γδ T Cells Support Pancreatic Oncogenesis by Restraining αβ T Cell Activation

Daley, Donnele; Zambirinis, Constantinos P.; Seifert, Lena; Akkad, Neha; Mohan, Navyatha; Werba, Gregor; Barilla, Rocky; Torres‐Hernandez, Alejandro; Hundeyin, Mautin; Mani, Vishnu R.; Avanzi, Antonina; Tippens, Daniel; Narayanan, Rajkishen; Jang, Jung Eun; Newman, Edwin B.; Pillarisetty, Venu G.; Dustin, Michael L.; Bar–Sagi, Dafna; Hajdu, Cristina; Miller, George

doi:10.1016/j.cell.2016.07.046

Cited by 265 publications

(276 citation statements)

References 43 publications

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“…As elegantly indicated in a recent review (58), murine models using human cells have shortcomings, such as harboring impaired immune infiltrates (e.g., lymphocytes, natural killer cells). This is particularly important, as a complex relationship exists between the immune system and pancreatic cancer development, and these complex interactions have important implications for disease progression and control (59,60). For example, CD8 + T cells and Th1-polarized CD4 + T cells mediate tumor protection in murine pancreatic cancer models and are associated with prolonged survival in humans (61,62).…”

Section: Discussionmentioning

confidence: 99%

Dabigatran Potentiates Gemcitabine-Induced Growth Inhibition of Pancreatic Cancer in Mice

Shi

Damhofer

Daalhuisen

et al. 2017

Mol Med

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Pancreatic cancer is one of the most lethal solid malignancies, with few treatment options. We have recently shown that expression of protease activated receptor (PAR)-1 in the tumor microenvironment drives the progression and induces the chemoresistance of pancreatic cancer. As thrombin is the prototypical PAR-1 agonist, here we address the effects of the direct thrombin inhibitor dabigatran on pancreatic cancer growth and drug resistance in an orthotropic pancreatic cancer model. We show that dabigatran treatment did not affect primary tumor growth, whereas it significantly increased tumor dissemination throughout the peritoneal cavity. Increased dissemination was accompanied by intratumoral bleeding and increased numbers of aberrant and/or collapsed blood vessels in the primary tumors. In combination with gemcitabine, dabigatran treatment limited primary tumor growth, did not induce bleeding complications and prevented tumor cell dissemination. Dabigatran was, however, not as efficient as genetic ablation of PAR-1 in our previous study, suggesting that thrombin is not the main PAR-1 agonist in the setting of pancreatic cancer. Overall, we show that dabigatran potentiates gemcitabine-induced growth inhibition of pancreatic cancer but does not affect primary tumor growth when used as monotherapy.

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Section: Discussionmentioning

confidence: 99%

Dabigatran Potentiates Gemcitabine-Induced Growth Inhibition of Pancreatic Cancer in Mice

Shi

Damhofer

Daalhuisen

et al. 2017

Mol Med

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“…Peri-pancreatic lymphocyte subsets have divergent effects on tumorigenesis by either suppressing cancer growth via antigen-restricted tumoricidal immune responses (CD8 + T-cells and Th1-polarized CD4 + T-cells) or by promoting tumor progression via induction of immune suppression (myeloid-derived suppressor cells; MDSCs and Th2-deviated CD4 + T-cells) (76,77). Another study showed that pancreatic adenocarcinoma-infiltrating γδ-T cells are a highly influential lymphocyte subset promoting pancreatic oncogenesis and reducing survival via novel cross-talk with the adaptive immune compartment; Nevertheless, they may also have prognostic significance of survival and response to immunotherapeutic regimen (77). Investigators from our Institution have reported an association between tumorassociated neutrophils (TANs) and advanced IPMN lesions (78).…”

Section: Peripheral Blood Cellmentioning

confidence: 99%

Updates and Critical Evaluation on Novel Biomarkers for the Malignant Progression of Intraductal Papillary Mucinous Neoplasms of the Pancreas

Moris

Damaskos

Spartalis

et al. 2017

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“…13 Along similar lines, gd T cells abundantly infiltrated mouse PDAs generated by the orthotopic implantation of malignant cells from Pdx1 Cre ;Kras G12D ;Tp53 R172H (KPC) mice (which spontaneously develop invasive PDAs by 8 weeks of age) into syngeneic immunocompetent hosts. In this system, gd T cells exhibited a peculiar phenotype (as compared to splenic gd T cells), as they were characterized by the upregulation of FAS ligand (FASLG), killer cell lectin-like receptor subfamily B member 1C (KLRB1C, best known as NK1.1), ectonucleoside triphosphate diphosphohydrolase 1 (ENTPD1, best known as CD39), junction adhesion molecule like (JAML), and TNF receptor superfamily member 4 (TNFRSF4, best known as OX40), as well as by enriched FOXP3…”

Section: Cd8mentioning

confidence: 95%

“…Similar observations were obtained in 6-month-old Ptf1a Cre ;Kras G12D (KC) mice, a model of preinvasive PDA. 13 Of note, KPC-derived cells orthotopically implanted into Ccr2 ¡/¡ , Ccr5 ¡/¡ , or Ccr6 ¡/¡ mice recruited limited amounts of gd T cells as compared to KPC-derived PDAs established in wild-type (WT) mice, demonstrating the importance of chemokine signaling in this setting. 13 To test whether gd T cells would play an etiologic role in pancreatic carcinogenesis, Daley and collaborators crossed KC mice with Tcrd ¡/¡ mice (which lack gd T cells but contain normal amounts of ab T lymphocytes).…”

Section: Cd8mentioning

confidence: 99%

“…11,12 Recent data from George Miller's laboratory (from New York University School of Medicine, New York, US) lend further support to this notion as they demonstrate that gd T cells foster pancreatic carcinogenesis by engaging immunological checkpoints on ab T cells. 13 Daley and collaborators observed that gd T cells are virtually absent from the normal human pancreas but account for up to 75% CD3 C T lymphocytes infiltrating human pancreatic ductal adenocarcinomas (PDAs). gd T cells outnumbered CD8…”

Section: Cd8mentioning

confidence: 99%

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