Design Strategy to Create Antibody Mimetics Harbouring Immobilised Complementarity Determining Region Peptides for Practical Use

Kadonosono, Tetsuya; Yimchuen, Wanaporn; Ota, Yumi; See, Kyra; Furuta, Tadaomi; Shiozawa, Tadashi; Kitazawa, Maika; Yu, Guoxian; Patil, Akash; Kuchimaru, Takahiro; Kizaka‐Kondoh, Shinae

doi:10.1038/s41598-020-57713-4

Cited by 19 publications

(27 citation statements)

References 30 publications

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“…The HBP of HBP-FLAP must be exposed on the surface of the molecule because the GA site was selected because it is a solvent exposed loop in the FN3 structure. 18 Therefore, the proteolysis resistance of the HBP in HBP-FLAP is not because of reduced protease access to the target sequence but is likely due to its immobilized structure, which restricts protease activity.…”

Section: Discussionmentioning

confidence: 99%

“…22,23 In addition, previous calculations revealed that residues 51-56 of FN3 are a gra acceptor (GA) site in which the structure of graed hexapeptides can be immobilized. 18 FN3 has been used for the development of affinity proteins targeting various antigens by protein engineering, 23,24 some of which have entered clinical trials, 25 suggesting that FN3 is a promising scaffold for creating HBP-FLAP. The HBPs were rst isolated from a phage-displayed peptide library ( Fig.…”

Section: Strategy For Creating Hbp-flapmentioning

confidence: 99%

“…17 Based on this nding, we reported a computational design strategy for developing antibody mimetics named FLAP, which is uctuation-regulated affinity protein (FLAP) having structurally immobilized mAb-derived peptide. 18 In this study, we focused on the development of a HER2targeting small protein with a structurally immobilized HBP, HBP-FLAP. The optimal HBP in an HBP-FLAP showed improved proteolysis resistance and exhibited specic HER2-binding in vitro and in vivo.…”

Section: Introductionmentioning

confidence: 99%

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Strategic design to create HER2-targeting proteins with target-binding peptides immobilized on a fibronectin type III domain scaffold

et al. 2020

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Section: Discussionmentioning

confidence: 99%

Section: Strategy For Creating Hbp-flapmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Strategic design to create HER2-targeting proteins with target-binding peptides immobilized on a fibronectin type III domain scaffold

et al. 2020

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“…This is in line with previous findings that light chain CDRs generally play a more secondary or supporting role in target binding, such as stabilization of other CDRs. [15][16][17] Finally, we calculated the RMSD values of the HER2-binding residues between the three models and the antigen-free and antigen-bound structures of trastuzumab Fab. The rank 1 model yielded RMSD values of 1.64 and 1.86 Å to the antigen-free and antigen-bound structures, respectively; rank 2, 1.73 and 2.00 Å; and rank 3, 1.74 and 2.10 Å.…”

Section: Evaluation Of D-flap Binding To Her2mentioning

confidence: 99%

“…[11,12] An alternative approach is to use mAb-derived CDRs. Since antibody paratopes are usually formed by a combination of dominant and ancillary CDRs [15][16][17] that bind to linear or planar epitopes, [14] optimal paratope reconstitution is difficult with a single CDR graft onto a small protein scaffold. However, grafting multiple CDR peptides onto a small protein scaffold is challenging.…”

Section: Introductionmentioning

confidence: 99%

Reconstitution of an Anti‐HER2 Antibody Paratope by Grafting Dual CDR‐Derived Peptides onto a Small Protein Scaffold

See

Kadonosono

Ota

et al. 2020

Biotechnology Journal

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Target-binding small proteins are promising alternatives to conventional monoclonal antibodies (mAbs), offering advantages in terms of tissue penetration and manufacturing costs. Recently, a design strategy to create small proteins called fluctuation-regulated affinity proteins (FLAPs) consisting of a structurally immobilized peptide from the complementarity-determining region (CDR) loops of mAbs (CDR-derived peptide) and a protein scaffold was developed. Because mAb paratopes are usually composed of multiple CDRs, FLAPs with multiple binding peptides may have an enhanced target-binding capability. Here, a strategy to create FLAPs bearing dual CDR-derived peptides (D-FLAPs) using the anti-human epithelial growth factor receptor type 2 (HER2) mAb trastuzumab as a basis is developed. Computationally selected CDR-derived peptides are first grafted onto two adjacent loops of the fibronectin type III domain (FN3) scaffold, yielding 80 D-FLAP candidates. After computational screening based on their similarity to the parental mAb with regard to the conformation of paratope residues, two candidates are selected. After further evaluation with ELISA, one D-FLAP with HYTTPP and GDGFYA peptides from CDR-L3 and CDR-H3 of the parental mAb, respectively, is found to bind HER2 with a dissociation constant of 58 nm. This method applies to various mAb drugs and allows the rational design of small protein alternatives.

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Antibody mimetics: The next generation antibody engineering, a retrospective and prospective analysis

Zhang,

Wu,

Dang

2023

Biotechnology Journal

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Antibody mimetics represent the fourth generation of antibody engineering, following polyclonal antibodies, monoclonal antibodies, and genetically engineered antibody fragments. Despite cumulative studies highlighting the advantages of antibody mimetics, including enhanced recognition properties, superior affinity, stability, penetrability, and cost‐effectiveness, a comprehensive review of this evolving field is notably absent. In this study, spanning 1986–2023 and analyzing 24,318 publications, we undertake a retrospective and prospective analysis to elucidate the evolution roadmap of antibody mimetics, providing insights into the current landscape, global contributions, and future trajectories. Concurrently, our aim is to establish standardized terminology and delineate the research scope within the realm of antibody mimetics. These endeavors not only chart the trajectory and scope of antibody mimetics research but also underscore its potential to revolutionize medicine, technology, and science.

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Design Strategy to Create Antibody Mimetics Harbouring Immobilised Complementarity Determining Region Peptides for Practical Use

Cited by 19 publications

References 30 publications

Strategic design to create HER2-targeting proteins with target-binding peptides immobilized on a fibronectin type III domain scaffold

Strategic design to create HER2-targeting proteins with target-binding peptides immobilized on a fibronectin type III domain scaffold

Reconstitution of an Anti‐HER2 Antibody Paratope by Grafting Dual CDR‐Derived Peptides onto a Small Protein Scaffold

Antibody mimetics: The next generation antibody engineering, a retrospective and prospective analysis

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