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Performance of Affinity-Improved DARPin Targeting HIV Capsid Domain in Interference of Viral Progeny Production

Previously, a designed ankyrin repeat protein, Ank(GAG)1D4, was generated for intracellular targeting of the HIV-1 capsid domain. The efficiency was satisfactory in interfering with the HIV assembly process. Consequently, improved Ank(GAG)1D4 binding affinity was introduced by substituting tyrosine...

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Autores principales: Sornsuwan, Kanokporn, Thongkhum, Weeraya, Pamonsupornwichit, Thanathat, Carraway, Tanawan Samleerat, Soponpong, Suthinee, Sakkhachornphop, Supachai, Tayapiwatana, Chatchai, Yasamut, Umpa
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8533564/
https://www.ncbi.nlm.nih.gov/pubmed/34680070
http://dx.doi.org/10.3390/biom11101437
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author Sornsuwan, Kanokporn
Thongkhum, Weeraya
Pamonsupornwichit, Thanathat
Carraway, Tanawan Samleerat
Soponpong, Suthinee
Sakkhachornphop, Supachai
Tayapiwatana, Chatchai
Yasamut, Umpa
author_facet Sornsuwan, Kanokporn
Thongkhum, Weeraya
Pamonsupornwichit, Thanathat
Carraway, Tanawan Samleerat
Soponpong, Suthinee
Sakkhachornphop, Supachai
Tayapiwatana, Chatchai
Yasamut, Umpa
author_sort Sornsuwan, Kanokporn
collection PubMed
description Previously, a designed ankyrin repeat protein, Ank(GAG)1D4, was generated for intracellular targeting of the HIV-1 capsid domain. The efficiency was satisfactory in interfering with the HIV assembly process. Consequently, improved Ank(GAG)1D4 binding affinity was introduced by substituting tyrosine (Y) for serine (S) at position 45. However, the intracellular anti-HIV-1 activity of Ank(GAG)1D4-S45Y has not yet been validated. In this study, the performance of Ank(GAG)1D4 and Ank(GAG)1D4-S45Y in inhibiting wild-type HIV-1 and HIV-1 maturation inhibitor-resistant replication in SupT1 cells was evaluated. HIV-1 p24 and viral load assays were used to verify the biological activity of Ank(GAG)1D4 and Ank(GAG)1D4-S45Y as assembly inhibitors. In addition, retardation of syncytium formation in infected SupT1 cells was observed. Of note, the defense mechanism of both ankyrins did not induce the mutation of target amino acids in the capsid domain. The present data show that the potency of Ank(GAG)1D4-S45Y was superior to Ank(GAG)1D4 in interrupting either HIV-1 wild-type or the HIV maturation inhibitor-resistant strain.
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spelling pubmed-85335642021-10-23 Performance of Affinity-Improved DARPin Targeting HIV Capsid Domain in Interference of Viral Progeny Production Sornsuwan, Kanokporn Thongkhum, Weeraya Pamonsupornwichit, Thanathat Carraway, Tanawan Samleerat Soponpong, Suthinee Sakkhachornphop, Supachai Tayapiwatana, Chatchai Yasamut, Umpa Biomolecules Article Previously, a designed ankyrin repeat protein, Ank(GAG)1D4, was generated for intracellular targeting of the HIV-1 capsid domain. The efficiency was satisfactory in interfering with the HIV assembly process. Consequently, improved Ank(GAG)1D4 binding affinity was introduced by substituting tyrosine (Y) for serine (S) at position 45. However, the intracellular anti-HIV-1 activity of Ank(GAG)1D4-S45Y has not yet been validated. In this study, the performance of Ank(GAG)1D4 and Ank(GAG)1D4-S45Y in inhibiting wild-type HIV-1 and HIV-1 maturation inhibitor-resistant replication in SupT1 cells was evaluated. HIV-1 p24 and viral load assays were used to verify the biological activity of Ank(GAG)1D4 and Ank(GAG)1D4-S45Y as assembly inhibitors. In addition, retardation of syncytium formation in infected SupT1 cells was observed. Of note, the defense mechanism of both ankyrins did not induce the mutation of target amino acids in the capsid domain. The present data show that the potency of Ank(GAG)1D4-S45Y was superior to Ank(GAG)1D4 in interrupting either HIV-1 wild-type or the HIV maturation inhibitor-resistant strain. MDPI 2021-09-30 /pmc/articles/PMC8533564/ /pubmed/34680070 http://dx.doi.org/10.3390/biom11101437 Text en © 2021 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Sornsuwan, Kanokporn
Thongkhum, Weeraya
Pamonsupornwichit, Thanathat
Carraway, Tanawan Samleerat
Soponpong, Suthinee
Sakkhachornphop, Supachai
Tayapiwatana, Chatchai
Yasamut, Umpa
Performance of Affinity-Improved DARPin Targeting HIV Capsid Domain in Interference of Viral Progeny Production
title Performance of Affinity-Improved DARPin Targeting HIV Capsid Domain in Interference of Viral Progeny Production
title_full Performance of Affinity-Improved DARPin Targeting HIV Capsid Domain in Interference of Viral Progeny Production
title_fullStr Performance of Affinity-Improved DARPin Targeting HIV Capsid Domain in Interference of Viral Progeny Production
title_full_unstemmed Performance of Affinity-Improved DARPin Targeting HIV Capsid Domain in Interference of Viral Progeny Production
title_short Performance of Affinity-Improved DARPin Targeting HIV Capsid Domain in Interference of Viral Progeny Production
title_sort performance of affinity-improved darpin targeting hiv capsid domain in interference of viral progeny production
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8533564/
https://www.ncbi.nlm.nih.gov/pubmed/34680070
http://dx.doi.org/10.3390/biom11101437
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