2014
DOI: 10.1016/j.steroids.2014.08.017
|View full text |Cite
|
Sign up to set email alerts
|

Synthesis and biological evaluation of 11′ imidazolyl antiprogestins and mesoprogestins

Help me understand this report

Search citation statements

Order By: Relevance

Paper Sections

Select...
2
1
1
1

Citation Types

1
9
0

Year Published

2016
2016
2022
2022

Publication Types

Select...
4
1

Relationship

2
3

Authors

Journals

citations
Cited by 5 publications
(10 citation statements)
references
References 20 publications
1
9
0
Order By: Relevance
“…Our in vivo study revealed that EC313 blocked the estrogenicity of E2 on uterus and mammary gland proliferation including ductal length, terminal end bud development and induced apoptosis. This results were matched with our previous findings classified EC313 as a mesoprogestin [ 38 ]. The context dependent progesterone action might help to explain the observed effects of EC313 on T47D breast cancer cells and benign mouse mammary glands.…”
Section: Discussionsupporting
confidence: 93%
See 3 more Smart Citations
“…Our in vivo study revealed that EC313 blocked the estrogenicity of E2 on uterus and mammary gland proliferation including ductal length, terminal end bud development and induced apoptosis. This results were matched with our previous findings classified EC313 as a mesoprogestin [ 38 ]. The context dependent progesterone action might help to explain the observed effects of EC313 on T47D breast cancer cells and benign mouse mammary glands.…”
Section: Discussionsupporting
confidence: 93%
“…These in vitro data correlate with in vivo data in guinea pigs that characterize EC-317, as a very pure antagonist and EC313 as mesoprogestin with strong partial agonistic activity [ 31 ]. In the case EC312, the receptor binding studies does not correlate with our previously published in vivo studies in guinea pigs [ 38 ]. This might be due to the difference in binding preference as seen in in silico studies ( S1 Text , S1 Fig , S1 Table ) or preference in the recruitment of co-factor/co-repressor and exerting non-genomic action.…”
Section: Resultsmentioning
confidence: 61%
See 2 more Smart Citations
“…To this end, we performed genomic analysis in T47D xenografts treated with various SERMs (tamoxifen, bazedoxifene, raloxifene), selective ER degrader fluvestrant, PR agonists (progesterone, medroxy progesterone acetate (MPA) or synthetic progestin R5020), PR antagonists CDB4124 and CDB4453, and SPRM EC313 (Figure 3A ). CDB4124 and CDB4453 are highly-selective PR ligands that antagonize R5020-induced transcriptional activity and proliferation of T47D cells [ 45 48 ]. In contrast, EC313 is a SPRM engineered on a PR agonist molecular backbone [ 47 , 48 ].…”
Section: Resultsmentioning
confidence: 99%