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Featured researches published by Amir P. Tamiz.


International Journal of Pharmaceutics | 2009

Mechanism of action of ZOT-derived peptide AT-1002, a tight junction regulator and absorption enhancer.

Shobha Gopalakrishnan; Niranjan B. Pandey; Amir P. Tamiz; John Vere; Rosa Carrasco; Robert Somerville; Amit Tripathi; Mark J. Ginski; Blake Paterson; Sefik S. Alkan

Tight junctions (TJs) are intercellular structures that control paracellular permeability and epithelial polarity. It is now accepted that TJs are highly dynamic structures that are regulated in response to exogenous and endogenous stimuli. Here, we provide details on the mechanism of action of AT-1002, the active domain of Vibrio choleraes second toxin, zonula occludens toxin (ZOT). AT-1002, a hexamer peptide, caused the redistribution of ZO-1 away from cell junctions as seen by fluorescence microscopy. AT-1002 also activated src and mitogen activated protein (MAP) kinase pathways, increased ZO-1 tyrosine phosphorylation, and rearrangement of actin filaments. Functionally, AT-1002 caused a reversible reduction in transepithelial electrical resistance (TEER) and an increase in lucifer yellow permeability in Caco-2 cell monolayers. In vivo, co-administration of salmon calcitonin with 1 mg of AT-1002 resulted in a 5.2-fold increase in AUC over the control group. Our findings provide a mechanistic explanation for AT-1002-induced tight junction disassembly, and demonstrate that AT-1002 can be used for delivery of other agents in vivo.


Bioorganic & Medicinal Chemistry Letters | 2008

Structure–activity relationship studies of permeability modulating peptide AT-1002

Min Li; Ed Oliver; Kelly Kitchens; John Vere; Sefik S. Alkan; Amir P. Tamiz

AT-1002 a 6-mer synthetic peptide belongs to an emerging novel class of compounds that reversibly increase paracellular transport of molecules across the epithelial barrier. The aim of this project was to elaborate on the structure-activity relationship of this peptide with the specific goal to replace the P2 cysteine amino acid. Herein, we report the discovery of peptides that exhibit reversible permeability enhancement properties with an increased stability profile.


Bioorganic & Medicinal Chemistry Letters | 1999

N-phenylalkyl-substituted tropane analogs of boat conformation with high selectivity for the dopamine versus serotonin transporter.

K.R.C. Prakash; Amir P. Tamiz; Gian Luca Araldi; Mei Zhang; Kenneth M. Johnson; Alan P. Kozikowski

A series of N-phenylalkyl-substituted tropane analogs of boat conformation was synthesized, and these tropanes were evaluated for their ability to inhibit high affinity uptake of dopamine (DA) and serotonin (5-HT) into striatal nerve endings (synaptosomes). Some of these compounds exhibit high affinity for the DA transporter with a 5-HT/DA transporter selectivity ratio of >50.


Bioorganic & Medicinal Chemistry Letters | 2000

Design, synthesis and biological evaluation of 7-azatricyclodecanes: analogues of cocaine

Amir P. Tamiz; Miles P. Smith; Alan P. Kozikowski

The synthesis and biological activity of a series of azatricyclodecane analogues of cocaine are described. All compounds studied in this series exhibit nanomolar potency and good selectivity for the serotonin transporter versus the dopamine transporter.


Bioorganic & Medicinal Chemistry Letters | 2000

A convenient procedure for the synthesis of nonsymmetrical bivalent selective serotonin reuptake inhibitors using polymer-supported reagents

Amir P. Tamiz; Paola Conti; Mei Zhang; Kenneth M. Johnson; Alan P. Kozikowski

A convenient synthesis of nonsymmetrical bivalent inhibitors of the serotonin transporter is described. The synthesis utilizes polymer-supported reagents that allow for rapid access to novel bivalent ligands without the need for isolation or purification of synthetic intermediates.


Bioorganic & Medicinal Chemistry Letters | 2000

Synthesis and biological evaluation of 1-azabicyclo-[3.2.1]octanes: new dopamine transporter inhibitors

Amir P. Tamiz; Miles P. Smith; Istvan J. Enyedy; Judith L. Flippen-Anderson; Mei Zhang; Kenneth M. Johnson; Alan P. Kozikowski

The synthesis and biological activity of a series of 6-substituted 1-azabicyclo[3.2.1]octanes are described. 1-Azabicyclo[3.2.1]octanes represent a new class of compounds that exhibit monoamine transporter inhibitory activity highly dependent on the overall topology and the absolute stereochemistry of the molecule.


Peptides | 2012

Larazotide acetate promotes tight junction assembly in epithelial cells

Shobha Gopalakrishnan; Amit Tripathi; Amir P. Tamiz; Sefik S. Alkan; Niranjan B. Pandey


Archive | 2010

Use of tight junction antagonists to treat inflammatory bowl disease

Blake Paterson; Amir P. Tamiz; Niranjan B. Pandey


Pharmacology, Biochemistry and Behavior | 2001

Novel monoamine transporter ligands reduce cocaine-induced enhancement of brain stimulation reward

Monika Trzcińska; Patricia Pimentel; James R. Stellar; Robert N. Hanson; Sung Woon Choi; David R. Elmaleh; Jianrong Zhang; K.R.C. Prakash; Amir P. Tamiz; Alan P. Kozikowski; Kenneth M. Johnson; Miles P. Smith; John W. Babich


Archive | 2009

INHIBITION OF GLIADIN PEPTIDES

Sefik S. Alkan; Amir P. Tamiz; Kelly Kitchens; Malarvizhi Durai; Neil Poloso; Rosa Carrasco

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Blake Paterson

Johns Hopkins University School of Medicine

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Kenneth M. Johnson

University of Texas Medical Branch

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Mei Zhang

University of Texas Medical Branch

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Miles P. Smith

Georgetown University Medical Center

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K.R.C. Prakash

Georgetown University Medical Center

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