Quantitative proteomic analysis of amniocytes reveals potentially dysregulated molecular networks in Down syndrome

Chan-Kyung J Cho; Andrei P Drabovich; George S Karagiannis; Eduardo Martínez-Morillo; Shawn Dason; Apostolos Dimitromanolakis; Eleftherios P Diamandis

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Quantitative proteomic analysis of amniocytes reveals potentially dysregulated molecular networks in Down syndrome

机译：羊水细胞的蛋白质组学定量分析显示唐氏综合症中潜在的分子网络失调

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Background Down syndrome (DS), caused by an extra copy of chromosome 21, affects 1 in 750 live births and is characterized by cognitive impairment and a constellation of congenital defects. Currently, little is known about the molecular pathogenesis and no direct genotype-phenotype relationship has yet been confirmed. Since DS amniocytes are expected to have a distinct biological behaviour compared to normal amniocytes, we hypothesize that relative quantification of proteins produced from trisomy and euploid (chromosomally normal) amniocytes will reveal dysregulated molecular pathways.

机译：背景唐氏综合症（DS）由21号染色体的额外副本引起，影响750例活产婴儿中的1例，其特征是认知障碍和先天性缺陷群。目前，关于分子发病机理的了解甚少，尚未确定直接的基因型-表型关系。由于预期DS羊膜细胞与正常羊膜相比具有独特的生物学行为，因此我们假设三体和整倍体（染色体正常）羊膜细胞产生的蛋白质的相对定量将揭示分子通路失调。

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《Clinical Proteomics》 |2013年第1期|1-13|共13页
作者
Chan-Kyung J Cho; Andrei P Drabovich; George S Karagiannis; Eduardo Martínez-Morillo; Shawn Dason; Apostolos Dimitromanolakis; Eleftherios P Diamandis;
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正文语种 eng
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Down syndrome Trisomy 21 Amniocyte Amniotic fluid cells Quantitative proteomics;

机译：唐氏综合症三体性21羊水羊水细胞蛋白质组学;

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1. Quantitative proteomic analysis of amniocytes reveals potentially dysregulated molecular networks in Down syndrome [J] . Chan-Kyung J Cho, Andrei P Drabovich, George S Karagiannis, Clinical proteomics. . 2013,第1期

机译：羊水细胞的蛋白质组学定量分析显示唐氏综合症中潜在的分子网络失调
2. Quantitative proteomic analysis of amniocytes reveals potentially dysregulated molecular networks in Down syndrome [J] . Chan-Kyung J Cho, Andrei P Drabovich, George S Karagiannis, Clinical proteomics. . 2013,第1期

机译：羊水细胞的蛋白质组学定量分析显示唐氏综合症中潜在的分子网络失调
3. Quantitative proteomics analysis reveals molecular networks regulated by epidermal growth factor receptor level in head and neck cancer [J] . Yang W., Cai Q., Lui V.W.Y., Journal of proteome research . 2010,第6期

机译：定量蛋白质组学分析揭示了头颈癌中受表皮生长因子受体水平调节的分子网络
4. Quantitative proteomic analysis reveals a molecular triad signature as biomarker candidates for astrocytomas and oligodendrogliomas [C] . Jose Cesar Rosa, Suely Kazue Nagahashi Marie, Sueli Oba-Shinjo, American Society for Mass Spectrometry Conference on Mass Spectrometry and Allied Topics . 2013

机译：定量蛋白质组学分析揭示了分子三合会签名作为星形细胞瘤和oligodendrogliomas的生物标志物候选者
5. Molecular classification and prediction of metastatic potential in early malignant melanoma: Improvement of prognostic accuracy by quantitative in situ proteomic analysis [D] . Berger, Aaron J. 2006

机译：早期恶性黑色素瘤的分子分类和转移潜能预测：通过定量原位蛋白质组学分析提高预后准确性
6. Quantitative proteomic analysis of amniocytes reveals potentially dysregulated molecular networks in Down syndrome [O] . Chan-Kyung J Cho, Andrei P Drabovich, George S Karagiannis, 2013

机译：羊水细胞的蛋白质组学定量分析显示唐氏综合症中潜在的分子网络失调
7. Quantitative proteomic analysis of amniocytes reveals potentially dysregulated molecular networks in Down syndrome [O] . Chan-Kyung J Cho, Andrei P Drabovich, George S Karagiannis, 2013

机译：羊水细胞的蛋白质组学定量分析显示唐氏综合症中潜在的分子网络失调

Quantitative proteomic analysis of amniocytes reveals potentially dysregulated molecular networks in Down syndrome

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