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首页> 美国卫生研究院文献>Journal of Neurotrauma >GFAP-BDP as an Acute Diagnostic Marker in Traumatic Brain Injury: Results from the Prospective Transforming Research and Clinical Knowledge in Traumatic Brain Injury Study
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GFAP-BDP as an Acute Diagnostic Marker in Traumatic Brain Injury: Results from the Prospective Transforming Research and Clinical Knowledge in Traumatic Brain Injury Study

机译:GFAP-BDP作为创伤性脑损伤的急性诊断标志物:前瞻性转化研究和创伤性脑损伤研究的临床知识的结果

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Reliable diagnosis of traumatic brain injury (TBI) is a major public health need. Glial fibrillary acidic protein (GFAP) is expressed in the central nervous system, and breakdown products (GFAP-BDP) are released following parenchymal brain injury. Here, we evaluate the diagnostic accuracy of elevated levels of plasma GFAP-BDP in TBI. Participants were identified as part of the prospective Transforming Research And Clinical Knowledge in Traumatic Brain Injury (TRACK-TBI) Study. Acute plasma samples (<24 h post-injury) were collected from patients presenting with brain injury who had CT imaging. The ability of GFAP-BDP level to discriminate patients with demonstrable traumatic lesions on CT, and with failure to return to pre-injury baseline at 6 months, was evaluated by the area under the receiver operating characteristic curve (AUC). Of the 215 patients included for analysis, 83% had mild, 4% had moderate, and 13% had severe TBI; 54% had acute traumatic lesions on CT. The ability of GFAP-BDP level to discriminate patients with traumatic lesions on CT as evaluated by AUC was 0.88 (95% confidence interval [CI], 0.84–0.93). The optimal cutoff of 0.68 ng/mL for plasma GFAP-BDP level was associated with a 21.61 odds ratio for traumatic findings on head CT. Discriminatory ability of unfavorable 6 month outcome was lower, AUC 0.65 (95% CI, 0.55–0.74), with a 2.07 odds ratio. GFAP-BDP levels reliably distinguish the presence and severity of CT scan findings in TBI patients. Although these findings confirm and extend prior studies, a larger prospective trial is still needed to validate the use of GFAP-BDP as a routine diagnostic biomarker for patient care and clinical research. The term “mild” continues to be a misnomer for this patient population, and underscores the need for evolving classification strategies for TBI targeted therapy. (ClinicalTrials.gov number ; NIH Grant 1RC2 NS069409)
机译:对创伤性脑损伤(TBI)的可靠诊断是主要的公共卫生需求。胶质纤维酸性蛋白(GFAP)在中枢神经系统中表达,并且在实质性脑损伤后释放分解产物(GFAP-BDP)。在这里,我们评估了血浆TBI中GFAP-BDP水平升高的诊断准确性。参与者被确定为创伤性脑损伤的前瞻性转化研究和临床知识(TRACK-TBI)研究的一部分。从患有脑损伤的CT成像患者中收集急性血浆样品(损伤后<24小时)。通过接受者工作特征曲线(AUC)下的面积评估了GFAP-BDP水平区分CT上可证实的外伤性病变并在6个月内未能恢复到损伤前基线的患者的能力。纳入分析的215名患者中,轻度TBI为83%,中度为4%,重度TBI为13%。 54%的患者在CT上有急性创伤性病变。通过AUC评估,GFAP-BDP水平对CT上有创伤性病变的患者的区分能力为0.88(95%置信区间[CI],0.84–0.93)。血浆GFAP-BDP水平的最佳临界值0.68 ng / mL与头部CT上的创伤发现的21.61比值比相关。不利的6个月结局的判别能力较低,AUC为0.65(95%CI,0.55-0.74),优势比为2.07。 GFAP-BDP水平可可靠地区分TBI患者CT扫描结果的存在和严重性。尽管这些发现证实并扩展了先前的研究,但仍需要进行更大的前瞻性试验,以验证将GFAP-BDP用作患者护理和临床研究的常规诊断生物标记物。 “轻度”一词仍然是该患者人群的误称,并强调了针对TBI靶向治疗的分类策略不断发展的需求。 (ClinicalTrials.gov编号; NIH授予1RC2 NS069409)

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