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通过流式细胞术测定小鼠脾脏中的红细胞生成和微核诱导情况。

Erythropoiesis and the induction of micronuclei in mouse spleen determined by flow cytometry.

作者信息

Abramsson-Zetterberg L, Grawé J, Zetterberg G

机构信息

Department of Genetics, Uppsala University, Sweden.

出版信息

Mutat Res. 1997 Nov 27;394(1-3):17-28. doi: 10.1016/s1383-5718(97)00119-8.

Abstract

Erythrocytes from the spleen of CBA mice have been prepared for analyses by flow cytometry. About 80% of the polychromatic erythrocytes (PCE) in the spleen originate from erythropoiesis in the spleen, while the remaining 20% come from the peripheral blood. Analyses of the RNA content of PCE revealed that splenic PCE do not mature into normochromatic erythrocytes (NCE) in the spleen but leave the organ at a more immature stage. A considerable part of the PCE from bone marrow also mature into NCE in the bone marrow. The rate of RNA breakdown in PCE follows an exponential function. Time-courses for the appearance of micronucleated PCE (MPCE) from spleen and from bone marrow were determined by analysis of samples taken with short intervals after an acute dose of 0.1 Gy X-rays. The time-courses were identical for MPCE from the spleen and the bone marrow. The frequency of MPCE (fMPCE) starts to increase at about 10 h after irradiation and reaches its maximum after about another 20 h upon which fMPCE returns to control level. The first induced MPCE in peripheral blood appear at about 20 h after irradiation. The effects of the carcinogen DMBA, 9,10-dimethyl-1,2-benzanthracene, at low doses were determined in PCE from spleen and bone marrow. The sensitivity was found to be about the same for erythroblasts in the spleen and the bone marrow. Protracted exposure to gamma-irradiation at a very low dose rate (44 mGy/day) gave a similar increase of fMPCE in bone marrow and spleen. The suitability of using splenic erythrocytes in the micronucleus test is discussed.

摘要

已制备CBA小鼠脾脏中的红细胞用于流式细胞术分析。脾脏中约80%的多色红细胞(PCE)起源于脾脏中的红细胞生成,而其余20%来自外周血。对PCE的RNA含量分析表明,脾脏中的PCE在脾脏中不会成熟为正色红细胞(NCE),而是在更不成熟的阶段离开该器官。来自骨髓的相当一部分PCE也在骨髓中成熟为NCE。PCE中RNA的分解速率遵循指数函数。通过分析在急性剂量0.1 Gy X射线照射后短时间间隔采集的样本,确定了脾脏和骨髓中微核PCE(MPCE)出现的时间进程。脾脏和骨髓中MPCE的时间进程相同。MPCE的频率(fMPCE)在照射后约10小时开始增加,在大约再过20小时后达到最大值,之后fMPCE恢复到对照水平。外周血中首次诱导的MPCE在照射后约20小时出现。在脾脏和骨髓的PCE中测定了低剂量致癌物DMBA(9,10-二甲基-1,2-苯并蒽)的作用。发现脾脏和骨髓中的成红细胞敏感性大致相同。以非常低的剂量率(44 mGy/天)长期暴露于γ射线,骨髓和脾脏中的fMPCE也有类似增加。讨论了在微核试验中使用脾脏红细胞的适用性。

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