Litcius/Paper detail

Myricetin suppresses traumatic brain injury-induced inflammatory response via EGFR/AKT/STAT pathway

Chenxing Wang, Siguang Ouyang, Xingjia Zhu, Yi Jiang, Zhichao Lu, Peipei Gong

2023Scientific Reports28 citationsDOIOpen Access PDF

Abstract

Traumatic brain injury (TBI) is a common disease in neurosurgery with a high fatality and disability rate which imposes a huge burden on society and patient's family. Inhibition of neuroinflammation caused by microglia activation is a reasonable strategy to promote neurological recovery after TBI. Myricetin is a natural flavonoid that has shown good therapeutic effects in a variety of neurological disease models, but its therapeutic effect on TBI is not clear. We demonstrated that intraperitoneal injection of appropriate doses of myricetin significantly improved recovery of neurological function after TBI in Sprague Dawley rats and inhibited excessive inflammatory responses around the lesion site. Myricetin dramatically reduced the expression of toxic microglia markers generated by TBI and LPS, according to the outcomes of in vivo and in vitro tests. In particular, the expression of inducible nitric oxide synthase, cyclooxygenase 2, and some pro-inflammatory cytokines was reduced, which protected learning and memory functions in TBI rats. Through network pharmacological analysis, we found that myricetin may inhibit microglia hyperactivation through the EGFR-AKT/STAT pathway. These findings imply that myricetin is a promising treatment option for the management of neuroinflammation following TBI.

Topics & Concepts

statProtein kinase BMedicineInterleukin 6Signal transductionTraumatic brain injuryMyricetinProinflammatory cytokineInflammatory responseCancer researchInflammationSTAT3ChemistryBiologyInternal medicineCell biologyPsychiatryAntioxidantKaempferolBiochemistryQuercetinTraumatic Brain Injury and Neurovascular DisturbancesNeuroinflammation and Neurodegeneration MechanismsLong-Term Effects of COVID-19
Myricetin suppresses traumatic brain injury-induced inflammatory response via EGFR/AKT/STAT pathway | Litcius