Transmembrane (cell surface) receptors

See also Membrane proteins.

Ion channel-linked (ionotropic) receptors

These receptors are typically the targets of fast neurotransmitters such as acetylcholine (nicotinic) and GABA; activation of these receptors results in changes in ion movement across a membrane.

• Ionotropic receptors
• 5-hydroxytryptamine receptor#Structural highlights/Specific Function of 5-HT3
• The extracellular subunit interface of the 5-HT3 receptors: a computational alanine scanning mutagenesis study^[1]
• 5-hydroxytryptamine receptor#5-HT3 receptor antagonists

5-HT3 receptor

The receptor is bullet-shaped and consists of 5 subunits (A-E) that form an oligomer. In the center of this pentamer of subunits is a ligand-gated ion channel full of water, which the 5 subunits enclose pseudo-symmetrically. Each subunit of the 5-HT3 receptor consists of 3 regions; the extracellular region, the transmembrane region, and the intracellular region.

The is relatively large compared to the other 2 regions, and contains a short C-terminus and a larger N-terminus. The N-terminus of the extracellular region is where the ligand binding occurs, and therefore deals with the agonists and antagonists.

These are located between 2 bordering subunits, assembled from 3 α-helices of 1 subunit and 3 β-strands from the other subunit. Such connection creates a binding pocket with a small, select number of residues from each subunit pointed into the binding pocket, as opposed to the large remainder of residues that are pointing from the binding pocket. This binding pocket shrinks around agonists, encapsulating them, and widens around antagonists, repulsing them.

The is within the C-terminus region, and contains 4 α-helical domains within it (M1-M4) that stretch the length of this inner, transmembrane area. These 4 α-helical domains conduct the channel openings via ion selectivity, depending on both charge and size. M2, the porous domain, contains rings of charged amino acids at both its start and its , accounting for M2’s main contribution to ion selectivity. The M3 and M4 α-helices create a large with one another, thus assembling the .

• Nicotinic Acetylcholine Receptors in general

The receptor is a transmembrane pentameric glycoprotein. It cylindrical in appearance by electron microscopy approximately 16nm in length and 8nm in diameter. The main ion channel is composed of a water pore that runs through the entire length of the protein. If viewed from the synaptic cleft, the protein will look like a pseudo-symmetrical rosette shown in the picture below composed of 10 different alpha and 4 different beta subunits.

• .
• .
• .

• Alpha-bungarotoxin is a nicotinic cholinergic antagonist that is found within the venom of Bungarus multicinctus, a South-asian snake.
• Binding site of AChR
• Acetylcholine Receptor and its Reaction to Cobra Venom

When cobra venom is introduced into the body is moves along the bloodstream to a diaphragm muscle. It works as a postsynaptic neurotoxin binding to the receptor as an extracellular ligand by interacting with OH group leaving the acetylcholine channel open which releases ions used in creating an action potential. There must be 5 molecules of cobra toxin (red) to block the receptor (blue) as each molecule binds with an individual alpha chain on the acetylcholine receptor. This molecule was generated by overlaying the receptor and venom using Swiss PDB viewer magic fit. The second image depicts an individual toxin binding with one chain on the receptor, both in the same color. This representation shows each molecule of the .

• AMPA glutamate receptor by University of Massachusetts Amherst Chemistry-Biology Interface Program at UMass Amherst and on display at the Molecular Playground.

Full view of the glutamate receptor shows the overall structure (amino-terminal, ligand-binding and transmembrane domains) in both (MF) and models.

Zooming in at the top of the receptor () (RCB) one can view the amino terminal domain, which is a part of the extracellular domain. This domain is implicated in receptor assembly, trafficking, and localization.

Moving toward the bottom of the receptor () (SM) one can view the transmembrane domain. Here is the same domain separated from the rest of the protein. (DM). This domain widens in response to glutamate binding allowing for positive ions to pass through the post-synaptic membrane.

This view () highlights the area where a receptor antagonist, 2K200225, will bind.

Close up view of the ligand binding site () (AH) of the endogenous ligand glutamate.

• Glutamate receptor (GluA2)

G protein-linked (metabotropic) receptors

This is the largest family of receptors and includes the receptors for several hormones and slow transmitters (dopamine, metabotropic glutamate). They are composed of 7 transmembrane alpha helices. The loops connecting the alpha helices form extracellular and intracellular domains. The binding-site for larger peptide ligands is usually located in the extracellular domain whereas the binding site for smaller non-peptide ligands is often located between the seven alpha helices and one extracellular loop. These receptors are coupled to different intracellular effector systems via G proteins

• G protein-coupled receptors
• Neurotensin receptor

Like other G protein-coupled receptors, NTSR1 is composed of 3 distinct regions. An where neurotensin binds and causes a conformational change of the protein. A region containing (PDB code:4GRV) that transduce the signal from the extracellular side of the cell membrane to the intracellular side. Lastly, an intracellular region that when activated by a conformational change in the protein activates a G-protein associated with this receptor.

The in NTSR1 is located at the top of the protein (Figure 1). NTSR1 also contains an allosteric , which is located directly beneath the ligand binding pocket and the two pockets, which are separated by the residue ^[2]. NTSR1 has been mutated to exist in both and states.

• CXC chemokine receptor type 4

(PDB code 3oe0).

.

.

• Mu Opioid Receptor Bound to a Morphinan Antagonist

In this crystal structure of the μ opioid receptor it is (β-FNA), a close relative of morphine that is bound in the pocket.

• μ Opioid Receptors
• Mu Opioid Receptor

In the case of the μ-opioid receptor, the binding of an opioid signaling molecule induces a in the receptor that activates an inhibitory G-protein (Gαi/o). This results in the dissociation of the G-protein complex. The Gα subunit then inhibits adenylyl cyclase. The Gβγ subunit acts to inhibit Ca2+ channels while activing K+ channels. While much has been learned about μ-opioid receptors since their discovery in 1973, there is still much that is unknown about their structure and .

• The κ-opioid receptor binds opium-type ligands.
• The δ-opioid receptor binds enkephalins
• Tutorial: The opioid receptor, a molecular switch
• Orexin and Orexin receptor

The through a constricted solvent-accessible channel. A ^[3].

• Belsomra and Orexin receptors
• Hypocretin and receptors
• Human Follicle-Stimulating Hormone Complexed with its Receptor
• GPR40
• Lysophosphatidic acid receptor
• Sphingosine 1-phosphate Receptor
• Rhodopsin
• Rhodopsin Structure and Function
• Serotonin receptors, main page
• 3D structures of Serotonin receptors
• Adrenergic receptors in general
• Beta-1 Adrenergic receptor
• Dobutamine: Beta-1 Adrenergic receptor, 2y00, 2y01, 6h7l
• Isoprenaline: Beta-1 Adrenergic receptor, 2y03
• Carmoterol: 2y02
• Salbutamol: 2y04
• Adrenergic receptor page.
• Article Beta-2 Adrenergic Receptor by Wayne Decatur, David Canner, Dotan Shaniv, Joel L. Sussman, Michal Harel
• Article Beta-2 adrenergic receptor by Joel L. Sussman, Tala Curry, Michal Harel, Jaime Prilusky
• Group:SMART:A Physical Model of the beta-Adrenergic Receptor
• G_s: adenylate cyclase activated, cAMP up. For G_s see Beta2 adrenergic receptor-Gs protein complex updated
• Dopamine receptors 1 page
• Dopamine receptors 2 page
• Histamine H1 receptor
• 3rze - human histamine H1 receptor with an antagonist doxepin
• Adenosine A2A receptor
• Effect of Caffeine (Trimethylxanthine) on Human A2A Receptor
• Muscarinic acetylcholine receptor
• Glucose-dependent Insulinotropic Polypeptide Receptor
• Glucagon receptor
• Glucagon-like peptide 1 receptor
• Metabotropic Glutamate Receptors
• Ligand Binding N-Terminal of Metabotropic Glutamate Receptors
• Metabotropic glutamate receptor 5

Kinase-linked, enzyme-linked and related receptors

Receptor tyrosine kinases

Receptor tyrosine kinases (RTKs) are part of the larger family of protein tyrosine kinases. They are the high-affinity cell surface receptors for many polypeptide growth factors, cytokines, and hormones. Approximately 20 different RTK classes have been identified.^[4]

• RTK class I Epidermal Growth Factor Receptor family
• RTK class II Insulin receptor family
• RTK class III Platelet-derived growth factor receptor family
• RTK class IV Vascular Endothelial Growth Factor Receptor family
• RTK class V Fibroblast growth factor receptor family
• RTK class VIII Hepatocyte growth factor receptor family
• RTK class IX Ephrin receptor family
• RTK class XIII Epithelial discoidin domain-containing receptor (DDR receptor) family
• Neurotrophin: High affinity nerve growth factor receptor (or Tyrosine kinase receptor) and TrkB tyrosine kinase receptor
• Insulin-like growth factor receptor

Enzyme-linked receptor

• TGF-beta receptor
• Activin receptor
• Crystal structure of the extracellular domain of the receptor-like kinase TMK3 from Arabidopsis thaliana
• Bone Morphogenetic Protein 7 and receptor
• Neurotrophin
• High affinity nerve growth factor receptor TrkA
• TrkB tyrosine kinase receptor
• Toll-like Receptors

Immune receptors

Leukocyte immunoglobulin-like receptors

• Leukocyte immunoglobulin-like receptor

Cytokine receptors

TNF receptor superfamily

• Tumor necrosis factor receptor
  • TRAIL (TNF-related apoptosis-inducing ligand) or TNF ligand superfamily 10

Colony-stimulating factor receptor

Type I cytokine receptors

• Erythropoietin receptor
• Prolactin receptor

Type II cytokine receptors

Interferon receptors

• Interferon receptor
• Structural linkage between ligand discrimination and receptor activation by type I interferons
• Multiple sclerosis and Interferon Receptors

Interleukin receptors

• Interleukin receptor

Interleukin-20 receptor:

• Flexible regions govern promiscuous binding of IL-24 to receptors IL-20R1 and IL-22R1

Chemokine receptors, two of which acting as binding proteins for HIV (CXCR4 and CCR5). They are G protein-coupled receptors

T-cell receptors

• T-cell receptor
• SP3.4-TCR-HLA-DQ8-α-1-gliadin complex

TGF-beta receptor

• TGF-beta receptor

LDL receptor

• LDL receptor

Transferrin receptor

• Transferrin receptor

Intracellular receptors

Signal recognition particle receptor

• Signal recognition particle receptor

Receptor for activated C kinase 1

• Receptor for activated protein kinase C 1

Nuclear receptors

• Nuclear receptors
• Thyroid hormone receptor
• Retinoic acid receptor
• RA Mediated T-reg Differentiation; Retinoic acid acts as the ligand for the Retinoic Acid Receptor-α (RARα) / Retinoid X Receptor-α (RXRα) heterodimer
• PPAR-gamma
• Pioglitazone is a selective agonist for Peroxisome Proliferator-Activated Receptor Gamma
• Liver X receptor
• Bile acid receptor
• Vitamin D receptor
• Pregnane X receptor
• Retinoid X receptor
• Estrogen receptor
• Ivan Koutsopatriy estrogen receptor
• Estrogen receptor#Structure of estradiol metal chelate and estrogen receptor complex: The basis for designing a new class of SERMs ^[5]
• Estrogen receptor#Estrogen receptor α complexed with raloxifene and a corepressor peptide
• Tamoxifen and the Estrogen receptor
• Student Project 10 for UMass Chemistry 423 Spring 2015
• Estrogen-related receptor
• Glucocorticoid receptor
• Mineralocorticoid receptor
• Progesterone receptor
• Androgen receptor
• Liver receptor homolog-1?

Endoplasmic reticulum/Sarcoplasmic reticulum receptors

Ligand-gated Calcium channels

Inositol 1,4,5-Trisphosphate Receptor

Ryanodine receptor

SEE ALSO:

• Hormones and their receptors
• Hormone
• Growth factors
• Neurotransmitters