![]() Contents Forward Modern-day ECG machines can make accurate measurements and analysis. So why bother to learn how to read an electrocardiogram? The answer is simple: A robotic machine can follow algorithms but it takes a human mind to read beyond and between the waveforms to make interpretation and collate it with clinical findings. Electrocardiography can be the topic of a lifelong study. This Primer is only meant to introduce the subject to medical students, interns, novice residents, and general physicians in community practice. It is hoped the liberal use of diagrams and pictures can help to improve understanding. DC Chung January 2008 Imagination is more important than knowledge. ![]() Albert Einstein Introduction Origin of the Heart Beat and Electrocardiogram Under physiological conditions, the sinoatrial (SA) node generates pacemaker impulses that spread to the right and left atria, converge on the atrioventricular (AV) node, and continue down the His bundle and bundle branches (right bundle branch or RBB and left bundle branch or LBB) to activate the ventricles. Depolarization is followed by repolarization and the sequence of depolarization [activation-and-contraction [repolarization repeats itself to generate rhythmical heart beats. Under abnormal conditions, ectopic foci in the atria, the AV junction, and the ventricles can usurp pacing dominance from this node and generate ectopic beats. The approach to supraventricular tachycardia (SVT) diagnosis can be complex because it involves. Change in the atrial activation sequence. The fact that an HRVPB can affect atrial timing indicates that an AP is present. If the atrial activation sequence is unaltered, one. Wider QRS complex and lengthening of the SH. Broad QRS complex tachycardias in the emergency. Causes of a Broad QRS Complex Tachycardia. Reversed activation sequence with left. Narrow complex tachycardia; Wide. Polymorphic ventricular tachycardia (top) and preexcited atrial. Color mapping of the electrical activation sequence. The wave of depolarization and repolarization described above can be mapped on the body surface by sensing electrodes placed on the extremities and the chest wall. The resultant waveform traced on graph paper is called the electrocardiogram (ECG). The ECG Graph Paper Horizontal axis of theECG graph paper represents time in milliseconds (ms) while the vertical axis represents amplitude or voltage in millivolts (mV). Each1-mm-division on the horizontal axis is 40 ms; each 5-mm-division is 200 ms. Two 5-mm-divisions on the vertical axis are calibrated to represent 1 mV. Despite the latter, ECG waves are commonly described by their height in mm rather than by their strength in mV. The ECG Leads The heart occupies a position in the center of the thorax anda 12-lead ECG is simply a recordingof the current flux of cardiac depolarization and repolarization obtained from 12 different sites on the body surface. There are six limb leads: Lead I records from the left at a coordinate of 0 o. Lead II records from the foot at a coordinate of 60 o. Lead III records from the foot at a coordinate of 120 o. Lead aVR records from the right shoulder at a coordinate of -150 o. Lead aVL records from the left shoulder at a coordinate of -30 o. Lead aVF recordsdirectly from the feet below at a coordinate of 90 o. There are also six chest leads with sensing electrodes positioned horizontally around the left anterior hemi-thorax between the 4 th and 5 th interspaces: Leads V1 and V2 record the current flux over the right ventricle directly. Leads V3 and V4 record directly the electrical activities of the ventricular septum and the anterior wall of the left ventricle. Leads V5 and V6 record the current flow generated by the left ventricle directly. In sinus rhythm when the SA node is the pacemaker, the mean direction of atrial depolarization (the P wave axis) points downward and to the left, in the general direction of lead II within a coordinate between 15 o and 75 o and away from lead aVR. On this count the P wave is always positive in lead II and always negative in lead aVR during sinus rhythm. Conversely, a P wave that is positive in lead II and negative in lead aVR indicates normal P wave axis and sinus rhythm. The QRS Complex The second wave is the QRS complex. Typically this complex has a series of 3 deflections that reflect the current associated with right and left ventricular depolarization. By convention the first deflection in the complex, if it is negative, is called a Q wave. The first positive deflection in the complex is called an R wave. A negative deflection after an R wave is called an S wave. A second positive deflection after the S wave, if there is one, is called the R ’ wave. Some QRS complexes do not have all three deflections. But irrespective of the number of waves present, they are all QRS complexes: A QRS complex with QRS deflections: A QRS complex with QR deflections: A QRS complex with RS deflections: A QRS complex with only an R wave: A QRS complex with RSR’ deflections: A QRS complex with a QS wave: (NB: The first wave of the last complex is a negative deflection. Therefore, it qualifies to be called a Q wave. Since all QRS complexes have an R wave, there must be one in this example as well, although it may be so small that it is not visible. A negative deflection following an R wave is an S wave. Hence this single negative deflection deserves to be called a QS wave.) QRS duration is the width of that complex from beginning to end, irrespective of the number of deflections present. Normally it lasts no more than 120 ms (three 1-mm-divisions). The normal QRS axis, like the P wave axis, points downward and to the left within a coordinate between -30 o and +90 o. This axis is said to be deviated to the left (left axis deviation or LAD) if it lies between -30 o and -90 o; and deviated to the right (right axis deviation or RAD) if it lies between +90 o and 180 o. It is either far right or far left axis deviation if it lies between 180 o and -90 o. The method of determining QRS axis will be explained in a later section. The ST Segment Following the QRS complex is the ST segment, extending from where the QRS ends (irrespective of what the last wave in the complex is) to where the T wave begins. The junction between the end of the QRS and the beginning of the ST segment is called the J point. ST segment reflects the current flow associated with phase 2 of ventricular repolarization. Since there is no current flow during this plateau phase of repolarization, the ST segment is normally isoelectric with the baseline. The T Wave The T wave represents the current of rapid phase 3 ventricular repolarization (see diagram above). The polarity of this wave normally follows that of the main QRS deflection in any lead. The ventricles are electrically unstable during that period of repolarization extending from the peak of the T wave to its initial downslope. A stimulus (e.g. A run away heart beat called a premature beat) falling on this vulnerable period has the potential to precipitate ventricular fibrillation: the so call R-on-T phenomenon. The PR Interval The PR interval extends from the beginning of the P wave to the beginning of the QRS, whatever the first wave of this complex may be. This interval measures the time from the initial depolarization of the atria to the initial depolarization of the ventricles and reflects a physiological delay in AV conduction imposed by the AV node. Normal range is 120 – 200 ms (3 to 5 1-mm-divisions) and no longer. The QT Interval The QT interval is measured from the beginning of the QRS to the end of the T wave. It represents the time in which the ventricles depolarize and repolarize and is a measure of ventricular action potential (AP) duration. This interval should be determined in the ECG lead where it is longest. Normal intervals are 120 ms) and has a shape different from that of the sinus beat. If the ventricular escape rhythm is the result of sinus node failure, no P wave of atrial contraction is seen as in the tracing above. If the ventricular escape rhythm is the result of 3 rd degree (complete) heart block, the sinus node paces the atria independently and regular P waves unrelated to the ventricular escape beats can be seen. The inherent rate of ventricular escape rhythm is between 20 and 40 beats/min. Premature Beats A premature beat also arises from an ectopic pacemaker: in the atria, the AV junction, or the ventricles. The non-sinus impulse is early, initiating a heart beat before the next anticipated sinus beat as its name implies. The reason the ectopic focus discharges a pacing impulse early in this instance is because the ectopic focus is irritable and competes with the sinus node. Atrial Premature Beat Atrial premature beat (APB) arises from an irritable focus in one of the atria. It depolarizes the atria prematurely (premature to the next timely sinus beat) and produces a P wave that looks different from a sinus-node generated P wave because the direction in which the atria depolarize is abnormal (abnormal P wave axis). Since the premature atrial impulse is conducted in a normal fashion via the AV node, the His bundle, and the bundle branches to depolarize the ventricles, the QRS complex associated with an APB has normal QRS duration and the same morphology as that of the sinus beat. Junctional Premature Beat Junctional premature beat (JPB) arises from an irritable focus at the AV junction. The P wave associated with atrial depolarization in this instance is usually buried inside the QRS complex and not visible (see “Junctional Escape ” above). However, the P wave may appear on occasions either immediately before or immediately after the QRS complex. When it is visible, the P wave is negative in lead II and positive in lead aVR because of retrograde atrial depolarization. Since the premature junctional impulse is conducted in a normal fashion down the His bundle and bundle branches to depolarize the ventricles, the QRS associated with JPB has normal duration and the same morphology as that of the sinus-node generated beat. Ventricular Premature Beat Ventricular premature beat arises from an irritable focus in the ventricles. Ventricular premature impulse is not transmitted to the rest of the ventricles along the His bundle and bundle branches. It is conducted along abnormal pathway in the ventricular myocardium. This slow process produces an abnormally wide QRS and bizarre looking T wave. Being a ventricle-generated beat, there is no P wave activity before the QRS complex. Tachycardias If an ectopic focus discharges a premature impulse only occasionally, the result is premature beats superimposed on the basic rhythm; if the irritable focus generates 3 premature beat repeatedly in a continuous sequence, the result is ectopic tachycardia. The run is called non-sustained if it lasts up to 30 seconds and sustained if longer than 30 seconds. Tachycardias, other than sinus tachycardia, can be classified into supraventricular tachycardia (SVT) or ventricular tachycardia (VT), depending on their site of origin. Supraventricular Tachycardia Tachycardias arising from an ectopic focus in the atria or AV junction are called supraventricular tachycardias (SVT). Heart rate is faster than 150 per minute and commonly around 180 per minute. At this very fast heart rate, the P waves of atrial contraction are buried within the waves of the beats before irrespective of whether the tachycardia is of atrial or junctional origin. Differentiation of the two is not possible on the surface ECG and they are simply called paroxysmal supraventricular tachycardia (PSVT) because of their paroxysmal (sudden) onset. Since PSVT impulses depolarize the ventricles by passing down the His bundle and bundle branches, the accompanying QRS complexes are of normal width and have the same morphology as that of sinus beats. Atrial Flutter In atrial flutter an atrial focus activates the atria at a rate of around 300 times per minute. The baseline of the ECG becomes all P waves, giving it a “saw tooth ” appearance in one or more leads. Since it is unusual for the AV node to conduct impulses at a rate faster than 200 per minute, AV block occurs: commonly at a 2 to 1, 3 to 1, or 4 to 1 ratio, yielding a ventricular response rate of 150, 100, or 75 per minute respectively. (NB: When the ratio of P waves to QRS complex is 2:1, 3:1, or 4:1 it would be more correct to use the term 2:1, 3:1, or 4:1 conduction rather than block. To avoid confusion, some authors simply use the term 2:1, 3:1, or 4:1 flutter.) Since the atrial flutter impulses depolarize the ventricles by passing down the His bundle and bundle branches, the accompanying QRS complexes are normal in width and have the same morphology as that of sinus beats. Atrial Fibrillation Atrial fibrillation is one of the most common arrhythmias in which multiple foci in the atria depolarize rapidly and erratically at a combined rate of 400 times/min or more. Instead of generating well recognized P waves, the atria just quiver and produce fine f waves on the ECG baseline seen in one or more leads. The AV node is constantly bombarded by depolarization impulses but only some of these impulses manage to get through. The ventricular response is totally irregular without discernible pattern (irregularly irregular) generally at a rate between 110 and 180 beats/min. Since impulses that manage to pass through the AV node are conducted down the His Bundle and bundle branches, the ventricles are activated normally and their QRS complexes are normal in width and have the same morphology as that of sinus beats. Monomorphic Ventricular Tachycardia Ventricular tachycardia (VT) arises from an irritable ventricular focus that discharges premature impulses for 3 or more beats without interruption. The rate of depolarization is 150/min or faster. Since these impulses are conducted to the rest of the ventricles via abnormal pathway in the ventricular myocardium and not via the His Bundle and bundle branches, the QRS complexes are broader than normal and without distinguishable T waves. In monomorphic VT, consecutive QRS complexes have the same appearance. Polymorphic Ventricular Tachycardia In polymorphic ventricular tachycardia, there is beat-to-beat variation in the QRS morphology. A common example is Torsades de Pointes (twisting of the points) shown below: Ventricular Fibrillation Ventricular fibrillation occurs when multiple ventricular foci discharge rapidly and chaotically. The ventricles twitch asynchronously and are not effective as pumps. No organized QRS complexes are seen —just disorganized oscillatory waves which can be coarse (as shown) or fine in appearance. Heart Blocks Heart block refers to a pathological delay in AV conduction, either at the AV node or beyond. Signs of heart block lie in the PR interval and P to QRS relationship. First Degree Heart Block In first degree heart block the cardiac rhythm is sinus in origin but the time from the initial depolarization of the atria to the initial depolarization of the ventricles is abnormally delayed. This pathologic delay is reflected in a PR interval longer than its upper limit of 200 ms. Nevertheless, each P wave of atrial contraction is followed by a QRS complex of ventricular contraction. Second Degree Heart Block When transmission of the depolarizing impulse from the sinus node through the AV conduction system of the heart is interrupted intermittently, P wave of atrial contraction is no longer followed by a QRS complex of ventricular contraction in the interrupted beat. This is second degree heart block. There are 2 types of second degree heart block: Mobitz type I & Mobitz type II. In Mobitz type I block there is progressive prolongation of the PR interval, indicating increasing delay in AV conduction, before it fails altogether. When failure in AV conduction occurs, the P wave of atrial contraction is not followed by a QRS complex. After this missed ventricular beat, the PR interval returns to its shorter duration and the cycle of progressive PR prolongation and missed ventricular beat repeats itself. In Mobitz Type II block, a non-conducted P wave not followed by a QRS complex occurs suddenly without progressive prolongation of the PR interval. That is, the PR interval, which can be normal or prolonged, is constant before the non-conducted beat materializes. Mobitz t ype II second degree heart block indicates more serious disease of the conduction system in regions below the AV node and can progress to total failure of AV conduction (third degree heart block) without warning. Third D egree H eart B lock In third degree (complete) heart block, all the SA node impulses are blocked and not conducted to the ventricles. In the absence of an alternative pacemaker, ventricular contraction comes to a standstill and the patient dies. But most probably an ectopic pacemaker below the block takes over ventricular pacing and the patient survives. Since the SA node and the ectopic pacemaker pace the atria and ventricles independently, the P waves bear no relationship to the QRS complexes. Two types of QRS complexes can be seen in third degree heart block: If the block is high in the AV node and the ventricular pacemaker is located lower in the AV junction, the QRS complex is normal in width because ventricular activation is via the bundle branches. If the block is low in the AV junction, the ventricles are paced by an idioventricular pacemaker and the QRS complexes will be wide rthan normal because the ventricles are no longer activated via the bundle branches. Bundle Branch Block This topic is covered in a later section. QRS Axis There are many ways to determine QRS axis. The one described below combines simplicity and efficiency. The limits of normal and abnormal QRS axis are summarized in the diagram to the right. QRS axis is the direction in which the mean QRS current flows. The normal axis points mostly downward and to the left because the more muscular left ventricle generates a stronger depolarizing current that overwhelms that generated by the less bulky right. Although both right axis deviation (RAD) and left axis deviation (LAD) are not necessarily associated with organic heart disease, they are seen in a number of settings and their presence can provide added evidence to support a clinical diagnosis. RAD is seen in right ventricular (RV) hypertrophy and in infarction involving the left ventricle ( LV). Right ventricular muscle bulk is relatively larger than that of the left in both conditions and generates a stronger depolarizing current in its direction. LAD is seen, but not always, in patients with left ventricular hypertrophy. More commonly the QRS axis is horizontal in this condition. It is only necessary to examine the QRS complexes in leads I and II to determine whether the QRS axis in normal or deviated to the left or the right; a precise calculation of the QRS axis is not required in clinical interpretation of the ECG. It has been explained in a previous section that a current flowing in the direction of a recording electrode (an ECG lead) registers a positive deflection and a current flowing away registers a negative deflection. Therefore, the QRS in lead I would be positive if the QRS current flows in the direction of lead I and negative if away. Similarly the QRS in lead II would be positive if the QRS axis points in the direction of lead II and negative if away. By overlapping the two circles representing leads I and II, it can be seen that the QRS axis is between +90 o and -30 o and normal if the QRS is positive both in lead I and lead II. QRS axis is between -30 o and -90 o or deviated to the left (left axis deviation or LAD) if the QRS is positive in lead I but negative in lead II. QRS axis is between +90 o and +150 o or deviated to the right (right axis deviation or RAD) if the QRS is negative in lead I but positive in lead II. On occasions the QRS complexes in all 6 limb leads are biphasic, neither positive nor negative. In these instances the QRS axis is said to be indeterminate. In summary: Normal QRS axis. Left axis deviation Right axis deviation Right and Left Atrial Abnormalities (NB: “Atrial abnormality” is a term being used increasingly in place of “atrial enlargement ”, “atrial dilatation ” or “atrial hypertrophy ”.) Look for signs of atrial abnormalities in leads in which the P wave is most prominent: usually lead II, but also leads III, aVF, and V1. In sinus rhythm the right atrial depolarization wave (brown) precedes that of the left atrium (blue) and the combined depolarization waves, the P wave, is less than 120 ms wide and less than 2.5 mm high. In right atrial abnormality, right atrial depolarization lasts longer than normal and its wave extends to the end of left atrial depolarization. Although the amplitude of the right atrial depolarization current remains unchanged, its peak now falls on top of that of the left atrial depolarization wave. As a result, the combined waves of right and left atrial depolarization, the P wave, is taller than normal (taller than 2.5 mm) but its width remains within 120 ms. In left atrial abnormality left atrial depolarization lasts longer than normal but its amplitude remains unchanged. Therefore, the height of the resultant P wave remains within normal limits but its duration is longer than120 ms. A notch (broken line) near its peak may or may not be present. A biphasic P wave in V1 is another sign suggesting atrial abnormality. In right atrial abnormality, the initial positive portion of the biphasic P wave is larger than the terminal negative portion. A biphasic P wave in V1, with its terminal negative deflection more than 40 ms wide and more than 1 mm deep is another ECG sign of left atrial abnormality. Right and Left Ventricular Hypertrophy Look for signs of right and left ventricular hypertrophy in the right chest leads (V1 and V2) and left chest leads (V5 and V6). When the ventricles are normal, the QRS complexes across the chest leads of an ECG have these configurations: In right chest leads V1 and V2, the QRS complexes are predominantly negative with small R waves and relatively deep S waves because the more muscular left ventricle produces depolarization current flowing away from these leads. In left chest leads V5 and V6, the QRS complexes are predominantly positive with tall R waves because the more muscular left ventricle produces net current flowing towards these leads. The QRS complexes in V3 and V4 reflect a transition between the right and left chest leads. The normal transition zone, where the R wave and S wave are equal, is between V3 and V4. Early transition may appear in V2 while late transition may not appear until V5 or V6. In right ventricular hypertrophy (RVH), the configurations of the QRS complexes across the chest leads are changed: In V1 the QRS are positive with tall R waves. This is because increased right ventricular muscle mass causes the net ventricular depolarization current to move toward s this right chest lead. R wavesthat are taller than S waves are deep in V1 are highly suggestive of RVH. The S waves are unusually deep in V6 and may be even deeper than the R wave is tall. Other ECG signs of RVH include: Right axis deviation due to the overpowering current generated by a hypertrophied right ventricle. Ventricular repolarization changes manifest as downward sloping of the ST segment and T wave inversion, the so called ventricular strain pattern, may or may not be present in the right chest leads. (See V1 in above ECG.) P wave > 2.5 mm tall in lead II, III, aVF or biphasic P wave in V1 suggesting the presence of right atrial enlargement. (Right atrial abnormality results from the right atrium having to pump blood into a thick-wall non-compliant hypertrophied right ventricle.) In left ventricular hypertrophy (LVH), the configurations of the QRS complexes across the chest leads are also changed and consist of: Unusually tall R wave in left chest leads V5 and V6 and unusually prominent S wave in right chest leads V1 and V2. These are exaggerations of the normal configurations due to increase in left ventricular muscle mass. The sum of the S wave in V1 and the R wave in V5 or V6 is > 35 mm. (Tall R waves in chest leads is common among young and slender individuals. This finding alone should not be used as the only criteria of LVH.) Additional ECG signs of LVH include: R waves taller than 14 mm in lead I or taller than 11 mm in Lead a VL. However, tall R waves in limb leads and chest leads do not always coexist. Left axis deviation may or may not be present. Repolarization abnormalities of ST segment depression and T wave inversion suggesting ventricular strain may be present in the left chest leads with tall R waves. (See leads V5 and V6 in above ECG.) Signs of left atrial enlargement in leads II, III, a VF or V1 may be present. Left atrial abnormality is the result of having to pump blood into a muscular non-compliant left ventricle. Bundle Branch Blocks Look for signs of bundle branch block (BBB) in V1 and V6. In the absence of BBB, passage of the depolarizing impulse down the His bundle and bundle branches is rapid and activation of the right and left ventricles is simultaneous and synchronous. The individual QRS complexes of the right and the left ventricles superimpose on each other and produce a composite QRS complex that is narrow in width ( 120 ms wide and has RSR ’ waves: the R wave belongs to the individual QRS of the not-blocked ventricle and the R ’ wave to the individual QRS of the blocked ventricle. The S wave between the R and R ’ waves may be deep and falls below the baseline; it may not be so deep and causes a notch between the R and R ’ waves only; or it may be hardly visible such that the QRS complex is simply a tall and wide R wave. In right bundle branch block (RBBB), the widened RR ’ complex is seen most typically in V1. Secondary T wave inversion can also be seen in this lead because when depolarization is abnormal repolarization can also be expected to be abnormal. Since the late right ventricular depolarization current moves away from left chest leads, it shows up as wide S waves in V6. When there is an RR ’ complex in V1 but it is less than 120 ms wide, the condition is called incomplete right bundle branch block. In left bundle branch block (LBBB) the widened RR ’ complex is seen most typically in V6. Secondary T wave inversion is present in the left but not right chest leads. Since the late left ventricular depolarization current moves away from the right chest leads, it shows up as deep and broad S waves in V1. Bundle branch block or ventricular rhythm? The QRS complexes are wider than normal in both BBB and ventricular rhythm. But the rhythm in BBB is supraventricular in origin. There is a one-to-one P wave to QRS relationship in BBB: In sinus rhythm with 3 rd degree heart block, there are regular P waves that are totally asynchronous with the QRS complexes, which represent escape rhythm from a ventricular focus. In ventricular rhythm with sinus arrest, only wide QRS complexes are seen and P waves are absent. Acute Myocardial Infarction Acute myocardial infarction (MI) affects both ventricular depolarization (appearance of pathological Q waves) and repolarization (ST-T wave changes). Specific manifestations depend on whether the lesion is subendocardial or transmural in location. The ECG sign of subendocardial ischemia is ST segment depression (A). Depression is reversible if ischemia is only transient but depression persists if ischemia is severe enough to produce infarction. T wave inversion with or without ST segment depression (B) is sometimes seen but not ST segment elevation or Q wave. That is why subendocardial infarction is also called non-ST-elevation myocardial infarction (NSTEMI) and less commonly non-Q wave myocardial infarction. ST segment depression seen in subendocardial ischemia or infarction can take on different patterns: The most typical being horizontal or down-sloping depression. Up-sloping ST depression is less specific. In exercise stress tests, horizontal or down-sloping depression of 1 mm or more (A, B, & C) or up-sloping depression of the same magnitude 80 ms beyond the J point (D) is considered positive signs of ischemia. Up-sloping depression of less than 1 mm at 80 ms beyond the J point (E) is simply J point depression and not ST segment depression. In transmural MI, ischemia in the subendocardium spreads to the epicardium and involves full thickness of the myocardium. In the acute phase, the ECG signs are ST segment elevation. The elevated ST segment may slope upward or be horizontal or dome-shape. Hyperacute (tall positive) T waves may precede ST segment elevation (A) or seen at the same time with ST elevation (B) during this acute phase. Hours to days later during the evolving phase, pathological Q waves appear, the elevated ST segments return towards baseline, and the T waves become inverted. Q wave is normal if it is shallow and brief (A). Q wave is pathological if it is wider than 40 ms or deeper than a third of the height of the entire QRS complex (B & C). Significant Q wave usually persists even after recovery. Localization of myocardial infarction By way of their position, the 12 ECG leads can be used to distinguish myocardial infarction occurring in different regions of the heart. The chest leads cluster around the heart in the horizontal plane and look in from the front (V1 to V4) and from the left (V5 and V6); leads I and aVL also look in from the left while leads II, III, and aVF look in at the under surface. Signs of anterior MI (grey area), territory supplied by the left anterior descending coronary artery (LAD), are seen in V1 to V4. Signs of lateral MI (grey area), territory supplied by the left circumflex coronary artery (LC), are seen in leads I, aVL, V5 and V6. Signs of inferior MI (grey area), territory supplied by the right coronary artery (RCA), are seen in leads II, III, and aVF. Signs of posterior MI on a 12-lead ECG are not the characteristic ST elevation and Q waves, which would be the case if there is a lead recording from the patient ’s back. Since V1 and V2 are attached to the patient ’s front, they will record changes reciprocal to changes seen from the back, which are ST depression and tall R waves. These uncharacteristic signs make the diagnosis of posterior MI difficult without heightened vigilance. Suffice it to say, pure posterior wall infarctions are rare. Most extend to involve the inferior wall or lateral wall and leads II, III, and aVF should be examined for characteristic signs of this extension in the former and leads I, aVL, V5 and V6 in the latter. MI in the presence of LBBB The presence of LBBB complicates the ECG diagnosis of acute MI. This is because LBBB alone can produce signs that may be confused with those of infarction: deep QS waves in the right chest leads and ST depression and T wave inversion in the left chest leads. Furthermore, the Q wave of left ventricular MI may be buried within the widened QRS complex. Therefore, the diagnosis of acute myocardial infarction should be made circumspectively in the presence of pre-existing LBBB. On the other hand, the appearance of new LBBB should be regarded as sign of acute MI until proven otherwise. Electrolyte Abnormalities Hyperkalemia and Hypokalemia Serum potassium is the major intracellular ion that participates in the depolarization and repolarization of myocardial cells. Hence its serum concentration has a profound effect on the QRS and ST-T complex. Narrow and tall peaked T wave (A) is an early sign of hyperkalemia. It is unusual for T waves to be taller than 5 mm in limb leads and taller than 10 mm in chest leads. Hyperkalemia should be suspect if these limits are exceeded in more than one lead. As serum potassium concentration continues to rise, the PR interval becomes longer, the P wave loses its amplitude and may disappear, and the QRS complex widens (B). When hyperkalemia is very severe, the widened QRS complexes merge with their corresponding T waves and the resultant ECG looks like a series of sine waves (C). If the rise in serum potassium continues unabated, the heart arrests in asystole. (NB: The narrow and tall peaked T wave of hyperkalemia may be confused with the hyper-acute T wave occasionally seen in transmural myocardial infarction. The patient ’s presenting history and physical findings would help to differentiate the two.) With hypokalemia, the T wave becomes flattened together with appearance of a prominent U wave. The ST segment may become depressed and the T wave inverted. Unlike hyperkalemia, these additional changes are not related to the degree of hypokalemia. Hypercalcemia and Hypocalcemia ECG signs of hypercalcemia and hypocalcemia may not be obvious even in patients who have deranged plasma calcium concentrations that are clinically significant. If they are present, hypercalcemia is associated with short QT interval (A) and hypocalcemia with long QT interval (B). Interval shortening or lengthening is mainly in the ST segment. Drug Effects Digoxin Digoxin is a potent pro-arrhythmic drug. At therapeutic plasma level, it causes nonspecific ST segment depression that has a scooping appearance (A) or looks like a reversed “ ̈” (B). (See Case 067: Abnormal ECG at At toxic levels, digoxin can cause virtually all kinds of arrhythmia but particularly sinus bradycardia, SA and AV blocks, atrial and junctional tachycardias, and VPB and ventricular tachycardia. Anti-arrhythmic Drugs Quinidine, procainamide, and disopyramide ( Class IA agents) prolong the QRS duration and the QT interval with or without the appearance of U wave and have the propensity to cause polymorphic ventricular tachycardia (torsade de pointes). Sotalol and amiodarone (Class III agents) can increase PR, QRS, and QT intervals, leading to similar risks of torsade de pointes. They also have significant beta-blocking properties, causing bradyarrhythmias. Pulmonary Embolism The classical ECG signs of acute pulmonary embolism are S IQ IIIT III, which are mnemonics representing deep S wave in lead I, pathological Q wave in lead III, and inverted T wave in lead III: Other nonspecific signs include (see ECG above): Sinus tachycardia and atrial and ventricular ectopic beats. Right axis deviation. Right ventricular strain pattern with inverted T waves in right chest leads. Incomplete or complete right bundle branch block pattern. Slow R wave progression in chest leads But all these ECG signs may not be present even in frank pulmonary embolism. The initial four QRS complexes have an atypical right bundle branch block morphology suggesting either ventricular tachycardia (VT) or a preexcited tachycardia. There is 1:1 AV relationship with the earliest atrial electrogram in the septum. In such a situation, the differential diagnosis includes VT with 1:1 VA conduction, atrial tachycardia or AV node reentry with anterograde conduction over an accessory pathway (AP), and antidromic tachycardia with anterograde conduction over an AP and retrograde conduction over either a second septal AP or the normal VA conduction system. An atrial stimulus (S2) introduced during tachycardia at the MCS electrode site terminates tachycardia without conduction to the ventricle. This eliminates VT as a diagnosis. Termination with a relatively late-coupled PAC also favors a macroreentrant tachycardia with close access of the PAC to the excitable gap, that is, antidromic reentry in this case. Additional pacing maneuvers during the study proved the mechanism to be antidromic tachycardia with retrograde conduction over the normal VA conduction system. The last two QRS complexes show no evidence of anterograde AP conduction. In fact, there is not even local evidence of preexcitation on the coronary sinus leads as demonstrated by a long conduction time between the local A and V ( arrow). In a patient with antidromic reciprocating tachycardia (ART) there is typically some evidence of anterograde AP activation during sinus rhythm. This was a very unusual AP that only became manifest with multiple premature atrial extrastimuli that resulted in block over the AV node and a very long conduction time over the AP.
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