SAT0249 Safety, pharmacokinetics, pharmacodynamics and inhibition of T-cell dependent antibody response (TDAR) with MEDI4920, a novel, engineered CD40 ligand (CD40L) antagonist: results of a first-time-in-human study

Albulescu, MG; Gunsior, Michele; Li, J; Bush, Jim; Godwood, A.; Miday, Robert; Grant, Ethan P.; Howe, David; Faggioni, Raffaella; Roskos, L

doi:10.1136/annrheumdis-2017-eular.3468

Cited by 2 publications

(2 citation statements)

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“…A tandem anti-CD40L monobody construct fused with serum albumin ( Figure 3B) was then designed for clinical applications under the names MEDI4920 then VIB4920 [105]. This construct was devoid of the reactive Fc region present in autoantibodies and reduced immunostimulatory action over time in humans, resulting in increased safety and reduced risk of thromboembolic events [108,109].…”

Section: Multi-valent and Multi-specific Monobodiesmentioning

confidence: 99%

Development and Differentiation in Monobodies Based on the Fibronectin Type 3 Domain

Chandler

Buckle

2020

Cells

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As a non-antibody scaffold, monobodies based on the fibronectin type III (FN3) domain overcome antibody size and complexity while maintaining analogous binding loops. However, antibodies and their derivatives remain the gold standard for the design of new therapeutics. In response, clinical-stage therapeutic proteins based on the FN3 domain are beginning to use native fibronectin function as a point of differentiation. The small and simple structure of monomeric monobodies confers increased tissue distribution and reduced half-life, whilst the absence of disulphide bonds improves stability in cytosolic environments. Where multi-specificity is challenging with an antibody format that is prone to mis-pairing between chains, multiple FN3 domains in the fibronectin assembly already interact with a large number of molecules. As such, multiple monobodies engineered for interaction with therapeutic targets are being combined in a similar beads-on-a-string assembly which improves both efficacy and pharmacokinetics. Furthermore, full length fibronectin is able to fold into multiple conformations as part of its natural function and a greater understanding of how mechanical forces allow for the transition between states will lead to advanced applications that truly differentiate the FN3 domain as a therapeutic scaffold.

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Section: Multi-valent and Multi-specific Monobodiesmentioning

confidence: 99%

Development and Differentiation in Monobodies Based on the Fibronectin Type 3 Domain

Chandler

Buckle

2020

Cells

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show abstract

“…A tandem anti-CD40L monobody construct fused with serum albumin [ Figure 4B] was then designed for clinical applications under the names MEDI4920 then VIB4920 [104]. This construct was devoid of the reactive Fc region present in autoantibodies and reduced immunostimulatory action over time in humans, resulting in increased safety and reduced risk of thromboembolic events [107,108].…”

Section: Multi-valent and Multi-specific Monobodiesmentioning

confidence: 99%

Development and Differentiation in Monobodies Based on the Fibronectin Type 3 Domain

Chandler

Buckle

2020

Preprint

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As a non-antibody scaffold, monobodies based on the fibronectin type III (FN3) domain overcome antibody size and complexity while maintaining analogous binding loops. However, antibodies and their derivatives remain the gold standard for design of new therapeutics. In response, clinical therapeutic proteins based on the FN3 domain are beginning to use native fibronectin function as a point of differentiation. The small and simple structure of monomeric monobodies confers increased tissue distribution and reduced half-life, whilst the absence of disulphide bonds improves stability in cytosolic environments. Where multi-specificity is challenging with an antibody format that is prone to mis-pairing of chains, FN3 domains in the fibronectin assembly already interact with a large number of molecules. As such, multiple monobodies engineered for interaction with therapeutic targets are being combined in a similar beads-on-a-string assembly which improves both efficacy and pharmacokinetics. Furthermore, full length fibronectin is able to fold into multiple conformations as part of its natural function and a greater understanding of how mechanical forces allow for the transition between states will lead to advanced applications that truly differentiate the FN3 domain as a therapeutic scaffold.

show abstract

SAT0249 Safety, pharmacokinetics, pharmacodynamics and inhibition of T-cell dependent antibody response (TDAR) with MEDI4920, a novel, engineered CD40 ligand (CD40L) antagonist: results of a first-time-in-human study

Cited by 2 publications

References 0 publications

Development and Differentiation in Monobodies Based on the Fibronectin Type 3 Domain

Development and Differentiation in Monobodies Based on the Fibronectin Type 3 Domain

Development and Differentiation in Monobodies Based on the Fibronectin Type 3 Domain

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