摘要
All synthetic and natural estrogen receptor agonists, in- cluding the most potent physiological molecule estrogen or estradiol (E2), work typically via activation of nuclear estrogen receptor alpha (ERα) and estrogen receptor beta (ERβ). Both ERα and ERβ modulate the expression of a variety of genes in the cells. Neurons and glial cells express ERa and ERβ. Many studies so far from our and other laboratories have firmly established the mode of actions that ERα and ERβ agonists are very promising anti-inflammatory and neuroprotective agents in the treatment of neurodegenera- rive diseases and injuries including spinal cord injury (SCI) (Chakrabarti et al., 2014a).
All synthetic and natural estrogen receptor agonists, in- cluding the most potent physiological molecule estrogen or estradiol (E2), work typically via activation of nuclear estrogen receptor alpha (ERα) and estrogen receptor beta (ERβ). Both ERα and ERβ modulate the expression of a variety of genes in the cells. Neurons and glial cells express ERa and ERβ. Many studies so far from our and other laboratories have firmly established the mode of actions that ERα and ERβ agonists are very promising anti-inflammatory and neuroprotective agents in the treatment of neurodegenera- rive diseases and injuries including spinal cord injury (SCI) (Chakrabarti et al., 2014a).
基金
supported in part by the grants from the South Carolina Spinal Cord Injury Research Fund(SC SCIRF-2015-I-01,Columbia,SC,USA)
the United Soybean Board(USB,Chesterfield,MO,USA)to SKR
