2014
DOI: 10.1016/j.bbagen.2014.04.001
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A mechanistic and structural investigation of modified derivatives of the diaryltriazine class of NNRTIs targeting HIV-1 reverse transcriptase

Abstract: Background Non-nucleoside reverse transcriptase inhibitors (NNRTIs) are vital in treating HIV-1 infection by inhibiting reverse transcriptase (RT). Drug toxicity and resistance drive the need for effective new inhibitors with improved physiochemical properties and potent antiviral activity. Computer-aided and structure-based drug design have guided the addition of solubilizing substituents to the diaryltriazine scaffold. These derivatives have markedly improved solubility and maintain low nanomolar antiviral a… Show more

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Cited by 12 publications
(14 citation statements)
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References 43 publications
(78 reference statements)
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“…The analogue with the cyanovinyl group replaced by a methyl group has similar solubility (15.3 μg/mL); the crystal structure for its complex with WT RT was subsequently determined and showed it was shifted 3-Å deeper into the NNRTI binding site than its analogue lacking the morpholinylpropoxy group. 70 The 2,6-difluoro-4-methyl analogue 34 is also interesting and more soluble at 22.9 μg/mL; it is extraordinarily potent towards the WT virus with an EC 50 of 0.190 nM (190 picomolar), while it shows 70 nM potency towards the double variant, but it oddly, like 33 , is significantly less potent at 350 nM towards the Y181C variant. Typically, the activity of an NNRTI is less towards the K103N/Y181C strain than it is towards either constituent single variant.…”
Section: Aqueous Solubilitymentioning
confidence: 99%
“…The analogue with the cyanovinyl group replaced by a methyl group has similar solubility (15.3 μg/mL); the crystal structure for its complex with WT RT was subsequently determined and showed it was shifted 3-Å deeper into the NNRTI binding site than its analogue lacking the morpholinylpropoxy group. 70 The 2,6-difluoro-4-methyl analogue 34 is also interesting and more soluble at 22.9 μg/mL; it is extraordinarily potent towards the WT virus with an EC 50 of 0.190 nM (190 picomolar), while it shows 70 nM potency towards the double variant, but it oddly, like 33 , is significantly less potent at 350 nM towards the Y181C variant. Typically, the activity of an NNRTI is less towards the K103N/Y181C strain than it is towards either constituent single variant.…”
Section: Aqueous Solubilitymentioning
confidence: 99%
“…“Het‐NH‐Ph” NNRTIs 72 , 73 showed substantially improved solubility compared with lead molecule 71 and the structurally related drugs ETR and RPV, while retaining low‐nanomolar anti‐HIV activity . DATA derivatives 74 and 75 also showed low‐nanomolar activity similar to that of ETR against WT HIV‐1 and key resistant strains . Subsequently, the determined cocrystal structures of 74 and 76 bound to RT revealed several salient features considered to be related to the substantial improvement of solubility (Figure ) .…”
Section: Exploitation Of Solvent‐exposed Regions For Structure‐basedmentioning
confidence: 97%
“…Subsequently, the determined cocrystal structures of 74 and 76 bound to RT revealed several salient features considered to be related to the substantial improvement of solubility (Figure ) . Specifically, the solubility enhancements appeared to result from strategic placement of the novel morpholinylalkoxy moiety at another RT/solvent interface (the entrance channel near Glu138) of the NNRTIs binding pocket …”
Section: Exploitation Of Solvent‐exposed Regions For Structure‐basedmentioning
confidence: 99%
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