Introduction
Major depressive disorder (MDD) and chronic pain are highly comorbid, especially in female patients (Bair et al., Reference Bair, Robinson, Eckert, Stang, Croghan and Kroenke2004). This comorbidity significantly decreases the quality of life of patients and represents one of the largest socioeconomic burdens worldwide (Leuchter et al., Reference Leuchter, Husain, Cook, Trivedi, Wisniewski, Gilmer and Rush2010; Walker, Kavelaars, Heijnen, & Dantzer, Reference Walker, Kavelaars, Heijnen and Dantzer2014). Pain symptoms can either precede or follow the onset of MDD (Bair, Robinson, Katon, & Kroenke, Reference Bair, Robinson, Katon and Kroenke2003; Chang et al., Reference Chang, Hsu, Huang, Su, Bai, Li and Chen2015; Gerrits, Van Oppen, Van Marwijk, Penninx, & Van Der Horst, Reference Gerrits, Van Oppen, Van Marwijk, Penninx and Van Der Horst2014), suggesting a bidirectional relationship between MDD and chronic pain. Several studies have suggested that affective disorders and chronic pain have an overlapping pathophysiology and may share similar circuit mechanisms (Bair et al., Reference Bair, Robinson, Katon and Kroenke2003; Taylor, Becker, Schweinhardt, & Cahill, Reference Taylor, Becker, Schweinhardt and Cahill2016). While both depression and pain symptoms can be alleviated by antidepressant medications (Gracely, Ceko, & Bushnell, Reference Gracely, Ceko and Bushnell2012; Maletic & Raison, Reference Maletic and Raison2009), this comorbidity has generally been associated with greater resistance to pharmacological treatment (Bair et al., Reference Bair, Robinson, Eckert, Stang, Croghan and Kroenke2004, Reference Bair, Robinson, Katon and Kroenke2003; Gerrits et al., Reference Gerrits, Vogelzangs, Van Oppen, Van Marwijk, Van Der Horst and Penninx2012; Leuchter et al., Reference Leuchter, Husain, Cook, Trivedi, Wisniewski, Gilmer and Rush2010; Von Korff & Simon, Reference Von Korff and Simon1996). In particular, pain severity has been reported to be a strong predictor of poorer antidepressant medication treatment outcome and health-related quality of life (Bair et al., Reference Bair, Robinson, Eckert, Stang, Croghan and Kroenke2004). Better recognition, assessment, and treatment of comorbid pain may thus enhance the outcome of antidepressant therapy.
Repetitive transcranial magnetic stimulation (rTMS) administered to the left dorsolateral prefrontal cortex (DLPFC) is an effective treatment for pharmaco-resistant depression (George et al., Reference George, Lisanby, Avery, McDonald, Durkalski, Pavlicova and Sackeim2010; Janicak et al., Reference Janicak, Dunner, Aaronson, Carpenter, Boyadjis, Brock and Demitrack2013). While the mechanism of action (MOA) of this neuromodulation technique is not yet fully understood, there is evidence to suggest that the therapeutic effect of rTMS arises through the resetting of resting-state functional networks beyond the stimulation site (Corlier et al., Reference Corlier, Carpenter, Wilson, Tirrell, Gobin, Kavanaugh and Leuchter2019a, Reference Corlier, Wilson, Hunter, Vince-Cruz, Krantz, Levitt and Leuchterb; Fox, Halko, Eldaief, & Pascual-Leone, Reference Fox, Halko, Eldaief and Pascual-Leone2012; Leuchter, Hunter, Krantz, & Cook, Reference Leuchter, Hunter, Krantz and Cook2015; To, De Ridder, Hart, & Vanneste, Reference To, De Ridder, Hart and Vanneste2018). rTMS also appears to be efficacious for the treatment of other neuropsychiatric disorders including post-traumatic stress disorder, obsessive-compulsive disorder (Tadayonnejad et al., Reference Tadayonnejad, Wilson, Corlier, Lee, Ginder, Levitt and Leuchter2020), generalized anxiety disorder, bipolar depression, tinnitus, neurodegenerative disorders (Carpenter et al., Reference Carpenter, Conelea, Tyrka, Welch, Greenberg, Price and Philip2018; Heath, Taylor, & McNerney, Reference Heath, Taylor and McNerney2018; Lefaucheur et al., Reference Lefaucheur, André-Obadia, Antal, Ayache, Baeken, Benninger and Garcia-Larrea2014, Reference Lefaucheur, Aleman, Baeken, Benninger, Brunelin, Di Lazzaro and Ziemann2020; Soleimani, Jalali, & Hasandokht, Reference Soleimani, Jalali and Hasandokht2016), and pain syndromes such as neuropathic pain, headache, fibromyalgia, and complex regional pain syndrome (Altas, Askin, Beşiroğlu, & Tosun, Reference Altas, Askin, Beşiroğlu and Tosun2019; Galhardoni et al., Reference Galhardoni, Correia, Araujo, Yeng, Fernandes, Kaziyama and de Andrade2015; Goudra et al., Reference Goudra, Shah, Balu, Gouda, Balu, Borle and Singh2017; Hou, Wang, & Kang, Reference Hou, Wang and Kang2016; Hsu, Daskalakis, & Blumberger, Reference Hsu, Daskalakis and Blumberger2018; Knijnik et al., Reference Knijnik, Dussán-Sarria, Rozisky, Torres, Brunoni, Fregni and Caumo2016; Saltychev & Laimi, Reference Saltychev and Laimi2017; Short et al., Reference Short, Borckardt, Anderson, Frohman, Beam, Reeves and George2011). Most studies of rTMS on pain have targeted the primary motor cortex, but stimulation to left DLPFC has also successfully reduced pain symptoms even in non-MDD populations (Galhardoni et al., Reference Galhardoni, Correia, Araujo, Yeng, Fernandes, Kaziyama and de Andrade2015; Johnson, Summers, & Pridmore, Reference Johnson, Summers and Pridmore2006; Lefaucheur et al., Reference Lefaucheur, André-Obadia, Antal, Ayache, Baeken, Benninger and Garcia-Larrea2014; Short et al., Reference Short, Borckardt, Anderson, Frohman, Beam, Reeves and George2011). One previous report demonstrated significant improvement in both mood and pain symptoms solely with 10 Hz rTMS treatment applied to left DLPFC (Phillips, Burr, & Dunner, Reference Phillips, Burr and Dunner2018). However, it remains unclear whether this effect was gender-specific and whether the presence and severity of pain symptoms was associated with inferior rTMS clinical outcome, as is the case with pharmacological treatment.
Identifying neurophysiological biomarkers of chronic pain would aid in the development of an rTMS protocol targeting this comorbidity. Such measures would allow the assessment of target engagement and could serve as early predictors of treatment outcome. Alpha band oscillations have previously been identified as a robust electroencephalographic (EEG) marker of chronic pain and might represent a possible biomarker for rTMS. For example, higher alpha power has been observed within the dynamic pain connectome in subjects with neuropathic pain, rheumatoid arthritis, and jaw pain (Kim & Davis, Reference Kim and Davis2020; Kisler et al., Reference Kisler, Kim, Hemington, Rogachov, Cheng, Bosma and Davis2020; Meneses et al., Reference Meneses, Queirós, Montoya, Miranda, Dubois-Mendes, Sá and Baptista2016; Wang et al., Reference Wang, Roy, Misra, Ho, Ribeiro-Dasilva, Fillingim and Coombes2019), while decreased alpha oscillations have been reported in tonic pain (cf. Ploner, Sorg, & Gross, Reference Ploner, Sorg and Gross2017). Lower peak alpha frequency [PAF, also called individual alpha frequency (IAF)] (Grandy et al., Reference Grandy, Werkle-Bergner, Chicherio, Schmiedek, Lövdén and Lindenberger2013; Petrosino, Zandvakili, Carpenter, & Philip, Reference Petrosino, Zandvakili, Carpenter and Philip2018) also has been observed in neuropathic pain and fibromyalgia (Kim et al., Reference Kim, Bosma, Hemington, Rogachov, Osborne, Cheng and Davis2019). Sensorimotor PAF has been reported as a reliable biomarker of subjective pain intensity and pain sensitivity, with slower PAF possibly reflecting pre-disease pain sensitivity (Babiloni et al., Reference Babiloni, Brancucci, Del Percio, Capotosto, Arendt-Nielsen, Chen and Rossini2006; Furman et al., Reference Furman, Meeker, Rietschel, Yoo, Muthulingam, Prokhorenko and Seminowicz2018, Reference Furman, Thapa, Summers, Cavaleri, Fogarty, Steiner and Seminowicz2019, Reference Furman, Prokhorenko, Keaser, Zhang, Chen, Mazaheri and Seminowicz2020) or marking a ‘chronification’ process of pain (de Vries et al., Reference de Vries, Wilder-Smith, Jongsma, van den Broeke, Arns, van Goor and van Rijn2013). Targeted modulation of alpha activity through visual stimulation, as well as transcranial alternating or direct current stimulation, also has been associated with chronic pain relief (Ahn, Prim, Alexander, McCulloch, & Fröhlich, Reference Ahn, Prim, Alexander, McCulloch and Fröhlich2019; Arendsen, Hugh-Jones, & Lloyd, Reference Arendsen, Hugh-Jones and Lloyd2018; Lopez-Diaz et al., Reference Lopez-Diaz, Henshaw, Casson, Brown, Taylor, Trujillo-Barreto and Sivan2021). Recent evidence indicates that alpha synchrony between relevant networks enables feedforward/feedback processing and flexible routing of information in the integration of sensory and contextual processes (Kim & Davis, Reference Kim and Davis2020; Kisler et al., Reference Kisler, Kim, Hemington, Rogachov, Cheng, Bosma and Davis2020; Ploner et al., Reference Ploner, Sorg and Gross2017). The examination of PAF/IAF and synchrony in the nociceptive network may therefore serve as an effective biomarker of target engagement and clinical response for rTMS treatment of chronic pain and depression.
Given the prevalence of comorbid chronic pain and MDD, and in light of their overlapping pathophysiology, it is of crucial importance to elucidate novel targets and integrated interventions to treat comorbid pain and depression, rather than targeting pain and depressive symptoms separately (Walker et al., Reference Walker, Kavelaars, Heijnen and Dantzer2014). The primary objectives of this study were thus to: (1) evaluate the effect of pain comorbidity on rTMS treatment response for MDD; (2) examine gender differences in rTMS treatment outcome; and (3) examine IAF and alpha band network synchrony as potential biomarkers for rTMS treatment outcome for comorbid MDD and chronic pain.
Methods
Subjects
Subjects were 162 outpatients with a primary diagnosis of MDD (Mini International Diagnostic Interview, MINI) (Sheehan et al., Reference Sheehan, Lecrubier, Sheehan, Amorim, Janavs, Weiller and Dunbar1998) referred for treatment in the TMS Clinical and Research Service at UCLA. The research protocol was approved by the UCLA IRB and all subjects provided informed consent prior to research procedures. Subjects presented with at least moderately severe depressive symptoms based upon a 17-item Hamilton Depression Rating Scale Score (HAM-D17, minimal score >17) (Hamilton, Reference Hamilton1960) and had failed to enter remission after at least three adequate antidepressant trials. Subjects were allowed to continue receiving psychotropic medication concurrent with rTMS and underwent standard safety screening and medical clearance before receiving rTMS treatment. The entire sample of 162 MDD subjects who completed a 30-session rTMS course for depression was categorized into subgroups as follows: Group (1) 105/162 who reported pretreatment comorbid pain; Group (2) 57/162 with no comorbid pain; Group (1A) 46/105 comorbid subjects with a spontaneous EEG recorded prior to the first session; Group (1B) 59/105 without EEG; Group (2A) 51/57 pain-free subjects with a baseline EEG recording; Group (2B) 6/57 pain-free subjects without EEG (see also Fig. 1). All procedures in this work comply with the ethical standards of the relevant national and institutional committees on human experimentation and with the Helsinki Declaration of 1975 as revised in 2008.
Clinical assessment
Depressive symptoms were assessed at baseline and session 30 with the 30-item Inventory of Depressive Symptomatology Self Report version (IDS-SR) (Trivedi et al., Reference Trivedi, Rush, Ibrahim, Carmody, Biggs, Suppes and Kashner2004). The reliability of IDS-SR is demonstrated by its use as the primary outcome in STAR*D, the largest open-label, pragmatic trial for MDD (Sinyor, Schaffer, & Levitt, Reference Sinyor, Schaffer and Levitt2010). Chronic pain was assessed at baseline and treatment 30 using the eight-question Visual Analog Scale (VAS) for pain with total scores ranging from 0 to 800 (Chiarotto et al., Reference Chiarotto, Maxwell, Ostelo, Boers, Tugwell and Terwee2019). Each question ranges [0–100] and assesses, during the last week, overall pain, along with separate items for headache, back, shoulder, stomach, and abdominal pain, interference with daily function, and nighttime awakenings due to pain. The VAS has been widely used in adult patients with various chronic pain conditions (Mori et al., Reference Mori, Codecà, Kusayanagi, Monteleone, Buttari, Fiore and Centonze2010; Onesti et al., Reference Onesti, Gabriele, Cambieri, Ceccanti, Raccah, Di Stefano and Inghilleri2013) and has been established as a reliable measure in a review of over 850 studies (Karcioglu, Topacoglu, Dikme, & Dikme, Reference Karcioglu, Topacoglu, Dikme and Dikme2018). Patients with different pain types were included in this sample, including fibromyalgia-like symptoms, neuropathic pain, chronic lower back pain, and complex regional pain syndrome, and the specific source of chronic pain for each individual was not formally diagnosed in the context of this study. We therefore were not able to perform separate analyses for each pain type.
EEG acquisition
Ninety-seven of 162 subjects had an EEG recording performed at baseline using the ANT Neuro TMS-compatible EEG system and EEGO v1.8 recording software (Advanced Neuro Technology (ANT); Enschede, the Netherlands). Electrodes were applied using the 64-electrode ‘WaveGuard’ cap with sintered Ag/AgCl electrodes positioned according to the Extended 10–20 System with EOG electrodes above and below the left eye. Data were recorded at a sampling rate of 2000 Hz using full-band EEG DC amplifiers without filters during data acquisition using a CPz electrode reference; data were converted to a common average reference offline for analysis. Impedances were kept below 10 kΩ. All subjects had at least 5 min of baseline resting-state EEG recording.
rTMS procedures
All TMS treatments were performed with either the Magstim Rapid 2 stimulator using a 70 mm coil (Magstim, Whitland, South Wales, UK), the Neuronetics Neurostar treatment system (Neuronetics, Malvern, PA, USA), or MagVenture (Alpharetta, GA, USA). Motor threshold (MT) determination was performed prior to the first treatment, with MT defined as the minimum stimulus intensity necessary to elicit an overt motor response in the right abductor pollicis brevis or first dorsal interosseus muscles for ⩾50% of applied stimuli. Following MT determination, treatments were performed with patients seated in a semi-reclined position using standard safety procedures and ear protection. All patients underwent treatment initially with 10 Hz stimulation to left DLPFC defined using the Beam F3 method (Beam, Borckardt, Reeves, & George, Reference Beam, Borckardt, Reeves and George2009), with a 40-pulse train and 26 s intertrain interval with a total of 3000 pulses per session (37.5 min duration). Clinicians adjusted stimulation intensity, coil angle, and number of pulses administered as needed to optimize tolerability. Treatment intensity was titrated to 120% MT as tolerated with parameters modified according to a measurement-based care paradigm. Participants completed IDS-SR ratings every five treatments. If there was an absence of early clinical response to rTMS or worsening in anxiety or depressive symptoms, the treatment protocol could be complemented by intermittent theta-burst stimulation priming (iTBS) at left DLPFC (Lee et al., Reference Lee, Wilson, Corlier, Tadayonnejad, Marder, Pleman and Leuchter2020) or by 1 Hz rTMS at the right DLPFC after the fifth session to optimize tolerability or augment clinical response (sequential bilateral treatment). In the total group of 162 subjects, 137 (84.5%) received modified treatment parameters and the use of these parameters was included as a categorical covariate in the analysis of variance.
Data analysis
We performed a t test comparing pre- to post-rTMS IDS-SR scores of the entire sample to assess the therapeutic efficacy of rTMS treatment. To characterize pain comorbidity in the current sample, we calculated proportions of MDD patients with no, moderate, or severe pain using the VAS scale for pain based on the observed trimodal distribution of the pain scores (Fig. 2a). Following the trimodal distribution of these data, we grouped subjects into (1) no pain or no significant chronic pain (termed ‘no pain’ or ‘pain-free’ subjects), (2) moderate pain, or (3) severe pain. The cutoffs were as follows: no pain: VAS = [0–200]; moderate pain: VAS = [201–450]; and severe pain: VAS = [451–800]. The proportions of subjects in each category were calculated.
We then calculated Pearson's correlation coefficients to evaluate the link (1) between baseline depression and pain severity, (2) between final outcome in depressive and pain symptoms, as well as (3) between baseline pain and final depression outcomes. Because pain and somatic symptom ratings were included in the overall IDS score, we also recalculated the IDS after removing pain- and sleep-related items [1 to 4 (sleep-related) and 20, 25, 26, 30 (pain- and energy-related)], to test whether relationships between depression and pain were affected by the removal of pain and somatic items [this reduced measure referred to as IDS-SR(22)].
An analysis of variance (ANOVA) was conducted to examine the effect of rTMS treatment (factor Treatment #) on pain including the five following covariates: age, gender, TMS device (1–3), use of modified rTMS protocol (yes/no), concomitant use of psychotropic medication during rTMS treatment (yes/no). Additionally, we compared response and remission rates for depression among groups of varying pain levels with response defined as a ⩾50% decrease in IDS-SR score from baseline and remission was defined as an IDS-SR score of ⩽13. Clinical rTMS response and remission rates across the three groups were compared using a Kruskal-Wallis test.
EEG analyses
EEGs (conducted on Groups 1A and 2A) were preprocessed using the semi-automated FASTER toolbox (Nolan, Whelan, & Reilly, Reference Nolan, Whelan and Reilly2010), an ICA-based algorithm to remove eye movement, muscular, and line noise artifacts, followed by visual inspection to manually remove remaining artifacts. Individual PAF was estimated using two complementary approaches: (1) a ‘center of gravity’ (COG) method previously used in pain research by Furman and colleagues (Seminowicz et al., Reference Seminowicz, Thapa, Furman, Summers, Cavaleri, Fogarty and Schabrun2018), and (2) the IAF method used in MDD research by Corlier et al. (Reference Corlier, Carpenter, Wilson, Tirrell, Gobin, Kavanaugh and Leuchter2019a, Reference Corlier, Wilson, Hunter, Vince-Cruz, Krantz, Levitt and Leuchterb). In both cases, the PAF was estimated based on the averaged power spectral density of postcentral channels Cz, C3, and C4 using a common average reference. We evaluated the relationship between IAF and pain severity by computing the Pearson's correlation coefficient between COG/IAF and the VAS baseline scores only for the patients with MDD and pain comorbidity (i.e. with a minimal VAS score >200).
We then performed phase-coherence analysis using channels-of-interest (ChOI) corresponding to the surface areas above motor, somatosensory, anterior and posterior cingulate cortices, as well as the precuneus. The 14 ChOI included: Fz, FCz, Cz, CPz, Pz, POz, FC1, FC2, FC3, FC4, C1, C2, C3, and C4 (ChOI are marked by blue spheres in Fig. 3c/d) with 91 total possible pairwise connections. Phase-coherence was calculated using the weighted phase lag index (wPLI), which has the advantage of yielding a reliable estimate even in noisy conditions. This metric weighs the observed phase leads and lags by the magnitude of the imaginary component of the cross-spectrum, is less sensitive to volume conduction, and provides greater statistical power to detect changes in phase-synchronization (Vinck, Oostenveld, Van Wingerden, Battaglia, & Pennartz, Reference Vinck, Oostenveld, Van Wingerden, Battaglia and Pennartz2011; Xing et al., Reference Xing, Ajilore, Wolfson, Abbott, Macnamara, Tadayonnejad and Leow2016a, Reference Xing, Tadayonnejad, Macnamara, Ajilore, Phan, Klumpp and Leow2016b). WPLI was estimated based on 4 s segments of artifact-free EEG data using the fieldtip toolbox function ‘ft_connectivityanalysis’. Baseline levels of wPLI were compared between comorbid responders/remitters and non-responders/non-remitters using t tests. Benjamini-Hochberg False Discovery Rate (FDR) method was used for the correction of multiple comparisons. We chose the top 25 connections with the largest Cohen's D effect sizes to compare the average network connectivity between responders/remitters and non-responders/non-remitters for the comorbid and the pain-free groups.
Results
In total, 35.2% of MDD subjects presented with no pain, 44.4% of subjects reported moderate pain, and 20.4% had severe pain symptoms, exhibiting a trimodal distribution of severity (Fig. 2a and b). Baseline and post-treatment depression scores were significantly higher in the comorbid than in the pain-free MDD individuals. There was no effect of age or gender on baseline pain severity (Table 1). On average, rTMS treatment significantly reduced depressive (two-tailed t test, T = 14.0, p < 0.0001) and pain symptoms (ANOVA, F = 3.8, p = 0.02), and posthoc t tests showed pain improvement by treatment 15 with further improvement seen at treatment 30 (T 15, p 15 = 0.0088, T 30, p 30 = 0.0067, Fig. 1c). There was no significant effect of gender (F = 2.4, p = 0.09, Fig. 1d), age (F = 0.1, p = 0.7), TMS device (F = 0.1, p = 0.9), use of psychotropic medication (F = 0.7, p = 0.4), or use of modified rTMS protocol (F = 2.7, p = 0.1) on outcome (Table 1).
There was no age or gender difference between groups. Both initial depression severity and final depression score were significantly higher in the pain group.
There was a significant positive correlation between the severity of pain and depression at baseline (r = 0.43, p = 1.56 × 10−08), between the final pain and depression outcome (r = 0.53, p = 9.59 × 10−11), and between baseline pain severity and final depression outcome (r = 0.36, p = 3.73 × 10−06). Response rates were significantly different across the three pain severity groups (χ2 = 8.5, p = 0.014), with 27% lower rTMS response probability among patients with more severe pain compared to the pain-free group (rTMS response rates of 39, 22, and 12% rates for no, moderate, and severe pain, respectively, Fig. 2c). Differences in remission rates among the three groups reached trend-level significance (χ2 = 5.26, p = 0.072, rTMS remission rates of 19, 11, and 3% for no, moderate, or severe pain, respectively). The significant association between pain and depression symptoms persisted even after removing eight pain, sleep, and energy-related items from the IDS-SR (r = 0.32, p = 0.008 at baseline and r = 0.35, p = 0.003 at endpoint).
EEG data in the comorbid patient subgroup revealed that a higher individual PAF was associated with more severe chronic pain complaints at baseline. This was confirmed for both COG and PAF measures (COG: r = 0.41, p = 0.00095; PAF: r = 0.39, p = 0.0047, Fig. 3a and b). Phase-coherence for the top 25 connections was significantly higher for comorbid responders/remitters than for non-responders/non-remitters at a level of p < 0.05 after FDR correction (Fig. 4b, Table 2). The average network connectivity across these 25 connections was also overall significantly different between responders/non-responders (t = 3.4, p = 0.001) and remitters/non-remitters (t = 3.1, p = 0.003; Fig. 4c and d, left panel). However, in the same network, there was no difference between pain-free responders/remitters and non-responders/non-remitters (t = 1.7, p = 0.1 and t = 1.3; p = 0.2, respectively; Fig. 4c and d, right panel).
All connections were significantly different between the groups at the level of p < 0.05, FDR-corrected.
Discussion
More than half of the MDD subjects in our sample presented with moderate to severe chronic pain symptoms, independent of age or gender, and the severity of depressive and pain symptoms were highly correlated. rTMS treatment was efficacious in reducing both comorbid symptoms although the presence of pain was associated with a worse antidepressant rTMS outcome. EEG analysis revealed that individual PAF was positively associated with chronic pain severity while baseline phase-coherence along the midline and sensorimotor regions was significantly lower among non-responders/non-remitters than in responders/remitters with comorbid pain.
Our finding that most MDD subjects report chronic pain symptoms that are associated with a poorer rTMS treatment outcome is consistent with the prior literature on medication treatment of MDD. The present findings confirm the high prevalence of this comorbidity and emphasize the need for a better understanding of the shared pathophysiology, as well as development of novel treatment strategies targeting both disorders (Bair et al., Reference Bair, Robinson, Eckert, Stang, Croghan and Kroenke2004). This study did not confirm previous reports of age- or gender-specific differences in pain prevalence and response (Phillips et al., Reference Phillips, Burr and Dunner2018). Women and men in this study were equally likely to report and improve in pain regardless of age, although there was a trend-level effect for gender with females responding at a smaller degree. Failure to separate pain intensity and pain unpleasantness may underlie this discrepancy; future studies should attempt to more clearly distinguish these elements of pain.
Baseline depressive and pain symptoms were positively correlated, and better depression outcomes correlated with greater pain improvement, even after removing the somatic symptoms from the IDS-SR. It is thus difficult to dissociate the pain response from the antidepressant effect of the rTMS treatment. Further studies are necessary to characterize the interaction of separate or common brain circuits that may be involved. These data suggest, however, that rTMS to left DLPFC may be a less effective treatment for depressed patients with comorbid pain than those without pain. This finding is consistent with prior studies that have reported a poorer outcome for MDD-pain comorbid patients when treated with medications (Bair et al., Reference Bair, Robinson, Katon and Kroenke2003; Gerrits et al., Reference Gerrits, Vogelzangs, Van Oppen, Van Marwijk, Van Der Horst and Penninx2012; Leuchter et al., Reference Leuchter, Husain, Cook, Trivedi, Wisniewski, Gilmer and Rush2010). It is also in line with previous findings showing that higher baseline depression severity is associated with poorer clinical response to rTMS (Fitzgerald, Hoy, Anderson, & Daskalakis, Reference Fitzgerald, Hoy, Anderson and Daskalakis2016; Janicak et al., Reference Janicak, Dunner, Aaronson, Carpenter, Boyadjis, Brock and Demitrack2013; Krepel, Rush, Iseger, Sack, & Arns, Reference Krepel, Rush, Iseger, Sack and Arns2019). We hypothesize, however, that the distinct MOA of rTMS may be better suited to target the shared neurophysiological pathways of depression and comorbid pain than antidepressant medication.
The present results confirm that rTMS administered to left DLPFC does ameliorate comorbid pain symptoms in MDD. Combined with the broad prior treatment literature, however, these findings suggest that a multi-target rTMS approach for the combined treatment of MDD and chronic pain may therefore represent a promising alternative therapeutic approach. Future studies should systematically evaluate possible secondary targets for rTMS treatment of pain, such as the primary motor cortex, ventromedial prefrontal cortex, or the anterior cingulate cortex, which all have been linked to pain processing or pain relief after rTMS. Given that difficult-to-treat MDD patients with chronic pain are more likely to be administered opioids for pain relief, a novel rTMS therapeutic approach may help reduce opioid prescriptions and drug dependency for these challenging comorbid patients (Cahill & Taylor, Reference Cahill and Taylor2017; Sullivan, Edlund, Steffick, & Unützer, Reference Sullivan, Edlund, Steffick and Unützer2005).
These results also extend previous findings of an association between individual PAF and pain susceptibility to acute and prolonged experimentally induced pain (Furman et al., Reference Furman, Meeker, Rietschel, Yoo, Muthulingam, Prokhorenko and Seminowicz2018; Seminowicz et al., Reference Seminowicz, Thapa, Furman, Summers, Cavaleri, Fogarty and Schabrun2018) and in chronic pain conditions (Babiloni et al., Reference Babiloni, Brancucci, Del Percio, Capotosto, Arendt-Nielsen, Chen and Rossini2006; de Vries et al., Reference de Vries, Wilder-Smith, Jongsma, van den Broeke, Arns, van Goor and van Rijn2013; Furman et al., Reference Furman, Thapa, Summers, Cavaleri, Fogarty, Steiner and Seminowicz2019, Reference Furman, Prokhorenko, Keaser, Zhang, Chen, Mazaheri and Seminowicz2020). Individual PAF represents a stable individual trait (Grandy et al., Reference Grandy, Werkle-Bergner, Chicherio, Schmiedek, Lövdén and Lindenberger2013; Petrosino et al., Reference Petrosino, Zandvakili, Carpenter and Philip2018) that multiple studies have shown to be associated with rTMS treatment outcome in MDD (Arns, Drinkenburg, Fitzgerald, & Kenemans, Reference Arns, Drinkenburg, Fitzgerald and Kenemans2012; Corlier et al., Reference Corlier, Carpenter, Wilson, Tirrell, Gobin, Kavanaugh and Leuchter2019a, Reference Corlier, Wilson, Hunter, Vince-Cruz, Krantz, Levitt and Leuchterb). While our observation stands in contrast to previously reported alpha-band slowing in multiple sclerosis subjects with neuropathic pain (Kim et al., Reference Kim, Bosma, Hemington, Rogachov, Osborne, Cheng and Davis2019), this discrepancy may be due to the different anatomical location of measured alpha rhythms, the specific type of pain, or the presence of MDD comorbidity. It is possible that MDD patients with higher PAF might have higher acute pain sensitivity prior to developing chronic pain, and that these patients may have a different intrinsic structure or function of brain circuits that conveys a higher likelihood of developing comorbid chronic pain. The present results suggest the possibility of neural circuitry common to both chronic pain and depression, and that certain neurophysiological features may define a biotype of depression that is both more susceptible to developing comorbid pain and more responsive to rTMS treatment.
These findings also suggest that EEG biomarkers may help guide the search for an alternative rTMS approach for the treatment of MDD and pain comorbidity. We have identified a network including midline and sensorimotor regions that displays lower baseline phase-coherence for rTMS non-responders/non-remitters compared to responders/remitters among all patients with MDD and chronic pain comorbidity. This observation is consistent with the idea of network reorganization with chronic pain (Farmer, Baliki, & Apkarian, Reference Farmer, Baliki and Apkarian2012). The topography of network should be further examined for its possible alignment with the dynamic pain connectome including the default mode network and/or salience network in chronic pain using source localization (Alshelh et al., Reference Alshelh, Marciszewski, Akhter, Di Pietro, Mills, Vickers and Henderson2018; Kucyi & Davis, Reference Kucyi and Davis2017; Van Ettinger-Veenstra et al., Reference Van Ettinger-Veenstra, Lundberg, Alföldi, Södermark, Graven-Nielsen, Sjörs and Gerdle2019). Future studies also should examine whether the PAF or phase-coherence metrics in comorbid patients normalize with successful rTMS treatment.
Two testable hypotheses for future studies are that: (a) a multi-target rTMS approach combining the established left DLPFC target for depression with a secondary pain target within the sensorimotor-midline network will enhance antidepressant response to rTMS, and (b) successful rTMS treatment for comorbid MDD and pain would re-establish non-comorbid levels of PAF and sensorimotor-midline functional connectivity. While the EEG findings among different pain types are beyond the scope of the present data, differences in PAF and network synchrony may be specific to certain chronic pain conditions and such possible differences should be systematically examined in future studies.
Limitations
The reported findings should be interpreted in the context of several limitations. First, these subjects were treated in a naturalistic setting with all individuals continuing their psychotropic medication during the rTMS course. Additionally, while all patients started with 10 Hz left DLPFC treatment, their stimulation protocol could be adjusted during the 30-session course according to a measurement-based care paradigm. While we did not detect a significant effect of medication or TMS parameters on outcome, it is possible that there may have been an interaction among types of concurrent medications and the rTMS effect on pain symptoms. Future trials should explicitly control for or exclude confounding medications. Second, we evaluated the severity of pain regardless of the specific etiology. Patients with fibromyalgia, neuropathic pain, chronic lower back pain, and complex regional pain syndrome were combined in this sample, despite their possibly different pathophysiological mechanisms. While rTMS has been previously shown to successfully improve various pain types, it remains unclear if the presence or direction of the association between pain symptoms and PAF or phase-coherence is clinically meaningful across different pain conditions. Follow-up research should systematically compare the effect of rTMS on different pain types.
Conclusions
We present preliminary evidence that MDD comorbidity with chronic pain results in lower rTMS response/remission rates for depression and propose that increased PAF and hypoconnectivity between sensorimotor and midline regions may predict this worse rTMS therapeutic prognosis in the comorbid population. Understanding the underlying circuitry and developing a more targeted treatment approach may help further develop a therapy for this common comorbidity. A multi-target rTMS approach represents a promising avenue for non-pharmacological treatment for comorbid MDD and chronic pain.
Acknowledgements
The authors would like to acknowledge the patients and their families who received treatment in the clinic during the study period, and the dedication of the technicians and administrative team that have made this work possible. This project was made possible by the Ryan Family Fund for TMS Research. We thank the Ryan Family for their generous support of innovative approaches to depression treatment and of groundbreaking TMS technology. Dr Corlier was supported by the Neuromodulation Postdoctoral Scholar Fund, which was established by the generous gifts of Janet and Barry Lang, Sally and David Weil, and in memory of Morris A. Hazan. Their contributions have advanced the university's education and research missions through the support of a postdoctoral scholar in the Neuromodulation Division.
Financial support
This research did not receive any specific grant from funding agencies in the public, commercial, or not-for-profit sectors.
Conflict of interest
Drs Corlier, Tadayonnejad, Marder, Ginder, Wilke, Levitt, and Krantz have no disclosures. Wilson has served as a consultant to HeartCloud, Inc. within the past 36 months. Dr Lee has received equipment in-kind support from Magventure Inc. Dr Leuchter discloses that within the past 36 months he has received research support from the National Institutes of Health, Department of Defense, CHDI Foundation, and NeuroSigma, Inc. He has served as a consultant to NeoSync, Inc., Ionis Pharmaceuticals, Inc., and ElMindA. He is Chief Scientific Officer of Brain Biomarker Analytics LLC (BBA). Dr Leuchter has an equity interest in BBA.