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利用新型心率分析实现新生儿败血症及败血症样疾病的早期诊断。

Toward the early diagnosis of neonatal sepsis and sepsis-like illness using novel heart rate analysis.

作者信息

Griffin M P, Moorman J R

机构信息

Department of, and Molecular Physiology and Biological Physics, and the Cardiovascular Research Center, University of Virginia Health Sciences Center, Charlottesville, Virginia, USA.

出版信息

Pediatrics. 2001 Jan;107(1):97-104. doi: 10.1542/peds.107.1.97.

Abstract

BACKGROUND AND OBJECTIVE

Abrupt clinical deterioration because of sepsis is a major cause of morbidity and mortality in neonates, and earlier diagnosis should improve therapy of this potentially catastrophic illness. In practice, clinical signs and laboratory data have not been perceived as sensitive or specific for early stages of sepsis. Because heart rate characteristics (HRC) are abnormal during fetal distress and neonatal illness, we hypothesized that abnormal HRC might precede the clinical diagnosis of neonatal sepsis, adding independent information to standard clinical parameters.

METHODS

In the neonatal intensive care unit at the University of Virginia, we prospectively studied infants admitted from August 1995 to April 1999 who were at risk for developing sepsis. Infants in the sepsis (culture-positive) and sepsis-like illness (culture-negative) groups had an abrupt clinical deterioration that raised clinical suspicion of infection and prompted physicians to obtain blood cultures and start antibiotic therapy. Infants without sepsis raised no clinical suspicion of illness and had no cultures obtained. We measured novel characteristics-moments and percentiles-of normalized heart rate (HR) time series for 5 days before and 3 days after sepsis, sepsis-like illness, or a random time in controls. We also calculated the Score for Neonatal Acute Physiology (SNAP) and the Neonatal Therapeutic Intervention Scoring System (NTISS) as clinical scores of the severity of illness.

RESULTS

There were 46 episodes of culture-positive sepsis in 40 patients and 27 episodes of culture-negative sepsis-like illness in 23 patients. We analyzed 29 control periods in 26 patients. Infants with sepsis and sepsis-like illness had lower birth weights and gestational ages and higher SNAP and NTISS scores than did infants without sepsis. The most important new finding was that the infants in the sepsis and sepsis-like illness groups had increasingly abnormal HRC for up to 24 hours preceding their abrupt clinical deterioration. The abnormal HRC were reduced baseline variability and short-lived decelerations in HR. These abnormalities led to significant changes in HRC measures, for example, the third moment (skewness:.59 +/-.10 for sepsis and.51 +/-. 12 for sepsis-like illness, compared with -.10 +/-.13 for control over the 6 hours before abrupt deterioration). Culture-positive and culture-negative patients had similar HRC and clinical scores, including a significant rise in SNAP in the 24 hours before the event. Multivariable logistic regression analysis showed that HRC and clinical scores independently added information in distinguishing infants with sepsis and sepsis-like illness from control patients in the 24 hours before abrupt deterioration.

CONCLUSIONS

Newborn infants who had abrupt clinical deterioration as a result of sepsis and sepsis-like illness had abnormal HRC and SNAP that worsened over 24 hours before the clinical suspicion of sepsis. A strategy for monitoring these parameters in infants at risk for sepsis and sepsis-like illness might lead to earlier diagnosis and more effective therapy.heart rate variability, neonatal sepsis, Score for Neonatal Acute Physiology, Neonatal Therapeutic Intervention Scoring System, newborn.

摘要

背景与目的

脓毒症导致的临床突然恶化是新生儿发病和死亡的主要原因,早期诊断应能改善对这种潜在灾难性疾病的治疗。在实际操作中,临床体征和实验室数据对于脓毒症早期阶段而言,并未被认为具有敏感性或特异性。由于胎儿窘迫和新生儿疾病期间心率特征(HRC)会出现异常,我们推测异常的HRC可能先于新生儿脓毒症的临床诊断出现,并为标准临床参数增添独立信息。

方法

在弗吉尼亚大学新生儿重症监护病房,我们对1995年8月至1999年4月收治的有发生脓毒症风险的婴儿进行了前瞻性研究。脓毒症(血培养阳性)组和类脓毒症疾病(血培养阴性)组的婴儿出现临床突然恶化,引发了对感染的临床怀疑,并促使医生进行血培养及开始抗生素治疗。无脓毒症的婴儿未引发临床疾病怀疑,也未进行血培养。我们测量了脓毒症、类脓毒症疾病发生前5天及发生后3天,或对照组随机时间段内标准化心率(HR)时间序列的新特征——矩和百分位数。我们还计算了新生儿急性生理学评分(SNAP)和新生儿治疗干预评分系统(NTISS)作为疾病严重程度的临床评分。

结果

40例患者中有46次血培养阳性的脓毒症发作,23例患者中有27次血培养阴性的类脓毒症疾病发作。我们分析了26例患者的29个对照时间段。与无脓毒症的婴儿相比,脓毒症和类脓毒症疾病组的婴儿出生体重和胎龄更低,SNAP和NTISS评分更高。最重要的新发现是,脓毒症和类脓毒症疾病组的婴儿在临床突然恶化前长达24小时内HRC异常情况不断增加。异常的HRC表现为基线变异性降低和HR短暂减速。这些异常导致HRC测量值发生显著变化,例如,在突然恶化前6小时内,第三矩(偏度:脓毒症组为0.59±0.10,类脓毒症疾病组为0.51±0.12,而对照组为-0.10±0.13)。血培养阳性和血培养阴性患者的HRC和临床评分相似,包括事件发生前24小时内SNAP显著升高。多变量逻辑回归分析表明,在突然恶化前24小时内,HRC和临床评分在区分脓毒症和类脓毒症疾病婴儿与对照患者方面独立地增添了信息。

结论

因脓毒症和类脓毒症疾病导致临床突然恶化的新生儿,其HRC和SNAP异常,且在临床怀疑脓毒症前24小时内不断恶化。对有脓毒症和类脓毒症疾病风险的婴儿监测这些参数的策略可能会带来更早的诊断和更有效的治疗。心率变异性、新生儿脓毒症、新生儿急性生理学评分、新生儿治疗干预评分系统、新生儿

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