Abstract

Obesity affects a significant adult population worldwide and is associated with many human diseases such as autoimmune diseases, cardiovascular disorders, type 2 diabetes, respiratory diseases, and cancers. However, obesity is less studied than other human diseases like cancer or blood disorder. The global prevalence and fast-growing pace of obesity reflects critical and complex causal factors in modern society. Some epidemiological studies have shown that dietary intake such as fat and sugar is highly associated with obesity. Thus, understanding the mechanisms of diet-induced obesity will provide fundamental knowledge to prevent or treat obesity clinically or in daily life. Interestingly, the human microbiome contributes vital functions to human health or disease traits. Emerging evidence shows that the gut microbiome is intrinsically associated with obesity risk. Microbes can also be used as a revolutionary medical treatment, i.e. through fecal microbiota transplantation. Understanding the metabolic role of gut microbes in diet-induced obesity may provide alternative strategies to prevent or treat obesity. Previous studies have revealed a common core of bacteria comprised of phyla Firmicutes, Bacteroidetes and Actinobacteria, while the rest of the population can be diverse. The insights of this complex and unculturable microbe community and the critical functionalities are still very preliminary, as is understanding of host-microbe interaction in the gut. Despite a collection of culturable microbes identified in the human gut, a systematic and cost-effective way to co-culture the arbitrary microbe community with host cells or tissues is lacking. Thus, the solution relies heavily on the computation algorithm to fill the gap between host and microbes in understanding diet-induced obesity. In this project, three specific aims are proposed to apply scalable computation methods to understand the role of gut microbe community, host intestine cells, and host-microbe interactions that contribute to diet-induced obesity.
These aims are to: (1) identify a broader range of gut microbiota (culturable and unculturable) associated with obesity; (2) characterize heterogeneous host cell functions by single-cell transcriptomics; and (3) resolve host-microbe interactions by metabolomic modeling and genetic marks. The datasets - including multi-modal meta-omics gut microbial data and intestinal single-cell transcriptomics - will be generated in-house on mouse models with high-fat, medium-fat, and control diet plans. Successful completion of this project will provide deeper biological insights of the metabolic roles of gut microbes, host cells and host-microbe interactions associated with diet induced obesity, and also a powerful set of large-scale computational tools and techniques to conduct the host-microbe research in obesity or other related phenotypes.

Public Health Relevance

The proposed studies further the mission of the Nebraska Center for the Prevention of Obesity Diseases (NPOD) and will provide insights to further develop novel therapeutic strategies for obesity. The strong support from NPOD, its facilities, and mentorship program will enable Dr. Yao and his lab to move beyond this project toward an independent NIH grant and achieve his long-term research goals in studying host-microbe systems in human disease traits.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Exploratory Grants (P20)
Project #
5P20GM104320-07
Application #
10240341
Study Section
Special Emphasis Panel (ZGM1)
Program Officer
Mcguirl, Michele
Project Start
2020-08-17
Project End
2023-08-16
Budget Start
2020-06-01
Budget End
2021-05-31
Support Year
7
Fiscal Year
2020
Total Cost
Indirect Cost

  Institution

Name
University of Nebraska Lincoln
Department
Type
DUNS #
555456995
City
Lincoln
State
NE
Country
United States
Zip Code
68503

  Publications

Hakguder, Zeynep; Shu, Jiang; Liao, Chunxiao et al. (2018) Genome-scale MicroRNA target prediction through clustering with Dirichlet process mixture model. BMC Genomics 19:658
McAtee, Caitlin O; Booth, Christine; Elowsky, Christian et al. (2018) Prostate tumor cell exosomes containing hyaluronidase Hyal1 stimulate prostate stromal cell motility by engagement of FAK-mediated integrin signaling. Matrix Biol :
Manca, Sonia; Upadhyaya, Bijaya; Mutai, Ezra et al. (2018) Milk exosomes are bioavailable and distinct microRNA cargos have unique tissue distribution patterns. Sci Rep 8:11321
E Silva, Bruno Vieira Resende; Rad, Milad Ghiasi; Cui, Juan et al. (2018) A Mobile-Based Diet Monitoring System for Obesity Management. J Health Med Inform 9:
Fan, Rong; Toney, Ashley Mulcahy; Jang, Yura et al. (2018) Maternal n-3 PUFA supplementation promotes fetal brown adipose tissue development through epigenetic modifications in C57BL/6 mice. Biochim Biophys Acta Mol Cell Biol Lipids 1863:1488-1497
Nordgren, Tara M; Heires, Art J; Zempleni, Janos et al. (2018) Bovine milk-derived extracellular vesicles enhance inflammation and promote M1 polarization following agricultural dust exposure in mice. J Nutr Biochem 64:110-120
Martínez, Inés; Maldonado-Gomez, Maria X; Gomes-Neto, João Carlos et al. (2018) Experimental evaluation of the importance of colonization history in early-life gut microbiota assembly. Elife 7:
Zhang, Hanyuan; Vieira Resende E Silva, Bruno; Cui, Juan (2018) miRDis: a Web tool for endogenous and exogenous microRNA discovery based on deep-sequencing data analysis. Brief Bioinform 19:415-424
Leiferman, Amy; Shu, Jiang; Grove, Ryan et al. (2018) A diet defined by its content of bovine milk exosomes and their RNA cargos has moderate effects on gene expression, amino acid profiles and grip strength in skeletal muscle in C57BL/6 mice. J Nutr Biochem 59:123-128
Okla, Meshail; Zaher, Walid; Alfayez, Musaad et al. (2018) Inhibitory Effects of Toll-Like Receptor 4, NLRP3 Inflammasome, and Interleukin-1? on White Adipocyte Browning. Inflammation 41:626-642

Showing the most recent 10 out of 68 publications