FAP Promotes Immunosuppression by Cancer-Associated Fibroblasts in the Tumor Microenvironment via STAT3–CCL2 Signaling

Yang, Xuguang; Lin, Yu‐Li; Shi, Ying‐Hong; Li, Bingji; Liu, Weiren; Yin, Wei; Dang, Yongjun; Chu, Yiwei; Fan, Jian‐Gao; He, Rui

doi:10.1158/0008-5472.can-15-2973

Cited by 505 publications

(412 citation statements)

References 45 publications

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“…Preliminary findings from our ongoing studies suggest that disruption of FAP protease inhibits pulmonary metastatic outgrowth and that this inhibition correlates with reduced macrophage infiltration (A. Lo et al, unpublished observations), which may be due to downregulation of CCL2 from FAP-deficient CAFs (12,13). Further studies are required to determine if this mechanism can be extended to PDA metastasis.…”

Section: Discussionmentioning

confidence: 88%

Fibroblast activation protein augments progression and metastasis of pancreatic ductal adenocarcinoma

Lo¹,

Buza

et al. 2017

JCI Insight

108

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Section: Discussionmentioning

confidence: 88%

Fibroblast activation protein augments progression and metastasis of pancreatic ductal adenocarcinoma

Lo¹,

Buza

et al. 2017

JCI Insight

108

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“…There is now ample evidence that CAF produce a large array of chemokines, including the ones specific for granulocytes, such as CXCL1 (Feig et al, 2013; Orimo and Weinberg, 2006). It has recently been reported that CAF also promote migration of monocytic cells to tumors (Yang et al, 2016), but the direct effect of fibroblasts on neutrophil migration has not been previously demonstrated. In our study, PMN-MDSC recruitment by CAF is consistent with the ability of CAF to produce granulocytic chemokines.…”

Section: Discussionmentioning

confidence: 99%

Cancer-Associated Fibroblasts Neutralize the Anti-tumor Effect of CSF1 Receptor Blockade by Inducing PMN-MDSC Infiltration of Tumors

et al. 2017

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Summary Tumor associated macrophages (TAM) contribute to all aspects of tumor progression. Use of CSF1R inhibitors to target TAM is therapeutically appealing, but has had very limited antitumor effects. Here, we have identified the mechanism that limited the effect of CSF1R targeted therapy. We demonstrated that carcinoma associated fibroblasts (CAF) are major sources of chemokines that recruit granulocytes to tumors. CSF1 produced by tumor cells caused HDAC2-mediated down-regulation of granulocyte-specific chemokine expression in CAF, which limited migration of these cells to tumors. Treatment with CSF1R inhibitors disrupted this cross talk and triggered a profound increase in granulocyte recruitment to tumors. Combining CSF1R inhibitor with a CXCR2 antagonist blocked granulocyte infiltration of tumors and showed strong anti-tumor effects.

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“…Incipient data are showing the role of the AXL in the paracrine feedback loop between cancer and fibroblastic cells with significant effects on resistance to conventional therapies, and likely, immunotherapy [149], paving the way for the design of new therapeutic strategies combining AXL targeting with ICBs. Growing evidence shows that FAP, selectively expressed on CAF subtypes and associated with ECM remodeling, induces tumor-promoting inflammation [150][151][152]. Furthermore, as mentioned before, FAP targeting has been shown to synergize with ICB-based immunotherapy [120,150,152].…”

Section: Tumor-extrinsic Factors Fostering Icb Resistancementioning

confidence: 77%

“…Growing evidence shows that FAP, selectively expressed on CAF subtypes and associated with ECM remodeling, induces tumor-promoting inflammation [150][151][152]. Furthermore, as mentioned before, FAP targeting has been shown to synergize with ICB-based immunotherapy [120,150,152].…”

Section: Tumor-extrinsic Factors Fostering Icb Resistancementioning

confidence: 77%

Mesenchymal traits at the convergence of tumor-intrinsic and -extrinsic mechanisms of resistance to immune checkpoint blockers

Trono¹,

Sistigu

Palermo³

et al. 2017

Emerging Topics in Life Sciences

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Correspondence: Paola Nisticò ( paola.nistico@ifo.gov.it)Targeting of immune checkpoint blockers (ICBs), such as cytotoxic T-lymphocyte antigen-4 and programmed-death 1/programmed-death ligand 1, has dramatically changed the landscape of cancer treatment. Seeing patients who were refractory to conventional therapy recover after immunotherapy, with high rates of objective durable responses and increased overall survival, has raised great enthusiasm in cancer care and research. However, to date, only a restricted portion of patients benefit from these therapies, due to natural and acquired resistance relying on the ever-evolving cross-talk between tumor and stromal cells. Here, we review the convergence of tumor-intrinsic and -extrinsic cues, both affecting tumor plasticity and tumor stroma leading to an immunosuppressive tumor microenvironment, which may account for the heterogeneous responses and resistance to ICB therapies. A deeper knowledge of the mechanisms and fingerprints involved in natural and acquired resistance is likely to bring clinical benefit to the majority of patients, offering important clues for overcoming drug resistance and boosting the effectiveness of treatment. We discuss the need to define tumor subtypes based on the tumor, immune and stromal gene signature and propose that the better we understand tumor mesenchymal traits, the more we will be able to identify predictive biomarkers of response to ICB treatments.

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FAP Promotes Immunosuppression by Cancer-Associated Fibroblasts in the Tumor Microenvironment via STAT3–CCL2 Signaling

Cited by 505 publications

References 45 publications

Fibroblast activation protein augments progression and metastasis of pancreatic ductal adenocarcinoma

Fibroblast activation protein augments progression and metastasis of pancreatic ductal adenocarcinoma

Cancer-Associated Fibroblasts Neutralize the Anti-tumor Effect of CSF1 Receptor Blockade by Inducing PMN-MDSC Infiltration of Tumors

Mesenchymal traits at the convergence of tumor-intrinsic and -extrinsic mechanisms of resistance to immune checkpoint blockers

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