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A Bioinorganic Approach to Matrix Metalloproteinase Inhibition

Author: David Thomas Puerta
Publisher:
ISBN:
Category :
Languages : en
Pages : 216

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Book Description
In an effort to develop potent inhibitors of matrix metalloproteinases (MMPs), a bioinorganic approach was employed. The synthesis of [(TpPh, Me)Zn(OH)] provided for a structural analogue of the zinc-(tris-histidine) catalytic site of MMPs. The model complex was used to gain insight into the discrepancy of MMP inhibitor (MPI) potencies between mercapto alcohols and mercapto ketones. This initial experiment validated the use of the inorganic model complex as a structural model of the MMP catalytic site. Novel ZBGs for incorporation into MPIs were identified. These ZBGs were complexed with [(TpPh, Me)Zn(OH)] to obtain structural information such as binding mode, bond lengths, and coordination geometry. All ZBG examined were found to bind the model complex in a bidentate fashion, indicating promise for incorporation into a full length MPI. The inhibitory ability of the novel ZBGs was examined in both fluorescent and colorimetric assays using either the catalytic domain of MMPs or native enzyme expressed in a cell culture of neonatal rat ventricular fibroblasts. All novel ZBGs examined were found to be better inhibitors of MMPs in vitro and in cell culture assays than acetohydroxamic acid (the representative ZBG used in the majority of MPIs to date). In order to design full-length MPIs, a combined computational-bioinorganic method was developed. Using the structural coordinates from the [(TpPh, Me)Zn(ZBG)] complexes, the novel ZBGs were modeled into an X-ray crystal structure of uninhibited MMP-3. This study allowed for the examination of the ZBGs in the active site of an MMP. The novel ZBGs were found to have orientations in the active site of MMP-3 amendable to the attachment of a peptidomimetic backbone, necessary for a full-length MPI. Finally, the first MPIs based on the heterocyclic ZBGs were developed. The combined computational-bioinorganic method was augmented with the drug discovery program LUDI. Using LUDI enhanced with structural coordinates from [(TpPh, Me)Zn(3-hydroxy-2-methyl-4-pyrone)], several MPIs were designed. The potential inhibitors were synthesized and were examined in a fluorescence-based assay of MMP-1, -2, and -3. The pyrone-based MPIs were found to be more potent than their hydroxamate analogues, demonstrating the efficacy of a bioinorganic approach to the development of metalloprotein inhibitors.

A Bioinorganic Approach to Matrix Metalloproteinase Inhibition

Author: David Thomas Puerta
Publisher:
ISBN:
Category :
Languages : en
Pages : 216

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Heterocyclic Metal-binding Groups for Matrix Metalloproteinase and Anthrax Lethal Factor Inhibition

Author: Jana Ann-Sook Lewis
Publisher:
ISBN: 9789516055742
Category :
Languages : en
Pages : 255

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Book Description
After presenting the syntheses of thiopyrone and hydroxypyridinethione ligands, the coordination chemistry with iron(III), nickel(II), copper(II), cobalt(II), zinc(II), and lead(II) ions will be described. Characterization of these complexes represents a fundamental step for considering the use of heterocyclic ligands for medicinal and environmental applications.

Matrix Metalloproteinase Inhibitors in Cancer Therapy

Author: Neil J. Clendeninn
Publisher: Springer Science & Business Media
ISBN: 159259011X
Category : Medical
Languages : en
Pages : 371

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Book Description
Cutting-edge investigators review the current status of the entire field, from the biology of MMPs through the current clinical studies. The authors include many leading scientists from pharmaceutical companies who present all the latest concepts and results on the preferred design strategies for MMP inhibitors, their molecular mechanisms, and their substrates. In addition, they fully describe their personal research on specific MMP inhibitors, detailing vanguard design strategies, their in vitro activity, the outcome of animal model studies and, where available, their toxicology, safety, efficacy in human clinical trials. Comprehensive and state-of-the-art, Matrix Metalloproteinase Inhibitors in Cancer Therapy offers basic and clinical investigators alike a richly informative summary of all the latest research on these powerful new drugs, and their high promise as emerging cancer therapeutics.

Bioinorganic Tools and Zinc Selective Inhibitors for Matrix Metalloproteinases

Author: Faith E. Jacobsen
Publisher:
ISBN:
Category :
Languages : en
Pages : 225

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Book Description
The use of bioinorganic tools for elucidating metal-ligand interactions has been examined. This thesis will first discuss the use of model complexes for the active site of the zinc(II)-dependent hydrolytic enzyme matrix metalloproteinases (MMP). Using these model complexes to understand how ligands bind the metal has helped in understanding the effects of pKa and hydrogen bonding on the binding mode of a variety of chelators. This binding mode can also be related to the potency of these groups as inhibitors of MMP-3. After discussing the use of zinc(II) model complexes, the use of cobalt(II) model complexes will be examined. Cobalt(II) model complexes are spectroscopic active analogs of the MMP active site. These model complexes were used to study the dynamics of these complexes in solution. These complexes have been studied by electronic absorption, X-ray diffraction, electron paramagnetic resonance and paramagnetic NMR to demonstrate how cobalt(II) complexes can be used as an alternative to protein crystallography to determine the binding mode of different ligands. After the study of cobalt(II) model complexes, the design of zinc(II) selective binding groups will be discussed. These nitrogen based groups preferentially bind zinc over iron. As well, synthesis of full length inhibitors based on these groups will be presented. These inhibitor studies have allowed a deeper understanding for how the binding groups orient in the active site of the MMP and reveal the best location for a backbone substituent. Finally, cellular studies of an inflammatory model will be discussed. This macrophage model contains five different metalloenzymes. In one experiment, the effect of each ligand on the activity of these metalloenzymes is analyzed. This allows us to understand some of the potential drawbacks and benefits of the metal binding groups utilized. As well, this method can be used as a screening tool for full length inhibitors of MMPfor full length inhibitors of MMPs.

Matrix Metalloproteinase Inhibitors

Author: Satya Prakash Gupta
Publisher: Springer Science & Business Media
ISBN: 303480363X
Category : Medical
Languages : en
Pages : 293

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Book Description
Matrix metalloproteinases (MMPs) are proteolytic enzymes that are involved in many physiological and pathological processes. The field of MMP research is very important due to the implications of the distinct paralogs in both human physiology and pathology. Over-activation of these enzymes results in tissue degradation, producing a wide array of disease processes such as rheumatoid arthritis, osteoarthritis, tumor growth and metastasis, multiple sclerosis, congestive heart failure, and others. Thus MMP inhibitors are candidates for therapeutic agents to combat a number of diseases. The present book discusses the design and development of different classes of inhibitors of important classes of MMPs, such as gelatinases and collagenases. The articles focus specifically on structure-activity relationships of all classes of compounds and on their modes of action and specificity of binding with the receptors based on experimental and theoretical studies. These studies constitute a valuable asset for all those involved in drug development.

Matrix Metalloproteinases

Author:
Publisher: Elsevier
ISBN: 0080535984
Category : Science
Languages : en
Pages : 375

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Book Description
The chapters in this book thoroughly cover the structure, regulation, and function of matrix metalloproteinases, and provide information on the latest strategies to inhibit enzyme activity. This work will be an indispensable reference tool for investigators with an interest in extracellular matrix biology, matrix turnover, enzymology and biochemistry of proteinases, developmental biology, pathology, and therapeutic interventions. - Provides state-of-the-art information on a field with broad implications to many areas of biology - Includes detailed coverage of the structure and regulation of all major matrix metalloproteinases - Chapters focus on a timely and expanding field - Topics have direct relevance to understanding human disease pathology of cancer, arthritis, and vascular disease - Discusses latest strategies used in the development of new therapeutics to inhibit metalloproteinase activity

Metalloendopeptidases—Advances in Research and Application: 2012 Edition

Author:
Publisher: ScholarlyEditions
ISBN: 1464994277
Category : Medical
Languages : en
Pages : 405

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Book Description
Metalloendopeptidases—Advances in Research and Application: 2012 Edition is a ScholarlyEditions™ eBook that delivers timely, authoritative, and comprehensive information about Metalloendopeptidases. The editors have built Metalloendopeptidases—Advances in Research and Application: 2012 Edition on the vast information databases of ScholarlyNews.™ You can expect the information about Metalloendopeptidases in this eBook to be deeper than what you can access anywhere else, as well as consistently reliable, authoritative, informed, and relevant. The content of Metalloendopeptidases—Advances in Research and Application: 2012 Edition has been produced by the world’s leading scientists, engineers, analysts, research institutions, and companies. All of the content is from peer-reviewed sources, and all of it is written, assembled, and edited by the editors at ScholarlyEditions™ and available exclusively from us. You now have a source you can cite with authority, confidence, and credibility. More information is available at http://www.ScholarlyEditions.com/.

Matrix Metalloproteinase Inhibitors

Author: Satya Prakash Gupta
Publisher: Springer
ISBN: 9783034803656
Category : Medical
Languages : en
Pages : 286

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Development of zine binding peptidominetics for inhibition of matrix metalloproteinases by application of a combinatorial solid phase approach

Author: Casper Christensen
Publisher:
ISBN:
Category :
Languages : da
Pages :

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Book Description

Metalloendopeptidases—Advances in Research and Application: 2013 Edition

Author:
Publisher: ScholarlyEditions
ISBN: 1481677578
Category : Medical
Languages : en
Pages : 242

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Book Description
Metalloendopeptidases—Advances in Research and Application: 2013 Edition is a ScholarlyEditions™ book that delivers timely, authoritative, and comprehensive information about Lysostaphin. The editors have built Metalloendopeptidases—Advances in Research and Application: 2013 Edition on the vast information databases of ScholarlyNews.™ You can expect the information about Lysostaphin in this book to be deeper than what you can access anywhere else, as well as consistently reliable, authoritative, informed, and relevant. The content of Metalloendopeptidases—Advances in Research and Application: 2013 Edition has been produced by the world’s leading scientists, engineers, analysts, research institutions, and companies. All of the content is from peer-reviewed sources, and all of it is written, assembled, and edited by the editors at ScholarlyEditions™ and available exclusively from us. You now have a source you can cite with authority, confidence, and credibility. More information is available at http://www.ScholarlyEditions.com/.