Clinical Complications

Fibromyalgia: Complications & Clinical Risks

Fibromyalgia is a chronic condition causing widespread musculoskeletal pain, fatigue, sleep disturbance, and cognitive difficulties ("fibro fog"). Central sensitization is the underlying mechanism; multimodal treatment includes exercise, cognitive behavioral therapy, and medications.

Overview of Major Complications

Musculoskeletal and autoimmune conditions generate complications through chronic inflammation, joint and organ destruction, immunosuppressive treatment consequences, and the physical disability resulting from progressive disease. Rheumatoid arthritis causes joint erosion and extra-articular organ involvement; systemic lupus erythematosus attacks kidneys, CNS, and vasculature; osteoporosis leads to fragility fractures. The bidirectional cardiovascular risk amplification from chronic inflammation creates a major source of premature mortality across this disease group.

Early Complications

  • Acute joint flare — severe pain, swelling, and functional loss requiring urgent anti-inflammatory treatment
  • Crystal arthropathy — gout or pseudogout precipitated by illness, surgery, or diuretics
  • Corticosteroid-induced adrenal suppression — dose reduction without tapering causes adrenal crisis
  • Septic arthritis — immunosuppressed patients at high risk; joint damage occurs within hours if untreated
  • Tendon rupture — in rheumatoid arthritis; extensor tendon involvement causes sudden loss of hand function
  • Deep vein thrombosis — antiphospholipid syndrome increases thrombosis risk 10-fold

Long-Term Complications

  • Joint destruction and deformity — irreversible in untreated RA; requires surgical intervention
  • Osteoporosis and fragility fractures — from chronic inflammation and corticosteroid use; vertebral fractures
  • Cardiovascular disease — RA, SLE, and psoriatic arthritis carry 2× higher MI and stroke risk
  • Lupus nephritis — kidney failure in 20–30% of SLE patients without adequate immunosuppression
  • Pulmonary fibrosis — complicates RA, myositis, scleroderma, and Sjögren's syndrome
  • Malignancy — increased lymphoma risk in RA, Sjögren's, and from immunosuppressive therapy
  • Drug toxicity — methotrexate hepatotoxicity, hydroxychloroquine retinopathy, leflunomide teratogenicity
  • Amyloidosis — secondary AA amyloidosis from chronic inflammation; renal involvement

Emergency Complications

Immediate clinical action required

  • Cervical spine instability — atlantoaxial subluxation in advanced RA; cord compression risk from minor trauma
  • Macrophage activation syndrome — life-threatening cytokine storm in SLE or systemic JIA
  • Pulmonary haemorrhage in vasculitis — haemoptysis with renal failure (Goodpasture, ANCA vasculitis)
  • Acute antiphospholipid syndrome — catastrophic multi-organ thrombosis; anticoagulation and immunosuppression
  • Septic arthritis — joint aspiration and IV antibiotics within hours to prevent destruction

What Increases Complication Risk

  • High disease activity — elevated CRP, ESR, active synovitis drive erosion and organ damage
  • Non-adherence to DMARD therapy — leads to progressive joint and organ damage
  • Corticosteroid dependence — contributes to osteoporosis, diabetes, infection, and cardiovascular risk
  • Smoking — worsens RA, psoriatic arthritis, and cardiovascular risk; impairs DMARD response
  • Obesity — promotes inflammation, reduces DMARD efficacy, and increases joint load
  • Delayed specialist referral — early window of opportunity for joint-sparing therapy is missed

What Reduces Complication Risk

  • Treat-to-target strategy — achieving DAS28 remission or low disease activity prevents erosion
  • Early DMARD initiation — methotrexate or biologic within 3 months of diagnosis reduces damage
  • Calcium and vitamin D supplementation — reduces fracture risk in corticosteroid-treated patients
  • Cardiovascular risk management — statins, antihypertensives, smoking cessation
  • Bone protection therapy (bisphosphonates) — in chronic corticosteroid users
  • Infection prophylaxis — vaccinations, PCP prophylaxis in heavily immunosuppressed patients

When Urgent Reassessment is Needed

The following signs may indicate a new or worsening complication requiring prompt clinical evaluation:

  • Hot, swollen monoarthritis with fever — septic arthritis until proven otherwise; urgent joint aspiration
  • New neurological symptoms in known RA — cervical myelopathy; urgent MRI cervical spine
  • Haemoptysis with haematuria in vasculitis patient — pulmonary-renal syndrome; immediate assessment
  • Fever with cytopaenia in inflammatory arthritis — macrophage activation syndrome or infection
  • Sudden visual loss in polymyalgia rheumatica — giant cell arteritis with AION; immediate high-dose steroids
  • Acute dyspnoea in autoimmune disease — exclude pulmonary haemorrhage, ILD exacerbation, PE

Special Populations

Elderly: osteoporosis and falls risk amplified by steroid use; cautious biologic dosing in frail patients
Pregnancy: RA often improves in pregnancy but flares post-partum; many DMARDs are teratogenic and must be stopped pre-conception
Children with JIA: eye disease (uveitis) often asymptomatic; requires regular slit-lamp surveillance
Males with ankylosing spondylitis: delayed diagnosis is common; axial involvement with significant functional limitation

Related Clinical Pages

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Evidence-based treatment pathway, medications, and escalation criteria

Prognosis & Outlook

Long-term clinical outlook, improving and worsening outcome factors

Differential Diagnosis

Conditions that mimic Fibromyalgia — distinguishing features & tests

Evidence & Guidelines

Clinical trials, guideline strength, and treatment evidence

Fibromyalgia Overview

Symptoms, causes, and general condition overview

Similar Conditions With Different Risk Profiles

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Medical References

Content on this page is informed by evidence-based clinical sources including: