Left anterior fascicular block
Left anterior fascicular block (LAFB), also known as left anterior hemiblock, is a common cardiac conduction abnormality characterized by delayed or interrupted electrical impulse conduction through the left anterior fascicle of the left bundle branch, resulting in altered ventricular activation and left axis deviation on the electrocardiogram (ECG).[1][2]Pathophysiology
The left bundle branch divides into anterior and posterior fascicles, with the anterior fascicle being longer and thinner, making it more susceptible to conduction delays due to its anatomical course across the left ventricular outflow tract and reliance on a single blood supply.[2] In LAFB, impulses bypass the blocked anterior fascicle and travel via the posterior fascicle, causing initial activation of the posterobasal left ventricle followed by the anterolateral region, which can lead to mild mechanical dyssynchrony and potential systolic dysfunction if combined with other conduction issues.[2][3]Diagnosis
Diagnosis is primarily based on 12-lead ECG findings, including left axis deviation between -45° and -90°, normal or slightly prolonged QRS duration (typically <120 ms), qR pattern in lead aVL with a prolonged R-wave peak time (>45 ms), and rS complexes in leads II, III, and aVF.[3][4] These criteria distinguish LAFB from other causes of left axis deviation, such as left ventricular hypertrophy, though increased QRS voltage in limb leads may mimic hypertrophy without the typical strain pattern.[1][3]Causes and Epidemiology
LAFB often arises in the context of underlying structural heart disease, including coronary artery disease, myocardial infarction, hypertension, left ventricular hypertrophy, cardiomyopathies (dilated or hypertrophic), myocarditis, amyloidosis, and degenerative conduction system disease; it can also occur in healthy individuals or due to electrolyte imbalances like hyperkalemia.[4][2] It is the most common fascicular block, with a prevalence of about 1-2% in general populations and higher rates among those with cardiovascular risk factors, particularly in older adults.[5][4]Clinical Significance
Isolated LAFB is typically asymptomatic and considered benign, with no specific treatment required beyond managing underlying conditions;[1][4] however, it has a low risk of progression to higher-degree conduction blocks, with the 10-year incidence of complete atrioventricular block estimated at 0-2%.[6] While unadjusted analyses suggest associations with increased risks of atrial fibrillation, heart failure, and mortality, these links largely disappear after adjusting for age and sex, although a small increase in all-cause mortality persists (HR 1.14); LAFB is not a strong independent predictor of adverse cardiovascular outcomes.[5][2] More recent analyses (as of 2022) suggest potential links to increased non-cardiovascular mortality, warranting monitoring in high-risk patients.[7]Overview
Definition
Left anterior fascicular block (LAFB), also known as left anterior hemiblock, is a cardiac conduction abnormality characterized by delayed or blocked electrical impulses in the anterior division of the left bundle branch, resulting in delayed activation of the anterosuperior region of the left ventricle.[8] This disruption occurs within the specialized Purkinje fibers that facilitate rapid conduction to the left ventricular myocardium, leading to altered ventricular depolarization patterns.[9] The condition was first described in the 1960s by Marcelo B. Rosenbaum and colleagues, who identified it through clinical observations of axis shifts in patients with coronary artery disease, establishing the concept of hemiblocks as part of the trifascicular conduction system.[10][8] Unlike complete left bundle branch block (LBBB), which involves failure of the entire left bundle branch and results in transseptal activation from the right ventricle with significant QRS widening, LAFB affects only the anterior fascicle while preserving conduction through the posterior fascicle and potentially septal fibers.[8] This selective involvement allows for more efficient overall left ventricular activation compared to LBBB, maintaining relatively normal synchronous contraction in much of the ventricle.[9] The primary physiological impact of LAFB is a shift in the frontal plane QRS axis to the left, typically between -45° and -90°, due to the delayed superior activation vector dominating the initial depolarization.[8][3] Importantly, this occurs without substantial prolongation of the QRS duration, which remains less than 120 ms in isolated cases, distinguishing it from broader conduction delays.[3]Epidemiology
Left anterior fascicular block (LAFB) is a relatively common electrocardiographic finding in the general population, with prevalence estimates ranging from 0.9% to 6.2% across various studies.[11] In healthy cohorts, such as 8,915 individuals in Argentina, the prevalence was approximately 2.8%, while in 1,450 young Israeli pilots, it was 1.0%.[8] The condition occurs more frequently in males than females, with male predominance observed in multiple outpatient and population-based analyses.[12][13] Prevalence increases significantly with age due to degenerative changes in the cardiac conduction system, rising to 4-6% in individuals aged 60 years or older.[14] LAFB is strongly associated with hypertension, with up to 30% of affected individuals having comorbid hypertension in cardiology cohorts, and hypertension identified as a significant risk factor in population studies.[8][15] In hypertensive patients, LAFB contributes to intraventricular conduction disturbances, appearing as the most common type in up to 10% of such cases.[16] Geographic variations reflect differences in cardiovascular risk profiles and aging demographics, with slightly higher rates reported in Western populations compared to younger or lower-risk groups elsewhere; for instance, prevalence is elevated in regions with high hypertension and coronary disease burdens.[8]Pathophysiology
Conduction System Anatomy
The cardiac conduction system is a specialized network of cells responsible for generating and propagating electrical impulses to coordinate heart contractions. It begins at the sinoatrial (SA) node, located at the junction of the superior vena cava and the upper right atrium, which serves as the primary pacemaker initiating impulses at a rate of 60-100 beats per minute. These impulses travel through internodal pathways to the atrioventricular (AV) node, situated in the lower interatrial septum within the triangle of Koch, where conduction slows to allow atrial contraction completion before ventricular activation. From the AV node, the impulse proceeds via the bundle of His, penetrating the central fibrous body of the heart, and then bifurcates into the right bundle branch (RBB), which descends along the right interventricular septum to the right ventricular apex, and the left bundle branch (LBB), which spreads as a broad subendocardial sheet across the left interventricular septum.[17][18] The LBB further divides into the anterior and posterior fascicles, which are key components for left ventricular activation. The anterior fascicle is a thin, elongated structure, approximately 35 mm in length and 3 mm in diameter, positioned superficially and subendocardially along the anterosuperior left ventricular septum, extending to the base of the anterolateral papillary muscle and supplying the anterosuperior and high lateral walls of the left ventricle. In contrast, the posterior fascicle is shorter, thicker, and more robust, coursing posteroinferiorly along the septum to the base of the posteromedial papillary muscle, innervating the posteroinferior and inferior regions of the left ventricle. These fascicles consist of Purkinje fibers that fan out from the LBB trunk, which itself measures about 10 mm in length and transitions from a 5 mm diameter proximally to 9 mm distally, forming a reverse trapezoid shape as it adheres to the endocardial surface.[19][17][18] In normal impulse propagation, the electrical signal reaches the LBB after a brief delay at the AV node, then splits to the anterior and posterior fascicles, which conduct rapidly (up to six times faster than surrounding myocardium) to the Purkinje network. The anterior fascicle activates the anterolateral and high lateral left ventricular walls first, directing depolarization superiorly and to the left, while the posterior fascicle simultaneously depolarizes the inferior and posteroinferior walls, directing it inferiorly and to the right. This dual pathway ensures synchronous left ventricular contraction from endocardium to epicardium, starting at the apex and progressing upward, optimizing ejection efficiency. The anterior fascicle's delicate, elongated structure and subendocardial location, combined with its reliance on a single arterial supply from septal perforators of the left anterior descending coronary artery, render it more prone to injury from ischemia, fibrosis, or trauma compared to the posterior fascicle's dual blood supply and thicker composition.[18][17][19]Mechanism and Causes
The left anterior fascicular block (LAFB) arises from an interruption or delay in electrical conduction through the anterior division of the left bundle branch, which normally activates the anterosuperior regions of the left ventricle. When this fascicle is blocked, the electrical impulse is redirected primarily through the posterior fascicle and homolateral Purkinje fibers, resulting in delayed depolarization of the anterosuperior left ventricular myocardium. This shift causes the primary QRS vector to deviate superiorly and leftward, altering the sequence of ventricular activation without significantly prolonging the QRS duration (typically less than 0.02 seconds due to compensatory Purkinje conduction).[8] Pathophysiologically, LAFB develops through processes that damage or fibrose the specialized conduction fibers of the anterior fascicle, such as ischemia-induced necrosis, inflammatory infiltration, or degenerative fibrosis. Ischemia, often from occlusion in the proximal left anterior descending coronary artery, disrupts fascicular blood supply and leads to localized cell death, shifting activation away from the affected region. In degenerative cases, progressive fibrosis of the conduction system—termed Lenègre's disease—impairs impulse propagation through sclerotic changes in the fascicular tissue, particularly in older adults. Inflammatory conditions can similarly infiltrate and scar the fascicle, while mechanical stress from hypertension or valvular calcification (as in Lev's disease) contributes to fibrotic remodeling over time.[8][13][9] The primary etiologies of LAFB include coronary artery disease, accounting for approximately 18% of cases, often linked to anterior myocardial infarction that selectively affects the anterior fascicle's vascular territory. Hypertension is another leading cause, present in about 30% of patients, where chronic pressure overload promotes left ventricular hypertrophy and associated conduction system fibrosis. Aortic valve disease, particularly calcification encroaching on the conduction pathways, and cardiomyopathies (dilated or hypertrophic) contribute through mechanical distortion and myocardial remodeling. Degenerative processes like Lenègre's and Lev's diseases are prevalent in the elderly, representing idiopathic or calcific fibrosis of the His-Purkinje system.[8][9][13] Less common causes encompass congenital anomalies (rare, such as isolated fascicular hypoplasia), infections like Lyme carditis causing inflammatory block, direct trauma to the conduction system, or iatrogenic injury following cardiac surgery or catheter ablation. In many older adults, LAFB is multifactorial, combining ischemic, hypertensive, and degenerative elements.[8][20]Diagnosis
Electrocardiographic Criteria
The diagnosis of left anterior fascicular block (LAFB) relies on specific electrocardiographic (ECG) features that indicate delayed conduction through the anterior division of the left bundle branch, altering the initial ventricular depolarization vector. These criteria were originally proposed by Rosenbaum et al. in 1968 based on clinical and vectorcardiographic observations, with subsequent standardization by the American Heart Association in the 1970s through collaborative studies confirming their reliability.[9] The core ECG criteria for LAFB include:- Frontal plane QRS axis deviation: Between -45° and -90°, representing marked left axis deviation, which must be isolated or newly developed without alternative explanations such as left ventricular hypertrophy or inferior myocardial infarction.
- QRS morphology in limb leads: A qR pattern (small initial q wave followed by a dominant R wave) in leads I and aVL, reflecting early activation of the posterobasal left ventricle followed by delayed high lateral activation; conversely, an rS pattern (small initial r wave and deep S wave) in leads II, III, and aVF, with the S wave in III often deeper than in II.[9]
- QRS duration: Normal, less than 120 ms, to exclude broader intraventricular conduction delays.
- R-wave peak time in lead aVL: ≥ 45 ms, indicating prolongation of the intrinsicoid deflection due to the conduction delay.