Drugs modifying cardiac rate and force

Question 1

what are the regulatory influences on heart rate?

Answer 1

• balance of autonomic input
• stretch
• temperature
• hypoxia
• blood pH
• thyroid hormones

Question 2

what is overdrive suppression?

Answer 2

the SA node sets the rhythm for the heart because it discharges APs at a greater frequency than AV and his system

Question 3

what four currents are important in the phase 4 (pacemaker potential ) of SA and AV nodes?

Answer 3

Ib - background sodium current inward

increased funny current - HCN channels open to conduct Na and K inward

ICaT - transient inward calcium current

and decreased Ik - delayed rectifier potassium current

Question 4

why is it called the funny current?

Answer 4

The inward movement of Na and Sodium is mediated by hyperpolarisation and cyclic nucleotide gated (HCN) channels

Question 5

what is the sequence of channel opening in

Answer 5

immediately after AP the membrane potential reaches its most negative value this is enough to open channles that conduct NA and K

then I cat switches on just before we hit threshold
at this point another class of VA channels opens

Question 6

what mediates phase 0 of nodal AP?

Answer 6

increased Ical - long calcium current

Question 7

what mediates phase 3 - downstroke of nodal AP ?

Answer 7

increased Ik - delayed rectifier potassium current

Question 8

what current/ s mediated phase 4( diastolic potential) of atrial and ventricular myocyte APs ?

Answer 8

Ik1 - inward rectifier potassium current - this steady membrane potential is determined by a constant trickle of K ions OUTWARD

Question 9

what does the outward trickle of K in phase 4 of atrial and ventricular myocyte APs result in?

Answer 9

the activation of VA I na - this is responsible for upstroke.

Question 10

the majority of Na channels do not remain conducting for long. They go into a _____ _______ state after a millisecond.

Answer 10

the majority of Na channels do not remain conducting for long. They go into a nonconducting inactivated state after a millisecond.

Question 11

what is responsible for the small flux after upstroke in atrial and ventricular myocyte APs ?

Answer 11

due to a combination of

1. Na ceasing
2. Ito - a transient outwards potassium current

Question 12

what mediates phase 2 (plateau) in atrial and ventricular myocyte APs?

Answer 12

1. Increased CaL - long calcium current (inward)
   as this happens K channels are slowly activated so the plateau is a fine balance of inward Ca movement by outwards K movement.

Question 13

what two other mechanisms support phase 2 of atrial and ventricular myocyte APs?

Answer 13

1. not all VA Na inactivate - about 1% remain open and this gives rise to INaL - this is a late (or persistent) sodium current inward.
2. This is not an ion channel but a transporter. The Na Ca exchanger. This is in several forms in the body but it is NX1 in the heart. At resting potential it allows 3Na in and expells 1 Ca - this Ca has a +2 charge though! If, however, the MP is at depolarising potential this transporter will run backwards.

Question 14

what mediates phase 3 of atrial and ventricular myocyte APs?

Answer 14

Ik - there are two components

• a fast activating one fast I kr which opens first
• a slow activating one - Iks

Question 15

Noradrenaline (postganglionic transmitter) and adrenaline (adrenomedullary hormone) activate _____ in nodal cells and myocardial cells to sympathetic system

Answer 15

b1 adrenoceptors

Question 16

B1 adrenoceptors are __ coupled. The__ protein that they couple to is __. This is a stimulatory_ ____ which activates the membrane enzyme _____ _____ which in turn generates ____ from ATP.

Answer 16

B1 adrenoceptors are G coupled. The G protein that they couple to is Gs. This is a stimulatory G protein which activates the membrane enzyme adenylyl cyclase which in turn generates cAMP from ATP.

Question 17

what happens to the heart rate when sympathetic system is stimulated?

Answer 17

increase HR - a positive chronotropic effect

Question 18

what two things happen to increase AP rate?

Answer 18

i) increase in the slope of phase 4 depolarisation

ii) reduction in the threshold for AP initiation

Question 19

what mediates the increase in the slope of phase 4 depolarisation from sympathetic stimulation?

Answer 19

increased If and ICa

Question 20

what mediates the decrease in threshold of phase 4 depolarisation from sympathetic stimulation?

Answer 20

I Ca - Because inward Ca is stimulated this means that the pacemaker potential reaches threshold at a more negative value than usual.

Question 21

what other things happen to the heart on sympathetic stimulation?

Answer 21

1. increased contractility
2. increased conduction velocity
3. increased automacity
4. decreased duration of systole
5. decrease in cardiac efficiency
6. increased activity of the Na/ K ATPase
7. increased mass of cardiac muscle

Question 22

what causes the increased contractility from sympathetic stimulation ?

Answer 22

i) an increase in phase 2 of the cardiac action potential in atrial and ventricular myocytes and enhanced Ca influx and
(ii) sensitisation of contractile proteins to Ca

Question 23

what causes increased conduction velocity in AV node in sympathetc stimulation?

Answer 23

due to enhancement of If and I ca (as in SA node) This occurs because of the calcium flux in the AV node is increased

Question 24

what causes increased automacity in sympathetc stimulation? (i.e. tendency for non-nodal regions to acquire spontaneous activity – explored in later

Answer 24

If the muscle cells are stimulated hard then even muscle cells can discharge AP at their own rhythm i.e. without SA control
this leads to ventricular fibrillation- very dangerous

Question 25

what causes a decrease in the duration of sytstole in sympathetic stimulation

Answer 25

due to cAMP due to increased uptake of Ca2+ into the sarcoplasmic reticulum

Question 26

why is there also a decrease in the duration of diastole in sympathetic stimulation?

Answer 26

the rate of relaxation must also increase because if it didnt then the ventricles would be partially filled with blood before the next filling.

Question 27

there is also a decrease in cardiac efficiency in sympathetic stimulation with respect to____ consumption which increases disproportionately with increasing work

Answer 27

there is also a decrease in cardiac efficiency in sympathetic stimulation with respect to oxygen consumption which increases disproportionately with increasing work

Question 28

Parasympathetic fibres are stimulated by the____ nerve.

_____ is the postganglionic transmitter and it activates ________ largely in ___ cells.

Answer 28

Parasympathetic fibres are stimulated by the vagus nerve.

Acetylcholine is the postganglionic transmitter and it activates M2 muscarinic cholinoceptors largely in NODAL cells.

Question 29

It is the ____ and ____ subunits that are important in the cardiac regulation of the parasympathetic system

Answer 29

It is the beta gamma subunits that are important in the cardiac regulation

Question 30

what do the beta and gamma subunits do in parasympathetic stimulation?

Answer 30

they switch on special K channels called GIRKs

Question 31

when do GIRKS do?

Answer 31

are found in the AV node and when they are activated they hyperpolarize the node so slow the impulse conduction.

Question 32

coupling through the G protein in parasympathetic stimulation does 2 things. what are they?

Answer 32

i) decreases activity by adenylate cyclase and reduces (cAMP)
ii) opens potassium channels (GIRK) to cause hyperpolarization of SA node (mediated by Gi βγ subunits)

Question 33

what three things cause the decrease in heart rate from parasympathetic stimulation?

Answer 33

(i) decreased slope of the pacemaker potential caused by reduced If and ICa,
(ii) hyperpolarization caused by the opening of GIRK channels,
(iii) increase in threshold for AP initiation caused by reduced ICa

Question 34

why is there decreased contractility in parasympathetic stimulation?

Answer 34

due to decrease in phase 2 of cardiac action potential and decreased Ca2+ entry
- this is only seen at the atria as ventricles dont have parasympathetic innervation

Question 35

why is there decreased conduction in parasympathetic stimulation?

Answer 35

due to decreased activity of voltage-dependent Ca2+ channels and hyperpolarization via opening of K+ channels

Question 36

what does parasympathetic stimulation have the ability to cause - bad?

Answer 36

may cause arrhythmias to occur in the atria (AP duration is reduced and correspondingly the refractory period – predisposes the re-entrant arrhythmias

Question 37

what is the pacemaker potential modulated by?

Answer 37

If

Question 38

what activates the funny current?

Answer 38

(i) hyperpolarization and

(ii) cyclic AMP [called hyperpolarization-activated cyclic nucleotide gated (HCN) channels

Question 39

how does cAMP increase the activation of HCN ?

Answer 39

cAMP increases the activation of the HCN channels by making the channel more sensitive so it is activated more readily.

Question 40

what does the ivabradine do?

Answer 40

it is a selective blocker of HCN 4 channels that is used to slow HR in angina. Slower HR reduces oxygen consumption

Question 41

what are the 6 steps in Ca contraction coupling in cardiac muscle

Answer 41

1. ventricular AP
2. opening of voltage - activated Ca channels (mainly L- type) during phase 2 of action potential
3. Ca influx into the cytoplasm
4. Ca release from the sarcoplasmic reticulum (CICR)
5. Ca binds to troponin C and shifts tropomyosin out of the actin cleft
6. cross bridge formation between actin and myosin resulting in contraction via the sliding filament mechanisms

Question 42

what are the 6 steps in Ca relaxation coupling in cardiac muscle

Answer 42

1. repolarisation in phase 3 to phase 4
2. VA l-type Ca channels close
3. Ca influx ceases. Ca efflux occurs by the Na/Ca exchanger NCX1 - a plasma membrane ATPase is less importatnt
4. Ca release from the sarcoplasmic reticulum ceases. Active sequestration via Ca- ATP ase (SERCA) of Ca from the cytoplasm now dominates
5. Ca dissociates from troponin C
6. Cross bridges between actin and myosin break resulting in relaxation

Question 43

what does adenylate cyclase convert ?

Answer 43

ATP to cAMP

Question 44

what does cAMP activate?

Answer 44

protein kinase A

Question 45

what three things does protein kinase A do?

Answer 45

1. phosphorylates L-type calcium channels leading to Ca influx
2. increase the sensitivity of the MLC to Ca which leads to increased contractility
3. phosphorylates phospholamban which increases the pumping of Ca and increases the rate of relaxation

Question 46

what can convert cAMP to inactive 5AMP?

Answer 46

a phosphodiesterase enzyme (PDE)

Question 47

what does inhibition of PDE cause ?

Answer 47

a positive inotropic effect that can be achieved with drugs such as mirinone that are now seldom used, except in heart failure.

Question 48

what are 3 examples of B adrenoceptor agonists?

Answer 48

dobutamine, adrenaline and noradrenaline (cetacholamines)

Question 49

what is the pharmacodynamic effects of beta agonists ? 2 things

Answer 49

• they increase the force, rate and cardiac output (i.e. HR xSV) and O2 consumption
• they decrease cadiac efficiency (O2 consumptions is increased more than cardiac work)

Question 50

what adverse effect can beta agonists have ?

Answer 50

can cause disturbances in cardiac rhythm

Question 51

what is the effect of adrenaline on beta 1 receptors ?

Answer 51

has a positive inotropic and chronotropic effect

Question 52

what is the effect of adrenaline on beta 2 receptors ?

Answer 52

dilate the coronary arteries

Question 53

what is the effect of adrenaline on alpha 1 receptors ?

Answer 53

redistribution of blood flow to the heart (constricts blood vessels in the skin, mucosa and abdomen

Question 54

what receptor does dobutamine act on?

Answer 54

selective for beta adrenoceptors

Question 55

what is dobutamine used for?

Answer 55

acute, but potentially reversible, heart failure (e.g. following cardiac surgery, or cardiogenic, or septic, shock). For reasons unknown, causes less tachycardia than other β1 agonists)

Question 56

what is the main effect of dobutamine on the heart?

Answer 56

it does not increase the heart rate too much but increases contractions

Question 57

what do the effects of beta antagonists depend on?

Answer 57

the degree to which the sympathetic nervous system is activated.

Question 58

give an example of a beta antagonist that blocks non- selectively

Answer 58

propranolol

Question 59

give an example of a beta antagonist that blocks selectively

Answer 59

atenolol, bisoprolol, metoprolol

Question 60

give an example of a beta antagonist that is non- selective and a partial agonist

Answer 60

alprenolol

Question 61

why do beta antagonists reduce maximal exercise tolerance?

Answer 61

during exercise, or stress, rate and force and CO are significantly depressed

Question 62

beta antagonists reduce the diameter of coronary vessels, why is there better oxygenation of the myocardium though?

Answer 62

the myocardial oxygen requirement falls

Question 63

what are b-adrenoceptor antagonists used for?

Answer 63

1. treatment of disturbances of cardiac rhythm (arrhythmias)
2. Treatment of Angina
3. heart failure
4. hypertension

Question 64

what can excessive sympathetic activity associated with stress, emotion, or disease (e.g. heart failure, myocardial infarction) lead to

Answer 64

tachycardia, or spontaneous activation of ‘latent cardiac pacemakers’ outside nodal tissue

Question 65

what do beta antagonists do to prevent arrhythmias?

Answer 65

they decrease excessive sympathetic drive and help to restore normal sinus rhythm

Question 66

what do beta blockers do in AF and SVT ?

Answer 66

they block conduction through the AV node and help restore sinus rhythm

Question 67

what are the adverse effects of beta blockers?

Answer 67

• non-specific may cause bronchospasm
• aggrevation of heart failure (patients with heart disease may rely on sympathetic drive to maintain an adequate CO)
• bradycardia
• hypoglycaemia
• fatigue
• cold extremities

Question 68

what is a complication of using beta blockers which are causing bradycardia?

Answer 68

heart block because in patients with coronary disease; β-adrenoceptors facilitate nodal conduction

Question 69

which patients may get hypoglycaemia in response to beta blockers? and why?

Answer 69

in patients with poorly controlled diabetes – the release of glucose from the liver is controlled by β2-adrenoceptors

Question 70

why do people experience cold extremities with beta blockers?

Answer 70

loss of β2-adrenoceptor mediated vasodilatation in cutaneous vessels

Question 71

why do people experience fatigue with beta blockers?

Answer 71

CO (β1) and skeletal muscle perfusion (β2) in exercise are regulated by adrenoceptors

Question 72

what is an example of a Non-Selective Muscarinic ACh Receptor Antagonist?

Answer 72

atropine

Question 73

what are the pharmacodynamic effects of atropine ?

Answer 73

• increases HR
• no effect upon arterial BP
• no effect upon the response to exercise

Question 74

why do Non-Selective Muscarinic ACh Receptor Antagonists have no effect upon arterial BP?

Answer 74

the resistance vessels lack a parasympathetic innervation

Question 75

what are Non-Selective Muscarinic ACh Receptor Antagonists used for clinically ?

Answer 75

First line in management of severe, or symptomatic bradycardia, particularly following myocardial infarction (in which vagal tone is elevated)

Some practitioners recommend no less than 600 micrograms as low-dose atropine may paradoxically transiently slow heart rate (see figure)

Question 76

what is digoxin ?

Answer 76

Digoxin - A Cardiac Glycoside That Increases Contractility of the Heart

Question 77

what is digoxin used in?

Answer 77

heart failure - as CO is insufficinet to produce adequate perfusion

Question 78

what three parts structurally make up digoxin?

Answer 78

Digoxin has a sugar, steroid and lactone part. The steroid and lactone make up the pharmacophore

Question 79

Digoxin increases the contractility by blocking the ____ ___ase.

Answer 79

Digoxin increases the contractility by blocking the sarcolemma ATPase.

Question 80

what does the Na/K ATP ase do to the membrane potential?

Answer 80

Na/K ATPase results in the movement of 1 positive charge out so this has a hyperpolarizing influence on the membrane.

Question 81

This ATP ase generates an ______ gradient for sodium and the ___/__ exchanger uses this energy from the gradient to pump __ back into the cell. note there is ____ net change in Na concentration.

Answer 81

This ATP ase generates an electrochemical gradient for sodium and the Na/Ca exchanger uses this energy from the gradient to pump Na back into the cell. note there is no net change in Na concentration.

Question 82

Digoxin blocks the Na/K ATPase which lead to

1. increased intracellular __ levels
2. slight _______ of the MP
3. Because there is an increased __ concentration there is a _______ driving force for ___ to enter the cell

Answer 82

Digoxin blocks the Na/K ATPase which lead to

1. increased intracellular Ca levels
2. slight depolarisation of the MP
3. Because there is an increased Ca concentration there is a decreased driving force for Na to enter the cell

Question 83

why can Ca not be transported out of the cell as effectively in the presence of digoxin? why dont you get increased Ca in the cell though?

what does digoxin do to the interaction between Ca and troponin C

Answer 83

The decreased energy from Na pump means that Ca cannot be transported out of the cell as effectively as normal

BUT you don’t get increased Ca because the excess Ca is actively transported into the sarcoplasmic reticulum

During the plateau of the AP the Ca channels that open Ca mean that there is a increased Ca release. This means that with digoxin there is increased Ca interaction with troponin

Question 84

Digoxin binds to the ___ subunit of Na/K ATPase in competition with _

Answer 84

Digoxin binds to the alpha subunit of Na/K ATPase in competition with K

Question 85

when can the effects of digoxin be dangerously enhanced?

Answer 85

enhanced by low plasma K because K and digoxin are effectively in competition and when there is low K, digoxin can bind. This is particularly important because D has a very low therapeutic ratio.

Question 86

what is the indirect effect of digoxin on electrical activity? 2 things

Answer 86

• increased vagal activity

- it slows SA node discharge and slows AV node conduction; increases the refractory period

Question 87

what is the direct effect of digoxin on electrical activity?

Answer 87

shortens the action potential and refractory period in atrial and ventricular myocytes

Question 88

what is the danger of digoxin for electrical activity ?

Answer 88

is pro-arrhythmatic; toxic concentration cause membrane depolarisation and oscillatory afterpotential

Question 89

what is the afterpotential caused by digoxin likely due to?

Answer 89

likely due to Ca overload. D promotes the accumulation of Ca in the cell meaning that a second AP can be conducted outwith the control of the SA node.

Question 90

what is the danger if you have an afterpotential from digoxin?

Answer 90

after a second triggered AP - get another ectopic beat and this could lead to ventricular tachycardia which is self sustaining to produce fibrillation

Question 91

what is digoxin used to treat clinically ?

Answer 91

• IV in acute heart failure, or orally in chronic heart failure, in patients remaining symptomatic despite optimal use of other drugs (e.g. ACE inhibitors, diuretics)
• Particularly indicated in heart failure with atrial fibrillation (AF)

Question 92

why is digoxin useful in heart failure with AF?

Answer 92

increase in AV node refractory period is beneficial, helps to prevent spreading of the arrhythmia to the ventricles

Question 93

what are 2 cardiac side effects of digoxin?

Answer 93

• excessive depression of AV node conduction (heart block)

- propensity to cause arrhythmias

Question 94

Extracardiac effects are numerous: this is because ___ ase is in LOADS of cells

Answer 94

Extracardiac effects are numerous: this is because ATP ase is in LOADS of cells

Question 95

what does levosimendan do?

Answer 95

• Increases the force of contraction

- vasodilates vascular smooth muscle

Question 96

why does levosimendan increase the force of contraction?

Answer 96

binds to troponin c in cardiac muscle sensitising the contractile proteins to action of Ca -this promotes Cross bridge formation increasing the force of contraction

Question 97

how does levosimendan cause vascular smooth muscle vasodilation ?

Answer 97

it opens K atp channels in the vascular smooth muscle

• when open this hyperpolarizes the cell
• if you hyperpolarize smooth muscle vasculature you get vasodilation

Question 98

what are two examples of Inodilators?

Answer 98

amrinone and milrinone

Question 99

what do inodilators do? 2 things

Answer 99

• increases the force of contraction

- it decreases peripheral resistance

Question 100

how do inodilators increase the force of contraction?

Answer 100

they inhibit PDE in cardiac and smooth muscle cells and hence increase cAMP

Question 101

what are inodilators used for clinically?

Answer 101

its use is limited to IV administration in acute heart failure