FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2009936700> ?p ?o ?g. }

• W2009936700 endingPage "4339" @default.
• W2009936700 startingPage "4335" @default.
• W2009936700 abstract "The pregnene derivatives with modifications at the 17,20-side chain and D-ring were synthesized and evaluated as inhibitors of human testicular 17α-hydroxylase/C17,20-lyase. The results demonstrate that compounds which have 20-substituents with moderate to strong dipole properties, such as 20-oxime (3, 20), 20β-ol (24, 30), and 20β-carboxaldehyde (27), are potent inhibitors of this enzyme complex. The 20-substituents with hydrophobic property were devoid of inhibitory activity, e.g., the dimethylhydrazones 8 and 9. The 16-ene together with 20-oxime (20) showed the most potent inhibition of this enzyme complex, whereas 17(20)-ene modification as in 17(20)-ene-20-carbonitrile (14) did not increase activity in comparison to the 20β-carbonitrile (16). The bioisostere of 27 with 20-aza (19) also reduced the inhibitory activity. The results showed that isomeric configurations at the 20-position of some steroidal compounds are important factors which influence the potency of the inhibition significantly (e.g., 20β-ols 24 and 30 were 3−5-fold more potent than 20α-ols 23 and 29). As expected, some compounds based on the pregn-5-en-3β-ol skeleton, which is similar to the natural substrate of human testicular 17α-hydroxylase/C17,20-lyase in A- and B-rings, showed more potent inhibition than similar compounds which are based on the pregn-4-en-3-one skeleton (e.g., 23−25 compared to 29−31). These results suggest that A- and B-rings make significant contributions to the binding of these steroidal compounds to the 17α-hydroxylase and C17,20-lyase. In comparison to ketoconazole, a nonsteroidal inhibitor of 17α-hydroxylase and C17,20-lyase which has been used in the treatment of prostatic cancer, the steroidal compounds 20, 24, and 27 demonstrate more potent inhibition for this enzyme complex. These inhibitors warrant further investigation in biological systems. The structural features of these compounds may serve as leads in the design of new inhibitors." @default.
• W2009936700 created "2016-06-24" @default.
• W2009936700 creator A5000820552 @default.
• W2009936700 creator A5011831156 @default.
• W2009936700 creator A5033224484 @default.
• W2009936700 creator A5091426157 @default.
• W2009936700 date "1996-01-01" @default.
• W2009936700 modified "2023-10-17" @default.
• W2009936700 title "Synthesis and Evaluation of Pregnane Derivatives as Inhibitors of Human Testicular 17α-Hydroxylase/C_17,20-Lyase^," @default.
• W2009936700 cites W1775749144 @default.
• W2009936700 cites W1977970500 @default.
• W2009936700 cites W1984313455 @default.
• W2009936700 cites W1986232120 @default.
• W2009936700 cites W1993808852 @default.
• W2009936700 cites W2000824159 @default.
• W2009936700 cites W2014592245 @default.
• W2009936700 cites W2022823613 @default.
• W2009936700 cites W2027081726 @default.
• W2009936700 cites W2064360128 @default.
• W2009936700 cites W2075646385 @default.
• W2009936700 cites W2092882807 @default.
• W2009936700 cites W2094011164 @default.
• W2009936700 cites W2313355038 @default.
• W2009936700 cites W2327532927 @default.
• W2009936700 cites W2328230950 @default.
• W2009936700 cites W2411272933 @default.
• W2009936700 cites W2605152026 @default.
• W2009936700 doi "https://doi.org/10.1021/jm960245f" @default.
• W2009936700 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/8863811" @default.
• W2009936700 hasPublicationYear "1996" @default.
• W2009936700 type Work @default.
• W2009936700 sameAs 2009936700 @default.
• W2009936700 citedByCount "38" @default.
• W2009936700 countsByYear W20099367002012 @default.
• W2009936700 countsByYear W20099367002013 @default.
• W2009936700 countsByYear W20099367002014 @default.
• W2009936700 countsByYear W20099367002015 @default.
• W2009936700 countsByYear W20099367002023 @default.
• W2009936700 crossrefType "journal-article" @default.
• W2009936700 hasAuthorship W2009936700A5000820552 @default.
• W2009936700 hasAuthorship W2009936700A5011831156 @default.
• W2009936700 hasAuthorship W2009936700A5033224484 @default.
• W2009936700 hasAuthorship W2009936700A5091426157 @default.
• W2009936700 hasConcept C114373084 @default.
• W2009936700 hasConcept C178790620 @default.
• W2009936700 hasConcept C181199279 @default.
• W2009936700 hasConcept C185592680 @default.
• W2009936700 hasConcept C202751555 @default.
• W2009936700 hasConcept C2776980637 @default.
• W2009936700 hasConcept C2777269803 @default.
• W2009936700 hasConcept C2779095896 @default.
• W2009936700 hasConcept C2779648554 @default.
• W2009936700 hasConcept C2780378348 @default.
• W2009936700 hasConcept C2780655410 @default.
• W2009936700 hasConcept C55493867 @default.
• W2009936700 hasConcept C57992300 @default.
• W2009936700 hasConcept C71240020 @default.
• W2009936700 hasConceptScore W2009936700C114373084 @default.
• W2009936700 hasConceptScore W2009936700C178790620 @default.
• W2009936700 hasConceptScore W2009936700C181199279 @default.
• W2009936700 hasConceptScore W2009936700C185592680 @default.
• W2009936700 hasConceptScore W2009936700C202751555 @default.
• W2009936700 hasConceptScore W2009936700C2776980637 @default.
• W2009936700 hasConceptScore W2009936700C2777269803 @default.
• W2009936700 hasConceptScore W2009936700C2779095896 @default.
• W2009936700 hasConceptScore W2009936700C2779648554 @default.
• W2009936700 hasConceptScore W2009936700C2780378348 @default.
• W2009936700 hasConceptScore W2009936700C2780655410 @default.
• W2009936700 hasConceptScore W2009936700C55493867 @default.
• W2009936700 hasConceptScore W2009936700C57992300 @default.
• W2009936700 hasConceptScore W2009936700C71240020 @default.
• W2009936700 hasIssue "21" @default.
• W2009936700 hasLocation W20099367001 @default.
• W2009936700 hasLocation W20099367002 @default.
• W2009936700 hasOpenAccess W2009936700 @default.
• W2009936700 hasPrimaryLocation W20099367001 @default.
• W2009936700 hasRelatedWork W1972711655 @default.
• W2009936700 hasRelatedWork W2001505620 @default.
• W2009936700 hasRelatedWork W2009936700 @default.
• W2009936700 hasRelatedWork W2015887859 @default.
• W2009936700 hasRelatedWork W2020980248 @default.
• W2009936700 hasRelatedWork W2026967030 @default.
• W2009936700 hasRelatedWork W2097588642 @default.
• W2009936700 hasRelatedWork W2164811489 @default.
• W2009936700 hasRelatedWork W2781021236 @default.
• W2009936700 hasRelatedWork W2950703075 @default.
• W2009936700 hasVolume "39" @default.
• W2009936700 isParatext "false" @default.
• W2009936700 isRetracted "false" @default.
• W2009936700 magId "2009936700" @default.
• W2009936700 workType "article" @default.