Establishing <i>in vitro in vivo</i> correlations to screen monoclonal antibodies for physicochemical properties related to favorable human pharmacokinetics

Avery, Lindsay B.; Wade, Jason; Wang, Mengmeng; Tam, Amy; King, Amy; Piché-Nicholas, Nicole; Kavosi, Mania; Penn, S.; Cirelli, David; Kurz, Jeffrey C.; Zhang, Minlei; Cunningham, Orla; Jones, Rhys D.O.; Fennell, Brian J.; McDonnell, Barry J.; Sakorafas, Paul; Apgar, James R.; Finlay, William J. J.; Lin, Laura; Bloom, Laird; O’Hara, Denise M

doi:10.1080/19420862.2017.1417718

Cited by 78 publications

(124 citation statements)

References 48 publications

(105 reference statements)

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“…5). This trend has been observed previously with a larger dataset of mAbs 32 and suggests that the AC-SINS assay is a useful screening tool to de-select mAbs that have the potential for fast clearance in humans.…”

Section: Discussionsupporting

confidence: 81%

“…An AC-SINS assay was used to screen 11 of the mAbs in the dataset. An AC-SINS score of >11 has been associated with high self-association 32 . The AC-SINS scores for the subset of mAbs tested from this dataset ranged from 0 to 24, with 3 mAbs exhibiting higher than typical CL having scores of 11–24.…”

Section: Discussionmentioning

confidence: 91%

“…The mechanism of this non-specificity has not been fully elucidated, but could be in part due to hydrophobicity/ positive charged patches on mAbs 31 . To test this, an in vitro high throughput assay measuring non-specific binding was implemented and used to identify mAbs with increased risk of having fast CL in humans 32 . An AC-SINS assay was used to screen 11 of the mAbs in the dataset.…”

Section: Discussionmentioning

confidence: 99%

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Linear pharmacokinetic parameters for monoclonal antibodies are similar within a species and across different pharmacological targets: A comparison between human, cynomolgus monkey and hFcRn Tg32 transgenic mouse using a population-modeling approach

Betts

Keunecke²,

Steeg³

et al. 2018

mAbs

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The linear pharmacokinetics (PK) of therapeutic monoclonal antibodies (mAbs) can be considered a class property with values that are similar to endogenous IgG. Knowledge of these parameters across species could be used to avoid unnecessary in vivo PK studies and to enable early PK predictions and pharmacokinetic/pharmacodynamic (PK/PD) simulations. In this work, population-pharmacokinetic (popPK) modeling was used to determine a single set of ‘typical’ popPK parameters describing the linear PK of mAbs in human, cynomolgus monkey and transgenic mice expressing the human neonatal Fc receptor (hFcRn Tg32), using a rich dataset of 27 mAbs. Non-linear PK was excluded from the datasets and a 2-compartment model was applied to describe mAb disposition. Typical human popPK estimates compared well with data from comparator mAbs with linear PK in the clinic. Outliers with higher than typical clearance were found to have non-specific interactions in an affinity-capture self-interaction nanoparticle spectroscopy assay, offering a potential tool to screen out these mAbs at an early stage. Translational strategies were investigated for prediction of human linear PK of mAbs, including use of typical human popPK parameters and allometric exponents from cynomolgus monkey and Tg32 mouse. Each method gave good prediction of human PK with parameters predicted within 2-fold. These strategies offer alternative options to the use of cynomolgus monkeys for human PK predictions of linear mAbs, based on in silico methods (typical human popPK parameters) or using a rodent species (Tg32 mouse), and call into question the value of completing extensive in vivo preclinical PK to inform linear mAb PK.

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Section: Discussionsupporting

confidence: 81%

Section: Discussionmentioning

confidence: 91%

Section: Discussionmentioning

confidence: 99%

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Linear pharmacokinetic parameters for monoclonal antibodies are similar within a species and across different pharmacological targets: A comparison between human, cynomolgus monkey and hFcRn Tg32 transgenic mouse using a population-modeling approach

Betts

Keunecke²,

Steeg³

et al. 2018

mAbs

Self Cite

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“…In conventional antibody drug discoveries, early screening and optimization steps focus on characteristics such as binding activity, potency, and stability for selection of lead constructs, while pharmacokinetic properties which can influence both efficacy and toxicity are typically characterized later in development and on a small number of lead monoclonal antibody constructs. Predicting pharmacokinetic properties of antibodies in the genotypebased screening can reduce the time needed for drug discovery and development by improving the lead monoclonal antibody selection process 33 . TrueRepertoire™ provides a highly accurate consensus sequence of the clones.…”

Section: Discussionmentioning

confidence: 99%

“…Using the consensus sequence and clonal frequency of the clones, characteristics of clones, including pharmacokinetics of antibodies, can be expected. Therefore, clones can be selected based on genotype-based screening results, and the selected clones can be retrieved by referring to the barcode information of the consensus sequence 7,33,34 . As a representative example of the genotype-based screening through TrueRepertoire™, charge distribution of antibodies can be analyzed by the consensus sequence of the clones, then clones expected to have poor pharmacokinetics can be excluded in the retrieval.…”

Section: Discussionmentioning

confidence: 99%

High-throughput retrieval of physical DNA for NGS-identifiable clones in phage display library

Noh

Kim

Jung³

et al. 2018

Preprint

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In antibody discovery, in-depth analysis of an antibody library and high-throughput retrieval of clones in the library are crucial to identifying and exploiting rare clones with different properties. However, existing methods have several technical limitations such as low process throughput from laborious cloning process and waste of the phenotypic screening capacity from unnecessary repetitive tests on the dominant clones. To overcome the limitations, we developed a new high-throughput platform for the identification and retrieval of clones in the library, TrueRepertoire™. TrueRepertoire™ provides highly accurate sequences of the clones with linkage information between heavy and light chains of the antibody fragment. Additionally, the physical DNA of clones can be retrieved in high throughput based on the sequence information. We validated the high accuracy of the sequences and demonstrated that there is no platform-specific bias. Moreover, the applicability of TrueRepertoire™ was demonstrated by a phage-displayed single-chain variable fragment (scFv) library targeting human hepatocyte growth factor (hHGF) protein.

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PBPK Modeling of Biotherapeutics

2021

Physiologically Based Pharmacokinetic (PBPK) Modeling and Simulations

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Establishing in vitro in vivo correlations to screen monoclonal antibodies for physicochemical properties related to favorable human pharmacokinetics

Cited by 78 publications

References 48 publications

Linear pharmacokinetic parameters for monoclonal antibodies are similar within a species and across different pharmacological targets: A comparison between human, cynomolgus monkey and hFcRn Tg32 transgenic mouse using a population-modeling approach

Linear pharmacokinetic parameters for monoclonal antibodies are similar within a species and across different pharmacological targets: A comparison between human, cynomolgus monkey and hFcRn Tg32 transgenic mouse using a population-modeling approach

High-throughput retrieval of physical DNA for NGS-identifiable clones in phage display library

PBPK Modeling of Biotherapeutics

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