Industry Perspective on the Pharmacokinetic and Absorption, Distribution, Metabolism, and Excretion Characterization of Heterobifunctional Protein Degraders

Volak, Laurie P; Duevel, Heide Marika; Humphreys, Sara C.; Nettleton, David O.; Phipps, Colin; Pike, Andy; Rynn, Caroline; Scott‐Stevens, Paul; Zhang, Donglu; Zientek, Michael

doi:10.1124/dmd.122.001154

Cited by 25 publications

(12 citation statements)

References 50 publications

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“…Second, there is an ongoing need for more predictive in vitro ADME assays for PROTACs. It has been noted as a general trend across multiple companies, , as well as at Arvinas, that such assays as configured for more traditional small molecules are often poorly predictive of in vivo PROTAC behavior. Third, greater attention to the potential of parenterally administered PROTACs is warranted.…”

Section: Discussionmentioning

confidence: 99%

Physicochemical Property Determinants of Oral Absorption for PROTAC Protein Degraders

Hornberger

Araujo

2023

J. Med. Chem.

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Heterobifunctional PROTAC degraders are gaining attention as a differentiated therapeutic modality with the potential for oral dosing in the clinic. Belonging to the beyond Rule of Five domain of physicochemical property space, we have sought to understand the determinants of oral absorption for this class of molecules for the rapid development of novel oral agents. We have collected a large data set from PROTAC molecules that have been dosed orally and intravenously in rats to estimate the fraction absorbed from oral dosing. Through this estimation, effects from differential hepatic clearance are normalized, allowing for a better assessment of the absorption. We demonstrate that rats are less permissive to PROTAC absorption than mice. The physicochemical properties of the molecules are then evaluated once compounds are rank-ordered by the fraction absorbed. We derive suggested design constraints on physicochemical properties for PROTAC molecules that are associated with higher probability of being orally absorbed.

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Section: Discussionmentioning

confidence: 99%

Physicochemical Property Determinants of Oral Absorption for PROTAC Protein Degraders

Hornberger

Araujo

2023

J. Med. Chem.

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“…It should be stated that others have found insolubility or non-specific binding to occasionally give confounding results for such high molecular weight compounds in similar assays, 7 echoing experience within GSK laboratories, and so this should be considered as a possibility when unexpected in vitro biological data is obtained. 55…”

Section: Degrader Discovery Using Dna-encoded Library (Del) Technologymentioning

confidence: 99%

Innovative, combinatorial and high-throughput approaches to degrader synthesis

Stevens,

Thompson,

Fournier

et al. 2024

Chem. Soc. Rev.

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“…PROTACs are also large molecules which extend into challenging non-traditional, “beyond rule of 5” (bRo5) property space ( Matsson et al, 2016 ; Volak et al, 2023 ). There are additional resulting challenges: (i) larger molecules can behave differently especially regarding permeability and transport ( Guimaraes et al, 2012 ; Doak et al, 2014 ; Matsson et al, 2016 ; Matsson and Kihlberg, 2017 ; Pye et al, 2017 ; Linker et al, 2023 ); (ii) available chemical space is larger; (iii) large molecules are often more conformationally complex ( Rossi Sebastiano et al, 2018 ; Mobitz, 2023 ); (iv) fewer molecules from bRo5 space have been studied; (v) those studied molecules cluster in niches (e.g., macrocycles) and represent a less even distribution ( Doak et al, 2014 ).…”

Section: Protac Molecular Design Constraintsmentioning

confidence: 99%

“…While the extent to which this behavior is observed in bRo5 chemical matter is debated ( Mobitz, 2023 ), accessible conformations of significantly lower polarity than suggested by TPSA values may be required ( Whitty et al, 2016 ; Mobitz, 2023 ). Tight restrictions on hydrogen bonding are suggested ( Doak et al, 2014 ; Matsson et al, 2016 ; Whitty et al, 2016 ; Mobitz, 2023 ; Volak et al, 2023 ).…”

Section: Protac Molecular Design Constraintsmentioning

confidence: 99%

“…Additionally, increased efflux is common in bRo5 ( Doak et al, 2014 ; Matsson et al, 2016 ; Cantrill et al, 2020 ; Cox et al, 2023 ) and PROTAC development space ( Klein et al, 2021 ). Beyond CNS considerations, the combination of differentiated property space (in particular lipophilicity) and pharmacology results in additional considerations around absorption, distribution, metabolism, and excretion (ADME) testing ( Cantrill et al, 2020 ; Pike et al, 2020 ; Apprato et al, 2023 ; Hornberger and Araujo, 2023 ; Volak et al, 2023 ).…”

Section: Protac Molecular Design Constraintsmentioning

confidence: 99%

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Targeted protein degradation in CNS disorders: a promising route to novel therapeutics?

Kuemper,

Cairns,

Birchall

et al. 2024

Front. Mol. Neurosci.

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Targeted protein degradation (TPD) is a rapidly expanding field, with various PROTACs (proteolysis-targeting chimeras) in clinical trials and molecular glues such as immunomodulatory imide drugs (IMiDs) already well established in the treatment of certain blood cancers. Many current approaches are focused on oncology targets, leaving numerous potential applications underexplored. Targeting proteins for degradation offers a novel therapeutic route for targets whose inhibition remains challenging, such as protein aggregates in neurodegenerative diseases. This mini review focuses on the prospect of utilizing TPD for neurodegenerative disease targets, particularly PROTAC and molecular glue formats and opportunities for novel CNS E3 ligases. Some key challenges of utilizing such modalities including molecular design of degrader molecules, drug delivery and blood brain barrier penetrance will be discussed.

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Industry Perspective on the Pharmacokinetic and Absorption, Distribution, Metabolism, and Excretion Characterization of Heterobifunctional Protein Degraders

Cited by 25 publications

References 50 publications

Physicochemical Property Determinants of Oral Absorption for PROTAC Protein Degraders

Physicochemical Property Determinants of Oral Absorption for PROTAC Protein Degraders

Innovative, combinatorial and high-throughput approaches to degrader synthesis

Targeted protein degradation in CNS disorders: a promising route to novel therapeutics?

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