Bioisosteric modification of PETT-HIV-1 RT-inhibitors: synthesis and biological evaluation

M Högberg, P Engelhardt, L Vrang, H Zhang

Index: Hoegberg, Marita; Engelhardt, Per; Vrang, Lotta; Zhang, Hong Bioorganic and Medicinal Chemistry Letters, 2000 , vol. 10, # 3 p. 265 - 268

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Citation Number: 35

Abstract

Bioisosteric substitution of the thiourea (3, 5, 7, 9) and urea (10) moiety of PETT compounds with sulfamide (1), cyanoguanidine (2, 4) and guanidine (6, 8) functionalities, and replacement of the phenethyl group with benzoylethyl group (compounds 11–20) have been studied. Synthesis and antiviral activities are described.

Induction of apoptosis promoted by Bang52; a small molecule that downregulates Bcl-x L

[Rossi, Matteo; Bang, Jeong-kyu; Mazur, Sharlyn; Iera, Jaclyn A.; Phillips, Darren C.; Zambetti, Gerard P.; Appella, Daniel H. Bioorganic and Medicinal Chemistry Letters, 2009 , vol. 19, # 9 p. 2429 - 2434]

Bioisosteric modification of PETT-HIV-1 RT-inhibitors: synthesis and biological evaluation

Abstract

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