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Beta-1 adrenergic receptor

August 29, 2023

The beta-1 adrenergic receptor1 adrenoceptor), also known as ADRB1, can either refer to the protein-encoding gene (gene ADRB1) or one of the four adrenergic receptors.[5] It is a G-protein coupled receptor associated with the Gs heterotrimeric G-protein that is expressed predominantly in cardiac tissue. In addition to cardiac tissue, beta-1 adrenergic receptors are also expressed in the cerebral cortex.

ADRB1
Available structures
PDBOrtholog search: PDBe RCSB
Identifiers
AliasesADRB1, ADRB1R, B1AR, BETA1AR, RHR, adrenoceptor beta 1, FNSS2
External IDsOMIM: 109630 MGI: 87937 HomoloGene: 20171 GeneCards: ADRB1
Orthologs
SpeciesHumanMouse
Entrez

153

11554

Ensembl

ENSG00000043591

ENSMUSG00000035283

UniProt

P08588

P34971

RefSeq (mRNA)

NM_000684

NM_007419

RefSeq (protein)

NP_000675

NP_031445

Location (UCSC)Chr 10: 114.04 – 114.05 MbChr 19: 56.71 – 56.72 Mb
PubMed search[3][4]
Wikidata
View/Edit HumanView/Edit Mouse

Historical Context Edit

W. B. Cannon postulated that there were two chemical transmitters or sympathins while studying the sympathetic nervous system in 1933. These E and I sympathins were involved with excitatory and inhibitory responses. In 1948, Raymond Ahlquist published a manuscript in the American Journal of Physiology establishing the idea of adrenaline having distinct actions on both alpha and beta receptors. Shortly afterward, Eli Lilly Laboratories synthesized the first beta-blocker, dichloroisoproterenol.

General Information Edit

Structure Edit

ADRB-1 is a transmembrane protein that belongs to the G-Protein-Coupled Receptor (GPCR) family.[6][7] GPCRs play a key role in cell signaling pathways and are primarily known for their seven transmembrane (7TM) helices, which have a cylindrical structure and span the membrane. The 7TM domains have three intracellular and three extracellular loops that connect these domains to one another. The extracellular loops contain sites for ligand binding on N-terminus of the receptor and the intracellular loops and C-terminus interact with signaling proteins, such as G-proteins. The extracellular loops also contain several sites for post-translational modification and are involved in ligand binding. The third intracellular loop is the largest and contains phosphorylation sites for signaling regulation. As the name suggests, GPCRs are coupled to G-proteins that are heterotrimeric in nature. Heterotrimeric G-proteins consist of three subunits: alpha, beta, and gamma.[8] Upon the binding of a ligand to the extracellular domain of the GPCR, a conformational change is induced in the receptor that allows it to interact with the alpha-subunit of the G-protein. Following this interaction, the G-alpha subunit exchanges GDP for GTP, becomes active, and dissociates from the beta and gamma subunits. The free alpha subunit is then able to activate downstream signaling pathways (detail more in interactions and pathway).

Function Edit

Pathways Edit

ADRB-1 is activated by the catecholamines adrenaline and noradrenaline. Once these ligands bind, the ADRB-1 receptor activates several different signaling pathways and interactions. Some of the most well-known pathways are:

  1. Adenylyl Cyclase: When a ligand binds to the ADRB-1 Receptor, the alpha-subunit of the heterotrimeric G-protein gets activated, which in turn, activates the enzyme adenylyl cyclase. Adenylyl cyclase then catalyzes the conversion of ATP to cyclic AMP (cAMP), which activates downstream effectors such as Protein Kinase A (PKA).
  2. cAMP Activation of PKA: cAMP generated by adenylyl cyclase activates PKA, which then phosphorylates numerous downstream targets such as ion channels, other enzymes, and transcription factors .
  3. Beta-arrestins: Activation of the ADRB-1 receptor can lead to the recruitment of Beta-arrestins, which are used to activate signaling pathways independent of G-proteins. An example of an independent pathway is the MAPK (mitogen-activated protein kinase) pathways.
  4. Calcium signaling: ADRB-1 signaling also activates the Gq/11 family of G proteins, which is a subfamily of heterotrimeric G proteins that activates phospholipase C (PLC). PLC cleaves phosphatidylinositol 4,5-bisphosphate (PIP2) into the second messengers inositol 1,4,5-triphosphate (IP3) and diacylglycerol (DAG). IP3 binds to IP3 receptors on the endoplasmic reticulum, which then leads to the release of calcium ions (Ca2+) into the cytoplasm, resulting in the activation of downstream signaling pathways.

Summary of Interactions Edit

Actions of the β1 receptor include:

System Effect Tissue
Muscular Increases cardiac output Cardiac muscle
Increases heart rate (chronotropic effect) Sinoatrial node (SA node) [9]
Increases atrial contractility (inotropic effect) Cardiac muscle
Increases contractility and automaticity Ventricular cardiac muscle [9]
Increases conduction and automaticity Atrioventricular node (AV node)[9]
Relaxation Urinary bladder wall[10]
Exocrine Releases renin Juxtaglomerular cells.[9]
Stimulates viscous, amylase-filled secretions

Salivary glands[11]

Other Lipolysis Adipose tissue[9]

The receptor is also present in the cerebral cortex.

Other pathways that play ADRB-1 receptor plays an important role in:

  1. Regulation of peripheral clock and central circadian clock synchronization: The suprachiasmatic nucleus (SCN) receives light information from the eyes and synchronizes the peripheral clocks to the central circadian clock through the release of different neuropeptides and hormones.[12] ADRB-1 receptors can play a role in modulating the release of neuropeptides like vasoactive intestinal peptide (VIP) and arginine vasopressin (AVP) from the SCN, which can then synchronize peripheral clocks.
  2. Regulation of glucose metabolism: The regulation of glucose metabolism is known to be linked with ADRB-1 receptor signaling.[13] The signal transduction pathway that is activated through the ADRB-1 receptor can regulate the expression of clock genes and glucose transporters. The disregulation of ADRB-1 receptor signaling has been implicated in metabolic disorders such as diabetes and obesity.
  3. ADRB-1 Receptor and Rhythmic Control of Immunity: Circadian oscillations in catecholamine signals influence various cellular targets which express adrenergic receptors, including immune cells.[12] The adrenergic system regulates a range of physiological functions which are carried out through catecholamine production. Humans are found to have low circulating catecholamine levels during the night and high levels during the day, while rodents exhibit the opposite pattern. Studies demonstrating the patterns of norepinephrine levels indicate that there is no circadian rhythmicity. Circulating rhythms in epinephrine, however, appear to be circadian and are regulated by the HPA axis:
    1. Cyclic variation in HPA signals are likely important in driving diurnal oscillations in adrenaline.
    2. The most well-characterized means through which adrenergic signals exert circadian control over immunity is by cell-trafficking regulation. Variation in the number of white blood cells seemed to be linked to adrenergic function.
  4. Cardiac rhythm and Cardiac Failure: The β-AR signaling pathway serves as a primary component of the interface between the sympathetic nervous system and the cardiovascular system.[14] The β-AR pathway dysregulation has been implicated in the pathogenesis of heart failure. It has been found that certain changes to β-AR signaling result in reduced levels of  β1-AR, by up to 50%, while levels of β2-AR remain constant. Other intracellular changes include a significant, sharp increase of GαI levels, and increased βARK1 activity. These changes suggest sharp decreases in  β-AR signaling, likely due to sustained, elevated levels of catecholamines.

Mechanism in cardiac myocytes Edit

Gs exerts its effects via two pathways. Firstly, it directly opens L-type calcium channels (LTCC) in the plasma membrane. Secondly, it renders adenylate cyclase activated, resulting in an increase of cAMP, activating protein kinase A (PKA) which in turn phosphorylates several targets, such as phospholamban, LTCC, Troponin I (TnI), and potassium channels. The phosphorylation of phospholamban deactivates its own function which normally inhibits SERCA on the sarcoplasmic reticulum (SR) in cardiac myocytes. Due to this, more calcium enters the SR and is therefore available for the next contraction. LTCC phosphorylation increases its open probability and therefore allows more calcium to enter the myocyte upon cell depolarisation. Both of these mechanisms increase the available calcium for contraction and therefore increase inotropy. Conversely, TnI phosphorylation results in its facilitated dissociation of calcium from troponin C (TnC) which speeds the muscle relaxation (positive lusitropy). Potassium channel phosphorylation increases its open probability which results in shorter refractory period (because the cell repolarises faster), also increasing lusitropy. Furthermore, in nodal cells such as in the SA node, cAMP directly binds to and opens the HCN channels, increasing their open probability, which increases chronotropy.[6]

Clinical Significance Edit

Familial Natural Short Sleep (FNSS) Edit

A rare mutation that changes a cytosine to a thymine in the ADRB-1 coding sequence results in a protein switch to valine from alanine at amino acid position 187 (A187) and leads to the FNSS behavior trait, where mutation carriers naturally wake up after only 4 to 6.5 hours of sleep. The ADRB-1 protein is involved in a cyclic adenosine monophosphate (cAMP)-mediated signaling pathway, and the ADRB1-A187V mutated protein leads to a lower cAMP production than the wild-type protein, given the same isoproterenol treatment, a nonselective agonist of ADRB-1.[15] It was also discovered that the mutated protein is less stable most likely due to post-translational modifications, as shown in an ADRB1 knockin experiment where a mutated ADRB-1 gene replaces the wild-type with CRISPR technology and the protein level displays a decrease while the mRNA level remains high.[15]

Mice with a heterozygous ADRB1-A187V mutation show increased activity time and shorter intervals of rapid eye movement (REM) sleep and non-REM sleep, suggesting that the mutation causes short sleep. In another experiment, the ADRB1-A187V mutation restored REM sleep in tau mice (PS19) and reduced tau accumulation, which can promote brain cell damage and death, in the locus coeruleus (LC) of PS19 mice.[16] Furthermore, a high expression level of ADRB-1 protein is observed in the dorsal pons (DP), referred to as ADRB1+ neurons. The activity of these ADRB1+ neurons in DP is shown to be closely linked with the sleep-wake behavior and altered by the ADRB1-A187V mutation. The ADRB1+ neurons can be either inhibitory or excitatory. In the brains of mutant mice, the percentage of ADRB1+ neurons that may be inhibited by agonists reduces significantly while the percentage of neurons that may be excited by agonists remains relatively unchanged.[15] It is thus speculated that the ADRB-1 protein has an inhibitory and an excitatory function, with the inhibitory function being more sensitive to its decreased protein levels and the excitatory function being less sensitive. Although the ADRB1-A187V mutation leads to lower protein levels, as discussed above, overall there are fewer ADRB1+ neurons inhibited, corresponding to the higher total activity of DP ADRB1+ neurons observed in mutant mice. These results collectively indicate that high activity levels in ADRB1+ neurons leads to shorter sleep or FNSS.

Polymorphisms in ADRB-1 Edit

One of the single nucleotide polymorphisms (SNPs) in ADRB-1 is the change from a cytosine to a guanine, resulting in a protein switch from arginine (389R) to glycine (389G) at the 389 codon position. Arginine at codon 389 is highly preserved across species and this mutation happens in the G-protein binding domain of ADRB-1, one of the key functions of ADRB-1 protein, so it is likely to lead to functional differences. In fact, this SNP causes dampened efficiency and affinity in agonist-promoted receptor binding.[17]

Another common SNP occurs at codon position 49, with a change of serine (49S) to glycine (49G) in the N-terminus sequence of ADRB-1. The 49S variant is shown to be more resistant to agonist-promoted down regulation and short intervals of agonist exposure. The receptor of the 49G variant is always expressed, which results in high coupling activity with adenylyl cyclase and increased sensitivity to agonists.[17]

Both of these SNPs have relatively high frequencies among populations and are thought to affect cardiac functions. Individuals who are homozygous for the 389R allele are more likely to have higher blood pressure and heart rates than others who have either one or two copies of the 389G allele. Additionally, patients with heart diseases that have a substitution of glycine for serine at codon 49 (49S > G) show improved cardiac functions and decreased mortality rate.[18] The cardiovascular responses induced by this polymorphism in the healthy population are also examined. Healthy individuals with a glycine at codon 49 show better cardiovascular functions at rest and response to maximum heart rate during exercise, evident for the cardioprotection related to this polymorphism.[18]

Pharmaceutical Interventions Edit

Because ADRB-1 play such a critical role in maintaining blood pressure homeostasis and cardiac output, many medications treat these conditions by either potentiating or inhibiting the functions of the ADRB-1. Dobutamine is one of the adrenergic drugs and agonists that selectively bind to ADRB-1 and is often used in treatments of cardiogenic shock and heart failure.[19] It is also important to note the use of illicit drug for ADRB-1 since cocaine, beta-blocking agents, or other sympathetic stimulators may cause a medical emergency.

Agonists Edit

ADRB-1 agonists mimic or initiate a physiological response when bound to a receptor. Isoprenaline has higher affinity for β1 than adrenaline, which, in turn, binds with higher affinity than noradrenaline at physiologic concentrations. As ADRB-1 increases cardiac output, selective agonists clinically function as potential treatments for heart failure. Selective agonists to the beta-1 receptor are:

  • Denopamine is used in the treatment of angina and has potential uses to treat congestive heart failure and pulmonary oedema.
  • Dobutamine[11] (in cardiogenic shock) is a beta-1 agonist that treats cardiac decompensation.
  • Xamoterol[11] (cardiac stimulant) acts as a partial agonist that improves heart function in studies with cardiac failure. Xamoterol plays a role in modulating the sympathetic nervous system, but does not have any agonistic action on beta-2 adrenergic receptors.
  • Isoproterenol is a nonselective agonist that potentiates the effects of agents like adrenaline and norepinephrine to increase heart contractility.

Antagonists Edit

ADRB-1 antagonists are a class of drugs also referred to as Beta Blockers β1-selective antagonists are used to manage abnormal heart rhythms and block the action of substances like adrenaline on neurons, allowing blood to flow more easily which lowers blood pressure and cardiac output. They may also shrink vascular tumors. Some examples of Beta-Blockers include:

See also Edit

References Edit

  1. ^ a b c GRCh38: Ensembl release 89: ENSG00000043591 - Ensembl, May 2017
  2. ^ a b c GRCm38: Ensembl release 89: ENSMUSG00000035283 - Ensembl, May 2017
  3. ^ "Human PubMed Reference:". National Center for Biotechnology Information, U.S. National Library of Medicine.
  4. ^ "Mouse PubMed Reference:". National Center for Biotechnology Information, U.S. National Library of Medicine.
  5. ^ "Entrez Gene: ADRB1 adrenergic, beta-1-, receptor".
  6. ^ a b Boron WF, Boulpaep EL (2012). Medical physiology : a cellular and molecular approach (Updated second ed.). Philadelphia, PA. ISBN 9781437717532. OCLC 756281854.{{cite book}}: CS1 maint: location missing publisher (link)
  7. ^ Rosenbaum DM, Rasmussen SG, Kobilka BK (May 2009). "The structure and function of G-protein-coupled receptors". Nature. 459 (7245): 356–363. doi:10.1038/nature08144. PMC 3967846. PMID 19458711.
  8. ^ Nestler, Eric J.; Duman, Ronald S. (1999). "Heterotrimeric G Proteins". Basic Neurochemistry: Molecular, Cellular and Medical Aspects. 6th edition.
  9. ^ a b c d e Fitzpatrick D, Purves D, Augustine G (2004). "Table 20:2". Neuroscience (Third ed.). Sunderland, Mass: Sinauer. ISBN 978-0-87893-725-7.
  10. ^ Moro C, Tajouri L, Chess-Williams R (January 2013). "Adrenoceptor function and expression in bladder urothelium and lamina propria". Urology. 81 (1): 211.e1–211.e7. doi:10.1016/j.urology.2012.09.011. PMID 23200975.
  11. ^ a b c d e Rang, H. P. (2003). Pharmacology. Edinburgh: Churchill Livingstone. ISBN 978-0-443-07145-4. Page 163
  12. ^ a b Leach S, Suzuki K (2020). "Adrenergic Signaling in Circadian Control of Immunity". Frontiers in Immunology. 11: 1235. doi:10.3389/fimmu.2020.01235. PMC 7344327. PMID 32714319.
  13. ^ Jovanovic, Aleksandra; Xu, Bing; Zhu, Chaoqun; Ren, Di; Wang, Hao; Krause-Hauch, Meredith; Abel, E. Dale; Li, Ji; Xiang, Yang K. (February 2023). "Characterizing Adrenergic Regulation of Glucose Transporter 4-Mediated Glucose Uptake and Metabolism in the Heart". JACC: Basic to Translational Science: S2452302X23000098. doi:10.1016/j.jacbts.2022.11.008. PMC 10322917.
  14. ^ Madamanchi A (July 2007). "Beta-adrenergic receptor signaling in cardiac function and heart failure". McGill Journal of Medicine. 10 (2): 99–104. PMC 2323471. PMID 18523538.
  15. ^ a b c Shi G, Xing L, Wu D, Bhattacharyya BJ, Jones CR, McMahon T, et al. (September 2019). "A Rare Mutation of β1-Adrenergic Receptor Affects Sleep/Wake Behaviors". Neuron. 103 (6): 1044–1055.e7. doi:10.1016/j.neuron.2019.07.026. PMC 6763376. PMID 31473062.
  16. ^ Dong Q, Ptáček LJ, Fu YH (April 2023). "Mutant β1-adrenergic receptor improves REM sleep and ameliorates tau accumulation in a mouse model of tauopathy". Proceedings of the National Academy of Sciences of the United States of America. 120 (15): e2221686120. doi:10.1073/pnas.2221686120. PMC 10104526. PMID 37014857. S2CID 257922859.
  17. ^ a b Sandilands AJ, O'Shaughnessy KM (September 2005). "The functional significance of genetic variation within the beta-adrenoceptor". British Journal of Clinical Pharmacology. 60 (3): 235–243. doi:10.1111/j.1365-2125.2005.02438.x. PMC 1884766. PMID 16120061.
  18. ^ a b Kelley EF, Snyder EM, Johnson BD (December 2018). "Influence of Beta-1 Adrenergic Receptor Genotype on Cardiovascular Response to Exercise in Healthy Subjects". Cardiology Research. 9 (6): 343–349. doi:10.14740/cr785. PMC 6306116. PMID 30627284.
  19. ^ Farzam, Khashayar; Kidron, Ariel; Lakhkar, Anand D. (2023), "Adrenergic Drugs", StatPearls, Treasure Island (FL): StatPearls Publishing, PMID 30480963, retrieved 2023-04-26
  20. ^ American Society of Health-System Pharmacists, Inc. (2005-01-01). . MedlinePlus Drug Information. U.S. National Library of Medicine, National Institutes of Health. Archived from the original on 2008-05-20. Retrieved 2008-06-06.

Further reading Edit

  • Frielle T, Kobilka B, Lefkowitz RJ, Caron MG (July 1988). "Human beta 1- and beta 2-adrenergic receptors: structurally and functionally related receptors derived from distinct genes". Trends in Neurosciences. 11 (7): 321–324. doi:10.1016/0166-2236(88)90095-1. PMID 2465637. S2CID 140209236.
  • Muszkat M (August 2007). "Interethnic differences in drug response: the contribution of genetic variability in beta adrenergic receptor and cytochrome P4502C9". Clinical Pharmacology and Therapeutics. 82 (2): 215–218. doi:10.1038/sj.clpt.6100142. PMID 17329986. S2CID 10381767.
  • Yang-Feng TL, Xue FY, Zhong WW, Cotecchia S, Frielle T, Caron MG, et al. (February 1990). "Chromosomal organization of adrenergic receptor genes". Proceedings of the National Academy of Sciences of the United States of America. 87 (4): 1516–1520. Bibcode:1990PNAS...87.1516Y. doi:10.1073/pnas.87.4.1516. PMC 53506. PMID 2154750.
  • Forse RA, Leibel R, Gagner M (January 1989). "The effect of Escherichia coli endotoxin on the adrenergic control of lipolysis in the human adipocyte". The Journal of Surgical Research. 46 (1): 41–48. doi:10.1016/0022-4804(89)90180-7. PMID 2536864.
  • Frielle T, Collins S, Daniel KW, Caron MG, Lefkowitz RJ, Kobilka BK (November 1987). "Cloning of the cDNA for the human beta 1-adrenergic receptor". Proceedings of the National Academy of Sciences of the United States of America. 84 (22): 7920–7924. Bibcode:1987PNAS...84.7920F. doi:10.1073/pnas.84.22.7920. PMC 299447. PMID 2825170.
  • Stiles GL, Strasser RH, Lavin TN, Jones LR, Caron MG, Lefkowitz RJ (July 1983). "The cardiac beta-adrenergic receptor. Structural similarities of beta 1 and beta 2 receptor subtypes demonstrated by photoaffinity labeling". The Journal of Biological Chemistry. 258 (13): 8443–8449. doi:10.1016/S0021-9258(20)82084-5. PMID 6305985.
  • Hoehe MR, Otterud B, Hsieh WT, Martinez MM, Stauffer D, Holik J, et al. (June 1995). "Genetic mapping of adrenergic receptor genes in humans". Journal of Molecular Medicine. 73 (6): 299–306. doi:10.1007/BF00231616. PMID 7583452. S2CID 27308274.
  • Elies R, Ferrari I, Wallukat G, Lebesgue D, Chiale P, Elizari M, et al. (November 1996). "Structural and functional analysis of the B cell epitopes recognized by anti-receptor autoantibodies in patients with Chagas' disease". Journal of Immunology. 157 (9): 4203–4211. doi:10.4049/jimmunol.157.9.4203. PMID 8892658. S2CID 44386743.
  • Oldenhof J, Vickery R, Anafi M, Oak J, Ray A, Schoots O, et al. (November 1998). "SH3 binding domains in the dopamine D4 receptor". Biochemistry. 37 (45): 15726–15736. doi:10.1021/bi981634+. PMID 9843378.
  • Mason DA, Moore JD, Green SA, Liggett SB (April 1999). "A gain-of-function polymorphism in a G-protein coupling domain of the human beta1-adrenergic receptor". The Journal of Biological Chemistry. 274 (18): 12670–12674. doi:10.1074/jbc.274.18.12670. PMID 10212248.
  • Moore JD, Mason DA, Green SA, Hsu J, Liggett SB (September 1999). "Racial differences in the frequencies of cardiac beta(1)-adrenergic receptor polymorphisms: analysis of c145A>G and c1165G>C". Human Mutation. 14 (3): 271. doi:10.1002/(SICI)1098-1004(1999)14:3<271::AID-HUMU14>3.0.CO;2-Q. PMID 10477438. S2CID 8860722.
  • Tang Y, Hu LA, Miller WE, Ringstad N, Hall RA, Pitcher JA, et al. (October 1999). "Identification of the endophilins (SH3p4/p8/p13) as novel binding partners for the beta1-adrenergic receptor". Proceedings of the National Academy of Sciences of the United States of America. 96 (22): 12559–12564. Bibcode:1999PNAS...9612559T. doi:10.1073/pnas.96.22.12559. PMC 22990. PMID 10535961.
  • Podlowski S, Wenzel K, Luther HP, Müller J, Bramlage P, Baumann G, et al. (2000). "Beta1-adrenoceptor gene variations: a role in idiopathic dilated cardiomyopathy?". Journal of Molecular Medicine. 78 (2): 87–93. doi:10.1007/s001090000080. PMID 10794544. S2CID 1072602.
  • Shiina T, Kawasaki A, Nagao T, Kurose H (September 2000). "Interaction with beta-arrestin determines the difference in internalization behavor between beta1- and beta2-adrenergic receptors". The Journal of Biological Chemistry. 275 (37): 29082–29090. doi:10.1074/jbc.M909757199. PMID 10862778.
  • Hu LA, Tang Y, Miller WE, Cong M, Lau AG, Lefkowitz RJ, Hall RA (December 2000). "beta 1-adrenergic receptor association with PSD-95. Inhibition of receptor internalization and facilitation of beta 1-adrenergic receptor interaction with N-methyl-D-aspartate receptors". The Journal of Biological Chemistry. 275 (49): 38659–38666. doi:10.1074/jbc.M005938200. PMID 10995758.
  • Börjesson M, Magnusson Y, Hjalmarson A, Andersson B (November 2000). "A novel polymorphism in the gene coding for the beta(1)-adrenergic receptor associated with survival in patients with heart failure". European Heart Journal. 21 (22): 1853–1858. doi:10.1053/euhj.1999.1994. PMID 11052857.
  • Xu J, Paquet M, Lau AG, Wood JD, Ross CA, Hall RA (November 2001). "beta 1-adrenergic receptor association with the synaptic scaffolding protein membrane-associated guanylate kinase inverted-2 (MAGI-2). Differential regulation of receptor internalization by MAGI-2 and PSD-95". The Journal of Biological Chemistry. 276 (44): 41310–41317. doi:10.1074/jbc.M107480200. PMID 11526121.
  • Hu LA, Chen W, Premont RT, Cong M, Lefkowitz RJ (January 2002). "G protein-coupled receptor kinase 5 regulates beta 1-adrenergic receptor association with PSD-95". The Journal of Biological Chemistry. 277 (2): 1607–1613. doi:10.1074/jbc.M107297200. PMID 11700307.
  • Ranade K, Jorgenson E, Sheu WH, Pei D, Hsiung CA, Chiang FT, et al. (April 2002). "A polymorphism in the beta1 adrenergic receptor is associated with resting heart rate". American Journal of Human Genetics. 70 (4): 935–942. doi:10.1086/339621. PMC 379121. PMID 11854867.

Further reading Edit

  • Alhayek S, Preuss CV (August 2022). "Beta 1 Receptors.". StatPearls [Internet]. Treasure Island (FL): StatPearls Publishing. PMID 30422499.

External links Edit

  • Human ADRB1 genome location and ADRB1 gene details page in the UCSC Genome Browser.
  • 1-adrenoceptor". IUPHAR Database of Receptors and Ion Channels. International Union of Basic and Clinical Pharmacology.
  • Overview of all the structural information available in the PDB for UniProt: P08588 (Beta-1 adrenergic receptor) at the PDBe-KB.

August 29, 2023
beta, adrenergic, receptor, beta, adrenergic, receptor, adrenoceptor, also, known, adrb1, either, refer, protein, encoding, gene, gene, adrb1, four, adrenergic, receptors, protein, coupled, receptor, associated, with, heterotrimeric, protein, that, expressed, . The beta 1 adrenergic receptor b1 adrenoceptor also known as ADRB1 can either refer to the protein encoding gene gene ADRB1 or one of the four adrenergic receptors 5 It is a G protein coupled receptor associated with the Gs heterotrimeric G protein that is expressed predominantly in cardiac tissue In addition to cardiac tissue beta 1 adrenergic receptors are also expressed in the cerebral cortex ADRB1Available structuresPDBOrtholog search PDBe RCSBList of PDB id codes2LSQIdentifiersAliasesADRB1 ADRB1R B1AR BETA1AR RHR adrenoceptor beta 1 FNSS2External IDsOMIM 109630 MGI 87937 HomoloGene 20171 GeneCards ADRB1Gene location Human Chr Chromosome 10 human 1 Band10q25 3Start114 043 866 bp 1 End114 046 904 bp 1 Gene location Mouse Chr Chromosome 19 mouse 2 Band19 D2 19 51 96 cMStart56 710 631 bp 2 End56 721 545 bp 2 RNA expression patternBgeeHumanMouse ortholog Top expressed inright ventricleparotid glandbronchial epithelial celllower lobe of lungendothelial cellplacentaBrodmann area 23postcentral gyrusentorhinal cortexleft ventricleTop expressed inparotid glandpineal glandright lungright lung lobesubmandibular glandleft lungprimary motor cortexprefrontal cortexnucleus accumbensconjunctival fornixMore reference expression dataBioGPSMore reference expression dataGene ontologyMolecular functionbeta adrenergic receptor activity PDZ domain binding G protein coupled receptor activity epinephrine binding norepinephrine binding signal transducer activity adrenergic receptor activity protein binding alpha 2A adrenergic receptor binding protein heterodimerization activity beta1 adrenergic receptor activity G protein coupled neurotransmitter receptor activity involved in regulation of postsynaptic membrane potentialCellular componentintegral component of membrane endosome membrane plasma membrane integral component of plasma membrane early endosome Schaffer collateral CA1 synapse integral component of postsynaptic density membraneBiological processfear response adenylate cyclase activating G protein coupled receptor signaling pathway negative regulation of multicellular organism growth cell cell signaling positive regulation of cAMP mediated signaling positive regulation of heart rate by epinephrine norepinephrine activation of adenylate cyclase activity norepinephrine epinephrine mediated vasodilation involved in regulation of systemic arterial blood pressure diet induced thermogenesis adenylate cyclase activating adrenergic receptor signaling pathway positive regulation of heart contraction positive regulation of GTPase activity positive regulation of the force of heart contraction by epinephrine norepinephrine heat generation brown fat cell differentiation response to cold temperature homeostasis signal transduction G protein coupled receptor signaling pathway adenylate cyclase modulating G protein coupled receptor signaling pathway regulation of postsynaptic membrane potential positive regulation of cold induced thermogenesisSources Amigo QuickGOOrthologsSpeciesHumanMouseEntrez15311554EnsemblENSG00000043591ENSMUSG00000035283UniProtP08588P34971RefSeq mRNA NM 000684NM 007419RefSeq protein NP 000675NP 031445Location UCSC Chr 10 114 04 114 05 MbChr 19 56 71 56 72 MbPubMed search 3 4 WikidataView Edit HumanView Edit Mouse Contents 1 Historical Context 2 General Information 2 1 Structure 2 2 Function 2 2 1 Pathways 2 2 2 Summary of Interactions 2 2 3 Mechanism in cardiac myocytes 3 Clinical Significance 3 1 Familial Natural Short Sleep FNSS 3 2 Polymorphisms in ADRB 1 3 3 Pharmaceutical Interventions 3 4 Agonists 3 5 Antagonists 4 See also 5 References 6 Further reading 7 Further reading 8 External linksHistorical Context EditW B Cannon postulated that there were two chemical transmitters or sympathins while studying the sympathetic nervous system in 1933 These E and I sympathins were involved with excitatory and inhibitory responses In 1948 Raymond Ahlquist published a manuscript in the American Journal of Physiology establishing the idea of adrenaline having distinct actions on both alpha and beta receptors Shortly afterward Eli Lilly Laboratories synthesized the first beta blocker dichloroisoproterenol General Information EditStructure Edit ADRB 1 is a transmembrane protein that belongs to the G Protein Coupled Receptor GPCR family 6 7 GPCRs play a key role in cell signaling pathways and are primarily known for their seven transmembrane 7TM helices which have a cylindrical structure and span the membrane The 7TM domains have three intracellular and three extracellular loops that connect these domains to one another The extracellular loops contain sites for ligand binding on N terminus of the receptor and the intracellular loops and C terminus interact with signaling proteins such as G proteins The extracellular loops also contain several sites for post translational modification and are involved in ligand binding The third intracellular loop is the largest and contains phosphorylation sites for signaling regulation As the name suggests GPCRs are coupled to G proteins that are heterotrimeric in nature Heterotrimeric G proteins consist of three subunits alpha beta and gamma 8 Upon the binding of a ligand to the extracellular domain of the GPCR a conformational change is induced in the receptor that allows it to interact with the alpha subunit of the G protein Following this interaction the G alpha subunit exchanges GDP for GTP becomes active and dissociates from the beta and gamma subunits The free alpha subunit is then able to activate downstream signaling pathways detail more in interactions and pathway Function Edit Pathways Edit ADRB 1 is activated by the catecholamines adrenaline and noradrenaline Once these ligands bind the ADRB 1 receptor activates several different signaling pathways and interactions Some of the most well known pathways are Adenylyl Cyclase When a ligand binds to the ADRB 1 Receptor the alpha subunit of the heterotrimeric G protein gets activated which in turn activates the enzyme adenylyl cyclase Adenylyl cyclase then catalyzes the conversion of ATP to cyclic AMP cAMP which activates downstream effectors such as Protein Kinase A PKA cAMP Activation of PKA cAMP generated by adenylyl cyclase activates PKA which then phosphorylates numerous downstream targets such as ion channels other enzymes and transcription factors Beta arrestins Activation of the ADRB 1 receptor can lead to the recruitment of Beta arrestins which are used to activate signaling pathways independent of G proteins An example of an independent pathway is the MAPK mitogen activated protein kinase pathways Calcium signaling ADRB 1 signaling also activates the Gq 11 family of G proteins which is a subfamily of heterotrimeric G proteins that activates phospholipase C PLC PLC cleaves phosphatidylinositol 4 5 bisphosphate PIP2 into the second messengers inositol 1 4 5 triphosphate IP3 and diacylglycerol DAG IP3 binds to IP3 receptors on the endoplasmic reticulum which then leads to the release of calcium ions Ca2 into the cytoplasm resulting in the activation of downstream signaling pathways Summary of Interactions Edit Actions of the b1 receptor include System Effect TissueMuscular Increases cardiac output Cardiac muscleIncreases heart rate chronotropic effect Sinoatrial node SA node 9 Increases atrial contractility inotropic effect Cardiac muscleIncreases contractility and automaticity Ventricular cardiac muscle 9 Increases conduction and automaticity Atrioventricular node AV node 9 Relaxation Urinary bladder wall 10 Exocrine Releases renin Juxtaglomerular cells 9 Stimulates viscous amylase filled secretions Salivary glands 11 Other Lipolysis Adipose tissue 9 The receptor is also present in the cerebral cortex Other pathways that play ADRB 1 receptor plays an important role in Regulation of peripheral clock and central circadian clock synchronization The suprachiasmatic nucleus SCN receives light information from the eyes and synchronizes the peripheral clocks to the central circadian clock through the release of different neuropeptides and hormones 12 ADRB 1 receptors can play a role in modulating the release of neuropeptides like vasoactive intestinal peptide VIP and arginine vasopressin AVP from the SCN which can then synchronize peripheral clocks Regulation of glucose metabolism The regulation of glucose metabolism is known to be linked with ADRB 1 receptor signaling 13 The signal transduction pathway that is activated through the ADRB 1 receptor can regulate the expression of clock genes and glucose transporters The disregulation of ADRB 1 receptor signaling has been implicated in metabolic disorders such as diabetes and obesity ADRB 1 Receptor and Rhythmic Control of Immunity Circadian oscillations in catecholamine signals influence various cellular targets which express adrenergic receptors including immune cells 12 The adrenergic system regulates a range of physiological functions which are carried out through catecholamine production Humans are found to have low circulating catecholamine levels during the night and high levels during the day while rodents exhibit the opposite pattern Studies demonstrating the patterns of norepinephrine levels indicate that there is no circadian rhythmicity Circulating rhythms in epinephrine however appear to be circadian and are regulated by the HPA axis Cyclic variation in HPA signals are likely important in driving diurnal oscillations in adrenaline The most well characterized means through which adrenergic signals exert circadian control over immunity is by cell trafficking regulation Variation in the number of white blood cells seemed to be linked to adrenergic function Cardiac rhythm and Cardiac Failure The b AR signaling pathway serves as a primary component of the interface between the sympathetic nervous system and the cardiovascular system 14 The b AR pathway dysregulation has been implicated in the pathogenesis of heart failure It has been found that certain changes to b AR signaling result in reduced levels of b1 AR by up to 50 while levels of b2 AR remain constant Other intracellular changes include a significant sharp increase of GaI levels and increased bARK1 activity These changes suggest sharp decreases in b AR signaling likely due to sustained elevated levels of catecholamines Mechanism in cardiac myocytes Edit Gs exerts its effects via two pathways Firstly it directly opens L type calcium channels LTCC in the plasma membrane Secondly it renders adenylate cyclase activated resulting in an increase of cAMP activating protein kinase A PKA which in turn phosphorylates several targets such as phospholamban LTCC Troponin I TnI and potassium channels The phosphorylation of phospholamban deactivates its own function which normally inhibits SERCA on the sarcoplasmic reticulum SR in cardiac myocytes Due to this more calcium enters the SR and is therefore available for the next contraction LTCC phosphorylation increases its open probability and therefore allows more calcium to enter the myocyte upon cell depolarisation Both of these mechanisms increase the available calcium for contraction and therefore increase inotropy Conversely TnI phosphorylation results in its facilitated dissociation of calcium from troponin C TnC which speeds the muscle relaxation positive lusitropy Potassium channel phosphorylation increases its open probability which results in shorter refractory period because the cell repolarises faster also increasing lusitropy Furthermore in nodal cells such as in the SA node cAMP directly binds to and opens the HCN channels increasing their open probability which increases chronotropy 6 Clinical Significance EditFamilial Natural Short Sleep FNSS Edit A rare mutation that changes a cytosine to a thymine in the ADRB 1 coding sequence results in a protein switch to valine from alanine at amino acid position 187 A187 and leads to the FNSS behavior trait where mutation carriers naturally wake up after only 4 to 6 5 hours of sleep The ADRB 1 protein is involved in a cyclic adenosine monophosphate cAMP mediated signaling pathway and the ADRB1 A187V mutated protein leads to a lower cAMP production than the wild type protein given the same isoproterenol treatment a nonselective agonist of ADRB 1 15 It was also discovered that the mutated protein is less stable most likely due to post translational modifications as shown in an ADRB1 knockin experiment where a mutated ADRB 1 gene replaces the wild type with CRISPR technology and the protein level displays a decrease while the mRNA level remains high 15 Mice with a heterozygous ADRB1 A187V mutation show increased activity time and shorter intervals of rapid eye movement REM sleep and non REM sleep suggesting that the mutation causes short sleep In another experiment the ADRB1 A187V mutation restored REM sleep in tau mice PS19 and reduced tau accumulation which can promote brain cell damage and death in the locus coeruleus LC of PS19 mice 16 Furthermore a high expression level of ADRB 1 protein is observed in the dorsal pons DP referred to as ADRB1 neurons The activity of these ADRB1 neurons in DP is shown to be closely linked with the sleep wake behavior and altered by the ADRB1 A187V mutation The ADRB1 neurons can be either inhibitory or excitatory In the brains of mutant mice the percentage of ADRB1 neurons that may be inhibited by agonists reduces significantly while the percentage of neurons that may be excited by agonists remains relatively unchanged 15 It is thus speculated that the ADRB 1 protein has an inhibitory and an excitatory function with the inhibitory function being more sensitive to its decreased protein levels and the excitatory function being less sensitive Although the ADRB1 A187V mutation leads to lower protein levels as discussed above overall there are fewer ADRB1 neurons inhibited corresponding to the higher total activity of DP ADRB1 neurons observed in mutant mice These results collectively indicate that high activity levels in ADRB1 neurons leads to shorter sleep or FNSS Polymorphisms in ADRB 1 Edit One of the single nucleotide polymorphisms SNPs in ADRB 1 is the change from a cytosine to a guanine resulting in a protein switch from arginine 389R to glycine 389G at the 389 codon position Arginine at codon 389 is highly preserved across species and this mutation happens in the G protein binding domain of ADRB 1 one of the key functions of ADRB 1 protein so it is likely to lead to functional differences In fact this SNP causes dampened efficiency and affinity in agonist promoted receptor binding 17 Another common SNP occurs at codon position 49 with a change of serine 49S to glycine 49G in the N terminus sequence of ADRB 1 The 49S variant is shown to be more resistant to agonist promoted down regulation and short intervals of agonist exposure The receptor of the 49G variant is always expressed which results in high coupling activity with adenylyl cyclase and increased sensitivity to agonists 17 Both of these SNPs have relatively high frequencies among populations and are thought to affect cardiac functions Individuals who are homozygous for the 389R allele are more likely to have higher blood pressure and heart rates than others who have either one or two copies of the 389G allele Additionally patients with heart diseases that have a substitution of glycine for serine at codon 49 49S gt G show improved cardiac functions and decreased mortality rate 18 The cardiovascular responses induced by this polymorphism in the healthy population are also examined Healthy individuals with a glycine at codon 49 show better cardiovascular functions at rest and response to maximum heart rate during exercise evident for the cardioprotection related to this polymorphism 18 Pharmaceutical Interventions Edit Because ADRB 1 play such a critical role in maintaining blood pressure homeostasis and cardiac output many medications treat these conditions by either potentiating or inhibiting the functions of the ADRB 1 Dobutamine is one of the adrenergic drugs and agonists that selectively bind to ADRB 1 and is often used in treatments of cardiogenic shock and heart failure 19 It is also important to note the use of illicit drug for ADRB 1 since cocaine beta blocking agents or other sympathetic stimulators may cause a medical emergency Agonists Edit ADRB 1 agonists mimic or initiate a physiological response when bound to a receptor Isoprenaline has higher affinity for b1 than adrenaline which in turn binds with higher affinity than noradrenaline at physiologic concentrations As ADRB 1 increases cardiac output selective agonists clinically function as potential treatments for heart failure Selective agonists to the beta 1 receptor are Denopamine is used in the treatment of angina and has potential uses to treat congestive heart failure and pulmonary oedema Dobutamine 11 in cardiogenic shock is a beta 1 agonist that treats cardiac decompensation Xamoterol 11 cardiac stimulant acts as a partial agonist that improves heart function in studies with cardiac failure Xamoterol plays a role in modulating the sympathetic nervous system but does not have any agonistic action on beta 2 adrenergic receptors Isoproterenol is a nonselective agonist that potentiates the effects of agents like adrenaline and norepinephrine to increase heart contractility Antagonists Edit ADRB 1 antagonists are a class of drugs also referred to as Beta Blockers b1 selective antagonists are used to manage abnormal heart rhythms and block the action of substances like adrenaline on neurons allowing blood to flow more easily which lowers blood pressure and cardiac output They may also shrink vascular tumors Some examples of Beta Blockers include Acebutolol in hypertension angina pectoris and arrhythmias Atenolol 11 in hypertension coronary heart disease arrhythmias and myocardial infarction Betaxolol in hypertension and glaucoma Bisoprolol 20 in hypertension coronary heart disease arrhythmias myocardial infarction and ischemic heart diseases Esmolol in arrhythmias Metoprolol 11 in hypertension coronary heart disease myocardial infarction and heart failure Nebivolol in hypertension Vortioxetine antidepressant See also EditOther adrenergic receptors Alpha 1 adrenergic receptor Alpha 2 adrenergic receptor Beta 2 adrenergic receptor Beta 3 adrenergic receptorReferences Edit a b c GRCh38 Ensembl release 89 ENSG00000043591 Ensembl May 2017 a b c GRCm38 Ensembl release 89 ENSMUSG00000035283 Ensembl May 2017 Human PubMed Reference National Center for Biotechnology Information U S National Library of Medicine Mouse PubMed Reference National Center for Biotechnology Information U S National Library of Medicine Entrez Gene ADRB1 adrenergic beta 1 receptor a b Boron WF Boulpaep EL 2012 Medical physiology a cellular and molecular approach Updated second ed Philadelphia PA ISBN 9781437717532 OCLC 756281854 a href Template Cite book html title Template Cite book cite book a CS1 maint location missing publisher link Rosenbaum DM Rasmussen SG Kobilka BK May 2009 The structure and function of G protein coupled receptors Nature 459 7245 356 363 doi 10 1038 nature08144 PMC 3967846 PMID 19458711 Nestler Eric J Duman Ronald S 1999 Heterotrimeric G Proteins Basic Neurochemistry Molecular Cellular and Medical Aspects 6th edition a b c d e Fitzpatrick D Purves D Augustine G 2004 Table 20 2 Neuroscience Third ed Sunderland Mass Sinauer ISBN 978 0 87893 725 7 Moro C Tajouri L Chess Williams R January 2013 Adrenoceptor function and expression in bladder urothelium and lamina propria Urology 81 1 211 e1 211 e7 doi 10 1016 j urology 2012 09 011 PMID 23200975 a b c d e Rang H P 2003 Pharmacology Edinburgh Churchill Livingstone ISBN 978 0 443 07145 4 Page 163 a b Leach S Suzuki K 2020 Adrenergic Signaling in Circadian Control of Immunity Frontiers in Immunology 11 1235 doi 10 3389 fimmu 2020 01235 PMC 7344327 PMID 32714319 Jovanovic Aleksandra Xu Bing Zhu Chaoqun Ren Di Wang Hao Krause Hauch Meredith Abel E Dale Li Ji Xiang Yang K February 2023 Characterizing Adrenergic Regulation of Glucose Transporter 4 Mediated Glucose Uptake and Metabolism in the Heart JACC Basic to Translational Science S2452302X23000098 doi 10 1016 j jacbts 2022 11 008 PMC 10322917 Madamanchi A July 2007 Beta adrenergic receptor signaling in cardiac function and heart failure McGill Journal of Medicine 10 2 99 104 PMC 2323471 PMID 18523538 a b c Shi G Xing L Wu D Bhattacharyya BJ Jones CR McMahon T et al September 2019 A Rare Mutation of b1 Adrenergic Receptor Affects Sleep Wake Behaviors Neuron 103 6 1044 1055 e7 doi 10 1016 j neuron 2019 07 026 PMC 6763376 PMID 31473062 Dong Q Ptacek LJ Fu YH April 2023 Mutant b1 adrenergic receptor improves REM sleep and ameliorates tau accumulation in a mouse model of tauopathy Proceedings of the National Academy of Sciences of the United States of America 120 15 e2221686120 doi 10 1073 pnas 2221686120 PMC 10104526 PMID 37014857 S2CID 257922859 a b Sandilands AJ O Shaughnessy KM September 2005 The functional significance of genetic variation within the beta adrenoceptor British Journal of Clinical Pharmacology 60 3 235 243 doi 10 1111 j 1365 2125 2005 02438 x PMC 1884766 PMID 16120061 a b Kelley EF Snyder EM Johnson BD December 2018 Influence of Beta 1 Adrenergic Receptor Genotype on Cardiovascular Response to Exercise in Healthy Subjects Cardiology Research 9 6 343 349 doi 10 14740 cr785 PMC 6306116 PMID 30627284 Farzam Khashayar Kidron Ariel Lakhkar Anand D 2023 Adrenergic Drugs StatPearls Treasure Island FL StatPearls Publishing PMID 30480963 retrieved 2023 04 26 American Society of Health System Pharmacists Inc 2005 01 01 Bisoprolol MedlinePlus Drug Information U S National Library of Medicine National Institutes of Health Archived from the original on 2008 05 20 Retrieved 2008 06 06 Further reading EditFrielle T Kobilka B Lefkowitz RJ Caron MG July 1988 Human beta 1 and beta 2 adrenergic receptors structurally and functionally related receptors derived from distinct genes Trends in Neurosciences 11 7 321 324 doi 10 1016 0166 2236 88 90095 1 PMID 2465637 S2CID 140209236 Muszkat M August 2007 Interethnic differences in drug response the contribution of genetic variability in beta adrenergic receptor and cytochrome P4502C9 Clinical Pharmacology and Therapeutics 82 2 215 218 doi 10 1038 sj clpt 6100142 PMID 17329986 S2CID 10381767 Yang Feng TL Xue FY Zhong WW Cotecchia S Frielle T Caron MG et al February 1990 Chromosomal organization of adrenergic receptor genes Proceedings of the National Academy of Sciences of the United States of America 87 4 1516 1520 Bibcode 1990PNAS 87 1516Y doi 10 1073 pnas 87 4 1516 PMC 53506 PMID 2154750 Forse RA Leibel R Gagner M January 1989 The effect of Escherichia coli endotoxin on the adrenergic control of lipolysis in the human adipocyte The Journal of Surgical Research 46 1 41 48 doi 10 1016 0022 4804 89 90180 7 PMID 2536864 Frielle T Collins S Daniel KW Caron MG Lefkowitz RJ Kobilka BK November 1987 Cloning of the cDNA for the human beta 1 adrenergic receptor Proceedings of the National Academy of Sciences of the United States of America 84 22 7920 7924 Bibcode 1987PNAS 84 7920F doi 10 1073 pnas 84 22 7920 PMC 299447 PMID 2825170 Stiles GL Strasser RH Lavin TN Jones LR Caron MG Lefkowitz RJ July 1983 The cardiac beta adrenergic receptor Structural similarities of beta 1 and beta 2 receptor subtypes demonstrated by photoaffinity labeling The Journal of Biological Chemistry 258 13 8443 8449 doi 10 1016 S0021 9258 20 82084 5 PMID 6305985 Hoehe MR Otterud B Hsieh WT Martinez MM Stauffer D Holik J et al June 1995 Genetic mapping of adrenergic receptor genes in humans Journal of Molecular Medicine 73 6 299 306 doi 10 1007 BF00231616 PMID 7583452 S2CID 27308274 Elies R Ferrari I Wallukat G Lebesgue D Chiale P Elizari M et al November 1996 Structural and functional analysis of the B cell epitopes recognized by anti receptor autoantibodies in patients with Chagas disease Journal of Immunology 157 9 4203 4211 doi 10 4049 jimmunol 157 9 4203 PMID 8892658 S2CID 44386743 Oldenhof J Vickery R Anafi M Oak J Ray A Schoots O et al November 1998 SH3 binding domains in the dopamine D4 receptor Biochemistry 37 45 15726 15736 doi 10 1021 bi981634 PMID 9843378 Mason DA Moore JD Green SA Liggett SB April 1999 A gain of function polymorphism in a G protein coupling domain of the human beta1 adrenergic receptor The Journal of Biological Chemistry 274 18 12670 12674 doi 10 1074 jbc 274 18 12670 PMID 10212248 Moore JD Mason DA Green SA Hsu J Liggett SB September 1999 Racial differences in the frequencies of cardiac beta 1 adrenergic receptor polymorphisms analysis of c145A gt G and c1165G gt C Human Mutation 14 3 271 doi 10 1002 SICI 1098 1004 1999 14 3 lt 271 AID HUMU14 gt 3 0 CO 2 Q PMID 10477438 S2CID 8860722 Tang Y Hu LA Miller WE Ringstad N Hall RA Pitcher JA et al October 1999 Identification of the endophilins SH3p4 p8 p13 as novel binding partners for the beta1 adrenergic receptor Proceedings of the National Academy of Sciences of the United States of America 96 22 12559 12564 Bibcode 1999PNAS 9612559T doi 10 1073 pnas 96 22 12559 PMC 22990 PMID 10535961 Podlowski S Wenzel K Luther HP Muller J Bramlage P Baumann G et al 2000 Beta1 adrenoceptor gene variations a role in idiopathic dilated cardiomyopathy Journal of Molecular Medicine 78 2 87 93 doi 10 1007 s001090000080 PMID 10794544 S2CID 1072602 Shiina T Kawasaki A Nagao T Kurose H September 2000 Interaction with beta arrestin determines the difference in internalization behavor between beta1 and beta2 adrenergic receptors The Journal of Biological Chemistry 275 37 29082 29090 doi 10 1074 jbc M909757199 PMID 10862778 Hu LA Tang Y Miller WE Cong M Lau AG Lefkowitz RJ Hall RA December 2000 beta 1 adrenergic receptor association with PSD 95 Inhibition of receptor internalization and facilitation of beta 1 adrenergic receptor interaction with N methyl D aspartate receptors The Journal of Biological Chemistry 275 49 38659 38666 doi 10 1074 jbc M005938200 PMID 10995758 Borjesson M Magnusson Y Hjalmarson A Andersson B November 2000 A novel polymorphism in the gene coding for the beta 1 adrenergic receptor associated with survival in patients with heart failure European Heart Journal 21 22 1853 1858 doi 10 1053 euhj 1999 1994 PMID 11052857 Xu J Paquet M Lau AG Wood JD Ross CA Hall RA November 2001 beta 1 adrenergic receptor association with the synaptic scaffolding protein membrane associated guanylate kinase inverted 2 MAGI 2 Differential regulation of receptor internalization by MAGI 2 and PSD 95 The Journal of Biological Chemistry 276 44 41310 41317 doi 10 1074 jbc M107480200 PMID 11526121 Hu LA Chen W Premont RT Cong M Lefkowitz RJ January 2002 G protein coupled receptor kinase 5 regulates beta 1 adrenergic receptor association with PSD 95 The Journal of Biological Chemistry 277 2 1607 1613 doi 10 1074 jbc M107297200 PMID 11700307 Ranade K Jorgenson E Sheu WH Pei D Hsiung CA Chiang FT et al April 2002 A polymorphism in the beta1 adrenergic receptor is associated with resting heart rate American Journal of Human Genetics 70 4 935 942 doi 10 1086 339621 PMC 379121 PMID 11854867 Further reading EditAlhayek S Preuss CV August 2022 Beta 1 Receptors StatPearls Internet Treasure Island FL StatPearls Publishing PMID 30422499 External links EditHuman ADRB1 genome location and ADRB1 gene details page in the UCSC Genome Browser b1 adrenoceptor IUPHAR Database of Receptors and Ion Channels International Union of Basic and Clinical Pharmacology Overview of all the structural information available in the PDB for UniProt P08588 Beta 1 adrenergic receptor at the PDBe KB Retrieved from https en wikipedia org w index php title Beta 1 adrenergic receptor amp oldid 1170234057, wikipedia, wiki, book, books, library,

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