Idiopathic Pulmonary Fibrosis (IPF)
NICE Clinical guideline [CG163] Idiopathic pulmonary fibrosis in adults: diagnosis and management. Last updated: May 2017.
Background Information
Definitions
Interstitial lung disease (ILD): group of lung disorders characterised by inflammation and/or fibrosis of the lung parenchyma – specifically affecting the interstitium – leading to impaired gas exchange and progressive dyspnoea. [Ref]
Idiopathic pulmonary fibrosis (IPF): most common type of ILD, that is of unknown cause (idiopathic), diagnosed by characteristic clinical, radiologic and/or histopathologic features, and by the exclusion of secondary causes . [Ref]
Usual interstitial pneumonia (UIP) pattern: hallmark radiologic and histopathologic pattern required for the diagnosis of IPF. Radiologically, this includes subpleural & basal lung zone predominant honeycombing (clustered cystic airspaces), traction bronchiectasis and ground-glass opacities. The histological pattern includes a patchy, heterogenous fibrosis of the interstitium. [Ref]
Epidemiology
IPF is the most common type of ILD → global prevalence of ~18 per 100,000 [Ref]
Mean age at diagnosis → ~67-72 years (rare <50 yrs) [Ref]
Sex → Male predominant (2-3:1 M:F ratio) [Ref]
Risk Factors
Although the cause of IPF is unknown, there are several risk factors:
- ↑ Age
- Male sex
- Environmental and occupational exposures: [Ref] ↑ risk with metal dust, wood dust, pesticides, farrming/agricultural work, asbestos exposure
- Family History
- Conditions (may contribute to disease risk / progression)
- GORD
- OSA
- Lung disease → emphysema / pulmonary hypertension
Clinical Features
IPF presents with typical interstitial lung disease features:
Symptoms
- Onset → Insidious (over months – years)
- Progressive dyspnoea
- Initially → extertional
- Progresses to dyspnoea at rest
- Progressive nonproductive cough
- Nonspecific → weight loss, fatigue
Signs / Examination findings
- Inspection → digital clubbing (30-50% of cases), cyanosis (advanced disease)
- Chest auscultation
- Fine-inspiratory crackles (velcro-like rales) → indication of pulmonary fibrosis
- Distribution → bibasal
- Loud inspiratory wheeze (advanced)
- Fine-inspiratory crackles (velcro-like rales) → indication of pulmonary fibrosis
Being an ILD, IPF manifests similar to other types of ILD; however, IPF is distinguished by its older age at onset, male predominance and lack of identifiable cause.
Complications
- Complications overlap between different types of ILD and include: [Ref]
- Acute exacerbations
- Progressive hypoxaemic (type 1) respiratory failure → leading cause of death
- Pulmonary hypertension → Cor pulmonale
- ↑ risk of lung cancer
Prognosis
- Poor prognosis overall (worst of all ILDs)→ median survival of 3-4 years from diagnosis [Ref]
- Interventions known to improve life expectancy [Ref]
- Antifibrotic therapy (pirfenidone, nintedanib)
- Lung transplantation
Diagnosis Guidelines
1st Line Tests
Perform ALL the following tests if IPF is suspected.
| Test | Purpose | Typical findings in IPF |
|---|---|---|
| Lung function test – spirometry | To distinguish between obstructive vs restrictive lung disease | IPF causes a restrictive pattern:
|
| Lung function test – gas transfer (DLCO) | Assess gas exchange efficiency | ↓ DLCO is typical of fibrosis |
| Chest X-ray | Non-specific findings:
|
|
| HRCT thorax | Gold standard imaging | Usual interstitial pneumonia pattern:
Changes are predominantly in basal and peripheral areas |
Further Tests (Specialist)
Specialist tests if diagnosis remains uncertain after 1st line tests:
- Bronchoalveolar lavage
- Useful to exclude hypersensitivity pneumonitis
- Trans-bronchial biopsy (via bronchoscopy)
- Surgical lung biopsy (usually via VATS) – most definitive testing
- Histology: usual interstitial pneumonia pattern
Management Guidelines
General Conservative Management
- Smoking cessation advice
- Offer pulmonary rehabilitation if appropriate
- Oxygen therapy as needed
- Ventilatory support if respiratory failure develops
Pharmacological Management
Symptomatic Management
Management of cough:
- Treat other causes of cough (e.g. GORD, post-nasal drip)
- Opioids, if the cough is debilitating
- Thalidomide – to be considered by a specialist if the cough is intractable
It is important to optimise treatment of GORD in IPF as it is common in IPF patients and can cause microaspiration of gastric contents into the lungs.
Disease-Modifying
Recommended treatment (FVC 50-80% of predicted)
- Nintedanib (small molecule tyrosine kinase inhibitor)
- Pirfenidone (anti-fibrotic and anti-inflammatory agent – via inhibition of TGF-β1)
Oral N‑acetylcysteine is used for managing IPF, but its benefits are uncertain
The following are NOT recommended to modify disease progression in IPF:
- Immunosuppressant (prednisolone, mycophenolate mofetil, azathioprine)
- Co-trimoxazole
- Pulmonary vasodilators
- Endothelin receptor antagonist (bosentan, ambrisentan)
- Sildenafil
- Warfarin
Lung Transplantation
All patients with IPF should be considered for lung transplantation if there are no contraindications
- Discussion and referral should take place 3-6 months after diagnosis or sooner
Most patients with IPF will eventually require lung transplantation if they are eligible, as IPF is a progressive, fatal disease with a median survival of ~3 years after diagnosis without transplant.
Lung transplantation offers a substantial improvement in survival (5-year post-transplant survival is ~50-55%).