenotype with
decreased contractile protein contents, low 200-kDa myosin heavy chain
(MHC) SM2, and significant nonmuscle MHC-B expression, whereas
umbilical VSM phenotype is incompletely described. We tested the
hypothesis that differences in vascular responsiveness could reflect
dissimilarities in VSM phenotype. Actin, MHC, MHC isoforms, and active
stresses were compared in strips of femoral arteries and aorta from
near-term fetal (n = 12) and adult
(n = 12) sheep to those in external
and intra-abdominal umbilical arteries. Actin contents in fetal femoral artery and aorta were less (P
0.006) than in external umbilical artery (7.37 ± 1.4 and 7.53 ± 0.7 vs. 21.6 ± 2.2 µg/mg wet wt, respectively) as were MHC
contents (3.17 ± 0.4 and 2.84 ± 0.3 vs. 7.16 ± 0.7, respectively). Whereas 204- and 200-kDa MHC were expressed equally in
fetal systemic arteries, umbilical and adult arteries predominantly
expressed the 204-kDa isoform (SM1); only fetal systemic VSM expressed
MHC-B. Fetal systemic artery stresses and myosin light chain
phosphorylation were less than those in umbilical and adult arteries
(P < 0.001). Compared with umbilical and adult arteries, fetal systemic VSM is biochemically and
functionally immature and thus umbilical VSM demonstrates precocious
maturation resembling adult VSM in protein expression and function.
fetal sheep; myosin heavy chain isoforms; smooth muscle phenotype; active stresses; myosin light chain phosphorylation
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