Abstract

Clark Atlanta University proposes to maintain the enhancements to the biomedical research infrastructure that it has established over thirteen years of RCMI funding. These enhancements include the establishment of a biomedical-oriented research center (Center for Cancer Research and Therapeutic Development) that focuses on understanding the cellular and molecular bases on the types of cancers that disproportionately affect African-American and other minority populations, the design of more effective drug therapies and drug delivery systems and the support of research-support facilities needed by Center drug therapies and drug delivery systems and the support of research-support facilities needed by Center scientists for performance of state-of-the-art experimentation. These facilities are the Molecular Biology Research Laboratory, the Cell Culture Research Laboratory, the Electron Microscopy Research Laboratory and the Nuclear Magnetic Resonance Center. Continued support of Center activities and research-support facilities for another funding cycle will help in the achievement of the following goals: (1) a minimum two-fold increase in the overall publication rate of center scientists; (2) the involvement (as presenters and/or organizers) of all center-affiliated scientists in a national or international conference on the molecular and cellular bases of cancer on cancer therapeutics and (3) the planning and implementation of an annual conference on cancer in minority populations by Clark Atlanta University. These goals will be accomplished by: (1) including only the most committed and productive scientists in this research area as members of the Center; (2) supporting their research endeavors through subproject grants that include funds for release time, technical support, supplied and travel; (3) providing a weekly forum via a journal club where all scientists can share ideas, receive constructive feedback on these ideas, and discuss possible collaborative efforts with their peers; (4) continuing to fund visits by research collaborators for each Center scientist; (5) continuing to fund speakers for the weekly Biomedical Research Seminar Series; and (6) further supporting the research endeavors of Center scientists by efficient administrative services that include management of requests such as purchasing, repair or service of equipment, arrangement of travel. Thus, continued support of the current Clark Atlanta University RCMI program will serve to assist the University in achieving one of its state goals, that of being a major player in a research area that affects it service population, African Americans.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Center for Research Resources (NCRR)
Type
Research Centers in Minority Institutions Award (G12)
Project #
3G12RR003062-16S1
Application #
6660595
Study Section
National Center for Research Resources Initial Review Group (RIRG)
Program Officer
Arora, Krishan
Project Start
1985-09-30
Project End
2003-07-31
Budget Start
2002-09-19
Budget End
2003-07-31
Support Year
16
Fiscal Year
2002
Total Cost
$533,646
Indirect Cost

  Institution

Name
Clark Atlanta University
Department
Biology
Type
Schools of Arts and Sciences
DUNS #
065325177
City
Atlanta
State
GA
Country
United States
Zip Code
30314

  Publications

Morton, Derrick J; Patel, Divya; Joshi, Jugal et al. (2017) ID4 regulates transcriptional activity of wild type and mutant p53 via K373 acetylation. Oncotarget 8:2536-2549
Joshi, Jugal Bharat; Patel, Divya; Morton, Derrick J et al. (2017) Inactivation of ID4 promotes a CRPC phenotype with constitutive AR activation through FKBP52. Mol Oncol 11:337-357
Wilder, Catera L; Walton, Charlene; Watson, Valencia et al. (2016) Differential cathepsin responses to inhibitor-induced feedback: E-64 and cystatin C elevate active cathepsin S and suppress active cathepsin L in breast cancer cells. Int J Biochem Cell Biol 79:199-208
Komaragiri, Shravan Kumar; Bostanthirige, Dhanushka H; Morton, Derrick J et al. (2016) ID4 promotes AR expression and blocks tumorigenicity of PC3 prostate cancer cells. Biochem Biophys Res Commun 478:60-66
Brown, Shanora G; Knowell, Ashley E; Hunt, Aisha et al. (2015) Interferon inducible antiviral MxA is inversely associated with prostate cancer and regulates cell cycle, invasion and Docetaxel induced apoptosis. Prostate 75:266-79
Muniyan, Sakthivel; Chou, Yu-Wei; Tsai, Te-Jung et al. (2015) p66Shc longevity protein regulates the proliferation of human ovarian cancer cells. Mol Carcinog 54:618-31
Chinaranagari, Swathi; Sharma, Pankaj; Bowen, Nathan J et al. (2015) Prostate cancer epigenome. Methods Mol Biol 1238:125-40
Burton, Liza J; Smith, Basil A; Smith, Bethany N et al. (2015) Muscadine grape skin extract can antagonize Snail-cathepsin L-mediated invasion, migration and osteoclastogenesis in prostate and breast cancer cells. Carcinogenesis 36:1019-27
Goodson 3rd, William H; Lowe, Leroy; Carpenter, David O et al. (2015) Assessing the carcinogenic potential of low-dose exposures to chemical mixtures in the environment: the challenge ahead. Carcinogenesis 36 Suppl 1:S254-96
Mandal, S; Abebe, F; Chaudhary, J (2014) -174G/C polymorphism in the interleukin-6 promoter is differently associated with prostate cancer incidence depending on race. Genet Mol Res 13:139-51

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