David Ian Yule, Ph.D.
See information for Patients. Viewing information for Researchers.
Contact
University of Rochester
School of Medicine and Dentistry
601 Elmwood Ave, Box 711
Rochester, New York 14642
Office: 585 273-2154 (primary)
Lab: 585 275-6128
Fax: 585 273-2652
In exocrine acinar cells regulation of intracellular calcium plays a pivotal role in controlling fluid and protein secretion. Exposure of cells to neurotransmitters and hormones results in a rapid elevation of intracellular calcium. This increase in [Ca2+]i carries complex spatial and temporal information important to the physiology of the acinar cell. Research in this laboratory focuses on gaining a better understanding of the mechanisms which underlie these signaling patterns with a primary goal of relating this knowledge to the physiology and pathophysiology of exocrine cells.
Although all Ca2+ mobilizing agonists in pancreatic acinar cells utilize the phosphoinositide-signaling (PI) pathway, stimulation by individual agents results in markedly different temporal and spatial patterns of Ca2+ signaling. One project is designed to understand at the molecular level how the cell effectively "knows" which PI-coupled agonist it is currently exposed to. Given that tremendous molecular diversity is expressed at all levels of this signaling pathway, our working hypothesis is that individual agonists do not couple to the signaling machinery in an identical fashion. This study involves precisely defining by molecular techniques the individual signaling proteins expressed in the acinar cell and then subsequently assessing if individual agonists utilize discrete and different elements of the PI-signaling pathway. We are utilizing fluorescence imaging techniques including high-speed confocal microscopy to monitor [Ca2+]i while manipulating the signaling pathway with neutralizing antibodies and antisense technology.
A further project relates to the organization and regulation of calcium release sites in exocrine cells. These organelles are defined by the expression of receptors for the second messenger Inositol 1,4,5-trisphosphate. In acinar cells the distribution of these receptors is tightly localized to an area associated with the actin cytoskeleton in the apical secretory pole of the cell. This distribution of receptors is the major factor in defining the spatial characteristics of the Ca2+ signal. The nature of the association with the cytoskeleton is being investigated. In addition the regulation of these receptors by phosphorylation and the consequences this may have for Ca2+ signaling are also being studied.
Current Appointments
- Professor - Department of Pharmacology and Physiology (SMD)
- Professor - Department of Medicine (SMD)
- Professor - Center for Oral Biology (SMD)
| Education | ||
|---|---|---|
| PhD Physiology | UK-Univ of Liverpool | 1989 |
| BS Pharmacology | UK-Portsmouth Polytechnic | 1985 |
| Post-Doctoral Training & Residency | |
|---|---|
| Department of Physiology, University of Michigan. Supervisor: Prof. J.A. Williams. | 1990 - 1992 |
| M.R.C. Secretory Control Group, Physiology Department, University of Liverpool. Supervisor: Prof. O.H. Petersen. | 1990 |
| Recent Journal Articles |
|---|
| Showing the 5 most recent journal articles. (81 available) |
| Betzenhauser, M.J.; Wagner II, L.E.; Park; H-S; Yule, D.I. "ATP Regulation of Type-1 Inositol 1,4,5-Trisphosphate Receptor Activity Does Not Require Walker A-type ATP-binding Motifs*". The Journal of Biological Chemistry 284 (2009): 16156-16163. |
| Schug ZT; da Fonseca PC; Bhanumathy CD; Wagner L; Zhang X; Bailey B; Morris EP; Yule DI; Joseph SK. "Molecular characterization of the inositol 1,4,5-trisphosphate receptor pore-forming segment." The Journal of biological chemistry. 2008; 283(5):2939-48. Epub 2007 Nov 19. |
| Betzenhauser MJ; Wagner LE; Iwai M; Michikawa T; Mikoshiba K; Yule DI. "ATP modulation of Ca2+ release by type-2 and type-3 inositol (1, 4, 5)-triphosphate receptors. Differing ATP sensitivities and molecular determinants of action." The Journal of biological chemistry. 2008; 283(31):21579-87. Epub 2008 May 27. |
| Wagner LE; Joseph SK; Yule DI. "Regulation of single inositol 1,4,5-trisphosphate receptor channel activity by protein kinase A phosphorylation." The Journal of physiology. 2008; 586(Pt 15):3577-96. Epub 2008 Jun 05. |
| Park HS; Betzenhauser MJ; Won JH; Chen J; Yule DI. "The type 2 inositol (1,4,5)-trisphosphate (InsP3) receptor determines the sensitivity of InsP3-induced Ca2+ release to ATP in pancreatic acinar cells." The Journal of biological chemistry. 2008; 283(38):26081-8. Epub 2008 Jul 24. |
