The long-term objective of this research is to continue to study the process by which Ca2+ controls vertebrate striated muscle contraction. A significant gap exists in our knowledge of the activation mechanism with respect to its operation in both intact and skinned fibers. The health relatedness of the proposal is the potential for application of the results to cardiac muscle, where Ca2+ is also the key regulator of contraction and many inotropic agents act by influencing Ca2+ fluxes.
Our Specific Aims are directed at testing a current model for activation in which Ca2+ acts as a rate modulator governing the transition of weakly bound cross-bridges to the strongly bound state, which is not in accordance with the classical view that Ca2+ regulates the number of attached cross-bridges via a recruitment mechanism.
Our Aims are as follows. 1) Test whether, during the early phases of contraction, particularly at low levels of activation, the transition from detached to attached but low or non-tension generating states depends on Ca2+, thus indicating an activation mechanism more complex than simple regulation of a transition from weakly to strongly bound attached states. 2) Test whether activation level is influenced by mechanical perturbation, particularly at low levels of activation, thus testing whether changes in contractile properties following perturbations can simply be attributed to the dependence of a specific rate constant on an unchanged activation level. 3) Test whether the velocity of unloaded shortening, (Vu) and the curvature of the force-velocity curve are reduced by a reduction in activation level, thus testing the rate modulation theory prediction that the only influence of Ca2+ is on the forward rate constant governing the weakly-to-strongly bound state. A key feature of the Experimental Design is the intent to carry out a parallel study in both intact and skinned fibers. The Methodology exploits many techniques already developed, such as the dissection, mounting, stimulation/activation, microscopic observation of intact and skinned fibers and measurements of shortening velocities. Attached cross-bridge states will be characterized by techniques based on small amplitude sinusoidal length oscillations. The resulting tension oscillations will be separated into in-phase components (indicating attached cross-bridges) and quadrature components (indicating attached cross-bridges undergoing state transitions). Fluorescent dye technology will be used to report intracellular Ca2+.

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL035032-07
Application #
2217717
Study Section
Physiology Study Section (PHY)
Project Start
1985-03-01
Project End
1998-06-30
Budget Start
1994-07-01
Budget End
1995-06-30
Support Year
7
Fiscal Year
1994
Total Cost
Indirect Cost
Name
Brigham and Women's Hospital
Department
Type
DUNS #
071723621
City
Boston
State
MA
Country
United States
Zip Code
02115
Jiang, Y; Julian, F J (1999) Effects of ramp shortening during linear phase of relaxation on [Ca2+]i in intact skeletal muscle fibers. Am J Physiol 276:C152-60
Claflin, D R; Morgan, D L; Julian, F J (1998) The effect of length on the relationship between tension and intracellular [Ca2+] in intact frog skeletal muscle fibres. J Physiol 508 ( Pt 1):179-86
Vandenboom, R; Claflin, D R; Julian, F J (1998) Effects of rapid shortening on rate of force regeneration and myoplasmic [Ca2+] in intact frog skeletal muscle fibres. J Physiol 511 ( Pt 1):171-80
Morgan, D L; Claflin, D R; Julian, F J (1996) The effects of repeated active stretches on tension generation and myoplasmic calcium in frog single muscle fibres. J Physiol 497 ( Pt 3):665-74
Claflin, D R; Morgan, D L; Stephenson, D G et al. (1994) The intracellular Ca2+ transient and tension in frog skeletal muscle fibres measured with high temporal resolution. J Physiol 475:319-25
Morgan, D L; Claflin, D R; Julian, F J (1991) Tension as a function of sarcomere length and velocity of shortening in single skeletal muscle fibres of the frog. J Physiol 441:719-32
Morgan, D L (1990) New insights into the behavior of muscle during active lengthening. Biophys J 57:209-21
Herland, J S; Julian, F J; Stephenson, D G (1990) Unloaded shortening velocity of skinned rat myocardium: effects of volatile anesthetics. Am J Physiol 259:H1118-25
Morgan, D L; Claflin, D R; Julian, F J (1990) Tension in frog single muscle fibers while shortening actively and passively at velocities near Vu. Biophys J 57:1001-7
Herland, J S; Julian, F J; Stephenson, D G (1990) Halothane increases Ca2+ efflux via Ca2+ channels of sarcoplasmic reticulum in chemically skinned rat myocardium. J Physiol 426:1-18

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