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Dive into the research topics where Eric M. Ostertag is active.

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Featured researches published by Eric M. Ostertag.


Molecular Cancer Therapeutics | 2018

Sprague Dawley Rag2 null rats created from engineered spermatogonial stem cells are immunodeficient and permissive to human xenografts

Fallon K. Noto; Valeriya V. Adjan Steffey; Min Tong; Kameswaran Ravichandran; Wei Zhang; Angela Arey; Christopher McClain; Eric M. Ostertag; Sahar Mazhar; Jaya Sangodkar; Analisa Difeo; Jack Crawford; Goutham Narla; Tseten Y Jamling

The rat is the preferred model for toxicology studies, and it offers distinctive advantages over the mouse as a preclinical research model including larger sample size collection, lower rates of drug clearance, and relative ease of surgical manipulation. An immunodeficient rat would allow for larger tumor size development, prolonged dosing and drug efficacy studies, and preliminary toxicologic testing and pharmacokinetic/pharmacodynamic studies in the same model animal. Here, we created an immunodeficient rat with a functional deletion of the Recombination Activating Gene 2 (Rag2) gene, using genetically modified spermatogonial stem cells (SSC). We targeted the Rag2 gene in rat SSCs with TALENs and transplanted these Rag2-deficient SSCs into sterile recipients. Offspring were genotyped, and a founder with a 27 bp deletion mutation was identified and bred to homozygosity to produce the Sprague-Dawley Rag2 - Rag2tm1Hera (SDR) knockout rat. We demonstrated that SDR rat lacks mature B and T cells. Furthermore, the SDR rat model was permissive to growth of human glioblastoma cell line subcutaneously resulting in successful growth of tumors. In addition, a human KRAS-mutant non–small cell lung cancer cell line (H358), a patient-derived high-grade serous ovarian cancer cell line (OV81), and a patient-derived recurrent endometrial cancer cell line (OV185) were transplanted subcutaneously to test the ability of the SDR rat to accommodate human xenografts from multiple tissue types. All human cancer cell lines showed efficient tumor uptake and growth kinetics indicating that the SDR rat is a viable host for a range of xenograft studies. Mol Cancer Ther; 17(11); 2481–9. ©2018 AACR.


Archive | 2012

METHODS FOR SITE-SPECIFIC GENETIC MODIFICATION IN STEM CELLS USING XANTHOMONAS TAL NUCLEASES (XTN) FOR THE CREATION OF MODEL ORGANISMS

Eric M. Ostertag; John Stuart Crawford; J. Keith Joung


Archive | 2012

Methods for site-specific genetic modification in spermatogonial stem cells using zinc finger nuclease (zfn) for the creation of model organisms

Eric M. Ostertag; John Stuart Crawford; J. Keith Joung; Franklin Kent Hamra


Archive | 2010

Genetically Modified Rat Models for Severe Combined Immunodeficiency (SCID)

Eric M. Ostertag; John Stuart Crawford; Joseph Ruiz


Archive | 2010

Genetically modified rat models for cancer

Eric M. Ostertag; John Stuart Crawford


Archive | 2010

Genetically modified rat models for pain

Eric M. Ostertag; John Stuart Crawford


Archive | 2010

TRP INHIBITORS AND USES THEREOF

John Stuart Crawford; Eric M. Ostertag


Archive | 2010

Genetically modified rat comprising a cytokine gene disruption and exhibiting a greater susceptibility to a cytokine-mediated autoimmune and/or inflammatory disease

Eric M. Ostertag; John Stuart Crawford


Archive | 2010

Genetically modified rat models for pharmacokinetics

Eric M. Ostertag; John Stuart Crawford


Archive | 2014

REPRODUCIBLE METHOD FOR TESTIS-MEDIATED GENETIC MODIFICATION (TGM) AND SPERM-MEDIATED GENETIC MODIFICATION (SGM)

Carlisle Landel; Eric M. Ostertag; Joseph Ruiz; Tseten Yeshi

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Christopher McClain

Icahn School of Medicine at Mount Sinai

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Sahar Mazhar

Case Western Reserve University

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