Abstract 1890: A solution to T-cell engager toxicity: An anti-CD3 Prodrug DARPin (CD3-PDD) shows no toxicity, but potent anti-tumor activity in a humanized mouse model

Bosshart, Andreas; Ahlskog, J.; Eggenschwiler, Aline; Schiegg, Dieter; Grübler, Yvonne; Wandel, Sandra; Fontaine, Simon; Paladino, María Emilia; Mangold, Susanne; Hospodarsch, Tanja; Neculcea, Alexandra; Iss, Chloé; Herzog, Christel; Schlereth, Bernd

doi:10.1158/1538-7445.am2021-1890

Cited by 1 publication

(2 citation statements)

References 0 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…161 This concept has recently been applied to a DARPin based CD3-binding T cell engager in which the CD3 effector function is masked until being activated in the tumor microenvironment. 162 The anti-CD3 prodrug molecule is composed of four distinct DARPin domains: an EGFR-and a CD3-binder as the core T cell redirecting entity, connected by a protease-cleavable linker to a DARPin domain that occupies the CD3-binding interface through intramolecular interactions. A fourth anti-HSA domain ensures prolonged blood circulation.…”

Section: Multi-specific Darpins In Cancer Therapymentioning

confidence: 99%

“…upon cleavage), the HSA domain is lost and, consequently, the T cell engager entity is quickly eliminated from circulation by renal clearance if not bound to its target, minimizing the exposure of the activated drug outside the tumor. 162 It will be interesting to see how this DARPin-based prodrug compares to 'muted' T cell bispecific antibodies (TCBs) that are similarly activated by cleavage of an anti-idiotypic anti-CD3 mask through tumor-associated proteases. 163…”

Section: Multi-specific Darpins In Cancer Therapymentioning

confidence: 99%

See 1 more Smart Citation

The DARPin Encyclopedia: from Basic Research towards Therapeutics

Wild¹,

Eapen²,

Forrer³

et al. 2022

Preprint

View full text Add to dashboard Cite

The adaptive immune system in vertebrates comes in two flavors. Historically, adaptive immunity focused on the study of immunoglobulins (also referred to as Ig-based antibodies herein); more recently, jawless vertebrates were found to use an entirely different class of proteins for their adaptive immunesystem. Specifically, these organisms express variable lymphocyte receptors (so called VLR antibodies) that create diversity based on the rearrangement of leucine-rich repeats. Meanwhile, various, naturally occurring repeat motifs have been used as building blocks for the design of artificial binding scaffolds which, among others, include designed ankyrin repeat proteins (DARPins). Such binding scaffolds are also referred to as non-Ig-based antibodies or non-Ig scaffolds herein). DARPins display several benefits such as a low molecular weight (~15 kDa), high thermal stability, high specificity and affinity, versatility (e.g., in terms of valency and multi-specificity), speedy preclinical development, low production costs and, thus, bear the potential to not only complement existing therapeutic Ig-based antibodies but also open up novel therapeutic strategies. The first generation DARPin therapeutic abicipar pegol has completed two Phase III studies in 2020 while several other DARPin drug candidates are currently undergoing clinical validation. Most recently, the rapid development of tri-specific SARSCoV-2 DARPin therapeutics showcases the immense potential of recombinant repeat proteins in adopting quickly e.g., new forms of target neutralization that a single Ig-based antibody cannot afford. Here, we highlight the design principles of repeat proteins in general and summarize in detail the continuous advancements of the DARPin scaffold that made it one of the most promising antibody mimetics to date. This review provides an overview of current and emerging applications of DARPins as both a research tool and therapeutic drug that can match or even surpass Ig-based antibody applications.

show abstract

Section: Multi-specific Darpins In Cancer Therapymentioning

confidence: 99%

Section: Multi-specific Darpins In Cancer Therapymentioning

confidence: 99%