TY - JOUR
T1 - Association of antithrombin with development of trauma-induced disseminated intravascular coagulation and outcomes
AU - JAAM FORECAST group
AU - Wada, Takeshi
AU - Shiraishi, Atsushi
AU - Gando, Satoshi
AU - Kabata, Daijiro
AU - Yamakawa, Kazuma
AU - Fujishima, Seitaro
AU - Saitoh, Daizoh
AU - Kushimoto, Shigeki
AU - Ogura, Hiroshi
AU - Abe, Toshikazu
AU - Mayumi, Toshihiko
AU - Otomo, Yasuhiro
N1 - Funding Information:
This study was supported by the Japanese Association for Acute Medicine (grant number JAAM, 2014-01). Acknowledgments
Funding Information:
We would like to thank Editage ( https://www.editage.com ) for English language editing. Unrelated to the submitted work, TW received research funding from Takeda Science Foundation.
Funding Information:
Keio University School of Medicine (Junichi Sasaki), Kobe University Graduate School of Medicine (Joji Kotani), Aichi Medical University Hospital (Naoshi Takeyama), Yamaguchi University Hospital (Ryosuke Tsuruta), Kawasaki Municipal Hospital (Kiyotsugu Takuma); Kurume University (Norio Yamashita), Aizu Chuo Hospital (Shin-ichiro Shiraishi), Teikyo University School of Medicine (Hiroto Ikeda), Kawasaki Medical School (Yasukazu Shiino), Kyorin University School of Medicine (Takehiko Tarui), Chiba University Graduate School of Medicine (Takaaki Nakada), St. Luke’s International Hospital (Toru Hifumi), Kitakyushu City Yahata Hospital (Kohji Okamoto), Saga University Hospital (Yuichiro Sakamoto), Center Hospital of the National Center for Global Health and Medicine (Akiyoshi Hagiwara), Nippon Medical School (Tomohiko Masuno), Community Healthcare Organization, Chukyo Hospital (Masashi Ueyama), Osaka General Medical Center (Satoshi Fujimi, Yutaka Umemura), and the JAAM FORECAST Trauma investigators: Osaka City University Hospital (Yasumitsu Mizobata); National Hospital Organization Sendai Medical Center (Yasuo Yamada); Saitama Medical University Saitama Medical Center (Satoru Sugiyama); Fukui Prefectural Hospital (Hiroshi Ishida); Sapporo Medical University (Eichi Narimatsu); Fukuyama City Hospital (Koji Miyasho); Hiratsuka City Hospital (Toshio Kanai); Saiseikai Utsunomiya Hospital (Satoru Miyatake); Japanese Red Cross Society Kyoto Daini Hospital (Ryouji Iiduka); Shinsyu University School of Medicine (Hiroshi Imamura); Rinku General Medical Center (Yasuaki Mizushima); Subaru Health Insurance Society Ota Memorial Hospital (Yoshitake Sato); Saitama Medical University International Medical Center (Manabu Nemoto); Aomori Prefectural Central Hospital (Hiroyuki Hanada); National Hospital Organization Hokkaido Medical Center (Yasuo Shichinohe); Saga-ken Medical Centre Koseikan (Kenji Hirahara); Hachinohe City Hospital (Akihide Kon); Juntendo University Nerima Hospital (Manabu Sugita); Kawaguchi Municipal Medical Center (Yasutaka Naoe); Kakogawa West City Hospital (Manabu Kirita); Osaka National Hospital (Daikai Sadamitsu); Kouseiren Takaoka Hospital (Masahiro Yoshida). Additionally, the JAAM FORECST Study Group thanks Shuta Fukuda for his special assistance in completing the study. This study was supported by the JAAM.
Publisher Copyright:
Copyright © 2022 Wada, Shiraishi, Gando, Kabata, Yamakawa, Fujishima, Saitoh, Kushimoto, Ogura, Abe, Mayumi and Otomo.
PY - 2022/12/9
Y1 - 2022/12/9
N2 - Introduction: Trauma activates the innate immune system to modulate hemostasis and minimize the damage caused by physiological bodily responses, including the activation of coagulation. Sufficiently severe trauma overwhelms physiological responses and elicits the systemic inflammatory response syndrome, which leads to the onset of disseminated intravascular coagulation (DIC), characterized by dysregulated inflammatory coagulofibrinolytic responses. Impaired anticoagulant mechanisms, including antithrombin, constitutes the pathology of DIC, while the dynamics of antithrombin and relevance to outcomes in trauma-induced coagulopathy have not been fully elucidated. This study investigated the associations of antithrombin activity with DIC onset and outcomes in severely injured patients. Methods: This retrospective sub-analysis of a multicenter, prospective study included patients with an injury severity score ≥16. We characterized trauma patients with low antithrombin activity (antithrombin <80% on hospital arrival, n = 75) in comparison with those who had normal antithrombin activity (antithrombin ≥80%, n = 200). Global markers of coagulation and fibrinolysis, molecular biomarkers for thrombin generation (soluble fibrin [SF]), and markers of anticoagulation (antithrombin) were evaluated to confirm the associations of antithrombin with DIC development and outcomes, including in-hospital mortality and the multiple organ dysfunction syndrome (MODS). Results: Patients with low antithrombin activity had higher prevalence of shock, transfusion requirements, and in-hospital mortality. Higher DIC scores and more severe organ dysfunction were observed in the low AT group compared to that in the normal AT group. Antithrombin activity on arrival at the hospital was an independent predictor of the development of DIC in trauma patients, and levels of SF increased with lower antithrombin values (antithrombin activity > 85%). Antithrombin activity at 3 h showed good predictive performance for in-hospital mortality, and a multivariable Cox proportional-hazard regression model with a cross-product term between the antithrombin and DIC showed that the in-hospital mortality in patients with DIC increased with decreased antithrombin activity. A multivariable logistic regression model showed that the odds for the development of MODS in patients with DIC increased with lower antithrombin values. Conclusion: Decreased antithrombin activity in trauma-induced coagulopathy is associated with poor outcomes through worsening of DIC.
AB - Introduction: Trauma activates the innate immune system to modulate hemostasis and minimize the damage caused by physiological bodily responses, including the activation of coagulation. Sufficiently severe trauma overwhelms physiological responses and elicits the systemic inflammatory response syndrome, which leads to the onset of disseminated intravascular coagulation (DIC), characterized by dysregulated inflammatory coagulofibrinolytic responses. Impaired anticoagulant mechanisms, including antithrombin, constitutes the pathology of DIC, while the dynamics of antithrombin and relevance to outcomes in trauma-induced coagulopathy have not been fully elucidated. This study investigated the associations of antithrombin activity with DIC onset and outcomes in severely injured patients. Methods: This retrospective sub-analysis of a multicenter, prospective study included patients with an injury severity score ≥16. We characterized trauma patients with low antithrombin activity (antithrombin <80% on hospital arrival, n = 75) in comparison with those who had normal antithrombin activity (antithrombin ≥80%, n = 200). Global markers of coagulation and fibrinolysis, molecular biomarkers for thrombin generation (soluble fibrin [SF]), and markers of anticoagulation (antithrombin) were evaluated to confirm the associations of antithrombin with DIC development and outcomes, including in-hospital mortality and the multiple organ dysfunction syndrome (MODS). Results: Patients with low antithrombin activity had higher prevalence of shock, transfusion requirements, and in-hospital mortality. Higher DIC scores and more severe organ dysfunction were observed in the low AT group compared to that in the normal AT group. Antithrombin activity on arrival at the hospital was an independent predictor of the development of DIC in trauma patients, and levels of SF increased with lower antithrombin values (antithrombin activity > 85%). Antithrombin activity at 3 h showed good predictive performance for in-hospital mortality, and a multivariable Cox proportional-hazard regression model with a cross-product term between the antithrombin and DIC showed that the in-hospital mortality in patients with DIC increased with decreased antithrombin activity. A multivariable logistic regression model showed that the odds for the development of MODS in patients with DIC increased with lower antithrombin values. Conclusion: Decreased antithrombin activity in trauma-induced coagulopathy is associated with poor outcomes through worsening of DIC.
KW - antithrombin
KW - disseminated intravascular coagulation
KW - innate immunity
KW - soluble fibrin
KW - thrombin
KW - trauma-induced coagulopathy
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U2 - 10.3389/fimmu.2022.1026163
DO - 10.3389/fimmu.2022.1026163
M3 - Article
C2 - 36569855
AN - SCOPUS:85144637100
SN - 1664-3224
VL - 13
JO - Frontiers in Immunology
JF - Frontiers in Immunology
M1 - 1026163
ER -