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创伤性脑损伤所致凝血病的病理生理学与伴有高纤维蛋白溶解的弥散性血管内凝血相同。

Pathophysiology of Coagulopathy Induced by Traumatic Brain Injury Is Identical to That of Disseminated Intravascular Coagulation With Hyperfibrinolysis.

作者信息

Wada Takeshi, Shiraishi Atsushi, Gando Satoshi, Yamakawa Kazuma, Fujishima Seitaro, Saitoh Daizoh, Kushimoto Shigeki, Ogura Hiroshi, Abe Toshikazu, Mayumi Toshihiko, Sasaki Junichi, Kotani Joji, Takeyama Naoshi, Tsuruta Ryosuke, Takuma Kiyotsugu, Shiraishi Shin-Ichiro, Shiino Yasukazu, Nakada Taka-Aki, Okamoto Kohji, Sakamoto Yuichiro, Hagiwara Akiyoshi, Fujimi Satoshi, Umemura Yutaka, Otomo Yasuhiro

机构信息

Division of Acute and Critical Care Medicine, Department of Anesthesiology and Critical Care Medicine, Hokkaido University Faculty of Medicine, Sapporo, Japan.

Emergency and Trauma Center, Kameda Medical Center, Kamogawa, Japan.

出版信息

Front Med (Lausanne). 2021 Nov 15;8:767637. doi: 10.3389/fmed.2021.767637. eCollection 2021.

Abstract

Traumatic brain injury (TBI)-associated coagulopathy is a widely recognized risk factor for secondary brain damage and contributes to poor clinical outcomes. Various theories, including disseminated intravascular coagulation (DIC), have been proposed regarding its pathomechanisms; no consensus has been reached thus far. This study aimed to elucidate the pathophysiology of TBI-induced coagulopathy by comparing coagulofibrinolytic changes in isolated TBI (iTBI) to those in non-TBI, to determine the associated factors, and identify the clinical significance of DIC diagnosis in patients with iTBI. This secondary multicenter, prospective study assessed patients with severe trauma. iTBI was defined as Abbreviated Injury Scale (AIS) scores ≥4 in the head and neck, and ≤2 in other body parts. Non-TBI was defined as AIS scores ≥4 in single body parts other than the head and neck, and the absence of AIS scores ≥3 in any other trauma-affected parts. Specific biomarkers for thrombin and plasmin generation, anticoagulation, and fibrinolysis inhibition were measured at the presentation to the emergency department (0 h) and 3 h after arrival. We analyzed 34 iTBI and 40 non-TBI patients. Baseline characteristics, transfusion requirements and in-hospital mortality did not significantly differ between groups. The changes in coagulation/fibrinolysis-related biomarkers were similar. Lactate levels in the iTBI group positively correlated with DIC scores (rho = -0.441, = 0.017), but not with blood pressure (rho = -0.098, = 0.614). Multiple logistic regression analyses revealed that the injury severity score was an independent predictor of DIC development in patients with iTBI (odds ratio = 1.237, = 0.018). Patients with iTBI were further subdivided into two groups: DIC ( = 15) and non-DIC ( = 19) groups. Marked thrombin and plasmin generation were observed in all patients with iTBI, especially those with DIC. Patients with iTBI and DIC had higher requirements for massive transfusion and emergency surgery, and higher in-hospital mortality than those without DIC. Furthermore, DIC development significantly correlated with poor hospital survival; DIC scores at 0 h were predictive of in-hospital mortality. Coagulofibrinolytic changes in iTBI and non-TBI patients were identical, and consistent with the pathophysiology of DIC. DIC diagnosis in the early phase of TBI is key in predicting the outcomes of severe TBI.

摘要

创伤性脑损伤(TBI)相关凝血病是继发性脑损伤广泛认可的危险因素,且会导致不良临床结局。关于其发病机制已提出了包括弥散性血管内凝血(DIC)在内的各种理论;但迄今为止尚未达成共识。本研究旨在通过比较孤立性TBI(iTBI)与非TBI患者的凝血纤溶变化,阐明TBI诱导凝血病的病理生理学,以确定相关因素,并明确iTBI患者DIC诊断的临床意义。这项多中心、前瞻性的二次研究评估了严重创伤患者。iTBI定义为头颈部简明损伤量表(AIS)评分≥4分,其他身体部位评分≤2分。非TBI定义为头颈部以外单一身体部位AIS评分≥4分,且其他任何受创伤部位AIS评分均<3分。在急诊科就诊时(0小时)及到达后3小时测量凝血酶和纤溶酶生成、抗凝及纤溶抑制的特定生物标志物。我们分析了34例iTBI患者和40例非TBI患者。两组患者的基线特征、输血需求和院内死亡率无显著差异。凝血/纤溶相关生物标志物的变化相似。iTBI组的乳酸水平与DIC评分呈正相关(rho = -0.441,P = 0.017),但与血压无关(rho = -0.098,P = 0.614)。多因素logistic回归分析显示,损伤严重程度评分是iTBI患者DIC发生的独立预测因素(比值比 = 1.237,P = 0.018)。iTBI患者进一步分为两组:DIC组(n = 15)和非DIC组(n = 19)。在所有iTBI患者中均观察到明显的凝血酶和纤溶酶生成,尤其是DIC患者。与无DIC的患者相比,iTBI合并DIC的患者大量输血和急诊手术需求更高,院内死亡率也更高。此外,DIC的发生与不良的医院生存率显著相关;0小时时的DIC评分可预测院内死亡率。iTBI和非TBI患者的凝血纤溶变化相同,且与DIC的病理生理学一致。TBI早期诊断DIC是预测重度TBI预后的关键。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1a08/8634586/502a7e836904/fmed-08-767637-g0001.jpg

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