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蛋白酶体和200 kDa蛋白酶体激活剂(PA200)在受到电离辐射时会在染色质上积累。

Proteasomes and proteasome activator 200 kDa (PA200) accumulate on chromatin in response to ionizing radiation.

作者信息

Blickwedehl Jennifer, McEvoy Sarah, Wong Irene, Kousis Philaretos, Clements James, Elliott Rosemary, Cresswell Peter, Liang Ping, Bangia Naveen

机构信息

Department of Immunology, Rosewell Park Cancer Institute, Buffalo, NY 14263, USA.

出版信息

Radiat Res. 2007 Jun;167(6):663-74. doi: 10.1667/RR0690.1.

Abstract

Proteasome activator 200 kDa (PA200) forms nuclear foci after exposure of cells to ionizing radiation and enhances proteasome activity in vitro. Within cells, it is unclear whether PA200 responds to radiation alone or in association with proteasomes. In the present study, we identified three forms of cellular PA200 (termed PA200i, ii and iii) at the mRNA and protein levels. Neither PA200ii nor PA200iii appears to associate with proteasomes. All detectable PA200i is associated with proteasomes, which indicates that PA200i and proteasomes function together within the cell. Consistent with this idea, we find that exposure of cells to radiation leads to an equivalent accumulation of both PA200i and core proteasomes on chromatin. This increase in PA200 and proteasomes on chromatin is not specific to the stage of cell cycle arrest since it occurs in cells that arrest in G(2)/M and cells that arrest in G(1)/S after exposure to radiation. These data provide evidence that PA200 and proteasomes function together within cells and respond to a specific radiation-induced damage independent of the stage of cell cycle arrest.

摘要

蛋白酶体激活因子200 kDa(PA200)在细胞暴露于电离辐射后形成核灶,并在体外增强蛋白酶体活性。在细胞内,尚不清楚PA200是单独对辐射作出反应还是与蛋白酶体结合作出反应。在本研究中,我们在mRNA和蛋白质水平上鉴定出三种细胞形式的PA200(称为PA200i、ii和iii)。PA200ii和PA200iii似乎都不与蛋白酶体结合。所有可检测到的PA200i都与蛋白酶体结合,这表明PA200i和蛋白酶体在细胞内共同发挥作用。与此观点一致,我们发现细胞暴露于辐射会导致PA200i和核心蛋白酶体在染色质上等量积累。染色质上PA200和蛋白酶体的这种增加并不特定于细胞周期停滞阶段,因为它发生在暴露于辐射后停滞在G(2)/M期的细胞以及停滞在G(1)/S期的细胞中。这些数据提供了证据,表明PA200和蛋白酶体在细胞内共同发挥作用,并对特定的辐射诱导损伤作出反应,而与细胞周期停滞阶段无关。

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