Abstract
The continued need to develop less invasive alternatives to surgical and radiologic interventions has driven the development of endoscopic ultrasound (EUS)-guided treatments. These include EUS-guided drainage of pancreatic fluid collections, EUS-guided necrosectomy, EUS-guided cholangiography and biliary drainage, EUS-guided pancreatography and pancreatic duct drainage, EUS-guided gallbladder drainage, EUS-guided drainage of abdominal and pelvic fluid collections, EUS-guided celiac plexus block and celiac plexus neurolysis, EUS-guided pancreatic cyst ablation, EUS-guided vascular interventions, EUS-guided delivery of antitumoral agents and EUS-guided fiducial placement and brachytherapy. However these procedures are technically challenging and require expertise in both EUS and interventional endoscopy, such as endoscopic retrograde cholangiopancreatography and gastrointestinal stenting. We undertook a systematic review to record the entire body of literature accumulated over the past 2 decades on EUS-guided interventions with the objective of performing a critical appraisal of published articles, based on the classification of studies according to levels of evidence, in order to assess the scientific progress made in this field.
Keywords: Endoscopic ultrasound, Pseudocyst drainage, Necrosectomy, Celiac plexus neurolysis, Levels of evidence, Fine needle injection
Core tip: Endoscopic ultrasound (EUS)-guided interventions have become increasingly popular. The advantages of EUS guidance over percutaneous and surgical routes are well established for pseudocyst drainage and celiac plexus neurolysis as they have been assessed in high level of evidence literature. However, for other very fashionable procedures such as bile duct and pancreatic duct drainage, the role of EUS guidance has only been reported as preliminary studies in limited number of patients. The level of evidence of each EUS-guided intervention is accurately reported in this review in order to provide the readers with the current status of knowledge and allow insights into potential future direction of research.
INTRODUCTION
Endoscopic ultrasound (EUS) has evolved from a purely diagnostic imaging modality to an interventional procedure that provides a minimally invasive alternative to interventional radiologic and surgical techniques.
Several innovative techniques now constitute the portfolio of interventional EUS, such as EUS-guided drainage (GD) of pancreatic fluid collections (PFCs), EUS-guided necrosectomy, EUS-guided cholangiography and biliary drainage (BD), EUS-guided pancreatography and pancreatic duct drainage (PDD), EUS-guided gallbladder drainage, EUS-GD of abdominal and pelvic fluid collections, EUS-guided celiac plexus block (CPB) and celiac plexus neurolysis (CPN), EUS-guided pancreatic cyst ablation, EUS-guided delivery of antitumoral agents and EUS-guided fiducial placement, brachytherapy and EUS-guided vascular interventions. However, EUS-guided treatments are technically challenging and require expertise in both standard diagnostic EUS and endoscopic interventional procedures, such as endoscopic retrograde cholangiopancreatography (ERCP) and gastrointestinal stenting.
For such a reason, it is important that we carefully monitor the results of our EUS-guided treatments in order to either implement them in clinical practice or abandon/thoroughly revise them. Evidence based medicine is known as a strategic tool to do so.
Following our previous systematic analysis of the levels of evidence (LE) of the EUS literature[1-4], we reviewed the entire body of literature accumulated over the past 2 decades on EUS-guided treatments. Our main aim was to critically appraise the published articles, based on the classification of studies according to LE, in order to assess the scientific progress made in this field.
All articles relevant to EUS-guided interventional procedures were extracted up to September 2013. Moreover, the references of reviewed articles were scrutinized to obtain any other reference that eluded the primary search.
This review is based on the results of searches carried out in PubMed and Google Scholar.Original research articles [randomized controlled trials (RCT), prospective studies (PS) and retrospective studies (RS)], meta-analyses, systematic reviews and surveys pertinent to EUS-guided interventional procedures were included.
Studies enrolling up to 10 patients were categorized as case series. We also included letters and case reports describing recent, innovative or original EUS-guided treatments. Commentaries, non-English language articles, congress proceedings and abstracts, and articles in which EUS did not represent the principal matter were not included.
In regard to data collection, priority was assigned to the study subject, design and methods, the type and year of publication and the number of patients enrolled. The content of each study was further analyzed to identify relevant clinical issues. In particular, when the same group of patients from the same institution was included in two consecutive papers (e.g., preliminary study and final results study), we included only the data from the most recent one to avoid duplicated results.
Levels of evidence were stratified according to the North of England evidence-based guidelines[5,6]. LE Ia: Evidence obtained from meta-analysis of RCTs; LE Ib: Evidence obtained from at least one RCT; LE IIa: Evidence obtained from at least one well designed controlled study without randomization; LE IIb: Evidence obtained from at least one other type of well-designed quasi-experimental study; LE III: Evidence obtained from well-designed non-experimental descriptive studies such as comparative studies, correlation studies, and case studies; LE IV: Evidence obtained from expert committee reports or opinions, or clinical experiences of respected authorities.
A total of 381 pertinent articles were finally included for the purpose of this systematic review. Published research focused primarily on EUS-guided cholangiography and biliary drainage (85 studies), followed by EUS-GD of pancreatic fluid collections (84 studies), EUS-guided CPN or CPB (52 studies), EUS-guided tumor ablation (34 studies), EUS-guided ethanol ablation (28 studies), EUS-guided fiducial placement (26 studies), EUS-guided vascular interventions (23 studies), EUS-guided necrosectomy (20 studies), EUS-guided pancreatography and pancreatic duct drainage (15 studies), EUS-guided gallbladder drainage (7 studies) and EUS-GD of abdominal (non-peripancreatic) and pelvic collections (7 studies). A detailed classification of the studies according to the subclasses and the corresponding LE is presented in Table 1. As expected, we identified a predominance of LE III and IV articles in all types of EUS-guided treatments, reflecting the relative novelty of these techniques. Nevertheless, a fair number of high LE articles (LE Ia and Ib) were identified for EUS-GD of pancreatic fluid collections and EUS-guided CPN, forming a solid base of evidence for these established indications. On the other hand, novel therapeutic applications, such as EUS-guided cholangiography and biliary drainage and EUS-guided tumor ablation, still lack relevant clinical data and should still be considered strictly investigational. A focused description of all forms of EUS-guided treatment is given below, in a schematic format.
Table 1.
Level of evidence | Ia | Ib | IIa | IIb | III | IV | Total |
EUS-GD of pancreatic fluid collections | 1 | 5 | 0 | 16 | 42 | 20 | 84 |
EUS-guided necrosectomy | 1 | 1 | 0 | 0 | 15 | 3 | 20 |
EUS-guided cholangiography and biliary drainage | 0 | 1 | 0 | 7 | 37 | 40 | 85 |
EUS-guided pancreatography and pancreatic duct drainage | 0 | 0 | 0 | 0 | 9 | 6 | 15 |
EUS-guided gallbladder drainage | 0 | 1 | 0 | 3 | 1 | 2 | 7 |
EUS-GD of abdominal (non-peripancreatic) and pelvic collections | 0 | 0 | 0 | 2 | 3 | 2 | 7 |
EUS-guided Celiac Plexus Neurolysis or Block | 4 | 7 | 1 | 5 | 16 | 19 | 52 |
EUS-guided ethanol ablation | 0 | 1 | 0 | 5 | 13 | 9 | 28 |
EUS-guided tumor ablation | 0 | 0 | 0 | 9 | 4 | 21 | 34 |
EUS-guided fiducial placement | 0 | 0 | 0 | 2 | 10 | 14 | 26 |
EUS-guided vascular intervention | 0 | 1 | 0 | 2 | 15 | 5 | 23 |
Total | 6 | 17 | 1 | 51 | 165 | 141 | 381 |
EUS-GD: Endoscopic ultrasound-guided drainage.
EUS-GUIDED DRAINAGE OF PFCs
EUS-GD is regarded as an established technique for the treatment of PFCs. Up to now, the reported evidence pertains about 2115 patients enrolled in safety and efficacy studies overall[7-64]. Mean technical and clinical success rates reported in series with more than 10 patients were 97% and 90%, respectively and mean overall recurrence rate was 8%[8-64] (Table 2). The mean overall complication rate was 17% including bleeding (69 cases), superinfection (52 cases), stents migration that required endoscopic reintervention (51 cases), perforation treated with surgery (27 cases) and pneumoperitoneum treated conservatively (18 cases). However, only 5 cases of death were deemed to be procedure related[8-64].
Table 2.
Ref. | Design | Cases | Technical success | Clinical success | Recurrence | Complications1 |
Binmoeller et al[8] | RS | 27 | 93% | 78% | 22% | 52% |
Pfaffenbach et al[9] | PS | 11 | 91% | 82% | 18% | None |
Giovannini et al[10] | PS | 35 | 100% | 89% | 9% | 3% |
Norton et al[11] | RS | 14 | 93% | 93% | 23% | 14% |
Vosoghi et al[12] | RS | 14 | 100% | 93% | 7% | 7% |
Enya et al[13] | PS | 13 | 100% | 85% | 0% | None |
Hookey et al[14] | RS | 32 | 96% | 93% | 12% | 11% |
Krüger et al[15] | PS | 35 | 94% | 88% | 12% | 33% |
Azar et al[16] | RS | 23 | 91% | 82% | 18% | 4% |
Antillon et al[17] | PS | 33 | 94% | 87% | 4% | 15% |
Kahaleh et al[18] | PS | 46 | 100% | 93% | NR | 19% |
Ahlawat et al[19] | PS | 11 | 100% | 82% | 18% | 18% |
Arvanitakis et al[20] | RCT | 46 | 100% | 94% | 11% | 22% |
Lopes et al[21] | RS | 51 | 94% | 84% | 17% | 25% |
Varadarajulu et al[22] | PS | 23 | 100% | 95% | 0% | None |
Lopes et al[23] | PS | 31 | 100% | 94% | 19% | 26% |
Ardengh et al[24] | PS | 77 | 94% | 91% | 11% | 6% |
Varadarajulu et al[25] | RS | 20 | 100% | 95% | NR | None |
Varadarajulu et al[26] | RCT | 24 | 100% | 96% | NR | 4% |
Varadarajulu et al[27] | PS | 60 | 95% | 93% | 4% | 2% |
Barthet et al[28] | PS | 28 | 100% | 89% | NR | 25% |
Talreja et al[29] | PS | 18 | 100% | 95% | 0% | 44% |
Park et al[30] | RCT | 39 | 95% | 95% | 6% | 7% |
Yasuda et al[31] | RS | 26 | 92% | 87% | 17% | None |
Itoi et al[32] | PS | 13 | 100% | 100% | 0% | None |
Varadarajulu et al[33] | PS | 10 | 100% | 90% | 0% | None |
Ang et al[34] | PS | 10 | 100% | 100% | 0% | 10% |
Ahn et al[35] | RS | 47 | 98% | 100% | 11% | 11% |
Jazrawi et al[36] | RS | 10 | 100% | 100% | 10% | None |
Sadik et al[37] | PS | 26 | 100% | 88% | 4% | 15% |
Will et al[38] | PS | 132 | 97% | 96% | 15% | 29% |
Seicean et al[39] | PS | 24 | 83% | 79% | 0% | 17% |
Heinzow et al[40] | RS | 42 | 88% | 78% | 21% | 21% |
Varadarajulu et al[41] | PS | 148 | 100% | 99% | NR | 5% |
Varadarajulu et al[42] | RS | 602 | 100% | 69% | 0% | 8% |
Varadarajulu et al[43] | RS | 20 | 100% | 100% | 5% | None |
Zheng et al[44] | PS | 14 | 90% | 90% | 0% | 19% |
Voermans et al[45] | RCT | 52 | 100% | 82% | 9% | 11% |
Mangiavillano et al[46] | PS | 21 | 86% | 81% | 14% | 5% |
Seewald et al[47] | RS | 80 | 97% | 83% | 13% | 26% |
Itoi et al[48] | RS | 15 | 100% | 100% | 0% | 6% |
Puri et al[49] | PS | 40 | 100% | 97% | 2% | 7% |
Fabbri et al[50] | PS | 20 | 100% | 95% | 5% | 15% |
Rasmussen et al[51] | RS | 22 | 86% | 86% | 18% | 18% |
Khashab et al[52] | RS | 10 | 100% | 100% | 0% | None |
Penn et al[53] | PS | 20 | 100% | 85% | 18% | 15% |
Weilert et al[54] | PS | 18 | 100% | 78% | NR | 33% |
Rana et al[55] | RS | 202 | 100% | 100% | 0% | 5% |
Binmoeller et al[56] | RS | 14 | 100% | 79% | NR | 21% |
Nan et al[57] | RS | 21 | 100% | 100% | NR | 5% |
Kato et al[58] | RS | 67 | 88% | 83% | 15% | 1% |
Künzli et al[59] | RS | 108 | 97% | 84% | 18% | 20% |
Siddiqui et al[60] | RS | 88 | 99% | 79% | 3% | 30% |
Rische et al[61] | RS | 18 | 100% | 94% | 6% | 33% |
Varadarajulu et al[62] | RCT | 20 | 100% | 95% | 0% | None |
Total | 55 studies | 1867 | 97% (83%-100%) | 90% (69%-100%) | 8% (0%-23%) | 17% (0%-52%) |
Complications include: early and late, procedural and stent related;
Only patients with walled-off pancreatic necrosis. RCT: Randomized controlled trial; PS: Prospective study; RS: Retrospective study; NR: Not reported.
EUS vs surgical drainage
A recent RCT[62] comparing EUS and surgery for pancreatic pseudocyst drainage, showed no pseudocyst recurrence during the follow-up in the former group and no evidence that surgical cystogastrostomy was superior to EUS. Moreover, EUS treatment was associated with shorter hospital stay, better physical and mental health of patients, and lower costs. EUS-GD of PFCs is not inferior to surgical drainage in terms of safety and efficacy (LE Ib).
EUS vs blind endoscopic drainage
Meta-analysis of EUS-GD of PFCs showed superior technical and treatment success rates and more favorable safety profiles than traditional non-EUS guided drainage[65] (LE Ia).
Varadarajulu et al[26] published the first RCT, randomizing 30 patients to undergo either EUS-GD or endoscopic conventional transmural drainage (ECTD). All patients assigned to EUS underwent successful drainage (100%), while the procedure was technically successful in only 5/15 patients (33%) assigned to ECTD. All 10 patients who failed drainage by ECTD underwent successful drainage of the PFC on a crossover to EUS. Major procedure-related bleeding was encountered in 2 patients in whom ECTD was performed (LE Ib). Park et al[30] enrolled 60 patients in a RCT with the same design as above. Technical success of the drainage was significantly higher in the EUS group (94%) than in the ECTD group (72%) (P = 0.039) in intention-to-treat analysis. In 8 cases where ECTD had failed because of non-bulging PFCs, crossover to EUS-GD was always successful. Complications occurred in 7% of the EUS group vs 10% of the ECTD group (P = NS). During follow-up, PFC resolution was achieved in 97% in the EUS group and in 91% in the ECTD group (P = NS) (LE Ib). EUS-GD of PFCs has superior technical and clinical outcomes compared to blind endoscopic drainage (LE Ia).
Forward view vs linear scanning EUS
EUS-GD of PFCs is commonly performed with linear scanning echoendoscopes, whose tangential approach to PFCs may be challenging for operators. Theoretically, technical difficulties might be overcome using a forward-viewing echoendoscope which allows a straight approach to PFCs. However, a recent RCT[45] comparing the performance of linear vs forward-viewing echoendoscopes in draining PFCs failed to demonstrate any significant difference in technical success, mean procedure time, safety or efficacy between the two types of echoendoscopes.
The use of forward-viewing echoendoscope for EUS-guided drainage of PFCs does not confer any significant advantage in terms of safety and efficacy compared to the use of linear scanning echoendoscope (LE Ib).
Timing of stent removal
In order to evaluate the incidence of PFCs recurrence after successful EUS-GD, 28 patients were randomized either to stent removal (n = 13) or to stent left in place (n = 15) and were followed up for a median period of 14 months. PFCs recurrence was observed in 5 patients in the stent retrieval group, as opposed to none in the other group (P = 0.013)[20]. After successful EUS-GD of PFCs, stent retrieval is associated with higher recurrence rate than leaving stent in place (LE Ib).
Nasocystic drainage to maintain patency: Siddiqui et al[60] evaluated in a RS EUS-guided nasocystic drainage alongside transmural stents in PFCs with viscous solid debris. Association with the nasocystic drainage resulted in lower stent occlusion rate and better short-term clinical outcomes compared to those patients who underwent standard EUS-GD. The placement of a nasocystic drainage may increase the clinical success rate, especially in PFCs containing abundant debris (LE III).
Multiple transluminal gateway technique: Varadarajulu et al[42], showed that drainage of necrotic PFCs with multiple instead of a single transmural access, placing multiple stents and a nasocystic drainage in each tract, led to better long-term clinical outcomes. Multiple instead of single transmural points of access allow better drainage of the necrotic contents and improve treatment success (LE III).
Use of covered self-expandable metal stents: Covered self-expandable metal stents have been recently tested for drainage of PFCs and walled-off pancreatic necrosis with the intent of creating a larger fistula compared to plastic stents. Increased success rate and reduced time to resolution were shown in case series and pilot studies[48,50,53,54] (LE IIb). However stents designed for other indications were used. Recently, new devices have been introduced for the purpose of PFCs drainage, provided with larger diameter and antimigration features such as the “NAGI” stent (Taewoong-Medical Co, Seoul, South Korea) or the “AXIOS” stent (Xlumena Inc., Mountain View, California, United States)[66,67].
A case series[68] described the use of the AXIOS stent in 9 patients who underwent EUS-guided drainage of PFCs. The technical success rate was 89% (8/9) due to one failure of the delivery system and all patients had successful outcome achieving complete PFC resolution. One patient developed a tension pneumothorax immediately after transesophageal drainage. No migrations were reported, and all stents were removed easily. Only one patient presented a recurrence 4 wk after stent removal. Use of covered self-expandable metal stents seems to improve the clinical outcome in these patients; however, larger studies comparing metal and plastic stents are warranted (LE IIb).
EUS-GUIDED NECROSECTOMY
Debridement of pancreatic necrosis has traditionally been managed surgically. In recent years, EUS-guided endoscopic necrosectomy has become an alternative.
This technique involves a transmural (transgastric or transduodenal) EUS-guided access to the necrotic area, followed by large caliber (e.g., 18 mm) balloon dilation of the tract between the collection and the gastrointestinal wall, allowing for passage of a gastroscope into the collection to visualize the necrotic material. A variety of tools, such as baskets, snares, and nets have been used to remove the necrotic tissue. EUS-guided necrosectomy has been reported in 283 published cases so far. In the published studies a median of 4 (1-35) sessions was required to achieve resolution of the necrotic collection[69]. Mean technical and clinical success rates reported were 100% and 88%, respectively; mean overall complication rate was 28% and mean overall recurrence rate was 7%[61,70-84] (Table 3). A recent RCT[78] by the Dutch Pancreatitis Study Group showed a lower rate of proinflammatory response, organ failure and major complications in patients undergoing EUS-guided necrosectomy as compared to surgical necrosectomy (LE Ib).
Table 3.
Ref. | Design | Cases | Technical success | Clinical success | Recurrence | Complications1 |
Seewald et al[70] | RS | 13 | 100% | 85% | 15% | 30% |
Charnley et al[71] | RS | 13 | 100% | 92% | 0% | None |
Voermans et al[72] | RS | 25 | 100% | 93% | 7% | 40% |
Hocke et al[73] | RS | 30 | 97% | 83% | 3% | 23% |
Schrover et al[74] | RS | 8 | 100 % | 75% | 12% | 25% |
Mathew et al[75] | RS | 6 | 100% | 100% | 0% | None |
Escourrou et al[76] | RS | 13 | 100% | 100% | 0% | 46% |
Jürgensen et al[77] | RS | 35 | 100% | 97% | 0% | 17% |
Bakker et al[78] | RCT | 10 | 100% | 100% | 20% | 40% |
Will et al[79] | RS | 18 | 100% | 100% | 11% | 17% |
Rische et al[61] | RS | 22 | 100% | 86% | 14% | 36% |
Yamamoto et al[80] | RS | 4 | 100% | 50% | NR | 25% |
Hritz et al[81] | RS | 4 | 100% | 100% | 0% | None |
Yasuda et al[82] | RS | 57 | 100% | 75% | 7% | 33% |
Ang et al[83] | RS | 8 | 100% | 87% | 13% | None |
Sarkaria et al[84] | RS | 17 | 100% | 88% | 0% | 6% |
Total | 16 studies | 283 | 100% (97%-100%) | 88% (50%-100%) | 7% (0%-20%) | 28% (0%-46%) |
Complications include: early and late, procedural and stent related. RCT: Randomized controlled trial; PS: Prospective study; RS: Retrospective study; NR: Not reported.
EUS-GUIDED CHOLANGIOGRAPHY AND BILIARY DRAINAGE
When biliary ductal access via endoscopic retrograde cholangiopancreatography (ERCP) fails, rescue measures include precut papillotomy, percutaneous transhepatic biliary drainage (PTBD), surgical bypass and EUS-guided BD. Three different EUS-guided BD approaches have been described: direct transluminal stenting via transgastric or transduodenal route, rendezvous technique passing a guidewire through an intrahepatic or extrahepatic access to the papilla, and antegrade stent placement.
EUS-guided BD has currently been performed in 1127 published cases, with mean technical and clinical success rates of 91% and 88%, respectively. However, mean overall complication rate was 26% with mortality of 0.4% (4/1127 patients)[85-113] (Table 4).
Table 4.
Ref. | Design | Cases | Technical success | Clinical success | Complications1 |
Bories et al[86] | RS | 11 | 91% | 80% | 72% |
Maranki et al[87] | RS | 49 | 84% | 80% | 18% |
Brauer et al[88] | PS | 12 | 92% | 72% | 16% |
Horaguchi et al[89] | PS | 16 | 100% | 94% | 37% |
Kim et al[90] | RS | 15 | 80% | 80% | None |
Fabbri et al[91] | PS | 16 | 75% | 75% | 8% |
Park et al[92] | RS | 57 | 96% | 89% | 47% |
Hara et al[93] | PS | 18 | 94% | 94% | 77% |
Komaki et al[94] | RS | 15 | 100% | 100% | 46% |
Ramírez-Luna et al[95] | PS | 11 | 91% | 82% | 18% |
Shah et al[96] | RS | 68 | 85% | 85% | 9% |
Iwashita et al[97] | RS | 40 | 73% | 73% | 12%2 |
Dhir et al[98] | RS | 58 | 98% | 98% | 3% |
Artifon et al[99] | RCT | 13 | 100% | 100% | 15% |
Song et al[100] | PS | 15 | 87% | 87% | 47% |
Kim et al[101] | PS | 13 | 92% | 84% | 38% |
Vila et al[102] | RS | 106 | 70% | 70% | 23% |
Horaguchi et al[103] | RS | 21 | 100% | 100% | 10% |
Hara et al[104] | PS | 18 | 94% | 89% | 27% |
Park et al[105] | PS | 45 | 91% | 87% | 11% |
Kawakubo et al[106] | RS | 14 | 100% | 100% | 14% |
Dhir et al[107] | RS | 35 | 97% | 97% | 23% |
Khashab et al[108] | RS | 35 | 94% | 91% | 14% |
Gornals et al[109] | RS | 15 | 87% | 73% | 40% |
Gupta et al[110] | RS | 240 | 99% | 87% | 35% |
Dhir et al[111] | RS | 68 | 97% | 97% | 21%3 |
Kawakubo et al[112] | RS | 64 | 95% | 95% | 42% |
Total | 27 studies | 1088 | 91% (70%-100%) | 87% (70%-100%) | 29% (3%-77%) |
Complications include: early and late, procedural- and stent-related;
2.5% mortality (1 patient );
4% mortality (3 patients). RCT: Randomized controlled trial; PS: Prospective study; RS: Retrospective study; NR: Not reported.
EUS-guided BD vs percutaneous BD
In a recent RCT 25 patients with unresectable malignant biliary obstruction and a previous failed ERCP attempt were assigned either to EUS-guided or to percutaneous transhepatic BD. The authors reported 100% technical and clinical success in both study groups, with no difference in incidence of adverse events[99] (LE Ib). Combining EUS and ERCP in the same procedure was a cost saving strategy compared to referring the patient for percutaneous transhepatic BD[109] (LE III). EUS-guided BD appears to be a valid alternative to percutaneous BD, showing similar efficacy and safety (LE Ib). However, data are still very preliminary and large RCT are needed to demonstrate whether EUS can represent a valid alternative to percutaneous route in this setting.
EUS-guided rendezvous BD vs precut papillotomy
The outcome of 58 patients undergoing EUS-guided rendezvous drainage because of bile duct obstruction, after failed selective biliary cannulation, was compared to an historical cohort of 144 patients treated with precut papillotomy. Treatment success was significantly higher for the EUS-guided rendezvous patients than for those who underwent precut papillotomy, while there was no difference in complications rate[98]. EUS-guided rendezvous drainage seems to be superior to precut papillotomy in patients with bile duct obstruction after failed ERCP (LE III).
EUS-guided rendezvous BD vs EUS-guided transluminal BD
A recent RS (33 patients) compared the outcome of two different techniques in patients who underwent a standardized approach to EUS-guided BD, with an initial attempt at using the rendezvous technique (n = 13) followed by the transluminal approach (n = 20) in case of rendezvous failure. The Authors reported that both techniques achieved the same effectiveness and safety[108]. Transluminal EUS-guided BD may represent a safe and effective alternative in case of failure of rendezvous technique (LE III).
EUS-guided transhepatic BD vs EUS-guided extrahepatic BD
EUS-guided BD can be performed either via intrahepatic (through the stomach) or via extrahepatic (through the duodenum) route. In a recent RS, despite similar technical and clinical success rate, extrahepatic access was associated with significantly shorter procedure and hospitalization time and with less complications[107] (LE III). Another multicenter RS enrolling 68 patients who underwent transluminal EUS-guided BD for malignant obstructive jaundice showed similar technical and clinical success both in patients who underwent transhepatic and extrahepatic drainage. However, transhepatic access was burdened with a significantly higher complication rate compared to the extrahepatic route (30.5% vs 9.3%, P = 0.03); multivariate analysis identified the transhepatic route as the only factor independently related to the risk of procedure-related adverse event[111] (LE III). EUS-guided BD shows similar technical and clinical success rate with both transhepatic and extrahepatic access. However, extrahepatic access seems to be safer than transhepatic access (LE III).
EUS-GUIDED PANCREATOGRAPHY AND PANCREATIC DUCT DRAINAGE
EUS-guided PDD has been reported in 248 published cases so far. They are usually indicated after failed ERCP in patients with benign conditions such as ductal stones, strictures or post-surgical stenosis[85,96,102,113-120] (Table 5).
Table 5.
Ref. | Design | Cases | Technical success | Clinical success | Complications1 |
Will et al[114] | RS | 12 | 100% (SPDD: 67%) | 50% | 43% |
Tessier et al[115] | RS | 36 | 92% (SPDD: 92%) | 69% | 55% |
Kahaleh et al[116] | RS | 13 | 100% (SPDD: 77%) | 77% | 15% |
Barkay et al[117] | RS | 21 | 86% (SPDD: 48%) | 86% | 10% |
Ergun et al[118] | RS | 20 | 100% (SPDD: 90%) | 72% | 20% |
Shah et al[96] | RS | 25 | 100% (SPDD: 86%) | 100% | 16% |
Vila et al[102] | RS | 19 | 58% (SPDD: NR) | NR | 26% |
Kurihara et al[119] | RS | 14 | 100% (SPDD: 93%) | 93% | 7% |
Fujii et al[120] | RS | 45 | 98% (SPDD: 73%) | 53% | 24% |
Total | 9 studies | 205 | 100% (58%-100%) | 74.5% (53%-100%) | 20%(7%-55%) |
Complications include: early and late, procedural and stent related. SPDD: Successful pancreatic duct drainage; RS: Retrospective study; NR: Not reported.
Outcomes of EUS-guided PDD
EUS-guided PDD is a challenging procedure and it is technically more demanding than EUS-guided BD. As a result, technical and clinical outcomes of EUS-guided PDD were less favorable than for EUS-guided BD with an overall technical success rate of 78%[96,102,113-120] (LE III). Technical failures were mainly due to difficult orientation of the echoendoscope along the axis of the pancreatic duct, inability to dilate the transmural tract because of dense fibrosis, and impossible endotherapy because of too acute angle of access to the pancreatic duct[96,102,113-120]. As a note of interest, successful ERCP was reported in some cases after EUS-guided pancreatography by needle injection of contrast medium with or without methylene-blue[96,117] (LE III). EUS-guided PDD is a challenging procedure, showing suboptimal clinical success and relevant complication rate (LE III).
Technical issues and complications
EUS-guided rendezvous technique was usually attempted first, followed by the transenteric EUS-guided PDD in case of rendezvous failure[119] (LE III). EUS-guided transenteric stenting required more dilation of the needle tract than rendezvous technique, leading to serious adverse events such as pancreatitis (4%), pancreatic juice leakage (3%), bleeding (3%), and perforation (3%)[119] (LE III). The most common site for pancreatic duct access was through the gastric body, in view of the straight and stable echoendoscope position and the ease of access to the pancreatic duct[96,102,113-120] (LE III). Plastic stents were used for EUS-guided PDD unlike metal stents. In fact, covered metal stents can block side branches leading to obstructive pancreatitis and uncovered metal stents can cause pancreatic juice leakage between the stomach and pancreas[96,102,113-120] (LE III). EUS-guided PDD via transenteric route shows higher complication rate than via rendezvous route (LE III).
EUS-GUIDED GALLBLADDER DRAINAGE
Patients with acute cholecystitis unresponsive to medical therapy, require decompression of the gallbladder if they are unsuitable for emergency surgery. Available treatments are percutaneous transhepatic gallbladder drainage and EUS-guided gallbladder drainage. The latter has been performed in 97 published cases with mean technical and clinical success rates are 98% and 98%, respectively; overall mean complication rate was 16%[48,121-134] (Table 6).
Table 6.
Ref. | Design | Cases | Technical success | Clinical success | Complications1 |
Baron et al[121] | CR | 1 | 100% | 100% | None |
Kwan et al[122] | RS | 3 | 100% | 100% | 33% |
Lee et al[123] | PS | 9 | 100% | 100% | 11% |
Takasawa et al[124] | CR | 1 | 100% | 100% | None |
Kamata et al[125] | CR | 1 | 100% | 100% | None |
Kamata et al[126] | CR | 1 | 100% | 100% | None |
Song et al[127] | PS | 8 | 100% | 100% | 37% |
Súbtil et al[128] | RS | 4 | 100% | 100% | 25% |
Itoi et al[129] | CR | 2 | 100% | 100% | None |
Jang et al[130] | PS | 15 | 100% | 100% | 13% |
Jang et al[131] | RCT | 30 | 97% | 97% | 7% |
Itoi et al[48] | RS | 5 | 100% | 100% | None |
Itoi et al[132] | CR | 1 | 100% | 100% | None |
de la Serna-Higuera et al[133] | RS | 13 | 85% | 85% | 15% |
Widmer et al[134] | RS | 3 | 100% | 100% | None |
Total | 15 studies | 97 | 100% (85%-100%) | 100% (85%-100%) | 0% (0%-37%) |
Complications include: early and late, procedural and stent related. RCT: Randomized controlled trial; PS: Prospective study; RS: Retrospective study; CR: Case report.
EUS-guided vs percutaneous gallbladder drainage
Recently a non-inferiority RCT[131] was conducted to evaluate the technical feasibility, efficacy and safety of EUS-guided vs percutaneous drainage in this setting. The authors enrolled 59 patients and reported similar technical success rate (97% vs 97%), clinical success (100% vs 96%) and rate of adverse events (7% vs 3%) in the two study groups (LE Ib).
Transgastric vs transduodenal approach
Both transgastric and transduodenal approaches have been performed to achieve EUS-guided gallbladder drainage. In a pilot study, plastic stent migration was observed in a patient 3 wk after trans-gastric drainage. The authors suggested that transduodenal approach toward the gallbladder neck could avoid plastic stent migration[127] (LE IIb). On these basis, specific lumen-apposing metal stents with large distal and proximal flares have been developed[48,130,133]. EUS-guided gallbladder drainage shows similar feasibility, efficacy and safety profiles to percutaneous drainage (LE Ib).
EUS-GUIDED DRAINAGE OF ABDOMINAL NON-PERIPANCREATIC AND PELVIC COLLECTIONS
EUS-GD represents a valid treatment of fluid collections located in anatomic regions adjacent to the gastrointestinal tract (i.e., subphrenic space, perihepatic, left lobe of the liver, proximal small bowel, left colon, perirectal space, etc.). EUS-GD of abdominal (non-peripancreatic) and pelvic collections has been performed in 120 published cases so far, with mean technical and clinical success rates of 99% and 92%, respectively[135-154] (LE IIb). Overall complication rate was 13% (Table 7). Pelvic collections may present a clinical challenge because of their location, usually surrounded by major organs and anatomic structures (urinary bladder, rectum, prostate, vagina or uterus). All published data available reported the use of a drainage catheter or plastic stents[136,146,153] (LE III). Fully covered metal stents have recently been adopted for the drainage of pelvic abscesses[154] in order to minimize the risk of peritoneal leaks, to provide a larger diameter fistula and to avoid early stent occlusion; all these characteristics were shown to increase the clinical success rate and the time to collection resolution (LE III). EUS-guided drainage represents a preferential treatment of deep-seated abdominal fluid collections (LE IIb).
Table 7.
Ref. | Design | Cases | Technical success | Clinical success | Complications1 |
Attwell et al[135] | CR | 1 | 100% | 100% | None |
Giovannini et al[136] | PS | 12 | 100% | 75% | 25% |
Seewald et al[137] | CR | 2 | 100% | 100% | None |
Seewald et al[138] | CR | 1 | 100% | 100% | None |
Kahaleh et al[139] | CR | 2 | 100% | 100% | None |
Lee et al[140] | CR | 1 | 100% | 100% | None |
Jah et al[141] | CR | 1 | 100% | 100% | None |
Shami et al[142] | RS | 5 | 100% | 100% | None |
Ang et al[143] | CR | 1 | 100% | 100% | None |
Piraka et al[144] | PS | 7 | 100% | 100% | 28% |
Noh et al[145] | PS | 3 | 100% | 100% | None |
Puri et al[146] | RS | 14 | 100% | 93% | None |
Itoi et al[147] | CR | 1 | 100% | 100% | None |
Decker et al[148] | CR | 1 | 100% | 100% | None |
Gupta et al[149] | RS | 20 | 90% | 90% | 35% |
Ulla-Rocha et al[150] | RS | 6 | 100% | 100% | None |
Varadarajulu et al[151] | CR | 1 | 100% | 100% | None |
Knuth et al[152] | CR | 1 | 100% | 100% | None |
Ramesh et al[153] | RS | 38 | 100% | 87% | None |
Luigiano et al[154] | CR | 2 | 100% | 100% | None |
Total | 20 studies | 120 | 100% (90%-100%) | 100% (75%-100%) | 0% (0%-35%) |
Complications include: early and late, procedural and stent related. PS: Prospective study; RS: Retrospective study; CR: Case report.
EUS-GUIDED CELIAC PLEXUS NEUROLYSIS AND BLOCK
CPN and CPB provide pain relief and reduces narcotic use in patients with intra-abdominal malignancies and chronic pancreatitis[155]. The injection of a neurolytic drug into the celiac plexus disrupts the signal transmission to spinal cord and central nervous system. Due to the anatomical location of the celiac plexus around the origin of the celiac trunk and the superior-mesenteric artery, EUS-CPN provides direct, real-time visualization leading to a safer approach than trans-abdominal or posterior access (Table 8).
Table 8.
Ref. | Design | Indications | Techniques | Technical success | Clinical success (pain relief) | Complications |
Wiersema et al[167] | RS | PC (n = 25) | CPN | 100% | 79%-88% | 4 transient diarrhea |
Metastases (n = 5) | ||||||
Gress et al[163] | RCT | CP (n = 10) | EUS-guided | 100% | 50% | None |
CP (n = 8) | CT-guided | 25% | ||||
Gunaratnam et al[168] | PS | PC (n = 58) | CPN | 100% | 78% | 5 transient abdominal pain |
Gress et al[169] | PS | CP (n = 90) | CPB | 100% | 55% | 3 diarrhea |
Tran et al[170] | RS | PC (n = 10) | CPN | 100% | 70% | NR |
Ramirez-Luna et al[171] | RS | PC (n = 11) | CPN | 100% | 72.20% | None |
Levy et al[172] | RS | PC (n = 18) | CGN (n = 17) | NR | 16/17 (94) | 12 hypotension |
CGB (n = 1) | 0/1 (0) | 6 diarrhea | ||||
CP (n = 18) | CGN (n = 5) | NR | 4/5 (80) | |||
CGB (n = 13) | 5/13 (38) | |||||
O'Toole et al[173] | RS | PC (n = 2) | CPB (n = 189) | NR | NR | 2 post-procedural pain |
CP (n = 187) | 1 retroperitoneal abscess | |||||
PC (n = 21) | CPN (n = 31) | NR | NR | 1 hypotension | ||
CP (n = 10) | ||||||
Santosh et al[164] | RCT | CP (n = 27) | EUS-CPB | 100% | 70% | 2 diarrhea |
CP (n = 29) | Percutaneous-CPB | - | 30% | |||
Leblanc et al[165] | RCT | CP (n = 23) | CPB (central) | 100% | 15/23 (65) | None |
CP (n = 27) | CPB (bilateral) | 16/27 (59) | ||||
Sahai et al[174] | RS | PC (n = 34)/CP (n = 37) | Central CPN | 100% | 45.90% | 1 adrenal artery bleeding |
PC (n = 45)/CP (n = 44) | Bilateral CPN | 70.40% | ||||
Sakamoto et al[175] | PS | PC (n = 67) | 34CPN | 100% | 72%-79% | None |
33 BPN | 96.90% | 19%-78% | ||||
Wyse et al[158] | RCT | PC (n = 96) | 48 CPN | 100% | 60.70% | None |
48 control | - | - | ||||
LeBlanc et al[160] | RCT | PC (n = 29) | CPB (central) | 100% | 20/29 (69) | None |
PC (n = 21) | CPB (bilateral) | 17/21 (81) | ||||
Téllez-Ávila et al[161] | RS | PC (n = 53) | Central (n = 21) | NR | 10/21 (48) | None |
Bilateral (n = 32) | 18/32 (56) | |||||
Iwata et al[176] | RS | PC (n = 47) | CPN | 100% | 68.10% | NR |
Ascunce et al[177] | RS | PC (n = 64) | CPN | 100% | 50% | 1 hypotension |
Stevens et al[166] | RCT | CP (n = 40) | Triamcinolone + bupivacaine (n = 21) | 100% | 68.4%-85.7% | 1 severe hypertension |
Bupivacaine (n = 19) | 4 pain exacerbation | |||||
1 gastric hematoma | ||||||
Wiechowska-Kozlowska et al[178] | RS | PC (n = 29) | CPN | 100% | 86% | 3 diarrhea |
1 hypotonia | ||||||
2 post-procedural pain | ||||||
Wang et al[179] | PS | PC (n = 23) | Celiac ganglion irradiation | 100% | 82.60% | None |
Leblanc et al[180] | PS | PC (n = 20) | 10 mL (n = 10) | 100% | 80% | 3 nausea and vomiting |
20 mL (n = 10) | 100% | 2 diarrhea | ||||
1 lightheadness | ||||||
Seicean et al[181] | PS | PC (n = 32) | CPN | 100% | 75% | NR |
Doi et al[162] | RCT | PC (n = 68) | CPN (n = 34) | 100% | 45.50% | 1 GI bleeding |
CGN (n = 34) | 88.20% | 73.50% | 3 hypotension | |||
5 diarrhea | ||||||
17 pain exacerbation | ||||||
Total | 23 studies | 1327 | - | 100% (88.2%-100%) | 71.9% (45.5%-90%) | - |
RCT: Randomized controlled trial; PS: Prospective study; RS: Retrospective study; PC: Pancreatic cancer; CP: Chronic pancreatitis; CPN: Celiac plexus neurolysis; CPB: Celiac plexus block; CT: Computed tomography; CGB: Celiac ganglia block; CGN: Celiac ganglia neurolysis; NR: Not reported.
EUS-CPN in patients with pancreatic cancer
EUS-CPN vs analgesics: EUS-CPN (8 studies, 283 patients) was demonstrated safe and effective in alleviating refractory pain due to pancreatic cancer: pooled proportion 80.1% (74.5%-85.2%)[156] (LE Ia). Alcohol-based EUS-CPN was found safe and effective in this setting: the pooled proportion of patients (5 studies, 119 patients) that experienced pain relief was 72.5%[157] (LE Ia). In a recent RCT, 96 patients with advanced pancreatic cancer were randomly assigned to early EUS-guided CPN or to conventional pain management; the authors observed greater pain relief in the early EUS-CPN group at three months than in conventional management group [-67% (-87 to -25), P = 0.01][158] (LE Ib). Finally, compared to opioids, EUS-CPN (6 studies, 358 patients) was demonstrated to reduce pain at four and eight wk [visual analog score -0.42 (-0.70 to -0.13) and -0.44 (-0.89 to -0.01)] and significantly reduced opioid consumptions in the EUS-CPN group (P < 0.00001)[159]. EUS-CPN is superior to analgesic therapy in reducing pain (LE Ia).
Single central injection vs bilateral injections: Leblanc et al[160] randomized 50 patients with pancreatic cancer to receive one or two injections of alcohol for CPN without observing any difference in onset or duration of pain relief in the two groups[161]. There is no difference between central vs bilateral injections in EUS-CPN (LE Ib).
EUS-CPN vs EUS-direct celiac ganglia neurolysis: Thirty-four patients were assigned to undergoing either EUS-celiac ganglia neurolysis (CGN) or classical EUS-CPN. The authors observed higher treatment response rate (73.5% vs 45.5%, P = 0.026) and complete response rate (50.0% vs 18.2%, P = 0.010) in the EUS-CGN group compared to the EUS-CPN group[162]. EUS-CGN is superior to conventional EUS-CPN in inducing pain relief (LE Ib).
EUS-CPN and EUS-CPB in patients with chronic pancreatitis
EUS-CPN vs analgesics: In patients with pain due to chronic pancreatitis (9 studies, 376 patients) alcohol-based EUS-CPN provided pain relief in 59.4% (95%CI: 54.5-64.3)[157]. EUS-CPN is effective in pain control due to chronic pancreatitis; however, in this setting, due to the relative lower efficacy than in oncologic disease, the development of techniques or new injected drugs seem to be needed (LE Ia).
EUS-CPB vs analgesic: Meta-analysis for efficacy of steroid-based EUS-guided celiac plexus block (EUS-CPB) in patients with refractory pain due to chronic pancreatitis (6 studies, 221 patients) showed an effective alleviation of abdominal pain only in 51.46% of them[158]. EUS-CPB is moderately effective in pain control due to chronic pancreatitis. In this setting, the development of new techniques and/or injected drugs is needed (LE Ia).
EUS-guided vs percutaneous-CPB: An RCT comparing the safety and efficacy of EUS-guided vs CT-guided celiac plexus block in patients with chronic pancreatitis showed that EUS-CPB was significantly more effective in short-term (50% vs 25% at 4 wk) and long-term (30% vs 12% at the end of follow-up) pain control[163] (LE Ib). Another RCT comparing EUS-guided (29 patients) vs percutaneous fluoroscopy-guided (27 patients) CPB with bupivacaine (10 mL) and triamcinolone (3 mL) in patients with chronic pancreatitis demonstrated an improvement in pain scores (visual analog score) in 70% of cases in the EUS group vs 30% of cases in the percutaneous group (P = 0.044)[164] (LE Ib). EUS-CPB provides better pain control than percutaneous-CPB (LE Ib).
Single central injection vs bilateral injections: LeBlanc et al[165] randomized 50 patients with chronic pancreatitis to receive one or two injections of bupivacaine and triamcinolone without observing any difference in duration of pain relief or onset of pain in the two groups. There is no difference between central vs bilateral injections in EUS-CPB (LE Ib).
Bupivacaine and triamcinolone vs bupivacaine alone: In order to evaluate the effect of the addition of triamcinolone to bupivacaine in EUS-CPB, 40 patients were randomized to receive either bupivacaine alone or bupivacaine and triamcinolone. There was no significant difference in pain control between the two groups (14.3% vs 15.8% for controls), therefore the trial was stopped for futility[166]. There is no advantage of adding triamcinolone to bupivacaine for EUS-CPB (LE Ib).
Complications of EUS-CPN and EUS-CPB
Most frequent (up to 30% of patients) adverse events related to EUS-CPN/CPB are represented by diarrhea, abdominal pain and hypotension; however, they are usually mild (grade I-II) and self-limiting[167-181] (Table 8). Nevertheless, we found reports of serious adverse events related to EUS-CPN/CPB including bleeding, abscess, abdominal ischemia, permanent paralysis and also death (LE III) (Table 9). In our opinion, the risk of serious morbidity and mortality should be weighed against expected benefits particularly in patients with a long life expectancy (i.e., patients with chronic pancreatitis).
Table 9.
Ref. | Journal | Year | Complication | Indication | Technique |
Gress et al[247] | Gastrointest Endosc | 1997 | 1 retroperitoneal bleeding | CP | EUS-CPN |
1 retroperitoneal abscess | CP | EUS-CPB | |||
Mahajan et al[248] | Gastrointest Endosc | 2002 | 3 empyema | CP | EUS-CPB |
Muscatiello et al[249] | Endoscopy | 2006 | 1 retroperitoneal abscess | PC | EUS-CPN |
Sahai et al[174] | Am J Gastroenterol | 2009 | 1 retroperitoneal bleeding | CP | EUS-CPB |
O’Toole et al[173] | Endoscopy | 2009 | 1 retroperitoneal abscess | CP | EUS-CPB |
Ahmed et al[250] | Endoscopy | 2009 | 1 ischemia | CP | EUS-CPN |
Shin SK et al[251] | Korean J Pain | 2010 | 1 ejaculatory failure | CP | EUS-CPB |
Lalueza et al[252] | Endoscopy | 2011 | 1 brain abscess | CP | EUS-CPN |
Gimeno-Garcia et al[253] | Endoscopy | 2012 | 1 ischemia/death | CP | EUS-CPN |
Fujii et al[254] | Endoscopy | 2012 | 1 spinal cord infarction/paralysis | PC | EUS-CPN-G |
Mittal et al[255] | Neurology | 2012 | 1 spinal cord infarction/paralysis | PC | EUS-CPN-G |
Loeve et al[256] | Gastrointest Endosc | 2013 | 1 gastric necrosis/death | PC | EUS-CPN |
Jang et al[257] | Clin Endosc | 2013 | 1 hepatic-bowel infarction/death | PC | EUS-CPN |
Doi et al[162] | Endoscopy | 2013 | 1 GI bleeding (puncture site) | PC | EUS-CGN |
CP: Chronic pancreatitis; PC: Pancreatic cancer; CPN: Celiac plexus neurolysis; CPB: Celiac plexus block.
EUS-GUIDED ETHANOL INJECTION
Pancreatic cystic lesions
The initial steps for performing EUS-guided ethanol cyst ablation are similar to those for pancreatic EUS-FNA including antibiotic prophylaxis and puncturing the cysts with a 22-gauge needle. After partial or total evacuation of cystic fluid for diagnostic purposes, a volume of ethanol equal to that aspirated should be injected and maintained for 3-5 min. After aspiration of the total amount of ethanol injected, a chemotherapeutic agent (i.e., paclitaxel) may be injected and left inside the cystic cavity[182-190] (Table 10).
Table 10.
Ref. | Design | Indications | Lesion size (mm) | Techniques | Clinical success | Complications |
Gan et al[187] | PS | Pancreatic cystic lesions (n = 25) | 6-30 | Ethanol | 35% | None |
Oh et al[185] | PS | Pancreatic cystic lesions (n = 14) | 17-52 | Ethanol and paclitaxel | 79% | 1 acute pancreatitis |
6 hyperamylasemia | ||||||
1 abdominal pain | ||||||
Oh et al[182] | PS | Septated pancreas cysts (n = 10) | 20-68 | Ethanol and paclitaxel | 60% | 1 acute pancreatitis |
DeWitt et al[183] | RCT | Pancreatic cystic lesions (n = 42) | 10-58 | Ethanol vs saline | 33% | 1 acute pancreatitis |
5 abdominal pain | ||||||
1 cystic bleeding | ||||||
DeWitt et al[184] | PS | Pancreatic cystic lesions (n = 12) | 10-50 | Ethanol | 75% at follow-up | - |
Oh et al[186] | PS | Pancreatic cystic lesions (n = 52) | 17-68 | Ethanol and paclitaxel | 62% | 1 acute pancreatitis |
1 abdominal pain | ||||||
1 fever | ||||||
1 splenic vein thrombosis | ||||||
DiMaio et al[189] | RS | Pancreatic cystic lesions (n = 13) | 20.1 ± 7.1 | Ethanol (single/multi) | 38% | 1 abdominal pain |
Oh et al[190] | RS | Pancreatic cystic lesions (n = 1) | 5.2 | Ethanol 99% 28 mL + paclitaxel | Failure, underwent surgery | Portal vein thrombosis |
Jurgensen et al[192] | RS | Pancreatic NET (n = 1) | 13 | Ethanol 95% 8 mL | Complete remission | Pain + lipase increase |
Muscatiello et al[193] | RS | Pancreatic NET (n = 1) | 11 and 7 | Ethanol 40% 2 mL | No recurrence at 18 mo | Small pancreatic necrosis |
Deprez et al[194] | RS | Pancreatic NET (n = 1) | 13 | Ethanol 98% 3.5 mL | Complete remission | Hematoma and duodenal ulcer |
Vleggaar et al[195] | RS | Pancreatic NET (n = 1) | 10 | Ethanol 96% 0.3 mL | Asymptomatic at 6 mo | None |
Levy et al[191] | RS | Pancreatic NET (n = 5) | 8-21 | Ethanol 95-99% 0.1-3 mL | 60% symptoms resolution | None |
Barclay et al[196] | RS | Solid Hepatic Metastasis (n = 1) | 33 | Ethanol 98% 6 mL | Good condition at 5.5 yr | Liver hematoma |
Gunter et al[197] | RS | GI stromal tumor (n = 1) | 40 | Ethanol 95% | Complete remission | Abdominal pain |
1.5 mL | Mucosal ulceration | |||||
Hu et al[198] | RS | Liver metastasis (n = 1) | 35 | Ethanol 100% 10 mL | Local control and decrease in size | Fever |
Artifon et al[199] | RS | Left adrenal metastasis (n = 1) | 50 | Ethanol 98% 15 mL | Palliation of related pain | None |
DeWitt et al[200] | RS | Metastatic lymph node (n = 1) | 10-11 | Ethanol | Locally successful | None |
4 + 2 mL | ||||||
Total (cystic lesion) | 8 studies | 169 patients | 6-68 | - | 60% (33%-79%) | - |
RCT: Randomized controlled trial; PS: Prospective study; RS: Retrospective study; NR: Not reported; NET: Neuroendocrine tumor.
Ethanol vs saline: Ethanol injection with EUS led to a greater reduction in cyst size compared to simple saline injection (43% vs 11%); moreover, ethanol injection resulted in complete cyst ablation in 33% of cases (12 out of 36)[183] (LE Ib). Follow-up by CT scan at 2 years of patients who had obtained complete cyst ablation after treatment showed persistent resolution of pancreatic cystic lesions in 75% of cases[184] (LE IIb). Ethanol injection and lavage induces a significantly greater reduction in cyst size and allows a significantly higher rate of cyst ablation than saline alone (LE Ib).
Ethanol plus paclitaxel: In their experience on 52 patients with uniloculated or oligoloculated pancreatic cyst treated with ethanol lavage followed by paclitaxel injection, Oh et al[186] observed complete resolution in 62% of patients after 1-year follow-up. The authors identified small cyst size as a positive predictive factor of treatment response. Addition of paclitaxel to ethanol injection is safe and effective and leads to a greater treatment rate of pancreatic cystic lesions compared to ethanol alone (LE IIb).
Solid lesions
EUS-guided injection of ethanol has been applied to a variety of solid tumors including pancreatic endocrine tumors, hepatic metastases, and submucosal tumors[191-200]. In a single-center RS, Levy et al[191] reported safety and efficacy of EUS-guided ethanol injection in five patients with pancreatic insulinoma. The authors obtained symptoms resolution in 60% of patients with no complications[191] (LE III). Ethanol injection is feasible and safe in solid pancreatic insulinomas (LE III).
EUS-GUIDED TUMOR ABLATION
EUS-guided fine needle injection
EUS-fine needle injection (FNI) is a simple technique to deliver chemotherapeutic agents into tumoral tissue for the treatment of locally advanced pancreatic or esophageal cancer. The technical outcome of all the studies about EUS-FNI reached 100%, paralleling the ability of performing EUS-FNA for cytological diagnosis. However, the clinical outcome varied greatly according to the different chemical or biological agents being tested[201] (Table 11).
Table 11.
Ref. | Design | Indications | Techniques | Type | Tumor response | Complications |
Chang et al[202] | PS | Pancreatic cancer (n = 8) | Injection | Cytoimplant | 2 partial; | None |
1 minor | ||||||
Hecht et al[203] | PS | Pancreatic cancer (n = 21) | Injection | ONYX-015 + iv gemcitabine | 2 partial; | 2 sepsis |
2 minor; | 2 duodenal perforations | |||||
6 stable; | ||||||
11 progression | ||||||
Chang et al[211] | RS | Pancreatic cancer (n = 1) | Injection | TNFerade + chemoradiotx | Surgical resection | None |
Hecht et al[205] | PS | Pancreatic cancer (n = 50) | Injection (27 EUS-guided) | TNFerade + chemoradiotx | 1 complete; | 6 GI bleeding |
3 partial; | 6 deep vein thrombosis | |||||
4 minor; | 2 pulmonary embolism | |||||
12 stable | 2 pancreatitis | |||||
6 cholangitis | ||||||
Irisawa et al[204] | PS | Pancreatic cancer (n = 7) | Injection | Immature dendritic cells | 2 mixed; | None |
2 stable; | ||||||
3 progressive | ||||||
Hanna et al[207] | PS | Pancreatic cancer (n = 9) | Injection (6 EUS-guided) | BC-819 + chemoradiotx | 2 surgically resectable; | None |
3 partial | ||||||
Chang et al[206] | PS | Esophageal cancer (n = 24) | Injection | TNFerade | 6 complete; | 5 thromboembolic events (highest dose) |
2 stable | ||||||
Arcidiacono[208] | PS | Pancreatic cancer (n = 22) | Cryothermal Ablation | EUS-CTP | 6 partial response (only 6 patients analyzed) | 3 hyperamylasemia |
Maier et al[212] | PS | Head/neck cancer (n = 21) | Brachytx | Ir-192 needles | 4 full; | None |
15 partial; | ||||||
3 none | ||||||
Lah et al[213] | RS | Metastatic celiac lymph nodes (n = 1) | Brachytx | I-125 seeds | Response | None |
Martinez-Monge et al[214] | RS | Metastatic mediastinal lymph node (n = 1) | Brachytx | I-125 seeds | Response | None |
Sun et al[209] | PS | Pancreatic cancer (n = 15) | Brachytx | I-125 seeds | 4 partial; | 1 site infection |
3 minor; | 3 hematologic side effects | |||||
5 stable; | ||||||
3 progressive | ||||||
Jin et al[210] | PS | Pancreatic cancer (n = 22 ) | Brachytx | I-125 seeds | 4 partial; | 1 seed migration |
10 stable |
RCT: Randomized controlled trial; PS: Prospective study; RS: Retrospective study; NR: Not reported; CTP: Cryothermal probe; GI: Gastrointestinal.
Allogeneic mixed lymphocyte culture: The first study assessing EUS-FNI for pancreatic cancer tested the safety and efficacy of allogeneic mixed lymphocyte culture in locally advanced pancreatic adenocarcinoma in 8 patients. The procedure (single session of EUS-guided injection) was safe and two partial responses and one minor response were reported (median survival 13.2 mo)[202] (LE IIb).
Adenovirus ONYX-015: ONYX-015, a modified adenovirus (deletion in the E1B gene) which replicate in tumor cells leading to cell death, was used for EUS-FNI in pancreatic cancer in combination with systemic gemcitabine. The authors enrolled 21 patients in this phase I study and reported two patients with partial regression and two with minor response. However, 4 serious adverse events were observed (two sepsis and two duodenal perforations)[203] (LE IIb).
Immature dendritic cells: Irisawa et al[204] reported a pilot study (phase I) with injection of immature dendritic cells (DCs). DCs were used for EUS-FNI in view of their potent induction of primary T-cell response against tumor antigens. Among 7 patients with locally advanced pancreatic adenocarcinoma, one complete and three partial responses were reported. No adverse events were described[204] (LE IIb).
TNFerade: EUS-FNI of TNFerade, a replication-deficient adenovirus vector carrying the tumor necrosis factor-α gene, was tested in a multicenter study on 50 patients with locally advanced pancreatic cancer in combination with systemic fluorouracil. The authors observed 1 complete response, 3 partial responses, and 12 patients with stable disease after treatment. Interestingly, seven patients became suitable for surgery after EUS-FNI and 6 of them underwent R0 resection. According to the authors, an RCT is warranted to further assess these encouraging results[205] (LE IIb).
The efficacy of EUS-FNI of TNFerade was also assessed in 24 patients with locally advanced but still resectable esophageal cancer (20% stage II, 80% stage III). EUS-FNI of TNFerade was combined with cisplatin, 5-fluorouracil and radiation therapy. Six complete responses and 2 stable diseases were observed. The median survival was 47.8 mo and 5-year survival and disease-free survival rates were 41% and 38%, respectively. Additionally, EUS-FNI proved to be safe[206] (LE IIb).
BC-819: The safety, tolerability and preliminary efficacy of EUS-FNI of BC-819, a DNA plasmid developed to target the expression of diphtheria-toxin gene under the control of H19 regulatory sequences, was recently tested in 6 patients with pancreatic cancer in combination with chemoradiotherapy. Three patients showed partial response and other two patients who were downstaged were able to undergo surgical resection[207]. Intratumoral EUS-FNI in patients with advanced pancreatic and esophageal cancer is technically easy, safe and can induce tumor downstaging in some cases (LE IIb).
EUS-guided cryothermal ablation
The safety and efficacy of cryothermal ablation was assessed using a newly developed cryotherm probe (CTP) in 22 patients with locally advanced pancreatic cancer. CTP is a large bore flexible bipolar device that combines radiofrequency with cryogenic cooling in the same session. EUS-guided CTP ablation was feasible in 16 patients. CT scan was performed in all cases after treatment; in 6/16 patients a reduction in tumor size was clearly seen. The procedure was well tolerated in all cases[208] (LE IIb).
EUS-guided brachytherapy
The feasibility, safety and efficacy of EUS-guided implantation of radioactive seeds in patients with locally advanced pancreatic cancer were assessed in a few studies[209-214]. Partial tumor response ranged from 13.6% to 27% while a stable disease was observed in 45.5%-53% of cases in two pilot studies[209,210]. In both series, up to 30% of patients reported transient pain reduction within the first period after treatment. Adverse event rate range was 0%-20% (pancreatitis and pseudocyst formation) in association to systemic, non-EUS-related, adverse events (LE IIb). EUS-guided CTP ablation and brachytherapy are feasible in a subset of patients with locally advanced pancreatic cancer. However, their safety and clinical outcome have to be further investigated (LE IIb).
EUS-guided fiducial placement
Imaging-guided radiation therapy is based upon a real-time tracking system to target the tumor to be irradiated. In order to minimize irradiation of adjacent normal tissue in pancreatic malignancies, the placement of radiopaque fiducials inside or near the tumor allows a radiographic marking enabling precise tumor targeting. Firstly, fiducials were placed in patients with advanced pancreatic cancer were placed with surgical or radiological techniques. In the last decade, the less invasive EUS-guided fiducial placement was shown to be safe and precise[215-227] (Table 12).
Table 12.
Ref. | Design | Indications | Techniques | Technical success | Needle | Complications |
Pishvaian et al[215] | PS | Abdominal/mediastinal cancer (n = 13) | Fiducial placement | 11/13 (84.6) | 19 Gauge | 1 infection |
Varadarajulu et al[222] | RS | Pancreatic cancer (n = 9) | Fiducial placement | 9/9 (100) | NR | None |
DiMaio et al[223] | RS | Abdominal/mediastinal cancer (n = 30) | Fiducial placement | 29/30 (97) | 22 Gauge | None |
Sanders et al[217] | PS | Pancreatic cancer (n = 51) | Fiducial placement | 46/51 (90) | 19 Gauge | 1 mild pancreatitis |
Park et al[216] | PS | Pancreatic cancer (n = 57) | Fiducial placement | 50/57 (88) | 19 Gauge | None |
Ammar et al[224] | RS | Abdominal cancer/lymph nodes (n = 13) | Single fiducial marker | 9/9 trans-gastric | 22 Gauge | None |
4/4 trans-duodenal | ||||||
Varadarajulu et al[225] | PS | Pancreatic cancer (n = 2) | Fiducial placement | 2/2 (100) | 19 Gauge flexible | None |
Khashab et al[218] | RS | Pancreatic cancer (n = 39) | Fiducial placement (traditional vs coiled) | 39/39 (100) | 19 and 22 Gauge | None |
Law et al[226] | RS | Small pancreatic NET (n = 2) | Fiducial placement | 2/2 (100) | 22 Gauge | None |
Majumder et al[219] | RS | Pancreatic cancer (n = 39) | Fiducial placement | 35/39 (89.7) | 19 Gauge | 1 mild pancreatitis |
4 abdominal pain | ||||||
Yang et al[220] | RS | Prostate cancer (n = 16) | Fiducial placement | 16/16 (100) | 19 Gauge | None |
Yang et al[221] | RS | Prostate cancer recurrence (n = 6) | Fiducial placement | 6/6 (100) | 19 Gauge | None |
Trevino et al[227] | RS | Rectal cancer (n = 1) | Fiducial placement | 3/3 (100) | 19 Gauge (forward-view EUS) | None |
Total | 13 studies | 278 | - | 100% (84.6%-100%) | - | 0% |
RCT: Randomized controlled trial; PS: Prospective study; RS: Retrospective study; NR: Not reported; NET: Neuroendocrine tumor:
Safety and effectiveness: Two PSs enrolling a total of 101 patients with locally advanced or recurrent pancreatic cancer reported high technical and clinical success rates (88%-90%). Overall complication rate was low with only few minor adverse events (one patient experienced minor bleeding from the site of EUS needle entrance and one experienced mild pancreatitis). Migration of the gold fiducials was reported in 7% of cases[216,217] (LE IIb).
Traditional vs coiled fiducials: Khashab et al[218] compared the technical success, safety, visibility and migration of two different types of fiducials (traditional vs coiled). In their RS, no differences were observed in visibility, degree of fiducial migration, number of fiducial placement, technical difficulty or complication rate (LE III).
Ideal fiducial geometry: A recent study compared the achievement of the iIdeal fiducial geometry (IGF) (defined as the placement of 3 fiducials with at least 2 cm of distance, at least 15 degrees angle, and non-planar placement) in 39 patients who underwent EUS-guided fiducial placement vs 38 who underwent surgical fiducial placement. In this RS, the authors identified a significantly higher rate of IGF reached with surgical vs EUS placement (47% vs 18%, P = 0.0011). However, it was observed that despite the lower IGF rate in the EUS group, fiducial tracking for irradiation therapy was successful in a similar percentage of patients from the two groups (> 80%)[219] (LE III). EUS-guided fiducial placement is safe and leads to technical and clinical success in about 90% of patients (LE IIb).
Non-pancreatic cancer: Two recent retrospective case series reported the feasibility and safety of fiducial placement in 16 patients with prostate cancer and in 6 with prostate cancer recurrence. The authors reported extremely high success rates (16/16 and 6/6 respectively) with no incidence of adverse events[220,221] (LE III). EUS-guided fiducial placement was feasible and safe in patients with prostate cancer or prostate cancer recurrence (LE III).
EUS-GUIDED VASCULAR INTERVENTIONS
EUS combined with color/power Doppler allows precise identification of vascular anatomy, potential high risk vessels with/without portal hypertension, and occult sources of bleeding such as Dieulafoy’s lesions and pseudoaneurysms. Moreover, EUS provides direct access to vascular structures next to gastrointestinal wall, allowing precise vascular interventions[228-246] (Table 13).
Table 13.
Ref. | Design | Indications | Techniques | Technical success | Rebleeding | Complications |
Fockens et al[229] | RS | Dieulafoy’s lesion (n = 4) | Polidocanol injection | 4/4 (100) | 2/4 (50) | None |
Levy et al[234] | RS | Dieulafoy’s lesion (n = 1) | Alcohol 99% injection | 1/1 (100) | No | None |
Gonzalez et al[235] | RS | Dieulafoy’s lesion (n = 2) | Polidocanol | 2/2 (100) | No | None |
or CYA injection | ||||||
Levy et al[234] | RS | Various (n = 4) | Alcohol 99% or CYA injection | 4/4 (100) | No | None |
Gonzalez et al[235] | RS | Pseudo-aneurysm (n = 3) | CYA injection | 3/3 (100) | No | None |
Gonzalez et al[235] | RS | Gastric varices (n = 2) | CYA injection | 2/2 (100) | No | None |
Lee et al[231] | RS | Gastric varices (n = 101) | EUS-assisted CYA injection | - | Early 4/54 (7.4) | None |
Late 10/54 (18) | ||||||
Lahoti et al[236] | RS | Esophageal varices (n = 5) | Sclerotherapy | 5/5 (100) | No | 1 esophageal stricture |
Romero-Castro et al[237] | RS | Gastric varices (n = 5) | CYA injection | 5/5 (100) | No | None |
De Paulo et al[230] | RCT | Esophageal varices (n = 50) | Endo vs EUS-guided CYA injection | 24/25 (96) | 2/24 recurrence of varices (8.3) | None |
Levy et al[238] | RS | Choledochojejunal anastomotic varices (n = 1) | Coil embolization | 1/1 (100) | No | None |
Romero-Castro et al[239] | RS | Gastric varices (n = 4) | Coil embolization | 3/4 (75) | No | None |
Binmoeller et al[233] | RS | Gastric varices (n = 30) | CYA injection + coil embolization | 30/30 (100) | 4/24 (16.6) | None |
Romero-Castro et al[232] | RS | Gastric varices (n = 30) | CYA injection (n = 19) vs coils (n = 11) | 97.4 % vs 90.9% | NR | 9 CYA embolization; |
1 chest pain; 1 fever; | ||||||
1 variceal bleeding | ||||||
Weilert et al[240] | RS | Rectal varices (n = 1) | CYA injection plus coils | 100% | No | None |
Gonzalez et al[241] | RS | Splenic artery aneurism (n = 1) | CYA injection | 1/1 (100) | No | None |
Roberts et al[242] | RS | Visceral pseudoaneurysm (n = 1) | HistoAcryl injection | 1/1 (100) | No | None |
Roach et al[243] | RS | SMA aneurysm (n = 1) | Thrombin injection | 1/1 (100) | No | None |
Chaves et al[244] | RS | SMA aneurysm (n = 1) | Thrombin injection | 1/1 (100) | No | None |
Robinson et al[245] | RS | Splenic artery aneurysm (n = 1) | Thrombin injection | 1/1 (100) | No | None |
Lameris et al[246] | RS | Visceral pseudoaneurysm (n = 1) | Thrombin + collagen injection | 1/1 (100) | No | None |
RCT: Randomized controlled trial; PS: Prospective study; RS: Retrospective study; NR: Not reported; CYA: Cyanoacrylate; SMA: Superior mesenteric artery.
EUS-guided treatment of non-variceal bleeding
The efficacy of EUS-guided treatments of non-variceal upper gastrointestinal bleeding was reported only in form of small case series and case reports. Fockens et al[229] first reported about the usefulness of EUS in the diagnosis of small abnormal vessels in 8 patients with Dieulafoy’s lesions. In 50% of cases it was possible to perform EUS-guided injection of sclerosing agent into the aberrant vessels[229] (LE III).
EUS-guided treatment of portal hypertension
Endoscopic vs EUS-guided sclerotherapy of esophageal collateral veins: An RCT compared the safety and efficacy of EUS-guided and endoscopic sclerotherapy (ethanolamine oleate injection) in 50 patients affected by liver cirrhosis. The authors did not observe any difference in variceal eradication, number of sessions needed to achieve the eradication, variceal recurrence and adverse event rates[230] (LE Ib). EUS-guided sclerotherapy does not confer any significant advantage in terms of safety and efficacy compared to classical endoscopic sclerotherapy (LE Ib).
Gastric variceal bleeding: In a RS, EUS-assisted cyanoacrylate (CYA) injection until obliteration of all gastric varices collateral was compared to an historical group of cirrhotic patients who underwent standard endoscopic injection, only in case of recurrent bleeding. While early re-bleeding rate was similar in the two groups (7.4% vs 12.8%, respectively, P = NS), late recurrent bleeding was significantly reduced in patients who underwent CYA injection under EUS control to check for complete obliteration (18.5% vs 44.7%, P = 0.0053, OR = 0.28)[231] (LE IIb). EUS guidance allows an higher rate of gastric variceal obliteration and reduces recurrent bleeding (LE IIb).
Coil embolization vs CYA injection for gastric varices: A multicenter RS compared feasibility, safety and applicability of coil embolization vs sclerotherapy (CYA injection) under EUS guidance. Thirty patients (11 coil group vs 19 CYA group) underwent EUS-guided treatment for gastric varices. The rate of variceal obliteration was similar in the two groups (90.9% vs 94.7%, respectively) without differences in number of EUS sessions. Eleven patients (11/19) in the sclerotherapy group experienced adverse events; in 9 of them an asymptomatic pulmonary glue embolism was found on CT scan, while 1 patient experienced fever and another experienced chest pain; on the other hand, only one patient treated with coil embolization experienced an adverse event (esophageal variceal bleeding). The comparison among the two treatment groups demonstrated a significantly lower incidence of any grade adverse events in the embolization group (58% vs 9%, P < 0.01); only 3 patients, two in the CYA and one in the coil group, experienced symptomatic adverse events[232] (LE IIb).
Combined coil embolization and CYA injection for gastric varices: The authors reported about 30 patients who underwent EUS-guided trans-esophageal combined embolization and sclerotherapy of gastric varices using in the majority of cases a forward-view echoendoscope. Successful treatment was achieved in all cases (30 out of 30, 100%) after a mean of 1.3 EUS sessions, including 2 cases with active bleeding. Rebleeding occurred in 16% of cases and no procedure-related adverse events were reported[233] (LE III). EUS-guided coil embolization and CYA injection are both effective for gastric varices treatment in patients with cirrhosis (LE IIb). While both sclerotherapy and embolization monotherapy present a high complication rate, combined coil embolization and CYA injection seems to be safe and effective in patients with gastric varices (LE III).
CONCLUSION
Several EUS-guided treatments are now available in endosonographer’s armamentarium. The usefulness of EUS-GD of PFCs and of EUS-CPN has been well established in studies with high LE. Other techniques including EUS-guided biliary drainage have been tested only in studies with medium-low LE and thus should still be performed either in referral centers by experienced endosonographers or in investigational/research settings. Well-designed RCTs are warranted to further elucidate the safety and benefits of EUS-guided treatments in comparison to the standards of care.
Footnotes
P- Reviewers: Chatterjee S, Gornals JB, Tellez-Avila F S- Editor: Zhai HH L- Editor: A E- Editor: Zhang DN
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