Erick Alves dos Santos1†
Beatriz Rodrigues Risuenho Peinado1†
Deborah Ribeiro Frazão1
Yago Gecy de Sousa Né1
Nathalia Carolina Fernandes Fagundes1,2
Marcela Baraúna Magno3
Lucianne Cople Maia3
Rafael Rodrigues Lima1*
Renata Duarte de Souza-Rodrigues1- 1Laboratory of Functional and Structural Biology, Institute of Biological Sciences, Federal University of Pará, Belém, Pará, Brazil
- 2School of Dentistry, Faculty of Medicine and Dentistry, University of Alberta, Edmonton, AB, Canada
- 3Department of Pediatric Dentistry and Orthodontics, School of Dentistry, Federal University of Rio de Janeiro, Rio de Janeiro, Brazil
Temporomandibular Joint Dysfunction (TMD) is an umbrella term that includes musculoskeletal and neuromuscular conditions affecting the temporomandibular joint. The present systematic review aimed to verify whether there is a specific association between TMD and anxiety. The searches were carried out in electronic databases, including PubMed, Scopus, Web of Science, and LILACS, without restrictions on publication date and language. The acronym PECO was used, whose participants (P) were humans exposed to TMD (E), compared to participants without TMD (C) and the presence of anxiety as an outcome (O). After the search retrieval, the duplicates were removed, and the articles were evaluated by title and abstract, following our inclusion and exclusion criteria; then, the papers were read and thoroughly assessed. After selection, the methodological quality was performed using the Newcastle-Ottawa Scale (NOS) for observational studies. The Grading of Recommendations, Assessment, Development, and Evaluation (GRADE) tool was used to assess the level of evidence. A total of 710 studies were found, and 33 articles were considered eligible and were included for the qualitative synthesis and the level of evidence assessment. The studies confirmed the association between anxiety and DTM, although there was a low certainty of evidence among the selected studies. Most articles showed a low risk of bias. Although the limitations of this systematic review, it suggested a significant association between anxiety and TMD, as well as highlights possible directions for future research.
Introduction
For the American Academy of Orofacial Pain (AAOP), Temporomandibular Joint Dysfunction (TMD) is described as an umbrella term that includes musculoskeletal and neuromuscular conditions, which can affect the Temporomandibular Joint (TMJ), masticatory muscles, and/or their associated structures (1). Usually, TMD is classified into subgroups, articular or muscular origin. In the first case, signs and symptoms are related to TMJ. And in the second case, symptoms and signs are related to stomatognathic structure (2).
The etiology of TMD is not fully understood; however, it is known to has a multifactorial origin, which can result from abnormal interference from psychological, physiological, structural (occlusion and trauma), and postural (parafunctional habits) and genetic conditions. These conditions may compromise the homeostasis state of the stomatognathic system, since they can act as initiating, predisposing, and perpetuating factors, resulting in the appearance of TMD signs and symptoms (3–5).
A recent study investigated the prevalence of temporomandibular disorders among the general population and concluded that the overall prevalence of TMD was approximately 31% on adults/elderly and 11% for children/adolescents. When evaluated according to joint or muscle subgroups, the authors found that the most prevalent TMD was disc displacement with reduction (DDwR), that was present in approximately 26% in adults/elderly and 7.5% in children/adolescents (2). The literature presents a range of acute or chronic symptoms commonly reported, such as pain and/or discomfort in the TMJ, ears, chewing muscles, eyes, and face; psychological distress; physical disability; noises, crackles or clicks on the joint; locking or considerable limitation of jaw opening, closing and laterality movements (3, 6, 7).
Previous studies have shown that psychosocial disorders and psychosocial impairment play an important role in the development of TMD (5, 8–14). The Orofacial Pain Prospective Evaluation and Risk Assessment (OPPERA) highlights that the prevalence of psychosocial factors is higher in TMD patients compared to the healthy individuals (15). It is presumed to act as both initiating and perpetuating factors (11). Anxiety stands out as a comorbidity frequently associated with TMJ disorders, as it can change pain sensations and release neurotransmitters related to parafunctional habits. Also, anxiety can potentiate the hyperactivity of chewing muscles associated with TMJ, resulting in joint overload (4, 5, 7, 16). It can be classified according to the frequency of manifestations: state anxiety, that is a pathological emotional response of varying intensity on a particular stressor, specific, unique; and trate anxiety, an emotional state changed variable intensity trend of reactions to different stressors, treated as a stable behavioral characteristic (17).
Recently, a systematic review (18) investigated whether there is a subtype of temporomandibular disorder that is more associated with the occurrence and severity of both anxiety and depression (together in the same patient) and the authors concluded that patients with myofascial pain are more anxious and depressed than others. In this way, it is clear how necessary to investigate separately biopsychosocial factors during the evaluation of TMD patients (5, 14). Thus, based on previously reported findings on the relationship between biopsychosocial factors and TMD, the present systematic review aims to investigate whether there is association between anxiety and TMD, regardless of the subtype.
Methodology
Protocol and registration
This systematic review was designed in accordance with the Preferred Reporting of Systematic Review and Meta-analyses (PRISMA) (19) and registered with Open Science Framework under the doi: https://doi.org/1017605/OSF.IO/YN3VJ.
Eligibility criteria and search strategy
The research question of this systematic review was “Is there an association between temporomandibular disorders and anxiety?” Therefore, our eligibility criteria were based on the PECO acrostic to look for observational studies in adult humans (P), exposed to a diagnostic of TMD of any kind, such as muscular, articular, or pain-related (TMD) (E), compared to participants without TMD diagnostic (C), having as an outcome the presence of anxiety (O). There was no restriction of year of publication nor language. Our exclusion criteria were case reports, descriptive, opinion, technical, animal, and in vitro studies.
The searches started in January 2022, with no language defined for the results, in which 4 (four) digital databases were consulted: PubMed, Scopus, Web of Science, and LILACS. It was planned in the registered protocol to search 8 databases but only 4 could be covered, excluding the grey literature. Besides, after selecting the articles, a hand research was done through the final studies' references. All publications complied with pre-defined combination requirements based on Medical Subjects Headings (MeSH) and entry terms. Boolean Operators (AND, OR) were used with different MeSH terms and related.
Selection process
The selection process was carried out by two examiners (EAS and BRRP), and a third examiner (DRF) was consulted to reduce the chances of errors and disagreements between the two evaluators. All the references collected were managed using EndNote Software, VX7. Duplicate studies were considered only once after identification and exclusion. After the exclusion of duplicate studies, the bibliographies were again submitted to inclusion and exclusion criteria based on the title and abstract analysis. The resulting articles were read in full and excluded if they did not comply with the authors' PECO search strategy.
Data extraction
An extraction table was made by two authors (EAS and DRF), separating the data in various aspects: author and year of publication, study design, country of study, characteristics of the participants (exposed and control group), sample size and age group, TMD and anxiety assessment methods, statistical tests and results obtained.
Methodological quality
The Newcastle-Ottawa Scale (NOS) assessed the methodological quality of the selected studies. According to the NOS' guideline, the system of stars/asterisks (*) was adopted to indicated the score attributed to each article in each domain of the NOS after two authors had performed the evaluation and judgement. For case–control and cohort studies, the maximum number was nine stars distributed in three domains: Selection (adequate definition of cases, representativeness of cases, selection of controls, and definition of controls), comparability, and exposure (exposure verification, the only evaluation method for cases and controls and non-response rate). For cross-sectional studies, the total number of stars could vary from 0 to 10, in which they were also distributed in three domains: selection (sample representativeness, sample size, non-response rate, and exposure verification), comparability, and outcome (outcome assessment and statistical test used). The criteria for each domain are exposed in Supplementary Table 1.
Level of evidence
GRADE (Grading of Recommendations Assessment, Development and Evaluation) was used to analyze the quality of evidence. GRADE is a grading system for the quality of evidence and strength of health recommendations. When serious or extremely serious issues related to the risk of bias, inconsistency, indirectness, imprecision, and publication bias are observed, the certainty of evidence decreases by one or two. If the effect of all plausible confounding factors is minimized or suggests a spurious effect, the quality of evidence tends to increase. The magnitude of an effect and dose-response could not be evaluated in the present GRADE and was not considered. GRADE was sub-grouped according to anxiety.
Results
Studies selection and characteristics
In total, 710 manuscripts were found through electronic database searches, 75 of which were rejected due to duplication criteria. The titles and abstracts of 635 studies were examined, resulting in the exclusion of 591 articles and the selection of 44 to read the full text. All articles that did not apply to the PECO established by the authors were removed. The reasons for exclusion were as follows: non-observational studies (20–22), the absence of a control group (23–27). Therefore, this systematic review included 33 studies for qualitative analysis (Figure 1).
Figure 1. Flow diagram of the selected studies according to the PRISMA protocol.
Results of individual studies
There were 13 cross-sectional studies and 20 case–control studies among the 33 studies included. The research question was answered after analyzing the data extraction table (Table 1), in which 30 studies indicated an association between the presence of TMD and anxiety, while only four articles did not indicate such an association in their results. Some studies have developed more detailed indexes for anxiety assessment, presenting, in addition to the diagnosis of this pathology, the classification into two major groups: trait anxiety and state anxiety.
Table 1. Extraction of the studies' results.
The included studies were carried out in 16 countries: Brazil (n = 10), Canada (n = 2), China (n = 2), Croatia (n = 1), Germany (n = 3), India (n = 1), Italy (n = 1), Nigeria (n = 1), Norway (n = 1), Poland (n = 1), Scotland (n = 1), Vietnam (n = 1), Singapore (n = 1), Socialist Democratic Republic of Sri Lanka (n = 1), Thailand (n = 1), and USA (n = 5).
Therefore, it is clear that the results used in this review came from epidemiological studies that used samples from 4 of the 5 continents of the globe.
In terms of sample origin, 14 studies used patients from dental schools or specific university departments in the area; 14 studies used patients from hospitals and/or large dental health centers; 5 from a university population; 5 from the general community selected according to the authors' methods; 3 from private dental offices; and 2 from university institutes. Certain studies may have developed their samples from more than one of the locations mentioned above.
The Research Diagnostic Criteria for Temporomandibular Disorders (RDC/TMD) (axis I and/or II) was the most commonly used parameter for the evaluation of TMD, followed by Fonseca's Anamnestic Index (FAI) and the Academy of Orofacial Pain's Guidelines for Diagnosis of TMD, besides the clinical evaluation of the signs and symptoms presented. For anxiety assessment, several instruments were available: Minnesota Multiphasic Personality Inventory (MMPI), Speilberger State-Trait Anxiety Inventory (STAI), The State-Trait Anxiety Inventory [STAI-S and -T]; Eysenck Personality Questionnaire (EPQ), Pennybaker Inventory of Limbic Languidness (PILL), Scale ranging from 1 to 5 (from very relaxed to extremely tense) after the electromyographical evaluation, Hospital Anxiety and Depression Scale questions (HADS), The Crown Crisp Experimental Index (CCEI), Taylor Manifest Anxiety State, State-Trait Personality Inventory (STPI), Emotion Assessment Scale (EAS), Positive and Negative Affect Scale (PANAS), Visual Analog Scale (VAS), The Symptom Checklist 90—Revised (SCL-90R); SCL-90 Questionnaire, The symptom check list of 90 revised questionnaire (SCL-90R), Self-report questionnaire PAS-SR (version of SCIPAS), The 28-item General Health Questionnaire (GHQ-28), Beck Anxiety Inventory (BAI), Life Events Scale, Anamnesis Index and the State-Trait Anxiety Inventory (IDATE), Composite International diagnostic Screener (CID-S), Zung self-rating scale, Young Schemes Questionnaire—reduced form, Young Schemes Questionnaire—reduced form, Four Dimensional Questionnaire (4DSQ), Sense of Coherence Orientation to Life Questionnaire, 2-item version of the Coping Strategies Questionnaire, The Depression, Anxiety and Stress Scale-21 (DASS-21), and Self-reported 7-item Generalized Anxiety Disorder Scale (GAD-7).
Qualitative synthesis of the studies
Tables 2, 3 summarize the findings of the NOS methodological quality assessment. As a result, 15 studies were judged to be of high quality (6–8, 16, 28, 34, 39, 40, 45, 47–49, 53, 55, 56); 10 as medium quality (35–37, 41, 42, 44, 50, 51, 54); and 9 as low quality with a high risk of bias (5, 17, 29–31, 38, 46, 52, 58).
Table 2. Newcastle-Ottawa Scale for cross-sectional studies.
Table 3. Newcastle-Ottawa Scale for case-control studies.
The main issues found in studies with a high risk of bias were case representativeness, no control group definition, lack of information about the verification of exposure, and no description of the non-response rate. Minimum defects in the representativeness of the cases, sample size, and non-response rate were perceived in articles with a moderate risk of bias. In studies that demonstrated a low risk of bias, only the verification of the exposure offered a minimum issue, since the assessment of anxiety was performed using questionnaires. Hence, according to the qualifier, questionnaires are regarded as a probable source of bias.
Quantitative analysis (meta-analysis)
We could not conduct a meta-analysis due to differences in study methodologies, such as subject age, TMD diagnosis, and finally, although the authors used the same anxiety indices (such as HADS and STAI-T), the outcomes were presented in different ways (median, mean, frequency, etc.). Furthermore, studies with the same TMD diagnosis and anxiety analysis methodology, as well as participants of similar ages, had varying methodological quality. As a result, the meta-results analysis's would be inconsistent and highly heterogeneous. Therefore, we decided to only include a summary of findings from the GRADE system.
Level of evidence (GRADE)
The level of evidence was evaluated for the following outcomes: anxiety-trait and TMD are not related; anxiety-state and TMD are positively related; anxiety-trait and state and TMD are positively related; anxiety-symptoms and TMD are positively related; anxiety-level and TMD are positively related. In general, the certainty of the evidence was rated as low and very low. Many of the studies included in the syntheses presented methodological limitations that could have seriously affected the estimates reported. Clearly, the methodological heterogeneity among the studies explains the inconsistency of the results. Finally, even for the outcomes that included more studies, the number of individuals considered when synthesizing the information was small; thus, it was deemed that the imprecision item was seriously affected. Only the outcome “Anxiety symptoms and TMD are positively related” did not demonstrate any serious problem, thus showing a low certainty of evidence. The results of certainty of evidence results are described in Table 4.
Table 4. Certainty of evidence.
Discussion
The relationship between TMD and psychosocial impairment is widely explored in the literature (12–14, 56). However, despite the specific association between TMD and anxiety has been the subject of some studies (5, 8–11), to our knowledge, this is the first systematic review that has evaluated this relationship individually. In the quantitative analysis, our results confirmed the association between anxiety and DTM, although a low certainty of evidence among the selected studies.
Several assessment instruments were used for the classification of TMD. It was noted that before the elaboration of the RDC/TMD (59), with took place in 1992, all studies (28–30, 34, 35) used different instruments, which were mainly based on clinical story, signs and symptoms, clinical diagnosis of TMJ and masticatory muscles. Only one study (31) used a validated questionnaire, The Helkimo Clinical Dysfunction Index (HCDI). Half of these studies indicated that patients with TMD showed higher state and/or trait anxiety levels, while the other half did not show significant differences regarding anxiety or anxiety traits between patients with and without TMD. The lack of standardization in the diagnosis of TMD may have influenced the studies' findings and made it impossible to compare them.
Since the introduction of the RDC/TMD (59), this has been used especially to standardize research findings and represented an important advance as it is composed of two axes: Axis I, with an emphasis on physical diagnosis, and Axis II, addresses biopsychosocial aspects and pain-related disability. From the emergence of this assessment instrument, evidence demonstrating the importance of psychological assessment and pain disability has been growing and psychological factors came to be considered at least as important for treatment outcome as pain intensity and physical diagnoses (60). However, not all selected studies have used RDC/TMD. Only 13 did so (5, 6, 8, 17, 36, 37, 39, 40, 42, 45–47, 53); while another 14 used different assessment methods, such as Fonseca Anamnestic Index and Diagnostic Criteria of The American Academy of Craniomandibular Disorders (7, 16, 38, 41, 43, 44, 48–52, 54, 56, 61).
Among the studies that used the RDC/TMD, 11 obtained results that were positively associated TMD with anxiety. Only 3 mentioned the related TMD subtype, such as myofascial pain or joint pain (39, 40, 42). A previous study (62) evaluated the correlation between Axis I and Axis II diagnosis of the RDC/TMD and investigated whether the presence of pain could mediate correlation to them. The authors concluded that there is no specific correlation between the two Axes findings and identified that the presence of pain, whether of muscular or joint origin, was correlated with Axis II findings. Besides that higher levels of pain-related impairment were associated with the most severe score of psychological symptoms evaluated, depression and somatization.
Among the studies evaluated in the present study, only one (55) has used DC/TMD (63), a more recent and updated RDC/TMD version, with the purpose of both research and clinical use. This assessment instrument includes revised and new validated tools for both the physical diagnosis (Axis I) and the psychological and disability assessment (Axis II). The latter Axis offers a brief assessment with a minimal number of short screening instruments for the most important variables that may influence the development or perpetuation of symptoms, or an expanded assessment with a more comprehensive set of instruments, some specific to orofacial pain (60). Perhaps just only this study has used it, because this is a relatively new tool, and the translation and validation of this questionnaire for other languages took place gradually (2). In the specific case of this study, the results demonstrated that one-third of the evaluated individuals presented symptoms of TMD and perceived more intensive symptoms of anxiety.
In none of the articles included in our systematic review, the International Classification of Orofacial Pain (ICOP) was used, most likely because it is a very recent instrument (64).
Regarding the diagnosis of anxiety, several validated tools were used. Among these, the most used were the following: The Spielberger State-Trait Anxiety Inventory (STAI) (65), which was used as the only assessment instrument by 7 studies (7, 17, 29, 41, 44, 47, 53). It consists of 2 self-administered questionnaires: one, about State-anxiety (STAI-S), a transient emotional state or condition that is characterized by consciously perceived unpleasant feelings of tension and increased activity of the autonomic nervous system; and the other, about Trait-anxiety (STAI-T), relatively stable individual differences in anxiety propensity, the difference in reacting into situations perceived as threatening, which can increase the intensity of anxiety state (66). Another tool was the Hospital Anxiety and Depression Scale (HADS), a reliable instrument for screening clinically significant anxiety and depression (33). It was used by 3 studies (8, 49, 51). Also, The Symptom Checklist 90 (SCL-90 Questionnaire), both in its revised and complete version (38, 39, 43) and comprises a 90-item self-report symptom scale, multidimensional, which included subcategories of somatization, obsessive-compulsive symptoms, interpersonal sensitivity, depression, anxiety, hostility, phobic anxiety, paranoid ideation, and psychoticism (67). In fact, some studies used more than one assessment instrument (5, 30, 31, 36, 37, 42, 46), and although this difference between methodological protocols makes it difficult to compare the results of the analyzed studies, it is possible to observe that most of them obtained as results a positive association between TMD and anxiety, i.e., patients with TMD had higher levels of anxiety when compared to individuals without TMD.
In summary, although all the articles selected in our systematic review have very different methodological approaches, with very diverse samples as well. Therefore some aspects are found to be coinciding with those previously described in the literature. For example, in most studies, the prevalence of TMD, as well as anxiety, was higher in women who were in adulthood, in an age group between 20 and 40 years. In these patients, the main signs and symptoms of TMD were muscle and/or joint pain and limitation in mandibular range of motion. All of these lasted more than 6 months and, in some cases, even years.
Previous systematic reviews have already revealed this positive association between TMD and psychosocial factors. Recently, Reis et al. (18) demonstrated the relationship between distinct subtypes of TMD and anxiety and depression. These results suggest that patients with myofascial pain are more anxious and more depressed than patients with other subtypes of TMD, especially disc displacement or arthralgia/degenerative joint disease. The authors suggest that the lower sensitivity of the RDC/TMD in arthralgia diagnosis could have overestimated myofascial pain diagnosis. Häggman-Henrikson et al. (12) suggest an association between catastrophizing and TMD. The findings of these authors pointed not only a higher level of catastrophizing in TMD patients but also an association between levels of catastrophizing, symptoms severity, and treatment outcomes. For the authors, higher levels of catastrophizing before treatment can be associated with patients who do not respond to treatment and report higher activity interference 1 year later. De La Torre Canales et al. (14) indicate that psychological disorders and psychosocial impairment are highly prevalent in TMD patients, mainly severe-to-moderate somatization and depression. Severe physical impairment was not commonly reported in this study.
Some hypotheses were elaborated by the studies selected in the present systematic review to explain this association between TMD and anxiety. Boscato et al. (49) emphasized that anxiety plays an important role in TMD and can be considered as an initiating or aggravating factor. For them, during clinical evaluation, anxious individuals report greater pain intensity. de Oliveira et al. (52) highlighted that trait anxiety appeared to play a role mainly as an etiological agent, whereas the anxiety state had a more psychosomatic impact on TMD severity. Monteiro et al. (47) ratified two basic concepts cited in the literature to explain this association: individuals with neuroticism tend to be often anxious and anxious subjects could increase attention to pain, thereby amplifying their perceived intensity. For Reissmann et al. (68), anxiety has an important role in TMD and, in this way, a person's general disposition to be anxious can be considered as a risk factor for TMD pain. From the results found in their study, Staniszewski et al. (56) hypothesized that psychological factors may contribute to chronic upregulation of the HPA axis, with higher salivary cortisol (F) secretion from the adrenal cortex.
The findings of the present systematic review are specific to TMD and anxiety. The level of evidence evaluation thought GRADE assessment presents a low level, which is related to observational studies evaluated since methodological discrepancies, such as different studies design, representativeness of the sample, sample size, control group criteria, and non-valid diagnostics instruments. Despite the low certainty of the evidence, it is important to note that the most selected studies demonstrated the association between TMD and anxiety.
Conclusions
Considering the limitations of this systematic review, it can be suggested a significant association between anxiety and TMD, as well as highlights possible directions for future research. Thereby, to establish a high certainty of evidence related to the association between anxiety and TMD, it is necessary to carry out further studies that focus on one of the TMD subtypes (articular or muscular) and that assess anxiety as a risk factor for the initiation, development, or perpetuation of TMD, which can make it difficult for patients to respond to TMD treatment.
Data availability statement
The original contributions presented in the study are included in the article/Supplementary material, further inquiries can be directed to the corresponding author/s.
Author contributions
ES, BP, and RS-R: study concept and design. ES, BP, DF, YN, NF, MM, LM, RRL, and RS-R: analysis and interpretation of data. ES, BP, DF, and YN: preparation of the manuscript. NF, MM, LM, RRL, and RS-R: critical revision of the manuscript. All authors contributed to the article and approved the submitted version.
Funding
RRL is a researcher from Conselho Nacional de Desenvolvimento Científico e Tecnológico (CNPq) and received Grant No. 312275/2021-8. The Article Processing Charges (APC) was funded by Pró-Reitoria de Pesquisa e Pós-graduação from Federal University of Pará (PROPESP-UFPA).
Acknowledgments
We would like to thank the Federal University of Pará, Federal University of Rio de Janeiro, and the University of Alberta for technical and scientific support.
Conflict of interest
The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest.
Publisher's note
All claims expressed in this article are solely those of the authors and do not necessarily represent those of their affiliated organizations, or those of the publisher, the editors and the reviewers. Any product that may be evaluated in this article, or claim that may be made by its manufacturer, is not guaranteed or endorsed by the publisher.
Supplementary material
The Supplementary Material for this article can be found online at: https://www.frontiersin.org/articles/10.3389/fpsyt.2022.990430/full#supplementary-material
References
1. de Leeuw R, Klasser GD. Orofacial Pain: Guidelines for Assessment, Diagnosis, and Management. New York, NY: Quintessence. (2013).
2. Valesan LF, Da-Cas CD, Réus JC, Denardin ACS, Garanhani RR, Bonotto D, et al. Prevalence of temporomandibular joint disorders: a systematic review and meta-analysis. Clin Oral Investig. (2021) 25:441–53. doi: 10.1007/s00784-020-03710-w
3. Chisnoiu AM, Picos AM, Popa S, Chisnoiu PD, Lascu L, Picos A, et al. Factors involved in the etiology of temporomandibular disorders - a literature review. Clujul Med. (2015) 88:473–8. doi: 10.15386/cjmed-485
4. Sójka A, Huber J, Kaczmarek E, Hȩdzelek W. Ascertaining of temporomandibular disorders (TMD) with clinical and instrumental methods in the group of young adults. J Med Sci. (2015) 84:20–6. doi: 10.20883/medical.e31
5. de Resende CMBM, da Silva Rocha LGD, de Paiva RP, da Silva Cavalcanti C, de Almeida EO, Roncalli AG, et al. Relationship between anxiety, quality of life, and sociodemographic characteristics and temporomandibular disorder. Oral Surg Oral Med Oral Pathol Oral Radiol. (2020) 129:125–32. doi: 10.1016/j.oooo.2019.10.007
6. Tay KJ, Yap AUJ, Wong JCM, Tan KBC, Allen PF. Associations between symptoms of temporomandibular disorders, quality of life and psychological states in Asian Military Personnel. J Oral Rehabil. (2019) 46:330–9. doi: 10.1111/joor.12751
7. do Patrocinio RT, dos Santos ACM, Penha ES, Almeida MSC, Guêmes GMT, Figueiredo CHM, et al. Disfunção temporomandibular e ansiedade em graduandos de Odontologia. Rev Cubana Estomatol. (2019) 56:42–51.
8. Giannakopoulos NN, Keller L, Rammelsberg P, Kronmüller KT, Schmitter M. Anxiety and depression in patients with chronic temporomandibular pain and in controls. J Dent. (2010) 38:369–76. doi: 10.1016/j.jdent.2010.01.003
9. Reiter S, Emodi-Perlman A, Goldsmith C, Friedman-Rubin P, Winocur E. Comorbidity between depression and anxiety in patients with temporomandibular disorders according to the research diagnostic criteria for temporomandibular disorders. J Oral Facial Pain Headache. (2015) 29:135–43. doi: 10.11607/ofph.1297
10. Bertoli E, de Leeuw R. Prevalence of suicidal ideation, depression, and anxiety in chronic temporomandibular disorder patients. J Oral Facial Pain Headache. (2016) 30:296–301. doi: 10.11607/ofph.1675
11. Simoen L, Van den Berghe L, Jacquet W, et al. Depression and anxiety levels in patients with temporomandibular disorders: comparison with the general population. Clin Oral Invest. (2020) 24:3939–45. doi: 10.1007/s00784-020-03260-1
12. Häggman-Henrikson B, Bechara C, Pishdari B, Visscher CM, Ekberg E. Impact of catastrophizing in patients with temporomandibular disorders-a systematic review. J Oral Facial Pain Headache. (2020) 34:379–97. doi: 10.11607/ofph.2637
13. Manfredini D, Winocur E, Ahlberg J, Guarda-Nardini L, Lobbezoo F. Psychosocial impairment in temporomandibular disorders patients. RDC/TMD axis II findings from a multicentre study. J Dent. (2010) 38:765–72. doi: 10.1016/j.jdent.2010.06.007
14. Canales GLT, Câmara-Souza MB, Lora VM, Guarda-Nardini L, Conti P, Garcia RMR, et al. Prevalence of psychosocial impairment in temporomandibular disorder patients: A systematic review. J Oral Rehabil. (2018) 45:881–9. doi: 10.1111/joor.12685
15. Slade GD, Ohrbach R, Greenspan JD, Fillingim RB, Bair E, Sanders AE, et al. Painful Temporomandibular Disorder: Decade of Discovery from OPPERA Studies. J Dent Res. (2016) 95:1084–92. doi: 10.1177/0022034516653743
16. Nguyen MS, Reemann P, Loorits D, Ilves P, Jagomägi T, Nguyen T, et al. Association of temporomandibular joint osseous changes with anxiety, depression, and limitation of mandibular function in elderly vietnamese. East Asian Arch Psychiat. (2019) 29:20–5. doi: 10.12809/eaap1749
17. Reissmann D, John M, Seedorf H, Doering S, Schierz O. Temporomandibular disorder pain is related to the general disposition to be anxious. J Oral Facial Pain Headache. (2018) 28:322–30.
18. Reis PH, Laxe LA, Lacerda-Santos R, Münchow EA. Distribution of anxiety and depression among different subtypes of temporomandibular disorder: A systematic review and meta-analysis. J Oral Rehabil. (2022) 49:754–767. doi: 10.1111/joor.13331
19. Page MJ, McKenzie JE, Bossuyt PM, Boutron I, Hoffmann TC, Mulrow CD, et al. The PRISMA 2020 statement: An updated guideline for reporting systematic reviews. PLoS Med. (2021) 18:1–15. doi: 10.1371/journal.pmed.1003583
20. Aghabeigi B, Feinmann C, Harris M. Prevalence of post-traumatic stress disorder in patients with chronic idiopathic facial pain. Br J Oral Maxillofac Surg. (1992) 30:360–4. doi: 10.1016/0266-4356(92)90201-s
21. Nally FF, Moore DS. Psychogenic, diagnostic and therapeutic aspects of temporomandibular joint pain: an analysis of 232 patients with discusssion. J Can Dent Assoc (Tor). (1975) 41:403–6.
22. Rosende MN, Peláez AN, Mazza SM. Niveles de ansiedad y su relación con los trastornos temporomandibulares / Anxiety levels and their relationship to temporomandibular disorders. Rev Ateneo Argent Odontol. (2016) 55:23–6.
23. De Leeuw R, Bertoli E, Schmidt JE, Carlson CR. Prevalence of traumatic stressors in patients with temporomandibular disorders. J Oral Maxillofac Surg. (2005) 63:42–50. doi: 10.1016/j.joms.2004.04.027
24. Mongini F, Ciccone G, Ceccarelli M, Baldi I, Ferrero L. Muscle tenderness in different types of facial pain and its relation to anxiety and depression: A cross-sectional study on 649 patients. Pain. (2007) 131:106–11. doi: 10.1016/j.pain.2006.12.017
25. Castro AR, Siqueira SR, Perissinotti DM, Siqueira JT. Psychological evaluation and cope with trigeminal neuralgia and temporomandibular disorder. Arquivos de neuro-psiquiatria. (2008) 66:716–9. doi: 10.1590/s0004-282x2008000500021
26. Kim HI, Lee JY, Kim YK, Kho HS. (2010). Clinical and psychological characteristics of TMD patients with trauma history. Oral Dis. 16:188–92. doi: 10.1111/j.1601-0825.2009.01626.x
27. Johnson J, Johansson M, Rydén A, Houltz E, Finizia C. Impact of trismus on health-related quality of life and mental health. Head Neck. (2015) 37:1672–9. doi: 10.1002/hed.23816
28. Solberg WK, Flint RT, Brantner JP. Temporomandibular joint pain and dysfunction: A clinical study of emotional and occlusal components. TMJ Pain Dysfunction. (1972) 28:412–22. doi: 10.1016/0022-3913(72)90243-0
29. Moss RA, Adams HE. The assessment of personality, anxiety and depression in mandibular pain dysfunction subjects. J Oral Rehabil. (1984) 11:233–5. doi: 10.1111/j.1365-2842.1984.tb00572.x
30. Southwell J, Deary IJ, And Geissler P. Personality and anxiety in temporomandibular joint syndrome patients. J Oral Rehabil. (1990) 17:239–43. doi: 10.1111/j.1365-2842.1990.tb00004.x
31. Schroeder H, Siegmund H, Santibáñez-H G, Kluge A. Causes and signs of temporomandibular joint pain and dysfunction: an electromyographical investigation. J Oral Rehabilit. (1991) 18:301–10. doi: 10.1111/j.1365-2842.1991.tb00061.x
32. Helkimo M. Studies on function and dysfunction of the masticatory system. II. Index for anamnestic and clinical dysfunction and occlusal state. Svensk tandlakare tidskrift. Swedish Dent J. (1974) 67:101–21.
33. Zigmond AS, Snaith RP. The hospital anxiety and depression scale. Acta Psychiatr Scand. (1983) 67:361–70. doi: 10.1111/j.1600-0447.1983.tb09716.x
34. Zarh GA, DDS MS, Andreasen K. Evaluation of the psychological profiles of patients with signs and symptoms of temporomandibular disorders. Craniomandib Function Dysfunct. (1991) 66:810–2. doi: 10.1016/0022-3913(91)90423-T
35. Stockstill JW, Callahan CD. Personality hardiness, anxiety, and depression as constructs of interest in the study of temporomandibular disorders. J Craniomandib Diso. (1991) 5:129–34.
36. Curran SL, Carlson CR, Okeson JP. Emotional and physiologic responses to laboratory challenges: patients with temporomandibular disorders versus matched control subjects. J Orofacial Pain. (1996) 10:701–707.
37. Jones DA, Rollman GB, Brooke RI. The cortisol response to psychological stress in temporomandibular dysfunction. Pain. (1997) 72:171–82. doi: 10.1016/S0304-3959(97)00035-3
38. Sirirungrojying S, Srisintorn S, Akkayanont P. Psychometric profiles of temporomandibular disorder patients in southern Thailand. J Oral Rehabil. (1998) 25:541–4. doi: 10.1046/j.1365-2842.1998.00298.x
39. Velly AM, Gornitsky M, Philippe P. Contributing factors to chronic myofascial pain: A case-control study. Pain. (2003) 104:491–9. doi: 10.1016/S0304-3959(03)00074-5
40. Manfredini D, Bandettini di Poggio A, Cantini E, Dell'Osso L, Bosco M. Mood and anxiety psychopathology and temporomandibular disorder: a spectrum approach. J Oral Rehabilit. (2004) 31:933–940. doi: 10.1111/j.1365-2842.2004.01335.x
41. Pallegama RW, Ranasinghe AW, Weerasinghe VS, Sitheeque MAM. Anxiety and personality traits in patients with muscle related temporomandibular disorders. J Oral Rehabil. (2005) 32:701–7. doi: 10.1111/j.1365-2842.2005.01503.x
42. Saheeb B, Otakpor A. Co-morbid pshychiatric disorders in nigerian patients suffering temporomandibular joint paint and dysfunction. Niger J Clin Pract. (2005) 8:23–8.
43. Xu WH, Ma XC, Guo C. bin, Wu RG. Psychological status in patients with temporomandibular disorders. Chin J Stomatol. (2005) 40:359–61.
44. Fernandes URA, Garcia A, Zuim RJP, Del L, Cunha PA, And Marchiori VA. Temporomandibular joint dysfunction and anxiety in graduate dentistry. Cienc Odontol Bras. (2007) 10:70–7.
45. Vedolin GM, Lobato VV, Conti PC, Lauris JR. The impact of stress and anxiety on the pressure pain threshold of myofascial pain patients. J Oral Rehabilit. (2009) 36:313–21. doi: 10.1111/j.1365-2842.2008.01932.x
46. Lajnert V, Frančišković T, GrŽic R, Kovačević Pavičić D, Bakarčić D, Buković D, Celebić A, Braut V, Fugošić V. Depression, somatization and anxiety in female patients with temporomandibular disorders (TMD). Collegium Antropol. (2010) 34:1415–1419.
47. Monteiro DR, Zuim PR, Pesqueira AA, do Prado Ribeiro P, Garcia AR. Relationship between anxiety and chronic orofacial pain of temporomandibular disorder in a group of university students. J Prosthodontic Res. (2011) 55:154–8. doi: 10.1016/j.jpor.2010.11.001
48. Bezerra BP, Ribeiro AI, Farias AB, Farias AB, Fontes LD, Nascimento SR, et al. Prevalence of temporomandibular joint dysfunction and different levels of anxiety among college students* Prevalência da disfunção temporomandibular e de diferentes níveis de ansiedade em estudantes universitários. Rev Dor. (2012) 13:235–42. doi: 10.1590/S1806-00132012000300008
49. Boscato N, Almeida RC, Koller CD, Presta AA, Goettems ML. Influence of anxiety on temporomandibular disorders - an epidemiological survey with elders and adults in Southern Brazil. J Oral Rehabil. (2013) 40:643–9. doi: 10.1111/joor.12076
50. Smriti JB, Patni VM, Mukta M, Gangotri S. Association between symptoms of temporomandibular disorders and gender, morphological occlusion, and psychological factor in dental student's. Int J Sci Study. (2014)2:55–8.
51. de Queiroz NB, Magalhães KM, Machado J, de Oliveira Viana M. Prevalência de disfunção temporomandibular e associação com fatores psicológicos em estudantes de Odontologia. Rev Cubana Estomatol. (2015) 10:52.
52. de Oliveira LK, Almeida GDA, Lelis ÉR, Tavares M, Neto AJF. Temporomandibular disorder and anxiety, quality of sleep, and quality of life in nursing professionals. Braz Oral Res. (2015) 29:1–7. doi: 10.1590/1807-3107BOR-2015.vol29.0070
53. Yu Q, Liu Y, Chen X, Chen D, Xie L, Hong X, et al. Prevalence and associated factors for temporomandibular disorders in Chinese civilian pilots. Int Arch Occup Environ Health. (2015) 88:905–11. doi: 10.1007/s00420-015-1018-1
54. Schmidt DR, Ferreira VRT, Wagner MF. Disfunção Temporomandibular: Sintomas de Ansiedade, Depressão e Esquemas Iniciais Desadaptativos. Temas em Psicologia. (2015) 23:973–85. doi: 10.9788/TP2015.4-13
55. Sójka A, Stelcer B, Roy M, Mojs E, Pryliński M. Is there a relationship between psychological factors and TMD? Brain Behav. (2019) 9:e01360. doi: 10.1002/brb3.1360
56. Staniszewski K, Lygre H, Bifulco E, Kvinnsland S, Willassen L, Helgeland E, et al. Temporomandibular disorders related to stress and HPA-axis regulation. Pain Res Manage. (2018) 2018:1–7. doi: 10.1155/2018/7020751
57. Zach GA, Andreasen K. Evaluation of the psychological profiles of patients with signs and symptoms of temporomandibular disorders. J Prosthet Dent. (1991) 66:810–2. doi: 10.1016/0022-3913(91)90423-t
58. Weihua X, Xuchen M, Chuan G, Rengang W. Investigation of the symptom self-assessment scale of patients with temporomandibular joint disorder. Chin J Stomatol. (2005) 40:1–3.
59. Dworkin SF, LeResche L. Research diagnostic criteria for temporomandibular disorders: review, criteria, examinations and specifications, critique. J Craniomandib Disord. (1992) 6:301–55.
60. Visscher CM, Baad-Hansen L, Durham J, Goulet JP, Michelotti A, Roldán Barraza C, et al. Benefits of implementing pain-related disability and psychological assessment in dental practice for patients with temporomandibular pain and other oral health conditions. J Am Dent Assoc. (2018) 149:422–31. doi: 10.1016/j.adaj.2017.12.031
61. Kindler S, Samietz S, Houshmand M, Grabe HJ, Bernhardt O, Biffar R, et al. Depressive and anxiety symptoms as risk factors for temporomandibular joint pain: a prospective cohort study in the general population. J Pain. (2012) 13:1188–97. doi: 10.1016/j.jpain.2012.09.004
62. De la Torre Canales G, Bonjardim LR, Poluha RL, Carvalho Soares FF, Guarda-Nardini L, Conti PR, et al. Correlation Between physical and psychosocial findings in a population of temporomandibular disorder patients. Int J Prosthodont. (2020) 33:155–9. doi: 10.11607/ijp.5847
63. Schiffman E, Ohrbach R, Truelove E, Look J, Anderson G, Goulet JP, et al. Diagnostic Criteria for Temporomandibular Disorders (DC/TMD) for Clinical and Research Applications: recommendations of the International RDC/TMD Consortium Network* and Orofacial Pain Special Interest Group†. J Oral Facial Pain Headache. (2014) 28:6–27. doi: 10.11607/jop.1151
64. ICOP. International Classification of Orofacial Pain, 1st edition. (2020) Cephalalgia: ICOP. Vol. 40. p. 129–221. doi: 10.1177/0333102419893823
65. Speilberger CD, Gorsuch R, Lushene R. Manual for the State-Trait Anxiety Inventory (“Self-Evaluation Questionnaire”). Palo Alto, CA: Consulting Psychologists Press. (1970).
66. Biaggio AMB, Natalício L, Spielberger CD. Desenvolvimento da forma experimental em português do Inventário de Ansiedade Traço-Estado (IDATE), de Spie1berger. Arq bras Psic apl, Rio de Janeiro. (1977) 29:3144.
67. Derogatis LR, Rickels K, Rock AF. The SCL-90 and the MMPI: A step in the validation of a new self-report scale. Br J Psychiatry. (1976) 128:280–9. doi: 10.1192/bjp.128.3.280
Keywords: Temporomandibular Joint Dysfunction, anxiety, psychosocial impairment, systematic review, oral health
Citation: Santos EA, Peinado BRR, Frazão DR, Né YGdS, Fagundes NCF, Magno MB, Maia LC, Lima RR and Souza-Rodrigues RD (2022) Association between temporomandibular disorders and anxiety: A systematic review. Front. Psychiatry 13:990430. doi: 10.3389/fpsyt.2022.990430
Received: 10 July 2022; Accepted: 25 August 2022;
Published: 13 October 2022.
Edited by:
Marco Tramontano, Santa Lucia Foundation (IRCCS), ItalyReviewed by:
Graziela De Luca Canto, Federal University of Santa Catarina, BrazilRavi Philip Rajkumar, Jawaharlal Institute of Postgraduate Medical Education and Research (JIPMER), India
Copyright © 2022 Santos, Peinado, Frazão, Né, Fagundes, Magno, Maia, Lima and Souza-Rodrigues. This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
*Correspondence: Rafael Rodrigues Lima, rafalima@ufpa.br
†These authors have contributed equally to this work and share first authorship