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新生儿感染中C反应蛋白的诊断性审计

Diagnostic audit of C-reactive protein in neonatal infection.

作者信息

Mathers N J, Pohlandt F

出版信息

Eur J Pediatr. 1987 Mar;146(2):147-51. doi: 10.1007/BF02343221.

Abstract

A prospective study of 250 consecutive neonatal admissions to a regional perinatal referral centre and of 10 additional consecutive cases with culture-proven neonatal septicaemia was undertaken. Quantitative C-reactive protein (CRP) determination, white cell count and differential were performed on blood samples obtained from all babies on admission, as well as 10-14 h and 22-26 h later. Using clinical signs, chest X-rays, blood cultures, tracheal aspirates obtained within 4 h of delivery and an abnormal immature/total neutrophil ratio (I/T), infected babies were defined as belonging to one of the following groups: culture-proven septicaemia (n = 19); clinical septicaemia (n = 35); congenital pneumonia (n = 28). The sensitivity, specificity, positive and negative predictive value of CRP were calculated for each sampling time and patient group. No baby had a rise in CRP (greater than 6 mg/l) before an abnormal I/T ratio was first detected. A delayed rise in CRP concentration in the majority of infected babies occurred approximately 12-24 h after the abnormal I/T ratio was first detected. The overall specificity of a CRP level of greater than or equal to 10 mg/l remained approximately constant (97%-94%) while sensitivity increased from 22%-61% with increasing time after admission. The same pattern emerged if each patient group was considered separately. The positive predictive value for a CRP level of greater than or equal to 10 mg/l 22-26 h after admission was 83% and the negative predictive value 82%. CRP had no value in the early diagnosis of neonatal infection. Its main role lies rather in the exclusion or confirmation of infection 24 h after the first clinical suspicion.

摘要

对一家地区围产期转诊中心连续收治的250例新生儿以及另外10例经培养证实患有新生儿败血症的连续病例进行了一项前瞻性研究。对所有入院婴儿入院时以及入院后10 - 14小时和22 - 26小时采集的血样进行定量C反应蛋白(CRP)测定、白细胞计数及分类。根据临床体征、胸部X线检查、血培养、分娩后4小时内获取的气管吸出物以及异常的未成熟/总中性粒细胞比值(I/T),将感染婴儿定义为属于以下组之一:经培养证实的败血症(n = 19);临床败血症(n = 35);先天性肺炎(n = 28)。计算每个采样时间和患者组的CRP敏感性、特异性、阳性和阴性预测值。在首次检测到异常I/T比值之前,没有婴儿的CRP升高(大于6mg/L)。大多数感染婴儿的CRP浓度在首次检测到异常I/T比值后约12 - 24小时出现延迟升高。CRP水平大于或等于10mg/L的总体特异性保持在大约恒定水平(97% - 94%),而敏感性随着入院后时间的增加从22% - 61%升高。如果分别考虑每个患者组,也会出现相同的模式。入院后22 - 26小时CRP水平大于或等于10mg/L的阳性预测值为83%,阴性预测值为82%。CRP在新生儿感染的早期诊断中没有价值。其主要作用在于在首次临床怀疑后24小时排除或确认感染。

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