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Gut Dysfunction and Intolerance to Enteral Nutrition in Critically 111 Patients

机译:肠道功能障碍和肠内营养的不耐受性111名患者

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For patients who survive the first 48 h of intensive care, sepsis-related multiple organ failure (MOF) is the leading cause for prolonged intensive care unit (ICU) stays and deaths. Several lines of clinical evidence convincingly link gut injury and subsequent dysfunction to MOF [1]. First, patients who experience persistent gut hypoperfusion (documented by gastric tonometry) after resuscitation are at high risk for abdominal compartment syndrome (ACS), MOF, and death [2]. Second, epidemiologic studies have consistently shown that the normally sterile proximal gut becomes heavily colonized with a variety of organisms. These same organisms have been identified to be pathogens that cause late nosocomial infections. Thus, the gut has been called the 'undrained abscess' of MOF [3]. Third, gut-specific therapies (selective gut decontamination, early enteral nutrition (EN), and most recently immune-enhancing enteral diets) have been shown to reduce these nosocomial infections [4-7]. Of these gut-specific therapies,early EN is most widely employed. However, the most severely ill patients who should benefit most from early EN are frequently intolerant to it and are at increased risk for EN-related complications [8-11].
机译:对于在重症监护前48小时生存的患者中,败血症相关的多器官衰竭(MOF)是长期重症监护单位(ICU)的主要原因(ICU)。几条临床证据令人信服地将肠道损伤链接和随后的功能障碍[1]。首先,复苏后经历持续的肠道失血(由胃髓作用的患者)的患者处于腹腔综合征(ACS),MOF和死亡的高风险(ACS)[2]。其次,流行病学研究一致地表明,通常无菌近端肠道与各种生物体变得严重殖民。已经鉴定了这些相同的生物是导致后期医院感染的病原体。因此,肠道已被称为MOF的“不义的脓肿”[3]。三,肠道疗法(选择性肠道净化,早期肠内营养(EN)和最近免疫增强肠内饮食)已被证明减少这些医院感染[4-7]。在这些肠道特定的疗法中,早期ZH最广泛使用。然而,最严重的病患者,应该从早期的患者那里受益于其往往是不耐受的,并且具有增加的与与相关的并发症有关的风险[8-11]。

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