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GE-Portuguese Journal of Gastroenterology

versão impressa ISSN 2341-4545

GE Port J Gastroenterol vol.27 no.2 Lisboa abr. 2020

https://doi.org/10.1159/000501405 

REVIEW ARTICLE

 

Secondary Sclerosing Cholangitis in Critically Ill Patients: An Underdiagnosed Entity

Colangite esclerosante secundária em doentes críticos: uma entidade subdiagnosticada

 

Pedro Martinsa, Mariana Verdelho Machadoa,b

aClínica Universitária de Gastrenterologia, Faculdade de Medicina, Universidade de Lisboa, Lisbon, Portugal; bServiço de Gastrenterologia, Hospital de Santa Maria, CHULN, Lisbon, Portugal

* Corresponding author.

 

ABSTRACT

Secondary sclerosing cholangitis in critically ill patients (SSCCIP) is a recently identified cholestatic liver disease occurring in patients without prior history of hepatobiliary disease, after receiving treatment in the intensive care unit (ICU) in different settings, including cardiothoracic surgery, infection, trauma, and burns. It is a rare entity, being estimated to occur in 1/2,000 patients in an ICU; however, it is a dismal condition, with up to half of the patients dying during the ICU stay and with rapid progression to liver cirrhosis over weeks to months. SSC-CIP should be considered in the differential diagnosis of cholestasis in the ICU, particularly when cholestasis persists after recovery from the critical event. Diagnosis is established with magnetic resonance cholangiopancreatography or endoscopic retrograde cholangiopancreatography showing dilations and stenoses of the intrahepatic bile ducts as well as biliary casts. No available treatment has been shown to slow the rapid progression of the disease, and liver transplant referral should be considered early after the diagnosis of SSC-CIP. Increased awareness and timely diagnosis are crucial in order to improve the current appalling outcome.

Keywords: Secondary sclerosing cholangitis, Critically ill patients, Intensive care unit

 

RESUMO

A colangite esclerosante secundária em doentes críticos (CEP-DC) é uma doença colestática, identificada recentemente, que ocorre em doentes sem antecedentes de patologia hepato-biliar, após internamento em unidade de cuidados intensivos (UCI) por diferentes indicações, incluindo: cirurgia cárdio-torácica, infeção, trauma e queimaduras. É uma entidade rara, com uma incidência estimada de um em cada 2,000 doentes em UCI. Ainda assim, trata-se de uma doença com um muito mau prognóstico, sendo que até metade dos doentes morre durante o internamento na UCI, e apresenta uma rápida progressão para cirrose em semanas a meses. A CEP-DC deve ser considerada no diagnóstico diferencial de colestase em UCI, particularmente se a colestase persistir após a recuperação do evento potencialmente fatal. O diagnóstico é estabelecido através de colangiopancreatografia por ressonância magnética ou colangiopancreatografia retrógrada endoscópica, que revelam estenoses e dilatações difusas dos canais biliares intra-hepáticos e cilindros biliares. Não está disponível uma terapêutica capaz de atrasar a rápida progressão da doença e a referenciação para transplantação hepática deve ser considerada logo após o diagnóstico. Para melhorar o mau prognóstico atual, é essencial um maior reconhecimento e diagnóstico precoce.

Palavras-Chave: Colangite esclerosante secundária, Doentes críticos, Unidade de cuidados intensivos

 

Introduction

Sclerosing cholangitis encompasses a group of progressive cholestatic diseases affecting the intra- and/or extrahepatic bile ducts that can progress to biliary cirrhosis. Primary sclerosing cholangitis (PSC) is an idiopathic disease characterized by a typical beaded appearance in cholangiographic studies, which has a strong association with inflammatory bowel disease [1, 2]. When we identify a cause for sclerosing cholangitis it is dubbed secondary sclerosing cholangitis (SSC). Examples of SSC are autoimmune IgG4-associated, infectious, drug-induced, ischemic, and obstructive [3]. SSC in critically ill patients (SSC-CIP) is a rare form of SSC that was first described by Scheppach et al. in 2001 [4]. SSC-CIP is believed to be ten times less frequent than PSC [5]; only 250 cases have been reported in the literature. Over half of the cases were published in the last 5 years, which reflects increasing awareness of this disease.

The pathogenesis of SSC-CIP is not fully understood, but the main pathogenic mechanisms seems to be ischemia of the bile ducts, changes in bile composition, and biliary infection [6–8].

SSC-CIP affects patients with no history of previous hepatobiliary disease, after treatment in an intensive care unit (ICU) for different underlying conditions including major surgery, sepsis, and trauma [5, 9]. SSC-CIP should be considered in the differential diagnosis of cholestasis in ICU patients when cholestasis persists beyond successful treatment of the underlying disease [6]. The diagnosis is made by endoscopic retrograde cholangiopancreatography (ERCP) or magnetic resonance cholangiopancreatography (MRCP) revealing PSC-like diffuse strictures and dilations of the intrahepatic bile ducts, and filling defects translating biliary casts [8, 10].

SSC-CIP typically has two different presentations: (1) acute liver failure during ICU treatment or (2) persistent cholestasis rapidly progressing to cirrhosis [6, 9, 11, 12]. The prognosis is dire, with around half the patients dying in the ICU and the other half requiring liver transplantation in the following 3–4 years [5, 13].

This review aims to summarize the most recent evidence regarding the pathogenesis, diagnosis, and prognosis of SSC-CIP. Emphasis is placed on differential diagnosis to help in the early diagnosis, which might improve outcomes, allowing earlier palliative endoscopic therapy and referral for liver transplantation.

Epidemiology

Critically ill patients who develop SSC are a very heterogeneous group, which reflects the range of possible underlying diseases that lead to ICU admission. The unifying feature is the lack of previous hepatobiliary disease [5, 14, 15]. Reasons for ICU admission include burns, trauma, acute respiratory distress syndrome, infections, subarachnoid hemorrhage, and major surgery [5, 10, 14, 16]. Cardiothoracic surgery seems to confer a particularly high risk of developing SSC-CIP [9, 17]. The mean age of patients at the time of diagnosis is 50 years, but ranges from 19 to 79 years, which can be explained by the unpredictable nature of some of the reasons for ICU admission [6, 18]. The average length of ICU stay is 30–40 days, though in some cases it may be as short as 9 days [5, 11, 19]. Similarly to PSC, there is a male predominance, with studies reporting a male:female ratio ranging from 2.2: 1 to 9: 1 [6–8, 14, 16, 20]. All reported patients required mechanical ventilation during their ICU stay for an average of > 30 days, and most patients presented severe hypotension requiring vasopressor treatment [6, 7, 14, 18, 21]. Weig et al. [22] evaluated patients with acute respiratory distress syndrome due to H1N1 pneumonia and found that obesity, increased visceral fat, and longer time spent in prone position were associated with a higher risk of developing SSC-CIP.

Although SSC-CIP is certainly rare, its true prevalence has not been ascertained. In fact, SSC-CIP is an underdiagnosed condition, with half of the patients dying during ICU stay before the diagnosis can be reached [9, 13]. Two retrospective studies found a similar prevalence of SSC-CIP, affecting about 1/2,000 patients admitted to an ICU [7, 14]. Leonhardt et al. [5] identified SSC-CIP as being responsible for 0.61% of all liver transplantations in one hospital, which was ten times less frequent than PSC accounting for 6.2%.

Pathophysiology

The exact mechanisms by which SSC-CIP develops are yet to be understood. Both critical illness and its intensive care treatment seem to contribute to the pathogenesis [7]. The most accepted theory is that ischemia (“ischemic cholangiopathy”) in combination with changes in bile composition (“toxic bile”) lead to necrosis of cholangiocytes and bile cast formation. The resulting biliary obstruction and biliary infection both participate in a process that leads to progressive and irreversible destruction and obliteration of the intrahepatic bile ducts, ultimately leading to secondary biliary cirrhosis [5–7, 23, 24].

Total parenteral nutrition is common in critically ill patients and can lead to steatosis and cholestatic liver dysfunction when used for > 1 week [25, 26]. However, epidemiological studies do not support total parenteral nutrition as a risk factor for SSC-CIP [7].

Idiosyncratic drug-induced liver injury could also promote the development of SSC-CIP. When drug-induced liver injury manifests as a cholestatic or mixed-type pattern in hepatic tests it is dubbed drug-induced cholangiopathy, reflecting damage to the biliary epithelium. Patients with drug-induced cholangiopathy can develop SSC [27, 28]. Several drugs commonly used in the ICU setting have been implicated in drug-induced SSC, including antibiotics and anesthetics such as ketamine [28–30]. Interestingly, in one case series, 15 out of 16 patients received ketamine prior to developing SSC-CIP [7]. Predisposition to drug-induced cholangiopathy seems to be genetically determined [31].

Ischemic Cholangiopathy

The hepatic parenchyma is supplied by both the hepatic arteries and the portal vein, whereas the common bile duct receives a dual arterial blood supply from both the hepatic artery and branches of the gastroduodenal artery [32]. However, the intrahepatic biliary tree is supplied exclusively by branches of the hepatic artery, which form the intrahepatic peribiliary vascular plexus [33, 34]. This provides the anatomical grounds for intrahepatic bile duct ischemic susceptibility and could explain why the extrahepatic bile duct is usually spared in SSC-CIP [5, 8, 10].

Macrocirculatory compromise seems to be the cornerstone of ischemic bile duct injury, particularly when associated with microcirculatory disturbances directly affecting the peribiliary vascular plexus [7, 33]. Around 33% of ICU patients have hemodynamic instability requiring vasopressors at some time during their stay [35]. In patients who develop SSC-CIP, this number rises to 60–100% [6, 7, 10]. Moreover, the onset of hypotension seems to be temporarily associated with the onset of cholestasis [7]. Previous researchers have hypothesized that use of high-dose vasopressors could promote the development of SSC-CIP [6, 10, 14, 21]. However, this hypothesis is not substantiated by the available data. All vasopressors and inotropes increase systemic blood pressure and cardiac output, but this does not necessarily translate into improved hemodynamics in the hepatosplanchnic territory [36]. Norepinephrine, based on its α-adrenergic agonist effects, has been assumed to induce splanchnic ischemia. However, the experimental data are hard to interpret because studies are very heterogeneous regarding their population and hemodynamic endpoints [36]. For example, norepinephrine has been shown to have no effect on mesenteric blood flow in a septic sheep model, but it decreased mesenteric blood flow in a septic porcine model [37, 38]. In one study with 10 septic human patients, norepinephrine was associated with a higher hepatosplanchnic blood flow to cardiac output ratio as compared with dopamine, resulting in improved hepatocellular energy balance [39]. This result was unexpected since regional vasodilating properties of dopaminergic activation should lead to a higher hepatosplanchnic to cardiac output ratio in dopamine-treated patients. These findings translate the contradictions found in the literature as well as the unreliability of biological plausibility as the sole argument for vasopressor-induced biliary ischemia. More recently, two small retrospective studies failed to demonstrate an association between high-dose vasopressor use and a higher risk of SSC-CIP development [7, 22].

All patients with SSC-CIP received mechanical ventilation, which is believed to contribute to hepatosplanchnic ischemia [18, 21]. In fact, mechanical ventilation with positive end-expiratory pressure > 10 cm H2O, prone position, and low tidal volumes were associated with negative effects on hepatosplanchnic blood flow in animal models [40–42]. Prone position in particular seems to be associated with the development of SSC-CIP in humans [22].

Leonhardt et al. [7] showed that all SSC-CIP patients presented at least one factor capable of disrupting the microcirculation blood flow, namely increased blood viscosity, red blood cell transfusions, and/or hypercoagulable states. Moreover, two different groups also supported the association with higher number of red blood cell units transfused [8, 10].

In summary, disturbances in the arterial supply of the peribiliary vascular plexus lead to necrosis of cholangiocytes with formation of biliary casts and inflammation/scarring of the bile ducts, which results in cholestasis [6, 17]. Biliary casts have also been described following orthotopic liver transplantation, in which two different types of casts have been identified based on their biochemical composition. One type is mainly composed of bilirubin (10–50%) and bile acids (10–15%) and is thought to arise due to mechanical obstruction. The other type is mainly composed of proteins, mostly collagen, and seems to be derived from necrotic cholangiocytes [43, 44]. Biliary casts in SSC-CIP are mainly composed of proteins and can be seen in the first weeks after the onset of cholestasis, further supporting ischemia as the primary insult in these patients [6].

The above considerations place SSC-CIP as a result of ischemic injury of the biliary tree. Whereas in the posttransplant setting and after chemoembolization biliary tree ischemia seems to be a result of local disturbances in the arterial supply of the biliary tree, in SSC-CIP, ischemia seems to be a consequence of systemic hemodynamic instability in critically ill patients.

Toxic Bile

Under physiological circumstances, cholangiocytes are protected from toxic hydrophobic bile salts through defense mechanisms that rely on hepatobiliary transporters. The formation of mixed micelles of bile salts is one such mechanism, and it is dependent on biliary phospholipid secretion by hepatocytes via MDR3/ABCB4 [24, 45]. Genetic defects with impaired MDR3/ABCB4 activity have been linked to cholestatic and ductopenic liver disease in humans [46]. It has been shown that MDR2 (human orthologue: MDR3) knockout mice develop sclerosing cholangitis secondary to complete absence of phospholipids from bile [47, 48]. Ischemia can negatively affect hepatobiliary transporters promoting cell injury and cholestasis [49, 50]. Trauner et al. [24] hypothesized that genetic variants with low MDR3 expression might predispose to the formation of toxic bile under ischemic or inflammatory conditions, explaining why some critically ill patients with cholestasis develop SSC-CIP. Another important mechanism of defense is the secretion of HCO3 – via AE2, which maintains a high pH near the apical surface of cholangiocytes, capable of preventing permeation of protonated bile acids. Beuers et al. [45] theorized that loss of this protective mechanism due to ischemia is implicated in SSC-CIP. Indeed, proinflammatory cytokines inhibit AE2 activity in animal models [51].

Systemic inflammatory response syndrome seems to also play a role. It occurs in > 50% of ICU patients [52]. Interestingly, Leonhardt et al. [7] found that all 16 of their SSC-CIP patients developed systemic inflammatory response syndrome prior to diagnosis. These findings suggest that inflammatory stress also promotes the development of toxic bile, which further contributes to cholangiocyte necrosis.

Biliary Infection

Few case reports have described SSC following a single severe episode of bacterial cholangitis; however, the development of SSC after recurrent bacterial cholangitis in the context of chronic biliary obstruction is much more frequent [53, 54].

Biliary obstruction is a prerequisite for bacterial cholangitis because it abrogates the antibacterial effects of bile flow and the biliary secretion of IgA [55]. In SSCCIP, biliary obstruction is the result of the development of biliary casts, which are present since the first weeks of cholestasis. As the disease progresses, the obstruction is perpetuated due to the development of multifocal intrahepatic biliary strictures [5, 6]. A meta-analysis found that bacteria and/or Candida species are detectable in the bile collected during ERCP in 98% of SSC-CIP patients [21]. Enterococci and Candida albicans are the most common agents, which frequently present a high rate of antibiotic resistance, presumably a reflection of the high rate of previous antibiotic treatment in critically ill patients [56]. Recurrent bacterial cholangitis is common in SSC-CIP patients and is associated with the progression to cirrhosis [5, 6, 19, 21]. The role of the microbiome is also highlighted by the recently described association between NOD2 gene mutations and higher susceptibility for developing SSC-CIP [57]. NOD2 is a pattern recognition receptor that regulates the gut-microbiome homeostasis and plays a key role in bacterial translocation. NOD2 gene mutations had already been identified as risk factors for Crohn’s disease and spontaneous bacterial peritonitis in patients with liver cirrhosis [57, 58]. The pathophysiology of SSC-CIP is summarized in Figure 1 .

 

 

Diagnosis

The diagnosis of SSC-CIP is difficult for several reasons: (1) it is an underrecognized entity; (2) it is asymptomatic in the early stages, manifesting only as a laboratorial cholestatic pattern; (3) the differential diagnosis of cholestasis in ICU patients is vast, being secondary to SSC-CIP in only a minority of patients; (4) the diagnosis can only be established by MRCP/ERCP; (5) mortality is high during ICU treatment, often precluding a timely diagnosis [5, 10, 59].

Laboratory Parameters

SSC-CIP manifests with a pattern of cholestasis. Gamma-glutamyl transpeptidase increases first, around 7–9 days after the initial insult, and is followed a few days later by alkaline phosphatase elevation. Bilirubin is the last to rise, taking around 20 days. Gamma-glutamyl transpeptidase elevation is also more pronounced, peaking at around 20–50 times the upper limit of normal (ULN), while alkaline phosphatase and bilirubin elevation reach a maximum of 15 times the ULN [5, 8]. Conversely, alanine aminotransferase and aspartate aminotransferase show only a moderate increase of up to three times the ULN [18]. Interestingly, bilirubin levels may spontaneously decrease after 2–6 months while SSC-CIP keeps progressing [10]. In one study there was a significant increase of cholesterol levels in SSC-CIP patients, around 2.5 times the ULN, differentiating it from PSC, in which hypercholesterolemia is uncommon [5, 60].

The differential diagnosis for cholestasis in the ICU setting is extensive, most notably sepsis-induced cholestasis, total parenteral nutrition, choledocholithiasis, and drug-induced liver injury [25, 59]. Hypoxic liver injury, although mostly characterized by hepatocellular necrosis, still merits discussion. Indeed, hypoxic liver injury affects 10% of ICU patients, and it is also associated with shock and manifests as jaundice in one-third of patients [61]. The different characteristics of these diseases are shown in Table 1 and a diagnostic algorithm is presented in Figure 2.

 

 

 

 

The single most important aspect that distinguishes SSC-CIP is the persistence of cholestasis beyond clinical recovery, which reflects irreversible anatomical damage rather than transient functional impairment [25, 54].

Imaging Studies

The first diagnostic study in a patient with cholestasis is an abdominal ultrasound (US), which can rule out other diagnoses such as choledocholithiasis, although lacking sensitivity for SSC-CIP [62]. Indeed, abdominal US suggested the diagnosis of SSC-CIP in only 30–40% of patients [5, 9]. This low sensitivity is due to the fact that echogenic biliary casts assume the shape of the biliary tree, mimicking a normal bile duct system. Hence, a normal abdominal US should not exclude further testing when SSC-CIP is suspected (i.e., when cholestasis persists beyond recovery from the ICU or when cholangitis develops) [9].

MRCP is the imaging method of choice following abdominal US since it is noninvasive and can accurately diagnose SSC-CIP. In the early stages, MRCP presents defects in the intrahepatic biliary tree corresponding to biliary casts and biliary leakages, occasionally forming bilomas. At later stages, diffuse intrahepatic bile duct strictures are observed. Notably, the distal common bile duct is preserved at all stages [8]. MRCP has some limitations: (1) it does not allow for interventional procedures, and (2) it is limited in patients with heart medical devices [9].

ERCP is the gold standard for the diagnosis of SSCCIP [5, 6, 10, 14]. However, most studies report a delay of around 60 days until ERCP is performed, though more recent studies reported lower delay of up to 25 days [5, 9, 14, 63]. This delay might be attributable to several factors: (1) lack of awareness of SSC-CIP, (2) dilated bile ducts on US (that would prompt the realization of ERCP) occur in < 50% of cases, and (3) SSC-CIP is seldom misdiagnosed as sepsis-induced cholestasis (the most common cause of cholestasis in the ICU) [5, 54, 64]. As such, it is often not until cholestasis fails to resolve after clinical recovery that the clinical suspicion of SSC-CIP becomes significant enough to merit an ERCP, inevitably leading to a delayed diagnosis [9, 54].

Similarly to MRCP, early ERCP findings consist of intraductal filling defects in the intrahepatic bile ducts due to biliary casts. As the disease progresses, diffuse irregular strictures and dilations with a typical beaded appearance become evident. In later stages the peripheral intrahepatic bile ducts are completely obliterated, leaving only a central biliary system that Leonhardt et al. described as a “pruned tree” [5, 6]. Concomitant extrahepatic bile duct involvement occurs in around 20% of cases, but it is always mild. In 6% of cases the strictures are confined to the extrahepatic bile ducts [5, 9]. During ERCP it is important to collect bile samples for microbiological examination, since in 98% of patients a pathogen is identified, allowing for guided antimicrobial therapy [21].

The differential diagnosis based on radiographic findings includes PSC and other forms of SSC. Differentiation between SSC-CIP and other forms of sclerosing cholangitis heavily relies on the clinical history that allows for the identification of the primary insult. However, some radiological features suggest SSC-CIP, namely sparing of the extrahepatic bile ducts and presence of biliary casts [5, 65]. In fact, biliary casts seem to be exclusive to SSC-CIP and ischemic sclerosing cholangitis [3, 5]. Ischemic sclerosing cholangitis is mostly associated with post-orthotopic liver transplantation hepatic artery thrombosis and hepatic arterial infusion of floxuridine in the context of colorectal liver metastases [54]. The different forms of SSC and their typical features are shown in Table 2.

 

 

Histopathology

Liver histology has limited diagnostic value because the early features are nonspecific and consistent with chronic bile duct obstruction [6]. Liver biopsy suggests SSC-CIP in only one-third of patients [9]. Furthermore, there seems to be no correlation between histological findings and laboratory values. Nonetheless, liver biopsy can be useful by excluding other conditions [16].

Histological findings can be localized in the portal/periportal areas and in the acini. In the early stages only the portal/periportal areas are affected, with edema of the small and medium portal tracts, mild inflammatory infiltrates consisting mostly of lymphocytes with occasional neutrophils, and cytological changes in the interlobular bile ducts (cytoplasmic vacuolization and loss of polarization) [6, 16]. As the disease progresses, marginal ductular proliferation, ductular metaplasia of periportal hepatocytes, and portal/periportal fibrosis can occur. Some patients present bile thrombi [6, 10, 16]. Only in later stages can the acini be affected, with bilirubinostasis, hepatocellular rosette formation, and cholestatic necrosis. Eventually, it can progress to biliary fibrosis and secondary biliary cirrhosis [66]. Esposito et al. [16] hypothesized that portal bile duct damage is the primary insult, which leads to inflammation and ductular proliferation in the portal/ periportal area and ultimately can induce the parenchymal changes.

Natural History of Disease and Prognosis

Persistent cholestasis in patients surviving a lifethreatening event is what clinically defines SSC-CIP [10]. SSC-CIP has an unspecific presentation but can have a dramatic course, with mortality rates reaching 50% during ICU treatment. Mortality is associated with renal failure and higher Model for End-Stage Liver Disease (MELD) scores [9, 13]. The cause for ICU admission also affects mortality, with burns and trauma in previously healthy patients being associated with better outcomes [8].

Typical sclerosing cholangitis manifestations, such as jaundice, pruritus, and abdominal discomfort, only occur in advanced disease in patients who survived the ICU period [54]. Severe weight loss occurs in most patients within the first year, with an average loss of 18 kg, in contrast with PSC, where weight loss only occurs in one-third of patients [5, 67]. Recurrent episodes of bacterial cholangitis secondary to bile duct destruction are common, with biliary stenoses impairing bile flow and limiting the effect of antibiotic treatment. Indeed, biliary sepsis is an important cause of death in these patients [5, 17].

Progression to liver cirrhosis can occur rapidly over a period of months, and in some patients it takes as little as weeks [5, 10, 63]. This rapid progression translates into an exceptionally high mortality. Transplant-free survival is 55% after 1 year and only 14% after 6 years. SSC-CIP median transplant-free survival is 13–44 months, which contrasts with 89 months for PSC and 72 months for SSC in general [5, 17, 68]. On the other hand, while in PSC cholangiocarcinoma occurs in 7–13% of patients, there are no reports of cholangiocarcinoma in SSC-CIP patients [1, 68–70]. This might be explained by the short life expectancy and the short follow-up in the studies so far.

The most common cause of death is hepatic failure, which occurs in 36% of patients. Out of the 60% of surviving patients, approximately 40% develop biliary cirrhosis and remain in stable condition, while the other 20% progress to end-stage liver disease requiring liver transplantation [18].

Treatment

Endoscopic removal of biliary casts and sphincterotomy improve biliary drainage, resulting in transient clinical and biochemical improvement even when biliary cirrhosis has already occurred [6, 15, 23]. Endoscopic balloon dilation and intermittent stenting of dominant stenoses also seem to improve cholestasis. However, in most cases this approach is not feasible because of the multifocal and intrahepatic localization of the stenoses [10, 15, 23]. Repeated endoscopic interventions are often necessary as biliary casts may recur [5, 11, 65]. Despite the transient improvement, disease progression seems inevitable and the outcome of patients is not affected by endoscopic therapy [16, 17].

Ursodeoxycholic acid is commonly used in an effort to improve bile flow [6, 11, 15, 23, 65]. It has not been studied in clinical trials in SSC-CIP, but its efficacy seems to be limited [10, 17].

Recurrent episodes of cholangitis are treated with endoscopic therapy to alleviate obstruction and antimicrobials. The antimicrobial therapy should be adjusted based on microbiological analysis, and it should be extended for 2 weeks [21, 55]. In many cases, biliary drainage is inadequate because ERCP cannot access excluded peripheral bile ducts, limiting the effectiveness of the treatment [5].

When SSC-CIP progresses and biliary cirrhosis develops, orthotopic liver transplantation is the only curative treatment [23]. Urgent liver transplantation may be required during ICU stay due to acute liver failure [6]. Up to 75% of SSC-CIP patients are referred for liver transplantation within the first year after the diagnosis [5]. The MELD score is widely used in Europe to guide the allocation of liver grafts and has prognostic value in SSC-CIP [9, 71]. However, MELD alone may not be a good measurement of the urgency for liver transplantation, since many patients with SSC-CIP maintain stable coagulation and liver function despite a dismal evolution, thus delaying transplantation [13]. In the case of PSC, recurrent bacterial cholangitis confers higher priority in the form of MELD exception points [72]. In a study by Leonhardt et al. [5], 2 out of 16 patients died of biliary sepsis while on the transplant waiting list, so probably the same rationale should be applied for SSC-CIP. Survival rates after liver transplantation are comparable to those of patients transplanted due to alcoholic liver cirrhosis, with 1- and 3-year survival rates around 90 and 85%, respectively [5, 13]. Most deaths after liver transplantation occur within the first year, sepsis being the main cause of death. Previously healthy trauma patients seem to have a better prognosis after liver transplant [63].

Conclusion

SSC-CIP is an underdiagnosed entity that poses a great challenge to both intensivists and gastroenterologists. In SSC-CIP both critical illness and ICU treatment are responsible for ischemic injury of the biliary tree that, together with changes in bile composition, leads to the formation of biliary casts and stricturing, with subsequent persistent bacterial infection driving the rapid progression of the disease. SSC-CIP shows a typical cholestatic pattern that persists after recovery from the critical illness, which should be a hint to differentiate from other causes of cholestasis in the ICU. The diagnosis requires MRCP/ERCP, but it is often delayed due to unawareness of the disease and unspecific presentation. SSC-CIP has a dismal prognosis with high mortality rates during the ICU stay and rapid progression to liver cirrhosis requiring liver transplantation. Medical treatment is lacking, and endoscopic interventions allow only for palliative treatment, hence the diagnosis of SSC-CIP should prompt early referral for liver transplantation.

 

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Disclosure Statement

The authors have no conflicts of interest to declare.

 

* Corresponding author.

Mariana Verdelho Machado

Serviço de Gastrenterologia, Hospital de Santa Maria

Av. Prof. Egas Moniz

PT–1649-035 Lisbon (Portugal)

E-Mail mverdelhomachado@gmail.com

 

Received: March 24, 2019: Accepted after revision: June 7, 2019

 

Author Contributions

P. Martins wrote the review. M. Verdelho Machado did the writing and corrected the review.

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