Cytokine profile in severe gram-positive and gram-negative abdominal sepsis

Šurbatović, Maja; Popović, Nikola; Vojvodić, Danilo; Milošević, Ivan; Acimovic, G.T.; Stojičić, Milan; Veljović, Milić; Jevdjić, Jasna; Djordjević, Dragan; Radaković, Sonja

doi:10.1038/srep11355

Cited by 105 publications

(100 citation statements)

References 47 publications

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“…[5][6][7][8] The magnitude in the elevation of proinflammatory cytokines in chronic HF is significantly less than what would be observed in cases of autoimmune diseases or acute infections, suggesting that low-grade chronic inflammation may be an important contributor to the maintenance or clinical deterioration of patients with established chronic HF. [9][10][11] Here, we will review what is known about the role of chronic inflammation in established HF. Importantly, we will highlight that although we have come to understand some of the intricate and contextdependent mechanisms in which inflammatory cells and pathways contribute to the development of HF in the acute setting, few of those insights have been extended to assessing the role of inflammation once chronic HF has been established.…”

mentioning

confidence: 99%

Chronic Heart Failure and Inflammation

Dick

Epelman

2016

Circulation Research

544

380

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As a greater proportion of patients survive their initial cardiac insult, medical systems worldwide are being faced with an ever-growing need to understand the mechanisms behind the pathogenesis of chronic heart failure (HF). There is a wealth of information about the role of inflammatory cells and pathways during acute injury and the reparative processes that are subsequently activated. We discuss the different causes that lead to chronic HF development and how the sum of initial inflammatory and reparative responses only sets the trajectory for disease progression. Unfortunately, comparatively little is known about the contribution of the immune system once the trajectory has been set, and chronic HF has been established—which clinically represents the majority of patients. It is known that chronic HF is associated with circulating inflammatory cytokines that can predict clinical outcomes, yet the causative role inflammation plays in disease progression is not well defined, and the majority of clinical trials that target aspects of inflammation in patients with chronic HF have largely been negative. This review will present what is currently known about inflammation in chronic HF in both humans and animal models as a means to highlight the gap in our knowledge base that requires further examination.

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confidence: 99%

Chronic Heart Failure and Inflammation

Dick

Epelman

2016

Circulation Research

544

380

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“…La diferencia en la cantidad de citocinas infl amatorias inducidas por uno u otro tipo de bacterias, ha llevado a que en diversos estudios se haya encontrado que la medición rápida de éstas se plantee como un indicador que puede ayudar a discriminar si la bacteremia del paciente es por gram positivas o por gram negativas, así se ha encontrado en algunos estudios que en el caso de la sepsis por bacterias gram negativas se detectan mayores niveles de TNFα-, IL-1α, IL-1β, e IL-8, y en sepsis por gram positivas el TNFα,, IL-1β TNF β , IL-4 α, IL-18; en otros estudios se enfatiza que las mayores diferencias se observan a nivel de TNFα, Il-6, e IL-10, siendo la IL-10 un potencial marcador de la bacteremia por gram negativos en pacientes pediátricos hematológicos u oncoló-gicos. Igualmente se ha encontrado que frente al efecto sobre la producción de marcadores de sepsis como es la procalcitonina (PCT en inglés), resulta más efectivo el Lipopolisacárido de las bacterias gram negativas de ahí que la PCT se esté considerando como un agente predictor de la etiopatogenia de la sepsis (42)(43)(44)(45)(46).…”

Section: Mediadores Químicos Y Disfunción Sistémicaunclassified

Fisiopatología de la sepsis por gram positivos

Fandiño¹,

Barrera²

2016

rev cuarzo

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Las bacterias gram positivas vienen cobrando importancia como agentes etiológicos de la sepsis siendo algunos de principales representantes Staphylococcus aureus, las cepas de S.aureus meticilino resistentes (MRSA del inglés) y el Streptococcus pyogenes o también llamado Streptococcus del grupo A invasivo (GAS). Dado que en su estructura celular presentan diversas moléculas que pueden ser reconocidas como patrones moleculares asociados a patógenos (PAMPs) como son el peptidoglicano (PNG) el ácido teicoico (LTA), las lipoproteínas; y otras que activan directamente el sistema inmune adaptativo como son los Superantígenos; los pacientes infectados pueden exponerse de manera simultánea a una respuesta inmune amplifi cada de manera sinérgica entre todos estos tipos de antígenos, que a través de vías de señalización intracelular desencadenarán la transcripción de genes codifi cadores de citocinas pro infl amatorias como el TNFα, la IL-1β, la IL-6, el INFγ, IL-8, IL-18, IL-2, IL-12, IL-10 que darán lugar a muchas de las manifestaciones clínicas de la sepsis y se vienen asociando como predictores del pronóstico de esta junto a otros marcadores moleculares de la misma.

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“…The incidence of sepsis and the consequent fatality risk has increased over the past years, especially in the United States [32] and the condition is considered the leading cause of death in intensive care units [1].…”

Section: Final Considerationsmentioning

confidence: 99%

“…Sepsis is a common cause for admission and fatal outcomes in intensive care units (ICU) [1]. Most of these hospital-acquired infections occur in infirmaries and ICUs [2], however, many of the patients requiring intensive treatment, acquire them outside of the hospital environment [3].…”

Section: Introductionmentioning

confidence: 99%