Cardiac Physiology Based On The Lecture and Text Material, You Should Be Able To Do The Following
Cardiac Physiology Based On The Lecture and Text Material, You Should Be Able To Do The Following
Cardiac Physiology Based On The Lecture and Text Material, You Should Be Able To Do The Following
Based on the lecture and text material, you should be able to do the following:
Like skeletal muscle, cardiac muscle is striated and contraction occurs using the
same sliding filament mechanism.
In contrast to skeletal muscle, cardiac muscle fibers are short, fat, branched and
interconnected.
Cardiac muscle fibers also have only one or two nuclei, contain more mitochondria, have
fewer T-tubules, and much less sarcoplasmic reticulum.
Adjacent cardiac muscle fibers are interlocked by finger like extensions called
intercalculated discs. These discs contain desmosomes and gap junctions.
Desmosomes hold the cells together and prevent separation during contraction.
Gap junctions allow the ions of the action potential to pass freely from cell to
cell so that the whole heart contracts instead of just a few cells.
Since all the cells of the heart are coupled electrically through gap junctions, it behaves
as a single functioning unit or a functional syncytium.
In contrast to skeletal muscle fibers which require independent stimulation, some cardiac
muscle cells (about 1%) are self excitable and can start their own depolarization which
leads to depolarization of the rest of the heart in a spontaneous and rhythmic way.
In skeletal muscles, impulses do not spread from cell to cell. As mentioned above, the
cardiac muscle is an all or none effect. The heart contracts as a whole unit, or not at all.
The absolute refractory period of the cardiac muscle cell is much longer than that of
neurons or skeletal muscle fibers. It lasts 250 ms, almost as long as the contraction. This
is to prevent tetanic contractions, which would stop the heart from pumping.
90% of cardiac cells are contractile muscle fibers, which are responsible for pumping the
heart.
10-20% of Ca2+ need for contraction enters from extracellular space. Once inside, this
calcium stimulates the release of much larger amounts (80%) of Ca2+ from the
sarcoplasmic reticulum.
Cardiac muscle contraction is very similar to that of skeletal muscle with the difference
arising from the presence of slow voltage-gated Ca2+ channel in the plasma membrane:
In a resting state, ionic calcium cannot enter the cardiac fibers.
When depolarization occurs, not only are fast Na+ channels opened, slow Ca2+
channels are also opened and allow an influx of Ca2+.
Ryanodine channels give off calcium sparks or bursts that dramatically increase
intracellular [Ca2+]i.
During this time, repolarization is already occurring, but the Ca2+ surge across the
membrane prolongs the depolarization, which is called a plateau.
This plateau leads to the contraction (action potential) lasting 200 ms or more (as
compared to the skeletal muscle contraction lasting 15 to 100 ms).
This provides the heart with the capability needed to eject blood from the
heart.
After the 200 ms, the action potential falls rapidly, Ca2+ channels close; K+
channels open and the cells are repolarized.
During this time, the Ca2+ ions are pumped back into the sarcoplasmic
reticulum and extracellular space.
The ionic events which occur in contractile cardiac cells are significantly different from
the ionic events which happen in the pacemaker cells. The primary difference is a lack
of a fast inward Na+ current.
Cardiac muscles have much more mitochondria than other cells, which is why it is
absolutely dependent on oxygen for it=s metabolism. It relies exclusively on aerobic
aspiration.
When a region of the heart is deprived of oxygen, the oxygen-starved cells begin
to metabolize anaerobically.
This produces lactic acid, which causes pH to fall (H + rises) and impairs
the cardiac cell=s ability to produce ATP that is needed to pump Ca2+ out
of the cell.
The rising levels of intracellular Ca2+ and H+ cause the gap junctions to
close and isolate the damaged cells.
The action potentials look for other paths to reach the cardiac cells beyond them, and the
damaged cells become ischaemic.
If the ischaemia persists, then the cells die, resulting in a myocardial infarction (a
common type of heart attack).
The heart does not depend on the nervous system to depolarize and contract, it has an
inbuilt mechanism called the intrinsic cardiac conduction system, which consist of
specialized non-contractile cells called pacemaker cells.
Pacemaker cells are self-excitatory and they initiate and distribute impulses throughout
the heart in a consistent, orderly fashion.
They have gap junctions that pass AP=s from one cell to the next, but only along a
specific conduction pathway.
The fast Ca2+ channels open and it is the explosive influx of Ca2+ that causes a
complete reversal of membrane potential.
The SA Node generates the action potential as it has the fastest rate of
depolarization.
The action potential generated will the spread to two places; the
gap junctions to the neighboring cells of atria (which in turn send
to their neighbors in the atria), and to the internodal pathways.
The impulse is delayed momentarily which allows the atria complete their
contraction before the ventricle contracts.
The AV node has small diameter fibers and fewer gap junctions to allow
this delay.
There are no gap junctions between cardiomyocytes of the atria and the
ventricles.
The AV Bundle is the only electrical connection between the atria and the
ventricles.
The AV bundle branches out into two paths that connect to the Purkinje Fibers.
Conduction along here is very rapid due to large fibers and a large number
of gap junctions, and allows the ventricles to contract as a unit.
Defects in the conduction system that cause irregular heart rhythms are called
arrhythmias.
Electrocardiography:
Standard, 12 Chest Leads is the most common ECG, three bipolar leads
(electrodes) on two arms and one leg, and nine chest leads are used.
The first is a small peak called the P wave that is the result of the depolarization
of the atria.
This is followed by the QRS complex. This is associated with the depolarization
of the ventricle and the repolarization of the atria which are occurring at the same
time
The interval between the P wave and the QRS complex is called the P-R interval.
It represents the time is takes for the impulse to travel from the SA Node to the
AV node, through the penetrating fibers and down the AV Bundle and Purkinje
Fibers.
The interval between the QRS complex and the T wave is called the Q-T interval. It
represents the time it takes for the ventricle to contract and relax again.
Starting with the heart in mid to late diastole, the events on the left side are as
follows:
The atria and ventricles are relaxed. Blood enters the heart passively from
the veins due to blood pressure. It flows through the atria and into the
ventricles.
The AV valves are open but the semilunar valves are closed.
70% of ventricular filling occurs during this time. Venous pressure = atrial
pressure = ventricular pressure. This is the phase of atrial and ventricular
diastole.
Once the SA Node initiates a cardiac contraction, the atria contract and atrial pressure
rises as the atrial contents are compressed. This is the phase of atrial systole and
ventricular diastole.
The atria relax and ventricles begin to contract. Blood in the ventricles is compressed
and the AV valves are forced shut.
This pressure in the ventricles is still not sufficient to open the semilunar valves
(it must rise above aortic pressure first). The ventricle is contracting, but no
blood is leaving it B this is the isovolumetric contraction phase.
The atria are in diastole but the ventricles are now in systole.
Blood now enters the aorta. Some blood will directly enter the arterial
tree, but much will remain in the aorta, which swells and the arterial
pressures rises. This is the ventricular ejection phase.
The ventricles begin to relax. Pressure begins to fall in the ventricles and blood
begins to flow backwards from the aorta and pulmonary arteries.
This closes the semilunar valves and causes a brief transient rise in aortic
pressure (the dictrotic notch).
The ventricles relax, but it takes a bit longer for the pressure to fall
in the ventricles. As a result, the AV valves remain closed. This
is the isovolumetric relaxation phase.
Throughout ventricular systole, the atria have been filling with blood from the
veins and atrial pressure rises slightly.
When ventricular pressure falls below this level, the AV valves open and
ventricular filling begins again.
The atrial pressure will fall slightly and then atrial and ventricular pressures will begin to
rise together as the chambers fill with blood.
When the thorax is auscultated (listened to) with a stethoscope, two distinct sounds can
be heard with each heartbeat.
The first sound is louder and longer, and is due to the closing of the AV valves.
The second sound is short and sharp and is due to the closing of the semilunar
valves.
Heart murmurs are a swishing sound that can be heard after the valves have closed and
blood flows backward through the valve or a high pitched sound that occurs just before
the valve closes and is due to blood flowing through narrow or stenotic valves.
Functional murmurs are common in children and elderly who have perfectly
healthy hearts. These are due to blood vibrating off of thin heart walls and make
the same sounds.
Cardiac pumping:
Cardiac output (CO) is the amount of blood pumped out by each ventricle in 1 minute.
Stroke volume is the amount of blood pumped out by a ventricle in each contraction.
Cardiac output is calculated by heart rate X stroke volume. Typically, adult cardiac
output is 5 L / minute.
Changing stroke volume and / or heart rate will alter cardiac output.
Cardiac output is highly variable and responds to changes in the heart rate, SV or both.
The difference between resting and maximal cardiac output is called the cardiac reserve.
In non-athletic people, the cardiac reserve is generally 4-5 times their normal CO.
In athletes, the cardiac reserve may reach 7 times their normal CO.
Stroke Volume is the difference between end diastolic volume and the end
systolic volume.
End systolic volume (ESV) is the amount of blood in the left in the
ventricle after it has contracted.
The EDV is determined by length of ventricular diastole and
venous pressure
SV (ml/beat) = EDV (120 ml) B ESV (50 ml) SV =70 ml/beat Hence, each ventricle
pumps out about 70 ml of blood (about 60%) of chamber with each heartbeat.
The factors contributing most to changes in the SV are preload, contractility, and
afterload.
The Frank-Starling law of the heart states the most critical factor in controlling
stroke volume is preload.
This is the degree of stretch of the cardiac muscle cells before they
contract.
The amount of blood that is returning to the heart and distending the ventricles,
the venous return, affects the EDV.
A higher contractility leads to a more complete ejection of blood from the heart,
which leads to a lower ESV.
Therefore, more blood remains in the heart after systole, which will
increase ESV and reduce stroke volume.
The sympathetic nervous system responds to times of stress or fright and releases
epinephrine and norepinephrine.
The sympathetic nerves which innervate the heart arise from the sympathetic
ganglia of the lower cervical vertebrae and the first 4 thoracic vertebrae.
Parasympathetic innervation of the heart comes from the tenth cranial nerve, which is
also known as the vagus nerve.
Therefore the heart is said to have a vagal tone, and a heart rate is slower than it
would be if the vagus nerve weren=t controlling it.
When either division of the autonomic nervous system is stimulated more strongly, the
stronger one inhibits the other.
Other factors such as age, gender, exercise and body temperature also affect
heartrate although they are not as important as neural factors.
The most common disorders are inadequate oxygenation (either localized or global), or
an unsustainable increase in the workload of the heart.
Congestive heart failure is disorder when the cardiac output is insufficient and blood
circulation is not meeting tissue needs.
In elderly people, sclerosis (hardening) of the valve flaps is common, as well as a decline
in cardiac reserve and sclerosis of the heart muscle itself.
Lack of exercise and high fat diet which can lead to hyperlipidemia
Diabetes Mellitus
Hypertension
Chronic elevation in mean arterial blood pressure forces the heart to work harder
to pump the same amount of blood.
Excess workload, over many years, simply wears out the heart.
The atria of the heart are sensitive to the pressure of the incoming blood, in particular
the venous pressure and the back-pressure of the pulmonary circulation.
If pressures get too high, the atria secrete a 28 amino acid peptide, atrial natriuretic
peptide (ANP).