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Pre-reg exam > Heart failure > Flashcards

Heart failure Flashcards

1
Q

Loop Diuretics

Common indications

A
  • For relief of breathlessness in acute pulmonary oedema in conjunction with oxygen and nitrates
  • For symptomatic treatment of fluid overload in HF
  • Symptomatic treatment of fluid overload in other oedematous states- H+R failure, where they may be given in combination with other diuretics
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2
Q

Loop diuretics

MOA

A
  • As their name suggests, loop diuretics act principally on the ascending limb of the loop of Henle, where inhibit Na+/K+/2Cl- Co-transporter
  • This protein is responsible for transporting sodium and potassium and chloride ions from the tubular lumen into the epithelial cell
  • Water then follows by osmosis. Inhibiting this process has a potent diuretic effect
  • Also, loop diuretics have a direct effect on blood vessels, causing dilation of capacitance veins
  • In acute HF, this reduces preload and improves contractile function of the overstretched heart muscles
  • Indeed, this is probably the main benefit of loop diuretics in acute HF, as illustrated by the fact that the clinical response is usually evident before a diuresis is established
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3
Q

Loop diuretics

Adverse effects

A
  • Water losses due to diuresis can lead to dehydration and hypotension
  • Inhibiting the Na/K/2Cl co-transporter increases urinary sodium, chloride and pottasium loss
  • Indirectly also causes increased excretion Mg, Ca and H ions
  • You can therefore associate loop diuretics with almost any low electrolyte state
  • A similar Na/K/2Cl co-transporter is responsible for regulating endolymph composition in the inner ear
  • At high doses, loop diuretics can affect this too, leading to hearing loss and tinnitus
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4
Q

Loop diuretics

Warnings

A
  • Loop diuretics are contraindicated in patients with hypovolaemia or dehydration
  • They should be used with caution in patients at risk of hepatic encephalopathy
  • Severe hypokalaemia and hyponatraemia
  • Taken chronically, loop diuretics inhibit uric acid excretion and this can worsen gout
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5
Q

Loop diuretics

Interactions

A
  • Loop diuretics have the potential to affect drugs that are excreted by the kidneys
  • For example, Lithium levels are increased due to reduced excretion
  • Digoxin toxicity may also increase
  • Increase ototoxicity and nephrotoxicity of aminoglycosides
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6
Q

Loop diuretics

Monitoring

A
  • For safety, periodic monitoring of serum sodium, pottasium and renal function is also advisable, particularly in the first few weeks of therapy
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7
Q

ACE inhibitors

Common indications

A
  • Hypertension- for the first or second-line treatment of hypertension
  • Chronic HF
  • Ischaemic heart disease
  • Diabetic nephopathy and CKD with proteinuria
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8
Q

ACE inhibitors

MOA

A
  • ACE inhibitors block the action of the ACE to prevent conversion of angiotensin I => II
  • Angiotensin II is a vasoconstrictor and stimulates aldosterone secretion
  • Blocking its action reduces peripheral vascular resistance (afterload), which lowers BP
  • It particularly dilates the efferent glomerular arteriole, which reduces intraglomerular pressure and slows the progression of CKD
  • Reducing the aldosterone level promotes sodium and water excretion
  • This can help to reduce venous return (pre-load), which has a beneficial effect in HF
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9
Q

ACE inhibitors

Adverse effects

A
  • Common side effects include hypotension (particular after the first dose), persistent dry cough (due to increased levels of bradykinin, which usually inactivated by ACE) and hyperkalaemia (because a lower aldosterone level promotes potassium retention)
  • They can cause or worsen renal failure
  • This is particularly relevant in patients with renal artery stenosis, who rely on the constriction of the efferent glomerular arteriole to maintain glomerular filtration
  • If detected early, these adverse effects are usually reversible on stopping the drug
  • Rare but important side effects of ACEI include angioedema and anaphylactoid reactions
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10
Q

ACE inhibitors

Warnings

A
  • ACEI should be avoided in patients with renal artery stenosis or acute kidney injury
  • Pregnant and breastfeeding
  • CKD, lower doses should be used and the effect on renal function monitored closely
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11
Q

ACE inhibitors

Interactions

A
  • Due to the risk of hyperkalaemia, avoid prescribing ACEI with other potassium-elevating drugs, including supplements and K-sparring diuretics
  • Incombination with other diuretics (profound first dose hypotension)
  • NSAID and ACEI increases the risk of renal failure
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12
Q

ACE inhibitors

Communication

A
  • Take the first dose before bed to reduce symptomatic hypotension
  • Common side effects: Dry cough, dizzieness, allergic reactions
  • Need blood test monitoring, explaining that ACEI can interfere with renal function and upset K balance
  • Advise to avoid taking OTC NSAID
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13
Q

ACE inhibitors

Monitoring

A
  • Monitor efficacy for reduced symptoms of breathlessness in HF
  • Check electrolyte and renal function before starting treatment
  • Repeat 1-2 weeks into treatment and increasing dose
  • Creatinine concentration should not rise by more than 30%
  • eGFR should not fall by more than 25%
  • K levels should not be above 6mmol/L
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14
Q

Beta-Blockers

Common indications

A
  1. Ischaemic heart disease- first line option to improve symptoms and prognosis associated with angina and acute coronary syndrome
  2. Chronic HF- as a first line option to improve prognosis
  3. Atrial fibrillation- As a first-line option to reduce the ventricular rate and in paroxysamal AF, to maintain sinus rhythm
  4. Supraventricular tachycardia (SVT)- first-line option in patients without circulatory compromise
  5. Hypertension
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15
Q

Beta-Blockers

MOA

A
  • Beta1-adrenoreceptors are located mainly in the heart, whereas B2-adrenoreceptors are found mostly in the smooth muscle of blood vessels and the airways
  • Beta-Blockers reduce the force of contraction and speed of conduction in the heart
  • This relieves myocardial ischaemia by reducing cardiac work and oxygen demand, and increasing myocardial perfusion
  • They improve prognosis in heart failure by protecting the heart from the effect of chronic sympathetic stimulation
  • They slow the ventricular rate in AF mainly by prolonging the refractory period of the atrioventricular node
  • In HTN, BB lower BP through a variety of means, one of which is by reducing renin secretion from the kidney, since this is mediated by B1-receptors
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16
Q

Beta-Blockers

Adverse effects

A
  • Beta-Blockers commonly cause fatigue, cold extremities, headache and GI disturbances
  • They can cause sleep disturbances and nightmares as well as impotence in men
17
Q

Beta-Blockers

Warnings

A
  • Asthma- BB can cause life-threatening bronchospasm and should be avoided
  • The effect is mediated by blockade of B2-adrenoreceptors in the airways
  • BB is usually safe in COPD, although it is prudent to choose a B1 selective receptor
  • In HF, BB should be started at a low dose and slowly increased, as they initially impair cardiac function
  • They should be avoided in patients with haemodynamic instability and are contraindicated in heart block
  • BB generally require dosage reduction in significant hepatic failure
18
Q

Beta-Blockers

Interactions + monitoring

A
  • BB must not be used with non-dihydropyridine calcium channel blockers
    • This combination can cause HF, bradycardia and asystole
  • The best guide to dosage adjustment is the patient’s symptoms and HR should be around 60BPM
19
Q

Statins

Common indications

A
  • Primary prevention of cardiovascular disease: to prevent cardiovascular events in people over 40 years of age with a 10-year cardiovascular risk >20%.
  • Secondary prevention of cardiovascular disease: the first-line alongside lifestyle changes, to prevent further cardiovascular events in those who already have evidence of cardiovascular disease.
  • Primary hyperlipidaemia: first-line, in conditions such as primary hypercholesterolaemia, mixed dyslipidaemia and familial hypercholesterolaemia.
20
Q

Statins

MOA

A
  • Statins reduce serum cholesterol levels. They inhibit 3-hydroxy-3- methyl-glutaryl coenzyme A (HMG CoA) reductase, an enzyme involved in making cholesterol
  • They decrease cholesterol production by the liver and increase the clearance of LDL-cholesterol from the blood, reducing LDL-cholesterol levels
  • They also indirectly reduce triglycerides and slightly increase HDL-cholesterol levels. Through these effects, they slow the atherosclerotic process and may even reverse it
21
Q

Statins

Adverse effects

A
  • Statins generally safe
  • headache and GIT disturbances
  • Myopathy and rhabdomyolysis
  • Raise in liver enzymes
22
Q

Statins

Warnings

A
  • Hepatic impairment- use with cautions
  • Renal impairment- use with caution- renal excretion
  • Pregnant/Breastfeeding- ChE essential for normal fetal development
23
Q

Statins

Interactions

A
  • CYP P450 inhibitors (Amiodarone, diltiazem, macrolides) leads to accumulation of statin in body increasing risk of adverse effects
  • Amlodipine- has a similar interaction though the mechanism is less clear. If taking the 2 together stop statin during acute antibiotic course (clarithromycin)
24
Q

Statins

Communication

A
  • Should be taken in the evening, as there is some evidence that they have a greater effect when food intake is at its lowest
  • Must seek medical attention if they experience muscle symptoms (pain or weakness)
  • Ask for blood tests in 3 and 12 months
  • Avoid grapefruit juice
25
Q

Statins

Monitoring

A
  • Primary prevention of CVD- Blood test before treatment but does not need regular check-ups
  • Secondary prevention-
  • For safety check Lover enzymes at 3 and 12 months
  • A rise in ALT up to three times the upper limit of normal may be acceptable, but above this should lead to discontinuation. The statin can be restarted at a lower dose when liver enzymes have returned to normal. You do not need to check creatine kinase routinely, but you should ask patients to report muscle symptoms
26
Q

Sacubitril

Indications + MOA

A
  • Symptomatic chronic HF with reduced ejection fraction (in combo with Valsartan)
  • Inhibiting neprilysin- increase cGMP, which results in vasodilation, natriuresis and diuresis, increased GFR and renal blood flow, inhibit renin and aldosterone release, Reduce sympathetic activity and antihypertrophic effect
27
Q
A

Pre-reg exam (113 decks)

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