Innate immune checkpoint inhibitor resistance is associated with melanoma sub-types exhibiting invasive and de-differentiated gene expression signatures

Hossain, Sultana Mehbuba; Gimenez, Grégory; Stockwell, Peter A.; Tsai, Peter; Print, Cristin G.; Ryś, Janusz; Cybulska-Stopa, Bożena; Ratajska, Magdalena; Harazin-Lechowska, Agnieszka; Almomani, Suzan N.; Jackson, Christopher B.; Chatterjee, Aniruddha; Eccles, Michael R.

doi:10.3389/fimmu.2022.955063

Cited by 13 publications

(9 citation statements)

References 75 publications

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“…These cells also have reduced IFNγ signaling activity (Fig 5D). This trajectory was recently reported in experimental data demonstrating that melanoma patients responding to anti-PD-1 therapy exhibit a more proliferative gene expression signature, while the non-responders were enriched in invasive and neural crest-like phenotypes (59). Moreover, vemurafenib-resistant clones of A375 and 451Lu cells display similar molecular attributes (Fig 5E).…”

Section: Combinatorial Control Of Pd-l1 Levels By Ifnγ Signaling and ...supporting

confidence: 80%

Dynamical modelling of proliferative-invasive plasticity and IFNγ signaling in melanoma reveals mechanisms of PD-L1 expression heterogeneity

Subhadarshini

Sahoo

Somarelli

et al. 2023

Preprint

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Phenotypic heterogeneity of melanoma cells contributes to drug tolerance, increased metastasis, and immune evasion in patients with progressive disease. Diverse mechanisms have been individually reported to shape extensive intra- and inter- tumoral phenotypic heterogeneity, such as IFN-gamma signaling and proliferative-invasive transition, but how their crosstalk impacts tumor progression remains largely elusive. Here, using dynamical systems modeling and analysis of publicly available transcriptomic data at both bulk and single-cell levels, we demonstrate that the emergent dynamics of a regulatory network comprising MITF, SOX10, SOX9, JUN and ZEB1 can recapitulate experimental observations about the co-existence of diverse phenotypes (proliferative, neural crest-like, invasive) and reversible cell-state transitions among them. These phenotypes have varied levels of PD-L1, thus driving variability in immunosuppression. We elucidate how this heterogeneity in PD-L1 levels can be aggravated by combinatorial dynamics of these regulators with IFN-gamma signaling. Our model predictions are corroborated by analysis of PD-L1 levels in pre- and post-treatment scenarios both in vitro and in vivo. Our calibrated dynamical model offers a platform to test combinatorial therapies and provide rational avenues for clinical management of metastatic melanoma.

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Section: Combinatorial Control Of Pd-l1 Levels By Ifnγ Signaling and ...supporting

confidence: 80%

Dynamical modelling of proliferative-invasive plasticity and IFNγ signaling in melanoma reveals mechanisms of PD-L1 expression heterogeneity

Subhadarshini

Sahoo

Somarelli

et al. 2023

Preprint

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“…Although immune checkpoint inhibitor-based therapies are somewhat more promising than targeted therapies in achieving complete cures, for most patients, intrinsic or acquired resistance remains a key obstacle. Hossain et al (2022) [ 50 ] showed that non-responding melanomas to anti-PD1 therapy are enriched for genes characteristic of undifferentiated and neural crest-like differentiation states, while in contrast, responding melanomas to anti-PD1 therapy exhibit expression signatures mainly characterized by transitory and melanocytic state gene signatures, supporting the notion that phenotype switching behavior characterizes responding versus non-responding melanomas ( Figure 1 ). The same study also showed an association between phenotype switching, immune cell composition in the TME, and the presence of innate resistance to anti-PD1 therapy.…”

Section: The Rheostat Model Of Mitfmentioning

confidence: 70%

Phenotype Switching and the Melanoma Microenvironment; Impact on Immunotherapy and Drug Resistance

Hossain

Eccles

2023

IJMS

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Melanoma, a highly heterogeneous tumor, is comprised of a functionally diverse spectrum of cell phenotypes and subpopulations, including stromal cells in the tumor microenvironment (TME). Melanoma has been shown to dynamically shift between different transcriptional states or phenotypes. This is referred to as phenotype switching in melanoma, and it involves switching between quiescent and proliferative cell cycle states, and dramatic shifts in invasiveness, as well as changes in signaling pathways in the melanoma cells, and immune cell composition in the TME. Melanoma cell plasticity is associated with altered gene expression in immune cells and cancer-associated fibroblasts, as well as changes in extracellular matrix, which drive the metastatic cascade and therapeutic resistance. Therefore, resistance to therapy in melanoma is not only dependent on genetic evolution, but it has also been suggested to be driven by gene expression changes and adaptive phenotypic cell plasticity. This review discusses recent findings in melanoma phenotype switching, immunotherapy resistance, and the balancing of the homeostatic TME between the different melanoma cell subpopulations. We also discuss future perspectives of the biology of neural crest-like state(s) in melanoma.

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“…To this end, ICI therapies have revolutionized the treatment of melanoma, but innate and acquired resistance remain as clinical challenges. Furthermore, clinical studies have shown that ICI resistance is associated with changes in TME composition (61, 62).…”

Section: Resultsmentioning

confidence: 99%

Tunable PhenoCycler Imaging of the Murine Pre-Clinical Tumour Microenvironments

Abraham,

Goncalves,

McCallum

et al. 2023

Preprint

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The tumour microenvironment (TME) consists of tumour-supportive immune cells, endothelial cells, and fibroblasts. PhenoCycler, a high-plex single cell imaging platform, is used to characterize the complexity of the TME. Here, we used PhenoCycler to spatially resolve the TME of 8 routinely employed pre-clinical models of lymphoma, breast cancer, and melanoma. Our data reveal distinct TMEs in the different cancer models that were imaged, and show that cell-cell contacts differ depending on the tumour type examined. For instance, we found that the immune infiltration in a murine model of melanoma is altered in cellular organization in melanomas that become resistant to αPD-1 therapy, with depletions in a number of cell-cell interactions. Furthermore, we provide detailed pipelines for the conjugation of antibodies that are optimized for PhenoCycler staining of murine FFPE tissues specifically, alongside open-source data analysis procedures. Overall, this is a valuable resource study seamlessly adaptable to any field of research involving murine models.

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Innate immune checkpoint inhibitor resistance is associated with melanoma sub-types exhibiting invasive and de-differentiated gene expression signatures

Cited by 13 publications

References 75 publications

Dynamical modelling of proliferative-invasive plasticity and IFNγ signaling in melanoma reveals mechanisms of PD-L1 expression heterogeneity

Dynamical modelling of proliferative-invasive plasticity and IFNγ signaling in melanoma reveals mechanisms of PD-L1 expression heterogeneity

Phenotype Switching and the Melanoma Microenvironment; Impact on Immunotherapy and Drug Resistance

Tunable PhenoCycler Imaging of the Murine Pre-Clinical Tumour Microenvironments

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