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小鼠体细胞和减数分裂细胞中DNA复制动力学及姐妹染色单体交换形成的体内BrdU-33258 Hoechst分析

In vivo BrdU-33258 Hoechst analysis of DNA replication kinetics and sister chromatid exchange formation in mouse somatic and meiotic cells.

作者信息

Allen J W, Latt S A

出版信息

Chromosoma. 1976 Nov 29;58(4):325-40. doi: 10.1007/BF00292841.

Abstract

BrdU (5-bromodeoxyuridine)-33258 Hoechst methods have been adapted for in vivo analyses of replication kinetics, sister chromatid differentiation and sister chromatid exchange (SCE) formation in mice. Sufficient in vivo BrdU substitution for cytological detection was effected with multiple intraperitoneal injections of the analogue. The combination of centromere staining asymmetry and sister chromatid differentiation at metaphase permits unambiguous determination of the number of replications in BrdU and dT (deoxythymidine) undergone by individual cells. Late-replicating regions in marrow and spermatogonial chromosomes are highlighted by bright fluorescence after sequential incorporation of BrdU followed by dT during a single DNA synthesis period. SCEs are analyzed in marrow and spermatogonial metaphases after successive complete cycles of BrdU and dT incorporation. Significant induction of SCE was observed with both mitomycin C and cyclophosphamide; the latter drug requires host-mediated activation to be effective. In meiotic metaphase cells harvested two weeks after BrdU incorporation, satellite DNA asymmetry, sister chromatid differentiation and SCE could be detected in a few chromosomes, most frequently the X and the Y.

摘要

5-溴脱氧尿苷(BrdU)-33258 Hoechst 方法已被用于小鼠体内复制动力学、姐妹染色单体分化和姐妹染色单体交换(SCE)形成的分析。通过多次腹腔注射该类似物,实现了足够的体内 BrdU 替代以进行细胞学检测。中期着丝粒染色不对称和姐妹染色单体分化的结合使得能够明确确定单个细胞经历的 BrdU 和脱氧胸苷(dT)复制次数。在单个 DNA 合成期先后掺入 BrdU 然后 dT 后,骨髓和精原细胞染色体中的晚期复制区域会被明亮的荧光突出显示。在连续完成 BrdU 和 dT 掺入的完整周期后,对骨髓和精原细胞中期的 SCE 进行分析。丝裂霉素 C 和环磷酰胺均观察到显著的 SCE 诱导;后一种药物需要宿主介导的激活才有效。在 BrdU 掺入两周后收获的减数分裂中期细胞中,在少数染色体中可以检测到卫星 DNA 不对称、姐妹染色单体分化和 SCE,最常见的是 X 染色体和 Y 染色体。

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