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Alcohol based tissue fixation as an alternative for formaldehyde: influence on immunohistochemistry

机译:以酒精为基础的组织固定替代甲醛:对免疫组织化学的影响

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Background Formaldehyde is commonly used in histopathology to fix tissue. Not only are the carcinogenic properties of this solution a hazard to the people in the workplace, it is also a major burden on the environment, and it crosslinks molecular groups that hinder immunohistochemistry. Aims The influence of two new alcohol based non-crosslinking fixatives on immunohistochemical staining properties was tested on various tissues. Methods Fresh tissue samples were cut into three equal pieces, which were then fixed in the alcohol based fixatives Boonfix or RCL2, or in neutral buffered formaldehyde (NBF) as control. After fixation, tissue was routinely processed to paraffin sections. Deparaffinised slides were blocked for endogenous peroxidase and subsequently submitted to the usual NBF based immunohistochemical protocols for 85 different common antibodies either not requiring antigen retrieval (AR), or AR in citrate buffer, EDTA or pepsin. Results NBF fixed tissues provided significantly better immunostaining results (84% good staining) than RCL2 (66% good) and Boonfix (60%). The lesser performance of RCL2 and Boonfix was especially caused by pepsin AR which caused significant tissue damage. Omission of pepsin AR resulted in better immunostaining for these antibodies for RCL2 fixed tissues which were overall no longer significantly worse than NBF fixed tissue. Conclusion Tissues fixed in non-crosslinking alcohol based fixatives can successfully be immunohistochemically stained for most antibodies following the usual NBF based protocols. Omission of pepsin pretreatment seems to be important to retain proper morphology of immunostained tissues preserved in alcohol based fixatives. Therefore, when switching to less toxic and non-carcinogenic alcohol-based fixatives like RCL2, no major changes in the daily routine of immunohistochemistry are anticipated.
机译:背景技术甲醛在组织病理学中通常用于固定组织。该解决方案的致癌特性不仅对工作场所的人们造成危害,而且还对环境造成重大负担,并且使阻碍免疫组织化学的分子基交联。目的在各种组织上测试了两种新的基于醇的非交联固定剂对免疫组织化学染色特性的影响。方法将新鲜的组织样本切成三等份,然后将其固定在酒精基固定剂Boonfix或RCL2中,或在中性缓冲甲醛(NBF)中作对照。固定后,将组织常规处理为石蜡切片。将去石蜡化的玻片上的内源性过氧化物酶封闭,然后将其用于85种常见抗体的常规NBF免疫组化方案,这些抗原不需要抗原修复(AR),也不需要柠檬酸盐缓冲液,EDTA或胃蛋白酶中的AR。结果NBF固定组织的免疫染色结果(良好染色为84%)明显优于RCL2(良好染色为66%)和Boonfix(60%)。 RCL2和Boonfix的性能较差尤其是由胃蛋白酶AR引起的,胃蛋白酶AR引起明显的组织损伤。胃蛋白酶AR的缺失导致这些抗体对RCL2固定组织的免疫染色效果更好,总体而言,这些抗体不再明显比NBF固定组织差。结论在非交联醇基固定剂中固定的组织可以按照常规的基于NBF的方法成功地对大多数抗体进行免疫组织化学染色。省略胃蛋白酶预处理对于保持酒精固定剂中保存的免疫染色组织的正确形态似乎很重要。因此,当改用毒性较小且无致癌性的醇类固定剂(如RCL2)时,预计免疫组织化学的日常工作不会发生重大变化。

著录项

  • 来源
    《Journal of Clinical Pathology》 |2010年第12期|p.1090-1094|共5页
  • 作者单位

    Department of Pathology, University Medical Center Utrecht, The Netherlands;

    Department of Pathology, University Medical Center Utrecht, The Netherlands;

    Department of Pathology, University Medical Center Utrecht, The Netherlands;

    Department of Pathology, University Medical Center Utrecht, The Netherlands;

    Department of Pathology, University Medical Center Utrecht, The Netherlands;

  • 收录信息 美国《科学引文索引》(SCI);美国《化学文摘》(CA);
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
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  • 入库时间 2022-08-18 01:36:16

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