Abstract

The Molecular Basis of Infectious Disease (MBID) research training program is centered on 22 faculty mentors from three Houston educational institutions: the University. of Texas Health Science Center at Houston, Baylor College of Medicine, and the Texas A&M University Institute for Biosciences and Technology. The overall purpose of the MBID training program is to provide trainees 1) an optimal environment for training new scientists in the latest concepts and techniques in microbiological research; 2) a better understanding of current challenges in clinical infectious diseases; and 3) the knowledge and tools to `bridge the gap' between basic research and clinical applications. The basis of this training grant is the Molecular Basis of Infectious Disease group, which was first formed in 1996. MBID has developed into highly interactive group of over 400 faculty, postdoctoral fellows, graduate students, and staff from the Houston area whose primary interest is in the molecular pathogenesis of bacterial infections. The 22 faculty members that form the core of this training grant have a record of high research productivity, extensive collaborations, and graduate student and postdoctoral fellow training. They have mentored 76 predoctoral trainees during the past ten years, and currently are mentoring 21 Ph.D. students. The training program includes a newly revised core curriculum, intensive and interactive research experiences, monthly MBID meetings, annual retreats, weekly seminars and journal clubs, and specialized training in translational research and clinical infectious diseases. The MBID program has a strong track record in terms of the recruitment, training, and career advancement of underrepresented groups. For the next grant period, enhancement of the successful MBID predoctoral program with an improved curriculum and the initiation of a new Research Scholar Program for the recruitment of outstanding underrepresented group trainees are proposed.

Public Health Relevance

The major goal of this ongoing, successful training grant is to provide microbiology trainees additional knowledge in clinical infectious diseases and translational research, thereby directing research toward the more rapid resolution of important infectious disease problems. In addition, the program will continue to recruit highly qualified trainees from underrepresented groups, increasing the diversity of scientists performing research at the cutting edge of the microbiology/infectious disease interface.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Institutional National Research Service Award (T32)
Project #
2T32AI055449-11A1
Application #
9150977
Study Section
Microbiology and Infectious Diseases B Subcommittee (MID)
Program Officer
Robbins, Christiane M
Project Start
2005-09-15
Project End
2021-05-31
Budget Start
2016-06-22
Budget End
2017-05-31
Support Year
11
Fiscal Year
2016
Total Cost
Indirect Cost

  Institution

Name
University of Texas Health Science Center Houston
Department
Pathology
Type
Schools of Medicine
DUNS #
800771594
City
Houston
State
TX
Country
United States
Zip Code
77225

  Publications

Oyaro, Micah O; Plants-Paris, Kimberly; Bishoff, Dayna et al. (2018) High rate of Clostridium difficile among young adults presenting with diarrhea at two hospitals in Kenya. Int J Infect Dis 74:24-28
Okyere, Ama; Bishoff, Dayna; Oyaro, Micah O et al. (2018) Analysis of Fish Commonly Sold in Local Supermarkets Reveals the Presence of Pathogenic and Multidrug-Resistant Bacterial Communities. Microbiol Insights 11:1178636118786925
Hunter, Robert L; Actor, Jefrey K; Hwang, Shen-An et al. (2018) Pathogenesis and Animal Models of Post-Primary (Bronchogenic) Tuberculosis, A Review. Pathogens 7:
Darkoh, Charles; Deaton, Magdalena; DuPont, Herbert L (2017) Nonantimicrobial drug targets for Clostridium difficile infections. Future Microbiol 12:975-985
Darkoh, Charles; DuPont, Herbert L (2017) The accessory gene regulator-1 as a therapeutic target for C. difficile infections. Expert Opin Ther Targets 21:451-453
Vesely, Elisa M; Williams, Robert B; Konopka, James B et al. (2017) N-Acetylglucosamine Metabolism Promotes Survival of Candida albicans in the Phagosome. mSphere 2:
Whitaker, Neal; Berry, Trista M; Rosenthal, Nathan et al. (2016) Chimeric Coupling Proteins Mediate Transfer of Heterologous Type IV Effectors through the Escherichia coli pKM101-Encoded Conjugation Machine. J Bacteriol 198:2701-18
Danhof, Heather A; Vylkova, Slavena; Vesely, Elisa M et al. (2016) Robust Extracellular pH Modulation by Candida albicans during Growth in Carboxylic Acids. MBio 7:
Stojanoski, Vlatko; Adamski, Carolyn J; Hu, Liya et al. (2016) Removal of the Side Chain at the Active-Site Serine by a Glycine Substitution Increases the Stability of a Wide Range of Serine ?-Lactamases by Relieving Steric Strain. Biochemistry 55:2479-90
Stojanoski, Vlatko; Sankaran, Banumathi; Prasad, B V Venkataram et al. (2016) Structure of the catalytic domain of the colistin resistance enzyme MCR-1. BMC Biol 14:81

Showing the most recent 10 out of 42 publications