Polo-like kinase 1 inhibition as a therapeutic approach to selectively target BRCA1-deficient cancer cells by synthetic lethality induction

Carbajosa González, Sofía; Pansa, Maria Florencia; Paviolo, Natalia Soledad; Castellaro, Andrés Marcos; Andino, Diego Leonardo; Nigra, Ayelén Denise; García, Iris Alejandra; Racca, Ana Cristina; Rodriguez, María Celeste; Angiolini, Virginia Andrea; Guantay, Maria Laura; Villafañez, Florencia; Federico, Maria Belén; Rodríguez, Lucía; Caputto, Beatriz Leonor; Drewes, Gerard; Madauss, Kevin P.; Gloger, Israel; Fernandez, Elmer Andres; Gil, German Alejandro; Bocco, Jose Luis; Gottifredi, Vanesa; Soria, Ramiro Gaston

info:eu-repo/semantics/article

Date

2019-03

Registration in:

Carbajosa González, Sofía; Pansa, Maria Florencia; Paviolo, Natalia Soledad; Castellaro, Andrés Marcos; Andino, Diego Leonardo; et al.; Polo-like kinase 1 inhibition as a therapeutic approach to selectively target BRCA1-deficient cancer cells by synthetic lethality induction; American Association for Cancer Research; Clinical Cancer Research; 25; 13; 3-2019; 4049-4062

1078-0432

http://hdl.handle.net/11336/130078

CONICET Digital

CONICET

https://repositorioslatinoamericanos.uchile.cl/handle/2250/4364387

Author

Carbajosa González, Sofía

Pansa, Maria Florencia

Paviolo, Natalia Soledad

Castellaro, Andrés Marcos

Andino, Diego Leonardo

Nigra, Ayelén Denise

García, Iris Alejandra

Racca, Ana Cristina

Rodriguez, María Celeste

Angiolini, Virginia Andrea

Guantay, Maria Laura

Villafañez, Florencia

Federico, Maria Belén

Rodríguez, Lucía

Caputto, Beatriz Leonor

Drewes, Gerard

Madauss, Kevin P.

Gloger, Israel

Fernandez, Elmer Andres

Gil, German Alejandro

Bocco, Jose Luis

Gottifredi, Vanesa

Soria, Ramiro Gaston

Institutions

Consejo Nacional de Investigaciones Científicas y Tecnológicas (Argentina)

Abstract

Purpose: BRCA1 and BRCA2 deficiencies are widespread drivers of human cancers that await the development of targeted therapies. We aimed to identify novel synthetic lethal relationships with therapeutic potential using BRCA-deficient isogenic backgrounds. Experimental Design: We developed a phenotypic screening technology to simultaneously search for synthetic lethal (SL) interactions in BRCA1- and BRCA2-deficient contexts. For validation, we developed chimeric spheroids and a dualtumor xenograft model that allowed the confirmation of SL induction with the concomitant evaluation of undesired cytotoxicity on BRCA-proficient cells. To extend our results using clinical data, we performed retrospective analysis on The Cancer Genome Atlas (TCGA) breast cancer database. Results: The screening of a kinase inhibitors library revealed that Polo-like kinase 1 (PLK1) inhibition triggers strong SL induction in BRCA1-deficient cells. Mechanistically, we found no connection between the SL induced by PLK1 inhibition and PARP inhibitors. Instead, we uncovered that BRCA1 downregulation and PLK1 inhibition lead to aberrant mitotic phenotypes with altered centrosomal duplication and cytokinesis, which severely reduced the clonogenic potential of these cells. The penetrance of PLK1/BRCA1 SL interaction was validated using several isogenic and nonisogenic cellular models, chimeric spheroids, and mice xenografts. Moreover, bioinformatic analysis revealed high-PLK1 expression in BRCA1-deficient tumors, a phenotype that was consistently recapitulated by inducing BRCA1 deficiency in multiple cell lines as well as in BRCA1-mutant cells. Conclusions: We uncovered an unforeseen addiction of BRCA1-deficient cancer cells to PLK1 expression, which provides a new means to exploit the therapeutic potential of PLK1 inhibitors in clinical trials, by generating stratification schemes that consider this molecular trait in patient cohorts.

Subjects

letalidad sintetica

expresion de genes

cancer

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