A Peptide Binder of E3 Ligase Adaptor SPOP Disrupts Oncogenic SPOP‐Protein Interactions in Kidney Cancer Cells

A Peptide Binder of E3 Ligase Adaptor SPOP Disrupts Oncogenic SPOP‐Protein Interactions in Kidney Cancer Cells

Main observation and conclusion The E3 ligase adaptor SPOP, overexpressed in the nucleus but frequently dislocated into the cytoplasm in all clear cell Renal Cell Carcinomas (ccRCC), serves as a regulatory hub to promote kidney cancer through the ubiquitination and degradation of multiple downstream...

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Veröffentlicht in:Chinese journal of chemistry 2021-02, Vol.39 (2), p.274-280
Hauptverfasser: Wang, Zhen, Zhang, Hao, Chen, Baoen, Ouyang, Sisheng, Zheng, Tong, Zhou, Ran, Dong, Ze, Huang, Yue, Zhang, Tao, Jiang, Hualiang, Gan, Jianhua, Luo, Cheng, Yang, Cai‐Guang
Format: Artikel
Sprache:eng
Schlagworte:
Binding
Cancer
Cell proliferation
Chemistry
Chemistry, Multidisciplinary
Clear cell Renal Cell Carcinomas
Clear cell-type renal cell carcinoma
Computer applications
Crystal structure
Cytoplasm
Domains
Homology
Kidney cancer
Kidneys
Peptide inhibitor
Peptide inhibitors
Peptides
Permeability
Physical Sciences
Protein interaction
Proteins
Protein‐protein interaction
PTEN protein
Science & Technology
Signal transduction
SPOP
Substrate inhibition
Tensin
Ubiquitin-protein ligase
Ubiquitination
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Zusammenfassung:Main observation and conclusion The E3 ligase adaptor SPOP, overexpressed in the nucleus but frequently dislocated into the cytoplasm in all clear cell Renal Cell Carcinomas (ccRCC), serves as a regulatory hub to promote kidney cancer through the ubiquitination and degradation of multiple downstream cancer proteins. Recently, our identification of a selective small‐molecule inhibitor of the SPOP‐phosphatase and tensin homolog (PTEN) interaction has demonstrated that the oncogenic SPOP‐protein interaction would be a druggable target specific to ccRCC therapy. To our knowledge, this is the first time such a small‐molecule inhibitor has been developed. Herein, we have identified a peptide binder for the SPOP‐MATH domain that disrupts the oncogenic SPOP‐protein interactions in kidney cancer cells. Computational design and biophysical characterization yielded peptide Pep38 that binds to the MATH domain of SPOP and competes on PTEN‐binding to SPOP in vitro. The X‐ray complex structure reveals that the peptide binder features the following combination: one, a mimic of the native peptide binder and two, an additional β‐strand motif in sequence, which could contribute to increased binding affinity. In order to improve cellular permeability, we fused Pep38 with the delivery peptide TAT to prepare peptide TAT38, which inhibits the endogenous substrate binding to SPOP and suppresses the proliferation of the ccRCC cells. Our identification of the peptide inhibitors for SPOP‐protein interactions provides further validation that the oncogenic SPOP‐signaling pathway in ccRCC could be a druggable target specifically applicable to the therapy of kidney cancers. The E3 ligase adaptor SPOP is overexpressed and dislocated into the cytoplasm in all ccRCC, which can promote proliferation and lead to kidney tumorigenesis. Through computational design, biophysical characterization and a TAT‐delivery sequence incorporated, we identified TAT38 that can disrupt SPOP‐substrate interactions. The peptide inhibitors provide that the oncogenic SPOP‐signaling pathway in ccRCC could be a druggable target specifically applicable to the therapy of kidney cancers.
ISSN:1001-604X
1614-7065
DOI:10.1002/cjoc.202000462