Abstract

There is a significant demand for successful acceptance of transplanted organs into the compromised patient. T cells interfere with this process;therefore, new approaches to block their activity against the graft must be identified. Previous work suggested that pharmacological agents that uncouple signal transducer and activator of transcription (Stat)5a and StatSb activity can prolong allograft survival and Stat5a/b knockout mice can display graft tolerance. This project is based on the hypothesis that Stat5a/b regulates previously uncharacterized T-cell survival genes, both pro- and anti-apoptotic, and seeks to identify these novel genes to monitor their induction during transplantation tolerance. The central hypothesis is that inhibition of Stat5a/b can promote permanent acceptance of allografts without chronic therapy associated with current and toxic immunosuppressants. The objective of this pilot study is to identify murine Stat5a/b responsive genes as regulators of T-cell activity believing that these new targets should result in novel biomarkers that can be used in the design of new tolerance inducing regimes within the following interrelated aims: 1. Identify Stat5a/b target genes (StatS Dependent Gene Database S5GD) responsible for T-cell death from Stat5a/b-/- mice as compared to Stat5a/b+/+ mice using Affymetrix microarrays. 2. (A) Identify """"""""Acceptor vs. Rejecter"""""""" Gene Database (ARGD) from C3H heart transplanted Stat5a/b-/- mice vs. Stat5a/b+/+ mice on Day 7 using Affymetrix microarrays. (B) Identify Graft Specific Gene Database (GSGD)from C3H heart acceptor Stat5a/b-/- mice on Day 7 compared to Day 50 using Affymetrix microarrays. 3. Identify the overlapping biomarker gene databases (by aligning S5GD, ARGD and GSGD) and validate putative T-cell regulatory genes in mice undergoing organ graft rejection compared to tolerized mice by Q RT PCR (heart rejection model). Relevance to public health: We propose to focus on two proteins critical for immune cells to cause rejection !of transplanted organs, namely StatSa and StatSb. We seek to understand the mechanism by which blocking these proteins can enhance the life of the transplanted organ. New strategies should result that will allow for therapeutic approaches to be designed. Additionally, novel biomarkers will be identified to more efficiently monitor a patient's response to a given therapy

Public Health Relevance

We propose to focus on two proteins critical for immune cells to cause rejection of transplanted organs, namely Stat5a and Stat5b. We seek to understand the mechanism by which blocking these proteins can enhance the life of the transplanted organ. New strategies should result that will allow for therapeutic approaches to be designed. Additionally, novel biomarkers will be identified to more efficiently monitor a patient's response to a given therapy.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Minority Biomedical Research Support - MBRS (S06)
Project #
5S06GM008012-40
Application #
8080333
Study Section
Minority Programs Review Committee (MPRC)
Project Start
Project End
Budget Start
2010-06-01
Budget End
2011-05-31
Support Year
40
Fiscal Year
2010
Total Cost
$61,932
Indirect Cost

  Institution

Name
University of Texas El Paso
Department
Type
DUNS #
132051285
City
El Paso
State
TX
Country
United States
Zip Code
79968

  Publications

Rocha-Gutiérrez, Beatriz A; Lee, Wen-Yee; Shane Walker, W (2016) Mass balance and mass loading of polybrominated diphenyl ethers (PBDEs) in a tertiary wastewater treatment plant using SBSE-TD-GC/MS. Water Sci Technol 73:302-8
Vargas-Medrano, Javier; Sierra-Fonseca, Jorge A; Plenge-Tellechea, Luis F (2016) 1,2-Dichlorobenzene affects the formation of the phosphoenzyme stage during the catalytic cycle of the Ca(2+)-ATPase from sarcoplasmic reticulum. BMC Biochem 17:5
Buhaya, Munir H; Galvan, Steven; Maldonado, Rosa A (2015) Incidence of Trypanosoma cruzi infection in triatomines collected at Indio Mountains Research Station. Acta Trop 150:97-9
Vasquez, Miguel A; Iniguez, Eva; Das, Umashankar et al. (2015) Evaluation of ?,?-unsaturated ketones as antileishmanial agents. Antimicrob Agents Chemother 59:3598-601
Serna, Carylinda; Lara, Joshua A; Rodrigues, Silas P et al. (2014) A synthetic peptide from Trypanosoma cruzi mucin-like associated surface protein as candidate for a vaccine against Chagas disease. Vaccine 32:3525-32
Rodrigues, Marcio L; Nakayasu, Ernesto S; Almeida, Igor C et al. (2014) The impact of proteomics on the understanding of functions and biogenesis of fungal extracellular vesicles. J Proteomics 97:177-86
Dagda, Ruben K; Gasanov, Sardar E; Zhang, Boris et al. (2014) Molecular models of the Mojave rattlesnake (Crotalus scutulatus scutulatus) venom metalloproteinases reveal a structural basis for differences in hemorrhagic activities. J Biol Phys 40:193-216
Rico-Martínez, Roberto; Walsh, Elizabeth J (2013) Sexual Reproductive Biology of a Colonial Rotifer Sinantherina socialis (Rotifera: Monogononta): Do mating strategies vary between colonial and solitary rotifer species? Mar Freshw Behav Physiol 46:419-430
Jin, Seoweon; Staniswalis, Joan G; Mallawaarachchi, Indika (2013) Principal Differential Analysis with a Continuous Covariate: Low Dimensional Approximations for Functional Data. J Stat Comput Simul 83:
Dagda, Ruben K; Gasanov, Sardar; De La Oiii, Ysidro et al. (2013) Genetic Basis for Variation of Metalloproteinase-Associated Biochemical Activity in Venom of the Mojave Rattlesnake (Crotalus scutulatus scutulatus). Biochem Res Int 2013:251474

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