Biological and physiological properties of reverse ankyrin engineered for dimer construction to enhance HIV-1 capsid interaction

Juntit, On-anong; Yasamut, Umpa; Sakkhachornphop, Supachai; Chupradit, Koollawat; Thongkum, Weeraya; Wisitponchai, Tanchanok; Prangkio, Panchika; Srisawat, Chatchawan; Lee, Vannajan; Chokepaichitkool, Tawan; Kongtawelert, Prachya; Nimmanpipug, Piyarat; Tayapiwatana, Chatchai

doi:10.22541/au.163432349.99058162/v1

2021

DOI: 10.22541/au.163432349.99058162/v1

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Biological and physiological properties of reverse ankyrin engineered for dimer construction to enhance HIV-1 capsid interaction

On-anong Juntit

Umpa Yasamut

Supachai Sakkhachornphop

et al.

Abstract: Assembly and budding in the late-stage of human immunodeficiency virus type 1 (HIV-1) production relies on the polymerization of Gag protein at the inner leaflet of the plasma membrane. We previously generated an ankyrin repeat protein (Ank1D4) that specifically interacts with the CAp24 protein. This study aimed to improve the binding activity of Ank1D4 by generating two platforms for the Ank1D4 dimer. The design of these constructs featured a distinct orientation of monomeric Ank1D4 connected by a linker pept… Show more

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Dimeric Ankyrin with Inverted Module Promotes Bifunctional Property in Capturing Capsid to Impede HIV-1 Replication

Juntit

Sornsuwan

Wisitponchai

et al. 2023

IJMS

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Several anti-HIV scaffolds have been proposed as complementary treatments to highly active antiretroviral therapy. AnkGAG1D4, a designed ankyrin repeat protein, formerly demonstrated anti-HIV-1 replication by interfering with HIV-1 Gag polymerization. However, the improvement of the effectiveness was considered. Recently, the dimeric molecules of AnkGAG1D4 were accomplished in enhancing the binding activity against HIV-1 capsid (CAp24). In this study, the interaction of CAp24 against the dimer conformations was elucidated to elaborate the bifunctional property. The accessibility of the ankyrin binding domains was inspected by bio-layer interferometry. By inverting the second module of dimeric ankyrin (AnkGAG1D4NC-CN), the CAp24 interaction KD was significantly reduced. This reflects the capability of AnkGAG1D4NC-CN in simultaneously capturing CAp24. On the contrary, the binding activity of dimeric AnkGAG1D4NC-NC was indistinguishable from the monomeric AnkGAG1D4. The bifunctional property of AnkGAG1D4NC-CN was subsequently confirmed in the secondary reaction with additional p17p24. This data correlates with the MD simulation, which suggested the flexibility of the AnkGAG1D4NC-CN structure. The CAp24 capturing capacity was influenced by the distance of the AnkGAG1D4 binding domains to introduce the avidity mode of AnkGAG1D4NC-CN. Consequently, AnkGAG1D4NC-CN showed superior potency in interfering with HIV-1 NL4-3 WT and HIV-1 NL4-3 MIRCAI201V replication than AnkGAG1D4NC-NC and an affinity improved AnkGAG1D4-S45Y.

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Dimeric Ankyrin with Inverted Module Promotes Bifunctional Property in Capturing Capsid to Impede HIV-1 Replication

Juntit

Sornsuwan

Wisitponchai

et al. 2023

IJMS

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Biological and physiological properties of reverse ankyrin engineered for dimer construction to enhance HIV-1 capsid interaction

Cited by 1 publication

References 0 publications

Dimeric Ankyrin with Inverted Module Promotes Bifunctional Property in Capturing Capsid to Impede HIV-1 Replication

Dimeric Ankyrin with Inverted Module Promotes Bifunctional Property in Capturing Capsid to Impede HIV-1 Replication

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