The role of clonal communication and heterogeneity in breast cancer

Martín-Pardillos, Ana; Chiva, Ángeles Valls; Vargas, Gemma Bande; Blanco, Pablo Hurtado; Piñeiro, Roberto; Guijarro, Pedro J.; Hümmer, Stefan; Serrano, Eva Bejar; Rodríguez‐Casanova, Aitor; Díaz‐Lagares, Ángel; Castellví, Josep; Miravet-Verde, Samuel; Serrano, Luís; Lluch‐Senar, María; Sebastián, Víctor; Bribián, Ana; López‐Mascaraque, Laura; López‐López, Rafael; Cajal, Santiago Ramón y

doi:10.1186/s12885-019-5883-y

Cited by 41 publications

(36 citation statements)

References 67 publications

(80 reference statements)

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“…The concept of clonal cooperation is based on a single clone being unable to acquire all the necessary properties to be an invasive tumor, such that various clones must act synergistically and complementarily to acquire the characteristics described by Hanahan and Weinberg [49] and the proposed biochemical changes in 10 or more cellular biochemical pathways. This cell cooperation can be observed in cell clusters in metastatic development: clusters of circulating tumor cells (CTCs) are associated with higher number of metastases than single circulating cells in models of breast cancer, pancreatic cancer, and melanoma [50,51,[102][103][104][105][106]. Moreover, our group made an effort to generate MDA-MB-231 breast cancer cell lines single clones and demonstrated that the clonal cooperation confers aggressiveness and tumor progression [106].…”

Section: Proteomic Heterogeneity: Going Beyond the Genomementioning

confidence: 91%

Clinical implications of intratumor heterogeneity: challenges and opportunities

et al. 2020

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In this review, we highlight the role of intratumoral heterogeneity, focusing on the clinical and biological ramifications this phenomenon poses. Intratumoral heterogeneity arises through complex genetic, epigenetic, and protein modifications that drive phenotypic selection in response to environmental pressures. Functionally, heterogeneity provides tumors with significant adaptability. This ranges from mutual beneficial cooperation between cells, which nurture features such as growth and metastasis, to the narrow escape and survival of clonal cell populations that have adapted to thrive under specific conditions such as hypoxia or chemotherapy. These dynamic intercellular interplays are guided by a Darwinian selection landscape between clonal tumor cell populations and the tumor microenvironment. Understanding the involved drivers and functional consequences of such tumor heterogeneity is challenging but also promises to provide novel insight needed to confront the problem of therapeutic resistance in tumors.

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Section: Proteomic Heterogeneity: Going Beyond the Genomementioning

confidence: 91%

Clinical implications of intratumor heterogeneity: challenges and opportunities

et al. 2020

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“…c The assignment of unique fingerprints to targeted progenitors enabled sibling cells to be identified and their relationships due to the generation of a specific and stable barcode in the cells. d However, the new tools generated to decipher genomic information in an entire organism enable a wealth of important information to be drawn that helps to reconstruct the lineage trees of cells and their sibling connections described in the progression of squamous carcinomas [119], sarcomas [120] and breast cancers [121]. In the CNS, glioblastoma cells engage in clonal communication based on cell-cell contact [122].…”

Section: Insights Into the Lineage Tracing Of Neural Cells From Clonamentioning

confidence: 99%

Deciphering neural heterogeneity through cell lineage tracing

Figueres-Oñate

Sánchez-González

López‐Mascaraque

2020

Cell. Mol. Life Sci.

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Understanding how an adult brain reaches an appropriate size and cell composition from a pool of progenitors that proliferates and differentiates is a key question in Developmental Neurobiology. Not only the control of final size but also, the proper arrangement of cells of different embryonic origins is fundamental in this process. Each neural progenitor has to produce a precise number of sibling cells that establish clones, and all these clones will come together to form the functional adult nervous system. Lineage cell tracing is a complex and challenging process that aims to reconstruct the offspring that arise from a single progenitor cell. This tracing can be achieved through strategies based on genetically modified organisms, using either genetic tracers, transfected viral vectors or DNA constructs, and even single-cell sequencing. Combining different reporter proteins and the use of transgenic mice revolutionized clonal analysis more than a decade ago and now, the availability of novel genome editing tools and single-cell sequencing techniques has vastly improved the capacity of lineage tracing to decipher progenitor potential. This review brings together the strategies used to study cell lineages in the brain and the role they have played in our understanding of the functional clonal relationships among neural cells. In addition, future perspectives regarding the study of cell heterogeneity and the ontogeny of different cell lineages will also be addressed.

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“…For SVs, no overlap of somatic SVs and genes were found between amplified bulk cancer and spike-in samples. One of the possible explanations for the discrepancy in the overlap of somatic alterations may be due to cellular heterogeneity within the same type of cancer cells [30,31]. Despite the importance of cellular heterogeneity, another reason may be due to the high variability of cell size.…”

Section: Optimization Of Wes In Spiked and Unspiked Breast Cancer Cellsmentioning

confidence: 99%

A Pilot Study for the Feasibility of Exome-Sequencing in Circulating Tumor Cells Versus Single Metastatic Biopsies in Breast Cancer

Kaur

Campo

Porras

et al. 2020

IJMS

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The comparison of the landscape of somatic alterations in circulating tumor cells (CTCs) versus metastases is challenging. Here, we comprehensively characterized the somatic landscape in bulk (amplified and non-amplified), spike-in breast cancer cells, CTCs, and metastases from breast cancer patients using whole-exome sequencing (WES). We determined the level of genomic concordance for somatic nucleotide variants (SNVs), copy number alterations (CNAs), and structural variants (SVs). The variant allele fractions (VAFs) of somatic variants were remarkably similar between amplified and non-amplified cell line samples as technical replicates. In clinical samples, a significant fraction of somatic variants had low VAFs in CTCs compared to metastases. The most frequently recurrent gene mutations in clinical samples were associated with an elevated C > T mutational signature. We found complex rearrangement patterns including intra- and inter-chromosomal rearrangements, singleton, and recurrent gene fusions, and tandem duplications. We observed high molecular discordance for somatic alterations between paired samples consistent with marked heterogeneity of the somatic landscape. The most prevalent copy number calls were focal deletion events in CTCs and metastases. Our results demonstrate the feasibility of an integrated workflow for the identification of a complete repertoire of somatic alterations and highlight the intrapatient genomic differences that occur between CTCs and metastases.

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The role of clonal communication and heterogeneity in breast cancer

Cited by 41 publications

References 67 publications

Clinical implications of intratumor heterogeneity: challenges and opportunities

Clinical implications of intratumor heterogeneity: challenges and opportunities

Deciphering neural heterogeneity through cell lineage tracing

A Pilot Study for the Feasibility of Exome-Sequencing in Circulating Tumor Cells Versus Single Metastatic Biopsies in Breast Cancer

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