The Effect of Low-Level Light Therapy on Capsaicin-Induced Peripheral and Central Sensitization in Healthy Volunteers: A Double-Blinded, Randomized, Sham-Controlled Trial.

INTRODUCTION: Several clinical trials have demonstrated that low-level light therapy (LLLT), a method of photobiomodulation, is an effective analgetic treatment. However, the mechanism of action has not yet been finally clarified. In particular, unanswered questions include whether it only affects peripheral or whether it also affects the spinal or supraspinal level. This study aimed to evaluate the effect of low-level light therapy on primary and secondary hyperalgesia in a human pain model.
METHODS: This study was planned as a randomized, sham-controlled, and double-blinded trial with repeated measures within subject design. Capsaicin was applied on both forearms of ten healthy volunteers to induce peripheral and central sensitization. One forearm was treated with low-level light therapy; the other served as sham control.
RESULTS: Low-level light therapy significantly increased the mechanical pain threshold, heat pain threshold, and decreased pain intensity.
CONCLUSIONS: Our data indicate that low-level light therapy is effective at reducing the heat and mechanical pain threshold in a human pain model, pointing to a significant modulating effect on peripheral and central sensitization. These effects-especially in the absence of reported side effects-make low-level light therapy a promising tool in pain management. The application of low-level light therapy to treat chronic pain should be considered for further clinical trials.

RCT Entities:   Population Interventions Outcomes

Key Summary Points

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Introduction

Low-level light therapy (LLLT), a method of photobiomodulation, is well established in various fields of medicine. In general, LLLT is the clinical application of light with wavelengths usually in the range of 600 to 1100 nm and a typical power density from 5 mWcm−2 to 5 Wcm−2 [1]. Indications for LLLT are the improvement of wound healing and tissue regeneration, scarring, and perfusion, as well as pain therapy.

In the last few decades, the phenomenon of sensitization has been increasingly studied for its fundamental role in pain medicine [2, 3]. Sensitization is generally regarded as a physiological, adaptive, and self-limiting process caused by nociceptive stimuli to facilitate healing of an injury. However, prolonged sensitization is maladaptive and represents a major contribution to the development of pain chronification. Systematically, sensitization can be grouped into central and peripheral mechanisms.

Peripheral sensitization causes the so-called primary hyperalgesia at the nociceptor level due to an excessive stimulus response by decreasing the threshold for nociception in the peripheral nervous system [4]. The heat pain threshold (HPT) is generally regarded as a marker of primary hyperalgesia [5]. In contrast, central sensitization causes secondary hyperalgesia, which is quantified by the mechanical pain threshold (MPT). Central sensitization is determined by the neuroplastic changes occurring at the spinal or supraspinal level [6].

The distinction between these two mechanisms is relevant because peripheral and central sensitization responds to different therapeutic approaches [7]. Clinically, the two are likely to coexist in the majority of patients experiencing pain; in pain chronification, however, the central processes reach major relevance [3]. They play a pivotal role in the development and maintenance of various chronic pain conditions [8]. For example, central sensitization contributes to the transition process from acute to chronic pain and the development of persistent postoperative pain [9].

Despite convincing results in some clinical trials [10-14], the mechanism of action by which LLLT relieves pain has not yet been clarified. In particular, unanswered questions include whether LLLT only takes effect peripherally or whether it also effects the neuroplastic changes on the spinal or supraspinal level.

To provide an answer to these questions, we use a human pain model developed to mimic different aspects of clinical pain and to study pain mechanisms in order to examine whether peripheral or central mechanisms contribute to the analgetic effect of LLLT.

Methods

Study Design and Ethics Statement

This study was designed as a randomized, sham-controlled, and double-blinded trial with repeated measures within subject design at the Medical University of Graz, Austria. After receiving approval from the ethics committee (EK 30-270 ex 17/18), healthy male and female subjects aged 20–60 willing to participate were included. Exclusion criteria were defined as: known allergies or hypersensitivity to capsaicin, history of skin diseases, neurological diseases, diabetes mellitus, pregnancy, and consummation of analgetic or psychotropic drugs taken within 1 month before study participation.

Those eligible were informed about the study details by the principal investigator and, after giving written consent, were included in the study. During the first visit, demographic information, including Fitzpatrick classification of skin color, was obtained from all patients [15].

A-Priori Sample-Size Calculation

No previously published data were available as a source for an a-priori sample-size calculation. Thus, we powered the study to meet the following parameters: the significance level of 0.05 and beta was 0.2. In a two-sided paired t test, a sample of ten participants is suitable for detecting an effect size of ≥ 1.

Setting

The trial took place in a quiet room with an average temperature of ~ 24 °C over the whole duration of the capsaicin application and irradiation procedure. Probands were situated in the room for at least 30 min to allow acclimatization.

Capsaicin Pain Model

We used a human pain model capable of inducing the central and peripheral mechanisms. Capsaicin application rapidly produces local neurogenic inflammation (characterized by edema and erythema) when locally administered to human skin by stimulating the TRPV1 receptors on dermal sensory nerve endings [5, 16–20]. In this pain model, heat hyperalgesia (i.e., the increased sensitivity to heat stimulation at the site of application of capsaicin) has been found to be due to peripheral sensitization, whereas mechanical hyperalgesia (i.e., increased sensitivity to mechanical stimulation beyond the area of capsaicin) is due to central sensitization [21].

Before the capsaicin application, skin temperature was measured using an infrared thermometer. In the case of skin temperature below 30 °C, the area was covered by a blanket until the required skin temperature was reached. A 30 mm × 30 mm cutaneous capsaicin patch 8% (Qutenza, Grünenthal, Aachen, Germany) with 640 mg of capsaicin per cm2 (corresponding to 5.76 mg of capsaicin in total) was applied in the volar side in the middle of both distal forearms of the participants. The patches were loosely fixed with bandages. After 60 min, the patches were removed, and the exposed skin areas were treated with the appropriate cleansing gel (supplied with Qutenza and intended for removal) according to the manufacturer’s recommendations.

Randomization and Blinding

During the capsaicin application, patients were randomized to determine which arm was treated with LLLT. The other arm received the same treatment with an unactivated device and served as sham-control. Randomization was carried out by a coin toss (left or right) by a nurse, who had no further involvement in the study except for the irradiation procedure. The observer was not present during the randomization and intervention. The nurse was instructed not to share any information about the allocation of the side of irradiation with the volunteers and observers.

The volunteers were blinded with opaque goggles. In addition, they wore earplugs to prevent them from hearing the ventilator noise of the LLLT system.

Intervention

Immediately after removing the capsaicin patch, the two forearms were positioned in the same way on a base divided by an opaque screen to avoid scattered radiation (Fig. 2). The nurse, who was also responsible for the randomization, positioned two identical LLLT devices (Repuls7, Repuls Lichtmedizintechnik GmbH, Vienna, Austria) simultaneously with a 7 cm-distance ring in direct contact with the skin. According to the randomization procedure, one LLLT device remained turned off. The other forearm was irradiated with pulsating and cold red light of 640 nm. The intensity was 175 mWcm−2, which corresponds to a power density of 4100 mW. The pulse frequency was set to 2.5 Hz. A duration of 12 min was chosen based on the manufacture’s recommendations.

Fig. 2

Setup of the intervention. Both forearms were positioned in the same way on a base divided by an opaque screen to avoid scattered radiation. One side was irradiated and the other side received a sham intervention (not displayed). The red area marks the neurogenic inflammation caused by the capsaicin application

Measurement

Measurement was performed directly after intervention. Pain intensity was quantified using a numeric rating scale (NRS 0–10) immediately after intervention on the irradiated and non-treated forearms. Assessment of the sensory thresholds was based on the specifications of the German Research Association for Neuropathic Pain [22, 23].

HPT was assessed on both the LLLT irradiated forearm and non-treated forearm (= control). It was evaluated using a computer-controlled Peltier element, the TSA-II Quantitative NeuroSensory Analyzer (Medoc Ltd., Ramat Yishai, Israel), with a 30 mm × 30 mm thermode. As heat hyperalgesia is only present in the area of primary hyperalgesia [24], the probe of the TSA was exactly positioned to match the marked edges of the capsaicin patch. The baseline temperature of the probe was 32 °C. The ramp for the temperature increase of the probe was set to 1 °C/s. The volunteers were instructed to press a button as soon as they felt a sensation that was not only warm but also accompanied by a burning, stinging, drilling, or dragging feeling.

MPT was assessed on both sides 1 cm proximal to the marked area using pinpricks with a calibrated force of 8, 16, 32, 64, 128, 256, and 512 mN and a flat contact area 0.2 mm in diameter (MRC Systems GmbH, Heidelberg, Germany). The pinpricks were applied with a stepwise which increased force. The volunteers were instructed to indicate the force where they first perceived a sharp sensation. They were then asked about any side effects at the end of the irradiation and the end of the measurement.

Statistical Analysis

The data were analyzed for normality by the Shapiro–Wilk test. Accordingly, a comparison of the sides was calculated using a paired t test or Wilcoxon signed-rank test, as appropriate. The significance level α was set to 0.05. To quantify the magnitude of the effect size, Cohen’s d for repeated measurement was calculated with their corresponding 95% confidence interval (95% CI). The effect sizes were summarized in three categories: small (0.2 < d < 0.5), medium (0.5 < d < 0.8), and large (d > 0.8) [25].

The force measurements of the mechanical pain sensitivity were transformed into decadic logarithms. Before the logarithmic transformation, a constant of 0.1 was added to all zero and non-zero raw data in order to avoid a loss of zero values [26]. The data were summarized as mean and standard deviations.

All analyses were conducted with NCSS [NCSS 12 Statistical Software (2018); NCSS, LLC. Kaysville, UT, USA]. Data analyses were performed by an independent researcher blinded to the group assignment.

This manuscript was prepared according to the Consort guidelines. All procedures were in accordance with the Helsinki Declaration.

Results

In July and August 2019, seven females and three males were assessed for eligibility and included in the trial. Patient demographics are presented in Table 1. The age of the probands ranged from 27 to 58 years. Eight subjects were right-handed and two were left-handed. All participants were Caucasian and had dark white skin, according to skin type 3 of the Fitzpatrick classification. The treatment side was randomly allocated to the right side in five subjects and to the left side in five subjects. Skin temperature was in the range of 32 ± 1 °C before the capsaicin application for all probands without the need for external warming.

Table 1

Demographic data

Sex (female/male)	7/3
Age (years)	41.2 ± 9.9
Weight (kg)	70.1 ± .8.3
Height (cm)	174.7 ± 8.5

A schematic diagram of the time-course of the study is presented in Fig. 1.

Fig. 1

Study flowchart

NRS pain values differed significantly between the LLLT-treated side and control side (3.6 ± 1.2 vs. 4.4 ± 1.1, p = 0.0107). Likewise, HPT (40.2 ± 2.5 °C vs. 36.9 ± 1.8 °C, p = 0.0026) and the mechanical pain sensitivity (MPS) [2.19 ± 0.43 log10 (mN) vs. 1.89 ± 0.45 log10 (mN), p = 0.0084] differed significantly.

The effect size was 0.682 (95% CI 0.385–1.03) for the NRS pain values, 1.037 (95% CI 0.103–1.97) for MPS and 1.54 (95% CI 0.544–2.541) for HPT.

All the participants completed the study. There were no unexpected side effects reported (Fig. 2).

Discussion

Our study shows that LLLT reduces pain intensity, as well as both peripheral and central sensitization in a human pain model.

Effect on Pain Intensity

A few clinical trials have demonstrated that LLLT alleviates pain. Most of these studies were carried out in postoperative scenarios. LLLT was shown to be effective in decreasing mean pain intensity in patients undergoing hip arthroplasty [11], coronary bypass surgery [13], and orthodontic tooth movement [10]. Likewise, in a non-surgical acute pain setting, pre-treatment with LLLT before radiotherapy in breast cancer patients had a dual beneficial effect in reducing the severity of radiodermatitis and ameliorating pain intensity due to radiation-induced skin toxicity.

There are very few studies that concentrate on LLLT and chronic pain. In patients with nonspecific chronic knee pain, treatment with LLLT decreased pain and improved quality of life [12].

The results of our trial are in line with the findings of the above-mentioned small number of clinical studies. The pain intensity our probands experienced on the irradiated forearm was reduced by nearly one-quarter compared with the intensity on the sham-treated forearm, representing a medium effect size.

Proposed mechanisms of analgetic action include local release of serotonin, endorphins, and anti-inflammatory effects [13]. Additionally, activation of peripheral opioid receptors may contribute [27].

Effect on Peripheral Sensitization

Our data have shown that HPT experienced a statistically significant increase in the LLLT-treated forearm compared with the sham-treated forearm. This corresponds to a reduction in peripheral sensitization.

The intracellular mechanisms of sensitization of nociceptors—the structure where the peripheral sensitization mainly takes place—are not yet fully understood. The complex processes of immunology, however, which have recently been well studied, should attract particular attention. Several studies have shown that pronociceptive cytokines like tumor necrosis factor α (TNF-α), IL-1β, and IL-6, as well as antinociceptive cytokines like IL-10 contribute to balanced nociceptor sensitivity. LLLT contributes to a decrease in the pro-inflammatory cytokines IL-1β and IL-6 as well as an increase in the anti-inflammatory cytokine IL-10 [28, 29]. In clinical trials, TNF-α and IL-6 showed decreased serum levels after hip arthroplasties were treated with LLLT [11, 30]. The effect of LLLT on pro-inflammatory TNF-α was studied in a sciatic nerve crush model in mice, but the results were controversial [29, 31].

The release of opioid peptides by immune cells is another peripheral endogenous antinociceptive mechanism involved in counteracting inflammatory hyperalgesia [32]. In this context, the LLLT-related activation of peripheral opioid receptors, which involve the recruitment of opioid-containing leukocytes, are certainly of great relevance [27].

Central Sensitization

Mechanical pain sensitivity differed significantly between the irradiated and non-irradiated forearms, pointing to an influence of LLLT on central sensitization. Although these results may appear counterintuitive at first glance, there are some possible explanations for how changes at the spinal and supraspinal level can be caused by topical treatment. However, as our study was not designed to elucidate the underlying mechanisms, we can only speculate on the potential explanations for our observed antihyperalgetic effect. Nitric oxide (NO) is regarded as an important element in central sensitization of nociceptive posterior horn neurons [33-35]. There are references that show the involvement of NO in cellular mechanisms of low-level light therapy [36, 37].

Glutamergic calcium conducting ion channels, in particular, NMDA receptor channels, as well as the activation of TRPV1 receptors, are essential for central sensitization processes (i.e., long-term potentiation) [6]. Pigatto et al. demonstrated in a very recent study the involvement of both TRPV1 and glutamate on the analgetic effect of LLLT [38]. One could therefore speculate that these mechanisms may also represent a potential rational for our findings.

Clinical Perspective

Peripheral and central sensitization are two pivotal mechanisms in our current understanding of pain physiology. While peripheral sensitization is often linked to inflammation, which is a typical component of various acute pain scenarios, central sensitization is regarded as a key domain in the chronification of pain [2, 3].

Previous clinical studies on the effectiveness of LLLT have been conducted primarily for the treatment of acute pain [10, 11, 13, 14]. These convincing results can be explained by the effect on peripheral sensitization, which we showed in the present study. Our results provide the mechanistic background of the effect of LLLT on acute pain disorders.

What surprised us was the central effect of LLLT. The effect size of these results was even larger than the effect on pain intensity. Until now, the application of LLLT in chronic pain scenarios has only been evaluated in a single clinical trial, which suggested it as an effective treatment option [12]. Our findings encourage further clinical trials on chronic pain.

Limitations

The present study has limitations that need to be addressed. First, the duration of the LLLT application was chosen arbitrarily. As no previously published evidence was available, we followed the manufacturer’s recommendations.

Another limitation is that we applied only a single LLLT treatment. Repeating the LLLT therapy several times would not have been reasonable due to the temporal dynamics of the chosen pain model [39]. However, even our single treatment resulted in medium to strong effects. Evaluation of repeated applications in a prolonged human pain model would thus be theoretically interesting but would raise major ethical issues. Therefore, the effectiveness of different treatment durations should be further studied in clinical scenarios related to chronic pain.

Another interesting parameter would have been the size of the flare area, which occurs as a result of neurogenic inflammation. Unfortunately, we did not have access to the necessary measurement systems for a valid assessment, such as a laser Doppler flowmeter.

Finally, we have to emphasize that this study was not designed for elucidating background mechanisms but to assign the analgetic effect to clinically relevant modes of action. All assumptions on potential underlying causes and contributors are speculative.

Conclusions

Our data indicate that LLLT is effective in reducing HPT and MPT in a human pain model, pointing to a significant modulating effect on peripheral and central sensitization. These effects—especially in the absence of reported side effects—make LLLT a promising tool in pain management. The application of LLLT to treat chronic pain should be considered for further clinical trials.

Peripheral and central sensitization are pivotal mechanisms in pain physiology.

Peripheral sensitization is often linked to inflammation and acute pain.

Central sensitization is regarded as a key domain in the chronification of pain.

We have shown that low-level light therapy (LLLT) reduces both central and peripheral sensitization.

The effect size of the central effect was even larger than the effect on pain intensity.

Our findings encourage further clinical trials with LLLT in chronic pain.