Development of PROTACs to address clinical limitations associated with BTK-targeted kinase inhibitors

Arthur, Rachael; Valle-Argos, Beatriz; Steele, Andrew J.; Packham, Graham

doi:10.37349/etat.2020.00009

Cited by 16 publications

(27 citation statements)

References 107 publications

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“…As expected, ibrutinib activity is highly susceptible to the C481S mutation due to this loss of covalent binding; a 74-fold potency decrease has been observed between mutant and wild-type BTK [ 51 ]. PROTACs are emerging as a promising alternative to circumvent the resulting ibrutinib resistance, with many examples now reported [ 52 ]. For example, PROTAC 16 ( Figure 5 ), developed by Sun et al [ 53 ], was able to degrade both wild-type and C481S mutant BTK with nanomolar potencies.…”

Section: Introductionmentioning

confidence: 99%

Current strategies for the design of PROTAC linkers: a critical review

Troup

Fallan

Baud

2020

Exploration of Targeted Anti-Tumor Therapy

185

182

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PROteolysis TArgeting Chimeras (PROTACs) are heterobifunctional molecules consisting of two ligands; an “anchor” to bind to an E3 ubiquitin ligase and a “warhead” to bind to a protein of interest, connected by a chemical linker. Targeted protein degradation by PROTACs has emerged as a new modality for the knock down of a range of proteins, with the first agents now reaching clinical evaluation. It has become increasingly clear that the length and composition of the linker play critical roles on the physicochemical properties and bioactivity of PROTACs. While linker design has historically received limited attention, the PROTAC field is evolving rapidly and currently undergoing an important shift from synthetically tractable alkyl and polyethylene glycol to more sophisticated functional linkers. This promises to unlock a wealth of novel PROTAC agents with enhanced bioactivity for therapeutic intervention. Here, the authors provide a timely overview of the diverse linker classes in the published literature, along with their underlying design principles and overall influence on the properties and bioactivity of the associated PROTACs. Finally, the authors provide a critical analysis of current strategies for PROTAC assembly. The authors highlight important limitations associated with the traditional “trial and error” approach around linker design and selection, and suggest potential future avenues to further inform rational linker design and accelerate the identification of optimised PROTACs. In particular, the authors believe that advances in computational and structural methods will play an essential role to gain a better understanding of the structure and dynamics of PROTAC ternary complexes, and will be essential to address the current gaps in knowledge associated with PROTAC design.

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Section: Introductionmentioning

confidence: 99%

Current strategies for the design of PROTAC linkers: a critical review

Troup

Fallan

Baud

2020

Exploration of Targeted Anti-Tumor Therapy

185

182

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“…BTK-PROTACs have demonstrated advantages for overcoming the drug resistance and toxicity of BTK inhibitors. − To identify orally bioavailable BTK-PROTACs, statistical methods such as PCA and DA were applied to identify the key structural features that may contribute to the oral absorption of PROTACs. After easing the interpretation and readability of the data of the structural features generated from the groups of drugs with MW < 500, MW > 500, LOB-PROTACs, and OB-PROTACs, we used a systematic investigation of model molecules to verify the features.…”

Section: Discussionmentioning

confidence: 99%

“…PROTACs are structurally composed of a target protein–ligand, a linker, and an E3 ubiquitin ligase ligand. BTK-PROTACs, including P13I and L18I , have been reported previously that demonstrate potential in overcoming drug resistance and off-target effects of ibrutinib. − Previous studies also showed that reversible covalent BTK-PROTACs, such as RC-1 , had better degradation activity and selectivity than irreversible covalent BTK-PROTACs (Figure ). − However, a major challenge preventing the widespread therapeutic application of PROTACs is their route of delivery, which limits oral bioavailability.…”

Section: Introductionmentioning

confidence: 99%

Structural Feature Analyzation Strategies toward Discovery of Orally Bioavailable PROTACs of Bruton’s Tyrosine Kinase for the Treatment of Lymphoma

et al. 2022

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Bruton's tyrosine kinase proteolysis-targeting chimeras (BTK-PROTACs) have emerged as a promising approach to address the limitations of BTK inhibitors. However, conducting the rational discovery of orally bioavailable BTK-PROTACs presents significant challenges. In this study, dimensionality reduction analysis and model molecule validation were utilized to identify some key structural features for improving the oral absorption of BTK-PROTACs. The results were applied to optimize the newly discovered BTK-PROTACs B1 and B2. Compound C13 was discovered with improved oral bioavailability, high BTK degradation activity, and selectivity. It exhibited inhibitory effects against different hematologic cancer cells and attenuated the BTK-related signaling pathway. The oral administration of C13 effectively reduced BTK protein levels and suppressed tumor growth. This study led to the discovery of a new orally bioavailable BTK-PROTAC for the treatment of lymphoma, and we hope that the strategy will find wide utility.

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“…A number of reversible BTK inhibitors such as fenebrutinib, rilzabrutinib, spebrutinib, ARQ 531, and LOXO-305 are currently being evaluated in clinical trials ( Estupinan et al, 2021 ). The second strategy is to develop BTK-targeted PROTACs ( Arthur et al, 2020 ), and several groups have explored this option. Because irreversible binding to the POI will likely negate the catalytic nature of PROTACs, reported BTK-PROTACs are mostly based on non-covalent inhibitors or convert irreversible inhibitors to reversible covalent binders ( Kiely-Collins, et al, 2021 ).…”

Section: Protacs Targeted Towards Treatment Of Various Types Of Drug ...mentioning

confidence: 99%

Overcoming Cancer Drug Resistance Utilizing PROTAC Technology

Burke

Smith

Zheng

2022

Front. Cell Dev. Biol.

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Cancer drug resistance presents a major barrier to continued successful treatment of malignancies. Current therapies inhibiting proteins indicated in cancer progression are consistently found to lose efficacy as a result of acquired drug resistance, often caused by mutated or overexpressed protein targets. By hijacking the cellular ubiquitin-proteasome protein degradation machinery, proteolysis-targeting chimeras (PROTACs) offer an alternative therapeutic modality to cancer treatments with various potential advantages. PROTACs specific for a number of known cancer targets have been developed in the last 5 years, which present new options for remission in patients with previously untreatable malignancies and provide a foundation for future-generation compounds. One notable advantage of PROTACs, supported by evidence from a number of recent studies, is that they can overcome some of the resistance mechanisms to traditional targeted therapies. More recently, some groups have begun researching the use of PROTACs to successfully degrade mutated targets conferring cancer resistance against first-line treatments. In this review, we focus on analyzing the developments in PROTACs geared towards cancer resistance and targets that confer it in the search for new and successful therapies.

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Development of PROTACs to address clinical limitations associated with BTK-targeted kinase inhibitors

Cited by 16 publications

References 107 publications

Current strategies for the design of PROTAC linkers: a critical review

Current strategies for the design of PROTAC linkers: a critical review

Structural Feature Analyzation Strategies toward Discovery of Orally Bioavailable PROTACs of Bruton’s Tyrosine Kinase for the Treatment of Lymphoma

Overcoming Cancer Drug Resistance Utilizing PROTAC Technology

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