Sin3B Expression Is Required for Cellular Senescence and Is Up-regulated upon Oncogenic Stress

Grandinetti, Kathryn B.; Jelinic, Petar; DiMauro, Teresa; Pellegrino, Jessica; Rodríguez, Rubén Fernández; Finnerty, Patricia M.; Ruoff, Rachel; Bardeesy, Nabeel; Logan, Susan K.; Gourichon, David

doi:10.1158/0008-5472.can-09-0537

Cited by 48 publications

(72 citation statements)

References 41 publications

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“…SIN3B was scarcely detected in control human pancreas and PDAC sections, but was strongly upregulated in both pancreatitis and PanINs, consistent with our previous observations in mouse tissues ( Figure 6A) (34). Interestingly, in most samples with high levels of SIN3B expression, we also observed p-STAT3 and IL-1α positivity, specifically at the sites of ADM and in PanIN lesions ( Figure 6A).…”

Section: Sin3b Levels Correlate With An Inflammatory Response In Humasupporting

confidence: 91%

“…Our recent discovery that the chromatin modifier SIN3B mediates RAS-induced senescence in mouse fibroblasts coupled with our observation that SIN3B is upregulated in RASdriven PanINs initially hinted toward a tumor-suppressive role for SIN3B in the pancreas (34). We demonstrate here that genetic inactivation of the chromatin-associated SIN3B protein impairs the occurrence of oncogene-induced senescence in vivo and results in a cell-autonomous defect in KRAS-driven production of the proinflammatory IL-1α cytokine.…”

Section: Discussionmentioning

confidence: 50%

Section: Introductionmentioning

confidence: 99%

“…We have recently demonstrated that mouse embryonic fibroblasts genetically inactivated for Sin3B are refractory to quiescence as well as oncogene-induced senescence (33)(34)(35). In addition, SIN3B levels are significantly upregulated in preneoplastic senescent lesions in a mouse model of PDAC (34). Unlike most perturbations that bypass oncogene-induced senescence, Sin3B inactivation is not sufficient to sensitize to oncogenic RAS-induced transformation, providing an experimental context in which these processes are uncoupled (34).…”

Section: Introductionmentioning

confidence: 99%

“…In addition, SIN3B levels are significantly upregulated in preneoplastic senescent lesions in a mouse model of PDAC (34). Unlike most perturbations that bypass oncogene-induced senescence, Sin3B inactivation is not sufficient to sensitize to oncogenic RAS-induced transformation, providing an experimental context in which these processes are uncoupled (34). Therefore, genetic inactivation of Sin3B represents a unique opportunity to dissect the physiological relevance of cellular senescence in pancreatic cancer progression.…”

Section: Introductionmentioning

confidence: 99%

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Senescence-associated SIN3B promotes inflammation and pancreatic cancer progression

Rielland¹,

Cantor²,

Graveline³

et al. 2014

J. Clin. Invest.

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Pancreatic ductal adenocarcinoma (PDAC) is strikingly resistant to conventional therapeutic approaches. We previously demonstrated that the histone deacetylase-associated protein SIN3B is essential for oncogeneinduced senescence in cultured cells. Here, using a mouse model of pancreatic cancer, we have demonstrated that SIN3B is required for activated KRAS-induced senescence in vivo. Surprisingly, impaired senescence as the result of genetic inactivation of Sin3B was associated with delayed PDAC progression and correlated with an impaired inflammatory response. In murine and human pancreatic cells and tissues, levels of SIN3B correlated with KRAS-induced production of IL-1α. Furthermore, evaluation of human pancreatic tissue and cancer cells revealed that Sin3B was decreased in control and PDAC samples, compared with samples from patients with pancreatic inflammation. These results indicate that senescence-associated inflammation positively correlates with PDAC progression and suggest that SIN3B has potential as a therapeutic target for inhibiting inflammation-driven tumorigenesis.

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Section: Sin3b Levels Correlate With An Inflammatory Response In Humasupporting

confidence: 91%

Section: Discussionmentioning

confidence: 50%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

Senescence-associated SIN3B promotes inflammation and pancreatic cancer progression

Rielland¹,

Cantor²,

Graveline³

et al. 2014

J. Clin. Invest.

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SIN3B Loss Heats up Cold Tumor Microenvironment to Boost Immunotherapy in Pancreatic Cancer

Zhang,

Tang,

Wang

et al. 2024

Advanced Science

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Despite progress significant advances in immunotherapy for some solid tumors, pancreatic ductal adenocarcinoma (PDAC) remains unresponsive poorly responsive to such interventions, largely due to its highly immunosuppressive tumor microenvironment (TME) with limited CD8+ T cell infiltration. This study explores the role of the epigenetic factor Sin3B in the PDAC TME. Using murine PDAC models, we found that tumor cell‐intrinsic Sin3B loss reshapes the TME, increasing CD8+ T cell infiltration and cytotoxicity, thus impeding tumor progression and enhancing sensitivity to anti‐PD1 treatment. Sin3B‐deficient tumor cells exhibited amplified CXCL9/10 secretion in response to Interferon‐gamma (IFNγ), creating a positive feedback loop via the CXCL9/10‐CXCR3 axis, thereby intensifying the anti‐tumor immune response against PDAC. Mechanistically, extensive epigenetic regulation is uncovered by Sin3B loss, particularly enhanced H3K27Ac distribution on genes related to immune responses in PDAC cells. Consistent with the murine model findings, analysis of human PDAC samples revealed a significant inverse correlation between SIN3B levels and both CD8+ T cell infiltration and CXCL9/10 expression. Notebly, PDAC patients with lower SIN3B expression showed a more favorable response to anti‐PD1 therapy. The findings suggest that targeting SIN3B can enhance cytotoxic T cell infiltration into the tumor site and improve immunotherapy efficacy in PDAC, offering potential avenues for therapeutic biomarker or target in this challenging disease.

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Zebrafish sin3b mutants are viable but have size, skeletal, and locomotor defects

Moravec

Yousef

Kinney

et al. 2017

Developmental Dynamics

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Surprisingly, Sin3b is not essential in zebrafish. sin3b mutants show a decrease in fitness, small size, changes to locomotor behavior, and delayed bone development. We did not detect a role for Sin3b in cell proliferation. Our analysis of the sin3b mutant revealed a more nuanced requirement for zebrafish Sin3b than would be predicted from analysis of mutants in other species. Developmental Dynamics 246:946-955, 2017. © 2017 Wiley Periodicals, Inc.

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Sin3B Expression Is Required for Cellular Senescence and Is Up-regulated upon Oncogenic Stress

Cited by 48 publications

References 41 publications

Senescence-associated SIN3B promotes inflammation and pancreatic cancer progression

Senescence-associated SIN3B promotes inflammation and pancreatic cancer progression

SIN3B Loss Heats up Cold Tumor Microenvironment to Boost Immunotherapy in Pancreatic Cancer

Zebrafish sin3b mutants are viable but have size, skeletal, and locomotor defects

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