Abstract

Allograft rejection, acute and chronic, is a common complication of organ transplantation, significantly Increases medical costs, but more Importantly It dramatically and negatively affects the lives of patients. In the previous grant period we have carried out a large-scale mass spectrometry-based proteomic analysis in clinical samples from patients undergoing acute and the chronic kidney transplant rejection and compared these to patients with healthy transplants. We have studied biopsies and peripheral blood Including purified, activated T and B cells. We have identified 1,000s of proteins differentially expressed among the patient cohorts with various clinical outcomes. Many of these proteins belong to key cellular, innate immunity, inflammatory and tissue remodeling pathways and are very likely the first proteomic signatures of rejection. We propose to continue our work with transplant proteomics and to extend our studies Into the areas of clinical proteomic assay development, heart transplant rejection, and human lymphocyte phosphoproteomlcs.
In Specific Aim #1 we are proposing to develop a diagnostic, high-throughput clinical proteomic blood-based assay for acute and chronic rejection based on selected reaction monitoring (SRM) targeted mass spectrometry. The large-scale discovery efforts from the previous grant period yielded many potential targets for candidate biomarkers that will be validated via SRM and developed into a diagnostic assay.
In Specific Aim #2 we are going to perform large-scale discovery-based mass spectrometry proteomic analysis of acute and chronic heart transplant rejection. We hope to unravel some of the molecular mechanisms and biological functions that are indicative of heart transplant rejection by further comparing our new data to the proteomic data from the kidney transplant system.
Specific Aim #3 is geared toward the phosphoproteomic analysis of transplant rejection. We are proposing to Identify and quantify proteins that become phosphorylated as a response to transplant rejection. We will profile the CD4 T and B cells from patients undergoing transplant rejection and Investigate signaling changes taking place due to the transplant related Immunosuppression, T and B cell activation and Inflammatory processes.

Public Health Relevance

The work proposed In this grant Involves the following novel approaches In mass spectrometry-based proteomics applied to a clinical study. First, we propose to develop the first blood-based proteomic assay for acute and chronic kidney transplant rejection using SRM. We plan a comprehensive study of protein expression post heart transplantation from both transplant biopsies and peripheral blood. We will investigate the driving forces behind transplant rejection and test the hypothesis that there are common, unifying mechanisms of rejection for both heart and kidney transplants. Finally, we plan to perform a novel discovery study into phosphorylation events that drive cell-mediated immune responses and the efficacy of immunosuppression.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program--Cooperative Agreements (U19)
Project #
5U19AI063603-09
Application #
8382163
Study Section
Special Emphasis Panel (ZAI1-MFH-I)
Project Start
Project End
Budget Start
2012-09-01
Budget End
2013-08-31
Support Year
9
Fiscal Year
2012
Total Cost
$150,117
Indirect Cost
$34,494

  Institution

Name
Scripps Research Institute
Department
Type
DUNS #
781613492
City
La Jolla
State
CA
Country
United States
Zip Code
92037

  Publications

Meng, Xiangzhi; Riley, Nicole; Thompson, Ryan et al. (2018) Investigate Global Chromosomal Interaction by Hi-C in Human Naive CD4 T Cells. Methods Mol Biol 1712:239-252
Gioia, Louis; Siddique, Azeem; Head, Steven R et al. (2018) A genome-wide survey of mutations in the Jurkat cell line. BMC Genomics 19:334
Kurian, S M; Velazquez, E; Thompson, R et al. (2017) Orthogonal Comparison of Molecular Signatures of Kidney Transplants With Subclinical and Clinical Acute Rejection: Equivalent Performance Is Agnostic to Both Technology and Platform. Am J Transplant 17:2103-2116
Buzby, Jeffrey S; Williams, Shirley A; Schaffer, Lana et al. (2017) Allele-specific wild-type TP53 expression in the unaffected carrier parent of children with Li-Fraumeni syndrome. Cancer Genet 211:9-17
Modena, Brian D; Bleecker, Eugene R; Busse, William W et al. (2017) Gene Expression Correlated with Severe Asthma Characteristics Reveals Heterogeneous Mechanisms of Severe Disease. Am J Respir Crit Care Med 195:1449-1463
Modena, B D; Milam, R; Harrison, F et al. (2017) Changes in Urinary Microbiome Populations Correlate in Kidney Transplants With Interstitial Fibrosis and Tubular Atrophy Documented in Early Surveillance Biopsies. Am J Transplant 17:712-723
LaMere, Sarah A; Thompson, Ryan C; Meng, Xiangzhi et al. (2017) H3K27 Methylation Dynamics during CD4 T Cell Activation: Regulation of JAK/STAT and IL12RB2 Expression by JMJD3. J Immunol 199:3158-3175
Kurian, Sunil M; Novais, Marta; Whisenant, Thomas et al. (2016) Peripheral Blood Cell Gene Expression Diagnostic for Identifying Symptomatic Transthyretin Amyloidosis Patients: Male and Female Specific Signatures. Theranostics 6:1792-809
Savaryn, John P; Toby, Timothy K; Catherman, Adam D et al. (2016) Comparative top down proteomics of peripheral blood mononuclear cells from kidney transplant recipients with normal kidney biopsies or acute rejection. Proteomics 16:2048-58
Weinsheimer, Shantel; Bendjilali, Nasrine; Nelson, Jeffrey et al. (2016) Genome-wide association study of sporadic brain arteriovenous malformations. J Neurol Neurosurg Psychiatry 87:916-23

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