9p21 loss confers a cold tumor immune microenvironment and primary resistance to immune checkpoint therapy

Han, Guangchun; Yang, Guoliang; Hao, Dapeng; Lü, Yang; Thein, Kyaw Zin; Simpson, Benjamin S.; Chen, Jianfeng; Sun, Ryan; Alhalabi, Omar; Wang, Ruiping; Dang, Minghao; Dai, Enyu; Zhang, Shaojun; Nie, Fengqi; Zhao, Shuangtao; Guo, Charles C.; Hamza, Ameer; Czerniak, Bogdan; Cheng, Chao; Siefker‐Radtke, Arlene O.; Bhat, Krishna; Futreal, Andrew; Peng, Guang; Wargo, Jennifer A.; Peng, Weiyi; Kadara, Humam; Ajani, Jaffer A.; Swanton, Charles; Litchfield, Kevin; Ahnert, Jordi Rodón; Gao, Jianjun; Wang, Linghua

doi:10.1038/s41467-021-25894-9

Cited by 86 publications

(92 citation statements)

References 76 publications

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“…Upregulation of VEGFA at 6p21.1 in C2 could increase the malignancy of tumor cells and was often accompanied by hypoxia, angiogenesis, and immunosuppressive TME, suggesting tolerance to immunotherapy ( Wang et al, 2020 ). 9p21 deletion (CDKN2A/B) in C2 also conferred primary resistance to immune checkpoint therapy ( Han et al, 2021 ). LAMC2 amplification at 1q25.3 could result in gemcitabine resistance via EMT ( Okada et al, 2021 ).…”

Section: Resultsmentioning

confidence: 99%

Multi-Omics Characterization of Tumor Microenvironment Heterogeneity and Immunotherapy Resistance Through Cell States–Based Subtyping in Bladder Cancer

Tao

et al. 2022

Front. Cell Dev. Biol.

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Due to the strong heterogeneity of bladder cancer (BC), there is often substantial variation in the prognosis and efficiency of immunotherapy among BC patients. For the precision treatment and assessment of prognosis, the subtyping of BC plays a critical role. Despite various subtyping methods proposed previously, most of them are based on a limited number of molecules, and none of them is developed on the basis of cell states. In this study, we construct a single-cell atlas by integrating single cell RNA-seq, RNA microarray, and bulk RNA-seq data to identify the absolute proportion of 22 different cell states in BC, including immune and nonimmune cell states derived from tumor tissues. To explore the heterogeneity of BC, BC was identified into four different subtypes in multiple cohorts using an improved consensus clustering algorithm based on cell states. Among the four subtypes, C1 had median prognosis and best overall response rate (ORR), which characterized an immunosuppressive tumor microenvironment. C2 was enriched in epithelial-mesenchymal transition/invasion, angiogenesis, immunosuppression, and immune exhaustion. Surely, C2 performed the worst in prognosis and ORR. C3 with worse ORR than C2 was enriched in angiogenesis and almost nonimmune exhaustion. Displaying an immune effective environment, C4 performed the best in prognosis and ORR. We found that patients with just an immunosuppressive environment are suitable for immunotherapy, but patients with an immunosuppressive environment accompanied by immune exhaustion or angiogenesis may resist immunotherapy. Furthermore, we conducted exploration into the heterogeneity of the transcriptome, mutational profiles, and somatic copy-number alterations in four subtypes, which could explain the significant differences related to cell states in prognosis and ORR. We also found that PD-1 in immune and tumor cells could both influence ORR in BC. The level of TGFβ in a cell state can be opposite to the overall level in the tissues, and the level in a specific cell state could predict ORR more accurately. Thus, our work furthers the understanding of heterogeneity and immunotherapy resistance in BC, which is expected to assist clinical practice and serve as a supplement to the current subtyping method from a novel perspective of cell states.

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Section: Resultsmentioning

confidence: 99%

Multi-Omics Characterization of Tumor Microenvironment Heterogeneity and Immunotherapy Resistance Through Cell States–Based Subtyping in Bladder Cancer

Tao

et al. 2022

Front. Cell Dev. Biol.

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“…Likewise, future studies will also investigate whether inclusion of single gene-based DNA biomarkers identified as potentially predictive in one or more tumor types (e.g. STK11, PBRM1, ARID1A, CDNK2A [68][69][70][71][72][73][74][75] or additional immune related genes assessed on the current expanded quantitative expression panel run in parallel with StrataNGS testing can improve the performance of the IRS model. Limited PD-L1 IHC data was available for subjects in the SCMD, and hence we are not able to directly compare performance of IRS and PD-L1 IHC for predicting pembrolizumab benefit; additionally, this limitation also biases against the overall proportion of patients outside of currently approved indications predicted to benefit from pembrolizumab by IRS, as herein we considered all patients in approved tumor types to be in an approved indication, although in many tumor types only a minority of patients are approved for pembrolizumab treatment based on PD-L1 IHC cutoffs.…”

Section: Discussionmentioning

confidence: 99%

Prediction of pan-solid tumor pembrolizumab benefit by integrating tumor mutation and gene expression profiling

Khazanov

Shreve

Lamb

et al. 2022

Preprint

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Pembrolizumab is approved in many advanced solid tumor types, however predictive biomarkers and the proportion of pembrolizumab-benefiting patients vary. Biomarkers beyond PD-L1 immunohistochemistry, microsatellite instability (MSI) status, and tumor mutation burden (TMB) may improve benefit prediction. Here, leveraging treatment data (time to next treatment [TTNT]) and comprehensive genomic and quantitative transcriptomic profiling on routine tumor tissue from 708 patients (24 tumor types) collected in an ongoing observational trial (NCT03061305), we report a multivariate, integrative predictor of pan-solid tumor pembrolizumab benefit. The Immune Response Score (IRS) model, which includes TMB and quantitative PD-1, PD-L2, ADAM12 and CD4 RNA expression, was confirmed as predictive through comparison of pembrolizumab TTNT with previous chemotherapy TTNT in a subset of 166 patients treated with both. Applying IRS to the entire NCT03061305 cohort (n=25,770 patients), 13.2-30.7% of patients (2.2-9.6% of patients outside of pembrolizumab approved tumor types [including TMB-High and MSI-High]) are predicted to benefit substantially from pembrolizumab. Hence, if prospectively validated, the IRS model may improve pembrolizumab benefit prediction across approved tumor types including patients outside of currently approved indications.

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“…Its effects mimic those generated by extrinsic manipulations of the cancer cell UPR (64,65), spontaneous UPR during tumor growth in vivo (74), and genetic manipulation of UPR branches (73,74). Of paramount relevance aneuploid cells impart changes to activated T cells such as decreased IFNg and Granzyme B production that are similar to changes reported for CD4 T cells in ascites of ovarian cancer patients (167), or changes in gene expression noted in head & neck and urothelial cancers with an aneuploid switch based on chromosome 9p arm loss or homozygous deletion of 9p21.3 (9p21) (168,169). Aneuploidy also has the potential to fuel inflammation at the tumor-immune interface through the mechanism illustrated herein.…”

Section: Conclusion and Perspectivementioning

confidence: 99%

The Unfolded Protein Response at the Tumor-Immune Interface

Zanetti

Dosset

et al. 2022

Front. Immunol.

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The tumor-immune interface has surged to primary relevance in an effort to understand the hurdles facing immune surveillance and cancer immunotherapy. Reports over the past decades have indicated a role for the unfolded protein response (UPR) in modulating not only tumor cell fitness and drug resistance, but also local immunity, with emphasis on the phenotype and altered function of immune cells such as myeloid cells and T cells. Emerging evidence also suggests that aneuploidy correlates with local immune dysregulation. Recently, we reported that the UPR serves as a link between aneuploidy and immune cell dysregulation in a cell nonautonomous way. These new findings add considerable complexity to the organization of the tumor microenvironment (TME) and the origin of its altered function. In this review, we summarize these data and also discuss the role of aneuploidy as a negative regulator of local immunity.

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9p21 loss confers a cold tumor immune microenvironment and primary resistance to immune checkpoint therapy

Cited by 86 publications

References 76 publications

Multi-Omics Characterization of Tumor Microenvironment Heterogeneity and Immunotherapy Resistance Through Cell States–Based Subtyping in Bladder Cancer

Multi-Omics Characterization of Tumor Microenvironment Heterogeneity and Immunotherapy Resistance Through Cell States–Based Subtyping in Bladder Cancer

Prediction of pan-solid tumor pembrolizumab benefit by integrating tumor mutation and gene expression profiling

The Unfolded Protein Response at the Tumor-Immune Interface

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