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Quantitative proteomics of primary tumors with varying metastatic capabilities using stable isotope-labeled proteins of multiple histogenic origins

机译:使用多种组织起源的稳定同位素标记的蛋白质,对具有不同转移能力的原发肿瘤进行定量蛋白质组学

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摘要

The development of metastasis is a complex, multistep process that remains poorly defined. To identify proteins involved in the colonization phase of the metastatic process, we compared the proteome of tumors derived from inoculation of a panel of isogenic human cancer cell lines with different metastatic capabilities into the mammary fat pad of immunodeficient mice. Using a protein standard generated by SILAC-labeling, a total of 675 proteins were identified and 30 were differentially expressed between at least two of the tumors. The protein standard contained the proteomes of seven cell lines from multiple histogenic origins and displayed superior features compared to standard super-SILAC. The expression of some proteins correlated with metastatic capabilities, such as myosin-9 (nonmuscle myosin II A) and L-lactate dehydrogenase A, while the expression of elongation factor tu correlated inversely to metastatic capabilities. The expression of these proteins was biochemically validated, and expression of myosin-9 in clinical breast cancer samples was further shown to be altered in primary tumors versus corresponding lymph node metastasis. Our study demonstrates an improved strategy for quantitative comparison of an unlimited number of tumor tissues, and provides novel insights into key proteins associated with the colonization phase of metastasis formation.
机译:转移的发展是一个复杂的,多步骤的过程,至今仍不清楚。为了鉴定与转移过程的定殖阶段有关的蛋白质,我们比较了将一组具有不同转移能力的同基因人类癌细胞系接种到免疫缺陷小鼠的乳腺脂肪垫中后得到的肿瘤蛋白质组。使用通过SILAC标记产生的蛋白质标准品,共鉴定出675种蛋白质,并且在至少两个肿瘤之间差异表达30种蛋白质。该蛋白质标准品包含来自多个组织起源的七个细胞系的蛋白质组,并且与标准的super-SILAC相比具有优越的功能。一些蛋白的表达与转移能力有关,例如肌球蛋白9(非肌球蛋白ⅡA)和L-乳酸脱氢酶A,而延伸因子tu的表达与转移能力成反比。这些蛋白质的表达已通过生化验证,并且在临床乳腺癌样本中,肌球蛋白9的表达在原发性肿瘤中相对于相应的淋巴结转移进一步发生了改变。我们的研究表明了一种改进的策略,用于定量比较无限数量的肿瘤组织,并为与转移形成的定居阶段相关的关键蛋白提供了新颖的见解。

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