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Featured researches published by Darlene Lee.


Nature Genetics | 2017

Spatial heterogeneity in medulloblastoma

A. Sorana Morrissy; Florence M.G. Cavalli; Marc Remke; Vijay Ramaswamy; David Shih; Borja L. Holgado; Hamza Farooq; Laura K. Donovan; Livia Garzia; Sameer Agnihotri; Erin Kiehna; Eloi Mercier; Chelsea Mayoh; Simon Papillon-Cavanagh; Hamid Nikbakht; Tenzin Gayden; Jonathon Torchia; Daniel Picard; Diana Merino; Maria Vladoiu; Betty Luu; Xiaochong Wu; Craig Daniels; Stuart Horswell; Yuan Yao Thompson; Volker Hovestadt; Paul A. Northcott; David T. W. Jones; John Peacock; Xin Wang

Spatial heterogeneity of transcriptional and genetic markers between physically isolated biopsies of a single tumor poses major barriers to the identification of biomarkers and the development of targeted therapies that will be effective against the entire tumor. We analyzed the spatial heterogeneity of multiregional biopsies from 35 patients, using a combination of transcriptomic and genomic profiles. Medulloblastomas (MBs), but not high-grade gliomas (HGGs), demonstrated spatially homogeneous transcriptomes, which allowed for accurate subgrouping of tumors from a single biopsy. Conversely, somatic mutations that affect genes suitable for targeted therapeutics demonstrated high levels of spatial heterogeneity in MB, malignant glioma, and renal cell carcinoma (RCC). Actionable targets found in a single MB biopsy were seldom clonal across the entire tumor, which brings the efficacy of monotherapies against a single target into question. Clinical trials of targeted therapies for MB should first ensure the spatially ubiquitous nature of the target mutation.


Genome Biology | 2007

A BAC clone fingerprinting approach to the detection of human genome rearrangements

Martin Krzywinski; Ian Bosdet; Carrie Mathewson; Natasja Wye; Jay Brebner; Readman Chiu; Richard Corbett; Matthew A. Field; Darlene Lee; Trevor Pugh; Stas Volik; Asim Siddiqui; Steven J.M. Jones; Jacquie Schein; Collin Collins; Marco A. Marra

We present a method, called fingerprint profiling (FPP), that uses restriction digest fingerprints of bacterial artificial chromosome clones to detect and classify rearrangements in the human genome. The approach uses alignment of experimental fingerprint patterns to in silico digests of the sequence assembly and is capable of detecting micro-deletions (1-5 kb) and balanced rearrangements. Our method has compelling potential for use as a whole-genome method for the identification and characterization of human genome rearrangements.


Prostate Cancer and Prostatic Diseases | 2017

Molecular alterations in prostate cancer and association with MRI features

Darlene Lee; Jacqueline Fontugne; Naveen Gumpeni; Kyung Kgi Park; Theresa Y. MacDonald; Brian D. Robinson; Andrea Sboner; Mark A. Rubin; Juan Miguel Mosquera; Christopher E. Barbieri

Background:Multiparametric magnetic resonance imaging (mpMRI) has been increasingly used for prostate cancer (PCa). Recent studies identified distinct molecular subclasses of PCa with recurrent genomic alterations. However, the associations between molecular alterations in PCa and characteristics on mpMRI are unknown. Therefore, the objective of this study was to investigate recurrent molecular alterations in PCa and their associations with mpMRI features.Methods:Sixty-two PCa nodules >0.5 cm had a preoperative mpMRI. Nodules were evaluated for ERG rearrangement, PTEN deletion, SPINK1 overexpression, SPOP mutation and CHD1 deletion. Each PCa focus was matched to the corresponding location on mpMRI. Lesions were scored by single observer according to the PI-RADSv2 scale.Results:Of the 62 nodules, 22 (35.5%) were ERG positive, 6 (9.7%) had SPINK1 overexpression, 6 (9.7%) had SPOP mutations, 4 (6.5%) had CHD1 deletions and 1 (1.6%) had PTEN deletion. All of the nodules with CHD1 deletions were not visible on mpMRI (P=0.037). All of the nodules with SPINK1 overexpression were visible on mpMRI, although the association was not statistically significant (P=0.06). There were no significant associations between any molecular alteration with the severity of the PI-RADS scores (all P>0.05).Conclusions:This investigation represents the first description of an association between recurrent molecular alterations and the characterization of PCa nodules on mpMRI. This study can be considered hypothesis-generating for future studies to rigorously evaluate the association of specific PCa molecular subclasses with imaging features and potentially define specific subsets of PCa for which the utility of MRI is higher or lower.


Development | 1999

TARGETED INACTIVATION OF THE EGF AND AMPHIREGULIN GENES REVEALS DISTINCT ROLES FOR EGF RECEPTOR LIGANDS IN MOUSE MAMMARY GLAND DEVELOPMENT

Noreen C. Luetteke; Ting Hu Qiu; S. E. Fenton; K. L. Troyer; Richard F. Riedel; Aileen Chang; Darlene Lee


Nucleic Acids Research | 2004

A set of BAC clones spanning the human genome

Martin Krzywinski; Ian Bosdet; Duane E. Smailus; Readman Chiu; Carrie Mathewson; Natasja Wye; Sarah Barber; Mabel Brown-John; Susanna Chan; Steve Chand; Alison Cloutier; Noreen Girn; Darlene Lee; Amara Masson; Michael Mayo; Teika Olson; Pawan Pandoh; Anna Liisa Prabhu; Eric F.P.M. Schoenmakers; Miranda Tsai; Donna G. Albertson; Wan L. Lam; Chik On Choy; Kazutoyo Osoegawa; Shaying Zhao; Pieter J. de Jong; Jacqueline E. Schein; Steven J.M. Jones; Marco A. Marra


Plant Journal | 2007

A physical map of the highly heterozygous Populus genome: integration with the genome sequence and genetic map and analysis of haplotype variation.

Colin T. Kelleher; Readman Chiu; Heesun Shin; Ian Bosdet; Martin Krzywinski; Chris Fjell; Jennifer Wilkin; Tongming Yin; Stephen P. DiFazio; Johar Ali; Jennifer Asano; Susanna Chan; Alison Cloutier; Noreen Girn; Stephen Leach; Darlene Lee; Carrie Mathewson; Teika Olson; Katie O’Connor; Anna-Liisa Prabhu; Duane E. Smailus; Jeffery M. Stott; Miranda Tsai; Natasja Wye; George S. Yang; Jun Zhuang; Robert A. Holt; Nicholas H. Putnam; Julia Vrebalov; James J. Giovannoni


Genome Research | 2004

Integrated and Sequence-Ordered BAC- and YAC-Based Physical Maps for the Rat Genome

Martin Krzywinski; John W. Wallis; Claudia Gosele; Ian Bosdet; Readman Chiu; Tina Graves; Oliver Hummel; Dan Layman; Carrie Mathewson; Natasja Wye; Baoli Zhu; Derek Albracht; Jennifer Asano; Sarah Barber; Mabel Brown-John; Susanna Chan; Steve Chand; Alison Cloutier; Jonathon Davito; Chris Fjell; Tony Gaige; Detlev Ganten; Noreen Girn; Kurtis Guggenheimer; Heinz Himmelbauer; Thomas Kreitler; Stephen Leach; Darlene Lee; Hans Lehrach; Michael Mayo


Blood | 2005

Towards the Human Cancer Genome Project: A Sequence-Ready Physical Map of a Follicular Lymphoma Genome.

Marco A. Marra; Martin Krzywinski; Readman Chiu; Matthew A. Field; Inanc Birol; Brian D’Souza; Ian Bosdet; Carrie Mathewson; Darlene Lee; Agnes Baross; Randy D. Gascoyne; Douglas E. Horsman; Robert A. Holt; Jacqueline E. Schein; Joseph M. Connors

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Ian Bosdet

University of British Columbia

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Natasja Wye

University of British Columbia

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Alison Cloutier

University of British Columbia

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Marco A. Marra

University of British Columbia

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Noreen Girn

University of British Columbia

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Susanna Chan

University of British Columbia

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Chris Fjell

University of British Columbia

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