Pain Medicine & Palliative Caremoderate

Neuropathic Pain.Care & specialists in Oman

In Oman, neuropathic Pain is managed by pain medicine & palliative cares. Neuropathic pain is chronic pain caused by damage or disease of the somatosensory nervous system itself, rather than ongoing tissue injury. It affects an estimated 7-10% of the general population, with diabetic peripheral neuropathy, postherpetic neuralgia, sciatica, post-stroke central pain, and chemotherapy-induced neuropathy accounting for most cases.

aliases · Neuropathic Pain (nerve pain)· तंत्रिकाजन्य दर्द (Tantrikajanya Dard)· Douleur neuropathique· Neuropathische Schmerzen· reviewed May 12, 2026

Reviewed by AIHealz Medical Editorial Board · Pain Medicine & Palliative CareLast reviewed May 12, 2026

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§ 01

What it is

Neuropathic pain (ICD-10: G89.4 chronic pain syndrome; G62.9 polyneuropathy, unspecified; G63 polyneuropathy in diseases classified elsewhere) is defined by the International Association for the Study of Pain (IASP, 2017) as pain caused by a lesion or disease of the somatosensory nervous system. The lesion can sit anywhere along the pain pathway — peripheral nerve, dorsal root ganglion, spinal cord, brainstem, thalamus, or cortex — and produces aberrant signalling rather than appropriate detection of tissue damage. Pathophysiology involves peripheral sensitisation through ectopic firing of injured axons and dorsal root ganglion neurons, upregulation of sodium channels Nav1.7 and Nav1.8, microglial activation in the dorsal horn, central sensitisation via NMDA-receptor potentiation, and loss of descending inhibitory control from brainstem nuclei. The 2015 NeuPSIG grading algorithm (Finnerup, Lancet Neurology) classifies a patient as having possible, probable, or definite neuropathic pain based on pain distribution in a plausible neuroanatomical territory, a relevant lesion on history, sensory signs on examination, and confirmatory testing.

key facts

Prevalence: Roughly 7-10% of adults globally have neuropathic pain (van Hecke 2014 meta-analysis); 6.9% in a French general-population survey (Bouhassira 2008)
Demographics: Women slightly more affected than men; prevalence rises with age and with diabetes duration
Avg. age: Most common in adults 50-70; postherpetic neuralgia mainly over age 60; diabetic neuropathy begins 5-15 years after diabetes diagnosis
Global cases: Estimated 400-700 million people worldwide have a neuropathic pain component to their chronic pain (IASP 2017 working estimates)
Specialist: Pain Medicine & Palliative Care

§ 02

How you might notice it

01Constant or near-constant burning pain in the affected territory, often worst at night and interfering with sleep — described by patients as 'on fire' or 'sunburned from the inside'.

02Brief, paroxysmal electric-shock-like or shooting pains lasting seconds, occurring spontaneously or triggered by minor stimuli such as touch or movement.

03Allodynia — pain provoked by stimuli that should not be painful, such as the brush of clothing, a bedsheet, or a light breeze across the skin.

§ 03

How it’s diagnosed

diagnosis

Diagnosis of neuropathic pain is primarily clinical, anchored on the 2015 NeuPSIG grading algorithm (Finnerup, Lancet Neurology). The clinician first establishes whether the pain has a plausible neuroanatomical distribution — does the territory correspond to a peripheral nerve, dermatome, plexus, spinal cord level, or central pathway. Step two is a history of a relevant lesion or disease that can explain the distribution, such as long-standing diabetes, a previous shingles rash, a known disc herniation, a stroke, or recent neurotoxic chemotherapy. Step three is a focused sensory examination — testing for hypoesthesia and hyperalgesia with pinprick, allodynia with a soft brush, thermal hypoesthesia with warm and cool objects, and vibration loss with a 128 Hz tuning fork. Reflex changes and motor signs are documented when present. Confirmatory testing depends on the suspected lesion. Nerve conduction studies and electromyography document large-fibre neuropathy and localise mononeuropathies and radiculopathies but are normal in pure small-fibre disease. Skin biopsy for intraepidermal nerve fibre density confirms small-fibre neuropathy. MRI defines structural lesions of brain, spinal cord, and roots. Quantitative sensory testing has a research role and helps phenotype patients for trial enrolment. Validated screening tools — the painDETECT, DN4, and LANSS questionnaires — distinguish neuropathic from nociceptive pain in primary care with sensitivities of 80-85%. Three certainty levels emerge from this workflow: possible (criteria 1-2 met), probable (criteria 1-3 met), and definite (criteria 1-4 met, with confirmatory testing). Most treatment guidelines apply once probable status is reached.

Key tests

Focused sensory examination (bedside)Documents the pattern of sensory loss and gain — hypoesthesia, allodynia, hyperalgesia, thermal and vibration thresholds — and maps the distribution against known neuroanatomy. The cornerstone of the NeuPSIG algorithm.

Validated screening questionnaire (DN4, painDETECT, or LANSS)

§ 04

Treatment & cost

medical treatments

✓Gabapentin (start 100-300 mg at night; titrate to 900-3600 mg/day divided in 3 doses)
✓Pregabalin (start 75 mg twice daily; titrate to 150-600 mg/day)
✓Duloxetine (start 30 mg once daily; titrate to 60-120 mg/day)
✓Amitriptyline or nortriptyline (start 10-25 mg at bedtime; titrate to 25-75 mg)

surgical options

Spinal cord stimulation (SCS), including 10 kHz high-frequency systemsRoughly 60-70% sustained responders (≥50% pain relief) at 12-24 months in current high-frequency systems.

Dorsal root ganglion (DRG) stimulationRoughly 75% responders at 3 months and 65% at 12 months in CRPS-I/causalgia (Deer 2017).

Microvascular decompression for trigeminal neuralgiaInitial pain-free outcome in 80-90%; durable freedom at 10 years in roughly 70%.

Decompressive spine surgery (microdiscectomy, laminectomy)Roughly 75-80% achieve significant leg-pain relief at 1-2 years; back pain improves less reliably (SPORT trial).

§ 05

Causes & risk factors

known causes

Diabetes mellitus: Chronic hyperglycaemia damages small unmyelinated and large myelinated fibres through polyol pathway flux, advanced glycation end products, oxidative stress, and microvascular ischaemia of the vasa nervorum. Accounts for the single largest share of neuropathic pain globally.
Herpes zoster (shingles) reactivation: Varicella-zoster virus reactivates from dorsal root ganglia in adults with waning cell-mediated immunity, producing dermatomal rash and direct neuronal injury that can persist as postherpetic neuralgia in 10-15% of patients over 60.
Mechanical nerve root compression: Disc herniation, foraminal stenosis, and spondylolisthesis compress lumbar or cervical nerve roots, producing radicular pain and sciatica. Inflammation around the root, not just mechanical pressure, drives much of the pain.
Chemotherapy and other neurotoxic drugs: Platinum compounds, taxanes, vinca alkaloids, bortezomib, thalidomide, isoniazid, metronidazole, and antiretrovirals damage peripheral axons or dorsal root ganglion neurons. Risk is dose-dependent and may be permanent.
Stroke, multiple sclerosis, and spinal cord lesions: Lesions in central somatosensory pathways — thalamus, brainstem, spinothalamic tract — produce central neuropathic pain. About 8-10% of stroke survivors develop central post-stroke pain, often months after the initial event.
Traumatic nerve injury and surgery: Direct nerve transection, stretch, or entrapment during surgery (hernia repair, mastectomy, thoracotomy, amputation) produces chronic post-surgical neuropathic pain in 5-30% of patients depending on procedure.
Autoimmune and inflammatory neuropathies: Chronic inflammatory demyelinating polyradiculoneuropathy, Sjögren syndrome, sarcoidosis, vasculitis, and HIV-related neuropathy damage peripheral nerves through immune mechanisms and produce neuropathic pain.

§ 06

Living with it

01Vaccinate adults over 50 with recombinant zoster vaccine (Shingrix) — over 90% protection against shingles and approximately 88% against postherpetic neuralgia in the ZOE-50 and ZOE-70 trials

02Maintain HbA1c below 7.0% in type 1 diabetes and an individualised target (typically 6.5-7.5%) in type 2 diabetes to slow progression of diabetic neuropathy

03Replete vitamin B12 in patients on long-term metformin or proton-pump inhibitors and screen older adults — replacement reverses early neuropathy

04Use the lowest effective dose of neurotoxic chemotherapy and consider dose reduction or substitution at the first sign of neuropathy; duloxetine has prevention-of-progression data for established CIPN

05Treat herpes zoster within 72 hours with antiviral therapy (valaciclovir, famciclovir, aciclovir) to shorten the acute attack and modestly reduce PHN risk

06Limit alcohol intake to under 14 standard drinks per week and avoid prolonged heavy drinking that produces nutritional neuropathy

recommended foods

•Mediterranean-style eating pattern rich in vegetables, fruit, legumes, fish, and olive oil — reduces inflammation and improves nerve health in observational studies

§ 07

When to seek help

why see a pain medicine & palliative care

Pain medicine specialist referral is warranted when two or more first-line agents at adequate dose and duration have failed, when an interventional option such as a nerve block or spinal cord stimulator is being considered, when pain involves a complex distribution (CRPS, central pain), or when high-risk medication combinations (opioids, multiple sedating agents) are being layered. A neurologist should be involved when the diagnosis is uncertain, when central nervous system disease is suspected, or when small-fibre neuropathy needs skin biopsy confirmation. Spine surgery referral is appropriate for radicular pain with progressive neurological deficit or imaging-concordant compressive lesions.

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01Sleep deprivation and depression — present in 30-50% of patients with persistent neuropathic pain and themselves worsen pain perception

02Opioid dependence when opioids are prescribed long-term without clear benefit; current guidelines explicitly recommend against routine opioid initiation

03Falls and fractures in older adults with peripheral neuropathy and impaired proprioception, especially when combined with sedating medication

04Diabetic foot ulceration, infection, and amputation when sensory neuropathy is unrecognised — annual foot examination prevents most events

Related conditions

Type 2 DiabetesUnderlying cause of painful diabetic peripheral neuropathy, the most common form of neuropathic pain worldwide.Read →Postherpetic NeuralgiaSpecific neuropathic pain syndrome after shingles; vaccinatable risk factor and a model condition for first-line therapy.Read →Trigeminal NeuralgiaDistinct facial neuropathic pain syndrome with a specialised first-line drug (carbamazepine) and surgical options.Read →SciaticaRadicular neuropathic pain from lumbar nerve root compression; the most common cause of leg-distributed neuropathic pain.Read →Complex Regional Pain Syndrome (CRPS)Severe regional neuropathic pain after limb injury; shares interventional treatment pathways such as DRG and spinal cord stimulation.Read →Multiple SclerosisCentral nervous system demyelinating disease that produces central neuropathic pain, including trigeminal neuralgia and Lhermitte sign, in a substantial minority of patients.Read →

Easily confused with

vs. Neuropathic Pain

FibromyalgiaFibromyalgia produces widespread pain with tender points, fatigue, and cognitive symptoms but lacks a single demonstrable nerve lesion. Neuropathic pain follows a neuroanatomical territory and has objective sensory signs; fibromyalgia pain is diffuse and is classified as nociplastic. Both can coexist and respond partially to duloxetine and pregabalin.Compare →

vs. Neuropathic Pain

Carpal Tunnel SyndromeCarpal tunnel syndrome is a focal median mononeuropathy at the wrist with classic nocturnal numbness and tingling in the thumb, index, and middle fingers. It is a neuropathic pain condition but localised and typically curable by surgical decompression — distinct from generalised peripheral neuropathic pain that requires systemic therapy.Compare →

vs. Neuropathic Pain

Complex Regional Pain Syndrome (CRPS)CRPS produces severe pain plus autonomic, motor, and trophic changes in a limb after injury, often without a clearly demonstrable nerve lesion (CRPS-I) or with one (CRPS-II). Unlike length-dependent neuropathy, CRPS is regional rather than territorial and is graded by the Budapest criteria.Compare →

vs. Neuropathic Pain

SciaticaSciatica is one specific neuropathic pain syndrome — radicular pain in the L4-S1 distribution from nerve root compression — rather than a separate disease. It is mentioned here because patients often use the term to mean any leg pain; a careful examination distinguishes radicular sciatica from referred lumbar facet pain or hip pathology.

Often appears alongside

Type 2 Diabetes →Postherpetic Neuralgia →Fibromyalgia →

Types and stages

Painful diabetic peripheral neuropathy (DPN)The most common cause worldwide. Length-dependent symmetric polyneuropathy beginning in the toes, with burning, tingling, and allodynia. Affects roughly 20% of people with diabetes for ten years or more.

Postherpetic neuralgia (PHN)Persistent dermatomal pain lasting more than 3 months after a shingles rash. Risk rises sharply with age — about 10-15% of patients over 60 with shingles develop PHN.

Radicular pain and sciaticaNerve root compression or inflammation, usually from disc herniation or foraminal stenosis. Pain follows a dermatomal pattern down the leg or arm.

Chemotherapy-induced peripheral neuropathy (CIPN)Distal symmetric neuropathy from platinum agents, taxanes, vinca alkaloids, bortezomib, and thalidomide. Symptoms can persist for years after treatment ends.

Trigeminal neuralgiaBrief, electric-shock-like facial pain in the distribution of one or more trigeminal divisions, typically triggered by light touch, chewing, or cold air.

Central post-stroke pain (CPSP)Burning or aching pain in the body region affected by stroke, usually beginning weeks to months after the event. Affects 8-10% of stroke survivors.

Spinal cord injury painBelow-level neuropathic pain after traumatic or inflammatory spinal cord injury; often described as burning or band-like.

Phantom limb and post-amputation painPain perceived in a missing limb, occurring in 50-80% of amputees. Mechanisms involve peripheral nerve injury, central reorganisation, and altered body schema.

Living with Neuropathic Pain

Timeline

Pharmacotherapy effects take time to assess. Gabapentin and pregabalin show benefit within 1-2 weeks of reaching an adequate dose. Duloxetine and tricyclic antidepressants typically need 4-6 weeks at target dose for full analgesic effect. Topical 5% lidocaine produces relief within hours but plateaus over days. A single 8% capsaicin application produces stable analgesia from week 2 through week 12 in responders. Spinal cord stimulator trials are usually 5-7 days; permanent implants show stable response by 3 months. Following recommended care, expect the first meaningful improvement at 2-6 weeks and a realistic stable endpoint at 3-6 months; treatment then continues to maintain that response.

Lifestyle

01Sleep optimisation — set consistent sleep and wake times, treat coexisting insomnia and obstructive sleep apnoea, and time sedating medications to night to support 7-8 hours of sleep
02Graded aerobic and resistance exercise — 150 minutes weekly of moderate-intensity activity reduces neuropathic pain intensity and improves nerve fibre density in diabetic neuropathy (Kluding 2012)
03Smoking cessation — nicotine accelerates microvascular nerve damage and reduces analgesic response
04Foot care for patients with diabetic neuropathy — daily inspection, well-fitted footwear, podiatry review, and prompt treatment of any wound to prevent ulceration
05Structured pain self-management programme — pacing, activity planning, and cognitive reframing reduce pain interference even when intensity changes little
06Address mood and anxiety actively — untreated depression and anxiety amplify central sensitisation and reduce response to every analgesic class

Complementary approaches

Cognitive behavioural therapy (CBT) and acceptance and commitment therapy (ACT)Improves pain interference, mood, sleep, and function with moderate effect sizes in randomised trials and Cochrane reviews. Often delivered alongside pharmacotherapy in pain-management programmes.

Transcutaneous electrical nerve stimulation (TENS)Low-risk option with modest evidence for short-term relief in diabetic peripheral neuropathy. Reasonable to trial; not a substitute for first-line pharmacotherapy.

Alpha-lipoic acid (600 mg IV or oral daily)Antioxidant with positive trials in symptomatic diabetic neuropathy (NATHAN-1, SYDNEY trials). Modest effect; widely used in Germany and selected European centres.

Choosing a doctor

Look for fellowship training in pain medicine, board certification, and access to image-guided injection, neuromodulation, and a structured multidisciplinary pain programme that includes a clinical psychologist and physical therapist. Ask whether the clinic uses validated outcome measures (Brief Pain Inventory, neuropathic pain scale, PROMIS) and follows current guidelines rather than defaulting to opioid prescribing. Continuity matters — neuropathic pain is a long-term condition managed over years, and abrupt provider changes degrade outcomes.

Patient support resources

International Association for the Study of Pain (IASP) — Neuropathic Pain Resources →Definitions, grading algorithms, and patient-facing resources from the global authority on pain.

American Chronic Pain Association →US patient organisation with self-management tools, peer support, and educational material on neuropathic pain conditions.

Foundation for Peripheral Neuropathy →US patient organisation focused on peripheral neuropathy with patient guides, research updates, and support networks.

NICE NG193 — Chronic Pain in Over 16s →UK clinical guideline on assessment and management of chronic primary pain and chronic secondary pain, freely accessible.

§ 08

Frequently asked

What does neuropathic pain feel like?

Most patients describe neuropathic pain as burning, electric-shock-like, shooting, or stabbing, often with tingling, pins-and-needles, and numbness in the same area. Light touch, clothing, or a breeze can feel painful (allodynia), and the skin may feel oddly numb and intensely painful at the same time. Pain is often worst at night and disturbs sleep.

How is neuropathic pain different from regular pain?

Regular (nociceptive) pain is the nervous system correctly reporting tissue injury such as a cut, burn, or arthritic joint. Neuropathic pain is the nervous system itself misfiring after damage to a nerve, the spinal cord, or the brain. It does not respond well to standard painkillers like paracetamol, NSAIDs, or opioids and needs different first-line drugs.

What are the most common causes of neuropathic pain?

The leading causes are diabetes (painful diabetic peripheral neuropathy), shingles (postherpetic neuralgia), nerve root compression from the spine (sciatica and cervical radiculopathy), chemotherapy, stroke (central post-stroke pain), spinal cord injury, surgery and trauma, and trigeminal neuralgia. Less common causes include autoimmune neuropathy, HIV, heavy alcohol use, and vitamin B12 deficiency.

How is neuropathic pain diagnosed?

Diagnosis is mainly clinical. A clinician maps the pain to a known nerve territory, looks for a relevant injury or disease in the history, and examines the area for altered sensation. Validated screening questionnaires (painDETECT, DN4, LANSS) help in primary care. Nerve conduction studies, skin biopsy for small-fibre density, and MRI are added when needed to confirm and localise the lesion.

What is the best first-line treatment for neuropathic pain?

Current guidelines (NeuPSIG 2015, NICE NG193, AAN 2022) recommend starting with one of four agents: gabapentin, pregabalin, duloxetine, or a tricyclic antidepressant such as amitriptyline or nortriptyline. Topical 5% lidocaine and 8% capsaicin patches are first-line for localised pain such as postherpetic neuralgia. Choice depends on other conditions, side effects, and access.

Do opioids work for neuropathic pain?

Opioids have modest short-term efficacy in neuropathic pain but tolerance, dependence, and harms grow with long-term use. Major guidelines (NeuPSIG, NICE, CDC) place opioids as third-line at best and recommend against routine initiation. Tramadol and tapentadol, which also act on noradrenergic pathways, may be used in selected refractory cases under specialist care.

How long do gabapentin and pregabalin take to work?

Both drugs need titration. Initial relief can appear within 1-2 weeks of reaching an adequate dose, with full effect by 4-6 weeks. Doses are increased gradually to limit dizziness, drowsiness, and swelling. About 30% of patients reach 50% pain reduction; if there is no meaningful response at maximum tolerated dose by week 6-8, switch to a different drug class rather than stacking similar agents.

Can neuropathic pain go away on its own?

Some forms resolve. Roughly half of postherpetic neuralgia cases improve within a year, and most acute radicular pain from disc herniation settles within 6-12 weeks. Diabetic, central post-stroke, and post-surgical neuropathic pain tend to persist and need ongoing treatment. Early evidence-based care improves the chance of recovery and prevents central sensitisation that makes pain harder to treat later.

Is neuropathic pain curable?

Some causes are curable when treated early — vitamin B12 replacement, alcohol cessation, decompression of a compressed nerve root, and treatment of an underlying autoimmune disease can resolve the pain. Many other forms are not curable but are controllable: most patients achieve meaningful pain reduction with first-line drugs, topical agents, or interventional therapy, allowing better sleep, mood, and function.

Can diabetes cause nerve pain?

Yes. Painful diabetic peripheral neuropathy affects roughly 20-25% of people with diabetes for 10 years or more. It usually begins as burning and tingling in the toes and spreads upward in a stocking pattern. Tight glycaemic control slows progression, and duloxetine, pregabalin, gabapentin, and topical capsaicin are first-line treatments per the 2022 AAN guideline.

What is postherpetic neuralgia?

Postherpetic neuralgia is persistent dermatomal pain lasting more than 3 months after a shingles rash. It is caused by varicella-zoster damage to sensory neurons and affects 10-15% of patients over 60 who develop shingles. First-line treatments include the 5% lidocaine patch, 8% capsaicin patch, gabapentin, pregabalin, and tricyclic antidepressants.

Can the shingles vaccine prevent nerve pain?

Yes. The recombinant zoster vaccine (Shingrix) prevents over 90% of shingles cases and approximately 88% of postherpetic neuralgia in adults over 50 in the ZOE-50 and ZOE-70 trials. Two doses are given 2-6 months apart. It is the most effective single intervention to prevent one of the most common causes of long-term neuropathic pain.

Does chemotherapy cause permanent nerve pain?

Chemotherapy-induced peripheral neuropathy affects 30-40% of patients on platinum agents, taxanes, vinca alkaloids, or bortezomib. Symptoms often improve over months after treatment ends, but roughly 30% have persistent symptoms at 6 months and a smaller share have long-term pain. Duloxetine has the strongest evidence for established CIPN; dose modification during treatment reduces risk.

When should I see a pain specialist?

Ask for a pain medicine referral when two or more first-line drugs at adequate dose and duration have failed, when interventional treatment such as a nerve block or spinal cord stimulator is being considered, when opioid use is escalating, or when pain involves a complex distribution such as CRPS or central pain. A neurologist should be involved when the diagnosis or underlying disease is uncertain.

What is spinal cord stimulation and how well does it work?

Spinal cord stimulation uses a small implanted electrode array in the epidural space to modulate dorsal horn signalling. In the SENZA-RCT, 10 kHz high-frequency stimulation produced sustained responder rates above 70% at 24 months for back and leg pain. The SENZA-PDN trial extended benefit to painful diabetic neuropathy. A 5-7 day external trial is used to confirm response before permanent implantation.

Can exercise help neuropathic pain?

Yes. Structured aerobic and resistance exercise reduces pain intensity, improves sleep and mood, and in diabetic neuropathy increases small-fibre nerve density in the skin (Kluding 2012). Aim for 150 minutes of moderate-intensity activity per week, building gradually. Pool-based exercise and stationary cycling are good options for patients with foot ulcer risk.

Is cannabis effective for nerve pain?

Cannabinoids show a small to modest analgesic effect in neuropathic pain in randomised trials and Cochrane reviews, with notable side effects including dizziness, sedation, and cognitive effects. Major guidelines list cannabinoids as fourth-line or experimental, behind first-line drugs, topical agents, and interventional options. Regulation and product quality vary widely by country.

Can stress and anxiety make nerve pain worse?

Yes. Anxiety, depression, and poor sleep amplify central sensitisation and reduce response to every analgesic class. Cognitive behavioural therapy, acceptance and commitment therapy, and treatment of coexisting depression improve pain interference and function even when pain intensity is only modestly reduced. Mental health care is part of a complete plan, not an add-on.

How is trigeminal neuralgia treated?

First-line drug therapy is carbamazepine, with over 70% initial response, or oxcarbazepine when tolerability matters. Patients with Asian ancestry should be screened for HLA-B*1502 before carbamazepine due to severe skin reaction risk. When medications fail or side effects are intolerable, microvascular decompression, gamma knife radiosurgery, and percutaneous procedures are effective surgical options.

Are topical patches worth trying?

Yes for localised peripheral neuropathic pain. The 5% lidocaine patch is well-tolerated and first-line in postherpetic neuralgia, particularly in older adults. The 8% capsaicin patch (QUTENZA) is applied once in a clinic and provides up to 12 weeks of analgesia in responders. Both avoid systemic side effects and combine well with oral therapy.

Can children get neuropathic pain?

Yes, though less commonly than adults. Causes include traumatic nerve injury, chemotherapy, inherited sodium-channel disorders, CRPS, and post-surgical pain. Treatment principles are similar but doses are weight-based and the evidence base is smaller. Pediatric pain specialists and multidisciplinary programmes give the best outcomes.

§ 09

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