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多胺生物合成在小鼠造血前体细胞增殖中的作用。

The role of polyamine biosynthesis in hematopoietic precursor cell proliferation in mice.

作者信息

Niskanen E, Kallio A, McCann P P, Baker D G

出版信息

Blood. 1983 Apr;61(4):740-5.

PMID:6831037
Abstract

Under the influence of a selective irreversible inhibitor of ornithine decarboxylase (ODC), DL-alpha-difluoromethylornithine (DFMO), early hematopoiesis was enhanced. In the bone marrow, the absolute number of cells that give rise to spleen colonies in lethally irradiated mice (CFU-S), granulocytic colonies in diffusion chambers in mice (CFU-DG), and granulocyte-monocyte colonies in agar in vitro (CFU-C) was increased 2-4 fold. This could be abrogated by administration of putrescine, confirming the association of the stimulatory effect with polyamine biosynthesis most likely via depression of ornithine decarboxylase activity and subsequent synthesis of putrescine. Analysis of cell cycle characteristics by 3H-TdR suicide technique demonstrated that the proportion of CFU-S, CFU-DG, and CFU-C in S-phase was significantly increased. Additionally, the stimulatory effect was reflected by enhanced colony formation in diffusion chambers implanted intraperitoneally in mice receiving DFMO. This could also be eliminated by treatment of the host animal with putrescine, again suggesting that polyamine biosynthesis plays an important role at the early stages of hematopoiesis in vivo. Effect of DFMO on colony formation in vitro (CFU-C) was inhibitory and not reversible with putrescine. It could be partially eliminated by aminoguanidine, which neutralizes diamine oxidase present in fetal calf serum used in the CFU-C assay. These data suggest that the effect of DFMO in vitro was nonspecific.

摘要

在鸟氨酸脱羧酶(ODC)的选择性不可逆抑制剂DL-α-二氟甲基鸟氨酸(DFMO)的影响下,早期造血功能得到增强。在骨髓中,在致死性照射小鼠中产生脾集落的细胞(CFU-S)、在小鼠扩散盒中产生粒细胞集落的细胞(CFU-DG)以及在体外琼脂中产生粒细胞-单核细胞集落的细胞(CFU-C)的绝对数量增加了2至4倍。给予腐胺可消除这种现象,这证实了刺激作用与多胺生物合成相关,很可能是通过抑制鸟氨酸脱羧酶活性以及随后腐胺的合成来实现的。通过3H-TdR自杀技术分析细胞周期特征表明,S期的CFU-S、CFU-DG和CFU-C的比例显著增加。此外,在接受DFMO的小鼠腹腔内植入的扩散盒中集落形成增强,这反映了刺激作用。用腐胺处理宿主动物也可消除这种现象,这再次表明多胺生物合成在体内造血的早期阶段起重要作用。DFMO对体外集落形成(CFU-C)的作用具有抑制性,且用腐胺处理后不可逆。用氨基胍可部分消除这种作用,氨基胍可中和CFU-C测定中所用胎牛血清中存在的二胺氧化酶。这些数据表明DFMO在体外的作用是非特异性的。

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