Association between symptoms of severe periodontitis and post-bronchodilator lung function: results from the China pulmonary health study

Background

The association between periodontitis and post-bronchodilator lung function is unclear. We aimed to determine the associations between symptoms of severe periodontitis (SSP) and post-bronchodilator lung function in the Chinese population.

Methods

A cross-sectional study (China Pulmonary Health study) was conducted from 2012 to 2015 in a large Chinese nationally representative sample of 49,202 participants aged 20–89 years. Data on demographic characteristics and periodontal symptoms of participants were collected by questionnaire. Participants who had at least one of the two severe symptoms (tooth mobility and natural tooth loss) in the past year were defined to have SSP, which was set as one variable for analyses. Post-bronchodilator lung function data including forced expiratory volume in 1 s (FEV₁) and forced vital capacity (FVC) were collected by spirometry.

Results

The values of post-FEV₁, post-FVC and post-FEV₁/FVC of the participants with SSP were all significantly lower than the participants without SSP (all p < 0.001). SSP were significantly associated with post-FEV₁/FVC < 0.7 (p < 0.001). In the multiple regression analyses, SSP were still negatively associated with post-FEV₁(b = -0.04, 95%CI (-0.05 -0.03), p < 0.001), post-FEV₁/FVC (b = -0.45, 95%CI (-0.63, -0.28), p < 0.001) and significantly associated with post-FEV₁/FVC < 0.7 (OR = 1.08, 95%CI 1.01—1.16, p = 0.03) after full adjustment for potential confounders.

Conclusions

Our data suggest that SSP were negatively associated with post-bronchodilator lung function in the Chinese population. Longitudinal cohort studies are needed to confirm these associations in the future.

Periodontitis is a chronic infection and inflammatory disease that is initially caused by periodontal pathogens infection and eventually leads to alveolar bone resorption, tooth mobility and tooth loss. The worldwide prevalence of severe periodontitis is 10.8% [1]. According to the 4th Chinese national oral health epidemiological survey, almost 90% of Chinese adults suffered from periodontal disease of various severities, and about 30% had severe periodontitis (Stage III and IV) in the population aged 35–74 years [2]. Although the infection and inflammation mainly manifest in the local periodontal tissue, periodontitis has been found to be associated with many systemic diseases such as cardiovascular disease, diabetes mellitus, rheumatoid arthritis, chronic kidney disease and Alzheimer's disease [3].

In the past decades, increased evidence demonstrated that periodontitis was associated with obstructive lung diseases including chronic obstructive pulmonary disease (COPD) [4]. Obstructive impaired lung function is the key feature of COPD, which can be determined by spirometry [5]. Several cross-sectional studies with relatively small sample sizes have assessed the potential association between periodontal health and impaired lung function previously [6,7,8,9]. Although these studies used different periodontal and lung function parameters to evaluate periodontal health and lung function, the results all showed that poor periodontal health was associated with airflow limitation or reduced lung function [6,7,8,9]. Recently, two large cross-sectional studies based on the national population of Korea and the United States have assessed the association between periodontitis and impaired lung function [10, 11]. However, the results showed that periodontitis was not significantly associated with obstructive lung function impairment which was defined as forced expiratory volume in 1 s (FEV₁)/forced vital capacity (FVC) < 0.7 [10, 11]. This inconsistency may be partly attributed to the different study populations. Therefore, the association between periodontitis and impaired lung function needs to be further clarified in large population-based studies.

The bronchodilator test is used to help diagnose obstructive airway diseases such as COPD and asthma by measuring the reversibility of obstructive impaired lung function after inhalation of bronchodilators [12]. The Global Initiative for Chronic Obstructive Lung Disease (GOLD) guidelines defined COPD as FEV₁/FVC < 0.7 from a post-bronchilator test [13]. A previous study used data on pre-bronchodilator lung function to access the association between periodontitis and lung function [8], and the others did not describe the lung function data were collected pre- or post-bronchodilator [6, 7, 9,10,11]. Therefore, whether periodontitis is associated with post-bronchodilator lung function needs to be studied.

Thus, we designed this study by using data from a nationally representative sample (57,779 subjects) of Chinese adults from a large nation-wide cross-sectional survey (China Pulmonary Health Study, CPHS) [14]. In this study, we aimed to determine the associations between symptoms of severe periodontitis (SSP) and post-bronchodilator lung function in the Chinese population.

Study population

The CPHS was a cross-sectional study in a nationally representative sample of adults aged 20-89y conducted in China from 2012 to 2015 [14]. The study was designed to investigate the pulmonary health status of the Chinese population. Information related to pulmonary health, such as environmental factors, psychological factors and other related systemic health status including oral health, were also collected in this study. The study was approved by the ethics review committee of Beijing Capital Medical University and other participating institutes, and was conducted in accordance with the Helsinki Declaration of 1975, as revised in 2013. Written informed consent was obtained from all study participants. Details of the study design have been published previously [14]. Briefly, 57,779 individuals which were enrolled by a multistage stratified cluster sampling procedure were invited to participate in nation-wide, of whom 49,202 had reliable lung function test results, with natural teeth in the mouth and with no missing data were included in this study. The flow diagram of the selection of study participants is shown in Fig. 1.

The flow diagram of the selection of study participants

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Symptoms of severe periodontitis (SSP)

As a part of the CPHS, trained interviewers asked all participants whether they had experienced SSP in the past year, including tooth mobility and natural tooth loss. The specific questions that interviewers asked were “Have you had loose teeth in the past year?”, and “Have you had spontaneous tooth loss in the past year?”. The answers for these two questions were both set as “Yes” or “No”. Participants who answered “Yes” for at least one of the two questions were defined as having SSP, which was set as one variable for analyses in this study.

Lung function variables

Trained and certified technicians performed pulmonary function tests on all participants with a MasterScreen Pneumo PC spirometer (CareFusion, Yorba Linda, CA, USA). Details of the pulmonary function tests have been published previously [14]. An expert panel was responsible for quality assurance based on the American Thoracic Society and European Respiratory Society criteria [15], and poor quality tests were excluded.

The values of the ventilation function variables FEV₁ and FVC after bronchodilator inhalation of all participants were collected. Post-FEV₁/FVC was calculated and post-FEV_1/FVC ≥ 0.7 and < 0.7 were set as categorical variables according to the GOLD guideline [13].

Other variables

Trained interviewers administered standardized questionnaires containing information on demographic characteristics, education background, smoking status, residence, biomass fuel exposure, occupational exposure, chronic cough during childhood, parental history of respiratory diseases, history of respiratory diseases and other systemic diseases. We divided the participants into three groups (20-39y, 40-59y and ≥ 60y) according to the age. We categorized the education background as “primary school and lower”; “middle and high school” and “college and higher”; and categorized the smoking status as “never smoker” and “current/former smoker”. Never smokers were defined as those who had smoked fewer than 100 cigarettes in their lifetime and did not currently smoke. Residence was categorized as “urban” and “rural”. Biomass fuel exposure was defined as using woody fuel or animal waste for cooking or heating during the past 6 months or longer. Occupational exposure was defined as people engaged in work with dust exposure such as mining, quarrying, textile and cotton for more than 3 months. History of chronic bronchitis was defined as cough and sputum production for at least 3 months in each of two consecutive years. We categorized chronic cough during childhood before age 14 years as frequent (cumulative > 3 months per year), sometimes (1–3 months per year), and rare (< 1 month per year). Participants and their parents with one or more of the following conditions were considered to have respiratory disease, including COPD, emphysema, chronic bronchitis, bronchiectasis, asthma, tuberculosis, idiopathic pulmonary fibrosis and lung cancer. Participants with one or more of the following conditions were considered to have systemic disease, including stroke, coronary heart disease, hypertension, diabetes mellitus, depression, osteoporosis and anemia. Body height and weight were determined using calibrated scales, and body mass index (BMI) was calculated as weight/ height squared.

Statistical analyses

Normally distributed continuous variables were expressed as mean ± sd. Categorical variables were presented as n%. For continuous variables, independent t-test or one-way ANOVA was used, and chi-square test was used for categorical variables in univariate analyses. SPSS statistical software (version 20.0; SPSS Inc., Chicago, IL, USA) was used for the data analyses, and statistical significance was considered at a two-sided p < 0.05.

Multiple linear regression analyses were performed to calculate the unstandardized coefficients (b) and 95% confidence interval (CI) for the associations between SSP and continuous lung function variables. Multiple logistic regression analyses were performed to calculate the odds ratios (OR) and 95%CI for the associations between SSP and FEV_1/FVC (≥ 0.7 and < 0.7). The adjusted model 1 was adjusted for age, gender, height, body mass index, education, smoking status, residence, occupational exposure and biomass fuel exposure. The adjusted model 2 was additionally adjusted for chronic cough during childhood, parental history of respiratory diseases, history of chronic bronchitis, other respiratory diseases and other systemic diseases.

In order to exclude effects of the confounding factors for lung function, subgroup analyses were performed for the associations between SSP and post-FEV₁ and post-FEV₁/FVC by multiple linear regression. The subgroup analyses were separately stratified by age, gender, smoking status, residence, history of chronic bronchitis and other respiratory diseases, which were grouped as described above. The multiple linear regression was adjusted for age, gender, height, body mass index, education, smoking status, residence, occupational exposure, biomass fuel exposure, chronic cough during childhood, parental history of respiratory diseases, history of chronic bronchitis, other respiratory diseases and other systemic diseases. When the study population was grouped by a variable, this variable was not included in the adjusted model.

The demographic characteristics of the total 49,202 participants are shown in Table 1 and 2. Age, height, BMI, education, smoking status, residence, biomass fuel exposure, occupational exposure, parental history of respiratory diseases, history of chronic bronchitis, other respiratory diseases and other systemic diseases were all significantly associated with SSP (all p < 0.001, Table 1). And all demographic characteristics were all significantly associated with post-FEV₁/FVC < 0.7 (all p < 0.001, Table 2).

The values of post-FEV₁, post-FVC and post-FEV₁/FVC of the participants with SSP were all significantly lower than the participants without SSP (all p < 0.001). SSP were significantly associated with post-FEV₁/FVC < 0.7 (p < 0.001) (Table 3).

In the multiple regression analyses, SSP were still negatively associated with post-FEV₁(b = -0.05, 95%CI (-0.06, -0.04), p < 0.001 and b = -0.04, 95%CI (-0.05 -0.03), p < 0.001), post-FEV₁/FVC (b = -0.56, 95%CI (-0.74, -0.38), p < 0.001 and b = -0.45, 95%CI (-0.63, -0.28), p < 0.001) and significantly associated with post-FEV₁/FVC < 0.7 (OR = 1.11, 95%CI 1.05—1.19, p = 0.001 and OR = 1.08, 95%CI 1.01—1.16, p = 0.03) both in the adjusted model 1 and model 2 (Table 4).

For subgroup analyses (Fig. 2), SSP were both negatively associated with post-FEV₁ and post-FEV₁/FVC in adjusted multiple linear regression analyses when the participants were stratified by age, gender, education, smoking status and residence separately (all p < 0.05) except for post-FEV₁/FVC in the ≥ 60y group that stratified by age (p > 0.05), which is consistent with the results in total participants. When the participants were stratified by history of chronic bronchitis or other respiratory diseases, SSP were only negatively associated with post-FEV₁ and post-FEV₁/FVC in participants without respiratory diseases (all p < 0.001).

Associations of symptoms of severe periodontitis with post-FEV₁ and post-FEV_1/FVC by subgroup multiple linear regression analyses (FEV₁: forced expiratory volume in 1 s; FVC: forced vital capacity. Other respiratory diseases included chronic obstructive pulmonary disease, emphysema, bronchiectasis, asthma, tuberculosis, idiopathic pulmonary fibrosis and lung cancer. Adjusted model: adjusted for age, gender, height, body mass index, education, smoking status, residence, occupational exposure, biomass fuel exposure, chronic cough during childhood, parental history of respiratory diseases, history of chronic bronchitis, other respiratory diseases and other systemic diseases. When the study population was grouped by a variable, this variable was not included in the adjusted model

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In this large nationally representative sample based cross-sectional study with 49,202 participants, we found that SSP were negatively associated with post-bronchodilator lung function variables FEV₁, FVC and FEV₁/FVC and significantly associated with post-FEV₁/FVC < 0.7 after adjusting for several confounding factors. To the best of our knowledge, this is the largest nationwide study of the general population and the first Chinese population-based study to comprehensively examine the associations between SSP and post-bronchodilator lung function.

The association between periodontitis and respiratory diseases has received much attention in recent decades. Several potential mechanisms have been proposed to explain how a localized inflammatory disease around the teeth can harm lung health, such as attributed to the migration of periodontal pathogens to the lung and hematopoietic transmission of proinflammatory mediators produced in diseased periodontal tissue to the lung [4]. Periodontal pathogens are key factors in the development of periodontitis and accumulate in periodontal environments. As periodontal pathogens may migrate to the airway directly by aspiration or through circulation by entering the capillary from the wound gingival epithelium [16]. These pathogens may cause airway and alveoli infections and inflammation [16, 17]. Inflammation is the key pathological feature of COPD, which may result in remodeling of the airways and destruction of the alveoli, reducing their capacity to expand, and may also increase the mucous secretions that obstruct the airways, thus causing obstructive lung function impairment[5]. Therefore, the migration of periodontal pathogens into the airways and alveoli may contribute to the association between periodontitis and reduced lung function. An intervention study showed that periodontal therapy in COPD patients with periodontitis could improve their lung function [18].

FEV₁ and FEV₁/FVC are the most commonly used lung function parameters to assess ventilation dysfunction. A longitudinal study in the general Japanese population found that periodontitis was a risk factor for rapid FEV₁ decline [8]. Two population-based studies showed that reduced FEV₁/FVC was associated with poor periodontal health [7, 11]. In this study, we found that SSP were negatively associated with post-FEV₁ and FEV₁/FVC after adjusted for several confounding factors, which were further confirmed by subgroup analyses. However, when participants were stratified by respiratory diseases, SSP were only significantly associated with post-FEV₁ and post-FEV₁/FVC in participants without respiratory diseases. This is likely because severe periodontitis has a weaker effect on lung function than these respiratory diseases do on lung function impairment.

In this study, we found that SSP were significantly associated with post-FEV₁/FVC < 0.7 in the adjusted models. These results were not consistent with the two previous large population-based studies that more likely used pre-FEV₁/FVC data [11, 12]. Meanwhile, the different study population and definition of periodontitis may also contribute to the inconsistence of the results. As the post-FEV₁/FVC < 0.7 is a requirement for COPD diagnosis [13], the results provide evidence for the association between periodontitis and COPD or irreversible airflow obstruction.

Our study has some strengths. First, the participants were enrolled by a multistage stratified cluster sampling procedure from the national population aged 20 to 89 years. The good representation of the study population and the large sample size make the results more reliable. Second, we used post-bronchodilator lung function data to further examine the associations between SSP and lung function.

There are also several limitations in this study. First, this is a cross-sectional study, so a cause and effect relationship can not be established by this study. Second, some participants were excluded due to missing data or unreliable lung function test results, which slightly decreased the good representation of the study population. Third, no clinical data on periodontitis was collected in this study. The CPHS was a nation-wide study on pulmonary health. Clinical examination of periodontal health for the participants was difficult in this study as its large sample size. Therefore, SSP including tooth mobility and natural tooth loss acquired from a questionnaire were used to alternate the periodontal clinical examination. About 22% of the participants had SSP in this study that was a little lower than the prevalence of severe periodontitis of China (about 30%) according to the 4th Chinese national oral health epidemiological survey [2]. In addition, recall bias may affect the validity of SSP. SSP may probably underestimate the real prevalence of severe periodontitis in the participants of the study. Last, some other risk factors for lung function decline, such as air pollution, were not included in this study. This may partially reduce the strength of the conclusions.

In conclusion, this large and nation-wide population based cross-sectional study showed that SSP were negatively associated with post-bronchodilator lung function in the Chinese population. Large-scale and long-term longitudinal cohort studies are needed to confirm these associations in the future.

The datasets used during the current study are available from the corresponding author.

COPD:

Chronic obstructive pulmonary disease

FEV₁ :

Forced expiratory volume in 1 s

FVC:

Forced vital capacity

SSP:

Symptoms of severe periodontitis

OR:

Odds ratios

CI:

Confidence interval

CPHS:

China Pulmonary Health Study

GOLD:

Global Initiative for Chronic Obstructive Lung Disease

BMI:

Body mass index

The authors are grateful to all the participants and staff of China Pulmonary Health

Study.

This study was supported by the National Natural Science Foundation of China [grant no. 81901003] and the Special Research Foundation for Public Welfare of Health, Ministry of Health of China [grant no. 201002008].

Authors and Affiliations

1. Department of Stomatology, Beijing Chao-Yang Hospital, Capital Medical University, 8 Gongti South Road, Chaoyang District, Beijing, 100020, China

   Zhiqiang Liu, Xuan Zhou & Zuomin Wang

2. Department of Clinical Epidemiology, Beijing Chao-Yang Hospital, Capital Medical University, Beijing, China

   Lirong Liang

3. Beijing Institute of Respiratory Medicine, Beijing, China

   Lirong Liang, Kewu Huang & Yingxiang Lin

4. Department of Oral Science and Translational Research, Nova Southeastern University College of Dental Medicine, Florida, USA

   Xiaozhe Han

5. Department of Pulmonary and Critical Care Medicine, Center of Respiratory Medicine, China-Japan Friendship Hospital, 2 Yinghuayuan Dongjie, Chaoyang District, Beijing, 100029, China

   Ting Yang & Chen Wang

6. National Clinical Research Center for Respiratory Diseases, Beijing, China

   Ting Yang & Chen Wang

7. Institute of Respiratory Medicine, Peking Union Medical College, Beijing, China

   Ting Yang & Chen Wang

8. Department of Respiratory Medicine, Capital Medical University, Beijing, China

   Ting Yang & Chen Wang

9. Department of Pulmonary and Critical Care Medicine, Beijing Key Laboratory of Respiratory and Pulmonary Circulation Disorders, Beijing Chao-Yang Hospital, Beijing, China

   Kewu Huang & Yingxiang Lin

10. WHO Collaborating Center for Tobacco Cessation and Respiratory Diseases Prevention, Beijing, China

    Chen Wang

Contributions

All authors have made substantial contributions to the conception and design of the study. ZL, XZ, LL, TY, KH, YL, ZW and CW have been involved in data collection and data analysis. ZL, LL, XH, ZW and CW have been involved in data interpretation, drafting the manuscript and revising it critically. All authors have given final approval for the version to be published.

Corresponding authors

Correspondence to Zuomin Wang or Chen Wang.

Ethics approval and consent to participate

The study was approved by the ethics review committee of Beijing Capital Medical University and other participating institutes and was conducted in accordance with the Helsinki Declaration of 1975, as revised in 2013. Written informed consent was obtained from all study participants.

Consent for publication

Not applicable.

Competing interests

The authors declare that they have no competing interests.

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