A minimal physiologically based pharmacokinetic model to study the combined effect of antibody size, charge, and binding affinity to FcRn/antigen on antibody pharmacokinetics

Patidar, Krutika; Pillai, Nikhil; Dhakal, Saroj; Avery, Lindsay B.; Mavroudis, Panteleimon D.

doi:10.1007/s10928-023-09899-z

Cited by 2 publications

(1 citation statement)

References 46 publications

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“…However, the dataset is limited to the clinical landscape and may not represent the full scope of properties observed in early campaign stages. 26 Patidar et al 52 recently described a PBPK model approach that incorporated physicochemical property measures of molecular weight, molecular size, Stoke’s radius, molecular charge and binding affinity to FcRn. Additionally, they incorporated K spino input for pinocytosis rate and nonspecific charge based off-target binding parameters ( K D,NSB , K p ) in the model-based structure.…”

Section: Discussionmentioning

confidence: 99%

Assessment and incorporation of in vitro correlates to pharmacokinetic outcomes in antibody developability workflows

Jain,

Prinz,

Marker

et al. 2024

mAbs

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In vitro assessments for the prediction of pharmacokinetic (PK) behavior of biotherapeutics can help identify corresponding liabilities significantly earlier in the discovery timeline. This can minimize the need for extensive early in vivo PK characterization, thereby reducing animal usage and optimizing resources. In this study, we recommend bolstering classical developability workflows with in vitro measures correlated with PK. In agreement with current literature, in vitro measures assessing nonspecific interactions, self-interaction, and FcRn interaction are demonstrated to have the highest correlations to clearance in hFcRn Tg32 mice. Crucially, the dataset used in this study has broad sequence diversity and a range of physicochemical properties, adding robustness to our recommendations. Finally, we demonstrate a computational approach that combines multiple in vitro measurements with a multivariate regression model to improve the correlation to PK compared to any individual assessment. Our work demonstrates that a judicious choice of high throughput in vitro measurements and computational predictions enables the prioritization of candidate molecules with desired PK properties.

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Section: Discussionmentioning

confidence: 99%

Assessment and incorporation of in vitro correlates to pharmacokinetic outcomes in antibody developability workflows

Jain,

Prinz,

Marker

et al. 2024

mAbs

View full text Add to dashboard Cite

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Development of a Minimal Physiologically-Based Pharmacokinetic Modeling / Machine Learning Framework for Early Target Pharmacology Assessment

Mavroudis,

Patidar,

Pillai

et al. 2024

Preprint

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Development of antibodies often begins with the assessment and optimizing of their physicochemical properties, and their efficient engagement to the target of interest. Decisions at the early optimization stage are critical for the success of the drug candidate but are constrained due to the limited knowledge of the antibody and target pharmacology. n the present work we propose a model-based target pharmacology assessment framework based on which optimal physicochemical properties of antibodies can be inferred from minimal physiologically based pharmacokinetic (mPBPK) modeling and machine learning (ML). Towards this goal, we aim to perform a high-throughput virtual exploration of physicochemical properties of antibody drug candidates and relate them to target occupancy (TO). We use a mPBPK model previously developed by our group that incorporates a multivariate quantitative relationship between antibodies’ physicochemical properties such as molecular weight (MW), size, charge, and in silico + in vitro derived descriptors with a known relation to PK properties. In this study, we perform an exploration of virtual antibody drug candidates with varying physicochemical properties, and virtual target candidates with varying characteristics to unravel rules for optimal antibody drug candidates and feasible drug-target interaction. We also identify that varying the antibody dose and dosing scheme, target form (soluble or membrane-bound), antibody charge, and site of action had significant effect on the optimal properties for antibody drug candidate selection. By unravelling new design rules for antibody drug properties that are dependent on model-based TO assessment, we deliver a first-in-class model-based framework towards better understanding of the biology-specific PK and ADME processes of antibody drug candidates proteins and reducing the overall time for drug development.

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A minimal physiologically based pharmacokinetic model to study the combined effect of antibody size, charge, and binding affinity to FcRn/antigen on antibody pharmacokinetics

Cited by 2 publications

References 46 publications

Assessment and incorporation of in vitro correlates to pharmacokinetic outcomes in antibody developability workflows

Assessment and incorporation of in vitro correlates to pharmacokinetic outcomes in antibody developability workflows

Development of a Minimal Physiologically-Based Pharmacokinetic Modeling / Machine Learning Framework for Early Target Pharmacology Assessment

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