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CD44在人神经母细胞瘤肿瘤及细胞系中的表达与调控

CD44 expression and modulation on human neuroblastoma tumours and cell lines.

作者信息

Gross N, Beck D, Beretta C, Jackson D, Perruisseau G

机构信息

Pediatrics Department, University Hospital, Lausanne, U.K.

出版信息

Eur J Cancer. 1995;31A(4):471-5. doi: 10.1016/0959-8049(95)00029-i.

Abstract

The human CD44 cell surface glycoprotein has been involved in a variety of functions including lymphocyte homing, extracellular cell matrix attachment and tumour metastasis. A large family of variants or isoforms, generated by alternative splicing of a single gene, has been reported to be involved in the malignant process, by conferring metastatic potential to non-metastatic cells. Neuroblastoma is a tumour characterised by an aggressive and metastatic behaviour in advanced stages, with amplification of the MYCN protooncogene. In this report, we show that the CD44 standard molecule was highly expressed in the majority of tumours of stages 1-3, in all stage 4s and ganglioneuromas, but only in a subset of stage 4 tumours. A lack of CD44 expression was observed in all MYCN amplified stage 4 tumours, thus demonstrating a highly significant inverse relationship between MYCN amplification and CD44 expression in neuroblastoma. In addition, the expression of 4 different CD44 isoforms was measured on all specimens and was always found to be negative. Using neuroblastoma cell lines and MYCN expressing transfectants, we show that CD44 expression by neuroblastoma cell lines is not directly related to MYCN amplification, but is associated to the stage of differentiation or lineage, and to the tumorigenic properties of the cells. In addition, CD44 expression can be upmodulated parallel to differentiation or maturation as induced by retinoic acid, bromodeoxyuridine or phorbol ester. In contrast, cytokines such as IFN gamma, TNF alpha, or growth factors such as bFGF, SCF and TGF beta were ineffective in modulating CD44 expression.

摘要

人类CD44细胞表面糖蛋白参与了多种功能,包括淋巴细胞归巢、细胞外基质附着和肿瘤转移。据报道,由单个基因的可变剪接产生的一大类变体或同工型通过赋予非转移性细胞转移潜能而参与恶性过程。神经母细胞瘤是一种在晚期具有侵袭性和转移行为的肿瘤,伴有MYCN原癌基因的扩增。在本报告中,我们表明CD44标准分子在大多数1-3期肿瘤、所有4期肿瘤和神经节神经瘤中高表达,但仅在一部分4期肿瘤中表达。在所有MYCN扩增的4期肿瘤中均观察到CD44表达缺失,从而证明神经母细胞瘤中MYCN扩增与CD44表达之间存在高度显著的负相关。此外,在所有标本上检测了四种不同CD44同工型的表达,结果均为阴性。使用神经母细胞瘤细胞系和表达MYCN的转染子,我们表明神经母细胞瘤细胞系的CD44表达与MYCN扩增无直接关系,但与分化阶段或谱系以及细胞的致瘤特性有关。此外,视黄酸、溴脱氧尿苷或佛波酯诱导分化或成熟时,CD44表达可平行上调。相反,细胞因子如IFNγ、TNFα或生长因子如bFGF、SCF和TGFβ在调节CD44表达方面无效。

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