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What are the questionnaire items most useful in identifying subjects with occupational asthma?

¹ Service de Pneumologie, Cliniques universitaires de Mont-Godinne, Université Catholique de Louvain, Yvoir, Belgium. ² Dept of Chest Medicine, Hôpital du Sacré-Coeur de Montréal, Canada. ³ Hopital Universitari Vall d'Hebron, Barcelona, Spain. ⁴ Salvatore Maugeri Foundation at Medical Centre of Pavia, Pavia, Italy.

CORRESPONDENCE: J-L. Malo, Dept of Chest Medicine, Hôpital du Sacré-Coeur de Montréal, 5400 West Gouin Blvd W., Montreal, H4J 1C5, Canada. Fax: 1 5143383123. E-mail: malojl{at}meddir.umontreal.ca

Keywords: Asthma, bronchial diseases, occupational asthma, occupational diseases

Received: March 2, 2005
Accepted August 7, 2005

	ABSTRACT

TOP ABSTRACT SUBJECTS AND METHODS RESULTS DISCUSSION APPENDIX 1. INFORMATION... APPENDIX 2. CLASSIFICATION TREE... APPENDIX 3. CLASSIFICATION TREE... ACKNOWLEDGEMENTS REFERENCES

 
The present study assessed the usefulness of key items obtained from a clinical "open" questionnaire prospectively administered to 212 subjects, referred to four tertiary-care hospitals for predicting the diagnosis of occupational asthma (OA). Of these subjects, 72 (34%) were diagnosed as OA (53% with OA due to high-molecular-weight agents) according to results of specific inhalation challenges, and 90 (42%) as non-OA.

Wheezing at work occurred in 88% of subjects with OA and was the most specific symptom (85%). Nasal and eye symptoms were commonly associated symptoms. Wheezing, nasal and ocular itching at work were positively, and loss of voice negatively associated with the presence of OA in the case of high-, but not low molecular-weight agents.

A prediction model based on responses to nasal itching, daily symptoms over the week at work, nasal secretions, absence of loss of voice, wheezing, and sputum, correctly predicted 156 out of 212 (74%) subjects according to the presence or absence of OA by final diagnosis.

In conclusion, key items, i.e. wheezing, nasal and ocular itching and loss of voice, are satisfactorily associated with the presence of occupational asthma in subjects exposed to high-molecular-weight agents. Therefore, these should be addressed with high priority by physicians. However, no questionnaire-derived item is helpful in subjects exposed to low-molecular-weight agents.

Various diagnostic tools have been proposed for a stepwise approach in the investigation of occupational asthma (OA) 1, 2. The first is the clinical history, which inquires about the nature of respiratory symptoms and their relationship to work and specific occupational exposures. Questions related to the presence of eye and nasal symptoms were also included because they often accompany respiratory symptoms, especially in the case of workplace high-molecular-weight proteinaceous agents 3. In the latter instance, occupational rhinoconjunctivitis is often associated with OA 4, 5.

Although several items were proposed 2 and generally included in these clinical questionnaires, their usefulness in regards to their association with the presence or absence of OA has not been properly assessed. A study has evaluated the association of one frequently used item, i.e. improvement in symptoms at weekends and on vacations, with the presence or absence of OA 6. It was found that improvement of symptoms at weekends and on vacations had sensitivities of 77 and 88% and specificities of 44 and 24%, respectively. In the present study, the general impression from questionnaire data obtained by the two physicians who were involved in the clinical investigation showed that an "open" questionnaire had a sensitivity of 87%, but a specificity of only 27% regarding the presence or absence of OA 6. However, a detailed analysis of the association of several relevant questionnaire items, alone and in combination, with the presence or absence of OA has not been carried out to the best of the current authors' knowledge.

Therefore, the purpose of the present study was to assess the usefulness of a variety of questionnaire items in predicting the presence or absence of OA. For this, 212 subjects referred for possible OA in four tertiary-care hospitals in different countries were first questioned by clinicians in a systematic way using a detailed list of items. The subjects subsequently underwent nonspecific and specific inhalation challenges in order to identify whether they had OA, asthma, or neither condition.

	SUBJECTS AND METHODS

TOP ABSTRACT SUBJECTS AND METHODS RESULTS DISCUSSION APPENDIX 1. INFORMATION... APPENDIX 2. CLASSIFICATION TREE... APPENDIX 3. CLASSIFICATION TREE... ACKNOWLEDGEMENTS REFERENCES

 
The current study includes the first 212 subjects who were prospectively assessed in outpatient clinics of four hospital centres and who underwent objective testing with specific inhalation challenges in: a hospital laboratory (n = 196); the workplace (n = 10); or in both (n = 6). Of these, 102 (48%) were seen in Yvoir, Belgium; 80 (38%) in Montreal, Canada (by three different chest physicians); 22 (10%) in Pavia, Italy; and 8 (4%) in Barcelona, Spain.

The items of information that were planned and obtained prospectively from each participant are listed in Appendix 1. Each investigator had a form containing the list of all items for which they had to elicit a response at the time of the interview with the worker. These items were derived from a list suggested for the clinical assessment of OA 2 and included information on: 1) the type of job, work shift and agents that the workers identified as potential causes of symptoms; 2) the nature of symptoms during working periods, i.e. chest symptoms (cough, sputum, chest tightness, wheezing, shortness of breath at rest and/or on exertion, change in voice), general symptoms (fever, chills, muscle or joint pain), nasal symptoms (blocked nose, runny nose, sneezing, nasal or throat itching), eye symptoms (itching, runny eyes, redness of the eyes), and skin symptoms (rash, eczema). Information was also obtained on the timing of the onset of symptoms in relation to the beginning of the occupation and the interval between the last occupational exposure and the questionnaire. The relationship between work and respiratory, nasal, conjunctival or skin symptoms was also addressed by asking whether symptoms differed on days at work and away from work, whether there was a specific product causing onset of symptoms and whether there was an improvement in or disappearance of symptoms at weekends and on vacation. The temporal pattern of asthmatic symptoms was also addressed (time interval necessary to develop symptoms after starting work, persistence of symptoms after the work shift and presence of symptoms only on return from work). Interviews were conducted in French in Yvoir and Montreal (except in a few instances in which English was used), in Catalan in Barcelona and in Italian in Pavia.

Atopy was defined by the presence of a significant skin-prick test response (3 mm wheal 10 min after the introduction of the antigen in the presence of a reaction to histamine phosphate 1 mg·mL^–1, and in the absence of a reaction to the diluent) to at least one of a battery of local inhalant allergens, which included 10–20 allergens depending on the centre. Spirometry 7 and bronchial responsiveness to methacholine 8 were assessed. The provocative concentration of methacholine causing a fall of 20% in forced expiratory volume in one second (PC₂₀) of 16 mg·mL^–1 was considered suggestive of bronchial hyperresponsiveness 9. Specific inhalation challenges were carried out using recommended methodologies 10–12. A sustained fall in forced expiratory volume in one second of 20% was confirmation of a positive specific challenge.

Analysis of results
A diagnosis of OA was made in the presence of a positive specific inhalation challenge. A diagnosis of non-OA was kept if the specific inhalation challenge was negative, but the PC₂₀ was 16 mg·mL^–1. If both the methacholine and the specific inhalation challenges were negative, the subject was categorised as having neither occupational nor non-OA. Univariate and multivariate regression analyses were used to examine the association between individual factors and a combination of factors derived from the questionnaire, and the presence or absence of OA and of probable asthma (defined as the presence of symptoms and bronchial hyperresponsiveness). Classification and regression trees 13 using the program Recursive Partitioning and Regression Trees in R 14 were used to examine which sequence of symptoms was the best predictor of the presence of OA. The order in the sequence of symptoms is given by the program in the process of building the classification tree. For this analysis, all factors were included in the model.

	RESULTS

TOP ABSTRACT SUBJECTS AND METHODS RESULTS DISCUSSION APPENDIX 1. INFORMATION... APPENDIX 2. CLASSIFICATION TREE... APPENDIX 3. CLASSIFICATION TREE... ACKNOWLEDGEMENTS REFERENCES

 
Table 1 shows baseline anthropometric and clinical characteristics of the 212 subjects. There was a preponderance of males, atopic and nonsmoking subjects in the whole group. Subjects had been exposed at work for a mean duration of nearly 12 yrs and took nearly 9 yrs at work before developing symptoms. On average, 8 months elapsed between the subjects' discontinuing work and filling out the questionnaire. This interval was significantly longer in Yvoir (15±17.5 months). Most subjects had bronchial hyperresponsiveness. The diagnosis of OA was confirmed in 72 subjects and 90 subjects had what can be interpreted as non-OA (symptoms and bronchial hyperresponsiveness) 15. Flour, latex and isocyanates were the most common causal agents, accounting for 60% of all cases. There were some disparities between types of agents in the various referral centres. Of the 32 cases for whom latex was the suspected agent, 23 (72%) were investigated at Yvoir and 22 (61%) of the 36 cases exposed to isocyanates were investigated in Montreal.

View larger version (19K): [in this window] [in a new window]   Fig. 1— Schematic diagram illustrating the results of the decision tree analysis for 212 subjects in total. Using the pathway, it is shown that a total of six questionnaire items proved useful in the classification of the presence or absence of occupational asthma (OA) with the final yield given in table 6. #: 99 or 74% correct; ¶: 16 or 73% correct; +: 10 or 83% correct; : 10 or 77% correct; : 5 or 71% correct; ##: 6 or 55% correct; ¶¶: 10 or 71% correct.

	DISCUSSION

TOP ABSTRACT SUBJECTS AND METHODS RESULTS DISCUSSION APPENDIX 1. INFORMATION... APPENDIX 2. CLASSIFICATION TREE... APPENDIX 3. CLASSIFICATION TREE... ACKNOWLEDGEMENTS REFERENCES

The diagnosis of OA is an important challenge to physicians. Several functional, immunological and inflammatory marker tools have been proposed alone or in conjunction in a stepwise approach specific inhalation challenges represent the most specific test 1, 2. The first diagnostic approach is the questionnaire addressed by a physician. A list of items to be included in such questionnaires has been proposed 2, but the usefulness of specific proposed items has not been assessed in details as this was proposed in the current study. To the current authors' knowledge, only one item has been prospectively examined in a previous study. Malo et al. 6 found that improvement of symptoms at weekends and on vacations had sensitivities of 77 and 88% and specificities of 44 and 24%, respectively. This compares, respectively, closely to sensitivity and specificity values of 75 and 55% in the current study. All subjects underwent specific inhalation challenges to confirm or eliminate OA. Although this test can be falsely negative at times, it is generally considered the gold standard in the diagnosis of OA.

The intention of the present study was not to validate a questionnaire to be used in the investigation of OA, but rather to assess the relative importance of items generally addressed by clinicians in an "open" interview, as this represents the usual situation of a clinical context. To do so, a series of items were used that have been proposed by others 2, and that were systematically and prospectively addressed by clinicians at the time of their interview of referred subjects. Although some items seem particularly useful, it would probably not be practical to suggest developing with these a standardised questionnaire, such as those used for epidemiological studies. Indeed, contrary to the situation in an epidemiological study, where questions have to be addressed in a standardised manner to ensure validity of results, an "open" questionnaire is the preferred clinical mean.

A clear distinction was found in the identification of questionnaire items for high- and low-molecular-weight agents. High-molecular-weight agents often cause nasal and eye symptoms 3, 5. In the current study, besides wheezing, nasal and ocular itching, runny nose was significantly associated with the presence of OA due to high-molecular-weight agents. Loss of voice was more prevalent in subjects without OA, suggesting that upper airway dysfunction could be responsible for work-related respiratory symptoms in some subjects. The current authors do not have an explanation for the fact that there were fewer instances of loss of voice in the group with OA. It cannot be attributed to inhaled steroids, as 56% of the subjects with OA were on inhaled steroids at the time of the visit as compared with 57% in the group of subjects with non-OA and 20% in the group with neither condition. In the case of low-molecular weight agents, no questionnaire item was found to be significantly predictive of the presence or absence of OA. The reasons for this are only speculative. First, low-molecular weight agents cause nasoconjunctival symptoms less often than high-molecular weight agents 3. Nasoconjunctival symptoms commonly accompanied asthma due to high-molecular-weight agents and are predictive of the presence or absence of OA. Secondly, low-molecular-weight agents are chemicals that may more easily cause nonspecific irritation of the airways with symptoms in subjects with non-OA, making distinction between OA and work-aggravated asthma more difficult. Thirdly, low-molecular-weight agents causing OA often induce late asthmatic reactions 12 that, contrary to immediate reactions, are more difficult to relate temporarily to work.

The decision-tree analysis showed an overall validity of 59% for the model that predicted OA, asthma and neither condition. This was less than the 74% obtained by categorising the subjects into those with and without OA. However, the figure obtained in the present study for the prediction of asthma (62%) was slightly lower than the figure for the prediction of OA (71%). The cross-validation analysis of the classification and regression analysis procedure testifies to the inherent difficulties of employing a culturally sensitive tool, such as a questionnaire, across heterogeneous populations (subjects were recruited in one North American and three European countries), exposed to various agents and living in countries where the expression of perceived symptoms and health as well as medicolegal systems differ. Besides geographical and cultural factors, the possibility that other determinants could explain these results cannot be excluded. This includes the following. 1) The longer interval between the end of exposure at work and the administration of the questionnaire at Yvoir, which could have generated a possible recall bias. 2) The nature of the agent; for the purpose of keeping a sufficient number of subjects in the analysis, the exposure was grouped under high- and low-molecular-weight agents, but this does not take into account the possibility that specific agents within each group (viz. flour, latex, isocyanates, persulfates, etc.) could induce different symptoms. Also, there were not enough subjects to cross-validate the analysis in each site independently. The majority of symptoms listed in table 2 were clearly not predictive, which is of great interest in the context of keeping only key features for questionnaires administered in the clinical investigation of OA.

The diagnosis of OA was based on the result of the specific inhalation challenge. Whereas this is generally considered as the gold standard 10–12, the possibility of false negative results cannot be excluded, especially in subjects who underwent testing several months after ending exposure. However, Lemière et al. 16 have shown that this test generally remains positive in subjects with OA who no longer demonstrate increased nonspecific responsiveness to methacholine even years after stopping exposure 16.

In conclusion, occupational asthma still poses important diagnostic challenges. Although several tools are available, they are not sufficiently nor properly used. Whereas some tests (e.g. peak expiratory flow assessment) have undergone a proper validation process, more has to be done using the simple and inexpensive tool, the clinical questionnaire. The current results show that improvement in symptoms at weekends and on vacations is sensitive, but the presence of wheezing at work is more specific. Inclusion of these questions might, therefore, result in either more sensitive or more specific results depending on the purpose of the study. More sensitive questions would be preferable in a surveillance programme, however, once subjects are referred to specialised centres, the use of more specific questions is relevant. This being said, sensitivity and specificity of questionnaire items still remains low and need to be improved, therefore, justifying the use of other diagnostic tools.

View larger version (24K): [in this window] [in a new window]   Fig. 2— Classification tree for subjects of Montreal. A: asthma; OA: occupational asthma. #: 9 or 53% correct; ¶: 7 or 78% correct; +: 10 or 91% correct; : 5 or 50% correct; : 10 or 63% correct.

View larger version (24K): [in this window] [in a new window]   Fig. 3— Classification tree for subjects of Europe. OA: occupational asthma; A: asthma. #: 6 or 55% correct; ¶: 5 or 90% correct; +: 10 or 77% correct; : 21 or 81% correct; : 3 or 43% correct; ##: 6 or 60% correct; ¶¶: 32 or 58% correct.

	APPENDIX 1. INFORMATION COLLECTED FROM THE QUESTIONNAIRE

TOP ABSTRACT SUBJECTS AND METHODS RESULTS DISCUSSION APPENDIX 1. INFORMATION... APPENDIX 2. CLASSIFICATION TREE... APPENDIX 3. CLASSIFICATION TREE... ACKNOWLEDGEMENTS REFERENCES

Job title

Duration of work under the same job title

Products made by the company

Workshift

Products causing symptoms

2. Nature of symptoms

2.1. Respiratory

Cough

Sputum

Chest tightness

Wheezing

Shortness of breath at rest

Shortness of breath on exercise

Loss of voice

2.2. Systemic

Fever

Chills

Muscle or joint aches

2.3. Rhinitis

Nasal obstruction

Runny nose

Sneezing

Nasal/pharyngeal itching

2.4. Conjunctivitis

Ocular itching

Watery eyes

Redness of the eyes

2.5. Skin symptoms

Rash/urticaria

Eczema

3. Timing of symptoms in relation to work

Interval between onset of exposure at work and onset of symptoms

Interval between onset of symptoms and current questionnaire

Interval between last occupational exposure and current questionnaire

4. Relationship of work and respiratory symptoms

4.1. Status of respiratory symptoms on working days as compared with days away from work

Better, Worse, The same

If better or worse:

1. Every day;

2. Progressively over the week;

3. As a function of working conditions; if yes,

On physical exertion

On exposure to mist, hot or cold temperature

On exposure to dust, fumes, gas

4.2. Possibility to identify a process or a product that is responsible for respiratory symptoms

Yes, No

If yes, identify the process or product

If yes, is this exposure regular or intermittent?

4.3. Status of respiratory symptoms on weekends

They disappear

They improve

No change

4.4. Status of respiratory symptoms on vacations (more than one week)

They disappear

They improve

No change

If they disappear or improve, after how many days?

4.5. Timing of respiratory symptoms in relation to work

Interval between onset of work and onset of symptoms

Persistence or reappearance of symptoms on return to home

Onset of symptoms only on returning home

Change of timing of symptoms over time

5. Relationship of work and nasal, conjunctival or skin symptoms

5.1. Status of symptoms on working days as compared with days away from work

Better, Worse, The same

If better or worse:

1. Every day;

2. Progressively over the week;

3. As a function of working conditions; if yes,

On physical exertion

On exposure to mist, hot or cold temperature

On exposure to dust, fumes, gas

6. Other information

6.1. Smoking habits: smoker, non-smoker, ex-smoker; number of pack-years

6.2. Presence of chronic bronchitis

6.3. Asthma before starting work that causes symptoms

6.4. Respiratory drugs at the time of investigation

	APPENDIX 2. CLASSIFICATION TREE OF PRESENCE AND ABSENCE OF OCCUPATIONAL ASTHMA (OA) OR ASTHMA (A) FOR SUBJECTS FROM MONTREAL

TOP ABSTRACT SUBJECTS AND METHODS RESULTS DISCUSSION APPENDIX 1. INFORMATION... APPENDIX 2. CLASSIFICATION TREE... APPENDIX 3. CLASSIFICATION TREE... ACKNOWLEDGEMENTS REFERENCES

 

	APPENDIX 3. CLASSIFICATION TREE OF PRESENCE AND ABSENCE OF OCCUPATIONAL ASTHMA (OA) OR ASTHMA (A) FOR SUBJECTS FROM EUROPE

TOP ABSTRACT SUBJECTS AND METHODS RESULTS DISCUSSION APPENDIX 1. INFORMATION... APPENDIX 2. CLASSIFICATION TREE... APPENDIX 3. CLASSIFICATION TREE... ACKNOWLEDGEMENTS REFERENCES

 

	ACKNOWLEDGEMENTS

TOP ABSTRACT SUBJECTS AND METHODS RESULTS DISCUSSION APPENDIX 1. INFORMATION... APPENDIX 2. CLASSIFICATION TREE... APPENDIX 3. CLASSIFICATION TREE... ACKNOWLEDGEMENTS REFERENCES

 
The authors would like to thank L. Schubert for reviewing this manuscript.

	REFERENCES

TOP ABSTRACT SUBJECTS AND METHODS RESULTS DISCUSSION APPENDIX 1. INFORMATION... APPENDIX 2. CLASSIFICATION TREE... APPENDIX 3. CLASSIFICATION TREE... ACKNOWLEDGEMENTS REFERENCES

 

1. Chan-Yeung M, Malo JL. Occupational asthma. N Engl J Med 1995;333:107–112.[Free Full Text]
2. Bernstein DI. Clinical assessment and management of occupational asthma. In: Bernstein IL, Chan-Yeung M, Malo JL, Bernstein DI, eds. Asthma in the Workplace. 2nd Edn. New York, Marcel Dekker Inc., 1999; pp. 145–157
3. Malo JL, Lemière C, Desjardins A, Cartier A. Prevalence and intensity of rhinoconjunctivitis in subjects with occupational asthma. Eur Respir J 1997;10:1513–1515.[Abstract]
4. Christiani DC, Malo JL. Upper airways involvement. In: Bernstein IL, Chan-Yeung M, Malo JL, Bernstein DI, eds. Asthma in the Workplace. New York, Marcel Dekker Inc., 1999; pp. 331–339
5. Siracusa A, Desrosiers M, Marabini A. Epidemiology of occupational rhinitis: prevalence, aetiology and determinants. Clin Exp Allergy 2000;30:1519–1534.[CrossRef][Web of Science][Medline] [Order article via Infotrieve]
6. Malo JL, Ghezzo H, L'Archevêque J, Lagier F, Perrin B, Cartier A. Is the clinical history a satisfactory means of diagnosing occupational asthma? Am Rev Respir Dis 1991;143:528–532.[Web of Science][Medline] [Order article via Infotrieve]
7. American Thoracic Society. Standardization of spirometry. Am J Respir Crit Care Med 1995;152:1107–1136.[Web of Science][Medline] [Order article via Infotrieve]
8. American Thoracic Society. Guidelines for methacholine and exercise challenge testing. Am J Respir Crit Care Med 1999;161:309–329.[Web of Science]
9. Dehaut P, Rachiele A, Martin RR, Malo JL. Histamine dose-response curves in asthma: reproducibility and sensitivity of different indices to assess response. Thorax 1983;38:516–522.[Abstract/Free Full Text]
10. Sterk PJ, Fabbri LM, Quanjer PH, et al. Airway responsiveness. Standardized challenge testing with pharmacological, physical and sensitizing stimuli in adults. Report working party standardization of lung function tests European Community for Steel and Coal. Official statement of the European Respiratory Society. Eur Respir J 1993;6: Suppl. 16 53–83.[Abstract]
11. Vandenplas O, Malo JL. Inhalation challenges with agents causing occupational asthma. Eur Respir J 1997;10:2612–2629.[Abstract]
12. Cartier A, Malo JL. Occupational challenge tests. In: Bernstein IL, Chan-Yeung M, Malo JL, Bernstein DI, eds. Asthma in the Workplace. 2nd Edn. New York, Marcel Dekker Inc., 1999; pp. 211–233
13. Breiman L, Friedman JH, Olshen RA, Stone CJ. Classification and regression trees. Wadsworth and Brooks, Monterey, CA, USA, 1984
14. Computing R development Core Team. R Foundation for Statistical. R: A language and environment for statistical computing. Vienna, Austria 2004. http://www.R-project.org
15. National Institutes of Health National Heart, Lung and Blood Institute. Global initiative for asthma (GINA). Global strategy for asthma management and prevention. NHLBI/SHO workshop report. National Institutes of Health publication, no. 95-3659, 1995
16. Lemière C, Cartier A, Malo JL, Lehrer SB. Persistent specific bronchial reactivity to occupational agents in workers with normal nonspecific bronchial reactivity. Am J Respir Crit Care Med 2000;162:972–980.

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This Article Abstract Full Text (PDF) Alert me when this article is cited Alert me if a correction is posted Permissions Request Permissions Citation Map Services Email this article to a friend Similar articles in this journal Similar articles in Web of Science Similar articles in PubMed Alert me to new issues of the journal Download to citation manager Citing Articles Citing Articles via HighWire Citing Articles via Web of Science (7) Citing Articles via Google Scholar Google Scholar Articles by Vandenplas, O. Articles by Malo, J-L. Search for Related Content PubMed PubMed Citation Articles by Vandenplas, O. Articles by Malo, J-L.