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Dive into the research topics where Ergang Shi is active.

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Featured researches published by Ergang Shi.


Angiogenesis | 2012

Binding and neutralization of vascular endothelial growth factor (VEGF) and related ligands by VEGF Trap, ranibizumab and bevacizumab

Nicholas J. Papadopoulos; Joel H. Martin; Qin Ruan; Ashique Rafique; Michael P. Rosconi; Ergang Shi; Erica A. Pyles; George D. Yancopoulos; Neil Stahl; Stanley J. Wiegand

Pharmacological inhibition of VEGF-A has proven to be effective in inhibiting angiogenesis and vascular leak associated with cancers and various eye diseases. However, little information is currently available on the binding kinetics and relative biological activity of various VEGF inhibitors. Therefore, we have evaluated the binding kinetics of two anti-VEGF antibodies, ranibizumab and bevacizumab, and VEGF Trap (also known as aflibercept), a novel type of soluble decoy receptor, with substantially higher affinity than conventional soluble VEGF receptors. VEGF Trap bound to all isoforms of human VEGF-A tested with subpicomolar affinity. Ranibizumab and bevacizumab also bound human VEGF-A, but with markedly lower affinity. The association rate for VEGF Trap binding to VEGF-A was orders of magnitude faster than that measured for bevacizumab and ranibizumab. Similarly, in cell-based bioassays, VEGF Trap inhibited the activation of VEGFR1 and VEGFR2, as well as VEGF-A induced calcium mobilization and migration in human endothelial cells more potently than ranibizumab or bevacizumab. Only VEGF Trap bound human PlGF and VEGF-B, and inhibited VEGFR1 activation and HUVEC migration induced by PlGF. These data differentiate VEGF Trap from ranibizumab and bevacizumab in terms of its markedly higher affinity for VEGF-A, as well as its ability to bind VEGF-B and PlGF.


Molecular Cancer Therapeutics | 2014

ERBB3/HER2 Signaling Promotes Resistance to EGFR Blockade in Head and Neck and Colorectal Cancer Models

Li Zhang; Carla Castanaro; Bo Luan; Katie Yang; Liangfen Fan; Jeanette L. Fairhurst; Ashique Rafique; Terra Potocky; Jing Shan; Frank Delfino; Ergang Shi; Tammy T. Huang; Joel H. Martin; Gang Chen; Douglas MacDonald; John S. Rudge; Gavin Thurston; Christopher Daly

EGFR blocking antibodies are approved for the treatment of colorectal cancer and head and neck squamous cell carcinoma (HNSCC). Although ERBB3 signaling has been proposed to limit the effectiveness of EGFR inhibitors, the underlying molecular mechanisms are not fully understood. To gain insight into these mechanisms, we generated potent blocking antibodies against ERBB3 (REGN1400) and EGFR (REGN955). We show that EGFR and ERBB3 are coactivated in multiple HNSCC cell lines and that combined blockade of EGFR and ERBB3 inhibits growth of these cell lines more effectively than blockade of either receptor alone. Blockade of EGFR with REGN955 strongly inhibited activation of ERK in HNSCC cell lines, whereas blockade of ERBB3 with REGN1400 strongly inhibited activation of Akt; only the combination of the 2 antibodies blocked both of these essential downstream pathways. We used a HER2 blocking antibody to show that ERBB3 phosphorylation in HNSCC and colorectal cancer cells is strictly dependent on association with HER2, but not EGFR, and that neuregulin 1 activates ERBB3/HER2 signaling to reverse the effect of EGFR blockade on colorectal cancer cell growth. Finally, although REGN1400 and REGN955 as single agents slowed the growth of HNSCC and colorectal cancer xenografts, the combination of REGN1400 plus REGN955 caused significant tumor regression. Our results indicate that activation of the Akt survival pathway by ERBB3/HER2 limits the effectiveness of EGFR inhibition, suggesting that REGN1400, which is currently in a phase I clinical trial, could provide benefit when combined with EGFR blocking antibodies. Mol Cancer Ther; 13(5); 1345–55. ©2014 AACR.


Archive | 2009

High affinity human antibodies to human IL-4 receptor

Sean Stevens; Tammy T. Huang; Joel H. Martin; Jeanette L. Fairhurst; Ashique Rafique; Marcela Torres; Kevin J. Pobursky; Raymond W. Leidich; Joan A. Windsor; Warren R. Mikulka; Diana M. Ahrens; Ergang Shi; Nicholas J. Papadopoulos


Archive | 2003

Modification assisted profiling (MAP) methodology

Czeslaw Radziejewski; Ergang Shi


Journal of Immunological Methods | 2006

Monoclonal antibody classification based on epitope-binding using differential antigen disruption.

Ergang Shi; Wen Fury; Wentian Li; Warren R. Mikulka; Thomas H. Aldrich; Ashique Rafique; Gang Chen; Simon Hoffenberg; Thomas J. Daly; Czeslaw Radziejewski


Archive | 2015

Vl antigen binding proteins exhibiting distinct binding characteristics

Robert Babb; Ashique Rafique; Tammy T. Huang; Ergang Shi; Lynn Macdonald; Andrew J. Murphy


Investigative Ophthalmology & Visual Science | 2012

Binding and Neutralization of Vascular Endothelial Growth Factor and Related Ligands by VEGF Trap, Ranibizumab and Bevacizumab

Ashique Rafique; Ergang Shi; Qin Ruan; Joel H. Martin; Michael P. Rosconi; Erica A. Pyles; Nick Papadopoulos; George D. Yancopoulos; Neil Stahl; Stanley J. Wiegand


Archive | 2010

Anticuerpos humanos con alta afinidad para el receptor IL-4 humano

Sean Stevens; Tammy T. Huang; Joel H. Martin; Jeanette L. Fairhurst; Ashique Rafique; Marcela Torres; Kevin J. Pobursky; Raymond W. Leidich; Joan A. Windsor; Warren R. Mikulka; Diana M. Ahrens; Ergang Shi; Nicholas J. Papadopoulos


Archive | 2007

Menschliche Antikörper mit hoher Affinität für den menschlichen IL-4-Rezeptor

Diana M. Ahrens; Jeanette L. Fairhurst; Tammy T. Huang; Raymond W. Leidich; Joel H. Martin; Warren R. Mikulka; Nicholas J. Papadopoulos; Kevin J. Pobursky; Ashique Rafique; Ergang Shi; Sean Stevens; Marcela Torres; Joan A. Windsor


Archive | 2007

human antibodies with high affinity for human IL-4 receptor

Sean Stevens; Tammy T. Huang; Joel H. Martin; Jeanette L. Fairhurst; Ashique Rafique; Marcela Torres; Kevin J. Pobursky; Raymond W. Leidich; Joan A. Windsor; Warren R. Mikulka; Diana M. Ahrens; Ergang Shi; Nicholas J. Papadopoulos

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