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Summary of events during skeletal muscle contraction

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Summary of events during skeletal muscle contraction Rest actin and myosin uncoupled calcium stored in SR Excitation nerve impulse generated ACH released from the ... – PowerPoint PPT presentation

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Title: Summary of events during skeletal muscle contraction


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Summary of events during skeletal muscle
contraction
3
Rest
  • actin and myosin uncoupled
  • calcium stored in SR

4
Excitation
  • nerve impulse generated
  • ACH released from the vesicles
  • sarcolemma depolarized
  • muscle impulse transmitted through the fiber
  • calcium released from the cisternae
  • calcium binds to troponin
  • actin binding sites activated
  • myosin ATPase activated

5
Contraction
  • Myosin cross-bridges swivel
  • Release ADP Pi
  • Actin slides over myosin

6
Regeneration
  • ATP attaches to myosin
  • actin and myosin dissociate
  • ATP ? ADP Pi
  • contraction process repeats

7
Relaxation
  • ACH decomposed by cholinesterase
  • nerve impulse stops
  • calcium removed by calcium pump
  • actin binding sites inhibited (Tn/tropomyosin
    complex returns to original position)
  • muscle returns to resting state

8
Excitation Contraction Coupling
  • process by which myofibrils translate nerve
    impulses into muscle contraction
  • depolarization of t-tubule membrane (a change in
    the membrane potential) results in the calcium
    release from the terminal cisternae of the SR
  • this results in muscle contraction

9
  • also know calcium is resequestered in the SR via
    active calcium-ATPase pumps
  • not clear is how the change in membrane potential
    of the t-tubule system is communicated into the
    SR to cause calcium release

10
Structure and Function of the Triad
  • t-tubules and SR communicate at the triad
    junction
  • a ryanodine receptor is a large protein complex
    which is the release channel of the sarcoplasmic
    calcium, located at the t-tubule SR junction
  • the receptor has two parts channel region and a
    large cytoplasmic region

11
  • within t-tubule is another protein complex,
    believed to be the voltage sensor which controls
    the opening and closing of the ryanodine
    receptor, this is the DHP or dihydropyridine
    receptor complex
  • hypothesized ryanodine receptor and the DHP
    receptor interact with each other to cause the
    action potential to induce calcium release from
    the SR

12
Theories of Communication
  • Calcium-induced tubule membranes
  • Voltage-induced changes in the t-tubule
  • Changes in the voltage gradient

13
Calcium induced tubule membranes
  • Cause an opening of the calcium channel calcium
    released
  • stimulation of t-tubule induces a release of
    calcium ions from the gates within the SR

14
  • Con block calcium release channels of the cell
    membrane does not inhibit calcium release from
    the SR
  • Nor reduce tension development
  • Also, amount of calcium needed to induce release
    is not clear (may not be physiologic)

15
Voltage-induced changes in the t-tubule
  • induce the formation of D-myosinositol
    1,4,5-triphosphate (IP3)
  • IP3 then increases the permeability of the SR
    membranes to cause calcium release

16
  • Pros elevated IP3 production has been
    demonstrated in skeletal muscle following
    electrical stimulation
  • Release of calcium in skinned fibers induced by
    IP3
  • An augmented muscle response following inhibition
    of IP3 breakdown
  • A reduction of IP3 release from RBCs
  • Cons is the concentration of IP3 necessary for
    activation and is its rate of activation
    physiologic?

17
Changes in the voltage gradient
  • Activation of calcium is due to perturbation of
    the normal H gradient across the SR membranes
  • Cons the pH changes during muscle contraction
    may be too small to induce the necessary
    gradients in order to stimulate calcium release

18
Hypothesized Mechanisms for ECC
  • Calcium-induced calcium release
  • Chemical intermediate
  • Allosteric Interaction

19
Calcium induced calcium release
  • stimulation of t-tubules causes a small amount of
    calcium to cross the t-tubule membrane
  • an amount insufficient to cause muscle
    contraction
  • This induces the release of additional calcium in
    greater amounts, from the SR (calcium channels
    are open)

20
  • Cons blocking the DHP channels of the t-tubule
    membrane does not inhibit calcium release from
    the SR
  • Or decrease force development
  • Are the amounts of calcium required physiologic?

21
Chemical Intermediate
  • voltage-induced changes in the t-tubules induce
    the formation of inositol 1,4,5 triphosphate
    (InsP3)
  • IP3 then increases the permeability of the SR
    membranes to cause calcium release

22
  • Pros after electrical stimulation, there is an
    elevated production IP3
  • The release of calcium in skinned fibers induced
    by IP3
  • If IP3 release from the RBCs is inhibited, there
    is a reduction of calcium transients in skeletal
    muscle
  • If IP3 breakdown is inhibited, there is an
    augmented skeletal muscle response

23
  • Cons is the concentration of IP3 necessary for
    activation?
  • Is its rate of activation physiologic?

24
Allosteric Interaction Hypothesis (aka, Plunger
Hypothesis)
  • there is a mechanical or allosteric link between
    DHP channels of the t-tubules and the ryanodine
    channels of the SR (junctional foot proteins)
  • There is a foot structure composed primarily of
    SR calcium channel proteins clustered next to the
    t-tubule membrane called channel protein or
    electron dense feet

25
  • This suggests a role for protein-protein
    interactions to transmit the depolarization
    signal across the junction. Most popular
    mechanism of signal transmission is a variant of
    the plunger hypothesis
  • Imagine a mobile positive charge in the t-tubule
    membrane (it may be associated with the DHP
    voltage sensor)

26
  • The charge is connected by a rod to a plug in the
    calcium release channel of the SR
  • Depolarization of the t-tubule membrane causes
    charge movement in the t-tubule membrane
  • Results in the unplugging of the SR calcium
    release channel

27
  • Suspect that the mobile charge is contained
    within specific amino acids contained within a
    segment of the DHP receptor complex
  • Ryanodine receptor complex has a large
    cytoplasmic portion spanning the gap between
    membranes, and able to contact the voltage
    sensors of the DHP complex

28
Skeletal Muscle Fiber Types
  • not all skeletal muscle has the same biochemical
    or functional characteristics
  • are generally classified according to their
    primary dependence on different metabolic
    pathways for the production of ATP.

29
Nomenclature based on
  • Myosin ATPase pH lability histochemical staining
  • Glycolytic staining
  • Oxidative staining

30
Fiber sub-types
  • Type I, SO (slow oxidative), red fibers, slow
  • Type IIa FOG (fast oxidative glycolytic),
    intermediate fibers
  • Type IIb FG (fast glycolytic), white, fast

31
  • Type IIc rare, undifferentiated fiber, perhaps
    found during re-innervation or motor unit
    transformation, between I and IIa on the
    continuum of metabolic potential
  • Type IIx, not classified

32
Slow twitch fibers
  • fatigue resistant, good for prolonged exercise
  • primarily synthesized ATP via aerobic energy
    transfer
  • recruited for aerobic activities such as
    prolonged moderate exercise
  • have a smaller resting membrane potential,
    -50-70mv, versus 80-90mv in fast muscle

33
  • longer latency period due to less extensive SR
  • low activity of myosin ATPase
  • slow speed of contraction
  • low glycolytic capacity
  • increased size and number of mitochondria

34
  • higher levels of myoglobin
  • higher concentrations of mitochondrial enzymes
  • increased blood flow -- increased capillarization

35
Fast twitch fibers
  • activated in short-term, sprint activities, and
    forceful contractions which rely primarily on
    anaerobic metabolism for energy
  • important in stop and go and change of pace
    activities
  • more extensive SR
  • greater capability for electrochemical AP
    transmission (due to increased SR)

36
  • high activity level of myosin ATPase
  • rapid SR calcium release and uptake
  • high rate of cross-bridge turnover development
  • intrinsic speed of contraction and tension is 2-3
    times that of ST fibers
  • primarily use the glycolytic system for energy
    transfer
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