A prospective longitudinal experimental study will be conducted to follow healthy individuals from the first induction of pain (day 0), as it develops and is sustained (day +2 and day +4), until 5 days after complete resolution of pain (Figure 1). Ethical approval has been obtained from the University of Western Ontario (reference 2025-125757-103291, January 9, 2025).

A total of 150 healthy, pain-free individuals aged 18-65 years will be included in the study. Each participant will be asked to refrain from consumption of tobacco [23], caffeine [24], and recreational substances at least 2 hours before data collection [25], and short-acting analgesics (eg, acetaminophen) at least 6 hours before data collection [26], so as not to interfere with the perception of pain. Individuals presenting with a history of other major disorders, psychiatric conditions, or contraindications to the use of transcranial magnetic stimulation (TMS) will be excluded. Only right-handed people will be included due to the device used to analyze motor variability, which is custom built for right-handed individuals, and the presence of differences in sensorimotor integration [27] that would influence consistency and increase variability. Participants will be recruited from the community using newspaper or online advertisements and social media sites such as Facebook. Testing will take place at the Western Interdisciplinary Research Building on the University of Western Ontario campus at London (Ontario, Canada). Participants shall receive financial compensation for their participation.

SEPs will be recorded following electrical stimulation of the radial nerve. The cathode (black negative electrode) will be positioned 1.5 cm radial to the dorsal tubercle of the radius, targeting the superficial branch of the radial nerve [66]. The anode (red positive electrode) will be placed over the tendinous area in the distal third of the forearm. Electrodes will be spaced 3 cm apart. The forearm will be supinated with slight wrist extension [67]. Two blocks of 500 stimuli of 1-ms square pulse duration at a frequency of 2 Hz will be delivered, and a randomized interstimulus interval of 20% (0.4‐0.6 seconds) will be programmed to reduce habituation. The perceptual threshold will be determined by starting with a low-intensity stimulus and gradually increasing it until the participant reports a sensation. The stimulation intensity for the experiment will be set just below pain threshold without creating muscle twitches. Two blocks of 500 stimuli will be delivered while ensuring that the participant remains relaxed and minimizes movement to reduce artifacts.

The same EEG setup and preparation will be used as for the PAF. Data from the 2 blocks of 500 stimuli will be analyzed to examine the N₂₀-P₂₅-N₃₃ complex as a marker of early cortical processing of somatosensory input. Data will be processed using MATLAB, resampled to 500 Hz, and auxiliary physiological channels will be excluded. EEG will be rereferenced to the right mastoid electrodes (M2). Band-pass filtering will be applied from 0.5 to 40 Hz (zero-phase finite impulse response), followed by a 59‐61 Hz notch filter. Data will be epoched from −50‐+150-milliseconds around each stimulus onset and baseline-corrected using the prestimulus interval (−50‐0 ms). Artifact rejection will be proceeded in 2 stages: automated z-value thresholding (cutoff = 4, FieldTrip ft_artifact_zvalue), followed by optional interactive summary rejection (ft_rejectvisual). All rejected trials will be logged with their rejection stage.

SEP will be extracted at electrode C3, contralateral to the stimulated right wrist, as it overlies the primary somatosensory cortex generating the early cortical response [68]. The area for the N₂₀–P₂₅–N₃₃ complex within a window of 18‐40 ms will be computed per trial [22].

It is hypothesized that motor behavior in response to pain is influenced by individual cognitive coping strategies toward threat. People typically adopt either a passive coping strategy, focusing on pain and avoiding movement, or an active coping strategy, focusing on task completion and problem-solving. Previous work has shown that during a cognitive task performed in pain, individuals naturally adopt one of these strategies, which impacts performance [69-73]. Passive coping is associated with worsening performance, while active coping improves it [71]. This project will be the first to explore how these cognitive strategies relate to motor behavior in pain.

MSIT is a cognitive task designed to probe conflict resolution and cognitive control by activating the anterior cingulate cortex and frontoparietal networks [74]. MSIT combined with EEG allows investigation of how cognitive load influences pain perception and how pain affects cognitive performance. The MSIT will be modified from the original version of the MSIT [75], will be run using PsychoPy (version 2025.2.1; Open Science Tools Ltd), and will include 2 levels of difficulty: “low load” and “high load” [76]. In both levels, participants will identify the number on the screen that differs from the other 2 characters. They will use their right index, middle, and ring fingers to press the corresponding buttons, labeled “1,” “2,” and “3” arranged from left to right on a separated 3-keys keyboard. The MSIT introduces cognitive conflict by manipulating spatial and size-related features. For the easy level, 2 of the 3 characters are identical, and the position of the target number aligns with its corresponding button on the response box (eg, “323” with the correct answer being “2”). For the difficult level, spatial and size conflicts are introduced, meaning the target number does not align spatially with its button (eg, “311” with the correct answer being “3”). Each stimulus will remain on the screen until the participant presses a button, after which there will be a 1.25-second delay before the next stimulus appears [77]. To minimize cognitive fatigue, the task will be divided into 4 blocks per difficulty level (4 low load +4 high load), with 30-second rest periods between blocks. The participant will first be offered a training session consisting of an easy block and then a difficult block (repeatable if the participant wishes), followed by 8 blocks of 24 random trials in the fixed order load low-high-low-high-low-high-low-high, each separated by 30-second rests. For visits on day +2 and day +4, a tight armband will be applied over the site of injection to generate pain approximately 3/10 if the pain is less than this value at rest. We will examine behavioral performance for the 2 levels of difficulty, focusing on accuracy, defined as the proportion of correct, and reaction time, defined as the elapsed time between stimulus onset and the participant’s motor response.

Central sensitization, defined as an increased sensitivity of spinal and cortical neurons, and impaired descending pain modulation are key mechanisms influencing motor behavior in pain. These changes may interfere with the link between pain experience and motor behavior, as movement recovery may not reflect tissue healing [78]. Central sensitization can sustain pain beyond peripheral injury and interfere with the analgesic effects of movement. Moreover, it may compete with motor learning processes, potentially impairing motor adaptation [79]. While animal and human studies suggest a relationship between central sensitization and altered motor behavior, evidence remains limited [80-84].

CPM will be used to assess the inhibitory pain mechanisms, using 2 different types of test stimuli according to guidelines [85-87]. In our study, this assessment will involve measuring changes in both heat pain thresholds (HPTs) and pressure pain thresholds (PPTs) through 3 consecutive measurements, conducted twice and separated by a conditioned stimulus to activate endogenous pain modulation mechanisms [88].

The HPTs will be determined using a thermode (TCS-II, QST.Lab) equipped with a 4.5 cm² rectangular probe (T09). First, participants will undergo a familiarization phase with the thermode: holding the thermode in the palm of their hand and experiencing the temperature rise. Starting from a baseline temperature of 32 °C, thermal stimuli will be applied on the proximal third of the anterior surface of the right forearm of the participants with a gradual increase of 1 °C per second until the participant reports the first sensation of pain by pressing a response button. The temperature at this moment will be recorded as the HPTs. To ensure reliability, 3 consecutive measurements will be performed, and the mean value will be calculated and will be used for analysis. After each trial, the temperature will return to baseline in less than 1 second. Safety cutoff temperatures will be set at 50 °C to prevent tissue damage.

The PPTs will be assessed using a pressure algometer (Mxmoonfree ZMF-300N Portable Digital) equipped with a flat metallic round tip of 1.4 cm in diameter by exerting a constant pressure of 50 kPa per second (approximately 0.5 kg/cm² s). During the assessment, the participants’ forearm will be placed on a table while an examiner will exert pressure perpendicular to the skin. Participants will be asked to say “stop” to signal when the sensation changes from pressure to pain. When the participant responded “stop,” the pressure will stop, the device will be removed from the skin, and the pressure value recorded. Three recordings will be made and averaged (1-minute intervals) over the right ECRB (on injection site) and used for analysis.

Both HPTs and PPTs will be assessed before and directly after a conditioning cold pressor test (CPT) in balanced order to allow us to measure several excitatory and inhibitory pain mechanisms. The CPT will be administered by immersing the participant’s left forearm in cold water at 10 °C with a water flow for 2 minutes [89].

The magnitude of CPM will be calculated by subtracting the average HPTs and PPTs measured after the CPT stimulus from those recorded before the CPT stimulus (pre-post). Therefore, a negative value will indicate pain inhibition (CPM response), while a positive value will suggest pain facilitation [90].

Repeated intramuscular injection of NGF induces progressive, persistent muscle pain that is mechanistically, functionally, and clinically relevant. Importantly, NGF induces a gradual onset of pain without tissue injury [91], mimicking key features of persistent musculoskeletal pain, including movement-evoked pain, spreading hyperalgesia, and functional limitation [92,93], which resolve spontaneously around 25 days after injections have ceased [39,94]. These characteristics make the NGF model a safe and clinically relevant approach to investigate the cortical mechanisms underlying pain-related motor behavior and its individual variability, as it replicates the time course, movement-evoked nature, and sensitization processes characteristic of persistent musculoskeletal pain.

After cleaning the skin with alcohol, a solution of recombinant human NGF (Active GMP Recombinant Human NGF Protein from Creative BioMart Inc) will be administered as a bolus injection of 5 μg, dissolved in 0.2 mL of sterile water, into the muscle belly of the right ECRB muscle at the end of visits on days 0 and day +2. The injection will be administered using a 1-mL syringe with a 27-gauge, 1-inch needle. The site of injection will be located 1 cm lateral to a point that is 5 cm distal to the lateral epicondyle, along a line connecting the lateral epicondyle to the midline of the wrist [39,95]. The participant’s upper limb will be supported on a table, with the elbow flexed to 90° and the forearm in pronation to ensure proper positioning and accessibility to the target area. A permanent marker will be used to circle the injection site to maintain consistent injection placement in the ECRB muscle throughout the visits. In order to ensure optimal effectiveness of the hyperalgesia, we will keep the NGF at a temperature of −80 °C until a few minutes before the injection [96].

All questionnaires will be computerized and sent via Qualtrics Survey Software (version XM; Qualtrics, LLC). Patient-Rated Tennis Elbow Evaluation (PRTEE) is a 15-item questionnaire designed to measure forearm pain and disability in patients with lateral epicondylitis, also known as tennis elbow [97-99]. It consists of 2 subscales: a 5-item pain subscale and a 10-item function subscale, with each item rated on a scale of 0-10. The pain subscale is scored out of 50, and the functional subscale is divided by 2 to bring it down to a score out of 50 for a total score out of 100. The PRTEE has demonstrated high test-retest reliability (intraclass correlation coefficient [ICC]=0.96), internal consistency (Cronbach α=0.96) [99], and shows good construct validity against other measures such as the Disabilities of the Arm, Shoulder and Hand (r=0.81) [100]. The PRTEE is considered a reliable and valid tool for assessing pain and functional disability in patients with lateral elbow tendinopathy.

Tampa Scale for Kinesiophobia (TSK) is a widely used self-report questionnaire using a 4-point Likert scale, designed to assess fear of movement [101]. The objective of the TSK is to quantify kinesiophobia, defined as an irrational and debilitating fear of physical movement resulting from a feeling of vulnerability to painful injury or reinjury [102]. The TSK has demonstrated good to excellent test-retest reliability (ICC=0.77-0.99) and good internal consistency (Cronbach α=0.68-0.91) across various versions [103,104]. We have selected the TSK-13 (13 items), which presents good construct validity and strong psychometric properties, for a reduced completion time [103,105]. Participants will be asked to rate their agreement with the item statements from “strongly disagree” to “strongly agree,” with total scores ranging from 13 to 52, where higher scores indicate greater kinesiophobia [106]. Because the questionnaire was initially designed for patients with musculoskeletal pain, the questionnaire’s instructions were adapted to align with our healthy participants, following the validated TSK-G version for the general population [107], as done in previous studies [108-110]. The revised instructions were as follows: “We are interested in the types of thoughts and feelings that you might have in response to pain. Please read each of the following statements and check the box that best represents your thoughts and feelings while experiencing muscle pain.”

Pain Beliefs Questionnaire (PBQ) is a self-report instrument designed to assess individuals’ beliefs about the causes and consequences of pain [111]. Initially developed as a 20-item questionnaire, it was later refined to a 12-item version comprising 2 subscales: the Organic Beliefs Scale (8 items) and the Psychological Beliefs Scale (4 items) [112]. The PBQ evaluates pain-related beliefs, particularly the perceived organic nature of pain and the role of psychological factors in pain perception. The questionnaire has demonstrated strong construct validity, with patients with chronic pain and healthy controls exhibiting significant differences in their endorsement of organic and psychological beliefs [111]. It also shows good internal consistency (Cronbach α=0.68-0.91) across different versions [113]. Respondents rate their agreement with each statement on a 6-point Likert scale from “always” to “never.” The PBQ has been effectively used in studies on chronic back pain and is applicable to both individuals experiencing pain and healthy controls [112]. Its ability to assess pain beliefs across diverse populations makes it a valuable tool for understanding pain perceptions and informing pain management strategies.

Coping Strategies Questionnaire–Revised (CSQ-R) is a 27-item self-report instrument designed to assess cognitive and behavioral strategies for coping with pain [114]. It evaluates 6 key domains: Distraction, Catastrophizing, Ignoring Pain Sensations, Distancing from Pain, Coping Self-Statements, and Praying. The CSQ-R demonstrates a robust factorial structure, high reliability, and strong validity across multiple studies. Its subscales show excellent internal consistency (Cronbach α=0.914-0.961) and good to excellent test-retest reliability (ICC=0.850-0.918). Construct validity is supported by significant correlations with measures of pain, disability, depression, and other coping inventories. Administered as a self-report measure, the CSQ-R requires respondents to rate the frequency of their use of each coping strategy on a Likert scale from 0 “never” to 6 “always.”

Likert Muscle Soreness Scale (LMSS) is a self-report tool designed to assess perceived muscle soreness, particularly in the context of delayed onset muscle soreness. Its primary objective is to quantify the severity of muscle soreness and its impact on functional tasks using a 7-point scale ranging from 0 (no pain) to 6 (severe pain limiting movement) [115]. It has demonstrated good construct validity, with significant correlations (r=0.65-0.941) to other pain measures, such as the visual analogue scale, and its reliability is sensitive to changes in soreness over time [116]. Administered as a self-report measure, participants rate their soreness based on predefined descriptors. The LMSS has been validated in various populations, including long-distance runners and soccer players, confirming its applicability across different athletic groups [115]. The LMSS will be tailored to best match the elbow pain we will induce with the NGF injection by adding the italicized words at the end of the instructions as follows: “Please tick the sentence below that best describes your level of muscle soreness over the past 12 hours related to the injection.” For the same reason, the last 4 items will be adapted for the elbow pain as follows: “A light muscle soreness when I move my elbow/wrist in a large amplitude or/and when I handle an object with force”, “A light muscle soreness, stiffness or weakness when I move my elbow/wrist or/and when I handle an object with finesse,” “A moderate muscle soreness, stiffness or weakness when I move my elbow/wrist or/and when I handle an object with finesse” and “A severe muscle soreness, stiffness or weakness that limits the ability to move my elbow/wrist or/and handle an object.”

McGill Pain Questionnaire–Short Form (MPQ-SF) is a widely used self-report instrument designed to assess the multidimensional nature of pain [117]. The MPQ-SF consists of 15 descriptors (11 sensory and 4 affective) each rated on a 0 “none” to 3 “severe” intensity scale. The MPQ-SF provides a concise yet comprehensive measure of both sensory and affective pain dimensions, making it suitable for clinical and research settings. The MPQ-SF has demonstrated strong psychometric properties across various chronic pain populations, with high internal consistency (Cronbach α=0.73-0.89) [118] and excellent test-retest reliability (ICC=0.96) [119]. Validity studies support its construct and concurrent validity, showing strong correlations with other pain measures and sensitivity to changes in pain intensity.

Body diagram in the McGill Pain Questionnaire is a widely used tool for assessing pain location and distribution. It provides a visual representation of a patient’s pain by allowing them to mark affected areas on anterior and posterior body schematics including 9 areas: trunk, head and neck, shoulder, arm, elbow, forearm, hand, thumb, and fingers. The test-retest for measuring pain distribution demonstrated a moderate to excellent reliability (ICC=0.58-0.94), but which shows a great variability of reliability to assess the localization of pain, according to the specific circumstances of the evaluation (κ=0.13-0.85) [120]. The administration of body diagrams is typically self-reported, with patients marking their pain on the diagram following standardized instructions.

The trial is conservatively powered based on the use of separate multiple regression models to determine which mechanistic variables predict motor outcome at each time point. This calculation is based on 20 mechanistic variables: sensorimotor cortex excitability × 4 (map, SEPs, SICI, and ICF), sensorimotor integration × 1 (PAF-EEG), pain modulation × 2 (HPTs and PPTs), cognitive response × 4 (MSIT-easy-hard × 2 conditions), and physical activity or cognitive response × 6 (MPQ-SF, TSK-13, CSQ-R, PRTEE, LMSS, and PBQ), plus 3 a priori selected interactions and demographic variables × 3 (age, sex, and gender). We require 150 participants to achieve a power of 80% with a 5% significance level to detect a medium effect size and allowing for 10% loss to follow-up (based on our prior studies). The significance level was adjusted for multiple testing using a Bonferroni correction with an assumed correlation between predictors of 0.1. Using an alternative approach of 5‐10 participants per parameter, a sample of 150 could accommodate 15-30 parameters.

The analysis will be performed using growth curve modeling (GCMs) with the R software (R Core Team; R Foundation for Statistical Computing) for the 2 main outcomes [121]. Advantages to the use of GCM to examine our aim are as follows: (1) GCM enables consideration of the time-varying nature of both outcome (motor behavior) and the mechanistic (central nervous system) variables in response to pain; (2) GCM allows mechanistic variables to be simultaneously adjusted, permitting estimation of the unique contribution of each mechanism to motor behavior, as well as interaction between mechanisms; and (3) GCM can use unevenly spaced measurements and all available data, even in the presence of missing data at random. Thus, we will investigate whether mechanistic variables (and the interaction between them) at each time point, and the change between time points, predict motor behavior. To address individual variation in motor behavior, the model will use a 2-level nested structure. Level 1 will be the within-participant model and level 2 the between-participants model. The within-participant component allows each participant to have a unique motor behavior via random effects, and the between-participants component represents variation in motor behavior between individuals with similar mechanistic characteristics. The issue of controlling many covariates in statistical modeling will be addressed using modern adjustment techniques (eg, shrinkage estimation or exposure modeling) [122]. In addition, bootstrapping will be used to identify variables to be included in the final model [123]. Two models will be developed, 1 for kinematic movement variability and 1 for muscle synergies.

All procedures will be conducted in accordance with the Declaration of Helsinki. Written informed consent will be obtained, and participants will be free to withdraw from the study at any time. Patient data will be stored in a secure and structured database requiring access authorization via key card. The study data from the questionnaires will be collected via Qualtrics, a secure, web-based software platform designed to facilitate data collection and management for research purposes. Data are available from the corresponding author after agreement of the ethics committee. All procedures will be conducted under continuous supervision by trained personnel, with safety monitoring implemented throughout NGF-induced pain and neurophysiological testing. Participants will undergo comprehensive screening prior to inclusion, including TMS-specific safety questionnaires and exclusion of individuals with contraindications (eg, neurological, psychiatric, or implanted electronic or metal devices). During experimental sessions, participants will be closely monitored for adverse events (eg, excessive pain, dizziness, anxiety, and skin irritation), and all procedures (TMS, EMG, EEG stimulation, pressure, and thermal testing) can be immediately paused or terminated upon request. NGF injections (GMP grade), which have been documented as safe in humans [124-126], will be administered using sterile techniques, and expected transient muscle soreness will be monitored during visits; participants will be instructed to report any unexpected or prolonged symptoms. Standardized adverse event reporting procedures will be followed, including documentation, clinical assessment, and, if necessary, referral for medical evaluation.

All study procedures have been approved by the Western University Health Science Research Ethics Board (review reference 2025-125757-103291). Funding was provided by the Canadian Institutes of Health Research under grant number 517,783 for the period 2024‐2029. Recruitment for the study began in April 2025, and all data collection is expected to be completed by 2028. As of April 2026, we have enrolled 26 participants. To date, 4 participants have been excluded: 1 due to a lack of pain, 1 due to a poor-quality EEG signal, and 2 due to the impossibility of obtaining TMS hot spot. Results are expected to be published at the end of 2028. Data will be made available on request. The results will be disseminated through peer-reviewed publications and presentations at national and international conferences.

Participants who do not develop NGF-induced pain (PRTEE=0 on days +2 and +4) will be excluded. Data quality criteria will be applied across modalities, including successful elicitation of MEPs for ≥90% of TMS pulses and ≥90% marker tracking for motion capture. EEG analyses will be restricted to high-quality, artifact-free data: segments contaminated by eye movements, muscle activity, or excessive amplitudes (±75‐100 µV) will be rejected using automated or visual procedures. For resting-state analyses, PAF will be estimated only when at least approximately 3 minutes of clean data are available and a clear, stable alpha peak (8‐12 Hz) is identifiable; datasets with excessive channel noise (>10% bad channels), insufficient data, or unstable spectra will be excluded. For somatosensory-evoked potentials, trials with artifacts will be discarded, and analyses will require ≥80% of clean trials; averaged waveforms must show identifiable and temporally consistent components (eg, N20 and P25); otherwise, they will be excluded [127-129]. Missing data across visits and modalities will be handled using full information maximum likelihood within growth curve models under a missing-at-random assumption, and all exclusions and missing data patterns will be reported.

This study is expected to show that NGF-induced sustained muscle pain alters motor coordination patterns, characterized by reduced kinematic variability and increased muscle synergy activation consistency. These changes are hypothesized to emerge during pain development (days +2 to +4) and to persist beyond pain resolution. We hypothesize that individuals with lower sensorimotor cortex excitability (reduced TMS map volume), elevated intracortical inhibition (increased SICI), impaired sensorimotor integration (reduced SEP area), and passive cognitive coping strategies will exhibit the most maladaptive motor responses, manifesting as stereotyped, low-variability movement patterns.

While acute pain studies document immediate motor inhibition and reduced corticomotor excitability [11,130], our longitudinal NGF model extends this work by capturing the transition from acute protection to potential maladaptation across pain development and resolution [131]. Unlike cross-sectional clinical pain research showing reduced movement variability in chronic conditions [132,133], our experimental pain model will allow us to examine the temporal precedence of cortical changes over motor adaptations. Preliminary NGF work demonstrates pain hypersensitivity and altered PPTs [131,134], but our comprehensive assessment linking cortical excitability, sensorimotor integration, cognitive coping, and multidimensional motor outcomes represents a novel mechanistic synthesis. The hypothesis that passive cognitive strategies predict maladaptive motor responses builds on evidence that such strategies impair cognitive performance during pain [135-137], suggesting a potential extension of this relationship to the emergence of rigid movement patterns.

Strengths include the longitudinal design tracking pain transition across multiple time points, comprehensive multimethod assessment (TMS/EEG/EMG/kinematics and questionnaires), and GCM accommodating individual differences and missing data. The NGF model produces clinically relevant sustained forearm pain-mirroring lateral epicondylalgia, enhancing translational validity. Limitations include reliance on healthy participants, limiting direct generalizability to clinical pain populations despite mechanistic parallels.

Future research should validate these cortical-motor biomarkers in chronic pain populations to establish clinical usefulness. Personalized neuromodulation targeting identified cortical mechanisms (eg, inhibitory rTMS for elevated SICI) warrants investigation. Integration with structural or functional neuroimaging and machine learning trajectory classification could refine precision medicine approaches. Finally, active coping interventions during pain development may prevent maladaptive motor learning, warranting randomized trials.

Findings will be disseminated via open-access publication in high-impact pain journals, preregistration updates on Open Science Framework, conference presentations (eg, IASP 2028, Society for Neuroscience), and community seminars. Raw data, analysis scripts, and processing pipelines will be deposited in Open Science Framework post publication.

This protocol describes a longitudinal experimental study designed to examine how NGF-induced sustained muscle pain influences motor adaptation, cortical excitability, sensorimotor integration, and pain-related cognition in healthy participants. By combining repeated assessments across the transition from pain development to recovery, the study will help clarify which neurophysiological and behavioral factors are associated with maladaptive movement responses and which may predict greater persistence of altered motor control.

The findings are expected to improve understanding of the mechanisms linking pain and movement and to provide a framework for future work in chronic musculoskeletal pain. In doing so, this study may support the development of more targeted, mechanism-based interventions for pain-related motor dysfunction.