Tumor-derived GDF-15 blocks LFA-1 dependent T cell recruitment and suppresses responses to anti-PD-1 treatment

Haake, Markus; Haack, Beatrice; Schäfer, Tina; Harter, Patrick N.; Mattavelli, Greta; Eiring, Patrick; Vashist, Neha; Wedekink, Florian; Genßler, Sabrina; Fischer, Birgitt; Dahlhoff, Julia; Mokhtari, Fatemeh; Kuzkina, Anastasia; Welters, Marij J.P.; Benz, Tamara; Sorger, Lena; Thiemann, Vincent; Almanzar, Giovanni; Selle, Martina; Thein, Kyaw Zin; Spath, James A.; González, Mario; Reitinger, Carmen; Ipsen-Escobedo, Andrea; Wistuba‐Hamprecht, Kilian; Eichler, Kristin; Filipski, Katharina; Zeiner, Pia S.; Beschorner, Rudi; Goedemans, Renske; Gogolla, Falk Hagen; Hackl, Hubert; Rooswinkel, Rogier W.; Thiem, Alexander; Roche, Patrick C.; Joshi, Hemant; Pühringer, Dirk; Wöckel, Achim; Diessner, Joachim; Rüdiger, Manfred; Leo, Eugen; Cheng, Phil F.; Levesque, Mitchell P.; Goebeler, Matthias; Sauer, Markus; Nimmerjahn, Falk; Schuberth-Wagner, Christine; Felten, Stefanie von; Mittelbronn, Michel; Mehling, Matthias; Beilhack, Andreas; Burg, Sjoerd H. van der; Riedel, Angela; Weide, Benjamin; Dummer, Reinhard; Wischhusen, Jörg

doi:10.1038/s41467-023-39817-3

Cited by 20 publications

(15 citation statements)

References 68 publications

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“…High expression of the integrin ITGB2 was previously shown to be associated with poor survival outcome [88], underscoring that high expression in TAMs is crucial. In contrast, ITGB2 is also associated with CD8+ T cells, as it encodes the beta chain of the LFA-1 protein, which has been shown to be essential in the assembly of the immune synapse or to influence lymphocyte extravasation and T-cell recruitment to the tumor and is regulated by GDF-15 [89]. This association is also underlined by a positive significant correlation of ITGB2 expression with M2 macrophages and, to a lesser extent, with estimated CD8+ T-cell infiltration in the TCGA cohort (Fig.…”

Section: Discussionmentioning

confidence: 99%

Integrated immunogenomic analyses of high-grade serous ovarian cancer reveal vulnerability to combination immunotherapy

Gronauer,

Madersbacher,

Monfort-Lanzas

et al. 2024

Preprint

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Background: High-grade serous ovarian cancer (HGSOC) remains the most lethal gynecologic malignancy despite new therapeutic concepts, including poly-ADP-ribose polymerase inhibitors (PARPis) and antiangiogenic therapy. The efficacy of immunotherapies is modest, but clinical trials investigating the potential of combination immunotherapy with PARPis are underway. Homologous recombination repair deficiency (HRD) or BRCAness and the composition of the tumor microenvironment appear to play a critical role in determining the therapeutic response. Methods: We conducted comprehensive immunogenomic analyses of HGSOC using data from several patient cohorts, including a new cohort from the Medical University of Innsbruck (MUI). Machine learning methods were used to develop a classification model for BRCAness from gene expression data. Integrated analysis of bulk and single-cell RNA sequencing data was used to delineate the tumor immune microenvironment and was validated by immunohistochemistry. The impact of PARPi and BRCA1 mutations on the activation of immune-related pathways was studied in vitro using ovarian cancer cell lines, RNA sequencing, and immunofluorescence analysis. Results: We identified a predictive 24-gene signature to determine BRCAness. Comprehensive analysis of the tumor microenvironment allowed us to identify patient samples with BRCAness and high immune infiltration. Further characterization of these samples revealed increased infiltration of immunosuppressive cells, including tumor-associated macrophages (TAMs) expressing TREM2, C1QA, and LILRB4, as identified by further analysis of single-cell RNA sequencing data and gene expression analysis of samples from patients receiving combination therapy with PARPi and anti-PD-1. PARPi activated the cGAS-STING signaling pathway and the downstream innate immune response in a similar manner to HGSOC patients with BRCAness status. We have developed a web application (https://ovrseq.icbi.at) and an associated R package OvRSeq, which allow for comprehensive characterization of ovarian cancer patient samples and assessment of a vulnerability score that enables stratification of patients to predict response to the mentioned combination immunotherapy. Conclusions: Genomic instability in HGSOC affects the tumor immune environment, and TAMs play a crucial role in modulating the immune response. Based on various datasets, we have developed a diagnostic application that uses RNA sequencing data not only to comprehensively characterize HGSOC but also to predict vulnerability and response to combination immunotherapy. Keywords: High-grade serous ovarian cancer, BRCAness, PARP inhibitor, immunotherapy, vulnerability, RNA sequencing, tumor-associated macrophages, tumor immune microenvironment

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Section: Discussionmentioning

confidence: 99%

Integrated immunogenomic analyses of high-grade serous ovarian cancer reveal vulnerability to combination immunotherapy

Gronauer,

Madersbacher,

Monfort-Lanzas

et al. 2024

Preprint

Self Cite

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“…In gall bladder cancer, GDF15 has been shown to increase PD-L1 expression in a PI3K/Akt/Erk dependent manner to result in immune suppression (33). In addition, a recent study has shown that GDF15 suppresses responses to anti-PD1 immune check point therapy, as GDF-15 impairs T-cell endothelial adhesion and thus recruitment to the tumor, with T-reg recruitment being less affected (34). Thus, GPX3 and GDF15 appear to share similarities in their correlation to tumor immune cell signatures.…”

Section: Discussionmentioning

confidence: 99%

GPX3 supports ovarian cancer tumor progressionin vivoand promotes expression of GDF15

Chang,

Cheng,

Kamlapurkar

et al. 2024

Preprint

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Objective: We previously reported that high expression of the extracellular glutathione peroxidase GPX3 is associated with poor patient outcome in ovarian serous adenocarcinomas, and that GPX3 protects ovarian cancer cells from oxidative stress in culture. Here we tested if GPX3 is necessary for tumor establishment in vivo and to identify novel downstream mediators of the pro-tumorigenic function of GPX3. Methods: GPX3 was knocked-down in ID8 ovarian cancer cells by shRNA to test the role of GPX3 in tumor establishment using a syngeneic IP xenograft model. RNA sequencing analysis was carried out in OVCAR3 cells following shRNA-mediated GPX3 knock-down to identify GPX3-dependent gene expression signatures. Results: GPX3 knock-down abrogated clonogenicity and intraperitoneal tumor development in vivo, and the effects were dependent on the level of GPX3 knock-down. RNA sequencing showed that loss of GPX3 leads to decreased gene expression patterns related to pro-tumorigenic signaling pathways. Validation studies identified GDF15 as strongly dependent on GPX3. GDF15, a member of the TGF-β growth factor family, has known oncogenic and immune modulatory activities. Similarly, GPX3 expression positively correlated with pro-tumor immune cell signatures, including regulatory T-cell and macrophage infiltration, and displayed significant correlation with PD-L1 expression. Conclusions: We show for the first time that tumor produced GPX3 is necessary for ovarian cancer growth in vivo and that it regulates expression of GDF15. The immune profile associated with GPX3 expression in serous ovarian tumors suggests that GPX3 may be an alternate marker of ovarian tumors susceptible to immune check-point inhibitors.

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“…Anamorelin, an oral ghrelin agonist, has been shown to increase oral intake and muscle mass (body weight) but not to augment the therapeutic effects of chemotherapy [28]. In addition, basic research has shown that GDF-15 is associated with metastatic potential [29], proliferative capacity [30], therapeutic e cacy [31], and decreased survival [32,33]. Moreover, anti-GDF-15 antibodies are also expected to potentiate the action of immune checkpoint inhibitors [31].…”

Section: Discussionmentioning

confidence: 99%

“…In addition, basic research has shown that GDF-15 is associated with metastatic potential [29], proliferative capacity [30], therapeutic e cacy [31], and decreased survival [32,33]. Moreover, anti-GDF-15 antibodies are also expected to potentiate the action of immune checkpoint inhibitors [31]. Future prospective studies evaluating anorexia, weight loss, and treatment e cacy, including biomarker studies, are required to further provide further clarity.…”

Section: Discussionmentioning

confidence: 99%

Exploring the Relationship Between Anorexia and Therapeutic Efficacy in Advanced Lung Cancer Treatment: A Retrospective Study

Doshita,

Naito,

Matsuda

et al. 2024

Preprint

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Background Chemotherapy-induced anorexia is frequently observed in patients with advanced lung cancer who are receiving chemotherapy. This study explored the relationship between chemotherapy-induced anorexia and therapeutic outcomes in patients with stage IV non-small cell lung cancer undergoing platinum-based chemotherapy combined with immune checkpoint inhibitors. Methods We retrospectively reviewed the medical records of 106 patients with stage IV non-small cell lung cancer treated with platinum-based chemotherapy combined with immune checkpoint inhibitors between January 2019 and October 2022. The incidence of weight loss and its association with treatment efficacy was assessed in the chemotherapy-induced anorexia group. Chemotherapy-induced anorexia and chemotherapy-induced nausea and vomiting were evaluated using Common Terminology Criteria for Adverse Events version 5.0. Progression-free and overall survival were used to measure treatment efficacy. Results Chemotherapy-induced anorexia was observed in 13.2% of patients. Patients with chemotherapy-induced anorexia showed significant weight loss at 6 and 9 weeks after treatment initiation compared to those in the non-chemotherapy-induced anorexia group. Progression-free and overall survival were shorter in the chemotherapy-induced anorexia group than in the non-chemotherapy-induced anorexia group, but the difference was not statistically significant. Conclusions Chemotherapy-induced anorexia was associated with significant weight loss and reduced treatment efficacy in patients with stage IV non-small cell lung cancer. These findings suggest the need for aggressive supportive therapy for chemotherapy-induced anorexia to prevent weight loss and maintain therapeutic efficacy during platinum-based chemotherapy combined with immune checkpoint inhibitors.

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Tumor-derived GDF-15 blocks LFA-1 dependent T cell recruitment and suppresses responses to anti-PD-1 treatment

Cited by 20 publications

References 68 publications

Integrated immunogenomic analyses of high-grade serous ovarian cancer reveal vulnerability to combination immunotherapy

Integrated immunogenomic analyses of high-grade serous ovarian cancer reveal vulnerability to combination immunotherapy

GPX3 supports ovarian cancer tumor progressionin vivoand promotes expression of GDF15

Exploring the Relationship Between Anorexia and Therapeutic Efficacy in Advanced Lung Cancer Treatment: A Retrospective Study

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