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粒细胞和单核细胞分化过程中DNA链断裂与ADP-核糖基化依赖性DNA连接的对比模式。

Contrasting patterns of DNA strand breakage and ADP-ribosylation-dependent DNA ligation during granulocyte and monocyte differentiation.

作者信息

Khan Z, Francis G E

出版信息

Blood. 1987 Apr;69(4):1114-9.

PMID:3030464
Abstract

Previous studies have shown that structural changes in DNA, including the ligation of pre-existing DNA breaks and the opening and closure of new breaks, occur shortly after exposure of granulomonocytic precursors (CFU-GM) to granulocyte-macrophage colony stimulating activity (GM-CSA). Monocytic differentiation of CFU-GM is selectively inhibited by compounds known to inhibit the nuclear enzyme ADP-ribosyl transferase (ADPRT). Since this enzyme, which transfers ADP-ribose units to chromatin proteins, is known to activate DNA ligase, we attempted to determine whether ligation of one or both types of DNA break is required for monocytic differentiation. Breaks in DNA were examined using the nucleoid sedimentation technique in which DNA breaks cause loss of DNA supercoiling in nucleoids and concomitant changes in their sedimentation through neutral sucrose gradients. We here report that two distinct patterns of DNA strand breakage and ligation are associated with differentiation to the granulocyte and monocyte lineages. Monocytic inducers (phorbolester and vitamin D3) predominantly produce closure of pre-existing strand breaks, whereas granulocytic inducers (granulocyte colony stimulating activity, G-CSA; retinoic acid) cause opening and closure of new breaks. Only ligation of the pre-existing breaks is highly sensitive to inhibition by 3-methoxybenzamide (a potent ADPRT inhibitor), and only monocytic differentiation is impaired by addition of this compound. These findings suggest that DNA structural changes may be directly involved in granulocyte-macrophage switching.

摘要

先前的研究表明,DNA的结构变化,包括预先存在的DNA断裂的连接以及新断裂的打开和闭合,在粒单核细胞前体(CFU-GM)暴露于粒细胞-巨噬细胞集落刺激活性(GM-CSA)后不久就会发生。CFU-GM向单核细胞的分化被已知抑制核酶ADP-核糖基转移酶(ADPRT)的化合物选择性抑制。由于这种将ADP-核糖单位转移到染色质蛋白上的酶已知可激活DNA连接酶,我们试图确定单核细胞分化是否需要一种或两种类型的DNA断裂的连接。使用核小体沉降技术检测DNA断裂,在该技术中,DNA断裂会导致核小体中DNA超螺旋的丧失以及它们通过中性蔗糖梯度沉降的伴随变化。我们在此报告,两种不同的DNA链断裂和连接模式与向粒细胞和单核细胞谱系的分化相关。单核细胞诱导剂(佛波酯和维生素D3)主要导致预先存在的链断裂的闭合,而粒细胞诱导剂(粒细胞集落刺激活性,G-CSA;视黄酸)导致新断裂的打开和闭合。只有预先存在的断裂的连接对3-甲氧基苯甲酰胺(一种有效的ADPRT抑制剂)的抑制高度敏感,并且添加这种化合物只会损害单核细胞的分化。这些发现表明DNA结构变化可能直接参与粒细胞-巨噬细胞的转换。

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