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α 和β整联蛋白亚基在转移性巨噬细胞-黑色素瘤融合杂种中的上调。

Upregulation of alpha and beta integrin subunits in metastatic macrophage-melanoma fusion hybrids.

机构信息

Department of Dermatology, Yale University School of Medicine, New Haven, Connecticut, USA.

出版信息

Melanoma Res. 2009 Dec;19(6):343-9. doi: 10.1097/CMR.0b013e32832fe121.

Abstract

Fusion of cancer cells with migratory bone-marrow-derived cells such as macrophages can produce cancer cells with increased metastatic potential. To study this, we fused mouse macrophages with weakly metastatic mouse melanoma cells and generated a panel of hybrid clones. About half of these showed increased metastatic potential in mice. These hybrids expressed traits and molecules that were known indicators of tumor progression in melanoma (chemotaxis toward fibronectin, melanogenesis, autophagy, cMet, MCR1, SPARC, cell surface LAMP-1, GnT-V and β1,6-branched oligosaccharides). Here, we investigated integrin subunit expression in selected hybrids. Integrins, especially those that are substrates for the glycosyltransferase GnT-V and carriers of β1,6-branched oligosaccharides, play an important role in cell migration. We report increased expression of the integrin subunits α3, α5, α6, αv, β1, and β3 in metastatic hybrids compared with parental melanoma cells and a weakly metastatic hybrid. Notably, each of these subunits is also a substrate for GnT-V. Integrin subunit expression was further increased by inducers of cyclic AMP. Expression of these integrin subunits is a characteristic of macrophages and also associated with progression in melanoma and other cancers. In summary, our studies of macrophage-melanoma hybrids show that several α and β integrin subunits are upregulated in the metastatic lines. This adds further support for the theory that generation of a metastatic phenotype may be initiated through a single event: fusion of migratory bone marrow-derived cells with cancer cells.

摘要

癌细胞与迁移的骨髓来源细胞(如巨噬细胞)融合可以产生具有更高转移潜力的癌细胞。为了研究这一点,我们将小鼠巨噬细胞与弱转移性的小鼠黑色素瘤细胞融合,生成了一组杂交克隆。这些杂交克隆中有大约一半在小鼠中表现出更高的转移潜力。这些杂种表达了黑色素瘤中已知的肿瘤进展标志物(向纤维连接蛋白的趋化性、黑色素生成、自噬、cMet、MCR1、SPARC、细胞表面 LAMP-1、GnT-V 和β1,6-分支寡糖)的特征和分子。在这里,我们研究了选定杂交体中整合素亚基的表达。整合素,特别是那些作为糖基转移酶 GnT-V 的底物和β1,6-分支寡糖载体的整合素,在细胞迁移中起着重要作用。我们报告说,与亲本黑色素瘤细胞和弱转移性杂交体相比,转移性杂交体中整合素亚基α3、α5、α6、αv、β1 和β3 的表达增加。值得注意的是,这些亚基中的每一个也是 GnT-V 的底物。环磷酸腺苷诱导物进一步增加了整合素亚基的表达。这些整合素亚基的表达是巨噬细胞的特征,也与黑色素瘤和其他癌症的进展有关。总之,我们对巨噬细胞-黑色素瘤杂交体的研究表明,几种α和β整合素亚基在转移性系中上调。这进一步支持了这样一种理论,即转移表型的产生可能是通过单个事件引发的:迁移的骨髓来源细胞与癌细胞融合。

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