Project description:The aim of this study is to profile the distribution of the active histone modification H3K4me3 in BMDMs from WT and SLC1A5_var transgenic mice after low-dose LPS training. We compared the data of ChIP-seq performed on fragmented chromatin immunoprecipitated with anti-H3K4me3 antibody in naive and trained BMDM from both genotypes. Inter-group comparisons revealed increased differentially enriched peaks near promoters of pro-inflammatory genes of trained WT BMDMs, where as this changes were blunted in Tg BMDMs. Since SLC1A5_var function as unique mitochondrial glutamine transporter, the results indicate that altered glutaminolysis could impact epigenetic regulation under LPS-training,

Project description:The aim of this study is to evaluate the changes in the chromatin accessibility landscape of BMDMs from WT and SLC1A5_var transgenic mice after low-dose LPS training. We compared the data of ATAC-seq performed on nuclei extracted from naive and trained BMDM from both genotypes. Inter-group comparisons revealed differentially accessible regions to occur between traind WT and Tg BMDMs. Since SLC1A5_var function as unique mitochondrial glutamine transporter, the results indicate that altered glutaminolysis could impact chromatin accessbility.

Project description:Trained immunity is the heightened state of innate immune memory that enhances immune response resulting in nonspecific protection. Epigenetic changes and metabolic reprogramming are critical steps that regulate trained immunity. In this study, we reported the involvement of O6-methylguanine DNA methyltransferase (MGMT), a DNA repair enzyme of lesion induced by alkylating agents, in regulation the trained immunity induced by β-glucan (BG). Pharmacological inhibition or silencing of MGMT expression altered LPS stimulated pro-inflammatory cytokine productions in BG-trained bone marrow derived macrophages (BMMs). Targeted deletion of Mgmt in BMMs resulted in reduction of the trained responses both in vitro and in vivo models. The transcriptomic analysis revealed that the dampening trained immunity in MGMT KO BMMs is partially mediated by ATM/FXR/AMPK axis affecting the MAPK/mTOR/HIF1α pathways and the reduction in glycolysis function. Taken together, a failure to resolve a DNA damage may have consequences for innate immune memory.

Project description:Trained immunity occurs when inflammatory stimulation reprograms myeloid cells to have increased effector functions upon secondary stimulation. Interestingly, the secondary stimulation can occur well beyond the lifetime of an individual myeloid cell, thus memory of immune training must reside in the hematopoietic system. After showing that long-term hematopoietic stem cells (HSCLT) from mice treated with pristane for eight weeks generate trained macrophages, we sought to uncover mechanisms underlying the heritable trained immunity program in myeloid cells. To do this we transplanted HSCLT from pristane mice into congenic recipients, and after 18 weeks of engraftment we generated bone marrow derived macrophages (BMDMs) in vitro. We then analyzed the chromatin landscape and transcriptome using low input chromatin accessibility and transcriptomics sequencing (LiCAT-seq) which allows for the co-generation of RNA-seq and ATAC-seq libraries from the same cellular pool. With this approach we found a unique epigenetic phenotype of reduced chromatin accessibility at metabolic genes in BMDMs from pristane HSCLT, which resulted in reduced transcription of metabolic genes, leading to reduced metabolism in BMDMs.

Project description:Trained immunity occurs when inflammatory stimulation reprograms myeloid cells to have increased effector functions upon secondary stimulation. Interestingly, the secondary stimulation can occur well beyond the lifetime of an individual myeloid cell, thus memory of immune training must reside in the hematopoietic system. After showing that long-term hematopoietic stem cells (HSCLT) from mice treated with pristane for eight weeks generate trained macrophages, we sought to uncover mechanisms underlying the heritable trained immunity program in myeloid cells. To do this we transplanted HSCLT from pristane mice into congenic recipients, and after 18 weeks of engraftment we generated bone marrow derived macrophages (BMDMs) in vitro. We then analyzed the chromatin landscape and transcriptome using low input chromatin accessibility and transcriptomics sequencing (LiCAT-seq) which allows for the co-generation of RNA-seq and ATAC-seq libraries from the same cellular pool. With this approach we found a unique epigenetic phenotype of reduced chromatin accessibility at metabolic genes in BMDMs from pristane HSCLT, which resulted in reduced transcription of metabolic genes, leading to reduced metabolism in BMDMs.

Project description:Trained immunity is defined by increased inflammatory cytokine production by macrophages that are sequentially activated by two stimuli, separated by a resting period. The models used to study trained immunity should reflect the definition of this process, which includes five different steps. Here, we developed an in vitro methodology to study trained immunity using murine bone marrow-derived macrophages (BMDM), following sequential stimulation with β-glucan and lipopolysaccharide (LPS). Kinetic analysis of cytokine production demonstrated, for the first time, that trained BMDM secrete high levels of tumor necrosis factor (TNF) and interleukin 6 (IL6) following stimulation with β-glucan (stimulus 1), compared to unstimulated BMDM (step 1). After a resting period, trained BMDM do not secrete significant levels of these cytokines (step 2), but rapidly produce enhanced levels of TNF and IL6 after secondary stimulation with LPS (stimulus 2), compared to BMDM stimulated with either β-glucan (step 3) or LPS (step 4) alone. In addition, the sum of cytokine levels produced by both BMDM stimulated with either β-glucan (stimulus 1) or LPS (stimulus 2) individually, was significantly lower than the cytokine levels produced by trained BMDM stimulated with both β-glucan and LPS (stimulus 1+2) (step 5). Our findings also demonstrate that trained BMDM produce higher levels of serum amyloid A3 (SAA3) protein due to metabolic and epigenetic reprogramming. Functionally, trained BMDM upregulate the expression of stimulatory molecules such as MHC-II, CD80, CD86, OX40L and PDL1; downregulate the inhibitory molecules ICOSL and CD206; and induce CD4+ and CD8+ T cell proliferation in vitro through a cell contact-dependent mechanism. Our results also revealed strain-specific differences in the training response among mice, the negative impact of cell cryopreservation on trained immunity, and the potential use of genetically modified mice in elucidating mechanistic pathways through which different training stimuli may induce long-lived memory macrophages. These results also highlight the applicability of mouse in vitro methods as an additional tool to study trained immunity, as the use of inbred mice reduce the genetic variability present in humans and minimize variables that affect trained immunity such as infections, vaccinations and lifestyle-related stimuli. The standardization of trained immunity protocols using murine BMDM will facilitate the development of therapeutic strategies that target the innate immune memory response for the treatment of multiple immune-based diseases.

Project description:Trained immunity is defined by increased inflammatory cytokine production by macrophages that are sequentially activated by two stimuli, separated by a resting period. The models used to study trained immunity should reflect the definition of this process, which includes five different steps. Here, we developed an in vitro methodology to study trained immunity using murine bone marrow-derived macrophages (BMDM), following sequential stimulation with β-glucan and lipopolysaccharide (LPS). Kinetic analysis of cytokine production demonstrated, for the first time, that trained BMDM secrete high levels of tumor necrosis factor (TNF) and interleukin 6 (IL6) following stimulation with β-glucan (stimulus 1), compared to unstimulated BMDM (step 1). After a resting period, trained BMDM do not secrete significant levels of these cytokines (step 2), but rapidly produce enhanced levels of TNF and IL6 after secondary stimulation with LPS (stimulus 2), compared to BMDM stimulated with either β-glucan (step 3) or LPS (step 4) alone. In addition, the sum of cytokine levels produced by both BMDM stimulated with either β-glucan (stimulus 1) or LPS (stimulus 2) individually, was significantly lower than the cytokine levels produced by trained BMDM stimulated with both β-glucan and LPS (stimulus 1+2) (step 5). Our findings also demonstrate that trained BMDM produce higher levels of serum amyloid A3 (SAA3) protein due to metabolic and epigenetic reprogramming. Functionally, trained BMDM upregulate the expression of stimulatory molecules such as MHC-II, CD80, CD86, OX40L and PDL1; downregulate the inhibitory molecules ICOSL and CD206; and induce CD4+ and CD8+ T cell proliferation in vitro through a cell contact-dependent mechanism. Our results also revealed strain-specific differences in the training response among mice, the negative impact of cell cryopreservation on trained immunity, and the potential use of genetically modified mice in elucidating mechanistic pathways through which different training stimuli may induce long-lived memory macrophages. These results also highlight the applicability of mouse in vitro methods as an additional tool to study trained immunity, as the use of inbred mice reduce the genetic variability present in humans and minimize variables that affect trained immunity such as infections, vaccinations and lifestyle-related stimuli. The standardization of trained immunity protocols using murine BMDM will facilitate the development of therapeutic strategies that target the innate immune memory response for the treatment of multiple immune-based diseases.

Project description:Trained immunity is the long-term functional reprogramming of innate immune cells, which results in altered responses toward a secondary challenge. Despite indoxyl sulfate (IS) being a potent stimulus associated with chronic kidney disease (CKD)-related inflammation, its impact on trained immunity has not been explored. Here, we demonstrate that IS induces trained immunity in monocytes via epigenetic and metabolic reprogramming, resulting in augmented cytokine production. Mechanistically, the aryl hydrocarbon receptor (AhR) contributes to IS-trained immunity by enhancing the expression of arachidonic acid (AA) metabolism-related genes such as Arachidonate 5-Lipoxygenase (ALOX5) and ALOX5 Activating Protein (ALOX5AP). Inhibition of AhR during IS training suppresses the induction of IS-trained immunity. Monocytes from end-stage renal disease (ESRD) patients have increased ALOX5 expression and after 6-day training, they exhibit enhanced TNF-α and IL-6 production to LPS. Furthermore, healthy control-derived monocytes trained with uremic sera from ESRD patients exhibit increased production of TNF-α and IL-6. Consistently, IS-trained mice and their splenic myeloid cells had increased production of TNF-α after in vivo and ex vivo LPS stimulation compared to that of control mice. These results provide insight into the role of IS in the induction of trained immunity, which is critical during inflammatory immune responses in CKD patients.

Project description:Trained immunity is the long-term functional reprogramming of innate immune cells, which results in altered responses toward a secondary challenge. Despite indoxyl sulfate (IS) being a potent stimulus associated with chronic kidney disease (CKD)-related inflammation, its impact on trained immunity has not been explored. Here, we demonstrate that IS induces trained immunity in monocytes via epigenetic and metabolic reprogramming, resulting in augmented cytokine production. Mechanistically, the aryl hydrocarbon receptor (AhR) contributes to IS-trained immunity by enhancing the expression of arachidonic acid (AA) metabolism-related genes such as Arachidonate 5-Lipoxygenase (ALOX5) and ALOX5 Activating Protein (ALOX5AP). Inhibition of AhR during IS training suppresses the induction of IS-trained immunity. Monocytes from end-stage renal disease (ESRD) patients have increased ALOX5 expression and after 6-day training, they exhibit enhanced TNF-α and IL-6 production to LPS. Furthermore, healthy control-derived monocytes trained with uremic sera from ESRD patients exhibit increased production of TNF-α and IL-6. Consistently, IS-trained mice and their splenic myeloid cells had increased production of TNF-α after in vivo and ex vivo LPS stimulation compared to that of control mice. These results provide insight into the role of IS in the induction of trained immunity, which is critical during inflammatory immune responses in CKD patients.

Project description:Trained immunity occurs when inflammatory stimulation reprograms myeloid cells to have increased effector functions upon secondary stimulation. We found that autoimmune inflammation indiced trained immunity in bone marrow derived macrophages (BMDMs) in mice treated with pristane for eight weeks. We then analyzed the chromatin landscape and transcriptome using low input chromatin accessibility and transcriptomics sequencing (LiCAT-seq) which allows for the co-generation of RNA-seq and ATAC-seq libraries from the same cellular pool. With this approach we found that BMDMs had increased chromatin accessibility at metabolic genes and inflammatory related genes in BMDMs from pristane treated mice, which resulted in increased transcription of metabolic and inflammatory genes, leading to enhanced metabolism and inflammatory functions in BMDMs.