Research Initiation Awards (RIAs) provide support for junior faculty at Historically Black Colleges and Universities (HBCUs) who are starting to build a research program, as well as for mid-career faculty who need to re-direct and re-build a research program. It is expected that the award helps to further the faculty member's research capability and effectiveness, improves research and teaching at the researcher's home institution, and involves undergraduate students in research experiences.

Fisk University's RIA project utilizes well established experimental structural biology and biophysical techniques to establish a transformative new paradigm for the mechanism of regulation of protein-protein interactions in signal transduction. The results will have a significant impact on the fields of structural biology and signal transduction. Characterization of the CP-RAGE VC1 complex at atomic-resolution represents a significant advance forward for S100 and RAGE biology. This would be the first high resolution structure of the RAGE ligand binding extracellular domain in complex with a protein, and one of few S100 proteins in complex with its cognate binding partner. Moreover, the approaches employed in this investigation represent a general approach to addressing mechanism of receptor activation.

This research addresses a critical gap in this knowledge by employing high resolution structural studies to reveal the atomic resolution details of the CP-RAGE complex. RAGE is a transmembrane protein comprised of three extracellular immunoglobulin domains (V, C1, and C2), a single transmembrane helix (TM), and a short intracellular peptide (IC). Like many other single pass receptors, activation is hypothesized to proceed through an oligomerization based conformational rearrangement that occurs during ligand binding.

The outcomes of the research initiation project will further the diversification of the STEM workforce by providing unparalleled training to students that have been historically underrepresented in STEM. This interdisciplinary program provides integrated research training and didactic coursework at the interface of chemistry, biology, and physics illustrating to students the impact of transdisciplinary research and high impact discovery. Undergraduate students will present their findings at regional and national meetings and will co-author peer-reviewed publications. As an NSF Experimental Program to Stimulate Competitive Research (EPSCoR) jurisdiction, the project will build research capability and capacity in the state as well as within this minority-serving institution.

Page A This research initiation award proposes to understand the molecular basis of interactions between the S100 calcium binding protein calprotectin (CP) and the receptor for advanced glycation endproducts (RAGE). CP binding to RAGE results in activation of the transcription factor NFkB, a molecule which plays a key role in inflammation. Despite the importance of this signaling axis, little is known about the structural details of the protein-protein interactions which govern CP-RAGE binding. This proposal addresses a critical gap in this knowledge by employing high resolution structural studies to reveal the atomic resolution details of the CP-RAGE complex. RAGE is a transmembrane protein comprised of three extracellular immunoglobulin domains (V, C1, and C2), a single transmembrane helix (TM), and a short intracellular peptide (IC). Like many other single pass receptors, activation is hypothesized to proceed through an oligomerization based conformational rearrangement that occurs during ligand binding. The focus of this proposal is on the V and C1 extracellular domains of RAGE (RAGE VC1) and how they contribute to CP binding and/or oligomerization during receptor activation. In order to address these questions, two complementary but independent objectives are proposed: Objective 1) Define the molecular basis for CP interaction with RAGE. Nuclear magnetic resonance spectroscopy (NMR) will be used to identify amino acid residues in CP and RAGE VC1 that are critical for binding. The NMR studies will be validated and used to guide strategies to create mutants in CP that are defective in RAGE binding as assayed by isothermal titration calorimetry. Objective 2) Characterize the oligomerization state of the CP-RAGE VC1 complex. X-ray crystallography will be used to determine the structure of the CP-RAGE VC1 complex. This structure will reveal high resolution details of the interaction between CP and RAGE, as well as interactions that define the oligomerization behavior of the overall complex. Intellectual Merit : The research initiation award utilizes well established experimental structural biology and biophysical techniques to establish a transformative new paradigm for the mechanism of regulation of protein-protein interactions in signal transduction. The results will have a significant impact on the fields of structural biology and signal transduction. Characterization of the CP-RAGE VC1 complex at atomic-resolution represents a significant advance forward for S100 and RAGE biology. This would be the first high resolution structure of the RAGE ligand binding extracellular domain in complex with a protein, and one of few S100 proteins in complex with its cognate binding partner. Moreover, the approaches employed in this proposal represent a general approach to addressing mechanism of receptor activation. Broader Impacts : The outcomes of this research initiation award will further the diversification of the STEM workforce by providing unparalleled training to students that have been traditionally underrepresented in STEM. This interdisciplinary program provides integrated research training and didactic coursework at the interface of chemistry, biology, and physics -illustrating to students the impact of transdisciplinary research and high impact discovery. Undergraduate students will present their findings at regional and national meetings, and will co-author peer-reviewed publications. Enhancements in research and curriculum infrastructure at Fisk University provided by this RIA will contribute to recruitment and retention of minorities in STEM disciplines, resulting in the development of early career scientists into discoverers and leaders in academic and research careers.

Agency
National Science Foundation (NSF)
Institute
Division of Human Resource Development (HRD)
Type
Standard Grant (Standard)
Application #
1400969
Program Officer
Martha James
Project Start
Project End
Budget Start
2014-08-01
Budget End
2017-07-31
Support Year
Fiscal Year
2014
Total Cost
$236,848
Indirect Cost
Name
Fisk University
Department
Type
DUNS #
City
Nashville
State
TN
Country
United States
Zip Code
37208