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Bisphenol-A impairs synaptic formation and function by RGS4-mediated regulation of BDNF signaling in the cerebral cortex

Sung‐Ae Hyun, Moon Yi Ko, Sumi Jang, Byoung‐Seok Lee, Jaerang Rho, Kee K. Kim, Woo-Yang Kim, Minhan Ka

2022Disease Models & Mechanisms36 citationsDOIOpen Access PDF

Abstract

Bisphenol-A (BPA) is a representative endocrine disruptor, widely used in a variety of products including plastics, medical equipment and receipts. Hence, most people are exposed to BPA via the skin, digestive system or inhalation in everyday life. Furthermore, BPA crosses the blood-brain barrier and is linked to multiple neurological dysfunctions found in neurodegenerative and neuropsychological disorders. However, the mechanisms underlying BPA-associated neurological dysfunctions remain poorly understood. Here, we report that BPA exposure alters synapse morphology and function in the cerebral cortex. Cortical pyramidal neurons treated with BPA showed reduced size and number of dendrites and spines. The density of excitatory synapses was also decreased by BPA treatment. More importantly, we found that BPA disrupted normal synaptic transmission and cognitive behavior. RGS4 and its downstream BDNF/NTRK2 pathway appeared to mediate the effect of BPA on synaptic and neurological function. Our findings provide molecular mechanistic insights into anatomical and physiological neurotoxic consequences related to a potent endocrine modifier.

Topics & Concepts

NeuroscienceBisphenol ACerebral cortexFunction (biology)BiologyPsychologyCell biologyChemistryEpoxyOrganic chemistryEffects and risks of endocrine disrupting chemicalsAnimal testing and alternativesMicroplastics and Plastic Pollution
Bisphenol-A impairs synaptic formation and function by RGS4-mediated regulation of BDNF signaling in the cerebral cortex | Litcius