首页> 美国卫生研究院文献>Journal of Neurotrauma >Predicting Progressive Hemorrhagic Injury after Traumatic Brain Injury: Derivation and Validation of a Risk Score Based on Admission Characteristics
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Predicting Progressive Hemorrhagic Injury after Traumatic Brain Injury: Derivation and Validation of a Risk Score Based on Admission Characteristics

机译:预测脑外伤后进行性出血性出血:基于入院特征的风险评分的推导和验证

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摘要

Previous studies have demonstrated that patients with traumatic brain injury (TBI) who also have progressive hemorrhagic injury (PHI), have a higher risk of clinical deterioration and worse outcomes than do TBI patients without PHI. Therefore, the early prediction of PHI occurrence is useful to evaluate the status of patients with TBI and to improve outcomes. The objective of this study was to develop and validate a prognostic model that uses information available at admission to determine the likelihood of PHI after TBI. Retrospectively collected data were used to develop a PHI prognostic model with a logistic regression analysis. The prediction model was validated in 114 patients from a separate hospital. Eight independent prognostic factors were identified: age ≥57 years (5 points), intra-axial bleeding/brain contusion (4 points), midline shift≥5 mm (6 points), platelet (PLT) count<100×109/L (10 points), PLT count≥100 but <150×109/L (4 points), prothrombin time>14 sec (7 points), D-dimer≥5 mg/L (12 points), and glucose≥10 mmol/L (10 points). Each patient was assigned a number of points proportional to the regression coefficient. We calculated risk scores for each patient and defined three risk groups: low risk (0–13 points), intermediate risk (14–22 points), and high risk (23–54 points). In the development cohort, the PHI rates after TBI for these three groups were 10.3%, 47.3%, and 85.2%, respectively. In the validation cohort, the corresponding PHI rates were 10.9%, 47.3%, and 86.9%. The C-statistic for the point system was 0.864 (p=0.509 by the Hosmer-Lemeshow test) in the development cohort, and 0.862 (p=0.589 by the Hosmer-Lemeshow test) in the validation cohort. In conclusion, a relatively simple risk score using admission predictors accurately predicted the risk for PHI after TBI.
机译:先前的研究表明,与没有PHI的TBI患者相比,还具有进行性出血性损伤(PHI)的外伤性脑损伤(TBI)患者具有更高的临床恶化风险和更差的预后。因此,对PHI发生的早期预测有助于评估TBI患者的状况并改善结局。这项研究的目的是开发和验证一种预后模型,该模型使用入院时可获得的信息来确定TBI后发生PHI的可能性。回顾性收集的数据用于通过逻辑回归分析建立PHI预后模型。在另一家医院的114名患者中验证了该预测模型。确定了八个独立的预后因素:年龄≥57岁(5分),轴内出血/脑挫伤(4分),中线移位≥5mm(6分),血小板(PLT)计数<100×10 9 / L(10分),PLT计数≥100但<150×10 9 / L(4分),凝血酶原时间> 14 sec(7分),D-二聚体≥ 5 mg / L(12分),葡萄糖≥10mmol / L(10分)。为每个患者分配与回归系数成比例的多个点。我们计算了每位患者的风险评分,并定义了三个风险组:低风险(0–13分),中风险(14–22分)和高风险(23–54分)。在发展队列中,这三组在TBI之后的PHI发生率分别为10.3%,47.3%和85.2%。在验证队列中,相应的PHI率分别为10.9%,47.3%和86.9%。在开发队列中,点系统的C统计量为0.864(通过Hosmer-Lemeshow检验,p = 0.509),在验证队列中为0.862(通过Hosmer-Lemeshow检验,p = 0.589)。总之,使用入院预测因子的相对简单的风险评分可准确预测TBI后发生PHI的风险。

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