Literature DB >> 32914936

Therapeutic Fc-fusion proteins: Current analytical strategies.

Bastiaan L Duivelshof1,2, Amarande Murisier1,2, Julien Camperi1,2, Szabolcs Fekete1,2, Alain Beck3, Davy Guillarme1,2, Valentina D'Atri1,2.   

Abstract

Fc-Fusion proteins represent a successful class of biopharmaceutical products, with already 13 drugs approved in the European Union and United States as well as three biosimilar versions of etanercept. Fc-Fusion products combine tailored pharmacological properties of biological ligands, together with multiple functions of the fragment crystallizable domain of immunoglobulins. There is a great diversity in terms of possible biological ligands, including the extracellular domains of natural receptors, functionally active peptides, recombinant enzymes, and genetically engineered binding constructs acting as cytokine traps. Due to their highly diverse structures, the analytical characterization of Fc-Fusion proteins is far more complex than that of monoclonal antibodies and requires the use and development of additional product-specific methods over conventional generic/platform methods. This can be explained, for example, by the presence of numerous sialic acids, leading to high diversity in terms of isoelectric points and complex glycosylation profiles including multiple N- and O-linked glycosylation sites. In this review, we highlight the wide range of analytical strategies used to fully characterize Fc-fusion proteins. We also present case studies on the structural assessment of all commercially available Fc-fusion proteins, based on the features and critical quality attributes of their ligand-binding domains.
© 2020 Wiley-VCH GmbH.

Entities:  

Keywords:  Fc-fusion proteins; hydrophilic interaction chromatography; ion-exchange chromatography; mass spectrometry; size exclusion chromatography

Year:  2020        PMID: 32914936     DOI: 10.1002/jssc.202000765

Source DB:  PubMed          Journal:  J Sep Sci        ISSN: 1615-9306            Impact factor:   3.645


  12 in total

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Review 3.  Agonist antibody discovery: Experimental, computational, and rational engineering approaches.

Authors:  John S Schardt; Harkamal S Jhajj; Ryen L O'Meara; Timon S Lwo; Matthew D Smith; Peter M Tessier
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4.  Development of a blocker of the universal phosphatidylserine- and phosphatidylethanolamine-dependent viral entry pathways.

Authors:  Da-Hoon Song; Gustavo Garcia; Kathy Situ; Bernadette A Chua; Madeline Lauren O Hong; Elyza A Do; Christina M Ramirez; Airi Harui; Vaithilingaraja Arumugaswami; Kouki Morizono
Journal:  Virology       Date:  2021-05-10       Impact factor: 3.513

5.  Comparison of Three Complementary Analytical Techniques for the Evaluation of the Biosimilar Comparability of a Monoclonal Antibody and an Fc-Fusion Protein.

Authors:  Alice Demelenne; Arij Ben Yahia; Delphine Lempereur; Jacques Crommen; Anne-Catherine Servais; Ines Fradi; Marianne Fillet
Journal:  Front Chem       Date:  2021-12-06       Impact factor: 5.221

Review 6.  David versus goliath: ACE2-Fc receptor traps as potential SARS-CoV-2 inhibitors.

Authors:  Mohamed A Alfaleh; Ayat Zawawi; Sawsan S Al-Amri; Anwar M Hashem
Journal:  MAbs       Date:  2022 Jan-Dec       Impact factor: 5.857

7.  Functionally diverse heteromeric traps for ligands of the transforming growth factor-β superfamily.

Authors:  Ravindra Kumar; Asya V Grinberg; Huiming Li; Tzu-Hsing Kuo; Dianne Sako; Lavanya Krishnan; Katia Liharska; Jia Li; Rosa Grenha; Michelle C Maguire; Steven D Briscoe; R Scott Pearsall; Brantley R Herrin; Rajasekhar N V S Suragani; Roselyne Castonguay
Journal:  Sci Rep       Date:  2021-09-15       Impact factor: 4.379

8.  A New Approach to Supramolecular Structure Determination in Pharmaceutical Preparation of Self-Assembling Peptides: A Case Study of Lanreotide Autogel.

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Journal:  Pharmaceutics       Date:  2022-03-20       Impact factor: 6.321

9.  Expression of an immunocomplex consisting of Fc fragment fused with a consensus dengue envelope domain III in Saccharomyces cerevisiae.

Authors:  Kum-Kang So; Jeesun Chun; Nguyen Ngoc Luong; Hee-Won Seo; Dae-Hyuk Kim
Journal:  Biotechnol Lett       Date:  2021-07-10       Impact factor: 2.461

10.  Progression of melanoma is suppressed by targeting all transforming growth factor‑β isoforms with an Fc chimeric receptor.

Authors:  Shingo Kodama; Katarzyna Α Podyma-Inoue; Toshihiro Uchihashi; Kyoko Kurioka; Hitomi Takahashi; Akinari Sugauchi; Kazuki Takahashi; Toshihiro Inubushi; Mikihiko Kogo; Susumu Tanaka; Tetsuro Watabe
Journal:  Oncol Rep       Date:  2021-07-23       Impact factor: 3.906

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