斯里兰卡被蝰蛇咬伤后三种血清生物标志物在早期检测系统性传染病中的实用性。

IF 5 1区 医学 Q1 EMERGENCY MEDICINE Annals of emergency medicine Pub Date : 2024-08-09 DOI:10.1016/j.annemergmed.2024.06.023
Supun Wedasingha MBBS , Anjana Silva MBBS, PhD , Kellie Fakes DipPathTech , Sisira Siribaddana MBBS, MD , Geoffrey K. Isbister BSc, MD
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引用次数: 0

摘要

研究目的:早期发现全身中毒对于早期抗蛇毒血清治疗以最大限度地降低蛇咬伤的发病率和死亡率至关重要。我们评估了 3 种血清生物标志物在早期发现斯里兰卡农村地区被毒蛇咬伤的全身性中毒中的诊断效用:方法:纳入 2020 年 7 月至 2021 年 6 月期间阿努拉德普勒教学医院收治的所有确诊蛇咬伤患者。入院时采血检测毒液浓度、凝血酶原时间/国际标准化比率、纤维蛋白原浓度、血清肌酐浓度和 3 种血清生物标志物,即分泌型磷脂酶 A2(sPLA2)活性、中性粒细胞明胶酶相关脂质体蛋白(sNGAL)浓度和集束素(sClu)浓度。出现毒液引起的消耗性凝血病、神经毒性、急性肾损伤或出现非特异性临床症状即为全身中毒:共招募了 237 名确诊为蛇咬伤的患者(罗素蝰 72 人、驼鼻蝰 80 人、无毒蛇 31 人、不明咬伤 54 人),这些患者在注射蛇毒前均采集了足够的血清样本[中位年龄:42 岁(四分位数间距 [IQR] 29 至 53 岁);男性 173 人(73%)]。68例(94%)罗素蝰咬伤、48例(60%)驼鼻蝰咬伤和45例(83%)不明咬伤发生了全身中毒。罗素蝰咬伤的 sPLA2 活性中位数为 72 nmol/mL/min(IQR 30 至 164),驼鼻蝰咬伤的 sPLA2 活性中位数为 12 nmol/mL/min(IQR 9 至 16),无毒咬伤的 sPLA2 活性中位数为 11 nmol/mL/min(IQR 9 至 14)。三组之间的 sNGAL 和 sCLu 浓度没有差异。全身性咬伤患者的 sPLA2 活性中位数为 16 nmol/min/mL(IQR 11 至 59),而非全身性咬伤患者的 sPLA2 活性中位数为 11 nmol/min/mL(IQR 9 至 14);中位数之间的差异为 5 nmol/min/mL(95% 置信区间 [CI] 4 至 12)。入院 sPLA2 活性的接收者操作特征曲线下面积 (AUC-ROC) 是所有蛇咬伤患者全身中毒的最佳预测指标(AUC-ROC 0.72,95% CI 0.66 至 0.79),而 sNGAL 和 sClu 浓度则是较差的预测指标。sPLA2 活性对罗素蝰蛇咬伤(AUC-ROC 0.90,95% CI 0.76 至 1.00)和咬伤后 2 小时内就诊者全身中毒的预测效果较好。sPLA2 活性超过 23.5 nmol/min/mL 的灵敏度为 97%(95% CI 91% 至 99.5%),但预测全身中毒的特异性较低,仅为 41%(95% CI 34% 至 49%)。入院时sPLA2活性超过46 nmol/min/mL对预测罗素蝰蛇咬伤后全身中毒的敏感性为100%(95% CI 51%至100%),特异性为67%(95% CI 55%至77%)。
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Utility of Three Serum Biomarkers for Early Detection of Systemic Envenoming Following Viper Bites in Sri Lanka

Study objective

Early detection of systemic envenoming is critical for early antivenom therapy to minimize morbidity and mortality from snakebite. We assessed the diagnostic utility of 3 serum biomarkers in the early detection of systemic envenoming in viper bites in rural Sri Lanka.

Methods

All confirmed snakebite patients admitted to Teaching Hospital Anuradhapura from July 2020 to June 2021 were included. On admission, blood was collected for venom concentrations, prothrombin time/international normalized ratio, fibrinogen concentration, serum creatinine concentration, and 3 serum biomarkers, namely secretory phospholipase A2 (sPLA2) activity, neutrophil gelatinase-associated lipocalin (sNGAL) concentration, and clusterin (sClu) concentration. Systemic envenoming was defined by the presence of venom-induced consumption coagulopathy, neurotoxicity, acute kidney injury, or the presence of nonspecific clinical effects.

Results

A total of 237 confirmed snakebite patients (Russell’s viper, 72; hump-nosed viper, 80; nonvenomous snakes, 31; and unidentified bites, 54) with sufficient preantivenom serum samples were recruited [median age: 42 years (interquartile range [IQR] 29 to 53 years); 173 men (73%)]. Systemic envenoming occurred in 68 (94%) Russell’s viper bites, 48 (60%) hump-nosed viper bites, and 45 (83%) unidentified bites. The median sPLA2 activity was 72 nmol/mL/min (IQR 30 to 164) for Russell’s viper envenoming, 12 nmol/mL/min (IQR 9 to 16) for hump-nosed viper envenoming, and 11 nmol/mL/min (IQR 9 to 14) for nonvenomous bites. There was no difference in sNGAL and sCLu concentrations among the 3 groups. The median sPLA2 activity of patients with systemic envenoming was 16 nmol/min/mL (IQR 11 to 59) compared to 11 nmol/min/mL (IQR 9 to 14) in patients without systemic envenoming; the difference between medians was 5 nmol/min/mL (95% confidence interval [CI] 4 to 12). The area under the receiver operator characteristic curve (AUC-ROC) of admission sPLA2 activity was the best predictor of systemic envenoming in all snakebites (AUC-ROC 0.72, 95% CI 0.66 to 0.79), whereas sNGAL and sClu concentrations were poor predictors. sPLA2 activity was a better predictor of systemic envenoming in Russell’s viper bites (AUC-ROC 0.90, 95% CI 0.76 to 1.00) and in those presenting within 2 hours of a bite. A sPLA2 activity more than 23.5 nmol/min/mL had a sensitivity of 41% (95% CI 34% to 49%), and a specificity of 97% (95% CI 91% to 99.5%) in predicting systemic envenoming. A sPLA2 activity of more than 46 nmol/min/mL on admission had a sensitivity of 67% (95% CI 55% to 77%) and a specificity of 100% (95% CI 51% to 100%) in predicting systemic envenoming in Russell’s viper bites.

Conclusions

sPLA2 activity is an early predictor of systemic envenoming following snakebite, particularly in Russell’s viper bites and in those who present early.
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来源期刊
Annals of emergency medicine
Annals of emergency medicine 医学-急救医学
CiteScore
8.30
自引率
4.80%
发文量
819
审稿时长
20 days
期刊介绍: Annals of Emergency Medicine, the official journal of the American College of Emergency Physicians, is an international, peer-reviewed journal dedicated to improving the quality of care by publishing the highest quality science for emergency medicine and related medical specialties. Annals publishes original research, clinical reports, opinion, and educational information related to the practice, teaching, and research of emergency medicine. In addition to general emergency medicine topics, Annals regularly publishes articles on out-of-hospital emergency medical services, pediatric emergency medicine, injury and disease prevention, health policy and ethics, disaster management, toxicology, and related topics.
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