Molecular Hybridization-Inspired Optimization of Diarylbenzopyrimidines as HIV-1 Nonnucleoside Reverse Transcriptase Inhibitors with Improved Activity against K103N and E138K Mutants and Pharmacokinetic Profiles

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المؤلفون: Yali Sang; Sheng Han; Yuan Tao; Erik De Clercq; Fen-Er Chen; Yan Wu; Chunlin Zhuang; Christophe Pannecouque
الموضوع:
0301 basic medicine; NNRTI; STRUCTURAL BASIS; PK; Efavirenz; Anti-HIV Agents; 030106 microbiology; Mutant; Etravirine; Chemistry, Medicinal; Pharmacology; RILPIVIRINE; Structure-Activity Relationship; 03 medical and health sciences; chemistry.chemical_compound; Pharmacokinetics; reverse transcriptase; medicine; Animals; Humans; Pharmacology & Pharmacy; BIOLOGICAL EVALUATION; WILD-TYPE; Cytotoxicity; Science & Technology; Chemistry; HIGHLY POTENT; diarylbenzopyrimidines; IMMUNODEFICIENCY-VIRUS TYPE-1; EFAVIRENZ DMP-266; Reverse transcriptase; Rats; Bioavailability; Molecular Docking Simulation; Pyrimidines; 030104 developmental biology; Infectious Diseases; DISCOVERY; Microsomes, Liver; Microsome; HIV-1; Reverse Transcriptase Inhibitors; COLORIMETRIC ASSAY; Life Sciences & Biomedicine; molecular hybridization; RESISTANCE; medicine.drug
اللغة:
English
الدخول الالكتروني :
https://explore.openaire.eu/search/publication?articleId=doi_dedup___::7a2d2a66cafd78386a8968a1eb75d60b
https://lirias.kuleuven.be/handle/20.500.12942/687834

معلومة اضافية
- بيانات النشر:
  AMER CHEMICAL SOC, 2020.
- الموضوع:
  2020
- نبذة مختصرة :
  Molecular hybridization is a powerful strategy in drug discovery. A series of novel diarylbenzopyrimidine (DABP) analogues were developed by the hybridization of FDA-approved drugs etravirine (ETR) and efavirenz (EFV) as potential HIV-1 nonnucleoside reverse transcriptase inhibitors (NNRTIs). Substituent modifications resulted in the identification of new DABPs with the combination of the strengths of the two drugs, especially compound 12d, which showed promising activity toward the EFV-resistant K103N mutant. 12d also had a favorable pharmacokinetic (PK) profile with liver microsome clearances of 14.4 μL/min/mg (human) and 33.2 μL/min/mg (rat) and an oral bioavailability of 15.5% in rat. However, its activity against the E138K mutant was still unsatisfactory; E138K is the most prevalent NNRTI resistance-associated mutant in ETR treatment. Further optimizations resulted in a highly potent compound (12z) with no substituents on the phenyl ring and a 2-methyl-6-nitro substitution pattern on the 4-cyanovinyl-2,6-disubstitued phenyl motif. The antiviral activity of this compound was much higher than those of ETR and EFV against the WT, E138K, and K103N variants (EC50 = 3.4, 4.3, and 3.6 nM, respectively), and the cytotoxicity was decreased while the selectivity index (SI) was increased. In particular, this compound exhibited acceptable intrinsic liver microsome stability (human, 34.5 μL/min/mg; rat, 33.2 μL/min/mg) and maintained the good PK profile of its parent compound EFV and showed an oral bioavailability of 16.5% in rat. Molecular docking and structure-activity relationship (SAR) analysis provided further insights into the binding of the DABPs with HIV-1 reverse transcriptase and provided a deeper understanding of the key structural features responsible for their interactions. ispartof: ACS INFECTIOUS DISEASES vol:6 issue:5 pages:787-801 ispartof: location:United States status: published
- File Description:
  Print-Electronic
- Rights:
  OPEN
- الرقم المعرف:
  edsair.doi.dedup.....7a2d2a66cafd78386a8968a1eb75d60b

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Molecular Hybridization-Inspired Optimization of Diarylbenzopyrimidines as HIV-1 Nonnucleoside Reverse Transcriptase Inhibitors with Improved Activity against K103N and E138K Mutants and Pharmacokinetic Profiles

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