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Calcitonin gene-related peptide

January 01, 1970

Calcitonin gene-related peptide (CGRP) is a member of the calcitonin family of peptides consisting of calcitonin, amylin, adrenomedullin, adrenomedullin 2 (intermedin) and calcitonin‑receptor‑stimulating peptide. Calcitonin is mainly produced by thyroid C cells whilst CGRP is secreted and stored in the nervous system.[1] This peptide, in humans, exists in two forms: CGRP alpha (α-CGRP or CGRP I), and CGRP beta (β-CGRP or CGRP II).[2] α-CGRP is a 37-amino acid neuropeptide and is formed by alternative splicing[3] of the calcitonin/CGRP gene located on chromosome 11. β-CGRP is less studied. In humans, β-CGRP differs from α-CGRP by three amino acids and is encoded in a separate, nearby gene.[4] The CGRP family includes calcitonin (CT), adrenomedullin (AM), and amylin (AMY).[5]

Calcitonin-related polypeptide alpha
Human calcitonin (black) bound to the calcitonin receptor. PDB: 7TYO
Identifiers
SymbolCALCA
Alt. symbolsCALC1
NCBI gene796
HGNC1437
OMIM114130
RefSeqNM_001741
UniProtP06881
Other data
LocusChr. 11 p15.2{{{LocusSupplementaryData}}}
Search for
StructuresSwiss-model
DomainsInterPro
Calcitonin-related polypeptide, beta
Identifiers
SymbolCALCB
Alt. symbolsCALC2
NCBI gene797
HGNC1438
OMIM114160
RefSeqNM_000728
UniProtP10092
Other data
LocusChr. 11 p15.2{{{LocusSupplementaryData}}}
Search for
StructuresSwiss-model
DomainsInterPro

Function edit

CGRP is produced in both peripheral and central neurons.[6] It is a potent peptide vasodilator and can function in the transmission of nociception.[7][8] In the spinal cord, the function and expression of CGRP may differ depending on the location of synthesis. CGRP is derived mainly from the cell bodies of motor neurons when synthesized in the ventral horn of the spinal cord and may contribute to the regeneration of nervous tissue after injury. Conversely, CGRP is derived from dorsal root ganglion when synthesized in the dorsal horn of the spinal cord and may be linked to the transmission of pain.[9] In the trigeminal vascular system, the cell bodies of the trigeminal ganglion are the main source of CGRP. CGRP is thought to play a role in cardiovascular homeostasis and nociception. In the heart, CGRP acts as a chronotrope by increasing heart rate.[10]: 202  Apart from these attributes, CGRP is known to modulate the autonomic nervous system and plays a role in ingestion.[10]: 201–204 

CGRP has moderate effects on calcium homeostasis compared to its extensive actions in other areas, such as the autonomic nervous system.

Appetite edit

As a neuropeptide, CGRP acts as an appetite suppressant and contributes to gastric acid secretion.[10] It also functions in temperature homeostasis, increases heart rate, and plays a role in the release of the pituitary hormones in a paracrine manner.[10] Because of these characteristics, it has been said that CGRP functions more as a neurotransmitter than a hormone.[10]

Stem cell mobilization edit

CGRP has a role in human stem cell mobilization. In investigations carried out during last five years, treatment with CGRP resulted in significantly increased CGRP levels in the bone marrow extracellular fluid and substantially increased the number of HSCs mobilized by G-CSF.[11] The results performed on different experiments by the same research group led to the conclusion that G-CSF-induced HSC mobilization is regulated by the nociceptor nerve-derived neuropeptide CGRP. This peptide exerts its effect on HSC mobilization via the RAMP1 pathway.[11]

Receptors edit

 
Structure of the human calcitonin recptor-Gs complex. The calcitonin transmembrane receptor (blue) is bound to human calcitonin (red) and the Gs complex (yellow). PDB: 7TYO

CGRP mediates its effects through a heteromeric receptor composed of a G protein-coupled receptor called calcitonin receptor-like receptor (CALCRL) and a receptor activity-modifying protein (RAMP1).[12] CGRP receptors are found throughout all the body, suggesting that the protein may modulate a variety of physiological functions in all major systems (e.g., respiratory, endocrine, gastrointestinal, immune, and cardiovascular).[13] The extracellular loop number 2 is fundamental for ligand induced activation, with key interactions of R274/Y278/D280/W283.[14]

Regulation edit

Regulation of the calcitonin gene-related peptide (CGRP) gene is in part controlled by the expression of the mitogen-activated protein kinases (MAPK) signaling pathway,[15] cytokines such as TNFα[16] and iNOS.[17]

5HT1 receptor agonists, such as sumatriptan, increase intracellular calcium, which cause decreases in CGRP promoter activity.[15]

CGRP receptor is found in myelinated A-fibers axon which is required for ligand specificity and function of the receptor. The CGRP receptor has three subunits: receptor activity-modifying protein 1 (RAMP1), calcitonin-like receptor (CLR) and receptor component protein (RCP).[18] The complex central receptor is the G protein-coupled receptor calcitonin receptor-like receptor (CALCRL) which is necessary for CGRP and adrenomedullin (AM receptors). For function CGRP, CALCRL must coincide with RAMP1 where the ligand-binding domain of CGRP is located. It also includes two cytoplasmic proteins that associate with the CALCRL-RAMP1 to form signal transduction. CALCRL contains the Gα subunit, which activates adenylyl cyclase and cAMP-dependent signaling pathways. Receptor-mediated transduction elevates in intracellular cAMP activate protein kinase A, which results in the phosphorylation of multiple targets, including potassium- sensitive ATP channels (KATP channels), extracellular signal-related kinases and transcription factors such as cAMP-responsive element-binding protein (CREB). In smooth muscle of neurovascular region, the elevation of cAMP upon CGRP activation results in vasodilation of the blood vessel. Chronic exposure to CGRP causes degradation of lysosomes.[19]

Research edit

Further information: Calcitonin gene-related peptide receptor antagonist

Increased levels of CGRP have been reported in migraine and temporomandibular joint disorder patients as well as a variety of other diseases such as cardiac failure, hypertension, and sepsis.[20][21][22][23][24][25][26]

There is mounting evidence to suggest that CGRP may be beneficial in preventing the development of hypertension and cardiovascular pathologies associated with hypertension.[2] Prophylactic therapy with calcitonin gene‐related peptides (CGRPs) may have unknown fertility consequences for women of child bearing age. This is of particular concern, as females (16.6%) are more genetically predisposed to migraine than are males (7.5%).[27]

Preclinical evidence suggests that, during a migraine, activated primary sensory neurons (meningeal nociceptors) in the trigeminal ganglion release CGRP from their peripherally projecting nerve endings located within the meninges.[28][26] This CGRP then binds to and activates CGRP receptors located around meningeal vessels, causing vasodilation, mast cell degranulation, and plasma extravasation.[13][28][29][30] Human observations have further implicated the role of CGRP in the pathophysiology of migraine. Activation of primary sensory neurons in the trigeminal vascular system in humans can cause the release of CGRP. During some migraine attacks, increased concentrations of CGRP can be found in both saliva and in plasma drawn from the external jugular vein.[13][28][29][30] Furthermore, intravenous administration of alpha-CGRP is able to induce headache in individuals susceptible to migraine.[31][26]

Medicines edit

New medicines are now on the market that contain antibodies against either CGRP itself, or its receptor. They are called monoclonal antibodies (MABs) and are large molecules that do not cross the blood-brain-barrier.[32] They typically are not metabolized by the liver and have little direct impact on the metabolism of more conventional small-molecule drugs.[33] They also tend to have relatively long half-lives in the body, but must be given parenterally (preferably by injection) due to very poor absorption from the digestive tract.[34] They have been proved to be effective in people who experience migraine headaches, both with and without aura, and both episodic and chronic cluster headache. These are the first class of preventive medications originally designed and approved for people with migraine.[26] Monoclonal means all the antibodies are made from the same genetic material, although different MABs may derive from different sources, e.g. from hamster ovarian cells, from yeast cells or from humanized cell cultures. The antibodies are also made repeatedly to make them all identical, which results in difficult and relatively expensive production lines. Antibodies are proteins that counter or interfere with very specific parts of another protein or the site where a protein is supposed to bind to the receptor. Most commonly thought of in being used to prevent or fight off infections.[35]

The first approved by the FDA is called erenumab (trade name Aimovig), produced by pharmaceutical company Amgen and Novartis. It interacts with the CGRP receptor. It is injected once monthly with a dose of 70 or 140 mg. Few adverse effects were reported (most related to injection site reactions) and patients had a significant reduction in migraines.[36][37]

The second approved by the FDA is called fremanezumab (trade name Ajovy), produced by the Teva pharmaceutical company. It interacts with the CGRP protein, whose expression is related to migraine attacks. It may be administered monthly or every three months, giving options for users. Trials have shown a reduction of greater than 50% of migraine days for those who responded. There were few significant side effects during trials, most related to injection site reactions.[38][39]

The third approved by the FDA is called galcanezumab (trade name Emgality), produced by the Eli Lilly Company. It interacts with the CGRP protein, whose expression is related to migraine attacks. It is injected once a month, after the first month having a double dose. The main side effects are injection site reactions.[40][41]

Approved by the FDA in February 2020, ubrogepant (Ubrelvy) is an oral medication manufactured by Allergan.

Also FDA approved in February 2020, eptinezumab (Vyepti), is an intravenous migraine prophylactic medication manufactured by Lundbeck.

The phytocannabinoids delta-9 tetrahydrocannabinol (Δ9-THC) and its oxidative byproduct cannabinol (CBN) are found to induce a CB1 and CB2 cannabinoid receptor-independent release of calcitonin gene-related peptide from capsaicin-sensitive perivascular sensory nerves, an action other psychotropic cannabinoids cannot do.[42][43]

References edit

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External links edit

January 01, 1970
calcitonin, gene, related, peptide, cgrp, member, calcitonin, family, peptides, consisting, calcitonin, amylin, adrenomedullin, adrenomedullin, intermedin, calcitonin, receptor, stimulating, peptide, calcitonin, mainly, produced, thyroid, cells, whilst, cgrp, . Calcitonin gene related peptide CGRP is a member of the calcitonin family of peptides consisting of calcitonin amylin adrenomedullin adrenomedullin 2 intermedin and calcitonin receptor stimulating peptide Calcitonin is mainly produced by thyroid C cells whilst CGRP is secreted and stored in the nervous system 1 This peptide in humans exists in two forms CGRP alpha a CGRP or CGRP I and CGRP beta b CGRP or CGRP II 2 a CGRP is a 37 amino acid neuropeptide and is formed by alternative splicing 3 of the calcitonin CGRP gene located on chromosome 11 b CGRP is less studied In humans b CGRP differs from a CGRP by three amino acids and is encoded in a separate nearby gene 4 The CGRP family includes calcitonin CT adrenomedullin AM and amylin AMY 5 Calcitonin related polypeptide alphaHuman calcitonin black bound to the calcitonin receptor PDB 7TYO IdentifiersSymbolCALCAAlt symbolsCALC1NCBI gene796HGNC1437OMIM114130RefSeqNM 001741UniProtP06881Other dataLocusChr 11 p15 2 LocusSupplementaryData Search forStructuresSwiss modelDomainsInterPro Calcitonin related polypeptide betaIdentifiersSymbolCALCBAlt symbolsCALC2NCBI gene797HGNC1438OMIM114160RefSeqNM 000728UniProtP10092Other dataLocusChr 11 p15 2 LocusSupplementaryData Search forStructuresSwiss modelDomainsInterPro Contents 1 Function 1 1 Appetite 1 2 Stem cell mobilization 2 Receptors 3 Regulation 4 Research 5 Medicines 6 References 7 External linksFunction editCGRP is produced in both peripheral and central neurons 6 It is a potent peptide vasodilator and can function in the transmission of nociception 7 8 In the spinal cord the function and expression of CGRP may differ depending on the location of synthesis CGRP is derived mainly from the cell bodies of motor neurons when synthesized in the ventral horn of the spinal cord and may contribute to the regeneration of nervous tissue after injury Conversely CGRP is derived from dorsal root ganglion when synthesized in the dorsal horn of the spinal cord and may be linked to the transmission of pain 9 In the trigeminal vascular system the cell bodies of the trigeminal ganglion are the main source of CGRP CGRP is thought to play a role in cardiovascular homeostasis and nociception In the heart CGRP acts as a chronotrope by increasing heart rate 10 202 Apart from these attributes CGRP is known to modulate the autonomic nervous system and plays a role in ingestion 10 201 204 CGRP has moderate effects on calcium homeostasis compared to its extensive actions in other areas such as the autonomic nervous system Appetite edit As a neuropeptide CGRP acts as an appetite suppressant and contributes to gastric acid secretion 10 It also functions in temperature homeostasis increases heart rate and plays a role in the release of the pituitary hormones in a paracrine manner 10 Because of these characteristics it has been said that CGRP functions more as a neurotransmitter than a hormone 10 Stem cell mobilization edit CGRP has a role in human stem cell mobilization In investigations carried out during last five years treatment with CGRP resulted in significantly increased CGRP levels in the bone marrow extracellular fluid and substantially increased the number of HSCs mobilized by G CSF 11 The results performed on different experiments by the same research group led to the conclusion that G CSF induced HSC mobilization is regulated by the nociceptor nerve derived neuropeptide CGRP This peptide exerts its effect on HSC mobilization via the RAMP1 pathway 11 Receptors edit nbsp Structure of the human calcitonin recptor Gs complex The calcitonin transmembrane receptor blue is bound to human calcitonin red and the Gs complex yellow PDB 7TYO CGRP mediates its effects through a heteromeric receptor composed of a G protein coupled receptor called calcitonin receptor like receptor CALCRL and a receptor activity modifying protein RAMP1 12 CGRP receptors are found throughout all the body suggesting that the protein may modulate a variety of physiological functions in all major systems e g respiratory endocrine gastrointestinal immune and cardiovascular 13 The extracellular loop number 2 is fundamental for ligand induced activation with key interactions of R274 Y278 D280 W283 14 Regulation editRegulation of the calcitonin gene related peptide CGRP gene is in part controlled by the expression of the mitogen activated protein kinases MAPK signaling pathway 15 cytokines such as TNFa 16 and iNOS 17 5HT1 receptor agonists such as sumatriptan increase intracellular calcium which cause decreases in CGRP promoter activity 15 CGRP receptor is found in myelinated A fibers axon which is required for ligand specificity and function of the receptor The CGRP receptor has three subunits receptor activity modifying protein 1 RAMP1 calcitonin like receptor CLR and receptor component protein RCP 18 The complex central receptor is the G protein coupled receptor calcitonin receptor like receptor CALCRL which is necessary for CGRP and adrenomedullin AM receptors For function CGRP CALCRL must coincide with RAMP1 where the ligand binding domain of CGRP is located It also includes two cytoplasmic proteins that associate with the CALCRL RAMP1 to form signal transduction CALCRL contains the Ga subunit which activates adenylyl cyclase and cAMP dependent signaling pathways Receptor mediated transduction elevates in intracellular cAMP activate protein kinase A which results in the phosphorylation of multiple targets including potassium sensitive ATP channels KATP channels extracellular signal related kinases and transcription factors such as cAMP responsive element binding protein CREB In smooth muscle of neurovascular region the elevation of cAMP upon CGRP activation results in vasodilation of the blood vessel Chronic exposure to CGRP causes degradation of lysosomes 19 Research editFurther information Calcitonin gene related peptide receptor antagonist This section relies excessively on references to primary sources Please improve this section by adding secondary or tertiary sources Find sources Calcitonin gene related peptide news newspapers books scholar JSTOR February 2018 Learn how and when to remove this message This section needs to be updated Please help update this article to reflect recent events or newly available information February 2018 Increased levels of CGRP have been reported in migraine and temporomandibular joint disorder patients as well as a variety of other diseases such as cardiac failure hypertension and sepsis 20 21 22 23 24 25 26 There is mounting evidence to suggest that CGRP may be beneficial in preventing the development of hypertension and cardiovascular pathologies associated with hypertension 2 Prophylactic therapy with calcitonin gene related peptides CGRPs may have unknown fertility consequences for women of child bearing age This is of particular concern as females 16 6 are more genetically predisposed to migraine than are males 7 5 27 Preclinical evidence suggests that during a migraine activated primary sensory neurons meningeal nociceptors in the trigeminal ganglion release CGRP from their peripherally projecting nerve endings located within the meninges 28 26 This CGRP then binds to and activates CGRP receptors located around meningeal vessels causing vasodilation mast cell degranulation and plasma extravasation 13 28 29 30 Human observations have further implicated the role of CGRP in the pathophysiology of migraine Activation of primary sensory neurons in the trigeminal vascular system in humans can cause the release of CGRP During some migraine attacks increased concentrations of CGRP can be found in both saliva and in plasma drawn from the external jugular vein 13 28 29 30 Furthermore intravenous administration of alpha CGRP is able to induce headache in individuals susceptible to migraine 31 26 Medicines editNew medicines are now on the market that contain antibodies against either CGRP itself or its receptor They are called monoclonal antibodies MABs and are large molecules that do not cross the blood brain barrier 32 They typically are not metabolized by the liver and have little direct impact on the metabolism of more conventional small molecule drugs 33 They also tend to have relatively long half lives in the body but must be given parenterally preferably by injection due to very poor absorption from the digestive tract 34 They have been proved to be effective in people who experience migraine headaches both with and without aura and both episodic and chronic cluster headache These are the first class of preventive medications originally designed and approved for people with migraine 26 Monoclonal means all the antibodies are made from the same genetic material although different MABs may derive from different sources e g from hamster ovarian cells from yeast cells or from humanized cell cultures The antibodies are also made repeatedly to make them all identical which results in difficult and relatively expensive production lines Antibodies are proteins that counter or interfere with very specific parts of another protein or the site where a protein is supposed to bind to the receptor Most commonly thought of in being used to prevent or fight off infections 35 The first approved by the FDA is called erenumab trade name Aimovig produced by pharmaceutical company Amgen and Novartis It interacts with the CGRP receptor It is injected once monthly with a dose of 70 or 140 mg Few adverse effects were reported most related to injection site reactions and patients had a significant reduction in migraines 36 37 The second approved by the FDA is called fremanezumab trade name Ajovy produced by the Teva pharmaceutical company It interacts with the CGRP protein whose expression is related to migraine attacks It may be administered monthly or every three months giving options for users Trials have shown a reduction of greater than 50 of migraine days for those who responded There were few significant side effects during trials most related to injection site reactions 38 39 The third approved by the FDA is called galcanezumab trade name Emgality produced by the Eli Lilly Company It interacts with the CGRP protein whose expression is related to migraine attacks It is injected once a month after the first month having a double dose The main side effects are injection site reactions 40 41 Approved by the FDA in February 2020 ubrogepant Ubrelvy is an oral medication manufactured by Allergan Also FDA approved in February 2020 eptinezumab Vyepti is an intravenous migraine prophylactic medication manufactured by Lundbeck The phytocannabinoids delta 9 tetrahydrocannabinol D9 THC and its oxidative byproduct cannabinol CBN are found to induce a CB1 and CB2 cannabinoid receptor independent release of calcitonin gene related peptide from capsaicin sensitive perivascular sensory nerves an action other psychotropic cannabinoids cannot do 42 43 References edit Jia S Zhang SJ Wang XD Yang ZH Sun YN Gupta A et al August 2019 Calcitonin gene related peptide enhances osteogenic differentiation and recruitment of bone marrow mesenchymal stem cells in rats Experimental and Therapeutic Medicine 18 2 1039 1046 doi 10 3892 etm 2019 7659 PMC 6601389 PMID 31316600 a b Russell FA King R Smillie SJ Kodji X Brain SD October 2014 Calcitonin gene related peptide physiology and pathophysiology Physiological Reviews 94 4 1099 142 doi 10 1152 physrev 00034 2013 PMC 4187032 PMID 25287861 Amara SG Jonas V Rosenfeld MG Ong ES Evans RM July 1982 Alternative RNA processing in calcitonin gene expression generates mRNAs encoding different polypeptide products Nature 298 5871 240 4 Bibcode 1982Natur 298 240A doi 10 1038 298240a0 PMID 6283379 S2CID 24188834 Rezaeian AH Isokane T Nishibori M Chiba M Hiraiwa N Yoshizawa M Yasue H October 2009 alphaCGRP and betaCGRP transcript amount in mouse tissues of various developmental stages and their tissue expression sites Brain amp Development 31 9 682 93 doi 10 1016 j braindev 2008 10 011 PMID 19062206 S2CID 21635386 Edvinsson L May 2017 The Trigeminovascular Pathway Role of CGRP and CGRP Receptors in Migraine Headache 57 Suppl 2 S2 47 55 doi 10 1111 head 13081 PMID 28485848 Rosenfeld MG Mermod JJ Amara SG Swanson LW Sawchenko PE Rivier J et al 1983 Production of a novel neuropeptide encoded by the calcitonin gene via tissue specific RNA processing Nature 304 5922 129 35 Bibcode 1983Natur 304 129R doi 10 1038 304129a0 PMID 6346105 S2CID 4322278 Brain SD Williams TJ Tippins JR Morris HR MacIntyre I 1985 Calcitonin gene related peptide is a potent vasodilator Nature 313 5997 54 6 Bibcode 1985Natur 313 54B doi 10 1038 313054a0 PMID 3917554 S2CID 4329128 McCulloch J Uddman R Kingman TA Edvinsson L August 1986 Calcitonin gene related peptide functional role in cerebrovascular regulation Proceedings of the National Academy of Sciences of the United States of America 83 15 5731 5 Bibcode 1986PNAS 83 5731M doi 10 1073 pnas 83 15 5731 PMC 386363 PMID 3488550 Chen LJ Zhang FG Li J Song HX Zhou LB Yao BC et al January 2010 Expression of calcitonin gene related peptide in anterior and posterior horns of the spinal cord after brachial plexus injury Journal of Clinical Neuroscience 17 1 87 91 doi 10 1016 j jocn 2009 03 042 PMID 19969463 S2CID 29249307 a b c d e Norman A Henry H Litwack G 2014 Hormones Amsterdam Elsevier ISBN 978 0 12 369444 7 a b Gao X Zhang D Xu C Li H Caron KM Frenette PS January 2021 Nociceptive nerves regulate haematopoietic stem cell mobilization Nature 589 7843 591 596 Bibcode 2021Natur 589 591G doi 10 1038 s41586 020 03057 y PMC 7856173 PMID 33361809 Poyner DR Sexton PM Marshall I Smith DM Quirion R Born W et al June 2002 International Union of Pharmacology XXXII The mammalian calcitonin gene related peptides adrenomedullin amylin and calcitonin receptors Pharmacological Reviews 54 2 233 46 doi 10 1124 pr 54 2 233 PMID 12037140 S2CID 17302944 a b c Arulmani U Maassenvandenbrink A Villalon CM Saxena PR October 2004 Calcitonin gene related peptide and its role in migraine pathophysiology European Journal of Pharmacology 500 1 3 315 30 doi 10 1016 j ejphar 2004 07 035 PMID 15464043 Woolley MJ Simms J Mobarec JC Reynolds CA Poyner DR Conner AC October 2017 Understanding the molecular functions of the second extracellular loop ECL2 of the calcitonin gene related peptide CGRP receptor using a comprehensive mutagenesis approach PDF Molecular and Cellular Endocrinology 454 39 49 doi 10 1016 j mce 2017 05 034 PMID 28572046 S2CID 13779528 a b Durham PL Russo AF February 2003 Stimulation of the calcitonin gene related peptide enhancer by mitogen activated protein kinases and repression by an antimigraine drug in trigeminal ganglia neurons The Journal of Neuroscience 23 3 807 15 doi 10 1523 JNEUROSCI 23 03 00807 2003 PMC 6741928 PMID 12574409 Schafers M Svensson CI Sommer C Sorkin LS April 2003 Tumor necrosis factor alpha induces mechanical allodynia after spinal nerve ligation by activation of p38 MAPK in primary sensory neurons The Journal of Neuroscience 23 7 2517 21 doi 10 1523 JNEUROSCI 23 07 02517 2003 PMC 6742090 PMID 12684435 Li J Vause CV Durham PL February 2008 Calcitonin gene related peptide stimulation of nitric oxide synthesis and release from trigeminal ganglion glial cells Brain Research 1196 22 32 doi 10 1016 j brainres 2007 12 028 PMC 2268710 PMID 18221935 Deen M Correnti E Kamm K Kelderman T Papetti L Rubio Beltran E et al September 2017 Blocking CGRP in migraine patients a review of pros and cons The Journal of Headache and Pain 18 1 96 doi 10 1186 s10194 017 0807 1 PMC 5612904 PMID 28948500 Edvinsson L Haanes KA Warfvinge K Krause DN June 2018 CGRP as the target of new migraine therapies successful translation from bench to clinic Nature Reviews Neurology 14 6 338 350 doi 10 1038 s41582 018 0003 1 PMID 29691490 S2CID 13810025 Buzzi MG Bonamini M Moskowitz MA 1995 Neurogenic model of migraine Cephalalgia 15 4 277 80 doi 10 1046 j 1468 2982 1995 1504277 x PMID 7585923 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AJMC com Retrieved 23 February 2019 Lattanzi S Brigo F Trinka E Vernieri F Corradetti T Dobran M Silvestrini M March 2019 Erenumab for Preventive Treatment of Migraine A Systematic Review and Meta Analysis of Efficacy and Safety Drugs 79 4 417 431 doi 10 1007 s40265 019 01069 1 PMID 30793254 S2CID 67790108 FDA Approves Second Anti CGRP Treatment for Migraines American Migraine Foundation Retrieved 23 February 2019 Bigal ME Rapoport AM Silberstein SD Walter S Hargreaves RJ Aycardi E November 2018 From LBR 101 to Fremanezumab for Migraine CNS Drugs 32 11 1025 1037 doi 10 1007 s40263 018 0579 4 PMID 30311143 S2CID 52962394 Lilly s Emgality galcanezumab gnlm Receives U S FDA Approval for the Preventive Treatment of Migraine in Adults Lilly Retrieved 23 February 2019 Lamb YN November 2018 Galcanezumab First Global Approval Drugs 78 16 1769 1775 doi 10 1007 s40265 018 1002 7 PMID 30378008 S2CID 53107438 Degradants Formed During Phytocannabinoid Processing www caymanchem com Retrieved 2023 05 10 Zygmunt PM Andersson DA Hogestatt ED June 2002 D9 Tetrahydrocannabinol and Cannabinol Activate Capsaicin Sensitive Sensory Nerves via a CB1 and CB2 Cannabinoid Receptor Independent Mechanism The Journal of Neuroscience 22 11 4720 7 doi 10 1523 JNEUROSCI 22 11 04720 2002 PMC 6758782 PMID 12040079 External links editCalcitonin Gene Related Peptide at the U S National Library of Medicine Medical Subject Headings MeSH Retrieved from https en wikipedia org w index php title Calcitonin gene related peptide amp oldid 1221494467, wikipedia, wiki, book, books, library,

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