脓毒症的进展,从生理性全身炎症反应到免疫失调,由于危及生命的感染

Nicholas J Daering, M. Al-Hasan
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引用次数: 0

摘要

1991年,全身性炎症反应综合征(SIRS)标准定义了脓毒症,该标准主要包括对感染或炎症的生理反应(发烧、心动过速、呼吸急促和白细胞增多)。这些标准最初被提出用于识别革兰氏阴性血流感染(BSI)患者。然而,大多数BSI患者在首次就诊时,使用客观的临床急性严重程度评分,如皮特菌血症评分(PBS),并不是危重症。缺乏特异性和低阳性预测值(PPV)是SIRS标准的其他缺陷。此外,基于这一过时定义的脓毒症干预措施的实施未能改善患者的预后,在某些情况下还与广谱抗生素的使用增加和艰难梭菌(C. difficile)感染有关。2016年,使用快速顺序器官衰竭评估(qSOFA)评分,败血症被重新定义为对危及生命的感染的失调宿主反应。三个床边临床变量中的两个(低血压、呼吸窘迫和精神状态改变)一直预测感染患者的死亡率,现在构成败血症。关于新标准的表现,医学文献中的科学争论仍在继续。一些医疗专业人员和质量组织认为这些对败血症定义的改变过于革命性,并且抵制改变现有的医疗实践。这篇叙述性综述认为感染是一个连续体,从局部感染到全身性感染(脓毒症前),如果延迟适当的抗生素治疗和源控制,可能会进展为脓毒症和感染性休克。该综述评估了宿主和微生物因素,这些因素可能会影响脓毒症级联的进展速度,并在每个步骤中提出诊断考虑和管理决策。它强调在选择经验性抗生素治疗时,需要利用精确医学概念,根据耐药细菌引起的感染的患者特异性风险因素和脓毒症范围内适当治疗的潜在益处。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
The progression of sepsis from physiologic systemic inflammatory response to immune dysregulation due to life-threatening infections
Sepsis was defined in 1991 by the systemic inflammatory response syndrome (SIRS) criteria which consisted mostly of physiologic responses to infection or inflammation (fever, tachycardia, tachypnea, and leukocytosis). These criteria were initially proposed to identify patients with gram-negative bloodstream infection (BSI). However, most patients with BSI are not critically ill at initial presentation using objective clinical scores for acute severity of illness, such as the Pitt bacteremia score (PBS). Lack of specificity and low positive predictive value (PPV) are other pitfalls of the SIRS criteria. Moreover, the implementation of sepsis interventions based on this outdated definition failed to improve patients’ outcomes and in some settings was associated with increased use of broad-spectrum antibiotics and Clostridioides difficile (C. difficile) infection. In 2016, sepsis was redefined as a dysregulatory host response to life-threatening infections using quick sequential organ failure assessment (qSOFA) score. The presence of two of three bedside clinical variables (hypotension, respiratory distress, and altered mental status) that have consistently predicted mortality in patients with infections now constitutes sepsis. The scientific debate continues in the medical literature regarding the performance of the new criteria. Some medical professionals and quality organizations consider these changes to the sepsis definition too revolutionary and are resistant to altering existing medical practice. This narrative review presents infection as a continuum from localized to systemic infection (pre-sepsis) with the potential progression into sepsis and septic shock if appropriate antibiotic therapy and source control are delayed. The review assesses host and microbial factors that may influence the rate of progression through the sepsis cascade and proposes diagnostic considerations and management decisions at each step of the way. It emphasizes the need to utilize precision medicine concepts in selecting empirical antibiotic therapy based on patient-specific risk factors for infections due to resistant bacteria and potential benefits from appropriate therapy across the sepsis spectrum.
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