Ueda Kazutaka, Karas Richard H
Molecular Cardiology Research Institute, Tufts Medical Center, Boston, MA 02111, USA.
Steroids. 2013 Jun;78(6):589-96. doi: 10.1016/j.steroids.2012.12.006. Epub 2012 Dec 29.
Estrogen receptors are classically known as ligand-activated transcription factors that regulate gene transcription in cells in response to hormone binding. In addition to this "genomic" signaling pathway, a "rapid, non-nuclear" signaling pathway mediated by cell membrane-associated estrogen receptors also has been recognized. Although for many years there was little evidence to support any physiological relevance of rapid-signaling, very recently evidence has been accumulating supporting the importance of the rapid, non-nuclear signaling as potentially critical for the protective effects of estrogen in the cardiovascular system. Better understanding of the rapid, non-nuclear signaling potentially provides an opportunity to design "pathway-specific" selective estrogen receptor modulators capable of differentially regulating non-nuclear vs. genomic effects that may prove useful ultimately as specific therapies for cardiovascular diseases.
雌激素受体传统上被认为是配体激活的转录因子,可响应激素结合来调节细胞中的基因转录。除了这种“基因组”信号通路外,由细胞膜相关雌激素受体介导的“快速、非核”信号通路也已得到认可。尽管多年来几乎没有证据支持快速信号传导具有任何生理相关性,但最近证据不断积累,支持快速、非核信号传导对雌激素在心血管系统中的保护作用可能至关重要。更好地理解快速、非核信号传导可能提供一个机会,来设计“通路特异性”选择性雌激素受体调节剂,其能够差异性地调节非核效应与基因组效应,最终可能被证明作为心血管疾病的特异性疗法是有用的。