Downregulation of Homologous Recombination DNA Repair Genes by HDAC Inhibition in Prostate Cancer Is Mediated through the E2F1 Transcription Factor

Kachhap, Sushant K.; Rosmus, Nadine; Collis, Spencer J.; Kortenhorst, Madeleine S.Q.; Wissing, Michel D.; Hedayati, Mohammad; Shabbeer, Shabana; Mendonca, Janet; Deangelis, Justin; Marchionni, Luigi; Lin, Jianqing; Höti, Naseruddin; Nortier, J.W.R.; DeWeese, Theodore L.; Hammers, Hans J.; Carducci, Michael A.

doi:10.1371/journal.pone.0011208

Cited by 141 publications

(130 citation statements)

References 54 publications

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“…proteins involved in HR repair of DSBs, BRCA1, and RAD51, were downregulated by both inhibitors. This is consistent with several studies that demonstrated HDAC inhibitors suppress HR gene expression through the E2F1 transcriptional regulator (17), translational repression via miRNAs such as miR182 (34), as well as posttranslational degradation through hyperacetylation of Hsp90 (35). Nonetheless, antineoplastic mechanism of action for HDAC inhibitors has not been well elucidated, and due to their broad range of possible targets, it is likely the SAHA may have affected the function of other proteins involved in DNA damage response.…”

Section: Discussionsupporting

confidence: 89%

“…HDACs regulate gene expression by modifying the chromatin structure as well as regulating the function of nonhistone proteins (15). HDAC inhibition has been reported to downregulate the expression of proteins involved in HR leading to impaired repair of DSBs, i.e., increase "BRCAness" in various types of cancers (16)(17)(18)(19). We hypothesize that HDAC inhibition by SAHA can modulate the expression of proteins involved in DSB repair and abrogate DNA damage response in prostate cancer cells, thereby sensitizing them to PARP inhibition.…”

Section: Introductionmentioning

confidence: 99%

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Synergistic Loss of Prostate Cancer Cell Viability by Coinhibition of HDAC and PARP

Chao

Goodman

2014

Molecular Cancer Research

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Tumors with BRCA germline mutations are defective in repairing DNA double-strand breaks (DSB) through homologous recombination (HR) pathways, making them sensitive to PARP inhibitors (PARPi). However, BRCA germline mutations are rare in prostate cancer limiting the ability to therapeutically target these pathways. This study investigates whether histone deacetylase (HDAC) inhibitors (HDACi), reported to modulate DSB repair pathways in sporadic cancers, can downregulate DSB repair pathways and sensitize prostate cancer cells to PARPi. Prostate cancer cells cotreated with the HDAC inhibitor, suberoylanilide hydroxamic acid (SAHA) and the PARPi, olaparib, demonstrated a synergistic decrease in cell viability compared with single-agent treatment (combination index < 0.9), whereas normal prostatic cells did not. Similarly, clonogenicity was significantly decreased after cotreatment. Flow cytometric cell-cycle analysis and Annexin-V staining revealed significant apoptosis upon treatment with SAHAþolaparib. This coincided with increased DNA damage observed by immunofluorescence microscopy analysis of gH2AX foci, a marker of DSBs. In addition, immunoblot analysis showed a significant and persistent increase in nuclear gH2AX levels. Both SAHA and olaparib downregulated the expression of HR-related proteins, BRCA1 and RAD51, whereas SAHA þ olaparib had an additive effect on RAD51. Silencing RAD51 sensitized prostate cancer cells to SAHA and olaparib alone. Collectively, cotreatment with HDACi and PARPi downregulated HR-related protein expression and concomitantly increased DNA damage, resulting in prostate cancer cell death.Implications: These findings provide a strong rationale for supporting the use of combined HDAC and PARP inhibition in treating advanced prostate cancer.

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Section: Discussionsupporting

confidence: 89%

Section: Introductionmentioning

confidence: 99%

Synergistic Loss of Prostate Cancer Cell Viability by Coinhibition of HDAC and PARP

Chao

Goodman

2014

Molecular Cancer Research

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“…Expression of LAFPs was previously shown to downregulate a number of BER genes (8). HDIs have been shown to downregulate a number of DNA repair enzymes including enzymes implicated in BER and DSB repair (14,40,41). Therefore, we sought to investigate the effect of vorinostat on these same genes in the presence or absence of PLZF-RARa or AML1-ETO.…”

Section: Waf1mentioning

confidence: 99%

Expression of Leukemia-Associated Fusion Proteins Increases Sensitivity to Histone Deacetylase Inhibitor–Induced DNA Damage and Apoptosis

Petruccelli

Pettersson

Rincón

et al. 2013

Molecular Cancer Therapeutics

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Histone deacetylase inhibitors (HDI) show activity in a broad range of hematologic and solid malignancies, yet the percentage of patients in any given malignancy who experience a meaningful clinical response remains small. In this study, we sought to investigate HDI efficacy in acute myeloid leukemia (AML) cells expressing leukemia-associated fusion proteins (LAFP). HDIs have been shown to induce apoptosis, in part, through accumulation of DNA damage and inhibition of DNA repair. LAFPs have been correlated with a DNA repairdeficient phenotype, which may make them more sensitive to HDI-induced DNA damage. We found that expression of the LAFPs PLZF-RARa, PML-RARa, and RUNX1-ETO (AML1-ETO) increased sensitivity to DNA damage and apoptosis induced by the HDI vorinostat. The increase in apoptosis correlated with an enhanced downregulation of the prosurvival protein BCL2. Vorinostat also induced expression of the cell-cycle regulators p19INK4D and p21 WAF1 and triggered a G 2 -M cell cycle arrest to a greater extent in LAFP-expressing cells. The combination of LAFP and vorinostat further led to a greater downregulation of several base excision repair (BER) enzymes. These BER genes represent biomarker candidates for response to HDI-induced DNA damage. Notably, repair of vorinostat-induced DNA double-strand breaks was found to be impaired in PLZFRARa-expressing cells, suggesting a mechanism by which LAFP expression and HDI treatment cooperate to cause an accumulation of damaged DNA. These data support the continued study of HDI-based treatment regimens in LAFP-positive AMLs.

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“…Downregulation of HDA703 by artificial miRNA reduced rice fertility (Hu et al, 2009). In mammals, HDAC inhibition down-regulates homologous recombination DNA repair pathways (Kachhap et al, 2010).…”

Section: The 1158 Pmc-preferential Genes and 127 Genes In Pmcs But Nmentioning

confidence: 99%

Global Gene Profiling of Laser-Captured Pollen Mother Cells Indicates Molecular Pathways and Gene Subfamilies Involved in Rice Meiosis

et al. 2010

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Pollen mother cells (PMCs) represent a critical early stage in plant sexual reproduction in which the stage is set for male gamete formation. Understanding the global molecular genetics of this early meiotic stage has so far been limited to whole stamen or floret transcriptome studies, but since PMCs are a discrete population of cells in developmental synchrony, they provide the potential for precise transcriptome analysis and for enhancing our understanding of the transition to meiosis. As a step toward identifying the premeiotic transcriptome, we performed microarray analysis on a homogenous population of rice (Oryza sativa) PMCs isolated by laser microdissection and compared them with those of tricellular pollen and seedling. Known meiotic genes, including OsSPO11-1, PAIR1, PAIR2, PAIR3, OsDMC1, OsMEL1, OsRAD21-4, OsSDS, and ZEP1, all showed preferential expression in PMCs. The Kyoto Encyclopedia of Genes and Genomes pathways significantly enriched in PMC-preferential genes are DNA replication and repair pathways. Our genome-wide survey showed that, in the buildup to meiosis, PMCs accumulate the molecular machinery for meiosis at the mRNA level. We identified 1,158 PMC-preferential genes and suggested candidate genes and pathways involved in meiotic recombination and meiotic cell cycle control. Regarding the developmental context for meiosis, the DEF-like, AGL2-like, and AGL6-like subclades of MADS box transcription factors are PMC-preferentially expressed, the trans-zeatin type of cytokinin might be preferentially synthesized, and the gibberellin signaling pathway is likely active in PMCs. The ubiquitin-mediated proteolysis pathway is enriched in the 127 genes that are expressed in PMCs but not in tricellular pollen or seedling.

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Downregulation of Homologous Recombination DNA Repair Genes by HDAC Inhibition in Prostate Cancer Is Mediated through the E2F1 Transcription Factor

Cited by 141 publications

References 54 publications

Synergistic Loss of Prostate Cancer Cell Viability by Coinhibition of HDAC and PARP

Synergistic Loss of Prostate Cancer Cell Viability by Coinhibition of HDAC and PARP

Expression of Leukemia-Associated Fusion Proteins Increases Sensitivity to Histone Deacetylase Inhibitor–Induced DNA Damage and Apoptosis

Global Gene Profiling of Laser-Captured Pollen Mother Cells Indicates Molecular Pathways and Gene Subfamilies Involved in Rice Meiosis

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