Abstract

Transport systems are responsible for the uptake of essential nutrients and ions, excretion of end products of metabolism, efflux of toxic substances and communication between cells and the environment. Fast growing genome-sequencing data and a wealth of biochemical, molecular and genetic literature has revealed thousands of members of transporter superfamilies. Most of the transporters share some common features, e.g. multiple alpha-helical transmembrane domains. However, they function differently in terms of mechanism and substrate specificity, and other characteristics. Analysis of sequence similarities suggests they may have different evolutionary origins and belong to unrelated families. In this research we use oligopeptide transporters as examples to investigate some of the structure-function relationships. The oligopeptide transport systems play an important role in the transporting of pharmacologically active peptide-like drugs in addition to the absorption and reclamation of natural small peptides. Understanding how oligopeptide transporters work is of great interest to both biological research and clinical application. Due to the difficulty to determine the 3-D structures of membrane proteins, we are using bioinformatics approaches in this research. The first goal of this project is to identify peptide transporters through database searching and analysis using available tools as well as those self-developed. At the end of the project, we expect to set up a criteria to assign each member to a specific subgroup. Another important goal is to investigate the literature to retrieve published information related to each of the transporters, e.g. substrate specificity and affinity, energy coupling mechanism, related disease pattern, function and regulation, etc. This information is essential to infer structure-function relationships of transporters. Finally, based on the research and information retrieved, the third goal of this project is to generate a prototype database for drug transporters that contains some of these relationships.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Center for Research Resources (NCRR)
Type
Biotechnology Resource Grants (P41)
Project #
5P41RR001081-23
Application #
6347879
Study Section
Project Start
2000-07-01
Project End
2001-06-30
Budget Start
1998-10-01
Budget End
1999-09-30
Support Year
23
Fiscal Year
2000
Total Cost
$136
Indirect Cost

  Institution

Name
University of California San Francisco
Department
Type
DUNS #
073133571
City
San Francisco
State
CA
Country
United States
Zip Code
94143

  Publications

Kozak, John J; Gray, Harry B; Garza-López, Roberto A (2018) Relaxation of structural constraints during Amicyanin unfolding. J Inorg Biochem 179:135-145
Alamo, Lorenzo; Pinto, Antonio; Sulbarán, Guidenn et al. (2018) Lessons from a tarantula: new insights into myosin interacting-heads motif evolution and its implications on disease. Biophys Rev 10:1465-1477
Viswanath, Shruthi; Chemmama, Ilan E; Cimermancic, Peter et al. (2017) Assessing Exhaustiveness of Stochastic Sampling for Integrative Modeling of Macromolecular Structures. Biophys J 113:2344-2353
Chu, Shidong; Zhou, Guangyan; Gochin, Miriam (2017) Evaluation of ligand-based NMR screening methods to characterize small molecule binding to HIV-1 glycoprotein-41. Org Biomol Chem 15:5210-5219
Portioli, Corinne; Bovi, Michele; Benati, Donatella et al. (2017) Novel functionalization strategies of polymeric nanoparticles as carriers for brain medications. J Biomed Mater Res A 105:847-858
Alamo, Lorenzo; Koubassova, Natalia; Pinto, Antonio et al. (2017) Lessons from a tarantula: new insights into muscle thick filament and myosin interacting-heads motif structure and function. Biophys Rev 9:461-480
Nguyen, Hai Dang; Yadav, Tribhuwan; Giri, Sumanprava et al. (2017) Functions of Replication Protein A as a Sensor of R Loops and a Regulator of RNaseH1. Mol Cell 65:832-847.e4
Sofiyev, Vladimir; Kaur, Hardeep; Snyder, Beth A et al. (2017) Enhanced potency of bivalent small molecule gp41 inhibitors. Bioorg Med Chem 25:408-420
Kozak, John J; Gray, Harry B; Garza-López, Roberto A (2016) Cytochrome unfolding pathways from computational analysis of crystal structures. J Inorg Biochem 155:44-55
Amlong, Corey A; Perkins, Mark G; Houle, Timothy T et al. (2016) Contrasting Effects of the ?-Aminobutyric Acid Type A Receptor ?3 Subunit N265M Mutation on Loss of Righting Reflexes Induced by Etomidate and the Novel Anesthetic Barbiturate R-mTFD-MPAB. Anesth Analg 123:1241-1246

Showing the most recent 10 out of 508 publications