Cardiac Rhythm problems Flashcards
Twin - died from ventricular fibrilation suddenly (Long QT syndrome)
-what are some questions we would want to know?
-want to know what she was doing before she died - because the different types of long QT can be triggered by different things
what is syncope
loss of tone and conciousness (faint)
What does loratadine do?
- antihistamine for nasal congestion
- can exasberate the QT elongation
- these can inhibit potassium channels, and can induce VT in people with LQT syndrome - K channels help with repolarisation however if you block these then will prolong the AP more
- increases risk of VT due to prolonged AP
Explain Long QT syndrome
- may be a problem with L type Caclium channles or sodium or potassium channels
- this can prolong the action potential, giving these channels time to reactivate and then they can become depolarisated again while the action potential is still occuring
- if this is big enough, it can depolarise ventricles early leading to a premature ventricular contraction
- However if some neighbouring cells are ready for a depolarisation, and some cells are not, then the wave of depolarisation can propgate through the cells that are ready and get blocked by the not ready cells, and then when those cells become ready, the wave can go around and depolarise those cells whcih can cause a re-entrant circuit which leads to reentrant tachycardia
- causes torstade de points
- can resolve, or can cause palpatations, syncope, dizziness, cardiac death
What can cause VT initiation when there is already a long QT interval
Drugs (amiodarone (prolongs AP by inhibiting potassium currents) , sotalol, antihistamine, …)
• Reduced extracellular potassium concentration (hypokalaemia – decreased [K+]o decreases IKr) (e.g vomiting, diuertics, diahorrhea)
• Potassium ion channel mutations which lead to reduced effectiveness of delayed rectifier IK : LQT1 [IKs] & LQT2 [IKr]
• Sodium ion channel mutations that affect inactivation of INa (LQT3)
Different types of QT syndrome and what they are triggered by
and what to avoid
- ong QT1 syndrome - often event occurs during exercise and stress
- long QT2 syndrome - when someone yells at you, load noises and stress
- long QT3 - person dies at night (sodium channel) - rest and sleep
- avoid these triggers
- history helps add to ECG
Why is it torstades de pointes
and what can happen
because there is no fixed anatomical substrate that the reentrant circuit is circulating around , the reentry is occurring within a region of functional block
- more unstable than monomorphic VT
- could resolved back to sinus rhythm or could progress to VF
What advice would you give someone with Long QT syndrome?
Prior cardiac events-beta blockers and a implatable cardioverter defibrillator
No prior events - beta blocker and lifestyle modificaiotsn
-E.g avoid triggers of cardiac events and medications (in slide above for specific QT syndromes)
How to describe monomorphic tachycardia on an ECG?
- ecg - monomorphic tachycardia, broad complex, regular
Why does patient have syncope, low BP and chest discomfort with VT
- heart not pumping as well due to VT, and not enough time to fill ventricles due to increase HR
- reduce CO, reduce BP - reduced perfusion to brain - syncope
- Chest discomfort - palpitations, imparied myocardial perfusion, pulmonary congestion due to poor LV pump
Why is there prolonged QRS complex?
QRS complexes are ectopic
- these originate somewhere in ventricle and spread, hence this is not using the fast conduction system so is a relatively slow process so has a wide QRS
- also has an abnormal QRS shape due to abnormal activation sequence
What are most common causes of the the arrhythmia (previous MI, and now has VT)
need a trigger, substrate, unidirection flow, AP length of ERP, circuit
-the circuit does not move and is resatabalised around or withint the region of the scar
How can you get an MI with current ischaemia
Slow conduction - low ATP, na/k ATPase reduced, NA/K gradients reduced, partial membrane depolarisation, inactivaiton of sodium channles, reduced gap junction coupling due to metabolic acidosis
AP duration shortened
-na/k atapase reduced, transmembrane potassium gradient reuced, hyperkalemia - shorteneds AP duration, - elad to inhomogenous electrical properties - can get regions of block and re-entry pathways
DADs - cannot pump calcium out of cell and into SR as well due to reduced ATP, leads delayed after depolarsiation
What do we do for person with VT?
- fibrilation
- low BP
- kidney
- dont want VF - want him in resuscitation area - can monitor and resusitate
- hypotension - treat rhythm disturbance to treat this
- troponin measurement
- kidney - give drugs if there is renal impairment (creatinine)
- defibrillate - sedate this person
- lifestyle behaviours- longterm care
- external defibrillator i drug deosnt help
- could do a left ventricular gram
- cut out anurysm of heart
- ablation of re-entrant circuits after percutaneous electrical mapping or implanation of an external defibrillator may be considered where VT is refractory to drug treatment
short term - stop rhythm distrubance, investigate other conditiosn (e.g kidney)
-long term - target and prevent arrhythmia
What features on an ecg are suggestive of an acute MI
ST segment elevation, T wave inversion
