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Disruption of the MSL complex inhibits tumour maintenance by exacerbating chromosomal instability

Nat Cell Biol. 2021-04; 
Josep Monserrat, Cristina Morales Torres, Louise Richardson, Thomas Stuart Wilson, Harshil Patel, Marie-Charlotte Domart, Stuart Horswell, Ok-Ryul Song, Ming Jiang, Margaret Crawford, Minh Bui, Yamini Dalal, Paola Scaffidi
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Plasmid DNA Preparation 4 different plasmids were obtained from GenScript: pcDNA3.3-Cas9 for Cas9 expression, pCR Blunt II TOPO-sgRNA1 and 2 against DCN’s 3’UTR Get A Quote

摘要

Rewiring of cellular programmes in malignant cells generates cancer-specific vulnerabilities. Here, using an unbiased screening strategy aimed at identifying non-essential genes required by tumour cells to sustain unlimited proliferative capacity, we identify the male-specific lethal (MSL) acetyltransferase complex as a vulnerability of genetically unstable cancers. We find that disruption of the MSL complex and consequent loss of the associated H4K16ac mark do not substantially alter transcriptional programmes but compromise chromosome integrity and promote chromosomal instability (CIN) that progressively exhausts the proliferative potential of cancer cells through a p53-independent mechanism. This effect is d... More

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