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97


Abnormal endocrine pancreas function at birth in cystic fibrosis ferrets

Olivier, Alicia K; Yi, Yaling; Sun, Xingshen; Sui, Hongshu; Liang, Bo; Hu, Shanming; Xie, Weiliang; Fisher, John T; Keiser, Nicholas W; Lei, Diana; Zhou, Weihong; Yan, Ziying; Li, Guiying; Evans, Turan I A; Meyerholz, David K; Wang, Kai; Stewart, Zoe A; Norris, Andrew W; Engelhardt, John F
Diabetes is a common comorbidity in cystic fibrosis (CF) that worsens prognosis. The lack of an animal model for CF-related diabetes (CFRD) has made it difficult to dissect how the onset of pancreatic pathology influences the emergence of CFRD. We evaluated the structure and function of the neonatal CF endocrine pancreas using a new CFTR-knockout ferret model. Although CF kits are born with only mild exocrine pancreas disease, progressive exocrine and endocrine pancreatic loss during the first months of life was associated with pancreatic inflammation, spontaneous hyperglycemia, and glucose intolerance. Interestingly, prior to major exocrine pancreas disease, CF kits demonstrated significant abnormalities in blood glucose and insulin regulation, including diminished first-phase and accentuated peak insulin secretion in response to glucose, elevated peak glucose levels following glucose challenge, and variably elevated insulin and C-peptide levels in the nonfasted state. Although there was no difference in lobular insulin and glucagon expression between genotypes at birth, significant alterations in the frequencies of small and large islets were observed. Newborn cultured CF islets demonstrated dysregulated glucose-dependent insulin secretion in comparison to controls, suggesting intrinsic abnormalities in CF islets. These findings demonstrate that early abnormalities exist in the regulation of insulin secretion by the CF endocrine pancreas.
PMCID:3534166
PMID: 22996690
ISSN: 1558-8238
CID: 4815412

Successful Treatment of Rapidly Recurrent FSGS with Plasmapheresis and Rituximab [Meeting Abstract]

Shetty, Rajesh; Reed, Alan; Myers, David; Brophy, Patrick; Stewart, Zoe
ISI:000286406500060
ISSN: 1600-6135
CID: 4816172

Case report: successful treatment of recurrent focal segmental glomerulosclerosis with a novel rituximab regimen [Case Report]

Stewart, Z A; Shetty, R; Nair, R; Reed, A I; Brophy, P D
Focal segmental glomerulosclerosis (FSGS) is the cause of renal failure in more than 10% of pediatric patients undergoing renal transplantation. Recurrent FSGS is a major cause of pediatric allograft failure, with the risk increasing for patients undergoing retransplantation. Standard therapy for recurrent posttransplantation FSGS includes the use of intensive plasmapheresis (PP) in conjunction with cyclophosphamide or high-dose cyclosporine. However, many patients exhibit refractory disease, with rapid progression to allograft loss despite these interventions. Prior studies have reported conflicting data on the efficacy of adding rituximab therapy to the standard treatment regimen for recurrent posttransplantation FSGS. Here we present a successful therapeutic protocol with rapid elimination of PP after initiation of rituximab therapy for an adolescent patient with recurrent FSGS in the immediate postoperative period. The patient has maintained excellent allograft function through 12 months posttransplantation.
PMID: 22172885
ISSN: 1873-2623
CID: 4815662

Hepatitis C Positive Simultaneous Liver-Kidney Recipients Have Significantly Reduced Early Post-Transplant Survival [Meeting Abstract]

Stewart, Z. A.; Collins, T. E.; Reed, A. I.; Segev, D. L.
ISI:000289318401546
ISSN: 1600-6135
CID: 4816202

Pre-emptive eculizumab and plasmapheresis for renal transplant in atypical hemolytic uremic syndrome [Case Report]

Nester, Carla; Stewart, Zoe; Myers, David; Jetton, Jennifer; Nair, Ramesh; Reed, Alan; Thomas, Christie; Smith, Richard; Brophy, Patrick
The case of a 12-year-old with a hybrid CFH/CFHL1 gene and atypical hemolytic uremic syndrome (aHUS) that had previously developed native kidney and then renal allograft loss is reported. This case illustrates the relatively common occurrence of renal loss from the late presentation of aHUS. Also presented is a protocol for the pre-emptive use of eculizumab and plasmapheresis as part of a renal transplant plan for the treatment of aHUS in patients deemed at high risk for recurrent disease. This protocol was a result of a multidisciplinary approach including adult and pediatric nephrology, transplant surgery, transfusion medicine, and infectious disease specialists. This protocol and the justifications and components of it can function as a guideline for the treatment of a group of children that have waited in limbo for the first U.S. transplant to open the door to this type of definitive care for this devastating disease.
PMCID:3109948
PMID: 21617085
ISSN: 1555-905x
CID: 2960342

Era Effect of Histidine-Tryptophan-Ketoglutarate (HTK) Preservation on Abdominal Allograft Survival [Meeting Abstract]

Stewart, Zoe A.; Collins, Thomas E.; Dagher, Nabil N.; Cameron, Andrew M.; Singer, Andrew L.; Segev, Dorry L.
ISI:000273297900042
ISSN: 1600-6135
CID: 4816222

Current Utilization of Preservation Solutions and Protocols for Abdominal Procurements: Results of a National Survey of OPOs. [Meeting Abstract]

Stewart, Zoe A.; Collins, Thomas E.; Katz, Daniel; Reed, Alan; Segev, Dorry L.
ISI:000275921701232
ISSN: 1600-6135
CID: 4816212

Use of Histidine-Tryptophan-Ketoglutarate for Pancreas Allograft Preservation Is Not Cost Effective Resource Utilization. [Meeting Abstract]

Stewart, Zoe A.; Cameron, Andrew M.; Dagher, Nabil N.; Singer, Andrew L.; Montgomery, Robert A.; Segev, Dorry L.
ISI:000265068800087
ISSN: 1600-6135
CID: 4815902

Surgical management of giant Brunner's gland hamartoma: case report and literature review [Case Report]

Stewart, Zoe A; Hruban, Ralph H; Fishman, Elliot F; Wolfgang, Christopher L
Brunner's gland hamartomas (BGH) are uncommon benign tumors of the duodenum forming mature Brunner's glands. We report here an unusual case of a giant BGH that was not amenable to endoscopic or surgical local resection thus requiring a pancreaticoduodenectomy for extirpation. The relevant literature is discussed.
PMCID:2749032
PMID: 19725968
ISSN: 1477-7819
CID: 2960382

Successful liver transplantation for Budd-Chiari syndrome in a patient with paroxysmal nocturnal hemoglobinuria treated with the anti-complement antibody eculizumab [Case Report]

Singer, Andrew L; Locke, Jamye E; Stewart, Zoe A; Lonze, Bonnie E; Hamilton, James P; Scudiere, Jennifer R; Anders, Robert A; Rother, Russell P; Brodsky, Robert A; Cameron, Andrew M
Paroxysmal nocturnal hemoglobinuria (PNH) is a rare, acquired hemolytic anemia caused by somatic mutations in the phosphatidylinositol glycan-complementation class A gene and the resulting absence of a key complement regulatory protein, CD59. Affected red blood cells in patients with PNH undergo intravascular complement-mediated lysis with resulting anemia, hemoglobinuria, and venous thromboses. Hepatic venous outflow thrombosis [Budd-Chiari syndrome (BCS)] is especially common in PNH patients and often fatal. The few case reports of outcomes in patients undergoing liver transplant for BCS secondary to PNH detail instances of recurrent BCS as well as early thrombotic portal vein occlusion and hepatic artery thrombosis requiring retransplantation. PNH is therefore generally considered a contraindication to liver transplantation. Here we present the first report of a patient with PNH and BCS undergoing successful liver transplantation while receiving eculizumab, a humanized monoclonal antibody that blocks the activation of the terminal complement at C5.
PMID: 19399743
ISSN: 1527-6473
CID: 2209372