FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2527838037> ?p ?o ?g. }

• W2527838037 endingPage "201" @default.
• W2527838037 startingPage "190" @default.
• W2527838037 abstract "To further explore the chemical space around the entrance channel of HIV-1 reverse transcriptase (RT), a series of novel indolylarylsulfones (IASs) bearing N-substituted piperidine at indole-2-carboxamide were identified as potent HIV NNRTIs by structure-guided scaffold morphing and fragment rearrangement. All the IASs exhibited moderate to excellent potency against wild-type HIV-1 with EC50 values ranging from 0.62 μM to 0.006 μM 8 (EC50 = 6 nM) and 18 (EC50 = 9 nM) were identified as the most potent compounds, which were more active than NVP and DLV, and reached the same order of EFV and ETV. Furthermore, most compounds maintained high activity agaist various single HIV-1 mutants (L100I, K103N, E138K, Y181C) as well as one double mutant (F227L/V106A) with EC50 values in low-micromolar to double-digit nanomolar concentration ranges. Especially, 8 displayed outstanding potency against L100I (EC50 = 17 nM with a 2.8-fold resistance ratio) and 18 was relatively more potent to E138K mutant (EC50 = 43 nM with a 4.7-fold resistance ratio). Preliminary SARs and molecular modeling studies were also discussed in detail, which may provide valuable insights for further optimization." @default.
• W2527838037 created "2016-10-14" @default.
• W2527838037 creator A5016395926 @default.
• W2527838037 creator A5016741562 @default.
• W2527838037 creator A5033988281 @default.
• W2527838037 creator A5040662398 @default.
• W2527838037 creator A5044707650 @default.
• W2527838037 creator A5047395375 @default.
• W2527838037 creator A5054111597 @default.
• W2527838037 creator A5059468550 @default.
• W2527838037 creator A5080351994 @default.
• W2527838037 creator A5081021967 @default.
• W2527838037 creator A5081479819 @default.
• W2527838037 creator A5084866278 @default.
• W2527838037 date "2017-01-01" @default.
• W2527838037 modified "2023-10-14" @default.
• W2527838037 title "Discovery of novel piperidine-substituted indolylarylsulfones as potent HIV NNRTIs via structure-guided scaffold morphing and fragment rearrangement" @default.
• W2527838037 cites W1493703283 @default.
• W2527838037 cites W1911648303 @default.
• W2527838037 cites W1969806407 @default.
• W2527838037 cites W1970573493 @default.
• W2527838037 cites W1972597223 @default.
• W2527838037 cites W1985321285 @default.
• W2527838037 cites W1988775904 @default.
• W2527838037 cites W1988847244 @default.
• W2527838037 cites W1991519292 @default.
• W2527838037 cites W2001473040 @default.
• W2527838037 cites W2006425659 @default.
• W2527838037 cites W2008791719 @default.
• W2527838037 cites W2018448679 @default.
• W2527838037 cites W2023878752 @default.
• W2527838037 cites W2024296689 @default.
• W2527838037 cites W2031081818 @default.
• W2527838037 cites W2031991206 @default.
• W2527838037 cites W2035126479 @default.
• W2527838037 cites W2037152211 @default.
• W2527838037 cites W2038163403 @default.
• W2527838037 cites W2038775337 @default.
• W2527838037 cites W2039971030 @default.
• W2527838037 cites W2045043030 @default.
• W2527838037 cites W2045778002 @default.
• W2527838037 cites W2048608017 @default.
• W2527838037 cites W2049421477 @default.
• W2527838037 cites W2049924143 @default.
• W2527838037 cites W2056072330 @default.
• W2527838037 cites W2062231842 @default.
• W2527838037 cites W2066568298 @default.
• W2527838037 cites W2067830848 @default.
• W2527838037 cites W2071059013 @default.
• W2527838037 cites W2081664414 @default.
• W2527838037 cites W2084302660 @default.
• W2527838037 cites W2091184487 @default.
• W2527838037 cites W2092762437 @default.
• W2527838037 cites W2103389647 @default.
• W2527838037 cites W2104410034 @default.
• W2527838037 cites W2109038325 @default.
• W2527838037 cites W2121517775 @default.
• W2527838037 cites W2132172963 @default.
• W2527838037 cites W2140534639 @default.
• W2527838037 cites W2206408428 @default.
• W2527838037 cites W2289318286 @default.
• W2527838037 cites W2317782935 @default.
• W2527838037 cites W2320039445 @default.
• W2527838037 cites W2337272231 @default.
• W2527838037 cites W2395531268 @default.
• W2527838037 cites W2918044000 @default.
• W2527838037 cites W2949931593 @default.
• W2527838037 cites W4239113273 @default.
• W2527838037 doi "https://doi.org/10.1016/j.ejmech.2016.10.009" @default.
• W2527838037 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/27750153" @default.
• W2527838037 hasPublicationYear "2017" @default.
• W2527838037 type Work @default.
• W2527838037 sameAs 2527838037 @default.
• W2527838037 citedByCount "17" @default.
• W2527838037 countsByYear W25278380372017 @default.
• W2527838037 countsByYear W25278380372018 @default.
• W2527838037 countsByYear W25278380372019 @default.
• W2527838037 countsByYear W25278380372020 @default.
• W2527838037 countsByYear W25278380372021 @default.
• W2527838037 countsByYear W25278380372022 @default.
• W2527838037 countsByYear W25278380372023 @default.
• W2527838037 crossrefType "journal-article" @default.
• W2527838037 hasAuthorship W2527838037A5016395926 @default.
• W2527838037 hasAuthorship W2527838037A5016741562 @default.
• W2527838037 hasAuthorship W2527838037A5033988281 @default.
• W2527838037 hasAuthorship W2527838037A5040662398 @default.
• W2527838037 hasAuthorship W2527838037A5044707650 @default.
• W2527838037 hasAuthorship W2527838037A5047395375 @default.
• W2527838037 hasAuthorship W2527838037A5054111597 @default.
• W2527838037 hasAuthorship W2527838037A5059468550 @default.
• W2527838037 hasAuthorship W2527838037A5080351994 @default.
• W2527838037 hasAuthorship W2527838037A5081021967 @default.
• W2527838037 hasAuthorship W2527838037A5081479819 @default.
• W2527838037 hasAuthorship W2527838037A5084866278 @default.
• W2527838037 hasConcept C104317684 @default.
• W2527838037 hasConcept C143065580 @default.
• W2527838037 hasConcept C156719811 @default.
• W2527838037 hasConcept C159047783 @default.

• next