Abstract

The objectives of the proposed Center for Studies of Host Response to Cancer Therapy are two-fold: (1) to help a group of promising new or early-stage investigators with a common research focus on host response to cancer therapy establish themselves as productive, independent scientists; and (2) to form a self-sustaining center within our institution dedicated to research on host response to cancer therapy. The ultimate goal of this effort is to create a vibrant, synergistic research environment to comprehensively address the mechanisms of short- and long-term side effects after cancer therapy and to develop effective strategies to prevent, mitigate, or treat such side effects. Within this COBRE, the Administrative and Scientific Development Core (Core A) will provide the necessary infrastructure to accomplish these objectives. Specifically, Core A will provide fiscal and organizational support for the Center by providing an efficient, integrated administrative infrastructure for the COBRE Center (Aim 1); accelerating scientific growth through faculty development and mentoring (Aim 2); and expanding and advancing the Center toward self-sustainability (Aim 3). Core A relies on a team of experienced mentors, Internal and External Advisory Committees, and a seasoned administrative team under the leadership of the Center Director to guide four Project Leaders with a focus on the Center?s common theme toward independent research careers. The Core?s leadership team will develop a ?pipeline? of new Project Leaders to replace those who successfully compete for R01-level research support and, thus, graduate from COBRE support. Moreover, Core A also will assume responsibility for training new mentors; initiate a Distinguished Lecturer Series to attract new scientists to the field; provide pilot funds for collaborative research to address the central scientific theme; oversee the other Center cores; and perform periodic evaluation of the Center and its projects and cores. Successful operation of Core A will enable the Center to achieve the following milestones within the initial 5 years of funding: two or more Project Leaders successfully competing for R01-level funding; two to four new or early-stage investigators added to the Center; two to four new mentors added (including Project Leaders recently graduated from COBRE support); and at least 25 manuscripts accepted for publication or published in reputable peer-reviewed journals.

Public Health Relevance

Many cancer survivors cured of their original malignancy subsequently suffer from treatment-related problems, ranging from mild psychosocial disabilities to life-threatening physical sequelae. Comparatively little effort has been directed toward determining the mechanisms that are responsible for side effects after cancer therapy and at developing effective interventions to prevent them. By addressing this unmet need, this COBRE will ultimately help ensure that advances in oncology go hand in hand with efforts to optimize the quality of life of cancer survivors and thereby maximize the number of uncomplicated cancer cures.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Exploratory Grants (P20)
Project #
1P20GM109005-01A1
Application #
8880634
Study Section
Special Emphasis Panel (ZGM1-TWD-A (1C))
Project Start
Project End
Budget Start
2015-06-24
Budget End
2016-03-31
Support Year
1
Fiscal Year
2015
Total Cost
$520,621
Indirect Cost
$171,211

  Institution

Name
University of Arkansas for Medical Sciences
Department
Type
DUNS #
122452563
City
Little Rock
State
AR
Country
United States
Zip Code
72205

  Publications

Cheema, Amrita K; Byrum, Stephanie D; Sharma, Neel Kamal et al. (2018) Proteomic Changes in Mouse Spleen after Radiation-Induced Injury and its Modulation by Gamma-Tocotrienol. Radiat Res 190:449-463
Skinner, Charles M; Miousse, Isabelle R; Ewing, Laura E et al. (2018) Impact of obesity on the toxicity of a multi-ingredient dietary supplement, OxyELITE Pro™ (New Formula), using the novel NZO/HILtJ obese mouse model: Physiological and mechanistic assessments. Food Chem Toxicol 122:21-32
Alam, Sinthia; Carter, Gwendolyn S; Krager, Kimberly J et al. (2018) PCB11 Metabolite, 3,3'-Dichlorobiphenyl-4-ol, Exposure Alters the Expression of Genes Governing Fatty Acid Metabolism in the Absence of Functional Sirtuin 3: Examining the Contribution of MnSOD. Antioxidants (Basel) 7:
Barham, Caroline; Fil, Daniel; Byrum, Stephanie D et al. (2018) RNA-Seq Analysis of Spinal Cord Tissues from hPFN1G118V Transgenic Mouse Model of ALS at Pre-symptomatic and End-Stages of Disease. Sci Rep 8:13737
Janganati, Venumadhav; Ponder, Jessica; Balasubramaniam, Meenakshisundaram et al. (2018) MMB triazole analogs are potent NF-?B inhibitors and anti-cancer agents against both hematological and solid tumor cells. Eur J Med Chem 157:562-581
Banerjee, Sudip; Shah, Sumit K; Melnyk, Stepan B et al. (2018) Cebpd Is Essential for Gamma-Tocotrienol Mediated Protection against Radiation-Induced Hematopoietic and Intestinal Injury. Antioxidants (Basel) 7:
Wang, Lei; Fang, Bin; Fujiwara, Toshifumi et al. (2018) Deletion of ferroportin in murine myeloid cells increases iron accumulation and stimulates osteoclastogenesis in vitro and in vivo. J Biol Chem 293:9248-9264
Harrill, Alison H; Lin, Haixia; Tobacyk, Julia et al. (2018) Mouse population-based evaluation of urinary protein and miRNA biomarker performance associated with cisplatin renal injury. Exp Biol Med (Maywood) 243:237-247
Zhang, Xin; Zhang, Suping; Liu, Xingui et al. (2018) Oxidation resistance 1 is a novel senolytic target. Aging Cell :e12780
Alexander, Tyler C; Butcher, Hannah; Krager, Kimberly et al. (2018) Behavioral Effects of Focal Irradiation in a Juvenile Murine Model. Radiat Res 189:605-617

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