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DOI: 10.1055/s-0041-1739236
Detection of Cytomegalovirus Infection in Infants with Biliary Atresia: A Meta-analysis
Funding This research did not receive any specific grant from funding agencies in the public, commercial, or not-for-profit sectors.
Abstract
Objectives Biliary atresia (BA) is the most common indication of liver transplantation in children. Several reports attributed BA to both prenatal and perinatal etiologies, including a viral infection-induced autoimmune response that targets the bile ducts. Cytomegalovirus (CMV) remains the most common virus being linked to BA. This meta-analysis aimed to estimate to what extent CMV infection is detected in patients with BA.
Methods This study was conducted according to the Preferred Reporting Items for Systematic Reviews and Meta-Analyses (PRISMA) guidelines. The databases of MEDLINE, Embase, Scopus, WHO-Virtual Health Library (VHL), ScienceDirect, and Google Scholar were used for the systematic search. The risk of bias was assessed using the Newcastle–Ottawa scale. Random effects model was used to estimate the pooled prevalence estimate with the corresponding 95% confidence interval (CI) using Comprehensive Meta-Analysis Software version 3.3.
Results A total of 19 studies that fulfilled the eligibility criteria were included in the meta-analysis. The total number of infants with BA was 630 patients, and the pooled overall prevalence of CMV infection among them was 25.4% (95% CI: 15.9%–38.0%). There was high heterogeneity among studies (I2 = 85.1%, p < .001), and subgroup analyses showed significant regional differences (X2 = 48.9, p <.001). Data on the prognosis of CMV-associated BA were scarce and obtainable from few studies that suggested an association between detection of CMV infection and poor prognosis of BA.
Conclusions The limited available data demonstrates that the rate of detection of CMV infection is high in infants with BA. There is still a need for large studies with appropriate controls for obtaining more reliable results about the various aspects of the association between CMV infection and BA.
Background
Biliary atresia (BA) is a common cause of neonatal cholestasis, characterized by extensive fibrosing inflammation of the extrahepatic bile duct, leading to obstruction of bile flow and subsequently resulting in permanent liver damage if not early managed.[1] [2] [3] BA is treatable by the Kasai portoenterostomy, which prevents liver injury, caused by cholestasis, if done early.[1] [2] [4] Despite using Kasai operation, BA is still a leading cause of end-stage liver disease and the most common indication of liver transplantation in children.[1] [4] [5] [6]
BA is believed to be a disorder of multifactorial etiology, involving both prenatal and perinatal factors.[1] [6] Several studies proposed a possible infectious etiology; primarily, a viral infection-induced auto-immune response that targets the bile duct, leading to chronic fibrosclerosing injury.[1] [2] [4] Patients with BA have been tested for several viruses in an attempt to determine the viruses associated with the disease onset. Among these viruses, Cytomegalovirus (CMV) remains the most common virus being linked to BA.[5] [7] [8] Fischler et al found that immunoglobulin deposits on the hepatocellular canalicular membrane were significantly higher in biopsies from CMV infected patients with BA than their controls.[9] Additionally, the histological findings in the porta hepatis and liver biopsy samples of patients with BA showed that perinatal CMV infection is an initiator of bile duct damage, supporting the link between CMV infection and BA.[10] [11]
Worldwide, several studies assessed the prevalence of CMV infection in infants with BA. These studies gave different results of the prevalence of CMV infection in infants with biliary atresia. To the best of our knowledge, there is no meta-analysis assessing the extent of CMV detection in BA patients. Moreover, establishing the role of perinatal viral infection in the pathogenesis of BA could propose and raise the question of a beneficial effect of antiviral as adjuvant therapy to manage and modulate the clinical outcome of BA. A more inclusive consideration of this systematic measurement would help show the magnitude of this finding and aid in a better understanding of the disease etiology and prognosis.
Methods
Search Strategy and Inclusion Criteria
In this study, we followed the guidelines of the Preferred Reporting Items for Systematic Reviews and Meta-Analyses (PRISMA) statement.[12] We searched the databases of MEDLINE, Embase, Scopus, WHO-Virtual Health Library (VHL), ScienceDirect, and Google Scholar for all studies which assessed the association between CMV infection and BA up to September 2019. The search words used were “Cytomegalovirus,” “CMV,” and “Biliary atresia” to ensure the maximal coverage of possible literature.
The inclusion criteria were all studies published in English that presented sufficient data for estimation of the prevalence of CMV infection in patients with BA. If two or more studies had the same patient population, the study with more complete data or larger sample size was included to avoid duplication. Case reports, case series, editorials, abstracts, reviews, and studies lacking the data of interest were excluded.
Since BA is a congenital malformation, we included only studies that used a reliable method for diagnosing congenital CMV infection (viral deoxyribonucleic acid [DNA] detection by polymerase chain reaction [PCR], viral isolation by culture, and viral antigen detection).[13] [14] [15] Studies that relied only on serological testing were not included because the presence of CMV-immunoglobulin G (IgG) does not differentiate between infant infection and transplacental transfer of maternal antibodies, and the presence of CMV-IgM is not sufficiently sensitive and does not differentiate between the congenital infection and acquired infection in the early neonatal period.[13] [14]
The titles and abstracts of all papers retrieved from this search were screened for potential inclusion in this review. Then, relevant studies were reviewed (full text) for inclusion, according to the defined eligibility criteria, and any disparity between the reviewers was resolved by discussion and consensus. The risk of bias was assessed using the Newcastle–Ottawa scale (NOS) for studies quality, a tool that determines the quality based on the selection of the study group, comparability of groups, and ascertainment of the exposure and outcomes. Data was extracted using a data extraction form developed to extract data of authors, study region, year of publication, diagnostic methods used for detection of CMV infection, number of patients with BA, and number of patients with confirmed CMV infection.
Statistical Analysis
The pooled prevalence from the random-effects models with the corresponding 95% confidence interval (CI) was calculated using Comprehensive Meta-Analysis Software version 3.3. Heterogeneity among studies was estimated using the I2 statistics, and publication bias was estimated through visual examination of the funnel plot and Begg's test.[16] To explore the sources of heterogeneity, we conducted subgroup analyses and meta-regression to determine the extent to which variables of interest moderated the overall result. Moreover, a sensitivity analysis was done by recalculating the pooled estimate by omitting studies. This was done to evaluate the effect or weight of each group of studies on the overall result. For the purpose of this review, the sensitivity analyses were performed to test whether the method of CMV detection affected the overall result. For subgroup analysis, the Chi-square (X2) test was used to assess the differences between the categorical subgroups, and the significance level was set at p < 0.05.
Results
The schematic flow of study identification and selection process is presented in ([Fig. 1]). The initial search retrieved records for 1584 published articles. We excluded 335 and 1156 articles that were duplicated in the databases or irrelevant articles, respectively. The remaining 84 studies were retrieved for a full-text assessment, and 65 studies were subsequently omitted because of a lack of sufficient data for estimation of the outcomes of interest. Finally, a total of 19 studies published from 1980 to 2020, which met the eligibility for data extraction and analyses were used for the quantitative synthesis; nine studies from Asia, five studies from Europe, four studies from the Americas, and a study from Africa.[17] [18] [19] [20] [21] [22] [23] [24] [25] [26] [27] [28] [29] [30] [31] [32] [33] [34] [35] The main characteristics of these included studies are shown in [Table 1].
|
Study |
Year |
Country |
Method of detection of CMV infection |
Patients with BA |
Patients with CMV-associated BA |
NOS results |
|---|---|---|---|---|---|---|
|
Numazaki et al[17] |
1980 |
Japan |
Viral isolation (culture) |
18 |
2 |
6 |
|
Tarr et al[18] |
1996 |
USA |
Viral isolation (culture) |
23 |
4 |
6 |
|
Fischler, et al[19] |
1998 |
Sweden |
PCR |
18 |
9 |
6 |
|
Domiati-Saad[20] |
1998 |
USA |
PCR |
12 |
0 |
5 |
|
Jevon et al[21] |
1999 |
Canada |
PCR |
12 |
0 |
5 |
|
Rauschenfels et al[22] |
2004 |
Germany |
PCR |
74 |
8 |
7 |
|
Shen et al[23] |
2004 |
China |
Antigen detection |
27 |
10 |
8 |
|
Fjær et al[24] |
2005 |
Norway |
PCR |
10 |
2 |
5 |
|
De-Thommaso et al[25] |
2005 |
Brazil |
PCR |
33 |
9 |
5 |
|
Goedhals et al[26] |
2008 |
South Africa |
Antigen detection |
42 |
1 |
6 |
|
Yaghobi et al[27] |
2010 |
Iran |
PCR |
34 |
0 |
5 |
|
Xu et al[28] |
2011 |
China |
PCR |
85 |
51 |
7 |
|
Soomro et al[29] |
2011 |
Pakistan |
PCR |
33 |
14 |
5 |
|
Schukfeh, et al[30] |
2012 |
Germany |
PCR |
70 |
8 |
7 |
|
Goel et al[31] |
2018 |
India |
PCR |
14 |
11 |
5 |
|
Gou et al[32] |
2018 |
China |
Antigen detection |
38 |
6 |
7 |
|
Situmorang et al[33] |
2018 |
Indonesia |
PCR |
16 |
7 |
6 |
|
Meshram et al[34] |
2020 |
India |
PCR |
21 |
19 |
6 |
|
Smith et al[35] |
2020 |
UK |
PCR |
50 |
8 |
7 |
Abbreviations: BA; biliary atresia; CMV, Cytomegalovirus; NOS, Newcastle–Ottawa scale; PCR, polymerase chain reaction.
Meta-analysis showed that CMV was detected in 25.4% (95% CI 15.9%–38.0%) of the patients with BA ([Fig. 2]). No publication bias was detected on visual examination of the funnel plot ([Fig. 3]) and from the results of Begg's test (p = 0.38). Duval and Tweedie trim and fill method showed that no potential studies are missing. However, there was high heterogeneity among studies (I2 = 85.1%, p < 0.001). In subgroup analysis, the detection of CMV infection in patients with BA was higher in the Asian studies (37.9%) than in European and American studies (25.5% and 15.3%, respectively). There was a statistical difference in prevalence between the aforementioned geographical areas (X2 = 48.9, p < 0.001). A meta-regression analysis was done to analyze whether the study period affected the heterogeneity among studies in this meta-analysis, and the results showed that the years were not correlated with the outcome (coefficient 0.054: p = 0.075). The sensitivity analyses showed some changes in the pooled prevalence estimates (from 22.2% for antigen detection to 35.0% for PCR).
Data on the association between viral infection and the risk of poor prognosis adverse outcome of BA were scarce and obtainable from few studies. Furthermore, the wide variability in defining and measuring the clinical outcome and prognosis of BA among studies made direct analysis and comparisons of the results across studies difficult. Among these clinical findings, Fischler et al found that infants CMV-associated BA had a more pronounced enlargement of the liver and significantly higher levels of serum bilirubin level.[19] Shen et al found that patients with CMV-associated BA had a higher degree of liver fibrosis, higher incidence of cholangitis, and longer time to achieve jaundice clearance.[23] On the other hand, Schukfeh et al showed a nonsignificant association between CMV-associated BA and prognosis after Kasai portoenterostomy in terms of laboratory parameters and survival with native liver.[30]
Discussion
CMV is a well-known cause of congenital viral infections in humans, and it has been proposed as a possible etiologic agent in the pathogenesis of BA. A previous meta-analysis conducted in 2007 reported that the overall birth prevalence of congenital CMV infection in the general population was only 0.64%, and the majority of the cases were asymptomatic.[36] However, this meta-analysis showed a remarkably higher prevalence of CMV infection in infants with BA (25.4%) than that of congenital CMV infection in the general population.
The studies included in this meta-analysis were mainly from the Americas, Asia, and Europe, while only one study was from Africa. Although there is limited literature published on the association between CMV infection and BA, the available data demonstrate that CMV infection is common in BA as around one-quarter of the infants with BA had evidence of CMV infection, using one of the more reliable methods of CMV detection (viral DNA detection by PCR, viral isolation by culture, and viral antigen detection).
The discrepancy between prevalence rates reported from the reviewed studies might be partially explained by the differences in sensitivity of the detection method used or by the presence of other etiological agents implicated in the pathogenesis of BA. This meta-analysis showed that CMV infection in patients with BA had regional epidemiological differences. While rates of CMV infection have been reported to be considerably lower in most European and American countries, the prevalence rate tends to be higher in Asian countries. This finding is consistent with a socioeconomic link with CMV that has been well-established in several studies, showing that CMV prevalence is higher in individuals of areas of lower socioeconomic groups.[37] Furthermore, some studies demonstrate that BA is more prevalent in Asia than in Europe; it occurs in ⅕ to ⅛,000 live births in Asia and 1/18 to 1/20,000 children in Europe, although no ethnic differences have been demonstrated.[21] [38] Also, the regional differences in times of CMV epidemics could aid in the understanding of this variation.[5]
Davenport et al have classified BA into four groups: isolated BA, cystic BA, syndrome BA with associated malformation, and CMV-associated BA.[39] Among these types of BA, several studies showed that the CMV-associated BA yielded the worst prognosis.[23] [40] Shen et al reported that the CMV infection group had a lower rate of jaundice disappearance and a higher incidence of postoperative ascending cholangitis, a significant complication of BA.[23] Zani et al findings suggest that CMV-associated BA is a distinct etiological and prognostic subgroup, with reduced clearance of jaundice, native liver survival, diminished response to Kasai portoenterostomy, and increased mortality.[41] Because of the lack of uniformity across the included studies, a systematic assessment of the prognosis of CMV-associated BA could not be done.
Another important concern claimed by several authors regarding the association between CMV infection and BA is that detection of CMV infection might confound the clinical evaluation of neonatal jaundice caused by BA and may lead to misdiagnosis, late referral, and a delay in therapeutic surgery. This usually occurs when the condition is misdiagnosed as neonatal hepatitis secondary to CMV infection.[25] [26] [40]
There is a suggested role of antiviral therapy in the treatment of BA patients infected with CMV, and it could be a possible intervention that might improve outcomes of BA.[23] [25] A recent trial done by Parolini et al showed that antiviral treatment with valganciclovir and ganciclovir appeared to improve outcomes in infants with CMV-associated BA.[42] Shen et al reported a case of a 2-month-old girl with BA who had persistent jaundice after 1 month of Kasai's operation surgery, and she was treated with valganciclovir for 6 weeks.[43] However, there is a need for more trials to confirm the effect of antiviral treatment among those patients.
Limitations
This meta-analysis emphasized the high rate of CMV-associated BA but did not prove causality. The main limitation to be considered in the current review is the paucity of publications on viral infections in BA. Data on the association between viral infection and the risk of poor prognosis adverse outcome of BA was obtainable from few studies. Another limitation is the inclusion of studies published only in English, which could compromise representativeness.
Conclusions
This review provided a comprehensive view of the high rate of detection of CMV infection in infants with BA (25.4%) compared with the previously reported rate of CMV infection among the general population. However, there is still a need for large prospective multicenter studies with appropriate controls to examine various aspects of the association between CMV infection and BA. The findings of this review should be considered in future prognostic models that may be made when exploring the clinical outcomes of BA.
Conflict of Interest
The authors declare that they have no competing interests.
Authors Contribution
S.M. conceptualized the research idea and designed the study; S.M., A.A., M.E. and A.I. undertook articles searching, articles assessment, and review; S.M., M.E., and A.E. undertook data extraction and analysis; All authors interpreted the results and drafted the manuscript. All authors revised and approved the final manuscript.
-
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14 December 2021
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References
- 1 Asai A, Miethke A, Bezerra JA. Pathogenesis of biliary atresia: defining biology to understand clinical phenotypes. Nat Rev Gastroenterol Hepatol 2015; 12 (06) 342-352
- 2 Sokol RJ, Mack C, Narkewicz MR, Karrer FM. Pathogenesis and outcome of biliary atresia: current concepts. J Pediatr Gastroenterol Nutr 2003; 37 (01) 4-21
- 3 Kodoa K, Sakamotoa K, Imaib T. et al. Cytomegalovirus-associated biliary atresia. J Pediatr Surg Case Rep 2018; 35: 17-20
- 4 Zagory JA, Nguyen MV, Wang KS. Recent advances in the pathogenesis and management of biliary atresia. Curr Opin Pediatr 2015; 27 (03) 389-394
- 5 Feng J, Huang L. The virus infection and biliary atresia. Curr Pediatr Rev 2008; 4: 164-168
- 6 Bezerra JA. Potential etiologies of biliary atresia. Pediatr Transplant 2005; 9 (05) 646-651
- 7 Feldman AG, Mack CL. Biliary atresia: cellular dynamics and immune dysregulation. Semin Pediatr Surg 2012; 21 (03) 192-200
- 8 Zhao D, Long XD, Xia Q. Recent advances in etiology of biliary atresia. Clin Pediatr (Phila) 2015; 54 (08) 723-731
- 9 Hill R, Hussain M, Quaglia A. et al. TH-17 cells infiltrate the liver in biliary atresia and are related to prognosis. Paper presented at: Proceedings of the 3rd EUPSA/BAPS Combined Congress; 13 - 16 June 2012; Rome, Italy
- 10 Fischler B, Woxenius S, Nemeth A, Papadogiannakis N. Immunoglobulin deposits in liver tissue from infants with biliary atresia and the correlation to cytomegalovirus infection. J Pediatr Surg 2005; 40 (03) 541-546
- 11 Brindley SM, Lanham AM, Karrer FM, Tucker RM, Fontenot AP, Mack CL. Cytomegalovirus-specific T-cell reactivity in biliary atresia at the time of diagnosis is associated with deficits in regulatory T cells. Hepatology 2012; 55 (04) 1130-1138
- 12
Liberati A,
Altman DG,
Tetzlaff J.
et al.
The PRISMA statement for reporting systematic reviews and meta-analyses of studies
that evaluate health care interventions: explanation and elaboration. J Clin Epidemiol
2009; 62 (10) e1-e34
MissingFormLabel
- 13 Ross SA, Novak Z, Pati S, Boppana SB. Overview of the diagnosis of cytomegalovirus infection. Infect Disord Drug Targets 2011; 11 (05) 466-474
- 14 Stagno S, Tinker MK, Elrod C, Fuccillo DA, Cloud G, O'Beirne AJ. Immunoglobulin M antibodies detected by enzyme-linked immunosorbent assay and radioimmunoassay in the diagnosis of cytomegalovirus infections in pregnant women and newborn infants. J Clin Microbiol 1985; 21 (06) 930-935
- 15 Centers for Disease Control and Prevention. Cytomegalovirus and congenital Infection—Interpretation of laboratory tests. Accessed September 2019 at: http://www.cdc.gov/cmv/clinical/lab-tests.html
- 16
Begg CB,
Mazumdar M.
Operating characteristics of a rank correlation test for publication bias. Biometrics
1994; 50 (04) 1088-1101
MissingFormLabel
- 17 Numazaki Y, Oshima T, Tanaka A. et al. Demonstration of IgG EA (early antigen) and IgM MA (membrane antigen) antibodies in CMV infection of healthy infants and in those with liver disease. J Pediatr 1980; 97 (04) 545-549
- 18 Tarr PI, Haas JE, Christie DL. Biliary atresia, cytomegalovirus, and age at referral. Pediatrics 1996; 97 (6 Pt 1): 828-831
- 19 Fischler B, Ehrnst A, Forsgren M, Örvell C, Nemeth A. The viral association of neonatal cholestasis in Sweden: a possible link between cytomegalovirus infection and extrahepatic biliary atresia. J Pediatr Gastroenterol Nutr 1998; 27 (01) 57-64
- 20 Domiati-Saad R, Dawson DB, Margraf LR, Finegold MJ, Weinberg AG, Rogers BB. Cytomegalovirus and human herpesvirus 6, but not human papillomavirus, are present in neonatal giant cell hepatitis and extrahepatic biliary atresia. Pediatr Dev Pathol 2000; 3 (04) 367-373
- 21 Jevon GP, Dimmick JE. Biliary atresia and cytomegalovirus infection: a DNA study. Pediatr Dev Pathol 1999; 2 (01) 11-14
- 22 Rauschenfels S, Krassmann M, Al-Masri AN. et al. Incidence of hepatotropic viruses in biliary atresia. Eur J Pediatr 2009; 168 (04) 469-476
- 23 Shen C, Zheng S, Wang W, Xiao XM. Relationship between prognosis of biliary atresia and infection of cytomegalovirus. World J Pediatr 2008; 4 (02) 123-126
- 24 Fjaer RB, Bruu AL, Nordbø SA. Extrahepatic bile duct atresia and viral involvement. Pediatr Transplant 2005; 9 (01) 68-73
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