Novel Compound Inhibitors of HIV-1NL4-3 Vpu

HIV-1 Vpu targets the host cell proteins CD4 and BST-2/Tetherin for degradation, ultimately resulting in enhanced virus spread and host immune evasion. The discovery and characterization of small molecules that antagonize Vpu would further elucidate the contribution of Vpu to pathogenesis and lay th...

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Main Authors: Ananthan, S. (Author), Augelli-Szafran, C.E (Author), Bostwick, R. (Author), Cai, Z. (Author), Evans, D.T (Author), Finzi, A. (Author), Gil, H.M (Author), Gupta, V.V (Author), Johnson, M.C (Author), Kuzmichev, Y.V (Author), Lyddon, T.D (Author), Nebane, N.M (Author), Ptak, R.G (Author), Rasmussen, L. (Author), Richard, J. (Author), Robinson, C.A (Author), Schader, S.M (Author), Welbourn, S. (Author), Wonderlich, E.R (Author)
Format: Article
Language:English
Published: NLM (Medline) 2022
Subjects:
HIV
HTS
MLV
Online Access:View Fulltext in Publisher
LEADER 03352nam a2200565Ia 4500
001 10.3390-v14040817
008 220510s2022 CNT 000 0 und d
020 |a 19994915 (ISSN) 
245 1 0 |a Novel Compound Inhibitors of HIV-1NL4-3 Vpu 
260 0 |b NLM (Medline)  |c 2022 
856 |z View Fulltext in Publisher  |u https://doi.org/10.3390/v14040817 
520 3 |a HIV-1 Vpu targets the host cell proteins CD4 and BST-2/Tetherin for degradation, ultimately resulting in enhanced virus spread and host immune evasion. The discovery and characterization of small molecules that antagonize Vpu would further elucidate the contribution of Vpu to pathogenesis and lay the foundation for the study of a new class of novel HIV-1 therapeutics. To identify novel compounds that block Vpu activity, we have developed a cell-based 'gain of function' assay that produces a positive signal in response to Vpu inhibition. To develop this assay, we took advantage of the viral glycoprotein, GaLV Env. In the presence of Vpu, GaLV Env is not incorporated into viral particles, resulting in non-infectious virions. Vpu inhibition restores infectious particle production. Using this assay, a high throughput screen of >650,000 compounds was performed to identify inhibitors that block the biological activity of Vpu. From this screen, we identified several positive hits but focused on two compounds from one structural family, SRI-41897 and SRI-42371. We developed independent counter-screens for off target interactions of the compounds and found no off target interactions. Additionally, these compounds block Vpu-mediated modulation of CD4, BST-2/Tetherin and antibody dependent cell-mediated toxicity (ADCC). Unfortunately, both SRI-41897 and SRI-42371 were shown to be specific to the N-terminal region of NL4-3 Vpu and did not function against other, more clinically relevant, strains of Vpu; however, this assay may be slightly modified to include more significant Vpu strains in the future. 
650 0 4 |a bone marrow stromal antigen 2 
650 0 4 |a Bone Marrow Stromal Antigen 2 
650 0 4 |a GaLV 
650 0 4 |a Gibbon ape leukemia virus 
650 0 4 |a glycosylphosphatidylinositol anchored protein 
650 0 4 |a GPI-Linked Proteins 
650 0 4 |a HIV 
650 0 4 |a HIV-1 
650 0 4 |a HTS 
650 0 4 |a Human immunodeficiency virus 1 
650 0 4 |a Human immunodeficiency virus protein 
650 0 4 |a Human Immunodeficiency Virus Proteins 
650 0 4 |a inhibitors 
650 0 4 |a Leukemia Virus, Gibbon Ape 
650 0 4 |a metabolism 
650 0 4 |a MLV 
650 0 4 |a viral protein 
650 0 4 |a Viral Regulatory and Accessory Proteins 
700 1 |a Ananthan, S.  |e author 
700 1 |a Augelli-Szafran, C.E.  |e author 
700 1 |a Bostwick, R.  |e author 
700 1 |a Cai, Z.  |e author 
700 1 |a Evans, D.T.  |e author 
700 1 |a Finzi, A.  |e author 
700 1 |a Gil, H.M.  |e author 
700 1 |a Gupta, V.V.  |e author 
700 1 |a Johnson, M.C.  |e author 
700 1 |a Kuzmichev, Y.V.  |e author 
700 1 |a Lyddon, T.D.  |e author 
700 1 |a Nebane, N.M.  |e author 
700 1 |a Ptak, R.G.  |e author 
700 1 |a Rasmussen, L.  |e author 
700 1 |a Richard, J.  |e author 
700 1 |a Robinson, C.A.  |e author 
700 1 |a Schader, S.M.  |e author 
700 1 |a Welbourn, S.  |e author 
700 1 |a Wonderlich, E.R.  |e author 
773 |t Viruses