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The Necrosome Promotes Pancreas Oncogenesis via CXCL1 and Mincle Induced Immune Suppression
Neoplastic pancreatic epithelial cells are widely believed to die via Caspase 8-dependant apoptotic cell death and chemotherapy is thought to further promote tumor apoptosis(1). Conversely, disruption of apoptosis is a basic modality cancer cells exploit for survival(2,3). However, the role of necro...
| Autores principales: | , , , , , , , , , , , , , , , , , , , , , |
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| Formato: | Online Artículo Texto |
| Lenguaje: | English |
| Publicado: |
2016
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| Materias: | |
| Acceso en línea: | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4833566/ https://www.ncbi.nlm.nih.gov/pubmed/27049944 http://dx.doi.org/10.1038/nature17403 |
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| author | Seifert, Lena Werba, Gregor Tiwari, Shaun Giao Ly, Nancy Ngoc Alothman, Sara Alqunaibit, Dalia Avanzi, Antonina Barilla, Rocky Daley, Donnele Greco, Stephanie H. Torres-Hernandez, Alejandro Pergamo, Matthew Ochi, Atsuo Zambirinis, Constantinos P. Pansari, Mridul Rendon, Mauricio Tippens, Daniel Hundeyin, Mautin Mani, Vishnu R. Hajdu, Cristina Engle, Dannielle Miller, George |
| author_facet | Seifert, Lena Werba, Gregor Tiwari, Shaun Giao Ly, Nancy Ngoc Alothman, Sara Alqunaibit, Dalia Avanzi, Antonina Barilla, Rocky Daley, Donnele Greco, Stephanie H. Torres-Hernandez, Alejandro Pergamo, Matthew Ochi, Atsuo Zambirinis, Constantinos P. Pansari, Mridul Rendon, Mauricio Tippens, Daniel Hundeyin, Mautin Mani, Vishnu R. Hajdu, Cristina Engle, Dannielle Miller, George |
| author_sort | Seifert, Lena |
| collection | PubMed |
| description | Neoplastic pancreatic epithelial cells are widely believed to die via Caspase 8-dependant apoptotic cell death and chemotherapy is thought to further promote tumor apoptosis(1). Conversely, disruption of apoptosis is a basic modality cancer cells exploit for survival(2,3). However, the role of necroptosis, or programmed necrosis, in pancreatic ductal adenocarcinoma (PDA) is uncertain. There are a multitude of potential inducers of necroptosis in PDA including ligation of TNFR1, CD95, TRAIL receptors, Toll-like receptors, ROS, and Chemotherapeutics(4,5). Here we report that the principal components of the necrosome, RIP1 and RIP3, are highly expressed in PDA and are further upregulated by chemotherapy. Blockade of the necrosome in vitro promoted cancer cell proliferation and induced an aggressive oncogenic phenotype. By contrast, in vivo RIP3 deletion or RIP1 inhibition was protective against oncogenic progression and was associated with the development of a highly immunogenic myeloid and T cell infiltrate. The immune-suppressive tumor microenvironment (TME) associated with intact RIP1/RIP3 signaling was in-part contingent on necroptosis-induced CXCL1 expression whereas CXCL1 blockade was protective against PDA. Moreover, we found that cytoplasmic SAP130 was expressed in PDA in a RIP1/RIP3-dependent manner, and Mincle – its cognate receptor – was upregulated in tumor-infiltrating myeloid cells. Mincle ligation by SAP130 promoted oncogenesis whereas Mincle deletion was protective and phenocopied the immunogenic reprogramming of the TME characteristic of RIP3 deletion. Cellular depletion experiments suggested that whereas inhibitory macrophages promote tumorigenesis in PDA, they lose their immune-suppressive effects in the context of RIP3 or Mincle deletion. As such, T cells which are dispensable to PDA progression in hosts with intact RIP3 or Mincle signaling become reprogrammed into indispensable mediators of anti-tumor immunity in absence of RIP3 or Mincle. Our work describes parallel networks of necroptosis-induced CXCL1 and Mincle signaling which critically promote macrophage-induced adaptive immune suppression enabling PDA progression. |
| format | Online Article Text |
| id | pubmed-4833566 |
| institution | National Center for Biotechnology Information |
| language | English |
| publishDate | 2016 |
| record_format | MEDLINE/PubMed |
| spelling | pubmed-48335662016-10-06 The Necrosome Promotes Pancreas Oncogenesis via CXCL1 and Mincle Induced Immune Suppression Seifert, Lena Werba, Gregor Tiwari, Shaun Giao Ly, Nancy Ngoc Alothman, Sara Alqunaibit, Dalia Avanzi, Antonina Barilla, Rocky Daley, Donnele Greco, Stephanie H. Torres-Hernandez, Alejandro Pergamo, Matthew Ochi, Atsuo Zambirinis, Constantinos P. Pansari, Mridul Rendon, Mauricio Tippens, Daniel Hundeyin, Mautin Mani, Vishnu R. Hajdu, Cristina Engle, Dannielle Miller, George Nature Article Neoplastic pancreatic epithelial cells are widely believed to die via Caspase 8-dependant apoptotic cell death and chemotherapy is thought to further promote tumor apoptosis(1). Conversely, disruption of apoptosis is a basic modality cancer cells exploit for survival(2,3). However, the role of necroptosis, or programmed necrosis, in pancreatic ductal adenocarcinoma (PDA) is uncertain. There are a multitude of potential inducers of necroptosis in PDA including ligation of TNFR1, CD95, TRAIL receptors, Toll-like receptors, ROS, and Chemotherapeutics(4,5). Here we report that the principal components of the necrosome, RIP1 and RIP3, are highly expressed in PDA and are further upregulated by chemotherapy. Blockade of the necrosome in vitro promoted cancer cell proliferation and induced an aggressive oncogenic phenotype. By contrast, in vivo RIP3 deletion or RIP1 inhibition was protective against oncogenic progression and was associated with the development of a highly immunogenic myeloid and T cell infiltrate. The immune-suppressive tumor microenvironment (TME) associated with intact RIP1/RIP3 signaling was in-part contingent on necroptosis-induced CXCL1 expression whereas CXCL1 blockade was protective against PDA. Moreover, we found that cytoplasmic SAP130 was expressed in PDA in a RIP1/RIP3-dependent manner, and Mincle – its cognate receptor – was upregulated in tumor-infiltrating myeloid cells. Mincle ligation by SAP130 promoted oncogenesis whereas Mincle deletion was protective and phenocopied the immunogenic reprogramming of the TME characteristic of RIP3 deletion. Cellular depletion experiments suggested that whereas inhibitory macrophages promote tumorigenesis in PDA, they lose their immune-suppressive effects in the context of RIP3 or Mincle deletion. As such, T cells which are dispensable to PDA progression in hosts with intact RIP3 or Mincle signaling become reprogrammed into indispensable mediators of anti-tumor immunity in absence of RIP3 or Mincle. Our work describes parallel networks of necroptosis-induced CXCL1 and Mincle signaling which critically promote macrophage-induced adaptive immune suppression enabling PDA progression. 2016-04-06 2016-04-14 /pmc/articles/PMC4833566/ /pubmed/27049944 http://dx.doi.org/10.1038/nature17403 Text en Users may view, print, copy, and download text and data-mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use:http://www.nature.com/authors/editorial_policies/license.html#terms |
| spellingShingle | Article Seifert, Lena Werba, Gregor Tiwari, Shaun Giao Ly, Nancy Ngoc Alothman, Sara Alqunaibit, Dalia Avanzi, Antonina Barilla, Rocky Daley, Donnele Greco, Stephanie H. Torres-Hernandez, Alejandro Pergamo, Matthew Ochi, Atsuo Zambirinis, Constantinos P. Pansari, Mridul Rendon, Mauricio Tippens, Daniel Hundeyin, Mautin Mani, Vishnu R. Hajdu, Cristina Engle, Dannielle Miller, George The Necrosome Promotes Pancreas Oncogenesis via CXCL1 and Mincle Induced Immune Suppression |
| title | The Necrosome Promotes Pancreas Oncogenesis via CXCL1 and Mincle Induced Immune Suppression |
| title_full | The Necrosome Promotes Pancreas Oncogenesis via CXCL1 and Mincle Induced Immune Suppression |
| title_fullStr | The Necrosome Promotes Pancreas Oncogenesis via CXCL1 and Mincle Induced Immune Suppression |
| title_full_unstemmed | The Necrosome Promotes Pancreas Oncogenesis via CXCL1 and Mincle Induced Immune Suppression |
| title_short | The Necrosome Promotes Pancreas Oncogenesis via CXCL1 and Mincle Induced Immune Suppression |
| title_sort | necrosome promotes pancreas oncogenesis via cxcl1 and mincle induced immune suppression |
| topic | Article |
| url | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4833566/ https://www.ncbi.nlm.nih.gov/pubmed/27049944 http://dx.doi.org/10.1038/nature17403 |
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