NAAG peptidase inhibitor increases dialysate NAAG and reduces glutamate, aspartate and GABA levels in the dorsal hippocampus following fluid percussion injury in the rat

Zhong, Chunlong; Zhao, Xueren; Van, Ken C.; Bzdega, Tomasz; Smyth, Aoife; Zhou, Jia; Kozikowski, Alan P.; Jiang, Jiyao; O’Connor, W.T.; Berman, Robert F.; Neale, Joseph H.; Lyeth, Bruce G.

doi:10.1111/j.1471-4159.2006.03786.x

Cited by 91 publications

(130 citation statements)

References 68 publications

(93 reference statements)

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“…Consistent with our behavioral data with ZJ43 and LY341495 and in the context of this model, a group II mGluR agonist reduces PCP-induced glutamate efflux as well as motor and cognitive behaviors (9). Similarly, we also found that ZJ43 induced elevation of synaptic NAAG levels reduces glutamate efflux (38).…”

Section: Models Of Naag and Schizophreniasupporting

confidence: 79%

“…Given the IC 50 and Ki of ZJ43 of 2.4 nM and 0.9 nM respectively when tested against human GCPII (37), these behaviorally effective doses of ZJ43 are clearly within the range required to substantially inhibit the activity of NAAG peptidases. Consistent with this conclusion, we have demonstrated that this dose range of ZJ43 significantly elevates extracellular NAAG levels and decreases glutamate release in the rat hippocampus following traumatic brain injury (38). While we do not yet know the full time course of inhibition of NAAG peptidases that is achieved by a single i.p.…”

Section: Efficacy Of Naag Peptidase Inhibitionsupporting

confidence: 70%

“…While we do not yet know the full time course of inhibition of NAAG peptidases that is achieved by a single i.p. dose of ZJ43, we found that 150 mg/kg of ZJ43 retained near maximal effectiveness for at least 2 hours in vivo (unpublished) and that this effect was fully blocked by a single dose of LY431495 (38).…”

Section: Efficacy Of Naag Peptidase Inhibitionmentioning

confidence: 94%

“…We directly tested this hypothesis in a brain injury paradigm and found that systemic injection of ZJ43 results in increased levels of extracellular NAAG and that this effect was completely blocked by the group II antagonist (38). One model of the role of glutamate in schizophrenia and PCP-induced behaviors proposes that hypoactivity of NMDA receptors, as is modeled by PCP, leads to reduced GABA-ergic inhibition, and excess release of glutamate and dopamine, particularly in the prefrontal cortex (45;46).…”

Section: Models Of Naag and Schizophreniamentioning

confidence: 99%

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Phencyclidine and Dizocilpine Induced Behaviors Reduced by N-acetylaspartylglutamate Peptidase Inhibition via Metabotropic Glutamate Receptors

Olszewski

Wegorzewska

Monteiro

et al. 2008

Biological Psychiatry

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Section: Models Of Naag and Schizophreniasupporting

confidence: 79%

Section: Efficacy Of Naag Peptidase Inhibitionsupporting

confidence: 70%

Section: Efficacy Of Naag Peptidase Inhibitionmentioning

confidence: 94%

Section: Models Of Naag and Schizophreniamentioning

confidence: 99%

See 2 more Smart Citations

Phencyclidine and Dizocilpine Induced Behaviors Reduced by N-acetylaspartylglutamate Peptidase Inhibition via Metabotropic Glutamate Receptors

Olszewski

Wegorzewska

Monteiro

et al. 2008

Biological Psychiatry

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“…Microdialysis was initiated 10 min prior to injury and treatment, resulting in one sample before stretch injury and two samples collected at 10 and 20 min after stretch injury. Dialysates were then frozen, and glutamate levels were later analyzed by HPLC as described previously (Zhong et al, 2006).…”

Section: Fig 1 Microdialysis Sampling Apparatus Flexcellmentioning

confidence: 99%

Neuroprotective Effects of Selective N-Type VGCC Blockade on Stretch-Injury-Induced Calcium Dynamics in Cortical Neurons

Shahlaie

Lyeth

Gurkoff

et al. 2010

Journal of Neurotrauma

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Acute elevation in intracellular calcium ([Ca 2þ ] i ) following traumatic brain injury (TBI) can trigger cellular mechanisms leading to neuronal dysfunction and death. The mechanisms underlying these processes are not completely understood, but calcium influx through N-type voltage-gated calcium channels (VGCCs) appears to play a central role. The present study examined the time course of [Ca 2þ ] i flux, glutamate release, and loss of cell viability following injury using an in vitro neuronal-glial cortical cell-culture model of TBI. The effects of N-channel blockade with SNX-185 (e.g. o-conotoxin TVIA) before or after injury were also examined. Neuronal injury produced a transient elevation in [Ca 2þ ] i , increased glutamate release, and resulted in neuronal and glial death. SNX-185 administered before or immediately after cell injury reduced glutamate release and increased the survival of neurons and astrocytes, whereas delayed treatment did not improve cell survival but significantly facilitated the return of [Ca 2þ ] i to baseline levels. The new findings that N-type VGCCs are critically involved in injury-induced glutamate release and recovery of [Ca 2þ ] i argue for continued investigation of this treatment strategy for the clinical management of TBI. In particular, SNX-185 may represent an effective class of drugs that can significantly protect injured neurons from the secondary insults that commonly occur after TBI.

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Mouse glutamate carboxypeptidase II (GCPII) has a similar enzyme activity and inhibition profile but a different tissue distribution to human GCPII

et al. 2017

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Glutamate carboxypeptidase II ( GCPII ), also known as prostate‐specific membrane antigen ( PSMA ) or folate hydrolase, is a metallopeptidase expressed predominantly in the human brain and prostate. GCPII expression is considerably increased in prostate carcinoma, and the enzyme also participates in glutamate excitotoxicity in the brain. Therefore, GCPII represents an important diagnostic marker of prostate cancer progression and a putative target for the treatment of both prostate cancer and neuronal disorders associated with glutamate excitotoxicity. For the development of novel therapeutics, mouse models are widely used. However, although mouse GCPII activity has been characterized, a detailed comparison of the enzymatic activity and tissue distribution of the mouse and human GCPII orthologs remains lacking. In this study, we prepared extracellular mouse GCPII and compared it with human GCPII . We found that mouse GCPII possesses lower catalytic efficiency but similar substrate specificity compared with the human protein. Using a panel of GCPII inhibitors, we discovered that inhibition constants are generally similar for mouse and human GCPII . Furthermore, we observed highest expression of GCPII protein in the mouse kidney, brain, and salivary glands. Importantly, we did not detect GCPII in the mouse prostate. Our data suggest that the differences in enzymatic activity and inhibition profile are rather small; therefore, mouse GCPII can approximate human GCPII in drug development and testing. On the other hand, significant differences in GCPII tissue expression must be taken into account when developing novel GCPII ‐based anticancer and therapeutic methods, including targeted anticancer drug delivery systems, and when using mice as a model organism.

show abstract

NAAG peptidase inhibitor increases dialysate NAAG and reduces glutamate, aspartate and GABA levels in the dorsal hippocampus following fluid percussion injury in the rat

Cited by 91 publications

References 68 publications

Phencyclidine and Dizocilpine Induced Behaviors Reduced by N-acetylaspartylglutamate Peptidase Inhibition via Metabotropic Glutamate Receptors

Phencyclidine and Dizocilpine Induced Behaviors Reduced by N-acetylaspartylglutamate Peptidase Inhibition via Metabotropic Glutamate Receptors

Neuroprotective Effects of Selective N-Type VGCC Blockade on Stretch-Injury-Induced Calcium Dynamics in Cortical Neurons

Mouse glutamate carboxypeptidase II (GCPII) has a similar enzyme activity and inhibition profile but a different tissue distribution to human GCPII

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