Chemotherapy-induced peripheral neuropathy (CIPN) (including taxanes, platinum, al pervenche from Madagascar alkaloids...), is a frequent secondary effect of treatments: 68% at 1-month post-chemotherapy, 60% at 3 months and 30% after 6 months. Symptoms associated with CIPN are usually symmetric and bilateral (typical distribution in "gloves and socks") inducing sensory alterations, paresthesias, dysesthesias, numbness and pain. Neuropathic Pain (NP) is an important characteristic of CIPN, affects 25-80% of patients with CIPN, and reduces quality of life (e.g., concomitant psychological distress, risks of falls, risks of neurocognitive impairments, and sleep disorders). In severe cases, it is even necessary to delay and/or reduce the dose of chemotherapy. The benefit of drug interventions on NP remains limited. To date, there are no proven preventive strategies and few evidence-based treatment options for CIPN. Also, the use of complementary or non-pharmacological interventions are common, including photobiomodulation (PBM). PBM is the therapeutic use of non-ionizing laser light for its anti-inflammatory and regenerative effects. Its use is currently recommended only for the prevention of oral mucositis related to cancer treatments. Recent preliminary clinical evidence suggests that PBM may be beneficial to established CIPN, with safety and improvement beyond the intervention. However, to date, clinical trials are rare, have methodological weaknesses, and/or focus on global CIPN. The overall objectives of the study are therefore to assess the effectiveness, feasibility and safety of the PBM for treating NP in the CIPN.
Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
Purpose
SUPPORTIVE_CARE
Masking
SINGLE
Enrollment
70
The treatment will be administered by an ATP38 device delivering a power of 4 Joules/cm2 at wavelengths of 620 and 820 nm
ICM
Montpellier, France
RECRUITINGEvaluation of the efficacy of photobiomodulation on neuropathic pain in a experimental group and evaluate the placebo effect in a controlled group
the proportion of responders to a photobiomodulation intervention on their neuropathic pain at 12 weeks
Time frame: from the baseline to 12 weeks after the treatment
Description of the evolution of neuropathic pain
description by the scores of the clinician-rated neuropathic pain questionnaire (from 0 to 10, 0 no neuropathic pain, 10 : worst neuropatic pain)
Time frame: from the baseline to 6 months after the treatment
Description of the evolution of neuropathic pain
description by the scores of the self-questionnaire Neuropathic Pain Symptom Inventory (from 0 to 100, 0 no neuropathic pain, 100 : worst neuropatic pain)
Time frame: from the baseline to 6 months after the treatment
Exploration of the evolution of global pain measures
The global pain will be assessed using the scores of the self-questionnaire Brief Pain Inventory (from 0 to 110, 0 no neuropathic pain, 110 : worst neuropatic pain)
Time frame: from the baseline to 6 months after the treatment
Exploration of the evolution of global pain measures
The global pain will be assessed using the scores of the Numeric Scale of pain (from 0 to 10, 0 no pain, 10 worst pain)
Time frame: from the baseline to 6 months after the treatment
Description of the evolution of the Chemotherapy-induced peripheral neuropathy
The chemotherapy-induced peripheral neuropathy will be described using the scores of the self-questionnaire FACT/GOG-Ntx-13, and the grade of chemotherapy-induced peripheral neuropathy assessed by the clinician via the Common Terminology Criteria for Adverse Events (ranging from 0 to 5, a high score indicates a strong neuropathy).
Time frame: from the baseline to 6 months after the treatment
Exploration of the evolution of quality of life
The quality of life will be explored using the self-questionnaire Functional Assessment of Chronic illness Therapy-Global scores \[the global score and its 4 sub-scales scores (physical, social/family, emotional, functional\] and the number of falls reported by the patient during the last month (from 0 to 108, 0 bad quality of life, 108 good quality of life)
Time frame: from the baseline to 6 months after the treatment
Exploration of the evolution of sleep disorders
Sleep disorders will be explored using the self-assessment Sleep Severity Index (ISI).
Time frame: from the baseline to 6 months after the treatment
Description of the evolution of neurocognitive executive functioning
Neurocognitive functioning will be assessed using the clinician-rated scores of the test modified-Delis-Kaplan Executive Function System (m-DKEFS)
Time frame: from the baseline to 6 months after the treatment
Description of the evolution of neurocognitive executive functioning
Neurocognitive functioning will be assessed using the scores of the Trail Making Test (TMT A and B)
Time frame: from the baseline to 6 months after the treatment
Assessment of the photobiomodulation adherence
The adherence to the intervention will be assessed by the number of PBM sessions performed by patients
Time frame: from the baseline to 4 weeks after the beginning of the treatment
Evaluation of the safety of the photobiomodulation
The safety of PBM will be assessed by the number and the severity of target adverse events recorded during the study period, using the CTCAE scale (v5.0)
Time frame: from the baseline to 6 months after the treatment
Assessment of emotional distress
Emotional distress will be measured by the score of the Hospital Anxiety and Depression Scale (HADS) Questionnaire at baseline and at the end of photobiomodulation treatment
Time frame: from the baseline to 4 weeks after the treatment
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