Literature DB >> 19117011

Estrogen receptor beta-mediated nuclear interaction between IRS-1 and Rad51 inhibits homologous recombination directed DNA repair in medulloblastoma.

Katarzyna Urbanska1, Paola Pannizzo, Adam Lassak, Elisa Gualco, Eva Surmacz, Sidney Croul, Luis Del Valle, Kamel Khalili, Krzysztof Reiss.   

Abstract

In medulloblastomas, which are highly malignant cerebellar tumors of the childhood genotoxic treatments such as cisplatin or gamma-irradiation are frequently associated with DNA damage, which often associates with unfaithful DNA repair, selection of new adaptations and possibly tumor recurrences. Therefore, better understanding of molecular mechanisms which control DNA repair fidelity upon DNA damage is a critical task. Here we demonstrate for the first time that estrogen receptor beta (ERbeta) can contribute to the development of genomic instability in medulloblastomas. Specifically, ERbeta was found highly expressed and active in mouse and human medulloblastoma cell lines. Nuclear ERbeta was also present in human medulloblastoma clinical samples. Expression of ERbeta coincided with nuclear translocation of insulin receptor substrate 1 (IRS-1), which was previously reported to interfere with the faithful component of DNA repair when translocated to the nucleus. We demonstrated that ERbeta and IRS-1 bind each other, and the interaction involves C-terminal domain of IRS-1 (aa 931-1233). Following cisplatin-induced DNA damage, nuclear IRS-1 localized at the sites of damaged DNA, and interacted with Rad51--an enzymatic component of homologous recombination directed DNA repair (HRR). In medulloblastoma cells, engineered to express HRR-DNA reporter plasmid, ER antagonist, ICI 182,780, or IRS mutant (931-1233) significantly increased DNA repair fidelity. These data strongly suggest that both molecular and pharmacological interventions are capable of preventing ERbeta-mediated IRS-1 nuclear translocation, which in turn improves DNA repair fidelity and possibly counteracts accumulation of malignant mutations in actively growing medulloblastomas.

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Year:  2009        PMID: 19117011      PMCID: PMC2679153          DOI: 10.1002/jcp.21683

Source DB:  PubMed          Journal:  J Cell Physiol        ISSN: 0021-9541            Impact factor:   6.384


  48 in total

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2.  NHEJ deficiency and disease.

Authors:  A J Pierce; M Jasin
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Review 3.  Genome maintenance mechanisms for preventing cancer.

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4.  Identification of a novel p53 mutation in JCV-induced mouse medulloblastoma.

Authors:  B Krynska; L Del Valle; J Gordon; J Otte; S Croul; K Khalili
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5.  Activation of the IGF-IR system contributes to malignant growth of human and mouse medulloblastomas.

Authors:  J Y Wang; L Del Valle; J Gordon; M Rubini; G Romano; S Croul; F Peruzzi; K Khalili; K Reiss
Journal:  Oncogene       Date:  2001-06-28       Impact factor: 9.867

6.  Estrogen receptor beta immunoreactivity in differentiating cells of the developing rat cerebellum.

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Journal:  J Comp Neurol       Date:  2001-02-12       Impact factor: 3.215

7.  Mechanisms of regulation of cell adhesion and motility by insulin receptor substrate-1 in prostate cancer cells.

Authors:  K Reiss; J Y Wang; G Romano; X Tu; F Peruzzi; R Baserga
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8.  Insulin receptor substrate 1 translocation to the nucleus by the human JC virus T-antigen.

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9.  Insulin-like growth factor I induces MDM2-dependent degradation of p53 via the p38 MAPK pathway in response to DNA damage.

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10.  Polymorphisms of human estrogen receptor (ER) gene alpha and beta in prostate cancer PC-EW and PC-OR cell lines.

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3.  Differential expression of type 2 3α/type 5 17β-hydroxysteroid dehydrogenase (AKR1C3) in tumors of the central nervous system.

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4.  Insulin receptor substrate 1 expression enhances the sensitivity of 32D cells to chemotherapy-induced cell death.

Authors:  Holly A Porter; Gregory B Carey; Achsah D Keegan
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Review 5.  Linking DNA Damage and Hormone Signaling Pathways in Cancer.

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6.  Molecular and Structural Traits of Insulin Receptor Substrate 1/LC3 Nuclear Structures and Their Role in Autophagy Control and Tumor Cell Survival.

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7.  Inhibition of ERβ induces resistance to cisplatin by enhancing Rad51-mediated DNA repair in human medulloblastoma cell lines.

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Review 8.  Regulators of homologous recombination repair as novel targets for cancer treatment.

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10.  Gender effect in experimental models of human medulloblastoma: does the estrogen receptor β signaling play a role?

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