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Dive into the research topics where Kristine Gouveia is active.

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Featured researches published by Kristine Gouveia.


Journal of Biomolecular Screening | 2013

A Selective ATP-Binding Cassette Subfamily G Member 2 Efflux Inhibitor Revealed via High-Throughput Flow Cytometry

J. Jacob Strouse; Irena Ivnitski-Steele; Hadya M. Khawaja; Dominique Perez; Jerec Ricci; Tuanli Yao; Warren S. Weiner; Chad E. Schroeder; Denise S. Simpson; Brooks E. Maki; Kelin Li; Jennifer E. Golden; Terry D. Foutz; Anna Waller; Annette M. Evangelisti; Susan M. Young; Stephanie E. Chavez; Matthew Garcia; Oleg Ursu; Cristian G. Bologa; Mark B. Carter; Virginia M. Salas; Kristine Gouveia; George P. Tegos; Tudor I. Oprea; Bruce S. Edwards; Jeffrey Aubé; Richard S. Larson; Larry A. Sklar

Chemotherapeutics tumor resistance is a principal reason for treatment failure, and clinical and experimental data indicate that multidrug transporters such as ATP-binding cassette (ABC) B1 and ABCG2 play a leading role by preventing cytotoxic intracellular drug concentrations. Functional efflux inhibition of existing chemotherapeutics by these pumps continues to present a promising approach for treatment. A contributing factor to the failure of existing inhibitors in clinical applications is limited understanding of specific substrate/inhibitor/pump interactions. We have identified selective efflux inhibitors by profiling multiple ABC transporters against a library of small molecules to find molecular probes to further explore such interactions. In our primary screening protocol using JC-1 as a dual-pump fluorescent reporter substrate, we identified a piperazine-substituted pyrazolo[1,5-a]pyrimidine substructure with promise for selective efflux inhibition. As a result of a focused structure-activity relationship (SAR)–driven chemistry effort, we describe compound 1 (CID44640177), an efflux inhibitor with selectivity toward ABCG2 over ABCB1. Compound 1 is also shown to potentiate the activity of mitoxantrone in vitro as well as preliminarily in vivo in an ABCG2-overexpressing tumor model. At least two analogues significantly reduce tumor size in combination with the chemotherapeutic topotecan. To our knowledge, low nanomolar chemoreversal activity coupled with direct evidence of efflux inhibition for ABCG2 is unprecedented.


PLOS ONE | 2015

A Pan-GTPase Inhibitor as a Molecular Probe.

Lin Hong; Yuna Guo; Soumik BasuRay; Jacob O. Agola; Elsa Romero; Denise S. Simpson; Chad E. Schroeder; Peter C. Simons; Anna Waller; Matthew Garcia; Mark B. Carter; Oleg Ursu; Kristine Gouveia; Jennifer E. Golden; Jeffrey Aubé; Angela Wandinger-Ness; Larry A. Sklar

Overactive GTPases have often been linked to human diseases. The available inhibitors are limited and have not progressed far in clinical trials. We report here a first-in-class small molecule pan-GTPase inhibitor discovered from a high throughput screening campaign. The compound CID1067700 inhibits multiple GTPases in biochemical, cellular protein and protein interaction, as well as cellular functional assays. In the biochemical and protein interaction assays, representative GTPases from Rho, Ras, and Rab, the three most generic subfamilies of the GTPases, were probed, while in the functional assays, physiological processes regulated by each of the three subfamilies of the GTPases were examined. The chemical functionalities essential for the activity of the compound were identified through structural derivatization. The compound is validated as a useful molecular probe upon which GTPase-targeting inhibitors with drug potentials might be developed.


Journal of Biomolecular Screening | 2016

Discovery of Small-Molecule Nonfluorescent Inhibitors of Fluorogen–Fluorogen Activating Protein Binding Pair

Yang Wu; Shaun R. Stauffer; Robyn L. Stanfield; Phillip H. Tapia; Oleg Ursu; Gregory W. Fisher; Christopher Szent-Gyorgyi; Annette M. Evangelisti; Anna Waller; J. Jacob Strouse; Mark B. Carter; Cristian G. Bologa; Kristine Gouveia; Mike Poslusney; Alan S. Waggoner; Craig W. Lindsley; Jonathan W. Jarvik; Larry A. Sklar

A new class of biosensors, fluorogen activating proteins (FAPs), has been successfully used to track receptor trafficking in live cells. Unlike the traditional fluorescent proteins (FPs), FAPs do not fluoresce unless bound to their specific small-molecule fluorogens, and thus FAP-based assays are highly sensitive. Application of the FAP-based assay for protein trafficking in high-throughput flow cytometry resulted in the discovery of a new class of compounds that interferes with the binding between fluorogens and FAP, thus blocking the fluorescence signal. These compounds are high-affinity, nonfluorescent analogs of fluorogens with little or no toxicity to the tested cells and no apparent interference with the normal function of FAP-tagged receptors. The most potent compound among these, N,4-dimethyl-N-(2-oxo-2-(4-(pyridin-2-yl)piperazin-1-yl)ethyl)benzenesulfonamide (ML342), has been investigated in detail. X-ray crystallographic analysis revealed that ML342 competes with the fluorogen, sulfonated thiazole orange coupled to diethylene glycol diamine (TO1-2p), for the same binding site on a FAP, AM2.2. Kinetic analysis shows that the FAP-fluorogen interaction is more complex than a homogeneous one-site binding process, with multiple conformational states of the fluorogen and/or the FAP, and possible dimerization of the FAP moiety involved in the process.


Combinatorial Chemistry & High Throughput Screening | 2014

The University of New Mexico Center for Molecular Discovery

Bruce S. Edwards; Kristine Gouveia; Tudor I. Oprea; Larry A. Sklar


Archive | 2013

A small molecule pan-inhibitor of Ras-superfamily GTPases with high efficacy towards Rab7

Lin Hong; Peter C. Simons; Anna Waller; Juan Strouse; Zurab Surviladze; Oleg Ursu; Cristian G. Bologa; Kristine Gouveia; Jacob O. Agola; Soumik BasuRay; Angela Wandinger-Ness; Larry A. Sklar; Denise S. Simpson; Chad E. Schroeder; Jennifer E. Golden; Jeffrey Aubé


Archive | 2015

Discovering Small Molecules that Overcome Differentiation Arrest in Acute Myeloid Leukemia

David B. Sykes; Mark K. Haynes; Anna Waller; Matthew R. Garcia; Oleg Ursu; Kristine Gouveia; Larry A. Sklar; Tim Lewis; Sivaraman Dandapani; Benito Munoz; David T. Scadden; Michelle Palmer; Stuart L. Schreiber


Archive | 2013

Inhibitors of FAP-fluorogen interaction as a multiplex assay tool compound for receptor internalization assays

Yang Wu; Philip H. Tapia; Kristine Gouveia; Larry A. Sklar; Gregory W. Fisher; Alan S. Waggoner; Jonathan W. Jarvik; Alison R. Gregro; Mike Poslusney; Craig W. Lindsley; Shaun R. Stauffer


PLOS ONE | 2013

Histologic grades of inflammation in respiratory tract tissues of ferrets infected with three pandemic H1N1 viruses.

Frederick Koster; Kristine Gouveia; Yue Zhou; Kristin Sannes Lowery; Robert B. Russell; Heather MacInnes; Zemmie Pollock; R. Colby Layton; Jennifer Cromwell; Denise Toleno; John Pyle; Michael Zubelewicz; Kevin S. Harrod; Rangarajan Sampath; Steven A. Hofstadler; Peng Gao; Yushi Liu; Yung-Sung Cheng


Archive | 2013

Figure 2, Graph depicting stability of ML282 after 48 h in PBS (no additives)

Lin Hong; Peter C. Simons; Anna Waller; Juan Strouse; Zurab Surviladze; Oleg Ursu; Cristian Bologa; Kristine Gouveia; Jacob O. Agola; Soumik BasuRay; Angela Wandinger-Ness; Larry A. Sklar; Denise S. Simpson; Chad E. Schroeder; Jennifer E. Golden; Jeffrey Aubé


Archive | 2013

[Table, Experimental Results].

Lin Hong; Peter C. Simons; Anna Waller; Juan Strouse; Zurab Surviladze; Oleg Ursu; Cristian Bologa; Kristine Gouveia; Jacob O. Agola; Soumik BasuRay; Angela Wandinger-Ness; Larry A. Sklar; Denise S. Simpson; Chad E. Schroeder; Jennifer E. Golden; Jeffrey Aubé

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Larry A. Sklar

Vanderbilt University Medical Center

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Anna Waller

University of New Mexico

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Oleg Ursu

University of New Mexico

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Lin Hong

University of New Mexico

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Soumik BasuRay

University of New Mexico

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