Ann F. McCue
Salk Institute for Biological Studies
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Neuropharmacology | 1993
Paul Brust; Susan Simerson; Ann F. McCue; Charles R. Deal; Susan Schoonmaker; Mark E. Williams; Gonul Velicelebi; Edwin C. Johnson; Michael Miller Harpold
Voltage-dependent calcium (Ca2+) channels, expressed in the CNS, appear to be multimeric complexes comprised of at least alpha 1, alpha 2 and beta subunits. Previously, we cloned and expressed human neuronal alpha 1, alpha 2 and beta subunits to study recombinant channel complexes that display properties of those expressed in vivo. The alpha 1B-mediated channel subtype binds omega-conotoxin (CgTx) GVIA with high affinity and exhibits properties of N-type voltage-dependent Ca2+ channels. Here we describe several alpha 2 and beta splice variants and report results on the expression of omega-CgTx GVIA binding sites, assembly of the subunit complex and biophysical function of alpha 1B-mediated channel complexes containing some of these splice variants. We optimized recombinant expression in human embryonic kidney (HEK) 293 cells of alpha 1B alpha 2b beta 1 subunit complexes by controlling the expression levels of subunit mRNAs and monitored cell surface expression by binding of omega-CgTx GVIA to the alpha 1B subunit. Co-expression of either alpha 2b or beta 1 subunits with an alpha 1B subunit increased expression of binding sites while the most efficient expression was achieved when both alpha 2b and beta 1 subunits were co-expressed with an alpha 1B subunit. The presence of alpha 2b affects the affinity of omega-CgTx GVIA binding and barium (Ba2+) current magnitudes, although it does not appear to alter kinetic properties of the Ba2+ current. This is the first evidence of an alpha 2 subunit modulating the binding affinity of a cell-surface Ca2+ channel ligand. Our results demonstrate that alpha 1, alpha 2 and beta subunits together contribute to the efficient assembly and functional expression of voltage-dependent Ca2+ channel complexes.
Science | 1992
Mark E. Williams; Pf Brust; Dh Feldman; S Patthi; S Simerson; A Maroufi; Ann F. McCue; G Velicelebi; Steven B. Ellis; Michael Miller Harpold
Science | 1990
Scott David Jay; Steven B. Ellis; Ann F. McCue; Mark E. Williams; Thomas S. Vedvick; Michael Miller Harpold; Keven P. Campbell
Archive | 1991
Michael Miller Harpold; Steven B. Ellis; Mark E. Williams; Daniel H. Feldman; Ann F. McCue; Robert Brenner
Archive | 1995
Michael Miller Harpold; Steven B. Ellis; Mark E. Williams; Daniel H. Feldman; Ann F. McCue; Robert Brenner
Archive | 1994
Michael Miller Harpold; Steven B. Ellis; Mark E. Williams; Daniel H. Feldman; Ann F. McCue; Robert Brenner
Archive | 1992
Michael Miller Harpold; Steven B. Ellis; Mark E. Williams; Daniel H. Feldman; Ann F. McCue; Robert Brenner
Archive | 1994
Michael Miller Harpold; Steven B. Ellis; Mark E. Williams; Daniel H. Feldman; Ann F. McCue; Robert Brenner
Archive | 1993
Michael Miller Harpold; Steven B. Ellis; Mark E. Williams; Daniel H. Feldman; Ann F. McCue; Robert Brenner
Canadian Journal of Microbiology | 1993
Deborah Y. Kwoh; Thomas S. Vedvick; Ann F. McCue; Diane Gevertz