ZLc002, a putative small-molecule inhibitor of nNOS interaction with NOS1AP, suppresses inflammatory nociception and chemotherapy-induced neuropathic pain and synergizes with paclitaxel to reduce tumor cell viability

Lee, Wan-Hung; Carey, Lawrence M.; Li, Lili; Xu, Zhili; Lai, Yvonne; Courtney, Michael J.; Hohmann, Andrea G.

doi:10.1177/1744806918801224

Cited by 14 publications

(12 citation statements)

References 40 publications

(92 reference statements)

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“…on day 0, 2, 4, and 6 (approximately 48 hours between injections); cumulative dose 16 mg/kg) to produce a CIPN condition, as described previously. 14,19,21,42,[48][49][50]52,54,[83][84][85][86][87][88] Control mice received an equal volume of cremophor-based vehicle on the same treatment schedule. Development of paclitaxel-induced allodynia was assessed on day 0, 4, 7, 11, and 14.…”

Section: General Experimental Protocolmentioning

confidence: 99%

A peripheral CB2 cannabinoid receptor mechanism suppresses chemotherapy-induced peripheral neuropathy: evidence from a CB2 reporter mouse

Lin

Carey

et al. 2021

Pain

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CB 2 cannabinoid receptors (CB 2 ) are a promising therapeutic target that lacks unwanted side effects of CB 1 activation. However, the cell types expressing CB 2 that mediate these effects remain poorly understood. We used transgenic mice with CB 2 promoter-driven expression of enhanced green fluorescent protein (EGFP) to study cell types that express CB 2 and suppress neuropathic nociception in a mouse model of chemotherapy-induced peripheral neuropathy. Structurally distinct CB 2 agonists (AM1710 and LY2828360) suppressed paclitaxel-induced mechanical and cold allodynia in CB 2 EGFP reporter mice with established neuropathy. Antiallodynic effects of AM1710 were blocked by SR144528, a CB 2 antagonist with limited CNS penetration. Intraplantar AM1710 administration suppressed paclitaxel-induced neuropathic nociception in CB 2 EGFP but not CB 2 knockout mice, consistent with a local site of antiallodynic action. mRNA expression levels of the anti-inflammatory cytokine interleukin-10 were elevated in the lumbar spinal cord after intraplantar AM1710 injection along with the proinflammatory cytokine tumor necrosis factor alpha and chemokine monocyte chemoattractant protein-1. CB 2 EGFP , but not wildtype mice, exhibited anti-GFP immunoreactivity in the spleen. However, the anti-GFP signal was below the threshold for detection in the spinal cord and brain of either vehicle-treated or paclitaxel-treated CB 2 EGFP mice. EGFP fluorescence was coexpressed with CB 2 immunolabeling in stratified patterns among epidermal keratinocytes. EGFP fluorescence was also expressed in dendritic cells in the dermis, Langerhans cells in the epidermis, and Merkel cells. Quantification of the EGFP signal revealed that Langerhans cells were dynamically increased in the epidermis after paclitaxel treatment. Our studies implicate CB 2 expressed in previously unrecognized populations of skin cells as a potential target for suppressing chemotherapy-induced neuropathic nociception.

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Section: General Experimental Protocolmentioning

confidence: 99%

A peripheral CB2 cannabinoid receptor mechanism suppresses chemotherapy-induced peripheral neuropathy: evidence from a CB2 reporter mouse

Lin

Carey

et al. 2021

Pain

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“…The actions observed in mice treated with ZL006 in our study have paved the way for future dose optimization in preclinical trials and subsequent clinical trials. Besides, we also inspired other studies that employ similar agents targeting the PSD95/nNOS or its downstream node in the pathway, including IC87201 or ZLc002 (Florio et al 2009 ; Lee et al 2018 ; Lee et al 2015 ; Zhu et al 2014 ).…”

Section: Discussionmentioning

confidence: 90%

Targeting PSD95/nNOS by ZL006 alleviates social isolation-induced heightened attack behavior in mice

et al. 2021

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Rationale Deregulated attack behaviors have devastating social consequences; however, satisfactory clinical management for the behavior is still an unmet need so far. Social isolation (SI) has been common during the COVID-19 pandemic and may have detrimental effects on mental health, including eliciting heightened attack behavior. Objectives This study aims to explore whether injection of ZL006 can alleviate SI-induced escalation of attack behavior in mice. Methods Pharmacological tools, biochemical methods, and behavioral tests were used to explore the potential therapeutic effects of ZL006 targeting postsynaptic density 95 (PSD95)/neuronal nitric oxide synthase (nNOS) pathway on escalation of attack behavior induced by SI in mice. Results ZL006 mitigated SI-induced escalated attack behaviors and elevated nitric oxide (NO) level in the cortex of the SI mice. The beneficial effects of ZL006 lasted for at least 72 h after a single injection of ZL006. Potentiation of NO levels by L-arginine blocked the effects of ZL006. Moreover, a sub-effective dose of 7-NI in combination with a sub-effective dose of ZL006 decreased both SI-induced escalated attack behaviors and NO levels in mice subjected to SI. Conclusions Our study highlights the importance of the PSD95/nNOS pathway in mediating SI-induced escalation of attack behavior. ZL006 may be a promising therapeutic strategy for treating aggressive behaviors. Supplementary Information The online version contains supplementary material available at 10.1007/s00213-021-06000-9.

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“…Also, stroke, neuropathic pain and early‐stage Alzheimer's disease are associated with the co‐morbid anxiety (Bierman, Comijs, Jonker, Scheltens, & Beekman, 2009; Campbell Burton et al, 2013; Knapp et al, 2017; Kwak, Yang, & Koo, 2017; Nicholson & Verma, 2004). Reportedly, nNOS–CAPON association mediates amyloid‐β‐induced neurotoxicity (Zhang et al, 2018), ischaemia‐induced impairment of structural plasticity (Ni et al, 2018) and inflammatory nociception and chemotherapy‐induced neuropathic pain (Lee, Carey, et al, 2018; Lee, Li, et al, 2018). We previously reported that dissociation of nNOS with CAPON by ZLc‐002 produces rapid onset of anxiolytic‐like effect (Zhu et al, 2014).…”

Section: Discussionmentioning

confidence: 99%

nNOS‐CAPON blockers produce anxiolytic effects by promoting synaptogenesis in chronic stress‐induced animal models of anxiety

Zhu

Shi

Chang

et al. 2020

British J Pharmacology

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Background and Purpose Anxiety disorder is a common mental health disorder. However, there are few safe and fast‐acting anxiolytic drugs available that can treat anxiety disorder. We previously demonstrated that the interaction of neuronal NOS (nNOS) with its carboxy‐terminal PDZ ligand (CAPON) is involved in regulating anxiety‐related behaviours. Here, we further investigated the anxiolytic effects of nNOS–CAPON disruptors in chronic stress‐induced anxiety in animals. Experimental Approach Mice were intravenously treated with nNOS–CAPON disruptors, ZLc‐002 or Tat‐CAPON12C, at the last week of chronic mild stress (CMS) exposure. We also infused http://corticosterone (CORT) into the hippocampus of mice to model anxiety behaviours and also delivered ZLc‐002 or Tat‐CAPON12C on the last week of chronic CORT treatment via pre‐implanted cannula. Anxiety‐related behaviours were examined using elevated plus maze, open field, novelty‐suppressed feeding and light–dark (LD) tests. The level of nNOS–CAPON interaction was determined by co‐immunoprecipitation (CO‐IP) and proximity ligation assay (PLA). The neural mechanisms underlying the behavioural effects of nNOS–CAPON uncoupling in anxiety animal models were assessed by western blot, immunofluorescence and Golgi‐Cox staining. Key Results ZLc‐002 and Tat‐CAPON12C reversed CMS‐ or CORT‐induced anxiety‐related behaviours. ZLc‐002 and Tat‐CAPON12C increased synaptogenesis along with improved dendritic remodelling in CMS mice or CORT‐treated cultured neurons. Meanwhile, blocking nNOS–CAPON interaction significantly activated the cAMP response element‐binding protein (CREB)–brain‐derived neurotrophic factor (BDNF) pathway, which is associated with synaptic plasticity. Conclusion and Implications Collectively, these results provide evidence for the anxiolytic effects of nNOS–CAPON uncouplers and their underlying mechanisms in anxiety disorders.

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ZLc002, a putative small-molecule inhibitor of nNOS interaction with NOS1AP, suppresses inflammatory nociception and chemotherapy-induced neuropathic pain and synergizes with paclitaxel to reduce tumor cell viability

Cited by 14 publications

References 40 publications

A peripheral CB2 cannabinoid receptor mechanism suppresses chemotherapy-induced peripheral neuropathy: evidence from a CB2 reporter mouse

A peripheral CB2 cannabinoid receptor mechanism suppresses chemotherapy-induced peripheral neuropathy: evidence from a CB2 reporter mouse

Targeting PSD95/nNOS by ZL006 alleviates social isolation-induced heightened attack behavior in mice

nNOS‐CAPON blockers produce anxiolytic effects by promoting synaptogenesis in chronic stress‐induced animal models of anxiety

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