Journal article
Cardiac contractility, motor function, and cross‐bridge kinetics in N47K‐RLC mutant mice
The FEBS journal, Vol.284(12), pp.1897-1913
06/2017
DOI: 10.1111/febs.14096
PMCID: PMC5490660
PMID: 28467684
Abstract
We have investigated the physiology and mechanical profiles of skinned papillary muscle fibers from transgenic mice expressing the N47K mutation in the myosin regulatory light chain (RLC), shown to cause hypertrophic cardiomyopathy in humans. The results were compared with wild‐type (WT) mice, both expressing the human ventricular RLC. Rate constants of a cross‐bridge (XB) cycle were deduced from tension transients induced by sinusoidal length changes during maximal Ca2+ activation, and were studied as a function of MgATP, MgADP, and Pi concentrations. N47K mutant showed slower XB cycles but higher actin‐activated ATPase activity compared with WT. Consequently, N47K exhibited larger tension than WT. K0 (ADP association constant) and K4 (equilibrium constant of force generation) were larger in N47K, and K1 (ATP association constant) was slightly larger in N47K vs. WT, demonstrating stronger nucleotide binding and force generation abilities of the mutant, but no changes in rigor acto‐myosin binding were observed. Tension per XB was similar among groups, but N47K exhibited more XB distribution in the attached state. Larger values of tension and higher ATPase in N47K suggested that more cross‐bridges participated in tension production in the mutant myocardium compared with WT. In vivo analysis of heart function, performed in ~ 12.5‐month‐old mice by echocardiography and invasive hemodynamics, demonstrated a significant decrease in dP/dtmax–end‐diastolic volume relationship, indicating a depression of ventricular contractility in N47K mice. Our findings suggest that the N47K mutation exerts its action through direct alterations of myosin motor function that ultimately result in pathological hypertrophic remodeling in N47K hearts.
Mechanical studies in papillary muscles from N47K‐RLC mice revealed larger tension production and slower cross‐bridge kinetics, paralleled by higher actin‐activated ATPase compared to WT‐RLC hearts. Echocardiography and hemodynamic evaluations showed hypertrophy and depressed ventricular contractility in the mutant. N47K mutation exerts its action through alterations of myosin motor function that ultimately result in hypertrophic cardiomyopathy in N47K‐positive patients.
Details
- Title: Subtitle
- Cardiac contractility, motor function, and cross‐bridge kinetics in N47K‐RLC mutant mice
- Creators
- Li Wang - University of IowaKatarzyna Kazmierczak - University of MiamiChen‐Ching Yuan - University of MiamiSunil Yadav - University of MiamiMasataka Kawai - University of IowaDanuta Szczesna‐Cordary - University of Miami
- Resource Type
- Journal article
- Publication Details
- The FEBS journal, Vol.284(12), pp.1897-1913
- DOI
- 10.1111/febs.14096
- PMID
- 28467684
- PMCID
- PMC5490660
- ISSN
- 1742-464X
- eISSN
- 1742-4658
- Number of pages
- 17
- Grant note
- American Heart Association (13GRNT16810043; 15PRE23020006) National Institutes of Health (HL123255; HL70041)
- Language
- English
- Date published
- 06/2017
- Academic Unit
- Anatomy and Cell Biology; Internal Medicine
- Record Identifier
- 9984284331602771
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