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Dive into the research topics where Richard A. Isbrucker is active.

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Featured researches published by Richard A. Isbrucker.


Biochemical Pharmacology | 2003

Tubulin polymerizing activity of dictyostatin-1, a polyketide of marine sponge origin.

Richard A. Isbrucker; Jennifer L. Cummins; Shirley A. Pomponi; Ross E. Longley; Amy E. Wright

Dictyostatin-1 had previously been isolated from a marine sponge of the genus Spongia sp. and described as a cytotoxic agent to murine and human cancer cells, but its mechanism of activity was unknown. In a routine screening assay used to detect cytotoxic compounds of marine origin, dictyostatin-1 was identified as a highly active component in an extract from a Lithistida sponge and exploration into its pharmacology was pursued. Initial studies demonstrated that dictyostatin-1 arrested cells in the G(2)/M phase of the cell cycle. Staining of these cells with antitubulin revealed cells having multiple aster formations and microtubule matrix bundling patterns similar to that seen in cells exposed to paclitaxel. Dictyostatin-1 was able to induce the polymerization of purified bovine brain tubulin in vitro and the polymerized tubulin remained stable at cold temperatures. Dictyostatin-1 also proved to be highly potent in two paclitaxel-resistant human cancer cell lines expressing active P-glycoprotein. Together, these results indicate that dictyostatin-1 is a potent inducer of tubulin polymerization and retains activity in cells expressing the P-glycoprotein efflux pump.


Angewandte Chemie | 2011

Leiodermatolide, a Potent Antimitotic Macrolide from the Marine Sponge Leiodermatium sp.

Ian Paterson; Stephen M. Dalby; Jill C. Roberts; Guy J. Naylor; Esther A. Guzmán; Richard A. Isbrucker; Tara P. Pitts; Pat Linley; Daniela Divlianska; John K. Reed; Amy E. Wright

Leiodermatolide is a structurally unique macrolide, isolated from the deep-water marine sponge Leiodermatium sp., which exhibits potent antiproliferative activity against a range of human cancer cell lines (IC50 <10 nM) and dramatic effects on spindle formation in mitotic cells. Its unprecedented polyketide skeleton and stereochemistry were established using a combination of experimental and computational (DP4) NMR methods, and molecular modelling.


Journal of Pharmacology and Experimental Therapeutics | 2009

Early Effects of Lasonolide A on Pancreatic Cancer Cells

Richard A. Isbrucker; Esther A. Guzmán; Tara P. Pitts; Amy E. Wright

Lasonolide A, a novel polyketide-derived macrolide, was previously identified from an extract of the marine sponge Forcepia sp. in an assay for protein kinase C (PKC) inhibitors. Cytotoxicity testing and profiling of lasonolide A in the National Cancer Institute (NCI) 60 cell panel screen revealed that it was potent toward a broad range of cell lines and also suggested a unique mechanism of action. Contrary to expected results, we found lasonolide A to be a strong activator of PKC in Panc-1 pancreatic carcinoma cells. Downstream mitogen-activated protein kinases, ERK 1/2 and p38 were also rapidly phosphorylated in response to lasonolide A, as was Akt. Microscopy studies revealed that lasonolide A induced blebbing and contraction of the cells within minutes of exposure, and the eventual loss of adherence. However, membrane integrity was maintained and the effects were reversible if lasonolide A was washed from the cells after their loss of adherence. Pretreatment of cells with a myosin II inhibitor, blebbistatin, slowed the early onset, but did not prevent the morphological effects of lasonolide A. Cells stained for actin filaments showed some reduction in stress fiber structure after lasonolide A exposure; however, it did not affect the polymerization of purified actin in vitro. Bisindolemaleimide, a PKC inhibitor, and wortmannin, a phosphoinositide 3-kinase; inhibitor, did not reduce lasonolide A-induced contraction or blebbing or the activation of mitogen-activated protein kinases, although Akt phosphorylation was prevented by wortmannin pretreatment. Our results indicate that lasonolide A activates multiple signal transduction pathways and suggest that the origin is upstream of PKC.


Journal of Natural Products | 2004

Plakolide a, a new γ-lactone from the marine sponge Plakortis sp.

Sarath P. Gunasekera; Richard A. Isbrucker; Ross E. Longley; Amy E. Wright; Shirley A. Pomponi; John K. Reed


Archive | 2001

Biologically active analogs of discodermolide

Sarath P. Gunasekera; Ross E. Longley; Richard A. Isbrucker; Gopal K. Paul; Shirley A. Pomponi; Amy E. Wright


Archive | 2001

Discalamide compounds and their use as anti-proliferative agents

Sarath P. Gunasekera; Ross E. Longley; Gopal K. Paul; Richard A. Isbrucker; Shirley A. Pomponi


Archive | 2001

Novel compositions and uses of dictyostatin compounds

Amy E. Wright; Jennifer L. Cummins; Shirley A. Pomponi; Ross E. Longley; Richard A. Isbrucker


Archive | 1999

Use of imidazole and indole compounds as inhibitors of nitric oxide synthase

Ross E. Longley; Richard A. Isbrucker; Amy E. Wright


Archive | 2003

Compositions and uses of dictyostatin compounds

Amy E. Wright; Jennifer L. Cummins; Shirley A. Pomponi; Ross E. Longley; Richard A. Isbrucker


Archive | 2000

Antiproliferative activity of microsclerodermins

Amy E. Wright; Shirley A. Pomponi; Ross E. Longley; Richard A. Isbrucker

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Amy E. Wright

Harbor Branch Oceanographic Institute

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Shirley A. Pomponi

Harbor Branch Oceanographic Institute

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Esther A. Guzmán

Harbor Branch Oceanographic Institute

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John K. Reed

Harbor Branch Oceanographic Institute

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Tara P. Pitts

Harbor Branch Oceanographic Institute

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Daniela Divlianska

Harbor Branch Oceanographic Institute

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Jill C. Roberts

Harbor Branch Oceanographic Institute

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Pat Linley

Harbor Branch Oceanographic Institute

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