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Meta-Analysis Open Access
©The Author(s) 2017. Published by Baishideng Publishing Group Inc. All rights reserved.
World J Gastroenterol. Feb 28, 2017; 23(8): 1497-1506
Published online Feb 28, 2017. doi: 10.3748/wjg.v23.i8.1497
Association between Helicobacter pylori and end-stage renal disease: A meta-analysis
Karn Wijarnpreecha, Charat Thongprayoon, Ridhmi Rajapakse, Department of Internal Medicine, Bassett Medical Center, Cooperstown, NY 13326, United States
Pitchaphon Nissaisorakarn, Department of Internal Medicine, Jacobi Medical Center, Albert Einstein College of Medicine, Bronx, NY 10461, United States
Natasorn Lekuthai, Department of Medicine, Faculty of Medicine Siriraj Hospital, Mahidol University, Bangkok 10700, Thailand
Veeravich Jaruvongvanich, Department of Medicine, University of Hawaii, Honolulu, HI 96822, United States
Kiran Nakkala, Cape Fear Center for Digestive Diseases, P.A., Fayetteville, NC 28312, United States
Wisit Cheungpasitporn, Division of Nephrology, Department of Internal Medicine, Mayo Clinic, Rochester, MN 55905, United States
Author contributions: Cheungpasitporn W contributed to conception and design of the study, and critical revision; Wijarnpreecha K, Thongprayoon C, Nissaisorakarn P and Jaruvongvanich V contributed to acquisition of data, Wijarnpreecha K, Nissaisorakarn P, Lekuthai N, Jaruvongvanich V, Nakkala K and Rajapakse R interpreted the data; Wijarnpreecha K and Thongprayoon C drafted the article; Lekuthai N, Nakkala K and Rajapakse R revised the article; all authors approved the final version.
Conflict-of-interest statement: The authors deny any conflict of interest.
Data sharing statement: No additional data are available.
Correspondence to: Wisit Cheungpasitporn, MD, Division of Nephrology, Department of Internal Medicine, Mayo Clinic, 200 First street SW, Rochester, MN 55905, United States. wcheungpasitporn@gmail.com
Telephone: +1-507-2848450 Fax: +1-507-2667891
Received: October 30, 2016
Peer-review started: November 6, 2016
First decision: December 2, 2016
Revised: December 9, 2016
Accepted: January 18, 2017
Article in press: January 18, 2017
Published online: February 28, 2017
Processing time: 119 Days and 5.1 Hours

Abstract
AIM

To investigate the prevalence and association of Helicobacter pylori (H. pylori) with end-stage renal disease (ESRD).

METHODS

SA comprehensive literature search was completed from inception until October 2016. Studies that reported prevalence, relative risks, odd ratios, hazard ratios or standardized incidence ratio of H. pylori among ESRD patients were included. Participants without H. pylori were used as comparators to assess the association between H. pylori infection and ESRD. Pooled risk ratios and 95%CI was calculated using a random-effect model. Adjusted point estimates from each study were combined by the generic inverse variance method of DerSimonian and Laird.

RESULTS

Of 4546 relevant studies, thirty-seven observational studies met all inclusion criteria. Thirty-five cross-sectional studies were included in the analyses to assess the prevalence and association of H. pylori with ESRD. The estimated prevalence of H. pylori among ESRD patients was 44% (95%CI: 40%-49%). The pooled RR of H. pylori in patients with ESRD was 0.77 (95%CI: 0.59-1.00) when compared with the patients without ESRD. Subgroup analysis showed significantly reduced risk of H. pylori in adult ESRD patients with pooled RR of 0.71 (95%CI: 0.55-0.94). The data on the risk of ESRD in patients with H. pylori were limited. Two cohort studies were included to assess the risk of ESRD in patients with H. pylori. The pooled risk RR of ESRD in patients with H. pylori was 0.61 (95%CI: 0.03-12.20).

CONCLUSION

The estimated prevalence of H. pylori in ESRD patients is 44%. Our meta-analysis demonstrates a decreased risk of H. pylori in adult ESRD patients.

Key Words: Helicobacter pylori; Kidney failure; Renal disease; Renal insufficiency; End stage kidney disease; Meta-analysis

Core tip:Helicobacter pylori (H. pylori) is the most common chronic bacterial infection in gastrointestinal tract of humans. The prevalence and association of H. pylori with end-stage renal disease (ESRD), however, are still unclear. To further investigate this potential relationship, we conducted this systematic review and meta-analysis of observational studies reporting the association between H. pylori infection and ESRD and prevalence in ESRD patients. We found an estimated prevalence of H. pylori in ESRD patients of 44%. In addition, our meta-analysis demonstrates a 0.71-fold decreased risk of H. pylori in adult ESRD patients.

Core tip:Helicobacter pylori (H. pylori) is the most common chronic bacterial infection in gastrointestinal tract of humans. The prevalence and association of H. pylori with end-stage renal disease (ESRD), however, are still unclear. To further investigate this potential relationship, we conducted this systematic review and meta-analysis of observational studies reporting the association between H. pylori infection and ESRD and prevalence in ESRD patients. We found an estimated prevalence of H. pylori in ESRD patients of 44%. In addition, our meta-analysis demonstrates a 0.71-fold decreased risk of H. pylori in adult ESRD patients.

INTRODUCTION

Helicobacter pylori (H. pylori) is the most common chronic bacterial infection in the gastrointestinal tract of humans[1]. It has been estimated that the prevalence of H. pylori infection is up to thirty percent in adult aged 18 to 30 years and to fifty percent in those older than 60 years old[2]. Many studies demonstrated that H. pylori infection is associated with a peptic and duodenal ulcer, chronic gastritis, and gastric cancer[3,4]. Recently, epidemiologic studies have demonstrated associations between H. pylori infection and extra-gastrointestinal organ involvements including coronary artery disease, dyslipidemia, insulin resistance, and hematologic disorders[5-7].

End-stage renal disease (ESRD) is a common and serious chronic disease worldwide that continues to increase in prevalence by approximately 21000 cases per year in the United States[8]. Although there is no visible evidence demonstrated that H. pylori infection is directly associated with renal disease, patients with ESRD usually have gastrointestinal problems such as gastritis, dyspeptic symptoms or ulcers[9-11]. Interestingly, recent investigations have demonstrated an association between H. pylori infection and ESRD[12-14]. In addition, an increase in renal resistance index due to systemic inflammation state H. pylori infection was also described[15-18]. However, many studies reported the conflict data regarding the association between H. pylori infection in ESRD and also the prevalence of H. pylori infection in ESRD patients[19-42]. Thus, we conducted the systematic review and meta-analysis that summarized all available evidence to determine the prevalence of H. pylori infection among ESRD patients and the association between H. pylori infection and ESRD.

MATERIALS AND METHODS
Literature search

Three investigators (Wijarnpreecha K, Thongprayoon C and Cheungpasitporn W) independently reviewed published studies indexed in MEDLINE and EMBASE database from their inception to October 2016 using the search strategy that included the terms for “Helicobacter”, “hemodialysis”, and “renal disease” as described in Item S1 in online Supplementary Data 1. A search for additional articles utilizing references from included studies was also performed. There was no confinement on language in the literature search. We conducted this systematic review following the Preferred Reporting Items for Systematic Reviews and Meta-Analysis statement.

Selection criteria

The inclusion criteria were: (1) observational studies appraising the association between H. pylori and ESRD and prevalence in hemodialysis; (2) prevalence, odds ratios, relative risks, or hazard ratios with 95%CI were presented; and (3) individuals without H. pylori were used as comparators in cohort studies while individuals without ESRD were used as comparators in the cross-sectional and case-control studies. Wijarnpreecha K, Thongprayoon C and Cheungpasitporn W individually examined the titles and abstracts of the studies. After the first phase, the full text of the included studies was subsequently examined to ascertain if they met the inclusion criteria. Discrepancies were also settled by discussion with all investigators.

Data abstraction

A structured data collection form was utilized to obtain the data from included studies including title of the study, year of publication, country where the study was conducted, name of the first author, demographic of subjects, method used to diagnose H. pylori, prevalence of H. pylori, effect estimates (hazard ratios, odds ratios, relative risks) with 95%CI, and factors adjusted in the multivariate analysis. To ensure the certainty, this data extraction process was reviewed by all investigators. The quality of each study was individually appraised by each investigator. We utilized the validated Newcastle-Ottawa quality assessment scale for cohort and case-control studies[43] and modified Newcastle-Ottawa scale[44] for the cross-sectional study.

Statistical analysis

MetaXL software (EpiGear International Pty Ltd)[45] was used for meta-analysis of prevalence. Otherwise, data analysis was performed using the Review Manager 5.3 software from the Cochrane Collaboration (London, United Kingdom). Adjusted point estimates from each study were combined by the generic inverse variance method of DerSimonian and Laird, which assigned the weight of each study based on its variance[46]. We used a random-effect model due to the high likelihood of between-study variance from different study designs, populations, and H. pylori testing. Cochran’s Q test and I2 statistic were used to ascertain the between-study heterogeneity. A value of I2 of 0%-25%, 25%-50%, 50%-75%, and > 75% embodied insignificant, low, moderate and high heterogeneity, respectively[47].

RESULTS

Of 4546 potentially relevant articles, 4466 articles were excluded due to the title and abstract not meeting inclusion criteria. Subsequently, 43 articles were excluded (6 articles were not observational studies, and 37 articles did not describe the outcomes of interest). Finally, thirty-seven observational studies (2 cohort[14,48] and 35 cross-sectional studies[12,13,16,19-42,49-56]) met all inclusion criteria. The literature retrieval, review, and selection process are shown in Figure 1. The characteristics and quality assessment of the included cross-sectional studies are presented in Table 1 while the characteristics of the included cohort studies are shown in Table 2.

Table 1 Main characteristics of the cross-sectional studies included in this meta-analysis.
StudyCountryYearStudy sampleH. pylori testingH. pylori prevalence (%)ORStudy quality
Offerhaus et al[36]The Netherland1989DialysisAntibody22/50 (44%)0.96 (0.42-2.22)S 3
C 0
O 2
Shousha et al[55]United Kingdom1990DialysisHistology12/50 (24%)0.43 (0.20-0.90)S 3
C 0
O 2
Loffeld et al[34]The Netherland1991HDAntibody13/30 (43%)1.24 (0.58-2.64)S 3
C 1
O 2
Davenport et al[22]United Kingdom1991HDAntibody27/76 (36%)1.29 (0.75-2.22)S 3
C 1
O 2
Ala-Kaila et al[16]Finland1991HDHistology3/23 (13%)0.68 (0.17-2.64)S 3
C 0
O 2
Gladziwa et al[27]Germany1993HDCumulative evaluation (urease, test, histology, culture and direct examiniation)12/35 (34%)0.44 (0.19 -1.00)S 3
C 0
O 2
Giachino et al[25]Italy1994HDUrease test, histology and culture13/40 (32%)0.51 (0.20-1.28)S 3
C 0
O 2
De Vecchi et al[51]Italy1995HD and PDAntibodyHD and PDHD and PDS 3
37/67 (55%)0.39 (0.18-0.81)C 1
HDHDO 2
17/29 (59%)0.54 (0.18-1.62)
PDPD
20/38 (53%)0.30 (0.11-0.81)
Jaspersen et al[31]Germany1995HDUrease test and histology7/34 (21%)0.44 (0.18-1.09)S 3
C 0
O 2
Seyrek et al[39]Turkey1996HDAntibody13/91 (14%)0.56 (0.21-1.50)S 3
C 1
O 2
Krawczyk et al[33]Poland1996HDUrease test and histology13/21 (62%)0.93 (0.27-3.20)S 3
C 1
O 2
Ozgür et al[38]Turkey1997HDUrease test28/47 (60%)0.83 (0.41-1.69)S 3
C 0
O 2
Hruby et al[30]Poland1997HDAntibody, culture9/26 (35%) by culture0.68 (0.19-2.44) by cultureS 3
16/26 (62%) by antibody0.53 (0.13-2.12)C 0
O 2
Yildiz et al[42]Turkey1999HDAntibody31/47 (66%)0.79 (0.34-1.84)S 3
C 0
O 2
Fabrizi et al[23]United States1999HDAntibody127/228 (56%)1.11 (0.74-1.66)S 3
C 1
O 2
Tamura et al[40]Japan1999HD and PDUrease test, histology, and culture25/49 (51%)0.88 (0.40-1.96)S 3
C 0
O 2
Gür et al[28]Turkey1999HDUrease test and histology25/45 (56%)1.04 (0.45-2.40)S 3
C 0
O 2
Araki et al[50]Japan1999HD and PDHistology and culture29/63 (46%)0.45 (0.22-0.91)S 3
C 1
O 2
Karari et al[32]Kenya2000CRFUrease test and histology41/77 (53%)0.90 (0.48-1.70)S 3
(HD - 36%)C 1
O 2
Nakajima et al[53]Japan2002HDUrease test, histology, and culture14/51 (28%)0.30 (0.11-0.81)S 3
C 0
O 2
Tsukada et al[41]Japan2003HDHistology9/36 (25%)0.28 (0.02-3.82)S 3
C 2
O 2
Olmos et al[37]Argentina2003HDAntibody44/93 (47%)0.62 (0.35-1.11)S 3
C 2
O 2
Nakajima et al[54]Japan2004HDAntibody51/138 (37%)0.35 (0.22-0.58)S 3
C 1
O 2
Nardone et al[35]Italy2005HDUrease test, histology, urea breath test and stool antigen7/11 (64%)3.04 (0.82-11.13)S 3
C 0
O 2
Blusiewicz et al[19]Poland2005HDUrease, histology19/30 (63%)0.71 (0.24-2.07)S 3
C 0
O 2
Khedmat et al[13]Iran2007HDUrease test46/73 (63%)3.20 (1.88-5.44)S 3
C 0
O 2
Khazaei et al[52]Iran2008HD - childrenUrease test, and histology16/24 (67%)8.00 (2.19-29.25)S 3
C 0
O 2
Gioè et al[26]Italy2008HDUrease test, and histology75/142 (53%)1.39 (0.86-2.23)S 3
C 0
O 2
Abdulrahman et al[49]Saudi Arabia2008ESRDHistology16/40 (40%)0.22 (0.09-0.56)S 3
C 1
O 2
Asl et al[12]Iran2009HDHistology23/40 (58%)2.81 (1.13-6.99)S 3
C 1
O 2
Sugimoto et al[56]Japan2009HDAntibody262/539 (49%)0.26 (0.19-0.35)S 3
C 0
O 2
Chang et al[21]South Korea2010HDUrease test and histology12/33 (36%)0.30 (0.12-0.74)S 3
C 0
O 2
Hooman et al[29]Iran2011HD - childrenHistology19/68 (28%)1.59 (0.65-3.92)S 3
C 0
O 2
Genç et al[24]Turkey2013HD and PD - childrenAntibody17/33 (52%)0.69 (0.26-1.83)S 3
C 1
O 2
Chang et al[20]Taiwan2014ESRDUrease test and histology81/144 (56%)0.54 (0.38-0.77)S 4
C 2
O 3
H. pylori: Helicobacter pylori; HD: Hemodialysis; PD: Peritoneal dialysis.
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Figure 1
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Figure 1 Literature review process.
Table 2 Main characteristics of the cohort studies included in this meta-analysis.
StudyLo et al[48]Lin et al[14]
CountryHong KongTaiwan
Study designCohort studyCohort study
Year20042015
Study sampleType 2 diabetic patients with clinical proteinuria and renal insufficiencyH. pylori-infected and non-infected patients without ESRD
H. pylori testingAntibodyDiagnosis of H. pylori infection (ICD-9 041.86) was used from inpatient database of The Taiwan National Health Insurance Research Database
Positive H. pylori (Titer > 1.1 U/mL)
ESRD definitionDoubling of baseline serum creatinine concentration or need for dialysis or serum creatinine ≥ 500 μmol/LESRD was identified from Registry for Catastrophic Illness Patient Database
Adjusted HR0.12 (0.03, 0.52)2.58 (2.33, 2.86)
Confounder adjustmentSex, H. pylori status, serum creatinine, hemoglobin, systolic blood pressure, ACE inhibitors, Hepatitis B surface antigen statusAge, sex, comorbidity
Quality assessment (Newcastle-Ottawa scale)Selection: 3Selection: 4
Comparability: 2Comparability: 2
Outcome: 3Outcome: 3
H. pylori: Helicobacter pylori; HD: Hemodialysis; PD: Peritoneal dialysis; ESRD: End-stage renal disease.
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The prevalence of H. pylori among ESRD patients

Thirty-five cross-sectional studies were included in the analyses to assess the prevalence and association of H. pylori with ESRD. The estimated prevalence of H. pylori among ESRD patients was 44% (95%CI: 40%-49%, I2 = 80%), as demonstrated in Figure 2. Subgroup analysis was also performed on thirty-two studies[12,13,16,19-23,25-28,30-42,49-51,53-56] that provided prevalence on adult subjects and three studies[24,29,52] that provided prevalence on pediatric patients and showed estimated prevalences of H. pylori among adult ESRD patients of 44% (95%CI: 39%-49%, I2 = 81%), and 47% (95%CI: 24%-71%, I2 = 84%) among ESRD children, respectively as demonstrated in Supplementary Figures 1 and 2.

Figure 2
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Figure 2 Forest plot of overall prevalence of Helicobacter pylori infection among end-stage renal disease patients.
The association between H. pylori and ESRD

We found a marginal but not significantly decreased risk of H. pylori infection in overall ESRD subjects compared with non-ESRD subjects[12,13,16,19-42,49-56] with pooled RR of 0.77 (95%CI: 0.59-1.00, I2 = 79%) (Figure 3). Subgroup analysis based on ageing as described above, we found a significant decreased risk of H. pylori infection among adult ESRD patients[12,13,16,19-23,25-28,30-42,49-51,53-56] with pooled RR of 0.71 (95%CI: 0.55-0.94, I2 = 79%) compared with non-ESRD patients (Supplementary Figure 3). Nevertheless, we did not find a significant association between H. pylori infection and ESRD among ESRD children[24,29,52]; pooled RR = 1.93 (95%CI: 0.55-6.82, I2= 77%), (Supplementary Figure 4).

Figure 3
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Figure 3 Forest plot of the association between Helicobacter pylori infection and end-stage renal disease.

The data on the risk of ESRD in patients with H. pylori were limited. Two cohort[14,48] studies were included to assess the risk of ESRD in patients with H. pylori. The pooled risk RR of ESRD in patients with H. pylori was 0.61 (95%CI: 0.03-12.20).

Evaluation for publication bias

A funnel plot assessing publication bias for the association between H. pylori infection in overall ESRD subjects was demonstrated in Figure 4. The funnel plot of the association between H. pylori infection in overall ESRD subjects was symmetric and suggested no publication bias.

Figure 4
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Figure 4 Funnel plot of the association between Helicobacter pylori infection and end-stage renal disease.
DISCUSSION

In this meta-analysis summarizing all presently available data on the prevalence of H. pylori infection among ESRD patients and the association between H. pylori infection and ESRD, we demonstrated an estimated prevalence of H. pylori in ESRD patients of 44%. In addition, we found a 0.71-fold decreased risk of H. pylori in adult ESRD patients.

Although the precise explanation of reduced risk of H. pylori among adult ESRD patients is still unclear, there are several plausible explanations for this association. First, it has been postulated in previous studies that administering antibiotics and antacid more frequently in ESRD patients may contribute to lower the prevalence of H. pylori infection[39,53]. Previous study proposed that ESRD patients may have a lower risk of H. pylori infection from routinely used of antacids to prevent renal osteodystrophy by reducing intestinal phosphate absorption[16]. Second, patients with ESRD have higher levels of inflammatory cytokines including tumor necrotic factor, interleukin-6 and -8 from infiltrative inflammatory cells in gastric mucosa[57] and chronic circulatory failure[58,59] could lead to gastric mucosal damage and progress to gastric atrophy or atrophic gastritis, increased in gastric pH mucosa, and eventually eradication of H. pylori infection[60-62].

Although the included studies in this meta-analysis are almost of good quality, there are several limitations to this study that need to be addressed. Firstly, there was a statistical heterogeneity in the completed analysis. Possible sources of this heterogeneity include differences in confounder-adjusted methods (e.g., age, gender, ethnicity and socioeconomic status), different test to detect H. pylori infection in each study, various grades of uremia. Secondly, our subgroup analysis revealed significantly decreased the risk of H. pylori infection among adult subjects with ESRD but not in children likely due to a limitation in some studies. Although the number of study assessing H. pylori in children was limited and the insignificant finding in ESRD children could be from the lack of power, further studies are required to determine the role of aging in the underlying pathogenesis of H. pylori infection among ESRD patients. Lastly, this study is a meta-analysis of observational studies. Thus, our study demonstrated an association, but could not establish causality as unknown confounders could play a role in the association between prevalence of H. pylori among hemodialysis and association between H. pylori and ESRD.

In conclusion, our meta-analysis demonstrated an estimated prevalence of H. pylori in ESRD patients of 44%. In addition, our meta-analysis demonstrates a decreased risk of H. pylori in adult ESRD patients. ESRD could be a potential protective factor for H. pylori infection.

COMMENTS
Background

Helicobacter pylori (H. pylori) is the most common chronic bacterial infection in the gastrointestinal tract of humans. Epidemiologic studies showed the link between H. pylori infection and extra-gastrointestinal tract including end-stage renal disease (ESRD). However, many studies reported the conflict data regarding the association between H. pylori infection in ESRD and also the prevalence of H. pylori infection in ESRD patients.

Research frontiers

The results of those epidemiologic studies were inconsistent. To further investigate this possible association of H. pylori infection and ESRD and determine the prevalence of H. pylori among ESRD patients, the authors conducted this systematic review and meta-analysis of observational studies reporting the association between H. pylori and ESRD and prevalence of H. pylori among ESRD patients.

Innovations and breakthroughs

The authors found an estimated prevalence of H. pylori in ESRD patients of 44% (95%CI: 40%-49%). Moreover, the authors also found a decreased risk of H. pylori infection among adult ESRD patients with pooled RR of 0.71 (95%CI: 0.55-0.94).

Applications

This study demonstrated a significantly decreased risk of H. pylori infection among ESRD patients. This finding suggests that ESRD may be an independent potential protective factor for H. pylori infection.

Peer-review

This meta-analysis investigated the prevalence and association of H. pylori with end-stage renal diseases and demonstrated a decreased risk of H. pylori in adult ESRD patients. The context is well organized and the conclusion is of interest.

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Manuscript source: Invited manuscript

Specialty type: Gastroenterology and hepatology

Country of origin: United States

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