Inhibition of multiple phases of human immunodeficiency virus type 1 replication by a dithiane compound that attacks the conserved zinc fingers of retroviral nucleocapsid proteins

Rice, William G.; Baker, David C.; Schaeffer, Catherine A.; Graham, Lisa M.; Bu, Ming; Terpening, S J; Clanton, David J.; Schultz, Robert J.; Bader, John P.; Buckheit, Robert W.; Field, Lyndsay; Singh, Parmit K.; Turpin, Jim A.

doi:10.1128/aac.41.2.419

Cited by 90 publications

(73 citation statements)

References 48 publications

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“…Because of the critical role of the cysteines in the zinc fingers, covalent binding zinc ejectors are not susceptible to the development of resistance (Jenkins et al, 2010). Various categories of compounds in this class were reported during the 1990s, including 3-nitrosobenzamide (NOBA) (Rice et al, 1993), 2,2’-dithiobisbenzamide (DIBA) (Rice et al, 1995), cyclic 2,2’- dithiobisbenzamide (Witvrouw et al, 1997), 1,2-dithiane-4,5-diol-1,1-dioxide (Rice et al, 1997a), azadicarbonamide (ADA) (Rice et al, 1997b) and pyridinioalkanoyl 2-mercaptobenzamide thioesters (PATE) (Turpin et al, 1999). The structure and activity of these zinc ejectors has been reviewed by Rocquigny et al (de Rocquigny et al, 2008).…”

Section: Zinc Finger Bindersmentioning

confidence: 99%

Advances in targeting nucleocapsid–nucleic acid interactions in HIV-1 therapy

Garg

Torbett

2014

Virus Research

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The continuing challenge of HIV-1 treatment resistance in patients creates a need for the development of new antiretroviral inhibitors. The HIV nucleocapsid (NC) protein is a potential therapeutic target. NC is necessary for viral RNA packaging and in the early stages of viral infection. The high level of NC amino acid conservation among all HIV-1 clades suggests a low tolerance for mutations. Thus, NC mutations that could arise during inhibitor treatment to provide resistance may render the virus less fit. Disruption of NC function provides a unique opportunity to strongly dampen replication at multiple points during the viral life cycle with a single inhibitor. Although NC exhibits desirable features for a potential antiviral target, the structural flexibility, size, and the presence of two zinc fingers makes small molecule targeting of NC a challenging task. In this review, we discuss the recent advances in strategies to develop inhibitors of NC function and present a perspective on potential novel approaches that may help to overcome some of the current challenges in the field.

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Section: Zinc Finger Bindersmentioning

confidence: 99%

Advances in targeting nucleocapsid–nucleic acid interactions in HIV-1 therapy

Garg

Torbett

2014

Virus Research

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“…54 Another compound, NSC 624151 was found to be active against wild type and drug resistant HIV-1 and HIV-2 viruses. 55 A third compound e Azodicarbonamide, when introduced in phase I and II trials in Europe for advanced AIDS, showed dose dependent side effects (nephrolithiasis, glucose intolerance, CD4 cytotoxicity). 56 The side effects are not unsurprising as zinc fingers are not unique targets or used by HIV alone and are found in mammalian cells.…”

Section: Novel Targets and Agents Undergoing Pre-clinical Or Early CLmentioning

confidence: 99%

Novel targets for anti-retroviral therapy

Bhattacharya

Osman

2009

Journal of Infection

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“…The non-dissociable tethered dithiane compound 1,2-dithiane-4,5-diol,1,1-dioxide, (NSC 624151) also mediates similar defects in Gag processing (Rice et al 1997). Although cellular proteins also contain zinc fingers, these inhibitors appear to preferentially target retro-viral zinc fingers.…”

Section: Targeting Hiv-1 Ncmentioning

confidence: 99%

Targeting Human Immunodeficiency Virus Type 1 Assembly, Maturation and Budding

Wapling

Srivastava

Shehu-Xhilaga

et al. 2007

Drug Target�Insights

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The targets for licensed drugs used for the treatment of human immunodeficiency virus type 1 (HIV-1) are confined to the viral reverse transcriptase (RT), protease (PR), and the gp41 transmembrane protein (TM). While currently approved drugs are effective in controlling HIV-1 infections, new drug targets and agents are needed due to the eventual emergence of drug resistant strains and drug toxicity. Our increased understanding of the virus life-cycle and how the virus interacts with the host cell has unveiled novel mechanisms for blocking HIV-1 replication. This review focuses on inhibitors that target the late stages of virus replication including the synthesis and trafficking of the viral polyproteins, viral assembly, maturation and budding. Novel approaches to blocking the oligomerization of viral enzymes and the interactions between viral proteins and host cell factors, including their feasibility as drug targets, are discussed.

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Inhibition of multiple phases of human immunodeficiency virus type 1 replication by a dithiane compound that attacks the conserved zinc fingers of retroviral nucleocapsid proteins

Cited by 90 publications

References 48 publications

Advances in targeting nucleocapsid–nucleic acid interactions in HIV-1 therapy

Advances in targeting nucleocapsid–nucleic acid interactions in HIV-1 therapy

Novel targets for anti-retroviral therapy

Targeting Human Immunodeficiency Virus Type 1 Assembly, Maturation and Budding

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