Abstract

The purpose of this proposal is develop a program to attract undergraduate and graduate students who are majoring in engineering, informatics and computational disciplines to consider careers in the areas of digestive disease and metabolism and their related health disorders. The program is sponsored by the Department of Molecular &Integrative Physiology at the University of Michigan Medical School, and includes two components. One component is to develop and offer a graduate-level course, which may also be available as an upper-level undergraduate course, to teach physiology, bioinformatics, engineering and computer science students computational applications related to NIDDK research missions such diabetes, obesity and gastrointestinal cancers. It is anticipated that this course will attract graduate students, who have not selected a mentor, to pursue PhD projects related to digestive disease and metabolism. Students will be exposed to the research programs of 17 proposed Program Faculty mentors. All Program Faculty are funded investigators carrying out research in the areas of digestive disease or metabolism, and have primary or joint appointments in Physiology but also have appointments with Medicine, Pediatrics or Surgery. The second component is to establish summer research fellowships that provide opportunities for engineering and computational students to gain laboratory experience in the research areas of digestive or metabolic physiology. Students will attend a noon lecture series that introduces them to multiple aspects of physiology-related research including the use of different model organisms, ethical issues in laboratory research, and career opportunities in biomedical sciences. The research experience will culminate in a half-day symposium that includes oral presentations given by the students summarizing their research projects. Program oversight will be provided by a highly qualified Internal Advisory Committee, and student selection and progress-monitoring will be done by a Student Selection and Mentoring Committee. To maximize the experience, students will be encouraged to enroll in two consecutive summers when possible. Anticipated outcomes include: (i) graduate students from engineering, informatics, and computational sciences will pursue research related to the NIDDK-mission, and (ii) undergraduate students from underrepresented scientific disciplines will perform laboratory research in the areas of digestive and metabolic physiology. We expect this experience to encourage them not only to pursue a research career but to also to consider the exciting opportunities related to solving health problems involving digestive diseases and metabolic disorders.

Public Health Relevance

The goal of the proposed program is to establish a course to teach graduate and undergraduate students from engineering and computational backgrounds the exciting challenges and opportunities pertaining to digestive health and metabolism. The program also offers summer research opportunities to undergraduate engineering students. Our goals are that the offered course and summer research experience will stimulate graduate and undergraduate students to engage in research careers that address the health problems pertaining to digestive disease and metabolic disorders such as diabetes and obesity.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Education Projects (R25)
Project #
5R25DK088752-02
Application #
8099503
Study Section
Diabetes, Endocrinology and Metabolic Diseases B Subcommittee (DDK)
Program Officer
Podskalny, Judith M,
Project Start
2010-07-01
Project End
2015-05-31
Budget Start
2011-06-01
Budget End
2012-05-31
Support Year
2
Fiscal Year
2011
Total Cost
$108,000
Indirect Cost

  Institution

Name
University of Michigan Ann Arbor
Department
Physiology
Type
Schools of Medicine
DUNS #
073133571
City
Ann Arbor
State
MI
Country
United States
Zip Code
48109

  Publications

Allison, Margaret B; Pan, Warren; MacKenzie, Alexander et al. (2018) Defining the Transcriptional Targets of Leptin Reveals a Role for Atf3 in Leptin Action. Diabetes 67:1093-1104
Halling, Peter; Fitzpatrick, Paul F; Raushel, Frank M et al. (2018) An empirical analysis of enzyme function reporting for experimental reproducibility: Missing/incomplete information in published papers. Biophys Chem 242:22-27
Schnell, Santiago (2018) ""Reproducible"" Research in Mathematical Sciences Requires Changes in our Peer Review Culture and Modernization of our Current Publication Approach. Bull Math Biol 80:3095-3105
Swainston, Neil; Baici, Antonio; Bakker, Barbara M et al. (2018) STRENDA DB: enabling the validation and sharing of enzyme kinetics data. FEBS J 285:2193-2204
Wynn, Michelle L; Egbert, Megan; Consul, Nikita et al. (2018) Inferring Intracellular Signal Transduction Circuitry from Molecular Perturbation Experiments. Bull Math Biol 80:1310-1344
Midani, Firas S; Wynn, Michelle L; Schnell, Santiago (2017) The importance of accurately correcting for the natural abundance of stable isotopes. Anal Biochem 520:27-43
Tong, Xin; Zhang, Deqiang; Charney, Nicholas et al. (2017) DDB1-Mediated CRY1 Degradation Promotes FOXO1-Driven Gluconeogenesis in Liver. Diabetes 66:2571-2582
Zhang, Deqiang; Tong, Xin; VanDommelen, Kyle et al. (2017) Lipogenic transcription factor ChREBP mediates fructose-induced metabolic adaptations to prevent hepatotoxicity. J Clin Invest 127:2855-2867
Snider, Natasha T; Portney, Daniel A; Willcockson, Helen H et al. (2016) Ethanol and Acetaminophen Synergistically Induce Hepatic Aggregation and TCH346-Insensitive Nuclear Translocation of GAPDH. PLoS One 11:e0160982
Chhabra, Kavaljit H; Adams, Jessica M; Fagel, Brian et al. (2016) Hypothalamic POMC Deficiency Improves Glucose Tolerance Despite Insulin Resistance by Increasing Glycosuria. Diabetes 65:660-72

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