Madacsy L*, Dubravcsik Z and Szepes A
Department of Gastroenterology, Bács-Kiskun Teaching Hospital of the University of Szeged, Kecskemét, Hungary
Corresponding Author : Madacsy L
Department of Gastroenterology
Bács-Kiskun Teaching Hospital of the University of Szeged, Kecskemét, Hungary
Tel: +3662544000
E-mail: endomabt1@gmail.com
Received September 02, 2015; Accepted November 16, 2015; Published November 19, 2015
Citation: Madacsy L, Dubravcsik Z, Szepes A (2015) Postcholecystectomy Syndrome: From Pathophysiology to Differential Diagnosis – A Critical Review. Pancreat Disord Ther 5:162. doi:10.4172/2165-7092.1000162
Abstract
Cholecystectomy has an excellent therapeutic outcome. Up to 15-20 % of cholecystectomized patients however, continue to have a variety of gastrointestinal symptoms. Post-cholecystectomy syndrome (PCS) can be defined as symptoms of biliary colic or persistent right upper quadrant (RUQ) abdominal pain with or without dyspepsia, which are similar to that experienced by the patient before cholecystectomy. PCS continue to be present as a diagnostic and therapeutic challenge. The aim of this paper was to critically review the literature about the magnitude of the problem and the possible pathophysiological explanations of PCS.
Keywords
Postcholecystectomy syndrome; Sphincter of oddi dysfunction; Functional abdominal pain
Introduction
Cholecystectomy has an excellent therapeutic outcome. Up to 15-20 % of cholecystectomized patients, however, continue to have a variety of gastrointestinal symptoms such as fatty food intolerance, nausea and vomiting, heartburn, flatulence, indigestion, diarrhea, mild occasional abdominal pain attacks and severe RUQ pain with extreme post-cholecystectomy distress. The term used to describe this condition is post-cholecystectomy syndrome (PCS), which was originally suggested by Pribram [1]. Post-cholecystectomy syndrome (PCS) defined as symptoms of biliary colic or persistent right upper quadrant (RUQ) abdominal pain with or without dyspepsia, which are similar to that experienced by the patient before cholecystectomy. Although a large volume of medical information accumulated since the first description, patients with PCS, continue to be present as a diagnostic and therapeutic challenge. Our current knowledge about the pathophysiology of PCS has significantly improved since the introduction of the endoscopic retrograde cholangiopancreatography (ERCP) and the endoscopic sphincter of Oddi manometry (ESOM) in the diagnostic opportunities. The aim of this paper was to review the literature critically on the magnitude of the problem and the possible pathophysiological explanations of PCS.
Magnitude of the Problem
The reported frequency of PCS varies widely in the literature. Several previous investigations have evaluated the effects of cholecystectomy on the symptoms, but their results were contradictory, which caused by the variations of the study design. It is also difficult to precisely analyze the current literature in regards to the frequency of post-cholecystectomy symptoms because the lack of clear distinction between biliary pain and dyspepsia. The reported frequency of postcholecystectomy pain ranged from 14% to 34% in the reviewed literature, but postoperative dyspepsia was a more frequent symptom that occurred in up to 54% of cholecystectomized patients. In an old study published by Burnett. 126 patients retrospectively interviewed one year after cholecystectomy, and demonstrated that 75% of patients were relieved of all symptoms [2]. In an excellent landmark study by Bodwall, two thousand patients were followed up symptomatically for 2-5 years after cholecystectomy, and the results were evaluated by computer-assisted analysis of multiple variables. Their results suggested that female sex, lower age, longer preoperative symptomatic period, the absence of gallbladder inflammation, and a functioning acalculous gallbladder were associated with higher frequency of PCS. The accurate interpretation of 351 intravenous cholangiography by the same working group has provided up to date evidence that patients with more severe symptoms of PCS associated with a larger common bile duct diameter [3]. Gunn emphasized that although dyspeptic symptoms were present in 88% of all patients preoperatively, as much as 69% of patients were symptomatically improved by cholecystectomy [4]. Bates published a prospective controlled study in 295 patients referred to cholecystectomy. They claimed that before the operation symptoms of dyspepsia were far more frequent in the gallstone group, and cholecystectomy reduced the dyspeptic symptoms to an incidence that was almost equal to the level of the age-matched control group [5]. Our working group demonstrated a positive correlation between post-cholecystectomy pain and the presence of dyspeptic symptoms after the operation [6]. Ros pointed out that the overall results of cholecystectomy mainly depended on the fact what was the patient’s expectation of the procedure [7]. In contrast, the type of the surgical access has not influenced the symptomatic outcome (neither open nor laparoscopic approach) [8]. The majority of PCS patients only suffered from dyspepsia with mild and occasional pain attacks that caused by functional motility disturbances of the upper gut and the sphincter of Oddi (SO). Only 2-5% of the PCS patients with continuous severe distress, intense right upper quadrant pain and recurrent cholangitis accounted from all cholecystectomized adults. In this group, the diagnostic strategy should be focused on the exploration of any organic causes [9].
Possible Pathophysiological Explanations
PCS may be caused by organic or functional diseases of the gastrointestinal tract. It can be further classified into two groups for systematic evaluation. Patients with symptoms of non-biliary tract origin and those with symptoms of biliary tract origin. If organic diseases are suspected, such as peptic ulcer, common bile duct stone, a benign or malignant tumor of the biliary tract or the head of the pancreas than the management is self-evident. However, functional causes of the PCS are more frequent in clinical practice and because of the lack of objective diagnostic criteria; it’s more difficult to diagnose and to treat properly.
Organic Extrabiliary Diseases
Differential diagnosis can be difficult since symptoms similar to PCS may originate from other organic diseases of the esophagus, stomach, small and large bowel or the pancreas. Careful case history, physical examination, laboratory studies, abdominal ultrasound, abdominal computer tomography and gastrointestinal endoscopy may be useful to identify an underlying organic disorder. Disease of the dorsal spine may manifest in a disabling, chronic abdominal pain and represent an important and treatable cause of PCS, which is unfortunately infrequently diagnosed [10]. The pain originated from the vertebral column can be discogenic and zygapophysial- joint (facet) mediated or it can be a result of spinal root compression [11]. The early phase of herpes zoster may also induce neuropathy and radiating burning pain a few days before the typical skin rash appears. Upper abdominal pain, which can be reproduced by pressure on the lower costal margin, may be caused by costochondritis or lesions of the intercostal nerves [12]. Regardless of the exact pathomechanism, the diagnosis requires clinical suspicion. Complete neurological and rheumatological examination should be always performed in these patients.
Organic Biliary Diseases
Residual or de novo formed common bile duct stones are the most common organic biliary causes of PCS. After cholecystectomy bile duct stones can occur in 5-15% of the patients depending on the population studied, whether operative or preoperative cholangiography was applied and the period of the follow-up [13]. Although retained bile duct stones are far more frequent, some stones are clearly formed (de novo) in the common bile duct [14]. Pathological elevation of liver enzymes (bilirubin and alkaline phosphatase) and a dilated common bile duct (CBD) can predict the presence of stones in the majority of cholecystectomized patients. In contrast, the absence of these clinical manifestations has a 95% negative predictive value for choledocholithiasis [15]. Magnetic resonance cholangiopancreatography (MRCP) is the first choice of diagnostic method to demonstrate CBD stones in these patients. In contrast, ERCP enables therapeutic intervention, such as endoscopic sphincterotomy and immediate stone extraction at the time of diagnosis [15]. Benign postoperative bile duct strictures are infrequent causes of PCS, and the majority of such strictures are initiated by accidental surgical trauma during cholecystectomy. While the incidence of duct injuries during open cholecystectomy was around 0.1%, recent reports suggested that the laparoscopic approach increases the frequency by ten times [16]. Commonly observed symptoms caused by bile duct strictures are fever, chills, and jaundice that are the characteristic signs of recurrent cholangitis [24]. ERCP and endoscopic biliary multiple plastic stenting after balloon dilatation can provide good and long-term biliary drainage in the majority of patients [17]. Benign or malignant tumors of the Vater papilla and the periampullary area can mimic symptoms related to a PCS, such as biliary colic and jaundice. The villous adenoma and the adenocarcinoma of the Vater papilla are represented in 5% and 0.2% of all gastrointestinal tumors [18]. ERCP is the most accurate diagnostic test since it provides direct visualization of the papilla of Vater with an access for biopsy and endoscopic papillectomy [19]. Choledochal cyst is a cystic dilatation of the common bile duct and is a rather rare condition. It can be classified into three types: (I) the segmental cystic dilatation of the common bile duct, (II) the solitary common bile duct diverticulum arising laterally, (III) the dilatation of the intra-duodenal portion of the common bile duct (choledochocele). It can be associated with the anomalous connection of the pancreatic and biliary duct (ACPBD), which may be demonstrated by ERCP, MRCP or by endoscopic ultrasonography. ACPBD can be visualized as a long common channel and a high connection between the pancreas and bile duct outside of the sphincter zone. The majority of patients with choledochal cysts are asymptomatic, but they may be presented with abdominal pain, nausea, vomiting, biliary colic, and jaundice. Gallstones and pancreatitis have been associated with this entity in 25 and 30% of the cases. There is an increased risk of development of cholangiocarcinoma within the cyst and also for gallbladder carcinoma due to pancreaticobiliary reflux of the pancreatic juice that must be taken into consideration during the follow-up. ERCP and endoscopic manometry seem to be useful in clarifying the pathophysiology of symptomatic choledochocele and ACPBD [20-23]. Several reports suggested that juxtapapillary diverticulum (JPD) might cause symptoms or diseases of the biliary and pancreatic duct. It has been proved, that the incidence of cholangitis and common bile duct stones were increased in patients with JPD, but there was no similar relationship between the gallbladder stones and JPD [24]. Common bile duct stones associated with JPD are usually pigment stones, which are thought to be associated with infections and stasis. In patients with JPD endoscopic manometry usually demonstrated decreased SO baseline pressure, which may be responsible for the increased risk of ascending cholangitis, but the compression of the distal bile duct by the distended diverticulum may cause obstructive symptoms as well [25]. Several authors have suggested that the cystic duct stump or gallbladder remnant left behind after cholecystectomy; so-called cystic duct stump may be responsible for PCS. Cystic duct syndrome (CDS) described in 1950 by Garlock in cholecystectomized patients with recurrent cholangitis [26]. Since the majority of their patients had common bile duct stones, they were convinced that the cystic duct remnant can form calculi, which are responsible for the symptoms. Ten years later, Glenn F. suggested, that’s a long cystic duct remnant can be a sole cause of postcholecystectomy pain, and indicated a satisfactory outcome after the operative removal of the cystic duct stump [27]. Unfortunately, in controlled studies no significant difference was found between symptomatic and asymptomatic cholecystectomized subjects in the frequency of cystic duct remnant [28]. Therefore, CDS should not be considered as a reliable cause of PCS.
Functional Extrabiliary Causes
It is obvious that irritable bowel syndrome (IBS) may occur after cholecystectomy, and, therefore, dyspeptic symptoms in patients with PCS may be caused by altered gut motility. Additionally, one paper has been shown a strong correlation between the presence of IBS and SO motility disorders [29]. RUQ pain can be also evoked by balloon distension in the upper gut as well as in the right-sided colon [30]. Altered antroduodenal motility, antroduodenal dyscoordination, and even duodenal wall spasm have been documented after cholecystectomy in patients with PCS [31]. Since there is a wellknown synchronization between the SO motility and the fasting phases of the duodenal motor activity), therefore, malfunction of the duodenal pace- maker may be one possible pathophysiological factor in the development of PCS. As a coincidence or as a consequence pathologically increased amount of duodenogastric bile reflux has been demonstrated after cholecystectomy, and also in association with PCS [32]. Although the prevalence of antral gastritis after cholecystectomy is significantly increased, probably caused by bile acids, but the role of the coexistent Helicobacter pylori infection is uncertain since the results are controversial [33]. Gastroesophageal reflux disease may also be exacerbated in patients with PCS and associated with a significant fall in the lower oesophageal sphincter pressure and a higher rate of bile reflux into the esophagus. Enhanced colon motility has been evoked after administration of exogenous CCK in patients with IBS, which might be responsible for some abdominal complaints after feeding. Finally, after cholecystectomy the pattern of the biliary excretion is also changed, and bile acids may induce an exaggerated motility and chronic minimal inflammatory response of the colon [34]. Psychosocial status may be an important factor too, for they can influence the threshold of the patient for seeking medical advice. Although there is a clear association between the Prevalence of functional gastrointestinal diseases and some psychiatric disorders such as psychosocial problems, anxiety syndrome, panic disorder and sexual victimization, but no specific psychiatric profile characterizes patients with PCS [35]. Altered pain perception and increased pain sensitivity might also have an influence on the development of functional abdominal pain and PCS [36].
Functional Biliary Causes
Sphincter of Oddi dysfunction (SOD), although extensively studied, is an uncommon clinical entity, accounts for only 1.5 – 3% of PCS patients [37]. Episodes of moderate to severe steady pain located in the epigastrium or the RUQ recurring more than three months are the most common presenting symptoms in patients with SOD. The RUQ pain may radiate to the epigastrium or the back, starts 15-30 min after a meal, lasts more than 60 minutes, and evoked by fatty food. The clinical suspicion is enhanced by the transient elevations of liver enzymes (AST/ALT/AP), and a dilated common bile or pancreatic duct in an absence of an obvious structural cause [38]. On the basis of the pathogenic mechanism SO dysfunction’s (SODs) can be further classified into two groups as follows. SO stenosis is a structural narrowing of the SO, which may be caused by inflammation, fibrosis or smooth muscle hypertrophy; and SO dyskinesia, which is a functional motility disorder of the SO, and thought to be caused by neuromuscular incoordination [39]. Traditionally, endoscopic retrograde cholangiopancreatography (ERCP) played a major role in the diagnostic evaluation of patients with SOD. The diagnostic cholangiographic criteria for SOD are dilated common bile duct (> 12 mm) and delayed contrast drainage time (> 45 min) without stone or obvious organic cause (Figure 1). Unfortunately, these ERCP findings prove to be more prevalent in patients with SO stenosis than in SO dyskinesia [40]. A useful way of classifying of these patients is to divide them into the following three groups by clinical presentation, laboratory results, and ERCP findings. SOD group I patients present with abdominal pain, abnormally elevated liver or pancreatic enzymes, dilated common bile or main pancreatic duct and delayed contrast drainage time. SOD group II patients have abdominal pain and at least one more above mentioned criteria. SOD group III patients have only abdominal pain and none of the other criteria. Since the risk of post- ERCP pancreatitis is relatively high in patients having SOD, recently we suggested that non-invasive classification of SOD. Abdominal ultrasound, endoscopic ultrasonography or MRCP (common bile duct anatomy and diameter) and hepatobiliary scintigraphy (delayed isotope contrast drainage time) may be useful before the clinical decision of further invasive diagnostic investigations [41] (Figures 2 and 3). The introduction of the endoscopic SO manometry into the clinical practice regarded as a major step both in the exploration of the physiological motor function of the human SO and also in the diagnosis of SOD [42,43]. Several motility abnormalities have been described, such as increased baseline pressure, increased the amplitude of phasic contractions, increased number of retrograde contractions, increased frequency of phasic contractions, and increased the pressure of the common bile duct and paradoxical response to cholecystokinin administration [44]. The manometrical evidence of an elevated SO basal pressure proved to be the most important diagnostic finding. Elevated basal pressure (manometric features of SO stenosis) had an excellent reproducibility [45,46] and regarded as a reliable predictor of the satisfactory therapeutic outcome in those patients, who were scheduled for endoscopic sphincterotomy [47]. In patients with SOD biliary type I or SO stenosis documented by ESOM, an endoscopic sphincterotomy are the therapy of choice since significant long-term symptomatic relief could be achieved [41]. In contrast, in a recent randomized trial, no significant differences in the symptomatic outcome could be demonstrated in between abnormal and normal SO manometry groups in those patients with SO dyskinesia (SOD biliary type III) [48]. Reduction of the elevated basal pressure and an acceleration of the trans papillary bile flow following administration of amyl nitrite demonstrated with endoscopic manometry and quantitative hepatobiliary scintigraphy, respectively, suggest functional dyskinesia rather than organic stenosis of the SO [49,50] (Figure 4). The reported frequencies of abnormal SO manometry in patients of SOD biliary group I, II and III were 85.7%, 55.1% and 28.1% respectively [51]. Manometric abnormalities of the SO were not only demonstrated in PCS but also in patients with intact gallbladder and acalculous biliary pain, which strongly support the evidence that SO dyskinesia had to exist before cholecystectomy [52]. Conclusively removal of the gallbladder without endoscopic sphincterotomy produces a high probability of the development of PCS in these patients by losing the reservoir and pressure equalizer function of the GB [53]. Cholecystokinin (CCK) is a potent inhibitor of SO basal and phasic activity. The release of CCK after food intake is the most important factor in the inhibition of the SO during the postprandial period, allowing the movement of an increased bile flow across the SO with decreased resistance. After intravenous administration of CCK, the inhibitory effect lasts 2-6 minutes, and afterward the SO activity returns to normal [54]. The mechanism of this dominant inhibitory action of CCK on the human SO appears to be via stimulation of nitric oxide and vasoactive intestinal polypeptide mediated non-adrenergic-noncholinergic (NANC) inhibitory neurons, overriding the direct smooth muscle stimulatory effect of CCK. The imbalance between the dominant inhibitory effect and the direct smooth muscle excitatory action of CCK on the SO (denervation pattern) in patients with SOD may lead to inappropriate spasm i.e. the paradoxical response of the SO after CCK administration [55]. It has also been suggested that the lack of inhibitory action of the CCK on the SO can be the consequence of denervation of the SO and cholecystectomy might be responsible for this, by directly dissecting the cholecysto-sphincteric nerve bundles. Although in a few patients with PCS, the reproduction of biliary pain was also observed at the time of paradoxical SO spasm during CCK administration, the frequency of this phenomenon is rather low for being an exclusive pathomechanism or a reliable provocation test [56]. There are early observations, which demonstrated that experimental distension of the common bile duct induces localized RUQ or epigastrial pain accompanied by nausea and vomiting [57]. Many patients with PCS have experienced the reproduction of biliary-type pain upon the injection of a small amount of contrast material into the common bile duct during diagnostic ERCP, thought to be caused by hypersensitivity of the biliary tract. Sometimes the cannulation of the papilla of Vater can be painful. ERCP filling pain proved to be highly reproducible regardless whether contrast material or physiologic saline has been injected. It was also claimed, that the pain had vanished after the aspiration of the contrast material. Simultaneous manometric measurements in the common bile duct revealed a marked pressure rise at the time of the evoked pain [58]. Unfortunately, controlled studies with endoscopic sphincter of Oddi manometry failed to show any correlation between positive ERCP filling pain test and manometric diagnosis of SOD [59]. Although pain during ERCP proved to have no diagnostic value for SOD, it can be regarded as a good indicator of an oversensitive biliary tract, which has a low compliance to volume changes and might act as a pain trigger zone. Although the presence of opioid receptors in the SO area is confirmed by immuno- histochemical studies, but their exact physiological role has not been established yet [60]. It is a well-known fact that morphine sulfate (MS) has a stimulatory effect on the human SO. Very small doses of MS (2.5 ug/kg) increases the frequency and the amplitude of phasic contractions, whereas larger doses can cause SO spasm with a substantial elevation of the SO basal pressure. The effect of MS can be antagonized by naloxone, but not by atropine [61]. This phenomenon suggests a direct smooth muscle stimulatory effect of MS by facilitating the Ca++ influx through the voltage dependent or receptor operated calcium channels. In patients with PCS, a marked rise in CBD pressure was demonstrated using endoscopic manometry during MS administration, which was associated with biliary pain [62]. Provocation tests based on MS administration, such as the Debray and the Nardi test have been used for several years in the evaluation of patients with SO dyskinesia [63,64], but the diagnostic usefulness of these tests has been criticized because of their low specificity and sensitivity [65]. In those patients with biliary pain and prolonged SO spasm due to the MS administration, a significant elevation of the CBD pressure and the stoppage of the bile flow over the SO can be demonstrated using intraoperative and endoscopic SO manometry and quantitative hepatobiliary scintigraphy. Therefore, MS augmentation of these diagnostic tests may improve the sensitivity and specificity of SO provocation tests [66,67] (Figure 5). It has been also proved, that the frequencies of abnormal SO manometric results were significantly higher in those patients with positive Nardi provocation test [68]. Finally, it can be hypothesized, that there is a subgroup of patients with PCS, who have exaggerated SO contractile response after MS administration, which is not always accompanied by basal motility disturbances on the SO manometry. Therefore, it seems likely, that factors influencing motor responses to morphine provocation tests are not related either to those which determine the basal SO motility or the responses to intravenous CCK [69].
Conclusions
Obviously, PCS symptoms could have several pathophysiological origins, but only the minority of PCS is caused by an organic disease of the gastrointestinal tract. In a substantial number of patients, no organic disease can be found as a cause of biliary type pain after cholecystectomy. Many patients in whom no organic abnormality can be found suffer from motility disorders of the biliary tract and the upper gut. Endoscopic SO manometry has become a valuable tool for clinical and experimental studies of the SO. After the introduction of SO manometry into the clinical practice, it has become obvious that although SOD exists and it is one important cause of PCS, the prevalence much lower than it had been originally expected. Several factors may be responsible for this discrepancy. One possible explanation is that the SO motor disorder may be intermittent so that abnormalities might be missed if the registration is made during an asymptomatic and quiescent period. Furthermore, the SO motor activity varies between the different phases of intestinal migrating motor complex, which may result in significant variations in the SO manometric findings. ESOM reproducibility is variable in SO dyskinesia patients regardless of the manometric parameter measured such as phasic contraction activity or SO basal pressure. Therefore studies searching for new aspects of motility disorders are extremely important [70]. Non-invasive methods such as MRCP and hepatobiliary scintigraphy must be preferred to classification of SOD patients, since ERCP and ESOM has a high inherent risk of post-ERCP pancreatitis [71]. If ERCP and endoscopic sphincterotomy are the therapy of choice, prophylactic pancreatic stents should be always applied to prevent complications [72]. As we already discussed, there are other possible aspects of PCS originate from the SO such as a hypersensitivity of the biliary tract and an exaggerated response to MS, which could not be revealed by SO manometry. It also seems to be evidence that altered gut motility, such as antroduodenal dyscoordination and IBS can be the pathophysiological explanation of the symptoms in patients with PCS, as a sole or coexisting condition. The variation of the individual pain sensitivity, as well as the psychosocial disturbances, might also influence the development of PCS in a given patient. Thus, further studies are needed to explore the significance and role of the possible pathogenic factors and find the optimal management of these patients.