High PD-1/PD-L1 Checkpoint Interaction Infers Tumor Selection and Therapeutic Sensitivity to Anti-PD-1/PD-L1 Treatment

Sánchez-Magraner, Lissete; Miles, James; Baker, Claire L.; Applebee, Christopher J.; Lee, Dae‐Jin; Elsheikh, Somaia; Lashin, Shaimaa; Withers, Katriona; Watts, Andrew G.; Parry, Richard V.; Edmead, Christine; López, José I.; Mehta, R. J.; Italiano, Antoîne; Ward, Stephen G.; Parker, Peter J.; Larijani, Banafshé

doi:10.1158/0008-5472.can-20-1117

Cited by 31 publications

(54 citation statements)

References 27 publications

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“…Therefore, immunotherapy should not be withheld for patients who are known to be PD-L1−. New imaging modalities are being developed to quantify PD-1 and PD-L1, which may help reduce some of the variability in future studies [ 78 , 79 ]. TMB, while recently approved as a tumor-agnostic biomarker for response to pembrolizumab, has been shown to be an unreliable predictor in RCC and should not be used in clinical decision making for these patients.…”

Section: Discussionmentioning

confidence: 99%

Predicting Response to Immunotherapy in Metastatic Renal Cell Carcinoma

Tucker

Rini

2020

Cancers

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Immunotherapy-based combinations, driven by PD-1, PD-L1, and CTLA-4 inhibitors, has altered the treatment landscape for metastatic renal cell carcinoma (RCC). Despite significant improvements in clinical outcomes, many patients do not experience deep or lasting benefits. Recent efforts to determine which patients are most likely to benefit from immunotherapy and immunotherapy-based combinations have shown promise but have not yet affected clinical practice. PD-L1 expression via immunohistochemistry (IHC) has shown promise in a few clinical trials, although variations in the IHC assays as well as the use of different values for positivity presents unique challenges for this potential biomarker. Several other candidate biomarkers were investigated including tumor mutational burden, gene expression signatures, single gene mutations, human endogenous retroviruses, the gastrointestinal microbiome, and peripheral blood laboratory markers. While individually these biomarkers have yet to explain the heterogeneity of treatment response to immunotherapy, using aggregate information from these biomarkers may inform clinically useful predictive biomarkers.

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Section: Discussionmentioning

confidence: 99%

Predicting Response to Immunotherapy in Metastatic Renal Cell Carcinoma

Tucker

Rini

2020

Cancers

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“…Consistent with their low expression, we could detect PD1-PDL1 protein complex formation via A-FRET in only 12 of the 58 analysed regions (Supplementary Table 2). Moreover, the values of A-FRET intensity were lower than in melanoma and renal cancer 16 . The proportion of regions with detectable PD1-PDL1 complex was significantly less in hypermutated than in non-hypermutated CRCs, while there was no difference between DB-and nDB-CRCs (Fig.4M).…”

Section: Hypermutated Db-crcs Are Enriched In Cd74 + Macrophagesmentioning

confidence: 69%

“…A total of 58 regions in slides K1-2 of the discovery cohort (Supplementary Table 2) were submitted to FASTBASE Solutions (Derio, Spain) to measure the interaction between PD1 and PDL1 in situ via amplified immune Förster Resonance Energy Transfer (i-FRET) 16 . Slides K1 were incubated overnight at 4 ºC with anti PD1 primary antibody (Supplementary Table 5) for donor only analyses.…”

Section: Detection Of Pd1-pdl1 Interaction In Situmentioning

confidence: 99%

Immunogenomic profile of colorectal cancer response to immune checkpoint blockade

Bortolomeazzi

Keddar

Montorsi

et al. 2020

Preprint

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Colorectal cancers (CRCs) show variable response to immune checkpoint blockade, which can only partially be explained by the variability of tumour mutational burden. To dissect the cellular and molecular determinants of response we performed a multi-omic screen of 721 cancer regions from patients treated with Pembrolizumab (KEYNOTE 177 clinical trial) or Nivolumab. Multi-regional whole exome, RNA and T-cell receptor sequencing show that, within hypermutated CRCs, response to both anti-PD1 agents is not positively associated with tumour mutational burden but with high clonality of immunogenic mutations, expanded T cells, low activation of the WNT pathway and active immune escape mechanisms. Coupling high-dimensional imaging mass cytometry with multiplexed immunofluorescence and computational spatial analysis, we observe that responsive hypermutated CRCs are rich in cytotoxic and proliferating PD1-expressing CD8 cells interacting with high-density clusters of PDL1-expressing antigen presenting macrophages. We propose that anti-PD1 agents release the PD1-PDL1 interaction between CD8 T cells and macrophages thus promoting cytotoxic anti-tumour activity.

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“…1a). 5 This assay is termed iFRET. Alternative assays exist which attempt to measure PD-1/PD-L1 interaction, however unlike iFRET these report on distances that likely reflect juxtaposition and cannot be relied upon to accurately report on checkpoint receptor engagement.…”

Section: Mainmentioning

confidence: 99%

“…Crucially, the iFRET assay was able to detect a PD-1/PD-L1 interaction in 10 of the 11 PD-L1 negative ccRCC patients. 5 This demonstrates that ligand expression is a poor surrogate of receptor engagement and that the direct functional PD-1/PD-L1 interaction needs to be quantified. Following this analysis, iFRET was used to assess PD-1/PD-L1 interaction states in 176 malignant melanoma patients with known clinical outcomes.…”

Section: Mainmentioning

confidence: 99%