Glycine Transporter Type 1 Occupancy by Bitopertin: a Positron Emission Tomography Study in Healthy Volunteers

Martin‐Facklam, Meret; Pizzagalli, Flavia; Zhou, Yun; Ostrowitzki, Susanne; Raymont, Vanessa; Brašić, James Robert; Parkar, Nikhat; Umbricht, Daniel; Dannals, Robert F.; Goldwater, Ron; Wong, Dean F.

doi:10.1038/npp.2012.212

Cited by 47 publications

(14 citation statements)

References 33 publications

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“…The only other change was a modest increase in dopamine by sarcosine (Table 1). These observations are important since, to our knowledge, this is the first comprehensive neurochemical characterisation of sarcosine, despite its extensive use as a specific "GlyT1 inhibitor" and an adjunctive agent in schizophrenia patients [12,73,74]. Lack of change in 5-HT is important given concerns about a potential interaction with serotonergic transmission at a clinical dose of 2 g [75] and a transient elevation of rat PFC 5-HT with an extremely high dose (2 g/kg p.o.)…”

Section: Modulation Of Extracellular Amino Acids Levels Of In Pfcmentioning

confidence: 98%

Comparative Pro-cognitive and Neurochemical Profiles of Glycine Modulatory Site Agonists and Glycine Reuptake Inhibitors in the Rat: Potential Relevance to Cognitive Dysfunction and Its Management

Fone

Watson

Billiras³

et al. 2020

Mol Neurobiol

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Frontocortical NMDA receptors are pivotal in regulating cognition and mood, are hypofunctional in schizophrenia, and may contribute to autistic spectrum disorders. Despite extensive interest in agents potentiating activity at the co-agonist glycine modulatory site, few comparative functional studies exist. This study systematically compared the actions of the glycine reuptake inhibitors, sarcosine (40-200 mg/kg) and ORG24598 (0.63-5 mg/kg), the agonists, glycine (40-800 mg/kg), and D-serine (10-160 mg/kg) and the partial agonists, S18841 (2.5 mg/kg s.c.) and D-cycloserine (2.5-40 mg/kg) that all dose-dependently prevented scopolamine disruption of social recognition in adult rats. Over similar dose ranges, they also prevented a delayinduced impairment of novel object recognition (NOR). Glycine reuptake inhibitors specifically elevated glycine but not D-serine levels in rat prefrontal cortical (PFC) microdialysates, while glycine and D-serine markedly increased levels of glycine and Dserine, respectively. D-Cycloserine slightly elevated D-serine levels. Conversely, S18841 exerted no influence on glycine, Dserine, other amino acids, monamines, or acetylcholine. Reversal of NOR deficits by systemic S18841 was prevented by the NMDA receptor antagonist, CPP (20 mg/kg), and the glycine modulatory site antagonist, L701,324 (10 mg/kg). S18841 blocked deficits in NOR following microinjection into the PFC (2.5-10 μg/side) but not the striatum. Finally, in rats socially isolated from weaning (a neurodevelopmental model of schizophrenia), S18841 (2.5 and 10 mg/kg s.c.) reversed impairment of NOR and contextual fear-motivated learning without altering isolation-induced hyperactivity. In conclusion, despite contrasting neurochemical profiles, partial glycine site agonists and glycine reuptake inhibitors exhibit comparable pro-cognitive effects in rats of potential relevance to treatment of schizophrenia and other brain disorders where cognitive performance is impaired.

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Section: Modulation Of Extracellular Amino Acids Levels Of In Pfcmentioning

confidence: 98%

Comparative Pro-cognitive and Neurochemical Profiles of Glycine Modulatory Site Agonists and Glycine Reuptake Inhibitors in the Rat: Potential Relevance to Cognitive Dysfunction and Its Management

Fone

Watson

Billiras³

et al. 2020

Mol Neurobiol

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“…Although no MRS, PET or SPECT studies of the glycine transporter have been performed in SCZ, several PET tracers that target the glycine transporter type 1 (GlyT-1), such as [ 11 C]GSK931145 (see refs. 105 and 106) and [ 11 C]RO5013853, 107,108 have been developed. These have proven useful for quantifying occupancy of GlyT-1 by other, unlabeled compounds, but it is not yet clear whether they are suitably sensitive enough for examining GlyT-1 availability in psychiatric populations including SCZ.…”

Section: Nmda Receptor Modulationmentioning

confidence: 99%

Imaging glutamate in schizophrenia: review of findings and implications for drug discovery

et al. 2013

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Currently, all treatments for schizophrenia (SCZ) function primarily by blocking D(2)-type dopamine receptors. Given the limitations of these medications, substantial efforts have been made to identify alternative neurochemical targets for treatment development in SCZ. One such target is brain glutamate. The objective of this article is to review and synthesize the proton magnetic resonance spectroscopy ((1)H MRS) and positron emission tomography (PET)/single-photon emission computed tomography (SPECT) investigations that have examined glutamatergic indices in SCZ, including those of modulatory compounds such as glutathione (GSH) and glycine, as well as data from ketamine challenge studies. The reviewed (1)H MRS and PET/SPECT studies support the theory of hypofunction of the N-methyl-D-aspartate receptor (NMDAR) in SCZ, as well as the convergence between the dopamine and glutamate models of SCZ. We also review several advances in MRS and PET technologies that have opened the door for new opportunities to investigate the glutamate system in SCZ and discuss some ways in which these imaging tools can be used to facilitate a greater understanding of the glutamate system in SCZ and the successful and efficient development of new glutamate-based treatments for SCZ.

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“…In preclinical studies, bitopertin has proven to be effective in rat models to reverse PCP-induced positive and negative symptoms of the SZ phenotype and it has good bioavailability in the brain with oral dosing in positive emission tomography (PET) studies in baboons 28 . Human PET studies with bitopertin have demonstrated an inverted U pharmacokinetic therapeutic window, and have provided evidence for ideal dosing of bitopertin to be 10mg orally and daily, with less pronounced but effective results at 30mg daily 29 .…”

Section: Glycine Transporter-1 Inhibitors: Non Sarcosine Derivativesmentioning

confidence: 99%

Glycine Reuptake Inhibitors in the Treatment of Negative Symptoms of Schizophrenia

Thomas

Baker

Dursun

et al. 2014

Klinik Psikofarmakoloji Bülteni-Bulletin of Clinical Psychophar

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Glycine reuptake inhibitors in the treatment of negative symptoms of schizophrenia Negative symptoms are present in over one quarter of patients with schizophrenia and are detrimental to prognosis, functionality and quality of life. Currently, the treatments for primary negative symptoms are inadequate. However, enhancing N-methyl-D-aspartate receptor hypofunctioning with glycine reuptake inhibitors has garnered optimism as a potential treatment. Trials of sarcosine-derivatives have yielded mixed results and potential severe side effects have halted progress to larger studies. Non-sarcosine derivatives such as bitopertin have proven to be less toxic and have shown success in phase II trials. Unfortunately, phase III trials of bitopertin to date have not met primary endpoints and a void in effective treatment options for negative symptoms persists. Further research to improve psychiatric study design, discover clinical biomarkers and build on early successes of other potential pharmacologic molecules is required.

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Glycine Transporter Type 1 Occupancy by Bitopertin: a Positron Emission Tomography Study in Healthy Volunteers

Cited by 47 publications

References 33 publications

Comparative Pro-cognitive and Neurochemical Profiles of Glycine Modulatory Site Agonists and Glycine Reuptake Inhibitors in the Rat: Potential Relevance to Cognitive Dysfunction and Its Management

Comparative Pro-cognitive and Neurochemical Profiles of Glycine Modulatory Site Agonists and Glycine Reuptake Inhibitors in the Rat: Potential Relevance to Cognitive Dysfunction and Its Management

Imaging glutamate in schizophrenia: review of findings and implications for drug discovery

Glycine Reuptake Inhibitors in the Treatment of Negative Symptoms of Schizophrenia

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