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血清诱导的小鼠细胞体外染色体损伤及肿瘤转化

Serum-induced chromosome damage and neoplastic transformation of mouse cells in vitro.

作者信息

Sanford K K, Parshad R, Handleman S L, Price F M, Gantt R R, Evans V J

出版信息

In Vitro. 1979 Jul;15(7):488-96. doi: 10.1007/BF02618150.

Abstract

In previous studies, mouse cells grown in medium supplemented with horse serum (HS) developed more chromosomal aberrations and underwent malignant transformation earlier than cells from the same pool grown with fetal bovine serum (FBS) supplement. In the present study cells derived from C3Hf/HeN mouse embryos were grown in medium NCTC-135 supplemented with various combinations of large- and small-molecule fractions of HS and FBS in an effort to determine the effective components. The results indicate that the large-molecule fraction of HS (mare or stallion) produces alterations in chromosome number and structure. HS is also shown to cause chromatid breaks and exchanges at or near the centromere in contrast to fluorescent-light-induced breaks and exchange at or near the centromere in contrast to fluorescent-light-induced breaks which occur randomly along the chromatid. However, efforts to control completely chromosome stability and malignant transformation through the use of large- and small-molecule fractions of HS and FBS or combinations thereof were unsuccessful. In connection with this study, diagnosis of malignant transformation in vitro was made by a direct sampling method based on cytologic criteria previously described and documented. With one exception, the diagnoses of 11 different cell lines were consistent with results of in vivo assays.

摘要

在先前的研究中,在添加马血清(HS)的培养基中培养的小鼠细胞比在添加胎牛血清(FBS)的相同细胞库中培养的细胞出现更多的染色体畸变,并且更早地发生恶性转化。在本研究中,将源自C3Hf/HeN小鼠胚胎的细胞在添加了HS和FBS的大分子和小分子组分的各种组合的NCTC-135培养基中培养,以确定有效成分。结果表明,HS的大分子组分(母马或公马)会导致染色体数目和结构发生改变。与荧光诱导的断裂不同,HS还显示出在着丝粒处或附近引起染色单体断裂和交换,荧光诱导的断裂沿着染色单体随机发生。然而,通过使用HS和FBS的大分子和小分子组分或其组合来完全控制染色体稳定性和恶性转化的努力并未成功。与此研究相关,通过基于先前描述和记录的细胞学标准的直接采样方法对体外恶性转化进行诊断。除了一个例外,11种不同细胞系的诊断结果与体内试验结果一致。

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