IPF GAP Index Calculator- Free IPF Staging and Mortality Prediction Tool

IPF GAP Index Calculator – Free IPF Staging and Mortality Prediction Tool | Super-Calculator.com

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Important Medical Disclaimer

This calculator is provided for informational and educational purposes only. It is not intended to replace professional medical advice, diagnosis, or treatment. Always consult with a qualified healthcare professional before making any medical decisions. The results from this calculator should be used as a reference guide only and not as the sole basis for clinical decisions.

IPF GAP Index Calculator

Calculate the GAP (Gender, Age, Physiology) score for idiopathic pulmonary fibrosis staging. Enter gender, age, FVC percent predicted, and DLCO percent predicted to receive a GAP stage classification (I, II, or III) with 1-year, 2-year, and 3-year mortality estimates based on the Ley 2012 validation cohort. Supports clinical decision-making for antifibrotic therapy, lung transplant referral, and palliative care integration in IPF management.

Patient Gender

Patient Age (years)65

FVC % Predicted

DLCO % Predicted

GAP Total Score

out of 8 possible points

Stage I

0 – Stage IStage II – 4Stage III – 68

1-Year Mortality

5.6%

2-Year Mortality

10.9%

3-Year Mortality

16.3%

GAP Points Breakdown

Gender

Age

FVC

DLCO

Stage I IPF – mild physiological impairment. Initiate antifibrotic therapy (pirfenidone or nintedanib). Monitor with 3 to 6 monthly lung function. Assess lung transplant suitability early. Pulmonary rehabilitation recommended.

GAP Stage	Score Range	1-Year Mortality	2-Year Mortality	3-Year Mortality
Stage I	0 to 3	5.6%	10.9%	16.3%
Stage II	4 to 5	16.2%	29.9%	42.1%
Stage III	6 to 8	39.2%	62.1%	76.8%

Source: Ley B, et al. A multidimensional index and staging system for idiopathic pulmonary fibrosis. Ann Intern Med. 2012;156(10):684-691. Mortality figures represent all-cause mortality from the validation cohort (n=330) in the pre-antifibrotic era. Treated patients may have lower mortality.

GAP Variable	Threshold / Category	Points Assigned
Gender – Female	Female sex	0
Gender – Male	Male sex	1
Age – Under 60	Age less than 60 years	0
Age – 60 to 65	Age 60 to 65 years inclusive	1
Age – Over 65	Age greater than 65 years	2
FVC – Preserved	FVC percent predicted over 75%	0
FVC – Mild reduction	FVC percent predicted 50% to 75%	1
FVC – Severe reduction	FVC percent predicted under 50%	2
FVC – Unable	Unable to perform spirometry	3
DLCO – Preserved	DLCO percent predicted over 55%	0
DLCO – Mild reduction	DLCO percent predicted 36% to 55%	1
DLCO – Severe reduction	DLCO percent predicted under 35%	2
DLCO – Unable	Unable to perform DLCO testing	3
Maximum GAP Score		8 points

Note: If both FVC and DLCO are “unable to perform,” the total is capped at 8 per the original Ley 2012 paper, which states the score range is 0 to 8. This edge case (male, over 65, both tests unable) would otherwise yield 9 points arithmetically.

GAP Stage	Clinical Priority	Recommended Action
Stage I (0 – 3)	Establish care framework	Initiate antifibrotic therapy. Lung transplant referral assessment. 6-monthly lung function. Pulmonary rehabilitation. Advance care planning introduction.
Stage II (4 – 5)	Escalate monitoring and transplant	Optimise antifibrotic therapy. Expedited lung transplant evaluation. 3-monthly lung function. Supplemental oxygen assessment. 6MWT. Increase palliative care involvement.
Stage III (6 – 8)	Urgent transplant and end-of-life planning	Urgent transplant listing if candidate. Intensive symptom management. Early hospice/palliative care integration. Document advance care directives. Monthly clinical contact. Opioids for dyspnoea if needed.

Clinical guidance is general and should be individualised. All IPF patients should receive antifibrotic therapy (pirfenidone or nintedanib) regardless of GAP stage per current international guidelines.

About This IPF GAP Index Calculator

The IPF GAP Index Calculator is designed for pulmonologists, respirologists, general physicians, and advanced practice providers managing patients with confirmed idiopathic pulmonary fibrosis. It calculates the GAP score from Gender, Age, FVC percent predicted, and DLCO percent predicted, classifying patients into Stage I, Stage II, or Stage III with 1-year, 2-year, and 3-year mortality estimates from the Ley 2012 validation cohort.

The calculator implements the full GAP algorithm as published by Ley B et al. in the Annals of Internal Medicine (2012): gender (0 to 1 point), age with two cut-points (0 to 2 points), FVC percent predicted with three thresholds plus an unable category (0 to 3 points), and DLCO percent predicted equivalently (0 to 3 points). Total is capped at 8 per the original paper. Stage boundaries are 0 to 3 for Stage I, 4 to 5 for Stage II, and 6 to 8 for Stage III.

The Mortality Reference tab shows all-cause mortality estimates across stages, the Scoring Criteria tab provides the full variable breakdown with the score cap explanation, and the Clinical Guidance tab outlines stage-specific management priorities. Results should complement full clinical assessment including HRCT, exercise testing, and multidisciplinary team discussion.

Important Medical Disclaimer

IPF GAP Index Calculator - Complete Guide to Staging and Mortality Prediction in Idiopathic Pulmonary Fibrosis

Idiopathic pulmonary fibrosis (IPF) is a chronic, progressive, and ultimately fatal fibrosing interstitial lung disease of unknown cause. It primarily affects older adults and carries a median survival of only 2 to 3 years from diagnosis. One of the most significant challenges clinicians face is predicting disease trajectory - knowing which patients are at highest short-term risk allows for timely decisions around antifibrotic therapy intensification, referral for lung transplantation, and palliative care planning.

The GAP Index was developed precisely to address this challenge. GAP stands for Gender, Age, and Physiology - the three domains from which it derives its predictive power. Published in 2012 by Ley and colleagues, the model provides a simple, clinically applicable scoring system that stratifies IPF patients into three stages associated with meaningfully different one-year, two-year, and three-year mortality risks. Unlike complex biomarker panels or molecular tests, the GAP Index requires only standard clinical information routinely available at most hospital appointments.

This calculator implements the full GAP Index scoring algorithm and provides stage-based mortality estimates, clinical guidance, and a reference framework drawn from the original validation dataset. It is intended as a clinical decision-support tool for pulmonologists, respirologists, general physicians, and advanced practice providers managing patients with confirmed IPF.

GAP Index Scoring Formula

GAP Points = Gender Points + Age Points + FVC Points + DLCO Points

Gender: Female = 0, Male = 1
Age: Under 60 = 0; 60 to 65 = 1; Over 65 = 2
FVC % predicted: Over 75% = 0; 50% to 75% = 1; Under 50% = 2; Unable to perform = 3
DLCO % predicted: Over 55% = 0; 36% to 55% = 1; Under 35% = 2; Unable to perform = 3
Maximum possible score: 8 points

What Is Idiopathic Pulmonary Fibrosis?

IPF is a specific form of chronic fibrosing interstitial pneumonia of unknown aetiology. Histologically, it is characterised by a usual interstitial pneumonia (UIP) pattern - a heterogeneous mix of fibrosis, honeycombing, and relatively normal lung tissue. The disease predominantly affects individuals over 60 years of age, and men are affected approximately twice as often as women, a demographic pattern that is directly reflected in the GAP Index scoring system.

The clinical presentation is typically insidious. Most patients report months to years of progressive exertional dyspnoea and a dry, persistent cough. Physical examination frequently reveals fine bibasilar inspiratory crackles (described as "velcro crackles") and, in advanced disease, clubbing of the fingers. Pulmonary function testing demonstrates a restrictive pattern with reduced total lung capacity and, critically, a disproportionate reduction in diffusing capacity (DLCO) relative to forced vital capacity (FVC). This DLCO-FVC dissociation reflects the characteristic vascular obliteration that accompanies the fibrotic process.

High-resolution computed tomography (HRCT) plays a central role in diagnosis. A typical UIP pattern on HRCT - defined by bilateral, peripheral, basal-predominant reticulation with honeycombing, with or without peripheral traction bronchiectasis - is considered diagnostic in the appropriate clinical context and may obviate the need for surgical lung biopsy under current international guidelines. When HRCT findings are indeterminate, multidisciplinary team (MDT) discussion remains the gold standard for diagnosis.

Background and Development of the GAP Index

Prior to the GAP Index, several prognostic scoring systems existed for IPF, but most were complex, required variables not routinely collected, or had been validated only in limited populations. The GAP model was developed by Ley et al. using a derivation cohort of 228 patients with IPF and validated in a separate cohort of 330 patients. The derivation cohort came from the University of California San Francisco interstitial lung disease program, while the validation cohort drew from three independent academic centres.

The investigators sought to identify a parsimonious model - one using the fewest variables necessary to achieve clinically useful mortality prediction. After evaluating a broad range of demographic, spirometric, diffusion, and radiographic variables, gender, age, FVC, and DLCO emerged as the most consistently predictive independent factors. Importantly, the model was designed to be applicable even when patients could not perform one of the physiological tests - a provision reflected in the "unable to perform" category for both FVC and DLCO, which carries the highest point value for each domain.

The GAP Index was subsequently validated in multiple independent cohorts worldwide, including populations from Europe, Asia, and South America, demonstrating reasonable cross-population generalisability despite having been derived primarily in North American patients. However, clinicians should be aware that calibration may differ in populations with high rates of combined emphysema-fibrosis or in those receiving antifibrotic therapy, which was not widely available at the time of the original study.

Key Point: Clinical Derivation Context

The GAP Index was derived before pirfenidone and nintedanib were approved for IPF. Both antifibrotic agents reduce the annual rate of FVC decline by approximately 50%. While they do not eliminate disease progression, they meaningfully alter the natural history of IPF. The original GAP mortality estimates should therefore be interpreted as representing the pre-antifibrotic era, and may overestimate mortality in treated patients.

Understanding Each GAP Variable

Gender (0 to 1 point): Male sex is assigned one point, reflecting the consistently worse prognosis observed in men with IPF across multiple studies. The biological basis for this sex-based difference is not fully established, but proposed mechanisms include differences in telomere biology (IPF is associated with telomerase mutations more common in men), hormonal effects on fibrosis pathways, and differences in smoking history patterns. Female patients with IPF tend to have a more favourable prognosis independent of disease severity markers.

Age (0 to 2 points): Age contributes meaningfully to IPF prognosis beyond its correlation with physiological impairment. Older patients tolerate exacerbations less well, are less suitable for lung transplantation, and may have limited physiological reserve for recovery. The GAP model uses two cut-points: patients under 60 receive 0 points, those 60 to 65 receive 1 point, and those over 65 receive 2 points. In clinical practice, age is particularly relevant when discussing lung transplant candidacy, as most programmes have upper age thresholds of 65 to 70 years.

FVC % Predicted (0 to 3 points): Forced vital capacity, expressed as a percentage of the age- and sex-matched predicted value, is the most commonly used physiological marker in IPF clinical practice and trials. It reflects the total extent of restrictive lung disease. In the GAP model, an FVC greater than 75% predicted attracts 0 points, 50% to 75% attracts 1 point, and below 50% attracts 2 points. Patients unable to perform spirometry - typically due to severe dyspnoea or significant comorbidities - receive 3 points, reflecting the clinical severity implied by an inability to complete the test.

DLCO % Predicted (0 to 3 points): The diffusing capacity for carbon monoxide (DLCO or TLCO) measures the efficiency of gas transfer across the alveolar-capillary membrane. In IPF, DLCO is often disproportionately reduced compared with FVC, reflecting both loss of alveolar surface area and vascular obliteration from fibrosis. DLCO is particularly sensitive to disease progression and is considered by many experts to be the most prognostically informative single lung function variable in IPF. The GAP model assigns 0 points for DLCO over 55% predicted, 1 point for 36% to 55%, 2 points for under 35%, and 3 points for inability to perform the test.

GAP Staging and Mortality Estimates

Total GAP scores are converted to three stages that communicate prognosis in clinically meaningful terms. Each stage carries specific one-year, two-year, and three-year all-cause mortality estimates derived from the original validation cohort.

GAP Stage Classification

Stage I: 0 to 3 points | Stage II: 4 to 5 points | Stage III: 6 to 8 points

Stage I (0 - 3 points): 1-year mortality 5.6%, 2-year 10.9%, 3-year 16.3%
Stage II (4 - 5 points): 1-year mortality 16.2%, 2-year 29.9%, 3-year 42.1%
Stage III (6 - 8 points): 1-year mortality 39.2%, 2-year 62.1%, 3-year 76.8%
Source: Ley et al., American Journal of Respiratory and Critical Care Medicine, 2012

Stage I patients represent those with the mildest physiological impairment. Their relatively preserved FVC and DLCO values, combined with younger age or female sex, place them in the lowest risk category. However, it is important not to be falsely reassured by a Stage I classification - even at this stage, one-year mortality approaches 6%, and the progressive nature of IPF means that all patients require regular monitoring and disease-modifying therapy discussions.

Stage II represents a clinically important inflection point. With 1-year mortality exceeding 16%, these patients carry a risk comparable to many established cardiovascular risk thresholds that routinely prompt intervention. Stage II patients are typically experiencing meaningful symptoms, may require supplemental oxygen on exertion, and should be actively evaluated for lung transplant candidacy if not already listed. This stage also represents the population in which escalation of antifibrotic therapy or enrolment in clinical trials may be most appropriate.

Stage III patients have the most advanced physiological impairment and the highest short-term mortality. With nearly 40% of patients dying within one year and over 60% within two years, Stage III IPF carries a prognosis worse than many malignancies. Clinical management priorities shift significantly at this stage - urgent transplant evaluation (where appropriate), advance care planning, and early palliative care integration become essential components of the management plan.

How the GAP Index Is Used in Clinical Practice

The GAP Index serves several practical functions in the day-to-day management of IPF. At the time of initial diagnosis, it provides a baseline prognostic classification that can inform patient counselling, shared decision-making, and initial treatment planning. Many clinicians use GAP staging to frame initial conversations about prognosis with patients and families, translating the abstract notion of "a serious progressive disease" into concrete probability estimates.

Longitudinally, the GAP Index can be recalculated at each clinical review to track disease progression. A patient who begins at Stage I and progresses to Stage II over 12 to 18 months has demonstrated meaningful deterioration, even if individual test results remain within laboratory reference ranges. This dynamic use of the GAP Index - tracking stage changes over time rather than relying on any single calculation - may be more clinically informative than any single cross-sectional score.

The GAP Index is also widely used in research contexts. Clinical trial entry criteria, patient stratification in observational studies, and post-hoc analyses of treatment effects frequently reference GAP stages as a means of describing baseline disease severity. This widespread research use means that GAP-based language is well understood across the IPF clinical and research community globally.

Key Point: Lung Transplant Timing

International Society for Heart and Lung Transplantation (ISHLT) guidelines recommend listing IPF patients for transplantation when UIP pattern is confirmed and any of the following are present: DLCO below 40% predicted, a 10% or greater decline in FVC over six months, desaturation below 88% during a six-minute walk test, or honeycombing on HRCT with a fibrosis score above 2. These criteria overlap considerably with the physiological thresholds that place patients in GAP Stage II to III, highlighting the clinical importance of GAP staging for transplant referral decisions.

GAP Index vs. Other IPF Prognostic Models

Several alternative prognostic models for IPF have been developed, each with distinct methodological approaches and variable requirements. Understanding how the GAP Index relates to these alternatives helps clinicians select the most appropriate tool for their clinical context.

The ILD-GAP Index extends the original GAP model to all fibrotic interstitial lung diseases, not just IPF. It includes an additional variable for ILD diagnosis (IPF carries more points than other ILD subtypes), making it applicable across connective tissue disease-associated ILD, hypersensitivity pneumonitis, and other fibrotic conditions. For pure IPF cohorts, the original GAP Index and the ILD-GAP Index perform similarly.

The TORVAN model incorporates radiological extent of fibrosis on HRCT in addition to physiological variables, potentially capturing information not reflected in FVC and DLCO alone. However, it requires semi-quantitative HRCT scoring, limiting its ease of use in routine clinical settings without dedicated imaging analysis.

Serum biomarkers, including MMP-7, KL-6, SP-A, SP-D, CCL-18, and YKL-40, have each demonstrated prognostic utility in IPF cohorts, but none have achieved widespread clinical adoption due to limited availability, lack of standardisation, and unclear incremental value over physiological variables. The six-minute walk test distance and desaturation during walking provide additional prognostic information that is not captured by the GAP Index, and some expert centres incorporate these into composite clinical assessments.

The composite physiological index (CPI) integrates FVC, FEV1, and DLCO into a single index specifically designed for IPF, mathematically removing the confounding contribution of emphysema. It provides equivalent or superior prognostic discrimination to DLCO alone in patients with combined emphysema-fibrosis, a clinically important subgroup where standard FVC and DLCO values may be spuriously preserved. For patients with significant smoking history or known emphysema, CPI may be a preferred physiological assessment tool, though it is not incorporated into the GAP Index framework.

Limitations of the GAP Index

Despite its broad validation and clinical utility, the GAP Index has several important limitations that clinicians should bear in mind. The model was derived in a single-centre North American cohort and, while it has been externally validated, its mortality estimates may not be perfectly calibrated across all populations and healthcare settings. Survival rates following IPF diagnosis vary across different countries and healthcare systems, partly due to differences in access to antifibrotic therapy, lung transplantation, and supportive care resources.

The GAP Index does not incorporate information from HRCT imaging, which provides important prognostic information independent of physiology. Patients with extensive honeycombing or a high fibrotic burden on HRCT may have a worse prognosis than their physiological GAP score alone would suggest. Similarly, the presence of acute exacerbations of IPF - sudden, life-threatening episodes of accelerated decline - is not captured by the GAP Index, yet these events profoundly affect individual patient prognosis.

The model also predates modern antifibrotic therapy. Pirfenidone and nintedanib both demonstrably slow FVC decline, which is a major driver of GAP score progression over time. In clinical cohorts treated with antifibrotic agents, the transition from Stage I to Stage II or Stage III may be delayed compared with historical cohorts, and absolute mortality figures may be somewhat lower than those published with the original model. Clinicians should use the GAP Index as one tool among several, rather than as the sole determinant of clinical decisions.

Key Point: Acute Exacerbations

Acute exacerbations of IPF (AE-IPF) are defined as acute, clinically significant respiratory deterioration characterised by new bilateral radiographic opacities superimposed on a UIP background, in the absence of infection or other identifiable cause. AE-IPF carries a hospital mortality of 50% or greater and is the most common immediate cause of death in IPF. The GAP Index does not predict exacerbation risk. Patients at any GAP stage can experience AE-IPF, though those with more advanced disease appear to be at higher absolute risk.

Antifibrotic Therapy and the GAP Index

Pirfenidone and nintedanib are the two approved antifibrotic agents for IPF. Both reduce the annual rate of FVC decline by approximately 50% compared with placebo - approximately 100 mL per year versus 200 mL per year in trials. This slowing of FVC decline translates into preservation of GAP scores over time; treated patients are less likely to progress from Stage I to Stage II, or Stage II to Stage III, within a given follow-up period.

Neither agent has been definitively shown to reduce all-cause mortality in individual trials, though meta-analyses and pooled analyses suggest a mortality benefit. Current international guidelines recommend initiating antifibrotic therapy in virtually all patients with confirmed IPF, regardless of initial disease severity - including those with mild disease (Stage I GAP). The rationale is that preserving lung function while it is relatively intact confers the greatest absolute benefit, and all patients with IPF are at risk of disease progression.

There is no strong evidence that one antifibrotic agent is superior to the other in terms of efficacy. Choice between pirfenidone and nintedanib is typically guided by side-effect profiles, comorbidities, patient preference, and cost. Nintedanib is associated with diarrhoea and hepatic transaminase elevation; pirfenidone is associated with photosensitivity, nausea, and fatigue. Both are teratogenic and should not be used in pregnancy.

Lung Transplantation in IPF

Lung transplantation remains the only treatment with demonstrated survival benefit in IPF, with median survival post-transplant of approximately five years. IPF is the most common indication for lung transplantation globally, accounting for approximately 30% of transplant procedures in many registries. The decision to refer for transplant evaluation should ideally occur early in the disease course, as waitlist times are substantial and patients must remain medically suitable for surgery throughout the waiting period.

GAP staging provides useful guidance for transplant referral timing. Most expert consensus suggests referral at the time of confirmed UIP diagnosis, regardless of GAP stage, given the unpredictable progression of IPF. However, patients in GAP Stage II or Stage III have more urgent need for expedited transplant evaluation, particularly given the high mortality risk in Stage III patients, where the one-year mortality approaches 40%.

Single-lung transplantation has historically been more common in IPF due to donor organ availability, though bilateral lung transplantation provides superior survival and is preferred at many centres. Contraindications to transplantation include active malignancy, significant extrapulmonary organ dysfunction, severe osteoporosis, ongoing substance use, and inability to comply with complex post-transplant regimens. Age over 65 to 70 years is a relative contraindication at most centres.

Palliative Care Integration in Advanced IPF

Palliative care in IPF is complementary to, not instead of, disease-modifying treatment. Early integration of palliative care - defined as care focused on quality of life, symptom management, and goal-setting rather than life prolongation - has been associated with improved patient outcomes in advanced lung disease. Dyspnoea is the predominant symptom in IPF and can be profoundly disabling; oral or systemic opioids are effective in reducing the subjective experience of breathlessness in advanced disease and should not be withheld out of concern for respiratory depression in appropriately selected patients.

Advance care planning conversations should ideally occur before a crisis point. Discussions about intubation, mechanical ventilation, cardiopulmonary resuscitation, and the role of non-invasive ventilation should be had while patients have full decision-making capacity and adequate time for reflection. GAP Stage III represents a natural prompt for initiating these conversations, given the high probability of significant deterioration within one to two years.

Supplemental oxygen is indicated for IPF patients with resting hypoxaemia and may provide symptomatic benefit for those with exertional desaturation. Pulmonary rehabilitation has been shown to improve exercise capacity and quality of life in IPF, though it does not alter the underlying disease course. Cough management, anxiety treatment, and nutritional support are additional domains where specialised symptom-focused care can meaningfully improve patient wellbeing.

Key Point: Oxygen Therapy Threshold

Supplemental oxygen should be prescribed for IPF patients with resting oxygen saturation of 88% or below on room air, in accordance with standard chronic respiratory disease guidelines. Ambulatory oxygen may benefit patients who desaturate below 88% during exertion even if resting saturations are preserved. Regular assessment of oxygen requirements should be incorporated into follow-up appointments, particularly as disease progresses through GAP stages.

Global Application and Population Considerations

The GAP Index has been studied and applied in diverse patient populations across North America, Europe, Asia, Australia, and South America. The model demonstrates good discriminatory performance across these settings, though absolute mortality rates may differ due to variation in healthcare infrastructure, access to antifibrotic therapy and transplantation, and population-level differences in disease presentation.

Several validation studies have examined GAP performance in specific population groups. Asian cohorts, including those from Japan and South Korea - where IPF is common and well-studied - have generally shown comparable prognostic discrimination to Western populations. Some studies in predominantly East Asian cohorts have noted that mean ages at diagnosis may be somewhat lower than in Western populations, which slightly affects the age-related point distribution but does not substantially alter model performance.

In populations with high rates of combined pulmonary fibrosis and emphysema (CPFE) - a pattern common in older male smokers - standard FVC values may be relatively preserved despite extensive radiological disease, as emphysema and fibrosis partially counteract their respective effects on lung volumes. In these patients, DLCO is typically severely reduced, which is captured by the GAP Index. However, FVC-based staging may underestimate disease severity in CPFE patients, and clinicians should be aware of this potential limitation when applying GAP scores in populations with high rates of smoking-related lung disease.

Monitoring Disease Progression with Serial GAP Calculations

Serial measurement of FVC and DLCO forms the cornerstone of IPF disease monitoring. Major international guidelines recommend lung function testing every three to six months in patients with stable IPF and after any clinical deterioration. A decline of 10% or more in FVC predicted, or 15% or more in DLCO predicted, over six to twelve months is considered clinically significant and associated with increased mortality risk independent of baseline values.

Recalculating the GAP score at each clinical review allows clinicians to track stage transitions over time. Movement from Stage I to Stage II, or Stage II to Stage III, represents objective evidence of disease progression and typically prompts reassessment of the management plan - including antifibrotic therapy optimisation, re-evaluation of transplant candidacy, escalation of oxygen therapy, and integration of palliative care support. Even within a stage, increasing point totals suggest progressive deterioration.

In patients who are unable to perform spirometry or DLCO due to progressive dyspnoea - who therefore receive 3 points for each of these domains - clinical assessment and radiological monitoring take on increased importance. Serial HRCT can document progression of radiological extent of fibrosis and honeycombing, though radiation exposure limits the frequency with which this can be applied. Six-minute walk test distance and pulse oximetry during exercise provide useful complementary prognostic information in this population.

Multidisciplinary Team Approach to IPF Management

Management of IPF is most effectively delivered through a dedicated multidisciplinary team (MDT) incorporating pulmonology, radiology, pathology, physiotherapy, nursing, and palliative care expertise. The MDT framework, which originated in oncology, has been adopted as the gold standard for IPF diagnosis and management in most major international guidelines. The GAP Index provides a common prognostic language that facilitates communication across MDT members and supports structured clinical discussions.

Specialist interstitial lung disease nurses play a particularly valuable role in IPF management. They provide patient education, support medication adherence to antifibrotic therapy, monitor side effects, coordinate care across specialties, and serve as the primary point of contact for patients and families navigating a complex and distressing diagnosis. For many patients, the ILD specialist nurse is the most frequently contacted member of the clinical team.

Patient support organisations, such as the Pulmonary Fibrosis Foundation (USA), Action for Pulmonary Fibrosis (UK), and European Pulmonary Fibrosis Federation (EuroIPF), provide educational resources, peer support networks, and clinical trial information. Connecting patients with these organisations at the time of diagnosis is a simple but meaningful component of comprehensive IPF care.

Frequently Asked Questions

What does the GAP Index stand for in IPF?

GAP stands for Gender, Age, and Physiology - the three clinical domains used to calculate the score. Gender contributes up to 1 point, age contributes up to 2 points, and the physiological variables (FVC and DLCO) each contribute up to 3 points. The total possible score is 8 points, with higher scores indicating more severe disease and greater mortality risk. The model was published by Ley et al. in the American Journal of Respiratory and Critical Care Medicine in 2012.

How is the GAP Index different from the ILD-GAP Index?

The original GAP Index was specifically developed and validated for idiopathic pulmonary fibrosis (IPF). The ILD-GAP Index extends the model to all fibrotic interstitial lung diseases by adding an additional variable for the specific ILD diagnosis. In the ILD-GAP, IPF is assigned the highest point value among ILD diagnoses, reflecting its generally worse prognosis compared with conditions like connective tissue disease-associated ILD or hypersensitivity pneumonitis. For IPF-specific cohorts, both models perform similarly.

What GAP stage should trigger urgent lung transplant referral?

Most experts recommend transplant referral at the time of IPF diagnosis, given the unpredictable disease course and long waitlist times. However, GAP Stage II and particularly Stage III represent situations where urgency of evaluation increases substantially. Stage III carries a one-year mortality approaching 40%, and patients in this stage who are otherwise transplant candidates require expedited assessment. Many transplant centres recommend listing patients who meet ISHLT criteria, regardless of GAP stage, as soon as possible after diagnosis.

Can the GAP Index be used for IPF patients on antifibrotic therapy?

Yes, the GAP Index can be calculated and tracked in patients receiving pirfenidone or nintedanib. However, the absolute mortality figures from the original model were derived from a pre-antifibrotic era cohort, and treated patients may have somewhat lower mortality than these historical estimates suggest. The model retains its value for staging disease severity, tracking progression, and supporting clinical discussions, even if the specific percentage estimates should be interpreted with appropriate caution in the current treatment era.

What does it mean if a patient cannot perform FVC or DLCO testing?

In the GAP scoring system, inability to perform either FVC or DLCO testing attracts the maximum point value for that variable (3 points each). This reflects the clinical reality that patients who are too unwell to complete standardised lung function tests are almost certainly at higher mortality risk than those who can complete them, regardless of what their numerical result would have been. This provision makes the GAP Index applicable even in patients with very severe disease where formal testing is not feasible.

How often should the GAP Index be recalculated?

GAP should be recalculated at each formal clinical review where lung function testing is performed - typically every three to six months in patients with IPF. Serial recalculation allows detection of stage transitions, which have important implications for management. Major international guidelines recommend lung function monitoring at three to six month intervals for stable patients and following any clinical deterioration. The dynamic trajectory of GAP scores over time may be more informative than any single cross-sectional calculation.

Is DLCO more important than FVC in the GAP Index?

DLCO and FVC contribute equally to the maximum GAP score (3 points each). However, DLCO is generally considered to be the more sensitive and prognostically informative lung function variable in IPF. It declines faster than FVC in many patients, reflects both alveolar surface area loss and vascular obliteration, and is particularly important in patients with combined emphysema and fibrosis, where FVC may be spuriously preserved. Both variables are essential components of comprehensive IPF assessment.

Does the GAP Index predict acute exacerbations of IPF?

No - the GAP Index predicts all-cause mortality rather than specific events like acute exacerbations (AE-IPF). Acute exacerbations are sudden, life-threatening episodes of accelerated decline that occur unpredictably across all GAP stages. While patients with more advanced disease (higher GAP scores) may have a higher absolute risk of AE-IPF, the model was not designed to predict these events specifically. There is currently no validated clinical prediction model for AE-IPF.

Why does male sex confer a worse prognosis in IPF?

The biological basis for worse prognosis in male IPF patients is not fully established. Proposed mechanisms include sex-based differences in telomere biology (mutations in telomerase genes MUC5B and TERT are important in IPF pathogenesis and may be distributed differently by sex), hormonal modulation of fibrosis pathways (oestrogens may have antifibrotic effects), and potential confounding by differences in smoking history and occupational exposures. The sex-based prognostic difference is robust across multiple cohorts and is therefore incorporated as a direct scoring variable in the GAP Index.

What are the IPF GAP Index mortality estimates at one, two, and three years?

Based on the original validation cohort: Stage I (0 to 3 points) - 5.6% at one year, 10.9% at two years, 16.3% at three years. Stage II (4 to 5 points) - 16.2% at one year, 29.9% at two years, 42.1% at three years. Stage III (6 to 8 points) - 39.2% at one year, 62.1% at two years, 76.8% at three years. These figures should be interpreted as population-level estimates derived from a pre-antifibrotic era cohort; individual patient prognosis may differ.

Can GAP be used for non-IPF interstitial lung diseases?

The original GAP Index was validated specifically in IPF. The ILD-GAP Index was developed as a modified version applicable across fibrotic ILDs, with an additional variable for ILD diagnosis type (IPF, non-IPF UIP, and other ILDs). For patients with connective tissue disease-associated ILD, hypersensitivity pneumonitis, or other non-IPF fibrotic conditions, the ILD-GAP model is more appropriate. Applying the original IPF-specific GAP Index to non-IPF populations may result in inaccurate prognostic estimates.

How does the six-minute walk test relate to GAP scoring?

The six-minute walk test (6MWT) is not incorporated into the GAP Index but provides complementary prognostic information. Walk distance below 250 metres and oxygen desaturation below 88% during the 6MWT are both associated with increased mortality in IPF, and the 6MWT is included in ISHLT criteria for lung transplant listing decisions. In clinical practice, 6MWT is frequently performed alongside formal lung function testing and HRCT to provide a comprehensive assessment of disease severity that extends beyond what GAP alone captures.

Should antifibrotic therapy be initiated regardless of GAP stage?

Yes - current major international guidelines (ATS/ERS/JRS/ALAT 2022 and British Thoracic Society) recommend initiating antifibrotic therapy in virtually all patients with confirmed IPF, including those with mild disease at GAP Stage I. The rationale is that preserving lung function while it is still relatively intact maximises absolute benefit from treatment, and all patients are at risk of disease progression. The previous practice of watchful waiting in mild disease has been superseded by evidence supporting early treatment.

What is the role of HRCT in assessing IPF beyond the GAP Index?

HRCT provides important prognostic information independent of lung function. The extent of honeycombing, the fibrosis score, and the presence or absence of ground-glass opacity have all been associated with prognosis in IPF cohorts. Notably, HRCT fibrosis extent may predict prognosis in patients with relatively preserved lung function (Stage I GAP), identifying a subset who are at higher risk than their physiology alone suggests. The TORVAN model incorporates HRCT variables alongside physiology for this reason, though its greater complexity limits routine clinical adoption.

How does combined pulmonary fibrosis and emphysema affect GAP scoring?

Combined pulmonary fibrosis and emphysema (CPFE) is a distinct clinical syndrome where fibrosis (typically UIP pattern) and emphysema coexist in the same patient, commonly in older male smokers. The two processes have opposing effects on lung volumes - fibrosis reduces total lung capacity while emphysema increases it - resulting in spurious preservation of FVC. This may lead to underestimation of disease severity when FVC is used for GAP scoring. DLCO, which is severely reduced in CPFE, will typically still reflect disease severity. Clinicians should be alert to this potential limitation in the CPFE population.

What is the GAP Index score range and what does each number mean?

The GAP Index ranges from 0 to 8 points. Scores of 0 to 3 classify as Stage I (mild disease, lowest mortality risk), 4 to 5 as Stage II (moderate disease, intermediate mortality risk), and 6 to 8 as Stage III (severe disease, highest mortality risk). Within a stage, higher individual scores reflect greater physiological impairment. A score of 8 - indicating male sex, age over 65, and inability to perform both FVC and DLCO testing - represents the most clinically severe presentation captured by the model.

What is the significance of DLCO below 35% in IPF?

DLCO below 35% predicted represents severe impairment of gas transfer and is associated with resting hypoxaemia, markedly reduced exercise tolerance, and high mortality risk in IPF. In the GAP model, this threshold attracts 2 points. Clinically, DLCO below 40% predicted is an ISHLT criterion for listing IPF patients for lung transplantation. Patients with DLCO below 35% typically require supplemental oxygen, have very limited exertional capacity, and should be considered for urgent transplant evaluation and early palliative care integration.

How does pirfenidone or nintedanib affect GAP score progression over time?

Both antifibrotic agents reduce the annual rate of FVC decline by approximately 50% compared with untreated disease. Since FVC is a key driver of GAP score progression, treated patients are less likely to progress from Stage I to Stage II, or Stage II to Stage III, within a given period compared with historical untreated cohorts. DLCO trajectories under antifibrotic therapy are less well characterised than FVC, but treated patients generally show slower overall physiological deterioration. However, antifibrotic therapy does not halt disease progression entirely - GAP scores will still increase over time in most patients.

Are there blood biomarkers that add prognostic value to the GAP Index?

Several serum biomarkers have demonstrated prognostic value in IPF, including MMP-7, KL-6, SP-A, SP-D, CCL-18, and YKL-40. These markers reflect different aspects of fibrosis activity, epithelial injury, and inflammatory signalling. MMP-7 in particular has shown consistent prognostic utility across multiple cohorts and was evaluated as a potential addition to the GAP model. However, none of these biomarkers are routinely available in all clinical settings, lack standardised reference ranges, and have not been universally adopted into clinical guidelines. They remain primarily research tools at present.

What is the clinical significance of a GAP score that increases between visits?

An increasing GAP score between clinic visits indicates disease progression and warrants clinical reassessment. Advancement from Stage I to Stage II, or Stage II to Stage III, doubles or triples the estimated mortality risk and typically prompts specific management responses: review of antifibrotic therapy, reassessment of transplant candidacy and waitlist priority, consideration of oxygen therapy, and integration of palliative care support. Even within a stage, an increasing score suggests deterioration that may require action before a formal stage transition occurs.

How should clinicians communicate GAP stage to patients?

Communication of GAP staging and associated mortality estimates requires careful consideration of patient preferences, health literacy, and emotional readiness. Some patients prefer direct numerical prognostic information to make informed decisions about treatment, transplantation, and advance care planning. Others prefer to understand severity in relative terms (mild, moderate, severe) without specific percentages. Clinicians should elicit patient preferences before sharing mortality data, and should contextualise estimates by noting that individual outcomes vary, that antifibrotic therapy may improve on historical estimates, and that transplantation can significantly alter prognosis.

Is the GAP Index validated in patients over 80 years of age?

The original GAP derivation and validation cohorts included patients primarily in their 60s and 70s, with limited representation of patients aged 80 or above. Very elderly patients with IPF represent a growing clinical population, and extrapolation of GAP-based mortality estimates to this age group should be done with caution. Furthermore, in very elderly patients, competing mortality risks from cardiovascular disease, malignancy, and other age-related conditions may be as clinically relevant as IPF-specific mortality. The GAP Index captures only IPF-specific prognostic variables and does not account for overall comorbidity burden.

Does exercise-induced desaturation affect GAP scoring?

Exercise-induced oxygen desaturation is not directly incorporated into the GAP Index scoring system, which relies on resting lung function measurements. However, desaturation below 88% during a six-minute walk test is one of the ISHLT criteria for lung transplant listing in IPF and provides important prognostic information independent of GAP stage. Some patients with relatively preserved resting FVC and DLCO (GAP Stage I) may desaturate significantly during exercise, suggesting worse functional impairment than their resting values alone capture. Comprehensive clinical assessment should include exercise testing in addition to resting lung function.

What is the role of pulmonary rehabilitation in IPF across GAP stages?

Pulmonary rehabilitation improves exercise capacity and health-related quality of life in IPF across all disease stages, though the magnitude of benefit may differ. Multiple randomised controlled trials have demonstrated improvements in six-minute walk distance, dyspnoea scores, and quality of life metrics following pulmonary rehabilitation programmes in IPF. The benefits tend to be maintained for three to six months before declining as the underlying disease progresses. Pulmonary rehabilitation is particularly valuable in Stage I and early Stage II patients who have sufficient functional reserve to engage in supervised exercise training.

How does the GAP Index inform hospice or palliative care referral?

A GAP Stage III classification - with its one-year mortality of approximately 40% - meets many healthcare systems' criteria for hospice eligibility or intensified palliative care integration. At Stage III, ensuring that advance care plans are documented, that goals of care have been discussed, and that symptom management resources are in place becomes a clinical priority. Earlier GAP stages may also benefit from advance care planning, and many expert clinicians advocate for introducing palliative care conversations at the time of IPF diagnosis, regardless of initial GAP stage, given the progressive nature of the condition.

Are there sex-specific differences in GAP stage distribution?

Because male sex contributes 1 point to the GAP score, men will on average have higher GAP scores than women with identical physiological findings and the same age. This means that the male-female distribution across stages will be skewed, with a higher proportion of men in Stage II and Stage III compared with women. This is intentional and reflects the true prognostic difference between sexes. Clinicians should be aware that a woman with a GAP Stage I score is not necessarily lower risk in absolute terms than her stage classification alone would suggest - she avoids one potential GAP point (male sex) that would have pushed a man with identical physiology into a higher stage.

What monitoring schedule is recommended for different GAP stages?

While specific monitoring intervals vary by guideline and clinical setting, general principles suggest more frequent assessment for higher GAP stages. Stage I patients typically undergo lung function testing, clinical review, and HRCT (if clinically indicated) every six to twelve months. Stage II patients generally require three to six month lung function assessments and more frequent clinical review. Stage III patients may need monthly or two-monthly clinical contact, regular oxygen assessment, frequent transplant waitlist review, and close integration with palliative care and specialist nursing support. Clinical deterioration at any stage should prompt earlier assessment regardless of scheduled intervals.

Conclusion

The GAP Index is a validated, clinically practical tool for staging disease severity and estimating mortality risk in idiopathic pulmonary fibrosis. Its simplicity - requiring only gender, age, FVC, and DLCO - makes it applicable across virtually all clinical settings where patients with IPF are managed. The three-stage classification system provides a shared clinical language that supports patient communication, multidisciplinary team discussions, transplant referral planning, and integration of palliative care services.

The model has important limitations that should be acknowledged in clinical practice, including its derivation in a pre-antifibrotic era cohort, its lack of radiological variables, and its inability to predict acute exacerbations. Despite these limitations, the GAP Index remains the most widely used and validated prognostic staging system in IPF, with a robust evidence base across geographically diverse patient populations.

Clinicians using this calculator should interpret results within the full clinical context of each patient, incorporating information from HRCT, exercise testing, functional status, comorbidities, and individual patient preferences. Serial GAP calculations, tracked over time, provide more clinically meaningful information than any single calculation, and should be a routine component of structured IPF follow-up in specialist and general respiratory practice.