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Molecular details of cAMP generation in mammalian cells: a tale of two systems
Authors:Kamenetsky Margarita  Middelhaufe Sabine  Bank Erin M  Levin Lonny R  Buck Jochen  Steegborn Clemens
Affiliation:Department of Pharmacology, Joan and Sanford I. Weill Medical College of Cornell University, New York, NY 10021, USA.
Abstract:The second messenger cAMP has been extensively studied for half a century, but the plethora of regulatory mechanisms controlling cAMP synthesis in mammalian cells is just beginning to be revealed. In mammalian cells, cAMP is produced by two evolutionary related families of adenylyl cyclases, soluble adenylyl cyclases (sAC) and transmembrane adenylyl cyclases (tmAC). These two enzyme families serve distinct physiological functions. They share a conserved overall architecture in their catalytic domains and a common catalytic mechanism, but they differ in their sub-cellular localizations and responses to various regulators. The major regulators of tmACs are heterotrimeric G proteins, which transduce extracellular signals via G protein-coupled receptors. sAC enzymes, in contrast, are regulated by the intracellular signaling molecules bicarbonate and calcium. Here, we discuss and compare the biochemical, structural and regulatory characteristics of the two mammalian AC families. This comparison reveals the mechanisms underlying their different properties but also illustrates many unifying themes for these evolutionary related signaling enzymes.
Keywords:AC, adenylyl cyclase   α,β-Me-ATP, α,β-methylene-adenosine-5′-triphosphate   ATPαS, adenosine-5′-α-thio-triphosphate   FRET, fluorescence resonance energy transfer   GC, guanylyl cyclase   Gβγ, G protein, β and γ subunits   Gsα, stimulatory G protein, α subunit   Giα, inhibitory G protein, α subunit   Km, Michaelis constant   MANT, 2′(3′)-O-(N-methylanthraniloyl)   PDE, phosphodiesterase   PKA, protein kinase A   PMC-6, 1R,4R-3-(6-aminopurin-9-yl)-cyclopentanecarboxylic acid hydroxyamide   sAC, soluble adenylyl cyclase   sACfl, full-length soluble adenylyl cyclase   sACt, truncated form of soluble adenylyl cyclase   tmAC, transmembrane adenylyl cyclase   TM, transmembrane   vmax, maximum reaction velocity
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