Literature DB >> 27461060

Exposure to Ambient Air Pollution and the Risk of Inflammatory Bowel Disease: A European Nested Case-Control Study.

Jorrit L Opstelten1, Rob M J Beelen2,3, Max Leenders2, Gerard Hoek2, Bert Brunekreef2, Fiona D M van Schaik1, Peter D Siersema1,4, Kirsten T Eriksen5, Ole Raaschou-Nielsen5,6, Anne Tjønneland5, Kim Overvad7, Marie-Christine Boutron-Ruault8,9, Franck Carbonnel8,9,10, Kees de Hoogh11,12,13, Timothy J Key14, Robert Luben15, Simon S M Chan16,17, Andrew R Hart16,17, H Bas Bueno-de-Mesquita1,18,19,20, Bas Oldenburg21.   

Abstract

BACKGROUND: Industrialization has been linked to the etiology of inflammatory bowel disease (IBD). AIM: We investigated the association between air pollution exposure and IBD.
METHODS: The European Prospective Investigation into Cancer and Nutrition cohort was used to identify cases with Crohn's disease (CD) (n = 38) and ulcerative colitis (UC) (n = 104) and controls (n = 568) from Denmark, France, the Netherlands, and the UK, matched for center, gender, age, and date of recruitment. Air pollution data were obtained from the European Study of Cohorts for Air Pollution Effects. Residential exposure was assessed with land-use regression models for particulate matter with diameters of <10 μm (PM10), <2.5 μm (PM2.5), and between 2.5 and 10 μm (PMcoarse), soot (PM2.5 absorbance), nitrogen oxides, and two traffic indicators. Conditional logistic regression analyses were performed to calculate odds ratios (ORs) with 95 % confidence intervals (CIs).
RESULTS: Although air pollution was not significantly associated with CD or UC separately, the associations were mostly similar. Individuals with IBD were less likely to have higher exposure levels of PM2.5 and PM10, with ORs of 0.24 (95 % CI 0.07-0.81) per 5 μg/m(3) and 0.25 (95 % CI 0.08-0.78) per 10 μg/m(3), respectively. There was an inverse but nonsignificant association for PMcoarse. A higher nearby traffic load was positively associated with IBD [OR 1.60 (95 % CI 1.04-2.46) per 4,000,000 motor vehicles × m per day]. Other air pollutants were positively but not significantly associated with IBD.
CONCLUSION: Exposure to air pollution was not found to be consistently associated with IBD.

Entities:  

Keywords:  Air pollution; Crohn’s disease; Inflammatory bowel disease; Particulate matter; Ulcerative colitis

Mesh:

Substances:

Year:  2016        PMID: 27461060      PMCID: PMC5020109          DOI: 10.1007/s10620-016-4249-4

Source DB:  PubMed          Journal:  Dig Dis Sci        ISSN: 0163-2116            Impact factor:   3.199


Introduction

Inflammatory bowel disease (IBD) is a disabling intestinal condition of unclear etiology affecting over two million people in Europe alone [1]. Both Crohn’s disease (CD) and ulcerative colitis (UC), the two main forms of IBD, are thought to result from a complex interplay between the immune system and gut microbiota in genetically susceptible individuals [2]. Yet, the changing epidemiology of IBD supports a key role for environmental factors in the development of this chronic disorder [3]. The incidence of IBD in Western countries has increased over the last century but currently appears relatively stable, whereas a rapid disease emergence is observed in developing nations, where IBD was formerly uncommon [4, 5]. Consequently, industrialization and westernization of lifestyle have been linked to the etiology of CD and UC [3, 6, 7]. Although various risk factors, such as diet [8], have previously been proposed, these do not fully explain the increase in the incidence of IBD and other environmental changes must therefore be involved [9]. Air pollution is associated with industrialization and consists of a complex mixture of different substances, such as particulate matter (PM). Although air pollution has mainly been associated with cardiorespiratory disorders [10], limited experimental and epidemiological data suggest that air pollutants may also exert deleterious gastrointestinal effects [11]. Potential mechanisms by which air pollutants may cause intestinal injury are thought to include direct adverse effects on epithelial cells, alterations in immune responses, or modulation of the gut microbiota [11-14]. Epidemiological studies examining the relationship between air pollution and IBD are scarce. In a case–control study from the UK, children and young adults, but not older individuals, living in areas with high-level exposure to nitrogen dioxide (NO2) and sulfur dioxide had an increased risk of developing CD and UC, respectively, indicating possible age-related effects [15]. However, this study was based on regional air pollution estimates, limiting exposure assessment. Therefore, we aimed to investigate the association between residential exposure to ambient air pollution and IBD in a nested case–control study within a multicenter European cohort. Based on previous studies, we hypothesized that air pollution exposure increases the risk of developing CD and UC.

Materials and Methods

Study Population

Subjects were identified from the European Prospective Investigation into Cancer and Nutrition (EPIC) study, a large multicenter cohort investigation designed to explore the association between lifestyle and environmental factors and chronic diseases. The methods of the main study were described previously [16]. In the present study, we made use of cases and controls drawn from a subset of this cohort, namely 227,620 initially healthy men and women recruited from five centers in Denmark, France, the Netherlands, and the UK between 1993 and 2000 (Table 1). At baseline, participants provided information on age, gender, habitual diet, and lifestyle factors, including smoking and physical activity, by self-administered questionnaires. Participants’ height and weight were measured by trained health professionals or obtained through self-reports.
Table 1

Participating centers, study areas, and characteristics of the individual cohorts

Country and centerIndividual EPIC cohortStudy area ESCAPECohort sizeNature of cohortNo. of incident CD casesa No. of incident UC casesa
Denmark, Aarhus, and CopenhagenDCHCopenhagen area57,054Population-based cohort of men and women aged 50–64 years. Enrollment period 1993–1997. Cases identified up to July 20071130
France, regions throughout countryE3NParis, Lyon, Grenoble and, Marseille72,996Female teachers and co-workers aged 40–65 years from a nationwide health insurance scheme. Enrollment period 1993–1997. Cases identified up to April 2008510
The Netherlands, BilthovenMORGENLarge regions of the country22,715Population-based cohort of men and women aged 20–65 years. Enrollment period 1993–1997. Cases identified up to December 2009927
The Netherlands, UtrechtProspectLarge regions of the country17,357Women aged 49–70 years in a breast cancer screening program. Enrollment period 1993–1997. Cases identified up to December 2009714
The UK, OxfordOxfordLarge regions of the country57,498Members of vegetarian societies and readers of health food magazines aged 20–80 years. Enrollment period 1993–2000. Cases identified up to May 2004623
Total227,62038104

CD, Crohn’s disease; DCH, Danish Diet, Cancer and Health cohort; E3N, Etude Épidémiologique des femmes de la Mutuelle Générale de l’Education Nationale; EPIC, European Prospective Investigation into Cancer and Nutrition; ESCAPE, European Study of Cohorts for Air Pollution Effects; UC, ulcerative colitis

aOnly incident cases (and their controls) with air pollution estimates were selected

Participating centers, study areas, and characteristics of the individual cohorts CD, Crohn’s disease; DCH, Danish Diet, Cancer and Health cohort; E3N, Etude Épidémiologique des femmes de la Mutuelle Générale de l’Education Nationale; EPIC, European Prospective Investigation into Cancer and Nutrition; ESCAPE, European Study of Cohorts for Air Pollution Effects; UC, ulcerative colitis aOnly incident cases (and their controls) with air pollution estimates were selected

Exposure Assessment

Air pollution data were obtained from the European Study of Cohorts for Air Pollution Effects (ESCAPE). The ESCAPE project was initiated to investigate the health effects of air pollution within European countries by linking exposure data to health data from ongoing cohort studies, including EPIC [17]. The study areas of ESCAPE generally included major cities with surrounding rural areas and included large regions of the country in some cohorts (Table 1). The methods of the standardized measurement procedures were published elsewhere [18, 19]. In summary, for each study area of ESCAPE, particulate matter with an aerodynamic diameter of <10 μm (PM10), particulate matter with an aerodynamic diameter of <2.5 μm (PM2.5), blackness of the PM2.5 exposed filter (PM2.5 absorbance) (a marker for black carbon or soot), nitrogen oxides (NO) and NO2 were measured within 1 year during three different seasons between 2008 and 2011 in at least 20 sites [20, 21]. The concentration of PMcoarse was calculated as the difference between concentrations of PM10 and PM2.5. Subsequently, the annual average concentration of each pollutant was calculated. Air pollution exposure at the baseline residential address of study participants was then estimated by land-use regression models. These models were developed for each pollutant in each study area to explain the spatial variation of air pollution concentrations, taking various geographical factors into account, including altitude, population density, industrial land use, green space, and traffic flow variables. In addition to the air pollution concentrations, within ESCAPE two traffic indicators at the participant’s residential address were evaluated: traffic intensity on the nearest road (vehicles per day) and total traffic load on all major roads in a 100-m buffer (sum of traffic intensity multiplied by the length of those roads). Considering that air pollution was measured after enrollment, concentrations were back-extrapolated to the baseline year of each participant according to a standardized protocol used in previous ESCAPE work [17]. Back-extrapolation was only possible for pollutants for which historical data were available.

Cases and Controls

The cohort was followed up until at least June 2004 and in some centers up to December 2009. Individuals with incident CD or UC were identified using population-based disease registries (Denmark, the Netherlands) or follow-up questionnaires (France, the UK). The medical reports of all potential cases were reviewed by local gastroenterologists to confirm the diagnoses and to obtain information on diagnostic investigations and disease extent. In this nested case–control analysis, each case was matched with four randomly selected unique controls for center, gender, age at recruitment (±6 months), and date of recruitment (±3 months). Controls were alive and had no CD, UC, microscopic or indeterminate colitis on the date of diagnosis of their matched case (incidence density sampling). For the present study, only cases with available air pollution estimates could be included. As the selection of controls was performed prior to the current study and the study areas of ESCAPE did not always cover the entire geographical area of the individual EPIC cohorts, air pollution measures were not available for all controls of a case.

Statistical Analysis

Continuous data were expressed as medians with percentiles, because of the skewed distribution. Categorical data were expressed as frequencies with percentages. Correlations between the individual air pollution measures and traffic indicators were assessed using the Pearson correlation coefficient. Air pollutant concentrations were divided into tertiles according to the distribution across all matched controls. Conditional logistic regression analyses were performed to determine the association between air pollution exposure and IBD. Accordingly, associations were assessed within each cohort rather than between study areas. Considering the relatively small numbers of cases, associations were studied for CD and UC separately and combined. Odds ratios (ORs) with 95 % confidence intervals (CIs) were calculated to estimate the risk of IBD according to the different air pollutant concentrations and traffic indicators used as continuous and categorical variables. In a multivariable model, analyses were adjusted for smoking status (categorized into never smoker, former smoker, and current smoker) and socioeconomic status using educational level (categorized into primary school, technical school, secondary school, and higher education) as previous studies documented associations between these factors and IBD [22, 23]. All models for traffic indicators were additionally adjusted for background NO2 concentration. Trends across tertiles were computed using the median value of each tertile as a continuous variable. In sensitivity analyses, analyses were repeated for air pollutant concentrations back-extrapolated to the baseline year of participants. Two-sided p values below 0.05 were considered statistically significant. All analyses were performed using SPSS version 21 (IBM Corp., Armonk, NY, USA).

Ethical Considerations

The original cohort studies were approved by the institutional medical ethics committees.

Results

A total of 38 CD cases (median age at diagnosis 56.2 years, 76.3 % female) and 104 UC cases (median age at diagnosis 55.2 years, 70.2 % female) with air pollution measures were identified (Table 2). The median time between recruitment and diagnosis was 4.5 years [interquartile range (IQR) 2.3–6.8 years] and 3.8 years (IQR 2.1–6.4 years) for CD and UC, respectively. Fourteen CD cases (36.9 %) had ileal disease. Left-sided colitis (involvement limited up to the splenic flexure) was the commonest disease phenotype in UC cases (n = 45, 43.6 %). Air pollution estimates were available for 100, 90, 83, 70, and 27 % of controls from the Dutch Prospect cohort, the British cohort, the Dutch MORGEN cohort, the Danish cohort, and the French cohort, respectively. The distribution of air pollutant concentrations and traffic indicators for all IBD cases and controls per individual cohort is presented in Supplementary Tables 1–5. These tables show that within cohorts, pollution distributions were generally very similar between cases and controls and that in some cohorts, the concentration ranges of especially PM2.5 and PM10 were very small. The correlations between these estimates are presented in Supplementary Tables 6–10.
Table 2

Characteristics of inflammatory bowel disease cases and controls

CD cases (n = 38)Controls (n = 152)UC cases (n = 104)Controls (n = 416)
Female, n (%)29 (76.3)116 (76.3)73 (70.2)292 (70.2)
Age (years) at recruitment, median (IQR)50.9 (44.7–60.9)50.3 (44.5–59.0)50.7 (43.2–56.1)50.9 (43.2–56.6)
Age (years) at diagnosis, median (IQR)56.2 (49.7–63.6)55.2 (48.1–60.9)
Distribution of Crohn’s disease, n (%)
 L1, ileal14 (36.9)
 L2, colonic13 (34.2)
 L3, ileocolonic10 (26.3)
 + L4, upper gastrointestinal disease1 (2.6)
 Unknown0 (0.0)
Distribution of ulcerative colitis, n (%)
 E1, ulcerative proctitis25 (24.3)
 E2, left-sided colitis45 (43.6)
 E3, extensive colitis26 (25.2)
 Unknown7 (6.8)
Smoking status at recruitment, n (%)
 Never smoker13 (34.2)52 (34.2)36 (34.6)180 (43.3)
 Former smoker10 (26.3)54 (35.5)34 (32.7)118 (28.4)
 Current smoker15 (39.5)44 (28.9)33 (31.7)116 (27.9)
 Unknown0 (0.0)2 (1.3)1 (1.0)2 (0.5)
Highest educational level at recruitment, n (%)
 Primary school4 (10.5)29 (19.1)15 (14.4)61 (14.7)
 Technical school17 (44.7)38 (25.0)36 (34.6)128 (30.8)
 Secondary school10 (26.3)39 (25.7)22 (21.2)91 (21.9)
 Higher education7 (18.4)45 (29.6)27 (26.0)116 (27.9)
 Not specified0 (0.0)1 (0.7)4 (3.8)14 (3.4)
 Unknown0 (0.0)0 (0.0)0 (0.0)6 (1.4)

CD Crohn’s disease, IQR interquartile range, UC ulcerative colitis

Characteristics of inflammatory bowel disease cases and controls CD Crohn’s disease, IQR interquartile range, UC ulcerative colitis No statistically significant associations were detected between air pollution exposure and either CD (Table 3) or UC (Table 4), apart from a positive association for total traffic load on all major roads within a 100-m buffer [OR 1.58 (95 % CI 1.00–2.49) per 4,000,000 motor vehicles m per day] in the crude analysis of UC. The effect sizes were largely similar for the univariable and multivariable analyses and for CD and UC. In the crude analysis of CD and UC combined, residential exposure to PM2.5 was inversely associated with IBD, with an OR of 0.28 (95 % CI 0.08–0.94) per 5 μg/m3 (Table 5). A positive association was found for total traffic load on all major roads [OR 1.60 (95 % CI 1.06–2.43) per 4,000,000 motor vehicles × m per day]. These associations remained statistically significant with similar effect sizes after adjusting for smoking status and educational level in the multivariable analysis. Additionally, PM10 concentrations were inversely associated with IBD in the multivariable model, with an OR of 0.25 (95 % CI 0.08–0.78) per 10 μg/m3. Excluding data of the French cohort, which had the lowest proportion of IBD cases (n = 15) and controls with air pollution measures (n = 20), did not affect the direction of the effect sizes materially (data not shown). The associations for PM2.5 per cohort are presented in Supplementary Fig. 1. In the analysis based on tertiles, significant inverse associations were detected for PM2.5 (p trend = 0.01) and PMcoarse (p trend = 0.04) in IBD (Supplementary Table 11). Air pollution estimates back-extrapolated to the baseline year of each participant were generally higher than those during 2008–2011. Although no statistically significant associations were found, the sensitivity analyses for IBD for back-extrapolated concentrations of NO2, NO, PM2.5 absorbance and PM10 showed similar effect sizes as for nonback-extrapolated concentrations, apart from PM2.5 absorbance (Table 5).
Table 3

Association between air pollution exposure and Crohn’s disease (n = 38 cases)

Odds of CD
Unadjusted OR (95 % CI)Adjusted OR (95 % CI)a
NO2 1.25 (0.68–2.30)1.13 (0.59–2.16)
NOx 1.26 (0.75–2.12)1.17 (0.67–2.03)
PM2.5 0.29 (0.03–2.71)0.12 (0.01–1.77)
PM2.5 absorbance 0.59 (0.11–3.03)0.34 (0.04–3.05)
PM10 0.45 (0.07–2.90)0.10 (0.01–1.37)
PMcoarse 1.07 (0.17–6.55)0.59 (0.07–4.98)
Traffic intensity on the nearest roadb 1.18 (0.82–1.70)1.16 (0.79–1.71)
Traffic intensity on major roads within 100-m bufferb 1.92 (0.64–5.82)1.81 (0.50–6.47)

ORs are presented for the following increments: 10 μg/m3 for NO2, 20 μg/m3 for NO, 5 μg/m3 for PM2.5, 10−5 m−1 for PM2.5 absorbance, 10 μg/m3 for PM10, 5 μg/m3 for PMcoarse, 5000 motor vehicles per day for the traffic intensity on the nearest road, 4,000,000 motor vehicles × m per day for the total traffic load on all major roads within a 100-m buffer

CD Crohn’s disease, NO nitrogen oxide, OR odds ratio, PM particulate matter

aAdjusted for smoking status and educational level

bAdditionally adjusted for background NO2 concentration (continuous variable)

Table 4

Association between air pollution exposure and ulcerative colitis (n = 104 cases)

Odds of UC
Unadjusted OR (95 % CI)Adjusted OR (95 % CI)a
NO2 1.03 (0.73–1.46)0.99 (0.70–1.41)
NOx 1.06 (0.79–1.43)1.03 (0.76–1.38)
PM2.5 0.27 (0.06–1.17)0.23 (0.05–1.02)
PM2.5 absorbance 1.19 (0.48–2.96)1.20 (0.48–2.98)
PM10 0.34 (0.09–1.27)0.28 (0.07–1.07)
PMcoarse 0.38 (0.11–1.35)0.31 (0.09–1.10)
Traffic intensity on the nearest roadb 1.08 (0.90–1.29)1.06 (0.88–1.27)
Traffic intensity on major roads within 100-m bufferb 1.58 (1.00–2.49)1.55 (0.97–2.46)

ORs are presented for the following increments: 10 μg/m3 for NO2, 20 μg/m3 for NO, 5 μg/m3 for PM2.5, 10−5 m−1 for PM2.5 absorbance, 10 μg/m3 for PM10, 5 μg/m3 for PMcoarse, 5000 motor vehicles per day for the traffic intensity on the nearest road, 4,000,000 motor vehicles × m per day for the total traffic load on all major roads within a 100-m buffer

NO nitrogen oxide, OR odds ratio, PM particulate matter, UC ulcerative colitis

aAdjusted for smoking status and educational level

bAdditionally adjusted for background NO2 concentration (continuous variable)

Table 5

Association between air pollution exposure and inflammatory bowel disease (n = 142 cases)

Odds of IBD
Unadjusted OR (95 % CI)Adjusted OR (95 % CI)a
NO2 1.08 (0.80–1.46)1.05 (0.77–1.42)
NOx 1.11 (0.86–1.43)1.08 (0.83–1.40)
PM2.5 0.28 (0.08–0.94)0.24 (0.07–0.81)
PM2.5 absorbance 0.99 (0.45–2.17)1.03 (0.45–2.34)
PM10 0.37 (0.13–1.09)0.25 (0.08–0.78)
PMcoarse 0.52 (0.19–1.45)0.42 (0.14–1.20)
Traffic intensity on the nearest roadb 1.09 (0.93–1.28)1.07 (0.92–1.26)
Traffic intensity on major roads within 100-m bufferb 1.60 (1.06–2.43)1.60 (1.04–2.46)
Back-extrapolated NO2 1.14 (0.78–1.66)1.07 (0.73–1.59)
Back-extrapolated NOx 1.15 (0.86–1.55)1.10 (0.81–1.49)
Back-extrapolated PM2.5 absorbance 0.46 (0.07–3.10)0.40 (0.06–2.78)
Back-extrapolated PM10 0.20 (0.02–2.22)0.17 (0.02–2.01)

ORs are presented for the following increments: 10 μg/m3 for NO2, 20 μg/m3 for NO, 5 μg/m3 for PM2.5, 10−5 m−1 for PM2.5 absorbance, 10 μg/m3 for PM10, 5 μg/m3 for PMcoarse, 5000 motor vehicles per day for the traffic intensity on the nearest road, 4,000,000 motor vehicles × m per day for the total traffic load on all major roads within a 100-m buffer

IBD inflammatory bowel disease, NO nitrogen oxide, OR odds ratio, PM particulate matter

aAdjusted for smoking status and educational level

bAdditionally adjusted for background NO2 concentration (continuous variable)

Association between air pollution exposure and Crohn’s disease (n = 38 cases) ORs are presented for the following increments: 10 μg/m3 for NO2, 20 μg/m3 for NO, 5 μg/m3 for PM2.5, 10−5 m−1 for PM2.5 absorbance, 10 μg/m3 for PM10, 5 μg/m3 for PMcoarse, 5000 motor vehicles per day for the traffic intensity on the nearest road, 4,000,000 motor vehicles × m per day for the total traffic load on all major roads within a 100-m buffer CD Crohn’s disease, NO nitrogen oxide, OR odds ratio, PM particulate matter aAdjusted for smoking status and educational level bAdditionally adjusted for background NO2 concentration (continuous variable) Association between air pollution exposure and ulcerative colitis (n = 104 cases) ORs are presented for the following increments: 10 μg/m3 for NO2, 20 μg/m3 for NO, 5 μg/m3 for PM2.5, 10−5 m−1 for PM2.5 absorbance, 10 μg/m3 for PM10, 5 μg/m3 for PMcoarse, 5000 motor vehicles per day for the traffic intensity on the nearest road, 4,000,000 motor vehicles × m per day for the total traffic load on all major roads within a 100-m buffer NO nitrogen oxide, OR odds ratio, PM particulate matter, UC ulcerative colitis aAdjusted for smoking status and educational level bAdditionally adjusted for background NO2 concentration (continuous variable) Association between air pollution exposure and inflammatory bowel disease (n = 142 cases) ORs are presented for the following increments: 10 μg/m3 for NO2, 20 μg/m3 for NO, 5 μg/m3 for PM2.5, 10−5 m−1 for PM2.5 absorbance, 10 μg/m3 for PM10, 5 μg/m3 for PMcoarse, 5000 motor vehicles per day for the traffic intensity on the nearest road, 4,000,000 motor vehicles × m per day for the total traffic load on all major roads within a 100-m buffer IBD inflammatory bowel disease, NO nitrogen oxide, OR odds ratio, PM particulate matter aAdjusted for smoking status and educational level bAdditionally adjusted for background NO2 concentration (continuous variable)

Discussion

In this European multicenter study, no consistent association between residential exposure to ambient air pollution and the risk of IBD was found. The effect sizes were mostly similar for CD and UC separately. Individuals with IBD were less likely to have higher exposure levels of PM2.5 and PM10, whereas a positive association was observed for total traffic load on all major nearby roads. Other air pollutants were mostly positively but not statistically significantly associated with IBD. Although not reaching statistical significance, the effect sizes were broadly similar when back-extrapolating air pollutant concentrations to the participants’ baseline year. Numerous studies have confirmed the association of ambient air pollution with a variety of diseases, and several underlying biological mechanisms have been proposed [10, 17, 24, 25]. The link between air pollution and intestinal health is, however, less well established with a few studies showing positive associations with colorectal cancer, appendicitis, and nonspecific abdominal pain [26-30]. In this respect, the adverse effects of smoking [31, 32], which may have some resemblance with air pollution, may help indicate the potential impact of air pollution exposure. It is hypothesized that exposure to air pollutants may contribute to the development of intestinal disorders, including IBD, through diverse biological mechanisms. First, ingestion of air pollutants by inhalation or contaminated foods may have direct toxic effects on epithelial cells, which may induce proinflammatory responses and increase gut permeability [11]. Second, various studies have shown that air pollution exposure may result in systemic inflammatory effects, such as changes in circulating cytokines, including tumor necrosis factor alpha [33]. Notably, air pollution has also been related to immunologically mediated disorders that may share some epidemiological and pathogenic aspects with IBD [34]. For instance, exposure to PM10 has been associated with an increased risk of relapse in multiple sclerosis [35], whereas traffic exposure has been found to be positively associated with incident rheumatoid arthritis [36]. Third, it is thought that air pollution may modulate the microbial composition of the gut [14], as recently exemplified in two studies in which PM exposure in mice led to significant alterations in the microbiota and induced acute and chronic intestinal inflammatory responses [12, 13]. To date, very few epidemiological studies explored the effects of air pollution in IBD. In a nested case–control study from the UK, in the whole population, no significant association between air pollution and incident IBD was found [15]. However, children and young adults living in areas with higher levels (within the upper three quintiles) of NO2 and sulfur dioxide, respectively, were more likely to develop CD [OR 2.31 (95 % CI 1.25–4.28) for individuals aged ≤23 years] and UC [OR 2.00 (95 % CI 1.08–3.72) for individuals aged ≤25 years]. Land-use regression models for more refined exposure assessments could not be incorporated in this study. An ecological analysis from the US related hospitalizations for IBD to air pollution emissions from an emission inventory, but was unable to estimate air pollution concentrations [37]. In our study, which included mainly middle aged to elderly people, we observed opposing associations. This could indicate that different pollutants have differential effects in specific groups. For example, younger people (with a developing immune system) might be more susceptible to air pollutants as compared to older people. Importantly, children and young adults are also likely to spend more time outdoors and near their home, which may increase and better reflect true personal exposure. Exposure assessment may therefore be more accurate in these individuals. There were no statistically significant associations for CD and UC separately, which presumably resulted from the relatively small numbers of cases. Disease-specific results may exist, as previously observed, for example, in the opposing associations for smoking between CD and UC [22], although the effect sizes were mostly similar for both forms of IBD in our study. We observed inverse associations for some pollutants, which appeared largely consistent across centers and in the analyses using pollution exposure as continuous and categorical variables. It remains unclear whether these associations reflect a true causal relationship or that these pollutants are a proxy for other variables. Interestingly, in the earlier mentioned study, PM10 and NO2 concentrations were inversely associated with CD in individuals aged 44–57 years with ORs of 0.48 (95 % CI 0.29–0.80) and 0.56 (95 % CI 0.33–0.95), respectively [15], demonstrating that inverse associations have previously been observed in older patients in another population using a different methodological approach. Overall, despite previous data suggesting that air pollutants may negatively impact IBD, no coherent associations have currently been confirmed to draw firm conclusions on the putative adverse effects of air pollution exposure in CD and UC, indicating the need for further research. This study had several strengths. First, the multicenter design enabled us to explore the association between air pollution and IBD in several European countries. Second, a significant advantage over previous studies was the use of land-use regression models to accurately determine small-scale variations in residential exposure to air pollution and traffic intensity for each participant according to a highly standardized protocol. Third, both cases and controls were drawn from the same baseline population, thereby reducing the risk of selection bias. Fourth, to ensure case ascertainment all diagnoses were confirmed by local physicians and participants with indeterminate or microscopic colitis were excluded. Fifth, the number of cases was similar to what was expected, which reduces the likelihood of follow-up bias [38]. Despite nesting in a well-characterized cohort, the limited sample size was an important drawback and our study may have been underpowered to detect statistical differences. Therefore, we chose to evaluate outcomes for CD and UC separately and for total IBD. Furthermore, air pollution estimates were assessed only at the residential address of each participant and not, for example, at their working address, where individuals may also be exposed. This could have resulted in misclassification of exposure. Moreover, air pollution was measured after diagnosis, which was a general issue in epidemiological studies using ESCAPE exposure data, such as in a previous study linking air pollution to mortality [17]. However, previous studies show that spatial air pollution contrasts remain stable over long periods of time and are well predicted with land-use regression models [39-43]. Using back-extrapolation, we evaluated the association for some pollutants at the baseline year of each participant, with effect sizes being broadly similar to the main analyses. It has been estimated that most of the participants did not move after enrollment [17], but exact data on moving were unavailable for all centers. The majority of cases developed IBD over the age of 50 years, indicating late-onset IBD, whereas CD and UC commonly present at an earlier age. This limited the opportunity to study age-specific effects, and the results may therefore not be generalizable to the whole IBD population as other phenotypes may have different environmental influences. Considering the limited sample size and multiple comparisons, we cannot entirely exclude that our results are due to chance findings. Finally, although we were able to either match or adjust for potential confounders, such as center and smoking, residual confounding (by unknown risk factors) could not be fully excluded in this observational study. To conclude, we were unable to demonstrate a consistent association between residential exposure to ambient air pollution and IBD risk in this European multicenter cohort. Below is the link to the electronic supplementary material. Supplementary Figure 1. Association between PM2.5 exposure and inflammatory bowel disease per cohort. CI: confidence interval; PM2.5: particulate matter with an aerodynamic diameter of less than 2.5 μm; OR: odds ratio. Adjustment for smoking status and educational level. ORs are presented for the following increment: 5 μg/m3 (TIFF 210 kb) Supplementary material 2 (DOCX 97 kb)
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Review 1.  Air pollution and health.

Authors:  Bert Brunekreef; Stephen T Holgate
Journal:  Lancet       Date:  2002-10-19       Impact factor: 79.321

2.  Geographic distribution and ecological studies of inflammatory bowel disease in southeastern Norway in 1990-1993.

Authors:  Geir Aamodt; Jørgen Jahnsen; May-Bente Bengtson; Bjørn Moum; Morten H Vatn
Journal:  Inflamm Bowel Dis       Date:  2008-07       Impact factor: 5.325

3.  Exposure to ingested airborne pollutant particulate matter increases mucosal exposure to bacteria and induces early onset of inflammation in neonatal IL-10-deficient mice.

Authors:  Saad Y Salim; Juan Jovel; Eytan Wine; Gilaad G Kaplan; Renaud Vincent; Aducio Thiesen; Herman W Barkema; Karen L Madsen
Journal:  Inflamm Bowel Dis       Date:  2014-07       Impact factor: 5.325

Review 4.  Disorders of a modern lifestyle: reconciling the epidemiology of inflammatory bowel diseases.

Authors:  Charles N Bernstein; Fergus Shanahan
Journal:  Gut       Date:  2008-05-30       Impact factor: 23.059

5.  Stability of measured and modelled spatial contrasts in NO(2) over time.

Authors:  Marloes Eeftens; Rob Beelen; Paul Fischer; Bert Brunekreef; Kees Meliefste; Gerard Hoek
Journal:  Occup Environ Med       Date:  2011-02-01       Impact factor: 4.402

6.  Effects of long-term exposure to air pollution on natural-cause mortality: an analysis of 22 European cohorts within the multicentre ESCAPE project.

Authors:  Rob Beelen; Ole Raaschou-Nielsen; Massimo Stafoggia; Zorana Jovanovic Andersen; Gudrun Weinmayr; Barbara Hoffmann; Kathrin Wolf; Evangelia Samoli; Paul Fischer; Mark Nieuwenhuijsen; Paolo Vineis; Wei W Xun; Klea Katsouyanni; Konstantina Dimakopoulou; Anna Oudin; Bertil Forsberg; Lars Modig; Aki S Havulinna; Timo Lanki; Anu Turunen; Bente Oftedal; Wenche Nystad; Per Nafstad; Ulf De Faire; Nancy L Pedersen; Claes-Göran Östenson; Laura Fratiglioni; Johanna Penell; Michal Korek; Göran Pershagen; Kirsten Thorup Eriksen; Kim Overvad; Thomas Ellermann; Marloes Eeftens; Petra H Peeters; Kees Meliefste; Meng Wang; Bas Bueno-de-Mesquita; Dorothea Sugiri; Ursula Krämer; Joachim Heinrich; Kees de Hoogh; Timothy Key; Annette Peters; Regina Hampel; Hans Concin; Gabriele Nagel; Alex Ineichen; Emmanuel Schaffner; Nicole Probst-Hensch; Nino Künzli; Christian Schindler; Tamara Schikowski; Martin Adam; Harish Phuleria; Alice Vilier; Françoise Clavel-Chapelon; Christophe Declercq; Sara Grioni; Vittorio Krogh; Ming-Yi Tsai; Fulvio Ricceri; Carlotta Sacerdote; Claudia Galassi; Enrica Migliore; Andrea Ranzi; Giulia Cesaroni; Chiara Badaloni; Francesco Forastiere; Ibon Tamayo; Pilar Amiano; Miren Dorronsoro; Michail Katsoulis; Antonia Trichopoulou; Bert Brunekreef; Gerard Hoek
Journal:  Lancet       Date:  2013-12-09       Impact factor: 79.321

Review 7.  Environmental risk factors for inflammatory bowel diseases: a review.

Authors:  Ashwin N Ananthakrishnan
Journal:  Dig Dis Sci       Date:  2014-09-10       Impact factor: 3.199

8.  Autoimmune disease concomitance among inflammatory bowel disease patients in the United States, 2001-2002.

Authors:  Russell Cohen; Don Robinson; Clark Paramore; Kathy Fraeman; Kevin Renahan; Mohan Bala
Journal:  Inflamm Bowel Dis       Date:  2008-06       Impact factor: 5.325

9.  European Prospective Investigation into Cancer and Nutrition (EPIC): study populations and data collection.

Authors:  E Riboli; K J Hunt; N Slimani; P Ferrari; T Norat; M Fahey; U R Charrondière; B Hémon; C Casagrande; J Vignat; K Overvad; A Tjønneland; F Clavel-Chapelon; A Thiébaut; J Wahrendorf; H Boeing; D Trichopoulos; A Trichopoulou; P Vineis; D Palli; H B Bueno-De-Mesquita; P H M Peeters; E Lund; D Engeset; C A González; A Barricarte; G Berglund; G Hallmans; N E Day; T J Key; R Kaaks; R Saracci
Journal:  Public Health Nutr       Date:  2002-12       Impact factor: 4.022

10.  Development and back-extrapolation of NO2 land use regression models for historic exposure assessment in Great Britain.

Authors:  John Gulliver; Kees de Hoogh; Anna Hansell; Danielle Vienneau
Journal:  Environ Sci Technol       Date:  2013-06-27       Impact factor: 9.028
View more
  7 in total

Review 1.  Environmental triggers in IBD: a review of progress and evidence.

Authors:  Ashwin N Ananthakrishnan; Charles N Bernstein; Dimitrios Iliopoulos; Andrew Macpherson; Markus F Neurath; Raja A Raja Ali; Stephan R Vavricka; Claudio Fiocchi
Journal:  Nat Rev Gastroenterol Hepatol       Date:  2017-10-11       Impact factor: 46.802

Review 2.  Air Pollution and Noncommunicable Diseases: A Review by the Forum of International Respiratory Societies' Environmental Committee, Part 2: Air Pollution and Organ Systems.

Authors:  Dean E Schraufnagel; John R Balmes; Clayton T Cowl; Sara De Matteis; Soon-Hee Jung; Kevin Mortimer; Rogelio Perez-Padilla; Mary B Rice; Horacio Riojas-Rodriguez; Akshay Sood; George D Thurston; Teresa To; Anessa Vanker; Donald J Wuebbles
Journal:  Chest       Date:  2018-11-09       Impact factor: 9.410

Review 3.  Ambient Air Pollution and Pediatric Inflammatory Bowel Diseases: An Updated Scoping Review.

Authors:  Ricardo G Suarez; Alvaro R Osornio-Vargas; Eytan Wine
Journal:  Dig Dis Sci       Date:  2022-06-25       Impact factor: 3.487

Review 4.  Inflammatory Bowel Disease: New Insights into the Interplay between Environmental Factors and PPARγ.

Authors:  Giulia Caioni; Angelo Viscido; Michele d'Angelo; Gloria Panella; Vanessa Castelli; Carmine Merola; Giuseppe Frieri; Giovanni Latella; Annamaria Cimini; Elisabetta Benedetti
Journal:  Int J Mol Sci       Date:  2021-01-20       Impact factor: 5.923

5.  The impact of selected food additives on the gastrointestinal tract in the example of nonspecific inflammatory bowel diseases.

Authors:  Sara Jarmakiewicz-Czaja; Dominika Piątek; Rafał Filip
Journal:  Arch Med Sci       Date:  2021-01-08       Impact factor: 3.707

6.  Quercetin Intervention Alleviates Offspring's Oxidative Stress, Inflammation, and Tight Junction Damage in the Colon Induced by Maternal Fine Particulate Matter (PM2.5) Exposure through the Reduction of Bacteroides.

Authors:  Wei Liu; Yalin Zhou; Yong Qin; Lanlan Yu; Ruijun Li; Yuhan Chen; Yajun Xu
Journal:  Nutrients       Date:  2020-10-11       Impact factor: 5.717

Review 7.  The Intestinal Barrier-Shielding the Body from Nano- and Microparticles in Our Diet.

Authors:  Marlene Schwarzfischer; Gerhard Rogler
Journal:  Metabolites       Date:  2022-03-02
  7 in total

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