The Second-Generation Maturation Inhibitor GSK3532795 Maintains Potent Activity Toward HIV Protease Inhibitor-Resistant Clinical Isolates

Publication date

2017-05-01

Authors

Ray, Neelanjana
Li, Tianbo
Lin, Zeyu
Protack, Tricia
van Ham, P.M.
Hwang, Carey
Krystal, Mark
Nijhuis, MoniqueISNI 0000000394085924
Lataillade, Max
Dicker, Ira

Editors

Advisors

Supervisors

Document Type

Article

Collections

Open Access logo

License

cc_by_nc_nd

Abstract

Background: Protease inhibitor (PI)-resistant HIV-1 isolates with primary substitutions in protease (PR) and secondary substitutions in Gag could potentially exhibit cross-resistance to maturation inhibitors. We evaluated the second-generation maturation inhibitor, GSK3532795, for activity toward clinical isolates with genotypic and phenotypic characteristics associated with PI resistance (longitudinal). Methods: Longitudinal clinical isolates from 15 PI-treated patients and 7 highly PI-resistant (nonlongitudinal) viruses containing major and minor PI resistance-associated mutations were evaluated for GSK3532795 sensitivity. Phenotypic sensitivity was determined using the PhenoSense Gag/PR assay (Monogram Biosciences) or in-house single-and multiple-cycle assays. Changes from baseline [CFB; ratio of post-to pre-treatment FC-IC50 (fold-change in IC50 versus wildtype virus)] ,3 were considered to be within the no-effect level. Results: All nonlongitudinal viruses tested were sensitive to GSK3532795 (FC-IC50 range 0.16-0.68). Among longitudinal isolates, all post-PI treatment samples had major PI resistance-associated mutations in PR and 17/21 had PI resistance-associated changes in Gag. Nineteen of the 21 post-PI treatment samples had GSK3532795 CFB ,3. Median (range) CFB was 0.83 (0.05-27.4) [Monogram (11 patients)] and 1.5 (1.0-2.2) [single-cycle (4 patients)]. The 2 post-PI treatment samples showing GSK3532795 CFB .3 (Monogram) were retested using single-and multiple-cycle assays. Neither sample had meaningful sensitivity changes in the multiple-cycle assay. Gag changes were not associated with an increased GSK3532795 CFB. Conclusions: GSK3532795 maintained antiviral activity against PI-resistant isolates with emergent PR and/or Gag mutations. This finding supports continued development of GSK3532795 in treatment-experienced patients with or without previous PI therapy.

Keywords

Cross-resistance, GSK3532795, HIV-1, In vitro, Maturation inhibitor, Protease inhibitor, Infectious Diseases, Pharmacology (medical)

Citation

Ray, N, Li, T, Lin, Z, Protack, T, van Ham, P M, Hwang, C, Krystal, M, Nijhuis, M, Lataillade, M & Dicker, I 2017, 'The Second-Generation Maturation Inhibitor GSK3532795 Maintains Potent Activity Toward HIV Protease Inhibitor-Resistant Clinical Isolates', Journal of Acquired Immune Deficiency Syndromes, vol. 75, no. 1, pp. 52-60. https://doi.org/10.1097/QAI.0000000000001304