臨床血液
Online ISSN : 1882-0824
Print ISSN : 0485-1439
ISSN-L : 0485-1439
臨床研究
慢性骨髄性白血病の慢性期延長の試み
—ブスルファンによる末梢白血球数正常域内維持療法—
松尾 辰樹朝長 万左男栗山 一孝陣内 逸郎重橋 亨野中 博章河野 友子塚崎 邦弘跡上 直糸山 貴浩前田 隆浩笹川 一平森内 幸美早田 央中村 秀男鳥谷 和洋樅田 三郎尼崎 辰彦八尾 栄一親川 幸信雨森 龍彦吉田 善春山田 恭暉田川 真須子池田 柊一上平 憲貞森 直樹市丸 道人
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1989 年 30 巻 5 号 p. 625-630

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To prolong the survival of patients with chronic myeloid leukemia (CML), 19 patients were treated with busulfan to keep their leukocyte counts within normal range by controlling bone marrow hyperplasia. The duration of chronic phase in these patients was significantly longer than that in historical controls who were treated conventionally with busulfan. This prolongation was not ascribable to the difference in such prognostic factors between the two therapy groups as splenomegaly, leukocyte count and percentage of peripheral blasts. There was a significant difference again in the duration of chronic phase between the two therapy group even when restricted to each 11 patients with intermediate relative risk (0.7∼1.5) according to Sokal et al. Four patients showed thrombocytopenia less than 5×104l, but all these patients recovered within 4 months and there was no further critical side effect except subcutaneous bleeding. This study suggests that maintenance of leukocyte count within normal range and suppression of granuloid hyperplasia in bone marrow with busulfan may prolong chronic phase of CML. Probability of clonal evolution may be decreased by reducing the total leukemic cell mass and suppressing cellular turnover of primitive CML stem cells. Another possibility is that prolongation of chronic phase might be dependent on the appearance of normal karyotype clone after long-term bone marrow suppression just like after intensive chemotherapy or α-interferon therapy.

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© 1989 日本臨床血液学会
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