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Featured researches published by Doron Lipson.


Clinical Cancer Research | 2013

BRAF Fusions Define a Distinct Molecular Subset of Melanomas with Potential Sensitivity to MEK Inhibition

Katherine E. Hutchinson; Doron Lipson; Philip J. Stephens; Geoff Otto; Brian D. Lehmann; Pamela L. Lyle; Cindy L. Vnencak-Jones; Jeffrey S. Ross; Jennifer A. Pietenpol; Jeffrey A. Sosman; Igor Puzanov; Vincent A. Miller; William Pao

Purpose: Recurrent “driver” mutations at specific loci in BRAF, NRAS, KIT, GNAQ, and GNA11 define clinically relevant molecular subsets of melanoma, but more than 30% are “pan-negative” for these recurrent mutations. We sought to identify additional potential drivers in “pan-negative” melanoma. Experimental Design: Using a targeted next-generation sequencing (NGS) assay (FoundationOne™) and targeted RNA sequencing, we identified a novel PAPSS1-BRAF fusion in a “pan-negative” melanoma. We then analyzed NGS data from 51 additional melanomas genotyped by FoundationOne™, as well as melanoma RNA, whole-genome and whole-exome sequencing data in The Cancer Genome Atlas (TCGA), to determine the potential frequency of BRAF fusions in melanoma. We characterized the signaling properties of confirmed molecular alterations by ectopic expression of engineered cDNAs in 293H cells. Results: Activation of the mitogen-activated protein kinase (MAPK) pathway in cells by ectopic expression of PAPSS1-BRAF was abrogated by mitogen-activated protein kinase kinase (MEK) inhibition but not by BRAF inhibition. NGS data analysis of 51 additional melanomas revealed a second BRAF fusion (TRIM24-BRAF) in a “pan-negative” sample; MAPK signaling induced by TRIM24-BRAF was also MEK inhibitor sensitive. Through mining TCGA skin cutaneous melanoma dataset, we further identified two potential BRAF fusions in another 49 “pan-negative” cases. Conclusions: BRAF fusions define a new molecular subset of melanoma, potentially comprising 4% to 8% of “pan-negative” cases. Their presence may explain an unexpected clinical response to MEK inhibitor therapy or assist in selecting patients for MEK-directed therapy. Clin Cancer Res; 19(24); 6696–702. ©2013 AACR.


Archive | 2013

NOVEL FUSION MOLECULES AND USES THEREOF

Doron Lipson; Roman Yelensky; Joel Greenbowe; Jie He


Oncoscience | 2015

Durable clinical benefit to trastuzumab and chemotherapy in a patient with metastatic colon adenocarcinoma harboring ERBB2 amplification

Umut Disel; Alexis Germain; Bahar Yilmazel; Huseyin Abali; Filiz Aka Bolat; Roman Yelensky; Julia A. Elvin; Doron Lipson; Juliann Chmielecki; Kai Wang; Philip J. Stephens; Jeffrey S. Ross; Vincent A. Miller; Siraj M. Ali; Thomas J. George


ASCO Meeting Abstracts | 2013

Next-generation sequencing of genomic and cDNA to identify a high frequency of kinase fusions involving ROS1, ALK, RET, NTRK1, and BRAF in Spitz tumors.

Phil Stephens; Thomas Wiesner; Jie He; Roman Yelensky; Rosaura Esteve-Puig; Geoff Otto; Michael F. Berger; Doron Lipson; Kristina Brennan; Vincent A. Miller; Maureen T. Cronin; Boris C. Bastian


Archive | 2014

FUSION POLYNUCLEOTIDES AND FUSION POLYPEPTIDES ASSOCIATED WITH CANCER AND PARTICULARLY MELANOMA AND THEIR USES AS THERAPEUTIC AND DIAGNOSTIC TARGETS

Boris C. Bastian; Maureen T. Cronin; Jie He; Doron Lipson; Philip J. Stephens; Thomas Wieser; Roman Yalensky


ASCO Meeting Abstracts | 2014

Next-generation sequencing (NGS) to identify actionable genomic alterations (GA) in "pan-negative" lung adenocarcinomas (ADC) from patients with no smoking or a light smoking (NS/LS) history.

Alexander Drilon; Lu Wang; Maria E. Arcila; Eun Jung Cho; Sohail Balasubramanian; Joel Greenbowe; Jeffrey S. Ross; Phil Stephens; Doron Lipson; Vincent A. Miller; M. G. Kris; Marc Ladanyi; Naiyer A. Rizvi


Archive | 2017

novas moléculas de fusão kif5b-ret e usos das mesmas

Alex Parker; Doron Lipson; Matthew J. Hawryluk; Philip J. Stephens; Sean Downing


Publisher | 2015

Genomic Profiling of Advanced-Stage, Metaplastic Breast Carcinoma by Next-Generation Sequencing Reveals Frequent, Targetable Genomic Abnormalities and Potential New Treatment Options

Jeffrey S. Ross; Sunil V. Badve; Kai Wang; Christine E. Sheehan; Ann Boguniewicz; Geoff Otto; Roman Yelensky; Doron Lipson; Siraj M. Ali; Deborah Morosini; Juliann Chliemlecki; Julia A. Elvin; Vincent A. Miller; Philip J. Stephens


Archive | 2015

ComprehensiveGenomicProfilingofAdvancedEsophagealSquamous CellCarcinomasandEsophagealAdenocarcinomasRevealsSimilarities and Differences

Kai Wang; Adrienne Johnson; Siraj M. Ali; Samuel J. Klempner; Tanios Bekaii-Saab; Depinder Khaira; Roman Yelensky; Juliann Chmielecki; Julia A. Elvin; Doron Lipson; Vincent A. Miller; Philip J. Stephens; Jeffrey S. Ross


Archive | 2014

Méthodes de traitement du cholangiocarcinome

Vincent A. Miller; Sirj Mahamed Ali; Matthew J. Hawryluk; Jie He; Doron Lipson; Jeffrey S. Ross; Philip J. Stephens

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Jeffrey S. Ross

University of Colorado Denver

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Jie He

Foundation Medicine

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