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腔面祖细胞和成熟细胞比基底细胞更容易受到辐射诱导的大鼠乳腺组织中 DNA 双链断裂的影响。

Luminal progenitor and mature cells are more susceptible than basal cells to radiation-induced DNA double-strand breaks in rat mammary tissue.

机构信息

Department of Radiation Effects Research, Institute for Radiological Science, National Institutes for Quantum Science and Technology, 4-9-1 Anagawa, Inage-ku, Chiba 263-8555, Japan.

Department of Electrical Engineering and Information Science, Faculty of Electrical Engineering and Information Science, National Institute of Technology Kure College, 2-2-11 Aga-minami, Kure, Hiroshima 737-8506, Japan.

出版信息

J Radiat Res. 2024 Sep 24;65(5):640-650. doi: 10.1093/jrr/rrae067.

Abstract

Ionizing radiation promotes mammary carcinogenesis. Induction of DNA double-strand breaks (DSBs) is the initial event after radiation exposure, which can potentially lead to carcinogenesis, but the dynamics of DSB induction and repair are not well understood at the tissue level. In this study, we used female rats, which have been recognized as a useful experimental model for studying radiation effects on the mammary gland. We focused on differences in DSB kinetics among basal cells, luminal progenitor and mature cells in different parts of the mammary duct. 53BP1 foci were used as surrogate markers of DSBs, and 53BP1 foci in each mammary epithelial cell in immunostained tissue sections were counted 1-24 h after irradiation and fitted to an exponential function of time. Basal cells were identified as cytokeratin (CK) 14+ cells, luminal progenitor cells as CK8 + 18low cells and luminal mature cells as CK8 + 18high cells. The number of DSBs per nucleus tended to be higher in luminal cells than basal cells at 1 h post-irradiation. A model analysis indicated that basal cells in terminal end buds (TEBs), which constitute the leading edge of the mammary duct, had significantly fewer initial DSBs than the two types of luminal cells, and there was no significant difference in initial amount among the cell types in the subtending duct. The repair rate did not differ among mammary epithelial cell types or their locations. Thus, luminal progenitor and mature cells are more susceptible to radiation-induced DSBs than are basal cells in TEBs.

摘要

电离辐射促进乳腺癌发生。DNA 双链断裂 (DSB) 的诱导是辐射暴露后的初始事件,它可能导致癌变,但在组织水平上,DSB 的诱导和修复动力学还不清楚。在这项研究中,我们使用了雌性大鼠,它们已被认为是研究辐射对乳腺影响的有用实验模型。我们专注于乳腺导管不同部位的基底细胞、腔前体细胞和成熟细胞之间 DSB 动力学的差异。53BP1 焦点被用作 DSB 的替代标志物,在照射后 1-24 小时,用免疫组织化学染色的组织切片中每个乳腺上皮细胞的 53BP1 焦点进行计数,并拟合到时间的指数函数。基底细胞被鉴定为细胞角蛋白 (CK) 14+细胞,腔前体细胞为 CK8+18low 细胞,腔成熟细胞为 CK8+18high 细胞。照射后 1 小时,细胞核内 DSB 的数量在腔细胞中比基底细胞更倾向于更高。模型分析表明,构成乳腺导管前缘的终末芽(TEB)中的基底细胞初始 DSB 的数量明显少于两种腔细胞,而在附属导管中,细胞类型之间的初始数量没有显著差异。修复率在乳腺上皮细胞类型或其位置之间没有差异。因此,与 TEB 中的基底细胞相比,腔前体细胞和成熟细胞对辐射诱导的 DSB 更敏感。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a335/11420845/6430196ec08b/rrae067f1.jpg

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