Abstract

Cancer, especially pediatric cancer, is a devastating diseases effecting a broad swath of humanity and consequently we must be able to understand the development of cancer in a holistic manner to develop the next generation of therapies. While there has been significant progress in elucidating genetic mutations which drive cancer initiation, many genetically engineered mouse models of cancer have indicated that necessary genetic mutations are oftentimes insufficient for tumor formation, i.e. not all cells harboring the necessary mutations form a tumor. Therefore, there must be other factors which license a cell with the capacity to form a tumor when the necessary mutations are present. We hypothesize that these cells are licensed as a consequence of the prior development of the cell. A cell's development is guided in large part by master regulators which are the key genes to define cell identity. As master regulators can induce cells to switch identity, a process known as reprogramming and which shares many characteristics to tumor initiation, we expect that misregulation of master regulators throughout development may be involved in the licensing of cells for cancer formation. We have shown that the master regulator, Sox2, is required for the formation of tumors that are initiated by the loss of the retinoblastoma tumor suppressor (Rb). Notably Sox2 is the master regulator to define the few cell types which form tumors when Rb is lost, most commonly neuroendocrine cells. We will therefore investigate the regulation of Sox2 during development in these neuroendocrine lineages and determine if misregulation of Sox2 is responsible for cancer licensing. We will pursue this investigation by pursuing the following aims: 1) To understand the mechanism of Sox2 regulation during development and how this goes awry in tumor formation, and 2) To determine if Sox2 derepressed cells are tumor initiating upon Rb-loss. We anticipate that the successful completion of these aims will lead to a greater understanding of how development might induce cancer later in life, and provide new avenues for cancer therapies and preventation.

Public Health Relevance

Understanding the potential contributions of development on the ability of some cells to initiate cancer can have broad impacts on future therapies. Indeed, we will investigate master regulator genes which throughout development can define cellular identity, yet also promote cancer when aberrantly activated. Our objective is to use these investigations to better derive new targeted therapies and open new avenues for cancer prevention.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Exploratory Grants (P20)
Project #
5P20GM103620-07
Application #
9767222
Study Section
Special Emphasis Panel (ZGM1)
Project Start
Project End
Budget Start
2019-09-01
Budget End
2020-08-31
Support Year
7
Fiscal Year
2019
Total Cost
Indirect Cost

  Institution

Name
Sanford Research/Usd
Department
Type
DUNS #
050113252
City
Sioux Falls
State
SD
Country
United States
Zip Code
57104

  Publications

Anderson, Ruthellen H; Lensing, Cody J; Forred, Benjamin J et al. (2018) Differentiating Antiproliferative and Chemopreventive Modes of Activity for Electron-Deficient Aryl Isothiocyanates against Human MCF-7 Cells. ChemMedChem 13:1695-1710
Johnson, Tyler B; Mechels, Keegan; Anderson, Ruth Ellen et al. (2018) Characterization of a recurrent missense mutation in the forkhead DNA-binding domain of FOXP1. Sci Rep 8:16161
Brudvig, J J; Cain, J T; Sears, R M et al. (2018) MARCKS regulates neuritogenesis and interacts with a CDC42 signaling network. Sci Rep 8:13278
Roux, Kyle J; Kim, Dae In; Burke, Brian et al. (2018) BioID: A Screen for Protein-Protein Interactions. Curr Protoc Protein Sci 91:19.23.1-19.23.15
Hussain, Sajjad; Bedekovics, Tibor; Liu, Qiuying et al. (2018) UCH-L1 bypasses mTOR to promote protein biosynthesis and is required for MYC-driven lymphomagenesis in mice. Blood 132:2564-2574
Brudvig, J J; Cain, J T; Schmidt-Grimminger, G G et al. (2018) MARCKS Is Necessary for Netrin-DCC Signaling and Corpus Callosum Formation. Mol Neurobiol 55:8388-8402
Anderson, Ruthellen H; Kerkvliet, Jason G; Otta, Jaelin J et al. (2018) Generation of a CLTA reporter human induced pluripotent stem cell line, CRMi001-A-1, using the CRISPR/Cas9 system to monitor endogenous clathrin trafficking. Stem Cell Res 33:95-99
Lucido, Christopher T; Callejas-Valera, Juan L; Colbert, Paul L et al. (2018) ?2-Adrenergic receptor modulates mitochondrial metabolism and disease progression in recurrent/metastatic HPV(+) HNSCC. Oncogenesis 7:81
McKenzie, Casey W; Preston, Claudia C; Finn, Rozzy et al. (2018) Strain-specific differences in brain gene expression in a hydrocephalic mouse model with motile cilia dysfunction. Sci Rep 8:13370
Miszuk, Jacob M; Xu, Tao; Yao, Qingqing et al. (2018) Functionalization of PCL-3D Electrospun Nanofibrous Scaffolds for Improved BMP2-Induced Bone Formation. Appl Mater Today 10:194-202

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