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首页> 外文期刊>Journal of Neuropathology and Experimental Neurology >Differential Distribution of erbB Receptors in Human Glioblastoma Multiforme: Expression of erbB3 in CD133-Positive Putative Cancer Stem Cells
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Differential Distribution of erbB Receptors in Human Glioblastoma Multiforme: Expression of erbB3 in CD133-Positive Putative Cancer Stem Cells

机译:erbB受体在人类胶质母细胞瘤中的差异分布:erbB3在CD133阳性推定的癌症干细胞中的表达

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Glioblastomas are the most common primary central nervous system tumors in adults, and they remain resistant to current treatments. erbB1 signaling is frequently altered in glioblastomas, suggesting thaterbB receptor family members may represent targets for molecular therapy. We performed a comprehensive analysis of erbB receptor and ligand expression profiles in a panel of 9 glioblastomas andcompared them to nonneoplastic cerebral tissue containing neocortex and adjacent white matter. Quantitative reverse transcription-polymerase chain reaction and Western blot analysis showed that erbB1signaling and erbB2 receptors exhibited highly variable deregulation profiles in the tumors, with patterns ranging from underexpression to overexpression; in contrast, erbB3 and erbB4 were downregulated. We next performed immunohistochemistry to determinethe distribution patterns of erbB receptors among the main neuralcell types in the tumors with special reference to the putative tumor stem cell population. Results revealed intertumoral and intratumoral heterogeneity in all 4 erbB expression profiles, but each receptor exhibited a distinct distribution pattern among glial fibrillary acidic protein-, Olig2-, NeuN-, and CD133-positive populations. Although erbB1 immunoreactivity was detected in only small subsets of CD133-positive putative tumor stem cells, erbB3 immunoreactivity was prominent in this population, suggesting that erbB3 may represent a new potential therapeutic target.
机译:胶质母细胞瘤是成人中最常见的原发性中枢神经系统肿瘤,并且它们仍然对当前的治疗有抵抗力。 erbB1信号在胶质母细胞瘤中经常发生变化,表明erbB受体家族成员可能代表分子治疗的靶标。我们对一组9个胶质母细胞瘤中的erbB受体和配体表达进行了全面分析,并将它们与含有新皮层和相邻白质的非肿瘤性脑组织进行了比较。定量逆转录-聚合酶链反应和Western印迹分析表明,erbB1信号和erbB2受体在肿瘤中表现出高度可变的失调特征,模式从表达不足到过度表达。相反,erbB3和erbB4被下调。接下来,我们进行免疫组织化学测定,以确定肿瘤中主要神经细胞类型中erbB受体的分布模式,并特别参考假定的肿瘤干细胞群体。结果显示,在所有4种erbB表达谱中,肿瘤间和瘤内异质性,但每个受体在神经胶质纤维酸性蛋白,Olig2-,NeuN和CD133阳性人群中均表现出独特的分布方式。尽管仅在CD133阳性假定肿瘤干细胞的一小部分中检测到erbB1免疫反应性,但erbB3免疫反应性在该人群中很突出,这表明erbB3可能代表了一个新的潜在治疗靶点。

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    Véronique Duhem-Tonnelle, MD, PhD, Ivan Bièche, PhD, Sophie Vacher, PhD, Anne Loyens, Claude-Alain Maurage, MD, PhD, Francis Collier, MD, PhD, Marc Baroncini, MD, PhD, Serge Blond, MD, PhD, Vincent Prevot, PhD, and Ariane Sharif, PhDFrom the Inserm, Jean-Pierre Aubert Research Centre, Development and Plasticity of the Postnatal Brain (VD-T, AL, C-AM, MB, SB, VP, AS), Université de Lille 2, IMPRT (VD-T, AL, FC, MB, SB, VP, AS), Clinique de Neurochirurgie, CHRU de Lille, Hôpital Roger Salengro (VD-T, MB, SB), Lille, INSERM U735 (IB, SV), Centre René Huguenin, FNCLCC (IB, SV), St-Cloud, Pôle de Pathologie, CHRU de Lille (C-AM), Département d'Histologie, Université de Lille 2 (C-AM), and Service de Gynécologie, CHRU de Lille, Hôpital Jeanne-de-Flandre (FC), Lille, France.Send correspondence and reprint requests to: Ariane Sharif, PhD, Inserm U837, Bâtiment Biserte, Place de Verdun, 59045 Lille Cedex, France, E-mail: ariane.sharif@inserm.fr or Vincent Prevot, PhD, Inserm U837, Bâtiment Biserte, Place de Verdun, 59045 Lille Cedex, France, E-mail: vincent.prevot@inserm.frThis research was supported by Inserm Grants U816 (to Vincent Prevot) and U837 (to Vincent Prevot), the University of Lille 2 (to Vincent Prevot), the Institut National du Cancer (to Vincent Prevot), the Agence National pour la Recherche (France) (to Vincent Prevot), the Fondation pour la Recherche Médicale (Equipe FRM, France) (to Vincent Prevot), a PHRC (Serge Blond, Marc Baroncini), and the Imaging Core of IFR114 (to Vincent Prevot). Ariane Sharif was a postdoctoral fellow supported by the Région Nord Pas de Calais and the FRM.Supplemental digital content is available for this article. Direct URL citations appear in the printed text and are provided in the HTML and PDF versions of this article on the journal's Web site (www.jneuropath.com).Online-only figures are available at http://www.jneuropath.com.,;

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