A Versatile and Sustainable Multicomponent Platform for the Synthesis of Protein Degraders: Proof-of-Concept Application to BRD4-Degrading PROTACs

Bhela, Irene Preet; Ranza, Alice; Balestrero, Federica Carolina; Serafini, M. Teresa; Aprile, Silvio; Martino, Rita Maria Concetta Di; Condorelli, Fabrizio; Pirali, Tracey

doi:10.1021/acs.jmedchem.2c01218

Cited by 24 publications

(28 citation statements)

References 57 publications

(172 reference statements)

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“…So far, MCRs have attracted little attention in the field of E3 ligase ligand discovery and optimization. 39,40 With the aid of the Petasis reaction, easy access to three-winged substances with excellent CRBN binding affinities was realized. Their effects on neosubstrates, such as IKZF3, seem to be highly correlated with the affinity data.…”

Section: Paper Rsc Chemical Biologymentioning

confidence: 99%

Accessing three-branched high-affinity cereblon ligands for molecular glue and protein degrader design

et al. 2023

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Section: Paper Rsc Chemical Biologymentioning

confidence: 99%

Accessing three-branched high-affinity cereblon ligands for molecular glue and protein degrader design

et al. 2023

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“…Current strategies for increasing synthetic throughput have been introduced through Staudinger ligation chemistry, 80 solid-phase synthesis, 81 copper-catalyzed click chemistry, 82 activated esters, 83 the rapid synthesis of PROTACs (Rapid-TAC) platform, 84 and the modular synthetic platform. 85 Notably, a late-stage single-step reductive deoxyge-nation method allows immediate conversion from thalidomidecontaining PROTACs to lenalidomide groups without a de novo synthesis. 86 A few studies have focused on the synthesis methodology of PROTAC fragments.…”

Section: Molecular Glue Functionmentioning

confidence: 99%

Advancing Strategies for Proteolysis-Targeting Chimera Design

Zhi

Liu

et al. 2023

J. Med. Chem.

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Proteolysis-targeting chimeras (PROTACs) have shown great therapeutic potential by degrading various disease-causing proteins, particularly those related to tumors. Therefore, the introduction of PROTACs has ushered in a new chapter of antitumor drug development, marked by significant advances over recent years. Herein, we describe recent developments in PROTAC technology, focusing on design strategy, development workflow, and future outlooks. We also discuss potential opportunities and challenges for PROTAC research.

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“…As a result, an ortho,ortho′-disubstituted aromatic ring directly attached to the ester moiety provided hydrolytic stability independent of the chemical nature of the R 2 group of the aldehyde (Scheme 2). However, when R 2 was a bulky substituent, an increased hydrolytic stability was observed only Recently, Pirali and colleagues 24 reported a cutting-edge application of MCRs to new chemical modalities, in particular to proteolysis targeting chimeras (PROTACs). 3 They leverage the versatility of the Passerini MCR as a modular synthetic platform to build heterobifunctional protein degraders.…”

Section: Reaction)mentioning

confidence: 99%

“…Recently, Pirali and colleagues reported a cutting-edge application of MCRs to new chemical modalities, in particular to proteolysis targeting chimeras (PROTACs) . They leverage the versatility of the Passerini MCR as a modular synthetic platform to build heterobifunctional protein degraders.…”

Section: Passerini Reaction (Three-component Reaction)mentioning

confidence: 99%

Accelerating Drug Discovery: Synthesis of Complex Chemotypes via Multicomponent Reactions

Buskes¹,

Coffin²,

Troast³

et al. 2023

ACS Med. Chem. Lett.

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The generation of multiple bonds in one reaction step has attracted massive interest in drug discovery and development. Multicomponent reactions (MCRs) offer the advantage of combining three or more reagents in a one-pot fashion to effectively yield a synthetic product. This approach significantly accelerates the synthesis of relevant compounds for biological testing. However, there is a perception that this methodology will only produce simple chemical scaffolds with limited use in medicinal chemistry. In this Microperspective, we want to highlight the value of MCRs toward the synthesis of complex molecules characterized by the presence of quaternary and chiral centers. This paper will cover specific examples showing the impact of this technology toward the discovery of clinical compounds and recent breakthroughs to expand the scope of the reactions toward topologically rich molecular chemotypes.

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A Versatile and Sustainable Multicomponent Platform for the Synthesis of Protein Degraders: Proof-of-Concept Application to BRD4-Degrading PROTACs

Cited by 24 publications

References 57 publications

Accessing three-branched high-affinity cereblon ligands for molecular glue and protein degrader design

Accessing three-branched high-affinity cereblon ligands for molecular glue and protein degrader design

Advancing Strategies for Proteolysis-Targeting Chimera Design

Accelerating Drug Discovery: Synthesis of Complex Chemotypes via Multicomponent Reactions

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