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Höpp HW, Treis-Müller I, Osterspey A, et al. Ventrikuläre Spätpotentiale bei akutem Myokardinfarkt. [Ventricular late potentials in acute myocardial infarct]. Herz. 1988;13(3):169-79
Höpp, H. W., Treis-Müller, I., Osterspey, A., Hombach, V., & Hilger, H. H. (1988). Ventrikuläre Spätpotentiale bei akutem Myokardinfarkt. [Ventricular late potentials in acute myocardial infarct]. Herz, 13(3), 169-79.
Höpp, H W, et al. "Ventrikuläre Spätpotentiale bei akutem Myokardinfarkt." [Ventricular late potentials in acute myocardial infarct]. Herz vol. 13,3 (1988): 169-79.
Höpp HW, Treis-Müller I, Osterspey A, Hombach V, Hilger HH. Ventrikuläre Spätpotentiale bei akutem Myokardinfarkt. [Ventricular late potentials in acute myocardial infarct]. Herz. 1988 Jun;13(3):169-79. German. PMID: 3042572.
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Herz. 1988 Jun;13(3):169-79.

[Ventricular late potentials in acute myocardial infarct].

Herz

[Article in German]
H W Höpp, I Treis-Müller, A Osterspey, V Hombach, H H Hilger

Affiliations

  1. Medizinische Klinik III der Universität zu Köln.

PMID: 3042572

Abstract

Ventricular late potentials are regarded as an expression of delayed impulse conduction in an area of myocardial ischemia and, accordingly, indicative of a preformed reentry circuit. Late potentials can be detected in chronic, stable coronary artery disease and their presence correlates closely with impairment of ventricular function and with the probability of future occurrence of tachyarrhythmic events or sudden cardiac death. While repetitive ventricular arrhythmias in the chronic stage of coronary artery disease result almost invariably from circling intraventricular wavefronts, tachyarrhythmias associated with acute myocardial infarction appear attributable to differing pathomechanisms. According to experimental studies, in acute myocardial infarction, three phases of arrhythmogenesis can be differentiated: phase 1 encompasses the first hours after vessel occlusion which generally corresponds with the prehospital phase. Due to the difference in potential of up to 25 mV between ischemic and nonischemic cardiac muscle areas, an injury current is called into existence which leads to depolarization of normal cardiac muscle tissue. The ectopic impulses so precipitated, the conduction of which is supported by the functional inhomogeneity of the infarcted region, are capable of initiating reentry tachycardia. During phase 2, a few hours to days after the ischemic event, only the subendocardial Purkinje fibers in the infarcted region exhibit focal arrhythmogenicity. In contrast to the working myocardial cells, the latter survive due to their immediate proximity to the cardiac chamber and show, ischemia-induced, a propensity to high-frequency impulse formation in terms of abnormal automaticity. Similar to the experimental findings, the cause of the frequently-observed ventricular arrhythmias in the early hospital phase appears predominantly attributable to a focal arrhythmia mechanism. During phase 3, several days to weeks after the acute myocardial ischemic event, reentry mechanisms again are in the foreground in which the electrophysiologic changes in the Purkinje fibers, in terms of increasing desynchronization, together with conduction barriers arising through the infarct scar, pave the way for reentry phenomenon. After abrupt restoration of patency of a previously occluded vessel the very frequent "reperfusion arrhythmias" are also attributable primarily to reentry mechanisms due to inhomogeneous improvement of the conduction properties in the region of the reperfused myocardium. Ventricular late potentials can be registered both invasively by means of epi- or endocardial leads as well as noninvasively from the body surface.(ABSTRACT TRUNCATED AT 400 WORDS)

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