The Advantages of Targeted Protein Degradation Over Inhibition: An RTK Case Study

Burslem, George M.; Smith, Blake E.; Lai, Ashton C.; Jaime‐Figueroa, Saul; McQuaid, Daniel; Bondeson, Daniel P.; Toure, Momar; Dong, Hanqing; Qian, Yimin; Wang, Jing; Crew, Andrew P.; Hines, John; Crews, Craig M.

doi:10.1016/j.chembiol.2017.09.009

Cited by 480 publications

(522 citation statements)

References 63 publications

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“…They showed that the PROTACs significantly decreased cellular levels of ALK fusion proteins in different cell lines including SU-DHL-1 (lymphoma) and NCI-H2228 (lung cancer). 94 Interestingly, the PROTAC mediated the internalization of EGFR and sorted to lysosomal degradation, 94 although the RTKs usually prefer to internalize into a recycle endosome. 80 Kang et al later on proved that a synthesized PROTACs against ALK (based on VHL) worked in vivo.…”

Section: Targeting Protein Kinasesmentioning

confidence: 99%

The PROTAC technology in drug development

Zou

Wang

2019

Cell Biochemistry & Function

197

135

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Currently, a new technology termed PROTAC, proteolysis targeting chimera, has been developed for inducing the protein degradation by a targeting molecule. This technology takes advantage of a moiety of targeted protein and a moiety of recognizing E3 ubiquitin ligase and produces a hybrid molecule to specifically knock down a targeted protein. During the first decade, three pedigreed groups worked on the development of this technology. To date, this technology has been extended by different groups, aiming to develop new drugs against different diseases including cancers. This review summarizes the contributions of the groups for the development of PROTAC. Significance of the study This review summarized the development of the PROTAC technology for readers and also presented the author's opinions on the application of the technology in tumor therapy.

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Section: Targeting Protein Kinasesmentioning

confidence: 99%

The PROTAC technology in drug development

Zou

Wang

2019

Cell Biochemistry & Function

197

135

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“…Compound 3i can completely knockdown TBK1 in several cancer cell lines at a concentration of 100 nM, indicating the excellent efficiency of this compound (Figure d) . In addition, VHL‐based PROCTACs have been shown to target transmembrane receptor tyrosine kinases (RTKs) as well as mutants of RTKs …”

Section: All‐small‐molecule Protacs: a Potent And Promising Tool To Ementioning

confidence: 95%

PROTACs: An Emerging Targeting Technique for Protein Degradation in Drug Discovery

et al. 2018

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Proteolysis-targeting chimeric molecules (PROTACs) represent an emerging technique that is receiving much attention for therapeutic intervention. The mechanism is based on the inhibition of protein function by hijacking a ubiquitin E3 ligase for protein degradation. The hetero-bifunctional PROTACs contain a ligand for recruiting an E3 ligase, a linker, and another ligand to bind with the protein targeted for degradation. Thus, PROTACs have profound potential to eliminate "undruggable" protein targets, such as transcription factors and non-enzymatic proteins, which are not limited to physiological substrates of the ubiquitin-proteasome system. These findings indicate great prospects for PROTACs in the development of therapeutics. However, there are several limitations related to poor stability, biodistribution, and penetrability in vivo. This review provides an overview of the main PROTAC-based approaches that have been developed and discusses the promising opportunities and considerations for the application of this technology in therapies and drug discovery.

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“…Targeted protein degradation, using heterobifunctional small molecules (PROTACs) to remove protein targets from within cells, has emerged as a novel strategy for drug development, with the opportunity of providing therapeutic interventions not achievable with existing occupancy‐based enzyme inhibition approaches . Small‐molecular‐weight synthetic PROTACs ( 185‐189 ) have been used to selectively degrade various specific proteins (Figure ), including pirin, sirt2, BET protein, androgen receptor, and BRD4 protein …”

Section: Exploitation Of Solvent‐exposed Regions For the Rational Desmentioning

confidence: 99%

“…into one molecule, to take advantage of the presence of large hydrophobic patches at the HDAC surface rim. 122 Some encouraging results have been reported (Figure 22), such as dual-acting HDAC and topoisomerase II inhibitor On the basis of these analyses, a structure-based hybridization strategy was used to discover novel Mcl-1/Bcl-xL dual inhibitors (159,160) with a suitable linker based on 157 and 158 ( Figure 22). Notably, compound 160 displayed the potent dual-inhibitory activities (Mcl-1, IC 50 = 0.088 μM; and Bcl-xL, IC 50 = 0.0037 μM) ( Figure 23).…”

Section: Many Of These Inhibitors Show Potency Against Rt and In At Mmentioning

confidence: 99%

Molecular design opportunities presented by solvent‐exposed regions of target proteins

Jiang

Zhou

et al. 2019

Medicinal Research Reviews

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Solvent‐exposed regions, or solvent‐filled pockets, within or adjacent to the ligand‐binding sites of drug‐target proteins provide opportunities for substantial modifications of existing small‐molecular drug molecules without serious loss of activity. In this review, we present recent selected examples of exploitation of solvent‐exposed regions of proteins in drug design and development from the recent medicinal‐chemistry literature.

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The Advantages of Targeted Protein Degradation Over Inhibition: An RTK Case Study

Cited by 480 publications

References 63 publications

The PROTAC technology in drug development

The PROTAC technology in drug development

PROTACs: An Emerging Targeting Technique for Protein Degradation in Drug Discovery

Molecular design opportunities presented by solvent‐exposed regions of target proteins

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