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从啮齿动物神经胶质前体细胞到少突胶质细胞 - 2型星形胶质细胞谱系中的人类神经胶质肿瘤形成

From rodent glial precursor cell to human glial neoplasia in the oligodendrocyte-type-2 astrocyte lineage.

作者信息

Noble M, Gutowski N, Bevan K, Engel U, Linskey M, Urenjak J, Bhakoo K, Williams S

机构信息

Ludwig Institute for Cancer Research, London, England.

出版信息

Glia. 1995 Nov;15(3):222-30. doi: 10.1002/glia.440150304.

Abstract

With only a few exceptions, the precursor cells representing the normal counterparts of human tumours are unknown. The comparative lack of information about the lineages involved in tissue development, and difficulties in growing many human tumors in a manner suitable for cellular biological analysis, together often make it difficult to study the differences between normal and tumor cells and to develop many of the model systems that would be useful in the study of human cancer. By applying techniques previously utilized to study glial progenitor cells, we have isolated a human glioblastoma multiforme (GBM)-derived population that expresses many properties otherwise uniquely expressed by oligodendrocyte-type-2 astrocyte (O-2A) progenitor cells. Hu-O-2A/Gb1 (for Human O-2A lineage Glioblastoma number 1) cells responded to similar mitogens and differentiation modulators as rodent O-2A progenitors, and generated cells with features of precursor cells, oligodendrocytes and astrocytes. Moreover, 1H-NMR analysis of amino acid composition demonstrated a striking conversation of types and quantities of free amino acids between the human tumour cells and the rodent primary cells. Hu-O-2A/Gb1 cells represent the first human glioma-derived population for which unambiguous lineage assignment has been possible, and our results indicate that the human O-2A lineage can contribute to one of the most malignant of glial tumours. In addition, the highly diagnostic 1H-NMR spectrum expressed by Hu-O-2A/Gb1 cells raises the possibility of eventual non-invasive identification of tumors of this lineage.

摘要

除了少数例外情况,代表人类肿瘤正常对应物的前体细胞尚不清楚。关于组织发育所涉及谱系的信息相对匮乏,以及以适合细胞生物学分析的方式培养许多人类肿瘤存在困难,这两者常常使得难以研究正常细胞与肿瘤细胞之间的差异,也难以开发许多对人类癌症研究有用的模型系统。通过应用先前用于研究神经胶质祖细胞的技术,我们分离出了一种源自多形性胶质母细胞瘤(GBM)的细胞群体,该群体表达了许多原本仅由少突胶质细胞 - 2型星形胶质细胞(O - 2A)祖细胞独特表达的特性。Hu - O - 2A/Gb1(人类O - 2A谱系胶质母细胞瘤1号)细胞对与啮齿动物O - 2A祖细胞类似的促有丝分裂原和分化调节剂有反应,并产生具有前体细胞、少突胶质细胞和星形胶质细胞特征的细胞。此外,对氨基酸组成的1H - NMR分析表明,人类肿瘤细胞与啮齿动物原代细胞之间游离氨基酸的类型和数量存在显著的一致性。Hu - O - 2A/Gb1细胞代表了首个能够明确进行谱系归属的源自人类胶质瘤的细胞群体,我们的结果表明人类O - 2A谱系可能与最恶性的胶质肿瘤之一有关。此外,Hu - O - 2A/Gb1细胞所表达的高度诊断性的1H - NMR谱图增加了最终对该谱系肿瘤进行非侵入性鉴定的可能性。

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