Figure 2
Figure 2. Histopathologic and immunohistochemical characteristics of the DTG lymphomas in relation to the B-cell lymphomas in parental IL-14α TG and c-myc TG mice. (A) H&E-stained paraffin sections (original magnification, × 400). (B) Sections stained with anti-B220 (original magnification, × 400). (C) Sections stained with anti–cyclin D (original magnification, × 400). DTG tumor staining is more uniform and intense than that of the c-myc TG tumor. IL-14α TG tumor is negative. (D) Flow cytometry of tumors from IL-14α TG, c-myc TG, and DTG mice showing CD19/CD5 and CD19/sIgM staining. (E) Semiquantitative RT-PCR of C57/BL6 spleen and tumors from IL-14α TG, DTG, or c-myc TG mice analyzed for cyclin D1 and actin, as described in “Patients, materials, and methods.” (F) Immunoglobulin gene rearrangements performed on tumors from IL-14α TG, c-myc TG, and DTG mice showing monoclonality of all of these tumors, as described in “Patients, materials, and methods.”

Histopathologic and immunohistochemical characteristics of the DTG lymphomas in relation to the B-cell lymphomas in parental IL-14α TG and c-myc TG mice. (A) H&E-stained paraffin sections (original magnification, × 400). (B) Sections stained with anti-B220 (original magnification, × 400). (C) Sections stained with anti–cyclin D (original magnification, × 400). DTG tumor staining is more uniform and intense than that of the c-myc TG tumor. IL-14α TG tumor is negative. (D) Flow cytometry of tumors from IL-14α TG, c-myc TG, and DTG mice showing CD19/CD5 and CD19/sIgM staining. (E) Semiquantitative RT-PCR of C57/BL6 spleen and tumors from IL-14α TG, DTG, or c-myc TG mice analyzed for cyclin D1 and actin, as described in “Patients, materials, and methods.” (F) Immunoglobulin gene rearrangements performed on tumors from IL-14α TG, c-myc TG, and DTG mice showing monoclonality of all of these tumors, as described in “Patients, materials, and methods.”

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