sensory nerves, motor nerves, autonomic nerves

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damage or disease affecting nerves, which may impair sensation, movement, gland or organ function, or other aspects of health, depending on the type of nerve affected o chronic: long term, begins subtly and progresses slowly o acute : sudden onset, rapid progress and slow resolution sensory nerves, motor nerves, autonomic nerves

neuropathy affecting just one nerve is called mononeuropathy neuropathy involving multiple nerves in roughly the same areas on both sides of the body is called "symmetrical polyneuropathy" two or more separate nerves in disparate areas of the body are affected is called " mononeuritis multiplex or multifocal mononeuropathy" or "multiple mononeuropathy.

Osteosclerotic myeloma (POEMS) 50-85% WM 30-50% MGUS 5-37% Amyloidosis (AL) 10-20% Cryoglobulinemia 7-15% Multiple myeloma 3-14% Lymphoma 2-8%

sensory function negative symptoms: o numbness to touch and vibration, o reduced sensitivity to temperature change and pain, o reduced position sense causing poor coordination and balance, and gait abnormality sensory function positive symptoms: o tingling, itching, crawling, pins and needles o pain or skin allodynia (severe pain from normally non-painful stimuli, such as light touch).

motor function negative symptoms (loss of function): o impaired balance and coordination o weakness and tiredness o heaviness and gait abnormalities motor function positive symptoms (gain of function): o cramps o tremors o muscle twitches (fasciculations)

autonomic nerve dysfunction: o poor bladder control o abnormal blood pressure or heart rate o reduced ability to sweat normally pain in the muscles (myalgias) Neuropathy may cause muscle loss, bone degeneration, and changes in the skin, hair, and nails.

Mono, multi, cranial neuropathy & radiculopathy o direct infiltration o nerve/root compression o hyperviscosity o bleeding diathesis o cryoglobulinemia Symmetric polyneuropathy o Amyloidosis o chemo/drug related toxicity o M-protein reactivity with nerve (IgM) o unknown

Antigens % PN o MAG 50% o Sulfatide 6% o GQ1b+Disyalo 2% o GD1a 3% o GM2 2% o GM1 <2%

Patients not impaired in their daily life: o symptomatic therapy for tremor and paresthesias o reassurance on the usually good prognosis for several years Slightly impaired patients: o due to its safe profile and efficacy plasma exchange is probably preferred as first line treatment or during worsening / flare-ups Moderately impaired patients: o Immunotherapy and/or chemo therapy o Rituximab is currently probably the preferred 1 st line option.

Rituximab (62%) Plasma exchange (45%) Chlorambucil (40%) Steroids (39%) Cyclophosphamide (47%) IVIg (18%) Interferon α (27%) Fludarabine (52%) Other therapies (14%)

The Cochrane Library Reviewers conclusions: There is inadequate reliable evidence from trials of immunotherapies in anti-mag neuropathy to recommend any particular immunotherapy. IVIg is relatively safe and may produce some shortterm benefit. Large randomized trials of at least 12 months duration are required to assess the efficacy of existing or novel therapies.

Pain is an unpleasant sensory and emotional experience associated with actual or potential tissue damage or described in terms of such damage. Chronic pain is a complex phenomenon where the intensity and impact of the pain is not always directly related to pathology.

the underlying cause of pain should be treated whenever possible oral medicines are key components of pain management some medicines should be given regularly ("by the clock") therapeutic regimes need to be individualized monitor and evaluate for therapeutic and side effects

anticonvulsants antidepressants benzodiazepines N-methyl-d-aspartate (NMDA) receptor antagonists nonsteroidal anti inflammatory drugs (NSAIDs) opioid therapy topical agents

controlled or extended release opioid therapy (e.g., morphine and oxycodone) provides effective pain relief for patients with neuropathic pain side effects: addiction / dependency, nausea or vomiting, constipation, dizziness, somnolence, and pruritus morphine, codeine, hydrocodone, oxycodone, buprenorphine, fentanyl, methadone, tramadol, etc

research done between 2005 and 2010 indicates that synthetic cannabinoids and inhaled cannabis are effective treatments for a range of neuropathic disorders opiate derivatives taken orally were found to be more effective than cannabis for most people smoked cannabis was found to relieve neuropathy associated with HIV-associated sensory neuropathy, CRPS type I, spinal cord injury, peripheral neuropathy, and nerve injury combination therapy with opioids and cannabinoids found to be synergistic in many studies from Israel

we are all different in many respects and patients who suffer from PN will need to try numerous combinations of therapies before finding the one that works well to control symptoms. the underlying cause of pain should be treated whenever possible and safe to do so.