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Association of domestic exposure to volatile organic compounds with asthma in young children
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     1 School of Public Health, Curtin University of Technology, Perth, WA 6845, Australia

    2 University of WA, School of Population Health, Faculty of Medicine and Dentistry, Crawley, WA 6009, Australia

    3 Princess Margaret Hospital for Children, Department of Respiratory Medicine, GPO Box D184, Perth, WA 6001, Australia

    Correspondence to:

    Dr K Rumchev

    School of Public Health, Curtin University of Technology, GPO Box U1987, Perth, WA 6845, Australia; k.rumchev@curtin.edu.au

    Received 23 July 2003

    Accepted for publication 8 April 2004

    ABSTRACT

    Aim: To investigate the association between domestic exposure to volatile organic compounds (VOCs) and asthma in young children.

    Methods: A population based case-control study was conducted in Perth, Western Australia in children aged between 6 months and 3 years. Cases (n = 88) were children recruited at Princess Margaret Hospital accident and emergency department and discharged with asthma as the primary diagnosis; 104 controls consisted of children from the same age group without an asthma diagnosis identified through the Health Department of Western Australia. Information regarding the health status of the study children and characteristics of the home was collected using a standardised questionnaire. Exposure to VOCs, average temperature and relative humidity were measured in winter and summer in the living room of each participating household.

    Results: Cases were exposed to significantly higher VOC levels (μg/m3) than controls (p<0.01). Most of the individual VOCs appeared to be significant risk factors for asthma with the highest odds ratios for benzene followed by ethylbenzene and toluene. For every 10 unit increase in the concentration of toluene and benzene (μg/m3) the risk of having asthma increased by almost two and three times, respectively.

    Conclusions: Domestic exposure to VOCs at levels below currently accepted recommendations may increase the risk of childhood asthma. Measurement of total VOCs may underestimate the risks associated with individual compounds.

    Keywords: volatile organic compounds; asthma; children; indoor air quality; early life exposure

    Asthma is the most common chronic disease of childhood in the developed world and its prevalence appears to have increased significantly over the past 30 years.1–3 Observations indicate that the rising prevalence has coincided with modifications to the home environment such as the introduction of soft furniture, fitted carpets, air conditioning, and central heating.4 In this context, the indoor environment could be of crucial importance since infants spend 80% of their time indoors at home.5 Hence, knowledge regarding the risks for asthma associated with indoor environmental factors will help us to understand how asthma is initiated.

    Volatile organic compounds (VOCs) are irritants and indoor sources include solvents, floor adhesive, paint, cleaning products, furnishings, polishes, and room fresheners.6 According to Samet,7 levels of most VOCs can be 5–10 times higher indoors than outdoors. Indoor exposure to VOCs has been related to asthma and asthmatic symptoms such as nocturnal breathlessness, increased bronchial responsiveness, and decreased lung function.8,9 Ware and colleagues10 reported an association between ambient concentrations of VOCs and asthma in children aged 7–13 years of age. Two other experimental studies have shown that VOCs may affect the airways and induce inflammation11 and airway obstruction.12

    The realisation that the early initiation phase of asthma is likely to occur during infancy and that infants spend most of their time indoors provides the rationale for our study of indoor air quality and asthma in young children.13 The primary aim of the study was to test the hypothesis that early exposure to VOCs increases the risk of asthma in young children.

    METHODS

    Study population

    A population based case-control study was carried out in the Perth metropolitan area, Western Australia, between 1997 and 1999. Children aged between 6 months and 3 years were recruited in order to identify risk factors for asthma that might be important early in life. The study was population based case-control so cases and controls were not matched by age or any other variables. The age group was restricted for cases and controls by defining an eligible age range (6 months–3 years) within which childhood asthma genesis was believed to occur. In order to standardise the diagnosis of asthma and ensure that the "asthma" group was as homogenous as possible, cases (n = 88) were children who attended the accident and emergency department at Princess Margaret Hospital and who were discharged with asthma as the primary diagnosis but not asthma ever. We used the discharge coding to help create a more homogenous group than would be possible from a community sample. Children were reviewed by a paediatric trainee in the emergency department and presumably were diagnosed as asthmatic based upon past history, family history of atopy, presentation, and response to anti-asthma treatment. Children with the final diagnostic coding of bronchiolitis were excluded. Controls (n = 104) were children of the same age group as cases, without ever having asthma diagnosed by a doctor, identified through the Health Department of Western Australia. The controls were recruited from the metropolitan community rather than the hospital accident and emergency department because the primary care facility within the accident and emergency department serves the whole metropolitan area and there are no other significant services for the management of acute severe asthma, particularly out of normal business hours.

    Written informed consent was obtained from the parents or guardians of all study children. The study protocol was approved by the Princess Margaret Hospital Ethics Committee, Confidentiality of Health Information Committee at the Health Department of Western Australia, and Curtin University Human Research Ethics Committee.

    Health outcomes and house characteristics

    A letter of recruitment was sent to the parent or guardian of each potential participating child. After obtaining informed consent, a modified American Thoracic Society questionnaire (some questions related to ear infections, cystic fibrosis, and pneumonia were omitted)14 was administered to parents or guardians of all study subjects who were asked to return the completed form to the research team. The questionnaire included questions regarding potential risk factors for asthma such as personal (age, sex) and susceptibility factors (child’s allergy, wheeze, cough, family history of asthma, parental asthma and allergy). Questions related to environmental exposures such as smoking inside (parents and visitors); exposure to gas heating and cooking; presence of kerosene space heaters, wood fire heaters, air conditioning, humidifier; type of floor covering, age of the house, and family pets were also included.

    Assessment of indoor exposure

    Indoor exposure measurements of VOCs for cases were performed within 2 weeks of the emergency visit in winter (middle of June to end of September 1998) and then during the opposite season, summer (December 1998 to middle of March 1999). Controls were monitored during the same period of time as the case subjects. VOCs were measured in the living room, 1 m above the floor, by active sampling using charcoal sorbent tubes. The air sampling rate was 1 l/min for 8 hours. The charcoal tubes were desorbed with 1 ml carbon disulfide before analysis which was performed with a Perkin Elmer Autosystem XL gas chromatograph equipped with a flame ionisation detector. Ten VOCs associated with respiratory symptoms with common sources found in the home environment such as carpet, furnishing, paints, consumer products6 were identified and quantified by comparing their retention times. Total VOCs were defined as the sum of the 10 identified compounds.

    The quantity of allergen levels of house dust mite (Der p I) was measured using a monoclonal antibody capture ELISA following the procedure described by Luczynska et al.15 Data were analysed using ELISA-AID software and expressed as μg Der p I/g fine dust.

    The indoor temperature and relative humidity were also measured in the living room using Tinytalk II Data Loggers (Scientific House, Chichester, UK).

    Assessment of atopy

    Skin prick tests were performed on all study children using the following common allergens (Miles Inc, Elkhart, IN, USA): cow’s milk, egg white, rye grass, grass mix, Dermatophagoides farinae, Dermatophagoides pteronyssinus (house dust mite), cat, dog, Alternaria and Aspergillus. A saline solution was used as a negative control and histamine as a positive control. The largest wheal diameter was determined after 15 minutes. The ratio of allergen wheal size divided by the histamine wheal size was calculated and the tests were considered positive if the ratio was = 0.5. Children with at least one positive skin test were defined as atopic.16 The tests were performed between July and September 1998.

    Statistical analysis

    Statistical analyses were performed with SPSS for Windows Version 11 and STATA statistical packages. VOC data were log transformed because of the skewed distribution. Simple 2 square tests and Student’s t tests were applied for initial comparisons. Multiple linear regression analysis was used to test the association between VOCs and house characteristics.

    A random effect of the logistic regression was used to identify important asthma risk factors. This is a modelling technique for use with dichotomous outcomes in which the responses are correlated. In the present study we have observations on the same individuals at two different time points and a common technique for analysing this type of data is known as generalised estimating equations (GEE), which is like logistic regression but has the capability to take care of multiple observations for the same person by treating the person as a "random effect". Each variable was assessed and was considered significant in the model if the Wald statistic p value was <0.05. All significant variables were entered into a multivariate model as the non-significant factors were systematically removed. Variables considered to be confounding such as age, sex, atopy, socioeconomic status, smoking indoors, presence of air conditioning and house dust mites were kept in the final model. Socioeconomic status was based on area of residence.17 Crude and adjusted odds ratios (ORs) for asthma with 10 μg/m3 increase of exposure to VOCs were calculated with a 95% confidence interval (CI). Interaction terms between VOCs and allergen levels of dust mites were also tested in the models. In all statistical analyses two tailed tests were used and a 5% level of significance was applied.

    We calculated that 104 cases and 104 controls would provide 90% power to detect as significant from 0 (p<0.05) a true OR of 2.0 for the association between asthma and exposure to VOCs.

    RESULTS

    Eighty percent of those approached agreed to take part in the study (90% cases and 70% controls). Results were obtained from 192 children (88 cases and 104 controls). The mean (SD) age of the asthmatic children was 25 (7.46) months and of the controls was 20 (7.54) months. Sixty eight cases (77%) were defined as atopic compared with 53 controls (51%). The most common allergy for both asthmatics and non-asthmatics was to house dust mite (D pteronyssinus). Sixty eight asthmatic children (77%) had at least one parent with an allergic problem and 57% had at least one asthmatic parent. More cases than controls reported having wheeze, runny nose, and cough (p<0.01, table 1).

    Table 1 Prevalence of demographic and health data in subjects with and without asthma

    Characteristics of the homes

    The VOCs identified in the homes of participants included benzene, toluene, m-xylene, o,p-xylene, ethylbenzene, styrene, chlorobenzene, 1,3-dichlorobenzene, 1,2-dichlorobenzene and 1,4-dichlorobenzene, with toluene, xylene, and benzene + toluene being detected in 99% of the homes studied, xylene in 93%, and benzene in 86%. The highest median concentration was measured for benzene (20.3 μg/m3 with a maximum of 81.9 μg/m3) followed by toluene (17.1 μg/m3 (range 0.01–153.9)) and 1,2-dichlorobenzene (16.7 μg/m3 (range 0.01–201.8)). The median concentration of total VOCs was 54.9 μg/m3 with a maximum of 622 μg/m3 measured in a house in which the walls of the living room had been recently painted. Recent painting in the house was reported for significantly more cases than for children without asthma (37 (22%) v 28 (14%), p<0.05). However, significantly more control subjects than cases had air conditioning (54 (52%) v 29 (33%), p = 0.008).

    In a multilinear regression model total VOC levels were significantly (p = 0.045) affected by recent painting. Ethylbenzene and xylene levels were significantly increased in association with smoking, the presence of a new carpet and new furniture (p<0.05). Dust mite allergen levels were also significantly associated with total VOC levels (p = 0.001).

    Childhood asthma in relation to domestic exposure to VOCs

    Exposure levels to total VOCs were higher during summer than in winter but the differences were not significant (fig 1). However, when exposure levels to total VOCs were compared between cases and control subjects, children who had received emergency treatment for asthma were found to have been exposed to significantly higher concentrations of total VOCs than controls (p<0.05, table 2).

    Table 3 Adjusted and unadjusted odds ratio (OR) for the risk of asthma for each mg increase in exposure to VOCs

    The ORs were adjusted for the effects of relative humidity and indoor temperature. Other potential confounding factors such as child’s age, sex, child’s allergy, family history of asthma, socioeconomic status, smoking indoors, season, air conditioning, house dust mites, and gas appliances were also considered in the analysis. Having controlled for these potential confounding variables, children exposed to concentrations of total VOCs of 60 μg/m3 (median level of exposure) had a fourfold increased risk of having asthma while children exposed to single compounds such as benzene at levels of 20 μg/m3 (median level of exposure) had an eightfold increased risk of asthma (fig 2).

    odds ratios adjusted for age, sex, atopy, socioeconomic status, smoking indoors, air conditioning, house dust mites, and gas appliances.

    Most of the individual VOCs appeared to be significant risk factors for asthma with the highest ORs for benzene followed by ethylbenzene and toluene (fig 3). For every 10 unit increase in the concentrations of toluene and benzene (μg/m3) the risk of having asthma increased by almost two and three times, respectively.

    305–10.(K Rumchev1, J Spickett1, )