Polyclonal breast cancer metastases arise from collective dissemination of keratin 14-expressing tumor cell clusters

Cheung, Kevin; Padmanaban, Veena; Silvestri, Vanesa L.; Schipper, Koen; Cohen, Joshua D.; Fairchild, Amanda N.; Gorin, Michael A.; Verdone, James E.; Pienta, Kenneth J.; Bader, Joel S.; Ewald, Andrew J.

doi:10.1073/pnas.1508541113

Cited by 613 publications

(781 citation statements)

References 54 publications

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“…43). Collective migration may be the rule rather than the exception in metastasis, despite the physical challenges posed by squeezing groups of cells into blood and lymphatic vessels (44). Additional examples of collective migrations include blood vessel sprouting, epithelial closures, and innumerable embryonic morphogenetic movements.…”

Section: Discussionmentioning

confidence: 99%

Modeling and analysis of collective cell migration in an in vivo three-dimensional environment

Cai

Dai

Prasad

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

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A long-standing question in collective cell migration has been what might be the relative advantage of forming a cluster over migrating individually. Does an increase in the size of a collectively migrating group of cells enable them to sample the chemical gradient over a greater distance because the difference between front and rear of a cluster would be greater than for single cells? We combined theoretical modeling with experiments to study collective migration of the border cells in-between nurse cells in the Drosophila egg chamber. We discovered that cluster size is positively correlated with migration speed, up to a particular point above which speed plummets. This may be due to the effect of viscous drag from surrounding nurse cells together with confinement of all of the cells within a stiff extracellular matrix. The model predicts no relationship between cluster size and velocity for cells moving on a flat surface, in contrast to movement within a 3D environment. Our analyses also suggest that the overall chemoattractant profile in the egg chamber is likely to be exponential, with the highest concentration in the oocyte. These findings provide insights into collective chemotaxis by combining theoretical modeling with experimentation.cell migration | theoretical modeling | three-dimensional | chemotaxis

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Section: Discussionmentioning

confidence: 99%

Modeling and analysis of collective cell migration in an in vivo three-dimensional environment

Cai

Dai

Prasad

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

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“…Considering the fate of cancer cells, a malignant cell will meet and surpass various pressures during cancer progression. According to a mouse model, recurrence of a primary tumor demands multiple propensities for each clone, such as invasion, local dissemination, vascular embolus, circulating tumor cells, and micrometastasis 42. Therefore, ITH might provide advantages for metastasis.…”

Section: Clonal Selective Factors For Fostering Ithmentioning

confidence: 99%

“…LOH is an immune escape mechanism that is subject to strong microenvironment later in tumor evolution. Subclonal LOH was observed on chromosome 6, which harbored HLA haplotypes, and the number of putative neoantigens presented to T cells was clearly impaired 42. Therefore, cells with a high number of somatic mutations might not present neoantigens and evade the immune response.…”

Section: Clonal Selective Factors For Fostering Ithmentioning

confidence: 99%

Cancer evolution and heterogeneity

Mimori

Saito

Niida

et al. 2018

Annals of Gastroent Surgery

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Undoubtedly, intratumor heterogeneity (ITH) is one of the causes of the intractability of cancers. Recently, technological innovation in genomics has promoted studies on ITH in solid tumors and on the pattern and level of diversity, which varies among malignancies. We profiled the genome in multiple regions of nine colorectal cancer (CRC) cases. The most impressive finding was that in the late phase, a parental clone branched into numerous subclones. We found that minor mutations were dominant in advanced CRC named neutral evolution; that is, driver gene aberrations were observed with high proportion in the early‐acquired phase, but low in the late‐acquired phase. Then, we validated that neutral evolution could cause ITH in advanced CRC by super‐computational analysis. According to the clinical findings, we explored a branching evolutionary process model in cancer evolution, which assumes that each tumor cell has cellular automaton. According to the model, we verified factors to foster ITH with neutral evolution in advanced CRC. In this review, we introduce recent advances in the field of ITH including the general component of ITH, clonal selective factors that consolidate the evolutionary process, and a representative clinical application of ITH.

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“…Presumably, this gives cancer cells an advantage in efficient seeding, given that they have been shown to have higher metastatic potential than single CTCs [13]. Indeed, polyclonal metastases have been documented in prostate cancer, and in mouse models of breast cancer [13,14]. Although CTC clusters retain cell-cell contacts, studies have shown that they are not fully epithelial, but rather, display a hybrid epithelial--mesenchymal phenotype [13,15].…”

Section: Routes Of Invasionmentioning

confidence: 99%

Circulating tumor cells and their clinical significance

Grzybowska

Fabisiewicz²

2017

Nowotwory. Journal of Oncology

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Metastases to other organs and the formation of secondary tumors are responsible for 90% of cancer-related deaths. However, even in the early stages of cancer, about 30-40% of patients with localized disease may have latent metastasis, which are likely derived from circulating tumor cells (CTCs) involved in disease progression. Therefore, detection and analysis of CTCs can play an important role in the diagnosis and decision-making of adjuvant treatment that aims to prevent metastasis. At present, patients' selection of treatment is based on the statistical risk of recurrence of metastatic disease, without considering whether the tumor cells have spread from the primary tumor. This may lead to unnecessary treatment of non-metastatic disease patients. Therefore, early detection of CTCs in the blood is critically important, and should allow for a more accurate assessment of disease severity. Here, we provide an overview of CTC phenotypes, including plasticity of CTCs, and their clinical significance. NOWOTWORY J Oncol 2017; 67, 4: 243-250

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Polyclonal breast cancer metastases arise from collective dissemination of keratin 14-expressing tumor cell clusters

Cited by 613 publications

References 54 publications

Modeling and analysis of collective cell migration in an in vivo three-dimensional environment

Modeling and analysis of collective cell migration in an in vivo three-dimensional environment

Cancer evolution and heterogeneity

Circulating tumor cells and their clinical significance

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