MRE11 Promotes Tumorigenesis by Facilitating Resistance to Oncogene-Induced Replication Stress

Spehalski, Elizabeth I.; Capper, Kayla; Smith, Cathy; Morgan, Mary J.; Dinkelmann, Maria; Buis, Jeffrey; Sekiguchi, Jo Ann M.; Ferguson, David O.

doi:10.1158/0008-5472.can-17-1355

Cited by 25 publications

(26 citation statements)

References 54 publications

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“…Spehalski et al 46 reported that Mre11 deficiency prevented tumorigenesis in mouse p53 −/− B-cell lymphoma models associated with oncogenic translocations involving Myc genes, indicating that MRE11 (and by extension the MRN complex) cannot be considered a standard tumor suppressor since its activity is required for cancer development. In line with this, we have now demonstrated that MRE11 is also required for an efficient RS control and for the survival of preclinical models of established MYCN-driven human cancer.…”

Section: Discussionmentioning

confidence: 99%

“…It has been recently reported that p53 orchestrates DNA replication restart homeostasis via a transcription- and apoptosis-independent function, by aiding MRE11 recruitment on stalled replication forks to prevent the activity of RAD52/Polθ mutagenic pathways 47 . While it is likely that MRE11 recruitment onto “stressed” forks is strictly connected to its tumor survival functions, data from Spehalski et al 46 imply that p53 is dispensable to this end, since they unveiled MRE11 oncogenic activity in p53 − /− B-cell lymphomas. Further studies will be definitely required to better define the complex relationships between p53 and the MRN complex at the replication forks, in normal and cancer cells.…”

Section: Discussionmentioning

confidence: 99%

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MRE11 inhibition highlights a replication stress-dependent vulnerability of MYCN-driven tumors

et al. 2018

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MRE11 is a component of the MRE11/RAD50/NBS1 (MRN) complex, whose activity is essential to control faithful DNA replication and to prevent accumulation of deleterious DNA double-strand breaks. In humans, hypomorphic mutations in these genes lead to DNA damage response (DDR)-defective and cancer-prone syndromes. Moreover, MRN complex dysfunction dramatically affects the nervous system, where MRE11 is required to restrain MYCN-dependent replication stress, during the rapid expansion of progenitor cells. MYCN activation, often due to genetic amplification, represents the driving oncogenic event for a number of human tumors, conferring bad prognosis and predicting very poor responses even to the most aggressive therapeutic protocols. This is prototypically exemplified by neuroblastoma, where MYCN amplification occurs in about 25% of the cases. Intriguingly, MRE11 is highly expressed and predicts bad prognosis in MYCN-amplified neuroblastoma. Due to the lack of direct means to target MYCN, we explored the possibility to trigger intolerable levels of replication stress-dependent DNA damage, by inhibiting MRE11 in MYCN-amplified preclinical models. Indeed, either MRE11 knockdown or its pharmacological inhibitor mirin induce accumulation of replication stress and DNA damage biomarkers in MYCN-amplified cells. The consequent DDR recruits p53 and promotes a p53-dependent cell death, as indicated by p53 loss- and gain-of-function experiments. Encapsulation of mirin in nanoparticles allowed its use on MYCN-amplified neuroblastoma xenografts in vivo, which resulted in a sharp impairment of tumor growth, associated with DDR activation, p53 accumulation, and cell death. Therefore, we propose that MRE11 inhibition might be an effective strategy to treat MYCN-amplified and p53 wild-type neuroblastoma, and suggest that targeting replication stress with appropriate tools should be further exploited to tackle MYCN-driven tumors.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

MRE11 inhibition highlights a replication stress-dependent vulnerability of MYCN-driven tumors

et al. 2018

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“…Intriguingly, 3 genes, MRE11A, TXN and TOP2A , had already been associated with the pathogenesis of lymphoma and, therefore, targeting their expression might be beneficial for tailored therapy ( Online Supplementary Table S3 ). 24 – 26 …”

Section: Discussionmentioning

confidence: 99%

Gene expression profiling reveals a close relationship between follicular lymphoma grade 3A and 3B, but distinct profiles of follicular lymphoma grade 1 and 2

et al. 2018

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A linear progression model of follicular lymphomas (FL) FL1, FL2 and FL3A has been favored, since FL3A often co-exist with an FL1/2 component. FL3B, in contrast, is thought to be more closely related to diffuse large B-cell lymphoma (DLBCL), and both are often simultaneously present in one tumor (DLBCL/FL3B). To obtain more detailed insights into follicular lymphoma progression, a comprehensive analysis of a well-defined set of FL1/2 (n=22), FL3A (n=16), FL3B (n=6), DLBCL/FL3B (n=9), and germinal center B-cell-type diffuse large B-cell lymphoma (n=45) was undertaken using gene expression profiling, immunohistochemical stainings and genetic analyses by fluorescence in situ hybridization. While immunohistochemical (CD10, IRF4/MUM1, Ki67, BCL2, BCL6) and genetic profiles (translocations of BCL2, BCL6 and MYC) delineate FL1-3A from FL3B and DLBCL/FL3B, significant differences were observed between FL1/2 and FL3A upon gene expression profiling. Interestingly, FL3B turned out to be closely related to FL3A, not categorizing within a separate gene expression cluster, and both FL3A and FL3B showed overlapping profiles in between FL1/2 and diffuse large B-cell lymphoma. Finally, based upon their gene expression pattern, DLBCL/FL3B represent a composite form of FL3B and DLBCL, with the majority of samples more closely resembling the latter. The fact that gene expression profiling clearly separated FL1/2 from both FL3A and FL3B suggests a closer biological relationship between the latter. This notion, however, is in contrast to immunohistochemical and genetic profiles of the different histological FL subtypes that point to a closer relationship between FL1/2 and FL3A, and separates them from FL3B.

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“…Cancer-related functions of PCBP2, TIA-1, HuR/ELAVL1, SERBP1, YTHDC2, YTHDF2 (Mapofthecell database) were described above. All experimentally defined partners of eEF1Bγ picked up by Cytoscape to build molecular networks, are linked to cancer as well [2,[125][126][127][128][129][130][131][132].…”

Section: Resultsmentioning

confidence: 99%

Analysis of eEF1Bγ interactome in the nuclear fraction of A549 human lung adenocarcinoma cells

et al. 2019

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Aim.To study the translation elongation factor eEF1B gamma (eEF1Bγ) in the nucleus of lung carcinoma cells. Methods. The protein partners of eEF1Bγin the nuclear fraction of A549 cells were identified by co-immunoprecipitation (co-IP) and liquid chromatography-tandem mass spectrometry (LC-MS/MS). The protein interaction network for nuclear eEF1Bγ was determined by Cytoscape 3.2.0 program using the MCODE plugin. Additional analysis of the eEF1Bγ partners was conducted by Map of the cell database. Results. 234 proteins interacting with eEF1Bγ in the nuclear fraction of A549 cells were identified. Possible functional networks involving these contacts were analyzed by two bioinformatic approaches. Conclusions. Splicing of pre-mRNA and regulation of mRNA stability are assumed to be the main processes in which nuclear eEF1Bγ can be involved. We hypothesize that a portion of eEF1Bγ leaves the cytoplasmlocalizede EF1B complex during carcinogenesis and enters the nucleus to regulate certain mRNAs by affecting the splicing of their pre-mRNA and/or stability of mRNA. K e y w o r d s: eEF1Bγ, protein-protein interactions, nucleus, A549 cell Structure and Function of Biopolymers

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MRE11 Promotes Tumorigenesis by Facilitating Resistance to Oncogene-Induced Replication Stress

Cited by 25 publications

References 54 publications

MRE11 inhibition highlights a replication stress-dependent vulnerability of MYCN-driven tumors

MRE11 inhibition highlights a replication stress-dependent vulnerability of MYCN-driven tumors

Gene expression profiling reveals a close relationship between follicular lymphoma grade 3A and 3B, but distinct profiles of follicular lymphoma grade 1 and 2

Analysis of eEF1Bγ interactome in the nuclear fraction of A549 human lung adenocarcinoma cells

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MRE11 Promotes Tumorigenesis by Facilitating Resistance to Oncogene-Induced Replication Stress

Cited by 25 publications

References 54 publications

MRE11 inhibition highlights a replication stress-dependent vulnerability of MYCN-driven tumors

MRE11 inhibition highlights a replication stress-dependent vulnerability of MYCN-driven tumors

Gene expression profiling reveals a close relationship between follicular lymphoma grade 3A and 3B, but distinct profiles of follicular lymphoma grade 1 and 2

Analysis of eEF1B&gamma; interactome in the nuclear fraction of A549 human lung adenocarcinoma cells

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Analysis of eEF1Bγ interactome in the nuclear fraction of A549 human lung adenocarcinoma cells