Skeletal & Smooth Muscle PDF

Summary

This document provides lecture notes on skeletal and smooth muscle. It includes topics like sarcomere structure, muscle contraction and relaxation, and nerve action potentials and how they are involved in the process of muscle contraction.

Full Transcript

SKELETAL & SMOOTH MUSCLE
DR. KATHLEEN O. BALMILERO, MD, DPBA |10/06/2020

OUTLINE The portion of a myofibril that lies between two successive Z
discs
I. SKELETAL MUSCLE Myofibrils>muscle fiber>fascicle>muscle
A. Sarcomere
Myocytes called muscle fibers
B. Muscle excitation
C. Excitation contraction coupling Sarcolemma – cell membrane
D. Muscle contraction Sarcoplasm – cytoplasm of cell
E. Molecular Basis of Contraction
F. Cross Bridge Cycling
1. Initiation of Cross Bridge Cycling at Rest
2. Formation of Actin-Myosin Complex
3. Power Stroke
4. Detachment of Myosin head of Cross bridge from the
active site of an active filament
5. Reactivation of Myosin head
G. Muscle contraction
II. SMOOTH MUSCLE
A. Types of Smooth Muscle
B. Membrane potential and action potential
C. Muscle contraction and relaxation
COMPARISON OF SKELETAL AND SMOOTH
III.
MUSCLE
IV. REVIEW OF NERVE ACTION POTENTIAL
A. Ion Channels
1. Voltage-gated
2. Ligand-gated
B. Diffusion Potential
C. Equilibrium Potential
D. Resting Membrane Potential
E. Action Potential
F. Formation of Action Potential
G. Depolarization of the Action Potential
H. Hyperpolarization and Return to Resting Potential
I. Myelin and Propagation of action potential
J. Nodes of Ranvier

Z lines (“Zwischenscheibe”): borders
M lines (“Mittelscheibe”): midline
A band (“Anisotrophic”): Entire length of myosin
H band (“Heler”): Inside A band, purely myosin, no actin
interspersed
Bare zone: Inside H band, no myosin heads
I band (“Isotrophic”): Purely actin, no myosin interspersed

A. Sarcomere

The smallest functional unit of a skeletal muscle fiber and is
a highly organized arrangement of contractile, regulatory,
and structural proteins
It is the shortening of these individual sarcomeres that lead
to the contraction of individual skeletal muscle fibers (and
ultimately the whole muscle)

PREPARED AND EDITED BY: Lacasandile, D., Lajara, P., Lamsis, V., Laniog, T., Natividad, J., Navarro, A.,
Navalta, C., Inferitis, K.
 SKELETAL & SMOOTH MUSCLE
DR. KATHLEEN O. BALMILERO, MD, DPBA |10/06/2020

C. Process of Excitation contraction coupling

When end-plate potential reaches threshold level, it
produces action potential which propagates over muscle
fibre and through it along transverse tubules
End plate potential- The sudden insurgence of sodium ions
into the muscle fiber when the acetylcholine-gated channels
open causes the electrical potential inside the fiber at the
local area of the end plate to increase in the positive direction
B. Process of muscle excitation as much as 50 to 75 millivolts, creating a local potential

Muscle – excitable tissue
When stimulated shows response
o Electrical response – production of action potential
o Mechanical response – contraction

Difference between excitation of nerve and muscles

Excitation – action potential
Contraction – muscle contraction
Linking of these 2 events is done by coupling done by Ca
ions
Ca ion is one of the most important ions in muscle
contraction

PREPARED AND EDITED BY: Lacasandile, D., Lajara, P., Lamsis, V., Laniog, T., Natividad, J., Navarro, A.,
Navalta, C., Inferitis, K.
 SKELETAL & SMOOTH MUSCLE
DR. KATHLEEN O. BALMILERO, MD, DPBA |10/06/2020

D. Process of muscle contraction

The initiation and execution of muscle contraction occur
in the following sequential steps.

An action potential travels along a motor nerve to its
endings on muscle fibers.
At each ending, the nerve secretes a small amount of the
neurotransmitter substance acetylcholine.
The acetylcholine acts on a local area of the muscle fiber
membrane to open “acetylcholine-gated” cation
channels through protein molecules floating in the
membrane.
Opening of the acetylcholine-gated channels allows
large quantities of sodium ions to diffuse to the interior
of the muscle fiber membrane. This action causes a
local depolarization that in turn leads to opening of
voltage-gated sodium channels, which initiates an
action potential at the membrane.

AP initiated in plasma membrane spread to surface and into
muscle fibre through T tubules
When reaches tip of T tubule activate voltage-gated DHP
(Dihydropyridine Receptors)

Ca ion get attached to troponin-C and starts chain of events
So Ca acts as linkage between excitation and contraction
process
Ca ion get attached to Troponin-C & starts chain of events
So Ca acts as linkage between excitation & contraction
process

Activated DHP receptors triggers opening of Ca release
channels on terminal cisterns i.e. Ryanodine Receptors
Ca diffuses into cytoplasm and ICF Ca increase (2000 times)

PREPARED AND EDITED BY: Lacasandile, D., Lajara, P., Lamsis, V., Laniog, T., Natividad, J., Navarro, A.,
Navalta, C., Inferitis, K.
 SKELETAL & SMOOTH MUSCLE
DR. KATHLEEN O. BALMILERO, MD, DPBA |10/06/2020

3. Power stroke
4. Detachment of myosin head of cross bridge from the active site
of an Actin filament
5. Reactivation of Myosin Head

E. Molecular Basis of Contraction

A.F.Huxley & H.E.Huxley put forward
o Sliding Filament theory or
-in relaxed state: the ends of the actin filaments extending
from two successive Z discs barely begin to overlap one
another.
-in contracted state: actin filaments have been pulled inward
among the myosin filaments, so their ends overlap one
another to their maximum extent. Also, the Z discs have
been pulled by the actin filaments up to the ends of the
myosin filaments
o Rachet theory or
o Walk-along theory or
o Modern theory of Muscular Contraction

1. Initiation of Cross Bridge Cycling at Rest

F. Cross Bridge Cycling Troponin I is lightly bound to actin & Myosin binding sites on
actin is covered by tropomyosin which lies in a groove
Steps in cross bridge cycling: between actin strands.
Troponin T attached to tropomyosin to form troponin-
1. Initiation of cross bridge cycling tropomyosin complex.
2. Formation of Actin-myosin complex

PREPARED AND EDITED BY: Lacasandile, D., Lajara, P., Lamsis, V., Laniog, T., Natividad, J., Navarro, A.,
Navalta, C., Inferitis, K.
 SKELETAL & SMOOTH MUSCLE
DR. KATHLEEN O. BALMILERO, MD, DPBA |10/06/2020

After Excitation – Ca released in cytosol is attached to
Troponin C.
Causes conformational change & Tropomyosin to move
laterally 3. Power Stroke
Uncover active binding sites on Actin.
Actin-Myosin-ADP-Pi complex triggers
o Release of Pi & ADP
o Conformational change in myosin & myosin head
flex toward arm.
This movements generate mechanical force – POWER
STROKE

2. Formation of Actin-Myosin Complex

Head of myosin binds with ATP
ATPase activity of head of myosin breaks ATP into ADP + Pi
cleavage products
Head gets energy move perpendicular toward Actin & gets
attached

Effects of Power Stroke

If load on muscle is small – Actin slides over myosin &
muscle shortening
If load is Large – flexion of myosin headstretching of elastic
neck & no sliding

PREPARED AND EDITED BY: Lacasandile, D., Lajara, P., Lamsis, V., Laniog, T., Natividad, J., Navarro, A.,
Navalta, C., Inferitis, K.
 SKELETAL & SMOOTH MUSCLE
DR. KATHLEEN O. BALMILERO, MD, DPBA |10/06/2020

4. Detachment of Myosin Head of Cross Bridge from the
Active Site of an Actin Filament

Release of ADP & Pi make new ATP to attach to myosin
head
This new ATP with myosin head has low affinity for Actin so
dissociation of myosin head with Actin occurs

5. Reactivation of Myosin Head

This bound ATP splits again into ADP & Pi
Which again give energy to myosin head & reactivate it
Again energized, head move towards Actin filaments & gets
attached to it

G. Muscle Contraction

Changes at Sarcomere Level During Muscle Contraction

Width of A band remains constant
H zone disappears
I band width decreases
Z line move closer
The Sarcomere shortens

Role of ATP in Muscle Contraction and Relaxation

ATP hydrolysis gives energy to cross bridges -- provide force
ATP binding to Myosin dissociate cross bridges & begin new
cycle
Ca ATPase by hydrolysis of ATP provide energy for Ca
pump to transport Ca back – ending contraction & Muscle
Relaxes
When a muscle contracts, work is performed and energy is
required. Large amounts of ATP are cleaved to form ADP
during the contraction process, and the greater the amount
of work performed by the muscle, the greater the amount of
ATP that is cleaved; this phenomenon is called the Fenn
effect.

Steps in Muscle Relaxation

1. After a few ms Ca pump transport Ca from Sarcoplasm
2. Sarcoplasmic Reticulum discharge to Terminal Cisterns
3. Removal of Ca from Troponin
4. Rotate Troponin Tropomyosin Complex
5. Cover active sites, closes cross bridge cycle & relaxes
Muscle

PREPARED AND EDITED BY: Lacasandile, D., Lajara, P., Lamsis, V., Laniog, T., Natividad, J., Navarro, A.,
Navalta, C., Inferitis, K.
 SKELETAL & SMOOTH MUSCLE
DR. KATHLEEN O. BALMILERO, MD, DPBA |10/06/2020

II. SMOOTH MUSCLE
No Troponin
Contains:
o Myosin-light chain kinase (MLCK): phosphorylates
and activates myosin heads
o Myosin-light chain phosphatase (MLCP):
dephosphorylates and inactivates myosin heads
o Calmodulin: binds with Ca
o Caldesmon and Calponin: inhibits muscle
contraction
o Dense Bodies: analogous to Z lines
o Rudimentary SR
o Rudimentary T-tubules (Caveoli)
Present in the walls of hollow organs
Controls movements of most organs

A. Types of smooth muscle
Contractile Response
The smooth muscle of each organ is distinctive from that of
Muscle stimulated -> Excited most other organs in several ways:
Response – Contraction (1) physical dimensions,
(2) organization into bundles or sheets,
Manifested by
(3) response to different types of stimuli,
o Shortening (Iso-Tonic) (4) characteristics of innervation, and
o Developing Tension (Iso-Metric) (5) function.
o Both Yet, for the sake of simplicity, smooth muscle can generally
be divided into two major types: multi-unit smooth muscle
and unitary (or single-unit) smooth muscle.
Types of muscle contraction

B. Membrane potential and action potential

More voltage-gated Ca channels as compared to voltage-
gated Na channels
Flow of Calcium ions into the cell is mainly responsible for
generation of action potentials
Calcium channels open slowly and remain open for a longer
duration resulting in prolonged plateau of action potentials
and muscle contraction

Slow wave rhythm

Not action potential itself
Caused mainly due to slow and rapid pumping of positive
ions, presumably Na+
Slow waves are also called “pacemaker waves”

PREPARED AND EDITED BY: Lacasandile, D., Lajara, P., Lamsis, V., Laniog, T., Natividad, J., Navarro, A.,
Navalta, C., Inferitis, K.
 SKELETAL & SMOOTH MUSCLE
DR. KATHLEEN O. BALMILERO, MD, DPBA |10/06/2020

C. Smooth Muscle Contraction and Relaxation

1. Hormones, NT, stretch triggers increased ICF Ca
2. ICF Ca binds with Calmodulin
3. Calcium-Calmodulin complex activates MLCK
4. MLCK phosphorylates (and activates) myosin heads
5. Activated myosin heads causes smooth muscle contraction
6. MLCP dephosphorylates (and inactivates) myosin heads
7. Inactivated myosin heads: causes smooth muscle relaxation
o Chemical studies have shown that actin and myosin
filaments derived from smooth muscle interact with
each other in much the same way that they do in
skeletal muscle. Further, the contractile process is
activated by calcium ions, and adenosine triphosphate
(ATP) is degraded to adenosine diphosphate (ADP) to
provide the energy for contraction.

Slowness of Onset of Contraction and Relaxation of the Total
Smooth Muscle Tissue.

A typical smooth muscle tissue begins to contract 50 to 100
milliseconds after it is excited, reaches full contraction about
0.5 second later, and then declines in contractile force in
another 1 to 2 seconds, giving a total contraction time of 1 to
3 seconds.
This is about 30 times as long as a single contraction of an
average skeletal muscle fiber. However, because there are
so many types of smooth muscle, con- traction of some types
can be as short as 0.2 second or as long as 30 seconds.

PREPARED AND EDITED BY: Lacasandile, D., Lajara, P., Lamsis, V., Laniog, T., Natividad, J., Navarro, A.,
Navalta, C., Inferitis, K.
 SKELETAL & SMOOTH MUSCLE
DR. KATHLEEN O. BALMILERO, MD, DPBA |10/06/2020

IV. REVIEW OF NERVE ACTION POTENTIAL
A. Ion channel
cell membrane integral proteins
that permit passages of certain ions
selective, maybe open or closed
Voltage-gated channels: opened or closed by changes in
membrane potential
e.g. activation vs inactivation gate of nerve Na
channel
When the inside of the membrane loses its negative charge,
these gates would open suddenly and allow sodium to pass
inward through the sodium pores.
Ligand-gated channels: opened or closed by hormones,
2nd messengers,
neurotransmitters
e.g. skeletal muscle AchR (Nm receptor) that
opens gate for Na and K when Ach binds
One of the most important instances of chemical gating is
the effect of acetylcholine on the so-called acetyl- choline
channel. Acetylcholine opens the gate of this channel,
providing a negatively charged pore about 0.65 nanometer
in diameter that allows uncharged molecules or positive ions
smaller than this diameter to pass through. This gate is
exceedingly important for the transmission of nerve signals
from one nerve cell to another.

B. Diffusion Potential
potential differences generated across a membrane
because of a concentration difference of an ion

C. Equilibrium Potential
diffusion potential that exactly balances (opposes) the
tendency for diffusion caused by concentration differences
aka Nernst potential
If an electrical potential is applied across the membrane, the
electrical charges of the ions cause them to move through
the membrane even though no concentration difference
exists to cause movement.

D. Resting membrane potential
established by diffusion potentials resulting from
III. COMPARISON OF SKELETAL AND concentration differences of various ions as each attempt to
SMOOTH MUSCLE drive the membrane potential towards its equilibrium
potential
normal nerve RMP: -70mV

E. Action Potential
consists of rapid depolarization/upstroke (“ON”)
followed by repolarization (“OFF”)
An action potential elicited at any one point on an
excitable membrane usually excites adjacent portions of
the membrane, resulting in propagation of the action
potential along the membrane.
Action potentials are formed when a stimulus causes the
cell membrane to depolarize past the threshold of
excitation, causing all sodium ion channels to open.
When the potassium ion channels are opened and
sodium ion channels are closed, the cell membrane
becomes hyperpolarized as potassium ions leave the
cell; the cell cannot fire during this refractory period.
The action potential travels down the axon as the
membrane of the axon depolarizes and repolarizes.
PREPARED AND EDITED BY: Lacasandile, D., Lajara, P., Lamsis, V., Laniog, T., Natividad, J., Navarro, A.,
Navalta, C., Inferitis, K.
 SKELETAL & SMOOTH MUSCLE
DR. KATHLEEN O. BALMILERO, MD, DPBA |10/06/2020

Myelin insulates the axon to prevent leakage of the current as Neurotransmitter molecules bind to receptors located on a neuron’s
it travels down the axon. dendrites; voltage-gated ion channels open
Nodes of Ranvier are gaps in the myelin along the axons; Excitatory synapses: positive ions flood the interior of the neuron and
they contain sodium and potassium ion channels, allowing the depolarize the membrane, decreasing the difference in voltage
action potential to travel quickly down the axon by jumping between the inside and outside of the neuron
from one node to the next. Stimulus from a sensory cell or another neuron depolarizes the target
Nodes of Ranvier- unmyelinated part of axons neuron to its threshold potential (-55 mV), and Na+ channels in the
axon hillock open, starting an action potential
Sodium channels open, the neuron completely depolarizes to a
membrane potential of about +40 mV. The action potential travels
down the neuron as Na+ channels open.

HYPERPOLARIZATION AND RETURN TO RESTING POTENTIAL
Action potentials are considered an “all-or nothing” event
--All-or-nothing principle. Once an action potential has been
elicited at any point on the membrane of a normal fiber, the
depolarization process travels 42 UNIT II Membrane
Physiology, Nerve, and Muscle over the entire membrane if
conditions are right, or it might not travel at all if conditions
are not right.
Threshold potential is reached, the neuron completely depolarizes
When depolarization is complete, the cell “resets” its membrane
voltage back to the resting potential. The Na+ channels close,
beginning the neuron’s refractory period.

F. FORMATION OF ACTION POTENTIAL
During the resting state, before the action potential begins,
the conductance for potassium ions about 100 times as great
as the conductance for sodium ions. This is caused by much
greater leakage of potassium ions than sodium ions through
the leak channels.
1. A stimulus from a sensory cell or another neuron causes the
target
cell to depolarize toward the threshold potential.
2. If the threshold of excitation is reached, all Na+ channels
open and the membrane depolarizes.
3. At the peak action potential, K+ channels open and K+
begins to leave the cell. At the same time, Na+ channels
close.
4. The membrane becomes hyperpolarized as K+ ions
continue to leave the cell. The hyperpolarized membrane is
Sodium ions-depolarization
in a refractory period and cannot fire.
Potassium ions-repolarization and hyperpolarization
5. The K+ channels close and the Na+/K+ transporter restores
the resting potential.
G. MYELIN AND PROPAGATION OF THE ACTION
POTENTIAL
For an action potential to communicate information to another
neuron, it must travel along the axon and reach the axon terminals
where it can initiate neurotransmitter release.
Speed of conduction of an action potential along an axon is
influenced by both the diameter of the axon and the axon’s resistance
to current leak.
Myelin acts as an insulator that prevents current from leaving the
axon, increasing the speed of action potential conduction.

DEPOLARIZATION AND THE ACTION POTENTIAL

PREPARED AND EDITED BY: Lacasandile, D., Lajara, P., Lamsis, V., Laniog, T., Natividad, J., Navarro, A.,
Navalta, C., Inferitis, K.
 SKELETAL & SMOOTH MUSCLE
DR. KATHLEEN O. BALMILERO, MD, DPBA |10/06/2020

Arranged according to the sequence of Action Potential.

A. A stimulus from a sensory cell or another neuron causes the
target cell to depolarize toward the threshold potential.
B. The membrane becomes hyperpolarized as K+ ions continue
to leave the cell. The hyperpolarized membrane is in a refractory
period and cannot fire.
C. The K+ channels close and the Na+/K+ transporter restores
the resting potential.
D. At the peak action potential, K+ channels open and K+ begins
to leave the cell. At the same time, Na+ channels close.
E. If the threshold of excitation is reached, all Na+ channels
open and the membrane depolarizes.

TEST YOUR KNOWLEDGE

1. __________ activates myosin heads while ___________
H. NODE OF RANVIER inactivates myosin heads in smooth muscle.
Natural gap in the myelin sheath along the axon A. Caldesmon; Calponin
Unmyelinated spaces are about one micrometer long and B. Myosin-light chain phosphatase; Myosin-light chain kinase
contain voltage gated Na+ and K+ channels C. Calmodulin; Calponin
The flow of ions through these channels, particularly the D. MLCK; MLCP
Na+ channels, regenerates the action potential over and
over again along the axon 2. In cross bridge cycling, after excitation, Ca released in
Action potential “jumps” from one node to the next in cytosol is attached to ________
saltatory conduction A. T tubules
B. Troponin T
C. Troponin C
Saltatory conduction is of value for two reasons: D. Calmodulin
Increased velocity
-by causing the depolarization process to jump long intervals 3. All are true except:
along the axis of the Membrane Potentials and 43 Action A. Width of A band remains constant
Potentials nerve fiber, this mechanism increases the velocity B. H zone disappears
of nerve transmission in myelinated fibers as much as 5- to C. I band width increases
50-fold. D. Z line move closer

Energy conservation 4. What is an example of a multi-unit muscle?
-conserves energy for the axon because only the nodes A. Bile duct
depolarize, allowing perhaps a hundred times smaller loss of B. Intestine
ions than would otherwise be necessary and therefore C. Uterus
requiring little energy for re-establishing the sodium and D. Piloerector muscle
potassium concentration differences across the membrane
after a series of nerve impulses 5. What is responsible for generation of action potentials in
smooth muscles?
A. Ca influx
B. Na influx
C. K influx
D. Ca binding to calmodulin

6. All are true except:
A. Resting membrane potential of nerves is -70 while skeletal
muscles is -90
B. When AP reaches tip of T tubules, activate voltage-gated Ca
channels
C. Sarcomere is the smallest functional unit of a skeletal muscle
fiber
D. I band (“Isotrophic”): Purely actin, no myosin interspersed

PREPARED AND EDITED BY: Lacasandile, D., Lajara, P., Lamsis, V., Laniog, T., Natividad, J., Navarro, A.,
Navalta, C., Inferitis, K.
 SKELETAL & SMOOTH MUSCLE
DR. KATHLEEN O. BALMILERO, MD, DPBA |10/06/2020

7. What is the sequence for cross-bridge linking?
____Power stroke
Answers: D, C, C, D, A, B, B, C, A-E-D-B-C
____Detachment of myosin head of cross bridge from the active site
of an Actin filament
____Formation of Actin-myosin complex
____Reactivation of Myosin Head REFERENCES
____Initiation of cross bridge cycling

A. 3,4,5,2,1 1. Guyton and Hall, Textbook of Medical Physiology, 13 th Edition
B. 3,4,2,5,1
C. 3,5,2,4,1
D. 3,2,5,4,1

8. What is the sequence for smooth muscle contraction and
relaxation?
____ICF Ca binds with Calmodulin
____Inactivated myosin heads: causes smooth muscle relaxation
____Calcium-Calmodulin complex activates MLCK
____Hormones, NT, stretch triggers increased ICF Ca
____MLCK phosphorylates (and activates) myosin heads
____MLCP dephosphorylates (and inactivates) myosin heads
____Activated myosin heads causes smooth muscle contraction

A. 7,5,6,2,4,1,3
B. 2,3,4,7,6,5,1
C. 2,7,3,1,4,6,5
D. 2,5,6,1,3,4,7

Arranged according to the sequence of Action Potential.

A. A stimulus from a sensory cell or another neuron causes the
target cell to depolarize toward the threshold potential.
B. The membrane becomes hyperpolarized as K+ ions continue
to leave the cell. The hyperpolarized membrane is in a refractory
period and cannot fire.
C. The K+ channels close and the Na+/K+ transporter restores
the resting potential.
D. At the peak action potential, K+ channels open and K+ begins
to leave the cell. At the same time, Na+ channels close.
E. If the threshold of excitation is reached, all Na+ channels
open and the membrane depolarizes.

PREPARED AND EDITED BY: Lacasandile, D., Lajara, P., Lamsis, V., Laniog, T., Natividad, J., Navarro, A.,
Navalta, C., Inferitis, K.