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RISK FACTORS FOR POST-LIVER TRANSPLANT BILIARY COMPLICATIONS IN THE ABSENCE OF ARTERIAL COMPLICATIONS

ABSTRACT

Background

- Biliary complications (BC) represent the most frequent complication after liver transplantation, up to 34% of cases.

Aim:

To identify modifiable risk factors to biliary complications after liver transplantation, essential to decrease morbidity.

Method:

Clinical data, anatomical characteristics of recipient and donors, and transplant operation features of 306 transplants with full arterial patency were collected to identify risk factors associated with BC.

Results:

BC occurred in 22.9% after 126 days (median) post-transplantation. In univariate analyses group 1 (without BC, n=236) and group 2 patients (with BC, n=70) did not differ on their general characteristics. BC were related to recipient age under 40y (p=0.029), CMV infection (p=0.021), biliary disease as transplant indication (p=0.018), lower pre-transplant INR (p=0.009), and bile duct diameter <3 mm (p=0.033). CMV infections occurred sooner in patients with postoperative biliary complications vs. control (p=0.07). In a multivariate analysis, only CMV infection, lower INR, and shorter bile duct diameter correlated with BC. Positive CMV antigenemia correlated with biliary complications, even when titers lied below the treatment threshold.

Conclusions:

Biliary complications after liver transplantation correlated with low recipient INR before operation, bile duct diameter <3 mm, and positive antigenemia for CMV or disease manifestation. As the only modifiable risk factor, routine preemptive CMV inhibition is suggested to diminish biliary morbidity after liver transplant.

HEADINGS:
Liver transplantation; Bile Ducts; Cytomegalovirus infections

RESUMO

Racional:

Complicações biliares (CB) são os eventos adversos mais frequentes após o transplante de fígado, ocorrendo em até 34% dos procedimentos.

Objetivo:

Identificar fatores de risco modificáveis para o aparecimento de complicações biliares após transplantes de fígado, essenciais para diminuir morbidade.

Método:

Investigação dos dados clínicos, características anatômicas de receptores e doadores e informações sobre a operação de 306 transplantes com artéria hepática pérvia, para identificar fatores de risco associados ao aparecimento de CB.

Resultados:

CB ocorreu em 22,9% após 126 dias (mediana) do transplante. Em análise univariada pacientes do grupo 1 (sem CB, n=236) e grupo 2 (com CB, n=70) não diferiram em suas características gerais. CB esteve relacionada à idade do receptor menor que 40 anos (p=0,029), infecção pelo citomegalovírus (CMV, p=0,021), doença biliar como indicação ao transplante (p=0,018), RNI pré-transplante mais baixo (p=0,009) e diâmetro do ducto biliar <3 mm (p=0,033). Infecções pelo CMV ocorreram mais precocemente em pacientes com CB (p=0,07). Na análise multivariada, somente infecção por ele, INR mais baixo e menor diâmetro do ducto biliar mantiveram correlação com CB. Antigenemia positiva para CMV correlacionou com CB mesmo em títulos inferiores ao cutoff para tratamento.

Conclusões:

CB após transplante hepático esteve relacionada com menores RNI do receptor antes da operação, diâmetro do ducto biliar <3 mm e antigenemia ou manifestação clínica positiva para CMV. Como único fator de risco evitável, tratamento preemptivo para inibição do CMV é sugerido para diminuir morbidade biliar após o transplante.

DESCRITORES:
Transplante de fígado; Ductos biliares; Infecções por citomegalovirus

INTRODUCTION

Biliary complications are frequent in patients who undergo deceased donor orthotopic liver transplantation. They occur mainly during the first year after transplantation, more often in the first three months, with an incidence between 11% and 34%22 Akamatsu N, Sugawara Y, Hashimoto D. Biliary reconstruction, its complications and management of biliary complications after adult liver transplantation: a systematic review of the incidence, risk factors and outcome. Transpl Int. 2011;24(4):379-92.,2222 Mejia GA, Olarte-Parra C, Pedraza A, Rivera JB, Benavides CA. Biliary Complications After Liver Transplantation: Incidence, Risk Factors and Impact on Patient and Graft Survival. Transplant Proc. 2016;48(2):665-8.. The frequency of these complications has important implications for the patients’ morbidity and further pressures overburdened health services.

The most common biliary complications include stenosis, occlusion and fistula. They are primarily associated with hepatic artery lesions, such as stenosis and thrombosis1111 Greif F, Bronsther OL, Van Thiel DH, Casavilla A, Iwatsuki S, Tzakis A, et al. The incidence, timing, and management of biliary tract complications after orthotopic liver transplantation. Ann Surg. 1994;219(1):40-5.. Therefore, biliary complications are not restricted to patients with arterial alterations, which suggests the presence of other risk factors for the development of such complications. Recent research investigated the relationships of further potential risk factors. The most commonly cited of those include: 1) type of anastomosis1515 Kochhar G, Parungao JM, Hanouneh IA, Parsi MA. Biliary complications following liver transplantation. World J Gastroenterol. 2013;19(19):2841-6.,2323 Neuhaus P, Blumhardt G, Bechstein WO, Steffen R, Platz KP, Keck H. Technique and results of biliary reconstruction using side-to-side choledochocholedochostomy in 300 orthotopic liver transplants. Ann Surg. 1994;219(4):426-34.; 2) warm and cold ischemia time55 Colonna JO, 2nd, Shaked A, Gomes AS, Colquhoun SD, Jurim O, McDiarmid SV, et al. Biliary strictures complicating liver transplantation. Incidence, pathogenesis, management, and outcome. Ann Surg. 1992;216(3):344-50; discussion 50-2.,3030 Welling TH, Heidt DG, Englesbe MJ, Magee JC, Sung RS, Campbell DA, et al. Biliary complications following liver transplantation in the model for end-stage liver disease era: effect of donor, recipient, and technical factors. Liver Transpl. 2008;14(1):73-80.; 3) type of preservation solution2020 Mangus RS, Fridell JA, Vianna RM, Milgrom MA, Chestovich P, Chihara RK, et al. Comparison of histidine-tryptophan-ketoglutarate solution and University of Wisconsin solution in extended criteria liver donors. Liver Transpl. 2008;14(3):365-73.,3030 Welling TH, Heidt DG, Englesbe MJ, Magee JC, Sung RS, Campbell DA, et al. Biliary complications following liver transplantation in the model for end-stage liver disease era: effect of donor, recipient, and technical factors. Liver Transpl. 2008;14(1):73-80.; 4) transplantations with ABO incompatibility1717 Lo CM, Shaked A, Busuttil RW. Risk factors for liver transplantation across the ABO barrier. Transplantation. 1994;58(5):543-7.,2424 Sanchez-Urdazpal L, Batts KP, Gores GJ, Moore SB, Sterioff S, Wiesner RH, et al. Increased bile duct complications in liver transplantation across the ABO barrier. Ann Surg. 1993;218(2):152-8.; 5) age of the donor and recipient88 Feng S, Goodrich NP, Bragg-Gresham JL, Dykstra DM, Punch JD, DebRoy MA, et al. Characteristics associated with liver graft failure: the concept of a donor risk index. Am J Transplant. 2006;6(4):783-90.,1919 Lue A, Solanas E, Baptista P, Lorente S, Araiz JJ, Garcia-Gil A, et al. How important is donor age in liver transplantation? World J Gastroenterol. 2016;22(21):4966-76.,2525 Serrano MT, Garcia-Gil A, Arenas J, Ber Y, Cortes L, Valiente C, et al. Outcome of liver transplantation using donors older than 60 years of age. Clin Transplant. 2010;24(4):543-9.,2929 Thorsen T, Aandahl EM, Bennet W, Olausson M, Ericzon BG, Nowak G, et al. Transplantation With Livers From Deceased Donors Older Than 75 Years. Transplantation. 2015;99(12):2534-42.; 6) receptor’s model for end-stage liver disease (MELD) score3030 Welling TH, Heidt DG, Englesbe MJ, Magee JC, Sung RS, Campbell DA, et al. Biliary complications following liver transplantation in the model for end-stage liver disease era: effect of donor, recipient, and technical factors. Liver Transpl. 2008;14(1):73-80.; 7) hepatitis C recurrence1313 Horster S, Bauerlein FJ, Mandel P, Raziorrouh B, Hopf C, Stemmler HJ, et al. Influence of hepatitis C virus infection and high virus serum load on biliary complications in liver transplantation. Transpl Infect Dis. 2013;15(3):306-13.; and 8) cytomegalovirus (CMV) infection77 Egawa H, Inomata Y, Uemoto S, Asonuma K, Kiuchi T, Fujita S, et al. Biliary anastomotic complications in 400 living related liver transplantations. World J Surg. 2001;25(10):1300-7.,1212 Halme L, Hockerstedt K, Lautenschlager I. Cytomegalovirus infection and development of biliary complications after liver transplantation. Transplantation. 2003;75(11):1853-8.,1414 Kim JM, Kim SJ, Joh JW, Kwon CH, Shin M, Kim EY, et al. Early and delayed onset cytomegalovirus infection of liver transplant recipients in endemic areas. Transplant Proc. 2010;42(3):884-9..

The aim of this research was to identify modifiable risk factors to biliary complications after liver transplantation, essential to decrease morbidity.

METHOD

This retrospective study used data from the medical records of patients undergoing liver transplantations between January 2007 and December 2015 at the Hospital of the Federal University of Minas Gerais (Hospital das Clínicas da Universidade Federal de Minas Gerais), Belo Horizonte, MG, Brazil. The data collection for the analysis was authorized by the Research Ethics Committee of the Federal University of Minas Gerais (CAAE: 64319717.2.0000.5149). During the study period, 496 transplants were performed at the institution, but only cases with patients older than 18 years, transplanted with deceased donor whole liver and followed up for at least six months after the procedure were considered (n=327 cases; 65.9% of total). The data were extracted from the Zeus® electronic health record, in which all findings and interventions before and after the transplantation were recorded.

The standard surgical technique for biliary reconstruction in transplantation is end-to-end biliary anastomosis, with a continuous suture using polydioxanone (PDS) 6.0 or 7.0. Surgeons were free to choose variations in the technique to accommodate the anatomy of the graft and recipient. Patients with primary biliary tract disease (primary or secondary sclerosing cholangitis) and cases of significant disproportion of diameter between the bile duct of the donor and recipient were reconstructed by Roux-en-Y hepaticojejunostomy. Biliary anastomoses were performed after arterial graft reperfusion.

Biliary complications were defined as being identified through diagnostic tests (magnetic resonance cholangiography and ERCP) and whose presence required an endoscopic, percutaneous or surgical intervention. The transplanted patients were divided into four groups: 1) absence of biliary and arterial complications (n=236); 2) biliary complications without arterial complications (n=70); 3) arterial complications without biliary complications (n=8); and 4) biliary and arterial complications (n=13). In these two latter cases, retransplantation was common, rendering a long-term observation of many of these cases impossible. Thus, only groups 1 and 2 (n=306) were analyzed in this study. Biliary complications occurred in 22.9% of patients.

Group 1 and 2 were compared by demographic and clinical aspects of the recipient and donor, as well as by the technical aspects of the operation. Potential risk factors were the age range of the recipient and donor, gender at birth of the recipient and donor, occurrence of CMV infection, transplant indication, MELD score used for selection, severity of liver disease using the MELD score calculated, blood group, laboratory tests of the donor (AST, ALT, sodium, HCO3and base excess - BE), cause of brain death of the donor, preservation solution used, diameter of the bile duct of the graft (≤3 mm or >3 mm), cold ischemia time (CIT), and biliary artery ischemia time (BAIT). CIT was the time interval between vascular clamping in the donor to portal reperfusion in the recipient, and BAIT was the time interval between portal reperfusion and arterial reperfusion in the recipient.

The cases were divided into patients and donors aged below 40 years or 40 years and older for comparison by age group. CMV infection was considered to be present when antigenemia (pp65) results or the presence of symptoms suggestive of cytomegalic infection led to ganciclovir treatment. Asymptomatic patients who displayed antigenemia with weak positivity (i.e. ≤2 leukocytes/100,000) were monitored with weekly serial exams and did not receive treatment.

Statistical analyses

The categorical variables are presented according to frequency and were compared using the chi-square test. For numerical variables we evaluated the distribution of normality (Kolmogorov-Smirnov test), expressed as the mean and standard deviation for normally distributed data or median and interquartile range (IQR) if data were not normally distributed. Comparisons of non-normal distribution variables were performed using the Mann-Whitney and Kruskal-Wallis tests. Variables with a normal distribution were compared using Student’s t-test. In all cases, differences were considered relevant for a level of significance lower than 5% (p<0.05). All comparisons that produced significant differences were included in a multivariate analysis with binary logistic regression, in addition to variables of clinical importance, whose comparison showed a difference with a significance level below 20% (p<0.2). These variables formed an initial multivariate model in which those whose level of significance did not reach a level lower than 5% (p<0.05) by the Wald test were deleted sequentially. The results with a trend towards statistical significance (p<0.10) are reported. For the regression analysis, odds ratios, 95% confidence intervals and p-values are reported. The data were analyzed using Stata for Mac, version 12.

RESULTS

Univariate analysis

The sample comprised 219 men (71.6%) and 87 women (28.4%), with a median age of 53.6 years (IQR 44.4-60.2). The indication for transplantation was hepatocyte cirrhosis (viral, alcoholic, or cryptogenic) in 239 cases (78.1%), biliary in 30 cases (9.8%), autoimmune cirrhosis in 19 cases (6.2%) and other etiologies in 18 cases (5.9%). In 57 cases (18.7%), patients with various chronic liver diseases had hepatocellular carcinoma as the main indication for transplantation. The grafts were obtained from male donors in 62.7% of cases, with a median age of 35.6 (IQR 22.9-47.2), the majority being victims of trauma (45.8%) or stroke (41.0%).

The median follow-up time was 2221 days (IQR 1528.5 - 2903.5), and biliary complications occurred in a median of 126 days (IQR 41.8 - 300.8), equivalent to medians of approximately six years and four months, respectively. Among patients in group 2 (n=70), 67 developed stenosis of the bile duct, and 10 patients developed a biliary fistula, seven of which were associated with stenosis and three isolated. The median time to diagnosis of stenosis was 131 days (IQR 48.0 - 329.0), and the median time to diagnosis of fistula was 73.5 days (IQR 18.8 - 149.3). Other clinical and demographic characteristics of the sample are provided in Table 1.

TABLE 1
Variables of the recipient, donor and intraoperative period

End-to-end biliary anastomoses were performed in 93.4% of cases and Roux-en-Y hepaticojejunostomy was performed in 6.6% of cases. The type of surgical technique used for anastomosis did not indicate a difference in the incidence of biliary complications (p=0.772).

CMV infection occurred within 35 days after surgery (IQR 20.0 - 53.5). Considering each study group separately, the group without biliary complications (group 1) showed infection by CMV in the median period of 39 days (IQR 25 - 56), while the group with biliary complications (group 2) showed a median of 22 days (IQR 16 - 37, Table 1). The comparison of the two groups showed a trend towards an earlier occurrence of infection in patients with biliary complications (p=0.07, Table 2).

TABLE 2
Time interval between transplantation and cytomegalovirus infection

Patients who showed positive CMV antigenemia (n=51) were divided into two subgroups according to the need for treatment with ganciclovir. There was no difference between the treated and untreated groups regarding the incidence of biliary complications (p=0.226). However, when the group of patients without CMV blood manifestation was compared with the group of patients with positive antigenemia at low titers (no indication for treatment with ganciclovir), there was a higher incidence of biliary complications in the latter group (p=0.040). The treatment of CMV infection with intravenous ganciclovir was associated with a lower incidence of biliary complications, for values that can be considered similar to those of patients without infection, even with a trend towards statistical significance (p=0.091, Table 3).

TABLE 3
Distribution of patients with and without biliary complications according to CMV antigenemia and treatment with ganciclovir

Multivariate analysis

For the multivariate analysis, the following variables were included: transplant indication group (p=0.042), diagnostic group (p=0.018), age range of the donor (p=0.145), age range of the recipient (p=0.029), CMV infection (p=0.021), recipient INR (p=0.009), and bile duct diameter ≤3 mm (p=0.033). The variables CMV infection, receptor INR, and bile duct diameter remained as factors associated with the occurrence of biliary complications (Table 4).

TABLE 4
Multivariate analysis including variables presenting with significant differences when comparing patients with or without biliary complications

A recipient INR <1.5 immediately before transplantation was associated with an increased risk of biliary complications compared to a pre-transplant INR between 1.5 and 2.5 (OR=2.2; p=0.020). No differences were observed for INR >2.5 and INR 1.5-2.5 (OR=1.4; p=0.470).

CMV infection was positively associated with the occurrence of biliary complications (OR=2.6; p=0.007). Finally, a bile duct diameter >3 mm was negatively associated with the biliary complications. The odds of biliary complications when the diameter was greater than 3 mm was 56% lower than those with a diameter ≤3 mm (OR=0.44; p=0.046).

DISCUSSION

Complications that occur after surgical procedures are often attributed to technical issues. However, the techniques of biliary anastomoses are insufficient to explain the frequent cases of stenosis and fistulas, which are the most common complications of liver transplants, affecting up to 34% of patients22 Akamatsu N, Sugawara Y, Hashimoto D. Biliary reconstruction, its complications and management of biliary complications after adult liver transplantation: a systematic review of the incidence, risk factors and outcome. Transpl Int. 2011;24(4):379-92.. It is possible that there are different factors involved in the genesis of these events after liver transplantation; however, the results found in the literature are varied and contradictory. Building on the large number of potential factors that have been associated with biliary complications and the variety of results obtained, we offer a large cohort of patients which received organs of young donors to contribute to clarify this challenging subject66 Costabeber AM, Lionco LC, Marroni C, Zanotelli ML, Cantisani G, Brandao A. D-MELD does not predict post-liver transplantation survival: a single-center experience from Brazil. Ann Hepatol. 2014;13(6):781-7.,99 Gastaca M, Matarranz A, Martinez L, Valdivieso A, Ruiz P, Ventoso A, et al. Risk factors for biliary complications after orthotopic liver transplantation with T-tube: a single-center cohort of 743 transplants. Transplant Proc. 2014;46(9):3097-9..

Variations of the surgical technique have been tested in an attempt to reduce the incidence of biliary stenosis and fistulas1818 Lopez-Andujar R, Oron EM, Carregnato AF, Suarez FV, Herraiz AM, Rodriguez FS, et al. T-tube or no T-tube in cadaveric orthotopic liver transplantation: the eternal dilemma: results of a prospective and randomized clinical trial. Ann Surg. 2013;258(1):21-9.. For some authors, choledochojejunostomy was related to a greater frequency of complications (especially anastomotic stenosis) compared to end-to-end biliary anastomosis1515 Kochhar G, Parungao JM, Hanouneh IA, Parsi MA. Biliary complications following liver transplantation. World J Gastroenterol. 2013;19(19):2841-6.,2323 Neuhaus P, Blumhardt G, Bechstein WO, Steffen R, Platz KP, Keck H. Technique and results of biliary reconstruction using side-to-side choledochocholedochostomy in 300 orthotopic liver transplants. Ann Surg. 1994;219(4):426-34.. In this study, this difference was not observed.

The clinical status and demographic characteristics of donors are frequently suspected causes in the development of biliary complications. Feng et al.88 Feng S, Goodrich NP, Bragg-Gresham JL, Dykstra DM, Punch JD, DebRoy MA, et al. Characteristics associated with liver graft failure: the concept of a donor risk index. Am J Transplant. 2006;6(4):783-90., showed that donor age >60 years was related to a higher number of biliary complications and lower survival of the graft. Other authors confirmed the relationship of older donor age with the incidence of biliary complications1919 Lue A, Solanas E, Baptista P, Lorente S, Araiz JJ, Garcia-Gil A, et al. How important is donor age in liver transplantation? World J Gastroenterol. 2016;22(21):4966-76.,2525 Serrano MT, Garcia-Gil A, Arenas J, Ber Y, Cortes L, Valiente C, et al. Outcome of liver transplantation using donors older than 60 years of age. Clin Transplant. 2010;24(4):543-9.,2727 Sundaram V, Jones DT, Shah NH, de Vera ME, Fontes P, Marsh JW, et al. Posttransplant biliary complications in the pre- and post-model for end-stage liver disease era. Liver Transpl. 2011;17(4):428-35.,2929 Thorsen T, Aandahl EM, Bennet W, Olausson M, Ericzon BG, Nowak G, et al. Transplantation With Livers From Deceased Donors Older Than 75 Years. Transplantation. 2015;99(12):2534-42., some of which differentiated anastomotic from non-anastomotic stenosis. The mean age of our younger donors (median=35.6 years) seems to be different than that European (only 58% are below 50 years) and American donors11 Adam R, Karam V, Cailliez V, JG OG, Mirza D, Cherqui D, et al. 2018 Annual Report of the European Liver Transplant Registry (ELTR) - 50-year evolution of liver transplantation. Transpl Int. 2018;31(12):1293-317.,2727 Sundaram V, Jones DT, Shah NH, de Vera ME, Fontes P, Marsh JW, et al. Posttransplant biliary complications in the pre- and post-model for end-stage liver disease era. Liver Transpl. 2011;17(4):428-35.. However, in this study, neither the donor nor recipient age remained a factor associated with biliary complications after multivariate analysis.

In this study, the etiology of liver disease did not influence the appearance of alterations in biliary drainage. Regarding laboratory tests, a lower INR value of the recipient, immediately before transplantation, was identified as a risk factor (p=0.020) for subsequent development of biliary complications. This finding was not present in any other study. However, the retrospective nature of the present investigation does not allow us to elucidate the causes for this relationship.

CMV infection and its relationship with a higher occurrence of biliary complications have been the subject of discussion33 Bittermann T, Goldberg DS. Cytomegalovirus and posttransplant biliary complications: Elusive offender or innocent bystander? Liver Transpl. 2013;19(10):1062-4.,77 Egawa H, Inomata Y, Uemoto S, Asonuma K, Kiuchi T, Fujita S, et al. Biliary anastomotic complications in 400 living related liver transplantations. World J Surg. 2001;25(10):1300-7.,99 Gastaca M, Matarranz A, Martinez L, Valdivieso A, Ruiz P, Ventoso A, et al. Risk factors for biliary complications after orthotopic liver transplantation with T-tube: a single-center cohort of 743 transplants. Transplant Proc. 2014;46(9):3097-9.,1010 Gotthardt DN, Senft J, Sauer P, Weiss KH, Flechtenmacher C, Eckerle I, et al. Occult cytomegalovirus cholangitis as a potential cause of cholestatic complications after orthotopic liver transplantation? A study of cytomegalovirus DNA in bile. Liver Transpl. 2013;19(10):1142-50.. In this sense, the high percentage of individuals serologically positive for CMV in Brazil stands out - a prevalence of 80 to 100% - compared to a prevalence of 40 to 60% in developed countries2121 Matos SB, Meyer, R., Lima, F.W.M. Seroprevalence of cytomegalovirus infection among healthy blood donors in Bahia State, Brazil. Rev Bras Hematol Hemoter. 2010;32(1):45-9.,2626 Souza MA, Passos AM, Treitinger A, Spada C. Seroprevalence of cytomegalovirus antibodies in blood donors in southern, Brazil. Revista da Sociedade Brasileira de Medicina Tropical. 2010;43(4):359-61.,3131 Zuhair M, Smit GSA, Wallis G, Jabbar F, Smith C, Devleesschauwer B, et al. Estimation of the worldwide seroprevalence of cytomegalovirus: A systematic review and meta-analysis. Reviews in medical virology. 2019:e2034.. However, the nature of this relationship is controversial, possibly due to the different forms used to detect infection - some studies use clinical criteria while others use antigenemia positivity or viral material detection via blood sample or liver biopsy (Polymerase Chain Reaction)1616 Kotton CN, Kumar D, Caliendo AM, Huprikar S, Chou S, Danziger-Isakov L, et al. The Third International Consensus Guidelines on the Management of Cytomegalovirus in Solid-organ Transplantation. Transplantation. 2018;102(6):900-31.. Standardization of CMV detection in the biliary tract could yield more consistent results33 Bittermann T, Goldberg DS. Cytomegalovirus and posttransplant biliary complications: Elusive offender or innocent bystander? Liver Transpl. 2013;19(10):1062-4.. Gotthardt et al. 10 identified CMV infection as a risk factor using the identification of viral DNA in the bile of transplanted patients as a detection method. In this study, multivariate analysis indicated a higher frequency of CMV infection in individuals who developed biliary complications (p=0.007). In addition, subgroups of patients with positive antigenemia were compared, and patients with positive antigenemia, treated or not, had the same incidence of biliary complications. Therefore, the innovation we introduce to the present knowledge concerns patients with positive antigenemia but below the cut-off point to indicate treatment. This subset had more biliary complications when compared to patients with negative antigenemia. This observation suggests value in preemptive treatment with ganciclovir in all patients or, at least, for any positive antigenemia level found after transplantation, to prevent such complications. Biliary complications have not been researched in publications involving prophylaxis and preemptive treatment1212 Halme L, Hockerstedt K, Lautenschlager I. Cytomegalovirus infection and development of biliary complications after liver transplantation. Transplantation. 2003;75(11):1853-8.. Specifically, no comparison was found with a subgroup of patients with pp65 antigenemia or PCR-positive low titers and its relation to biliary complications.

Limitations of this study include its retrospective nature, which could lead to information bias and can show correlation but not provide evidence of causation. However, posttransplant complications were prospectively recorded in a specific transplantation software system, which increases the reliability of the data obtained. Another limitation was the use of pp65 antigenemia as the tool to detect CMV instead of viremia-detecting methods.

The identification of these factors may help hepatic transplantation teams take preemptive steps to reduce the impact of early biliary complications. Pretransplant INR and bile duct graft diameter are noncontrollable factors, however, their presence should prompt closer monitoring for biliary complications to trigger early interventions. CMV manifestations, on the other hand, are modifiable. This study justifies the use of ganciclovir for all patients with positive antigenemia for CMV, including cases that are below the cut-off values that usually warrant preemptive treatment. Alternatively, early use of everolimus, a known CMV inhibiting immunosuppressive agent should be considered44 Bowman LJ, Brueckner AJ, Doligalski CT. The Role of mTOR Inhibitors in the Management of Viral Infections: A Review of Current Literature. Transplantation. 2018;102(2S Suppl 1):S50-s9.,2828 Tan L, Sato N, Shiraki A, Yanagita M, Yoshida Y, Takemura Y, et al. Everolimus delayed and suppressed cytomegalovirus DNA synthesis, spread of the infection, and alleviated cytomegalovirus infection. Antiviral Res. 2019;162:30-8.. However, further investigation may be required to confirm that the presence of the cytomegaly virus is a risk factor for biliary complications.

CONCLUSION

In our population, three important risk factors were associated with biliary complication: 1) low recipient INR immediately before transplantation; 2) bile duct diameter ≤3 mm; and 3) the occurrence of any title of positive antigenemia for CMV or disease manifestation in the first six months after transplantation.

REFERENCES

  • 1
    Adam R, Karam V, Cailliez V, JG OG, Mirza D, Cherqui D, et al. 2018 Annual Report of the European Liver Transplant Registry (ELTR) - 50-year evolution of liver transplantation. Transpl Int. 2018;31(12):1293-317.
  • 2
    Akamatsu N, Sugawara Y, Hashimoto D. Biliary reconstruction, its complications and management of biliary complications after adult liver transplantation: a systematic review of the incidence, risk factors and outcome. Transpl Int. 2011;24(4):379-92.
  • 3
    Bittermann T, Goldberg DS. Cytomegalovirus and posttransplant biliary complications: Elusive offender or innocent bystander? Liver Transpl. 2013;19(10):1062-4.
  • 4
    Bowman LJ, Brueckner AJ, Doligalski CT. The Role of mTOR Inhibitors in the Management of Viral Infections: A Review of Current Literature. Transplantation. 2018;102(2S Suppl 1):S50-s9.
  • 5
    Colonna JO, 2nd, Shaked A, Gomes AS, Colquhoun SD, Jurim O, McDiarmid SV, et al. Biliary strictures complicating liver transplantation. Incidence, pathogenesis, management, and outcome. Ann Surg. 1992;216(3):344-50; discussion 50-2.
  • 6
    Costabeber AM, Lionco LC, Marroni C, Zanotelli ML, Cantisani G, Brandao A. D-MELD does not predict post-liver transplantation survival: a single-center experience from Brazil. Ann Hepatol. 2014;13(6):781-7.
  • 7
    Egawa H, Inomata Y, Uemoto S, Asonuma K, Kiuchi T, Fujita S, et al. Biliary anastomotic complications in 400 living related liver transplantations. World J Surg. 2001;25(10):1300-7.
  • 8
    Feng S, Goodrich NP, Bragg-Gresham JL, Dykstra DM, Punch JD, DebRoy MA, et al. Characteristics associated with liver graft failure: the concept of a donor risk index. Am J Transplant. 2006;6(4):783-90.
  • 9
    Gastaca M, Matarranz A, Martinez L, Valdivieso A, Ruiz P, Ventoso A, et al. Risk factors for biliary complications after orthotopic liver transplantation with T-tube: a single-center cohort of 743 transplants. Transplant Proc. 2014;46(9):3097-9.
  • 10
    Gotthardt DN, Senft J, Sauer P, Weiss KH, Flechtenmacher C, Eckerle I, et al. Occult cytomegalovirus cholangitis as a potential cause of cholestatic complications after orthotopic liver transplantation? A study of cytomegalovirus DNA in bile. Liver Transpl. 2013;19(10):1142-50.
  • 11
    Greif F, Bronsther OL, Van Thiel DH, Casavilla A, Iwatsuki S, Tzakis A, et al. The incidence, timing, and management of biliary tract complications after orthotopic liver transplantation. Ann Surg. 1994;219(1):40-5.
  • 12
    Halme L, Hockerstedt K, Lautenschlager I. Cytomegalovirus infection and development of biliary complications after liver transplantation. Transplantation. 2003;75(11):1853-8.
  • 13
    Horster S, Bauerlein FJ, Mandel P, Raziorrouh B, Hopf C, Stemmler HJ, et al. Influence of hepatitis C virus infection and high virus serum load on biliary complications in liver transplantation. Transpl Infect Dis. 2013;15(3):306-13.
  • 14
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  • Financial source:

    none

  • Distribuição dos pacientes com e sem complicações biliares, de acordo com antigenemia para CMV e tratamento com ganciclovir
  • Central message

    Cytomegalovirus infection may play a role in the development of biliary complications after liver transplantations and its prevention opens up nice perspectives to decrease this inconvenient morbidity.
  • Perspective

    Biliary complications are not rare after liver transplantation, inflicting troubles to the patient and increasing costs to health system. Reviewing a large cohort of patients, cytomegalovirus infection or reactivation was identified as a modifiable risk factor for this complication. Virus expression, even at low titers, could be related to development of biliary stenosis and fistulae. Inhibition of cytomegalovirus brings a new perspective to diminish post-transplant morbidity.

Publication Dates

  • Publication in this collection
    18 Dec 2020
  • Date of issue
    2020

History

  • Received
    30 Mar 2020
  • Accepted
    03 July 2020
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