Single cell spatial analysis reveals the topology of immunomodulatory purinergic signaling in glioblastoma

Coy, Shannon; Wang, Shu; Stopka, Sylwia A.; Lin, Jia-Ren; Yapp, Clarence; Ritch, Cecily C.; Salhi, Lisa; Baker, Gregory J.; Rashid, Rumana; Baquer, Gerard; Regan, Michael S.; Khadka, Prasidda; Cole, Kristina A.; Wen, Patrick Y.; Bandopadhayay, Pratiti; Santi, Mariarita; Raedt, Thomas De; Ligon, Keith L.; Agar, Nathalie Y.R.; Sorger, Peter K.; Touat, Mehdi; Santagata, Sandro

doi:10.1038/s41467-022-32430-w

Cited by 34 publications

(22 citation statements)

References 98 publications

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“…Remodeling in response to hypoxic or low glucose environments occurs through various mechanisms including epigenetic modification ( 3 , 126 , 127 ), HIF-1α signaling ( 125 , 128 , 129 ), and altered expression of metabolic enzymes and transporters ( 49 , 130 ). In general, metabolic profiles in GBM cells are spatially distinct and attributed to TME interactions and restricted nutrient availability ( 122 , 125 , 131 , 132 ) with different GSC subsets having distinct metabolic preferences and dependencies ( 121 , 133 , 134 ).…”

Section: Contribution Of Gscs To the Immunosuppressive Microenvironme...mentioning

confidence: 99%

“…Furthermore, Coy et al. identified increased levels of extracellular immune-suppressive adenosine in GBM attributed to high expression of CD73, which functions alongside CD39 to metabolize ATP into adenosine, in hypoxia-responsive GBM cells ( 131 ). Collectively, these findings demonstrate a connection between TME-driven metabolic reprogramming and GSC-mediated immune suppression, and prompt further investigation into therapeutically relevant metabolic vulnerabilities in these immune-suppressive cells.…”

Section: Contribution Of Gscs To the Immunosuppressive Microenvironme...mentioning

confidence: 99%

“…While many of the above spatial technologies have yet to be applied in the context of GBM, RNAScope and MSI methods have been utilized with the former identifying expression-based prognostic markers from GBM tissues ( 214 , 215 ). On the other hand, MSI methods have investigated GBM heterogeneity based on metabolic and proteomic profiles and drug distribution in tumors ( 131 , 216 – 220 ).…”

Section: Analytical Tools To Explore Gbm Heterogeneitymentioning

confidence: 99%

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Exploring glioblastoma stem cell heterogeneity: Immune microenvironment modulation and therapeutic opportunities

2022

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Despite its growing use in cancer treatment, immunotherapy has been virtually ineffective in clinical trials for gliomas. The inherently cold tumor immune microenvironment (TIME) in gliomas, characterized by a high ratio of pro-tumor to anti-tumor immune cell infiltrates, acts as a seemingly insurmountable barrier to immunotherapy. Glioma stem cells (GSCs) within these tumors are key contributors to this cold TIME, often functioning indirectly through activation and recruitment of pro-tumor immune cell types. Furthermore, drivers of GSC plasticity and heterogeneity (e.g., reprogramming transcription factors, epigenetic modifications) are associated with induction of immunosuppressive cell states. Recent studies have identified GSC-intrinsic mechanisms, including functional mimicry of immune suppressive cell types, as key determinants of anti-tumor immune escape. In this review, we cover recent advancements in our understanding of GSC-intrinsic mechanisms that modulate GSC-TIME interactions and discuss cutting-edge techniques and bioinformatics platforms available to study immune modulation at high cellular resolution with exploration of both malignant (i.e., GSC) and non-malignant (i.e., immune) cell fractions. Finally, we provide insight into the therapeutic opportunities for targeting immunomodulatory GSC-intrinsic mechanisms to potentiate immunotherapy response in gliomas.

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Section: Contribution Of Gscs To the Immunosuppressive Microenvironme...mentioning

confidence: 99%

Section: Contribution Of Gscs To the Immunosuppressive Microenvironme...mentioning

confidence: 99%

Section: Analytical Tools To Explore Gbm Heterogeneitymentioning

confidence: 99%

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Exploring glioblastoma stem cell heterogeneity: Immune microenvironment modulation and therapeutic opportunities

2022

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“…To deepen our understanding of SLC11A1’s function in glioma’s tumor immune microenvironment (TIME), we utilized glioma single-cell data derived from the GEO dataset (GSE131928) ( 9 ), unsupervised analyses of this data identified 7 cell states representing the stromal, immune, and neoplastic cells commonly observed in glioma. According to the marker genes in the study of Neftel et al, neoplastic cells were split across four pan-glioma cell states, AC-like (EGFR), MES-like (CHI3L1), NPC-like (ELAVL4) and OPC-like (PDGFRA) ( 9 ), that observed across many glioma single-cell studies ( 36 , 37 ). We also identified macrophages/monocytes by C1QB, C1QC and FCER1G ( 38 ), CD8 Tex cells by CD3D and IFITM1 ( 39 ), and oligodendrocyte by ERMN and KLK6 ( 40 ).…”

Section: Resultsmentioning

confidence: 99%

SLC11A1 as a stratification indicator for immunotherapy or chemotherapy in patients with glioma

Zhang

Fang

et al. 2022

Front. Immunol.

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BackgroundGlioma is a fatal tumor originating from the brain, which accounts for most intracranial malignancies. Currently, Immunotherapy has turned into a novel and promising treatment in glioma patients. however, there are still few effective biomarkers to mirror the reaction to immunotherapy in patients with glioma. Therefore, we intended to elucidate the evaluable efficacy of SLC11A1 in glioma patients.MethodsIn this study, samples from Shanghai General Hospital and data from TCGA, GEO, CGGA datasets were used to investigate and validate the relationship between SLC11A1 and the progression of glioma. We evaluated the predictive value of SLC11A1 on the prognosis of glioma with cox regression analysis. Then the relationship between immune infiltration and SLC11A1 was also analyzed. Ultimately, we performed the prediction on the immunotherapeutic response and therapeutic drugs according to the expression of SLC11A1.ResultsExpression of SLC11A1 increased with progression and predicted unfavorable prognosis for glioma patients. The hazard ratio for SLC11A1 expression was 2.33 with 95% CI (1.92-2.58) (P < 0.001) in cox analysis. And based on expression, we found SLC11A1 stratified glioma patients into subgroups with different immune activation statuses. Moreover, we observed that patients with higher SLC11A1 levels companied with better immunotherapeutic response, while those with lower SLC11A1 levels may respond better to temozolomide.ConclusionThis study provided evidence that SLC11A1 was a novel prognostic marker and immunotherapy response indicator for gliomas. In some cases, SLC11A1 could be an effective marker for identifying patients who might benefit from immunotherapy or chemotherapy.

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“…Immunohistochemical expression of CD73 was evaluated using a semiquantitative scoring system. 25 In brief, cases were scored according to the following system: Absent (0): No expression of CD73 by tumor cells, or weak membranous staining in <10% of tumor cells; Weak (1): Weak membranous staining in >10% of tumor cells; Moderate (2): Moderate membranous staining in >10% of tumor cells, or strong/ circumferential membranous staining in <10% of tumor cells; Strong (3): Strong/circumferential membranous staining in >10% of tumor cells. The overall percentage of tumor cells expressing CD73 in each specimen was also assessed (Table 1).…”

Section: ■ Introductionmentioning

confidence: 99%

Chemical QuantArray: A Quantitative Tool for Mass Spectrometry Imaging

Stopka,

Ruiz,

Baquer

et al. 2023

Anal. Chem.

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Matrix-assisted laser desorption ionization mass spectrometry imaging (MALDI-MSI) is a powerful analytical technique that provides spatially preserved detection and quantification of analytes in tissue specimens. However, clinical translation still requires improved throughput, precision, and accuracy. To accomplish this, we created “Chemical QuantArray”, a gelatin tissue microarray (TMA) mold filled with serial dilutions of isotopically labeled endogenous metabolite standards. The mold is then cryo-sectioned onto a tissue homogenate to produce calibration curves. To improve precision and accuracy, we automatically remove pixels outside of each TMA well and investigated several intensity normalizations, including the utilization of a second stable isotope internal standard (IS). Chemical QuantArray enables the quantification of several endogenous metabolites over a wide dynamic range and significantly improve over current approaches. The technique reduces the space needed on the MALDI slides for calibration standards by approximately 80%. Furthermore, removal of empty pixels and normalization to an internal standard or matrix peak provided precision (<20% RSD) and accuracy (<20% DEV). Finally, we demonstrate the applicability of Chemical QuantArray by quantifying multiple purine metabolites in 14 clinical tumor specimens using a single MALDI slide. Chemical QuantArray improves the analytical characteristics and practical feasibility of MALDI-MSI metabolite quantification in clinical and translational applications.

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Single cell spatial analysis reveals the topology of immunomodulatory purinergic signaling in glioblastoma

Cited by 34 publications

References 98 publications

Exploring glioblastoma stem cell heterogeneity: Immune microenvironment modulation and therapeutic opportunities

Exploring glioblastoma stem cell heterogeneity: Immune microenvironment modulation and therapeutic opportunities

SLC11A1 as a stratification indicator for immunotherapy or chemotherapy in patients with glioma

Chemical QuantArray: A Quantitative Tool for Mass Spectrometry Imaging

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