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Dive into the research topics where Melinda Hollingshead is active.

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Featured researches published by Melinda Hollingshead.


Clinical Cancer Research | 2016

Pharmacodynamic Response of the MET/HGF-Receptor to Small Molecule Tyrosine Kinase Inhibitors Examined with Validated, Fit-for-Clinic Immunoassays

Apurva K. Srivastava; Melinda Hollingshead; Weiner J; Tony Navas; Yvonne A. Evrard; Sonny Khin; Jiuping Ji; Yujian Zhang; Thomas D. Pfister; Robert J. Kinders; Donald P. Bottaro; Linehan Wm; Joseph Tomaszewski; James H. Doroshow

Purpose: Rational development of targeted MET inhibitors for cancer treatment requires a quantitative understanding of target pharmacodynamics, including molecular target engagement, mechanism of action, and duration of effect. Experimental Design: Sandwich immunoassays and specimen handling procedures were developed and validated for quantifying full-length MET and its key phosphospecies (pMET) in core tumor biopsies. MET was captured using an antibody to the extracellular domain and then probed using antibodies to its C-terminus (full-length) and epitopes containing pY1234/1235, pY1235, and pY1356. Using pMET:MET ratios as assay endpoints, MET inhibitor pharmacodynamics were characterized in MET-amplified and -compensated (VEGFR blockade) models. Results: By limiting cold ischemia time to less than two minutes, the pharmacodynamic effects of the MET inhibitors PHA665752 and PF02341066 (crizotinib) were quantifiable using core needle biopsies of human gastric carcinoma xenografts (GTL-16 and SNU5). One dose decreased pY1234/1235 MET:MET, pY1235-MET:MET, and pY1356-MET:MET ratios by 60% to 80% within 4 hours, but this effect was not fully sustained despite continued daily dosing. VEGFR blockade by pazopanib increased pY1235-MET:MET and pY1356-MET:MET ratios, which was reversed by tivantinib. Full-length MET was quantifiable in 5 of 5 core needle samples obtained from a resected hereditary papillary renal carcinoma, but the levels of pMET species were near the assay lower limit of quantitation. Conclusions: These validated immunoassays for pharmacodynamic biomarkers of MET signaling are suitable for studying MET responses in amplified cancers as well as compensatory responses to VEGFR blockade. Incorporating pharmacodynamic biomarker studies into clinical trials of MET inhibitors could provide critical proof of mechanism and proof of concept for the field. Clin Cancer Res; 22(14); 3683–94. ©2016 AACR.


Cancer Research | 2005

In vivo efficacy of an aldehyde degradation product of dimethane sulfonate (NSC 281612) in an orthotopic RXF-393 human renal tumor model

John Carter; Howard Stotler; Melinda Hollingshead


Cancer Research | 2007

A validated assay for gamma-H2AX as a pharmacodynamic biomarker of response to DNA damage

Jay Jiuping Ji; Ravithat Putvatana; Yiping Zhang; Christophe Redon; Olga Sedelnikova; Sherry Yang; Yves Pommier; William Bonner; Robert J. Kinders; Ralph E. Parchment; Melinda Hollingshead; Jennifer Low; Anthony Murgo; Joseph Tomaszewski; James H. Doroshow


Cancer Research | 2006

A sterol mesylate activator of CEBPα signaling induces monocytic differentiation in human leukemia cells in vitro and in vivo

Erik Harris; Constance J. Glover; Joseph W. Adelsberger; Melinda Hollingshead; Ronald L. Felsted; Robert H. Shoemaker; Anne Monks


Clinical Cancer Research | 2008

Development and preclinical modeling of a topoisomerase I pharmacodynamic immunoassay for use in clinical trials

Thomas D. Pfister; Sonny Khin; Melinda Hollingshead; Ralph E. Parchment; Joseph Tomaszewski; James H. Doroshow; Robert J. Kinders


Cancer Research | 2008

Preclinical pharmacologic evaluations of R406/R788, a multi-kinase inhibitor which exhibits unique, differential in vitro anticancer activity as well as in vivo antitumor efficacy following oral adminstration.

Michael Alley; Melinda Hollingshead; Christine Pacula-Cox; John Carter; William Jacob; Polly Pine


Molecular Cancer Therapeutics | 2007

Evidence of in vivo efficacy for the indenoisoquinolines linked with pharmacodynamic markers for γH2AX

Melinda Hollingshead; Suzanne Borgel; John Carter; Carrie Bonomi; Raymond Divelbiss; Howard Stotler; Kelly Dougherty; Nathaniel Greenberg; Gurmeet Kaur; Yves Pommier; P Monks; Ralph E. Parchment; Robert J. Kinders; Joseph Tomaszewski; James H. Doroshow


Molecular Cancer Therapeutics | 2007

Development and validation of a quantitative assay for γH2AX in needle biopsies using topoisomerase I inhibitors

Robert J. Kinders; Melinda Hollingshead; Scott M. Lawrence; Jay Ji; Joseph Tomaszewski; James H. Doroshow; Ralph E. Parchment


Molecular Cancer Therapeutics | 2007

Synergistic antitumor activity of Bevacizumab in combination with HIF-1 inhibition.

Annamaria Rapisarda; Melinda Hollingshead; Mark Raffeld; Bradley Gehrs; Suzanne Borgel; John Carter; Carrie Bonomi; Robert H. Shoemaker; Giovanni Melillo


Molecular Cancer Therapeutics | 2007

Phosphorylated histone H2Ax in PBMCs as a pharmacodynamic surrogate response to DNA damage by topoisomerase I inhibitors

Jay Ji; Will Yutzy; Ravithat Putvatana; Yiping Zhang; Robert J. Kinders; Ralph E. Parchment; Melinda Hollingshead; Joseph Tomaszewski; James H. Doroshow

Collaboration


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James H. Doroshow

City of Hope National Medical Center

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Joseph Tomaszewski

Science Applications International Corporation

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John Carter

Science Applications International Corporation

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Ralph E. Parchment

Science Applications International Corporation

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Carrie Bonomi

Science Applications International Corporation

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Suzanne Borgel

Science Applications International Corporation

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Anne Monks

Science Applications International Corporation

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Erik Harris

Science Applications International Corporation

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Howard Stotler

Science Applications International Corporation

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