Abstract
Objective
Temporomandibular disorders (TMD) comprise a cluster of conditions with a wide range of etiological factors that causes pain and discomfort in the masticatory muscles (TMD-M) and temporomandibular joints (TMD-J). More than 50% of the patients with TMD report regular usage of drugs. However, there is still no consensus, nor is there any evidence-based support for clinicians when choosing between different drugs. Therefore, this systematic review, including a network meta-analysis (NMA), aimed to evaluate the scientific evidence and discuss the pharmacological treatment options available to treat painful TMD.
Method
An electronic search was undertaken to identify randomized controlled trials (RCTs) investigating pharmacological treatments for TMD-M and/or TMD-J, published until 6 April 2023. Since only 11 articles could be used for an NMA regarding TMD-M, a narrative synthesis was also performed for all 40 included RCTs. The quality of evidence was rated according to Cochrane’s tool for assessing risk of bias, while the certainty of evidence was rated according to Grading of Recommendations Assessment, Development and Evaluation (GRADE).
Results
When it comes to TMD-M, evidence arises for wet needling therapies with BTX-A, granisetron, and PRP as well as muscle relaxants. For TMD-J, evidence points toward pharmacological treatment approaches including non-steroidal antiinflammatory drugs (NSAIDs) and glucocorticosteriods (for inflammatory conditions) as well as hyaluronic acid and dextrose.
Conclusions
The evidence clearly indicates that the pharmacological treatment approaches differ between TMD-M and TMD-J. Therefore, it is of great importance to first try to uncover each patient’s individual and multifactorial etiology and then employ a multifaceted treatment strategy, including pharmacological treatment approaches.
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Evidence clearly indicates that the pharmacological treatment approaches differ between temporomandibular disorders of muscular and arthrogenous origin. |
For temporomandibular disorders of muscular origin, evidence arises for wet needling therapies with BTX-A, granisetron, and PRP as well as muscle relaxants. |
For temporomandibular disorders of arthrogenous origin, evidence arises for non-steroidal antiinflammatory drugs (NSAIDs) and glucocorticosteriods (for inflammatory conditions) as well as hyaluronic acid and dextrose. |
1 Introduction
Temporomandibular disorders (TMD) comprise a cluster of conditions that causes pain and discomfort in the masticatory muscles, temporomandibular joints (TMJ), and surrounding structures [1, 2]. TMD encompasses a range of painful symptoms, such as ear and facial pain, headache in the temporal region, and tooth sensitivity, as well as non-painful symptoms such as clicking, popping, or crepitus of the TMJ, limited jaw-movements, and muscle fatigue or stiffness [2, 3].
TMD impacts approximately 10–15% of the adult population [4, 5] and seems to be three times more frequent in women [6]. Painful TMD of musculoskeletal origin, e.g., TMD-M, is the most common diagnosis with a frequency of 42–70% [7, 8]. It is often characterized as a persistent dull, mild-to-moderate muscle pain, which can be intensified into a sharper pain sensation and radiate to adjacent structures when provoked by jaw function [9]. Another typical sign of TMD-M is tenderness or pain on palpation of the masticatory muscles [2]. TMD-M has been shown to negatively affect quality of life [10] and is often associated with psychological distress such as depression and anxiety [11]. The underlying etiology is complex and likely to be both multifactorial and biopsychosocial [1, 12].
Painful TMD of arthrogenous origin, e.g., TMD-J, can manifest within a healthy TMJ or in a TMJ affected by inflammation, such as arthritis [2]. In a healthy TMJ, pain arises from nociceptors located in the surrounding soft tissue of the joint. This pain occurs mainly during mandibular movements and ceases as soon as the jaw returns to its natural resting position [13]. However, in an inflamed TMJ, pain also emerges from nociceptors in the subarticular bone, exposed by the inflammatory processes [13, 14]. In this case, pain is constantly throbbing and worsens with jaw function. TMJ arthritis can generally be categorized on the basis of its underlying causes as local arthritis or arthritis associated with systemic disease [15]. Examples of local arthritis include synovitis, traumatic arthritis, or capsulitis. While the etiology remains largely unknown, there are some reported contributing factors. Mechanical overload of the TMJ [16], a perforation of the TMJ disc [17], or a disc displacement in the TMJ [18,19,20] have been reported as potential contributing factors. Further, systemic arthritis stems from underlying systemic diseases such as rheumatoid arthritis, juvenile arthritis, and psoriatic arthritis, representing a localized manifestation of a broader systemic inflammatory process. As with local arthritis, the etiology remains largely unknown for systemic arthritis [21].
On the basis of the multifactorial etiology of painful TMD [22], and since painful TMD exhibit a range of intricate symptoms and underlying causes, it is advisable to employ a multifaceted treatment strategy [23,24,25]. This strategy encompasses a diverse range of therapeutic modalities, including occlusal splints [26], physiotherapy [27] and/or jaw exercises [28], behavioral medicine [24], TMJ surgery [29], and pharmacological interventions [30]. While reversible non-pharmacological interventions are often recommended as first-line treatments [24], pharmacological options can play a crucial role in pain management and enhancement of overall life quality in patients with painful TMD. Further, as many as 50% of patients with painful TMD have reported usage of drugs [31]. Numerous studies have investigated the efficacy of various pharmacological treatment in painful orofacial pain conditions, including TMD [32]. Non-steroidal antiinflammatory drugs (NSAIDs), opioids, corticosteroids, anxiolytics, antidepressant, muscle relaxants, and anticonvulsants are the most frequently used pharmacological agents prescribed by clinicians [33]. Nonetheless, the best pharmacological treatment modality with predictable outcomes based on solid evidence is still largely unknown. Therefore, this systematic review, including a network meta-analysis (NMA), aimed to evaluate the scientific evidence and discuss the pharmacological treatment options available to treat painful TMD.
2 Materials and Methods
2.1 Protocol
This systematic review, including an NMA, followed the protocol that was registered a priori in PROSPERO (the International Prospective Register of Systematic Reviews, registration no. CRD42023406861). Further, the included NMA of randomized controlled trials (RCTs) was conducted according to the Preferred Reporting Items for the PRISMA Extension Statement for Reporting of Systematic Reviews Incorporating Network Meta-Analyses of Health Care Interventions (the PRISMA-P checklist) (Supplementary information 1) [34].
2.2 Selection Criteria
The following inclusion criteria were adopted on the basis of the PICOTS approach:
Population (P), Intervention (I), Comparator (C), Outcome (O), Time (T), Study (S)
The population (P) was adult patients having painful temporomandibular disorders. In the analysis they were subgrouped according to the location of pain to either (a) TMD-M; i.e., pain of myogenous origin, and (b) TMD-J; i.e., pain of arthrogenous origin. However, there were not enough studies on TMD-J, so this is only presented in the narrative part of the results.
The intervention (I) was any type of pharmacological treatment for painful TMD.
The comparators (C) were other pharmacological treatments, no treatment, placebo, or on waiting list.
The primary outcome (O) was pain reduction using a visual analogue scale (VAS; 0–100) or a numeric rating scale (NRS; 0–10). For the analysis the NRS was transformed to a 0–100 scale. The secondary outcome was changes in maximum mouth opening (MMO). However, there too few studies to do an NMA, so this is only presented in the narrative part of the results.
The follow-up time (T) was either short term ≤ 3 months, intermediate term 3–5 months, or long term ≥ 6 months
The study design (S) was composed only of randomized controlled trials that reported the outcomes of interest.
The following exclusion criteria were used: (1) studies presented in languages other than English and Scandinavian languages; (2) editorials, letters, legal cases, interviews, case-series, duplicates, observational studies, cross-sectional studies and case-control studies, non-randomized clinical trials, cohort studies, and review articles; (3) publications using duplicated data; (4) studies not investigating pharmacological treatments for painful TMD; and an additional criterion for the NMA (5) studies with missing data required to perform a meta-analysis, such as the post-treatment mean and standard deviation for the outcomes of interest.
2.3 Search Strategy
In collaboration with the librarians Lovisa Liljegren (LL) and Narcisa Hannerz (NH) at the Karolinska Institutet University Library, we designed a search strategy that identified randomized controlled studies reporting data on pharmacological treatments in a patient population with painful TMD. The electronic search was performed on 6 April 2023 and included all relevant RCTs, in any language and with any publication date, from the databases MEDLINE, EMBASE, CINAHL, the Cochrane Central Registry of Controlled Trials (CENTRAL), and Web of Science from the inception of each database to 6 April 2023.
The search strategy was developed in MEDLINE (Ovid) in collaboration LL and NH. The search strategies were peer-reviewed by NH before LL performed the search. For each search concept medical subject headings (MeSH-terms) and free-text terms were identified. The search was then translated, in part using Polyglot Search Translator [35], into the other databases. Finally, de-duplication was performed with the method presented by Bramer et al. in 2016 [36]. One final extra step was added to compare DOIs. Grey literature was not included. The complete search strategies for all databases are available in Supplementary information 2.
The Rayyan tool was used to assist with screening of titles and abstracts [37]. Two of the authors (MC and GB) independently and blinded screened the titles and the abstracts. When there was a conflict regarding potentially eligible articles for inclusion, a third author (NC) solved this disagreement by discussion, thus having the role of judge. All potentially eligible studies were then retrieved, and the full-text articles were reviewed by the same authors (MC and GB) to determine whether they met the inclusion criteria. Any disagreement was again resolved by discussion with the third author (NC).
2.4 Data Extraction
A data extraction form was developed for this review and pilot tested independently on two randomly selected studies by two of the authors (MC and GB) to ensure consistency in extraction. The extraction form was refined accordingly. Any disagreement in data extraction was resolved by discussion with a third author having the role of judge (NC). The extracted information included the characteristics of the studies and participants, i.e., authors, title, study design, subgroup diagnoses, diagnostic criteria used, age of patients, male–female ratio, treatment groups (number), duration of treatments/frequency, and outcome measures.
2.5 Assessment of Risk of Bias and Certainty of Evidence
Risk of bias was determined by two authors (MCh and JS) independently, using version 2 of the Cochrane risk-of-bias tool for randomized trials (RoB2) [38]. Any disagreement was resolved by discussion, with a third author having the role of judge (NC). The tool is structured into a fixed set of five domains of bias evaluating different aspects of the article including design, conduct, and reporting. Through an algorithm, judgment about the risk of bias is generated. The judgment can be that the article has either a low or a high risk of bias or that it can express some concerns.
Certainty of evidence was assessed (by EA) using the Grading of Recommendations Assessment, Development and Evaluation (GRADE) approach of meta-analysis [39] GRADE was implemented to identify the certainty of effect estimates from the meta-analysis for the outcomes of interest, i.e., pain intensity, in the present NMA. The certainty of evidence for RCTs, as assessed by the GRADE system, includes four levels of quality of evidence: (1) high quality of evidence—i.e., the real effect is close to that of the estimated effect; (2) moderate quality evidence—i.e., the real effect is likely to be close to the estimated effect, but there is a possibility that there is a substantial difference; (3) low-quality evidence—i.e., the real effect may be significantly different from the estimated effect; and finally (4) very low-quality evidence—i.e., the real effect is likely to be significantly different from the estimate of the effect. Thus, the certainty of evidence for RCTs, as assessed by the GRADE system, begins as high-quality evidence and is then down-rated due to limitations in study design (risk of bias), inconsistency, imprecision, indirectness, and publication bias.
2.6 Data synthesis
Before conducting the NMA in this review, a network plot was performed to present the network geometry. This was performed to assess whether the included RCTs were connected [40]. NMA was connected for the outcome of post-treatment pain intensity for TMD-M, while the other outcomes of post-treatment pain intensity for TMD-J as well as MMO with and without pain were not analyzed using NMA, but instead reported narratively.
As presented previously by our group [24, 41,42,43], the post-treatment pain intensity values, which were the outcome of interest, were used to calculate the standardized mean difference (SMD). For each possible pair of treatments, the results from the NMA are presented as a summary of relative effect sizes (SMD). The statistical unit used was number of patients.
The method used in this review follows our previous publications step by step and has been previously described by our group [24, 41,42,43]. Statistical models used in this NMA were according to multiple published statistics and assumptions [44,45,46,47,48].
To conduct the NMA, using the mvmeta command, the software STATA (StataCorp. 2011. Stata Statistical Software: Release 15. College Station, TX) was used [49,50,51]. To identify any local inconsistency, the loop-specific approach was performed separately in each closed loop of the network. The inconsistency factor was analyzed by analyzing the difference between direct and indirect estimates for a defined comparison in the loop of the network. The amount of the inconsistency factors and their 95% confidence intervals (CI) were used to infer the detection of inconsistency in each loop. In addition, a common heterogeneity estimate, within each loop, was assumed [47]. By using the ifplot command in STATA, the results of this approach were presented in a forest plot [46]. To control for the assumption of consistency in the entire network the design-by treatment model using STATA and the mvmeta command were performed, as described by Higgins and colleagues [52,53,54]. A meta-regression analysis of the mean of pain reduction based on VAS and follow-up time was used to assess whether the duration of follow-up influenced the post-treatment pain intensity. RCTs with a high risk of bias were excluded, and the analysis was then repeated to assess the robustness of the results. Ranking probabilities for all treatments at each possible rank for each intervention was then estimated. The treatment hierarchy was analyzed using the surface under the cumulative ranking (SUCRA) curve and mean ranks [54, 55]. SUCRA can also be presented as a percentage of treatment that can be ranked first without uncertainty [55].
3 Results
3.1 Literature Search Outcome
The full electronic search resulted in 4357 articles from all databases, but after removal of 1677 duplicates, a total of 2680 article titles and abstracts were screened. Out of the 2680 articles, 2527 were excluded after reading the titles and abstracts, resulting in 153 articles sought for retrieval. An additional ten were found from other sources. Finally, after reading the 163 full-text articles, 123 did not meet the inclusion criteria and were excluded, resulting in a total of 40 RCTs [56,57,58,59,60,61,62,63,64,65,66,67,68,69,70,71,72,73,74,75,76,77,78,79,80,81,82,83,84,85,86,87,88,89,90,91,92,93,94,95] included in this systematic review, out of which 11 were used in the NMA [56, 59, 69, 70, 72, 75, 76, 81, 83, 85, 93]. Figure 1 shows the PRISMA flow diagram with the process of evaluating RCTs for inclusion.
3.2 Presentation of Network Geometry
Nine interventions (botulinum toxin-A, clonazepam, morphine 5 mg, morphine 1.5 mg, magnesium sulfate, lidocaine, melatonin, cyclobenzaprine, and placebo) were included in the network diagrams for the outcome of post-treatment pain intensity via VAS, as shown in Fig. 2.
3.3 Study Characteristics, Individual Data, and Certainty of Evidence
The extracted study characteristics of the included RCTs are presented in Table 1. In total, 25 of the included studies showed a low risk of bias (green), 11 some concerns (orange), and 4 a high risk of bias (red), as presented with color and text in Table 2. For the NMA estimates, the certainty of evidence for all comparisons ranged from low (cyclobenzaprine) to very low (botulinum toxin-A, clonazepam, morphine 5 mg, morphine 1.5 mg, magnesium sulfate, lidocaine, melatonin, and placebo).
3.4 Results of Individual Studies
Individual results of every included RCT such as means, standard deviations, and sample size for overall post-treatment pain intensity, short to intermediate term (i.e., ranging from 2 days to ≤ 6 months) and long term (≥ 6 months), are reported in Supplementary information 3.
3.5 Narrative Synthesis of Pharmacological Treatment Outcomes for TMD of Muscular Origin
3.5.1 Non-steroidal Antiinflammatory Drugs
The electronic search revealed two RCT-studies that investigated the effect of naproxen as pharmacological treatment of TMD-M. On the basis of these studies, naproxen alone does not seem to have a pain-reducing effect. In the study by Cigerim and Kaplan (2023), treatment of TMD-M was more effective when naproxen was combined with codeine than when used alone or in combination with dexamethasone [60]. In the study by Khalighi et al. (2016), naproxen alone did not show any pain-reducing effect nor any increase in MMO [76].
3.5.2 Muscle Relaxants
When it comes to muscle relaxants, three RCT studies were found in the databases. These studies used skeletal muscle relaxants in addition to self-care management. However, there were diverging results concerning the treatment outcome regarding reduction in TMD-M pain. For example, cyclobenzaprine, a serotonin type 2 (5-HT2) receptor antagonist, was shown to have a significantly better pain-reducing effect when compared with the benzodiazepine clonazepam and with placebo [72]. On the contrary, when tizanidine, an alpha-2 adrenergic receptor agonist, was compared with placebo, no significant pain-reducing effect was found and there were no differences between substances [56]. Finally, in the third study, 10 weeks of treatment with propranolol, a nonselective beta-adrenergic receptor antagonist, reduced TMD-M to a slightly higher degree than placebo. However, in this study, propranolol was more prone to adverse effects [90].
3.5.3 Melatonin
Only one RCT study was found investigating the pain-reducing effect of melatonin on TMD-M. This study showed that melatonin reduces pain scores in a significantly higher degree than placebo and that this effect was independent of the effect on sleep quality [93].
3.5.4 Wet Needling Therapies
There are several different types of wet needling therapies for TMD-M, and the focus seems to be on botulinum toxin-A (BTX-A) [62,63,64,65,66,67, 69, 81], but other wet needling therapies such as lidocaine [75, 81, 83], magnesium sulfate [85], granisetron (5-HT3 receptor antagonist) [59], platelet-rich plasma (PRP) [88], and morphine [75] have been investigated in RCTs as well.
Several studies investigating which effect BTX-A has on pain intensity in patients with TMD-M were found. BTX-A has been shown to be more effective than placebo in reducing local pain of muscular origin in bruxers and patients with TMD-M [62, 63, 69, 81]. Two studies also reported a long-lasting pain-reducing effect of BTX-A in patients with localized TMD-M [63, 81]. The pain-reducing effect in patients with localized TMD-M does not seem to depend on dosage [63]. Further, it does not depend on whether only the masseter muscle is treated or both the temporal and masseter muscles are treated [62]. However, when it comes to the patient group with persistent TMD-M, it was shown in a study by Ernberg et al. (2011) that BTX-A had no effect on pain and that the number needed to treat (NNT) at the 1-month follow-up was 11 [67]. When BTX-A has been compared with other non-pharmacological treatments, it has been shown that the pain-reducing effect was equivalent to physiotherapy [70], acupuncture [64], and occlusal appliances [65]. Similar findings have been shown when it comes to MMO. BTX-A has been shown to improve MMO in a greater extent when compared with placebo in bruxers [69] and patients with localized TMD-M [81], regardless of dosage [66].
When it comes to other wet needling therapies, there are several one-of-a-kind studies showing promising results included in this review. First, in a study by Christidis et al. (2015), the 5-HT3 receptor antagonist granisetron was shown to have a 30–50% pain-reducing effect, which also was significantly higher than placebo, lasting for more than 6 months, with a NNT of 4. Further, granisetron also increased the MMO significantly [59]. Second, in a study by Kang et al. (2018), a single dose of morphine had an analgesic effect for 48 h and was significantly more effective than placebo. The same study also indicated that a higher dose, 5 mg, is more effective than a dose of 1.5 mg [75]. The third study by Refahee et al. (2022) indicates that a single injection with magnesium sulfate significantly reduced pain and increased MMO up to 3 months in patients with TMD-M [85]. In the fourth study, Nitecka-Buchta et al. (2018) showed that repeated intramuscular injections with collagen were significantly more efficient in pain reduction than injections with lidocaine [83]. In the fifth study by Sakalys et al. (2020), a single injection with PRP resulted in a significantly greater pain reduction after 4 weeks than a single injection with lidocaine [88]. In the sixth and final study on wet needling therapies (except for BTX-A), four different treatment strategies for painful TMD-M were compared. The treatments were either an occlusal splint alone or in combination with either betamethasone, sodium hyaluronate, or PRP. Even though all four treatment approaches were effective, the one with the combination of occlusal splint and PRP was the only that achieved long-term success [89].
3.6 Network Meta-analysis and Treatment Ranking of Pharmacological Treatment Outcomes for TMD of Muscular Origin, Post-treatment Pain Intensity, Other Comparisons versus Placebo, SMD
Altogether, 11 RCTs with a total of 457 patients were identified [56, 59, 69, 70, 72, 75, 76, 81, 83, 85, 93]. All these reported pain reductions using the VAS after pharmacological treatment of TMD-M. The post-treatment pain intensity compared post-treatment pain intensity in eight comparisons versus placebo. The eight comparisons included intramuscular injections of BTX-A [69, 70, 81], intramuscular injection of lidocaine [81], cyclobenzaprine [56, 72], melatonin [93], magnesium sulfate [85], morphine 1.5 mg [75], morphine 5 mg [75], and clonazepam [72, 83].
The follow-up times ranged from 2 days [75], 2 weeks [83], 3 weeks [56, 72], 4 weeks [93], 3 months [70], and 6 months [69, 81, 85].
The NMA revealed a significant pain reduction after pharmacological treatment with magnesium sulfate when compared with placebo (SMD = −5.81; CI −10.09 to −1.53; very low-quality evidence). However, there were no statistically significant differences between the other comparisons and placebo as shown in Fig. 3.
3.7 Treatment Ranking
The most effective pharmacological treatment option in reducing TMD-M pain at follow-up times ranging from 2 days to 6 months was magnesium sulfate (96.9%; very low-quality evidence), which was followed by BTX-A (64%; very low-quality evidence), cyclobenzaprine (53.6%; low-quality evidence), clonazepam (52.6%; very low-quality evidence), melatonin (50.9%; very low-quality evidence), morphine 5 mg (42%; very low-quality evidence), placebo (34.4%; very low-quality evidence), morphine 1.5 mg (33.7%; very low-quality evidence), and lastly, lidocaine (22%; very low-quality evidence), as illustrated in Fig. 4 and Table 3.
3.8 Narrative Synthesis of Pharmacological Treatment Outcomes for TMD of Arthrogenous Origin
3.8.1 Non-steroidal Antiinflammatory Drugs
The electronic search revealed four RCT studies investigating the effect of NSAIDs as pharmacological treatment for TMD-J. In one study investigating patients with TMD-J, diclofenac sodium was shown to have a significant pain-reducing effect, but that the effect is even better if it is combined with bromelain, rutoside, trihydrate, and trypsin [74]. In another study, ibuprofen was compared with the endocannabinoid-like lipid mediator palmitoylethanolamide (PEA). Even though ibuprofen was shown to have a significant pain-reducing effect and increased MMO, PEA was more effective [79]. Two studies comparing the effect of ibuprofen and glucosamine sulfate showed that ibuprofen resulted in similar or less pain reduction than glucosamine [71, 91].
3.8.2 Glucosamine Sulfate
When it comes to glucosamine sulfate, the findings are diverging. One study could not show any difference between treatment with glucose amine sulfate and placebo, neither regarding pain intensity nor MMO in patients with TMD-J [58]. However, when glucosamine sulfate was compared with ibuprofen it showed similar [91] and better [71] effects on both TMD-J pain and MMO. In the case with similar effect immediately after 90-day treatment, there was a long-term difference after 120 days where glucosamine sulfate was superior to ibuprofen [91].
3.8.3 Topical Treatment—Capsaicin
One study investigating topical treatment of painful TMD-J fulfilled the inclusion criteria. That study showed that both placebo and capsaicin cream resulted in a significant improvement of unilateral TMD-J. There was, however, no statistically significant difference in either pain intensity or MMO when capsaicin was compared with placebo [94].
3.8.4 Wet Needling Therapies
There are several different types of wet needling therapies for TMD-J, some are antiinflammatory [68, 73] since TMD-J can be a painful condition assumed to be associated with local inflammation, and others focus on pain reduction with local anesthetics [78, 92, 95].
When it comes to antiinflammatory needling therapies, no difference in TMD-J pain was found after a single dose of methylprednisolone when compared with placebo (saline), however, the adverse effects were twice as common after treatment with methylprednisolone [73]. Similar findings were also reported in another study with the unselective NSAIDs betamethasone and tenoxicam, which were found to have less pain-reducing effect when compared with hyaluronic acid. However, all three pharmacological treatments were significantly superior when compared with placebo [68].
Further, for anesthetics, a combination of dextrose and lidocaine is superior to just lidocaine for reducing TMD-J pain intensity and increasing MMO [78, 95]. Likewise, the local anesthetic ultracain shows a short-term reduction in pain intensity, but no effect on MMO [92].
In regard to internal derangements of the TMJ with pain, dextrose prolotherapy has been found to have a significant long-term pain relief [82, 84, 95] and improved MMO [80, 83, 86, 95].
3.8.5 Pharmacological Treatment in Combination with Arthrocentesis
Pharmacological treatment can be used in combination with surgical procedures such as arthrocentesis of TMJs in patients with osteoarthritis and/or osteoarthrosis to alleviate joint pain. Only one study was found to have investigated this matter. When comparing the effect of postoperative injections with either hyaluronic acid or PRP, there were no differences in pain reduction or MMO [61].
3.9 Network Meta-analysis and Treatment Ranking of Pharmacological Treatment Outcomes for TMD of Arthrogenous Origin
There were not enough studies included to be able perform an NMA for this patient group.
4 Discussion
Currently there is no consensus regarding pharmacological treatments for painful TMD. The main findings of this systematic review provide some support for pharmacological treatment approaches for TMD of both muscular and arthrogenous origin. However, due to the small number of present and included RCTs on pharmacological treatments, in combination with the results presented in the narrative synthesis, one cannot generalize nor rank the pharmacological treatment options. Thus, there must be an individual assessment considering the multifactorial etiology of painful TMD with a range of intricate symptoms and causes. Thus, it is advisable to employ a multifaceted treatment strategy, including pharmacological treatment approaches [22,23,24,25].
For the large patient group with TMD-M [5], i.e., the TMD-M group, the NMA could only show a significant pain-reducing effect by the use of magnesium sulfate when compared with placebo, however, with very low-quality evidence. When the treatment alternatives were ranked, magnesium sulfate was placed first, followed by BTX-A, cyclobenzaprine, and clonazepam. Surprisingly, local anesthetics were ranked last, after placebo. On the basis of the narrative synthesis of this review, muscle relaxants, BTX-A, and some other wet needling agents such as granisetron, morphine, and PRP seem to be promising both when it comes to reduction of TMD-M pain and the increasing of MMO. These findings were not surprising and are in consistency with a previous NMA that also suggested that there might be a possible pain-reducing effect by BTX-A, and the muscle relaxant cyclobenzaprine could be a promising pharmacological treatment approach although lacking long-term follow-ups [32]. Further, two other NMAs also concluded that BTX-A, granisetron, and muscle relaxants could have a possible pain-reducing effect, thus ranking them high [24, 41]. When considering treatment with muscle relaxants, the reported side effects (drowsiness, dizziness, weakness, and ataxia) limits the usability [96] . In contrast to this NMA, the local anesthetic lidocaine was ranked among the highest in those NMAs [24, 41]. When it comes to non-opioid analgesic drugs, this systematic review could not provide any scientific evidence. However, they can be considered as a good complement to other treatment modalities for painful TMD-M. This and other studies suggest that non-opioid analgesic drugs can be recommended for patients with mild-to-moderate TMD-M pain, mainly as a complement to other treatment approaches [97, 98].
For the patient group with TMD-J, no NMA could be performed. Therefore, the discussion is based on the narrative synthesis of this review. The results from the synthesis of the included RCTs support pharmacological treatments of TMD-J with NSAIDs, glucocorticosteroids, and hyaluronic acid, which is in accordance with the findings from previous systematic reviews [25, 32, 99]. However, this review also indicates that the effect of prolotherapy with dextrose is promising, showing long-term pain-relieving effects and increased MMO. However, more studies are necessary to draw any conclusions. As for TMD-M, local anesthetics do not seem to provide any significant pain-reducing effects. Just like TMD-M, painful conditions arising from TMJ can be mechanical, inflammatory, due to mechanical overload, systemic diseases, etc., i.e., having a divergent, multifactorial etiology and individualized treatment plans including pharmacological treatment approaches [25, 32, 99].
4.1 Study Strengths and Limitations
The strengths of the present review encompass the following key aspects: (1) this research marks the inaugural publication of a network meta-analysis (NMA) that systematically compares the effectiveness of 39 distinct pharmacotherapeutic treatment options for TMD of muscular origin, according to the authors’ knowledge; (2) by exclusively incorporating RCTs within the NMA, the researchers ensured the presence of high-quality evidence while mitigating potential biases stemming from selection and performance factors; and (3) the integration of the GRADE-system into the analytical process effectively assigned accurate grades to all findings, preventing both overestimation and underestimation of outcomes.
Nevertheless, there exist several limitations associated with this study that warrant consideration: (1) owing to unavailable data, NMA was not executed for every comparison group, and not for TMD of articular origin either; (2) certain NMA-groups were characterized by a restricted number of RCTs and participants, highlighting the imperative need for additional RCTs with larger sample sizes to comprehensively assess effectiveness before arriving at definitive conclusions; (3) variations in follow-up durations across RCTs and inadequate follow-up periods in specific instances exerted additional influence on the analysis. Moreover, the absence of essential mean and standard deviation information hindered the execution of subgroup analyses; (4) limited data availability precluded statistical analysis of outcomes such as MMO with and without pain, necessitating a narrative presentation of results. Finally, most evidence acquired exhibited notably low quality. It is also important to note that certain included RCTs had limited sample sizes for patients with disc displacement, potentially compromising the reliability and robustness of the conclusions drawn. Therefore, a cautious approach is recommended when interpreting these findings.
4.2 Conclusions
This systematic review presents the current knowledge and evidence regarding pharmacological treatment approaches for painful temporomandibular disorders. Although a limited number of RCTs were included, there is some evidence, though not sufficient, to generalize the results. The evidence clearly indicates that the pharmacological treatment approaches differ between TMD-M and TMD-J. Therefore, it is of great importance to first try to uncover each patient’s individual and multifactorial etiology and then employ a multifaceted treatment strategy, including pharmacological treatment. When it comes to TMD-M evidence, an increasing body of evidence points toward wet needling therapies with BTX-A, granisetron, and PRP as well as muscle relaxants. For TMD-J, the evidence points toward pharmacological treatment approaches including NSAIDs and glucocorticosteriods (for inflammatory conditions) as well as hyaluronic acid and dextrose.
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Acknowledgements
The authors thank the librarians Lovisa Liljegren (LL) and Narcisa Hannerz (NH) at the Karolinska Institutet University Library for the assistance with the electronic literature search.
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Nikolaos Christidis had the main idea for the article. However, all authors contributed to the study conception and design. Nikolaos Christidis, Malin Collin, and Essam Ahmed Al-Moraissi performed the literature search with help from the university library at Karolinska Institutet. Selection of papers was performed by Malin Collin and Golnaz Barjandi. Analysis of risk of bias was performed by Johanna Svedenlöf and Maria Christidis. Maria Christidis is a senior lecturer and responsible for the course “Scientific theory and methods” and teaches specifically about the different methods existing for risk of bias and certainty of evidence. Further, both Nikolaos Christidis and Essam Al-Moraissi are very experienced in carrying out systematic reviews and have, together with Maria Christidis, double checked all parts of the assessment of risk of bias and certainty of evidence. Data were analyzed by Essam Al-Moraissi. Nikolaos Christidis, Maria Christidis, Malin Collin, and Hajer Jasim drafted the first manuscript that was critically revised by all authors, who commented on previous versions of the manuscript. All authors read and approved the final version manuscript.
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Open access funding provided by Karolinska Institute.
Conflict of Interest
Authors Nikolaos Christidis, Essam Ahmed Al-Moraissi, Golnaz Barjandi, Johanna Svedenlöf, Hajer Jasim, Maria Christidis, and Malin Collin declare that they have no conflicts of interest that might be relevant to the contents of this manuscript.
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The datasets generated during and/or analyzed during the current study are available from the corresponding author on reasonable request.
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Christidis, N., Al-Moraissi, E.A., Barjandi, G. et al. Pharmacological Treatments of Temporomandibular Disorders: A Systematic Review Including a Network Meta-Analysis. Drugs 84, 59–81 (2024). https://doi.org/10.1007/s40265-023-01971-9
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DOI: https://doi.org/10.1007/s40265-023-01971-9