We read with interest the state of the art review by Umetsu on mechanisms by which obesity impacts asthma [1]. He has clearly outlined the extent to which molecular targets, both within allergic (T-helper 2 [TH2]) and non-allergic mechanistic pathways of asthma, need further evaluation and drug development for obese asthmatics. This was on the basis that current standard therapies for asthma such as inhaled corticosteroids (ICS) appear to be less effective in these individuals. Whilst these novel molecular targets are clearly an exciting step forward, we believe there are several other issues that need to be addressed as well when it comes to standard asthma treatment with ICS in the obese. Umetsu touched on altered lung mechanics in the obese stating more restriction of lung volumes[2]. We have found previously that overweight asthmatics (body mass index [BMI]???25kg/m2) appear to have attenuated fractional exhaled nitric oxide (FeNO) and symptom responses as the dose of inhaled budesonide was increased up to 800?g/day compared to normal weight (BMI<25kg/m2) counterparts receiving the same ICS dose ramp[3]. However, there were no differences seen between responses in airway calibre as measured by forced expiratory volume in 1s (FEV1), or indeed airway hyperresponsiveness (AHR) to methacholine. Therefore, altered corticosteroid response at a molecular level alone does not necessarily explain the equal response in these latter two outcomes. Certainly, in significantly overweight individuals their lung volumes are reduced, but we did not see this difference in our cohort, presumably reflecting a modestly increased mean BMI of 30kg/m2. It may be, therefore, that either the ICS is not being delivered to the peripheral small airways sufficiently in obese asthmatics, in the presence of normal proximal delivery[4]. A previous study examined the effects of bariatric surgery on measures of peripheral small airway function and asthma between asthmatic and non-asthmatic obese individuals finding that the peripheral airways are more collapsible in obese asthmatics than in their non-asthmatic counterparts[5]. Indeed small airway dysfunction itself is associated with poorer asthma control[6 7], which could feasibly have a greater impact in obese asthmatics. Therefore, strategies to improve delivery of ICS to the peripheral airways might be a more cost-effective first step for certain obese asthmatics than going directly to more expensive biological therapies to improve their asthma control. We believe further prospective study is required into the lung distribution and clinical utility of extra-fine particle ICS in obese asthmatics, as well to establish if higher than usual doses of ICS are required to achieve the same effect as in normal weight asthmatics. It goes without saying that strategies which target significant weight loss - including bariatric surgery where necessary - are likely to be even more cost-effective in the first place, as this will not only impact on improving asthma control but also on comorbidities such as diabetes and hypertension.

References

1. Umetsu DT. Mechanisms by which obesity impacts asthma. Thorax 2016.

2. King GG, Brown NJ, Diba C, et al. The effects of body weight on airway calibre. Eur Respir J 2005;25(5):896-901.

3. Anderson WJ, Lipworth BJ. Does body mass index influence responsiveness to inhaled corticosteroids in persistent asthma? Ann Allergy Asthma Immunol 2012;108(4):237-42.

4. Lipworth B, Manoharan A, Anderson W. Unlocking the quiet zone: the small airway asthma phenotype. The Lancet Respiratory medicine 2014;2(6):497-506.

5. Al-Alwan A, Bates JH, Chapman DG, et al. The nonallergic asthma of obesity. A matter of distal lung compliance. Am J Respir Crit Care Med 2014;189(12):1494-502.

6. Manoharan A, Anderson WJ, Lipworth J, et al. Small airway dysfunction is associated with poorer asthma control. Eur Respir J 2014;44(5):1353-5.

7. Shi Y, Aledia AS, Tatavoosian AV, et al. Relating small airways to asthma control by using impulse oscillometry in children. J Allergy Clin Immunol 2012;129(3):671-8.

Conflict of Interest:

None declared

To the Editor,

The diagnosis of hypersensitivity pneumonitis (HP) is difficult and often relies on an array of clinical symptoms and signs developed in an appropriate setting, with the demonstration of radiographic and tomographic abnormalities, serum precipitating antibodies against offending antigens, a lymphocytic alveolitis on bronchoalveolar lavage, and/or a granulomatous reaction on lung biopsies. Taken separately, all these manifestations are nonspecific and only the combination of several of them may help clinicians to arrive at a correct diagnosis. By providing better estimates of the probability of a disease than clinical judgement, prediction rules (i.e., tools that quantifies the contribution that various components of the history, physical examination and basic laboratory results makes toward the diagnosis in an individual patient) may guide clinical practice.[1] In this regard, we read with much interest Johannson and colleagues' report of a multidimensional diagnostic model for chronic hypersensitivity pneumonitis (HP).[2] This research parallels the HP Study previously reported, the objective of which was to develop a clinical prediction rule for the diagnosis of active HP.[3]

Johannson's study bears some resemblance to the HP study, especially in its statistical methods. However, similarities end here. The HP study was a prospective multicenter study of 661 patients presenting with an acute pulmonary syndrome for which HP was considered in the differential diagnosis. Johannson's study is a single-center retrospective analysis of 190 patients with biopsy-proven, chronic HP. The HP study specifically applied to active acute, subacute and chronic HP, and only excluded inactive residual HP. It included consecutive patients, chosen in an unbiased fashion and representing a wide spectrum of diseases from a variety of institutions, hence increasing generalizability. By including only patients who required surgical lung biopsy, Johannson and colleagues likely preselected difficult cases of HP and non-HP interstitial lung disease, with the consequence of underestimating the accuracy of their prediction models. The HP Study looked at simple and objective clinical criteria and used high resolution computed tomography (HRCT) in the gold standard definition of HP, whereas Johansson's study incorporated radiological features from HRCT and a radiologist's diagnostic impression in their prediction model. Bronchoalveolar lavage was obtained in all patients in the HP study but it was not considered in Johannson's study.

Johannson's study and the HP Study are not competing studies; they are complementary and their results cannot be directly compared. Although the two studies had different patient populations and case selection, they may be useful in the appropriate setting. Both studies have another point in common: to be elevated in the hierarchy of evidence for clinical decision rules, they should be validated again in different populations.[1]

Yves Lacasse MD, Institut universitaire de cardiologie et de pneumologie de Quebec, Universite Laval, Quebec, Canada

Moises Selman MD, Instituto Nacional de Enfermedades Respiratorias, Mexico DF, Mexico

Ulrich Costabel MD, Ruhrlandklinik, Essen, Germany

Jean-Charles Dalphin MD, Centre Hospitalier Universitaire de Besancon, Besancon, France

Thomas V. Colby MD, Mayo Clinic Scottsdale, Scottsdale, USA

Riitta Erkinjuntti-Pekkanen MD, Social Insurance Institution, Helsinki, Finland

Ferran Morell MD, Hospital Universitari Vall d'Hebron, Barcelona, Spain

Yvon Cormier MD, Universite Laval, Quebec, Canada

for the HP Study Group.

References

1 McGinn TG, Guyatt GH, Wyer PC, et al. Users' guides to the medical literature: XXII: how to use articles about clinical decision rules. Evidence-Based Medicine Working Group. JAMA 2000;284:79-84.

2 Johannson KA, Elicker BM, Vittinghoff E, et al. A diagnostic model for chronic hypersensitivity pneumonitis. Thorax 2016;71:951-4.

3 Lacasse Y, Selman M, Costabel U, et al. Clinical diagnosis of hypersensitivity pneumonitis. Am J Respir Crit Care Med 2003;168:952-8.

Conflict of Interest:

Yves Lacasse was the principal investigator of the HP Study. All co-authors of this letter were co-investigators of the HP Study.

Dear Editor,

We appreciate the comments by Dr Eisenhut.(1) We did not focus on the sensitivity analysis in our study as we were primarily interested in establishing the impact of BCG on interpretation of tuberculin skin test (TST) responses, which we considered especially relevant in the context of the new NICE guidance.(2) The points raised by Dr Eisenhut are interesting and we agree that the hypotheses put forward need further exploration.

However, we strongly disagree with the conclusion that interferon- gamma release assays (IGRAs) can be used to reliably exclude tuberculosis (TB) infection in children. We and others have very clearly shown that IGRA is a rule in test, not a rule out test, given that there is no gold standard for TB infection in adults or children.(3) The negative predictive value cannot be easily determined in young children who are routinely placed on isoniazid preventive treatment in accordance with published guidelines. Both TST and IGRA have acknowledged flaws as screening tests. Neither can rule out TB infection or indeed disease; both tests can be negative even in individuals with microbiologically confirmed TB.

References 1. Eisenhut M. Hypotheses to explain the reduced sensitivity of tuberculin skin test in BCG immunised young children. Thorax. 2016. 2. National Institue for Health and Care Excellence. Tuberculosis 2016. Available at: http://www.nice.org.uk/guidance/ng33/resources/tuberculosis- prevention-diagnosis-management-and-service-organisation-1837390683589 (accessed 16 September 2016) 3. Kampmann B, Whittaker E, Williams A, et al. Interferon-gamma release assays do not identify more children with active tuberculosis than the tuberculin skin test. Eur Respir J. 2009;33(6):1374-1382.

Conflict of Interest:

None declared

We thank Vanfleteren and colleagues for their comments on our recently published equivalence trial comparing home-based and centre-based pulmonary rehabilitation in people with stable chronic obstructive pulmonary disease (COPD).[1] We agree that there is a compelling need to increase the implementation, utilization and delivery of pulmonary rehabilitation.[2] We welcome further discussion regarding the role of new pulmonary rehabilitation models, such as our home-based model, in achieving these aims.

Despite the best efforts of clinicians and the plethora of evidence supporting its benefits, only a small minority of people with COPD currently undertake pulmonary rehabilitation.[2] Increasing financial support for existing programmes and establishing new centre-based programmes may be important to improve capacity and reduce waiting times. However these strategies cannot comprehensively address the well documented barriers of travel, transport, inconvenient location, inconvenient timing and disruption to routines that prevent debilitated people with COPD from engaging in centre-based programmes.[3] In Australia, like many large countries, we must also address health inequalities related to geography and low population density, with limited pulmonary rehabilitation options available for those living in remote areas where the burden of lung disease is high. Our home-based model was designed to enhance access to pulmonary rehabilitation for patients who cannot engage in the traditional centre-based model.

As noted by Vanfleteren and colleagues, our study recruited 166 people with COPD who had been referred to pulmonary rehabilitation. We considered this to be a highly relevant target population. A referral to pulmonary rehabilitation is no guarantee of programme attendance or completion; in fact a recent audit in the United Kingdom showed that one in three of those referred to centre-based pulmonary rehabilitation do not ever attend an assessment, and 39% of those who attend an assessment do not complete the programme.[4] In our study, programme completion was higher in those who underwent home-based pulmonary rehabilitation than in those who participated in centre-based programmes. Attaining the benefits of pulmonary rehabilitation is dependent on achieving a sufficient rehabilitation 'dose'; in our study, patients who completed a programme (regardless of location) had fewer hospitalisations in the year following pulmonary rehabilitation.[1] We also found that 54 patients (18% of those assessed) declined to participate in the trial because they wished to attend a centre-based programme. It was important to document the preference of this group who are already motivated to attend centre-based pulmonary rehabilitation. The home-based model does not remove such an opportunity for those who wish to engage in centre-based care.

Pulmonary rehabilitation is a core component of integrated and comprehensive care for people with COPD.[5] We agree with Vanfleteren and colleagues that this goes beyond exercise and education; it includes (but is not limited to) problem solving, goal setting, skill acquisition, decision making and collaboration with health professionals.[5] Our home- based programme was designed to incorporate these features. Weekly telephone calls were delivered by highly experienced pulmonary rehabilitation physiotherapists who were trained in motivational interviewing. Consistent with a patient-centred approach to care, participants were encouraged to identify the health problems that were most relevant to them and to set appropriate health goals. Commonly set goals related to weight loss, management of chest infections and smoking cessation. Where relevant, the physiotherapist made a referral to an appropriate member of the multidisciplinary team. Unexpectedly and importantly, some patients actively addressed their goals by finding services that better suited them outside the pulmonary rehabilitation team, including community based health services that were closer to their homes. We also note that anxiety and depression decreased in both home- based and centre-based groups over the trial, with no difference according to programme location.[1] Our participants were typical of those seen in many centre-based pulmonary rehabilitation programmes, with a median of four comorbidities. However, we acknowledge that some patients with complex co-existing medical conditions may be more suitable for a supervised, centre-based programme. The severity and impact of comorbidities should be assessed prior to commencing pulmonary rehabilitation as part of a comprehensive patient assessment,[6] allowing patients and clinicians to make sound decisions about the best location of care.

We support the authors' call to embrace 'P4 medicine' which is Predictive, Preventive, Personalized and Participatory.[7] This model places strong emphasis on the participation of the individual, empowering them to make informed choices about their health care. If participation in pulmonary rehabilitation is to become a reality for the majority who need it, more choices are necessary. We look forward to a time when people with COPD can choose from a suite of evidence-based models of pulmonary rehabilitation, in order to optimise access to this important treatment and to ensure its benefits are reaped by all patients with COPD rather than a few.

References

1. Holland AE, Mahal A, Hill CJ, et al. Home-based rehabilitation for COPD using minimal resources: a randomised, controlled equivalence trial. Thorax, published online Sept 26th 2016. doi: 10.1136/thoraxjnl-2016- 208514.

2. Rochester CL, Vogiatzis I, Holland AE, et al. An Official American Thoracic Society/European Respiratory Society Policy Statement: Enhancing Implementation, Use, and Delivery of Pulmonary Rehabilitation. Am J Respir Crit Care Med 2015;192:1373-86.

3. Keating A, Lee A, Holland AE. What prevents people with chronic obstructive pulmonary disease from attending pulmonary rehabilitation? A systematic review. Chronic Respiratory Disease 2011;8:89-99.

4. Steiner M, Holzhauer-Barrie J, Lowe D, et al. Pulmonary Rehabilitation: Steps to breathe better. National Chronic Obstructive Pulmonary Disease (COPD) Audit Programme: Clinical audit of Pulmonary Rehabilitation services in England and Wales 2015. National clinical audit report. London: Royal College of Physicians, 2016.

5. Wagg K. Unravelling self-management for COPD: what next? Chronic Respiratory Disease 2012;9:5-7.

6. Spruit MA, Singh SJ, Garvey C, et al. An official American Thoracic Society/European Respiratory Society statement: key concepts and advances in pulmonary rehabilitation. American Journal of Respiratory and Critical Care Medicine 2013;188:e13-64.

7. Hood L, Friend SH. Predictive, personalized, preventive, participatory (P4) cancer medicine. Nature Reviews Clinical Oncology 2011;8:184-7.

Conflict of Interest:

None declared