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Septic cardiomyopathy - A not yet discovered cardiomyopathy?

Standard

Septic cardiomyopathy - A not yet discovered cardiomyopathy? / Muller-Werdan, Ursula; Buerke, Michael; Ebelt, Henning; Heinroth, Konstantin M; Herklotz, Anja; Loppnow, Harald; Ruß, Martin; Schlegel, Frithjof; Schlitt, Axel; Schmidt, Hendrik B; Soeffker, Gerold; Werdan, Karl.

in: EXP CLIN CARDIOL, Jahrgang 11, Nr. 3, 3, 2006, S. 226-236.

Publikationen: SCORING: Beitrag in Fachzeitschrift/ZeitungSCORING: ZeitschriftenaufsatzForschungBegutachtung

Harvard

Muller-Werdan, U, Buerke, M, Ebelt, H, Heinroth, KM, Herklotz, A, Loppnow, H, Ruß, M, Schlegel, F, Schlitt, A, Schmidt, HB, Soeffker, G & Werdan, K 2006, 'Septic cardiomyopathy - A not yet discovered cardiomyopathy?', EXP CLIN CARDIOL, Jg. 11, Nr. 3, 3, S. 226-236. <http://www.ncbi.nlm.nih.gov/pubmed/18651035?dopt=Citation>

APA

Muller-Werdan, U., Buerke, M., Ebelt, H., Heinroth, K. M., Herklotz, A., Loppnow, H., Ruß, M., Schlegel, F., Schlitt, A., Schmidt, H. B., Soeffker, G., & Werdan, K. (2006). Septic cardiomyopathy - A not yet discovered cardiomyopathy? EXP CLIN CARDIOL, 11(3), 226-236. [3]. http://www.ncbi.nlm.nih.gov/pubmed/18651035?dopt=Citation

Vancouver

Muller-Werdan U, Buerke M, Ebelt H, Heinroth KM, Herklotz A, Loppnow H et al. Septic cardiomyopathy - A not yet discovered cardiomyopathy? EXP CLIN CARDIOL. 2006;11(3):226-236. 3.

Bibtex

@article{51433ade03b34a4d9fb71abb69f0a533,
title = "Septic cardiomyopathy - A not yet discovered cardiomyopathy?",
abstract = "Myocardial depression in human sepsis was only unequivocally proven in the 1980s by the group of Parrillo, who used nuclear imaging techniques to measure heart volumes and function in intensive care patients. Heart failure in sepsis is frequently masked by a seemingly normal cardiac output. However, relative to the lowered systemic vascular resistance - resulting in a reduced afterload - cardiac outputs and ventricular ejection fractions are often not adequately enhanced. This septic cardiomyopathy (impairment of the heart within the scope of systemic sepsis) involves both the right and the left ventricles, and is potentially reversible. In response to volume substitution, the heart can be considerably enlarged. The cardiomyopathy is not primarily hypoxic in nature, but may be aggravated by ischemia. Autonomic dysfunction, documented by a reduced heart rate variability and impaired baroreflex and chemoreflex sensitivities, forms part of the disease entity. The severity of myocardial depression correlates with a poor prognosis. Noninfectious systemic inflammatory response syndrome can give rise to an analogous disease entity, namely, systemic inflammatory response syndrome cardiomyopathy.The etiology of septic cardiomyopathy is multifactorial. Several candidates with a potential pathogenetic impact on the heart were identified: bacterial toxins; cytokines and mediators including tumour necrosis factor-alpha, interleukin-1 and nitric oxide; cardiodepressant factors; oxygen reactive species; and catecholamines. Symptomatic treatment consists of volume substitution and catecholamine support; causal therapeutic approaches aiming at an interruption of the proinflammatory mediator cascades are being tested.",
author = "Ursula Muller-Werdan and Michael Buerke and Henning Ebelt and Heinroth, {Konstantin M} and Anja Herklotz and Harald Loppnow and Martin Ru{\ss} and Frithjof Schlegel and Axel Schlitt and Schmidt, {Hendrik B} and Gerold Soeffker and Karl Werdan",
year = "2006",
language = "Deutsch",
volume = "11",
pages = "226--236",
number = "3",

}

RIS

TY - JOUR

T1 - Septic cardiomyopathy - A not yet discovered cardiomyopathy?

AU - Muller-Werdan, Ursula

AU - Buerke, Michael

AU - Ebelt, Henning

AU - Heinroth, Konstantin M

AU - Herklotz, Anja

AU - Loppnow, Harald

AU - Ruß, Martin

AU - Schlegel, Frithjof

AU - Schlitt, Axel

AU - Schmidt, Hendrik B

AU - Soeffker, Gerold

AU - Werdan, Karl

PY - 2006

Y1 - 2006

N2 - Myocardial depression in human sepsis was only unequivocally proven in the 1980s by the group of Parrillo, who used nuclear imaging techniques to measure heart volumes and function in intensive care patients. Heart failure in sepsis is frequently masked by a seemingly normal cardiac output. However, relative to the lowered systemic vascular resistance - resulting in a reduced afterload - cardiac outputs and ventricular ejection fractions are often not adequately enhanced. This septic cardiomyopathy (impairment of the heart within the scope of systemic sepsis) involves both the right and the left ventricles, and is potentially reversible. In response to volume substitution, the heart can be considerably enlarged. The cardiomyopathy is not primarily hypoxic in nature, but may be aggravated by ischemia. Autonomic dysfunction, documented by a reduced heart rate variability and impaired baroreflex and chemoreflex sensitivities, forms part of the disease entity. The severity of myocardial depression correlates with a poor prognosis. Noninfectious systemic inflammatory response syndrome can give rise to an analogous disease entity, namely, systemic inflammatory response syndrome cardiomyopathy.The etiology of septic cardiomyopathy is multifactorial. Several candidates with a potential pathogenetic impact on the heart were identified: bacterial toxins; cytokines and mediators including tumour necrosis factor-alpha, interleukin-1 and nitric oxide; cardiodepressant factors; oxygen reactive species; and catecholamines. Symptomatic treatment consists of volume substitution and catecholamine support; causal therapeutic approaches aiming at an interruption of the proinflammatory mediator cascades are being tested.

AB - Myocardial depression in human sepsis was only unequivocally proven in the 1980s by the group of Parrillo, who used nuclear imaging techniques to measure heart volumes and function in intensive care patients. Heart failure in sepsis is frequently masked by a seemingly normal cardiac output. However, relative to the lowered systemic vascular resistance - resulting in a reduced afterload - cardiac outputs and ventricular ejection fractions are often not adequately enhanced. This septic cardiomyopathy (impairment of the heart within the scope of systemic sepsis) involves both the right and the left ventricles, and is potentially reversible. In response to volume substitution, the heart can be considerably enlarged. The cardiomyopathy is not primarily hypoxic in nature, but may be aggravated by ischemia. Autonomic dysfunction, documented by a reduced heart rate variability and impaired baroreflex and chemoreflex sensitivities, forms part of the disease entity. The severity of myocardial depression correlates with a poor prognosis. Noninfectious systemic inflammatory response syndrome can give rise to an analogous disease entity, namely, systemic inflammatory response syndrome cardiomyopathy.The etiology of septic cardiomyopathy is multifactorial. Several candidates with a potential pathogenetic impact on the heart were identified: bacterial toxins; cytokines and mediators including tumour necrosis factor-alpha, interleukin-1 and nitric oxide; cardiodepressant factors; oxygen reactive species; and catecholamines. Symptomatic treatment consists of volume substitution and catecholamine support; causal therapeutic approaches aiming at an interruption of the proinflammatory mediator cascades are being tested.

M3 - SCORING: Zeitschriftenaufsatz

VL - 11

SP - 226

EP - 236

IS - 3

M1 - 3

ER -