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Enhancement of shortening velocity, power, and acto‐myosin crossbridge (CB) kinetics following long‐term treatment with propionyl‐ L ‐carnitine, coenzyme Q 10 , and omega‐3 fatty acids in BIO TO‐2 cardiomyopathic Syrian hamsters papillary muscle
Author(s) -
Vargiu Romina,
Littarru Gian Paolo,
Fraschini Matteo,
Perinu Anna,
Tiano Luca,
Capra Alessandro,
Mancinelli Rino
Publication year - 2010
Publication title -
biofactors
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.204
H-Index - 94
eISSN - 1872-8081
pISSN - 0951-6433
DOI - 10.1002/biof.95
Subject(s) - isometric exercise , papillary muscle , myosin , medicine , crossbridge , endocrinology , chemistry , kinetics , coenzyme a , biology , biochemistry , enzyme , physics , quantum mechanics , reductase
Abstract Impaired functions of myocardial muscle cells in human and animals, is a primary defect associated with idiopathic dilated cardiomyopathy (DCM). The pathophysiological mechanisms implicated in the DCM are yet to be clarified and an effective therapy is still not available. The BIO TO‐2 cardiomyopathic Syrian Hamsters (CMSHs) represent an animal model of idiopathic DCM. The aim of this study was to investigate the effect of long‐term treatment (2 months) with propionyl‐ L ‐carnitine (PLC), coenzyme Q 10 , omega‐3 fatty acids and a combination of these three agents (formulation HS12607) on mechanical properties and acto‐myosin crossbridges (CBs) kinetics of left ventricular (LV) papillary muscle from control and treated 10 month old BIO TO‐2 CMSHs. Isometric and isotonic contractile properties of isolated papillary muscle from control and treated CMSHs were investigated, and acto‐myosin CB number, force and kinetics were calculated using Huxley's equations. Mechanical parameter values were higher in treated than in control hamsters, particularly when substances were administered together in a coformulation (HS12607). Compared to control, HS12607‐treated papillary muscles showed a significant increase of maximum peak isometric tension ( P o ) (30.06 ± 4.91 vs. 19.74 ± 5.00 mN/mm 2 ), maximum extent of muscle shortening (0.13 ± 0.03 vs. 0.07 ± 0.02 L / L max ), maximum unloaded shortening velocity (1.18 ± 0.24 vs. 0.53 ± 0.13 L / L max s −1 ) and maximum peak of power output (5.52 ± 1.61 vs. 1.58 ± 0.83). The curvature of the hyperbolic force‐velocity relationships did not differ between control and treated hamsters. When compared to controls, acto‐myosin CB number increased in treated hamsters [(6.67 ± 1.91) 10 10 /mm 2 vs. (3.55 ± 2.08) 10 10 /mm 2 ], whereas the unitary force of single CB was similar in control and treated animals. The peak value of the rate constant for CB attachment ( f 1 ) and detachment ( g 2 ) was higher in treated animals when compared to control. (93.87 ± 25.82 vs.47.28 ± 10.88 s −1 and 214.40 ± 44.64 vs. 95.56 ± 23.49 s −1 , respectively). In conclusion, the present study illustrates that supplementation with PLC, CoQ 10 and omega‐3 fatty acids improved motor parameters, energetic, and CB kinetics of BIO TO‐2 CMSH papillary muscle indicating that these naturally occurring substances may be a valid adjuvant to conventional therapy in DCM.