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Molecular and Immunohistochemical Characterization of Historical Long-Term Preserved Fixed Tissues from Different Human Organs

机译:来自不同人体器官的历史长期保存的固定组织的分子和免疫组织化学表征

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摘要

University and museum collections are very important sources of biological samples that can be used to asses the past and present genetic diversity of many species. Modern genetic and immunohistochemical techniques can be used on long-term preserved fixed tissues from museum specimens to answer epidemiological questions. A proof of principle was established to apply modern molecular genetics and immunohistochemical methods to these old specimens and to verify the original diagnosis. We analysed 19 specimens from our university collection including human organs that had been in fixative for more than 80 years. The tissues originated from lung, colon, brain, heart, adrenal gland, uterus and skin. We isolated amplifiable DNA from these wet preparations and performed mutational analysis of BRAF, KRAS and EGFR. The tissues were also embedded in paraffin and used for modern histology and immunohistochemistry. Our data show that amplifiable DNA is extractable and ranged from 0.25 to 22.77 μg of total DNA. In three specimens BRAFV600E or KRASG12D mutations were found. Additionally, expression of different proteins like vimentin and GFAP was detected immunohistochemical in six investigated specimens. On the basis of our results the original diagnosis was altered in three specimens. Our work showed that it is possible to extract amplifiable DNA suitable for sequence analysis from long-term fixed tissue. Furthermore, histology and immunohistochemistry is feasible in specimens fixed long time ago. We conclude that these old preparations are suitable for further epidemiological research and that our methods open up new opportunities for future studies.
机译:大学和博物馆的收藏品是非常重要的生物样品来源,可用于评估许多物种过去和现在的遗传多样性。现代遗传和免疫组织化学技术可用于博物馆标本的长期保存的固定组织,以回答流行病学问题。建立了原理证明,以将现代分子遗传学和免疫组化方法应用于这些老样本并验证原始诊断。我们分析了我们大学收藏中的19个标本,包括固定了80多年的人体器官。这些组织起源于肺,结肠,脑,心脏,肾上腺,子宫和皮肤。我们从这些湿制剂中分离了可扩增的DNA,并进行了BRAF,KRAS和EGFR的突变分析。该组织还被包埋在石蜡中,并用于现代组织学和免疫组织化学。我们的数据表明,可扩增的DNA可提取,总DNA的范围为0.25至22.77μg。在三个标本中发现了BRAF V600E 或KRAS G12D 突变。此外,在六个调查标本中检测到了不同蛋白如波形蛋白和GFAP的表达。根据我们的结果,最初的诊断在三个样本中发生了变化。我们的工作表明,可以从长期固定的组织中提取适合序列分析的可扩增DNA。此外,组织学和免疫组化在很久以前固定的标本中是可行的。我们得出的结论是,这些旧的制剂适合进一步的流行病学研究,我们的方法为将来的研究开辟了新的机会。

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