Pediatric Swine Model of Methicillin-Resistant Staphylococcus aureus Sepsis-Induced Coagulopathy, Disseminated Microvascular Thrombosis, and Organ Injuries.

Critical Care Explorations Pub Date : 2023-05-26 eCollection Date: 2023-06-01 DOI:10.1097/CCE.0000000000000916
Trung C Nguyen, Juan C Marini, Bobby Guillory, Christian Valladolid-Brown, Marina Martinez-Vargas, Deepika Subramanyam, Daniel Cohen, Sonya C Cirlos, Fong Lam, Barbara Stoll, Inka C Didelija, Caitlin Vonderohe, Renan Orellana, Arun Saini, Subhashree Pradhan, Dalia Bashir, Moreshwar S Desai, Saul Flores, Manpreet Virk, Hossein Tcharmtchi, Amir Navaei, Sheldon Kaplan, Linda Lamberth, Kristina G Hulten, Brooks P Scull, Carl E Allen, Ayse Akcan-Arikan, K Vinod Vijayan, Miguel A Cruz
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Abstract

Sepsis-induced coagulopathy leading to disseminated microvascular thrombosis is associated with high mortality and has no existing therapy. Despite the high prevalence of Gram-positive bacterial sepsis, especially methicillin-resistant Staphylococcus aureus (MRSA), there is a paucity of published Gram-positive pediatric sepsis models. Large animal models replicating sepsis-induced coagulopathy are needed to test new therapeutics before human clinical trials.

Hypothesis: Our objective is to develop a pediatric sepsis-induced coagulopathy swine model that last 70 hours.

Methods and models: Ten 3 weeks old piglets, implanted with telemetry devices for continuous hemodynamic monitoring, were IV injected with MRSA (n = 6) (USA300, Texas Children's Hospital 1516 strain) at 1 × 109 colony forming units/kg or saline (n = 4). Fluid resuscitation was given for heart rate greater than 50% or mean arterial blood pressure less than 30% from baseline. Acetaminophen and dextrose were provided as indicated. Point-of-care complete blood count, prothrombin time (PT), activated thromboplastin time, d-dimer, fibrinogen, and specialized coagulation assays were performed at pre- and post-injection, at 0, 24, 48, 60, and 70 hours. Piglets were euthanized and necropsies performed.

Results: Compared with the saline treated piglets (control), the septic piglets within 24 hours had significantly lower neurologic and respiratory scores. Over time, PT, d-dimer, and fibrinogen increased, while platelet counts and activities of factors V, VII, protein C, antithrombin, and a disintegrin and metalloproteinase with thrombospondin-1 motifs (13th member of the family) (ADAMTS-13) decreased significantly in septic piglets compared with control. Histopathologic examination showed minor focal organ injuries including microvascular thrombi and necrosis in the kidney and liver of septic piglets.

Interpretations and conclusions: We established a 70-hour swine model of MRSA sepsis-induced coagulopathy with signs of consumptive coagulopathy, disseminated microvascular thrombosis, and early organ injuries with histological minor focal organ injuries. This model is clinically relevant to pediatric sepsis and can be used to study dysregulated host immune response and coagulopathy to infection, identify potential early biomarkers, and to test new therapeutics.

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耐甲氧西林金黄色葡萄球菌败血症诱发凝血病、弥散性微血管血栓和器官损伤的小猪模型
败血症诱发的凝血病导致弥散性微血管血栓形成,死亡率很高,而且目前还没有治疗方法。尽管革兰氏阳性细菌败血症的发病率很高,尤其是耐甲氧西林金黄色葡萄球菌(MRSA),但已发表的革兰氏阳性儿科败血症模型却很少。在人体临床试验之前,需要复制败血症诱发凝血病的大型动物模型来测试新疗法:我们的目标是建立一个持续 70 小时的小儿败血症诱发凝血病猪模型:方法和模型:10头3周大的小猪,植入遥测装置以持续监测血流动力学,静脉注射1×109菌落形成单位/千克的MRSA(n = 6)(USA300,德克萨斯儿童医院1516株)或生理盐水(n = 4)。如果心率超过 50%,或平均动脉血压低于基线的 30%,则进行输液复苏。根据指示提供对乙酰氨基酚和葡萄糖。在注射前、注射后、0、24、48、60 和 70 小时时进行全血细胞计数、凝血酶原时间 (PT)、活化凝血活酶时间、d-二聚体、纤维蛋白原和专门的凝血测定。对仔猪实施安乐术并进行尸体解剖:结果:与生理盐水处理的仔猪(对照组)相比,24 小时内败血症仔猪的神经系统和呼吸系统评分明显降低。随着时间的推移,PT、d-二聚体和纤维蛋白原增加,而与对照组相比,败血症仔猪的血小板计数和因子 V、VII、蛋白 C、抗凝血酶以及具有凝血酶原-1 矩阵(家族第 13 个成员)的溶解酶和金属蛋白酶(ADAMTS-13)的活性明显降低。组织病理学检查显示,败血症仔猪的肾脏和肝脏存在轻微的病灶器官损伤,包括微血管血栓和坏死:我们建立了一个 70 小时的 MRSA 败血症诱发凝血病的猪模型,该模型具有消耗性凝血病、弥散性微血管血栓形成和早期器官损伤的迹象,组织病理学显示有轻微的病灶器官损伤。该模型与小儿败血症临床相关,可用于研究宿主对感染的失调免疫反应和凝血病,确定潜在的早期生物标志物,以及测试新疗法。
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