Amino Acid Derivatives as New Zinc Binding Groups for the Design of Selective Matrix Metalloproteinase Inhibitors | Zendy

Mariateresa Giustiniano | Zendy; Paolo Tortorella | Zendy; Mariangela Agamen | Zendy; Antonella Di Pizio | Zendy; Armando Rossello | Zendy; Elisa Nuti | Zendy; Isabel GómezMonterrey | Zendy; Ettore Novellino | Zendy; Pietro Campiglia | Zendy; Ermelinda Vernieri | Zendy; Marina Sala | Zendy; Alessia Bertamino | Zendy; Alfonso Carotenuto | Zendy

AI Assistant Blog Pricing

Home ZAIA Blog

Open Access

Amino Acid Derivatives as New Zinc Binding Groups for the Design of Selective Matrix Metalloproteinase Inhibitors

Author(s) -

Mariateresa Giustiniano,

Paolo Tortorella,

Mariangela Agamen,

Antonella Di Pizio,

Armando Rossello,

Elisa Nuti,

Isabel GómezMonterrey,

Ettore Novellino,

Pietro Campiglia,

Ermelinda Vernieri,

Marina Sala,

Alessia Bertamino,

Alfonso Carotenuto

Publication year - 2013

Publication title -

journal of amino acids

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 0.188

H-Index - 5

eISSN - 2090-0112

pISSN - 2090-0104

DOI - 10.1155/2013/178381

Subject(s) - matrix metalloproteinase , sulfonamide , biochemistry , binding site , small molecule , enzyme , zinc , matrix metalloproteinase inhibitor , amino acid , hydroxamic acid , medicine , drug discovery , combinatorial chemistry , computational biology , chemistry , biology , stereochemistry , organic chemistry

A number of matrix metalloproteinases (MMPs) are important medicinal targets for conditions ranging from rheumatoid arthritis to cardiomyopathy, periodontal disease, liver cirrhosis, multiple sclerosis, and cancer invasion and metastasis, where they showed to have a dual role, inhibiting or promoting important processes involved in the pathology. MMPs contain a zinc (II) ion in the protein active site. Small-molecule inhibitors of these metalloproteins are designed to bind directly to the active site metal ions. In an effort to devise new approaches to selective inhibitors, in this paper, we describe the synthesis and preliminary biological evaluation of amino acid derivatives as new zinc binding groups (ZBGs). The incorporation of selected metal-binding functions in more complex biphenyl sulfonamide moieties allowed the identification of one compound able to interact selectively with different MMP enzymatic isoforms.

The content you want is available to Zendy users.

Already have an account? Click here to sign in.

Having issues? You can contact us here

Accelerating Research