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20 resultsShowing papers similar to Primary astrocytes as a cellular depot of polystyrene nanoparticles
ClearNeurotoxic potential of polystyrene nanoplastics in primary cells originating from mouse brain
Researchers exposed three types of primary mouse brain cells to 100 nm polystyrene nanoplastics and found that neurons underwent apoptosis while astrocytes survived but developed reactive astrocytosis with elevated inflammatory markers, suggesting that neuronal vulnerability to nanoplastic accumulation may be amplified by astrocyte-driven neuroinflammation.
Polystyrene Micro- and Nanoplastic Exposure Triggers an Activation and Stress Response in Human Astrocytes
Researchers exposed primary human astrocytes to polystyrene micro- and nanoplastics and found that these particles triggered cellular stress responses, including increased production of reactive oxygen species and activation of inflammatory pathways. Nanoplastics were particularly effective at penetrating cells and disrupting normal astrocyte function. The findings suggest that plastic particle exposure may contribute to neuroinflammatory processes in the brain, warranting further investigation into potential neurotoxic effects.
Alleviation of neurotoxicity induced by polystyrene nanoplastics by increased exocytosis from neurons
Researchers investigated how polystyrene nanoplastics accumulate in neurons and cause toxic effects on brain cells. They found that inhibiting a specific protein involved in transporting particles within cells promoted the export of nanoplastics from neurons, reducing their harmful effects. The study suggests that enhancing the cell's natural ability to expel nanoplastics could be a potential strategy for alleviating their neurotoxic impact.
Microglial clearance of Alzheimer's amyloid-beta obstructed by nanoplastics
Researchers found that polystyrene nanoplastics interfere with the brain's ability to clear amyloid-beta, the protein that builds up in Alzheimer's disease. The nanoplastics accelerated amyloid clumping and drained the energy of brain immune cells that normally clean up these harmful proteins. This study suggests that nanoplastic exposure could worsen or contribute to the development of Alzheimer's disease.
Crossing barriers – tracking micro- and nanoplastic pathways into the human brain
Researchers tracked potential pathways by which micro- and nanoplastics may enter the human brain, examining both in vitro cell models and post-mortem brain tissue. They found that human monocytes rapidly internalized polystyrene particles into endocytic vesicles and mitochondria, and detected plastic particles in brain tissue samples, providing evidence that nanoplastics may be capable of crossing brain barriers.
Disruption of cerebral cholesterol homeostasis by PS-NPs: astrocytic endoplasmic reticulum stress
Researchers found that polystyrene nanoplastics disrupt cholesterol production in brain support cells called astrocytes, which in turn prevents neurons from forming the connections needed for brain function. By triggering stress responses and blocking key cholesterol-making pathways, nanoplastics ultimately inhibit synapse formation — raising concerns about their potential role in neurological disease.
Neurotoxic effects of polystyrene nanoplastics on memory and microglial activation: Insights from in vivo and in vitro studies
In a mouse study, tiny nanoplastics (30-50 nanometers) that were swallowed reached the brain and caused memory problems by activating the brain's immune cells, called microglia, which triggered inflammation. This is concerning because it shows that nanoplastics small enough to be found in everyday products like cosmetics could cross into the brain and impair cognitive function.
Exposure to microplastics/ nanoplastics induces responses of microglia and astrocytes: roles of oxidative stress and autophagy
This study examined how microplastic and nanoplastic exposure affects glial cells in the central nervous system, specifically investigating responses of microglia and astrocytes, which are the brain's primary immune and support cells. Results showed that micro- and nanoplastic exposure triggered inflammatory-type responses in these cells, raising concern for neurological effects.
Human neurons are susceptible to the internalization of small-sized nanoplastics
Researchers studied how human neurons take up nanoplastics and found that the cells readily absorbed 50-nanometer polystyrene particles through specific cellular pathways. The nanoplastics accumulated in cell compartments and, at higher concentrations, triggered oxidative stress and reduced cell survival. The study provides evidence that very small plastic particles can enter human brain cells, raising concerns about potential neurological effects of nanoplastic exposure.
Polystyrene nanoplastics penetrate across the blood-brain barrier and induce activation of microglia in the brain of mice
Researchers demonstrated that 50-nanometer polystyrene nanoplastics can cross the blood-brain barrier in mice, accumulate in brain tissue, and activate immune cells called microglia that then damage neurons. The nanoplastics disrupted the tight junctions that normally protect the brain, creating openings for the particles to pass through. This study provides direct evidence that nanoplastics can reach the brain and trigger inflammation, raising concerns about potential neurological effects of long-term nanoplastic exposure in humans.
Polystyrene Nano- and Microplastic Particles Induce an Inflammatory Gene Expression Profile in Rat Neural Stem Cell-Derived Astrocytes In Vitro
Researchers exposed brain cells derived from rat neural stem cells to polystyrene nano- and microplastics and found that astrocytes -- the most abundant brain support cells -- were the most affected, showing reduced survival and widespread changes in gene activity. The activated genes were involved in brain inflammation and immune responses, while genes for fat metabolism were turned down. These findings suggest that plastic particles reaching the brain could trigger inflammation that may contribute to neurological problems.
Brain under siege: the role of micro and nanoplastics in neuroinflammation and oxidative stress
This review examines emerging evidence that micro- and nanoplastics can cross the blood-brain barrier and accumulate in nervous tissue, potentially triggering neuroinflammation and oxidative stress. Researchers summarized findings showing these particles may act as neurotoxicants that contribute to synaptic dysfunction and pathological changes in brain cells. The study highlights the need for further research into how chronic plastic particle exposure may affect central nervous system health over time.
Exposure to microplastics/ nanoplastics induces responses of microglia and astrocytes: roles of oxidative stress and autophagy
This study investigated how microplastic and nanoplastic exposure affects glial cells including microglia and astrocytes in the central nervous system, which are essential for neurological immune defense and homeostasis. Exposure triggered reactive responses in both cell types, raising concern that plastic particle accumulation in the brain could contribute to neuroinflammation.
Molecular effects of polystyrene nanoplastics on human neural stem cells
Researchers exposed human brain stem cells to tiny polystyrene nanoplastics and found they caused oxidative stress, DNA damage, inflammation, and cell death. These findings suggest that nanoplastics could potentially harm brain development if they reach neural tissue, though more research is needed to understand real-world exposure levels.
Polystyrene nanoplastics induce cognitive dysfunction and dendritic spine deterioration via excessive mitochondrial fission
Researchers demonstrated that polystyrene nanoplastics can cross the blood-brain barrier and accumulate in mouse brains, leading to cognitive impairment and loss of connections between brain cells. The damage was driven by excessive splitting of mitochondria, the energy-producing structures within cells, which triggered runaway cellular cleanup processes. Importantly, a drug that blocks this mitochondrial splitting reversed the cognitive damage, suggesting a potential therapeutic approach to nanoplastic-related brain injury.
Polystyrene nanoplastics induced learning and memory impairments in mice by damaging the glymphatic system
Mice exposed to polystyrene nanoplastics through different routes developed learning and memory problems linked to damage in their brain's waste-clearing system, called the glymphatic system. Amino-modified nanoplastics caused the most severe effects, disrupting the channels that normally flush toxins from the brain during sleep, suggesting a mechanism by which plastic pollution could contribute to cognitive decline.
Toxic Effects of Polylactic Acid Nanoplastics on in Vitro Models of Astrocytes and Neurons
PLA nanoplastics were tested on in vitro astrocyte and neuron models derived from human cells, demonstrating cytotoxicity, mitochondrial dysfunction, and inflammatory activation in both cell types, suggesting that biodegradable plastic nanoplastics pose neurological risks.
A Multisystemic Approach Revealed Aminated Polystyrene Nanoparticles-Induced Neurotoxicity.
Aminated polystyrene nanoparticles caused neurotoxicity in multiple model systems, including effects on neuronal cell viability, oxidative stress markers, and behavioral changes in exposed organisms, demonstrating that surface charge of nanoplastics influences their capacity to damage nervous tissue.
Short-term PS-NP exposure in early adulthood induces neuronal damage in middle-aged mice via microglia-mediated neuroinflammation
Researchers orally dosed young mice with polystyrene nanoplastics for one week and observed, ten months later, that particles persisted in brain tissue and drove microglial-mediated neuroinflammation, synapse loss, and cognitive impairment — with minocycline treatment confirming that microglial activation was the key driver of long-term neuronal damage.
Cerebral to SystemicRepresentations of Alzheimer’sPathogenesis Stimulated by Polystyrene Nanoplastics
Researchers exposed both wild-type and APP/PS1 Alzheimer's model mice to environmental levels of polystyrene nanoplastics and measured Alzheimer's-like pathology progression. Nanoplastics exacerbated cognitive decline, microglial activation, and hippocampal neuronal death, particularly in the Alzheimer's model, with systemic inflammatory effects suggesting plastic particles may accelerate neurodegeneration.