4.7 Article

Breast cancer metastasis: Is it a matter of OMICS and proper ex-vivo models?

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ELSEVIER
DOI: 10.1016/j.csbj.2022.07.044

关键词

Metastatic breast cancer; Organoids; PDTO; Genomic; Proteomic; multi-OMICS

资金

  1. Fondazione AIRC under 5 per mille grant [22759]
  2. IRCCS Regina Elena National Cancer Institute

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Genomics has provided insights into breast cancer, but the study of metastatic breast cancer lags behind. Integrated multi-OMICS characterization and the use of clinically relevant patient-derived tumor-organoids may enhance our understanding and treatment of metastatic breast cancer.
Genomics has greatly increased the understanding of the study of breast cancer (BC) and has shaped the concept of intra-tumor heterogeneity, currently recognized as a propelling force for cancer progression. In this context, knowledge and understanding of metastatic breast cancer (mBC) has somehow lagged behind that of primary breast cancer. This may be explained by the relative scarcity of matched mBC samples, however it is possible that the mutation spectrum obtained from primary BC does not capture the full complexity of the metastatic disease. Here, we provide a few examples supporting this possibility, from public databases. We evoke the need to perform an integrated multi-OMICS characterization of mBC, to obtain a broad understanding of this complex disease, whose evolution cannot be explained solely by genomics. Pertinent to this, we suggest that rather an infrequent use of Patient-Derived Tumor-Organoids (PDTOs) may be influenced by assuming that the metastatic conditions of PDTOs growth (mPDTOs) should be similar to those of the tissue of origin. We challenge this view by suggesting that the use of target-organ inspired growth conditions for mPDTOs, may better fit the emerging knowledge of metastatic disease. Thus, the integrated use of multi-OMICS and of clinically relevant mPDTOs may allow a further understanding of such disease and foster therapeutically relevant advances. We believe that our points may be valid for other solid cancers. (c) 2022 The Author(s). Published by Elsevier B.V. on behalf of Research Network of Computational and Structural Biotechnology.

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