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Exposure to polystyrene microplastics reduces sociality and brain oxytocin levels through the gut-brain axis in mice

The Science of The Total Environment 2024 23 citations ? Citation count from OpenAlex, updated daily. May differ slightly from the publisher's own count. Score: 65 ? 0–100 AI score estimating relevance to the microplastics field. Papers below 30 are filtered from public browse.
Limin Wang, Liyun Yin, Shuxin Li, Xu Liu, Liyun Yin, Liyun Yin, Liyun Yin, Yaotong Hao, Yaotong Hao, Shuxin Li, Liyun Yin, Shuxin Li, Liyun Yin, Yaotong Hao, Liyun Yin, Liyun Yin, Xu Liu, Xu Liu, Xu Liu, Shuxin Li, Yaqing Liu, Lirong Zuo, Lirong Zuo, Fadao Tai, Dongming Li Liyun Yin, Liyun Yin, Dongming Li Larry J. Young, Dongming Li Dongming Li

Summary

Adolescent mice exposed to polystyrene microplastics for 10 weeks showed reduced social behavior and lower levels of oxytocin -- a hormone important for social bonding -- in a key brain region. The microplastics damaged the gut lining and altered gut bacteria, and when researchers blocked the nerve connection between the gut and brain, the social behavior problems improved. This provides strong evidence that microplastics can affect brain function and social behavior through the gut-brain axis.

Polymers
Body Systems
Models

The rising global prevalence of microplastics (MPs) has highlighted their diverse toxicological effects. The oxytocin (OT) system in mammals, deeply intertwined with social behaviors, is recognized to be vulnerable to environmental stressors. We hypothesized that MP exposure might disrupt this system, a topic not extensively studied. We investigated the effects of MPs on behavioral neuroendocrinology via the gut-brain axis by exposing adolescent male C57BL/6 mice to varied sizes (5 μm and 50 μm) and concentrations (100 μg/L and 1000 μg/L) of polystyrene MPs over 10 weeks. The results demonstrated that exposure to 50 μm MPs significantly reduced colonic mucin production and induced substantial alterations in gut microbiota. Notably, the 50 μm-100 μg/L group showed a significant reduction in OT content within the medial prefrontal cortex and associated deficits in sociality, along with damage to the blood-brain barrier. Importantly, blocking the vagal pathway ameliorated these behavioral impairments, emphasizing the pivotal role of the gut-brain axis in mediating neurobehavioral outcomes. Our findings confirm the toxicity of MPs on sociality and the corresponding neuroendocrine systems, shedding light on the potential hazards and adverse effects of environmental MPs exposure on social behavior and neuroendocrine frameworks in social mammals, including humans.

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