Dear Editors,
This journal published the BTS guidelines for the management of pulmonary nodules in August 2015 (1), leading to widespread evidence-based management of this common clinical problem. The use of the Herder score (2) to estimate or predict the likelihood of malignancy has since become routine in lung cancer MDMs around the country.
We therefore wish to highlight that the Herder prediction model was developed using the intensity of FDG uptake (absent, faint, moderate or intense) from the uncorrected PET images. However, as far as we are aware, lung cancer MDMs routinely assess the intensity of FDG uptake from the corrected images which is not in accordance with the original Herder model.
The use of uncorrected images in the original Herder study (2) to distinguish between uptake categories potentially alters the perceived evidence base of the recommendations in the BTS guidelines (1) to distinguish between faint and moderate uptake according to mediastinal blood pool given that this scale of uptake was not used in the original score, has not been validated and could mean we are not using the correct category in the risk model.
Furthermore, when considering the widespread use of the Herder score, it should be appreciated that it was formulated from patients scanned between 1997 and 2001. The Herder paper describes that “emission scans were acquired in a two-dimensional mode … and were reconstructed using ordered subset expectation maximisation with two iterations and 16 subsets followed by post smoothing… using a Hanning 0.5 filter”.
PET cameras and reconstruction techniques have advanced considerably since then and the imaged intensity of FDG uptake within nodules <3cm in diameter acquired on modern cameras is likely to be quite different to twenty years ago. In particular it is now standard to have 3-dimensional mode acquisition and reconstructions which routinely include point spread function and time-of-flight data. This results in an increase in the SUVmax of small nodules and a potential upgrade in the avidity category of these lesions.
A validation study by Al-Ameri et al published in 2015 (3) provides some reassurance the use of corrected images on modern scanners is still sufficiently accurate as they used corrected images to distinguish between faint, moderate and intense FDG uptake by the use of SUVmax ≤2.5, 2.6-10 and >10 as parameters respectively.
There is now widespread use of PET-CT to characterise pulmonary nodules and increasing use of electronic databases to record patient characteristics and outcomes. We suggest that this data could be used to produce an updated version of the Herder model. For simplicity, and given its previous proven accuracy in the validating study, the same variables (age, smoking, previous history of cancer, diameter, spiculation, upper lobe) as in the original Herder model could be used. Large sample sizes and potential multi-centre data aggregation would result in model more accurate and appropriate to modern cameras than the original Herder score.
We therefore suggest that the recommendation to use the Herder model to characterise pulmonary nodules is reviewed addressing:
1. Clarifying whether the corrected or uncorrected PET images should be used.
2. Determining whether the scale for distinguishing between faint and moderate uptake using mediastinal blood pool is sufficiently evidence-based.
3. Supporting the development of an updated model using data acquired on modern day PET-CT scanner technology.

References:
1. Callister ME, Baldwin DR, Akram AR, Barnard S, Cane P, Draffan J, et al. British Thoracic Society guidelines for the investigation and management of pulmonary nodules. Thorax. 2015;70 Suppl 2:ii1-ii54.
2. Herder GJ, van Tinteren H, Golding RP, Kostense PJ, Comans EF, Smit EF, et al. Clinical prediction model to characterize pulmonary nodules: validation and added value of 18F-fluorodeoxyglucose positron emission tomography. Chest. 2005;128(4):2490-6.
3. Al-Ameri A, Malhotra P, Thygesen H, Plant PK, Vaidyanathan S, Karthik S, et al. Risk of malignancy in pulmonary nodules: A validation study of four prediction models. Lung Cancer. 2015;89(1):27-30.

Title: Extracorporeal CO2 removal (ECCO2R) in patients with stable COPD with chronic hypercapnia: applying the concept.
Pradipta Bhakta, Antonio M. Esquinas, Brian O’Brien.
Authors:
1. Dr. Pradipta Bhakta (MD, MNAMS, FCAI, EDRA, EDIC)
Consultant,
Department of Anaesthesia and Intensive Care,
University Hospital Kerry, Tralee, Kerry, Ireland.
Phone: 00353894137596.
Email: bhaktadr@hotmail.com
2. Dr. Antonio M. Esquinas (PhD, MD)
Consultant,
Department of Intensive Care,
Hospital Morales Meseguer,
Murcia, Spain.
Phone: 0034609321966
Email: antmesquinas@gmail.com
3. Dr. Brian O’Brien [FCARCSI, FJFICMI, FCICM (ANZ)]
Consultant and Chair,
Department of Anaesthesia and Intensive Care,
Cork University Hospital, Cork, Ireland.
Mobile: 00353877931656
Email: drbobrien@hotmail.com
Authors and their role:
1. Dr. Pradipta Bhakta: Was involved analysis of the article, writing and editing the letter.
2. Dr. Antonio M. Esquinas: Was involved analysis of the article, writing and editing the letter.
3. Dr. Brian O’Brien: Was involved analysis of the article, writing and editing the letter.
Corresponding Author: Dr. Pradipta Bhakta,
Consultant,
Department of Anaesthesia and Intensive Care,
University Hospital Kerry, Tralee, Kerry, Ireland.
Phone: 00353894137596
Email: bhaktadr@hotmail.com
Category of the article: Correspondence in response to article by Pisani L et al.
Running Title: Letter replying to Pisani L et al.
Financial support: No funding other than personal was used in conducting the audit as well as writing the manuscript. We declare that we have no financial and/or personal relationships with other people or organizations that could inappropriately influence (bias) our work.
Conflict of Interest: The authors report no conflicts of interest.
Ethical Approval: Not applicable.
Word Count: 500.
Figure no: 0.
Table No: 0.

Keywords: Chronic Obstructive Pulmonary Disease; Hypercapnia; Extracorporeal CO2 Removal, Non-Invasive Ventilation.

To The Editor,
We read with interest the proof-of-concept by Pisani and colleagues and congratulate them on this important work.1 We believe that several methodological details warrant analysis to facilitate extrapolation of their findings into the clinical context.
In particular, it appears the authors characterise non-invasive ventilation (NIV) entirely as a mode of carbon dioxide (CO2) removal. We would emphasize its value as a modality to improve oxygenation. Many patients with chronic obstructive pulmonary disease (COPD) are hypoxic in part because of alveolar displacement of oxygen by expired CO2.2 The consequent type 2 respiratory failure, characteristic of advanced COPD with alveolar hypoventilation, by definition incorporates accompanying hypoxia.3 In evaluating the efficacy of ECCO2R in such patients, they only concentrated on the hypercapnic rather than the hypoxic aspect. NIV however offers both benefits.4 In selecting hypercapnic patients who have failed NIV therapy for the ECCO2R group, we would suggest that in such severe cases symptomatic relief and long-term CO2 reduction cannot occur without improved oxygenation. Effectively oxygen (O2) replaces CO2 eliminated from the alveoli, haemoglobin and cells. But if this aspect is ignored, the use of ECCO2R for 24 hours cannot contribute in the longer term. If we have understood correctly, in the ECCO2R rather than use additional O2, air flow was used to eliminate CO2. Patients in the ECCO2R group, having failed NIV trials in the preceding 6 months, were spontaneously breathing room air. This raises the question of how they were able to tolerate this. In this context we also wonder if the cases were matched for disease severity. Is it possible that milder cases were included, perhaps who were intolerant of NIV due to claustrophobia, discomfort or asynchrony? These points might be clarified further.
A second broad point we would raise is the acceptance of normalized pH in chronic COPD patients with chronic acid-base disturbances, which are typically compensated by the kidney and by buffers in the circulation.5 We agree that in patients with severely diseased functional lung tissue the elimination of CO2 can provide temporary improvement in the arterial blood gas values, but wonder how the authors might speculate on future innovations to extend or capitalise on these benefits.
Thirdly, while studying severe cases of COPD, the study included patients with pH levels above 7.35 while their PaCO2 exceeded 50 mmHg. There is no value given for HCO3 which is clearly important. Ideally full data might be provided to allow categorisation as per the GOLD staging classification.6
Fourthly, in highlighting the role of ECCO2R in severe COPD patients, they have emphasised the failure of NIV. It ought to be observed that ECCO2R has similarly failed to benefit patients with acute respiratory distress syndrome.7 In severe cases of COPD, CO2 load is not the sole mediator of improved outcomes nor of symptomatic benefit, although it is a major issue with multiple adverse effects.3 We would welcome the authors’ views on these points and their thoughts on how their findings may become relevant to clinical practice in the future.
Pradipta Bhakta,
Antonio M. Esquinas,
Brian O’Brien.
References
1. Pisani L, Nava S, Desiderio E, Polverino M, Tonetti T, Ranieri VM. Extracorporeal CO2 removal (ECCO2R) in patients with stable COPD with chronic hypercapnia: a proof-of-concept study [published online ahead of print, 2020 Aug 5]. Thorax. 2020;thoraxjnl-2020-214744. doi:10.1136/thoraxjnl-2020-214744.
2. Kent BD, Mitchell PD, McNicholas WT. Hypoxemia in patients with COPD: cause, effects, and disease progression. Int J Chron Obstruct Pulmon Dis. 2011;6:199-208.
3. Agustí A, Hogg JC. Update on the Pathogenesis of Chronic Obstructive Pulmonary Disease. N Engl J Med. 2019;381(13):1248-1256.
4. Coleman JM 3rd, Wolfe LF, Kalhan R. Noninvasive Ventilation in Chronic Obstructive Pulmonary Disease. Ann Am Thorac Soc. 2019;16(9):1091-1098.
5. Bruno CM, Valenti M. Acid-base disorders in patients with chronic obstructive pulmonary disease: a pathophysiological review. J Biomed Biotechnol. 2012;2012:915150.
6. Singh D, Agusti A, Anzueto A, et al. Global Strategy for the Diagnosis, Management, and Prevention of Chronic Obstructive Lung Disease: the GOLD science committee report 2019. Eur Respir J. 2019;53(5):1900164.
7. Fitzgerald M, Millar J, Blackwood B, et al. Extracorporeal carbon dioxide removal for patients with acute respiratory failure secondary to the acute respiratory distress syndrome: a systematic review. Crit Care. 2014;18(3):222.

Caretto et al’s brief communication[1] shines some additional light on an unresolved question of the role of alpha-1 antitrypsin deficiency (AATD) screening in patients with bronchiectasis. The authors conclude that testing of an unselected UK population (presumably with a primary diagnosis of bronchiectasis) identifies severe AATD in less than 1% of cases and that routine screening does not significantly impact on clinical management. Whilst these conclusions may be broadly applicable, it may be advisable to qualify the recommendation with some further detail to avoid potential misinterpretation and the consequent complete avoidance of AATD testing in patients with bronchiectasis.

The study rationale originates from apparent conflicting recommendations of guidelines for bronchiectasis[2] and those for AATD[3]. It is stated by the authors that the latter advises AATD testing in all cases of bronchiectasis, whereas the guidelines (in recommendation 1c) in fact advocate testing in cases of ‘unexplained’ bronchiectasis. The use of the term ‘unexplained’ implies the use of a staged approach to the investigation of bronchiectasis with AATD testing reserved for a selected bronchiectasis population in which a diagnosis remains elusive despite clinically appropriate initial investigations.

Studies of bronchiectasis in AATD are few in number and relatively small in size. Nevertheless, there is some consistency in the findings. In their conclusions from a study of the distribution of AATD alleles in an unselected bronchiectasis population, the presence of bronchiectasis in PiZ patients was considered by Cuvelier et al[4] to be a consequence of emphysema rather than a primary effect. This association had been previously suggested by small case series[5,6] and, in our subsequent study of 74 individuals with the PiZ phenotype, we were able to demonstrate using quantitative CT imaging that there is a clear association between the severity of emphysema and the severity of bronchiectasis, and a tendency for co-location of the two pathologies[7] (comparable associations between emphysema and bronchiectasis are also seen in patients with non-deficient or usual COPD). Whilst this relationship held true for the majority of our study population, we identified a sub-group of 6 patients in whom the bronchiectasis was of the greatest severity but with a relative paucity of emphysema. This sub-group also included the only 3 patients with cystic bronchiectasis. Our interpretation of these findings was that the sub-group was representative of a distinct clinical phenotype, possibly with individuals who had an alternative underlying cause for their bronchiectasis, perhaps amplified by AATD. On the basis of our results, screening for AATD in patients who have bronchiectasis alone will likely not identify patients with severe AATD and other causes should first be sought. In the absence of any other cause, testing for AATD should then be considered. Testing for AATD in patients with bronchiectasis and co-existing emphysema, particularly when basal and panlobular in nature, should be undertaken according to the advice on testing for AATD in COPD guidelines for the investigation of patients with emphysema.

It would, therefore, seem that AATD testing in patients with bronchiectasis would be best reserved for patients with unexplained bronchiectasis in whom initial investigations have failed to identify a cause, and particularly in patients with co-existing emphysema. Whether the bronchiectasis in such patients would respond positively to AAT augmentation therapy remains unknown but, since bronchiectatic change is relatively common in AATD patients with emphysema, review of sequential scans in those who are or have been taking part in the placebo-controlled trials of augmentation with a focus on sequential bronchiectatic changes may prove informative.

References:

1 Caretto L, Morrison M, Donovan J, et al. Utility of routine screening for alpha-1 antitrypsin deficiency in patients with bronchiectasis. Thorax 2020; 75:592-593.

2 Hill AT, Sullivan AL, Chalmers JD, et al. British thoracic Society guideline for
bronchiectasis in adults. Thorax 2019;74:1–69.

3 Sandhaus RA, Turino G, Brantly ML, et al. The diagnosis and management of alpha-1
antitrypsin deficiency in the adult. Chronic Obstr Pulm Dis 2016;3:668–82.

4 Cuvelier A, Muir JF, Hellot MF, et al. Distribution of alpha(1)-antitrypsin alleles in patients with bronchiectasis. Chest 2000;117:415–9.

5 Guest PJ, Hansell DM. High resolution computed tomography (HRCT) in emphysema associated with alpha-1 antitrypsin deficiency. Clin Radiol 1992; 45:260–266

6 King MA, Stone JA, Diaz PT, et al. a1-Antitrypsin deficiency: evaluation of bronchiectasis with CT. Radiology 1996; 199:137–141

7 Parr DG, Guest PG, Reynolds JH, et al. Prevalence and impact of bronchiectasis in
alpha1-antitrypsin deficiency. Am J Respir Crit Care Med 2007;176:1215–21.

Thank you for inviting us to respond to correspondence from Dr. Andrea Vila, entitled “Active searching for pseudo-asymptomatic contacts during outbreak, as containment measure”.

We would like to establish in greater details what we defined as “asymptomatic” on board our cruise ship. For the first 8 days, prior to the development of fever in the first subject, our 2 ship’s physicians regularly checked for fever in all passengers in a common area, and attended to calls which were predominantly for sea sickness. After day 8, all passengers and crew were seen by one of the two ship’s physicians twice daily, and had body temperature checks. During these visits, symptoms were enquired about. This includes fever, sore throat, cough and myalgias. In mid-March, anosmia was a recognised symptom of Covid-19 infection and was thus included, but dysgeusia and ageusia were not, and thus Vila makes a valid point. However, given that all passengers and crew were seen twice daily between day 8 and day 28, we are confident in the accuracy of the data presented (81% of Covid-19 subjects being asymptomatic), with the above rider. We do not feel that language was a barrier in communication, with the overwhelming number of passengers and crew either having English as their native language, or being fluent in English. In addition one of the ship’s physicians was multilingual.

Vila also accurately states that asymptomatic subjects may be pre-symptomatic. We have follow-up on all passengers and crew until day 28, when 116 passengers disembarked and were repatriated. While we are confident our data is accurate till Day 28, we do not at present have complete follow up after Day 28, and do not have a complete dataset as to how many asymptomatic Covid-19 positive subjects went on to develop symptoms after disembarkation. This is the focus of an ongoing research study.

We agree with Vila, that to truly define a subject as asymptomatic, we should include in the questioning and history taking known specific symptoms to help prompt an accurate response. Vila’s list of atypical symptoms will help identify such subjects.