Raymond R. Mattingly, Ph.D.
Education
- B.A. (Hons.), Natural Sciences/Pharmacology, University of Cambridge, Cambridge, U.K., 1987
- Ph.D., Pharmacology, University of Virginia, Charlottesville, VA, 1993
Research Interests
Our studies focus on the physiological roles and pharmacological significance of small GTPases of the Ras superfamily. In particular, we are interested in how to target disorders where the Ras pathway is activated without direct oncogenic mutation of the Ras protein itself. While such activating changes in Ras are the most common oncogenic mutations in human cancer, the majority of cancers and many other hyperproliferative disorders have increased Ras signal transduction that is driven through other mechanisms. In recent years, our efforts have concentrated in the areas of Type 1 Neurofibromatosis (NF1) and breast cancer, with the development of novel 3D in vitro models. We believe that this approach will provide more relevant results than are obtained from testing new drugs in conventional cell culture in 2D on plastic dishes, while being significantly more rapid and with higher throughput than testing in animals.
NF1 is the most frequent genetic cause of both tumors and neurological problems, with a birth incidence of about 1 in 3,000. Nearly all patients have benign neurofibromas, and there is increased risk of malignant peripheral nerve sheath tumors and other cancers. We have developed collaborative projects with the goal of the identification of non-toxic and mechanistically specific drugs for NF1 treatment. Our hypothesis is that increased activation of Ras signaling underlies the pathological development of NF1 and provides therapeutic targets.
Our work in breast cancer research is focused on the identification of new therapeutic approaches to address two main problems: 1. discovery of the factors that cause the progress from ductal carcinoma in situ (DCIS) to find how to block malignant progression; and 2. identification of a viable targeted approach to triple-negative disease/basal-type breast cancer. We expect that the models and approaches that we are developing will address both of those challenges, and also be useful to other investigators who are tackling other important issues in breast cancer.
Recent Publications
Kraniak JM, Chalasani A, Wallace MR, Mattingly RR. Development of 3D culture models of plexiform neurofibroma and initial application for phenotypic characterization and drug screening. Exp Neurol. 2018 Jan;299(Pt B):289-298. PMID: 29055717; PMCID: PMC6863155 .
Shah S, Brock EJ, Ji K, Mattingly RR. Ras and Rap1: A tale of two GTPases. Semin Cancer Biol. 2019 Feb;54:29-39. PMID: 29621614; PMCID: PMC6170734.
Shah S, Brock EJ, Jackson RM, Ji K, Boerner JL, Sloane BF, Mattingly RR. Downregulation of Rap1Gap: A Switch from DCIS to Invasive Breast Carcinoma via ERK/MAPK Activation. Neoplasia 2018. Sep;20(9):951-963. PMID: 30144784; PMCID: PMC6106701 .
Brock EJ, Ji K, Shah S, Mattingly RR, Sloane BF. In Vitro Models for Studying Invasive Transitions of Ductal Carcinoma In Situ. J Mammary Gland Biol Neoplasia. 2019 Mar;24(1):1-15. PMID: 30056557; PMCID: PMC6641861.
Ji K, Sameni M, Osuala K, Moin K, Mattingly RR, Sloane BF. Spatio-temporal modeling and live-cell imaging of proteolysis in the 4D microenvironment of breast cancer. Cancer Metastasis Rev. 2019 Sep;38(3):445-454. PMID: 31605250 ; PMCID: PMC6893099.
Brock EJ, Jackson RM, Boerner JL, Li Q, Tennis MA, Sloane BF, Mattingly RR. Sprouty4 negatively regulates ERK/MAPK signaling and the transition from in situ to invasive breast ductal carcinoma. PLoS One. 2021 May 28;16(5):e0252314. PMID: 34048471; PMCID: PMC8162601 .
Ji K, Zhao Z, Sameni M, Moin K, Xu Y, Gillies RJ, Sloane BF, Mattingly RR. Modeling Tumor: Lymphatic Interactions in Lymphatic Metastasis of Triple Negative Breast Cancer. Cancers (Basel). 2021 Nov 30;13(23):6044. PMID: 34885152; PMCID: PMC8656640.