Toward Drug-Like Multispecific Antibodies by Design

Sawant, Manali; Streu, Craig; Wu, Lina; Tessier, Peter M.

doi:10.3390/ijms21207496

Cited by 38 publications

(40 citation statements)

References 259 publications

(360 reference statements)

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“…Multi-specific antibody therapeutics are at high risk for chemical or physical stability issues, 6 , 8 which are difficult to predict from the primary amino acid sequence alone. 7 Usually, such issues become apparent at late discovery stages during comprehensive developability assessments of the drug pre-candidates. To mitigate the risk of late-stage failure, it is therefore desirable to select variants for developability assessments from large variant panels that comprise significant diversity on the sequence or structural level.…”

Section: Discussionmentioning

confidence: 99%

An end-to-end automated platform process for high-throughput engineering of next-generation multi-specific antibody therapeutics

Furtmann

Schneider

Spindler

et al. 2021

mAbs

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Next-generation multi-specific antibody therapeutics (MSATs) are engineered to combine several functional activities into one molecule to provide higher efficacy compared to conventional, mono-specific antibody therapeutics. However, highly engineered MSATs frequently display poor yields and less favorable drug-like properties (DLPs), which can adversely affect their development. Systematic screening of a large panel of MSAT variants in very high throughput (HT) is thus critical to identify potent molecule candidates with good yield and DLPs early in the discovery process. Here we report on the establishment of a novel, format-agnostic platform process for the fast generation and multiparametric screening of tens of thousands of MSAT variants. To this end, we have introduced full automation across the entire value chain for MSAT engineering. Specifically, we have automated the in-silico design of very large MSAT panels such that it reflects precisely the wet-lab processes for MSAT DNA library generation. This includes mass saturation mutagenesis or bulk modular cloning technologies while, concomitantly, enabling library deconvolution approaches using HT Sanger DNA sequencing. These DNA workflows are tightly linked to fully automated downstream processes for compartmentalized mammalian cell transfection expression, and screening of multiple parameters. All sub-processes are seamlessly integrated with tailored workflow supporting bioinformatics. As described here, we used this platform to perform multifactor optimization of a next-generation bispecific, cross-over dual variable domain-Ig (CODV-Ig). Screening of more than 25,000 individual protein variants in mono- and bispecific format led to the identification of CODV-Ig variants with over 1,000-fold increased potency and significantly optimized production titers, demonstrating the power and versatility of the platform.

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Section: Discussionmentioning

confidence: 99%

An end-to-end automated platform process for high-throughput engineering of next-generation multi-specific antibody therapeutics

Furtmann

Schneider

Spindler

et al. 2021

mAbs

View full text Add to dashboard Cite

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“…The complex structures of multispecific molecules also present significant challenges in achieving their drug-like properties [32], including favorable physical and chemical stability, solubility, viscosity, polyspecificity, immunogenicity, and pharmacokinetic properties. Compared to conventional monospecific antibody, much less is known about the developability properties of multispecific biotherapeutics.…”

Section: Challenges and Future Directionmentioning

confidence: 99%

“…The topic of multispecific biotherapeutics represents a fast-growing field regarding formats, design strategies, and applications. A number of outstanding review articles have been written on this topic or related themes for the past few years [2][3][4][5][6][9][10][11][15][16][17][18][19][20][21][22][23][24][25][26][27][28][29][30][31][32][33]. This review summarizes comprehensively the recent advances in molecular design and applications of the multispecific biotherapeutics from the early stages of research discovery to the late stages of clinical and regulatory development.…”

Section: Introductionmentioning

confidence: 99%

Recent Advances in the Molecular Design and Applications of Multispecific Biotherapeutics

Zhong

D’Antona

2021

Antibodies

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Recombinant protein-based biotherapeutics drugs have transformed clinical pipelines of the biopharmaceutical industry since the launch of recombinant insulin nearly four decades ago. These biologic drugs are structurally more complex than small molecules, and yet share a similar principle for rational drug discovery and development: That is to start with a pre-defined target and follow with the functional modulation with a therapeutic agent. Despite these tremendous successes, this “one target one drug” paradigm has been challenged by complex disease mechanisms that involve multiple pathways and demand new therapeutic routes. A rapidly evolving wave of multispecific biotherapeutics is coming into focus. These new therapeutic drugs are able to engage two or more protein targets via distinct binding interfaces with or without the chemical conjugation to large or small molecules. They possess the potential to not only address disease intricacy but also exploit new therapeutic mechanisms and assess undruggable targets for conventional monospecific biologics. This review focuses on the recent advances in molecular design and applications of major classes of multispecific biotherapeutics drugs, which include immune cells engagers, antibody-drug conjugates, multispecific tetherbodies, biologic matchmakers, and small-scaffold multispecific modalities. Challenges posed by the multispecific biotherapeutics drugs and their future outlooks are also discussed.

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“…Both diabodies and tandem scFvs can have two different binding specificities, and in this case, they are called bispecific (bs). Interestingly, even the VH and VL arrangement in the scFv fusion protein can influence the binding activity, and it is currently possible to predict the best functional structure so as to design scFvs that meet all requirements by molecular modelling using a computer-aided homology method [6,7]. A few decades ago, it was observed that the N-terminal IgG fragment including the VH and VL retains the same antigen-binding capacity as the whole IgG molecule.…”

Section: Different Antibody Formats: Mabs Scfvs and Nanobodiesmentioning

confidence: 99%

Targeting Human Papillomavirus-Associated Cancer by Oncoprotein-Specific Recombinant Antibodies

Donà

Bonito

Chiantore

et al. 2021

IJMS

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In recent decades, recombinant antibodies against specific antigens have shown great promise for the therapy of infectious diseases and cancer. Human papillomaviruses (HPVs) are involved in the development of around 5% of all human cancers and HPV16 is the high-risk genotype with the highest prevalence worldwide, playing a dominant role in all HPV-associated cancers. Here, we describe the main biological activities of the HPV16 E6, E7, and E5 oncoproteins, which are involved in the subversion of important regulatory pathways directly associated with all known hallmarks of cancer. We then review the state of art of the recombinant antibodies targeted to HPV oncoproteins developed so far in different formats, and outline their mechanisms of action. We describe the advantages of a possible antibody-based therapy against the HPV-associated lesions and discuss the critical issue of delivery to tumour cells, which must be addressed in order to achieve the desired translation of the antibodies from the laboratory to the clinic.

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Toward Drug-Like Multispecific Antibodies by Design

Cited by 38 publications

References 259 publications

An end-to-end automated platform process for high-throughput engineering of next-generation multi-specific antibody therapeutics

An end-to-end automated platform process for high-throughput engineering of next-generation multi-specific antibody therapeutics

Recent Advances in the Molecular Design and Applications of Multispecific Biotherapeutics

Targeting Human Papillomavirus-Associated Cancer by Oncoprotein-Specific Recombinant Antibodies

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