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⚗️ Metals 1041
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neuroscience (64)cognitive function (30)synaptic plasticity (25)stress (15)antidepressant (14)pharmacology (11)cognitive dysfunction (10)toxicology (9)cognition (9)serotonin (8)major depressive disorder (7)molecular biology (7)spinal cord injury (7)prefrontal cortex (7)chronic stress (6)autism spectrum disorder (6)chronic pain (6)exosomes (6)ptsd (6)cognitive (6)irisin (5)pregnancy (5)memory impairment (5)network pharmacology (5)cognitive performance (5)endoplasmic reticulum stress (5)neuropharmacology (5)environmental enrichment (4)homeostasis (4)oncology (4)neuroprotective effects (4)traumatic brain injury (4)molecular mechanisms (4)depressive disorder (4)cardiovascular (4)psychopharmacology (4)neuroregeneration (4)resveratrol (4)post-traumatic stress disorder (4)chitosan (4)affective disorders (3)osteoporosis (3)insomnia (3)high-intensity interval training (3)neurobiological mechanisms (3)serum (3)treatment-resistant depression (3)mirna (3)nerve regeneration (3)animal model 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📌 LLM 852
▸ LLM (77)
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🦠 Diseases 57
▸ Diseases — Other (15)
neurodegenerative diseases (15)neurodegenerative disorder (10)neurodegenerative disorders (10)diabetes (5)cancer (3)type 2 diabetes (2)lung cancer (2)alzheimer disease (2)type 2 diabetes mellitus (2)type 3 diabetes (1)neurodegenerative (1)non-small cell lung cancer (1)diabetes mellitus (1)anticancer (1)gestational diabetes mellitus (1)
⚙️ Mechanisms 56
▸ Mechanisms — Other (43)
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🎯 Targets 22
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micrornas (4)microrna (3)maternal separation (2)lncrna (2)maternal immune activation (2)maternal exercise (2)microrna-34a (1)maternal (1)mtor pathway (1)rna (1)dna methylation (1)mrna (1)fibrinolytic enzymes (1)
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antioxidant (11)sensory nerves (1)antioxidant activity (1)pet imaging (1)in vivo imaging (1)bioluminescence imaging (1)sensory neurotoxicity (1)neuroimaging (1)antioxidants (1)antioxidant properties (1)
🔗 Ligands 19
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ketamine (4)monoamine deficiency (2)monoaminergic (2)dopamine (2)dopaminergic neurons (2)dopaminergic neuron (1)histaminergic transmission (1)esketamine (1)monoamine (1)dopaminergic (1)methamphetamine (1)histamine (1)
🧠 Concepts 5
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metabolism (2)immunometabolism (1)brain metabolism (1)energy metabolism (1)
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quercetin (2)oxaliplatin (1)paclitaxel (1)

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Jujuboside A alleviates visceral pain and depression comorbidity and modulates the P2X7R-BDNF signaling axis.

Jian Liu, Yeqing Liu, Changtie Liu +9 more · 2026 · Phytomedicine : international journal of phytotherapy and phytopharmacology · Elsevier · added 2026-04-24
Visceral pain is frequently accompanied by depression, a comorbidity involving central neuroinflammation and abnormal neuronal plasticity. The P2X7 receptor (P2X7R) plays a crucial role in neuroinflam Show more
Visceral pain is frequently accompanied by depression, a comorbidity involving central neuroinflammation and abnormal neuronal plasticity. The P2X7 receptor (P2X7R) plays a crucial role in neuroinflammation and pyroptosis, while Jujuboside A (JuA), a major saponin extracted from Ziziphus jujuba seeds, has been reported to exert significant antidepressant and analgesic effects. In this study, we systematically evaluated the regulatory effects of JuA on the P2X7R-brain-derived neurotrophic factor (BDNF) pathway and on pyroptosis and apoptosis using a rat model of colorectal distension (CRD) and primary neuron/astrocyte cultures. JuA markedly alleviated visceral hypersensitivity and depressive-like behaviors in CRD rats and reduced P2X7R expression in both the spinal cord (SC) and hippocampus (HPC). Further investigations in vitro revealed that JuA inhibited excessive P2X7R activation in SC astrocytes, thereby decreasing the expression of NLRP3, Caspase-1, GSDMD, IL-1β and TNF-α, indicating suppression of pyroptosis. Similarly, JuA exerted an anti-pyroptotic effect in HPC astrocytes and inhibited neuronal apoptosis by reducing Caspase-3 and Bax levels while increasing Bcl2 expression, leading to upregulation of HPC BDNF. Collectively, JuA targets P2X7R and suppresses downstream pyroptotic and apoptotic signaling in vitro, which may contribute to its neuroprotective effects. These findings provide experimental evidence supporting the potential of JuA as a therapeutic agent for comorbid visceral pain and depression. Show less
no PDF DOI: 10.1016/j.phymed.2026.157764
BDNF bdnf depression neuroinflammation neuroplasticity p2x7r pyroptosis visceral pain