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. 2021 May;20(5):775-786.
doi: 10.1158/1535-7163.MCT-20-0283. Epub 2021 Mar 1.

The Discovery of a Novel Antimetastatic Bcl3 Inhibitor

Jitka Soukupová  1   2 Cinzia Bordoni  1 Daniel J Turnham  2 William W Yang  2 Gillian Seaton  2 Aleksandra Gruca  2 Rhiannon French  2 Kok Yung Lee  1 Athina Varnava  2 Luke Piggott  2 Richard W E Clarkson  2 Andrew D Westwell  1 Andrea Brancale  3
Affiliations

The Discovery of a Novel Antimetastatic Bcl3 Inhibitor

Jitka Soukupová et al. Mol Cancer Ther. 2021 May.

Abstract

The development of antimetastatic drugs is an urgent healthcare priority for patients with cancer, because metastasis is thought to account for around 90% of cancer deaths. Current antimetastatic treatment options are limited and often associated with poor long-term survival and systemic toxicities. Bcl3, a facilitator protein of the NF-κB family, is associated with poor prognosis in a range of tumor types. Bcl3 has been directly implicated in the metastasis of tumor cells, yet is well tolerated when constitutively deleted in murine models, making it a promising therapeutic target. Here, we describe the identification and characterization of the first small-molecule Bcl3 inhibitor, by using a virtual drug design and screening approach against a computational model of the Bcl3-NF-kB1(p50) protein-protein interaction. From selected virtual screening hits, one compound (JS6) showed potent intracellular Bcl3-inhibitory activity. JS6 treatment led to reductions in Bcl3-NF-kB1 binding, tumor colony formation, and cancer cell migration in vitro; and tumor stasis and antimetastatic activity in vivo, while being devoid of overt systemic toxicity. These results represent a successful application of in silico screening in the identification of protein-protein inhibitors for novel intracellular targets, and confirm Bcl3 as a potential antimetastatic target.

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