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Autoimmune Connective Tissue Disease Following Carbon Monoxide Poisoning: A Nationwide Population-Based Cohort Study

Authors Huang CC , Ho CH , Chen YC , Hsu CC, Lin HJ, Wang JJ, Guo HR 

Received 5 June 2020

Accepted for publication 3 November 2020

Published 20 November 2020 Volume 2020:12 Pages 1287—1298

DOI https://doi.org/10.2147/CLEP.S266396

Checked for plagiarism Yes

Review by Single anonymous peer review

Peer reviewer comments 3

Editor who approved publication: Professor Irene Petersen



Chien-Cheng Huang,1– 3 Chung-Han Ho,4,5 Yi-Chen Chen,4 Chien-Chin Hsu,1,6 Hung-Jung Lin,1,7 Jhi-Joung Wang,4,8 How-Ran Guo2,9,10

1Department of Emergency Medicine, Chi Mei Medical Center, Tainan, Taiwan; 2Department of Environmental and Occupational Health, College of Medicine, National Cheng Kung University, Tainan, Taiwan; 3Department of Senior Services, Southern Taiwan University of Science and Technology, Tainan, Taiwan; 4Department of Medical Research, Chi Mei Medical Center, Tainan, Taiwan; 5Department of Hospital and Health Care Administration, Chia Nan University of Pharmacy and Science, Tainan, Taiwan; 6Department of Biotechnology, Southern Taiwan University of Science and Technology, Tainan, Taiwan; 7Department of Emergency Medicine, Taipei Medical University, Taipei, Taiwan; 8Allied AI Biomed Center, Southern Taiwan University of Science and Technology, Tainan, Taiwan; 9Department of Occupational and Environmental Medicine, National Cheng Kung University Hospital, Tainan, Taiwan; 10Occupational Safety, Health and Medicine Research Center, National Cheng Kung University Hospital, Tainan, Taiwan

Correspondence: How-Ran Guo
Department of Environmental and Occupational Health, College of Medicine, National Cheng Kung University, 1 Daxue Road, East District, Tainan City 701, Taiwan
Tel +886-6-235-3535
Fax +886-6-275-2484
Email [email protected]

Background: In addition to hypoxia, oxidative stress and inflammation due to carbon monoxide (CO) poisoning cause adverse health effects. These mechanisms are related to the occurrence of autoimmune connective tissue disease, but studies on the association between CO poisoning and autoimmune connective tissue disease are limited. We conducted a study to evaluate the occurrence of autoimmune connective tissue disease following CO poisoning.
Methods: We identified participants with CO poisoning diagnosed between 1999 and 2012 from the Nationwide Poisoning Database and selected participants without CO poisoning from the Taiwan National Health Insurance Research Database with matching age and index dates at a 1:3 ratio. Sex, underlying comorbidities, and monthly income were also included in the analyses. We followed up the participants until 2013 and made comparison of the risk of autoimmune connective tissue disease between participants with and without CO poisoning.
Results: The 23,877 participants with CO poisoning had a higher risk for autoimmune connective tissue disease than the 71,631 participants without CO poisoning (adjusted hazard ratio [AHR], 3.5; 95% confidence interval [CI], 3.1– 3.9) after adjustment for sex, diabetes, Lyme disease, herpes zoster, infectious mononucleosis, hepatitis, HIV infection, liver disease, renal disease, non-CO poisoning or drug abuse, malignancy, hypertension, hyperlipidemia, coronary artery disease, congestive heart failure, chronic obstructive pulmonary disease, and monthly income. An increased risk was observed even after 4 years of follow-up (AHR, 3.6; 95% CI, 3.0– 4.4).
Conclusion: The risk of autoimmune connective tissue disease increased following CO poisoning. Close follow-up of the patients with CO poisoning for the development of connective tissue disease is recommended, and further investigation of the detailed mechanisms is warranted.

Keywords: autoimmune, carbon monoxide poisoning, connective tissue disease, hypoxia, inflammation, oxidative stress

Introduction

Carbon monoxide (CO) poisoning is an important health problem worldwide. It accounts for more than 50,000 emergency department visits per year1 and 1319 deaths in 2014 in the United States.2 In Taiwan, there were 25,912 cases diagnosed between 1999 and 2012 as having CO poisoning, which resulted in about 500 deaths after acute poisoning.3 In addition to acute fatality, CO poisoning also contributed to increased long-term mortality and neurological sequelae including impairments of concentration or language, affective behavioral changes, memory loss, inability to calculate, vestibular problem, Parkinsonism, or corticospinal tract signs of damage, etc.3–7

A major mechanism through which CO poisoning introduces adverse health effects is the hypoxic injury to the tissue, which is a result of the nearly 250 times greater affinity that hemoglobin (Hb) has for CO than oxygen and leftward shift of O2Hb dissociation curve.1,8 Another mechanism of CO poisoning is the inflammatory reaction that increases oxidative stress and the production of reactive oxygen species (ROS), which can lead to ongoing inflammation and necrosis.1 The main target organs are the heart and brain due to their high need for oxygen.1 A study based on a nationwide database in Taiwan found that CO poisoning results in a nearly 2-fold increase in the risk of diabetes9 and argued that hypoxic injury, as well as inflammatory and immunological reactions in the brain and other organs, including the pancreas, led to the increased risk.9

Autoimmune connective tissue disease, which includes systemic lupus erythematosus, rheumatoid arthritis, Sjögren’s syndrome, scleroderma (systemic sclerosis; systemic scleroderma), and mixed connective tissue disease, is characterized by spontaneous overactivity of the immune system that results in over-production of antibodies which are found in the circulatory system.10 In Taiwan, the prevalence and incidence of autoimmune connective tissue disease were 101.3 per 100,000 populations and 41.3 per 100,000 person‐years, respectively.11 Patients with autoimmune connective tissue disease had a significant higher mortality and morbidity than the general population.11 In addition to genetic factors, environmental factors are found to be associated with autoimmune connective tissue disease.12,13 Hypoxia, oxidative stress, and inflammation induced by CO poisoning may increase the risk of autoimmune connective tissue disease through the production of autoantibodies.14–19 Oxidative stress contributes to the pathogenesis, organ damages, and comorbidities in systemic lupus erythematosus.19 The effects of oxidative stress include oxidative modification of self-antigens and T-cell dysfunction.19 Oxidative stress is also suggested to be associated with mitochondrial dysfunction, which may lead to Sjøgren’s syndrome.18 There were no reports on the association between CO poisoning and autoimmune connective tissue disease in a literature search using “carbon monoxide poisoning,” “connective tissue disease,” “systemic lupus erythematosus,” “rheumatoid arthritis,” “Sjögren’s syndrome,” “scleroderma,” “systemic sclerosis,” and “systemic scleroderma” as keywords through PubMed and Google Scholar. Therefore, we hypothesized that CO poisoning may be associated with autoimmune connective tissue disease through hypoxic injury, oxidative stress, or both and thus conducted a study to evaluate this potential association.

Materials and Methods

Data Sources

In this nationwide population-based cohort study, we used two subsets of data from the Taiwan National Health Insurance Research Database (NHIRD), namely, the Nationwide Poison Database (NPD) and the Longitudinal Health Insurance Database 2000 (LHID2000). The National Health Research Institutes maintain the NHIRD, which covers nearly 100% of the population in Taiwan, and provides it to scientists for research purposes.3 The NPD includes all the cases of poisonings between 1999 and 2013 in Taiwan, and the LHID2000 contains all the registration and claim data on 1,000,000 individuals randomly selected from the original NHIRD.3

Study Design, Setting, and Participants

We identified all patients diagnosed with CO poisoning between 1999 and 2012 from the NPD as the study cohort. The comparison cohort was made up of participants without CO poisoning who were randomly selected from the LHID2000 through exact matching of ages and index dates with the study cohort at a 1:3 ratio. According to our previous studies,20,21 the 1:3 ratio for matching is sufficient for providing statistical power to answer the research question with adjustment for major potential confounding factors. The index date was defined as the date of hospitalization or visit to the emergency department by the participant with CO poisoning (Figure 1).

Figure 1 Flowchart of this study.

Definitions of Variables

We defined a patient with CO poisoning as a participant who has been assigned diagnosis codes 986, E868, E952, or E982 according to the International Classification of Diseases, Ninth Revision, Clinical Modification (ICD-9-CM) during hospitalization or a visit to the emergency department. The use of both ICD-9-CM of 986 and E-codes (including E868, E952, and E982) has been validated as an effective method to identify patients with CO poisoning22 and adopted in many studies.3,7,9,20,21 A patient of autoimmune connective tissue disease was defined as a participant who has been assigned ICD-9-CM diagnosis codes 710 or 714 during at least one hospitalization or at least three visits for ambulatory care. Those who had been diagnosed with autoimmune connective tissue disease before the index date were excluded. Therefore, all patients with CO poisoning were right censored on December 31, 2013 or on the date of autoimmune connective tissue disease diagnosis, withdrew from the insurance program, lost for follow-up, or presence of mortality records. The person-years of follow-up were calculated accordingly for each participant, and the maximum follow-up period for participants was 15 years.

The age subgroups were defined as <20, 20–34, 35–49, 50–64, and ≥65 years. We studied underlying comorbidities and potential confounders for autoimmune connective tissue disease in the analyses,23–25 including diabetes (ICD-9-CM: 250), Lyme disease (ICD-9-CM: 088.81), herpes zoster (ICD-9-CM: 053), infectious mononucleosis (ICD-9-CM: 075), hepatitis (ICD-9-CM: 070), HIV infection (ICD-9-CM: 042, 07953, or V08), liver disease (ICD-9-CM: 570–576), renal disease (ICD-9-CM: 580–593), non-CO poisoning or drug abuse (ICD-9-CM: 960–989, 303–305), malignancy (ICD-9-CM: 140–208), hypertension (ICD-9-CM: 401–405), hyperlipidemia (ICD-9-CM: 272), coronary artery disease (ICD-9-CM: 410–414), congestive heart failure (ICD-9-CM: 428), and chronic obstructive pulmonary disease (ICD-9-CM: 496). Liver disease included acute and subacute necrosis of liver (ICD-9-CM: 570), chronic liver disease and cirrhosis (ICD-9-CM: 571), liver abscess and sequelae of chronic liver disease (ICD-9-CM: 572), other disorders of liver (ICD-9-CM: 573), cholelithiasis (ICD-9-CM: 574), other disorders of gallbladder (ICD-9-CM: 575), and other disorders of biliary tract (ICD-9-CM: 576). The subgroups of monthly income were defined as <20,000, 20,000–40,000, and >40,000 New Taiwan Dollars (NTD).

Comparison of the Risk of Autoimmune Connective Tissue Disease Between the Two Cohorts

We compared the risk of autoimmune connective tissue disease between the two cohorts by following up the participants until 2013. Stratified analyses were also performed according to the common types of autoimmune connective tissue disease (systemic lupus erythematosus [ICD-9-CM: 710.0], rheumatoid arthritis [ICD-9-CM: 714], and Sjögren’s syndrome and Scleroderma [ICD-9-CM: 710.2, 710.1]), age group, sex, underlying comorbidities, and follow-up period.

Ethical Statement

We conducted this study strictly according to the Declaration of Helsinki. This study was reviewed and approved by the Institutional Review Board (IRB) at Chi Mei Medical Center (approval number: 10407-E01). The NHIRD is not freely available and is limited to research purposes only. Applicants must follow the regulations of National Health Insurance Administration and National Health Research Institutes. All applications are reviewed for approval of data release. Informed consent from the participants was waived by the IRB because the NHIRD contains de-identified information only. The waiver did not affect the rights and welfare of the participants.

Statistical Methods

In the comparisons of demographic data, underlying comorbidities, and monthly income between the two cohorts, we used independent t-tests to evaluate the differences in continuous variables and chi-square tests to evaluate those in categorical variables. The comparison of the risk for autoimmune connective tissue disease between the two cohorts was performed using Cox proportional hazard regression analysis with adjustment for sex, monthly income, and comorbidities. Crude hazard ratio (HR) was defined as the incidence rate of autoimmune connective tissue disease in the participants with CO poisoning divided by that in the participants without CO poisoning. Adjusted HR (AHR) was obtained through including potential confounders in the regression model. Because “death” is a competing risk with the outcome measurement of “autoimmune connective tissue disease” in this study, we also performed a competing risk survival analysis to compare with the results by Cox proportional hazard regression analysis. The Kaplan–Meier’s method and the Log rank test were used to compare the risk for autoimmune connective tissue disease between the two cohorts during the follow-up. We used Cox proportional hazard regression analysis to identify independent predictors for autoimmune connective tissue disease and evaluate their effects. All the analyses were performed using SAS 9.4 for Windows (SAS Institute, Cary, NC, USA) at a two-tailed significance level of 0.05.

Results

In total, we identified 23,877 participants with CO poisoning and 71,631 participants without CO poisoning for this study. The mean age was 36.4 (standard deviation=15.5) years, and 39.2% of participants with CO poisoning were 20–34 years of age, followed by 31.7% in 35–49 years (Table 1). The sex ratio within participants with CO poisoning was nearly 1 to 1. There were higher rates of prevalence of many underlying comorbidities in the participants with CO poisoning than in the participants without CO poisoning, including diabetes, alcohol abuse, HIV infection, liver disease, renal disease, non-CO poisoning or drug abuse, malignancy, hypertension, hyperlipidemia, coronary artery disease, congestive heart failure, and chronic obstructive pulmonary disease. However, participants with CO poisoning had a lower prevalence rate of hepatitis. Participants with CO poisoning also had a higher percentage of earning low monthly income than the participants without CO poisoning.

Table 1 Age, Sex, Underlying Comorbidities, and Monthly Income in Participants with and without CO Poisoning

Compared to participants without CO poisoning, participants with CO poisoning had an increased risk for autoimmune connective tissue disease after adjusting for sex, diabetes, Lyme disease, herpes zoster, infectious mononucleosis, hepatitis, HIV infection, liver disease, renal disease, non-CO poisoning or drug abuse, malignancy, hypertension, hyperlipidemia, coronary artery disease, congestive heart failure, chronic obstructive pulmonary disease, and monthly income (AHR, 3.5; 95% confidence interval [CI], 3.1–3.9) (Table 2). Competing risk survival analysis showed the similar finding (AHRcompeting, 3.2; 95% CI, 2.8–3.6). The results were similar in the subgroup analyses for systemic lupus erythematosus, rheumatoid arthritis, and Sjögren’s syndrome and scleroderma. Both Kaplan–Meier’s method and Log rank test showed an increased risk for autoimmune connective tissue disease in the participants with CO poisoning compared to in the participants without CO poisoning (Figure 2). Stratified analyses showed that the increased risk was more prominent in the subgroups with non-CO poisoning or drug abuse (AHR, 5.1; 95% CI, 2.2–11.9) and the subgroups with chronic obstructive pulmonary disease (AHR, 5.3; 95% CI, 2.1–13.4). An increased risk was observed during the whole follow-up period, even after 4 years (AHR, 3.6; 95% CI, 3.0–4.4). We took all the participants including study and comparison cohorts together for analysis and found that CO poisoning, older age, female sex, liver disease, renal disease, and coronary artery disease were independent predictors for autoimmune connective tissue disease (Table 3).

Table 2 Comparison of the Risk for Autoimmune Connective Tissue Disease Between Participants with and without CO Poisoning Using Cox Proportional Hazard Regression Analysis

Table 3 Independent Predictors for Autoimmune Connective Tissue Disease in the All Participants by Cox Proportional Hazard Regression Analysis

Figure 2 Comparison of the risk of autoimmune connective tissue disease between participants with and without CO poisoning during follow-up by Kaplan–Meier’s method and the Log rank test.

Discussion

This study showed that participants with CO poisoning had an increased risk of autoimmune connective tissue disease than the participants without CO poisoning, including those who had systemic lupus erythematosus, rheumatoid arthritis, or Sjögren’s syndrome and scleroderma and that the increase was observed during the whole follow-up period, even after 4 years. The increased risk was more prominent in participants with chronic obstructive pulmonary disease and participants with non-CO poisoning or drug abuse. In addition to CO poisoning, older age, female sex, liver disease, renal disease, and coronary artery disease were also identified as independent predictors for autoimmune connective tissue disease.

Connective tissue disease is complex and includes various genetic and environmental factors.13 A possible explanation for increased autoimmune connective tissue disease is the hypoxia and oxidative stress induced by CO poisoning.13–17 The pathogenesis of autoimmune oxidative stress, a kind of environment factor, is the excess production of ROS and reactive nitrogen species.26–28 Excessive oxidative stress may enhance inflammation, break down the immunological tolerance, and induce apoptotic cell death, gene activation and generation of novel autoantigens, which are thought to play important roles in the development of autoimmune connective tissue disease.13,28 Hypoxia leads to higher collagen synthesis, myofibroblast differentiation of fibroblasts, and productions of cytokine, chemokine, and TGF-β by dendritic cells, which all induce the autoimmune reaction.17 There is no direct evidence of the association between hypoxia and autoimmune connective tissue disease. However, a study reported that obstructive sleep apnea may increase disease severity and circulating inflammatory markers in patients with autoimmune connective tissue disease.29 Many environmental factors, including infections, UV irradiation, coldness, and emotional stress, have been well recognized as developing and exacerbating factors for autoimmune connective tissue disease.13 This study showed an association between CO poisoning and subsequent diagnosis of autoimmune connective tissue disease, which is a novel finding and worthy of further investigation.

Previous studies showed that delayed neuropsychiatric sequelae, a sequela following CO poisoning, may be caused by immunological response.30,31 In rats, CO poisoning causes adduct formation between myelin basic protein (MBP) and malondialdehyde, which results in an immunological cascade.30 In the brain tissues of rats with CO poisoning, a variety of microglia and expression of immune factors, including major histocompatibility complex II (MHCII), CD4, vascular cell adhesion molecule-1 (VCAM-1), and interferon-gamma (IFN-gamma) were found.31

This study also found that the increased risk for autoimmune connective tissue disease was more prominent in the participants with chronic obstructive pulmonary disease. Smoking is the major causative factor of chronic obstructive pulmonary disease32 and some studies have shown that carbon monoxide from smoking, an environmental factor, increased the risk for systemic lupus erythematosus.12,33 Carbon monoxide and other toxic components from smoking (including tars, polycyclic aromatic hydrocarbons, nicotine, and free radicals) can induce oxidative stress and directly damage endogenous proteins and DNA, leading to genetic mutations and gene activation, which could be involved in development of systemic lupus erythematosus.33 Via the same pathophysiology pathway, smoking is also implicated as one of the most important extrinsic risk factors for the development and consequent severity of rheumatoid arthritis.34 The association between smoking and rheumatoid arthritis has been demonstrated through epidemiologic studies, in vivo experiments, and animal models.34 In patients with primary Sjögren’s syndrome, smoking also has a positive association with anti-nuclear antibody positivity.35 Smoking is suggested to have negative effects on the vascular, gastrointestinal, and respiratory outcomes of scleroderma.36 A possible explanation for the prominent risk in the participants with chronic obstructive pulmonary disease is that smoking, in conjunction with CO poisoning, might have an additional effect on the development of autoimmune connective tissue disease.

The association between non-CO poisoning or drug abuse and autoimmune connective tissue disease has not been determined. Some studies have found that recreational drugs such as cocaine, amphetamines, marijuana, and heroin, acting as environmental toxins, may stress and injury immune stem cells and engender subsequent autoimmune disease development and progression.37,38

Older age and female sex were independent predictors for autoimmune connective tissue disease in this study. Using participants <20 years old as references, we found the risk of autoimmune connective tissue disease increased with age (AHR = 1.7 in age 20–34 years, AHR = 2.9 in age 35–49 years, AHR = 4.3 in age 50–64 years, and AHR = 5.0 in age ≥65 years). Therefore, older age appeared to be a predictor for autoimmune connective tissue disease. In systemic lupus erythematosus, peak incidence occurs between the age of 15 and 40 years old, with a female-to-male ratio of 6:1 to 10:1.39 In a study of the geriatric population, the prevalence of rheumatoid arthritis predominated in participants of the female sex, increased together with age, and reached approximately 2%.40 Sjögren’s syndrome increases with age and dominates in the female sex with a female-to-male ratio of 9:1.39 The onset of scleroderma is most common in those 30–50 years old, and the female-to-male ratio is between 5:1 and 14:1.39

It is well known that complications of the liver, kidneys, and coronary artery may develop in autoimmune connective tissue disease.41–43 In the current study, however, we found that liver disease, renal disease, and coronary artery disease were independent predictors for autoimmune connective tissue disease, which is has not been reported in the literature. A possible explanation is that these complications were sometimes recognized before the diagnosis of autoimmune connective tissue disease. It is also possible that there are bi-directional causal relationships between these diseases and autoimmune connective tissue disease.

The strength of this study is its novel finding of a higher risk of autoimmune connective tissue disease in patients with CO poisoning. It provides an insight into a previously unknown relationship between CO poisoning and autoimmune diseases. In addition to having the potential of informing public health practices, it may also help understanding the contributions of environmental risk factors to autoimmune diseases. It also has some limitations, however. First, the claim data used in this study is not collected for the purposes of research. Validation of definitions for CO poisoning, connective tissue disease, and underlying comorbidities are needed. Second, the participants without CO poisoning might have CO poisoning before 1999. Because the NPD includes the data between 1999 and 2013, we could not exclude the participants who had CO poisoning in the comparison cohort. In addition, some participants with CO poisoning might not be recognized or diagnosed due to insignificant symptoms and thus selected as members of the comparison cohort. This will lead to underestimation of the effect. However, this study showed an increased risk for autoimmune connective tissue disease in the study cohort using the comparison cohort as the reference and so the conclusion would not be affected by such misclassification. Third, there were no data on family history, smoking, lifestyle, or environmental exposure in this study, all of which are factors with the potential of confounding the results. However, we have adjusted for common underlying comorbidities, and they might serve as the surrogates for some of the unavailable data. For example, chronic obstructive pulmonary disease might serve as a surrogate measurement of smoking and diabetes, hypertension, and hyperlipidemia might serve as surrogate measurements of lifestyle. Fourth, we did not evaluate the effects of the severity of CO poisoning on risk for autoimmune connective tissue disease. Further studies which are able to determine the severity of CO poisoning in the participants are warranted. Fifth, although we included all four major autoimmune connective tissue diseases (systemic lupus erythematosus, rheumatoid arthritis, Sjögren’s syndrome, and scleroderma) as the outcomes in the analysis, the results may not stand for all the autoimmune connective tissue diseases. Sixth, despite this being a nationwide study that covered a large population, the result may not be generalized to other nations with different genetic makeups. Validation of the result in other nations is needed. Seventh, this study reported an epidemiological result based on the rationale of hypoxia and oxidative stress; however, further basic studies are needed to clarify the detailed pathophysiology.

Conclusions

This nationwide population-based cohort study found that the risk for autoimmune connective tissue disease increased following CO poisoning, even in the subgroup’s analyses for systemic lupus erythematosus, rheumatoid arthritis, and Sjögren’s syndrome and scleroderma. The increase in the risk was observed throughout the whole follow-up period, even after 4 years. Hypoxia, oxidative stress, and inflammation are suspected to be the causes. In addition to CO poisoning, we also identified older age, female sex, liver disease, renal disease, and coronary artery disease as in dependent predictors for autoimmune connective tissue disease. The positive association between smoking and autoimmune connective tissue disease may explain the increased risk of being more prominent in the subgroup with chronic obstructive pulmonary disease. Further studies, including validation in other nations and those that delineate the detailed pathophysiology of the development of autoimmune connective tissue disease as caused by hypoxia and oxidative stress are warranted.

Acknowledgments

This study was supported by grants MOST 109-2314-B-384-005-MY3 and MOST 108-2638-B-006-001-MY2 from the Ministry of Science and Technology and grants CMFHR10734 and CMFHR10832 from Chi Mei Medical Center. We thank Miss Ti Hsu for the English revision.

Author Contributions

All authors made substantial contributions to conception and design, acquisition of data, or analysis and interpretation of data; took part in drafting the article or revising it critically for important intellectual content; agreed to submit to the current journal; gave final approval of the version to be published; and agree to be accountable for all aspects of the work.

Disclosure

The authors report no conflicts of interest in this work.

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