Background
Total knee arthroplasty (TKA) is usually performed to treat end-stage knee arthritis [
1]. However, this surgical procedure has been associated with postoperative hidden blood loss (HBL) [
2]. Tranexamic acid (TXA) effectively reduces HBL after TKA and is thus recommended for use as a routine antifibrinolytic agent in all TKA surgeries [
3]. Robust data from several large-scale multicenter randomized controlled trials (RCTs) have indicated that the timing is crucial and TXA should be administered soon after the onset of bleeding [
4‐
6]. Moreover, TXA should be empirically used in all cases of bleeding to reduce blood loss and decrease mortality [
4].
Nevertheless, recent evidence from the cases of traumatic and acute bleeding warns against the universal use of TXA after injury [
7]. A previous study has demonstrated various fibrinolytic phenotypes after injury and suggested that clinicians should not focus on the timing alone when considering TXA administration [
8]. Approximately 46% of patients reportedly present with pathologically downregulated fibrinolysis after injury, which is known as fibrinolytic shutdown (FSD) [
9]. Functioning as an antifibrinolytic agent, TXA inhibits the activity of the fibrinolytic system, stabilizes the formed clots that seal the broken vessels, and effectively reduces blood loss secondary to hyperfibrinolysis. Therefore, researchers argue that TXA may be administered with caution in bleeding patients presenting with FSD, as there was nothing to inhibit in fact, and this phenotype has been associated with an increased risk of venous thromboembolism (VTE) and postinjury mortality [
10,
11].
As mentioned earlier, TXA administration after TKA has been demonstrated to be beneficial for the patients [
2]. However, the aforementioned recent evidence poses some important questions: (1) Do patients exhibit similar but different fibrinolytic phenotypes after TKA? and (2) do all patients with different fibrinolytic phenotypes benefit from antifibrinolytic therapy after TKA? Therefore, this study aimed to evaluate the efficacy of TXA in patients presenting with distinct fibrinolytic phenotypes after TKA.
Methods
Study design
This is a retrospective study. All patients consecutively admitted to our center between September 2016 and November 2019 for TKA were screened for eligibility. All eligible patients received 1.5 g of intravenous TXA 30 min before incision and 1 g of topical TXA before wound closure during TKA. Patients who received no postoperative TXA constituted Group A, whereas those who received postoperative TXA (1 g of intravenous TXA at 3, 12, 24, 48, and 72 h after surgery) constituted Group B. The two groups were further divided into a total of four subgroups based on postoperative fibrinolytic phenotypes (non-FSD [NFSD] or FSD): (1) NFSD, percentage of clot lysis 30 min after maximum strength (LY30) ≥ 0.8% on postoperative day 1 (POD1), and (2) FSD, LY30 < 0.8% on POD1.
Eligibility criteria
We applied strict inclusion and exclusion criteria to control the potential heterogeneity among the patients. Table
1 presents the specific inclusion and exclusion criteria.
Table 1
The inclusion and exclusion criteria
1. Receiving unilateral primary TKA due to end-stage knee diseases | 1. UKA |
2. Receiving pre- and intraoperative TXA or pre-, intra-, and postoperative TXA | 2. Bilateral TKA |
3. Preoperative hemoglobin level > 90 g/L | 3. Tumor-related TKA |
| 4. Revision TKA |
| 5. Combined with significant hepatic or renal dysfunction |
| 6. Combined with coagulation dysfunction preoperatively |
| 7. Combined with knee infection preoperatively |
Surgical procedure
Under general anesthesia, all patients underwent TKA performed by the same surgical team comprising three senior orthopedists. All TKA surgeries were performed following the paramedian approach with patients in the supine position. Pneumatic tourniquet with a set pressure of 30 mmHg was routinely applied throughout the duration of surgery.
Postoperative management
The indication for perioperative allogeneic blood transfusion (ABT) at our center is follows: (1) hemoglobin level < 70 g/L, with or without anemia symptoms, or (2) 70 g/L < hemoglobin level < 100 g/L, with anemia symptoms. As thromboprophylaxis, 4000 IU of low molecular weight heparin or 10 mg of rivaroxaban was administered daily after surgery. Patient-controlled analgesia and nerve block combined with selective cyclooxygenase-2 inhibitors (i.e., celecoxib and etoricoxib) were used for postoperative pain management. As postoperative infection prophylaxis, 1.5 g of cefuroxime sodium was administered twice daily from POD1 to POD3.
Outcome assessments
The primary outcomes of this study included HBL and decrease in the hemoglobin level (ΔHb). The former was calculated using formulas reported by Gross and Nadler [
12,
13]. The latter was calculated using perioperatively monitored hemoglobin levels. Moreover, the fibrin degradation product (FDP) level, D-dimer (D-D), prothrombin time (PT), and activated partial thromboplastin time (APTT) were determined as secondary outcomes. During their hospital stay, the aforementioned parameters of the patients were routinely evaluated on POD1, POD3, POD5, and POD7 at the Department of Clinical Laboratory of our medical center. In addition, data on other clinical characteristics such as sex, age, body mass index (BMI), and surgery duration were also collected and compared.
Thromboelastography
Thromboelastography (TEG) includes seven parameters: (1) reaction time (R), period to 2 mm amplitude, representing enzymatic reaction function; (2) kinetics (K), period from 2 to 20 mm amplitude, representing clot kinetics; (3) alpha angle (α-angle), slope between R and K, representing fibrinogen level; (4) maximum amplitude (MA), representing maximum platelet function; (5) percentage of clot lysis 30 min after MA (LY30), representing fibrinolytic activity; (6) estimated percent lysis within 30 min after MA, representing fibrinolytic activity; and (7) comprehensive coagulation index, representing a linear combination of R, K, α-angle, and MA values. TEG was performed using TEG® Hemostasis Analyzer, Model 5000 (Haemonetics Corporation, Braintree, MA, USA).
Sample size calculation
Sample size was determined using the PASS (version 11; NCSS, LLC. Kaysville, UT, USA) software. According to a previously published study [
2], the maximum ΔHb was 15.79 g/L after administration of a dosage of 1.5 g intravenous TXA 30 min before skin incision, 1 g of intra-articular TXA before wound closure, and 1 g of TXA at 3, 12, 24, 48, and 72 h after surgery. To detect a difference of 4 g/L in the maximum ΔHb, with a power of 0.90 and significance level of 0.05, 46 patients were needed per arm.
Statistical analysis
Excel (Microsoft Corporation, WA, USA) was used to collect and manage the study data, and SPSS version 24.0 (IBM Corporation, Armonk, NY, USA) was used to perform data analyses. The quantitative data were presented as mean ± standard deviation, whereas the qualitative data were presented as frequencies with percentages. Independent t test was used to detect the differences in normally distributed numerical values, whereas the Mann–Whitney U test was used to detect the differences in non-normally distributed numerical values. For qualitative parameters, Pearson's Chi-square or Fisher’s exact test was used. Statistical significance was set at a p value of < 0.05.
Discussion
Fibrinolysis is an essential physiological process that maintains hemostatic balance and prevents thrombosis [
14]. This process is activated concurrently with coagulation after injury and facilitates the removal of mature fibrin, thereby playing a role in hemostasis to prevent the extension of clots beyond the damaged areas [
14]. Pathologically upregulated fibrinolysis, known as hyperfibrinolysis, contributes to insufficient clotting and reduced hemostasis [
14]. Hyperfibrinolysis after injury is reportedly associated with increased blood loss, which occurs mainly during the first few hours after injury [
15]. During the last decade, several large-scale multicenter RCTs consistently suggested the timely use of antifibrinolytic agents such as TXA soon after the onset of bleeding considering its excellent efficacy in reducing blood loss and decreasing bleeding-related mortality [
4,
6]. Currently, TXA is widely recommended as a routine hemostatic agent for all bleeding patients.
Recent evidence from traumatic and bleeding patients, however, has cast doubt on the reasonability of the universal administration of TXA after injury. The fibrinolytic system is not always upregulated after injury but shows a biphasic response (activated or shutdown) [
16]. FSD is the most common fibrinolytic phenotype noted after injury, the incidence rate of which has been reported to approximately 59% [
17,
18]. Moreover, 70% of patients presenting with FSD could maintain this phenotype for up to 120 h after injury [
18]. Owing to the deficiency in fibrinolysis, this phenotype fails to promptly dissolve the excessive clots; it was found to be associated with an increased risk of VTE [
11]. Therefore, researchers suggest careful administration of TXA in patients presenting with FSD, for there was nothing to inhibit and may increase VTE risk instead [
19].
Existing evidence suggests that the surgical injury associated with TKA significantly activates the fibrinolytic system [
20]. Monitoring of the dynamic changes in the D-D level revealed that postoperative hyperfibrinolysis peaks within 24 h after surgery [
21]. Thus, sequential administration of TXA within 72 h after TKA may effectively inhibit fibrinolysis activity and reduce HBL [
2]. However, recent evidence regarding postinjury fibrinolysis reminds us that the D-D level may fail to act as an accurate parameter for fibrinolytic activity in real time or guide TXA administration.
The fibrinolytic system may be activated in the initial stages after trauma but eventually progress toward a state of shutdown by the time blood is drawn [
16,
22]. Given the prolonged residence of D-D in the circulation, assessing the hyperfibrinolysis state on the basis of its level may not be accurate [
23]. Notably, TEG, as a comprehensive test comprising both coagulation and fibrinolysis parameters, can evaluate the real-time coagulation and fibrinolytic activities [
24]. The seeming paradoxical phenomenon of the elevated D-D levels in injured patients and low fibrinolysis activity measured using TEG is speculated as occult fibrinolysis [
22]. Results obtained in the present study demonstrated the existence of occult fibrinolysis in patients who underwent TKA. Furthermore, we found that the fibrinolytic phenotypes after TKA were similar to those after trauma, with FSD accounting for majority of the cases (64.81%). Moreover, although the levels of FDP and D-D were comparable between the two groups, postoperative TXA exerted fairly different effects in patients presenting with different postoperative fibrinolytic phenotypes. Patients presenting with NFSD exhibited significantly lower HBL and ΔHb after postoperative antifibrinolytic therapy, whereas those presenting with FSD did not. This may be explained by the fact that TXA could only improve the fibrin clot strength of patients with NFSD but failed to strengthen that of those with FSD [
22]. Our study also showed that the D-D level failed to distinguish patients presenting with FSD or guide targeted therapeutic intervention. Instead, our findings showed that LY30 can be a promising parameter that provides a practicable method for the timely identification of patients who truly require postoperative TXA after TKA. Therefore, given the lack of evidence supporting the administration of antifibrinolytic agents such as TXA in the absence of a target to inhibit, we do not recommend administering TXA after TKA in patients presenting with FSD.
The present study has several limitations. First, this study was retrospective in nature. However, we applied strict inclusion and exclusion criteria to minimize potential bias. Second, we failed to determine dynamic changes in the LY30 level postoperatively because of the retrospective study design. Third, HBL was calculated using widely used formulas based on hematocrit levels, which can be easily influenced by perioperative rehydration strategies. However, the enrolled patients were admitted consecutively and received the same perioperative rehydration protocols. Thus, this should have little effect on the comparisons between groups. Finally, although previous studies have shown increased VTE risk after TXA administration in patients presenting with FSD, we could not obtain sufficient follow-up data to further assess this potential risk.
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