Homotaurine: Difference between revisions
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| verifiedrevid = 415530375 |
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| Reference =<ref> |
| Reference = <ref>{{cite web | url = http://www.sigmaaldrich.com/catalog/search/ProductDetail/ALDRICH/A76109 | title = Homotaurine | publisher = [[Sigma-Aldrich]]}}</ref> |
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| ImageFile_Ref = {{chemboximage|correct|??}} |
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| ImageFile = Homotaurine.svg |
| ImageFile = Homotaurine.svg |
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| ImageFile1 = Homotaurine-3D-balls.png |
| ImageFile1 = Homotaurine-3D-balls.png |
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| ImageAlt1 = Ball-and-stick model |
| ImageAlt1 = Ball-and-stick model |
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| PIN = 3-Aminopropane-1-sulfonic acid |
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| OtherNames =Tramiprosate; Alzhemed; 3-APS |
| OtherNames = Tramiprosate; Alzhemed; 3-APS |
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|Section1={{Chembox Identifiers |
|Section1={{Chembox Identifiers |
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⚫ | |||
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| ChEBI = 1457 |
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| ChemSpiderID_Ref = {{chemspidercite|correct|chemspider}} |
| ChemSpiderID_Ref = {{chemspidercite|correct|chemspider}} |
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| ChemSpiderID = 1584 |
| ChemSpiderID = 1584 |
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| DrugBank = DB06527 |
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| EC_number = 222-977-4 |
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| KEGG_Ref = {{keggcite|correct|kegg}} |
| KEGG_Ref = {{keggcite|correct|kegg}} |
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| KEGG = D06202 |
| KEGG = D06202 |
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| UNII_Ref = {{fdacite|correct|FDA}} |
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| UNII = 5K8EAX0G53 |
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| InChI = 1/C3H9NO3S/c4-2-1-3-8(5,6)7/h1-4H2,(H,5,6,7) |
| InChI = 1/C3H9NO3S/c4-2-1-3-8(5,6)7/h1-4H2,(H,5,6,7) |
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| InChIKey = SNKZJIOFVMKAOJ-UHFFFAOYAT |
| InChIKey = SNKZJIOFVMKAOJ-UHFFFAOYAT |
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| StdInChI_Ref = {{stdinchicite|correct|chemspider}} |
| StdInChI_Ref = {{stdinchicite|correct|chemspider}} |
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| StdInChI = 1S/C3H9NO3S/c4-2-1-3-8(5,6)7/h1-4H2,(H,5,6,7) |
| StdInChI = 1S/C3H9NO3S/c4-2-1-3-8(5,6)7/h1-4H2,(H,5,6,7) |
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| StdInChIKey_Ref = {{stdinchicite|correct|chemspider}} |
| StdInChIKey_Ref = {{stdinchicite|correct|chemspider}} |
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| StdInChIKey = SNKZJIOFVMKAOJ-UHFFFAOYSA-N |
| StdInChIKey = SNKZJIOFVMKAOJ-UHFFFAOYSA-N |
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| SMILES = O=S(=O)(O)CCCN |
| SMILES = O=S(=O)(O)CCCN |
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}} |
}} |
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|Section2={{Chembox Properties |
|Section2={{Chembox Properties |
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| C=3 | H=9 | N=1 | O=3 | S=1 |
| C=3 | H=9 | N=1 | O=3 | S=1 |
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| FlashPt = |
| FlashPt = |
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| AutoignitionPt = |
| AutoignitionPt = |
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| GHS_ref=<ref>{{cite web |title=Tramiprosate |url=https://pubchem.ncbi.nlm.nih.gov/compound/1646#section=Safety-and-Hazards |website=pubchem.ncbi.nlm.nih.gov |access-date=13 December 2021 |language=en}}</ref> |
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| RPhrases ={{R36/37/38}} |
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| GHSPictograms = {{GHS07}} |
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| GHSSignalWord = Warning |
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| HPhrases = {{H-phrases|315|319|335}} |
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| PPhrases = {{P-phrases|261|264|271|280|302+352|304+340|305+351+338|312|321|332+313|337+313|362|403+233|405|501}} |
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}} |
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'''Homotaurine''' ('''3-amino-1-propanesulfonic acid''' |
'''Homotaurine''' (also known as '''tramiprosate''' ([[International Nonproprietary Name|INN]]), '''3-amino-1-propanesulfonic acid''', or '''3-APS''') is a natural sulfonic acid found in seaweed.<ref>{{cite journal |last1=Martorana |first1=Alessandro |last2=Di Lorenzo |first2=Francesco |last3=Manenti |first3=Guglielmo |last4=Semprini |first4=Roberta |last5=Koch |first5=Giacomo |title=Homotaurine Induces Measurable Changes of Short Latency Afferent Inhibition in a Group of Mild Cognitive Impairment Individuals |journal=Frontiers in Aging Neuroscience |date=23 September 2014 |volume=6 |page=254 |doi=10.3389/fnagi.2014.00254 |pmid=25295005 |pmc=4172065 |doi-access=free }}</ref> It is analogous to [[taurine]], but with an extra carbon in its chain. It has [[GABAergic]] activity, apparently by mimicking GABA, which it resembles.<ref name=OrgChem2007/> |
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Homotaurine was investigated in a [[Phase III clinical trials|Phase III]] clinical trial as a potential treatment for [[Alzheimer's disease]] (AD) that did not show efficacy. However, post-hoc analyses have shown positive and significant effects of homotaurine on secondary endpoints and subgroups of patients, including a reduction in hippocampal volume loss and lower decline in memory function in the overall cohort, as well as a reduction in global cognitive decline in APOE4 allele carriers, suggesting a [[Disease-modifying treatment|disease-modifying effect]].<ref name=AD2012rev>{{cite journal |last1=Caltagirone |first1=C |last2=Ferrannini |first2=L |last3=Marchionni |first3=N |last4=Nappi |first4=G |last5=Scapagnini |first5=G |last6=Trabucchi |first6=M |title=The potential protective effect of tramiprosate (homotaurine) against Alzheimer's disease: a review |journal=Aging Clinical and Experimental Research |date=December 2012 |volume=24 |issue=6 |pages=580–587 |doi=10.3275/8585 |pmid=22961121 |s2cid=10816430 }}</ref> A study in cognitive impairment done in 2018 did show positive benefits.<ref>{{cite journal |last1=Martorana |first1=A. |last2=Motta |first2=C |last3=Koch |first3=G. |last4=Massaia |first4=M. |last5=Mondino |first5=S. |last6=Raniero |first6=I. |last7=Vacca |first7=A. |last8=Di Lorenzo |first8=F. |last9=Cavallo |first9=G. |last10=Oddenino |first10=E. |last11=Pavanelli |first11=E. |last12=Maniscalco |first12=M. |last13=Montano |first13=V. |last14=Mastropietro |first14=A. |last15=Bellia |first15=N. C. |last16=Ciravegna |first16=E. |last17=La Rocca |first17=M. |last18=Vitale |first18=E. |last19=Lorico |first19=F. |last20=Zacchettin |first20=B. |last21=Scalise |first21=A. |last22=Codemo |first22=A. |last23=Gabelli |first23=C. |last24=Spano |first24=M. |last25=Poli |first25=S. |last26=Panuccio |first26=D. |last27=Bruno |first27=P. |last28=Alfieri |first28=P. |last29=Ruggiero |first29=R. |last30=Cursi |first30=F. |last31=Levi Della Vida |first31=G. |title=Effect of homotaurine in patients with cognitive impairment: results from an Italian observational retrospective study |journal=Journal of Gerontology and Geriatrics |date=15 March 2018 |volume=66 |pages=15–20 |url=http://www.jgerontology-geriatrics.com/article/view/97 }}</ref> |
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In a phase 2 study Homotaurine reduced Abeta(42) levels a type of amyloid beta (Abeta), a toxic protein known to aggregate, leading to amyloid plaque deposition in the brain.<ref name=pmid17082468>{{cite journal |doi=10.1212/01.wnl.0000244346.08950.64 |pmid=17082468 |title=A Phase II study targeting amyloid- with 3APS in mild-to-moderate Alzheimer disease |journal=Neurology |volume=67 |issue=10 |pages=1757 |year=2006 |last1=Aisen |first1=P. S |last2=Saumier |first2=D |last3=Briand |first3=R |last4=Laurin |first4=J |last5=Gervais |first5=F |last6=Tremblay |first6=P |last7=Garceau |first7=D }}</ref> |
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Homotaurine is currently in a phase 3 study with expected FDA approval as the first disease modifying drug for AD.<ref name="Tolar et al 2020">{{cite journal |last1=Tolar |first1=Martin |last2=Abushakra |first2=Susan |last3=Hey |first3=John A. |last4=Porsteinsson |first4=Anton |last5=Sabbagh |first5=Marwan |title=Aducanumab, gantenerumab, BAN2401, and ALZ-801—the first wave of amyloid-targeting drugs for Alzheimer's disease with potential for near term approval |journal=Alzheimer's Research & Therapy |date=December 2020 |volume=12 |issue=1 |pages=95 |doi=10.1186/s13195-020-00663-w |pmid=32787971 |pmc=7424995 |doi-access=free }}</ref><ref>{{cite journal |last1=Abushakra |first1=S. |last2=Porsteinsson |first2=A. |last3=Scheltens |first3=P. |last4=Sadowsky |first4=C. |last5=Vellas |first5=B. |last6=Cummings |first6=J. |last7=Gauthier |first7=S. |last8=Hey |first8=J. A. |last9=Power |first9=A. |last10=Wang |first10=P. |last11=Tolar |first11=M. |last12=Tolar |first12=M |title=Clinical effects of tramiprosate in apoe4/4 homozygous patients with mild alzheimer's disease suggest disease modification potential |journal=Journal of Prevention of Alzheimer's Disease |date=1 September 2017 |volume=4 |issue=3 |pages=149–156 |doi=10.14283/jpad.2017.26 |pmid=29182706 |s2cid=44515548 |doi-access=free }}</ref> |
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In 2012 Homotaurine was investigated in a [[Phase III]] clinical trial as a potential treatment for [[Alzheimer's disease]] that did not show efficacy in its primary endpoints but did show positive and significant effects of homotaurine on secondary endpoints and subgroups of patients, including a reduction in hippocampal volume loss and lower decline in memory function in the overall cohort, as well as a reduction in global cognitive decline in APOE4 allele carriers, suggesting a disease-modifying effects.<ref name=pmid22961121>{{cite journal |doi=10.3275/8585 }}</ref> |
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==Medical use== |
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October 24, 2017 The FDA Granted Fast Track Designation to Alzheon’s ALZ-801 Development Program for the Treatment of Alzheimer’s Disease. <ref>https://alzheon.com/fda-grants-fast-track-designation-to-alzheons-alz-801-development-program-for-the-treatment-of-alzheimers-disease/{{full}}</ref> |
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[[Acamprosate]] (''N''-acetyl homotaurine) was approved by the FDA in 2004 to treat [[alcohol dependence]].<ref name=OrgChem2007>{{cite book | last1 = Lednicer | first1 = Daniel | name-list-style = vanc | title = The Organic Chemistry of Drug Synthesis | date = 2008 | publisher = John Wiley & Sons | location = Hoboken | isbn = 978-0-470-18066-2 | edition = 7th | url = https://books.google.com/books?id=N6OAhuiHqiIC&pg=PA15 | page = 15 }}</ref> |
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In 2018 a new phase 3 study for genetically-defined subpopulation of high risk patients who are homozygous for the ε4 allele of apolipoprotein E (APOE4/4 homozygotes) at the Mild stage of AD has been filed with the FDA under the name ALZ-801 by the drug company Alzheon.<ref>https://alzheon.com/{{full}}</ref><ref>https://www.iadvanceseniorcare.com/article/alzheon-goes-public-fund-alzheimers-drug{{full}}</ref> |
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It is approved by Canada's FDA to sell as a dietary supplement.<ref>http://www.canadadrugcenter.com/Health-Canada-Approves-VIVIMIND.asp{{full}}</ref> |
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It is approved in Israel as a dietary supplement.<ref>http://www.levpharm.com/site/flash/flashDetail.asp?flash_id=1124719{{full}}</ref> |
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==Biochemical properties== |
==Biochemical properties== |
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In preclinical studies it had been found to bind to soluble [[amyloid beta]] and inhibit the formation of neurotoxic aggregates.<ref name= |
In preclinical studies it had been found to bind to soluble [[amyloid beta]] and inhibit the formation of neurotoxic aggregates.<ref name=AD2012rev/><ref name="pmid17908052">{{cite journal |last1=Aisen |first1=Paul |last2=Gauthier |first2=Serge |last3=Vellas |first3=Bruno |last4=Briand |first4=Richard |last5=Saumier |first5=Daniel |last6=Laurin |first6=Julie |last7=Garceau |first7=Denis |title=Alzhemed: A Potential Treatment for Alzheimers Disease |journal=Current Alzheimer Research |date=1 September 2007 |volume=4 |issue=4 |pages=473–478 |doi=10.2174/156720507781788882 |pmid=17908052 }}</ref> Homotaurine has also shown [[anticonvulsant]] activities, reduction in skeletal [[muscle tonus]], and [[hypothermic]] activity.<ref name=Metabolism2013/> |
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⚫ | Homotaurine has been reported as a [[GABA]] antagonist<ref name=OrgChem2007/> as well as a GABA agonist.<ref name=Metabolism2013> |
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One study suggests Homotaurine increases dopamine levels.<ref name=pmid9871492>{{cite journal |doi=10.1007/BF01345285 |pmid=9871492 |title=Locally infused taurine, GABA and homotaurine alter differently the striatal extracellular concentrations of dopamine and its metabolites in rats |journal=Amino Acids |volume=15 |issue=1–2 |pages=117–34 |year=1998 |last1=Ruotsalainen |first1=M |last2=Majasaari |first2=M |last3=Salim�Ki |first3=J |last4=Ahtee |first4=L }}</ref> |
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⚫ | Homotaurine has been reported as a [[GABA]] antagonist,<ref name=OrgChem2007/> as well as a GABA agonist.<ref name=Metabolism2013>{{cite book |last1=Lajtha |first1=Abel |title=Metabolism in the Nervous System |date=2013 |publisher=Springer Science & Business Media |isbn=978-1-4684-4367-7 |page=520 |url=https://books.google.com/books?id=du_TBwAAQBAJ&pg=PA520 }}</ref><ref name=PharmPrinc2011>{{cite book |last1=Tashjian |first1=Armen H. |last2=Armstrong |first2=Ehrin J. |title=Principles of Pharmacology: The Pathophysiologic Basis of Drug Therapy |date=2011 |publisher=Lippincott Williams & Wilkins |isbn=978-1-4511-1805-6 |page=308 |url=https://books.google.com/books?id=kjCCMZHInigC&pg=PA308 }}</ref> ''[[In vitro]]'' studies have found that homotaurine is a [[GABAA receptor|GABA<sub>A</sub>]] partial agonist<ref>{{cite journal |last1=Reyes-Haro |first1=Daniel |last2=Cabrera-Ruíz |first2=Elizabeth |last3=Estrada-Mondragón |first3=Argel |last4=Miledi |first4=Ricardo |last5=Martínez-Torres |first5=Ataúlfo |title=Modulation of GABA-A receptors of astrocytes and STC-1 cells by taurine structural analogs |journal=Amino Acids |date=November 2014 |volume=46 |issue=11 |pages=2587–2593 |doi=10.1007/s00726-014-1813-0 |pmid=25119985 |s2cid=10319072 }}</ref> as well as a [[GABAB receptor|GABA<sub>B</sub>]] receptor partial agonist with low efficacy, becoming an antagonist and displacing the full agonists GABA and [[baclofen]] at this receptor.<ref>{{cite journal |last1=Giotti |first1=A. |last2=Luzzi |first2=S. |last3=Spagnesi |first3=S. |last4=Zilletti |first4=L. |title=Homotaurine: a GABAB antagonist in guinea-pig ileum. |journal=British Journal of Pharmacology |date=August 1983 |volume=79 |issue=4 |pages=855–862 |doi=10.1111/j.1476-5381.1983.tb10529.x |pmid=6652358 |pmc=2044932 }}</ref> In a study in rats, homotaurine reversed the [[catatonia]] induced by [[baclofen]] (the prototypical GABA<sub>B</sub> agonist),<ref>{{cite journal |last1=Mehta |first1=A |last2=Ticku |first2=M |title=Baclofen induces catatonia in rats |journal=Neuropharmacology |date=September 1987 |volume=26 |issue=9 |pages=1419–1423 |doi=10.1016/0028-3908(87)90108-0 |pmid=2823166 |s2cid=24010833 }}</ref> and was able to produce analgesia via the GABA<sub>B</sub> receptor, an effect that was abolished when [[CGP-35348]], a GABA<sub>B</sub> receptor antagonist was applied.<ref>{{cite journal |last1=Serrano |first1=M.Isabel |last2=Serrano |first2=Jose S. |last3=Fernández |first3=Ana |last4=Asadi |first4=Ihklas |last5=Serrano-Martino |first5=M.Carmen |title=GABAB Receptors and Opioid Mechanisms Involved in Homotaurine-Induced Analgesia |journal=General Pharmacology: The Vascular System |date=March 1998 |volume=30 |issue=3 |pages=411–415 |doi=10.1016/s0306-3623(97)00279-6 |pmid=9510095 }}</ref><ref>{{cite journal |last1=Serrano |first1=Maria Isabel |last2=Serrano |first2=Jose S. |last3=Asadi |first3=Ikhlas |last4=Fernandez |first4=Ana |last5=Serrano-Martino |first5=Maria Carmen |title=Role of K+-channels in homotaurine-induced analgesia |journal=Fundamental and Clinical Pharmacology |date=16 June 2001 |volume=15 |issue=3 |pages=167–173 |doi=10.1046/j.1472-8206.2001.00026.x |pmid=11468027 |s2cid=19694376 }}</ref> |
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⚫ | One study in rats showed that homotaurine suppressed ethanol-stimulated dopamine release, as well as ethanol intake and preference in rats in a way similar to the ''N''-acetyl [[derivative (chemistry)|derivative]] of homotaurine, [[acamprosate]].<ref |
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In a human study homotaurine selectively and fully inhibits the formation of Aβ42 oligomers at the clinical dose, without evidence of vasogenic edema.<ref name="Tolar et al 2020"/> |
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Homotaurine has shown pain relieving effects in animal studies that may involve the opioid receptors.<ref name=pmid9510095/> |
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⚫ | One study in rats showed that homotaurine suppressed ethanol-stimulated dopamine release, as well as ethanol intake and preference in rats in a way similar to the ''N''-acetyl [[derivative (chemistry)|derivative]] of homotaurine, [[acamprosate]].<ref>{{cite journal |last1=Olive |first1=M.Foster |last2=Nannini |first2=Michelle A |last3=Ou |first3=Christine J |last4=Koenig |first4=Heather N |last5=Hodge |first5=Clyde W |title=Effects of acute acamprosate and homotaurine on ethanol intake and ethanol-stimulated mesolimbic dopamine release |journal=European Journal of Pharmacology |date=February 2002 |volume=437 |issue=1–2 |pages=55–61 |doi=10.1016/s0014-2999(02)01272-4 |pmid=11864639 }}</ref> |
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==See also== |
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*[[Acamprosate]] – a derivative of homotaurine |
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*[[Teprosilic acid]] |
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== References == |
== References == |
Latest revision as of 19:21, 6 August 2024
Names | |
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Preferred IUPAC name
3-Aminopropane-1-sulfonic acid | |
Other names
Tramiprosate; Alzhemed; 3-APS
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Identifiers | |
3D model (JSmol)
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ChEBI | |
ChEMBL | |
ChemSpider | |
DrugBank | |
ECHA InfoCard | 100.020.889 |
EC Number |
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KEGG | |
PubChem CID
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UNII | |
CompTox Dashboard (EPA)
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Properties | |
C3H9NO3S | |
Molar mass | 139.17 g·mol−1 |
Melting point | 293 °C (559 °F; 566 K) (decomposition) |
Hazards | |
GHS labelling:[2] | |
Warning | |
H315, H319, H335 | |
P261, P264, P271, P280, P302+P352, P304+P340, P305+P351+P338, P312, P321, P332+P313, P337+P313, P362, P403+P233, P405, P501 | |
Except where otherwise noted, data are given for materials in their standard state (at 25 °C [77 °F], 100 kPa).
|
Homotaurine (also known as tramiprosate (INN), 3-amino-1-propanesulfonic acid, or 3-APS) is a natural sulfonic acid found in seaweed.[3] It is analogous to taurine, but with an extra carbon in its chain. It has GABAergic activity, apparently by mimicking GABA, which it resembles.[4]
Homotaurine was investigated in a Phase III clinical trial as a potential treatment for Alzheimer's disease (AD) that did not show efficacy. However, post-hoc analyses have shown positive and significant effects of homotaurine on secondary endpoints and subgroups of patients, including a reduction in hippocampal volume loss and lower decline in memory function in the overall cohort, as well as a reduction in global cognitive decline in APOE4 allele carriers, suggesting a disease-modifying effect.[5] A study in cognitive impairment done in 2018 did show positive benefits.[6]
Homotaurine is currently in a phase 3 study with expected FDA approval as the first disease modifying drug for AD.[7][8]
Medical use
[edit]Acamprosate (N-acetyl homotaurine) was approved by the FDA in 2004 to treat alcohol dependence.[4]
Biochemical properties
[edit]In preclinical studies it had been found to bind to soluble amyloid beta and inhibit the formation of neurotoxic aggregates.[5][9] Homotaurine has also shown anticonvulsant activities, reduction in skeletal muscle tonus, and hypothermic activity.[10]
Homotaurine has been reported as a GABA antagonist,[4] as well as a GABA agonist.[10][11] In vitro studies have found that homotaurine is a GABAA partial agonist[12] as well as a GABAB receptor partial agonist with low efficacy, becoming an antagonist and displacing the full agonists GABA and baclofen at this receptor.[13] In a study in rats, homotaurine reversed the catatonia induced by baclofen (the prototypical GABAB agonist),[14] and was able to produce analgesia via the GABAB receptor, an effect that was abolished when CGP-35348, a GABAB receptor antagonist was applied.[15][16]
In a human study homotaurine selectively and fully inhibits the formation of Aβ42 oligomers at the clinical dose, without evidence of vasogenic edema.[7]
One study in rats showed that homotaurine suppressed ethanol-stimulated dopamine release, as well as ethanol intake and preference in rats in a way similar to the N-acetyl derivative of homotaurine, acamprosate.[17]
References
[edit]- ^ "Homotaurine". Sigma-Aldrich.
- ^ "Tramiprosate". pubchem.ncbi.nlm.nih.gov. Retrieved 13 December 2021.
- ^ Martorana, Alessandro; Di Lorenzo, Francesco; Manenti, Guglielmo; Semprini, Roberta; Koch, Giacomo (23 September 2014). "Homotaurine Induces Measurable Changes of Short Latency Afferent Inhibition in a Group of Mild Cognitive Impairment Individuals". Frontiers in Aging Neuroscience. 6: 254. doi:10.3389/fnagi.2014.00254. PMC 4172065. PMID 25295005.
- ^ a b c Lednicer D (2008). The Organic Chemistry of Drug Synthesis (7th ed.). Hoboken: John Wiley & Sons. p. 15. ISBN 978-0-470-18066-2.
- ^ a b Caltagirone, C; Ferrannini, L; Marchionni, N; Nappi, G; Scapagnini, G; Trabucchi, M (December 2012). "The potential protective effect of tramiprosate (homotaurine) against Alzheimer's disease: a review". Aging Clinical and Experimental Research. 24 (6): 580–587. doi:10.3275/8585. PMID 22961121. S2CID 10816430.
- ^ Martorana, A.; Motta, C; Koch, G.; Massaia, M.; Mondino, S.; Raniero, I.; Vacca, A.; Di Lorenzo, F.; Cavallo, G.; Oddenino, E.; Pavanelli, E.; Maniscalco, M.; Montano, V.; Mastropietro, A.; Bellia, N. C.; Ciravegna, E.; La Rocca, M.; Vitale, E.; Lorico, F.; Zacchettin, B.; Scalise, A.; Codemo, A.; Gabelli, C.; Spano, M.; Poli, S.; Panuccio, D.; Bruno, P.; Alfieri, P.; Ruggiero, R.; Cursi, F.; Levi Della Vida, G. (15 March 2018). "Effect of homotaurine in patients with cognitive impairment: results from an Italian observational retrospective study". Journal of Gerontology and Geriatrics. 66: 15–20.
- ^ a b Tolar, Martin; Abushakra, Susan; Hey, John A.; Porsteinsson, Anton; Sabbagh, Marwan (December 2020). "Aducanumab, gantenerumab, BAN2401, and ALZ-801—the first wave of amyloid-targeting drugs for Alzheimer's disease with potential for near term approval". Alzheimer's Research & Therapy. 12 (1): 95. doi:10.1186/s13195-020-00663-w. PMC 7424995. PMID 32787971.
- ^ Abushakra, S.; Porsteinsson, A.; Scheltens, P.; Sadowsky, C.; Vellas, B.; Cummings, J.; Gauthier, S.; Hey, J. A.; Power, A.; Wang, P.; Tolar, M.; Tolar, M (1 September 2017). "Clinical effects of tramiprosate in apoe4/4 homozygous patients with mild alzheimer's disease suggest disease modification potential". Journal of Prevention of Alzheimer's Disease. 4 (3): 149–156. doi:10.14283/jpad.2017.26. PMID 29182706. S2CID 44515548.
- ^ Aisen, Paul; Gauthier, Serge; Vellas, Bruno; Briand, Richard; Saumier, Daniel; Laurin, Julie; Garceau, Denis (1 September 2007). "Alzhemed: A Potential Treatment for Alzheimers Disease". Current Alzheimer Research. 4 (4): 473–478. doi:10.2174/156720507781788882. PMID 17908052.
- ^ a b Lajtha, Abel (2013). Metabolism in the Nervous System. Springer Science & Business Media. p. 520. ISBN 978-1-4684-4367-7.
- ^ Tashjian, Armen H.; Armstrong, Ehrin J. (2011). Principles of Pharmacology: The Pathophysiologic Basis of Drug Therapy. Lippincott Williams & Wilkins. p. 308. ISBN 978-1-4511-1805-6.
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