Physiology Lec: 2 Cardiovascular System دــيز .د يجقراطلا

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Physiology

Lec: 2 Cardiovascular System ‫ زيــد الطارقجي‬.‫د‬

The specialized non contractile cardiac cells capable of auto rhythmicity


form 1% of the heart muscle. They are as follow:

1. The sino-atrial node [SA-node] discharge 70-80 per minute.

2. atrio-ventricular node [AV-node] discharge 40-60 per minute.

3. The bundle of Hiss [atrio ventricular bundle]

4. Purkinje fibers.

Discharge rate of bundle of His and Purkinje fibers 20-40 per minute.

The heart cells with the faster rate of action potential initiation are localized
in the S-A node. Once an action potential occurs in any cardiac muscle cell it
is propagated throughout the rest of myocardium via gap junctions and the
specialized system.

Therefore the S-A node which normally has the fastest rate of auto
rhythmicity at 70-80 action potential per minute drives the rest of the heart
at this rate and thus is known as the pace-maker of the heart. That is the
entire heart becomes excited, triggering the contractile cells to contract and
the heart to beat at the pace or the rate set by S-A node auto rhythmicity
normally at 70-80 beats per minute.

The other auto rhythmic tissues cannot assume their own naturally slower
rates because they are activated by action potentials originated in the S-A
node before they can reach threshold at their own slower rhythm.

The spread of action potential is coordinated to ensure efficient pumping.


Once initiated in the S-A node an action potential spreads throughout the
rest of the heart.

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For efficient cardiac function the spread of excitation should satisfy three
criteria

1. Atrial excitation and contraction should be complete before the onset of


ventricular contraction. The atria must become excited and contract before
ventricular excitation and contraction. During a normal heart beat atrial
contraction occurs about 160 msec before ventricular contraction.

Excitation of cardiac muscle fibers should be coordinated to ensure that


each heart chamber contracts as a unite to pump efficiently. If the muscle
fibers in a heart chamber become excited and contracted randomly rather
than contracting simultaneously in a coordinated fashion they would be
unable to eject blood .

A smooth uniform ventricular contraction is essential to squeeze out the


blood.

Contraction of isolated cardiac muscle fibers is not successful in pumping


blood .such random uncoordinated excitation and contraction of the cardiac
cells is known as fibrillation.

The pair of atria and pair of ventricles should functionally coordinate so that
both members of the pair contract simultaneously this coordination permits
synchronized pumping of blood into the pulmonary and systemic
circulation.

Atrial excitation

An action potential originating in the S-A node spread rapidly throughout


both atria primarily from cell to cell via gap junction; in addition several
poorly delineated specialized conduction pathways spreads up conduction
of the impulse through the atria.

Inter-atrial pathway:

Extends from the S-A node within the right atrium to the left atrium. This
pathway rapidly transmits the action potential from the S-A node to the

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pathways termination in the left atrium. A wave of excitation can spread
across the gap junctions throughout the left atrium at the same time
excitation is similarly spreading throughout the right atrium this ensure that
atria become depolarized to contract simultaneously.

Inter- nodal pathway:

Extends from the S-A node to the A-V node. The A-V node is the only point
of electrical contact between the atria and ventricles because atria are
separated by non conductive fibrous tissue. The inter-nodal conduction
pathway directs the spread of an action potential originating at the S-A
node to the A-V node to ensure sequential contraction of the ventricles
following atrial contraction. Hastened by this pathway the action potential
arrives at the A-V node within 30 msec after the S-A node firing.

The action potential is conducted relatively slowly through the A-V node.
This slowness is advantageous because it allows time for complete
ventricular filing. The impulse is delayed about 100 mesc[the A-V nodal
delay]which enables the atria to become completely depolarized and to
contract emptying their contents into the ventricles before ventricular
depolarization and contraction occur.

Ventricular –excitation:

After the A-V nodal delay the impulse travels rapidly down the septum to
the right and left branches of the bundle of Hiss and throughout the
ventricular myocardium via the purkinje fibers. The network of fibers in this
ventricular conduction system is specialized for rapid propagation of action
potentials. Its presence hastens and coordinates the spread of ventricular
excitation to ensure that the ventricles contract as a unit. The action
potential is transmitted through the entire purkinje fiber system within 30
msec.

Although this system carries the action potential rapidly to a large number
of cardiac muscle cells it does not terminate on every cell. The impulse
quickly spreads from the excited cells to the rest of the ventricular muscle
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cells by means of gap junctions. Purkinje fibers can transmit an action
potential six times faster than the ventricular syncytium of contractile cells
could. If the entire ventricular depolarization process depends on cell to
cell spread of the impulse via gap junctions the ventricular tissue
immediately next to the A-V node would become excited and contract
before the impulse have even passed to the heart apex this of course would
not allow efficient pumping.

Rapid conduction of the action potential down the bundle of Hiss and its
swift diffuse distribution throughout the purkinje network lead to almost
simultaneous activation of the ventricular myocardial cells in both
ventricular chambers which ensures a single, smooth, coordinated
contraction that can efficiently eject blood into both the systemic and
pulmonary circulation at the same time.

Action –potential of contractile muscle cells:

Unlike the membrane of auto rhythmic cells the membrane of contractile


cells remains essentially at rest at about -90 mV until excited by electrical
activity propagated from the pace-maker of the heart.

Phases of action potential in myocardial contractile cell:

1. Rising –phase of action potential up to +30mV as a result of activation of


voltage –gated Na+ channels and Na+ subsequently rapidly entering the
myocardial cell.

2. plateau-phase is maintained by two voltage –dependent permeability


changes. These are the activation of slow L-type Ca+ channels and marked
decrease in K+ permeability in the contractile cell membrane.

3. The rapid falling of the action –potentials results from inactivation of the
Ca+ channels and delayed activation of voltage –gated K+-channels. So the
return to its resting level as the K+ leaves the cell.

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Effect of elevated K+ ion on the heart:

Normally there is substantially more K+ inside the cells than in the ECF. But
with elevated ECF K+ levels this gradient is reduced. Associated with this
change is a reduction in resting membrane potential [that is the membrane
is less negative on the inside than normal because less K+ leaves]. Among
the consequences is tendency to develop ectopic foci , prolongation in
conduction , weak cardiac muscle as well as cardiac arrhythmias.

Effect of ECF Ca+ on the heart:

Elevated ECF calcium concentration augments the strength of cardiac


contraction by prolonging the plateau phase of action potential and by
increasing the cytosolic concentration of Ca+.

Contraction tends to be of longer duration with little time to rest between


contractions.

Calcium channel blockers block Ca+ influx during an action potential


reducing the force of cardiac contraction.

Effect of temperature on the heart

Increased temperature as occurs when one has fever, causes greatly


increased heart rate, sometimes it reach as great as double the normal .
Decreased temperature causes greatly decrease heart rate falling to as low
as a few beats per minute when a person is near death from hypothermia.
These effects result from the fact that heat cause increased permeability of
the muscle membrane to the ions, resulting in acceleration of the self-
excitation process.

Contractile strength of the heart is often enhanced temporarily by a


moderate increase in temperature, but prolonged elevation of the
temperature exhausts the metabolic system of the heart and cause
weakness.

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