A systematic review on the rotational thrombelastometry (ROTEM®) values for the diagnosis of coagulopathy, prediction and guidance of blood transfusion and prediction of mortality in trauma patients

In a study conducted by Rugeri [36], thresholds were determined by evaluating the extent of correlation between ROTEM® parameters with corresponding SCTs (CA15-EXTEM with PT: r = 0.66, p < 0.0001); clot formation time [CFT]-INTEM with aPTT: r = 0.91, p < 0.0001; CA10-FIBTEM with fibrinogen level: r = 0.85, p < 0.0001; CA15-INTEM with PLT count: r = 0.57, p < 0.0001). The group found cut-off values of EXTEM CA15 < 32 mm and FIBTEM CA10 < 5 mm to detect laboratory PT > 1.5 and fibrinogen level <1 g/L, with high sensitivity (87 % and 91 %) and specificity (100 and 85 %), respectively. In another study, Levrat determined the cut off values by assessing correlation between ROTEM® parameters and euglobin lysis time (ELT), used as the gold standard control [37]. In this study, a threshold of 18 mm (MCF-EXTEM), 71 % (CLI30) AND 7 % increase of MCF-APTEM, sensitivity was, 100, 75 and 80 %, respectively with a specificity of 100 %. Moreover, Davenport [41] and Rourke [42] used ROTEM® CA5 < 35 mm as threshold based on correlation with normal PT values to discriminate normal from the abnormal curves in patients with ACoTS. Hagemo used ROTEM® threshold value of EXTEM CA5 ≤ 37 mm and FIBTEM A5 ≤ 8 mm to detect ACoTS [43]. These authors used INR > 1.2 and fibrinogen concentration of ≤1.61 g/L to define ACoTS, respectively [43]. A feasibility study [25] in a deployed military trauma setting demonstrated that an abnormal CA10 was associated with a subsequent development of an abnormal MCF (<45 mm). MCF <45 mm was present in a 100 % of MT patients. When PT > 18 s and aPTT >60s were used as the gold standard for ACoTS, only 10.5 % of patients were defined as coagulopathic. By comparing these results with ROTEM® results, it was found that 64 % were coagulopathic (FIBTEM-MCF < 45 mm), (p = 0.0005). Another study [41] reported that the threshold EXTEM CA5 ≤ 35 mm predicted INR > 1.2 in 77 % of cases. In TBI patients, Schochl [39] reported a cut off value of EXTEM-CT > 80s, compared to PTI < 70 %, to define coagulopathy (p = 0.003). Finally, in another study in the military setting [30] the authors compared PT > 18 s (gold standard) to diagnose coagulopathy and identified that early CA5 < 32 mm and CA10 < 40 mm predicted the hypocoagulation state with a sensitivity/specificity of CA5 96/58 % and CA10 100/70 %, respectively, compared to SCTs.

Two studies investigated the use of FIBTEM CA10 < 5 mm and FIBTEM CA5 < 10 mm for diagnosing different degrees of hypofibrinogenemia. In the first study [36], FIBTEM CA10 < 5 mm diagnosed fibrinogen levels below 1.0 g/L with sensitivity of 87 % and specificity of 91 %. The second study [42] reported EXTEM CA5 < 36 mm with a sensitivity of 53 % and specificity of 87 % for discerning patients with fibrinogen levels <1.5 g/L. For FIBTEM CA5 < 10 mm, the reported sensitivity and specificity were 78 and 70 % respectively for predicting a fibrinogen level below 1.5 g/L.

Three studies [26, 37, 40] reported thresholds of different ROTEM® parameters to diagnose degrees of hyperfibrinolysis (HF) such as mild, moderate and fulminant. Two studies [26, 37] compared their findings with SCTs. The first study [37] defined HF as euglobulin lysis time (ELT) <90 min (used as gold standard) in a series of 23 patients. The authors used EXTEM MCF ≤ 18 mm, clot lysis index at 30 min (CLI30) < 71 % and APTEM MCF 7 % increase to define hyperfibrinolysis (HF) (sensitivity 100, 75, 80 % and specificity 100 % for all, respectively) in these patients with an abnormal ELT test. The second study [26] enrolled 33 trauma patients diagnosed with HF by ROTEM®. They used clot lysis in EXTEM and INTEM assays at different time points across the ROTEM® tracing to define the three patterns of HF, confirmed by the APTEM test. A complete clot lysis (ML = 100 %) within 30 min was used to define patients with fulminant HF; complete clot lysis between 30 and 60 min defined intermediate HF and complete clot lysis after 1 h to define late HF. The median values of laboratory fibrinogen was lower in fulminant HF group and intermediate HF group when compared with late HF group (fulminant HF: 0.5 g/L; intermediate HF: 0.49 g/L compared with late HF 1.04 g/L, p = 0.048 for both).

A single study [36] evaluated the correlation between platelet count and INTEM CA15 (r = 0.57, p < 0.0001). However, the threshold value of INTEM CA15 = 46 mm showed poor positive predictive (PPV) values in the diagnosis of laboratory platelet count below 50 × 10⁻⁹L⁻¹ (sensitivity: 100 % [95 % CI 71–100], specificity 83 % [95 % CI 82–83]; PPV 17 % [95 % CI 12–17], negative predictive value [NPV] 100 % [95 % CI 98–100]; AUC 0.92).

Six studies reported ROTEM® thresholds either in predicting transfusion [28, 38, 40, 41, 43], including MT [28, 38, 41, 43], or guiding transfusion [27] (Table 5). Massive transfusion was defined by the need for transfusion of ≥10U of RBCs within the first 12 h [41] or 24 h [28, 38] of hospital admission in three studies. Values outside the reference range for EXTEM and INTEM CT, CFT, CA at 10, 20 and 30 min, as well as reduced MCF were more likely in patients who required a MT vs. patients who did not (p < 0.0001, for all) [28, 38]. The reference ranges used in this study were the same established by the same group, in a previous study that used SCTs as control [26].

Davenport [41] demonstrated that EXTEM CA5 ≤ 35 mm predicted the need for MT with higher detection rate compared to INR > 1.2 (71 vs. 43 %, p < 0.001). Schochl [28], using threshold pre-established in a previous study by the same group [26] reported that both FIBTEM A10 ≤ 4 mm (ROC AUC = 0.83) and FIBTEM MCF ≤ 7 mm (ROC AUC = 0.84) were predictive of the need for MT. Lastly, Hagemo [43] demonstrated that threshold values of EXTEM CA5 ≤ 40 mm predicted MT in 72.7 % and FIBTEM CA5 ≤ 9 mm predicted MT in 77.5 %, respectively. However detection rate for MT was found to be highest for INR, as compared to EXTEM CA5 (51.1 and 45.5 %, respectively). The optimum threshold value for fibrinogen in predicting MT was ≤1.90 g/L with a detection rate of 77.8 % and a positive predictive value of 14.

Schochl [27], in a retrospective analysis of trauma patients who received ≥5U RBCs within 24 h, and whose coagulation management was guided by ROTEM®, developed a clinical practice guideline using thresholds of ROTEM® parameters to guide transfusion. The group used a threshold of FIBTEM MCF < 10 mm to guide transfusion of fibrinogen concentrate (FC) and used EXTEM CT > 1.5 times normal to guide PCC administration. Reference ranges used for these ROTEM® tests’ parameters were previously determined in a multi-center investigation by Lang [45]. The authors were able to demonstrate a reduction in the number of RBC units transfused. The use of RBC units was avoided in 29 % of patients receiving FC and PCC therapy compared to only 3 % avoided in the group receiving fresh frozen plasma (FFP) (p < 0.001).

Six studies evaluated ROTEM® thresholds in predicting mortality (Table 6) [26, 27, 37, 39, 40, 42]. These studies evaluated mortality at different time points, including: within 24 h of arrival [40]; death in hospital [26, 40]; death within 24 h and 28 days [42], 30 days [40], and two studies did not define the time to death [27, 37]. Two studies reported that trauma patients with the diagnosis of HF had higher rates of mortality [26, 37]. The studies defined HF differently: Schochl defined HF as a complete clot lysis (ML = 100 %) on ROTEM® at different time intervals as fulminant HF, intermediate HF and late HF as described above [26]. Finally, Levrat defined HF as an ELT < 90 min. [37] We describe here under the studies that adjusted their findings for confounders, or compared findings with previously validated trauma scores [46, 47]. The full description of the evidence is on Table 6.

Tauber [40] found a significant increase in mortality with FIBTEM < 7 mm (21 vs. 9 %, p = 0.006) and EXTEM MCF < 45 mm (25.4 vs 9.4 %, p < 0.001). Similarly, EXTEM MCF was independently and negatively associated with early mortality (OR 0.94, 95 % CI 0.9–0.99). The author additionally reported 85.7 % mortality in patients with fulminant HF (ML100% within 30 min), and 11.1 % mortality in patients with moderate HF (ML100% between 30 and 60 min). Rourke [42] reported that a low FIBTEM A5 < 9.5 mm was an independent predictor of 24 h and 28 days mortality (p < 0.001).

In a study in brain injury patients, Schochl [39] demonstrated an independent association between FIBTEM MCF < 9 mm (ROC: 0.77; 95 % CI, 0.665–0.850, p < 0.001) and aPTT > 35 s (ROC 0.79; 95 % CI 0.686–0.868, p < 0.001), and mortality. Moreover, in this study, ROTEM® revealed shorter CT in EXTEM and INTEM (p < 0.001), shorter CFT in EXTEM and INTEM (p < 0.0001), and higher MCF in EXTEM and INTEM (p < 0.01) in survivors compared with non-survivors. Finally, in another study conducted the Schochl [27], where trauma patient resuscitation was guided by ROTEM® with FC and PCC, a reduction in the observed mortality than the predicted mortality by TRISS and RSS was demonstrated (24.4 vs. 33.7 %, p = 0.032).