Abstract

The TSU-MARC program began in 1980 and had a change of program director beginning with the most recent cycle of the program (2012-2013 academic year). 7 MARC alumni have received Ph.D.s from 2012-2015. All Ph.D.s received by TSU alumni in biomedical sciences during this period were from MARC alumni, emphasizing the importance of the TSU MARC program in attainment of Ph.D.s by URM at TSU. Historically, the TSU MARC program has produced a significant number of minority biomedical researchers. 7 of the 15 MARC graduates from the most recent cycle (2013-2015) have enrolled in Ph.D. pograms (40%). This is above the the rate of Ph.D. program enrollment, 34%, from the previous 12 years of the grant, but it is still below the desired level of Ph.D. program enrollment. Funding for 10 MARC trainees to particpate in the program is requested. The following specifc goals of the current application address the need of the TSU MARC program to increase enrollment in Ph.D. programs by MARC graduates and their persistence to completion of the Ph.D. once enrolled. A number of new strategies and activities have been proposed to achieve the folowing goals: 1. Increase the number of URM students who apply to Ph.D. graduate programs in the biomedical sciences. In the current cycle 60% of MARC graduates have applied to Ph.D. programs. The objective is to have 80% of our graduates applying to Ph.D. programs upon graduation, a 33% increase. 2. Increase the acceptance rate of students applying to Ph.D. programs. The specific objective is to increase the success rate of our students applying to Ph.D. programs from the current 55% to 80%.3. Increase the persistence of TSU MARC graduates entering Ph.D. programs to successful completion of their degrees. In the last 15 years of the TSU MARC program, 27 MARC graduates have entered Ph.D. programs but only 21 have persisted in their programs. The objective is to drop this attrition level of 22% to 15% during the next cycle of the grant, a 32% improvement. 4. Increase critical thinking skills of TSU-MARC graduates to prepare them for the level of analytical rigor needed for graduate program admission and completion. The measurable objective is have an increase in verbal and quatitative GRE scores from the current average of 151 to 153, which would put the verbal score at the 59th percentile and the quantitative at the 52nd percentile. This would be an 18% increase in the verbal percentile and a 16% increase in the quantitative percentile. 5. Improve TSU MARC student presentation effectiveness and publication record. Specifically to increase the number of trainee scientific presentations at discipline-related professional meetings from 4 per year to 6 per year and publications from 10 per five year period to 12 per five year period.

Public Health Relevance

The proposed MARC U-STAR grant would increase the pool of under-represented minority (URM) research scientists, this will be achieved by offering enhanced curricula and rigorous undergraduate research experiences to maximize the competitiveness of students in entering and completing Ph.D. programs in biomedical research. The diversity of the students that emerge from the program will provide a more nuanced and sensitive approach to the host of public health challenges that occur among the increasingly diverse population.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
MARC Undergraduate NRSA Institutional Grants (T34)
Project #
5T34GM007663-37
Application #
9485330
Study Section
NIGMS Initial Review Group (TWD)
Program Officer
Koduri, Sailaja
Project Start
1980-06-01
Project End
2022-05-31
Budget Start
2018-06-01
Budget End
2019-05-31
Support Year
37
Fiscal Year
2018
Total Cost
Indirect Cost

  Institution

Name
Tennessee State University
Department
Chemistry
Type
Schools of Arts and Sciences
DUNS #
108814179
City
Nashville
State
TN
Country
United States
Zip Code
37209

  Publications

Vercruysse, Koen; Clark, Astiney; Alatas, Noor et al. (2018) Polysaccharide-mediated synthesis of melanins from serotonin and other 5-hydroxy indoles. Future Sci OA 4:FSO280
Brown, Shyretha; Boules, Mariam; Hamza, Nafisa et al. (2018) Synthesis of interleukin 1 beta and interleukin 6 in human lymphocytes is stimulated by tributyltin. Arch Toxicol 92:2573-2586
Brown, Shyretha; Wilburn, Wendy; Martin, Tyesha et al. (2018) Butyltin compounds alter secretion of interleukin 6 from human immune cells. J Appl Toxicol 38:201-218
Maxcey, Ashleigh M; Glenn, Hannah; Stansberry, Elisabeth (2018) Recognition-induced forgetting does not occur for temporally grouped objects unless they are semantically related. Psychon Bull Rev 25:1087-1103
Al-Masum, Mohammad; Quinones, Linda; Cain, Laurance T (2016) Microwave Application and Anhydrous Cu(OAc)2 Mediated O-Arylation of Aliphatic Amino Alcohols. Int J Org Chem (Irvine) 6:100-106
Turo, Michael J; Shen, Xiao; Brandon, Nazharie K et al. (2016) Dual-mode crystal-bound and X-type passivation of quantum dots. Chem Commun (Camb) 52:12214-12217
Amara, Suneetha; Lopez, Karina; Banan, Babak et al. (2015) Synergistic effect of pro-inflammatory TNF? and IL-17 in periostin mediated collagen deposition: potential role in liver fibrosis. Mol Immunol 64:26-35
Brown, Shyretha; Whalen, Margaret (2015) Tributyltin alters secretion of interleukin 1 beta from human immune cells. J Appl Toxicol 35:895-908
Lawrence, Shanieek; Reid, Jacqueline; Whalen, Margaret (2015) Secretion of interferon gamma from human immune cells is altered by exposure to tributyltin and dibutyltin. Environ Toxicol 30:559-71
Cato, Anita; Celada, Lindsay; Kibakaya, Esther Caroline et al. (2014) Brominated flame retardants, tetrabromobisphenol A and hexabromocyclododecane, activate mitogen-activated protein kinases (MAPKs) in human natural killer cells. Cell Biol Toxicol 30:345-60

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