Isabel Zaror
Chiron Corporation
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Publication
Featured researches published by Isabel Zaror.
ACS Medicinal Chemistry Letters | 2011
Matthew Burger; Sabina Pecchi; Allan S. Wagman; Zhi-Jie Ni; Mark Knapp; Thomas Hendrickson; Gordana Atallah; Keith B. Pfister; Yanchen Zhang; Sarah Bartulis; Kelly Frazier; Simon Ng; Aaron Smith; Joelle Verhagen; Joshua Haznedar; Kay Huh; Ed Iwanowicz; Xiaohua Xin; Daniel Menezes; Hanne Merritt; Isabelle Lee; Marion Wiesmann; Susan Kaufman; Kenneth Crawford; Michael Chin; Dirksen E. Bussiere; Kevin Shoemaker; Isabel Zaror; Sauveur-Michel Maira; Charles Voliva
Phosphoinositide-3-kinases (PI3Ks) are important oncology targets due to the deregulation of this signaling pathway in a wide variety of human cancers. Herein we describe the structure guided optimization of a series of 2-morpholino, 4-substituted, 6-heterocyclic pyrimidines where the pharmacokinetic properties were improved by modulating the electronics of the 6-position heterocycle, and the overall druglike properties were fine-tuned further by modification of the 4-position substituent. The resulting 2,4-bismorpholino 6-heterocyclic pyrimidines are potent class I PI3K inhibitors showing mechanism modulation in PI3K dependent cell lines and in vivo efficacy in tumor xenograft models with PI3K pathway deregulation (A2780 ovarian and U87MG glioma). These efforts culminated in the discovery of 15 (NVP-BKM120), currently in Phase II clinical trials for the treatment of cancer.
PLOS ONE | 2017
Johanna M. Jansen; Charles Wartchow; Wolfgang Jahnke; Susan Fong; Tiffany Tsang; Keith B. Pfister; Tatiana Zavorotinskaya; Dirksen E. Bussiere; Jan Marie Cheng; Kenneth Crawford; Yumin Dai; Jeffrey H. Dove; Eric Fang; Yun Feng; Jean-Michel Florent; John Fuller; Alvar D. Gossert; Mohammad Hekmat-Nejad; Chrystèle Henry; Julia Klopp; William P. Lenahan; Andreas Lingel; Sylvia Ma; Arndt Meyer; Yuji Mishina; Jamie Narberes; Gwynn Pardee; Savithri Ramurthy; Sebastien Rieffel; Darrin Stuart
RAS mutations lead to a constitutively active oncogenic protein that signals through multiple effector pathways. In this chemical biology study, we describe a novel coupled biochemical assay that measures activation of the effector BRAF by prenylated KRASG12V in a lipid-dependent manner. Using this assay, we discovered compounds that block biochemical and cellular functions of KRASG12V with low single-digit micromolar potency. We characterized the structural basis for inhibition using NMR methods and showed that the compounds stabilized the inactive conformation of KRASG12V. Determination of the biophysical affinity of binding using biolayer interferometry demonstrated that the potency of inhibition matches the affinity of binding only when KRAS is in its native state, namely post-translationally modified and in a lipid environment. The assays we describe here provide a first-time alignment across biochemical, biophysical, and cellular KRAS assays through incorporation of key physiological factors regulating RAS biology, namely a negatively charged lipid environment and prenylation, into the in vitro assays. These assays and the ligands we discovered are valuable tools for further study of KRAS inhibition and drug discovery.
Archive | 2004
Li Long; Mohammad Luqman; Asha Yabannavar; Isabel Zaror; Bao-Lu Chen; Xiaofeng Lu; Sang Hoon Lee; Deborah Hurst
Archive | 2004
Li Long; Mohammad Luqman; Asha Yabannavar; Isabel Zaror
Archive | 1996
Kenneth A. Crawford; Isabel Zaror; Robert J. Bishop; Michael A. Innis
FEBS Journal | 1993
Isabel Zaror; Frank Marcus; Donna L. Moyer; James W. Tung; Jeffrey R. Shuster
Archive | 2004
Li Long; Mohammad Luqman; Asha Yabannavar; Isabel Zaror
Archive | 1996
Michael A. Innis; Isabel Zaror; Abla A. Creasey
Thrombosis and Haemostasis | 1998
Kirk Johnson; Isabel Zaror; Diane Bauer; Yoon Choi; Abla A. Creasey; Michael A. Innis
Archive | 2011
Sharon Lea Aukerman; Li Long; Mohammad Luqman; Asha Yabannavar; Isabel Zaror; ヤバンナバー アシャ; ザロー イザベル; リー オーカーマン シャロン; ルクマン モハンマド; ロン リ