Second-Generation Estrogen Receptor Down-Regulators for Medical Therapy
More effective than the first-generation commercial drug (Faslodex; fulvestrant) in suppressing tumor growth. Faslodex has poor bioavailability and must be administered by intramuscular injection. This is a significant barrier to achieving optimal therapeutic efficacy as an anticancer drug. Our second-generation SERD compounds are designed to have greater aqueous solubility and show more potent antitumor effects in preclinical experiments than Faslodex. May overcome endocrine resistance in breast cancer therapy. The estrogen receptor is often expressed in tumors with endocrine resistance to both antiestrogens (such as tamoxifen) and aromatase inhibitors. Hence, SERD compounds that can down-regulate estrogen receptors can be effective in overcoming endocrine resistance to both antiestrogens and to aromatase inhibitors.
These selective estrogen receptor down-regulators (SERDs) can be used as therapeutics for endocrine-sensitive and -resistant breast cancers.
Researchers in UCLA School of Medicine have developed a series of novel estrogen receptor antagonists that are very effective in inhibiting the growth of breast cancer. These unique, selective estrogen receptor down-regulators optimally target the estrogen receptor for degradation and elimination, thereby blocking downstream growth-promoting signaling pathways induced by estrogen receptors in breast cancer. These never before reported compounds are more potent than fulvestrant and are effective in endocrine-resistant disease models. They exhibit the proper biologic and pharmacologic profile to be developed as therapeutics for endocrine-sensitive and -resistant cancers in the clinic.
State Of Development Background Tech ID/UC Case 24862/2015-166-0 Related Cases 2015-166-0
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