Yes. Multiple randomised controlled trials and systematic reviews support near-infrared PBM for chronic pain, including knee osteoarthritis, neck pain, lower back pain, and fibromyalgia. The mechanism involves two simultaneous pathways: (1) anti-inflammatory — ATP-driven NF-κB modulation reduces TNF-alpha, IL-1β and IL-6 in the affected tissue; (2) neurological — nitric oxide modulates substance P and reduces peripheral nerve pain sensitivity. Both mechanisms produce cumulative effects that deepen over weeks of consistent use.

Near-infrared light at 880nm penetrates 6–30mm into tissue and is absorbed by Cytochrome c Oxidase in mitochondria of immune cells and fibroblasts. This produces an ATP surge that activates the NF-κB anti-inflammatory pathway, downregulating pro-inflammatory cytokines including TNF-alpha, IL-1β and IL-6 — the primary chemical drivers of chronic pain. Simultaneously, displaced nitric oxide dilates local blood vessels and modulates substance P — the neuropeptide responsible for pain signal amplification.

Near-infrared light at 880nm penetrates 6–30mm depending on tissue composition — through skin, subcutaneous fat, and into muscle, joint capsule, and connective tissue. This is sufficient to reach the synovial membrane of knee, hip, shoulder, and finger joints, the paraspinal muscles and facet joints of the lumbar spine, and the disc-nerve interface in cervical and lumbar regions. Celluma's flexible zero-gap contact panel maximises irradiance delivery at depth by eliminating the air gap that reduces effective dose in flat panel devices.

Many users report reduced pain intensity within the first 1–3 sessions due to the immediate vasodilation and nitric oxide effects. Measurable anti-inflammatory changes in cytokine levels occur within 2 weeks of daily use. Sustained pain reduction — where the baseline pain level has genuinely shifted rather than being temporarily suppressed — typically becomes apparent at 4–8 weeks of consistent daily sessions. This cumulative effect is the meaningful clinical outcome.

Osteoarthritis is one of the most clinically studied applications of PBM and has the strongest evidence base. Cochrane reviews and multiple systematic analyses support PBMT for knee and hip osteoarthritis pain reduction, improvement in joint function, and reduction in analgesic use. The mechanism targets synovial inflammation directly — reducing the inflammatory mediators that drive cartilage degradation and joint pain. Early and consistent use produces the best outcomes.

Red light therapy is not a replacement for prescribed pain management — it is a powerful adjunct that addresses the underlying inflammatory mechanism rather than blocking the pain signal. Many consistent users report reduced reliance on NSAIDs and analgesics over time as their baseline inflammation decreases. This transition should be managed with medical guidance. Unlike pain medication, PBM has no systemic side effects and does not carry gastrointestinal, cardiovascular or dependency risks.

Inflammatory pain (arthritis, tendinopathy, bursitis, inflammatory back pain) responds most dramatically — PBM directly targets the cytokine cascade driving inflammation. Neuropathic pain (peripheral neuropathy, nerve compression) also responds well via the substance P and nerve conduction modulation mechanism. Musculoskeletal pain (muscle tension, post-exercise soreness, soft tissue injuries) responds through the combined anti-inflammatory and ATP-restoration effects. Purely mechanical pain with no inflammatory component (e.g. structural spinal instability) responds least.

Daily sessions for the first 4 weeks establish the anti-inflammatory baseline. Anti-inflammatory effects from PBM are cumulative — each session builds on the last. Daily use during this initial phase produces the fastest and most durable pain reduction. After 4 weeks, maintenance at 3–5 sessions per week maintains the lowered inflammatory state. A 30-minute session in pain mode (880nm dominant) per day is the standard clinical protocol.