Ras proteins play a central role in many aspects of biology. These monomeric GTPases cycle between an inactivate GDP-bound state and an active GTP-bound state. Mutational activation of Ras occurs in approximately 30% of human tumors with some cancers such as pancreatic cancer having Ras mutations in >90% of tumors. These cancer associated mutations trap Ras in the GTP-bound state, leading to chronic activation of Ras-regulated signaling pathways and oncogenic transformation. Thus, RasGTP has been considered the only biologically important form of the molecule. However, we have discovered a novel role for nucleotide-free Ras (nfRas) in the negative regulation of cell signaling. This form of Ras, formed as an intermediate in the transition from RasGDP to RasGTP, negatively regulates phosphatidylinositol 3-kinase, class 2beta (PI3KC2?). These finding have profound implications for the understanding of Ras-mediated signaling and transformation. We propose that nfRas binds targets, e.g., PI3KC2?, leading to the mutual inhibition of both Ras and the associated target. Our model predicts that oncogenic activation of Ras leads to loss of repression of these targets resulting in their activation without binding RasGTP. Thus, our findings point to a new class of molecules important for Ras-driven tumorigenesis yet do not bind activated Ras. To better understand the role of nfRas in cell signaling, we have generated high affinity, high specificity monobody reagents that selectively bind different states of Ras. Using these reagents we demonstrate that nfRas represents a significant pool of total cellular Ras. In addition, one of our Ras monobodies which binds to all three forms of Ras (GTP, GDP, and nucleotide free) acts as a highly potent inhibitor of oncogenic Ras- mediated signaling. Using these reagents we will characterize the regulation of nfRas in vivo and determine the role of nfRas in regulating specific targets. Finally, we will utilize these novel monobody reagents to perturb Ras function in vivo using a novel chemical-genetic approach to interfere with pancreatic cancer development and progression. Given the prevalence of Ras mutations in human cancers, it is critical to understand the mechanisms through which Ras contributes to tumorigenesis. Our work represents an entirely new concept in Ras biology that defines a new class of targets that participate in Ras-mediated signaling and transformation. These studies will provide new insights into the mechanisms of Ras-mediated tumorigenesis and are therefore of high translational significance. This work will be beneficial to Veterans as well as the general population, both of which suffer from cancer. However, the incidence for certain cancers, such as lung and pancreatic cancer the latter of which has a high incidence of Ras mutations (<90%), has been reported to be up to 5-7x higher in Veteran populations making these studies particularly relevant to Veterans. Additionally, the goals of our proposal are consistent with the recently established National Cancer Moonshots Program to accelerate research efforts to improve cancer treatment. Finally, given the ubiquity of Ras family members in eukaryotes and their roles in many aspects of biology these results will be of broad scientific interest and importance to many areas of biomedical research.

Public Health Relevance

The application will fill a critical knowledge gap in our understanding of Ras family GTPases which play a central role in many aspects of biology including growth, differentiation, and development. The medical importance of Ras is highlighted by its frequent mutational activation in human cancers. We have discovered an entirely new paradigm in Ras signaling in which nucleotide-free Ras (nfRas) inhibits cellular signaling pathways. We have isolated unique reagents to probe the function of nfRas in cells and animal models for cancer. Our work will define a new paradigm in Ras signaling that has important implications for our understanding of Ras-driven cancers. Given the evolutionary conservation of Ras and its involvement in human biology, these studies are of broad interest to many investigators. In addition, this work will have translational significance and relevance to Veterans which are at an increased risk for many Ras mutant cancers.

Agency
National Institute of Health (NIH)
Institute
Veterans Affairs (VA)
Type
Non-HHS Research Projects (I01)
Project #
2I01BX002095-04
Application #
9240249
Study Section
Oncology C (ONCC)
Project Start
2013-10-01
Project End
2020-12-31
Budget Start
2017-01-01
Budget End
2017-12-31
Support Year
4
Fiscal Year
2017
Total Cost
Indirect Cost
Name
Jesse Brown VA Medical Center
Department
Type
Independent Hospitals
DUNS #
010299204
City
Chicago
State
IL
Country
United States
Zip Code
60612
Sudhahar, Varadarajan; Okur, Mustafa Nazir; Bagi, Zsolt et al. (2018) Akt2 (Protein Kinase B Beta) Stabilizes ATP7A, a Copper Transporter for Extracellular Superoxide Dismutase, in Vascular Smooth Muscle: Novel Mechanism to Limit Endothelial Dysfunction in Type 2 Diabetes Mellitus. Arterioscler Thromb Vasc Biol 38:529-541
O'Bryan, John P (2018) Pharmacological targeting of RAS: Recent success with direct inhibitors. Pharmacol Res :
Spencer-Smith, Russell; O'Bryan, John P (2017) Direct inhibition of RAS: Quest for the Holy Grail? Semin Cancer Biol :
Spencer-Smith, Russell; Li, Lie; Prasad, Sheela et al. (2017) Targeting the ?4-?5 interface of RAS results in multiple levels of inhibition. Small GTPases :1-10
Harris, Jamie; Herrero-Garcia, Erika; Russo, Angela et al. (2017) Silencing Intersectin 1 Slows Orthotopic Neuroblastoma Growth in Mice. J Pediatr Hematol Oncol 39:e413-e418
Spencer-Smith, Russell; Koide, Akiko; Zhou, Yong et al. (2017) Inhibition of RAS function through targeting an allosteric regulatory site. Nat Chem Biol 13:62-68
Burmeister, Brian T; Wang, Li; Gold, Matthew G et al. (2015) Protein Kinase A (PKA) Phosphorylation of Shp2 Protein Inhibits Its Phosphatase Activity and Modulates Ligand Specificity. J Biol Chem 290:12058-67
Wang, Li; Burmeister, Brian T; Johnson, Keven R et al. (2015) UCR1C is a novel activator of phosphodiesterase 4 (PDE4) long isoforms and attenuates cardiomyocyte hypertrophy. Cell Signal 27:908-22
Russo, Angela; Okur, Mustafa Nazir; Bosland, Maarten et al. (2015) Phosphatidylinositol 3-kinase, class 2 beta (PI3KC2?) isoform contributes to neuroblastoma tumorigenesis. Cancer Lett 359:262-8