Abstract
The REDISCOVER guidelines present 34 recommendations for the selection and perioperative care of borderline-resectable (BR-PDAC) and locally advanced ductal adenocarcinoma of the pancreas (LA-PDAC). These guidelines represent a significant shift from previous approaches, prioritizing tumor biology over anatomical features as the primary indication for resection. Condensed herein, they provide a practical management algorithm for clinical practice. However, the guidelines also highlight the need to redefine LA-PDAC to align with modern treatment strategies and to solve some contradictions within the current definition, such as grouping "difficult" and "impossible" to resect tumors together. Furthermore, the REDISCOVER guidelines highlight several areas requiring urgent research. These include the resection of the superior mesenteric artery, the management strategies for patients with LA-PDAC who are fit for surgery but unable to receive multi-agent neoadjuvant chemotherapy, the approach to patients with LA-PDAC who are fit for surgery but demonstrate high serum Ca 19.9 levels even after neoadjuvant treatment, and the optimal timing and number of chemotherapy cycles prior to surgery. Additionally, the role of primary chemoradiotherapy versus chemotherapy alone in LA-PDAC, the timing of surgical resection post-neoadjuvant/primary chemoradiotherapy, the efficacy of ablation therapies, and the management of oligometastasis in patients with LA-PDAC warrant investigation. Given the limited evidence for many issues, refining existing management strategies is imperative. The establishment of the REDISCOVER registry (https://rediscover.unipi.it/) offers promise of a unified research platform to advance understanding and improve the management of BR-PDAC and LA-PDAC.
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Introduction
Pancreatic ductal adenocarcinoma (PDAC) is recognized for its aggressive biological behavior, often resulting in a fatal outcome for the majority of affected individuals. This heightened mortality rate is predominantly attributed to early hematogenous spread and intrinsic resistance to conventional oncological treatments. Consequently, distant metastases are frequently detectable at the time of diagnosis in approximately 60% of patients, rendering curative resection of the primary tumor unattainable. Tumor size stands out as a key prognostic factor in resected PDAC. While larger tumor sizes increase the risk of distant metastases, such metastases can also manifest in up to one-third of patients with tumors measuring 0.5 cm or less. Given the significant morbidity and mortality associated with pancreatic resection, surgical intervention is generally reserved for patients with localized disease [1,2,3,4,5,6,7,8].
Localized PDAC can be classified into three subgroups: resectable, borderline resectable (BR-PDAC), and locally advanced (LA-PDAC). These categories are based on the degree of vascular involvement and the probability of achieving a margin-negative resection. BR-PDAC and LA-PDAC comprise approximately one-third of all PDAC cases. Recently, the concept of anatomical resectability has been expanded to include biologic resectability, primarily assessed by levels of Ca 19-9, and conditional resectability, which considers the patient's overall health status and any comorbidities. The contemporary approach to resectability in pancreatic cancer integrates these concepts into what is commonly referred to as the A, B, C criteria [9].
Recent advancements in chemotherapy have shifted the focus towards the biologic aspect of resectability, leading to the emergence of "prognosis-based resectability", also known as conversion surgery [10, 11]. A study employing an intention-to-treat analysis of neoadjuvant FOLFIRINOX for PDAC demonstrated that surgical exploration and the attainment of negative margins at pathology were equally achievable across all anatomical resectability categories [12]. Similarly, the NORPATC-2 trial corroborated that the response to preoperative chemotherapy remains unaffected by local tumor growth. Notably, the necessity for vascular resection was consistent across the three resectability categories, and both BR-PDAC and LA-PDAC exhibited comparable survival rates. Moreover, surgical resection was found to enhance survival outcomes relative to continued medical treatment [13].
The recent REDISCOVER guidelines have issued a consensus document endorsing a prognosis-based approach to resection in PDAC over an anatomy-based approach, while also offering insights into perioperative care specifics. However, the level of evidence supporting these recommendations was predominantly low, and several issues could not be endorsed due to insufficient evidence or reservations about incorporating avant-garde strategies into the guideline document [14].
This second report from the REDISCOVER consensus meeting aims to introduce a management algorithm for BR-PDAC and LA-PDAC Additionally, it addresses the questions that were not approved, highlighting the most crucial areas for future research.
The REDISCOVER guidelines were an initiative of the Italian Society of Surgery, endorsed by the Pancreas Club Inc. and the European-African Hepato-Pancreato-Biliary Association (blue seal).
Methods
The REDISCOVER guidelines encompassed 34 recommendations that received approval during the final consensus conference held in Pisa, Italy, on September 17 and 18, 2023. The comprehensive PRISMA flowchart detailing the literature review and the consensus conference workflow is depicted in Figs. 1 and 2, respectively.
Utilizing these endorsed recommendations, we formulated a management algorithm tailored for the perioperative care of patients diagnosed with BR- and LA-PDAC. The clinical questions that did not garner approval were scrutinized to identify the most pressing areas requiring further clinical investigation.
Results
The consensus conference witnessed participation from 136 attendees spanning 18 countries, including Australia, Austria, China, Italy, England, France, Germany, Greece, India, Ireland, Japan, Portugal, Russia, Spain, Sweden, Switzerland, The Netherlands, and the USA. The total audience count surpassed 150 participants.
Although all recommendations received consensus after the online Delphi rounds, only 34 were ultimately endorsed. Twelve distinct clinical questions were amalgamated into 6, while 12 recommendations were dismissed. Among these, three were discarded by the assembly, and nine were rejected by the validation committee. Table 1 delineates the 34 approved recommendations. Notably, 85% of the clinical questions (29 out of 34) were supported by low-level evidence. Consequently, the strength of the recommendations predominantly relied on expert opinion (22 times), followed by weak (10 times), and strong (2 times, one of which was upgraded by experts) evidence. Figure 3 illustrates the management algorithm derived from the 34 validated recommendations.
Table 2 enumerates the 12 recommendations that failed to gain approval. These recommendations addressed eight pivotal areas:
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1.
Resection and reconstruction of the superior mesenteric artery.
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2.
Management strategies for LA-PDAC patients fit for surgery unable to undergo multi-agent neoadjuvant chemotherapy.
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3.
Management of LA-PDAC patients fit for surgery exhibiting elevated serum Ca 19.9 levels post-neoadjuvant oncology treatments.
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4.
Optimal number of chemotherapy cycles pre-surgery.
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5.
Comparative efficacy of primary chemoradiotherapy versus chemotherapy alone in LA-PDAC.
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6.
Appropriate timing for surgical resection post-neoadjuvant/primary chemoradiotherapy
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7.
Role of ablation therapies.
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8.
Management of patients with oligometastasis and LA-PDAC.
Furthermore, insights from literature reviews and deliberations during the consensus meeting highlighted the need to redefine the current anatomic-based definition of LA-PDAC. This revision aims to align with the emerging concept of prognosis-based resectability and conform to the A, B, C paradigm of borderline resectability.
Post-consensus, the REDISCOVER registry was initiated to amass comprehensive global data. Accessible at https://rediscover.unipi.it/, this registry acts as a pivotal platform for ongoing research and developmental initiatives in this domain. Its primary ambition is to collate an exhaustive dataset focusing on BR-PDAC and LA-PDAC. The REDISCOVER registry invites researchers and healthcare practitioners to contribute vital data, fostering collaborative endeavors to enhance comprehension, treatment modalities, and outcomes for patients afflicted with BR-PDAC and LA-PDAC.
Discussion
Recently, the REDISCOVER guidelines were released [14]. They provide the first recommendations for the perioperative care of patients with BR-PDAC and LA-PDAC. In this report, the REDISCOVER recommendations were arranged to create a management algorithm based on the progression of clinical decisions. During the REDISCOVER consensus conference, some disruptive concepts were addressed and approved; however, several were either rejected or deemed to be at a nascent stage and early to be included in the guidelines. These important topics are covered in this article.
In general, the REDISCOVER guidelines are based on a low level of evidence thus highlighting the urgent need for further high-quality research. At least in part, the low level of evidence is explained by many studies reporting on BR-PDAC and LA-PDAC as a unique entity. Discussions at the consensus conferences also demonstrated that current definitions of BR-PDAC and LA-PDAC are rather subjective and lack clear prognostic implications. Possibly, newer definitions of BR-PDAC and LA-PDAC should be provided that best match the dynamic view of PDAC "stage" based on response to primary and neoadjuvant oncology treatments.
Indeed, the primary message from the REDISCOVER guidelines is that the more dynamic and, to some extent, logical concept of tumor biology predicting prognosis has superseded the static paradigm of vascular involvement as a marker of poor prognosis/unresectability. On the other hand, our understanding of PDAC biology is still incomplete. Chemotherapy response is currently employed as a surrogate marker of good tumor biology; nevertheless, some patients who appear to respond well to oncology therapies still have early tumor recurrence and are unlikely to benefit from radical resection. The use of molecular biomarkers appears to be the most sensible development of the biological selection theory [15]. However, because of the current low probability of obtaining key prognostic information and the high costs, routine molecular testing cannot be advised in current clinical practice. While the NCCN guidelines currently recommend molecular profiling in LA-PDAC, the probability to identify potentially actionable somatic mutations is quite low and most public health systems do not cover the costs of molecular testing. On practical grounds, only BRCA testing has a real chance to impact oncology decisions, but has no clear implications in the selection of surgical candidates. BRCA mutations are identified in 5%-7% of Caucasian patients [16]. These patients are more susceptible to treatment with platinum compounds and poly (ADP-ribose) polymerase inhibitors [17]. In addition, a study in patients with metastatic PDAC and germline BRCA mutations showed that maintenance treatment with olaparib versus placebo improved median progression-free survival in patients who had stable disease after a 16-week platinum-containing chemotherapy regimen. However, median overall survival was not affected [18]. Therefore, outside clinical trials, molecular testing should be reserved for high-risk individuals and patients with a family history of PDAC for the purpose of genetic counseling [19]. Identification of reliable prognostic markers for the selection of surgical candidates is a main target of future research projects.
In light of the REDISCOVER guidelines, the need to resect peripancreatic vessels after neoadjuvant oncology treatments should be mainly considered a marker of technical difficulty without clear prognostic implications. While adding further technical complexity to pancreatectomy increases the incidence and severity of postoperative complications, several recent studies have shown improved results even in patients requiring arterial resection [20,21,22,23,24]. It is important to underscore here that ensuring acceptable postoperative results in the context of BR-PDAC and LA-PDAC does not only require the ability to perform vascular reconstructions. It rather entails additional technical skills that begin with preoperative planning and end up with a wide range of intraoperative strategies aiming to provide a safe approach to target vessels while respecting the golden principles of surgical oncology and minimizing surgical trauma in terms of intestinal and hepatic ischemia, bowel congestion, and intraoperative bleeding. While vascular reconstruction can be left to either vascular or transplant surgeons, the other tasks require specific skills. Therefore, patients with BR-PDAC and LA-PDAC should be centralized to centers with specific experience in these procedures. The REDISCOVER guidelines defined these institutions as centers of excellence. A recent Scandinavian study demonstrated that a center with a recruitment area of approximately 3 million is expected to manage approximately 75–80 patients with BR-PDAC and LA-PDAC per year, leading to approximately 15 resections for BR-PDAC and 5 for LA-PDAC per year [13]. Pancreatic surgery is sensitive to the effects of centralization. Figures from the Scandinavian study further reinforce the importance of centralization for BR-PDAC and LA-PDAC.
It is crucial to underscore that there comes a point where technical complexity, the patient's physiological status, and the prognostic outlook must be considered collectively. In other words, when anticipating high surgical difficulty in patients with less than optimal performance status and/or tumors exhibiting intermediate biology, the decision to proceed with tumor resection should be discouraged regardless of technical feasibility. These factors should be thoroughly discussed and openly weighed when obtaining informed consent for resection.
Resection and reconstruction of the superior mesenteric artery
The REDISCOVER guidelines recommend LA-PDAC resection in carefully selected patients. However, pancreatectomy with resection and reconstruction of the superior mesenteric artery (PRR-SMA) could not be recommended because of lack of consensus after the audience vote (72%). The majority of experts had agreed on PRR-SMA on the online Delphi rounds (88%).
There is no evidence that involvement of the superior mesenteric artery portends a worse prognosis when compared to the same degree of local tumor spread around the celiac trunk [25]. In fact, following neoadjuvant treatments, there is even no evidence that the prognosis of LA-PDAC is inferior to that of BR-PDAC, further reinforcing the concept of prognosis-based resectability [13, 25]. Most audience's concerns regarding PRR-SMA regarded the high level of technical difficulty of this procedure that typically leads to high rates of morbidity and mortality.
PRR-SMA is clearly a complex procedure, but postoperative outcomes are rapidly improving because of technical refinements and growing experience [20]. Two recent studies from China proposed the adoption of intestinal autotransplantation to overcome the challenges of PRR-SMA. Combining the data of these two studies, 46 PRR-SMAs were performed. Severe postoperative complications occurred in 17 patients (37%) and two patients died (4.3%) [23, 24]. In a recent Western study, 95 PRR-SMA were reported from a single center. In 91 and 32 patients, respectively, the superior mesenteric vein (96%) and the celiac trunk/hepatic artery (34%) were also resected. Upon completion of the learning curve (37 procedures) 3 of 58 patients died within 90 days (5.2%) [21]. These data favorably compare with the prohibitive mortality (11.8%) reported, only 10 years ago, for all types of pancreatectomy with arterial resection (11.8%), as well as, with a more recent systematic review on 70 PRR-SMA (20%) [26, 27].
Further experience with PRR-SMA should continue, beyond the REDISCOVER guidelines, only in centers with specific skills and experience. Data should be recorded in international registries, such as the REDISCOVER registry, or reported in prospective observational studies. Diffusion of PRR-SMA is unlikely to occur quickly, but denying resection solely because of lack of surgical experience should be carefully considered. While proficiency is progressively gained in relatively less complex procedures, consideration should be given to refer these patients to expert centers.
Management strategies for LA-PDAC patients fit for surgery unable to undergo multi-agent neoadjuvant chemotherapy
Most data concerning the survival advantage of neoadjuvant chemotherapy refer to multi-agent chemotherapy [28]. In a recent Scandinavian study approximately 20% of the patients with BR-PDAC and LA-PDAC could only receive best supportive care. FOLFIRINOX was delivered to only 50% of the patients while 15% received single-agent chemotherapy with gemcitabine. In the FOLFIRINOX group 53% of the patients suffered grade 3–5 adverse events and two of them died (1.9%) [13]. In an intention-to-treat study, 216 of 254 patients (85.0%) experienced FOLFIRINOX-related toxicity. Grade 3–4 toxicity was documented in 109 patients (42.9%), 100 patients required inpatient admission and management, while 73 patients (28.7%) required an emergency department admission. Poor tolerability (46.3%) was the main reason for not completing the 8 planned cycles of FOLFIRINOX [12]. The probability to receive multi-agent chemotherapy is mostly influenced by age and performance status. Only 10% of the patients aged 75 years or older can receive FOLFIRINOX and less than half of them complete the treatment [29]. More than half of patients receiving FOLFIRINOX require a biliary stent and almost a third of them requires additional endoscopic interventions for obstructed stents and/or cholangitis resulting in treatment delay and/or dose reduction. Overall, over 20% of the patients who are initiated on FOLFIRINOX fail to complete the number of planned cycles [12]. The possibility to receive FOLFIRINOX chemotherapy is not influenced by local tumor status [12, 29].
Therefore, it is clear that not all patients can receive multi-agent primary/neoadjuvant chemotherapy. Some of these patients, however, may be fit for surgery. The REDISCOVER guidelines acknowledged that upfront surgery may improve survival in BR-PDAC when multi-agent neoadjuvant chemotherapy cannot be delivered, but could not provide a similar recommendation for LA-PDAC. In these patients, efforts should be maximized to permit delivery of multi-agent neoadjuvant chemotherapy, failing which proceeding with resection does not appear to provide a clear oncological advantage.
Management of LA-PDAC patients fit for surgery exhibiting elevated serum Ca 19.9 levels post-neoadjuvant oncology treatments
The probability of radical resection is predicted by the Ca 19.9 level, which carries clear prognostic implications in PDAC [30, 31]. Ca 19.9 levels of > 500 kU/L are a biologic factor associated with borderline resectability [9]. Long-term survival following resection is predicted by both a decrease in Ca 19.9 of ≥ 50% and a normalization of Ca 19.9 in response to neoadjuvant oncology therapies [32, 33]. Depending on pretreatment levels, between 66 and 22% of patients achieve normalization of Ca 19.9 levels [32]. The best indicators to anticipate favorable survival are a baseline level of Ca 19.9 < 80 kU/L and a response to treatment of ≥ 85% [33, 34]. Predicting post-resection outcomes is further improved by Ca 19.9 dynamics during oncology treatments [35].
However, following neoadjuvant oncology therapies, Ca 19.9 level does not decrease or rises in approximately 10% of patients [33]. Some of these patients are fit for surgery, have no evidence of distant metastasis, and harbor a potentially resectable tumor. If “high” Ca 19.9 levels persist following chemotherapy switch, the surgeon is faced with the difficult dilemma of denying resection based only on Ca 19.9 levels. In these patients, according to oncology guidelines, the most sensible course of action is radiation treatment [15, 19]. However, the REDISCOVER guidelines recommended resection for BR-PDAC with stable/rising Ca 19.9 levels but denied this possibility for LA-PDAC. Considering LA-PDAC and BR-PDAC share the same biology, once again, technical complexity and higher operative risk were the main reasons to deny resection in LA-PDAC in the absence of favorable Ca 19.9 response.
Optimal number of chemotherapy cycles pre-surgery
There is no agreement about the ideal number of cycles of chemotherapy before resection. The 2024 NCCN guidelines recommend ≥ 2 to 6 cycles of gemcitabine plus cisplatin in BRAC mutated patients, and ≥ 4 to 6 cycles of all the other chemotherapy regimens (namely, FOLFIRINOX, m FOLFIRINOX, NALIRIFOX, and gemcitabine plus albumin-bound paclitaxel) [15]. The 2023 ESMO guidelines do not recommend a specific number of cycles [19]. A recent, phase 2, randomized and controlled trial employed 8 cycles of mFOLFIRINOX as a neoadjuvant chemotherapy regimen for BR-PDAC and found that this regimen was superior to 7 treatment cycles of mFOLFIRINOX followed by stereotactic body radiotherapy or hypofractionated image-guided radiotherapy [36]. The ESPAC5 trial compared different short-course neoadjuvant oncology regimens (gemcitabine plus capecitabine: two cycles; FOLFIRINOX: four cycles; and capecitabine-based chemoradiotherapy: capecitabine 830 mg/m2 twice a day orally over the 5.5 weeks of radiotherapy) versus upfront surgery in BR-PDAC. Neoadjuvant chemotherapy (either gemcitabine plus capecitabine or FOLFIRINOX) had the best survival compared with upfront surgery [37].
An international cohort study of 520 patients evaluated adjuvant chemotherapy in patients with resected pancreatic cancer after at least 2 cycles of neoadjuvant FOLFIRINOX treatment (47% resectable PDAC; 40% BR-PDAC; 10% LA-PDAC; 3% stage unknown). The median number of neoadjuvant FOLFIRINOX cycles was 6 for patients who received adjuvant therapy and for those who did not [38]. In a recent systematic review and meta-analysis, the median number of FOLFIRINOX cycles administered to with LA-PDAC ranged from 4.9 to 11.5. The number of FOLFIRINOX cycles did not influence the rate of surgical resection and R0 resection [39]. In a similar study on BR-PDAC the median number of FOLFIRINOX cycles was ranged from 4 to 9. The median number of chemotherapy cycles did not affect overall survival [40].
In a systematic review and meta-analysis on neoadjuvant gemcitabine plus nab-paclitaxel in BR-PDAC and LA-PDAC, the median number of chemotherapy cycles ranged from 2 to 8 [41]. In a single-center retrospective study the median number of neoadjuvant gemcitabine plus nab-paclitaxel for BR-PDAC was 3 (range 1–10) [42]. In the recent NORPACT-2 trial, the number of neoadjuvant chemotherapy cycles was 4 for FOLFIRINOX and 2 for gemcitabine plus nab-paclitaxel [13].
It is evident that we lack clarity regarding the ideal number of chemotherapy cycles to administer before surgery in patients with BR-PDAC and LA-PDAC. Moreover, the influence of dose reductions and the extent of dose reduction on the identification of suitable surgical candidates remains uncertain. There is an urgent need for further research to address these critical questions.
Comparative efficacy of primary chemoradiotherapy versus chemotherapy alone in LA-PDAC
Primary chemotherapy is typically favored in LA-PDAC due to its ability to achieve systemic disease control and potentially induce downstaging of the primary tumor. However, it may not adequately address local disease control in all patients.
Primary chemoradiotherapy combines the cytotoxic effects of chemotherapy with the locoregional control provided by radiotherapy. In theory, it should be beneficial for LA-PDAC where achieving local disease control is a priority. Studies evaluating primary chemoradiotherapy in LA-PDAC have shown promising results in terms of local tumor response, downstaging, and achieving negative surgical margins. However, chemoradiotherapy does not seem to improve overall survival. A meta-analysis of 5 randomized controlled trials revealed that chemoradiotherapy did not confer a survival advantage compared to chemotherapy alone but increased the rates of grade 3 to 4 adverse events [43, 44].
Some patients receive primary chemotherapy followed by consolidation radiotherapy. Although these patients are not initially considered surgical candidates, some of them may eventually undergo surgery due to stable disease and good clinical conditions. However, surgery in these patients is technically more complex due to the consolidation of radiotherapy effects into retroperitoneal scarring tissue. Whenever possible, radiotherapy should be used for neoadjuvant purposes.
The choice of oncological treatment in LA-PDAC is often based on the practices and preferences of individual institutions. Therefore, defining the optimal treatment pathway is a key research objective.
Appropriate timing for surgical resection post-neoadjuvant/primary chemoradiotherapy
The optimal timing for surgical resection in patients with BR-PDAC or LA-PDAC following neoadjuvant or primary chemoradiotherapy is still a topic of debate and ongoing research.
A study demonstrated that prolonging the interval between completion of chemoradiotherapy and surgery, with continued chemotherapy, for up to 20 weeks was linked with several benefits. These included an enhanced pathologic response and an extended median overall survival [45].
However, despite these findings, consensus has yet to be reached regarding the precise timeframe for surgery after chemoradiotherapy in these patient populations. Consequently, determining the optimal timing for surgical intervention after chemoradiotherapy remains a significant research objective.
Role of ablation therapies
Different ablation techniques have been developed and proposed especially for LA-PDAC. Non-thermal ablation techniques include irreversible electroporation, stereotactic body radiation, photodynamic therapy, and brachytherapy. Thermal ablation therapies include high-intensity focused ultra-sound, cryoablation, radiofrequency ablation, microwave ablation, and laser-induced thermotherapy. Irreversible electroporation holds significant promise; however, to date, all of these approaches are still considered investigational and lack an established role in the management of BR-PDAC and LA-PDAC [46, 47].
Management of patients with oligometastasis and LA-PDAC
PDAC often exhibits early metastatic dissemination. Initially, metastases may be microscopic and undetectable. Once metastases become visible, regardless of their number, the disease is considered systemic, and treatment typically revolves around chemotherapy.
The concept of oligometastasis has emerged as a result of recent advancements in oncology. In this scenario, the number and sites of metastases are limited making localized cancer treatments of potential benefit. Examples include liver metastases from colorectal cancer, lung metastases from various primary tumors, and adrenal metastases from lung cancer [48]. However, a clear definition specifying the maximum number of metastases qualifying as oligometastasis is lacking.
In PDAC, metastases are primarily found in the liver, peritoneum, or lungs. Lung metastases may exhibit a less aggressive biological behavior. Resection of isolated lung metastases in PDAC is already considered a treatment option for carefully selected patients [49]. In the abdomen, the concept of oligometastasis primarily pertains to liver metastases. Generally, in patients who demonstrate a robust response to chemotherapy over 8–9 months and exhibit no signs of tumor progression shortly after discontinuing chemotherapy, resection of liver metastases alongside the primary tumor is being considered for carefully selected individuals [50].
In LA-PDAC, the concept of oligometastasis has not been extensively explored, likely due to concerns regarding the complexity of surgery. Furthermore, when metastases were initially occult, distinguishing between synchronous metastases that responded to treatment and metastases that developed despite oncology treatments can be challenging.
Future studies should endeavor to establish a clear definition of oligometastasis in PDAC and elucidate its prognostic implications and treatment options, particularly for LA-PDAC.
Conclusions
The REDISCOVER consensus conference marks a milestone by introducing the first surgical guidelines for BR-PDAC and LA-PDAC. This manuscript presents a management algorithm derived from these guidelines and discusses unresolved clinical questions.
The REDISCOVER guidelines unequivocally mark a shift in the indication for resection of BR-PDAC and LA-PDAC, prioritizing tumor biology over anatomical features as the primary indication for resection. These guidelines also underscore the necessity of revising the anatomical definition of LA-PDAC, as shown by the discrepancy in surgical recommendations based on involvement of the celiac trunk versus the superior mesenteric artery. Furthermore, the current definition of LA-PDAC includes the scenario of an unreconstructible superior mesenteric/portal vein, signifying the tumor as unresectable by definition, regardless of considerations about treatment response and tumor biology. Finally, the new definition should aim to establish a clearer distinction between BR-PDAC and LA-PDAC.
Finally, it is important to refine existing management strategies. The establishment of the REDISCOVER registry (https://rediscover.unipi.it/) holds promise as a unified research platform aimed at advancing our understanding and improving the management of BR-PDAC and LA-PDAC.
Data availability
This manuscript provides guidelines on the perioperative care of surgical patients with borderline and locally advanced pancreatic cancer. As such, it followed the methodology required for this type of action that does not require individual patient data. Detailed results of systematic literature reviews can be provided, upon reasonable request.
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Acknowledgements
REDISCOVER guidelines group (Institutions): Division of Hepato-Pancreato-Biliary Surgery and Liver Transplantation, Hôpital de Hautepierre-Hôpitaux Universitaires de Strasbourg, Université de Strasbourg, Strasbourg, France; Gemelli Pancreatic Center, CRMPG (Advanced Pancreatic Research Center), Fondazione Policlinico Universitario "Agostino Gemelli" IRCCS, Rome, Italy; Department of Clinical and Experimental Sciences, University of Brescia and UOC General Surgery, ASST Cremona, Italy; Division of Pancreatic Surgery, Pancreas Translational and Clinical Research Center, IRCCS San Raffaele Scientific Institute, Vita-Salute University, Milan, Italy; Division of General and Transplant Surgery, University of Pisa, Pisa, Italy; Department of General Surgery & HPB Unit, APSS, Trento, Italy; Division of Pancreatobiliary Surgery and Liver Transplantation, Department of Surgery, Bellvitge University Hospital, IDIBELL, L´Hospitalet de Llobregat, Barcelona, Spain; Hepatopancreatobiliary Surgery, Pederzoli Hospital, Peschiera del Garda, Verona, Italy; Research Unit of General Surgery, Department of Medicine and Surgery, University Campus, Bio-Medico di Roma, Via Alvaro del Portillo 200,00128 Rome, Italy; Operative Research Unit of General Surgery, Fondazione Policlinico Universitario Campus, Bio-Medico, Roma, Italy; Department of Internal Medicine and Surgery (DIMEC), Alma Mater Studiorum, University of Bologna, Italy, Division of Pancreatic Surgery, IRCCS, Azienda Ospedaliero-Universitaria di Bologna (IRCCS AOUBO); Pancreas Center, The First Affiliated Hospital of Nanjing Medical University; Pancreas Institute, Nanjing Medical University; Department of General Surgery, The First Affiliated Hospital of Nanjing Medical University; Department of General Surgery, “G. Mazzini” Hospital, Teramo, Italy; Department of General and Emergency Surgery, AUSL Toscana Sud Est, Misericordia Hospital of Grosseto, Italy; Division of General, Oncological and Robotic Surgery, San Giuseppe Moscati Hospital, Avellino Italy; Department of Medicine and Surgery, HPB Unit, University of Parma, Parma, Italy; Division of HPB Surgery and Transplantation, Niguarda Hospital, University of Milano-Bicocca, Milan, Italy; Department of Surgery, Erasmus MC Cancer Institute, Erasmus University Medical Center, Rotterdam, the Netherlands; Department of Surgery, University of Colorado School of Medicine. Aurora, Colorado, USA; Hepato-Pancreato-Biliary Surgery and Liver Transplantation Unit, University of Modena and Reggio Emilia, Modena, Italy; Surgical Oncology, Pierangeli Clinic, Department of Innovative Technology in Medicine & Dentistry, G. D’Annunzio University Chieti-Pescara, Italy; Department of HPB surgery and liver transplantation, Beaujon hospital, Clichy, France. University Paris Cité, Paris, France; Division of HPB Surgery, Department of Surgery, NorthShore University HealthSystem, Evanston, IL, USA; Department for Surgical Oncology and HPB Surgery, Ilyinskaya Hospital, Moscow, Russia; Department of Medical and Surgical Sciences—DIMEC; Alma Mater Studiorum Università di Bologna; Bologna, Italy; Department of General Surgery and Transplantation. San Camillo Forlanini Hospital-POIT. Rome, Italy; Division of Minimally-invasive Surgical Oncology, ASST Grande Ospedale Metropolitano Niguarda, Milan, Italy; Department of General and Oncological Surgery, "Umberto I" Mauriziano Hospital, Turin, Italy; Department of Surgery Galliera Hospital, Genova, Italy; Division of HepatoBiliaryPancreatic Surgery, AOU Careggi, Department of Experimental and Clinical Medicine, University of Florence, Florence, Italy; Department for the Treatment and Study of Abdominal Diseases and Abdominal Transplantation, Istituto di Ricovero e Cura a Carattere Scientifico-Istituto Mediterraneo per i Trapianti e Terapie ad Alta Specializzazione (IRCCS-ISMETT), University of Pittsburgh Medical Center Italy (UPMC Italy), Palermo, Italy; Department of General Surgery and Medical-Surgical Specialties, University of Catania, Catania, Italy; Department of general visceral and thoracic surgery, University Hospital Eppendorf University of Hamburg, Hamburg, Germany; Department of Surgery, Alma Mater Studiorum University of Bologna, IRCCS Azienda Ospedaliera Universitaria di Bologna; The University of Texas MD Anderson Cancer Center, Houston, TX, USA; Department of Surgery, University Medical Center Schleswig–Holstein, Campus Lübeck, Lübeck, Germany; Department of High Technology Surgery, Moscow Clinical Scientific Center. Moscow, Russia; Department of Surgery, Hirakata Kohsai Hospital, Osaka, Japan; Department of Surgery, Emory University School of Medicine, Atlanta, GA, USA; University Medical Centre of the Johannes Gutenberg University Mainz, Germany; General and Pancreatic Surgery Unit, Pancreas Institute, University of Verona, Verona, Italy; Department of Surgery, Regional Hospital of Treviso, Treviso, Italy; Department of Oncology and Hemato-oncology, University of Milan; HPB Surgery and Liver Transplantation Fondazione IRCCS Istituto Nazionale Tumori, Milan, Italy; Department of HPB Surgery, Miulli Hospital, Acquaviva delle Fonti, Bari, Italy; Pancreas Center, The Affiliated BenQ Hospital of Nanjing Medical University, Nanjing, Jiangsu Province, People's Republic of China; Research Institute against Digestive Cancer (IRCAD), Strasbourg, France; Department of General and Speciality Surgery, General and Pancreatic Surgery Team 1, AORN A. Cardarelli, Naples, Italy; Department of Gastrointestinal and Pediatric Surgery, Tokyo Medical University, Tokyo, Japan; Department of Surgery and Oncology, Graduate School of Medical Sciences, Kyushu University, Fukuoka, Japan; Division of General Surgery, Department of Surgery and Robotic, Annunziata Hub Hospital, School of Medicine Surgery and TD, University of Calabria, Cosenza, Italy; Department of Surgery, Division of HBP Surgery & Transplantation. Montpellier University Hospital School of Medicine, Montpellier, France; Pancreatic & Digestive Endocrine Surgery Research Group—Department of Surgery, Oncology and Gastroenterology, DiSCOG, University of Padua, Padua, Italy; Section for Upper Abdominal Surgery at the Department of Surgery, Sahlgrenska University Hospital, Gothenburg, Sweden; Department of Surgery at the Institute of Clinical Sciences, Sahlgrenska Academy, University of Gothenburg, Sweden; Second Department of Hepatopancreatobiliary Surgery, Chinese People's Liberation Army (PLA) General Hospital, Beijing 100,853, China; Division of General Surgery 2U—Liver Transplant Unit, Azienda Ospedaliero Universitaria Città della Salute e della Scienza di Torino, University of Turin, Turin, Italy; Division of General Surgery II and HPB Unit, A.O.U. Maggiore della Carità di Novara, Novara, Italy; Service de Chirurgie Générale, Mini-Invasive et Robotique, Centre Hôspitalier de Luxembourg, Luxembourg City, Luxembourg; Regional Hepato-Pancreato-Biliary Unit, Manchester Royal Infirmary, Manchester, UK; Department of General and Minimally Invasive Surgery, “Vito Fazzi” Hospital, Lecce, Italy; Luxembourg, Luxembourg, Luxembourg; Department of General Surgery, Division of Visceral Surgery, Medical University of Vienna, Vienna, Austria; Department of Precision and Regenerative Medicine and Ionian Area (DiMePre-J) University of Bari, Italy; Division of HBP, Minimally Invasive and Robotic Surgery, Transplantation Service, Federico II University Hospital—Naples, Italy; Department of Surgery, ASL3 Genovese, Genoa, Italy; Chirurgia Generale, Infermi Hospital Rimini, AUSL Romagna, Rimini, Italy; IRCCS Humanitas Research Hospital, Rozzano, Milan, Italy; Sanchinarro University Hospital, General Surgery Department, San Pablo University, CEU, Madrid, Spain; Division of General Surgery and Transplantation, Department of Biotechnological and Applied Clinical Sciences, University of L’Aquila, L’Aquila, Italy; Division of Hepatobiliary, Pancreatic and Transplantation Surgery, Polytechnic University of Marche, Ospedali Riuniti delle Marche, Ancona, Italy; Center for Advanced Treatment of Hepatobiliary and Pancreatic Diseases, Ageo Central General Hospital, Saitama, Japan; Second Division of Surgery-Treviso-Department of Surgery, Oncology and Gastroenterology, DiSCOG, University of Padua, Padua, Italy; Division of Surgical Oncology, University of Pittsburgh Medical Center, Pittsburgh, PA, USA; Department of Surgery, Indiana University School of Medicine, Indianapolis, IN, USA; Department of Surgery, Sapienza University of Rome, Rome, Italy; Department of Surgery, HEBIPA—Hepatobiliary and Pancreatic Unit, Hospital de Santo António, Centro Hospitalar Universitário do Porto, Porto, Portugal; Department HPB Surgery, Metropolitan Hospital, Athens, Greece; School of Medicine, Trinity College Dublin, Dublin, Ireland; Department of Surgery, Weill Cornell Medicine, New York-Presbyterian Hospital at Weill Cornell, New Yourk, NY, USA; Department of Biomedical Sciences, Humanitas University, Italy; Division of General and Digestive Surgery, Department of General Surgery, IRCCS Humanitas Research Hospital, Rozzano, Milan, Italy; Department of Surgery, Donald and Barbara Zucker School of Medicine at Hofstra/Northwell, Manhasset, NY, USA; Zucker School of Medicine at Hofstra, New Hyde Park, NY, USA; Department of Clinical and Experimental Sciences, Surgical Clinic, University of Brescia, Italy; Associazione per Donare la Vita Onlus, Pisa, Italy; Associazione Nastro Viola, Brescia, Italy; Associazione Oncologica Pisana P. Trivella, Pisa, Italy; Division of Radiology, Azienda Ospedaliero Universitaria Pisana, Pisa, Italy; Division of Pathology, University of Pisa, Pisa, Italy; Department of Oncology and Haematology, University Hospital of Modena, Modena, Italy; Institute of Pathology, Heinrich-Heine-University and University Hospital Duesseldorf, Duesseldorf, Germany; Radiotherapy Department, Università Cattolica del Sacro Cuore, Roma, Italy.; Radiotherapy Department, Fondazione Policlinico Universitario A. Gemelli IRCCS, Roma, Italy; Endoscopy Unit, Azienda Ospedaliero Universitaria Pisana, Pisa, Italy; Division of Medical Oncology, Department of Translational Research and New Technologies in Medicine and Surgery, Pisa University Hospital, Pisa, Italy; Department of Medical and Surgical Sciences, DIMEC, Alma Mater Studiorum University of Bologna, Bologna, Italy; Radiation Oncology, IRCCS Azienda Ospedaliero-Universitaria di Bologna, Bologna, Italy; Digestive and Interventional Endoscopy Unit, ASST Niguarda Hospital, Milan, Italy; Academic Radiology, Department of Translational Research, University of Pisa, Pisa, Italy; Division of Radiotherapy, Department of Translational Research and New Technologies in Medicine and Surgery, University of Pisa, Pisa, Italy; Università Vita-Salute San Raffaele, Milan, Italy; IRCCS Ospedale San Raffaele, Department of Medical Oncology, Milan, Italy; Department of Human Pathology in Adulthood and Childhood Gaetano Barresi, University of Messina, Messina, Italy; Medical Oncology, Department of Medical and Surgical Sciences, Fondazione Policlinico Universitario Agostino Gemelli IRCCS, Rome, Italy; Medical Oncology, Department of Translational Medicine and Surgery, Catholic University of the Sacred Heart, Rome, Italy; Unit of Medical Oncology, Azienda Ospedaliero-Universitaria Pisana, Pisa, Italy; Regional Center of Nuclear Medicine, University Hospital of Pisa, Pisa, Italy.
Authorship
The REDISCOVER guidelines are grounded in the preparatory work, online Delphi rounds, and in-person discussions of the REDISCOVER International Consensus Meeting (September 17–18, 2024, Pisa—Italy). The authors of this manuscript include members of the steering committee, members of the research groups, or individuals who made significant contributions to the development of the REDISCOVER guidelines. Therefore, all authors meet the criteria for authorship of this manuscript.
Funding
Open access funding provided by Università di Pisa within the CRUI-CARE Agreement. The REDISCOVER consensus conference received a main unrestricted grant from “Fondazione Pisa” (https://fondazionepisa.it/). The patient association “per donare la vita onlus” also provided an unrestricted grant (https://www.perdonarelavitaonlus.it/). The REDISCOVER occurred during the 125th National Congress of the Italian Society. The Italian Society (https://www.sicplus.it/) endorsed the consensus conference and warmly supported it this initiative. Finally, the University of Pisa (https://www.unipi.it/) and the Municipality of Pisa (https://www.comune.pisa.it/it) provided external support to the REDISCOVER consensus conference. Fondazione Pisa, Associazione per Donare la Vita Onlus, Società Italiana di Chirurgia, Università di Pisa, Comune di Pisa. There was no funding from commercial companies.
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S. George Barreto has the following conflicts of interest to disclose: support from Flinders Foundation grant: 49358025, NHMRC Ideas Grant: 2021009, Pankind 21.R7.INV.CB.UOSA.6.2. All the other authors have no conflict of interest to disclose.
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Boggi, U., Kauffmann, E.F., Napoli, N. et al. REDISCOVER guidelines for borderline-resectable and locally advanced pancreatic cancer: management algorithm, unanswered questions, and future perspectives. Updates Surg (2024). https://doi.org/10.1007/s13304-024-01860-0
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DOI: https://doi.org/10.1007/s13304-024-01860-0