We thank Professors Lipworth and Anderson for their very thoughtful comments in their response to our piece1, and for pointing out clear strategies for treating obesity-associated asthma without expensive therapies, e.g., with improved delivery of inhaled corticosteroids and/or weight reduction.

It should be noted however, that the focus of the piece was on mechanisms by which obesity might cause asthma, with the idea that a greater understanding of disease mechanisms causing obesity-associated asthma might lead to improved therapies, and possibly to even cost effective ones. From a pathogenesis point of view, even pilot studies showing the efficacy of any therapy might be extremely valuable in identifying specific molecular mechanisms of disease. In that regard, the impetus of the article was that obesity-associated asthma represents a significant and growing unmet medical need, characterized by increased healthcare utilization and reduced quality of life, and refractory to even oral corticosteroid treatment and other current therapies. These current therapies include inhaled corticosteroids and weight reduction programs, although improved delivery or compliance with these measures, as suggested by Professors Lipworth and Anderson, could improve the clinical result.

It is also worth mentioning that studies of obesity-associated asthma, as mentioned in the piece1, indicate that there are at least two forms of the disease, an early onset form and a late onset form, one of which is much more responsive to weight reduction (late onset form) than the other. We would therefore advocate further study of disease mechanisms causing asthma in obese individuals, including subpopulations thereof, along with improved implementation of current inexpensive treatments, that might lead to an improved understanding and possibly to new therapies for this very significant, growing and costly public heath problem.

1. Umetsu, D.T. Mechanisms by which obesity impacts asthma. Thorax (2016).

Conflict of Interest:

I am an employee of Genentech

We thank Dr. Lacasse and the HP Study Group for their correspondence regarding 'A diagnostic model for chronic hypersensitivity pneumonitis', and appreciate their thoughtful consideration of our work.(1) We agree that these two studies are complementary, and hope that both will serve to improve diagnostic accuracy in the evaluation of patients with suspected HP. We further concur that much work remains to be done to advance our understanding of HP.

The HP Study was a pivotal paper in our field, the first to define a clinically applicable prediction model to diagnose acute, subacute and chronic HP.(2) However, the HP Study cohort included patients with 'active' disease, specifically excluding patients with fibrotic sequelae or 'residual inactive HP'. Notably, an inciting antigen was identified in 114/116 (97%) of patients with HP. Our focus was on a different clinical population and conundrum - the differentiation of chronic, commonly fibrotic HP from other fibrotic interstitial lung diseases, in particular idiopathic pulmonary fibrosis (IPF). These HP patients typically do not present with an acute pulmonary syndrome, and previous data from our center have demonstrated 60% to be antigen indeterminate, despite thorough investigation,(3) consistent with data from similar sub-specialty centers.(4) We required surgical lung biopsy as part of our gold standard multi-disciplinary discussion-based diagnosis of HP given the lack of universally accepted non-histopathological criteria in this clinical scenario.

The study of HP is challenging, attributable to a lack of universally accepted diagnostic criteria, the conundrum of antigen indeterminate disease and controversies over the clinical utility of bronchoalveolar lavage fluid analysis, serum specific antibodies, and inhalational challenge. A recent review suggests focused areas for future research and we are enthused by the increasing interest in this area.(5) Along with the HP Study group, we remain hopeful that our complementary contributions to clinical prediction models will lead to an overall better diagnostic accuracy of HP in all its forms, and ultimately improved patient care.

Kerri A. Johannson MD MPH, University of Calgary, Calgary AB Canada; Brett M. Elicker MD, University of California, San Francisco, San Francisco CA USA; Eric Vittinghoff PhD, University of California, San Francisco, San Francisco CA USA; Deborah Assayag MD, McGill University, Montreal QC Canada; Kaissa de Boer MD, University of Ottawa, Ottawa ON Canada; Jeffrey A. Golden MD, University of California, San Francisco, San Francisco CA USA; Kirk D. Jones MD, University of California, San Francisco, San Francisco CA USA; Talmadge E. King Jr. MD, University of California, San Francisco, San Francisco CA USA; Laura L. Koth MD, University of California, San Francisco, San Francisco CA USA; Joyce S. Lee MD, University of Colorado, Denver, Aurora CO USA; Brett Ley MD, University of California, San Francisco, San Francisco CA USA; Paul J. Wolters MD, University of California, San Francisco, San Francisco CA USA; Harold R. Collard MD, University of California, San Francisco, San Francisco CA USA.

References

1. Johannson KA, Elicker BM, Vittinghoff E, Assayag D, de Boer K, Golden JA, Jones KD, King TE, Koth LL, Lee JS, Ley B, Wolters PJ, Collard HR. A diagnostic model for chronic hypersensitivity pneumonitis. Thorax 2016.

2. Lacasse Y, Selman M, Costabel U, Dalphin JC, Ando M, Morell F, Erkinjuntti-Pekkanen R, Muller N, Colby TV, Schuyler M, Cormier Y. Clinical diagnosis of hypersensitivity pneumonitis. Am J Respir Crit Care Med 2003; 168: 952-958.

3. Mooney JJ, Elicker BM, Urbania TH, Agarwal MR, Ryerson CJ, Nguyen ML, Woodruff PG, Jones KD, Collard HR, King TE, Koth LL. Radiographic fibrosis score predicts survival in hypersensitivity pneumonitis. Chest 2013; 144: 586-592.

4. Fernandez Perez ER, Swigris JJ, Forssen AV, Tourin O, Solomon JJ, Huie TJ, Olson AL, Brown KK. Identifying an inciting antigen is associated with improved survival in patients with chronic hypersensitivity pneumonitis. Chest 2013; 144: 1644-1651.

5. Salisbury ML, Myers JL, Belloli EA, Kazerooni EA, Martinez FJ, Flaherty KR. Diagnosis and Treatment of Fibrotic Hypersensitivity Pneumonia. Where We Stand and Where We Need to Go. Am J Respir Crit Care Med 2016.

Conflict of Interest:

None declared

We would like to congratulate Bissett et al on performing a clinically important study in a challenging cohort of Intensive Therapy Unit (ITU) patients. Any information in assisting the weaning process of ITU patients is clearly very important and clinically very useful.

It is interesting that Maximum Inspiratory Pressure (MIP) was used to assess the inspiratory muscle strength (IMS), one of the primary endpoints. A reliable MIP requires patients to achieve a good mouth seal, which may not always be possible on ITU. Patients are unlikely to be familiar with the manoeuvre and this may lead to suboptimal technique. Sniff Nasal Inspiratory Pressure (SNIP) is a simple, non-invasive test but as a natural process, patients will have greater aptitude for this investigation. It is particularly useful in patients with neuromuscular disorders with facial weakness (1). It has a smaller range of normal values than mouth pressures (2,3) achieving equal or more pressure than static maximal efforts (3,4). We believe this should be considered as an adjunctive test of IMS as this involves a similar technique to MIP manoeuvre and may only be conferring training to perform this investigation and therefore we would recommend multiple assessments of respiratory muscle strength (5).

However, as are volitional assessments of IMS, SNIP and MIP rely on motivation, co-operation and functional ability which may be impaired in ITU patients. It can be difficult to prevent learning and training from repeated testing affecting the results (6,7). Non-volitional investigations using magnetic stimulation of the phrenic nerve to measure twitch trans diaphragmatic pressure (TwDPI) measurement (8,9,10) and diaphragmatic EMG using multi-pair oesophageal probes have been found to be effective in measuring diaphragmatic muscle strength and can be performed in ITU patients(11). Although these are invasive investigations and not widely available, they would more definitively confirm the validity of inspiratory muscle training (IMT) in this patient group. The importance of this must be emphasised as IMT has not universally been shown to improve outcomes in healthy volunteers and Chronic Obstructive Pulmonary Disease (COPD) patients (5,6,7) and a review (12) suggested that improvement in outcomes following IMT seen in a meta-analysis (13) might be a placebo effect. In conclusion, we congratulate Bissett et al for performing a challenging and a clinically relevant study. We would however suggest using multiple assessments of IMS, such as SNIP in addition to MIP. However the value of IMT in ITU patients can only definitively be determined by including a non -volitional investigation of IMS.

References

(1) N. Mustfa, J. Moxham. Respiratory muscle assessment in motor neurone disease. QJM Sep 2001, 94 (9) 497-502

(2) Miller JM, Moxham J, Green M. The maximal sniff in the assessment of diaphragm function in man. Clin Sci 1985;69:91-96.

(3) Laroche CM, Mier AK, Moxham J, Green M. The value of sniff esophageal pressures in the assessment of global inspiratory muscle strength. Am Rev Respir Dis 1988;138:598-603.

(4) Polkey MI, Green M, Moxham J. Measurement of respiratory muscle strength. Thorax 1995;50:1131-1135.

(5) Nikoletou D, Man WD, Mustfa N, Moore J, Rafferty G, Grant RL, Johnson L, Moxham J. Evaluation of the effectiveness of a home-based inspiratory muscle training programme in patients with chronic obstructive pulmonary disease using multiple inspiratory muscle tests. Disability and rehabilitation. 2016 Jan 30;38(3):250-9.

(6) Polkey MI, Moxham J. Improvement in volitional tests of muscle function alone may not be adequate evidence that inspiratory muscle training is effective. Eur Respir J 2004; 23: 5-6.

(7) Hart N, Sylvester K, Ward S, et al. Evaluation of an inspiratory muscle trainer in healthy humans. Respir Med 2001; 95: 526-531.

(8) Similowski T, Fleury B, Launois S, Cathala HP, Bouche P, Derenne JP. Cervical magnetic stimulation: a new painless method for bilateral phrenic nerve stimulation in conscious humans. J Appl Physiol 1989; 67:1311-1318

(9) Hamneg?rd CH, Wragg SD, Mills GH, et al. Clinical assessment of diaphragm strength by cervical magnetic stimulation of the phrenic nerves. Thorax. 1996;51(12):1239-1242.

(10) Mills GH, Kyroussis D, Hamnegard CH, et al. Bilateral magnetic stimulation of the phrenic nerves from an anterolateral approach. Am J Respir Crit Care Med 1996;154:1099-105.

(11) Luo YM, Moxham J, Polkey MI. Diaphragm electromyography using an oesophageal catheter: current concepts. Clin Sci (Lond). 2008 Oct;115(8):233-44.

(12) Polkey MI, Moxham J, Green M. The case against inspiratory muscle training in COPD. European Respiratory Journal Feb 2011, 37 (2) 236-237;

(13) Gosselink R, De Vos J, van denHeuvel SP, et al. Impact of inspiratory muscle training in patients with COPD: what is the evidence? Eur Respir J 2011; 37: 416-425

Conflict of Interest:

None declared

F.Guarino and R.Polosa

We read with great curiosity the article by Garcia-Arcos et al. (1) suggesting nicotine as a novel causative factor for the onset and progression of COPD/emphysema. Chronic nicotine exposure from nebulized e- liquid (in toxic concentrations) appears to modify inflammation, ion conductance and mucociliary function in HBECs and induces airway hyper- reactivity and air space enlargement in A/J mice.

To reach any meaningful conclusion about toxicity of nicotine, it is important that the toxic effect has to be compounded with that of an equivalent dose from cigarette smoking or vaping. Because a 60-kg person absorbs approximately 1 mg of nicotine (0.017 mg nicotine/kg bodyweight) from smoking one cigarette (2), the max dose of nicotine equivalent to smoking 25 cigarettes per day (i.e. the mean level of cigarette consumption in the US (3)) should be 0.017 x 25 cigarettes = 0.425 ? 0.43 mg nicotine/kg bodyweight in humans. In this study, A/J mice were whole body exposed daily to 0.4 mL of an e-liquid containing 18 mg/mL nicotine (i.e. 7.2 mg). If we assume that A/J mice nicotine intake is only 10% (best case scenario), total daily absorption is 0.72 mg, which nearly doubles the nicotine/kg bodyweight in humans. Moreover, when we consider that the average adult A/J mice is about 25 g of weight, then the daily dose exceed by approx. 80 times that of a 25 cigarette/day smoker. This has nothing to do with realistic dosing and essentially equates acute intoxication.

Previous animal studies have shown contradictory results. In particular, when using different mice strain, it is not possible to replicate features of COPD in a nicotine-dependent manner. Interestingly, chronic intraperitoneal injections of much lower concentrations of nicotine have been shown to induce similar air space enlargement in A/J mice (4). Therefore, it is likely that the A/J mice has an innate predisposition at developing emphysematous features when challenged with a range of noxious stimuli.

Moreover, given that it is well established that the protease:anti protease ratio is the central component of our understanding of emphysema.This hypothesis is also at variance with the epidemiological evidence: for example biomass fuel combustion is a well known non nicotine-dependent causative factor for COPD (5,6)

References:

1. Garcia-Arcos I, Geraghty P, Baumlin N, Campos M, Dabo AJ, Jundi B, Cummins N, Eden E, Grosche A, Salathe M, Foronjy R. Chronic electronic cigarette exposure in mice induces features of COPD in a nicotine- dependent manner. Thorax. 2016 Aug 24. pii: thoraxjnl-2015-208039. doi: 10.1136/thoraxjnl-2015-208039. [Epub ahead of print]

2. Benowitz NL, Hukkanen J, Jacob P., 3rd Nicotine chemistry, metabolism, kinetics and biomarkers. Handb Exp Pharmacol. 2009:29-60.

3. American Lung Association; Trends in Tobacco Use [Internet] 2011 Jul; Available from: http://www.lung.org/finding-cures/our-research/trend -reports/Tobacco-Trend-Report.pdf.

4. Iskandar AR, Liu C, Smith DE, Hu KQ, Choi SW, Ausman LM, Wang XD. ?-cryptoxanthin restores nicotine-reduced lung SIRT1 to normal levels and inhibits nicotine-promoted lung tumorigenesis and emphysema in A/J mice. Cancer Prev Res (Phila). 2013 Apr;6(4):309-20.

5. Kurmi OP, Semple S, Simkhada P, Smith WC, Ayres JG. COPD and chronic bronchitis risk of indoor air pollution from solid fuel: a systematic review and meta-analysis. Thorax. 2010 Mar;65(3):221-8.

6. Salvi SS, Barnes PJ. Chronic obstructive pulmonary disease in non- smokers. Lancet. 2009 Aug 29;374(9691):733-43.

Conflict of Interest:

None declared