Bone marrow studies including morphological,morphometrical and ultrastructural aspects were performed in 35 patients with M2/t(8;21)and and 23 patients with M2/NN.It was found that M2/t(8;21)patients had higher cellul...Bone marrow studies including morphological,morphometrical and ultrastructural aspects were performed in 35 patients with M2/t(8;21)and and 23 patients with M2/NN.It was found that M2/t(8;21)patients had higher cellularity in bone marrow.Type(Ⅱ)myeloblast cells were predominant among myeoloblasts.Deformation of nuclei,nucleocytoplasmic asynchronism and dysmegakaryctytopoiesis were more evident n M2/t (8;21) than in M2/NN patients.展开更多
Granulocytic sarcoma is a form of acute myeloid leukemia which may occur in any anatomical site. Isolated pancreatic granulocytic sarcoma is however, extremely rare. Translocation t(8;21) is the most common cytogeneti...Granulocytic sarcoma is a form of acute myeloid leukemia which may occur in any anatomical site. Isolated pancreatic granulocytic sarcoma is however, extremely rare. Translocation t(8;21) is the most common cytogenetic abnormality found in leukemia patients with granulocytic sarcoma and is associated with a relatively good prognosis when treated with chemotherapy. Variants of the t(8;21) are uncommon and account for approximately 3% to 4% of acute myeloid leukemia associated with t(8;21) and are rarely described in acute myeloid leukemia cases associated with granulocytic sarcoma. We report here a patient with acute myeloid leukemia and a novel variant t(8;9;21)(q22;p24;q22) with suspected granulocytic sarcoma in pancreas. A dual-color fluorescence in situ hybridization analysis with RUNX1T1 and RUNX1 probes, revealed the presence of an RUNX1/RUNX1T1 fusion signal in this translocation. To the best of our knowledge, a variant of t(8;21) in GS was rarely described and the involvement of the 9q22 region is the first time described here even in isolated AML-M2. We conclude that further accumulation of similar cases is needed and that genetic exploring of variants of t(8;21) may be helpful for a better understanding of molecular pathogenetic mechanism.展开更多
文摘Bone marrow studies including morphological,morphometrical and ultrastructural aspects were performed in 35 patients with M2/t(8;21)and and 23 patients with M2/NN.It was found that M2/t(8;21)patients had higher cellularity in bone marrow.Type(Ⅱ)myeloblast cells were predominant among myeoloblasts.Deformation of nuclei,nucleocytoplasmic asynchronism and dysmegakaryctytopoiesis were more evident n M2/t (8;21) than in M2/NN patients.
文摘Granulocytic sarcoma is a form of acute myeloid leukemia which may occur in any anatomical site. Isolated pancreatic granulocytic sarcoma is however, extremely rare. Translocation t(8;21) is the most common cytogenetic abnormality found in leukemia patients with granulocytic sarcoma and is associated with a relatively good prognosis when treated with chemotherapy. Variants of the t(8;21) are uncommon and account for approximately 3% to 4% of acute myeloid leukemia associated with t(8;21) and are rarely described in acute myeloid leukemia cases associated with granulocytic sarcoma. We report here a patient with acute myeloid leukemia and a novel variant t(8;9;21)(q22;p24;q22) with suspected granulocytic sarcoma in pancreas. A dual-color fluorescence in situ hybridization analysis with RUNX1T1 and RUNX1 probes, revealed the presence of an RUNX1/RUNX1T1 fusion signal in this translocation. To the best of our knowledge, a variant of t(8;21) in GS was rarely described and the involvement of the 9q22 region is the first time described here even in isolated AML-M2. We conclude that further accumulation of similar cases is needed and that genetic exploring of variants of t(8;21) may be helpful for a better understanding of molecular pathogenetic mechanism.
