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Cycloserine

April 13, 2024

This article is about the tuberculosis medicine. For the nerve agent, see Cyclosarin.

Cycloserine, sold under the brand name Seromycin, is a GABA transaminase inhibitor and an antibiotic, used to treat tuberculosis.[1][2] Specifically it is used, along with other antituberculosis medications, for active drug resistant tuberculosis.[2] It is given by mouth.[2]

Cycloserine
Clinical data
Trade namesSeromycin
Other namesD-cycloserine, 4-amino-3-isoxazolidinone
AHFS/Drugs.comMonograph
License data
ATC code
Legal status
Legal status
Pharmacokinetic data
Bioavailability~70% to 90%
MetabolismLiver
Elimination half-life10 hrs (normal kidney function)
ExcretionKidney
Identifiers
  • (R)-4-Amino-1,2-oxazolidin-3-one
CAS Number
  • 68-41-7 Y
PubChem CID
  • 6234
DrugBank
  • DB00260 Y
ChemSpider
  • 5998 Y
UNII
  • 95IK5KI84Z
KEGG
  • D00877 Y
ChEBI
  • CHEBI:40009 Y
ChEMBL
  • ChEMBL771 Y
NIAID ChemDB
  • 007654
CompTox Dashboard (EPA)
  • DTXSID8022870
ECHA InfoCard100.000.626
Chemical and physical data
FormulaC3H6N2O2
Molar mass102.093 g·mol−1
3D model (JSmol)
  • Interactive image
Melting point155 to 156 °C (311 to 313 °F) (dec.)
  • O=C1NOC[C@H]1N
  • InChI=1S/C3H6N2O2/c4-2-1-7-5-3(2)6/h2H,1,4H2,(H,5,6)/t2-/m1/s1 Y
  • Key:DYDCUQKUCUHJBH-UWTATZPHSA-N Y
  (verify)

Common side effects include allergic reactions, seizures, sleepiness, unsteadiness, and numbness.[2] It is not recommended in people who have kidney failure, epilepsy, depression, or are alcoholics.[2] It is unclear if use during pregnancy is safe for the baby.[2] Cycloserine is similar in structure to the amino acid D-alanine and works by interfering with the formation of the bacteria's cell wall.[2]

Cycloserine was discovered in 1954 from a type of Streptomyces.[3] It is on the World Health Organization's List of Essential Medicines.[4]

Medical uses edit

Tuberculosis edit

For the treatment of tuberculosis, cycloserine is classified as a second-line drug. Its use is only considered if one or more first-line drugs cannot be used. Hence, cycloserine is restricted for use only against multiple drug-resistant and extensively drug-resistant strains of M. tuberculosis. Another reason for limited use of this drug is the neurological side effects it causes, since it is able to penetrate into the central nervous system (CNS) and cause headaches, drowsiness, depression, dizziness, vertigo, confusion, paresthesias, dysarthria, hyperirritability, psychosis, convulsions, and shaking (tremors).[5][6] Overdose of cycloserine may result in paresis, seizures, and coma, while alcohol consumption may increase the risk of seizures.[6] Coadministration of pyridoxine can reduce the incidence of some of these CNS side effects (e.g. convulsions) caused by cycloserine.[citation needed]

Psychiatry edit

A 2015 Cochrane review found no evidence of benefit in anxiety disorders as of 2015.[7] Another review found preliminary evidence of benefit.[8] Evidence for use in addiction is tentative but also unclear.[9]

Mechanism of action edit

Cycloserine works as an antibiotic by inhibiting cell-wall biosynthesis in bacteria.[10][11] As a cyclic analogue of D-alanine, cycloserine acts against two crucial enzymes important in the cytosolic stages of peptidoglycan synthesis: alanine racemase (Alr) and D-alanine:D-alanine ligase (Ddl).[11] The first enzyme is a pyridoxal 5'-phosphate-dependent enzyme which converts the L-alanine to the D-alanine form.[11] The second enzyme is involved in joining two of these D-alanine residues together by catalyzing the formation of the ATP-dependent D-alanine-D-alanine dipeptide bond between the resulting D-alanine molecules.[11] If both of these enzymes are inhibited, then D-alanine residues cannot form and previously formed D-alanine molecules cannot be joined.[11] This effectively leads to inhibition of peptidoglycan synthesis.[11]

Psychiatric use is suggested based on partial NMDA receptor agonism, which improves neural plasticity in lab animals. The degree of clinical usefulness is, as aforementioned, very unclear and still being explored.[8]

Chemical properties edit

Under mildly acidic conditions, cycloserine hydrolyzes to give hydroxylamine and D-serine.[12][13] Cycloserine can be conceptualized as a cyclized version of serine, with an oxidative loss of dihydrogen to form the nitrogen-oxygen bond.[citation needed]

Cycloserine is stable under basic conditions, with the greatest stability at pH = 11.5.[12]

Synthesis edit

Initial approaches to synthesize the compound was first published in 1955, when the Stammer group produced a racemic synthesis from DL‐β‐aminoxyalanine ethyl ester. In 1957, Platter et al. managed to synthesis the pure D-enantiomer by cyclizing the corresponding α‐amino‐β‐chlorohydroxamic acids. Chemical synthesis of the compound was revolutionized in the 2010s, when several approaches starting with the cheap D-serine (mirror form of normal L-serine) were published by different groups.[14]

The biosynthesis of the compound is defined by a ten-gene cluster. L-serine and L-arginine are converted to O-ureido-L-serine, flipped to O-ureido-D-serine, then turned into the final compound by cyclization. In 2013, Uda et al. successfully used recombinant versions of three enzymes in the cluster to produce the compound.[15]

A 1963 patent describes industrial production of the drug by bacterial fermentation.[16] It is unclear what process is used in the 21st century, fermentation, or chemical synthesis.[citation needed]

History edit

The compound was first isolated nearly simultaneously by two teams. Workers at Merck isolated the compound, which they called oxamycin, from a species of Streptomyces.[17] The same team prepared the molecule synthetically.[18] Workers at Eli Lilly isolated the compound from strains of Streptomyces orchidaceus. It was shown to hydrolyze to serine and hydroxylamine.[19]

Economics edit

In the U.S., the price of cycloserine increased from $500 for 30 pills to $10,800 in 2015 after the Chao Center for Industrial Pharmacy and Contract Manufacturing changed ownership to Rodelis Therapeutics in August 2015.[20]

The price increase was rescinded after the previous owner, the Purdue University Research Foundation, which retained "oversight of the manufacturing operation" intervened and Rodelis returned the drug to an NGO of Purdue University. The foundation now will charge $1,050 for 30 capsules, twice what it charged before". Eli Lilly has been criticised for not ensuring that the philanthropic initiative continued. Due to US antitrust laws, however, no company may control the price of a product after it is outlicensed.[21]

In 2015, the cost in the United States was increased to US$3,150 a month and then decreased to US$1,050 per month.[21]

Research edit

Some experimental evidence suggests that D-cycloserine aids in learning by helping form stronger neural connections.[22] It has been investigated as an aid to facilitate exposure therapy in people with PTSD and anxiety disorders,[23][24][25] and treatment with schizophrenia.[26] In a clinical trial, a course of D-cycloserine combined with a single dose of ketamine was investigated for treatment resistant bipolar depression. When administered for 8 weeks after a ketamine infusion, cycloserine appeared to potentiate the antidepressant effects in all trial participants.[27] However, a 2019 clinical trial showed no statistically significant difference between the D-cycloserine and placebo groups when it came to maintaining the antidepressant effect of a single ketamine infusion. The authors suggest several possible explanations for this nonsignificance, namely the inclusion of high-risk or severely treatment-resistant participants as well as a possible confounding carryover effect from the ketamine infusion phase. Although the results point to D-cycloserine having a stronger antisuicidal effect than placebo, the authors caution that this difference might be attributed to the placebo group feeling worse than the D-cycloserine feeling better.[28] A combination drug, cycloserine/lurasidone, containing D-cycloserine and the atypical antipsychotic lurasidone is being developed for acute suicidal ideation/behavior.[29]

References edit

  1. ^ Polc P, Pieri L, Bonetti EP, Scherschlicht R, Moehler H, Kettler R, et al. (April 1986). "L-cycloserine: behavioural and biochemical effects after single and repeated administration to mice, rats and cats". Neuropharmacology. 25 (4). Elsevier BV: 411–418. doi:10.1016/0028-3908(86)90236-4. PMID 3012401. S2CID 462885.
  2. ^ a b c d e f g "Cycloserine". The American Society of Health-System Pharmacists. from the original on 20 December 2016. Retrieved 8 December 2016.
  3. ^ Gottlieb D, Shaw PD (2012). Mechanism of Action. Springer Science & Business Media. p. 41. ISBN 9783642460517. from the original on 2016-12-20.
  4. ^ World Health Organization (2019). World Health Organization model list of essential medicines: 21st list 2019. Geneva: World Health Organization. hdl:10665/325771. WHO/MVP/EMP/IAU/2019.06. License: CC BY-NC-SA 3.0 IGO.
  5. ^ Nitsche MA, Jaussi W, Liebetanz D, Lang N, Tergau F, Paulus W (August 2004). "Consolidation of human motor cortical neuroplasticity by D-cycloserine" (PDF). Neuropsychopharmacology. 29 (8): 1573–8. doi:10.1038/sj.npp.1300517. PMID 15199378.
  6. ^ a b "CYCLOSERINE: Human Health Effects". National Institutes of Health. from the original on 2014-04-16.
  7. ^ Ori R, Amos T, Bergman H, Soares-Weiser K, Ipser JC, Stein DJ (May 2015). "Augmentation of cognitive and behavioural therapies (CBT) with d-cycloserine for anxiety and related disorders". The Cochrane Database of Systematic Reviews. 2015 (5): CD007803. doi:10.1002/14651858.CD007803.pub2. PMC 8939046. PMID 25957940.
  8. ^ a b Schade S, Paulus W (April 2016). "D-Cycloserine in Neuropsychiatric Diseases: A Systematic Review". The International Journal of Neuropsychopharmacology. 19 (4): pyv102. doi:10.1093/ijnp/pyv102. PMC 4851259. PMID 26364274.
  9. ^ Myers KM, Carlezon WA (June 2012). "D-cycloserine effects on extinction of conditioned responses to drug-related cues". Biological Psychiatry. 71 (11): 947–55. doi:10.1016/j.biopsych.2012.02.030. PMC 4001849. PMID 22579305.
  10. ^ Lambert MP, Neuhaus FC (June 1972). "Mechanism of D-cycloserine action: alanine racemase from Escherichia coli W". Journal of Bacteriology. 110 (3): 978–87. doi:10.1128/JB.110.3.978-987.1972. PMC 247518. PMID 4555420.
  11. ^ a b c d e f Prosser GA, de Carvalho LP (February 2013). "Kinetic mechanism and inhibition of Mycobacterium tuberculosis D-alanine:D-alanine ligase by the antibiotic D-cycloserine". The FEBS Journal. 280 (4): 1150–66. doi:10.1111/febs.12108. PMID 23286234. S2CID 22305408.
  12. ^ a b Kaushal G, Ramirez R, Alambo D, Taupradist W, Choksi K, Sirbu C (October 2011). "Initial characterization of D-cycloserine for future formulation development for anxiety disorders". Drug Discoveries & Therapeutics. 5 (5): 253–60. doi:10.5582/ddt.2011.v5.5.253. PMID 22466372.
  13. ^ Silverman R (1998). "An Aromatization Mechanism of Inactivation of γ-Aminobutyric Acid Aminotransferase for the Antibiotic l-Cycloserine". Journal of the American Chemical Society. 120 (10): 2256–2267. doi:10.1021/ja972907b.
  14. ^ Holt GR (6 December 2021). "Principles of plastic surgery of congenital facial abnormalities". Facial Plastic Surgery. 3 (3): 147–154. doi:10.1002/cmdc.202100503. PMC 9293202. PMID 3459696.
  15. ^ Uda N, Matoba Y, Kumagai T, Oda K, Noda M, Sugiyama M (June 2013). "Establishment of an in vitro D-cycloserine-synthesizing system by using O-ureido-L-serine synthase and D-cycloserine synthetase found in the biosynthetic pathway". Antimicrobial Agents and Chemotherapy. 57 (6): 2603–2612. doi:10.1128/AAC.02291-12. PMC 3716191. PMID 23529730.
  16. ^ Harned RL (21 May 1963). "US3090730A Process for the production of cycloserine". Google Patents.
  17. ^ Kuehl Jr FA, Wolf FJ, Trenner NR, Peck RL, Buhs RP, Howe E, et al. (1955). "D-4-Amino-3-isoxazolidinone, a new antibiotic". Journal of the American Chemical Society. 77 (8): 2344–5. doi:10.1021/ja01613a105.
  18. ^ Hidy PH, Hodge EB, Young VV, Harned RL, Brewer GA, Phillips WF, et al. (1955). "Synthesis of D-4-amino-3-isoxazolidinone". Journal of the American Chemical Society. 77 (8): 2346–7. doi:10.1021/ja01613a107.
  19. ^ Hidy PH, Hodge EB, Young VV, Harned RL, Brewer GA, Phillips WF, et al. (1955). "Structure and reactions of cycloserine". Journal of the American Chemical Society. 77 (8): 2345–6. doi:10.1021/ja01613a106.
  20. ^ Pollack A (20 September 2015). "Drug Goes From $13.50 a Tablet to $750, Overnight". The New York Times. from the original on 25 September 2015. Retrieved 21 September 2015.
  21. ^ a b Pollack A (21 September 2015). "Big Price Increase for Tuberculosis Drug Is Rescinded". NYT. from the original on 26 September 2015. Retrieved 24 September 2015.
  22. ^ "Learning and Brain Activity Are Boosted by a Dose of a Small-Molecule Compound". Scientific American. from the original on 2015-12-23.
  23. ^ Bowers ME, Ressler KJ (September 2015). "An Overview of Translationally Informed Treatments for Posttraumatic Stress Disorder: Animal Models of Pavlovian Fear Conditioning to Human Clinical Trials". Biological Psychiatry. 78 (5): E15-27. doi:10.1016/j.biopsych.2015.06.008. PMC 4527085. PMID 26238379.
  24. ^ Hofmann SG, Wu QJ, Boettcher H (May 2013). "D-cycloserine as an augmentation strategy for cognitive behavioral therapy for anxiety disorders". Biology of Mood & Anxiety Disorders. 3 (1): 11. doi:10.1186/2045-5380-3-11. PMC 3686620. PMID 23768232.
  25. ^ Singewald N, Schmuckermair C, Whittle N, Holmes A, Ressler KJ (May 2015). "Pharmacology of cognitive enhancers for exposure-based therapy of fear, anxiety and trauma-related disorders". Pharmacology & Therapeutics. 149: 150–90. doi:10.1016/j.pharmthera.2014.12.004. PMC 4380664. PMID 25550231.
  26. ^ Goff DC (September 2012). "D-cycloserine: an evolving role in learning and neuroplasticity in schizophrenia". Schizophrenia Bulletin. 38 (5): 936–41. doi:10.1093/schbul/sbs012. PMC 3446239. PMID 22368237.
  27. ^ Kantrowitz J, Halberstam B, Gangwisch J (June 2015). "Single-Dose Ketamine Followed by Daily d-Cycloserine in Treatment-Resistant Bipolar Depression". The Journal of Clinical Psychiatry. 76 (6): 737–738. doi:10.4088/JCP.14l09527. PMID 26132675.
  28. ^ Chen MH, Cheng CM, Gueorguieva R, Lin WC, Li CT, Hong CJ, et al. (November 2019). "Maintenance of antidepressant and antisuicidal effects by D-cycloserine among patients with treatment-resistant depression who responded to low-dose ketamine infusion: a double-blind randomized placebo-control study". Neuropsychopharmacology. 44 (12). Springer Nature (published 2019-08-17): 2112–2118. doi:10.1038/s41386-019-0480-y. PMC 6898334. PMID 31421635. S2CID 201057546.
  29. ^ . Archived from the original on 2020-07-09. Retrieved 2023-10-22.

April 13, 2024
cycloserine, this, article, about, tuberculosis, medicine, nerve, agent, cyclosarin, sold, under, brand, name, seromycin, gaba, transaminase, inhibitor, antibiotic, used, treat, tuberculosis, specifically, used, along, with, other, antituberculosis, medication. This article is about the tuberculosis medicine For the nerve agent see Cyclosarin Cycloserine sold under the brand name Seromycin is a GABA transaminase inhibitor and an antibiotic used to treat tuberculosis 1 2 Specifically it is used along with other antituberculosis medications for active drug resistant tuberculosis 2 It is given by mouth 2 CycloserineClinical dataTrade namesSeromycinOther namesD cycloserine 4 amino 3 isoxazolidinoneAHFS Drugs comMonographLicense dataUS DailyMed SeromycinATC codeJ04AB01 WHO Legal statusLegal statusUS onlyPharmacokinetic dataBioavailability 70 to 90 MetabolismLiverElimination half life10 hrs normal kidney function ExcretionKidneyIdentifiersIUPAC name R 4 Amino 1 2 oxazolidin 3 oneCAS Number68 41 7 YPubChem CID6234DrugBankDB00260 YChemSpider5998 YUNII95IK5KI84ZKEGGD00877 YChEBICHEBI 40009 YChEMBLChEMBL771 YNIAID ChemDB007654CompTox Dashboard EPA DTXSID8022870ECHA InfoCard100 000 626Chemical and physical dataFormulaC 3H 6N 2O 2Molar mass102 093 g mol 13D model JSmol Interactive imageMelting point155 to 156 C 311 to 313 F dec SMILES O C1NOC C H 1NInChI InChI 1S C3H6N2O2 c4 2 1 7 5 3 2 6 h2H 1 4H2 H 5 6 t2 m1 s1 YKey DYDCUQKUCUHJBH UWTATZPHSA N Y verify Common side effects include allergic reactions seizures sleepiness unsteadiness and numbness 2 It is not recommended in people who have kidney failure epilepsy depression or are alcoholics 2 It is unclear if use during pregnancy is safe for the baby 2 Cycloserine is similar in structure to the amino acid D alanine and works by interfering with the formation of the bacteria s cell wall 2 Cycloserine was discovered in 1954 from a type of Streptomyces 3 It is on the World Health Organization s List of Essential Medicines 4 Contents 1 Medical uses 1 1 Tuberculosis 1 2 Psychiatry 2 Mechanism of action 3 Chemical properties 4 Synthesis 5 History 6 Economics 7 Research 8 ReferencesMedical uses editTuberculosis edit For the treatment of tuberculosis cycloserine is classified as a second line drug Its use is only considered if one or more first line drugs cannot be used Hence cycloserine is restricted for use only against multiple drug resistant and extensively drug resistant strains of M tuberculosis Another reason for limited use of this drug is the neurological side effects it causes since it is able to penetrate into the central nervous system CNS and cause headaches drowsiness depression dizziness vertigo confusion paresthesias dysarthria hyperirritability psychosis convulsions and shaking tremors 5 6 Overdose of cycloserine may result in paresis seizures and coma while alcohol consumption may increase the risk of seizures 6 Coadministration of pyridoxine can reduce the incidence of some of these CNS side effects e g convulsions caused by cycloserine citation needed Psychiatry edit A 2015 Cochrane review found no evidence of benefit in anxiety disorders as of 2015 7 Another review found preliminary evidence of benefit 8 Evidence for use in addiction is tentative but also unclear 9 Mechanism of action editCycloserine works as an antibiotic by inhibiting cell wall biosynthesis in bacteria 10 11 As a cyclic analogue of D alanine cycloserine acts against two crucial enzymes important in the cytosolic stages of peptidoglycan synthesis alanine racemase Alr and D alanine D alanine ligase Ddl 11 The first enzyme is a pyridoxal 5 phosphate dependent enzyme which converts the L alanine to the D alanine form 11 The second enzyme is involved in joining two of these D alanine residues together by catalyzing the formation of the ATP dependent D alanine D alanine dipeptide bond between the resulting D alanine molecules 11 If both of these enzymes are inhibited then D alanine residues cannot form and previously formed D alanine molecules cannot be joined 11 This effectively leads to inhibition of peptidoglycan synthesis 11 Psychiatric use is suggested based on partial NMDA receptor agonism which improves neural plasticity in lab animals The degree of clinical usefulness is as aforementioned very unclear and still being explored 8 Chemical properties editUnder mildly acidic conditions cycloserine hydrolyzes to give hydroxylamine and D serine 12 13 Cycloserine can be conceptualized as a cyclized version of serine with an oxidative loss of dihydrogen to form the nitrogen oxygen bond citation needed Cycloserine is stable under basic conditions with the greatest stability at pH 11 5 12 Synthesis editInitial approaches to synthesize the compound was first published in 1955 when the Stammer group produced a racemic synthesis from DL b aminoxyalanine ethyl ester In 1957 Platter et al managed to synthesis the pure D enantiomer by cyclizing the corresponding a amino b chlorohydroxamic acids Chemical synthesis of the compound was revolutionized in the 2010s when several approaches starting with the cheap D serine mirror form of normal L serine were published by different groups 14 The biosynthesis of the compound is defined by a ten gene cluster L serine and L arginine are converted to O ureido L serine flipped to O ureido D serine then turned into the final compound by cyclization In 2013 Uda et al successfully used recombinant versions of three enzymes in the cluster to produce the compound 15 A 1963 patent describes industrial production of the drug by bacterial fermentation 16 It is unclear what process is used in the 21st century fermentation or chemical synthesis citation needed History editThe compound was first isolated nearly simultaneously by two teams Workers at Merck isolated the compound which they called oxamycin from a species of Streptomyces 17 The same team prepared the molecule synthetically 18 Workers at Eli Lilly isolated the compound from strains of Streptomyces orchidaceus It was shown to hydrolyze to serine and hydroxylamine 19 Economics editIn the U S the price of cycloserine increased from 500 for 30 pills to 10 800 in 2015 after the Chao Center for Industrial Pharmacy and Contract Manufacturing changed ownership to Rodelis Therapeutics in August 2015 20 The price increase was rescinded after the previous owner the Purdue University Research Foundation which retained oversight of the manufacturing operation intervened and Rodelis returned the drug to an NGO of Purdue University The foundation now will charge 1 050 for 30 capsules twice what it charged before Eli Lilly has been criticised for not ensuring that the philanthropic initiative continued Due to US antitrust laws however no company may control the price of a product after it is outlicensed 21 In 2015 the cost in the United States was increased to US 3 150 a month and then decreased to US 1 050 per month 21 Research editSome experimental evidence suggests that D cycloserine aids in learning by helping form stronger neural connections 22 It has been investigated as an aid to facilitate exposure therapy in people with PTSD and anxiety disorders 23 24 25 and treatment with schizophrenia 26 In a clinical trial a course of D cycloserine combined with a single dose of ketamine was investigated for treatment resistant bipolar depression When administered for 8 weeks after a ketamine infusion cycloserine appeared to potentiate the antidepressant effects in all trial participants 27 However a 2019 clinical trial showed no statistically significant difference between the D cycloserine and placebo groups when it came to maintaining the antidepressant effect of a single ketamine infusion The authors suggest several possible explanations for this nonsignificance namely the inclusion of high risk or severely treatment resistant participants as well as a possible confounding carryover effect from the ketamine infusion phase Although the results point to D cycloserine having a stronger antisuicidal effect than placebo the authors caution that this difference might be attributed to the placebo group feeling worse than the D cycloserine feeling better 28 A combination drug cycloserine lurasidone containing D cycloserine and the atypical antipsychotic lurasidone is being developed for acute suicidal ideation behavior 29 References edit Polc P Pieri L Bonetti EP Scherschlicht R Moehler H Kettler R et al April 1986 L cycloserine behavioural and biochemical effects after single and repeated administration to mice rats and cats Neuropharmacology 25 4 Elsevier BV 411 418 doi 10 1016 0028 3908 86 90236 4 PMID 3012401 S2CID 462885 a b c d e f g Cycloserine The American Society of Health System Pharmacists Archived from the original on 20 December 2016 Retrieved 8 December 2016 Gottlieb D Shaw PD 2012 Mechanism of Action Springer Science amp Business Media p 41 ISBN 9783642460517 Archived from the original on 2016 12 20 World Health Organization 2019 World Health Organization model list of essential medicines 21st list 2019 Geneva World Health Organization hdl 10665 325771 WHO MVP EMP IAU 2019 06 License CC BY NC SA 3 0 IGO Nitsche MA Jaussi W Liebetanz D Lang N Tergau F Paulus W August 2004 Consolidation of human motor cortical neuroplasticity by D cycloserine PDF Neuropsychopharmacology 29 8 1573 8 doi 10 1038 sj npp 1300517 PMID 15199378 a b CYCLOSERINE Human Health Effects National Institutes of Health Archived from the original on 2014 04 16 Ori R Amos T Bergman H Soares Weiser K Ipser JC Stein DJ May 2015 Augmentation of cognitive and behavioural therapies CBT with d cycloserine for anxiety and related disorders The Cochrane Database of Systematic Reviews 2015 5 CD007803 doi 10 1002 14651858 CD007803 pub2 PMC 8939046 PMID 25957940 a b Schade S Paulus W April 2016 D Cycloserine in Neuropsychiatric Diseases A Systematic Review The International Journal of Neuropsychopharmacology 19 4 pyv102 doi 10 1093 ijnp pyv102 PMC 4851259 PMID 26364274 Myers KM Carlezon WA June 2012 D cycloserine effects on extinction of conditioned responses to drug related cues Biological Psychiatry 71 11 947 55 doi 10 1016 j biopsych 2012 02 030 PMC 4001849 PMID 22579305 Lambert MP Neuhaus FC June 1972 Mechanism of D cycloserine action alanine racemase from Escherichia coli W Journal of Bacteriology 110 3 978 87 doi 10 1128 JB 110 3 978 987 1972 PMC 247518 PMID 4555420 a b c d e f Prosser GA de Carvalho LP February 2013 Kinetic mechanism and inhibition of Mycobacterium tuberculosis D alanine D alanine ligase by the antibiotic D cycloserine The FEBS Journal 280 4 1150 66 doi 10 1111 febs 12108 PMID 23286234 S2CID 22305408 a b Kaushal G Ramirez R Alambo D Taupradist W Choksi K Sirbu C October 2011 Initial characterization of D cycloserine for future formulation development for anxiety disorders Drug Discoveries amp Therapeutics 5 5 253 60 doi 10 5582 ddt 2011 v5 5 253 PMID 22466372 Silverman R 1998 An Aromatization Mechanism of Inactivation of g Aminobutyric Acid Aminotransferase for the Antibiotic l Cycloserine Journal of the American Chemical Society 120 10 2256 2267 doi 10 1021 ja972907b Holt GR 6 December 2021 Principles of plastic surgery of congenital facial abnormalities Facial Plastic Surgery 3 3 147 154 doi 10 1002 cmdc 202100503 PMC 9293202 PMID 3459696 Uda N Matoba Y Kumagai T Oda K Noda M Sugiyama M June 2013 Establishment of an in vitro D cycloserine synthesizing system by using O ureido L serine synthase and D cycloserine synthetase found in the biosynthetic pathway Antimicrobial Agents and Chemotherapy 57 6 2603 2612 doi 10 1128 AAC 02291 12 PMC 3716191 PMID 23529730 Harned RL 21 May 1963 US3090730A Process for the production of cycloserine Google Patents Kuehl Jr FA Wolf FJ Trenner NR Peck RL Buhs RP Howe E et al 1955 D 4 Amino 3 isoxazolidinone a new antibiotic Journal of the American Chemical Society 77 8 2344 5 doi 10 1021 ja01613a105 Hidy PH Hodge EB Young VV Harned RL Brewer GA Phillips WF et al 1955 Synthesis of D 4 amino 3 isoxazolidinone Journal of the American Chemical Society 77 8 2346 7 doi 10 1021 ja01613a107 Hidy PH Hodge EB Young VV Harned RL Brewer GA Phillips WF et al 1955 Structure and reactions of cycloserine Journal of the American Chemical Society 77 8 2345 6 doi 10 1021 ja01613a106 Pollack A 20 September 2015 Drug Goes From 13 50 a Tablet to 750 Overnight The New York Times Archived from the original on 25 September 2015 Retrieved 21 September 2015 a b Pollack A 21 September 2015 Big Price Increase for Tuberculosis Drug Is Rescinded NYT Archived from the original on 26 September 2015 Retrieved 24 September 2015 Learning and Brain Activity Are Boosted by a Dose of a Small Molecule Compound Scientific American Archived from the original on 2015 12 23 Bowers ME Ressler KJ September 2015 An Overview of Translationally Informed Treatments for Posttraumatic Stress Disorder Animal Models of Pavlovian Fear Conditioning to Human Clinical Trials Biological Psychiatry 78 5 E15 27 doi 10 1016 j biopsych 2015 06 008 PMC 4527085 PMID 26238379 Hofmann SG Wu QJ Boettcher H May 2013 D cycloserine as an augmentation strategy for cognitive behavioral therapy for anxiety disorders Biology of Mood amp Anxiety Disorders 3 1 11 doi 10 1186 2045 5380 3 11 PMC 3686620 PMID 23768232 Singewald N Schmuckermair C Whittle N Holmes A Ressler KJ May 2015 Pharmacology of cognitive enhancers for exposure based therapy of fear anxiety and trauma related disorders Pharmacology amp Therapeutics 149 150 90 doi 10 1016 j pharmthera 2014 12 004 PMC 4380664 PMID 25550231 Goff DC September 2012 D cycloserine an evolving role in learning and neuroplasticity in schizophrenia Schizophrenia Bulletin 38 5 936 41 doi 10 1093 schbul sbs012 PMC 3446239 PMID 22368237 Kantrowitz J Halberstam B Gangwisch J June 2015 Single Dose Ketamine Followed by Daily d Cycloserine in Treatment Resistant Bipolar Depression The Journal of Clinical Psychiatry 76 6 737 738 doi 10 4088 JCP 14l09527 PMID 26132675 Chen MH Cheng CM Gueorguieva R Lin WC Li CT Hong CJ et al November 2019 Maintenance of antidepressant and antisuicidal effects by D cycloserine among patients with treatment resistant depression who responded to low dose ketamine infusion a double blind randomized placebo control study Neuropsychopharmacology 44 12 Springer Nature published 2019 08 17 2112 2118 doi 10 1038 s41386 019 0480 y PMC 6898334 PMID 31421635 S2CID 201057546 Official page about NeuroRX NRX100 NRX101 Archived from the original on 2020 07 09 Retrieved 2023 10 22 Portal nbsp Medicine Retrieved from https en wikipedia org w index php title Cycloserine amp oldid 1207304981, wikipedia, wiki, book, books, library,

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