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辐射敏感型消瘦小鼠中胸腺增殖细胞核抗原(PCNA)表达的调节发生改变。

Regulation of thymus PCNA expression is altered in radiation-sensitive wasted mice.

作者信息

Woloschak G E, Paunesku T, Libertin C R, Chang-Liu C M, Churchill M, Panozzo J, Grdina D, Gemmell M A, Giometti C

机构信息

Center for Mechanistic Biology and Biotechnology, Argonne National Laboratory, IL 60439-4833, USA.

出版信息

Carcinogenesis. 1996 Nov;17(11):2357-65. doi: 10.1093/carcin/17.11.2357.

Abstract

Mice bearing the autosomal recessive mutation 'wasted' (wst/wst) express a disease syndrome characterized by neurologic dysfunction, immunodeficiency, and increased sensitivity to the killing effects of ionizing radiation relative to normal littermates (wst/-) and to parental control mice (BCF1, BALB/c, and C57BL/6). Many of these abnormalities, evident as early as 21 days of age, have been localized to thymic tissues and T-lymphocyte populations. Comparison of two-dimensional gel electrophoresis patterns of proteins from wst/wst and control mouse thymus revealed that an acidic protein with a molecular mass of approximately 30 kDa was consistently expressed at lower levels in wasted mice than in controls. Microsequencing of this protein revealed a sequence of 19 N-terminal amino acids identical to the sequence of murine proliferating cell nuclear antigen (PCNA). Northern blot analyses of PCNA expression in thymus and spleen demonstrated lower accumulation of PCNA-specific transcripts in wasted mice compared with that in controls. Because PCNA expression is associated with cell cycle progression, the percentages of thymic and splenic cells in each stage of the cell cycle were examined; there were no differences in the cell stage distribution of lymphocytes freshly isolated from wasted mice compared with littermate or parental controls. After activation with concanavalin A, however, splenocytes from wst/wst mice showed a lower percentage of cells in S phase compared with that in controls. Southern blots with PCNA probes showed that the PCNA loci from the wasted mice and their normal littermates have the same restriction maps. While differences in polymerase chain reaction (PCR) priming were obtained, these could be attributed to strain-specific differences in mouse PCNA pseudogenes. These results suggest the presence of an alteration in the pathway leading to PCNA expression in radiation-sensitive tissues of wasted mice.

摘要

携带常染色体隐性突变“消瘦”(wst/wst)的小鼠表现出一种疾病综合征,其特征为神经功能障碍、免疫缺陷,且相对于正常同窝小鼠(wst/-)和亲本对照小鼠(BCF1、BALB/c和C57BL/6),对电离辐射的杀伤作用更为敏感。早在21日龄时就已显现的许多此类异常,已定位到胸腺组织和T淋巴细胞群体。对wst/wst小鼠和对照小鼠胸腺中的蛋白质进行二维凝胶电泳图谱比较,结果显示,一种分子量约为30 kDa的酸性蛋白在消瘦小鼠中的表达水平始终低于对照小鼠。对该蛋白进行微量测序后发现,其19个N端氨基酸序列与小鼠增殖细胞核抗原(PCNA)的序列相同。对胸腺和脾脏中PCNA表达进行的Northern印迹分析表明,与对照相比,消瘦小鼠中PCNA特异性转录本的积累较少。由于PCNA表达与细胞周期进程相关,因此检测了细胞周期各阶段胸腺和脾脏细胞的百分比;与同窝或亲本对照相比,从消瘦小鼠中新鲜分离出的淋巴细胞在细胞阶段分布上没有差异。然而,在用伴刀豆球蛋白A激活后,wst/wst小鼠的脾细胞处于S期的细胞百分比低于对照。用PCNA探针进行的Southern印迹显示,消瘦小鼠及其正常同窝小鼠的PCNA基因座具有相同的限制性图谱。虽然在聚合酶链反应(PCR)引物方面存在差异,但这些差异可归因于小鼠PCNA假基因中的品系特异性差异。这些结果表明,在消瘦小鼠对辐射敏感的组织中,导致PCNA表达的途径存在改变。

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