Benzophenone-3 Passes Through the Blood-Brain Barrier, Increases the Level of Extracellular Glutamate, and Induces Apoptotic Processes in the Hippocampus and Frontal Cortex of Rats

Author:

Pomierny Bartosz1,Krzyżanowska Weronika1,Broniowska Żaneta1,Strach Beata1,Bystrowska Beata2,Starek-Świechowicz Beata1,Maciejska Alicja1,Skórkowska Alicja1,Wesołowska Julita3,Walczak Maria2,Budziszewska Bogusława1

Affiliation:

1. Department of Biochemical Toxicology

2. Department of Toxicology, Chair of Toxicology, Medical College, Jagiellonian University, 30-688 Kraków, Poland

3. Laboratory for In vivo and In Vitro Imaging, Maj Institute of Pharmacology, Polish Academy of Sciences, 31-343 Kraków, Poland

Abstract

Abstract Benzophenone-3 is the most commonly used UV filter. It is well absorbed through the skin and gastrointestinal tract. Its best-known side effect is the impact on the function of sex hormones. Little is known about the influence of BP-3 on the brain. The aim of this study was to show whether BP-3 crosses the blood-brain barrier (BBB), to determine whether it induces nerve cell damage in susceptible brain structures, and to identify the mechanism of its action in the central nervous system. BP-3 was administered dermally during the prenatal period and adulthood to rats. BP-3 effect on short-term and spatial memory was determined by novel object and novel location recognition tests. BP-3 concentrations were assayed in the brain and peripheral tissues. In brain structures, selected markers of brain damage were measured. The study showed that BP-3 is absorbed through the rat skin, passes through the BBB. BP-3 raised oxidative stress and induced apoptosis in the brain. BP-3 increased the concentration of extracellular glutamate in examined brain structures and changed the expression of glutamate transporters. BP-3 had no effect on short-term memory but impaired spatial memory. The present study showed that dermal BP-3 exposure may cause damage to neurons what might be associated with the increase in the level of extracellular glutamate, most likely evoked by changes in the expression of GLT-1 and xCT glutamate transporters. Thus, exposure to BP-3 may be one of the causes that increase the risk of developing neurodegenerative diseases.

Funder

National Science Centerof Poland

Publisher

Oxford University Press (OUP)

Subject

Toxicology

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