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Back table preparation of the pancreas for transplantation

Chapter by: Stewart, Zoe A
in: Operative techniques in surgery by Mulholland, Michael W (Ed)
Philadelphia, PA : Wolters Kluwer, 2015
pp. ?-?
ISBN: 1451190204
CID: 4815872

Optimization of Recombinant Adeno-Associated Virus-Mediated Expression for Large Transgenes, Using a Synthetic Promoter and Tandem Array Enhancers

Yan, Ziying; Sun, Xingshen; Feng, Zehua; Li, Guiying; Fisher, John T; Stewart, Zoe A; Engelhardt, John F
The packaging capacity of recombinant adeno-associated viral (rAAV) vectors limits the size of the promoter that can be used to express the 4.43-kb cystic fibrosis transmembrane conductance regulator (CFTR) cDNA. To circumvent this limitation, we screened a set of 100-mer synthetic enhancer elements, composed of ten 10-bp repeats, for their ability to augment CFTR transgene expression from a short 83-bp synthetic promoter in the context of an rAAV vector designed for use in the cystic fibrosis (CF) ferret model. Our initial studies assessing transcriptional activity in monolayer (nonpolarized) cultures of human airway cell lines and primary ferret airway cells revealed that three of these synthetic enhancers (F1, F5, and F10) significantly promoted transcription of a luciferase transgene in the context of plasmid transfection. Further analysis in polarized cultures of human and ferret airway epithelia at an air-liquid interface (ALI), as well as in the ferret airway in vivo, demonstrated that the F5 enhancer produced the highest level of transgene expression in the context of an AAV vector. Furthermore, we demonstrated that increasing the size of the viral genome from 4.94 to 5.04 kb did not significantly affect particle yield of the vectors, but dramatically reduced the functionality of rAAV-CFTR vectors because of small terminal deletions that extended into the CFTR expression cassette of the 5.04-kb oversized genome. Because rAAV-CFTR vectors greater than 5 kb in size are dramatically impaired with respect to vector efficacy, we used a shortened ferret CFTR minigene with a 159-bp deletion in the R domain to construct an rAAV vector (AV2/2.F5tg83-fCFTRΔR). This vector yielded an ∼17-fold increase in expression of CFTR and significantly improved Cl(-) currents in CF ALI cultures. Our study has identified a small enhancer/promoter combination that may have broad usefulness for rAAV-mediated CF gene therapy to the airway.
PMCID:4492606
PMID: 25763813
ISSN: 1557-7422
CID: 4815452

Ferret and pig models of cystic fibrosis: prospects and promise for gene therapy

Yan, Ziying; Stewart, Zoe A; Sinn, Patrick L; Olsen, John C; Hu, Jim; McCray, Paul B; Engelhardt, John F
Large animal models of genetic diseases are rapidly becoming integral to biomedical research as technologies to manipulate the mammalian genome improve. The creation of cystic fibrosis (CF) ferrets and pigs is an example of such progress in animal modeling, with the disease phenotypes in the ferret and pig models more reflective of human CF disease than mouse models. The ferret and pig CF models also provide unique opportunities to develop and assess the effectiveness of gene and cell therapies to treat affected organs. In this review, we examine the organ disease phenotypes in these new CF models and the opportunities to test gene therapies at various stages of disease progression in affected organs. We then discuss the progress in developing recombinant replication-defective adenoviral, adeno-associated viral, and lentiviral vectors to target genes to the lung and pancreas in ferrets and pigs, the two most affected organs in CF. Through this review, we hope to convey the potential of these new animal models for developing CF gene and cell therapies.
PMCID:4367511
PMID: 25675143
ISSN: 2324-8645
CID: 4815442

UW solution: still the "gold standard" for liver transplantation [Comment]

Stewart, Z A
PMID: 25612481
ISSN: 1600-6143
CID: 4815402

The challenge in diagnosing de novo minimal change disease after transplantation [Letter]

Kuppachi, Sarat; Suneja, Manish; Stewart, Zoe; Nair, Ramesh; Thomas, Christie P
PMID: 25651122
ISSN: 1534-6080
CID: 2960352

The Majority of Living Kidney Donor Candidates Fail to Complete a Full Donor Evaluation: The University of Iowa Experience [Meeting Abstract]

Stewart, Zoe
ISI:000328999400091
ISSN: 1600-6135
CID: 4816022

The Majority of Living Kidney Donor Candidates Fail to Complete a Full Donor Evaluation for Non-Medical Reasons [Meeting Abstract]

Stewart, Z.
ISI:000338033302181
ISSN: 1600-6135
CID: 4816032

A Pre-Screening Algorithm for Living Kidney Donor Candidates Significantly Reduces Futile Clinical Evaluations. [Meeting Abstract]

Stewart, Z.
ISI:000339104603013
ISSN: 0041-1337
CID: 4816062

The Majority of Living Kidney Donor Candidates Fail to Complete a Full Donor Evaluation for Non-Medical Reasons. [Meeting Abstract]

Stewart, Z.
ISI:000339104603012
ISSN: 0041-1337
CID: 4816052

A Pre-Screening Algorithm for Living Kidney Donor Candidates Significantly Reduces Futile Clinical Evaluations [Meeting Abstract]

Stewart, Z.
ISI:000338033302182
ISSN: 1600-6135
CID: 4816042