[학술논문] 감염성 존재량과 뇌졸중 위험

감염성 존재량과 뇌졸중 위험(Infectious Burden and Risk of Stroke)

미첼 엘킨드(컬럼비아대학 메디칼센터, 신경과전문의) 박사팀이 [신경학 기록(Archives of Neurology)]에 기고한 논문입니다.

뉴욕의 맨하튼에 거주하는 1625명이 성인(평균연령 68.4세)을 평균 7.6년동안 5가지 전염병 원인체에 대한 혈청학적 조사 분석해본 결과라고 합니다. 조사기간 동안 뇌졸증이 나타난 환자들의 대다수가 5가지 중에서 1가지 이상의 병원체에 감염된 것으로 밝혀졌다고 합니다.

혈청학적 조사 분석 대상 5가지 병원체는 클라미디아 폐렴균(Chlamydiapneumoniae), 헬크코박터 파일로리균(Helicobacter pylori), 사이토메갈로바이러스(cytomegalovirus), and 단순포진 바이러스 1, 2(herpessimplex virus 1 and 2)였습니다.

이러한 결과는 뇌졸증과 병원체의 연관 가능성을 시사하는 것이지만… 연구자들은 병원체들이 동맥기능에 어떤 손상을 입히는지를 명확히 규명하지는 못했습니다. 교신저자인 미첼 엘킨드 박사는 언론과 인터뷰에서 “만성감염이 혈관에 염증을 일으켜 혈류를 위축시키거나 병원균 자체가 동맥벽의 기능을 손상시키기 때문”에 뇌졸증을 유발하는 것으로 추정한다고 밝혔습니다.

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Infectious Burden and Risk of Stroke

The Northern Manhattan Study

Mitchell S. V. Elkind, MD, MS; Pankajavalli Ramakrishnan, MD, PhD; Yeseon P. Moon, MS; Bernadette Boden-Albala, DrPH; Khin M. Liu, BS; Steve L. Spitalnik, MD, PhD; Tanja Rundek, MD, PhD; Ralph L. Sacco, MD, MS; Myunghee C. Paik, PhD

출처 : Arch Neurol. 2010;67(1):(doi:10.1001/archneurol.2009.271).
http://archneur.ama-assn.org/cgi/content/full/2009.271?home

ABSTRACT

Objective To determine the association between a compositemeasure of serological test results for common infections (Chlamydiapneumoniae, Helicobacter pylori, cytomegalovirus, and herpessimplex virus 1 and 2) and stroke risk in a prospective cohortstudy.

Design Prospective cohort followed up longitudinally formedian 8 years.

Setting Northern Manhattan Study.

Patients Randomly selected stroke-free participants froma multiethnic urban community.

Main Outcome Measure Incident stroke and other vascularevents.

Results All 5 infectious serological results were availablefrom baseline samples in 1625 participants (mean [SD] age, 68.4[10.1] years; 64.9% women). Cox proportional hazards modelswere used to estimate associations of each positive serologicaltest result with stroke. Individual parameter estimates werethen combined into a weighted index of infectious burden andused to calculate hazard ratios and confidence intervals forassociation with risk of stroke and other outcomes, adjustedfor risk factors. Each individual infection was positively,though not significantly, associated with stroke risk afteradjusting for other risk factors. The infectious burden indexwas associated with an increased risk of all strokes (adjustedhazard ratio per standard deviation, 1.39; 95% confidence interval,1.02-1.90) after adjusting for demographics and risk factors.Results were similar after excluding those with coronary disease(adjusted hazard ratio, 1.50; 95% confidence interval, 1.05-2.13)and adjusting for inflammatory biomarkers.

Conclusions A quantitative weighted index of infectiousburden was associated with risk of first stroke in this cohort.Future studies are needed to confirm these findings and to furtherdefine optimal measures of infectious burden as a stroke riskfactor.

INTRODUCTION

Stroke is the third leading cause of death in the United Statesand the leading cause of serious disability.¹ Classic modifiablerisk factors include hypertension, cardiac disease, dyslipidemia,and smoking, but many strokes occur in patients without anyof these risk factors.¹ There is therefore interest in identifyingadditional modifiable stroke risk factors. Seroepidemiologicalstudies in patients with coronary artery disease and strokehave provided evidence of an association of risk with serologicalevidence of prior infections with various pathogens such asChlamydia pneumoniae, Helicobacter pylori, and herpesviruses.^2-8In addition, several of these organisms have been identifiedin atherosclerotic tissue specimens, and some have been foundcapable of inducing atherosclerosis in animal models.^9-10

Mechanistically, these pathogens are thought to promote inflammation,thus contributing to atherosclerosis.^11-12 Prospective studiesand meta-analyses, however, have suggested that the associationof individual serological test results with risk of vascularevents is modest.² A more likely scenario is that a compositemeasure of multiple serological results, or infectious burden(IB), is associated with risk.^13-16 According to this hypothesis,the greater the number of infectious exposures during one’slifetime, the higher the chance of promoting atherosclerosisvia inflammation, thus increasing the risk of cardiovasculardisease. Some investigators have provided support for this conceptby correlating the number of positive serological test resultswith the presence of atherosclerosis and carotid plaque progressionor risk of vascular events, including stroke.^13-15,17 In thesestudies, however, all positive serological test results aregiven equal weight in predictive models. It is plausible, however,that different infections would each carry different weightsof association with risk of vascular disease.

We hypothesized that a weighted measure of IB would be associatedwith risk of incident stroke in a prospective cohort study ina multiethnic urban adult population. We further hypothesizedthat this same weighted measure would also be associated withother vascular event outcomes.

METHODS

PARTICIPANT SELECTION

The Northern Manhattan Study is a community-based prospectivecohort study designed to investigate stroke incidence, riskfactors, and predictors of severity and outcome, as describedpreviously.^18-19 Briefly, this is a stroke-free, multiethnic,urban population with a race/ethnic distribution of 63% Hispanic,20% non-Hispanic black, and 15% non-Hispanic white participantswho were recruited by random-digit dialing. A total of 3298participants were enrolled between 1993 and 2001 if they (1)had no prior diagnosis of stroke, (2) were older than 39 years,and (3) resided in northern Manhattan, New York, for at least3 months in a household with a telephone. All participants gaveinformed consent and the study was approved by Columbia UniversityMedical Center institutional review board.

Baseline data were obtained via interviews with bilingual researchassistants, physical and neurological examination by study physicians,inpatient assessments, and fasting blood specimen analysis.¹⁸Blood pressure, height, weight, fasting lipid panels, leukocytecount, and glucose level were measured by standard techniques.High-sensitivity C-reactive protein (hsCRP) level was measuredusing a BNII nephelometer (Dade-Behring, Deerfield, Illinois).Hypertension (history, taking medications, or systolic bloodpressure $≥$ 140 mm Hg or diastolic blood pressure $≥$ 90 mm Hg) anddiabetes mellitus (history, taking medications, or fasting bloodglucose level $≥$ 126 mg/dL [to convert to millimoles per liter,multiply by 0.0555]) were defined as described previously.¹⁹Blood samples collected at enrollment were centrifuged and frozenat –70°C in 1-mL aliquots until the time of analysis.Because not all participants had sufficient blood samples availablefor the multiple serological analyses required for this study,a subsample of 1625 participants was used for the present analyses.

SEROLOGICAL ANALYSES

Serological test results against 5 common pathogens that haveeach been linked to atherosclerotic disease in prior studieswere assessed. Enzyme-linked immunoassay was used to measureantibody titers against C pneumoniae (Savyon Diagnostics, Ashdod,Israel), H pylori, cytomegalovirus (CMV) (Wampole Laboratories,Princeton, New Jersey), and herpes simplex virus 1 (HSV-1) andherpes simplex virus 2 (HSV-2) (Focus Diagnostics, Cypress,California). Both IgG and IgA titers were measured for C pneumoniae,but based on previous results in our population^5-6 and others,³IgA titers were used for further analyses. IgG titers were assessedfor the other pathogens. Positive serological test results werebased on recommendations from the commercial laboratories providingthe assays. All serological testing was conducted by personnelblinded to clinical outcomes.

FOLLOW-UP ASSESSMENTS

Annual follow-up conducted by telephone included assessmentof vital status (dead or alive), interval hospitalizations,and presence of symptoms and events consistent with stroke ormyocardial infarction (MI) as previously described.^18-19 Strokeswere independently classified by 2 neurologists according toa modified Stroke Data Bank scheme,²⁰ with subtype assessmentsdetermined by consensus. Disagreements were adjudicated by athird neurologist evaluator. A study cardiologist reviewed MIsfor validation. First presentation of any type of stroke, ischemicor hemorrhagic, was defined according to the criteria establishedby the World Health Organization. Myocardial infarction wasdefined by criteria specified by the Cardiac Arrhythmia PilotStudy²¹ and the Lipid Research Clinics Coronary Primary PreventionTrial.²² All deaths were verified by a study physician and classifiedas vascular (stroke, MI, heart failure, pulmonary embolus, cardiacarrhythmia, and other vascular causes) or nonvascular.

STATISTICAL ANALYSES

The primary end point was all strokes; secondary end pointswere ischemic stroke, MI, vascular deaths, nonvascular deaths,all deaths, and a combined end point of stroke, MI, and vasculardeath. First, Cox proportional hazards models were used to estimatethe regression coefficients and 95% confidence intervals (CIs)for the association of each individual serological test resultwith risk of stroke in unadjusted models and models adjustedfor demographics, blood pressure, coronary artery disease, waistsize, alcohol consumption, physical activity, smoking, and levelsof blood glucose, high-density lipoprotein cholesterol, andlow-density lipoprotein cholesterol. We included variables inmultivariate models that were significant in prior analysesof vascular outcomes in the Northern Manhattan Study and thatare traditionally accepted risk factors for stroke. We usedcontinuous measures for blood pressure and blood glucose levelrather than cruder dichotomous measures such as hypertensionand diabetes in our main models based on evidence of continuousrelationships between these physiologic measures and risk ofvascular disease.²³ Additional models were run using hypertensionand diabetes mellitus as categorical variables.

Parameter estimates, or β coefficients, from a model containingonly the individual serological test results were then usedto derive a weighted index designated as the IB. Each parameterestimate represents the strength of the association betweenthe individual positive serological test result and stroke asan outcome. Individual parameter estimates for positive serologicaltest results were added together to form the IB index. Parameterestimates for negative serological test results would not becounted toward the total index score. For example, the IB fora participant with individual positive serological results forCMV and HSV-2 would equal the sum of the parameter estimatesfor only CMV and HSV-2. This index was then used as the independentvariable in unadjusted and adjusted models to calculate thehazard ratios (HRs) and CIs for association with risk of strokeand other outcomes. Further models were calculated among thosewithout history of MI. The final models among those withoutMI satisfied proportionality assumptions. Associations wereexpressed per change in standard deviation of IB.

RESULTS

Characteristics among the 1625 participants with serologicaldata are shown in Table 1 and were similar to those in the overallNorthern Manhattan Study cohort, with the exception that theparticipants in this study had enrolled later compared withthose who did not have all 5 infectious serological resultsat the time of enrollment. Mean (SD) age of participants was68.4 (10.1) years, and the median follow-up was 7.6 years (interquartilerange, 6.4-9.0 years). In follow-up, there were 67 strokes,of which 56 were ischemic; 98 MIs; 150 vascular deaths; 215nonvascular deaths; and 390 deaths of all causes. Frequenciesof positive serological results, using prespecified thresholds,for C pneumoniae, H pylori, CMV, HSV-1, and HSV-2 are givenin Table 1. Positive titers were common for these organisms,ranging from 55% for H pylori to 86% for HSV-1.

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Table 1. Participant Characteristics

Each infectious serological result was positively associatedwith an increased risk for all strokes, with HRs adjusted forage, sex, race/ethnicity, high school education, systolic bloodpressure, low-density lipoprotein cholesterol level, high-densitylipoprotein cholesterol level, blood glucose level, moderateto heavy activity level, waist size, and coronary artery diseaseranging between 1.13 for H pylori to 2.19 for CMV, althoughnone of these associations reached statistical significance(Table 2).

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Table 2. Risk of Stroke Associated With Positive Serological Results for C pneumoniae, H pylori, CMV, HSV-1, and HSV-2

To determine whether composite seropositivity was associatedwith risk of stroke, individual unadjusted parameter estimateswere added, as earlier, to generate the weighted IB index (mean[SD], 1.00 [0.33]; median, 1.08). The mean [SD] IB index forthose with positive results for each serological test is shownin the Figure. The mean IB index was higher in non-Hispanicblack (1.05 [0.31]) and Hispanic (1.07 [0.27]) individuals comparedwith non-Hispanic white individuals (0.75 [0.41]; P < .001for both comparisons). It was slightly higher in women (1.02[0.31]) than men (0.97 [0.36]; P = .002). There wasno difference by age.

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Figure. Mean infectious burden index (IBI) by serological status for each of the 5 infections. CMV indicates cytomegalovirus; C pneumoniae, Chlamydia pneumoniae; H pylori, Helicobacter pylori; HSV, herpes simplex virus.

Infectious burden was associated with risk of stroke (unadjustedHR per standard deviation, 1.39; 95% CI, 1.04-1.87), and theeffect was essentially unchanged after adjusting for demographics(adjusted HR, 1.42; 95% CI, 1.04-1.94) (Table 3). After adjustingfor age, sex, race/ethnicity, high school education, systolicblood pressure, low-density lipoprotein cholesterol level, high-densitylipoprotein cholesterol level, blood glucose level, moderateto heavy activity level, waist size, and coronary artery disease,the association remained (adjusted HR, 1.39; 95% CI, 1.02-1.90).Further adjusting for leukocyte count and hsCRP level had noeffect on this estimate. The magnitude of the correlation ofhsCRP level with IB index was only modest (r = 0.09;P < .001).

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Table 3. Risk of Stroke Associated With IB Index

Additional models were run using history of hypertension anddiabetes mellitus, as previously defined,¹⁹ in place of bloodpressure and blood glucose measurements, and the results wereessentially unchanged (adjusted HR per standard deviation changein IB, 1.42; 95% CI, 1.03-1.97). Further analyses limited tothose without history of MI (n = 1525) showed a modestlyincreased magnitude of effect (fully adjusted HR per standarddeviation, 1.50; 95% CI, 1.05-2.13).

Tests for interactions with age, sex, race/ethnicity, and otherrisk factors demonstrated a significant interaction with diabetesmellitus (P = .02). Among diabetic individuals, therewas an increased risk of stroke associated with IB (adjustedHR per standard deviation, 1.63; 95% CI, 1.16-2.29). The effectin nondiabetic individuals was reduced in magnitude and notstatistically significant (adjusted HR per standard deviation,1.29; 95% CI, 0.94-1.78). Other interactions were not significant.

All secondary end points were positively associated with IB.Nonvascular deaths (adjusted HR per standard deviation, 1.23;95% CI, 1.04-1.45) and the combined end point of all stroke,MI, and deaths (adjusted HR per standard deviation, 1.15; 95%CI, 1.03-1.29) reached statistical significance (Table 4).

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Table 4. Risk of Secondary Outcomes Associated With IB

COMMENT

In this prospective cohort study, a weighted index of exposureto 5 common infections previously implicated in atheroscleroticdisease was associated with risk of first stroke. Although individuallyeach infection was positively associated with increased strokerisk, none were individually statistically significant. Ourmeasure of IB considered the association of infections withstroke risk as a weighted measure rather than simply summingup the number of positive serological results, as had been donein prior studies. We therefore did not have an a priori assumptionabout the strength of association between each of the individualinfections and stroke risk. These results need to be validatedin independent populations, however, before they can be generalized.These results provide evidence that there is probably no singleinfectious agent responsible for atherosclerosis or stroke,but that a more likely mechanism for any possible associationof infection with stroke is through a more general proinflammatorymechanism.

The rationale for investigating these particular 5 pathogensis multifold. First, each of these common pathogens may persistafter an acute infection and thus contribute to perpetuatinga state of chronic, low-level infection. Second, prior studiesdemonstrated an association between each of these pathogensand cardiovascular diseases.^2-12 C pneumoniae, the best studiedof these infections in relation to atherosclerosis, is an atypicalrespiratory pathogen that has been investigated as a strokerisk factor in several case-control and prospective studies,with mixed results. In prior case-control studies from the northernManhattan population, C pneumoniae IgA titers were associatedwith increased stroke risk, though IgG titers were not.^5-6 Studiesin other populations have similarly found IgA to be a bettermarker of stroke risk than IgG titers.³ These results have notbeen confirmed in other studies, however, and prospective studieshave demonstrated at best a very modest association of C pneumoniaetiters with stroke risk.² Our present prospective study confirmsthat the effect of C pneumoniae IgA titers is likely to be modest.Further studies in large populations using well-standardizedassays with generally accepted titer cutoffs may be needed tomore definitively elucidate the relationship between C pneumoniaeand stroke.²

Recent studies have implicated H pylori, which is well recognizedas a cause of chronic gastric inflammation, ulceration, andcancer,²⁴ as another pathogen whose persistence might be associatedwith increased stroke risk. Several case-control studies havedemonstrated an increased risk of stroke in seropositive subjects.^25-27A meta-analysis of case-control studies on H pylori serostatusrevealed an increased risk for stroke (odds ratio, 1.41; 95%CI, 1.11-1.78), and especially for large-vessel stroke.²⁸ Thestroke risk appeared to be especially apparent in subjects seropositivefor strains with the virulence factor cytotoxin-associated geneproduct A (CagA) toxin.²⁸ Other studies have not found thisassociation, however.^{8, 17, 29-30} We did not limit our analysesto large-vessel stroke, however, nor did we measure H pyloriCagA toxin serostatus.

Cytomegalovirus is a common viral pathogen, and it can reactivateand cause particularly severe complications in immunocompromisedhosts, though even immunocompetent hosts can develop CMV disease.Cytomegalovirus has been implicated as a cause of transplantvasculopathy.^31-32 There is also some evidence that CMV is associatedwith stroke risk in otherwise healthy individuals. In 2 case-controlstudies, CMV seropositivity was associated with increased strokerisk,^33-34 though this was not confirmed in several prospectivestudies.^{7, 17, 35-36} It has been shown that in immunocompromisedhosts such as those with diabetes,³⁷ or in post–renaltransplant patients,³¹ the risk of atherosclerotic events includingstrokes is increased with CMV seropositivity. Cytomegaloviruswas most strongly associated with stroke risk among the 5 pathogenswe studied, though it did not reach statistical significance.Many of our participants (21%) had diabetes, and this may haveinfluenced our findings.

Herpes simplex virus 1 and HSV-2 are also viral pathogens withchronic persistence in a latent state. Early work on Marek diseasevirus, a type of chicken herpesvirus, demonstrated that thevirus was associated with atherosclerosis in a chicken model.³⁸Few studies have investigated the association of HSV with strokerisk, and their findings are conflicting. In 1 case-controlstudy, HSV-1 was associated with increased stroke risk,³⁴ butin another nested case-control study, neither HSV-1 nor HSV-2increased stroke risk.⁷ As with CMV, immunocompetent status,even when associated with diabetes, might be a confounding factor.

Our results extend the findings of previous prospective studiesaimed at investigating the association of IB and other vascularevents. In a secondary analysis of the Heart Outcomes PreventionEvaluation trial, combined serostatus for 4 pathogens vs zeroto 1 pathogen was associated with risk of MI, stroke, or cardiovasculardeath with a magnitude similar to what we found (HR, 1.41; 95%CI, 1.02-1.96).¹⁵ In that study, however, pathogen burden wasnot associated with stroke as an independent outcome. In theFramingham study, pathogen burden based on serostatus for Cpneumoniae, H pylori, and CMV was not associated with pooledprimary end points of MI, atheroembolic stroke, and coronaryheart disease death.¹⁷ A small case-control study did show amodest association between pathogen burden based on serologicalresults for Legionella pneumophila, Mycoplasma pneumoniae, andC pneumoniae and risk of stroke and transient ischemic attack.³⁹However, other small case-control studies investigating thepathogen burden using similar serological results did not findan increased risk for stroke, though they may have been underpowered.^{8, 34}

There are several differences between our study and these otherstudies. Most importantly, our weighted measure of IB avoideda priori assumptions about the strength of association betweeneach of the individual infections and stroke risk. Our studyalso included HSV-1 and HSV-2 serostatus in the calculationof the IB index, which may have enhanced the ability to detectits influence on first stroke. Small sample size, selectionbias, and case-control study design may account for some ofthe other differences. The Heart Outcomes Prevention Evaluationtrial, moreover, was a secondary prevention trial rather thana population-based study.

Our study also explored the association between IB and secondaryvascular outcomes. Nonvascular deaths and the combined end pointof all stroke, MI, and death were associated with the IB index,though MI and vascular death were not. Studies of periodontalinfection and vascular disease have similarly found that theremay be a stronger association for stroke than for MI.^40-41

Our study could have potential clinical implications. For example,treatment and eradication of these chronic pathogens might mitigatefuture risk of stroke. Antibiotic therapy directed against Cpneumoniae has been tested in randomized controlled trials withoutevidence of benefit against heart disease.^42-43 Whether thesame holds true for stroke has not yet been established. Morestudies will be required to further explore IB as a potentialmodifiable risk factor for stroke.

Our study has several strengths. First, this was a large, multiethnic,population-based prospective study with routine assessment ofrisk factors and minimal loss to follow-up. We had a large proportionof Hispanic individuals, a traditionally understudied group,in our population. Incidence of first stroke was assessed afteradjusting for traditional risk factors, as well as for hsCRPlevel and white blood cell count, variables previously shownto be associated with incident stroke.^{19, 44} The limitationsof our study include that participant information regardingthe use of specific cholesterol-lowering agents such as statins,preexisting inflammatory diseases, anti-inflammatory medicationuse, immunosuppression status, and infection status at the timeof stroke or other outcomes was unavailable. Availability ofthese data could have better accounted for known and other unknownconfounding factors. Further studies will be needed to confirmthe independent predictive effect of IB as a stroke risk factor.

AUTHOR INFORMATION

Correspondence: Mitchell S. V. Elkind, MD, MS, NeurologicalInstitute, 710 W 168th St, Box 182, New York, NY 10032 (mse13@columbia.edu

).

Accepted for Publication: May 31, 2009.

Published Online: November 9, 2009 (doi:10.1001/archneurol.2009.271).

Author Contributions: Dr Elkind had full access to all of thedata in the study and takes responsibility for the integrityof the data and the accuracy of the data analysis. Study conceptand design: Elkind, Rundek, Sacco, and Paik. Acquisition ofdata: Elkind, Boden-Albala, Liu, Spitalnik, and Rundek. Analysisand interpretation of data: Elkind, Ramakrishnan, Moon, Boden-Albala,Rundek, Sacco, and Paik. Drafting of the manuscript: Elkindand Ramakrishnan. Critical revision of the manuscript for importantintellectual content: Elkind, Moon, Boden-Albala, Liu, Spitalnik,Rundek, Sacco, and Paik. Statistical analysis: Moon and Paik.Obtained funding: Elkind and Sacco. Administrative, technical,and material support: Elkind, Ramakrishnan, Boden-Albala, Liu,Spitalnik, Rundek, and Sacco. Study supervision: Elkind, Spitalnik,Rundek, and Sacco.

Financial Disclosure: None reported.

Funding/Support: This research was supported by National Institutesof Health/National Institute of Neurological Disorders and Strokegrants R37 29993 (Drs Elkind and Sacco) and R01 48134(Dr Elkind).

Author Affiliations: Departments of Neurology (Drs Elkind and Boden-Albala and Ms Moon) and Pathology and Cell Biology (Ms Liu and Dr Spitalnik), College of Physicians and Surgeons, and Department of Biostatistics, Joseph P. Mailman School of Public Health (Dr Paik), Columbia University, New York, New York; Department of Neurology, Massachusetts General Hospital, Boston (Dr Ramakrishnan); and Departments of Neurology (Drs Rundek and Sacco) and Epidemiology and Genetics (Dr Sacco), Miller School of Medicine, University of Miami, Miami, Florida.

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