Supporting metadata for Therapeutic targeting of BRCA1 and TP53 Mutant Breast Cancer Through Mutant p53 Reactivation
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https://springernature.figshare.com/articles/dataset/Supporting_metadata_for_Therapeutic_targeting_of_BRCA1_and_TP53_Mutant_Breast_Cancer_Through_Mutant_p53_Reactivation/7688537/1
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This data record describes the statistical data supporting the figures in the related publication "Therapeutic targeting of BRCA1 and TP53 Mutant Breast Cancer Through Mutant p53 Reactivation".<br>Triple negative breast cancer (TNBC) is an aggressive subset of breast cancers, for which a significant portion of patients have have germline or somatic mutations in BRCA1, or epigenetic silencing of BRCA1, which renders them deficient in DNA repair. TNBC is typically treated with chemotherapy.<br>The related study hypothesizes that restoring wild type p53 function in BRCA1 deficient breast cancer would be therapeutic. It is suggested that inactivation of TP53 is a requirement for tumor progression in the setting of BRCA1 deficiency.<br>Zinc metallochaperones (ZMCs) are a new class of anti-cancer drugs that reactivate zinc deficient mutant p53 by restoring zinc binding. An aim of the study is preclinical validation of a novel therapeutic approach for BRCA1 deficient breast cancer through reactivation of mutant p53. This includes a novel formulation of ZMC1 and test of its efficacy.<br><b>Study design summary</b><br>Study includes use of ZMC1 in human breast cancer lines expressing zinc-deficient p53 and use of murine breast cancer models with BRCA1 deficiency to explore survival rates in mice bearing tumors harboring the zinc-deficient Trp53<sup>R172H</sup> allele but not the Trp53<sup>-/-</sup>.<br>A cell survival assay was performed in the context of ZMC1 treatment in human cell lines and mouse models.<br>Western blot raw data are available within the supplementary information of the related publication. Tumour volume analyses were performed in R statistical package.<br>All animal experiments were conducted in accordance with the protocols approved by the Institutional Animal Care and Use Committee (IACUC) of Rutgers Robert Wood Johnson Medical School.<br><b>Data files and formats</b><br><br>The data supporting the figures of the related manuscript consist of 16 Excel files, 16 Graphpad prism files, 2 jpeg image files and Photoshop image file. All files are accessible through openly available office or image viewer software.<br>These include cell survival rates in human cell lines and in genetically engineered mouse models treated with ZMC1. Tumor volumes and ZMC sensitivity data are also included.<br>See the file <b>data_summary_form.xlsx </b>for a more detailed breakdown of the data files supporting each figure.<br><b>Data access and terms of use:</b><br><br>Data files are stored in institutional file storage and available on request from Rutgers Cancer Institute of New Jersey:<br>Darren R. Carpizo, Rutgers Cancer Institute of New Jersey, 195 Little Albany Street, New Brunswick, NJ 08901. Phone: 732-235-7701. Fax: 732-235-8098. Email: carpizdr@cinj.rutgers.edu
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figshare
创建时间:
2019-04-17



