Yvonne Yip
Eli Lilly and Company
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Publication
Featured researches published by Yvonne Yip.
Molecular Cancer Therapeutics | 2016
Michele C. Smith; Mary M. Mader; James A. Cook; Philip W. Iversen; Rose T. Ajamie; Everett J. Perkins; Laura J. Bloem; Yvonne Yip; David Anthony Barda; Philip Parker Waid; Douglas J. Zeckner; Debra A. Young; Manuel Sanchez-Felix; Gregory P. Donoho; Volker Wacheck
The PI3K/AKT/mTOR pathway is among the most frequently altered pathways in cancer cell growth and survival. LY3023414 is a complex fused imidazoquinolinone with high solubility across a wide pH range designed to inhibit class I PI3K isoforms and mTOR kinase. Here, we describe the in vitro and in vivo activity of LY3023414. LY3023414 was highly soluble at pH 2–7. In biochemical testing against approximately 266 kinases, LY3023414 potently and selectively inhibited class I PI3K isoforms, mTORC1/2, and DNA-PK at low nanomolar concentrations. In vitro, inhibition of PI3K/AKT/mTOR signaling by LY3023414 caused G1 cell-cycle arrest and resulted in broad antiproliferative activity in cancer cell panel screens. In vivo, LY3023414 demonstrated high bioavailability and dose-dependent dephosphorylation of PI3K/AKT/mTOR pathway downstream substrates such as AKT, S6K, S6RP, and 4E-BP1 for 4 to 6 hours, reflecting the drugs half-life of 2 hours. Of note, equivalent total daily doses of LY3023414 given either once daily or twice daily inhibited tumor growth to similar extents in multiple xenograft models, indicating that intermittent target inhibition is sufficient for antitumor activity. In combination with standard-of-care drugs, LY3023414 demonstrated additive antitumor activity. The novel, orally bioavailable PI3K/mTOR inhibitor LY3023414 is highly soluble and exhibits potent in vivo efficacy via intermittent target inhibition. It is currently being evaluated in phase I and II trials for the treatment of human malignancies. Mol Cancer Ther; 15(10); 2344–56. ©2016 AACR.
Bioorganic & Medicinal Chemistry Letters | 2004
Yvonne Yip; Frantz Victor; Jason Lamar; Robert B. Johnson; Q.May Wang; Donna Barket; John Irvin Glass; Ling Jin; Lifei Liu; Daryl Venable; Mark Wakulchik; Congping Xie; Beverly A. Heinz; Elcira C. Villarreal; Joe Colacino; Nathan Yumibe; Mark Joseph Tebbe; John E. Munroe; Shu-Hui Chen
Bioorganic & Medicinal Chemistry Letters | 2004
Yvonne Yip; Frantz Victor; Jason Lamar; Robert B. Johnson; Q.May Wang; John Irvin Glass; Nathan Yumibe; Mark Wakulchik; John E. Munroe; Shu-Hui Chen
Archive | 2005
Melendo Ana Belen Bueno; Shu-Hui Chen; Jon A. Erickson; Maria Rosario Gonzalez-Garcia; Deqi Guo; Llorente Alicia Marcos; James R. McCarthy; Timothy Alan Shepherd; Scott Martin Sheehan; Yvonne Yip
Bioorganic & Medicinal Chemistry Letters | 2004
Frantz Victor; Jason Lamar; Nancy June Snyder; Yvonne Yip; Deqi Guo; Nathan Yumibe; Robert B. Johnson; Q.May Wang; John Irvin Glass; Shu-Hui Chen
Archive | 2006
David Anthony Barda; Timothy Paul Burkholder; Joshua Ryan Clayton; Yan Hao; Perry Clark Heath; James Robert Henry; John Monte Knobeloch; David Mendel; Johnathan Alexander Mclean; David Michael Remick; Mark Edward Rempala; Zhao-Qing Wang; Yvonne Yip; Boyu Zhong
Letters in Drug Design & Discovery | 2005
Shu-Hui Chen; Jason Lamar; Yvonne Yip; Frantz Victor; Robert B. Johnson; Q.May Wang; John Irvin Glass; Beverly A. Heinz; Joseph M. Colacino; Deqi Guo; Mark Joseph Tebbe; John E. Munroe
Bioorganic & Medicinal Chemistry Letters | 2004
David X Sun; Lifei Liu; Beverly A. Heinz; Alexander Kolykhalov; Jason Lamar; Robert B. Johnson; Q.May Wang; Yvonne Yip; Shu-Hui Chen
Bioorganic & Medicinal Chemistry Letters | 2004
Shu-Hui Chen; Jason Lamar; Deqi Guo; Todd J. Kohn; Hsiu-Chiung Yang; James McGee; David E. Timm; Jon A. Erickson; Yvonne Yip; Patrick C. May; James R. McCarthy
Archive | 2006
David Anthony Barda; Timothy Paul Burkholder; Joshua Ryan Clayton; Yan Hao; James Rober Henry; John Monte Knobeloch; David Mendel; David Michael Remick; Mark Eward Rempala; Zhao-Quing Wang; Yvonne Yip; Perry Clark Heath; Johnathan Alexander Mclean; Boyu Zhong