Distinct responses of newly identified monocyte subsets to advanced gastrointestinal cancer and COVID-19

Rigamonti, Alessandra; Castagna, Alessandra; Viatore, Marika; Colombo, Federico; Terzoli, Sara; Peano, Clelia; Marchesi, Federica; Locati, Massimo

doi:10.3389/fimmu.2022.967737

Cited by 9 publications

(15 citation statements)

References 71 publications

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“…While some clusters occupied definite positions on the UMAP, the Mϕ populations expressing high levels of lineage markers (Mϕ, CD68 hi Mϕ, CD14 hi /CD16 hi Mϕ and CD163 hi Mϕ) were closer and overlapping, suggesting that they might represent the same population at different maturation states ( Fig. 3F ), confirming previous evidence obtained by trajectory analyses of transcriptomic data ( 36, 37 ). By UMAP visualization of the cluster arrangement with respect to their tissue location ( Fig.…”

Section: Resultssupporting

confidence: 86%

“…The regional specialization of macrophage subtypes in tumor tissues is an important feature that can control their functional profile and correlate with survival benefit, as shown in melanoma ( 47 ) and in human colo-rectal liver metastasis ( 37 ). In line with previous studies, a considerable fraction of the Mϕ granularity was accounted by very similar populations (occupying the same position on a UMAP representation), possibly representing the same cell in different maturation states ( 36, 37 ). Another interesting aspect emerging from the integrative analysis was that tumor cells were significantly more frequent in poorly fibrotic tumors, while the presence of fibrosis did not correlate with the K score (i.e., the distribution pattern of tumor cells).…”

Section: Discussionsupporting

confidence: 90%

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Integrating AI-Powered Digital Pathology and Imaging Mass Cytometry Identifies Key Classifiers of Tumor Cells, Stroma, and Immune Cells in Non–Small Cell Lung Cancer

Rigamonti,

Viatore,

Polidori

et al. 2024

Cancer Research

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Artificial intelligence (AI)-powered approaches are becoming increasingly used as histopathological tools to extract sub-visual features and improve diagnostic workflows. On the other hand, hi-plex approaches are widely adopted to analyze the immune ecosystem in tumor specimens. Here, we aimed at combining AI-aided histopathology and imaging mass cytometry (IMC) to analyze the ecosystem of non-small cell lung cancer (NSCLC). An AI-based approach was used on H&E sections from 158 NSCLC specimens to accurately identify tumor cells, both adenocarcinoma and squamous carcinoma cells, and to generate a classifier of tumor cell spatial clustering. Consecutive tissue sections were stained with metal-labeled antibodies and processed through the IMC workflow, allowing quantitative detection of 24 markers related to tumor cells, tissue architecture, CD45+ myeloid and lymphoid cells, and immune activation. IMC identified 11 macrophage clusters that mainly localized in the stroma, except for S100A8+ cells, which infiltrated tumor nests. T cells were preferentially localized in peritumor areas or in tumor nests, the latter being associated with better prognosis, and they were more abundant in highly clustered tumors. Integrated tumor and immune classifiers were validated as prognostic on whole slides. In conclusion, integration of AI-powered H&E and multiparametric IMC allows investigation of spatial patterns and reveals tissue relevant features with clinical relevance.

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Section: Resultssupporting

confidence: 86%

Section: Discussionsupporting

confidence: 90%

Integrating AI-Powered Digital Pathology and Imaging Mass Cytometry Identifies Key Classifiers of Tumor Cells, Stroma, and Immune Cells in Non–Small Cell Lung Cancer

Rigamonti,

Viatore,

Polidori

et al. 2024

Cancer Research

Self Cite

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“…Totally, we sequenced 20890 cells, which decreased to 19085 after quality control. Dimensionality reduction by UMAP ( 26 ) clearly demonstrated a net segregation of the NC/slan + /slan − - and CL-monocyte groups, with INT-monocytes placing exactly in between them ( Figures 4A, B ), as expected ( 8 , 12 , 27 , 28 ). Moreover, in line with the bulk transcriptomic ( Figure 2A ) and proteomic ( Figure 3A ) results, the same UMAP confirmed that slan − /NC-monocytes stand closer to CL-and INT-monocytes than to slan + /NC-monocytes ( Figures 4A, B ).…”

Section: Resultssupporting

confidence: 69%

The slan antigen identifies the prototypical non-classical CD16+-monocytes in human blood

Tamassia,

Bianchetto-Aguilera,

Gasperini

et al. 2023

Front. Immunol.

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IntroductionPeripheral monocytes in humans are conventionally divided into classical (CL, CD14++CD16−), intermediate (INT, CD14++CD16+) and non-classical (NC, CD14dim/−CD16++) cells, based on their expression levels of CD14 and CD16. A major fraction of the NC-monocytes has been shown to express the 6-sulfo LacNAc (slan) antigen, but whether these slan+/NC-monocytes represent the prototypical non-classical monocytes or whether they are simply a sub-fraction with identical features as the remainder of NC monocytes is still unclear.MethodsWe analyzed transcriptome (by bulk and single cell RNA-seq), proteome, cell surface markers and production of discrete cytokines by peripheral slan+/NC- and slan−/NC-monocytes, in comparison to total NC-, CL- and INT- monocytes.ResultsBy bulk RNA-seq and proteomic analysis, we found that slan+/NC-monocytes express higher levels of genes and proteins specific of NC-monocytes than slan−/NC-monocytes do. Unsupervised clustering of scRNA-seq data generated one cluster of NC- and one of INT-monocytes, where all slan+/NC-monocytes were allocated to the NC-monocyte cluster, while slan−/NC-monocytes were found, in part (13.4%), within the INT-monocyte cluster. In addition, total NC- and slan−/NC-monocytes, but not slan+/NC-monocytes, were found by both bulk RNA-seq and scRNA-seq to contain a small percentage of natural killer cells.ConclusionIn addition to comparatively characterize total NC-, slan−/NC- and slan+/NC-monocyte transcriptomes and proteomes, our data prove that slan+/NC-, but not slan−/NC-, monocytes are more representative of prototypical NC-monocytes.

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“…Ym1 + Mos were deemed crucial for inflammation resolution, simultaneously producing higher levels of anti-inflammatory IL-10 and lower pro-inflammatory cytokines (IL-6, IL-12) than Ym1 − monocytes. NeuMos were also discovered to be present in the steady-state BM and blood [ 30 , 31 ], perhaps suggesting the presence of a background signal that maintains a basal level differentiation of GMPs into NeuMos in the BM. On the other hand, a deviation of GMP differentiation into cMoPs into a unique progenitor state could also occur in particular diseases such as bleomycin-induced fibrosis, whereby cells termed segregated-nucleus-containing atypical monocytes (SatMs) were discovered [ 32 ].…”

Section: Monocyte Development: Different Fates Before Birthmentioning

confidence: 99%

“…However, many questions still remain: How do these circulating phenotypes differ from monocytes that arise through the priming of BM progenitors such as NeuMos and DCMos? In a recent study, Rigamonti et al have attempted to address this question by demonstrating nine distinct functional populations of human circulating monocytes in healthy donors [ 31 ]. Specifically, there were five populations related either to inflammatory, neutrophil-like, interferon-related, or platelet-related pathways among the classical subset of monocytes.…”

Section: Monocyte Reservoirs In the Periphery: Strategically Position...mentioning

confidence: 99%

Behind the monocyte’s mystique: uncovering their developmental trajectories and fates

Teh

Chooi

Chong

2023

Discovery Immunology

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Monocytes are circulating myeloid cells that are derived from dedicated progenitors in the bone marrow. Originally thought of as mere precursors for the replacement of tissue macrophages, it is increasingly clear that monocytes execute distinct effector functions and may give rise to monocyte-derived cells with unique properties from tissue resident macrophages. Recently, the advent of novel experimental approaches such as single cell analysis and fate mapping tools has uncovered an astonishing display of monocyte plasticity and heterogeneity, which we believe has emerged as a key theme in the field of monocyte biology in the last decade. Monocyte heterogeneity is now recognized to develop as early as the progenitor stage through specific imprinting mechanisms, giving rise to specialized effector cells in the tissue. At the same time, monocytes must overcome their susceptibility towards cellular death to persist as monocyte-derived cells in the tissues. Environmental signals that preserve their heterogenic phenotypes and govern their eventual fates remain incompletely understood. In this review, we will summarize recent advances on the developmental trajectory of monocytes and discuss emerging concepts that contributes to the burgeoning field of monocyte plasticity and heterogeneity.

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Distinct responses of newly identified monocyte subsets to advanced gastrointestinal cancer and COVID-19

Cited by 9 publications

References 71 publications

Integrating AI-Powered Digital Pathology and Imaging Mass Cytometry Identifies Key Classifiers of Tumor Cells, Stroma, and Immune Cells in Non–Small Cell Lung Cancer

Integrating AI-Powered Digital Pathology and Imaging Mass Cytometry Identifies Key Classifiers of Tumor Cells, Stroma, and Immune Cells in Non–Small Cell Lung Cancer

The slan antigen identifies the prototypical non-classical CD16+-monocytes in human blood

Behind the monocyte’s mystique: uncovering their developmental trajectories and fates

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