Figure 2.
Suv39h DKO results in thymic involution, selective loss of CD8+ T cells, myeloid skewing, and increased frequency of memory cells. (A) Frequencies of CD4+, CD8+, double negative (DN), and DP thymocytes from the thymus of Suv39h1 and h2 DKO and control bone marrow chimeras. (B) Representative images of the dissected thymus from WT, Suv39h1-deficient (h1KO), Suv39h2-deficient (h2KO), and DKO donor bone marrow chimeras. (C) Total thymocyte numbers obtained from mechanical homogenization and red-cell lysis of thymus tissue from donor cells of different genotypes. (D) Representative flow cytometry plots of T cells (PI−CD45.2+TCRβ+) from peripheral lymph nodes of DKO and control bone marrow chimeras. (E) Splenic frequencies of CD8+, CD4+ T cells, and B cells (CD19+) from bone marrow chimeras of different genotype donor cells. (F) Splenic frequencies of myeloid cells from bone marrow chimeras of different genotype donor cells. Total myeloid cells (CD11b+CD11c−), neutrophils (CD11b+Ly6g+Ly6cmid), eosinophils (CD11b+SiglecF+SSChi), inflammatory monocytes/macrophages (CD11b+Ly6g−Ly6cHi), and resident monocytes/macrophages (CD11b+Ly6g−Ly6cLo) are shown. Frequencies of naive (CD62L+CD44−), central memory (CD62L+CD44+), and effector memory (CD62L−CD44+) CD8+ T cells from the (G) peripheral lymph nodes and (H) spleens of different donor genotypes. Data in panels C, E, F, and H are depicted as individual data points together with mean and SEM and were statistically analyzed by 1-way ANOVA with Sidak multiple comparisons test comparing each genotype with relevant control.

Suv39h DKO results in thymic involution, selective loss of CD8+ T cells, myeloid skewing, and increased frequency of memory cells. (A) Frequencies of CD4+, CD8+, double negative (DN), and DP thymocytes from the thymus of Suv39h1 and h2 DKO and control bone marrow chimeras. (B) Representative images of the dissected thymus from WT, Suv39h1-deficient (h1KO), Suv39h2-deficient (h2KO), and DKO donor bone marrow chimeras. (C) Total thymocyte numbers obtained from mechanical homogenization and red-cell lysis of thymus tissue from donor cells of different genotypes. (D) Representative flow cytometry plots of T cells (PICD45.2+TCRβ+) from peripheral lymph nodes of DKO and control bone marrow chimeras. (E) Splenic frequencies of CD8+, CD4+ T cells, and B cells (CD19+) from bone marrow chimeras of different genotype donor cells. (F) Splenic frequencies of myeloid cells from bone marrow chimeras of different genotype donor cells. Total myeloid cells (CD11b+CD11c), neutrophils (CD11b+Ly6g+Ly6cmid), eosinophils (CD11b+SiglecF+SSChi), inflammatory monocytes/macrophages (CD11b+Ly6gLy6cHi), and resident monocytes/macrophages (CD11b+Ly6gLy6cLo) are shown. Frequencies of naive (CD62L+CD44), central memory (CD62L+CD44+), and effector memory (CD62LCD44+) CD8+ T cells from the (G) peripheral lymph nodes and (H) spleens of different donor genotypes. Data in panels C, E, F, and H are depicted as individual data points together with mean and SEM and were statistically analyzed by 1-way ANOVA with Sidak multiple comparisons test comparing each genotype with relevant control.

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