Michele Dunning scite author profile

Vascular access port implantation by saphenous vein puncture or saphenous vein cutdown is safe and effective in NHPs. It is less invasive than conventional procedures, has fewer complications, provides outstanding patency, and reduces surgery time. Furthermore, it allows for cooperative in-homecage VAP use, minimizing handling stress. We recommend these refined methods for long-term vascular access in NHPs.

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Rodents Versus Pig Model for Assessing the Performance of Serotype Chimeric Ad5/3 Oncolytic Adenoviruses

Koodie

Robertson

Chandrashekar

et al. 2019

Cancers

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Oncolytic adenoviruses (Ad) are promising tools for cancer therapeutics. Most Ad-based therapies utilize species C serotypes, with Adenovirus type 5 (Ad5) most commonly employed. Prior clinical trials demonstrated low efficiency of oncolytic Ad5 vectors, mainly due to the absence of Ad5 primary receptor (Coxsackie and Adenovirus Receptor, CAR) on cancer cells. Engineering serotype chimeric vectors (Ad5/3) to utilize Adenovirus type 3 (Ad3) receptors has greatly improved their oncolytic potential. Clinical translation of these infectivity-enhanced vectors has been challenging due to a lack of replication permissive animal models. In this study, we explored pigs as a model to study the performance of fiber-modified Ad5/3 chimeric vectors. As a control, the Ad5 fiber-unmodified virus was used. We analyzed binding, gene transfer, replication, and cytolytic ability of Ad5 and Ad5/3 in various non-human cell lines (murine, hamster, canine, porcine). Among all tested cell lines only porcine cells supported active binding and replication of Ad5/3. Syrian hamster cells supported Ad5 replication but showed no evidence of productive viral replication after infection with Ad5/3 vectors. Transduction and replication ability of Ad5/3 in porcine cells outperformed Ad5, a phenomenon often observed in human cancer cell lines. Replication of Ad5 and Ad5/3 was subsequently evaluated in vivo in immunocompetent pigs. Quantitative PCR analyses 7 days post infection revealed Ad5 and Ad5/3 DNA and replication-dependent luciferase activity in the swine lungs and spleen indicating active replication in these tissues. These studies demonstrated the flaws in using Syrian hamsters for testing serotype chimeric Ad5/3 vectors. This is the first report to validate the pig as a valuable model for preclinical testing of oncolytic adenoviruses utilizing Adenovirus type 3 receptors. We hope that these data will help to foster the clinical translation of oncolytic adenoviruses including those with Ad3 retargeted tropism.

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Risk factors associated with surgical site infection and the development of short‐term complications in macaques undergoing indwelling vascular access port placement

Graham

Rieke

Wijkstrom

et al. 2008

J of Medical Primatology

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Portal Donor-Specific Blood Transfusion and Mycophenolate Mofetil Allow Steroid Avoidance and Tacrolimus Dose Reduction With Sustained Levels of Chimerism in a Pig Model of Intestinal Transplantation

Gruessner

Levay‐Young

Nakhleh

et al. 2004

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Donor-Specific Portal Blood Transfusion in Intestinal Transplantation

et al. 1998

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Michele Dunning

A novel alternative placement site and technique for totally implantable vascular access ports in non‐human primates

Rodents Versus Pig Model for Assessing the Performance of Serotype Chimeric Ad5/3 Oncolytic Adenoviruses

Risk factors associated with surgical site infection and the development of short‐term complications in macaques undergoing indwelling vascular access port placement

Portal Donor-Specific Blood Transfusion and Mycophenolate Mofetil Allow Steroid Avoidance and Tacrolimus Dose Reduction With Sustained Levels of Chimerism in a Pig Model of Intestinal Transplantation

Donor-Specific Portal Blood Transfusion in Intestinal Transplantation

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