醛脱氢酶（ALDH）活性不会选择具有增强侵袭性的恶性黑色素瘤细胞。

Aldehyde dehydrogenase (ALDH) activity does not select for cells with enhanced aggressive properties in malignant melanoma.

机构信息

Department of Tumour Biology, Oslo University Hospital Radiumhospitalet, Oslo, Norway.

出版信息

PLoS One. 2010 May 20;5(5):e10731. doi: 10.1371/journal.pone.0010731.

DOI:10.1371/journal.pone.0010731

PMID:20505780

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2874003/

Abstract

BACKGROUND

Malignant melanoma is an exceptionally aggressive, drug-resistant and heterogeneous cancer. Recently it has been shown that melanoma cells with high clonogenic and tumourigenic abilities are common, but markers distinguishing such cells from cells lacking these abilities have not been identified. There is therefore no definite evidence that an exclusive cell subpopulation, i.e. cancer stem cells (CSC), exists in malignant melanoma. Rather, it is suggested that multiple cell populations are implicated in initiation and progression of the disease, making it of importance to identify subpopulations with elevated aggressive properties.

METHODS AND FINDINGS

In several other cancer forms, Aldehyde Dehydrogenase (ALDH), which plays a role in stem cell biology and resistance, is a valuable functional marker for identification of cells that show enhanced aggressiveness and drug-resistance. Furthermore, the presence of ALDH(+) cells is linked to poor clinical prognosis in these cancers. By analyzing cell cultures, xenografts and patient biopsies, we showed that aggressive melanoma harboured a large, distinguishable ALDH(+) subpopulation. In vivo, ALDH(+) cells gave rise to ALDH(-) cells, while the opposite conversion was rare, indicating a higher abilities of ALDH(+) cells to reestablish tumour heterogeneity with respect to the ALDH phenotype. However, both ALDH(+) and ALDH(-) cells demonstrated similarly high abilities for clone formation in vitro and tumour initiation in vivo. Furthermore, both subpopulations showed similar sensitivity to the anti-melanoma drugs, dacarbazine and lexatumumab.

CONCLUSIONS

These findings suggest that ALDH does not distinguish tumour-initiating and/or therapy-resistant cells, implying that the ALDH phenotype is not associated with more-aggressive subpopulations in malignant melanoma, and arguing against ALDH as a "universal" marker. Besides, it was shown that the ability to reestablish tumour heterogeneity is not necessarily linked to the more aggressive phenotype.

摘要

背景

恶性黑色素瘤是一种极具侵袭性、耐药性和异质性的癌症。最近有研究表明，具有高克隆形成和致瘤能力的黑色素瘤细胞很常见，但尚未确定能够将这些细胞与缺乏这些能力的细胞区分开来的标志物。因此，没有明确的证据表明恶性黑色素瘤中存在单一的细胞亚群，即癌症干细胞（CSC）。相反，多个细胞群体被认为参与了疾病的发生和进展，因此识别具有高侵袭性的亚群非常重要。

方法和发现

在其他几种癌症形式中，醛脱氢酶（ALDH）在干细胞生物学和耐药性中发挥作用，是鉴定具有增强侵袭性和耐药性的细胞的有价值的功能标志物。此外，这些癌症中 ALDH(+)细胞的存在与不良的临床预后相关。通过分析细胞培养物、异种移植物和患者活检，我们发现侵袭性黑色素瘤中存在一个大的、可区分的 ALDH(+)亚群。在体内，ALDH(+)细胞产生 ALDH(-)细胞，而相反的转化很少见，这表明 ALDH(+)细胞具有更高的能力来重建肿瘤异质性，相对于 ALDH 表型。然而，ALDH(+)和 ALDH(-)细胞在体外克隆形成和体内肿瘤起始方面均表现出相似的高能力。此外，这两个亚群对治疗黑色素瘤的药物达卡巴嗪和 lexatumumab 均表现出相似的敏感性。

结论

这些发现表明 ALDH 不能区分肿瘤起始和/或耐药细胞，这意味着 ALDH 表型与恶性黑色素瘤中侵袭性更强的亚群无关，并反对 ALDH 作为“通用”标志物。此外，研究还表明，重建肿瘤异质性的能力不一定与更具侵袭性的表型相关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6857/2874003/78f335e45a5e/pone.0010731.g001.jpg

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醛脱氢酶（ALDH）活性不会选择具有增强侵袭性的恶性黑色素瘤细胞。

Aldehyde dehydrogenase (ALDH) activity does not select for cells with enhanced aggressive properties in malignant melanoma.

机构信息

Department of Tumour Biology, Oslo University Hospital Radiumhospitalet, Oslo, Norway.