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Small lymphocytic lymphoma during the course of pure red cell aplasia

机译:纯红细胞血清淋巴细胞淋巴瘤纯红细胞APLASIA

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A 29-year-old woman was diagnosed as having pure red cell aplasia (PRCA) in 1983. Her serum and IgG inhibited erythroid colony formation of bone marrow cells from a normal individual, suggesting antibody-mediated suppression of erythropoiesis. She was first successfully treated with corticosteroids, azathiopurine and cyclophosphamide. However, she relapsed in 1995 and her anemia became refractory to immunosuppressive therapy. In 1998, she developed systemic lymph node enlargement and was diagnosed as having B-cell small lymphocytic lymphoma. Combination chemotherapy resulted in regression of the lesion, but failed to improve the anemia. In this patient's case, we can speculate that B cells producing autoantibodies against erythroid cells have undergone transformation, or alternatively that the immunosuppressive state caused by the PRCA therapy promoted generation of a neoplastic B cell clone.
机译:1983年,一名29岁的女性被诊断为具有纯红细胞Aplasia(PRCA)。她的血清和IgG从正常个体中抑制了骨髓细胞的红细胞菌落形成,表明抗体介导的促进促进的促红细胞抑制。 她首先成功地用皮质类固醇,Azathiopuline和环磷酰胺治疗。 然而,她于1995年复发,她的贫血成为免疫抑制治疗的难治性。 1998年,她开发了系统性淋巴结扩大,被诊断为具有B细胞小淋巴细胞淋巴瘤。 组合化疗导致病变的回归,但未能改善贫血。 在该患者的情况下,我们可以推测产生针对红细胞细胞的自身抗体的B细胞经过转化,或者可选地,由PRCA治疗引起的免疫抑制状态促进产生肿瘤B细胞克隆。

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