2020
DOI: 10.1016/j.psyneuen.2020.104830
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Bazedoxifene – a promising brain active SERM that crosses the blood brain barrier and enhances spatial memory

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Cited by 9 publications
(3 citation statements)
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“…All in all, BZX lacks breast and endometrial side effects, and thereby has an improved safety profile [139]. BZX crosses the blood-brain barrier (BBB), and enhances spatial memory in OVX rats, a model of postmenopausal estrogen decline [140].…”
Section: Selective Estrogen-receptor Modulators (Serms)mentioning
confidence: 99%
“…All in all, BZX lacks breast and endometrial side effects, and thereby has an improved safety profile [139]. BZX crosses the blood-brain barrier (BBB), and enhances spatial memory in OVX rats, a model of postmenopausal estrogen decline [140].…”
Section: Selective Estrogen-receptor Modulators (Serms)mentioning
confidence: 99%
“…In the resulting antagonist conformation, the ER LBD exhibits a different coregulator recruitment profile with a preference for corepressor binding. , Therein, ER modulation by SERMs varies in different tissues, which is rationalized by differential coregulator equipment of different cell types and tissues. They act as ER antagonists in breast tissue, as partial agonists in bone, and activity in endometrium varies depending on the SERM. , Brain penetration and activation of ER signaling in the CNS were recently demonstrated for the SERM bazedoxifene ( 108 ), which could hence serve as an attractive tool to further probe ER modulation in neurodegeneration. Following the SERMs as ER modulatory drugs, the antiestrogen fulvestrant ( 110 ) acting as a selective estrogen receptor degrader (SERD) has introduced another strategy to inhibit ER activity, and several further SERDs have been developed of which elacestrant ( 111 ) was found to cross the blood–brain barrier suggesting it as a potential tool to study inhibition of ER signaling in the CNS.…”
Section: Nuclear Receptors and Neurodegenerationmentioning
confidence: 99%
“…They act as ER antagonists in breast tissue, as partial agonists in bone, and activity in endometrium varies depending on the SERM. 532,533 Brain penetration and activation of ER signaling in the CNS were recently demonstrated 536 for the SERM bazedoxifene (108), which could hence serve as an attractive tool to further probe ER modulation in neurodegeneration. Following the SERMs as ER modulatory drugs, the antiestrogen fulvestrant (110) 537 acting as a selective estrogen receptor degrader (SERD) has introduced another strategy to inhibit ER activity, and several further SERDs have been developed 533 of which elacestrant (111) 538 was found to cross the blood−brain barrier 539 suggesting it as a potential tool to study inhibition of ER signaling in the CNS.…”
Section: Nurr1 In Admentioning
confidence: 99%