Evolution of Metastases in Space and Time under Immune Selection

Angelova, Mihaela; Mlecnik, Bernhard; Vasaturo, Angela; Bindea, Gabriela; Fredriksen, Tessa; Lafontaine, Lucie; Buttard, Bénédicte; Morgand, Erwan; Bruni, Daniela; Jouret‐Mourin, Anne; Hubert, Catherine; Kartheuser, Alex; Humblet, Yves; Ceccarelli, Michele; Syed, Najeeb; Marincola, Francesco M.; Bedognetti, Davide; Eynde, Marc Van den; Galon, Jérôme

doi:10.1016/j.cell.2018.09.018

Cited by 351 publications

(317 citation statements)

References 37 publications

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“…Infiltrating and invasive phenotypes are often observed among high-ploidy cells. Converging evidence from different cancer types, including colorectal-, breast-, lung-and brain cancers, suggests a strong enrichment of high ploidy cells among metastatic lesions as compared to the primary tumor [14,15]. Even in normal development: trophoblast giant cells -the first cell type to terminally differentiate during embryogenesis -are responsible for invading the placenta and these cells often have hundreds of copies of the genome [16].…”

Section: Introductionmentioning

confidence: 99%

Invasion of homogeneous and polyploid populations in nutrient-limiting environments

Kimmel

Dane

Heiser

et al. 2020

Preprint

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Breast cancer progresses in a multistep process from primary tumor growth and stroma invasion to metastasis. Progression is accompanied by a switch to an invasive cell phenotype. Nutrient-limiting environments exhibit chemotaxis with aggressive morphologies characteristic of invasion. The mTOR pathway senses essential nutrients, informing the cell to respond with either increased chemotaxis and nutrient uptake or cell cycle progression. Randomized clinical trials have shown that mTOR inhibitors (mTOR-I) improve the outcome of metastatic breast cancer patients. However, there are considerable differences between and within tumors that impact the effectiveness of mTOR-I, including differences in access to nutrients. It is unknown how co-existing cells differ in their response to nutrient limitations and how this impacts invasion of the metapopulation as a whole. We integrate modeling with microenvironmental perturbations data to investigate invasion in nutrient-limiting environments inhabited by one or two cancer cell subpopulations. Hereby subpopulations are defined by their energy efficiency and chemotactic ability. We calculate the invasion-distance traveled by a homogeneous population. For heterogeneous populations, our results suggest that an imbalance between nutrient efficacy and chemotactic superiority accelerates invasion. Such imbalance will segregate the two populations spatially and only one type will dominate at the invasion front. Only if these two phenotypes are balanced do the two populations compete for the same space, which decelerates invasion. We investigate ploidy as a candidate biomarker of this phenotypic heterogeneity to discern circumstances when inhibiting chemotaxis amplifies innternal competition and decelerates tumor progression, from circumstances that render clinical consequences of chemotactic inhibition unfavorable. Significance: A better understanding of the nature of the double-edged sword of high ploidy is a prerequisite to personalize combinationtherapies with cytotoxic drugs and inhibitors of signal transduction pathways such as MTOR-Is.

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Section: Introductionmentioning

confidence: 99%

Invasion of homogeneous and polyploid populations in nutrient-limiting environments

Kimmel

Dane

Heiser

et al. 2020

Preprint

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“…The composition of the various cell types making up the microenvironment can significantly affect the way in which the immune system activates cancer rejection mechanisms (Bedognetti et al, 2016; Joyce and Fearon, 2015; Zhang et al, 2019) and influences the response to immune therapies (Ceccarelli et al, 2016; Cristescu et al, 2018). Therefore, the elucidation of the tumor-host interaction mechanisms plays a crucial role in the understanding of the tumor growth and evolution (Angelova et al, 2018; Bedognetti et al, 2019) and for the identification immuno-oncology therapeutic targets (Hoos, 2016). Immune checkpoint inhibitor (ICI) therapies are aimed to targeting the specific cell-cell interaction between PD1 and PD-L1 or CTLA4 and B7-1/B7-2 (Pardoll, 2012).…”

Section: Introductionmentioning

confidence: 99%

A MAP of tumor-host interactions in glioma at single cell resolution

Caruso

Garofano

D’Angelo

et al. 2019

Preprint

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Single-cell RNA sequencing is the reference technique to characterize the heterogeneity of tumor microenvironment and can be efficiently used to discover cross-talk mechanisms between immune cells and cancer cells. We present a novel method, single cell Tumor-Host Interaction tool (), to identify significantly activated ligand-receptor interactions across clusters of cells from single-cell RNA sequencing data. We apply our approach to uncover the ligand-receptor interactions in glioma using six publicly available human glioma datasets encompassing 71 patients. We provide a comprehensive map of the signalling mechanisms between malignant cells and non-malignant cells in glioma uncovering potential novel therapeutic targets.

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“…Given that soft sweeps from recurrent mutation happen (which means that the rate of input of new mutations in the population must be fairly high) and that simultaneous sweeps happen (suggesting that mutations can stay linked), it appears likely that clonal interference also happens in adapting HIV populations. We show Muller plots (Muller, 1932) or evolvograms (Angelova et al, 2018) for several examples, where we think that clonal interference is occurring.…”

mentioning

confidence: 96%

Drug resistance evolution in HIV in the late 1990s: hard sweeps, soft sweeps, clonal interference and the accumulation of drug resistance mutations

Williams¹,

Pennings²

2019

Preprint

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The goal of this paper is to provide examples of evolutionary dynamics of HIV within patients who are treated with antiretrovirals. We hope that the figures in this paper will be used in evolution and population genetics classes. We show a wide variety of patterns, specifically: soft sweeps, hard sweeps, softening sweeps and hardening sweeps, simultaneous sweeps, accumulation of mutations and clonal interference.

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Evolution of Metastases in Space and Time under Immune Selection

Cited by 351 publications

References 37 publications

Invasion of homogeneous and polyploid populations in nutrient-limiting environments

Invasion of homogeneous and polyploid populations in nutrient-limiting environments

A MAP of tumor-host interactions in glioma at single cell resolution

Drug resistance evolution in HIV in the late 1990s: hard sweeps, soft sweeps, clonal interference and the accumulation of drug resistance mutations

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