Cellular electrophysiology of human myocardial infarction. 1. Abnormalities of cellular activation.

Jf, Spear; Ln, Horowitz; Ab, Hodess; MacVaugh, Horace; En, Moore

doi:10.1161/01.cir.59.2.247

Cited by 141 publications

(34 citation statements)

References 28 publications

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“…Note that the VPC, and VPC, intervals gradually shorten as the driving cycle length (CL) progressively decreases. fast sodium channel rather than the calcium-dependent slow channel response (45,46) in our group I patients.…”

Section: Discussionmentioning

confidence: 57%

Effects of verapamil on ventricular tachycardias possibly caused by reentry, automaticity, and triggered activity.

et al. 1983

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A B S T R A C T To define the role of verapamil in the treatment of ventricular tachycardia (VT), we studied 21 patients with chronic recurrent VT. Electrophysiologic studies were performed before and during intravenous infusion of verapamil (0.15 mg/kg followed by 0.005 mg/kg per min). On the basis of the mode of VT initiation and termination, we identified three groups of patients: (a) 11 patients had VT suggestive of reentry, as VT could be initiated with ventricular extrastimulation and terminated with overdrive ventricular pacing. Verapamil did not affect the inducibility and cycle length of VT. (b) 7 patients had VT suggestive of catecholamine-sensitive automaticity as VT could not be initiated with programmed electrical stimulation but could be provoked by isoproterenol infusion. Moreover, the VT could not be converted to a sustained sinus rhythm with overdrive ventricular pacing and it resolved only with discontinuing isoproterenol infusion. Verapamil exerted no effects on VT. (c) 3 patients had VT with electrophysiologic characteristics suggestive of triggered activity related to delayed afterdepolarizations. Characteristically, after attaining a range of cycle lengths, the sinus, atrial or ventricular paced rhythm could initiate VT without ventricular extrastimulation. The first beat of VT invariably occurred late in the cardiac cycle with a premature coupling interval 0-80 ms shorter than the preceding QRS cycle length; the premature coupling interval gradually decreased as the sinus, atrial or ventricular paced cycle length progressively shortened. Of

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Section: Discussionmentioning

confidence: 57%

Effects of verapamil on ventricular tachycardias possibly caused by reentry, automaticity, and triggered activity.

et al. 1983

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“…The effects of verapamil and diltiazem on the mechanical alternans are summarized in figure 6. Verapamil attenuated the 34 We have previously shown that the STA is a correlative to the alternation in phase 2 of a membrane action potential, and that STA is not always accompanied by the alternation of the duration of the action potential.5 Therefore, it seems that the alternation in the calcium flow during the phase 2 may be involved in STA. In this study, verapamil and diltiazem prominently attenuated the degree of STA.…”

Section: Resultsmentioning

confidence: 93%

Effects of calcium antagonists on the electrical alternans of the ST segment and on associated mechanical alternans during acute coronary occlusion in dogs.

Hashimoto¹,

Suzuki²,

Miyake³

et al. 1983

Circulation

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Effects of calcium antagonists on the ST alternans and associated mechanical altemans during acute coronary occlusion were examined in anesthetized dogs. The heart rate was fixed by atrial pacing. The intravenous administration of 0.2 mg/kg verapamil attenuated the ST alternans as did 0.5 mg/kg diltiazem. Although these drugs significantly attenuated TQ depression during occlusion, the attenuation was observed after a longer period of occlusion and when the degree of TQ depression was comparable to that during the control occlusion. Nifedipine, 0.03 mg/kg, slightly attenuated the ST alternans, but 0.5 mg/kg dipyridamole had no effect. These results support the idea that slow inward currents are involved in the ST altemans. On the other hand, the mechanical altemans was attenuated in six of 11 dogs. It is probable that factors other than the electrical altemans may also contribute to the mechanical altemans. Circulation 68, No. 3, 667472, 1983. ALTERNANS of the ST segment of the electrocardiogram (ST alternans, STA) has been frequently observed in experimental animals'`" and cases of STA also have been observed in patients with ischemic heart disease.5' 8, 9 Because STA is frequently followed by ventricular arrhythmia, many authors have suggested a causal relationship between the two phenomena. of these drugs on the electrical and the mechanical alternans during left anterior descending coronary artery (LAD) occlusion have not been examined. Thus, the purpose of our study was to examine the effects of calcium antagonists on STA and associated mechanical altemans during acute coronary occlusion in dogs. MethodsTwenty-seven mongrel dogs weighing 6.5 to 12.0 kg were anesthetized with 30 mg/kg of intravenous sodium pentobarbital. Under artificial respiration, a left lateral thoracotomy was performed through the fifth left intercostal space and the heart was cradled in the opened pericardium. Standard lead II of the electrocardiogram, an epicardial unipolar electrogram (EPeg), amount of isometric myocardial contraction (contractile force) in the ischemic area, and left ventricular pressure (LVP) were recorded. For measuring LVP a catheter was placed in the left ventricle through the femoral artery. The contractile force was measured by a strain-gauge arch with adjustable feet (HD-IT, Nihon Kohden). The myocardial segment between the two feet of the strain-gauge arch was stretched to about 20% of its diastolic length. The EPeg from the ischemic area was recorded by a tungsten wire with a diameter of 0.2 mm. The electrode for EPeg and the strain-gauge arch were set at the same area in order to examine the relationship between the electrical and the mechanical alternans. The indifferent electrode for EPeg was connected with Wilson's central terminal. The lead II, EPeg, contractile force, and LVP were amplified by a polygraph (RM-85M, Nihon Kohden) and recorded on a mingograph (800-6 Nihon Kohden). To produce transient ischemia, the LAD was occluded below its first diagonal branch for 3 to 10 min. The time int...

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“…The loss of cells and cell-to-cell connection that occurs in chronic infarction has been associated with both generalized and local abnormalities of activation in other preparations.20 22 The changes in P layer activation noted in the present study, specifically generalized slowing, local conduction block, and fragmentation as well as electrotonic distortion of action potentials, are strikingly similar qualitatively to abnormalities noted in canine epicardial muscle overlying a chronic infarction20-22 and in isolated human tissue. 23,[36][37][38] It seems clear from our late studies of P and VM activation that the P layer in ischemic regions remains quite viable electrophysiologically, despite complete loss of the underlying VM layer. Despite rather modest generalized slowing, 1:1 conduction was routinely maintained even to sites deep within the ischemic zone.…”

Section: Discussionmentioning

confidence: 99%

Alterations in endocardial activation of the canine papillary muscle early and late after myocardial infarction.

et al. 1987

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Permanent coronary occlusion produces time-dependent changes in surviving subendocardial cellular properties. We compared the functional alterations in Purkinje (P) and ventricular muscle (VM) activation early (24 hr) and late (4 weeks or greater) after permanent coronary occlusion in an in vitro preparation of canine papillary muscle. High-density extracellular (1 to 2 mm resolution) and selected intracellular recordings were made in five animals early and seven animals late during stimulation of a free-running P strand. Activation patterns of P and VM layers from ischemic and unaffected papillary muscles were compared in the same animal. Average P layer conduction velocity was determined in normal and ischemic regions with the use of a linear array of recording and stimulating electrodes. Purkinje activation was altered little in the early phase of infarction, while healing was associated with a generalized 25% reduction in P layer conduction velocity and localized block and fragmentation of P waveforms. Intracellular recordings at sites of nonsynchronous P activation revealed electrotonic interaction between cell groups. At 24 hr, small groups of VM were present but with abnormal activation patterns in regions of necrosis with fragmented and delayed extracellular waveforms produced by partially uncoupled groups of cells. Local delay and block could be modulated by rate and site of stimulation. After healing, VM activation abruptly stopped at the visual infarct border, marked by a characteristic "end potential." These studies demonstrate important differences in the functional attributes of the P and VM layers studied early and late after coronary occlusion. Alterations in cell-to-cell relationships are likely very important in determining abnormalities of activation in both settings.

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Cellular electrophysiology of human myocardial infarction. 1. Abnormalities of cellular activation.

Cited by 141 publications

References 28 publications

Effects of verapamil on ventricular tachycardias possibly caused by reentry, automaticity, and triggered activity.

Effects of verapamil on ventricular tachycardias possibly caused by reentry, automaticity, and triggered activity.

Effects of calcium antagonists on the electrical alternans of the ST segment and on associated mechanical alternans during acute coronary occlusion in dogs.

Alterations in endocardial activation of the canine papillary muscle early and late after myocardial infarction.

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