Project description:The CCAAT/enhancer-binding proteins (CEBPs) are transcription factors involved in hematopoietic cell development and induction of several inflammatory mediators. Here, we generated CEBP-beta (CEBPB) and CEBP-epsilon (CEBPE) double-knockout (bbee) mice and compared their phenotypes to those of single-deficient (bbEE and BBee) and wild-type (BBEE) mice. The bbee mice were highly susceptible to fatal infections and died within 2-3 months. Morphologically, their neutrophils were blocked at the myelocytes/metamyelocytes stage, and clonogenic assays of bone marrow cells indicated a significant decrease in the number of myeloid colonies of the bbee mice. In addition, the proportion of hematopoietic progenitor cells [Lin(-)Sca1(+)c-Kit(+)] in the bone marrow of the bbee mice was significantly increased, reflecting the defective differentiation of the myeloid compartment. Furthermore, microarray expression analysis of lipopolysaccharide (LPS)- and interferon-gamma (IFN-gamma)-activated bone marrow-derived macrophages from bbee compared to single knockout mice revealed decreased expression of essential immune response-related genes and networks, including some direct CEBP targets such as Marco and Clec4e. Overall, the phenotype of the bbee mice is distinct from either the bbEE or BBee mice, demonstrating that both transcription factors are crucial for the maturation of neutrophils and macrophages, as well as the innate immune system, and can at least in part compensate for each other in the single knockout mice. To rule out the regulatory influence of both CEBPB and CEBPE on macrophage-related genes, expression analysis of bone marrow-derived macrophages was performed. Macrophages were derived from murine bone marrow with the use of murine M-CSF. The macrophages were stimulated with both LPS (100 ng) and IFN-gamma (100 ng) for 24h, and RNA was extracted for array analysis. Overall, RNA was extracted from stimulated macrophages of one WT mouse, one CEBPB-KO mouse, one CEBPE-KO mouse and one double-KO mouse.

Project description:We aimed to investigate the effect of CD40L on neutrophil development by comparing the transcription profile of wild-type and knockout mice. Thus, we performed RNA-sequencing of bone marrow neutrophils from wild-type mice (C57BL/6) and CD40LG knockout mice.

Project description:Proteome comparison between bone-marrow cells isolated from wildtype and NUDT2 knockout mice.

Project description:RNA-seq of bone marrow neutrophils from wild-type mice (C57BL/6) and CD40LG knockout mice.

Project description:RNA expression in Srf wildtype and knockout primary bone marrow derived mature neutrophils was determined via RNA sequencing Mature Gr1 high, 7/4 high, SSC high neutrophils were sorted from Srf WT and KO mouse bone marrow and submitted for RNA sequencing

Project description:We analyzed the effect of Calr deficiency on Mac1 and Gr1 positive bone marrow cells using hematopoietic cell specific Calr knockout (Mx-cre;Calrf/-) mice and control (Mx-cre;Calr+/+) mice.

Project description:Matrix remodeling associated 7 (Mxra7) belongs to the matrix remodeling-related gene family and is implicated in inflammatory neovascularization, liver injury, and autoimmune skin diseases. To elucidate the composition and transcriptional changes of bone marrow cells in Mxra7 knockout mice, we conducted single-cell RNA sequencing (scRNA-seq) in two-month-old and two-year-old mice. Our investigation revealed that Mxra7 knockout influences early B cell development and normal cell cycle functioning, impacting processes such as chromosome segregation and cell mitosis. Additionally, bone marrow B cells from knockout mice exhibited heightened differentiation potential compared to wild-type counterparts in aged mice. Mxra7 knockout initially suppressed basophil development at two months of age, only to yield an increased basophil proportation in two-year-old mice. Moreover, knockout mice exhibited elevated basophil numbers within bone marrow granulocytes. Kyoto Encyclopedia of Genes and Genomes (KEGG) enrichment analysis indicated alterations in neurological disease-related functions in Mxra7 knockout bone marrow granulocytes. Cell communication analysis highlighted heightened quantity and quality of cellular interactions within bone marrow cells of knockout mice, notably enriching three inflammation-regulating signaling pathways. These findings underscore the pivotal role of Mxra7 in bone marrow immune cell development, with age-dependent effects on immune and inflammatory responses.

Project description:RNA expression in Srf wildtype and knockout primary bone marrow derived mature neutrophils was determined via RNA sequencing

Project description:Murine neutrophils derived from bone marrow of wild-type and cPLA2alpha-knockin mice (with the C1P interaction site of cPLA2alpha ablated) proteomes were compared

Project description:Gene expression profiling for mouse N1 and N2 neutrophils. Neutrphils were isolated form the bone marrow of C57BL/6J mice between 12-16 weeks old. Approximately 8x10^7 neutrophils were used per condition and were split into 3 biological replicates. Freshly isolated neutrophils were cultured for 2h in RPMI medium, in the presence of 100 ng/ml lipopolysaccharide (LPS) and 20 ng/ml interferon gamma (IFNγ) or 20 ng/ml interleukin 4 (IL-4). Total RNA was isolated with TRIzol reagent and Phasemaker tubes. A sample from the LPS+IFNγ polarization did not pass the quality control test and was excluded from the downstream analysis.