Postnatal Development of Right Ventricular Myofibrillar Biomechanics in Relation to the Sarcomeric Protein Phenotype in Pediatric Patients with Conotruncal Heart Defects

Fatiha Elhamine; Bogdan Iorga; Martina Krüger; Mona Hunger; Jan Eckhardt; Narayanswami Sreeram; Gerardus Bennink; Konrad Brockmeier; Gabriele Pfitzer; Robert Stehle

doi:10.1161/JAHA.116.003699

Postnatal Development of Right Ventricular Myofibrillar Biomechanics in Relation to the Sarcomeric Protein Phenotype in Pediatric Patients with Conotruncal Heart Defects

J Am Heart Assoc. 2016 Jun 27;5(6):e003699. doi: 10.1161/JAHA.116.003699.

Authors

Affiliations

¹ Institute of Vegetative Physiology, University of Cologne, Köln, Germany.
² Institute of Vegetative Physiology, University of Cologne, Köln, Germany Department of Physical Chemistry, University of Bucharest, Romania.
³ Clinics for Anesthesiology and Surgical Intensive Care, University of Cologne, Köln, Germany.
⁴ Pediatric Cardiology, University of Cologne, Köln, Germany.
⁵ Pediatric Heart Surgery, University of Cologne, Köln, Germany.
⁶ Institute of Vegetative Physiology, University of Cologne, Köln, Germany gabriele.pfitzer@uni-koeln.de.

Abstract

Background: The postnatal development of myofibrillar mechanics, a major determinant of heart function, is unknown in pediatric patients with tetralogy of Fallot and related structural heart defects. We therefore determined the mechanical properties of myofibrils isolated from right ventricular tissue samples from such patients in relation to the developmental changes of the isoforms expression pattern of key sarcomere proteins involved in the contractile process.

Methods and results: Tissue samples from the infundibulum obtained during surgery from 25 patients (age range 15 days to 11 years, median 7 months) were split into half for mechanical investigations and expression analysis of titin, myosin heavy and light chain 1, troponin-T, and troponin-I. Of these proteins, fetal isoforms of only myosin light chain 1 (ALC-1) and troponin-I (ssTnI) were highly expressed in neonates, amounting to, respectively, 40% and 80%, while the other proteins had switched to the adult isoforms before or around birth. ALC-1 and ssTnI expression subsequently declined monoexponentially with a halftime of 4.3 and 5.8 months, respectively. Coincident with the expression of ssTnI, Ca(2+) sensitivity of contraction was high in neonates and subsequently declined in parallel with the decline in ssTnI expression. Passive tension positively correlated with Ca(2+) sensitivity but not with titin expression. Contraction kinetics, maximal Ca(2+)-activated force, and the fast phase of the biphasic relaxation positively correlated with the expression of ALC-1.

Conclusions: The developmental changes in myofibrillar biomechanics can be ascribed to fetal-to-adult isoform transition of key sarcomeric proteins, which evolves regardless of the specific congenital cardiac malformations in our pediatric patients.

Keywords: cardiac myofibrils; contractile function; contractile proteins; force kinetics; heart development; human myocardium; sarcomere physiology; tetralogy of Fallot.

Publication types

Observational Study
Research Support, Non-U.S. Gov't

MeSH terms

Biomechanical Phenomena / physiology
Child
Child, Preschool
Connectin / metabolism
Heart / growth & development
Heart Defects, Congenital / physiopathology*
Humans
Infant
Infant, Newborn
Muscle Proteins / physiology
Myocardial Contraction / physiology
Myofibrils / physiology*
Myosin Heavy Chains / metabolism
Myosin Light Chains / metabolism
Sarcomeres / physiology
Troponin I / metabolism
Troponin T / metabolism

Substances

Connectin
Muscle Proteins
Myosin Light Chains
Troponin I
Troponin T
Myosin Heavy Chains