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对从己烯雌酚诱导的叙利亚仓鼠肾肿瘤建立的细胞系的特性分析。

Characterization of a cell line established from diethylstilbestrol-induced renal tumors in Syrian hamsters.

作者信息

Laurent G, Nonclercq D, Journé F, Brohée R, Toubeau G, Falmagne P, Heuson-Stiennon J A

机构信息

Laboratory of Histology and Experimental Cytology, Faculty of Medicine and Pharmacy, Université de Mons-Hainaut, Mons, Belgium.

出版信息

In Vitro Cell Dev Biol Anim. 1999 Jun;35(6):339-45. doi: 10.1007/s11626-999-0084-7.

Abstract

This article describes HKT-1097, a new cell line established from renal tumors induced by the protracted administration of diethylstilbestrol (DES) to male Syrian golden hamsters. Cell culture was initiated from tumor samples obtained from two 14-mo.-old animals which had undergone exposure to DES for a period of 11 mo. The HKT-1097 cell line was characterized between Passages 16 and 22 with respect to cell morphology, growth properties, karyology, and the presence of estrogen receptors. Moreover, immunostaining with a panel of antisera was performed to identify the cytological profile of the cell line and establish a parallel with tumor tissue in vivo. HKT-1097 cells are fibroblastoid; their most distinctive feature is that they exhibit strikingly long processes. The HKT-1097 cell line grows as a monolayer with a tendency toward a less stringent density-dependent inhibition of growth. The modal chromosome number is 44, but more than 50% of the cells are aneuploid, suggesting a substantial degree of karyotype instability. HKT-1097 cells express estrogen receptors. They contain immunoreactive vimentin and desmin, but appear negative upon cytokeratin immunostaining. In addition, these cells express glial fibrillary acidic protein and other markers of the neuroectodermal lineage, but lack neurofilament protein. Insofar as the same lineage markers have been demonstrated in DES-induced Syrian hamster kidney tumors (SHKT), we conclude that HKT-1097 cells retain some of the original tumor cell phenotype. The current observations suggest that estrogen-induced SHKT derive from the renal interstitium and point to an involvement of neuroectodermal cells in the development of these neoplasms.

摘要

本文描述了HKT - 1097,这是一种从给雄性叙利亚金仓鼠长期服用己烯雌酚(DES)诱导产生的肾肿瘤中建立的新细胞系。细胞培养起始于从两只14月龄动物获取的肿瘤样本,这两只动物曾暴露于DES达11个月。HKT - 1097细胞系在第16至22代时,针对细胞形态、生长特性、核型以及雌激素受体的存在情况进行了特征描述。此外,用一组抗血清进行免疫染色,以鉴定该细胞系的细胞学特征,并与体内肿瘤组织建立平行关系。HKT - 1097细胞呈成纤维细胞样;其最显著的特征是它们表现出极长的突起。HKT - 1097细胞系以单层形式生长,对生长的密度依赖性抑制倾向较弱。众数染色体数为44,但超过50%的细胞为非整倍体,表明核型存在相当程度的不稳定性。HKT - 1097细胞表达雌激素受体。它们含有免疫反应性波形蛋白和结蛋白,但细胞角蛋白免疫染色呈阴性。此外,这些细胞表达胶质纤维酸性蛋白和神经外胚层谱系的其他标志物,但缺乏神经丝蛋白。鉴于在DES诱导的叙利亚仓鼠肾肿瘤(SHKT)中已证实存在相同的谱系标志物,我们得出结论,HKT - 1097细胞保留了一些原始肿瘤细胞的表型。目前的观察结果表明,雌激素诱导的SHKT起源于肾间质,并表明神经外胚层细胞参与了这些肿瘤的发生发展。

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