Chronic Inflammatory Demyelinating Polyneuropathy (CIDP)

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Overview

Chronic Inflammatory Demyelinating Polyneuropathy (CIDP) is an autoimmune disorder that causes progressive weakness and sensory loss in the arms and legs. It is the chronic counterpart of Guillain-Barré syndrome and is characterized by immune-mediated demyelination of peripheral nerves. CIDP represents the most common chronic autoimmune neuropathy worldwide.

Epidemiology

  • Prevalence: 1-2 per 100,000 population

  • Age of onset: Can occur at any age, most commonly in adults aged 40-60

  • Gender distribution: Slight male predominance (M:F = 1.5:1)

  • Course: Variable—some patients have monophasic illness, others have relapsing-remitting or progressive pattern

Pathophysiology

Immune-Mediated Demyelination

CIDP is characterized by immune-mediated damage to the myelin sheath of peripheral nerves. The exact trigger is unknown, but the disease involves both cellular and humoral immune responses:

  1. T-cell mediated damage: Autoreactive T-cells target myelin proteins

  2. Macrophage-mediated demyelination: Activated macrophages attack myelin

  3. Antibody-mediated injury: Autoantibodies target myelin proteins and lipids

Associated Conditions

In some cases, CIDP may be associated with other conditions:

  • Diabetes mellitus

  • HIV infection

  • Monoclonal gammopathy (MGUS)

  • Lymphoma

  • Systemic lupus erythematosus

Clinical Features

Symptoms

  • Progressive weakness: Arms and legs, typically symmetric

  • Sensory loss: Numbness, particularly in hands and feet

  • Loss of deep tendon reflexes: Diminished or absent

  • Difficulty walking: Gait disturbance

  • Fatigue: Generalized fatigue

  • Pain: Particularly in back and legs

  • Balance problems: Due to sensory and motor impairment

Clinical Variants

  • Typical CIDP: Classic presentation with symmetric proximal and distal weakness

  • Atypical CIDP: Includes pure sensory, pure motor, or focal variants

  • MADSAM: Multifocal acquired demyelinating sensory and motor neuropathy (Lewis-Sumner syndrome)

Diagnosis

Clinical Criteria

Diagnosis is based on a combination of:

  • Clinical presentation: Progressive,relatively symmetric motor and sensory neuropathy

  • Nerve conduction studies: Showing demyelination (temporal dispersion, conduction block, slowed velocities)

  • Cerebrospinal fluid analysis: Elevated protein with normal cell count (albuminocytologic dissociation)

  • Nerve biopsy: May be performed in atypical cases

Diagnostic Workup

  1. Neurological examination: Assess strength, sensation, reflexes

  2. Nerve conduction studies/EMG: Confirm demyelination

  3. Lumbar puncture: CSF protein elevation

  4. Blood tests: Rule out associated conditions

  5. Nerve biopsy: In selected cases

Differential Diagnosis

CIDP must be distinguished from:

  • Guillain-Barré syndrome (acute inflammatory demyelinating polyradiculoneuropathy)

  • Multifocal motor neuropathy

  • Charcot-Marie-Tooth Disease (hereditary)

  • Diabetic neuropathy

  • Vasculitic neuropathy

Treatment

First-Line Therapies

  1. Corticosteroids (prednisone): Effective but significant long-term side effects

  2. Intravenous immunoglobulin (IVIG): Often preferred due to rapid onset and favorable side effect profile

  3. Plasma exchange (plasmapheresis): Used in severe or refractory cases

Second-Line and Adjunctive Therapies

  • Immunosuppressive agents: Azathioprine, mycophenolate, cyclophosphamide, rituximab

  • Subcutaneous immunoglobulin: Alternative for maintenance therapy

Treatment Response

  • IVIG: Response in 50-70% of patients; effects typically last weeks to months

  • Corticosteroids: Effective in many patients; require maintenance therapy

  • Plasma exchange: Particularly useful for acute exacerbations

Prognosis

The prognosis for CIDP varies significantly among patients:

  • Monophasic course: Some individuals experience complete recovery

  • Relapsing-remitting pattern: Periodic treatments needed

  • Progressive course: Gradual worsening despite treatment

Factors associated with better outcomes:

  • Early diagnosis and treatment

  • Fewer relapses

  • Younger age at onset

  • Absence of underlying disease

Research Directions

Current research focuses on:

  • Biomarkers for treatment response: Identifying predictors of therapeutic benefit

  • Underlying autoimmune mechanisms: Understanding the exact pathophysiology

  • Novel therapies: Investigating targeted immunosuppressive agents

  • Stem cell therapy: Exploring regenerative approaches

  • Gene therapy: Potential future treatments

Pathway & Interaction Diagram

Interactive diagram showing cidp’s key relationships in the SciDEX knowledge graph (7 connections shown).

flowchart TD
    cidp["cidp"]
    Autoimmune["Autoimmune"]
    Neuropathy["Neuropathy"]
    FCGRT("FCGRT")
    disease["disease"]

    cidp -->|"regulates"| Autoimmune
    cidp -->|"regulates"| Neuropathy
    cidp -->|"regulates"| FCGRT
    cidp -->|"causes"| Autoimmune
    cidp -->|"causes"| Neuropathy
    cidp -->|"causes"| disease
    cidp -->|"interacts with"| Neuropathy

    style cidp fill:#1a237e,stroke:#4fc3f7,stroke-width:3px,color:#fff

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