The Myocardium

THE
MYOCARDIUM
ADEBOYE OLUWAJUYITAN

 The myocardium is the muscular wall of the heart, or
the heart muscle. It contracts to pump blood out of the
heart and then relaxes as the heart refills with
returning blood.
 The myocardium's smooth outer membrane is called
the epicardium. Its inner lining is called the
endocardium.

WORD Origin
 Myo – Muscle
 Cardio – Heart
 ‘-ium’ – Tissue, Structure
 Myocardium – muscular tissue of the heart

 Myo – Muscle
 Cardio – Heart
 ‘-cyte’ – cell
 Cardiomyocyte – Cardiac Muscle Cell
 ‘pathy’ – disease
 Cardiomyopathy – disease (chronic) of the heart
muscle

THE HEART MUSCLE
 The MYOCARDIUM, or cardiac muscle, is the thickest
section of the heart wall and contains
CARDIOMYOCYTES, which are the contractile cells of
the heart.
 The thickness of the myocardium determines the
strength of the heart's ability to pump blood.

PROPERTIES OF CARDIAC
MUSCLE
 Striations
 T-tubules
 Intercalated disks

MYOCYTE
 A myocyte (also known as a muscle cell) is the type of
cell found in muscle tissue (myocardium).
 There are two types of cells within the heart:
the Cardiomyocytes and the Pacemaker cells.
 Cardiomyocytes make up the atria and the ventricles.
 Pacemaker cells in the conduction system are
specialized cardiomyocytes that generate and conduct
electrical impulses.

CARDIOMYOCYTES
a) Make up the muscular walls of the atrium and
ventricles of the heart
b) Possess specific properties
(1) contractility – the ability of the cell to shorten and
lengthen its fibers
(2) extensibility – the ability of the cell to stretch

ELECTRICAL CELLS
a) Make up the conduction system of the heart
b) Are distributed in an orderly fashion through the heart
c) Possess specific properties
▪ automaticity – the ability to spontaneously generate
and discharge an electrical impulse
▪ excitability – the ability of the cell to respond to
an electrical impulse
▪ conductivity – the ability to transmit an electrical
impulse from one cell to the next

MYOFIBRIL
 A myofibril (also known as a muscle fibril) is a basic
rod-like unit of a muscle cell. Muscles are composed of
tubular cells called myocytes, known as muscle fibers
in striated muscle, and these cells in turn contain many
chains of myofibrils.
 Myofibrils are composed of long proteins
including actin, myosin, and titin, and other proteins that
hold them together. These proteins are organized into
thick and thin filaments called myofilaments, which repeat
along the length of the myofibril in sections
called SARCOMERES.
 Muscles contract by sliding the thick (MYOSIN) and thin
(ACTIN) filaments along each other.

MUSCLE TYPES
 There are 3 types of muscle tissue:
 Skeletal muscle tissue,
 Cardiac muscle tissue, and
 Smooth muscle tissue.
 The functions of muscle tissues depend on the type of
muscle tissues and their locations in the body.

 Cardiac muscle fibres are essentially long, cylindrical
cells with one (or sometimes two) nuclei. These are
centrally located within the cell.
 Each muscle fiber connects to the plasma membrane
(sarcolemma) with distinctive tubules (T-tubules).

 At these T-tubules, the sarcolemma is studded with a
large number of calcium channels which allow calcium
ion exchange.
 The flux of calcium ions into the muscle cells
stimulates an ACTION POTENTIAL, which causes the
cells to contract.

 Between the ends of adjacent cardiac muscle cells are
specialised intercellular junctions called
INTERCALATED DISKS. These are irregular
transverse thickenings of the sarcolemma that contain
structures called DESMOSOMES. Desmosomes are
like spot-rivets, that hold adjacent cardiac muscle
fibres together.

 The intercalated discs also act as points of anchorage
for the contractile proteins, and they contain important
channels called GAP JUNCTIONS. These connect the
cytoplasm of adjacent cardiac muscle fibres and
permit the extremely rapid low-resistance spread of
action potentials from one cell to another.

SARCOMERE
 SARCOMERE is the contractile unit of the myocardial
cell. Sarcomeres are composed of long, fibrous proteins
that slide past each other when the muscles contract and
relax.
 Two of the important proteins found in sarcomeres are
MYOSIN, which forms the thick filament, and ACTIN,
which forms the thin filament. Myosin has a long, fibrous
tail and a globular head, which binds to actin.
 Two other proteins present in sarcomeres are
TROPONIN and TROPOMYOSIN.

 TROPONIN is attached to the protein TROPOMYOSIN
and lies within the groove between actin filaments in
muscle tissue. In a relaxed
muscle, tropomyosin blocks the attachment site for the
myosin cross-bridge, thus preventing contraction.

TROPONIN
 Troponin is a complex of three polypeptides found in
striated muscle fibres.
 One polypeptide (TnI) binds to actin, another (TnT)
binds to tropomyosin, and the third (TnC) binds to
calcium ions.
 When calcium ions bind to troponin, the troponin
changes shape, forcing tropomyosin away from the
actin filaments. This allows myosin cross-bridges to
attach onto the actin, enabling contractions to occur.

Cardiomyocyte Perfusion
 Contain the protein myoglobin, which stores oxygen.
 Adapted to be highly resistant to fatigue.
Cardiomyocytes have a large number of mitochondria,
enabling continuous aerobic respiration.
 Large blood supply relative to its size, which provides
a continuous stream of nutrients and oxygen, while
providing ample removal of metabolic waste.

Myocardial Thickness
 The myocardium has variable levels of thickness within
the heart. Chambers of the heart with a thicker
myocardium are able to pump blood with more
pressure and force compared to chambers of the heart
with a thinner myocardium. The myocardium is
thinnest within the atria, as the atria fill largely through
passive blood flow.
 The thickness of the myocardium may change in some
individuals as a compensatory adaptation to disease.
The myocardium may thicken and become stiff, or it
may become thinner and flabby.

Myocardial Thickness and
Disease
 Cardiac hypertrophy is a common result of
hypertension (high blood pressure) in which the cells
of the myocardium enlarge as an adaptive response to
pumping against the higher pressure. Eventually it may
become so severe that heart failure occurs when the
heart becomes so stiff that it can no longer pump
blood.
 A flabby heart is typically the result of myocardial
infections (myocarditis), in which the heart muscle
becomes so weak that it cannot efficiently pump blood,
which also leads to heart failure.

Functions of the Myocardium
 Providing a scaffolding for the heart chambers
 Assisting in contraction and relaxation of the cardiac
walls so that blood can pass between the chambers.
 Conducting electro-stimulation through its own tissues
and into the epicardium (The Conducting system of the
heart).

FRANK-STERLING LAW OF
THE HEART
 The greater the initial length of cardiac muscle fibers,
the greater the strength of contraction
 The Frank-Starling mechanism describes how the
heart changes its force of contraction, and therefore
stroke volume, in response to venous blood return.
 Greater venous blood return results in an increase in
ventricular filling and preload. In turn, the length of
cardiac muscle fibers increases (they are stretched as
the heart fills with blood), resulting in greater strength
of contraction.

Conduction System of the
Heart
This pathway is made up of 5 elements:
 The Sino-atrial (SA) node
 The Atrio-ventricular (AV) node
 The Bundle of His
 The Left and Right Bundle Branches
 The Purkinje fibers

SINOATRIAL NODE
 Inherent firing rate is the rate at which the SA NODE
or another pacemaker site normally generates
electrical impulses
 SA Node
 Dominant or primary pacemaker of the heart
 Inherent rate 60 – 100 beats per minute
 Located in the wall of the right atrium, near the inlet of
the superior vena cava
 Once an impulse is initiated, it usually follows a specific
path through the heart, and usually does not flow
backward

BACHMANN’S BUNDLE
 As the electrical
impulse leaves the
SA node, it is
conducted through
the left atria by way
of the Bachmann's
bundle, through the
right atria, via the
atrial tracts.

ATRIO-VENTRICULAR
JUNCTION
1. AV node
a) Is responsible for delaying the impulses that reach it
b) Located in the lower right atrium near the interatrial septum
c) Waits for the completion of atrial emptying and ventricular filling, to
allow the cardiac muscle to stretch to it's fullest for peak cardiac output
d) The nodal tissue itself has no pacemaker cells, the tissue surrounding
it (called the junctional tissue) contains pacemaker cells that can fire at an
inherent rate of 40 – 60 beats per minute

BUNDLE OF HISS
 a) Resumes rapid conduction of the impulses through
the ventricles
 b) Makes up the distal part of the AV junction then
extends into the ventricles next to the interventricular
septum
 c) Divides into the Right and Left bundle branches
 Hiss bundle have a rate is 30-40bpm; Bundle branches
20-30bpm.

PURKINJE FIBERS
 a) Conduct impulses rapidly through the muscle to assist
in depolarization and contraction
 b) Can also serve as a pacemaker, discharges at an
inherent rate of 15 – 20 beats per minute or even more
slowly
 a) Are not usually activated as a pacemaker unless
conduction through the bundle of His becomes blocked or
a higher pacemaker such as the SA node or AV junction
do not generate an impulse
 b) Extends form the bundle branches into the
endocardium and deep into the myocardial tissue

ACTION POTENTIAL
medical definition of ACTION POTENTIAL
: a momentary reversal in the potential difference
across a plasma membrane (as of a nerve cell or
muscle fiber) that occurs when a cell has been
activated by a stimulus—called also spike potential.
(Merriam-Webstar)

 Action potentials occur in several types of animal cells, called
excitable cells, which include neurons, muscle cells,
and endocrine cells, as well as in some plant cells.
 In muscle cells, an action potential is the first step in the chain of
events leading to contraction

 In animal cells, there are two primary types of action
potentials. One type is generated by voltage-gated
sodium channels, the other by voltage-gated calcium
channels.
 Sodium-based action potentials usually last for under one
millisecond, whereas calcium-based action potentials
may last for 100 milliseconds or longer.
 In cardiac muscle cells, an initial fast sodium spike
provides a "primer" to provoke the rapid onset of a
calcium spike, which then produces muscle contraction

Cardiac Action Potential
 The action potential of a cardiac muscle fiber can be broken
down into several phases:
0- depolarization,
1- initial rapid repolarization,
2- plateau phase,
3- late rapid repolarization,
4- baseline.

DEPOLARIZATION &
REPOLARIZATION
 1. Cardiac cells at rest are considered polarized, meaning no electrical
activity takes place.
 2. The cell membrane of the cardiac muscle cell separates different
concentrations of ions, such as sodium, potassium, and calcium. This is
called the resting potential.
 3. Electrical impulses are generated by automaticity of specialized
cardiac cells.
 4. Once an electrical cell generates an electrical impulse, this electrical
impulse causes ions to cross the cell membrane and leads to an action
potential, also called DEPOLARIZATION.
 5. The movement of ions across the cell membrane through sodium,
potassium and calcium channels, is the drive that causes contraction of
the cardiac cells/muscle.

 6. Depolarization with corresponding contraction of
myocardial muscle moves as a wave through the heart.
 7. REPOLARIZATION is the return of the ions to their
previous resting state, which corresponds with relaxation
of the myocardial muscle.
 8. Depolarization and repolarization are electrical
activities which cause muscular activity.
 9. The action potential curve shows the electrical
changes in the myocardial cell during the depolarization –
repolarization cycle.
 10. This electrical activity is what is detected on ECG,
not the muscular activity.

Key Points
 All cells in the heart can spontaneously generate action potential
(AP).
 The heart is myogenic, it does not require the nervous system to
work, in contrast to the skeletal muscles which are neurogenic.
 Not all heart cells generate APs at the same speed.
 The cells that have the fastest rate of intrinsic activity/automaticity
are called the Pacemaker Cells of the heart.

 All heart cells are electrically joined together by
intercalated disks (Gap Junctions).
 That means that once one heart muscle cell generates
an AP, it just spreads to the others.
 Thus APs generated by pacemaker cells normally
spread throughout the heart before the other cells
have a chance to generate an AP.
 So the heart functions as a single unit.

What are the Autonomic
Neurons for?
 To VARY the rate of activity of the heart.
 The ANS modulates the HR by speeding it up (SANS)
when you exercise or slowing it down (PANS) when
you go to sleep.

Sympathetic nervous
system (or Adrenergic)
 1. Accelerates the heart
 2. Two chemicals are influenced by the sympathetic
system – epinephrine & norepinephrine
 3. These chemicals increase heart rate, contractibility,
automaticity, and AV conduction

Parasympathetic nervous system (
or Cholinergic)
 1. Slows the heart
 2. The Vagus nerve is one of this systems nerves, when stimulated
slows heart rate and AV conduction.

THE ACTION POTENTIAL
CURVE
 It consists of 5 phases

Ions and Concentration
Gradients
 Na+ – Higher in E.C.F. (Outside cell)
 K+ – Higher in I.C.F. (Inside cell)
 Ca+ – Higher in E.C.F. (Outside cell; Inside the cell it is
stored in Sarcoplasmic reticulum)

Types of Ion Channels
 Leakage–gated Ion Channels
 Voltage–gated Ion Channels
 Ligand–gated Ion Channels

PHASE 4 - REST
 1) this is the cells resting phase
 (2) the cell is ready to receive an electrical stimulus

PHASE 0 – UPSTROKE
 (1) is characterized by a sharp, tall upstroke of the
action potential
 (2) the cell receives an impulse from a neighbouring
cell and depolarizes
 (3) during this phase the cell depolarizes and begins
to contract

PHASE 1 - SPIKE
 (1) contraction is in process
 (2) the cell begins an early, rapid, partial
repolarization

PHASE 2 - PLATEAU
 (1) contraction completes, and the cell begins relaxing
 (2) this is a prolonged phase of slow repolarization

PHASE 3 - DOWNSLOPE
 (1) this is the final phase of
rapid repolarization
 (2) repolarization is complete
by the end of phase 3

PHASE 4 - REST
 (1) return to the rest period
 (2) the period between action potentials

The Myocardium

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