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Systematic review and validation of prediction rules for identifying children with serious infections in emergency departments and urgent-access primary care.

机译:对预测规则进行系统的审查和确认,以识别急诊部门和急诊基层医疗机构中有严重感染的儿童。

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摘要

BACKGROUND: Although the vast majority of children with acute infections are managed at home, this is one of the most common problems encountered in children attending emergency departments (EDs) and primary care. Distinguishing children with serious infection from those with minor or self-limiting infection is difficult. This can result in misdiagnosis of children with serious infections, which results in a poorer health outcome, or a tendency to refer or admit children as a precaution; thus, inappropriately utilising secondary-care resources. OBJECTIVES: We systematically identified clinical features and laboratory tests which identify serious infection in children attending the ED and primary care. We also identified clinical prediction rules and validated those using existing data sets. DATA SOURCES: We searched MEDLINE, Medion, EMBASE, Cumulative Index to Nursing and Allied Health Literature and Database of Abstracts of Reviews of Effects in October 2008, with an update in June 2009, using search terms that included terms related to five components: serious infections, children, clinical history and examination, laboratory tests and ambulatory care settings. We also searched references of included studies, clinical content experts, and relevant National Institute for Health and Clinical Excellence guidelines to identify relevant studies. There were no language restrictions. Studies were eligible for inclusion if they were based in ambulatory settings in economically developed countries. REVIEW METHODS: Literature searching, selection and data extraction were carried out by two reviewers. We assessed quality using the quality assessment of diagnostic accuracy studies (QUADAS) instrument, and used spectrum bias and validity of the reference standard as exclusion criteria. We calculated the positive likelihood ratio (LR+) and negative likelihood ratio (LR-) of each feature along with the pre- and post-test probabilities of the outcome. Meta-analysis was performed using the bivariate method when appropriate. We externally validated clinical prediction rules identified from the systematic review using existing data from children attending ED or primary care. RESULTS: We identified 1939 articles, of which 35 were selected for inclusion in the review. There was only a single study from primary care; all others were performed in the ED. The quality of the included studies was modest. We also identified seven data sets (11,045 children) to use for external validation. The most useful clinical features for ruling in serious infection was parental or clinician overall concern that the illness was different from previous illnesses or that something was wrong. In low- or intermediate-prevalence settings, the presence of fever had some diagnostic value. Additional red flag features included cyanosis, poor peripheral circulation, rapid breathing, crackles on auscultation, diminished breath sounds, meningeal irritation, petechial rash, decreased consciousness and seizures. Procalcitonin (LR+ 1.75-2.96, LR- 0.08-0.35) and C-reactive protein (LR+ 2.53-3.79, LR- 0.25-0.61) were superior to white cell counts. The best performing clinical prediction rule was a five-stage decision tree rule, consisting of the physician's gut feeling, dyspnoea, temperature ≥ 40 °C, diarrhoea and age. It was able to decrease the likelihood of serious infections substantially, but on validation it provided good ruling out value only in low-to-intermediate-prevalence settings (LR- 0.11-0.28). We also identified and validated the Yale Observation Scale and prediction rules for pneumonia, meningitis and gastroenteritis. LIMITATIONS: Only a single study was identified from primary-care settings, therefore results may lack generalisability. CONCLUSIONS: Several clinical features are useful to increase or decrease the probability that a child has a serious infection. None is sufficient on its own to substantially raise or lower the risk of serious infection. Some are highly specific ('red flags'), so when present should prompt a more thorough or repeated assessment. C-reactive protein and procalcitonin demonstrate similar diagnostic characteristics and are both superior to white cell counts. However, even in children with a serious infection, red flags will occur infrequently, and their absence does not lower the risk. The diagnostic gap is currently filled by using clinical 'gut feeling' and diagnostic safety-netting, which are still not well defined. Although two prediction rules for serious infection and one for meningitis provided some diagnostic value, we do not recommend widespread implementation at this time. Future research is needed to identify predictors of serious infection in children in primary-care settings, to validate prediction rules more widely, and determine the added value of blood tests in primary-care settings. FUNDING: The National Institute for Health Research Health Technology Assessment programme.
机译:背景:尽管绝大多数急性感染儿童是在家中管理的,但这是在急诊室和基层医疗中遇到的最普遍的问题之一。很难将感染严重的儿童与感染轻微或自我限制的儿童区分开。这可能导致严重感染儿童的误诊,从而导致健康状况较差,或倾向于将儿童转介或接纳为预防措施;因此,不适当地利用二级保健资源。目的:我们系统地鉴定了临床特征和实验室测试,以鉴定参加急诊和初级保健的儿童中的严重感染。我们还确定了临床预测规则,并使用现有数据集验证了这些规则。数据来源:我们于2008年10月搜索了MEDLINE,Medion,EMBASE,护理和相关健康文献累积索引和效果评价摘要数据库,并于2009年6月进行了更新,使用的搜索词包括与以下五个成分相关的术语:严重感染,儿童,临床病史和检查,实验室检查和非卧床护理设置。我们还搜索了纳入研究的参考文献,临床内容专家以及相关的美国国立卫生研究院和临床卓越指南,以识别相关研究。没有语言限制。如果研究基于经济发达国家的动态环境,则符合纳入条件。评审方法:由两名评审进行文献检索,选择和数据提取。我们使用诊断准确性研究(QUADAS)仪器的质量评估来评估质量,并使用光谱偏差和参考标准的有效性作为排除标准。我们计算了每个特征的正似然比(LR +)和负似然比(LR-)以及结果的测试前和测试后概率。适当时使用双变量方法进行荟萃分析。我们使用来自参加ED或初级护理的儿童的现有数据,从系统评价中外部验证了临床预测规则。结果:我们鉴定了1939篇文章,其中35篇被纳入评论。初级保健只有一项研究。其他所有手术均在急诊室进行。纳入研究的质量中等。我们还确定了七个数据集(11,045名儿童)用于外部验证。裁决严重感染最有用的临床特征是父母或临床医生总体上担心该疾病与以前的疾病不同或出了问题。在低或中等流行的环境中,发烧的诊断价值。其他红旗功能包括紫osis,周围循环不良,呼吸急促,听诊时有crack啪声,呼吸音减弱,脑膜刺激,皮疹,意识下降和癫痫发作。降钙素原(LR + 1.75-2.96,LR- 0.08-0.35)和C反应蛋白(LR + 2.53-3.79,LR- 0.25-0.61)优于白细胞计数。表现最佳的临床预测规则是五阶段决策树规则,包括医师的肠胃感觉,呼吸困难,温度≥40°C,腹泻和年龄。它能够大幅降低发生严重感染的可能性,但经验证,它仅在中低患病率设置下具有良好的排除价值(LR- 0.11-0.28)。我们还确定并验证了耶鲁观察量表和肺炎,脑膜炎和胃肠炎的预测规则。局限性:仅从基层医疗机构中识别出一项研究,因此结果可能缺乏普遍性。结论:几种临床特征可用于增加或减少儿童发生严重感染的可能性。仅靠其自身不足以大大提高或降低严重感染的风险。有些是高度特定的(“红色标志”),因此,如果存在,应该提示进行更彻底或重复的评估。 C反应蛋白和降钙素显示出相似的诊断特征,并且均优于白细胞计数。但是,即使在严重感染的儿童中,也很少出现危险信号,并且没有危险信号不会降低危险。目前,通过使用尚不确定的临床“肠道感觉”和诊断安全网来填补诊断空白。尽管针对严重感染的两个预测规则和针对脑膜炎的两个预测规则提供了一定的诊断价值,但我们不建议您在此时广泛实施该规则。需要进一步的研究来确定初级保健机构中儿童严重感染的预测因素,更广泛地验证预测规则,并确定初级保健机构中血液测试的附加值。资金:美国国立卫生研究院健康技术评估计划。

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