Keith Yamamoto, Ph.D.
We study the activity of the intracellular receptors (IRs) in signal transduction and transcriptional control, including receptors for glucocorticoids (GR), androgens (AR) and thyroid hormone (TR).These hormone-receptor complexes bind to specific DNA sequences termed hormone response elements, which enhance or repress linked promoters.
We have defined IR domains for hormone and DNA binding, dimerization, nuclear localization, phosphorylation, interac-tion with various cellular factors and transcriptional regulation. IRs functions faithfully when expressed in simpler organisms such as yeast and Drosophila, thus facilitating genetic analyses of their actions and identification of other factors involved in its activities. We are also pursuing 3D structure analyses of various domains of the receptor, and we employ biochemical strategies with purified components for mechanistic analyses. Thus, using genetic, structural, molecular and biochemical approaches, we use IRs as 3biological probes2 to define how a single regulatory protein can specify diverse pat-terns of specific gene expression in different cellular contexts.
These reductionist strategies can increasingly be applied to studies of complex physiological and pathological processes. Thus, we are pursuing: (a) a signaling 3crosstalk2 pathway in developing T-cells in which activation of the T-cell receptor abrogates glucocorticoid-induced apoptosis; (b) dramatic shifts in AR activity and ligand responses during prostate cancer ontogeny and progression; (c) the consequences of glutamine repeat expansion in AR, leading to motor neuron degeneration in spinal and bulbar muscular atrophy.