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一种抑制性内肽对正常和白血病人类白细胞的体外增殖控制

In vitro proliferation of normal and leukaemic human leukocytes controlled by an inhibitory endopeptide.

作者信息

Balázs A, Mann J, Takácsi-Nagy L, Zimonyi I, Molnár A, Klupp T

出版信息

Folia Haematol Int Mag Klin Morphol Blutforsch. 1983;110(1):24-31.

PMID:6192050
Abstract

GI-3, an endogenous inhibitory fraction isolated from leukocytes, selectively inhibits the proliferation of granuloid precursor cells in a non-toxic manner. Its active principle was determined as an acidic chlor-tolidine positive decapeptide [ 3 ]. The in vitro effect on normal and acute leukaemic human bone marrow and blood cells was examined. A dose dependent inhibition by GI-3 of 3H-TdR incorporation into myeloid cells of normal bone marrow was found, the sensitivity of human cells being higher than that of rat cells. The proliferation of the target leukaemic bone marrow and blood cells (AML, AMMoL) was also decreased by the endogenous inhibitor in a dose dependent manner in untreated subjects as well as in patients in remission or relapse. The rate of inhibition of leukaemic of well-known cytostatics (adriamycin hydrochloride, dianhydrogalactitol) applied for comparison. Beyond its direct cytostatic effect, GI-3 could be used in the differential diagnosis of blastic leukaemias, complementing the routine cytochemical methods.

摘要

GI-3是一种从白细胞中分离出的内源性抑制成分,它能以无毒方式选择性抑制粒细胞前体细胞的增殖。其活性成分被确定为一种酸性氯甲苯胺阳性十肽[3]。研究了其对正常和急性白血病患者的人骨髓及血细胞的体外作用。发现GI-3对3H-胸苷掺入正常骨髓髓细胞有剂量依赖性抑制作用,人细胞的敏感性高于大鼠细胞。在未经治疗的受试者以及缓解期或复发期患者中,内源性抑制剂也以剂量依赖性方式降低了目标白血病骨髓和血细胞(急性髓细胞白血病、急性单核细胞白血病)的增殖。还比较了知名细胞抑制剂(盐酸阿霉素、双脱水半乳糖醇)对白血病的抑制率。除了直接的细胞抑制作用外,GI-3可用于原始细胞白血病的鉴别诊断,作为常规细胞化学方法的补充。

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