The overarching goal of the Bioinformatics, Data Analytics and Predictive Modeling Core is to support our users' informatics needs and to create innovative informatics resources for the addiction and neuroscience fields to advance our understanding of the cell-cell signaling, drug addiction and drug exposure processes. High- throughput peptidomics, proteomics, metabolomics, transcriptomics, and genomics studies advance our understanding of the molecular processes associated with health and disease, and encompass sequencing, identification, and profiling of peptides, proteins, protein assemblies, metabolites, transcripts, and genes. The integration of this information strengthens the characterization of molecular pathways underlying the effects of exposure to drugs of abuse. Challenges arise from examining complex mixtures of proteins and peptides, and from analyzing massive volumes of data from peptides, protein and transcript isoforms, and genes. These challenges are magnified when studying neuropeptides because of their complex post-transcriptional and post- translational processing. Studying neurotransmitters, proteins, protein complexes, and metabolites present comparable challenges. Our Core's steadfast mission is to develop and facilitate the use of robust and sensitive analytical tools to advance the understanding of molecular processes associated with drug exposure and cell signaling. We have become a premier resource for the annotation, prediction, and characterization of neuropeptides and proteoforms while sharing our findings through public repositories and open source discovery tools. Our mission is accomplished by (a) developing needed bioinformatics resources; and (b) collaborating with the Sampling and Separation Core and the Molecular Profiling and Characterization Core in assisting users on bioinformatics matters, including experimental design; advanced analysis, benchmarking, and cross-validation; and visualization of the findings. Addressing present bioinformatic limitations, four Aims are proposed: (1) rigorous identification of peptides and proteins; (2) precise detection and quantification of the peptides linked to cell-cell signaling; (3) enhanced characterization of driver molecules and molecular relationships associated with cell signaling and drug exposure; and (4) precise characterization and quantification of the proteoforms and protein complexes linked to cell-cell signaling and dug exposure. The significance of the proposed efforts centers on the development of bioinformatics resources that will improve the accuracy and precision of peptide, protein, proteoform, protein complex, metabolite, and transcript identification and characterization through the integration of multi-omic information. The developed approaches will be applied to augment our understanding of addiction- associated pathways and shared with the neuroscience community.

Agency
National Institute of Health (NIH)
Institute
National Institute on Drug Abuse (NIDA)
Type
Center Core Grants (P30)
Project #
2P30DA018310-16
Application #
9793942
Study Section
Special Emphasis Panel (ZDA1)
Project Start
Project End
Budget Start
2019-06-01
Budget End
2020-05-31
Support Year
16
Fiscal Year
2019
Total Cost
Indirect Cost
Name
University of Illinois Urbana-Champaign
Department
Type
DUNS #
041544081
City
Champaign
State
IL
Country
United States
Zip Code
61820
Tillmaand, Emily G; Sweedler, Jonathan V (2018) Integrating Mass Spectrometry with Microphysiological Systems for Improved Neurochemical Studies. Microphysiol Syst 2:
Greenwood, Michael P; Greenwood, Mingkwan; Romanova, Elena V et al. (2018) The effects of aging on biosynthetic processes in the rat hypothalamic osmoregulatory neuroendocrine system. Neurobiol Aging 65:178-191
Shen, Mei; Qu, Zizheng; DesLaurier, Justin et al. (2018) Single Synaptic Observation of Cholinergic Neurotransmission on Living Neurons: Concentration and Dynamics. J Am Chem Soc 140:7764-7768
Sorokina, Anastasia M; Saul, Michael; Goncalves, Tassia M et al. (2018) Striatal transcriptome of a mouse model of ADHD reveals a pattern of synaptic remodeling. PLoS One 13:e0201553
Anapindi, Krishna D B; Romanova, Elena V; Southey, Bruce R et al. (2018) Peptide identifications and false discovery rates using different mass spectrometry platforms. Talanta 182:456-463
Southey, Bruce R; Romanova, Elena V; Rodriguez-Zas, Sandra L et al. (2018) Bioinformatics for Prohormone and Neuropeptide Discovery. Methods Mol Biol 1719:71-96
Neumann, Elizabeth K; Do, Thanh D; Comi, Troy J et al. (2018) Exploring the Fundamental Structures of Life: Non-targeted, Chemical Analysis of Single Cells and Subcellular Structures. Angew Chem Int Ed Engl :
Welle, Theresa M; Alanis, Kristen; Colombo, Michelle L et al. (2018) A high spatiotemporal study of somatic exocytosis with scanning electrochemical microscopy and nanoITIES electrodes. Chem Sci 9:4937-4941
Zheng, Jianbin; Chen, Long; Skinner, Owen S et al. (2018) ?-Glucocerebrosidase Modulators Promote Dimerization of ?-Glucocerebrosidase and Reveal an Allosteric Binding Site. J Am Chem Soc 140:5914-5924
Zhang, Guo; Yuan, Wang-Ding; Vilim, Ferdinand S et al. (2018) Newly Identified Aplysia SPTR-Gene Family-Derived Peptides: Localization and Function. ACS Chem Neurosci 9:2041-2053

Showing the most recent 10 out of 227 publications