Human IL-2R[alpha] subunit binding modulation of IL-2 through a decline in electrostatic interactions: A computational and experimental approach

Human IL-2R[alpha] subunit binding modulation of IL-2 through a decline in electrostatic interactions: A computational and experimental approach

Although high-dose IL-2 has clear antitumor effects, severe side effects like severe toxicity and activation of Tregs by binding of IL-2 to high-affinity IL-2R, hypotension, and vascular leak syndrome limit its applications as a therapeutic antitumor agent. Here in this study, a rational computation...

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Veröffentlicht in:PloS one 2022-02, Vol.17 (2), p.e0264353
Hauptverfasser: Beig Parikhani, Arezoo, Bagherzadeh, Kowsar, Dehghan, Rada, Biglari, Alireza, Shokrgozar, Mohammad Ali, Riazi Rad, Farhad, Zeinali, Sirous, Talebkhan, Yeganeh, Ajdary, Soheila, Ahangari Cohan, Reza, Behdani, Mahdi
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Sprache:eng
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Analysis
Antimitotic agents
Antineoplastic agents
Blood circulation disorders
Care and treatment
Diagnosis
Dosage and administration
Immune response
Immunotherapy
Molecular dynamics
Patient outcomes
Risk factors
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container_issue 2
container_start_page e0264353
container_title PloS one
container_volume 17
creator Beig Parikhani, Arezoo
Bagherzadeh, Kowsar
Dehghan, Rada
Biglari, Alireza
Shokrgozar, Mohammad Ali
Riazi Rad, Farhad
Zeinali, Sirous
Talebkhan, Yeganeh
Ajdary, Soheila
Ahangari Cohan, Reza
Behdani, Mahdi
description Although high-dose IL-2 has clear antitumor effects, severe side effects like severe toxicity and activation of Tregs by binding of IL-2 to high-affinity IL-2R, hypotension, and vascular leak syndrome limit its applications as a therapeutic antitumor agent. Here in this study, a rational computational approach was employed to develop and design novel triple-mutant IL-2 variants with the aim of improving IL-2-based immunotherapy. The affinity of the mutants towards IL-2R[alpha] was further computed with the aid of molecular dynamic simulations and umbrella sampling techniques and the obtained results were compared to those of wild-type IL-2. In vitro experiments by flow cytometry showed that the anti-CD25 mAb was able to bind to PBMC cells even after mutant 2 preincubation, however, the binding strength of the mutant to [alpha]-subunit was less than of wtIL-2. Additionally, reduction of IL-2R[alpha] subunit affinity did not significantly disturb IL-2/IL2R[beta][gamma]c subunits interactions.
doi_str_mv 10.1371/journal.pone.0264353
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subjects Analysis
Antimitotic agents
Antineoplastic agents
Blood circulation disorders
Care and treatment
Diagnosis
Dosage and administration
Immune response
Immunotherapy
Molecular dynamics
Patient outcomes
Risk factors
title Human IL-2R[alpha] subunit binding modulation of IL-2 through a decline in electrostatic interactions: A computational and experimental approach
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