Your search keyword '"B. Gala-Lopez"' showing total 35 results

1. 2021 Canadian Surgery Forum01. Design and validation of a unique endoscopy simulator using a commercial video game03. Is ethnicity an appropriate measure of health care marginalization?: A systematic review and meta-analysis of the outcomes of diabetic foot ulceration in the Aboriginal population04. Racial disparities in surgery — a cross-specialty matched comparison between black and white patients05. Starting late does not increase the risk of postoperative complications in patients undergoing common general surgical procedures06. Ethical decision-making during a health care crisis: a resource allocation framework and tool07. Ensuring stability in surgical training program leadership: a survey of program directors08. Introducing oncoplastic breast surgery in a community hospital09. Leadership development programs for surgical residents: a review of the literature10. Superiority of non-opioid postoperative pain management after thyroid and parathyroid operations: a systematic review and meta-analysis11. Timing of ERCP relative to cholecystectomy in patients with ductal gallstone disease12. A systematic review and meta-analysis of randomized controlled trials comparing intraoperative red blood cell transfusion strategies13. Postoperative outcomes after frail elderly preoperative assessment clinic: a single-institution Canadian perspective14. Selective opioid antagonists following bowel resection for prevention of postoperative ileus: a systematic review and meta-analysis15. Peer-to-peer coaching after bile duct injury16. Laparoscopic median arcuate ligament release: a video abstract17. Retroperitoneoscopic approach to adrenalectomy19. Endoscopic Zenker diverticulotomy: a video abstract20. Variability in surgeons’ perioperative management of pheochromocytomas in Canada21. The contribution of surgeon and hospital variation in transfusion practice to outcomes for patients undergoing elective gastrointestinal cancer surgery: a population-based analysis22. Perioperative transfusions for gastroesophageal cancers: risk factors and short- and long-term outcomes23. The association between frailty and time alive and at home after cancer surgery among older adults: a population-based analysis24. Psychological and workplace-related effects of providing surgical care during the COVID-19 pandemic in British Columbia, Canada25. Safety of venous thromboembolism prophylaxis in endoscopic retrograde cholangiopancreatography: a systematic review26. Complications and reintervention following laparoscopic subtotal cholecystectomy: a systematic review and meta-analysis27. Synchronization of pupil dilations correlates with team performance in a simulated laparoscopic team coordination task28. Receptivity to and desired design features of a surgical peer coaching program: an international survey9. Impact of the COVID-19 pandemic on rates of emergency department utilization due to general surgery conditions30. The impact of the current COVID-19 pandemic on the exposure of general surgery trainees to operative procedures31. Association between academic degrees and research productivity: an assessment of academic general surgeons in Canada32. Laparoscopic endoscopic cooperative surgery (LECS) for subepithelial gastric lesion: a video presentation33. Effect of the COVID-19 pandemic on acute care general surgery at an academic Canadian centre34. Opioid-free analgesia after outpatient general surgery: a pilot randomized controlled trial35. Impact of neoadjuvant immunotherapy or targeted therapies on surgical resection in patients with solid tumours: a systematic review and meta-analysis37. Surgical data recording in the operating room: a systematic review of modalities and metrics38. Association between nonaccidental trauma and neighbourhood socioeconomic status during the COVID-19 pandemic: a retrospective analysis39. Laparoscopic repair of a transdiaphragmatic gastropleural fistula40. Video-based interviewing in medicine: a scoping review41. Indocyanine green fluorescence angiography for prevention of anastomotic leakage in colorectal surgery: a cost analysis from the hospital payer’s perspective43. Perception or reality: surgical resident and faculty assessments of resident workload compared with objective data45. When illness and loss hit close to home: Do health care providers learn how to cope?46. Remote video-based suturing education with smartphones (REVISE): a randomized controlled trial47. The evolving use of robotic surgery: a population-based analysis48. Prophylactic retromuscular mesh placement for parastomal hernia prevention: a retrospective cohort study of permanent colostomies and ileostomies49. Intracorporeal versus extracorporeal anastomosis in laparoscopic right hemicolectomy: a retrospective cohort study on anastomotic complications50. A lay of the land — a description of Canadian academic acute care surgery models51. Emergency general surgery in Ontario: interhospital variability in structures, processes and models of care52. Trauma 101: a virtual case-based trauma conference as an adjunct to medical education53. Assessment of the National Surgical Quality Improvement Program Surgical Risk Calculator for predicting patient-centred outcomes of emergency general surgery patients in a Canadian health care system54. Sustainability of a narcotic reduction initiative: 1 year following the Standardization of Outpatient Procedure (STOP) Narcotics Study55. Barriers to transanal endoscopic microsurgery referral56. Geospatial analysis of severely injured rural patients in a geographically complex landscape57. Implementation of an incentive spirometry protocol in a trauma ward: a single-centre pilot study58. Impostor phenomenon is a significant risk factor for burnout and anxiety in Canadian resident physicians: a cross-sectional survey59. Understanding the influence of perioperative education on performance among surgical trainees: a single-centre experience60. The effect of COVID-19 pandemic on current and future endoscopic personal protective equipment practices: a national survey of 77 endoscopists61. Case report: delayed presentation of perforated sigmoid diverticulitis as necrotizing infection of the lower limb62. Investigating disparities in surgical outcomes in Canadian Indigenous populations63. Fundoplication is superior to medical therapy for Barrett esophagus disease regression and progression: a systematic review and meta-analysis64. Development of a novel online general surgery learning platform and a qualitative preimplementation analysis65. Hagfish slime exudate as a potential novel hemostatic agent: developing a standardized assessment protocol66. The effect of the first wave of the COVID-19 pandemic on surgical oncology case volumes and wait times67. Safety of same-day discharge in high-risk patients undergoing ambulatory general surgery68. External validation of the Codman score in colorectal surgery: a pragmatic tool to drive quality improvement69. Improved morbidity and gastrointestinal restoration rates without compromising survival rates for diverting loop ileostomy with colonic lavage versus total abdominal colectomy for fulminant Clostridioides difficile colitis: a multicentre retrospective cohort study70. Potential access to emergency general surgical care in Ontario71. Immersive virtual reality (iVR) improves procedural duration, task completion and accuracy in surgical trainees: a systematic review01. Clinical validation of the Canada Lymph Node Score for endobronchial ultrasound02. Venous thromboembolism in surgically treated esophageal cancer patients: a provincial population-based study03. Venous thromboembolism in surgically treated lung cancer patients: a population-based study04. Is frailty associated with failure to rescue after esophagectomy? A multi-institutional comparative analysis of outcomes05. Routine systematic sampling versus targeted sampling of lymph nodes during endobronchial ultrasound: a feasibility randomized controlled trial06. Gastric ischemic conditioning reduces anastomotic complications in patients undergoing esophagectomy: a systematic review and meta-analysis07. Move For Surgery, a novel preconditioning program to optimize health before thoracic surgery: a randomized controlled trial08. In case of emergency, go to your nearest emergency department — Or maybe not?09. Does preoperative SABR increase the risk of complications from lung cancer resection? A secondary analysis of the MISSILE trial10. Segmental resection for lung cancer: the added value of near-infrared fluorescence mapping diminishes with surgeon experience11. Toward competency-based continuing professional development for practising surgeons12. Stereotactic body radiotherapy versus surgery in older adults with NSCLC — a population-based, matched analysis of long-term dependency outcomes13. Role of adjuvant therapy in esophageal cancer patients after neoadjuvant therapy and curative esophagectomy: a systematic review and meta-analysis14. Evaluation of population characteristics on the incidence of thoracic empyema: an ecological study15. Determining the optimal stiffness colour threshold and stiffness area ratio cut-off for mediastinal lymph node staging using EBUS elastography and AI: a pilot study16. Quality assurance on the use of sequential compression stockings in thoracic surgery (QUESTs)17. The relationship between fissureless technique and prolonged air leak for patients undergoing video-assisted thoracoscopic lobectomy18. CXCR2 inhibition as a candidate for immunomodulation in the treatment of K-RAS-driven lung adenocarcinoma19. Assessment tools for evaluating competency in video-assisted thoracoscopic lobectomy: a systematic review20. Understanding the current practice on chest tube management following lung resection among thoracic surgeons across Canada21. Effect of routine jejunostomy tube insertion in esophagectomy: a systematic review and meta-analysis22. Recurrence of primary spontaneous pneumothorax following bullectomy with pleurodesis or pleurectomy: a retrospective analysis23. Surgical outcomes following chest wall resection and reconstruction24. Outcomes following surgical management of primary mediastinal nonseminomatous germ cell tumours25. Does robotic approach offer better nodal staging than thoracoscopic approach in anatomical resection for non–small cell lung cancer? A single-centre propensity matching analysis26. Competency assessment for mediastinal mass resection and thymectomy: design and Delphi process27. The contemporary significance of venous thromboembolism (deep venous thrombosis [DVT] and pulmonary embolus [PE]) in patients undergoing esophagectomy: a prospective, multicentre cohort study to evaluate the incidence and clinical outcomes of VTE after major esophageal resections28. Esophageal cancer: symptom severity at the end of life29. The impact of pulmonary artery reconstruction on postoperative and oncologic outcomes: a systematic review30. Association with surgical technique and recurrence after laparoscopic repair of paraesophageal hernia: a single-centre experience31. Enhanced recovery after surgery (ERAS) in esophagectomy32. Surgical treatment of esophageal cancer: trends in surgical approach and early mortality at a single institution over the past 18 years34. Adverse events and length of stay following minimally invasive surgery in paraesophageal hernia repair35. Long-term symptom control comparison of Dor and Nissen fundoplication following laparoscopic para-esophageal hernia repair: a retrospective analysis36. Willingness to pay: a survey of Canadian patients’ willingness to contribute to the cost of robotic thoracic surgery37. Radiomics in early-stage lung adenocarcinoma: a prediction tool for tumour immune microenvironments38. Effectiveness of intraoperative pyloric botox injection during esophagectomy: how often is endoscopic intervention required?39. An artificial intelligence algorithm for predicting lymph node malignancy during endobronchial ultrasound40. The effect of major and minor complications after lung surgery on length of stay and readmission41. Measuring cost of adverse events following thoracic surgery: a scoping review42. Laparoscopic paraesophageal hernia repair: characterization by hospital and surgeon volume and impact on outcomes43. NSQIP 5-Factor Modified Frailty Index predicts morbidity but not mortality after esophagectomy44. Trajectory of perioperative HRQOL and association with postoperative complications in thoracic surgery patients45. Variation in treatment patterns and outcomes for resected esophageal cancer at designated thoracic surgery centres46. Patient-reported pretreatment health-related quality of life (HRQOL) predicts short-term survival in esophageal cancer patients47. Analgesic efficacy of surgeon-placed paravertebral catheters compared with thoracic epidural analgesia after Ivor Lewis esophagectomy: a retrospective noninferiority study48. Rapid return to normal oxygenation after lung surgery49. Examination of local and systemic inflammatory changes during lung surgery01. Implications of near-infrared imaging and indocyanine green on anastomotic leaks following colorectal surgery: a systematic review and meta-analysis02. Repeat preoperative endoscopy after regional implementation of electronic synoptic endoscopy reporting: a retrospective comparative study03. Consensus-derived quality indicators for operative reporting in transanal endoscopic surgery (TES)04. Colorectal lesion localization practices at endoscopy to facilitate surgical and endoscopic planning: recommendations from a national consensus Delphi process05. Black race is associated with increased mortality in colon cancer — a population-based and propensity-score matched analysis06. Improved survival in a cohort of patients 75 years and over with FIT-detected colorectal neoplasms07. Laparoscopic versus open loop ileostomy reversal: a systematic review and meta-analysis08. Posterior mesorectal thickness as a predictor of increased operative time in rectal cancer surgery: a retrospective cohort study09. Improvement of colonic anastomotic healing in mice with oral supplementation of oligosaccharides10. How can we better identify patients with rectal bleeding who are at high risk of colorectal cancer?11. Assessment of long-term bowel dysfunction in rectal cancer survivors: a population-based cohort study12. Observational versus antibiotic therapy for acute uncomplicated diverticulitis: a noninferiority meta-analysis based on a Delphi consensus13. Radiotherapy alone versus chemoradiotherapy for stage I anal squamous cell carcinoma: a systematic review and meta-analysis14. Is the Hartmann procedure for diverticulitis obsolete? National trends in colectomy for diverticulitis in the emergency setting from 1993 to 201515. Sugammadex in colorectal surgery: a systematic review and meta-analysis16. Sexuality and rectal cancer treatment: a qualitative study exploring patients’ information needs and expectations on sexual dysfunction after rectal cancer treatment17. Video-based interviews in selection process18. Impact of delaying colonoscopies during the COVID-19 pandemic on colorectal cancer detection and prevention19. Opioid use disorder associated with increased anastomotic leak and major complications after colorectal surgery20. Effectiveness of a rectal cancer education video on patient expectations21. Robotic-assisted rectosigmoid and rectal cancer resection: implementation and early experience at a Canadian tertiary centre22. An online educational app for rectal cancer survivors with low anterior resection syndrome: a pilot study23. The effects of surgeon specialization on the outcome of emergency colorectal surgery24. Outcomes after colorectal cancer resections in octogenarians and older in a regional New Zealand setting — What are the predictors of mortality?25. Long-term outcomes after seton placement for perianal fistulae with and without Crohn disease26. A survey of patient and surgeon preference for early ileostomy closure following restorative proctectomy for rectal cancer — Why aren’t we doing it?27. Crohn disease independently associated with longer hospital admission after surgery28. Short-stay (≤ 1 d) diverting loop ileostomy closure can be selectively implemented without an increase in readmission and complication rates: an ACS-NSQIP analysis29. A comparison of perineal stapled rectal prolapse resection and the Altemeier procedure at 2 Canadian academic hospitals30. Mental health and substance use disorders predict 90-day readmission and postoperative complications following rectal cancer surgery31. Early discharge after colorectal cancer resection: trends and impact on patient outcomes32. Oral antibiotics without mechanical bowel preparation prior to emergency colectomy reduces the risk of organ space surgical site infections: a NSQIP propensity score matched study33. The impact of robotic surgery on a tertiary care colorectal surgery program, an assessment of costs and short-term outcomes — a Canadian perspective34. Should we scope beyond the age limit of guidelines? Adenoma detection rates and outcomes of screening and surveillance colonoscopies in patients aged 75–79 years35. Emergency department admissions for uncomplicated diverticulitis: a nationwide study36. Obesity is associated with a complicated episode of acute diverticulitis: a nationwide study37. Green indocyanine angiography for low anterior resection in patients with rectal cancer: a prospective before-and-after study38. The impact of age on surgical recurrence of fibrostenotic ileocolic Crohn disease39. A qualitative study to explore the optimal timing and approach for the LARS discussion01. Racial, ethnic and socioeconomic disparities in diagnosis, treatment and survival of patients with breast cancer: a SEER-based population analysis02. First-line palliative chemotherapy for esophageal and gastric cancer: practice patterns and outcomes in the general population03. Frailty as a predictor for postoperative outcomes following pancreaticoduodenectomy04. Synoptic electronic operative reports identify practice variation in cancer surgery allowing for directed interventions to decrease variation05. The role of Hedgehog signalling in basal-like breast cancer07. Clinical and patient-reported outcomes in oncoplastic breast conservation surgery from a single surgeon’s practice in a busy community hospital in Canada08. Upgrade rate of atypical ductal hyperplasia: 10 years of experience and predictive factors09. Time to first adjuvant treatment after oncoplastic breast reduction10. Preparing to survive: improving outcomes for young women with breast cancer11. Opioid prescription and consumption in patients undergoing outpatient breast surgery — baseline data for a quality improvement initiative12. Rectal anastomosis and hyperthermic intraperitoneal chemotherapy: Should we avoid diverting loop ileostomy?13. Delays in operative management of early-stage, estrogen-receptor positive breast cancer during the COVID-19 pandemic — a multi-institutional matched historical cohort study14. Opioid prescribing practices in breast oncologic surgery15. Oncoplastic breast reduction (OBR) complications and patient-reported outcomes16. De-escalating breast cancer surgery: Should we apply quality indicators from other jurisdictions in Canada?17. The breast cancer patient experience of telemedicine during COVID-1918. A novel ex vivo human peritoneal model to investigate mechanisms of peritoneal metastasis in gastric adenocarcinoma (GCa)19. Preliminary uptake and outcomes utilizing the BREAST-Q patient-reported outcomes questionnaire in patients following breast cancer surgery20. Routine elastin staining improves detection of venous invasion and enhances prognostication in resected colorectal cancer21. Analysis of exhaled volatile organic compounds: a new frontier in colon cancer screening and surveillance22. A clinical pathway for radical cystectomy leads to a shorter hospital stay and decreases 30-day postoperative complications: a NSQIP analysis23. Fertility preservation in young breast cancer patients: a population-based study24. Investigating factors associated with postmastectomy unplanned emergency department visits: a population-based analysis25. Impact of patient, tumour and treatment factors on psychosocial outcomes after treatment in women with invasive breast cancer26. The relationship between breast and axillary pathologic complete response in women receiving neoadjuvant chemotherapy for breast cancer01. The association between bacterobilia and the risk of postoperative complications following pancreaticoduodenectomy02. Surgical outcome and quality of life following exercise-based prehabilitation for hepatobiliary surgery: a systematic review and meta-analysis03. Does intraoperative frozen section and revision of margins lead to improved survival in patients undergoing resection of perihilar cholangiocarcinoma? A systematic review and meta-analysis04. Prolonged kidney procurement time is associated with worse graft survival after transplantation05. Venous thromboembolism following hepatectomy for colorectal metastases: a population-based retrospective cohort study06. Association between resection approach and transfusion exposure in liver resection for gastrointestinal cancer07. The association between surgeon volume and use of laparoscopic liver resection for gastrointestinal cancer08. Immune suppression through TIGIT in colorectal cancer liver metastases09. 'The whole is greater than the sum of its parts' — a combined strategy to reduce postoperative pancreatic fistula after pancreaticoduodenectomy10. Laparoscopic versus open synchronous colorectal and hepatic resection for metastatic colorectal cancer11. Identifying prognostic factors for overall survival in patients with recurrent disease following liver resection for colorectal cancer metastasis12. Modified Blumgart pancreatojejunostomy with external stenting in laparoscopic Whipple reconstruction13. Laparoscopic versus open pancreaticoduodenectomy: a single centre’s initial experience with introduction of a novel surgical approach14. Neoadjuvant chemotherapy versus upfront surgery for borderline resectable pancreatic cancer: a single-centre cohort analysis15. Thermal ablation and telemedicine to reduce resource utilization during the COVID-19 pandemic16. Cost-utility analysis of normothermic machine perfusion compared with static cold storage in liver transplantation in the Canadian setting17. Impact of adjuvant therapy on overall survival in early-stage ampullary cancers: a single-centre retrospective review18. Presence of biliary anaerobes enhances response to neoadjuvant chemotherapy in pancreatic ductal adenocarcinoma19. How does tumour viability influence the predictive capability of the Metroticket model? Comparing predicted-to-observed 5-year survival after liver transplant for hepatocellular carcinoma20. Does caudate resection improve outcomes in patients undergoing curative resection for perihilar cholangiocarcinoma? A systematic review and meta-analysis21. Appraisal of multivariable prognostic models for postoperative liver decompensation following partial hepatectomy: a systematic review22. Predictors of postoperative liver decompensation events following resection in patients with cirrhosis and hepatocellular carcinoma: a population-based study23. Characteristics of bacteriobilia and impact on outcomes after Whipple procedure01. Inverting the y-axis: the future of MIS abdominal wall reconstruction is upside down02. Progressive preoperative pneumoperitoneum: a single-centre retrospective study03. The role of radiologic classification of parastomal hernia as a predictor of the need for surgical hernia repair: a retrospective cohort study04. Comparison of 2 fascial defect closure methods for laparoscopic incisional hernia repair01. Hypoalbuminemia predicts serious complications following elective bariatric surgery02. Laparoscopic adjustable gastric band migration inducing jejunal obstruction associated with acute pancreatitis: aurgical approach of band removal03. Can visceral adipose tissue gene expression determine metabolic outcomes after bariatric surgery?04. Improvement of kidney function in patients with chronic kidney disease and severe obesity after bariatric surgery: a systematic review and meta-analysis05. A prediction model for delayed discharge following gastric bypass surgery06. Experiences and outcomes of Indigenous patients undergoing bariatric surgery: a mixed-methods scoping review07. What is the optimal common channel length in revisional bariatric surgery?08. Laparoscopic management of internal hernia in a 34-week pregnant woman09. Characterizing timing of postoperative complications following elective Roux-en-Y gastric bypass and sleeve gastrectomy10. Canadian trends in bariatric surgery11. Common surgical stapler problems and how to correct them12. Management of choledocholithiasis following Roux-en-Y gastric bypass: a systematic review and meta-analysis

Author

M. Connell, W. Lin, A. Jarrar, A. Mierzwa, J. Shiroky, Z. Cloutier, F. Deaninck, W. He, Y. Lee, S. Keshavjee, M. Fortin, C. McLean, M. Melland-Smith, J. Frigault, G. Chartrand, N. Zuker, S. Elbekri, Z. Mir, R. Gilbert, V. Smith, H. Shrader, Y. Essaji, A. Webb, J. Glinka, E. Waugh, L. Park, M. Lund, M. Lemke, D. Henault, J. Zuckerman, N. Hanna, F. Reyna-Sepulveda, T. Lenet, K. Verhoeff, M. Parapini, D. Lim, S. Langer, D. Nguyen, C. Mardinger, A. Allard-Coutu, D. Cyr, K. Allen, D. Ng, L. Cadili, H. Kapur, S. Mysuria, É. Di Lena, V. Pravong, A. Alqaydi, A. Hunter-Smith, N. Gagnon, A. DiPasquale, W. Marini, M. Jacobson, V. Li, S. Merchant, A. Azin, R. Szwimer, N. Kasteel, E. Papillon, N. Alghaithi, M. Hegagi, Z. Harra, V. Wiseman, E. Salama, J. Moon, H. Roy, J. Liang, Z. Bayat, N. Caminsky, M.K. Motamedi, R. Ruxton, O. AlAamer, O. Monton, M. Li, C. Brown, J. Holland, R. Selvam, V. Brissette, T. McKechnie, H. AlSulaim, G. Talwar, R. Garfinkle, K. Purich, R. Hajjar, C. Cahill, G. Johnson, A. Bruinooge, K. Graham, H. Wang, M. Robinson, V. Gupta, E. Peters, L. Qu, D. Jones, C. Finley, I. Churchill, N. Hunka, M. Kaafarani, Y. Patel, D. Le Nguyen, S. Abdul, M. Humer, D. Sisson, A. Al Rawahi, C. Huynh, B. Greenberg, Y. Shargall, S. Turner, A. Alghamedi, V. Resende, S. Brophy, L. Esther, A. Kammili, M. De Meo, R. Razzak, N. Mistry, R. Nayak, D. Hirpara, J. Alaichi, A. Ednie, M. Abbas, U. Jogiat, K. Sullivan, G. Akhtar-Danesh, R. He, L. Lan, K. Larsen, M. Abou Khalil, K. Guidolin, G. Pang, J. Drung, C. Li, H. Wilson, N. Patro, E. Schmitz, W. Sun, R. Liu, C. Dwyer, R. Raskin, R. Wigen, K. Singh, G. Skelhorne-Gross, A. Rosenzveig, H. Muaddi, K. Ren, A. Lee, E. Walser, H. Forbes, C. Kruse, P.E. Serrano Aybar, U. Do, D. Skubleny, A. Fecso, A. Miles, S. Balvardi, L. Lee, L. Kerr, L. Glass, K. D’Souza, M. Nguyen, A. Zhu, K. Nabata, E. Ertel, R. Guo, J. Gentles, F. Shariff, K. Hickey, A. Vergis, B. Unger, J. Park, L. Gillman, D. Pace, K. Lam-Tin-Cheung, S. Chadi, F. Quereshy, J. Catton, B. Rubin, J. Bell, J. Marangos, A. Heesters, T. Stuart-McEwan, F. Wright, N. Ahmed, A. Nadler, J. Hallet, L. Chen, H. Hwang, R. Sidhu, T. Scott, A. Karimuddin, A. Nguyen, J. Osborn, S. Wiseman, L. Baker, M. Vered, A. Zahrai, R. Shorr, A. Davis, D. McIsaac, A. Tinmouth, D. Fergusson, G. Martel, S. Rummel, M. Stefic-Cubic, M. Stewart, A. Melck, T. Anpalagan, S. Ichhpuniani, K. Ramji, C. Eskicioglu, S. Deng, B. Greene, M. Tsang, V. Palter, S. Jayaraman, A. Mann, J. Tittley, M. Cadeddu, A. Madani, J. Pasternak, D. Hong, A. Istl, E. Tang, D. Gray, N. Coburn, J. Callum, R. McLeod, E. Pearsall, Y. Lin, A. Turgeon, A. Mahar, P. Kriviraltcheva-Kaneva, J. Cools-Lartigue, L. Ferri, C. Mueller, B. Haas, B. Tillman, M. Guttman, T. Chesney, V. Zuk, A. Hsu, W. Chan, R. Vasdev, L. Cadili J. Ling, R. Warburton, M. Hameed, H. Williamson, P. Murphy, K. Leslie, J. Hawel, S. Zablotny, H. Roldan, X. Jiang, B. Zheng, J. Fiore, L. Feldman, G. Fried, S. Valanci, J. Cipolla, P. Kaneva, S. Demyttenaere, M. Boutros, M. Alhashemi, J. Shapiro, D. Bigam, J. Kung, J. Mosko, P. Hamilton, S. Ghosh, S. Widder, D. Schiller, C. El Kefraoui, M. Pook, N. Barone, H. Montgomery, P. Nguyen-Powanda, F. Rajabiyazdi, H. Elhaj, M. Lapointe-Gagner, G. Olleik, A. Antoun, N. Safa, E. Di Lena, S. Meterissian, A. Meguerditchian, F. Lee, G. Baldini, S. Parpia, L. Ruo, K. Tywonek, S. Lee, C. O’Neill, N. Faisal, A. Alfayyadh, M. Gundayao, B.M. Meyers, R. Habashi, M. Levin, K. Aldrich, T. Grantcharov, A. Langerman, R. Anantha, V. Fawcett, A. Hetherington, M. Gervais, G. Rakovich, R. Hu, R. Musselman, I. Raiche, H. Moloo, A. Elnahas, N. Alkhamesi, A. Alnumay, C. Schlachta, C. Zhang, S. Cristancho, M. Ott, B. Niu, F. Balaa, N. Gawad, Y. Qiu, K. Hamann, N. How, C. Leveille, A. Davidson, A. Eqbal, Y. Sardiwalla, M. Korostensky, E. Lee, I. Yang, T. Stukel, C. de Mestral, A. Nathens, P. Karanicolas, S. Lemieux, D. Breton, P. Bouchard, A. Bouchard, R. Grégoire, F. Letarte, G. Bouchard, S. Drolet, S. Avoine, J. Gagné, C. Thibault, N. Jutras Bouthillette, M. Gosselin, T. Stuleanu, N. Kolozsvari, R. Nenshi, A. Jerath, D. Gomez, T. Amir, E. Liu, S. Farquharson, R. Mao, J. Yan, R. Tin, R. Brisebois, N. Bradley, L. Hartford, J. Van Koughnett, K. Vogt, R. Hilsden, N. Parry, L. Allen, J. Jones, K. Neumann, M. Strickland, D. O’Dochartaigh, K. Lobay, A. Kabaroff, E. Chang, J. Beck, J. Davidson, S. Jones, T. Van Hooren, M. El Hafid, J. Dang, V. Mocanu, G. Lutzak, R. Sultanian, C. Wong, S. Karmali, M. Petrera, M. Pickell, R. Auer, B. Li, N. Switzer, A. Al Hinai, A. Cieply, H. Hawes, E. Joos, A. Saleh, P. Engels, M. Kwong, J. Ellsmere, D. Chang, M. Hutter, R. Spence, C. Vasilevsky, N. Morin, Y. Longtin, S. Liberman, P. Montpetit, M. Poirier, K. Mukherjee, H. Sebajang, R. Younan, F. Schwenter, E. De Broux, A. Beckett, J. Nantais, J. Kay, R. Lohre, O. Ayeni, D. Goel, D. de SA, D. Hylton, E. Bedard, S. Johnson, B. Laing, A. Valji, W. Hanna, N. Akhtar-Danesh, B. Kidane, J. Limbachia, F. Farrokhyar, G. Leontiadis, F. Xie, A. Seely, J. Spicer, K. Yasufuku, M. Beauchamp, J. Wald, L. Mbuagbaw, J. Agzarian, C. Fahim, O. Olaiya, H. Begum, D. Palma, A. Warner, R. Malthaner, D. Fortin, M. Qiabi, T. Nguyen, A. Louie, G. Rodrigues, B. Yaremko, J. Laba, R. Inculet, B. Mador, H. Lai, J. White, M. Kim, G. Darling, M. Rousseau, Y. Samarasinghe, M. Lee, L. Thiru, O. Levine, R. Juergens, S. Brogly, W. Li, D. Lougheed, D. Petsikas, A. Gatti, C. Anestee, S. Gilbert, S. Sundaresan, P. Villeneuve, D. Maziak, A. Ashrafi, N. Tregobov, N. Hassanzadeh, S. Stone, A. Panjwani, T. Bong, R. Bond, A. Hafizi, R. Rayes, S. Milette, M. Vagai, M. Usatii, A. Chandrasekaran, B. Giannias, F. Bourdeau, V. Sangwan, N. Bertos, C. Moraes, S. Huang, D. Quail, L. Walsh, S. Camilleri-Broet, P. Fiset, E. Bilgic, A. Quaiattini, M. Maurice-Ventouris, S. Najmeh, J. Lu, R. Malhan, K. Brennan, D. French, M. Momtazi, O. Solaja, L. Donahoe, P. Bedard, A. Hansen, M. De Perrot, A. Simone, J. Huang, S. Murthy, J. Lin, H. Li, M. Crowther, L. Linkins, E. Lau, L. Schneider, J. Douketis, C. Allen-Avodabo, L. Davis, H. Zhao, C. Sirois, D. Mulder, S. Aftab Abdul, C. Anstee, E. Delic, H. Sasewich, T. Islam, D. Low, M. Kay, B. Shayegan, A. Adili, F. Chouiali, N. Muthukrishnan, F. Maleki, K. Ovens, M. Gold, M. Sorin, R. Falutz, R. Forghani, R. Kennedy, R. Bigsby, S. Bharadwaj, S. Gowing, K. Pearce, S. Kumar, M. Gingrich, Z. Ahmadzai, K. Thavorn, A. Namavarian, A. Mohammed, S. Uddin, A. Behzadi, A. Brar, G. Buduhan, L. Tan, S. Srinathan, J. Levy, J. Ringash, R. Sutradhar, L. Bednarek, D. MacDonald, S. Enns, A. Tan, E. Poole, C. Pascoe, T. Karakach, A. Halayko, B. Fang, D. Birch, H. Singh, O. Hershorn, D. Hochman, R. Helewa, R. Robertson, M. Lipson, A. Afzal, A. Maclean, S. Roen, W. Buie, M. Chu, N. Amin, H. Jaffer, R. Rebello, A. Doumouras, M. Oliero, T. Cuisiniere, G. Fragoso, A. Calvé, S. Djediai, B. Annabi, C. Richard, M. Santos, Y. Zhou, S. Dodd, B. Ring, Y. Yuan, S. Dell’Aniello, S. Bhatnagar, G. Ghitulescu, J. Faria, P. Brassard, A. Amar-Zifkin, R. Daniel, M. Alqahtani, S. Al-Masrouri, A. Chen, A. Patel, N. Al Busaidi, M. Demian, H. MacRae, F. Alam, M. Cwintal, G. Rigas, A. Pang, D. Marinescu, M. Raval, P. Phang, A. Ghuman, S. Muncner, I. Mihajlovic, M. Dykstra, R. Snelgrove, A. Smith, N. AlSelaim, M. AlMalki, A. Al-osail, P. Manuel, F. Mohamed, S. Serahati, L. Rajendran, T. Phang, K. Alavi, I. Paquette, T. MacLean, S. Wexner, S. Steele, S. Patel, L. Bordeianou, P. Sylla, E. Kennedy, C. Victor, A. Govindarajan, Z. Baig, A. Karimmudin, D. Gill, N. Ginther, F. Alrashid, L. Zhang, P. MacDonald, S.M. Merchant, K. Wattie Barnett, A. Caycedo-Marulanda, S.V. Patel, G. Kaur, S. Bindra, A. Malhotra, C. Graham, A. MacLean, P. Beck, H. Jijon, J. Ferraz, W. Kong, B. Gyawali, T. Hanna, W. Chung, S. Nanji, C. Booth, A. Awan, P. Serrano, M. Chanco, V. Wen, N. Singh, L. Peiris, J. Pasieka, P. Ghatage, D. Buie, A. Bouchard-Fortier, L. Mack, W. Zheng, C. Swallow, M. Reedijk, Z. Prus-Czrnecka, L. Delmar, R. Villiard, É. Martel, A. Cadrin-Chênevert, É. Ledoux, C. Racicot, A. Bazzarelli, J. Pao, M. Zhang, E. McKevitt, U. Kuusk, N. Van Laeken, E. Bovill, K. Isaac, C. Dingee, C. Cuthbert, K. Fergus, L. Barbera, Y. Efegoma, D. Howell, S. Isherwood, N. Levasseur, A. Scheer, C. Simmons, A. Srikantham, C. Temple-Orberle, Y. Xu, K. Metcalfe, M. Quan, J. la, G. Digby, A. Brind’Amour, L. Sidéris, P. Dubé, L. De Guerke, S. Fortin, M. Auclair, B. Trilling, J. Tremblay, B. Hopkins, S. Wong, S. Dumitra, A. Bazarelli, K. DeGirolamo, A. Ali, D. Eymae, K. Lee, S. Brar, J. Conner, M. Magalhaes, C. Baliski, A. Sari, D. Messenger, D. Driman, N. Assarzadegan, A. Juda, M. Brar, R. Kirsch, A. Lamontagne, Y. Gamache, C. Lee, R. Duckworth, M. Brindle, F. Fraulin, L. Austen, J. Kortbeek, M. Hyndman, G. Jamjoum, Y. Yuan Xu, S. Kong, H. Retrouvey, I. Kerrebijn, K. Butler, A. O’Neill, T. Cil, T. Zhong, S. Hofer, D. McCready, N. Look Hong, J. Skipworth, A. Mah, S. Desai, S. Chung, C. Scudamore, M. Segedi, E. Vasilyeva, J. Li, P. Kim, A. Deprato, K. Dajani, R. Smoot, C. Tzeng, F. Rocha, L. Yohanathan, S. Cleary, K. Bertens, D. Badrudin, B. Gala-Lopez, X. Wei, Y. Kaliwal, A. Wei, B. Barrette, S. Pelletier, P. Thebault, E. Beaudry-Simoneau, Z. Rong, M. Plasse, A. Roy M. Dagenais, R. Létourneau, R. Lapointe, F. Vandenbroucke-Menu, B. Nguyen, G. Soucy, S. Turcotte, D. Quan, A. Skaro, G. Jada, J. Daza, H. Msallak, B. Zhang, A. Workneh, S. Faisal, R. Faisal, M. Fabbro, C. Gu, M. Claassen, G. Sapisochin, D. Breadner, S. Welch, E. Lester, A. Shapiro, D. Eurich, A. Nayyar, M. Suraju, S. Williams-Perez, P. Ear, C. Chan, M. Rivers-Bowerman, A. Costa, A. Stueck, N. Campbell, S. Allen, H. Golding, S. McKeown, J. Flemming, P. Groome, M. Djerboua, E. Girard, P. Morency-Potvin, M. Dagenais, A. Roy, R. Letourneau, E. Simoneau, M. Oakley, B. Misheva, Y. Bendavid, L. Smith, J. Tan, U. Kahn, X. Paré, A. Doyon, K. Schwenger, J. Yadav, S. Fischer, T. Jackson, J. Allard, A. Okrainec, S. Anvari, O. Lovrics, I. Aditya, A. Khondker, M. Walsh, K. Hardy, R. Romanescu, J. Linton, M. Fowler-Woods, A. Fowler-Woods, G. Shingoose, M. Zmudzinski, V. Archer, J. Abu Halimah, V. Boudreau, G. Marcil, A. Hardy-Henry, and J. Hagen

Subjects

Surgery

Published

2021

2. A Novel Pre-Vascularized Subcutaneous Site Safely Accommodates Stem Cell Derived Therapies for Treating Diabetes

Author

B, Gala-Lopez, primary

Published

2017

3. THE USE OF A MODIFIED HEPATOJEJUNOSTOMY IN LIVER TRANSPLANTATION

Author

J Gonzalez Escobar, J Copo Jorge, Danyel Elias da Cruz Perez, S Sainz Lopez, F Gonzalez Castillo, B Gala Lopez, R Sarría Duvergel, and O Clausell Wong

Subjects

Transplantation, medicine.medical_specialty, business.industry, medicine.medical_treatment, medicine, Liver transplantation, business, Surgery

Published

2008

4. 2024 Canadian Surgery Forum: Sept. 25-28, 2024.

Author

Li C, Guo M, Karimuddin A, Guo M, Li C, Karimuddin A, Sutherland J, Huo B, McKechnie T, Ortenzi M, Lee Y, Antoniou S, Mayol J, Ahmed H, Boudreau V, Ramji K, Eskicioglu C, de Jager P, Urbach D, Poole M, Abbad A, Al-Shamali H, Al-Faraj Z, Wen C, Pescarus R, Bechara R, Hong D, Park LJ, Marcucci M, Ofori S, Bogach J, Serrano PE, Simunovic M, Yang I, Cadeddu M, Marcaccio MJ, Borges FK, Nenshi R, Devereaux PJ, Urbanellis P, Douglas J, Nemeth E, Ellsmere J, Spence R, Cunningham J, Falk R, Skinner T, Ebert N, Galbraith L, Prins M, Joharifard S, Joos E, Orovec A, Lethbridge L, Spence R, Hoogerboord M, Stuart H, Bergeron AM, Yang I, Bogach J, Nguyen L, Reade C, Eiriksson L, Morais M, Hanley G, Mah S, Brar K, Seymour KA, Eckhouse SR, Sudan R, Greenberg JA, Portenier D, Jung JJ, Light A, Dingley B, Delisle M, Apte S, Mallick R, Hamilton T, Stuart H, Talbot M, McKinnon G, Jost E, Thiboutot E, Nessim C, Katote N, Drohan A, Spence R, Neumann K, Shi G, Leung R, Lim C, Van Oirschot M, Grant A, Knowles S, Van Koughnett JA, Brousseau K, Monette L, McIsaac D, Wherrett C, Mallick R, Workneh A, Ramsay T, Tinmouth A, Shaw J, Carrier FM, Fergusson D, Martel G, Cornacchia M, Ivankovic V, Mamalchi SA, Choi D, Glen P, Matar M, Balaa F, Caminsky N, Mashal S, Boulanger N, Watt L, Campbell J, Grushka J, Fata P, Wong E, Guo M, Karimuddin A, Sutherland J, Li C, Lin W, Karimuddin A, Huo B, Calabrese E, Kumar S, Slater B, Walsh DS, Vosburg W, Jogiat U, Turner S, Baracos V, Eurich D, Filafilo H, Bedard E, Khan S, Waddell T, Yasufuku K, Pierre A, Keshavjee S, Wakeam E, Donahoe L, Cypel M, Safieddine N, Ko M, Leighl N, Feng J, Yeung J, De Perrot M, Salvarrey A, Ahmadi N, Simone C, Sayf G, Parente D, Cheung V, Rabey MR, Cabanero M, Le LW, Pipinikas C, Chevalier A, Chaulk R, Sahai D, Malthaner R, Qiabi M, Fortin D, Inculet R, Nayak R, Campbell J, White P, Bograd A, Farivar A, Louie B, Berger G, French D, Houston S, Gallardo F, Macek B, Liu R, Kidane B, Hanna NM, Patel YS, Browne I, Provost E, Farrokhyar F, Haider E, Hanna WC, Johnson G, Okoli G, Askin N, Abou-Setta A, Singh H, Coxon-Meggy A, Cornish J, Group LISM, Sharma S, Khamar J, Petropolous JA, Ghuman A, Lin W, Li C, Brown C, Phang T, Raval M, Ghuman A, Clement E, Karimuddin A, McKechnie T, Khamar J, Chu C, Hatamnejad A, Jessani G, Lee Y, Doumouras A, Hong D, Eskicioglu C, Sticca G, Poirier M, Tremblay JF, Latulippe JF, Bendavid Y, Trépanier JS, Lacaille-Ranger A, Henri M, McKechnie T, Kazi T, Shi V, Grewal S, Aldarraji A, Brennan K, Patel S, Amin N, Doumouras A, Parpia S, Eskicioglu C, Bhandari M, Talwar G, McKechnie T, Khamar J, Heimann L, Anant S, Eskicioglu C, Shi V, McKechnie T, Anant S, Ahmed M, Sharma S, Talwar G, Hong D, Eskicioglu C, Kazi T, McKechnie T, Lee Y, Alsayari R, Talwar G, Doumouras A, Hong D, Eskicioglu C, Park LJ, Moloo H, Ramsay T, Thavorn K, Presseau J, Zwiep T, Martel G, Devereaux PJ, Talarico R, McIsaac DI, Lemke M, Lin W, Brown C, Clement E, Ghuman A, Phang T, Raval M, Karimuddin A, Li C, Lin W, Clement E, Ghuman A, Hague C, Karimuddin A, Phang PT, Raval M, Tiwari P, Vos P, Brown C, Ricci A, Farooq A, Patel S, Brennan K, Wiseman V, McKechnie T, Keeping A, Johnson P, Bentley H, Messak K, Bogach J, Pond G, Forbes S, Grubac V, Tsai S, Van Der Pol C, Simunovic M, Bondzi-Simpson A, Behman R, Ribeiro T, Perera S, Lofters A, Sutradhar R, Snyder R, Clarke C, Coburn N, Hallet J, Caminsky N, Chen A, Moon J, Brassard P, Marinescu D, Dumitra T, Salama E, Vasilevsky CA, Boutros M, Brennan K, McKechnie T, Wiseman V, Ricci A, Farooq A, Patel S, Kazi T, McKechnie T, Jessani G, Shi V, Sne N, Doumouras A, Hong D, Eskicioglu C, Jogendran M, Flemming J, Djerboua M, Korzeniowski M, Wilson B, Merchant S, Bennett S, Hickey K, Gill S, Breen Z, Harding K, Yaremko H, Power P, Mathieson A, Pace D, Neveu J, Bennett S, Wilson B, Chen N, Kong W, Patel S, Booth C, Merchant S, Bennett S, Nelson G, AlMarzooqi N, Jogendran M, Djerboua M, Wilson B, Flemming J, Merchant S, Park LJ, Wang C, Archer V, McKechnie T, Cohen D, Bogach J, Simunovic M, Serrano PE, Breau RH, Karanicolas P, Devereaux PJ, Nelson G, AlMarzooqi N, Merchant S, Bennett S, Charbonneau J, Gervais MK, Brind'Amour A, Singbo N, Soucisse ML, Sidéris L, Leblanc G, Tremblay JF, Dubé P, Kouzmina E, Castelo M, Hong NL, Hallet J, Coburn N, Write F, Nguyen L, Gandhi S, Jerzak K, Eisen A, Roberts A, Vidovic D, Cruickshank B, Helyer L, Giacomantonio C, Mir Z, Faleiro M, Hiebert S, Livingstone S, Walsh M, Gala-Lopez B, Jatana S, Krys D, Jogiat U, Kung J, Verhoeff K, Lenet T, Carrier FM, Brousseau K, Vandenbroucke-Menu F, Collin Y, Gilbert RWD, Segedi M, Khalil JA, Bertens KA, Balaa F, Fergusson DA, Martel G, Wherrett C, Mallette K, Monette L, Workneh A, Ruel M, Sabri E, Maddison H, Tokessym M, Wong PBY, Massicotte L, Chassé M, Perrault MA, Hamel-Perreault É, Park J, Lim S, Maltais V, Leung P, Ramsay T, Tinmouth A, Czarnecka Z, Dadheeech N, Pawlick R, Razavy H, Shapiro J, Pouramin P, Allen S, Gala-Lopez B, Amhis N, Hennessey RL, Yang Y, Guan R, Zhang Y, Meneghetti A, Chiu C, Srikrishnaraj D, Hawel J, Schlachta C, Elnahas A, Yilbas A, Mainprize M, Svendrovski A, Paasch C, Netto FS, Khamar J, McKechnie T, Hatamnejad A, Lee Y, Huo B, Passos E, Sne N, Eskicioglu C, Hong D, Bennett S, Flemming J, Djerboua M, Wiseman V, Moore J, Szasz P, Nanji S, Moore J, Wiseman V, Szasz P, Lunsky I, Nanji S, Flemming JA, Bennett S, McKeown S, Mouhammed O, Gibb C, Verhoeff K, Kim M, Strickland M, Anantha R, Georgescu I, Lee Y, Shin T, Tessier L, Javidan A, Jung J, Hong D, McKechnie T, Strong A, Kroh M, Dang J, Faran M, McKechnie T, O'Callaghan E, Anvari S, Hughes T, Crowther M, Anvari M, Doumouras A, Andalib A, Safar A, Bouchard P, Demyttenaere S, Court O, Parmar S, Brand B, Switzer N, Gil R, Aujla S, Schellenberg M, Owattanapanich N, Emigh B, Van Gent JM, Egodage T, Murphy PB, Ball C, Spencer AL, Vogt KN, Keeley JA, Doris S, Inaba K, Nantais J, Baxter N, Saskin R, Calzavara A, Gomez D, Le A, Dawe P, Hameed M, Hassanpour A, Shlomovitz E, Gomez D, Al-Sukhni E, Wiseman V, Patel S, Bennett S, Mir Z, Roberts S, Hawes H, Merali K, Morris R, de Moya M, Neideen T, Kastenmeier A, Somberg L, Holena D, Murphy P, Nantais J, Baxter N, Saskin R, Calzavara A, Gomez D, Naveed A, Deshpande U, Gomez D, Rezende-Neto J, Ahmed N, and Beckett A

Published

2024

5. Canadian National Pancreas Conference 2023: A Review of Multidisciplinary Engagement in Pancreatic Cancer Care.

Author

Nickerson JL, Cyr C, Arseneau RJ, Lee SN, Condon-Oldreive S, Zogopoulos G, Roberts K, Kim CA, Ng SSW, Haider M, Villalba E, Stephenson L, Tsang E, Johnston B, Gala-Lopez B, Cooper V, Hannon B, Gangloff A, Gill S, Servidio-Italiano F, and Ramjeesingh R

Subjects

Humans, Canada, Pancreatic Neoplasms therapy

Abstract

Pancreatic cancer is a complex malignancy associated with poor prognosis and high symptom burden. Optimal patient care relies on the integration of various sectors in the healthcare field as well as innovation through research. The Canadian National Pancreas Conference (NPC) was co-organized and hosted by Craig's Cause Pancreatic Cancer Society and The Royal College of Physicians and Surgeons in November 2023 in Montreal, Canada. The conference sought to bridge the gap between Canadian healthcare providers and researchers who share the common goal of improving the prognosis, quality of life, and survival for patients with pancreatic cancer. The accredited event featured discussion topics including diagnosis and screening, value-based and palliative care, pancreatic enzyme replacement therapy, cancer-reducing treatment, and an overview of the current management landscape. The present article reviews the NPC sessions and discusses the presented content with respect to the current literature.

Published

2024

6. 2023 Canadian Surgery Forum: Sept. 20-23, 2023.

Author

Brière R, Émond M, Benhamed A, Blanchard PG, Drolet S, Habashi R, Golbon B, Shellenberger J, Pasternak J, Merchant S, Shellenberger J, La J, Sawhney M, Brogly S, Cadili L, Horkoff M, Ainslie S, Demetrick J, Chai B, Wiseman K, Hwang H, Alhumoud Z, Salem A, Lau R, Aw K, Nessim C, Gawad N, Alibhai K, Towaij C, Doan D, Raîche I, Valji R, Turner S, Balmes PN, Hwang H, Hameed SM, Tan JGK, Wijesuriya R, Tan JGK, Hew NLC, Wijesuriya R, Lund M, Hawel J, Gregor J, Leslie K, Lenet T, McIsaac D, Hallet J, Jerath A, Lalu M, Nicholls S, Presseau J, Tinmouth A, Verret M, Wherrett C, Fergusson D, Martel G, Sharma S, McKechnie T, Talwar G, Patel J, Heimann L, Doumouras A, Hong D, Eskicioglu C, Wang C, Guo M, Huang L, Sun S, Davis N, Wang J, Skulsky S, Sikora L, Raîche I, Son HJ, Gee D, Gomez D, Jung J, Selvam R, Seguin N, Zhang L, Lacaille-Ranger A, Sikora L, McIsaac D, Moloo H, Follett A, Holly, Organ M, Pace D, Balvardi S, Kaneva P, Semsar-Kazerooni K, Mueller C, Vassiliou M, Al Mahroos M, Fiore JF Jr, Schwartzman K, Feldman L, Guo M, Karimuddin A, Liu GP, Crump T, Sutherland J, Hickey K, Bonisteel EM, Umali J, Dogar I, Warden G, Boone D, Mathieson A, Hogan M, Pace D, Seguin N, Moloo H, Li Y, Best G, Leong R, Wiseman S, Alaoui AA, Hajjar R, Wassef E, Metellus DS, Dagbert F, Loungnarath R, Ratelle R, Schwenter F, Debroux É, Wassef R, Gagnon-Konamna M, Pomp A, Richard CS, Sebajang H, Alaoui AA, Hajjar R, Dagbert F, Loungnarath R, Sebajang H, Ratelle R, Schwenter F, Debroux É, Wassef R, Gagnon-Konamna M, Pomp A, Santos MM, Richard CS, Shi G, Leung R, Lim C, Knowles S, Parmar S, Wang C, Debru E, Mohamed F, Anakin M, Lee Y, Samarasinghe Y, Khamar J, Petrisor B, McKechnie T, Eskicioglu C, Yang I, Mughal HN, Bhugio M, Gok MA, Khan UA, Fernandes AR, Spence R, Porter G, Hoogerboord CM, Neumann K, Pillar M, Guo M, Manhas N, Melck A, Kazi T, McKechnie T, Jessani G, Heimann L, Lee Y, Hong D, Eskicioglu C, McKechnie T, Tessier L, Archer V, Park L, Cohen D, Parpia S, Bhandari M, Dionne J, Eskicioglu C, Bolin S, Afford R, Armstrong M, Karimuddin A, Leung R, Shi G, Lim C, Grant A, Van Koughnett JA, Knowles S, Clement E, Lange C, Roshan A, Karimuddin A, Scott T, Nadeau K, Macmillan J, Wilson J, Deschenes M, Nurullah A, Cahill C, Chen VH, Patterson KM, Wiseman SM, Wen B, Bhudial J, Barton A, Lie J, Park CM, Yang L, Gouskova N, Kim DH, Afford R, Bolin S, Morris-Janzen D, McLellan A, Karimuddin A, Archer V, Cloutier Z, Berg A, McKechnie T, Wiercioch W, Eskicioglu C, Labonté J, Bisson P, Bégin A, Cheng-Oviedo SG, Collin Y, Fernandes AR, Hossain I, Ellsmere J, El-Kefraoui C, Do U, Miller A, Kouyoumdjian A, Cui D, Khorasani E, Landry T, Amar-Zifkin A, Lee L, Feldman L, Fiore J, Au TM, Oppenheimer M, Logsetty S, AlShammari R, AlAbri M, Karimuddin A, Brown C, Raval MJ, Phang PT, Bird S, Baig Z, Abu-Omar N, Gill D, Suresh S, Ginther N, Karpinski M, Ghuman A, Malik PRA, Alibhai K, Zabolotniuk T, Raîche I, Gawad N, Mashal S, Boulanger N, Watt L, Razek T, Fata P, Grushka J, Wong EG, Hossain I, Landry M, Mackey S, Fairbridge N, Greene A, Borgoankar M, Kim C, DeCarvalho D, Pace D, Wigen R, Walser E, Davidson J, Dorward M, Muszynski L, Dann C, Seemann N, Lam J, Harding K, Lowik AJ, Guinard C, Wiseman S, Ma O, Mocanu V, Lin A, Karmali S, Bigam D, Harding K, Greaves G, Parker B, Nguyen V, Ahmed A, Yee B, Perren J, Norman M, Grey M, Perini R, Jowhari F, Bak A, Drung J, Allen L, Wiseman D, Moffat B, Lee JKH, McGuire C, Raîche I, Tudorache M, Gawad N, Park LJ, Borges FK, Nenshi R, Jacka M, Heels-Ansdell D, Simunovic M, Bogach J, Serrano PE, Thabane L, Devereaux PJ, Farooq S, Lester E, Kung J, Bradley N, Best G, Ahn S, Zhang L, Prince N, Cheng-Boivin O, Seguin N, Wang H, Quartermain L, Tan S, Shamess J, Simard M, Vigil H, Raîche I, Hanna M, Moloo H, Azam R, Ko G, Zhu M, Raveendran Y, Lam C, Tang J, Bajwa A, Englesakis M, Reel E, Cleland J, Snell L, Lorello G, Cil T, Ahn HS, Dube C, McIsaac D, Smith D, Leclerc A, Shamess J, Rostom A, Calo N, Thavorn K, Moloo H, Laplante S, Liu L, Khan N, Okrainec A, Ma O, Lin A, Mocanu V, Karmali S, Bigam D, Bruyninx G, Georgescu I, Khokhotva V, Talwar G, Sharma S, McKechnie T, Yang S, Khamar J, Hong D, Doumouras A, Eskicioglu C, Spoyalo K, Rebello TA, Chhipi-Shrestha G, Mayson K, Sadiq R, Hewage K, MacNeill A, Muncner S, Li MY, Mihajlovic I, Dykstra M, Snelgrove R, Wang H, Schweitzer C, Wiseman SM, Garcha I, Jogiat U, Baracos V, Turner SR, Eurich D, Filafilo H, Rouhi A, Bédard A, Bédard ELR, Patel YS, Alaichi JA, Agzarian J, Hanna WC, Patel YS, Alaichi JA, Provost E, Shayegan B, Adili A, Hanna WC, Mistry N, Gatti AA, Patel YS, Farrokhyar F, Xie F, Hanna WC, Sullivan KA, Farrokhyar F, Patel YS, Liberman M, Turner SR, Gonzalez AV, Nayak R, Yasufuku K, Hanna WC, Mistry N, Gatti AA, Patel YS, Cross S, Farrokhyar F, Xie F, Hanna WC, Haché PL, Galvaing G, Simard S, Grégoire J, Bussières J, Lacasse Y, Sassi S, Champagne C, Laliberté AS, Jeong JY, Jogiat U, Wilson H, Bédard A, Blakely P, Dang J, Sun W, Karmali S, Bédard ELR, Wong C, Hakim SY, Azizi S, El-Menyar A, Rizoli S, Al-Thani H, Fernandes AR, French D, Li C, Ellsmere J, Gossen S, French D, Bailey J, Tibbo P, Crocker C, Bondzi-Simpson A, Ribeiro T, Kidane B, Ko M, Coburn N, Kulkarni G, Hallet J, Ramzee AF, Afifi I, Alani M, El-Menyar A, Rizoli S, Al-Thani H, Chughtai T, Huo B, Manos D, Xu Z, Kontouli KM, Chun S, Fris J, Wallace AMR, French DG, Giffin C, Liberman M, Dayan G, Laliberté AS, Yasufuku K, Farivar A, Kidane B, Weessies C, Robinson M, Bednarek L, Buduhan G, Liu R, Tan L, Srinathan SK, Kidane B, Nasralla A, Safieddine N, Gazala S, Simone C, Ahmadi N, Hilzenrat R, Blitz M, Deen S, Humer M, Jugnauth A, Buduhan G, Kerr L, Sun S, Browne I, Patel Y, Hanna W, Loshusan B, Shamsil A, Naish MD, Qiabi M, Nayak R, Patel R, Malthaner R, Pooja P, Roberto R, Greg H, Daniel F, Huynh C, Sharma S, Vieira A, Jain F, Lee Y, Mousa-Doust D, Costa J, Mezei M, Chapman K, Briemberg H, Jack K, Grant K, Choi J, Yee J, McGuire AL, Abdul SA, Khazoom F, Aw K, Lau R, Gilbert S, Sundaresan S, Jones D, Seely AJE, Villeneuve PJ, Maziak DE, Pigeon CA, Frigault J, Drolet S, Roy ÈM, Bujold-Pitre K, Courval V, Tessier L, McKechnie T, Lee Y, Park L, Gangam N, Eskicioglu C, Cloutier Z, McKechnie T (McMaster University), Archer V, Park L, Lee J, Patel A, Hong D, Eskicioglu C, Ichhpuniani S, McKechnie T, Elder G, Chen A, Logie K, Doumouras A, Hong D, Benko R, Eskicioglu C, Castelo M, Paszat L, Hansen B, Scheer A, Faught N, Nguyen L, Baxter N, Sharma S, McKechnie T, Khamar J, Wu K, Eskicioglu C, McKechnie T, Khamar J, Lee Y, Tessier L, Passos E, Doumouras A, Hong D, Eskicioglu C, McKechnie T, Khamar J, Sachdeva A, Lee Y, Hong D, Eskicioglu C, Fei LYN, Caycedo A, Patel S, Popa T, Boudreau L, Grin A, Wang T, Lie J, Karimuddin A, Brown C, Phang T, Raval M, Ghuman A, Candy S, Nanda K, Li C, Snelgrove R, Dykstra M, Kroeker K, Wang H, Roy H, Helewa RM, Johnson G, Singh H, Hyun E, Moffatt D, Vergis A, Balmes P, Phang T, Guo M, Liu J, Roy H, Webber S, Shariff F, Helewa RM, Hochman D, Park J, Johnson G, Hyun E, Robitaille S, Wang A, Maalouf M, Alali N, Elhaj H, Liberman S, Charlebois P, Stein B, Feldman L, Fiore JF Jr, Lee L, Hu R, Lacaille-Ranger A, Ahn S, Tudorache M, Moloo H, Williams L, Raîche I, Musselman R, Lemke M, Allen L, Samarasinghe N, Vogt K, Brackstone M, Zwiep T, Clement E, Lange C, Alam A, Ghuman A, Karimuddin A, Phang T, Raval M, Brown C, Clement E, Liu J, Ghuman A, Karimuddin A, Phang T, Raval M, Brown C, Mughal HN, Gok MA, Khan UA, Mughal HN, Gok MA, Khan UA, Mughal HN, Gok MA, Khan UA, Mughal HN, Gok MA, Khan UA, James N, Zwiep T, Van Koughnett JA, Laczko D, McKechnie T, Yang S, Wu K, Sharma S, Lee Y, Park L, Doumouras A, Hong D, Parpia S, Bhandari M, Eskicioglu C, McKechnie T, Tessier L, Lee S, Kazi T, Sritharan P, Lee Y, Doumouras A, Hong D, Eskicioglu C, McKechnie T, Lee Y, Hong D, Dionne J, Doumouras A, Parpia S, Bhandari M, Eskicioglu C, Hershorn O, Ghuman A, Karimuddin A, Brown C, Raval M, Phang PT, Chen A, Boutros M, Caminsky N, Dumitra T, Faris-Sabboobeh S, Demian M, Rigas G, Monton O, Smith A, Moon J, Demian M, Garfinkle R, Vasilevsky CA, Rajabiyazdi F, Boutros M, Courage E, LeBlanc D, Benesch M, Hickey K, Hartwig K, Armstrong C, Engelbrecht R, Fagan M, Borgaonkar M, Pace D, Shanahan J, Moon J, Salama E, Wang A, Arsenault M, Leon N, Loiselle C, Rajabiyazdi F, Boutros M, Brennan K, Rai M, Farooq A, McClintock C, Kong W, Patel S, Boukhili N, Caminsky N, Faris-Sabboobeh S, Demian M, Boutros M, Paradis T, Robitaille S, Dumitra T, Liberman AS, Charlebois P, Stein B, Fiore JF Jr, Feldman LS, Lee L, Zwiep T, Abner D, Alam T, Beyer E, Evans M, Hill M, Johnston D, Lohnes K, Menard S, Pitcher N, Sair K, Smith B, Yarjau B, LeBlanc K, Samarasinghe N, Karimuddin AA, Brown CJ, Phang PT, Raval MJ, MacDonell K, Ghuman A, Harvey A, Phang PT, Karimuddin A, Brown CJ, Raval MJ, Ghuman A, Hershorn O, Ghuman A, Karimuddin A, Raval M, Phang PT, Brown C, Logie K, Mckechnie T, Lee Y, Hong D, Eskicioglu C, Matta M, Baker L, Hopkins J, Rochon R, Buie D, MacLean A, Ghuman A, Park J, Karimuddin AA, Phang PT, Raval MJ, Brown CJ, Farooq A, Ghuman A, Patel S, Macdonald H, Karimuddin A, Raval M, Phang PT, Brown C, Wiseman V, Brennan K, Patel S, Farooq A, Merchant S, Kong W, McClintock C, Booth C, Hann T, Ricci A, Patel S, Brennan K, Wiseman V, McClintock C, Kong W, Farooq A, Kakkar R, Hershorn O, Raval M, Phang PT, Karimuddin A, Ghuman A, Brown C, Wiseman V, Farooq A, Patel S, Hajjar R, Gonzalez E, Fragoso G, Oliero M, Alaoui AA, Rendos HV, Djediai S, Cuisiniere T, Laplante P, Gerkins C, Ajayi AS, Diop K, Taleb N, Thérien S, Schampaert F, Alratrout H, Dagbert F, Loungnarath R, Sebajang H, Schwenter F, Wassef R, Ratelle R, Debroux É, Cailhier JF, Routy B, Annabi B, Brereton NJB, Richard C, Santos MM, Gimon T, MacRae H, de Buck van Overstraeten A, Brar M, Chadi S, Kennedy E, Baker L, Hopkins J, Rochon R, Buie D, MacLean A, Park LJ, Archer V, McKechnie T, Lee Y, McIsaac D, Rashanov P, Eskicioglu C, Moloo H, Devereaux PJ, Alsayari R, McKechnie T, Ichhpuniani S, Lee Y, Eskicioglu C, Hajjar R, Oliero M, Fragoso G, Ajayi AS, Alaoui AA, Rendos HV, Calvé A, Cuisinière T, Gerkins C, Thérien S, Taleb N, Dagbert F, Sebajang H, Loungnarath R, Schwenter F, Ratelle R, Wassef R, Debroux E, Richard C, Santos MM, Kennedy E, Simunovic M, Schmocker S, Brown C, MacLean A, Liberman S, Drolet S, Neumann K, Stotland P, Jhaveri K, Kirsch R, Alnajem H, Alibrahim H, Giundi C, Chen A, Rigas G, Munir H, Safar A, Sabboobeh S, Holland J, Boutros M, Kennedy E, Richard C, Simunovic M, Schmocker S, Brown C, MacLean A, Liberman S, Drolet S, Neumann K, Stotland P, Jhaveri K, Kirsch R, Bruyninx G, Gill D, Alsayari R, McKechnie T, Lee Y, Hong D, Eskicioglu C, Zhang L, Abtahi S, Chhor A, Best G, Raîche I, Musselman R, Williams L, Moloo H, Caminsky NG, Moon JJ, Marinescu D, Pang A, Vasilevsky CA, Boutros M, Al-Abri M, Gee E, Karimuddin A, Phang PT, Brown C, Raval M, Ghuman A, Morena N, Ben-Zvi L, Hayman V, Hou M (University of Calgary), Nguyen D, Rentschler CA, Meguerditchian AN, Mir Z, Fei L, McKeown S, Dinchong R, Cofie N, Dalgarno N, Cheifetz R, Merchant S, Jaffer A, Cullinane C, Feeney G, Jalali A, Merrigan A, Baban C, Buckley J, Tormey S, Benesch M, Wu R, Takabe K, Benesch M, O'Brien S, Kazazian K, Abdalaty AH, Brezden C, Burkes R, Chen E, Govindarajan A, Jang R, Kennedy E, Lukovic J, Mesci A, Quereshy F, Swallow C, Chadi S, Habashi R, Pasternak J, Marini W, Zheng W, Murakami K, Ohashi P, Reedijk M, Hu R, Ivankovic V, Han L, Gresham L, Mallick R, Auer R, Ribeiro T, Bondzi-Simpson A, Coburn N, Hallet J, Cil T, Fontebasso A, Lee A, Bernard-Bedard E, Wong B, Li H, Grose E, Brandts-Longtin O, Aw K, Lau R, Abed A, Stevenson J, Sheikh R, Chen R, Johnson-Obaseki S, Nessim C, Hennessey RL, Meneghetti AT, Bildersheim M, Bouchard-Fortier A, Nelson G, Mack L, Ghasemi F, Naeini MM, Parsyan A, Kaur Y, Covelli A, Quereshy F, Elimova E, Panov E, Lukovic J, Brierley J, Burnett B, Swallow C, Eom A, Kirkwood D, Hodgson N, Doumouras A, Bogach J, Whelan T, Levine M, Parvez E, Ng D, Kazazian K, Lee K, Lu YQ, Kim DK, Magalhaes M, Grigor E, Arnaout A, Zhang J, Yee EK, Hallet J, Look Hong NJ, Nguyen L, Coburn N, Wright FC, Gandhi S, Jerzak KJ, Eisen A, Roberts A, Ben Lustig D, Quan ML, Phan T, Bouchard-Fortier A, Cao J, Bayley C, Watanabe A, Yao S, Prisman E, Groot G, Mitmaker E, Walker R, Wu J, Pasternak J, Lai CK, Eskander A, Wasserman J, Mercier F, Roth K, Gill S, Villamil C, Goldstein D, Munro V, Pathak A (University of Manitoba), Lee D, Nguyen A, Wiseman S, Rajendran L, Claasen M, Ivanics T, Selzner N, McGilvray I, Cattral M, Ghanekar A, Moulton CA, Reichman T, Shwaartz C, Metser U, Burkes R, Winter E, Gallinger S, Sapisochin G, Glinka J, Waugh E, Leslie K, Skaro A, Tang E, Glinka J, Charbonneau J, Brind'Amour A, Turgeon AF, O'Connor S, Couture T, Wang Y, Yoshino O, Driedger M, Beckman M, Vrochides D, Martinie J, Alabduljabbar A, Aali M, Lightfoot C, Gala-Lopez B, Labelle M, D'Aragon F, Collin Y, Hirpara D, Irish J, Rashid M, Martin T, Zhu A, McKnight L, Hunter A, Jayaraman S, Wei A, Coburn N, Wright F, Mallette K, Elnahas A, Alkhamesi N, Schlachta C, Hawel J, Tang E, Punnen S, Zhong J, Yang Y, Streith L, Yu J, Chung S, Kim P, Chartier-Plante S, Segedi M, Bleszynski M, White M, Tsang ME, Jayaraman S, Lam-Tin-Cheung K, Jayaraman S, Tsang M, Greene B, Pouramin P, Allen S, Evan Nelson D, Walsh M, Côté J, Rebolledo R, Borie M, Menaouar A, Landry C, Plasse M, Létourneau R, Dagenais M, Rong Z, Roy A, Beaudry-Simoneau E, Vandenbroucke-Menu F, Lapointe R, Ferraro P, Sarkissian S, Noiseux N, Turcotte S, Haddad Y, Bernard A, Lafortune C, Brassard N, Roy A, Perreault C, Mayer G, Marcinkiewicz M, Mbikay M, Chrétien M, Turcotte S, Waugh E, Sinclair L, Glinka J, Shin E, Engelage C, Tang E, Skaro A, Muaddi H, Flemming J, Hansen B, Dawson L, O'Kane G, Feld J, Sapisochin G, Zhu A, Jayaraman S, Cleary S, Hamel A, Pigeon CA, Marcoux C, Ngo TP, Deshaies I, Mansouri S, Amhis N, Léveillé M, Lawson C, Achard C, Ilkow C, Collin Y, Tai LH, Park L, Griffiths C, D'Souza D, Rodriguez F, McKechnie T, Serrano PE, Hennessey RL, Yang Y, Meneghetti AT, Panton ONM, Chiu CJ, Henao O, Netto FS, Mainprize M, Hennessey RL, Chiu CJ, Hennessey RL, Chiu CJ, Jatana S, Verhoeff K, Mocanu V, Jogiat U, Birch D, Karmali S, Switzer N, Hetherington A, Verhoeff K, Mocanu V, Birch D, Karmali S, Switzer N, Safar A, Al-Ghaithi N, Vourtzoumis P, Demyttenaere S, Court O, Andalib A, Wilson H, Verhoeff K, Dang J, Kung J, Switzer N, Birch D, Madsen K, Karmali S, Mocanu V, Wu T, He W, Vergis A, Hardy K, Zmudzinski M, Daenick F, Linton J, Zmudzinski M, Fowler-Woods M, He W, Fowler-Woods A, Shingoose G, Vergis A, Hardy K, Lee Y, Doumouras A, Molnar A, Nguyen F, Hong D, Schneider R, Fecso AB, Sharma P, Maeda A, Jackson T, Okrainec A, McLean C, Mocanu V, Birch D, Karmali S, Switzer N, MacVicar S, Dang J, Mocanu V, Verhoeff K, Jogiat U, Karmali S, Birch D, Switzer N, McLennan S, Verhoeff K, Purich K, Dang J, Kung J, Mocanu V, McLennan S, Verhoeff K, Mocanu V, Jogiat U, Birch DW, Karmali S, Switzer NJ, Jeffery L, Hwang H, Ryley A, Schellenberg M, Owattanapanich N, Emigh B, Nichols C, Dilday J, Ugarte C, Onogawa A, Matsushima K, Martin MJ, Inaba K, Schellenberg M, Emigh B, Nichols C, Dilday J, Ugarte C, Onogawa A, Shapiro D, Im D, Inaba K, Schellenberg M, Owattanapanich N, Ugarte C, Lam L, Martin MJ, Inaba K, Rezende-Neto J, Patel S, Zhang L, Mir Z, Lemke M, Leeper W, Allen L, Walser E, Vogt K, Ribeiro T, Bateni S, Bondzi-Simpson A, Coburn N, Hallet J, Barabash V, Barr A, Chan W, Hakim SY, El-Menyar A, Rizoli S, Al-Thani H, Mughal HN, Bhugio M, Gok MA, Khan UA, Warraich A, Gillman L, Ziesmann M, Momic J, Yassin N, Kim M, Makish A, Walser E, Smith S, Ball I, Moffat B, Parry N, Vogt K, Lee A, Kroeker J, Evans D, Fansia N, Notik C, Wong EG, Coyle G, Seben D, Smith J, Tanenbaum B, Freedman C, Nathens A, Fowler R, Patel P, Elrick T, Ewing M, Di Marco S, Razek T, Grushka J, Wong EG, Park LJ, Borges FK, Nenshi R, Serrano PE, Engels P, Vogt K, Di Sante E, Vincent J, Tsiplova K, Devereaux PJ, Talwar G, Dionne J, McKechnie T, Lee Y, Kazi T, El-Sayes A, Bogach J, Hong D, Eskicioglu C, Connell M, Klooster A, Beck J, Verhoeff K, Strickland M, Anantha R, Groszman L, Caminsky NG, Watt L, Boulanger N, Razek T, Grushka J, Di Marco S, Wong EG, Livergant R, McDonald B, Binda C, Luthra S, Ebert N, Falk R, and Joos E

Published

2023

7. The Use of Donation After Circulatory Death Organs for Simultaneous Liver-kidney Transplant: To DCD or Not to DCD?

Author

Vinson AJ, Gala-Lopez B, Tennankore K, and Kiberd B

Subjects

Cause of Death, Clinical Decision-Making, Graft Survival, Humans, Markov Chains, Postoperative Complications etiology, Quality-Adjusted Life Years, Risk Assessment, Risk Factors, Time Factors, Treatment Outcome, Waiting Lists, Decision Support Techniques, Donor Selection, Kidney Transplantation adverse effects, Kidney Transplantation mortality, Liver Transplantation adverse effects, Liver Transplantation mortality, Tissue Donors supply & distribution

Abstract

Background: Because of the challenges with organ scarcity, many centers performing simultaneous liver-kidney transplant (SLKT) are opting to accept donation after circulatory death (DCD) organs as a means of facilitating earlier transplant and reducing death rates on the waitlist. It has been suggested, however, that DCD organs may have inferior graft and patient survival posttransplant compared with donation after neurologic death (DND) organs., Methods: We created a Markov model to compare the overall outcomes of accepting a DCD SLKT now versus waiting for a DND SLKT in patients waitlisted for SLKT, stratified by base Model for End-Stage Liver Disease (MELD) score (≤20, 21-30, >30)., Results: Waiting for DND SLKT was the preferred treatment strategy for patients with a MELD score of 30 or less (incremental value of 0.54 and 0.36 quality-adjusted life years for MELD score of 20 or less and MELD score of 21 to 30 with DND versus DCD SLKT, respectively). The option to accept a DCD SLKT became the preferred choice for those with a MELD score greater than 30 (incremental value of 0.31 quality-adjusted life years for DCD versus DND SLKT). This finding was confirmed in a probabilistic sensitivity analysis and persisted when analyzing total life years obtained for accept DCD versus do not accept DCD., Conclusions: There is a benefit to accepting DCD SLKT for patients with MELD score greater than 30. Although not accepting DCD SLKT and waiting for DND SLKT is the preferred option for patients with MELD of 30 or less, the incremental value is small.

Published

2019

8. Bioengineered human pseudoislets form efficiently from donated tissue, compare favourably with native islets in vitro and restore normoglycaemia in mice.

Author

Yu Y, Gamble A, Pawlick R, Pepper AR, Salama B, Toms D, Razian G, Ellis C, Bruni A, Gala-Lopez B, Lu JL, Vovko H, Chiu C, Abdo S, Kin T, Korbutt G, Shapiro AMJ, and Ungrin M

Subjects

Animals, Apoptosis, Cell Survival, DNA analysis, Diabetes Mellitus, Experimental therapy, Female, Gene Expression Profiling, Glucose metabolism, Graft Survival, Humans, Hyperglycemia, Hypoxia, Insulin metabolism, Male, Mice, Mice, Transgenic, Diabetes Mellitus therapy, Insulin blood, Islets of Langerhans cytology, Islets of Langerhans Transplantation, Tissue Engineering

Abstract

Aims/hypothesis: Islet transplantation is a treatment option that can help individuals with type 1 diabetes become insulin independent, but inefficient oxygen and nutrient delivery can hamper islet survival and engraftment due to the size of the islets and loss of the native microvasculature. We hypothesised that size-controlled pseudoislets engineered via centrifugal-forced-aggregation (CFA-PI) in a platform we previously developed would compare favourably with native islets, even after taking into account cell loss during the process., Methods: Human islets were dissociated and reaggregated into uniform, size-controlled CFA-PI in our microwell system. Their performance was assessed in vitro and in vivo over a range of sizes, and compared with that of unmodified native islets, as well as islet cell clusters formed by a conventional spontaneous aggregation approach (in which dissociated islet cells are cultured on ultra-low-attachment plates). In vitro studies included assays for membrane integrity, apoptosis, glucose-stimulated insulin secretion assay and total DNA content. In vivo efficacy was determined by transplantation under the kidney capsule of streptozotocin-treated Rag1 -/- mice, with non-fasting blood glucose monitoring three times per week and IPGTT at day 60 for glucose response. A recovery nephrectomy, removing the graft, was conducted to confirm efficacy after completing the IPGTT. Architecture and composition were analysed by histological assessment via insulin, glucagon, pancreatic polypeptide, somatostatin, CD31 and von Willebrand factor staining., Results: CFA-PI exhibit markedly increased uniformity over native islets, as well as substantially improved glucose-stimulated insulin secretion (8.8-fold to 11.1-fold, even after taking cell loss into account) and hypoxia tolerance. In vivo, CFA-PI function similarly to (and potentially better than) native islets in reversing hyperglycaemia (55.6% for CFA-PI vs 20.0% for native islets at 500 islet equivalents [IEQ], and 77.8% for CFA-PI vs 55.6% for native islets at 1000 IEQ), and significantly better than spontaneously aggregated control cells (55.6% for CFA-PI vs 0% for spontaneous aggregation at 500 IEQ, and 77.8% CFA-PI vs 33.4% for spontaneous aggregation at 1000 IEQ; p < 0.05). Glucose clearance in the CFA-PI groups was improved over that in the native islet groups (CFA-PI 18.1 mmol/l vs native islets 29.7 mmol/l at 60 min; p < 0.05) to the point where they were comparable with the non-transplanted naive normoglycaemic control mice at a low IEQ of 500 IEQ (17.2 mmol/l at 60 min)., Conclusions/interpretation: The ability to efficiently reformat dissociated islet cells into engineered pseudoislets with improved properties has high potential for both research and therapeutic applications.

Published

2018

9. Determination of Minimal Hemoglobin Level Necessary for Normothermic Porcine Ex Situ Liver Perfusion.

Author

Bral M, Gala-Lopez B, Thiesen A, Hatami S, Bigam DL, Freed DM, and James Shapiro AM

Subjects

Animals, Aorta pathology, Cold Ischemia, Hepatic Artery, Hepatocytes enzymology, Hydrogen-Ion Concentration, Lactic Acid analysis, Liver enzymology, Liver Function Tests, Liver Transplantation, Oxygen chemistry, Oxygen Consumption, Swine, Temperature, Transaminases analysis, Vascular Resistance, Hemoglobins analysis, Liver pathology, Perfusion

Abstract

Background: In current studies of ex situ liver perfusion there exists considerable variability in perfusate composition, including the type of oxygen carrier. Herein, we aim to clarify the minimal hemoglobin level necessary during normothermic porcine ex situ liver perfusion., Methods: Livers procured from 35 to 45 kg domestic pigs were connected to our experimental ex situ circuit (n = 10). In the treatment group, perfusate was sequentially diluted hourly to predetermined hemoglobin levels. At the end of each hemoglobin dilution, perfusate samples were analyzed for liver transaminases, lactate dehydrogenase (LD), total bilirubin, and lactate levels. Liver oxygen consumption was measured. In the control group, livers were perfused continually for a duration of 24 hours at target hemoglobin levels of 30 and 20 g/L., Results: Rising liver transaminases, significantly higher lactate (P < 0.001), and LD levels (P < 0.001) were noted at lower perfusate hemoglobin levels in the treatment group. Liver oxygen utilization (P < 0.001) and hepatic artery oxygen delivery (P < 0.001) were significantly lower at lower hemoglobin levels, whereas liver vessel resistance remained relatively constant. Histology demonstrated increasing parenchymal damage at lower hemoglobin levels. In control livers, higher perfusate transaminases, higher lactate, and LD levels were noted at a perfusion hemoglobin level of 20 g/L., Conclusions: Ex situ liver function decompensated during perfusion between a mean hemoglobin level of 30 to 20 g/L, as evidenced by notably rising lactate and LD levels. This study demonstrates optimal hemoglobin concentration during normothermic ex situ liver perfusion to ensure a fully metabolically functioning graft.

Published

2018

10. BMX-001, a novel redox-active metalloporphyrin, improves islet function and engraftment in a murine transplant model.

Author

Bruni A, Pepper AR, Pawlick RL, Gala-Lopez B, Gamble A, Kin T, Malcolm AJ, Jones C, Piganelli JD, Crapo JD, and Shapiro AMJ

Subjects

Animals, Cells, Cultured, Diabetes Mellitus, Experimental metabolism, Diabetes Mellitus, Experimental pathology, Glucose pharmacology, Graft Survival, Humans, Insulin metabolism, Islets of Langerhans cytology, Islets of Langerhans metabolism, Islets of Langerhans Transplantation, Male, Mice, Mice, Inbred BALB C, Oxidation-Reduction, Superoxide Dismutase metabolism, Apoptosis drug effects, Biomimetic Materials pharmacology, Diabetes Mellitus, Experimental prevention & control, Islets of Langerhans drug effects, Metalloporphyrins pharmacology

Abstract

Islet transplantation has become a well-established therapy for select patients with type 1 diabetes. Viability and engraftment can be compromised by the generation of oxidative stress encountered during isolation and culture. We evaluated whether the administration of BMX-001 (MnTnBuOE-2-PyP 5+ [Mn(III) meso-tetrakis-(N-b-butoxyethylpyridinium-2-yl)porphyrin]) and its earlier derivative, BMX-010 (MnTE-2-PyP [Mn(III) meso-tetrakis-(N-methylpyridinium-2-yl)porphyrin]) could improve islet function and engraftment outcomes. Long-term culture of human islets with BMX-001, but not BMX-010, exhibited preserved in vitro viability. Murine islets isolated and cultured for 24 hours with 34 μmol/L BMX-001 exhibited improved insulin secretion (n = 3 isolations, P < .05) in response to glucose relative to control islets. In addition, 34 μmol/L BMX-001-supplemented murine islets exhibited significantly reduced apoptosis as indicated by terminal deoxynucleotidyl transferase dUTP nick end labeling, compared with nontreated control islets (P < .05). Murine syngeneic islets transplanted under the kidney capsule at a marginal dose of 150 islets revealed 58% of 34 μmol/L BMX-001-treated islet recipients became euglycemic (n = 11 of 19) compared with 19% of nontreated control islet recipients (n = 3 of 19, P < .05). Of murine recipients receiving a marginal dose of human islets cultured with 34 μmol/L BMX-001, 92% (n = 12 of 13) achieved euglycemia compared with 57% of control recipients (n = 8 of 14, P = .11). These results demonstrate that the administration of BMX-001 enhances in vitro viability and augments murine marginal islet mass engraftment., (© 2018 The American Society of Transplantation and the American Society of Transplant Surgeons.)

Published

2018

11. Ex situ liver perfusion: Organ preservation into the future.

Author

Bral M, Gala-Lopez B, Bigam DL, Freed DH, and Shapiro AMJ

Subjects

Humans, Liver Transplantation, Organ Preservation trends, Perfusion trends, Liver, Organ Preservation methods, Perfusion methods

Abstract

In recent years, remarkable progress has occurred in the development of technologies to support ex situ liver perfusion. Building upon extensive preclinical studies in large animal models, pilot and randomized clinical trials have been initiated, and preliminary outcomes suggest more optimal protection of both standard and extended criteria liver grafts. There currently exists an incredible opportunity and need to further refine this technology, determine appropriate viability measures to predict usable liver grafts, and to explore potent protective additive strategies to further optimize the quality of extended criteria organs. These findings will have major bearing in expanding the limited liver donor pool, and may save lives where up to a quarter of listed patients die on wait-lists. Herein we offer a brief overview of the history and current status of ex situ liver perfusion, and discuss future directions that will likely have major impact on the practice of clinical liver transplantation., (Copyright © 2018 Elsevier Inc. All rights reserved.)

Published

2018

12. Ferroptosis-inducing agents compromise in vitro human islet viability and function.

Author

Bruni A, Pepper AR, Pawlick RL, Gala-Lopez B, Gamble AF, Kin T, Seeberger K, Korbutt GS, Bornstein SR, Linkermann A, and Shapiro AMJ

Subjects

Animals, Carbolines pharmacology, Cells, Cultured, Cyclohexylamines pharmacology, Deferoxamine pharmacology, Glucose pharmacology, Humans, Insulin Secretion drug effects, Islets of Langerhans drug effects, L-Lactate Dehydrogenase metabolism, Mice, Inbred C57BL, Phenylenediamines pharmacology, Piperazines pharmacology, RNA, Messenger genetics, RNA, Messenger metabolism, gamma-Glutamylcyclotransferase genetics, gamma-Glutamylcyclotransferase metabolism, Apoptosis drug effects, Iron metabolism, Islets of Langerhans physiology, Tissue Survival drug effects

Abstract

Human islet transplantation has been hampered by donor cell death associated with the islet preparation procedure before transplantation. Regulated necrosis pathways are biochemically and morphologically distinct from apoptosis. Recently, ferroptosis was identified as a non-apoptotic form of iron-dependent regulated necrosis implicated in various pathological conditions. Mediators of islet oxidative stress, including glutathione peroxidase-4 (GPX4), have been identified as inhibitors of ferroptosis, and mechanisms that affect GPX4 function can impact islet function and viability. Ferroptosis has not been investigated directly in human islets, and its relevance in islet transplantation remains unknown. Herein, we sought to determine whether in vitro human islet viability and function is compromised in the presence of two distinct ferroptosis-inducing agents (FIA), erastin or RSL3, and whether these effects could be rescued with ferroptosis inhibitors, ferrostatin-1 (Fer-1), or desferrioxamine (DFO). Viability, as assessed by lactate dehydrogenase (LDH) release, revealed significant death in erastin- and RSL3-treated islets, 20.3% ± 3.8 and 24.4% ± 2.5, 24 h post culture, respectively. These effects were ameliorated in islets pre-treated with Fer-1 or the iron chelator, desferrioxamine (DFO). Stimulation index, a marker of islet function revealed a significant reduction in function in erastin-treated islets (control 1.97 ± 0.13 vs. 50 μM erastin 1.32 ± 0.1) (p < 0.05). Fer-1 and DFO pre-treatment alone did not augment islet viability or function. Pre-treatment of islets with erastin or Fer-1 did not impact in vivo engraftment in an immunodeficient mouse transplant model. Our data reveal that islets are indeed susceptible to ferroptosis in vitro, and induction of this novel cell death modality leads to compromised islet function, which can be recoverable in the presence of the ferroptosis inhibitors. The in vivo impact of this pathway in islet transplantation remains elusive given the constraints of our study, but warrants continued investigation.

Published

2018

13. Engraftment Site and Effectiveness of the Pan-Caspase Inhibitor F573 to Improve Engraftment in Mouse and Human Islet Transplantation in Mice.

Author

Pepper AR, Bruni A, Pawlick R, Wink J, Rafiei Y, Gala-Lopez B, Bral M, Abualhassan N, Kin T, and Shapiro AMJ

Subjects

Animals, Biomarkers blood, Blood Glucose metabolism, Cell Survival drug effects, Diabetes Mellitus, Experimental blood, Diabetes Mellitus, Experimental chemically induced, Diabetes Mellitus, Type 1 blood, Diabetes Mellitus, Type 1 chemically induced, Enzyme Activation, Heterografts, Humans, Islets of Langerhans enzymology, Islets of Langerhans pathology, Male, Mice, Inbred C57BL, Signal Transduction drug effects, Streptozocin, Time Factors, Tissue Culture Techniques, Amino Acid Chloromethyl Ketones pharmacology, Apoptosis drug effects, Caspase 3 metabolism, Caspase Inhibitors pharmacology, Diabetes Mellitus, Experimental surgery, Diabetes Mellitus, Type 1 surgery, Graft Survival drug effects, Islets of Langerhans drug effects, Islets of Langerhans surgery, Islets of Langerhans Transplantation methods

Abstract

Background: Islet transplantation is an effective therapy in type 1 diabetes and recalcitrant hypoglycemia. However, there is an ongoing need to circumvent islet loss posttransplant. We explore herein the potential of the pan-caspase inhibitor F573 to mitigate early apoptosis-mediated islet death within portal and extrahepatic portal sites in mice., Methods: Mouse or human islets were cultured in standard media ±100 μM F573 and subsequently assessed for viability and apoptosis via terminal deoxynucleotidyl transferase dUTP nick end labeling staining and caspase-3 activation. Diabetic mice were transplanted with syngeneic islets placed under the kidney capsule (KC) or into the subcutaneous deviceless (DL) site at a marginal islet dose (150 islets), or into the portal vein (PV) at a full dose (500 islets). Human islets were transplanted under the KC of diabetic immunodeficient mice at a marginal dose (500 islet equivalents). Islets were cultured in the presence of F573, and F573 was administered subcutaneously on days 0 to 5 posttransplant. Control mice were transplanted with nontreated islets and were injected with saline. Graft function was measured by nonfasting blood glucose and glucose tolerance testing., Results: F573 markedly reduced human and mouse islet apoptosis after in vitro culture (P < 0.05 and P < 0.05, respectively). Furthermore, F573 improved human islet function when transplanted under the KC (P < 0.05); whereas F573 did not enhance murine islet marginal KC transplants. Conversely, F573 significantly improved mouse islet engraftment in the PV and DL site (P < 0.05 and P < 0.05, respectively)., Conclusions: The pan-caspase inhibitor F573 markedly reduces human and mouse islet apoptosis and improves engraftment most effectively in the portal and DL subcutaneous sites.

Published

2017

14. Low energy X-ray (grenz ray) treatment of purified islets prior to allotransplant markedly decreases passenger leukocyte populations.

Author

Pawlick R, Gala-Lopez B, Pepper AR, Abualhassan N, Bruni A, Suzuki K, Rayat G, Elliott JF, and Shapiro AMJ

Subjects

Animals, Antibodies, Monoclonal administration & dosage, Antibodies, Monoclonal adverse effects, Antibodies, Monoclonal therapeutic use, CTLA-4 Antigen antagonists & inhibitors, Cell Survival radiation effects, Combined Modality Therapy adverse effects, Diabetes Mellitus, Experimental drug therapy, Diabetes Mellitus, Experimental immunology, Diabetes Mellitus, Experimental metabolism, Dose-Response Relationship, Drug, Dose-Response Relationship, Radiation, Graft Rejection immunology, Graft Rejection metabolism, Graft Rejection pathology, Graft Survival drug effects, Graft Survival radiation effects, Hyperglycemia prevention & control, Immunosuppression Therapy adverse effects, Immunosuppressive Agents administration & dosage, Immunosuppressive Agents adverse effects, Immunosuppressive Agents therapeutic use, Islets of Langerhans immunology, Islets of Langerhans metabolism, Islets of Langerhans Transplantation immunology, Islets of Langerhans Transplantation pathology, Leukocytes immunology, Leukocytes metabolism, Leukocytes pathology, Male, Mice, Inbred BALB C, Mice, Inbred C57BL, Recombinant Proteins administration & dosage, Recombinant Proteins adverse effects, Recombinant Proteins therapeutic use, Tissue Culture Techniques, X-Rays, Diabetes Mellitus, Experimental surgery, Graft Rejection prevention & control, Islets of Langerhans radiation effects, Islets of Langerhans Transplantation adverse effects, Leukocytes radiation effects

Abstract

Grenz rays, or minimally penetrating X-rays, are known to be an effective treatment of certain recalcitrant immune-mediated skin diseases, but their use in modulating allograft rejection has not been tested. We examined the capacity of grenz ray treatment to minimize islet immunogenicity and extend allograft survival in a mouse model. In a preliminary experiment, 1 of 3 immunologically intact animals demonstrated long-term acceptance of their grenz ray treated islet allograft. Further experiments revealed that 28.6% (2 of 7) grenz ray treated islet allografts survived >60 d. A low dose of 20Gy, was important; a 4-fold increase in radiation resulted in rapid graft failure, and transplanting a higher islet mass did not alter this outcome. To determine whether increased islet allograft survival after grenz treatment would be masked by immunosuppression, we treated the recipients with CTLA-4 Ig, and found an additive effect, whereby 17.5% more animals accepted the graft long-term versus those with CTLA-4 Ig alone. Cell viability assays verified that islet integrity was maintained after treatment with 20Gy. As well, through splenocyte infiltration analysis, donor CD4+ T cell populations 24-hours after transplant were decreased by more than16-fold in recipients receiving irradiated islets compared with control. Donor CD8+ T cell populations, although less prevalent, decreased in all treatment groups compared with control. Our results suggest that brief treatment of isolated islets with low energy grenz rays before allotransplantation can significantly reduce passenger leukocytes and promote graft survival, possibly by inducing donor dendritic cells to differentiate toward a tolerogenic phenotype.

Published

2017

15. Transplantation of Human Pancreatic Endoderm Cells Reverses Diabetes Post Transplantation in a Prevascularized Subcutaneous Site.

Author

Pepper AR, Pawlick R, Bruni A, Wink J, Rafiei Y, O'Gorman D, Yan-Do R, Gala-Lopez B, Kin T, MacDonald PE, and Shapiro AMJ

Subjects

Animals, Blood Glucose analysis, Blood Glucose metabolism, C-Peptide metabolism, Calcium metabolism, Cell Differentiation, Diabetes Mellitus, Experimental chemically induced, Diabetes Mellitus, Experimental therapy, Endoderm cytology, Endoderm metabolism, Human Embryonic Stem Cells cytology, Human Embryonic Stem Cells metabolism, Humans, Injections, Subcutaneous, Insulin-Secreting Cells cytology, Insulin-Secreting Cells metabolism, Mice, Oxygen Consumption, Transplantation, Heterologous, Endoderm transplantation, Neovascularization, Physiologic physiology, Pancreas cytology

Abstract

Beta-cell replacement therapy is an effective means to restore glucose homeostasis in select humans with autoimmune diabetes. The scarcity of "healthy" human donor pancreata restricts the broader application of this effective curative therapy. "β-Like" cells derived from human embryonic stem cells (hESC), with the capacity to secrete insulin in a glucose-regulated manner, have been developed in vitro, with limitless capacity for expansion. Here we report long-term diabetes correction in mice transplanted with hESC-derived pancreatic endoderm cells (PECs) in a prevascularized subcutaneous site. This advancement mitigates chronic foreign-body response, utilizes a device- and growth factor-free approach, facilitates in vivo differentiation of PECs into glucose-responsive insulin-producing cells, and reliably restores glycemic control. Basal and stimulated human C-peptide secretion was detected throughout the study, which was abolished upon graft removal. Recipient mice demonstrated physiological clearance of glucose in response to metabolic challenge and safely retrieved grafts contained viable glucose regulatory cells., (Copyright © 2017 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2017

16. Preliminary Single-Center Canadian Experience of Human Normothermic Ex Vivo Liver Perfusion: Results of a Clinical Trial.

Author

Bral M, Gala-Lopez B, Bigam D, Kneteman N, Malcolm A, Livingstone S, Andres A, Emamaullee J, Russell L, Coussios C, West LJ, Friend PJ, and Shapiro AM

Subjects

Adolescent, Adult, Aged, Extracorporeal Circulation, Female, Graft Survival, Humans, Liver Function Tests, Male, Middle Aged, Tissue Donors, Young Adult, Liver Transplantation, Organ Preservation methods, Perfusion methods, Postoperative Complications, Warm Ischemia

Abstract

After extensive experimentation, outcomes of a first clinical normothermic machine perfusion (NMP) liver trial in the United Kingdom demonstrated feasibility and clear safety, with improved liver function compared with standard static cold storage (SCS). We present a preliminary single-center North American experience using identical NMP technology. Ten donor liver grafts were procured, four (40%) from donation after circulatory death (DCD), of which nine were transplanted. One liver did not proceed because of a technical failure with portal cannulation and was discarded. Transplanted NMP grafts were matched 1:3 with transplanted SCS livers. Median NMP was 11.5 h (range 3.3-22.5 h) with one DCD liver perfused for 22.5 h. All transplanted livers functioned, and serum transaminases, bilirubin, international normalized ratio, and lactate levels corrected in NMP recipients similarly to controls. Graft survival at 30 days (primary outcome) was not statistically different between groups on an intent-to-treat basis (p = 0.25). Intensive care and hospital stays were significantly more prolonged in the NMP group. This preliminary experience demonstrates feasibility as well as potential technical risks of NMP in a North American setting and highlights a need for larger, randomized studies., (© 2016 The American Society of Transplantation and the American Society of Transplant Surgeons.)

Published

2017

17. Long-term function and optimization of mouse and human islet transplantation in the subcutaneous device-less site.

Author

Pepper AR, Bruni A, Pawlick RL, Gala-Lopez B, Rafiei Y, Wink J, Kin T, and Shapiro AM

Subjects

Animals, Blood Glucose, Humans, Male, Mice, Diabetes Mellitus, Experimental pathology, Graft Survival, Islets of Langerhans pathology, Islets of Langerhans Transplantation methods

Abstract

Clinical islet transplantation has routinely been demonstrated to be an efficacious means of restoring glycemic control in select patients with autoimmune diabetes. Notwithstanding marked progress and improvements, the broad-spectrum application of this treatment option is restricted by the complications associated with intrahepatic portal cellular infusion and the scarcity of human donor pancreata. Recent progress in stem cell biology has demonstrated that the potential to expand new β cells for clinical transplantation is now a reality. As such, research focus is being directed toward optimizing safe extrahepatic transplant sites to house future alternative β cell sources for clinical use. The present study expands on our previous development of a prevascularized subcutaneous device-less (DL) technique for cellular transplantation, by demonstrating long-term (>365 d) durable syngeneic murine islet graft function. Furthermore, histological analysis of tissue specimens collected immediately post-DL site creation and acutely post-human islet transplantation demonstrates that this technique results in close apposition of the neovascularized collagen to the transplanted cells without dead space, thereby avoiding hypoxic luminal dead-space. Murine islets transplanted into the DL site created by a larger luminal diameter (6-Fr.) (n = 11), reversed diabetes to the similar capacity as our standard DL method (5-Fr.)(n = 9). Furthermore, glucose tolerance testing did not differ between these 2 transplant groups (p > 0 .05). Taken together, this further refinement of the DL transplant approach facilitates a simplistic means of islet infusion, increases the transplant volume capacity and may provide an effective microenvironment to house future alternative β cell sources.

Published

2016

18. Reparixin, a CXCR1/2 inhibitor in islet allotransplantation.

Author

Pawlick RL, Wink J, Pepper AR, Bruni A, Abualhassen N, Rafiei Y, Gala-Lopez B, Bral M, and Shapiro AM

Subjects

Animals, Diabetes Mellitus, Experimental immunology, Diabetes Mellitus, Type 1 immunology, Glucose Tolerance Test, Graft Rejection immunology, Graft Survival immunology, Islets of Langerhans Transplantation immunology, Male, Mice, Mice, Inbred BALB C, Sulfonamides pharmacology, Diabetes Mellitus, Experimental surgery, Diabetes Mellitus, Type 1 surgery, Graft Rejection prevention & control, Graft Survival drug effects, Islets of Langerhans Transplantation methods, Sulfonamides therapeutic use

Abstract

Quality of life in Type 1 diabetic patients may be improved with islet transplantation, but lifelong immunosuppression is required to prevent rejection. Allo-immune response is a key player in graft dysfunction and although the adaptive immune response is well characterized, the effect of the innate immune reaction after transplantation is only recently becoming appreciated. In this study, we address how the innate response affects long-term outcomes in a murine islet allotransplant model. CTLA-4 Ig treatment is known to significantly prolong kidney subcapsular islet allograft survival and enhance glucose tolerance. The combination of CTLA-4 Ig with reparixin, which blocks against inflammatory neutrophil infiltration, yielded no long-term graft survival in an intrahepatic allotransplant model but had similar long-term graft survival in the kidney subcapsular model. Seven days after transplant, serum blood IFN-γ levels were significantly lower in the CTLA-4 Ig with reparixin treatment group compared to controls. IL-12p70 cytokine levels were increased with combination treatment, a positive modulation of the inflammatory response to the allograft. Furthermore, KC GRO, also known as CXCL1, was decreased in serum 7 d after transplant. Histologically, we found that immune cell infiltrate, CD4+ and CD8+ T cell populations along with both CXCR1+ and CXCR2+ cell populations were decreased within the CTLA-4 Ig and reparixin islet transplant graft. Overall these data provide insight into the down regulation of T-cell recruitment by CTLA-4 Ig and decreased neutrophil activation and recruitment with reparixin after long-term islet graft survival.

Published

2016

19. A novel redox-active metalloporphyrin reduces reactive oxygen species and inflammatory markers but does not improve marginal mass engraftment in a murine donation after circulatory death islet transplantation model.

Author

Bruni A, Pepper AR, Gala-Lopez B, Pawlick R, Abualhassan N, Crapo JD, Piganelli JD, and Shapiro AM

Subjects

Animals, Anti-Inflammatory Agents pharmacology, Antioxidants pharmacology, Cytokinesis physiology, Glucose Tolerance Test, Inflammation, Islets of Langerhans physiology, Mice, Models, Biological, Oxidation-Reduction, Shock, Tissue Survival drug effects, Islets of Langerhans Transplantation methods, Metalloporphyrins pharmacology, Reactive Oxygen Species metabolism

Abstract

Islet transplantation is a highly effective treatment for stabilizing glycemic control for select patients with type-1 diabetes. Despite improvements to clinical transplantation, single-donor transplant success has been hard to achieve routinely, necessitating increasing demands on viable organ availability. Donation after circulatory death (DCD) may be an alternative option to increase organ availability however, these organs tend to be more compromised. The use of metalloporphyrin anti-inflammatory and antioxidant (MnP) compounds previously demonstrated improved in vivo islet function in preclinical islet transplantation. However, the administration of MnP (BMX-001) in a DCD islet isolation and transplantation model has yet to be established. In this study, murine donors were subjected to a 15-min warm ischemic (WI) period prior to isolation and culture with or without MnP. Subsequent to one-hour culture, islets were assessed for in vitro viability and in vivo function. A 15-minute WI period significantly reduced islet yield, regardless of MnP-treatment relative to yields from standard isolation. MnP-treated islets did not improve islet viability compared to DCD islets alone. MnP-treatment did significantly reduce the presence of extracellular reactive oxygen species (ROS) (p < 0 .05). Marginal, syngeneic islets (200 islets) transplanted under the renal capsule exhibited similar in vivo outcomes regardless of WI or MnP-treatment. DCD islet grafts harvested 7 d post-transplant exhibited sustained TNF-α and IL-10, while MnP-treated islet-bearing grafts demonstrated reduced IL-10 levels. Taken together, 15-minute WI in murine islet isolation significantly impairs islet yield. DCD islets do indeed demonstrate in vivo function, though MnP therapy was unable to improve viability and engraftment outcomes.

Published

2016

20. Harnessing the Foreign Body Reaction in Marginal Mass Device-less Subcutaneous Islet Transplantation in Mice.

Author

Pepper AR, Pawlick R, Bruni A, Gala-Lopez B, Wink J, Rafiei Y, Bral M, Abualhassan N, and Shapiro AM

Subjects

Animals, Blood Glucose, Collagen chemistry, Diabetes Mellitus, Experimental therapy, Glucose Tolerance Test, Graft Survival, Injections, Subcutaneous, Male, Mice, Mice, Inbred C57BL, Microcirculation, Pancreatectomy, Transplantation, Isogeneic, Diabetes Mellitus, Type 1 therapy, Foreign-Body Reaction immunology, Insulin-Secreting Cells immunology, Islets of Langerhans Transplantation methods

Abstract

Background: Islet transplantation is a successful β-cell replacement therapy for selected patients with type 1 diabetes mellitus. However, despite early insulin independence, long-term graft attrition gradually reverts recipients to exogenous insulin dependency. Undoubtedly, as insulin producing stem cell therapies progress, a transplant site that is retrievable is desirable. This prerequisite is currently incompatible with intrahepatic islet transplantation. Herein, we evaluate the functional capacity of a prevascularized subcutaneous site to accommodate marginal islet mass transplantation in mice., Methods: Syngeneic mouse islets (150) were transplanted either under the kidney capsule (KC), into a prevascularized subcutaneous device-less (DL) site, or into the unmodified subcutaneous (SC) tissue. The DL site was created 4 weeks before diabetes induction and islet transplantation through the transient placement of a 5-Fr vascular catheter. Recipient mice were monitored for glycemic control and intraperitoneal glucose tolerance., Results: A marginal islet mass transplanted into the DL site routinely reversed diabetes (n = 13 of 18) whereas all SC islet recipients failed to restore glycemic control (n = 0 of 10, P < 0.01, log-rank). As anticipated, nearly all islet-KC mice (n = 15 of 16) became euglycemic posttransplant. The DL recipients' glucose profiles were comparable to KC islet grafts, postintrapertioneal glucose tolerance testing, whereas SC recipients remained hyperglycemic postglucose challenge. All normoglycemic mice maintained graft function for 100 days until graft retrieval. DL and KC islet grafts stained positively for insulin, microvessels, and a collagen scaffold., Conclusions: The device-less prevascularized approach supports marginal mass islet engraftment in mice.

Published

2016

21. Photoacoustic imaging of angiogenesis in a subcutaneous islet transplant site in a murine model.

Author

Shi W, Pawlick R, Bruni A, Rafiei Y, Pepper AR, Gala-Lopez B, Choi M, Malcolm A, Zemp RJ, and Shapiro AM

Subjects

Animals, Disease Models, Animal, Humans, Mice, Diabetes Mellitus, Experimental therapy, Islets of Langerhans Transplantation diagnostic imaging, Islets of Langerhans Transplantation methods, Neovascularization, Physiologic, Photoacoustic Techniques

Abstract

Islet transplantation (IT) is an established clinical therapy for select patients with type-1 diabetes. Clinically, the hepatic portal vein serves as the site for IT. Despite numerous advances in clinical IT, limitations remain, including early islet cell loss posttransplant, procedural complications, and the inability to effectively monitor islet grafts. Hence, alternative sites for IT are currently being explored, with the subcutaneous space as one potential option. When left unmodified, the subcutaneous space routinely fails to promote successful islet engraftment. However, when employing the previously developed subcutaneous “deviceless” technique, a favorable microenvironment for islet survival and function is established. In this technique, an angiocatheter was temporarily implanted subcutaneously, which facilitated angiogenesis to promote subsequent islet engraftment. This technique has been employed in preclinical animal models, providing a sufficient means to develop techniques to monitor functional aspects of the graft such as angiogenesis. Here, we utilize photoacoustic imaging to track angiogenesis during the priming of the subcutaneous site by the implanted catheter at 1 to 4 weeks postcatheter. Quantitative analysis on vessel densities shows gradual growth of vasculature in the implant position. These results demonstrate the ability to track angiogenesis, thus facilitating a means to optimize and assess the pretransplant microenvironment.

Published

2016

22. Lung-Derived Microscaffolds Facilitate Diabetes Reversal after Mouse and Human Intraperitoneal Islet Transplantation.

Author

Abualhassan N, Sapozhnikov L, Pawlick RL, Kahana M, Pepper AR, Bruni A, Gala-Lopez B, Kin T, Mitrani E, and Shapiro AM

Subjects

Animals, Graft Survival, Humans, Islets of Langerhans blood supply, Male, Mice, Mice, Inbred BALB C, Mice, Inbred C57BL, Mice, Inbred NOD, Mice, SCID, Diabetes Mellitus, Experimental prevention & control, Extracellular Matrix chemistry, Hyperglycemia prevention & control, Insulin-Secreting Cells cytology, Insulin-Secreting Cells metabolism, Islets of Langerhans Transplantation, Lung cytology

Abstract

There is a need to develop three-dimensional structures that mimic the natural islet tissue microenvironment. Endocrine micro-pancreata (EMPs) made up of acellular organ-derived micro-scaffolds seeded with human islets have been shown to express high levels of key beta-cell specific genes and secrete quantities of insulin per cell similar to freshly isolated human islets in a glucose-regulated manner for more than three months in vitro. The aim of this study was to investigate the capacity of EMPs to restore euglycemia in vivo after transplantation of mouse or human islets in chemically diabetic mice. We proposed that the organ-derived EMPs would restore the extracellular components of the islet microenvironment, generating favorable conditions for islet function and survival. EMPs seeded with 500 mouse islets were implanted intraperitoneally into streptozotocin-induced diabetic mice and reverted diabetes in 67% of mice compared to 13% of controls (p = 0.018, n = 9 per group). Histological analysis of the explanted grafts 60 days post-transplantation stained positive for insulin and exhibited increased vascular density in a collagen-rich background. EMPs were also seeded with human islets and transplanted into the peritoneal cavity of immune-deficient diabetic mice at 250 islet equivalents (IEQ), 500 IEQ and 1000 IEQ. Escalating islet dose increased rates of normoglycemia (50% of the 500 IEQ group and 75% of the 1000 IEQ group, n = 3 per group). Human c-peptide levels were detected 90 days post-transplantation in a dose-response relationship. Herein, we report reversal of diabetes in mice by intraperitoneal transplantation of human islet seeded on EMPs with a human islet dose as low as 500 IEQ.

Published

2016

23. Diabetes Is Reversed in a Murine Model by Marginal Mass Syngeneic Islet Transplantation Using a Subcutaneous Cell Pouch Device.

Author

Pepper AR, Pawlick R, Gala-Lopez B, MacGillivary A, Mazzuca DM, White DJ, Toleikis PM, and Shapiro AM

Subjects

Animals, Blood Glucose metabolism, Diabetes Mellitus, Experimental blood, Diabetes Mellitus, Experimental physiopathology, Diabetes Mellitus, Type 1 blood, Diabetes Mellitus, Type 1 physiopathology, Equipment Design, Glucagon metabolism, Insulin metabolism, Islets of Langerhans blood supply, Islets of Langerhans metabolism, Male, Mice, Inbred BALB C, Microvessels physiopathology, Neovascularization, Physiologic, Time Factors, Transplantation, Isogeneic, Bioartificial Organs, Diabetes Mellitus, Experimental surgery, Diabetes Mellitus, Type 1 surgery, Islets of Langerhans surgery, Islets of Langerhans Transplantation instrumentation, Pancreas, Artificial

Abstract

Background: Islet transplantation is a successful β-cell replacement therapy for selected patients with type 1 diabetes mellitus. Although high rates of early insulin independence are achieved routinely, long-term function wanes over time. Intraportal transplantation is associated with procedural risks, requires multiple donors, and does not afford routine biopsy. Stem cell technologies may require potential for retrievability, and graft removal by hepatectomy is impractical. There is a clear clinical need for an alternative, optimized transplantation site. The subcutaneous space is a potential substitute, but transplantation of islets into this site has routinely failed to reverse diabetes. However, an implanted device, which becomes prevascularized before transplantation, may alter this equation., Methods: Syngeneic mouse islets were transplanted subcutaneously within Sernova Corp's Cell Pouch (CP). All recipients were preimplanted with CPs 4 weeks before diabetes induction and transplantation. After transplantation, recipients were monitored for glycemic control and glucose tolerance., Results: Mouse islets transplanted into the CP routinely restored glycemic control with modest delay and responded well to glucose challenge, comparable to renal subcapsular islet grafts, despite a marginal islet dose, and normoglycemia was maintained until graft explantation. In contrast, islets transplanted subcutaneously alone failed to engraft. Islets within CPs stained positively for insulin, glucagon, and microvessels., Conclusions: The CP is biocompatible, forms an environment suitable for islet engraftment, and offers a potential alternative to the intraportal site for islet and future stem cell therapies.

Published

2015

24. A prevascularized subcutaneous device-less site for islet and cellular transplantation.

Author

Pepper AR, Gala-Lopez B, Pawlick R, Merani S, Kin T, and Shapiro AM

Subjects

Animals, Blood Glucose, Diabetes Mellitus, Experimental blood, Diabetes Mellitus, Experimental pathology, Graft Survival, Humans, Liver, Mice, Neovascularization, Pathologic blood, Neovascularization, Pathologic pathology, Translational Research, Biomedical, Cell- and Tissue-Based Therapy, Diabetes Mellitus, Experimental therapy, Islets of Langerhans Transplantation, Neovascularization, Pathologic therapy

Abstract

Transplantation of donor-derived islets into the liver is a successful cellular replacement therapy for individuals with diabetes. However, the hepatic vasculature is not an optimal transplant site for several reasons, including graft attrition and the inability to retrieve or image the islets. Here we describe islet transplantation into a prevascularized, subcutaneous site created by temporary placement of a medically approved vascular access catheter. In mice with streptozotocin (STZ)-induced diabetes, transplantation of ∼500 syngeneic islets into the resulting 'device-less' space reversed diabetes in 91% of mice and maintained normoglycemia for >100 days. The approach was also effective in mice with pre-existing diabetes, in another mouse strain that mounts a more vigorous inflammatory response, and across an allogeneic barrier. These results demonstrate that transient priming of a subcutaneous site supports diabetes-reversing islet transplantation in mouse models without the need for a permanent cell-encapsulation device.

Published

2015

25. The combination of anti-NKG2D and CTLA-4 Ig therapy prolongs islet allograft survival in a murine model.

Author

Pawlick R, Gala-Lopez B, Pepper AR, McCall M, Ziff O, and Shapiro AM

Subjects

Animals, Lymphocyte Culture Test, Mixed, Mice, Mice, Inbred C57BL, CTLA-4 Antigen immunology, Graft Survival immunology, Immunoglobulins administration & dosage, Islets of Langerhans Transplantation, Models, Animal, NK Cell Lectin-Like Receptor Subfamily K immunology

Abstract

Islet transplantation is an effective means of treating severe type 1 diabetes in patients with life-threatening hypoglycemia. Improvements in glycemic control with correction of HbA1C enhance quality of life irrespective of insulin independence. By antagonizing the Natural Killer Group 2, member D (NKG2D) receptor expression on NK and CD8+ T cells, in combination with blocking CTLA-4 binding sites, we demonstrate a significant delay of graft rejection in islet allotransplant. Anti-NKG2D combined with CTLA-4 Ig (n = 15) results in prolonged allograft survival, with 84.6 ± 10% of the recipients displaying insulin independence compared to controls (n = 10, p < 0.001). The effect of combination therapy on graft survival is superior to treatments alone (CTLA-4 Ig vs. combination p = 0.024, anti-NKG2D vs. combination p < 0.001) indicating an interaction between these pathways. In addition, combination treatment also improves glucose tolerance when compared to controls (n = 10, p = 0.018). Histologically, NKG2D+ cells were significantly decreased within the allograft after 7 days of combination treatment (n = 6, p = 0.029). T cell proliferation was significantly reduced with anti-NKG2D therapy and CD8+ T cell daughter fractions were also significantly decreased with mAb and combination treatment when measured by in vitro mixed lymphocyte reaction (n = 5, p = 0.015, p = 0.005 and p = 0.048). These results demonstrate that inhibition of NKG2D receptors and costimulatory pathways enhance islet allograft survival., (© Copyright 2014 The American Society of Transplantation and the American Society of Transplant Surgeons.)

Published

2014

26. Human islet viability and function is maintained during high-density shipment in silicone rubber membrane vessels.

Author

Kitzmann JP, Pepper AR, Gala-Lopez B, Pawlick R, Kin T, O'Gorman D, Mueller KR, Gruessner AC, Avgoustiniatos ES, Karatzas T, Szot GL, Posselt AM, Stock PG, Wilson JR, Shapiro AM, and Papas KK

Subjects

Animals, Cell Count, Cell Culture Techniques, Cell Hypoxia physiology, Cell Survival, Humans, Insulin metabolism, Insulin Secretion, Mice, Oxygen Consumption physiology, Islets of Langerhans physiology, Islets of Langerhans Transplantation, Product Packaging instrumentation, Silicone Elastomers, Specimen Handling instrumentation

Abstract

Background: The shipment of human islets (IE) from processing centers to distant laboratories is beneficial for both research and clinical applications. The maintenance of islet viability and function in transit is critically important. Gas-permeable silicone rubber membrane (SRM) vessels reduce the risk of hypoxia-induced death or dysfunction during high-density islet culture or shipment. SRM vessels may offer additional advantages: they are cost-effective (fewer flasks, less labor needed), safer (lower contamination risk), and simpler (culture vessel can also be used for shipment)., Method: IE were isolated from two manufacturing centers and shipped in 10-cm(2) surface area SRM vessels in temperature- and pressure-controlled containers to a distant center after at least 2 days of culture (n = 6). Three conditions were examined: low density (LD), high density (HD), and a microcentrifuge tube negative control (NC). LD was designed to mimic the standard culture density for IE preparations (200 IE/cm(2)), while HD was designed to have a 20-fold higher tissue density, which would enable the culture of an entire human isolation in 1-3 vessels. Upon receipt, islets were assessed for viability (measured by oxygen consumption rate normalized to DNA content [OCR/DNA)]), quantity (measured by DNA), and, when possible, potency and function (measured by dynamic glucose-stimulated insulin secretion measurements and transplants in immunodeficient B6 Rag(+/-) mice). Postshipment OCR/DNA was not reduced in HD vs LD and was substantially reduced in the NC condition. HD islets exhibited normal function postshipment. Based on the data, we conclude that entire islet isolations (up to 400,000 IE) may be shipped using a single, larger SRM vessel with no negative effect on viability and ex vivo and in vivo function., (Copyright © 2014 Elsevier Inc. All rights reserved.)

Published

2014

27. Islet cell transplantation for the treatment of type 1 diabetes: recent advances and future challenges.

Author

Bruni A, Gala-Lopez B, Pepper AR, Abualhassan NS, and Shapiro AJ

Abstract

Islet transplantation is a well-established therapeutic treatment for a subset of patients with complicated type I diabetes mellitus. Prior to the Edmonton Protocol, only 9% of the 267 islet transplant recipients since 1999 were insulin independent for >1 year. In 2000, the Edmonton group reported the achievement of insulin independence in seven consecutive patients, which in a collaborative team effort propagated expansion of clinical islet transplantation centers worldwide in an effort to ameliorate the consequences of this disease. To date, clinical islet transplantation has established improved success with insulin independence rates up to 5 years post-transplant with minimal complications. In spite of marked clinical success, donor availability and selection, engraftment, and side effects of immunosuppression remain as existing obstacles to be addressed to further improve this therapy. Clinical trials to improve engraftment, the availability of insulin-producing cell sources, as well as alternative transplant sites are currently under investigation to expand treatment. With ongoing experimental and clinical studies, islet transplantation continues to be an exciting and attractive therapy to treat type I diabetes mellitus with the prospect of shifting from a treatment for some to a cure for all.

Published

2014

28. Three-dimensional tumor volume and serum alpha-fetoprotein are predictors of hepatocellular carcinoma recurrence after liver transplantation: refined selection criteria.

Author

Kashkoush S, El Moghazy W, Kawahara T, Gala-Lopez B, Toso C, and Kneteman NM

Subjects

Carcinoma, Hepatocellular blood, Carcinoma, Hepatocellular surgery, Female, Follow-Up Studies, Humans, Liver Neoplasms blood, Liver Neoplasms surgery, Male, Middle Aged, Neoplasm Recurrence, Local blood, Neoplasm Recurrence, Local surgery, Prognosis, Prospective Studies, Retrospective Studies, Risk Factors, Survival Rate, Tumor Burden, Carcinoma, Hepatocellular diagnosis, Liver Neoplasms diagnosis, Liver Transplantation, Neoplasm Recurrence, Local diagnosis, Patient Selection, alpha-Fetoproteins metabolism

Abstract

Total tumor volume (TTV), as a better predictor of hepatocellular carcinoma (HCC) recurrence after liver transplant, has been explored by our center. Some tumors are not typically spherical but rather ellipsoid or spheroid, and calculating their TTV based on one dimension only may overestimate their volume and exclude them from candidacy for transplantation. Our aim was to study the actual tumor volume (ATV) calculated using the ellipsoid formula and assess its impact on recurrence. HCC patients transplanted between 1990 and 2010 at University of Alberta Hospital were analyzed. Tumor volumes were calculated using both formulas: [(4/3) πr(3)] (r = max. radius) and [(4/3) πabc] (a, b, c = the 3 radiuses). A total of 115 patients were included with a mean follow-up of 4.99 ± 4.23 yr. Five-yr recurrence-free survival was 79.8%. Univariate analysis for predictors of recurrence included: maximum tumor diameter, ATV, TTV, and alpha-fetoprotein (AFP) ≥ 400 ng/mL. Multivariate analysis showed that ATV and AFP ≥ 400 ng/mL were the only predictors of recurrence. Combining both variables provides better predication of recurrence with accuracy that exceeds 80%. Three-dimensional calculation of tumor volume is of critical importance for the group of patients with ellipsoid tumors where volumes are overestimated with the spherical formula and could lead to inappropriate exclusion from transplant., (© 2014 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2014

29. Current status of clinical islet transplantation.

Author

Pepper AR, Gala-Lopez B, Ziff O, and Shapiro AJ

Abstract

Islet transplantation (IT) is today a well-established treatment modality for selected patients with type 1 diabetes mellitus (T1DM). After the success of the University of Alberta group with a modified approach to the immune protection of islets, the international experience grew along with the numbers of transplants in highly specialized centers. Yet, long-term analysis of those initial results from the Edmonton group indicated that insulin-independence was not durable and most patients return to modest amounts of insulin around the fifth year, without recurrent hypoglycemia events. Many phenomena have been identified as limiting factor for the islet engraftment and survival, and today all efforts are aimed to improve the quality of islets and their engrafting process, as well as more optimized immunosuppression to facilitate tolerance and ultimately, better long term survival. This brief overview presents recent progress in IT. A concise historical perspective is provided, along with the latest efforts to improve islet engraftment, immune protection and ultimately, prolonged graft survival. It is apparent that as the community continues to work together further optimizing IT, it is hopeful a cure for T1DM will soon be achievable.

Published

2013

30. Fulminant hepatic failure necessitating transplantation following the initiation of infliximab therapy: a cautionary tale times two.

Author

Rowe BW, Gala-Lopez B, Tomlinson C, Girgis S, and Shapiro JA

Subjects

Adult, Colitis, Ulcerative complications, Female, Hidradenitis complications, Humans, Infliximab, Liver Failure, Acute pathology, Middle Aged, Antibodies, Monoclonal adverse effects, Liver Failure, Acute chemically induced, Liver Failure, Acute surgery, Liver Transplantation

Published

2013

31. Biologic agents in islet transplantation.

Author

Gala-Lopez B, Pepper AR, and Shapiro AM

Subjects

Animals, Biological Factors history, Biological Factors therapeutic use, History, 20th Century, Humans, Inflammation drug therapy, Biological Factors pharmacology, Islets of Langerhans Transplantation

Abstract

Islet transplantation is today an accepted modality for treating selected patients with frequent hypoglycemic events or severe glycemic lability. Despite tremendous progress in islet isolation, culture, and preservation, clinical use is still restricted to a limited subset, and lifelong immunosuppression is required. Issues surrounding limited islet revascularization and immune destruction remain. One of the major challenges is to prevent alloreactivity and recurrence of autoimmunity against β-cells. These two hurdles can be effectively reduced by immunosuppressive therapy combining induction and maintenance treatments. The introduction of highly potent and selective biologic agents has significantly reduced the frequency of acute rejection and has prolonged graft survival, while minimizing the complications of this therapeutic scheme. This review will address the most important biological agents used in islet transplantation. We provide a historical perspective of their introduction into clinical practice and their role in current clinical protocols, aiming at improved engraftment efficiency, increased long-term survival, and better overall results of clinical islet transplantation.

Published

2013

32. Microbial contamination of clinical islet transplant preparations is associated with very low risk of infection.

Author

Gala-Lopez B, Kin T, O'Gorman D, Pepper AR, Senior P, Humar A, and Shapiro AM

Subjects

Adult, Anti-Bacterial Agents administration & dosage, Diabetes Mellitus, Type 1 complications, Diabetes Mellitus, Type 1 therapy, Equipment Contamination, Female, Humans, Immunocompromised Host, Islets of Langerhans Transplantation methods, Male, Microbial Sensitivity Tests, Middle Aged, Patient Selection, Risk Assessment, Treatment Outcome, Diabetes Mellitus, Type 1 immunology, Diabetes Mellitus, Type 1 surgery, Graft Survival immunology, Gram-Negative Bacteria isolation & purification, Gram-Positive Bacteria isolation & purification, Islets of Langerhans Transplantation immunology

Abstract

Background: Several published studies have analyzed microbial contamination rates of islet products, ranging from 0% to 16%. However, few studies make reference to potential clinical consequences for transplant recipients and possible impact on islet survival., Materials and Methods: The current study defines rates of microbiological contamination of islet products under current good manufacturing practice conditions in 164 patients receiving 343 transplants at a single institution., Results: Nineteen (5.5%) islet preparations showed positive microbial growth with a majority (79.4%) due to Gram-positive organisms. The most frequently identified microorganism was coagulase-negative Staphylococcus (nine of 19 [47.3%]), followed by polymicrobial organisms (eight of 19 [42.1%]). No patient developed signs of clinical infection, and there were no hepatic abscesses evident on imaging by ultrasound or magnetic resonance imaging (none of 19 [0%]), despite the use of potent T-depletional induction. Finally, we could not demonstrate any negative impact of microbiological contamination on long-term islet graft survival., Conclusions: Microbiological contamination of the final islet preparation appears to have little or no effect on patients or on islet survival when appropriate antibiotics are given. However, preparation sterility should be guaranteed at all cost in order maximize patient safety and avoid potential complications in immunosuppressed patients.

Published

2013

33. Revascularization of transplanted pancreatic islets and role of the transplantation site.

Author

Pepper AR, Gala-Lopez B, Ziff O, and Shapiro AM

Subjects

Animals, Cellular Microenvironment, Humans, Microcirculation, Neovascularization, Physiologic, Islets of Langerhans blood supply, Islets of Langerhans Transplantation

Abstract

Since the initial reporting of the successful reversal of hyperglycemia through the transplantation of pancreatic islets, significant research efforts have been conducted in elucidating the process of revascularization and the influence of engraftment site on graft function and survival. During the isolation process the intrinsic islet vascular networks are destroyed, leading to impaired revascularization after transplant. As a result, in some cases a significant quantity of the beta cell mass transplanted dies acutely following the infusion into the portal vein, the most clinically used site of engraftment. Subsequently, despite the majority of patients achieving insulin independence after transplant, a proportion of them recommence small, supplemental exogenous insulin over time. Herein, this review considers the process of islet revascularization after transplant, its limiting factors, and potential strategies to improve this critical step. Furthermore, we provide a characterization of alternative transplant sites, analyzing the historical evolution and their role towards advancing transplant outcomes in both the experimental and clinical settings.

Published

2013

34. Recovery of locked-in syndrome following liver transplantation with calcineurin inhibitor cessation and supportive treatment.

Author

El Moghazy W, Gala-Lopez B, Wong W, and Kneteman N

Abstract

Background: Locked-in syndrome represents the most severe form of central pontine myelinolysis (CPM) and has been associated with a dismal outcome., Case Report: In this report we describe a case of severe locked-in syndrome after liver transplantation with spontaneous recovery with cessation of calcneurin inhibitor therapy and supportive treatment. A 54-year old male received deceased-donor liver transplantation and developed decreased level of consciousness with spastic quadriplegia. A diagnosis of central pontine myelinolysis with extrapontine manifestations was confirmed by magnetic resonance imaging. His immunosuppresion was modified by switching from tacrolimus to sirolimus and addition of prednisone. The patient started to recover from symptoms fourth months after transplantation., Conclusions: Tacrolimus is known to have neurotoxic side effects and it may precipitate CPM in patients who have predisposing factors. Sirolimus and steroids should be considered as safe and an effective alternative for immunosuppression in the setting of CPM after liver transplantation.

Published

2013

35. Portal vein thrombosis is a potentially preventable complication in clinical islet transplantation.

Author

Kawahara T, Kin T, Kashkoush S, Gala-Lopez B, Bigam DL, Kneteman NM, Koh A, Senior PA, and Shapiro AM

Subjects

Canada epidemiology, Diabetes Mellitus, Type 1 surgery, Humans, Incidence, Postoperative Hemorrhage epidemiology, Postoperative Hemorrhage etiology, Prognosis, Prospective Studies, Risk Factors, Treatment Outcome, Vascular Surgical Procedures, Venous Thrombosis epidemiology, Islets of Langerhans Transplantation adverse effects, Portal Vein physiopathology, Postoperative Complications, Postoperative Hemorrhage prevention & control, Venous Thrombosis etiology, Venous Thrombosis prevention & control

Abstract

Percutaneous transhepatic portal access avoids surgery but is rarely associated with bleeding or portal venous thrombosis (PVT). We herein report our large, single-center experience of percutaneous islet implantation and evaluate risk factors of PVT and graft function. Prospective data were collected on 268 intraportal islet transplants (122 subjects). A portal venous Doppler ultrasound was obtained on Days 1 and 7 posttransplant. Therapeutic heparinization, complete ablation of the portal catheter tract with Avitene paste and limiting packed cell volume (PCV) to <5 mL completely prevented any portal thrombosis in the most recent 101 islet transplant procedures over the past 5 years. In the previous cumulative experience, partial thrombosis did not affect islet function. Standard liver volume correlated negatively (r =-0.257, p < 0.001) and PCV correlated positively with portal pressure rise (r = 0.463, p < 0.001). Overall, partial portal thrombosis occurred after 10 procedures (overall incidence 3.7%, most recent 101 patient incidence 0%). There were no cases of complete thrombosis and no patient developed sequelae of portal hypertension. In conclusion, portal thrombosis is a preventable complication in clinical islet transplantation, provided therapeutic anticoagulation is maintained and PCV is limited to <5 mL., (©Copyright 2011 The American Society of Transplantation and the American Society of Transplant Surgeons.)

Published

2011