Project description:Rewiring T cell metabolism can improve intratumoral infiltration and function. By performing a CRISPR/Cas9 metabolic survey in CD8+ T cells, we identified 83 targets enriched at the primary and/or metastatic niche in the context of pancreatic cancer. We applied single-cell RNA sequencing to disclose transcriptome changes associated with each metabolic perturbation. This revealed Elongation of Very-Long-chain fatty acids protein 1 (Elovl1) as a metabolic target to sustain proliferation and both effector and memory functions in CD8+ T cells. Accordingly, Elovl1 inactivation in adoptively transferred T cells combined with αPD-1 showed therapeutic efficacy in resistant pancreatic and melanoma tumors. Loss of Elovl1 in T cells rewired lipid metabolism and changed the plasma membrane composition mainly through SREBP2 activation, leading to higher cholesterol content and stronger TCR signaling. Finally, ELOVL1 in CD8+ T cells correlated with αPD-1 response in melanoma patients. Altogether, Elovl1 targeting synergizes with αPD-1 to promote effective anti-tumor T cell responses

Project description:Rewiring T cell metabolism can improve intratumoral infiltration and function. By performing a CRISPR/Cas9 metabolic survey in CD8+ T cells, we identified 83 targets enriched at the primary and/or metastatic niche in the context of pancreatic cancer. We applied single-cell RNA sequencing to disclose transcriptome changes associated with each metabolic perturbation. This revealed Elongation of Very-Long-chain fatty acids protein 1 (Elovl1) as a metabolic target to sustain proliferation and both effector and memory functions in CD8+ T cells. Accordingly, Elovl1 inactivation in adoptively transferred T cells combined with αPD-1 showed therapeutic efficacy in resistant pancreatic and melanoma tumors. Loss of Elovl1 in T cells rewired lipid metabolism and changed the plasma membrane composition mainly through SREBP2 activation, leading to higher cholesterol content and stronger TCR signaling. Finally, ELOVL1 in CD8+ T cells correlated with αPD-1 response in melanoma patients. Altogether, Elovl1 targeting synergizes with αPD-1 to promote effective anti-tumor T cell responses

Project description:Rewiring T cell metabolism can improve intratumoral infiltration and function. By performing a CRISPR/Cas9 metabolic survey in CD8+ T cells, we identified 83 targets enriched at the primary and/or metastatic niche in the context of pancreatic cancer. We applied single-cell RNA sequencing to disclose transcriptome changes associated with each metabolic perturbation. This revealed Elongation of Very-Long-chain fatty acids protein 1 (Elovl1) as a metabolic target to sustain proliferation and both effector and memory functions in CD8+ T cells. Accordingly, Elovl1 inactivation in adoptively transferred T cells combined with αPD-1 showed therapeutic efficacy in resistant pancreatic and melanoma tumors. Loss of Elovl1 in T cells rewired lipid metabolism and changed the plasma membrane composition mainly through SREBP2 activation, leading to higher cholesterol content and stronger TCR signaling. Finally, ELOVL1 in CD8+ T cells correlated with αPD-1 response in melanoma patients. Altogether, Elovl1 targeting synergizes with αPD-1 to promote effective anti-tumor T cell responses

Project description:Dendritic cells (cDCs) are essential mediators of anti-tumor immunity. Cancers have developed mechanisms to render DCs dysfunctional within the tumor microenvironment. Utilizing CD63 as a unique surface marker, we demonstrate that mature regulatory DCs (mregDCs) suppress DC antigen cross-presentation while driving TH2 and regulatory T cell differentiation within tumor-draining lymph node tissues. Transcriptional and metabolic studies show that mregDC functionality is dependent upon the mevalonate biosynthetic pathway and the master transcription factor, SREBP2. Melanoma-derived lactate activates DC SREBP2 in the tumor microenvironment (TME) and drives mregDC development from conventional DCs. DC-specific genetic silencing and pharmacologic inhibition of SREBP2 promotes anti-tumor CD8+ T cell activation and suppresses melanoma progression. CD63+ mregDCs reside within the sentinel lymph nodes of melanoma patients. Collectively, this work describes a tumor-driven SREBP2-dependent program that promotes CD63+ mregDC development and function while serving as a promising therapeutic target for overcoming immune tolerance in the TME.

Project description:Dendritic cells (cDCs) are essential mediators of anti-tumor immunity. Cancers have developed mechanisms to render DCs dysfunctional within the tumor microenvironment. Utilizing CD63 as a unique surface marker, we demonstrate that mature regulatory DCs (mregDCs) suppress DC antigen cross-presentation while driving TH2 and regulatory T cell differentiation within tumor-draining lymph node tissues. Transcriptional and metabolic studies show that mregDC functionality is dependent upon the mevalonate biosynthetic pathway and the master transcription factor, SREBP2. Melanoma-derived lactate activates DC SREBP2 in the tumor microenvironment (TME) and drives mregDC development from conventional DCs. DC-specific genetic silencing and pharmacologic inhibition of SREBP2 promotes anti-tumor CD8+ T cell activation and suppresses melanoma progression. CD63+ mregDCs reside within the sentinel lymph nodes of melanoma patients. Collectively, this work describes a tumor-driven SREBP2-dependent program that promotes CD63+ mregDC development and function while serving as a promising therapeutic target for overcoming immune tolerance in the TME.

Project description:Dendritic cells (cDCs) are essential mediators of anti-tumor immunity. Cancers have developed mechanisms to render DCs dysfunctional within the tumor microenvironment. Utilizing CD63 as a unique surface marker, we demonstrate that mature regulatory DCs (mregDCs) suppress DC antigen cross-presentation while driving TH2 and regulatory T cell differentiation within tumor-draining lymph node tissues. Transcriptional and metabolic studies show that mregDC functionality is dependent upon the mevalonate biosynthetic pathway and the master transcription factor, SREBP2. Melanoma-derived lactate activates DC SREBP2 in the tumor microenvironment (TME) and drives mregDC development from conventional DCs. DC-specific genetic silencing and pharmacologic inhibition of SREBP2 promotes anti-tumor CD8+ T cell activation and suppresses melanoma progression. CD63+ mregDCs reside within the sentinel lymph nodes of melanoma patients. Collectively, this work describes a tumor-driven SREBP2-dependent program that promotes CD63+ mregDC development and function while serving as a promising therapeutic target for overcoming immune tolerance in the TME.

Project description:Dendritic cells (cDCs) are essential mediators of anti-tumor immunity. Cancers have developed mechanisms to render DCs dysfunctional within the tumor microenvironment. Utilizing CD63 as a unique surface marker, we demonstrate that mature regulatory DCs (mregDCs) suppress DC antigen cross-presentation while driving TH2 and regulatory T cell differentiation within tumor-draining lymph node tissues. Transcriptional and metabolic studies show that mregDC functionality is dependent upon the mevalonate biosynthetic pathway and the master transcription factor, SREBP2. Melanoma-derived lactate activates DC SREBP2 in the tumor microenvironment (TME) and drives mregDC development from conventional DCs. DC-specific genetic silencing and pharmacologic inhibition of SREBP2 promotes anti-tumor CD8+ T cell activation and suppresses melanoma progression. CD63+ mregDCs reside within the sentinel lymph nodes of melanoma patients. Collectively, this work describes a tumor-driven SREBP2-dependent program that promotes CD63+ mregDC development and function while serving as a promising therapeutic target for overcoming immune tolerance in the TME.

Project description:Dendritic cells (cDCs) are essential mediators of anti-tumor immunity. Cancers have developed mechanisms to render DCs dysfunctional within the tumor microenvironment. Utilizing CD63 as a unique surface marker, we demonstrate that mature regulatory DCs (mregDCs) suppress DC antigen cross-presentation while driving TH2 and regulatory T cell differentiation within tumor-draining lymph node tissues. Transcriptional and metabolic studies show that mregDC functionality is dependent upon the mevalonate biosynthetic pathway and the master transcription factor, SREBP2. Melanoma-derived lactate activates DC SREBP2 in the tumor microenvironment (TME) and drives mregDC development from conventional DCs. DC-specific genetic silencing and pharmacologic inhibition of SREBP2 promotes anti-tumor CD8+ T cell activation and suppresses melanoma progression. CD63+ mregDCs reside within the sentinel lymph nodes of melanoma patients. Collectively, this work describes a tumor-driven SREBP2-dependent program that promotes CD63+ mregDC development and function while serving as a promising therapeutic target for overcoming immune tolerance in the TME.

Project description:We have compared the transcriptome of cultured human fibroblasts from 2 patientes with a mutation in the ELOVL1 gene with the transcriptome of four healthy age-matched controls.

Project description:PARP inhibitors sensitize pancreatic ductal adenocarcinoma (PDAC) to radiation by inducing DNA damage and replication stress. These mechanisms also have the potential to enhance radiation-induced type I interferon (T1IFN) mediated anti-tumoral immune responses. We hypothesized that the PARP inhibitor olaparib would also potentiate radiation-induced T1IFN to promote anti-tumor immune responses and sensitization of otherwise resistant PDAC to immunotherapy. To test this hypothesis, we assessed the effects of olaparib and radiation on T1IFN production and sensitivity to αPD-L1 immunotherapy, as well as consequent effects on the tumor microenvironment by single-cell RNA sequencing (scRNA-seq). We found that olaparib enhanced T1IFN production following radiation and had superior therapeutic efficacy in immune competent models. Treatment with olaparib and radiation sensitized PDAC tumors to αPD-L1 resulting in decreased tumor burden and a 33% complete response rate. Combination treatment provided durable immune responses as shown by tumor rejection upon tumor rechallenge of previously cured mice. Furthermore, scRNA-seq analysis revealed that combination treatment induced an immunogenic tumor microenvironment, characterized by interferon responses in both PDAC and myeloid cell populations, macrophage polarization, and increased CD8+ terminal effector T cell frequency and activity. Furthermore, CD8+ T cells and T1IFN signaling were required for therapeutic efficacy as host depletion of CD8+ T cells or the T1IFN receptor diminished treatment responses. Taken together, our results indicate that olaparib enhances radiation-induced T1IFN-mediated immune signaling and subsequently an adaptive immune response thus sensitizing pancreatic cancer to αPD-L1 therapy, supporting an ongoing clinical trial of this therapy in patients with PDAC.