GPER
G protein-coupled estrogen receptor 1, also known as G protein-coupled receptor 30, is a protein that in humans is encoded by the GPER gene. GPER binds to and is activated by the female sex hormone estradiol and is responsible for some of the rapid effects that estradiol has on cells.
Discovery
The classical estrogen receptors first characterized in 1958 are water-soluble proteins located in the interior of cells that are activated by estrogenenic hormones such as estradiol and several of its metabolites such as estrone or estriol. These proteins belong to the nuclear hormone receptor class of transcription factors that regulate gene transcription. Since it takes time for genes to be transcribed into RNA and translated into protein, the effects of estrogens binding to these classical estrogen receptors is delayed. However, estrogens are also known to have effects that are too fast to be caused by regulation of gene transcription. In 2005, it was discovered that a member of the G protein-coupled receptor family, GPR30 also binds with high affinity to estradiol and is responsible in part for the rapid non-genomic actions of estradiol. Based on its ability to bind estradiol, GPR30 was renamed as G protein-coupled estrogen receptor. GPER is localized in the plasma membrane but is predominantly detected in the endoplasmic reticulum.Ligands
GPER binds estradiol with high affinity though not other endogenous estrogens, such as estrone or estriol, nor other endogenous steroids, including progesterone, testosterone, and cortisol. Although potentially involved in signaling by aldosterone, GPER does not show any detectable binding towards aldosterone. Niacin and nicotinamide bind to the receptor in vitro with very low affinity. CCL18 has been identified as an endogenous antagonist of the GPER. GPER-selective ligands include the agonist G-1 and the antagonists G15 and G36.Agonists
- 2-Methoxyestradiol
- 2,2',5'-PCB-4-OH
- Afimoxifene
- Aldosterone
- Atrazine
- Bisphenol A
- Daidzein
- DDT
- Diarylpropionitrile
- Equol
- Estradiol
- Ethynylestradiol
- Fulvestrant )
- G-1
- Genistein
- GPER-L1
- GPER-L2
- Hydroxytyrosol
- Kepone
- LNS8801
- Niacin
- Nicotinamide
- Nonylphenol
- Oleuropein
- Protocatechuic aldehyde
- Propylpyrazoletriol
- Quercetin
- Raloxifene
- Resveratrol
- STX
- Tamoxifen
- Tectoridin
Antagonists
- CCL18
- Estriol
- G15
- G36
- MIBE
Unknown
- Diethylstilbestrol
- Zearalenone
Non-ligand
- 17α-Estradiol
- Estrone
Function
Role in cancer
GPER expression has been studied in cancer using immunohistochemical and transcriptomic approaches, and has been detected in: colon, lung, melanoma, pancreatic, breast, ovarian, and testicular cancer.Many groups have demonstrated that GPER signaling is tumor suppressive in cancers that are not traditionally hormone responsive, including melanoma, pancreatic, lung and colon cancer. Additionally, many groups have demonstrated that GPER activation is also tumor suppressive in cancers that are classically considered sex hormone responsive, including endometrial cancer, ovarian cancer, prostate cancer, and Leydig cell tumors. Although GPER signaling was originally thought to be tumor promoting in some breast cancer models, subsequent reports show that GPER signaling inhibits breast cancer. Consistent with this, recent studies showed that the presence of GPER protein in human breast cancer tissue correlates with longer survival. In summary, many independent groups have demonstrated that GPER activation may be a therapeutically useful mechanism for a wide range of cancer types.
Linnaeus Therapeutics is currently running NCI clinical trial using GPER agonist, LNS8801, as monotherapy and in combination with the immune checkpoint inhibitor, pembrolizumab, for the treatment of multiple solid tumor malignancies. Activation of GPER with LNS8801 has demonstrated efficacy in humans in cutaneous melanoma, uveal melanoma, lung cancer, neuroendocrine cancer, colorectal cancer, and other PD-1 inhibitor refractory cancers.