MRI-based Assessment of Masticatory Muscle Changes in TMD Patients After Whiplash Injury 

DOI: https://doi.org/10.21203/rs.3.rs-151508/v1

Abstract

Objective: To investigate the change in volume and signal in the masticatory muscles and temporomandibular joint (TMJ) of patients with temporomandibular disorder (TMD) after whiplash injury based on magnetic resonance imaging (MRI) and to correlate them with other clinical parameters.

Methods: Ninety patients (64 women, 26 men; mean age: 39.36±15.40 years), including 45 patients with symptoms of TMD after whiplash injury (wTMD), and 45 age- and sex-matched controls with TMD due to idiopathic causes (iTMD) were included. TMD was diagnosed using the study diagnostic criteria for TMD Axis I, and MRI findings of the TMJ and masticatory muscles were investigated. To evaluate the severity of TMD pain and muscle tenderness, we used a visual analog scale (VAS), palpation index (PI), and neck PI.

Results: TMD indexes, including VAS, PI, and neck PI were significantly higher in the wTMD group. In the wTMD group, muscle tenderness was highest in the masseter muscle (71.1%), and muscle tenderness in the temporalis (60.0%), lateral pterygoid muscle (LPM) (22.2%), and medial pterygoid muscle (15.6%) was significantly more frequent than that in the iTMD group (all p<0.05). The most noticeable structural changes in the masticatory muscles occurred in the LPM with whiplash injury. Volume (57.8% vs. 17.8%) and signal changes (42.2% vs. 15.6%) of LPM were significantly more frequent in the wTMD group than in the iTMD group. The presence of signal changes in the LPM was positively correlated with the increased VAS scores only in the wTMD group (r=0.346, p=0.020). The prevalence of anterior disc displacement without reduction (ADDWoR) (53.3% vs. 28.9%) and disc deformity (57.8% vs. 40.0%) were significantly higher in the wTMD group (p<0.05). The presence of headache, sleep problems, and psychological distress was significantly higher in the wTMD group than in the iTMD group.

Conclusion: Abnormal MRI findings and their correlations with clinical characteristics of the wTMD group were different from those of the iTMD group. The underlying neuropathophysiology may differ depending on the cause of TMD, raising the need for a treatment strategy accordingly.

Introduction

Whiplash injury refers to a macrotrauma that occurs with a hyperextension of the head and neck vertebrae followed by hyperflexion when a sudden or excessive force is applied 1. In road traffic accidents, injuries occur mainly due to side-impact or rear-end collisions 2,3 (Fig. 1). Such cases present with a variety of clinical manifestations, including neck stiffness, neck pain disability, psychological distress, headache, and temporomandibular disorder (TMD) 46. The incidence of TMD in patients with whiplash injury is low to moderate and ranges from 14–37.5%7. It is important to note that patients commonly suffer from chronic whiplash injury and clinically have pain in a wider range of the body 8. Approximately 40% of patients with whiplash injuries suffer from persistent pain and chronic disability.9

TMD is an umbrella term for pain and dysfunction in the temporomandibular joint (TMJ), masticatory muscles, and adjacent structures. Population-based studies showed that 60–70% of the general population has at least one sign of TMD, 12.1% have TMD-related pain, and only 5% seek treatment 10,11. Plausible risk factors for TMD, either alone or more likely in combination include macrotrauma, microtrauma, other body pain conditions, self-reported previous pain experience, and psychological status. The etiology of TMD moved from a mechanical-based phenomenon to a chronic pain biopsychosocial model 12. Typical and frequent TMD symptoms include TMJ noise and pain, followed by restriction of mandibular movement, headache, neck pain, ear pain, and tinnitus. Whiplash injury is considered an initiating or aggravating factor of TMD.5,13 Thus, patients with TMD suffering from whiplash injury have wider and stronger pain than those with only microtrauma.

The neuropathology of TMD development and aggravation related to whiplash injury can be distinguished from other TMD etiologies. In general, pain in whiplash injury can occur as a result of direct trauma to the muscles, ligaments, and tendons, which may lead to substantial tissue damage 14. TMD caused by the accumulation of microtrauma, such as parafunctional habits or malocclusion, occurs due to changes at the peripheral level. However, sudden large impact can be transmitted to the central nervous system (CNS) because of the occurrence of diffuse axonal injury throughout the injury 15. Sometimes referral patterns may develop because of CNS involvement resulting from prolonged masticatory muscle pain, and the pain pattern in individuals becomes more complex. Additionally, experiences of emotional trauma from the injury that pose a potential threat to life can negatively impact personal future health and finances 16. These physical and psychosocial risk factors create combined synergies and form complex neuropathologies of pain amplification in TMD.

Masticatory muscles are poorly understood in terms of posttraumatic sequelae. All four main masticatory muscles, including the masseter, temporalis, medial pterygoid muscle (MPM), and lateral pterygoid muscle (LPM), are attached to the mandible and govern the function to move the mandible (Fig. 2). The masseter and temporalis muscles on the outside of the jaw bones have been studied, and it has been reported that these muscles are commonly affected in patients with TMD 17. The masseter is a jaw-closing muscle that elevates the mandible and is one of the strongest in the human body. The temporalis muscle enables elevation and retraction of the mandible. An important role of the MPM is the fine control and stabilization of the vertical mandibular position, concentrically activating jaw closing 18. Among all four muscles of mastication, the LPM is the only muscle that depresses the mandible. Traumatic injury results in muscle pain, muscle wasting, skeletal demineralization, and disability 19. However, there is limited information on the changes in the masticatory muscles of patients with TMD after whiplash injury.

Magnetic resonance imaging (MRI) is the gold standard for evaluating the abnormalities in the TMJ and masticatory muscles, and for determining the disc–condyle relationship. 6,13 Atrophy, fibrotic change, and fatty replacement of the masticatory muscle regularly occur with either disuse or denervation 20, which can occur as a consequence of immobilization or disuse after whiplash injury. On T1- and T2-weighted MRI images, masticatory muscles with myotonic dystrophy present as high signal intensity areas because of fatty replacement 21. In addition, the huge tensile force throughout the whiplash injury exerted on a muscle may lead to excessive stretching of the muscle fibers and consequently a tear, and impair the muscle-tendon junction 22. According to our previous MRI-based studies, patients with TMD due to whiplash injury suffered more distortion of the disc–condyle relationship and LPM changes 6,13. TMJ disc displacement leads to degenerative changes in the disc deformity and condylar degeneration,23 and the symptoms of TMD might become chronic. Until now, most MRI studies in patients with TMD evaluated intra-articular changes 24.

Thus, the present study aimed to investigate the relationship between changes in the masticatory muscles and TMJ on MRI and clinical pain intensity in patients with TMD due to whiplash injury, and to compare their clinical and MRI characteristics with those of patients with TMD due to idiopathic causes. We also investigated the factors that affect subjective pain intensity and whether these results differ between the TMD due to idiopathic causes (iTMD) and TMD after whiplash injury (wTMD) groups. Our hypotheses were as follows: (1) compared to the patients with iTMD, patients with wTMD will have higher pain intensity and more changes in the masticatory muscles, and have more tenderness upon palpation; (2) structural changes in the TMJ and masticatory muscles will be associated with a higher severity of TMD symptoms, and differences between the wTMD and iTMD groups can be observed. Our study is the first study to examine the changes in the four major masticatory muscles in patients with whiplash injury using MRI, and to determine which muscular factors increase discomfort and pain in patients with wTMD.

Methods

Participants and demographic data

The present study was carried out in accordance with the Declaration of Helsinki and approved by the Institutional Review Board (IRB) of the Kyung Hee University Dental Hospital. Informed consent was obtained from all patients.

This retrospective case-control study involved 45 randomly selected patients with wTMD and 45 randomly selected patients with iTMD, who were selected using a simple random sampling procedure employing a random number table. The “wTMD” group (n = 45) included patients who had first-onset TMD after sustaining a whiplash injury; the “iTMD” group (n = 45) comprised patients who had presented with idiopathic or non-traumatic TMD symptoms without any history of head/neck trauma.

The patients were diagnosed with TMD using the research diagnostic criteria (RDC) for TMD axis I,25,26 and the experience of whiplash injury was judged according to the Quebec Task Force on Whiplash-Associated Disorders.2 We identified the patients who had TMD and retrospectively reviewed all MRIs of their TMJs and TMJ reports from March 2017 through 2020. The inclusion criteria were as follows: no history of neck pain prior to the whiplash injury, no treatment on the current TMD symptoms other than medication, and no history of direct trauma to the jaw before or during the accident—the patients had no history of a TMD prior to the present TMD episode. The exclusion criteria were serious injuries, such as facial fracture and unstable multiple traumas, previous injury, neurological disorder unrelated to the trauma, and musculoskeletal disorder predating injury, rheumatism, psychological problems, and pregnancy. To assess the impact of whiplash injury in terms of distribution of TMD signs and symptoms, and MRI findings, all variables were compared by group.

MRI acquisition and analysis

All 90 patients underwent MRI examination on bilateral TMJs and masticatory muscles. High-resolution MRI images were obtained on a 3T MRI system (Signa™ Genesis, GE Healthcare, Chicago, IL, USA) with a 6-cm × 8-cm diameter surface coil. MRI examination was dependent on the MR sequences and protocol of Kyung Hee University Medical Center, and the details has also been revealed in our previous studies 13,27: All scans involved sagittal oblique sections (section thickness, 3 mm or less,; field of view, 15-cm; matrix dimensions, 256 × 224 matrix) and spin-echo sagittal MR images were obtained on the axial localizer images. T1-weighted images (T1WIs) and T2-weighted images (T2WIs) were obtained using a 650/14 TR/TE sequence and 2,650/82 TR/TE sequence, respectively. The proton density images were obtained using a 2,650/82 TR/TE sequence.

TMJs and adjacent masticatory muscles were evaluated in both the sagittal and coronal planes (Fig. 3) to determine the abnormalities in the TMJ and the alteration of each masticatory muscle. Two head and neck radiologists with at least 8 years of experience in their field and who were blinded to the patients’ clinical information visually analyzed the MRI findings. After determining the existence of MRI abnormalities, the TMJ and masticatory muscle measurements were evaluated using the INFINITT PACS (INFINITT Corp., Seoul, Korea).

Validation of MRI findings

We investigated the presence of MRI abnormalities of the TMJ and masticatory muscles, including disc displacement, effusion, disc deformity, condylar degeneration, and volume changes (VCs) and signal changes (SCs) in the four masticatory muscles, including the masseter muscle, temporalis muscle, LPM, and MPM. The detailed procedure of validation has been described in our previous papers.6,13 The disc position in the oblique sagittal plane was determined in the closed and open-mouth positions. In addition, disc position was classified as anterior disc displacement with reduction (ADDWR) or without reduction (ADDWoR) (Fig. 4). In the T1WI, T2WI, and proton density (PD) weighted images, each muscle was considered to have an SC when the fatty replacement tissue accompanying the high intensity signal was observed widely across the muscle. In the same images, it was considered to have a VC when the masticatory muscle had decreased volume and fibrosis. To determine whether the difference between the measurements was statistically significant, the values of the masticatory muscles acquired in each MRI sequence on the right and left sides of the same patient were compared.

Validation of clinical signs and symptoms of TMD

Contributing factors

We investigated self-reported parafunctional activities using the Oral Behavior Checklist, which includes jaw-related behaviors, such as teeth clenching and bruxism.28 Self-reported headache was evaluated using the dichotomous question “Do you have any headaches associated with TMD?” Self-assessment of tinnitus, psychological distress, and sleep problems was also reported. Each parameter was recorded as a binary answer (yes/no) in all patients.

Characteristics of pain

The duration of pain derived from the TMJ and adjacent structures was reported in days. Temporomandibular pain was scored by the patients subjectively, ranging from 0 (no pain at all) to 10 (the worst pain imaginable) using the visual analog scale (VAS).

Palpation index (PI) and neck PI

PI is a reliable scoring system that analyzes the severity of myofascial pain, allowing TMD symptoms to be objectively evaluated. In each patient, we palpated 20 intra- and extraoral muscle sites and three sites in the neck. The index-finger palpation pressure was 1 kg/cm2 and was applied for 5 s, as recommended in previous studies.29,30 To calibrate palpation pressures, we regularly pre-tested our index-finger pressure using a hand-held pressure algometer. For each site, a binary answer (yes/no) was provided. To calculate the PI score, we added all the positive answers and divided the sum by the number of events.31 To further investigate the intensity of neck pain, we calculated the neck PI, which was defined as the number of positive responses to the palpation of neck muscles, including the sternocleidomastoid, splenius capitis, and trapezius muscles, divided by the number of events. Using these two indexes, we quantified clinical myofascial pain.

Statistical methods

For all discrete variables, the absolute and relative percentage distributions were calculated. Continuous variables are presented as means and standard deviations. Various statistical methods were used for data analysis. Using the Mann–Whitney U test, we examined the difference in the means of the continuous variables between the wTMD and iTMD groups. Chi-square and Fisher's exact tests were used to calculate the proportional equivalence of discrete variables, such as the presence of MRI abnormalities (%) and patient's “yes” (%) response describing TMD contributing factors. Through Spearman's correlation analysis, we examined the MRI findings that were correlated with a significant increase in each TMD index score. A p < 0.05 level was set to be statistically significant. Data were analyzed using the Statistical Package for the Social Sciences for Windows version 25.0 (IBM Corp., Armonk, NY, USA).

Results

Demographic patient characteristics

Data from 45 patients with wTMD (mean age: 37.94 ± 12.27) and 45 patients with iTMD (mean age: 40.77 ± 18.02 years) were analyzed and compared. Among the patients with TMD who visited the hospital during the study period, female predominance (female:male = 2.45:1) was observed, and this sex ratio was reflected in both the wTMD (female: 68.9%) and iTMD groups (female: 73.3%). In addition, the mean symptom duration of wTMD (66.27 ± 58.06 days) was not different from that of iTMD (57.78 ± 48.33 days) (p = 0.453).

Analysis of pain intensity

The mean VAS score in the wTMD group was significantly higher than that in the iTMD group (6.73 ± 1.84 vs. 4.32 ± 2.80, p < 0.001). Interestingly, TMD indexes, including PI and neck PI, were significantly higher in the wTMD group than in the iTMD group (Table 1). That is, the mean PI (0.27 ± 0.21 vs. 0.16 ± 0.18, p < 0.01) and neck PI (0.45 ± 0.31 vs. 0.27 ± 0.23, p < 0.01) scores in the wTMD group were significantly higher than that in the iTMD group.

Clinical characteristics in wTMD and iTMD groups

Table 2 shows the putative contributing factors and clinical symptoms of TMD in each group. The distributions of clenching habits, headache, sleep problems, and psychological distress in the wTMD group were different from those in the iTMD group. Specifically, the patients with wTMD were more likely to have headache (71.1% vs. 40.0%) and sleep problems (57.8% vs. 35.6%), and psychological distress (33.3% vs. 13.3%), whereas clenching habits (8.9% vs. 26.7%) were less common in the wTMD group (all p<0.05). The distributions of bruxism and tinnitus in the wTMD group were different from those in the iTMD group.

Distribution of MRI Findings

The distributions of MRI variables on the TMJ (Table 3) and masticatory muscles (Table 4) were significantly different between the wTMD and iTMD groups. Interestingly, patients with wTMD were more likely to have ADDWoR (53.3% vs. 28.9%) and disc deformity (64.4% vs. 33.3%), which were significantly higher than those in the iTMD group (all p < 0.05). The distributions of effusion, ADDWR, and condylar degeneration in the wTMD group were not significantly different from those in the iTMD group. The most prominent abnormal MRI finding in the wTMD group was disc deformity (64.4%), followed by condylar degeneration (57.8%), ADDWoR (53.3%), ADDWR (24.4%), and effusion (22.2%) (Figure 5).

Regarding the masticatory muscles, the structural change in LPM was the most frequent change among the four major masticatory muscles in both groups (Figure 6). Specifically, both VC (57.8% vs. 17.8%) and SC (42.2% vs. 15.6%) of the LPM were significantly more prevalent in the wTMD group than in the iTMD group (all p<0.05). In contrast, VC (2.2% vs. 2.2%) and SC (2.2% vs. 2.2%) of the temporalis muscle were very rare in both groups. In addition, changes in MPM were not observed in any case in the wTMD group, and both VC and SC were observed in only two patients (4.4%) in the iTMD group. The structural changes in the masseter muscle on MRI were not observed in any case (0.0%) in either group (Figure 7).

Distribution of muscle tenderness

The distributions of muscle tenderness on palpation test were significantly different between the groups in the temporalis muscle, LPM, and MPM except for the masseter muscle (Table 5). Muscle tenderness was significantly higher in the temporalis muscle (60.0% vs. 35.6%), LPM (22.2% vs. 2.2%), and MPM (15.6% vs. 0.0%) in the wTMD group than in the iTMD group (all p < 0.05). On the other hand, tenderness was most frequently observed in the masseter muscle in both wTMD (71.1%) and iTMD (64.4%) groups. In contrast to the remarkable frequent observations of actual structural changes in the LPM observed on MRI, muscle tenderness of the LPM was scarcely observed in the iTMD group (2.2%) and only in 22.2% of patients in the wTMD group.

Associated MRI findings with increasing TMD index

VAS, which represents the degree of subjective pain, was positively correlated with masticatory muscle changes in wTMD, and with internal derangement of the TMJ in iTMD. Specifically, the presence of signal changes in the LPM was positively correlated with the increased VAS scores only in the wTMD group (r = 0.346, p = 0.020). In contrast, the presence of ADDWoR (r = 0.325, p = 0.029) and condylar degeneration (r = 0.297, p = 0.047) was positively correlated with the increase in VAS scores in the iTMD group. In the iTMD group, the VAS score was moderately positively correlated with PI (r = 0.300, p = 0.045) and neck PI (r = 0.301, p = 0.044), and these correlations were not observed in the wTMD group. Regarding PI and neck PI scores, there were no significant MRI variables that were correlated. However, neck PI and PI were strongly positively correlated with each other in both the wTMD (r = 0.866, p < 0.001) and iTMD (r = 0.764, p < 0.001) groups (Table 6).

Diagnostic classification of pain-related TMD

Depending on the cause of TMD pain, the most common pain-related diagnostic criteria for TMD fall into two categories: muscular and joint pain. Pain of muscular origin includes subcategories of myofascial pain and myofascial pain with limited mouth opening. On the other hand, pain of joint origin means arthralgia. In this study, the TMD diagnosis was established according to RDC/TMD, and TMD was diagnosed into three subgroups 26: pain of muscle origin, pain of joint origin, and mixed type. Because 93% of patients with wTMD and 89% of iTMDs were diagnosed with TMD with mixed muscle and joint pain, the data were not analyzed based on subgroups.

Discussion

Whiplash, a unique type of microtrauma mainly occurring in vehicle collisions, is caused by sudden dynamics of hyperextension-hyperflexion on the cervical spine. 32 Among the patients with whiplash injury, approximately 23% suffered chronic pain and disabilities. 33 Thus, it lowers the patient's quality of life and increases health costs. Neck pain and stiffness, and headache are the most prominent symptoms in whiplash injury 6. Recently, a possible association between whiplash injury and TMD has been studied. Carroll et al. reported that TMD was more prevalent in individuals with whiplash injury (15.8%) than in those without (4.7%) 34. Conversely, the prevalence of whiplash injury in populations with TMD (median 35%) is higher than that in control groups without TMD (1.7–13%).5 Although there is limited information on the neuropathophysiologies of TMD development and aggravation after whiplash injury, research to explore this is ongoing. As hypothesized, many of the clinical symptoms and MRI findings of masticatory muscles of whiplash-related TMD can be distinguished from those of TMD resulting from an unknown cause.

One of our main findings was that patients with wTMD had higher pain intensity across wider jaw and neck areas compared to those with iTMD. This was consistent with previous results that patients with whiplash injury report higher pain scores and larger areas of local and referred pain than healthy controls 35. The increased clinical pain observed in the wTMD group may be due to impaired diffuse noxious inhibitory controls (DNICs), a measure of central nervous system pain inhibition36. Moreover, sleep disturbance is related to decreased DNICs in patients with TMD 37. Reduced reactivity of the hypothalamic–pituitary adrenal (HPA) axis has been associated with chronic widespread body pain 38. Furthermore, thalamic activity also contributes significantly to the pain processing. Decreased thalamic activity can cause exaggerated pain following innocuous peripheral stimulation 39. Collectively, changes to the process of central endogenous pain inhibition through interference with DNICs, HPA axis, or thalamic activity can occur in patients with whiplash-related TMD, and pain is more likely to be amplified and prolonged in such patients.

Widespread pain, which is not limited to the injured area and increased pain intensity, is derived from the dynamics of the nociceptive pathway at the CNS level. Hypersensitivity after whiplash injury occurs both locally, i.e., throughout the neck area, and at more distant sites beyond the boundary of the damaged peripheral nerve 40. Thus, deep tissue is damaged in the cervical joint by direct application of shear force, compression, and excessive stretching through whiplash injury, but it can also affect the TMJ area. Pain wind-up refers to the phenomenon of increased excitability of CNS induced by frequency-dependent electrical stimulation of afferent C-fibers 41. Pain wind-up can also be a mechanism of hypersensitivity and in whiplash-associated TMD. There were clear experimental results showing that patients with painful TMD have reduced pain thresholds and sensory impairment after innoxious stimuli 40. Interestingly, central hypersensitivity is not only specific to whiplash injury, even though this phenomenon is seen in a variety of chronic pain syndromes 40,42. Similar neuropathology may underlie a variety of chronic pain, including TMD, and further investigation is required on how it serves in detail.

Regarding MRI findings on TMJ, more than 50% of patients with wTMD had ADDWoR and condylar degeneration, and were significantly more prevalent than those with iTMD. In general, the TMJ is the most affected structure from TMD 43. To the best of our knowledge, only a few MRI studies have validated the signs and symptoms of whiplash injury-induced TMD. During sudden macrotrauma, abrupt changes in the position of the mandible and TMJ disc followed by TMJ-ligament elongation and TMJ disc displacement may occur.44 In a previous MRI study, displacement (56%) and abnormal joint fluid or edema (65%) of the TMJ were observed in the patients who had TMD after sustaining whiplash injury 45. In addition, proper disc positioning is a prerequisite for normal movement of the mandibular condyle. Disc displacement progresses from reducible to non-reducible, and ADDWoR and condylar degeneration can be associated with each other 46. Abnormal positioning of the articular disc may cause closed lock jaw position, which evokes TMJ clicking and pain, as well as limits jaw function 47. Interestingly, the VAS score was positively related with ADDWoR and disc deformity only in iTMD, and this correlation was not observed in wTMD.

Our main MRI finding was that patients with wTMD had remarkable structural changes in the LPM. Substantial structural change in the LPM may have been observed considerably more frequently in wTMD than in iTMD because LPM is more susceptible to whiplash injury than other masticatory muscles. Additionally, LPM is a direct major factor in the occurrence of whiplash injury-related TMD. The LPM controls the rotation and translation of the disc and condyle, protrudes the mandible, and stabilizes the articular disc 48. LPM plays a somewhat secondary role in mastication, but it is directly related to changes in the mandibular condyle and disc. Pathologic changes in the LPM can be associated with TMJ disc displacement 49,50. Recent MRI results have shown structural muscle changes in the form of reduced muscle volume, fatty infiltration, and muscle atrophy in patients with whiplash-related disorders. 51,52 In our previous LPM-related MRI study, significant positive correlations were reported between structural changes in the LPM, ADDWoR, disc deformity, and condylar degeneration in patients with TMD after whiplash injury6. Furthermore, rapid LPM stretching induces reflex contracture with disc displacement, resulting in pain 6,53. On the contrary, no muscle changes were observed in asymptomatic individuals or individuals with idiopathic or non-traumatic neck pain 51. We found that the VAS score was correlated with the structural changes of LPM only in wTMD.

Among and/or within the human masticatory muscles, many anatomical differences exist, indicating that different muscles are specialized for their resistance against whiplash injury. In our results, more than 60% of patients with wTMD had muscle tenderness in the masseter and temporalis muscles. Architecturally, the masseter and temporalis muscles can deliver higher forces than the pterygoid muscles. Thus, masseter and temporalis muscles play a more crucial role in mastication, which can lead to fatigue build-up and become vulnerable to tenderness 54. In addition, the average thickness values of the masseter muscle (13.65 ± 2.19 mm), temporalis muscle (6.66 ± 1.14 mm), MPM (14.73 ± 1.32 mm), and LPM (15.59 ± 1.40 mm) were different 5557. Specialization in fiber type composition and fiber cross-sectional area can be reflected in these intramuscular differences. Compared to the masseter and pterygoid muscles, the temporalis has significantly larger fibers and a notably different fiber type composition 58. Furthermore, the myosin heavy chain (MyHC) content of muscle fibers mainly determines their force–velocity properties 59. A regionally higher proportion of MyHC type I, expressed in slow muscle fibers, was found in the anterior temporalis, deep masseter, and anterior MPM. 60. However, a previous study showed that MyHC type and isoform composition do not sufficiently explain the difference between the form and function of the muscles 61. Further research is needed to reach a clearer conclusion about the impact of whiplash-related TMD on each masticatory muscle.

Finally, we observed that headache, sleep problems, and psychological distress were significantly more prevalent in the wTMD group than in the iTMD group. We must focus on the fact that CNS-related factors were more prevalent in the wTMD group. Headache and sleep problems possibly co-occur from the result of the dysregulation of shared brain regions, such as the trigeminal nucleus caudalis and thalamus 62. Sleep problems deleteriously affect central pain modulatory systems 37. Headache has been suggested as an aggravating and potential risk factor for TMD symptoms 63. Psychological distress is often accompanied by CNS-level symptoms, and is associated with more pain and disability in whiplash injury 42. In addition, psychological factors, along with physical factors, can play a role in the progress or recovery from whiplash injury 64. This suggests that neuropathophysiologies of wTMD may differ from that of iTMD, and that TMD should be understood in a biopsychosocial model considering macrotrauma. The interconnectivity between biological factors and psychological factors can involve the development, processing, and chronicity of whiplash-related TMD symptoms. Furthermore, we need to have specific coping and treatment strategies for patients with wTMD.

This study has several limitations. In our study, we only checked for the presence of self-reported psychological distress, not through elaborate questionnaires or diagnostic tests. To understand whiplash injury-related TMD in the biopsychosocial model, further systematic investigation of the psychological aspects of patients will be required. Axis II of the DC/TMD or RDC/TMD diagnostic tool might be helpful in examining psychosocial factors.65,66 In addition, this study has the advantage that it had a randomized controlled design, but a large-scale population-based study is needed to avoid bias due to data composition and to reach a more general conclusion. Because the masticatory muscles function cooperatively and elaborately during jaw movement,67 the pathological changes in one masticatory muscle will ultimately affect other muscle pathologies. Therefore, it is necessary to further study the differences before and after whiplash injury of each muscle over a long period of observation, and the relationships among the masticatory muscles.

Conclusions

We investigated and analyzed the clinical and MRI findings of patients with TMD caused by whiplash injury, and compared the results of patients with idiopathic causes to TMD. This is the first study to comprehensively investigate the four major masticatory muscles after whiplash injury using MRI, and their correlation with clinical TMD indexes. We suggest that patients with TMD who have whiplash macrotrauma can have different neurophysiological responses and pain control mechanisms than those with idiopathic causes. Although consistent results for drawing a general conclusion are limited, we hope our results can help in understanding the clinical symptoms and neuropathophysiology of whiplash-related TMD, and provide information for the appropriate wTMD-specific treatment strategy.

Declarations

Data Availability Statement

The datasets generated and/or analyzed during this study are available from the corresponding author upon reasonable request. Because patient consent is required for data disclosure, we may disclose data conditionally through internal discussion and the Institutional Review Board (IRB) of the Kyung Hee University Dental Hospital.

Acknowledgments: None.

Conflicts of Interest: The authors declare no conflicts of interest.

Consent to participate/Consent to publish: Y.-H.L. wrote the paper. Y.-H.L. and Q.-S.A contributed to data acquisition, Y.-H.L. and K.-M.L. for both data analysis and interpretation. Y.-H.L., and K.-M.L. provided their expertise and contributed to the figures. Y.-H.L. provided her expertise and contributed to the revisions. All authors have read and agreed to the published version of the manuscript.

Funding: This research was supported by the National Research Foundation of Korea (NRF) Grant funded by the Korean government (MIST) (No. NRF 2020R1F1A1070072 obtained by Y.-H.L.), and by the Korea Medical Device Development Fund grant funded by the Korean government (the Ministry of Science and ICT, the Ministry of Trade, Industry and Energy, the Ministry of Health & Welfare, Republic of Korea, the Ministry of Food and Drug Safety) (Project No. 202011B17).

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Tables

Table 1. Comparison of demographics, and VAS and TMD index scores

 

 

wTMD group

mean ± SD or n (%)

iTMD group

mean ± SD or n (%)

  

 

 

(n= 45)

(n=45)

p-value

 

Demographics

 

 

 

 

Age, yearsa  

37.94 ± 12.27

40.77 ± 18.02

0.387

 

Femaleb

31 (68.9 %)

33 (73.3 %)

0.816

 

Pain characteristics

 

 

 

 

Symptom duration, days a

66.27 ± 58.06

57.78 ± 48.33

0.453

 

VAS-I a

6.73 ±1.84

4.32 ± 2.80

<0.001***

 

TMD indexes

 

 

 

 

 PI a

0.27 ± 0.21

0.16 ± 0.18

0.0086**

 

 Neck PI a

0.45 ± 0.31

0.27 ± 0.23

0.003**

 

           

TMD, temporomandibular disorder; wTMD, the patients had experienced whiplash injury and had no TMD symptoms before the injury; iTMD, the patients who presented with idiopathic/ non-traumatic TMD symptoms without any history of head/neck trauma; VAS, visual analog scale; PI, palpation index; SD, standard deviation.

TMD, temporomandibular disorder; VAS, visual analog scale; PI, palpation index; SD, standard deviation

a: Results were obtained via Mann–Whitney U test, b: chi-square test (two-sided).

A p-value < 0.05 was considered significant. *: p-value < 0.05, **: p-value < 0.01, ***: p-value < 0.001. Significant results are in bold text.

 

Table 2. Distribution of contributing factors

 

 

wTMD group

iTMD group

 

 

n = 45

Column (%)

n = 45

Column (%)

p-value

Bruxism a

         

     No

40

(88.9)

40

(88.9)

1.000

     Yes

5

(11.1)

5

(11.1)

 

Clenching b

         

      No

41

(91.1)

33

(73.3)

0.026*

      Yes

4

(8.9)

12

(26.7)

 

Tinnitus a

         

      No

30

(66.7)

35

(77.8)

0.347

      Yes

15

(33.3)

10

(22.2)

 

Headache a

         

      No

13

(28.9)

27

(60.0)

0.006**

      Yes

32

(71.1)

18

(40.0)

 

Sleep problem a

       

      No

29

(64.4)

19

(42.2)

0.028*

      Yes

26

(57.8)

16

(35.6)

 

Psychological distress a

 

 

 

 

 

      No

39

(86.7)

30

(66.7)

0.045*

      Yes

15

(33.3)

6

 (13.3)

 

             

TMD, temporomandibular disorder, wTMD, the patients had experienced whiplash injury and had no TMD symptoms before the injury, iTMD; the patients who presented with idiopathic or non-traumatic TMD symptoms without any history of head/neck trauma.

The results were obtained via a chi-square test (two-sided), and b: Fisher’s exact test. A p-value < 0.05 was considered significant. *: p-value < 0.05, **: p-value < 0.01. Significant results are in bold text.

 

Table 3. Comparison of joint abnormalities from MRI

 

wTMD group

iTMD group

 

 

n = 45

Column (%)

n = 45

Column (%)

p-value

 

ADDWR

No

34

(75.6)

32

(71.1)

0.812

 

 

Yes

11

(24.4)

13

(28.9)

 

 

ADDWoR

No

21

(46.7)

32

(71.1)

0.032*

 

 

Yes

24

(53.3)

13

(28.9)

 

 

Disc deformity

No

16

(35.6)

30

(66.7)

0.006**

 

 

Yes

29

(64.4)

15

(33.3)

 

 

Condylar degeneration

No

19

(42.2)

27

(60.0)

0.140

 

 

Yes

26

(57.8)

18

(40.0)

 

 

Effusion

No

35

(77.8)

36

(80.0)

1.000

 

 

Yes

10

(22.2)

9

(20.0)

 

 

TMD, temporomandibular disorder; wTMD, the patients had experienced whiplash injury and had no TMD symptoms before the injury; iTMD, the patients who presented with idiopathic or non-traumatic TMD symptoms without any history of head/neck trauma; ADDWR, anterior disc displacement with reduction; ADDWoR, anterior disc displacement without reduction

The results were obtained via the chi-square test (two-sided). A p-value < 0.05 was considered significant. *: p-value < 0.05, **: p-value < 0.01. Significant results are in bold text.

 

Table 4. Comparison of masticatory muscle abnormalities from MRI

 

 

wTMD group

iTMD group

 

 

 

n = 45

Column (%)

n=45

Column (%)

p-value

 

Masseter muscle b

VC

No

45

(100.0)

45

(100.0)

.

 

   

Yes

0

(0.0)

0

(0.0)

 

 

 

SC

No

45

(100.0)

45

(100.0)

 

 

   

Yes

0

(0.0)

0

(0.0)

 

 

Temporalis muscle b

VC

No

44

(97.8)

44

(97.8)

1.000

 

   

Yes

1

(2.2)

1

(2.2)

 

 

 

SC

No

44

(97.8)

44

(97.8)

1.000

 

   

Yes

1

(2.2)

1

(2.2)

 

 

LPM a

VC

No

19

(42.2)

37

(82.2)

<.0001***

 

   

Yes

26

(57.8)

8

(17.8)

 

 

 

SC

No

26

(57.8)

38

(84.4)

0.010**

 

   

Yes

19

(42.2)

7

(15.6)

 

 

MPM b

VC

No

45

(100.0)

43

(95.6)

0.494

 

   

Yes

0

(0.0)

2

(4.4)

 

 

 

SC

No

45

(100.0)

43

(95.6)

0.494

 

 

 

Yes

0

(0.0)

2

(4.4)

 

 

                     

TMD, temporomandibular disorder; wTMD, the patients had experienced whiplash injury and had no TMD symptoms before the injury; iTMD, the patients who presented with idiopathic/ non-traumatic TMD symptoms without any history of head/neck trauma; LPM, lateral pterygoid muscle; MPM, medial pterygoid muscle; VC, volume change; SC, signal change.

The results were obtained via a chi-square test (two-sided), and b: Fisher’s exact test. A p-value < 0.05 was considered significant. **: p-value < 0.01, ***: p-value < 0.001. Significant results are in bold text.

 

Table 5. Comparison of muscle tenderness upon palpation test

 

 

wTMD group

iTMD group

 

 

 

 

n=45

Column (%)

n=45

Column (%)

p-value

 

Masseter muscle tenderness a

 

 

No

13

(28.9)

16

(35.6)

0.652

 

 

Yes

32

(71.1)

29

(64.4)

 

 

Temporalis muscle tenderness a

 

 

No

18

(40.0)

29

(64.4)

0.034*

 

 

Yes

27

(60.0)

16

(35.6)

 

 

LPM tenderness b

         

 

No

35

(77.8)

44

(97.8)

0.007**

 

 

Yes

10

(22.2)

1

(2.2)

 

 

MPM tenderness b

         

 

No

38

(84.4)

45

(100.0)

0.012*

 

 

Yes

7

(15.6)

0

(0.0)

 

 

                           

TMD, temporomandibular disorder; wTMD, the patients had experienced whiplash injury and had no TMD symptoms before the injury; iTMD, the patients who presented with idiopathic/ non-traumatic TMD symptoms without any history of head/neck trauma; LPM, lateral pterygoid muscle; MPM, medial pterygoid muscle.

The results were obtained via a chi-square test (two-sided), and b: Fisher’s exact test. A p-value < 0.05 was considered significant. *: p-value < 0.05, **: p-value < 0.01. Significant results are in bold text.

 

Table 6. Associated abnormal MRI findings with increasing TMD index

 

wTMD

 

iTMD

 

VAS

PI

Neck PI

 

VAS

PI

Neck PI

 

r

p-value

r

p-value

r

p-value

 

r

p-value

r

p-value

r

p-value

TMD index

 

 

 

 

 

 

 

 

 

 

 

 

 

PI

0.174

0.252

1.000

 

.866***

<0.001

 

.300*

0.045

1.000

 

.764***

<0.001

Neck PI

0.081

0.597

.866***

<0.001

1.000

 

 

.301*

0.044

.764***

<0.001

1.000

 

Abnormality of masticatory muscle

Temp. VC

-0.124

0.416

-0.180

0.236

-0.006

0.970

 

-0.029

0.849

-0.059

0.703

-0.035

0.820

Temp. SC

-0.124

0.416

-0.180

0.236

-0.006

0.970

 

-0.029

0.849

-0.059

0.703

-0.035

0.820

LPM VC

-0.254

0.092

-0.089

0.563

0.094

0.540

 

-0.135

0.377

-0.210

0.167

-0.092

0.547

LPM SC

.346*

0.020

0.069

0.650

0.229

0.130

 

-0.185

0.224

0.061

0.689

-0.171

0.262

MPM VC

-

-

-

-

-

-

 

-0.217

0.153

-0.293

0.051

-0.064

0.674

MPM SC

-

-

-

-

-

-

 

-0.217

0.153

-0.293

0.051

-0.064

0.674

Abnormality of TMJ

ADDWR

-0.043

0.781

0.208

0.171

0.130

0.395

 

0.064

0.674

-0.202

0.184

-0.178

0.241

ADDWoR

0.040

0.793

-0.158

0.299

-0.084

0.582

 

.325*

0.029

0.124

0.418

0.169

0.268

Disc deformity

-0.175

0.251

0.000

1.000

-0.029

0.852

 

0.200

0.187

-0.082

0.591

-0.007

0.962

Condylar degeneration

-0.053

0.730

-0.089

0.563

-0.144

0.345

 

.297*

0.047

-0.070

0.646

0.098

0.521

Effusion

0.021

0.891

-0.274

0.068

-0.134

0.379

 

0.180

0.236

0.181

0.234

0.067

0.664

TMD, temporomandibular disorder; wTMD, the patients had experienced whiplash injury and had no TMD symptoms before the injury; iTMD, the patients who presented with idiopathic/ non-traumatic TMD symptoms without any history of head/neck trauma; PI, palpation index; Temp, temporalis muscle; LPM, lateral pterygoid muscle; MPM, medial pterygoid muscle; VC, volume change; SC, signal change; ADDWR, anterior disc displacement with reduction; ADDWoR, anterior disc displacement without reduction. Volume and signal changes of the masseter muscle were not observed at all, so the correlation coefficient related to this muscle could not be determined.

The results were obtained via Spearman’s correlation analysis. A p-value < 0.05 was considered significant. **: p-value < 0.01, ***: p-value < 0.001. Significant results are in bold text.