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成人慢性纯红细胞再生障碍性贫血中的红系祖细胞:体外红系集落与治疗反应的关系。

Erythroid progenitors in adult chronic pure red cell aplasia: relationship of in vitro erythroid colonies to therapeutic response.

作者信息

Lacombe C, Casadevall N, Muller O, Varet B

出版信息

Blood. 1984 Jul;64(1):71-7.

PMID:6733284
Abstract

Twenty-two cases of idiopathic chronic pure red cell aplasia (PRCA) in adults have been studied to evaluate their erythroid progenitors in vitro using the plasma clot technique. Three types of culture growth patterns were observed and classified as follows. Type I: showing a normal number of autologous CFU-E; type II: CFU-E and BFU-E were detectable but constantly decreased; type III: CFU-E and BFU-E were undetectable. The results were reproducible when patients were studied on two or more occasions. A strong correlation was found between the in vitro growth of autologous erythroid colonies and the results of immunomodulating therapy in 18 evaluable patients. A constant response to immunomodulating treatment was observed in type I patients. A constant failure of treatment was observed in type III patients, whereas results of therapy were unpredictable in type II patients. Two patients with chronic PRCA associated with thymoma and three with chronic myeloproliferative disorders were also studied. Patients with PRCA and thymoma behaved in vitro like type I patients. Patients with chronic myeloproliferative disorders exhibited very low numbers or no CFU-E or BFU-E (type II or III). These data support the hypothesis that at least two mechanisms are responsible for PRCA--one immunologically mediated and the other resulting from a stem cell defect. Moreover, they suggest that the study of erythroid progenitors in vitro might be useful in predicting the immunosuppressive therapy effect in adult chronic PRCA.

摘要

对22例成人特发性慢性纯红细胞再生障碍性贫血(PRCA)患者进行了研究,采用血浆凝块技术在体外评估其红系祖细胞。观察到三种培养生长模式,并分类如下。I型:自体CFU-E数量正常;II型:可检测到CFU-E和BFU-E,但持续减少;III型:未检测到CFU-E和BFU-E。当对患者进行两次或更多次研究时,结果具有可重复性。在18例可评估患者中,发现自体红系集落的体外生长与免疫调节治疗结果之间存在密切相关性。I型患者对免疫调节治疗有持续反应。III型患者治疗持续失败,而II型患者的治疗结果不可预测。还研究了2例合并胸腺瘤的慢性PRCA患者和3例慢性骨髓增殖性疾病患者。合并胸腺瘤的PRCA患者在体外表现类似于I型患者。慢性骨髓增殖性疾病患者的CFU-E或BFU-E数量非常低或未检测到(II型或III型)。这些数据支持以下假设,即PRCA至少由两种机制引起——一种是免疫介导的,另一种是由干细胞缺陷导致的。此外,它们表明体外红系祖细胞的研究可能有助于预测成人慢性PRCA的免疫抑制治疗效果。

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