Ventricular premature beats (VPBs), or premature ventricular complexes/contractions (PVCs), are ectopic beats that arise from within the ventricles. They are common and can occur in a wide variety of clinical scenarios and a diverse population. They can present in patients both with and without preexisting cardiac disease.[1] Reports show that frequent VPBs can cause progressive left ventricular (LV) dysfunction and dilation, which may return to normal after successful catheter ablation of the VPBs.[2][3]
The morphology of VPBs is highly variable, and it depends upon its place of origin, underlying structural disease, or the use of antiarrhythmic drugs. The VPBs usually originate from the ventricle that leads to a prolonged ORS complex duration greater than 120 ms because of the delay in the spread of activation to the contralateral ventricle through non-specialized myocardium. However, in certain instances, a QRS complex of duration less than 120 ms can occur, leading to activation of both ventricles "synchronously" because of electrical stimulus from one of the fascicles through a specific conduction system.[4]
Premature ventricular contractions classify according to coupling interval (early and delayed), QRS duration (wide and narrow), morphology, and complexity. The 12-lead EKG helps to identify the precise location of the origin of VPBs only by the morphology of ectopic beats. Those VPBs that originates in the left ventricle are usually associated with a right bundle branch block (RBBB), and VPBs that arise in the right ventricle show a left bundle branch block (LBBB) pattern.
A patient presenting with ventricular premature beats usually complains of palpitations. A thorough history and examination can help identify the etiological cause of VPBs. Several risk factors or potential causes can lead to frequent VPBs. Benignly occurring ventricular premature beats are usually due to excessive adrenergic stimulation. Other factors include various medications, electrolyte abnormalities, hypoxia, etc. The following describes several specific etiological causes:
Researchers conducted a study in a healthy military population with a recording of 12-lead EKG that showed almost 0.8% of subjects with VPBs with a 0.5% prevalence in the population under the age of 20 years and in those over the age of 50 years it was found to be 2.2%.[5] According to the Framingham Heart Study, the prevalence of VPBs was found to be higher than one VPBs in one hour continuous EKG monitoring with 33% being the men and 32% women with no history of any coronary artery disease. Those patients with coronary artery disease, the prevalence was comparatively higher, with 58% in men and women 49%.[6] The variability in the reported data differs due to the different monitoring techniques and duration used to calculate VPBs prevalence. Several factors are involved in this diversity, including coronary heart disease, African-American ethnicity, male gender, older age, hypertension, faster sinus rates, lower serum potassium or magnesium levels, and lower education level.[7]
The pathophysiological mechanisms for VPBs include enhanced automaticity, re-entry, and triggered activity. The enhanced automaticity characteristically results from an ectopic ventricular focus that fires spontaneously. A variety of stimuli, including myocardial ischemia, electrolyte imbalance, and heightened adrenergic state, can cause enhanced automaticity. An impulse can trigger the premature ventricular ectopics during the early-depolarization phase due to exceeding the cell membrane activation threshold. The VPBs associated with bradycardia is often caused by this mechanism, along with other factors like electrolyte abnormalities, ischemia, and digoxin toxicity. The re-entry mechanism leading to VPBs occurs typically in the areas of scarring or ischemia.
Most often, VPBs are asymptomatic. However, some patients will report fatigue, palpitations, lightheadedness, or dizziness. In patients with pre-existing heart disease, frequent VPBs can cause dyspnea, angina, and palpitations. Patients may often report a sense of abnormal neck pulsation with palpitations when they experience VPBs. VPBs rarely may cause hemodynamic compromise leading to presyncope or syncope, mainly if they occur in sustained or frequent runs. In asymptomatic individuals, VPBs may be initially identified on a routine physical exam by an irregular rhythm consisting of a premature beat followed by a compensatory pause with subsequent return of regular rhythm, or cardiac auscultation revealing a sharp first heart sound or splitting of S2 or on a routine office electrocardiogram.
In some cases, VPB is the first manifestation of underlying structural heart disease. For this reason, in all patients with VPBs, one must perform a detailed clinical history of 12-lead EKG and chest X-ray. The indication for further evaluation by Holter-monitoring, stress test, or echocardiogram, depends on whether VPBs persist after the initial assessment of suspected structural heart disease or the onset of complex forms of ventricular arrhythmias.
For over 20 years, the accepted view is that the presence of VPBs in the absence of structural heart disease presents a favorable, benign prognosis, even when they arise frequently. Therefore treatment strategies of VPBs are planned according to the frequency of occurrence and symptoms. In some of the cases, very frequent VPBs can produce cardiomyopathy, being an indication for treatment, even in the absence of symptoms. However, the clinical importance of frequent VPBs in patients without any left ventricular dysfunction is still unclear.
Initial workup should start with a resting EKG. The ventricular premature beat (VPB) is defined electrocardiographically as a premature QRS complex that has an abnormal morphology and duration greater than 120 milliseconds. A large T-wave classically follows it with discordant deflection (opposite polarity) from the QRS complex. There are typically no preceding P waves; however, often, the impulse generated from the VPB can be propagated in a retrograde fashion to the atria and can cause a classic compensatory pause following the VPB. This pause is due to the atrioventricular (AV) nodal blockade due to depolarization from the retrograde impulse and subsequent refractory period of the AV node. Though the sinus node fires at the appropriate time, its impulse is not propagated, as the AV node has been rendered refractory, thus causing an R-R interval that is precisely double the intrinsic R-R interval.
Usually, a VPB is followed by a full compensatory pause because the sinus node timing is not interrupted; one sinus P-wave is not able to reach the ventricles because they are still refractory from the VPB; the following sinus impulse thus occurs on time based on the sinus rate. In contrast, premature atrial contractions (PACs) are usually associated with an incomplete pause because the PAC usually enters the SA node and resets its timing, which enables the following sinus impulse to appear earlier than expected. Not all PVCs, however, get followed by a pause. If a VPB occurs early enough, especially with prolonged heart rates, it may appear sandwiched between the two normal heartbeats. This phenomenon is called an 'interpolated PVC.' The sinus impulse following the VPB is conducted with a longer PR interval because of the retrograde concealed conduction by the premature ventricular impulse into the AV-node junction, slowing the subsequent conduction of the sinus impulse.
The morphology of the QRS complex can be a means to determine the origin of the ventricular premature beat. Left and right ventricular outflow tracts are the most common sites of origin of VPBs and account for approximately two-thirds of all VPBs. The electrocardiographic morphology can similarly determine the ectopic origin of the source of ventricular tachycardia. VPBs with the morphology of a typical left bundle branch block (LBBB) and an inferior axis originating from the right ventricular outflow tract, while VPBs with the morphology of a standard right bundle branch block (RBBB) and an inferior axis originate from the left ventricular outflow tract. VPBs can originate from numerous other locations such as the ventricular free wall, ventricular septum, aortic cusp, tricuspid or mitral annuli, pulmonary artery, fascicles, or papillary muscles. Individuals with multiple abnormal QRS complexes classify as having multifocal VPBs, which are more common than unifocal VPBs. VPBs are also definable by the pattern in which they occur relative to intrinsic beats. Bigeminy indicates a VPB following a single, standard QRS complex, whereas trigeminy indicates a VPB following two normal QRS complexes. Multiple successive VPBs also have a distinct annotation; two VPBs successively is a couplet, three VPBs successively is a triplet, and more than three successive VPBs classify as a run of VPBs or ventricular tachycardia. When there are more than three consecutive VPBs, the term used is non-sustained ventricular tachycardia, and the term sustained VT is when the duration lasts more than 30 seconds. Couplets can be further defined by the interval between the ectopic, ventricular premature beat, and the subsequent usually conducted beat from the SA node. When the interval between the VPB and a regular beat is stable, it is called fixed coupling. Variable coupling is when these intervals change from beat to beat. VPBs are considered "frequent" if they occur more significant than 30 times per hour or greater than 20% of total heartbeats.
In addition to a resting EKG, the clinician should obtain ambulatory EKG monitoring for a minimum of 24-hours with a device such as a Holter monitor. If patients are particularly symptomatic, and the initial 24-hour monitoring is unrevealing, an event recorder or loop recorder can provide prolonged monitoring. It is also reasonable to evaluate for underlying electrolytes abnormality, with specific attention to serum potassium and magnesium levels. Additional laboratory evaluation with urine drug screen, TSH level, cardiac biomarkers (troponin), and serum digoxin level merit consideration when indicated. In most patients, especially those who are symptomatic, evaluation with transthoracic echocardiogram should be considered to evaluate for underlying structural cardiac abnormalities. Further evaluation with exercise/chemical stress testing, nuclear myocardial perfusion imaging, coronary angiography, and cardiac magnetic resonance imaging (MRI), should also be considered on a case-by-case basis for each patient.
Patients with ventricular premature beats in the setting of underlying structural heart disease should receive guideline-directed medical therapy (GDMT) as indicated in their specific disease process. Treatment is a consideration in patients who are symptomatic with a high burden of ectopic beats or who have frequent episodes of nonsustained ventricular tachycardia. Most notably, VPCs that transform into ventricular fibrillation (usually mediated by R-on-T phenomenon) should receive immediate defibrillation. If treatment is indicated, beta-blockers are typically first-line therapy. Catecholamine-sensitive or exercise-induced VPBs have an excellent response to the initiation of beta-blocker therapy. VPBs in the setting of CHF or myocardial infarction should be treated with beta-blockers as first-line therapy, as directed by GDMT.
Similarly, non-dihydropyridine calcium channel blockers can be a consideration in patients with a contraindication for beta-blockers. Patients can start antiarrhythmic treatment with class Ic agents (flecainide or propafenone) when their symptoms have not improved after initiation of beta-blocker or calcium channel blocker therapy. However, these agents are proarrhythmic, increase mortality, and are contraindicated in patients with pre-existing coronary artery disease. For this specific patient population, amiodarone has proven to be effective in suppressing VPBs; however, due to side effect profile, the administration should generally be reserved under close clinical monitoring for patients with underlying structural heart disease or coronary disease and significant symptomatology.
Patients who cannot tolerate the therapy, as mentioned earlier, should be referred to an electrophysiologist for consideration of ablation. VPB ablation is also the recommended intervention in patients who develop VPB-induced cardiomyopathy, especially in those with a significant VPB burden.[8] The definition of high VPB burden is greater than 10000 ectopic ventricular beats or greater than 10% of all beats recorded on 24-hour ambulatory monitoring.
The accepted thinking is that cardiomyopathy is more likely in patients whose ventricular premature beats have a very wide QRS complex, the beats arise from the epicardium, or in patients with VPBs occurring higher than a quarter of all beats on 24-hour Holter monitor (VPB burden of over 25%). This cardiomyopathy is generally considered to be reversible after ablation; however, some degree of left ventricular systolic dysfunction may rarely persist after the ablation of the ectopic focus.[9] Patients who have already developed cardiomyopathy due to high-frequency VPBs should also have a referral for radiofrequency ablation, as evidenced by a 2014 meta-analysis demonstrating that catheter ablation of VPBs originating from the RVOT significantly reduced ventricular ectopy burden and improved left ventricular ejection fraction. Ablation may also be indicated in patients with frequent VPBs that interfere with cardiac resynchronization therapy.[10]
Several cardiology societies have provided guidelines on the utilization of ablations for patients with VPBs. The 2019 AHA/ACC/HRS Guideline for Management of Patients with Ventricular Arrhythmia and the Prevention of Sudden Cardiac Death recommends that catheter ablation may be useful for patients with reduced left ventricular ejection fraction suspected to have been caused by frequent VPBs (defined as more than 15 percent of all beats) who failed to respond or could not tolerate antiarrhythmic medications.[11] The 2015 European Society of Cardiology Guidelines recommends considering ablation therapy for patients with reduced left ventricular ejection fraction and frequent symptomatic VPBs or nonsustained ventricular tachycardia.[12] Additionally, the European Heart Rhythm Association/Heart Failure Association recommends that patients with heart failure with reduced ejection fraction and a high burden of VPBs, defined as greater than 10000 VPBs/24 hours, should be aggressively treated with catheter ablation if they have failed, declined, or are intolerant to antiarrhythmic therapy (especially if there is a single dominant VPB morphology).[13]
Differentiating VPBs from other arrhythmias can be challenging, because several arrhythmias may mimic VPBs, as listed below;
In almost all heart diseases, due to the high incidence and complexity, VPBs can be the major cause of mortality in coronary artery disease and dilated cardiomyopathy. According to the MRIFT and Framingham Heart Study, frequent occurrence of VPBs correlates with an increased risk of sudden cardiac death.[14][15]. As these studies lack the diligent measures taken to investigate underlying heart disease, they are under great criticism because they can halve the death outcome.
The benign premature ventricular contractions that occur occasionally do not interfere with the average lifespan, but their frequent occurrence implies an ominous prognosis. The patients post-MI with frequent VPBs are prone to sudden cardiac death. However, patients treated either with medication or catheter ablation therapy can improve and recover from the LV dysfunction.[3]
The characteristics of VPBs that confer poor prognosis include:
Frequent VPBs are often associated with complications if remained unattended, which include;
Cardiac rehabilitation comprises of comprehensive long-term and short term goals. The long term goals focus on medical evaluation, cardiovascular risk assessment, health education, lifestyle modification, regular exercise motivation, counseling, and behavioral therapy. These goals alter the natural history of cardiac disease associated with VPBs and stabilize and reverse the progression of LV dysfunction and reduce the risk of sudden cardiac death. The short term goals consist of controlling the cardiac symptoms, limiting the physiological and psychological effects of cardiac illness, improving functional capacity, and boosting the vocational and psychosocial status.[16][17]
The cardiac rehabilitation improves the patients' outcome through improving the quality of life, increasing the patient's perception of physical development and motivation, altering risk factors, adjusting the interpersonal roles, and potentially advancing at work.
Patients with VPBs usually require consultation with a general physician, cardiologist, interventional cardiologist, and cardiac electrophysiologist.
Patients presenting to family physicians with symptoms like palpitations or skipped beats require detailed assessment. Although various cardiac etiologies can cause palpitations, their association with non-cardiac causes like anemia, fever, or drug use or even anxiety in otherwise healthy individuals should also remain in view. Reassurance and lifestyle modification is the mainstay of management in benign occurring VPBs. The patients should also undergo screening for anxiety or panic disorder with the help of a questionnaire. Education of patients about when to seek advice in case of a worsening of symptoms is essential. With the help of an interdisciplinary approach, patients will have the chance to interact with multiple members of the patient care team. Relaying changes in the regimen to the patients is a vital aspect of educating the patients. It should be emphasized to keep a scheduled follow-up of the appointments. If warranted, patients should receive counsel and education regarding the benefits of quitting smoking and losing weight. With the help of written pamphlets or illustrations, patient education should be to enhance the patient's learning.
The general population with frequent VPBs defined as the presence of at least one VPB on a 12-lead EKG or greater than 30 VPBs per hour is usually associated with increased cardiovascular risk and mortality. The cardiac MRI and methods used to suppress the VPBs aid in reversing the LV dysfunction. Therefore, differentiation of primary cardiomyopathy from VPB-mediated LV dysfunction is of prime importance.[18]
A detailed cardiovascular risk assessment and management is necessary for the clinical finding of VPBs on EKG of even healthy patients.[19] A poor prognosis associated with cardiac pathology caused by VPBs can be altered simply by early prevention and prompt treatment. The patients should be subjected to long-term followup by continuous monitoring, especially in cases of arrhythmia or heart failure after they have undergone specific treatment or intervention.[20]
Healthcare providers from different specialties, along with collaboration from the patient, constitute an interprofessional team that works in harmony and improves patient outcomes. It is a complex process, and it requires working together and sharing expertise, skills, and knowledge, all impacting patient care. Improvement in interprofessional teamwork tends to focus on specific activities like sharing of patient case-files, meeting style, frequency, or case-conferencing approach. Collaboration among health care professionals is a crucial component with trust and respect for oneself and others.[21] This interprofessional team includes a general physician, primary cardiologist, interventional cardiologist, radiologist, pharmacist, and cardiac electrophysiologist who work together to help focus on specific patient considerations and expectations.
Close communication between the interprofessional team members is vital for improved patient outcomes. [Level 5]
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