Cohesin is a multi-protein complex that tethers sister chromatids during mitosis and mediates DNA repair, genome compartmentalisation and regulation of gene expression. Cohesin subunits frequently acquire cancer loss-of-function alterations and act as tumour suppressors in several tumour types. This has led to increased interest in cohesin as potential target in anti-cancer therapy. Here we show that the loss-of-function of STAG2, a core component of cohesin and an emerging tumour suppressor, leads to synthetic dependency of mutated cancer cells on its paralog STAG1. STAG1 and STAG2 share high sequence identity, encode mutually exclusive cohesin subunits and retain partially overlapping functions. We inhibited STAG1 and STAG2 in several cancer cell lines where the two genes have variable mutation and copy number status. In all cases, we observed that the simultaneous blocking of STAG1 and STAG2 significantly reduces cell proliferation. We further confirmed the synthetic lethal interaction developing a vector-free CRISPR system to induce STAG1/STAG2 double gene knockout. We provide strong evidence that STAG1 is a promising therapeutic target in cancers with inactivating alterations of STAG2.

Synthetic lethal interaction between the tumour suppressor STAG2 and its paralog STAG1 / L. Benedetti, M. Cereda, L. Monteverde, N. Desai, F.D. Ciccarelli. - In: ONCOTARGET. - ISSN 1949-2553. - 8:23(2017), pp. 37619-37632. [10.18632/oncotarget.16838]

Synthetic lethal interaction between the tumour suppressor STAG2 and its paralog STAG1

L. Benedetti
Primo
;
M. Cereda;
2017

Abstract

Cohesin is a multi-protein complex that tethers sister chromatids during mitosis and mediates DNA repair, genome compartmentalisation and regulation of gene expression. Cohesin subunits frequently acquire cancer loss-of-function alterations and act as tumour suppressors in several tumour types. This has led to increased interest in cohesin as potential target in anti-cancer therapy. Here we show that the loss-of-function of STAG2, a core component of cohesin and an emerging tumour suppressor, leads to synthetic dependency of mutated cancer cells on its paralog STAG1. STAG1 and STAG2 share high sequence identity, encode mutually exclusive cohesin subunits and retain partially overlapping functions. We inhibited STAG1 and STAG2 in several cancer cell lines where the two genes have variable mutation and copy number status. In all cases, we observed that the simultaneous blocking of STAG1 and STAG2 significantly reduces cell proliferation. We further confirmed the synthetic lethal interaction developing a vector-free CRISPR system to induce STAG1/STAG2 double gene knockout. We provide strong evidence that STAG1 is a promising therapeutic target in cancers with inactivating alterations of STAG2.
Cancer vulnerability; Cohesin complex; Paralog dependency; Precision medicine; Synthetic lethality; Antigens, Nuclear; CRISPR-Cas Systems; Cell Cycle Proteins; Cell Line, Tumor; Cell Proliferation; Gene Editing; Gene Expression Regulation, Neoplastic; Humans; Loss of Function Mutation; MCF-7 Cells; Neoplasms; Nuclear Proteins; Protein Binding; RNA Interference; Tumor Suppressor Proteins
Settore BIO/11 - Biologia Molecolare
2017
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2434/898681
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