Synergistic Effects of PARP Inhibition and Cholesterol Biosynthesis Pathway Modulation.

Rutkowska, Anna; Eberl, H Christian; Werner, Thilo; Hennrich, Marco L; Sévin, Daniel C; Petretich, Massimo; Reddington, James P; Pocha, Shirin; Gade, Stephan; Martinez-Segura, Amalia; Dvornikov, Dmytro; Karpiak, Joel; Sweetman, Gavain M A; Fufezan, Christian; Duempelfeld, Birgit; Braun, Florian; Schofield, Christopher; Keles, Hakan; Alvarado, David; Wang, Zhuo; Jansson, Keith H; Faelth-Savitski, Maria; Curry, Edward; Remlinger, Katja; Stronach, Euan A; Feng, Bin; Sharma, Geeta; Coleman, Kevin; Grandi, Paola; Bantscheff, Marcus; Bergamini, Giovanna

Rutkowska, Anna; Eberl, H Christian; Werner, Thilo; Hennrich, Marco L; Sévin, Daniel C; Petretich, Massimo; Reddington, James P; Pocha, Shirin; Gade, Stephan; Martinez-Segura, Amalia; Dvornikov, Dmytro; Karpiak, Joel; Sweetman, Gavain M A; Fufezan, Christian; Duempelfeld, Birgit; Braun, Florian; Schofield, Christopher; Keles, Hakan; Alvarado, David; Wang, Zhuo; Jansson, Keith H; Faelth-Savitski, Maria; Curry, Edward; Remlinger, Katja; Stronach, Euan A; Feng, Bin; Sharma, Geeta; Coleman, Kevin; Grandi, Paola; Bantscheff, Marcus; Bergamini, Giovanna.

Afiliação

Rutkowska A; Cellzome, GSK, R&D, Heidelberg, Germany.
Eberl HC; Cellzome, GSK, R&D, Heidelberg, Germany.
Werner T; Cellzome, GSK, R&D, Heidelberg, Germany.
Hennrich ML; Cellzome, GSK, R&D, Heidelberg, Germany.
Sévin DC; Cellzome, GSK, R&D, Heidelberg, Germany.
Petretich M; Cellzome, GSK, R&D, Heidelberg, Germany.
Reddington JP; Cellzome, GSK, R&D, Heidelberg, Germany.
Pocha S; Cellzome, GSK, R&D, Heidelberg, Germany.
Gade S; Cellzome, GSK, R&D, Heidelberg, Germany.
Martinez-Segura A; Genomic Sciences, R&D, GSK, Heidelberg, Germany.
Dvornikov D; Cellzome, GSK, R&D, Heidelberg, Germany.
Karpiak J; Medicine Design-Computational Sciences, R&D, GSK, Heidelberg, Germany.
Sweetman GMA; Cellzome, GSK, R&D, Heidelberg, Germany.
Fufezan C; Data Streams and Operations, and Data Science and Data Engineering, R&D, GSK, Heidelberg, Germany.
Duempelfeld B; Centre for Organismal Studies, Heidelberg University, Heidelberg, Germany.
Braun F; Cellzome, GSK, R&D, Heidelberg, Germany.
Schofield C; Chemical Biology Core Facility, EMBL Heidelberg, Heidelberg, Germany.
Keles H; Genomic Sciences, R&D, GSK, Heidelberg, Germany.
Alvarado D; Genomic Sciences, R&D, GSK, Heidelberg, Germany.
Wang Z; Oncology, Synthetic Lethality Research Unit, R&D, GSK, Heidelberg, Germany.
Jansson KH; Oncology, Synthetic Lethality Research Unit, R&D, GSK, Heidelberg, Germany.
Faelth-Savitski M; Genomic Sciences, R&D, GSK, Heidelberg, Germany.
Curry E; Cellzome, GSK, R&D, Heidelberg, Germany.
Remlinger K; Genomic Sciences, R&D, GSK, Heidelberg, Germany.
Stronach EA; Biostatistics R&D, GSK, Heidelberg, Germany.
Feng B; Genomic Sciences, R&D, GSK, Heidelberg, Germany.
Sharma G; Oncology, Advanced Analytics Experimental Medicine Unit, R&D, GSK, Heidelberg, Germany.
Coleman K; Oncology, Synthetic Lethality Research Unit, R&D, GSK, Heidelberg, Germany.
Grandi P; Oncology, Synthetic Lethality Research Unit, R&D, GSK, Heidelberg, Germany.
Bantscheff M; Cellzome, GSK, R&D, Heidelberg, Germany.
Bergamini G; Cellzome, GSK, R&D, Heidelberg, Germany.

Cancer Res Commun ; 4(9): 2427-2443, 2024 Sep 01.

Article em En | MEDLINE | ID: mdl-39028932

ABSTRACT

ABSTRACT

An in-depth multiomic molecular characterization of PARP inhibitors revealed a distinct poly-pharmacology of niraparib (Zejula) mediated by its interaction with lanosterol synthase (LSS), which is not observed with other PARP inhibitors. Niraparib, in a similar way to the LSS inhibitor Ro-48-8071, induced activation of the 24,25-epoxysterol shunt pathway, which is a regulatory signaling branch of the cholesterol biosynthesis pathway. Interestingly, the combination of an LSS inhibitor with a PARP inhibitor that does not bind to LSS, such as olaparib, had an additive effect on killing cancer cells to levels comparable with niraparib as a single agent. In addition, the combination of PARP inhibitors and statins, inhibitors of 3-hydroxy-3-methylglutaryl-coenzyme A reductase, an enzyme catalyzing the rate-limiting step in the mevalonate pathway, had a synergistic effect on tumor cell killing in cell lines and patient-derived ovarian tumor organoids. These observations suggest that concomitant inhibition of the cholesterol biosynthesis pathway and PARP activity might result in stronger efficacy of these inhibitors against tumor types highly dependent on cholesterol metabolism.

SIGNIFICANCE:

The presented data indicate, to our knowledge, for the first time, the potential benefit of concomitant modulation of cholesterol biosynthesis pathway and PARP inhibition and highlight the need for further investigation to assess its translational relevance.

Assuntos

Colesterol; Sinergismo Farmacológico; Inibidores de Poli(ADP-Ribose) Polimerases; Humanos; Colesterol/biossíntese; Colesterol/metabolismo; Inibidores de Poli(ADP-Ribose) Polimerases/farmacologia; Linhagem Celular Tumoral; Feminino; Neoplasias Ovarianas/tratamento farmacológico; Neoplasias Ovarianas/metabolismo; Neoplasias Ovarianas/patologia; Inibidores de Hidroximetilglutaril-CoA Redutases/farmacologia

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Texto completo: 1 Coleções: 01-internacional Base de dados: MEDLINE Limite: Female / Humans Idioma: En Ano de publicação: 2024 Tipo de documento: Article

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Texto completo: 1 Coleções: 01-internacional Base de dados: MEDLINE Limite: Female / Humans Idioma: En Ano de publicação: 2024 Tipo de documento: Article