2. These are a large family of cell membrane receptors.These are a large family of cell membrane receptors.
These are linked to effectors such as enzyme, channel, carrierThese are linked to effectors such as enzyme, channel, carrier
proteins for response effectuation.proteins for response effectuation.
All such receptors have a common pattern of structuralAll such receptors have a common pattern of structural
organization.organization.
Molecule has 7Molecule has 7 αα-helical membrane spanning hydrophobic-helical membrane spanning hydrophobic
amino acid segments, which run into 3 extra cellular 3 intraamino acid segments, which run into 3 extra cellular 3 intra
cellular loops.cellular loops.
3. The agonist binding site is located some were between the helicesThe agonist binding site is located some were between the helices
on the extra cellular face, while another recognition site formedon the extra cellular face, while another recognition site formed
by cytosolic segments.by cytosolic segments.
In the inactive state GDP is bound to their exposed domainIn the inactive state GDP is bound to their exposed domain
Displacement of GDP by GTP occurs.Displacement of GDP by GTP occurs.
The activeThe active αα-subunit carring GTP dissociates from the other two-subunit carring GTP dissociates from the other two
subunits and either activates or inhibits the effector.subunits and either activates or inhibits the effector.
ββ-subunits also been shown to modulate certain effectors like-subunits also been shown to modulate certain effectors like
adenylylcyclase and phospholipase C.adenylylcyclase and phospholipase C.
TheThe αα-subunit has GTPase activity.-subunit has GTPase activity.
.
4. There are 3 major effector path ways,through which GPCRs Functions
Adenylylcylase (AC) :-
cyclic AMP pathway:
Activation of AC
Intracellular accumulation of second messenger cAMP
Protein kinase (PKA)
Alters the functions of many enzymes, ion channels.
5. Phospholipase C: IP3-DAG pathway :-
Activation of phospholipase C
Hydrolyses of the membrane phopholipid
phosphatidyl inositol 4,5-bis-phosphate
Generate second messenger IP3 andDAG
Protein kinase (PKC )
Ca 2+
Modulates Contraction, secretion, metabolism
6. Channel regulation :-
Activated G-proteins can also open or close ionic channels
specipic for Ca2+
or K+
or Na+
with out intervention of cAMP
or IP3
Hyper polarization / depolarization
Changes in Physiological responses
7. Maribissen & Gutkind, 2001. G-protein coupled receptors and signaling
networks: emerging paradigms. Trend Pharm. Sci. 22:368-376.
Luttrel, et al., 1999. Regulation of tyrosine kinase cacades by G protein coupled
receptors. Curr. Opin.Cell Biol. 11:177-183.
Schonberg, T, et al., 1999. Structural basis of G protein-coupled receptor
function. Mol. Cell. Endocrin. 151:181-193.
Hamm, H. 1998. The many faces of G protein signaling. JBC 273:669-672.
Ji et al., 1998. G protein coupled receptors I. Diversity of receptor-ligand
interactions. JBC 273:17299-17302.
Gether and Koblikas, 1998. G protein coupled receptors: II. Mechansim of
agonist actiavtion. JBC 273:17979-17982.
Lefkowitz, RJ. 1998. G protein coupled receptors III: New roles for receptor
kinases and b-arrestins in receptor signaling and desensitization. JBC 273:18677.
Gutkind, S. 1998. The pathways connecting G protien coupled receptors to the
nucleus through divergent mitogen-activated protein kinase cascades. JBC
273:1839.
Fukuhara et al., 2000. Signaling from G p receptors to the nucleus, text.
32. Fukuhara, et al. 2000.
Signaling from G protien-
coupled receptors to the
nucleus. From: signaling
networks and cell cycle
control: The molecular
basis of cancer and other
diseases, Ed. JS Gutkind,
Humana Press, NJ.
38. Miller & Lefkowitz, 2001.
Expanding roles for -
arrestins as scaffolds and
adaptors in GPCR
signaling and trafficking.
Curr. Opin. Cell Biol.
13:139-145.