Neuronal exosome proteins: novel biomarkers for predicting neonatal response to therapeutic hypothermia

外体 医学 脑病 内科学 自然循环恢复 生物标志物 体温过低 微泡 麻醉 复苏 心肺复苏术 生物 生物化学 基因 小RNA
作者
Beth L. Pineles,Arunmani Mani,Livia Sura,Candace Rossignol,Sait Albayram,Michael D. Weiss,Laura Goetzl
出处
期刊:Archives of Disease in Childhood-fetal and Neonatal Edition [BMJ]
卷期号:107 (1): 60-64 被引量:18
标识
DOI:10.1136/archdischild-2020-321096
摘要

Central nervous system (CNS) derived exosomes can be purified from peripheral blood and have been used widely in adult neurological disease. Application to neonatal neurological disease deserves investigation in the setting of hypoxic-ischaemic encephalopathy (HIE).Observational cohort.Level III neonatal intensive care unit.Term/near-term neonates undergoing therapeutic hypothermia (TH) for HIE.Blood samples were collected at 0-6, 12, 24, 48 and 96 hours of life.CNS exosomes were purified from serum using previously described methods. Biomarker protein levels were quantified using standard ELISA methods and normalised to exosome marker CD-81. The slope of change for biomarker levels was calculated for each time interval. Our primary outcome was MRI basal ganglia/watershed score of ≥3.26 subjects were included (umbilical artery pH range 6.6-7.29; 35% seizures). An increasing MRI injury score was significantly associated with decreasing levels of synaptopodin between 0-6 and 12 hours (p=0.03) and increasing levels of lipocalin-2 (NGAL) between 12 and 48 hours (p<0.0001). Neuronal pentraxin was not significant. The negative predictive values for increasing synaptopodin and decreasing NGAL was 70.0% and 90.9%, respectively.Our results indicate that CNS exosome cargo has the potential to act as biomarkers of the severity of brain injury and response to TH as well as quantify pharmacological response to neuroactive therapeutic/adjuvant agents. Rigorous prospective trials are critical to evaluate potential clinical use of exosome biomarkers.
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