A Glycoengineered Interferon-β Mutein (R27T) Generates Prolonged Signaling by an Altered Receptor-Binding Kinetics

Lee, Saehyung; Son, Woo Sung; Yang, Hyun-Kwon; Rajasekaran, Nirmal; Kim, Sung‐Su; Hong, Sang Hyun; Choi, Joon-Seok; Choi, Jun Young; Song, Kyoung; Shin, Young Kee

doi:10.3389/fphar.2018.01568

Cited by 7 publications

(9 citation statements)

References 78 publications

(89 reference statements)

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“…Interesting in this respect are cytokines, whose glycosylation status regulates receptor binding, biological stability, and function [ 134 ]. Glycoengineered versions of interferon‐α and ‐β have been developed that show enhanced pharmacokinetic properties and prolonged signaling capacities [ 135 , 136 ]. Glycosylated forms of interferon‐β are currently used in the clinic for the treatment multiple sclerosis [ 137 ].…”

Section: New Glyco‐based Strategies To Steer Immune Responses In Infection Cancer and Autoimmunitymentioning

confidence: 99%

Emerging glyco‐based strategies to steer immune responses

et al. 2021

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Glycan structures are common posttranslational modifications of proteins, which serve multiple important structural roles (for instance in protein folding), but also are crucial participants in cell–cell communications and in the regulation of immune responses. Through the interaction with glycan‐binding receptors, glycans are able to affect the activation status of antigen‐presenting cells, leading either to induction of pro‐inflammatory responses or to suppression of immunity and instigation of immune tolerance. This unique feature of glycans has attracted the interest and spurred collaborations of glyco‐chemists and glyco‐immunologists to develop glycan‐based tools as potential therapeutic approaches in the fight against diseases such as cancer and autoimmune conditions. In this review, we highlight emerging advances in this field, and in particular, we discuss on how glycan‐modified conjugates or glycoengineered cells can be employed as targeting devices to direct tumor antigens to lectin receptors on antigen‐presenting cells, like dendritic cells. In addition, we address how glycan‐based nanoparticles can act as delivery platforms to enhance immune responses. Finally, we discuss some of the latest developments in glycan‐based therapies, including chimeric antigen receptor (CAR)‐T cells to achieve targeting of tumor‐associated glycan‐specific epitopes, as well as the use of glycan moieties to suppress ongoing immune responses, especially in the context of autoimmunity.

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Section: New Glyco‐based Strategies To Steer Immune Responses In Infection Cancer and Autoimmunitymentioning

confidence: 99%

Emerging glyco‐based strategies to steer immune responses

et al. 2021

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“…In our previous studies, we developed a glycoengineered variant of recombinant human IFN-β-1a, IFN-β-R27T, which has two N-glycosylation sites at the 80th (original site) and an additional one at the 25th amino acid residue due to a mutation of Thr to Arg at position 27 of IFN-β ( Song et al, 2014 ). IFN-β-R27T exhibited superior stability, solubility, productivity, and pharmacokinetic properties compared to wild-type IFN-β-1a ( Lee et al, 2019 ; Song et al, 2020 ). Herein, we constructed fusion proteins consisting of an anti-HER2 antibody (trastuzumab) with IFN-β mutein and investigated its antitumor effect on a HER2-positive model.…”

Section: Introductionmentioning

confidence: 97%

Antibody-Based Targeting of Interferon-Beta-1a Mutein in HER2-Positive Cancer Enhances Antitumor Effects Through Immune Responses and Direct Cell Killing

et al. 2021

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Type I interferon (IFN) has been approved as an anticancer agent to treat some malignancies. However, IFNs have a short in vivo half-life, systemic toxicity, and poor biophysical properties, which prevent it from being widely used for cancer therapy. This study aimed to construct recombinant IFN-β-1a mutein immunocytokines that comprise a human epidermal growth factor receptor 2 (HER2)-targeting antibody and IFN-β muteins with an additional glycosylation, which can overcome the limitation of the cytokine itself. Hence, the molecular design aims to 1) enhance productivity and biophysical properties by adding secondary glycosylation in IFN-β, 2) increase the therapeutic index of IFN-β therapy by preferential retention at the tumor by possessing high affinity for HER2-expressing cancer cells, and 3) improve the pharmacokinetics and, thus, the convenience of IFN-β administration. The yield of trastuzumab-IFN-β mutein was higher than that of trastuzumab-wild-type IFN-β in the mammalian cell culture system. Trastuzumab-IFN-β mutein showed similar IFN activity and HER2-targeting ability equivalent to that of IFN-β mutein and trastuzumab, respectively. Trastuzumab-IFN-β mutein directly inhibited the growth of HER2-positive gastric cancer cell lines and was more effective than trastuzumab or IFN-β mutein alone. Trastuzumab-IFN-β mutein and IFN-β mutein displayed enhanced immune cell-mediated cytotoxicity. Collectively, trastuzumab-IFN-β mutein may have indirect immune cell-mediated antitumor effects and direct cell growth inhibitory effects. Tumor-targeting effect of trastuzumab-IFN-β mutein was analyzed using in vivo fluorescence imaging. The accumulation of trastuzumab-IFN-β mutein was observed in HER2-positive tumors rather than other tissues except the liver. To evaluate the both direct tumor growth inhibition effect and indirect immune cell-mediated antitumor effect, we tested the effect of trastuzumab-IFN-β mutein in HER2-positive cancer xenograft models using nude mice or humanized mice. Trastuzumab-IFN-β mutein could significantly enhance tumor regression when compared with trastuzumab or IFN-β mutein. In addition, an increase in tumor-infiltrating lymphocytes was observed in the trastuzumab-IFN-β mutein-treated group, implying that the tumor-targeting IFN-β may have an enhanced antitumor effect through increased immune response. Therefore, targeting IFN-β with an anti-HER2 monoclonal antibody makes the immunocytokine more potent than either agent alone. These novel findings suggest that trastuzumab-IFN-β mutein merits clinical evaluation as a new candidate of anticancer therapeutics.

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“…Surprisingly, rhIFN-β containing a larger proportion of higher antennary glycoforms showed more sustained bioactivity over time (Mastrangeli et al, 2015). Indeed, in our previous study, R27T exhibited more prolonged signaling than the mono-glycosylated rhIFN-β, with altered receptor-binding kinetics (Lee et al, 2018). A larger portion of higher antennary components in R27T may therefore influence cellular signaling effects.…”

Section: N-glycan Profiles Based On Aex-and Hilic-hplcmentioning

confidence: 81%

“…To address these issues, in our previous study, an additional single-glycosylation site was introduced at amino acid 25 in rhIFN-β 1a, resulting in R27T in which Arg at position 27 is mutated to Thr (Song et al, 2014). The additional glycosylation site increases the half-life and in vitro biological activity, as well as thermostability, allowing less frequent dosing (Lee et al, 2018;Song et al, 2014).…”

Section: Introductionmentioning

confidence: 99%

Glycosylation Heterogeneity of Hyperglycosylated Recombinant Human Interferon-β (rhIFN-β)

Song

Moon

Kim³

et al.

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We previously developed a biobetter version of rhIFN-β (R27T) that possesses an additional glycosylation site compared with rhIFN-β 1a. Herein, we characterized N-glycosylation heterogeneity of R27T. N-glycan site occupancy manifested as distinct differences in size. The analysis of complex carbohydrate moieties of R27T involved the common biopharmaceutical glycosylation critical quality attributes like core fucosylation, antennary composition, sialylation, lactosamine extensions, linkages, and overall glycan profiles using weak anion exchange and hydrophilic interaction HPLC with 2-aminobenzoic acid-labeled N-glycans. The double-glycosylated form accounted for approx. 94% R27T, while the single-glycosylated form accounted for 6% R27T. N-glycans consisted of a mixture of bi-, tri-, and tetra-antennary glycans, some with lactosamine extensions, but neither outer arm fucose nor α-galactose was detected. Sialic acid major variants, N-acetyl-and N-glycolyl-neuraminic acid were more abundant in R27T than in Rebif. The major N-glycan, accounting for 42% of total N-glycans, had a di-sialylated, core-fucosylated biantennary structure.

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A Glycoengineered Interferon-β Mutein (R27T) Generates Prolonged Signaling by an Altered Receptor-Binding Kinetics

Cited by 7 publications

References 78 publications

Emerging glyco‐based strategies to steer immune responses

Emerging glyco‐based strategies to steer immune responses

Antibody-Based Targeting of Interferon-Beta-1a Mutein in HER2-Positive Cancer Enhances Antitumor Effects Through Immune Responses and Direct Cell Killing

Glycosylation Heterogeneity of Hyperglycosylated Recombinant Human Interferon-β (rhIFN-β)

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