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市售抗血清缺乏特异性:需要更好的规格说明。

Lack of specificity of commercially available antisera: better specifications needed.

作者信息

Pradidarcheep Wisuit, Labruyère Wil T, Dabhoiwala Noshir F, Lamers Wouter H

机构信息

AMC Liver Center, Academic Medical Center, University of Amsterdam, Meibergdreef 69-71, 1105 BK Amsterdam, The Netherlands.

出版信息

J Histochem Cytochem. 2008 Dec;56(12):1099-111. doi: 10.1369/jhc.2008.952101. Epub 2008 Sep 15.

Abstract

The ideal antiserum for immunohistochemical (IHC) applications contains monospecific high-affinity antibodies with little nonspecific adherence to sections. Many commercially available antibodies are "affinity" purified, but it is unknown if they meet "hard" specificity criteria, such as absence of staining in tissues genetically deficient for the antigen or a staining pattern that is identical to that of an antibody raised against a different epitope on the same protein. Reviewers, therefore, often require additional characterization. Although the affinity-purified antibodies used in our study on the distribution of muscarinic receptors produced selective staining patterns on sections, few passed the preabsorption test, and none produced bands of the anticipated size on Western blots. More importantly, none showed a difference in staining pattern on sections or Western blots between wild-type and knockout mice. Because these antibodies were used in most studies published thus far, our findings cast doubts on the validity of the extant body of morphological knowledge of the whole family of muscarinic receptors. We formulate requirements that antibody-specification data sheets should meet and propose that journals for which IHC is a core technique facilitate consumer rating of antibodies. "Certified" antibodies could avoid fruitless and costly validation assays and should become the standard of commercial suppliers.

摘要

用于免疫组织化学(IHC)应用的理想抗血清应包含单特异性高亲和力抗体,且对切片的非特异性黏附极少。许多市售抗体是经过“亲和”纯化的,但它们是否符合“严格”的特异性标准尚不清楚,例如在缺乏该抗原的基因缺陷组织中无染色,或者染色模式与针对同一蛋白质上不同表位产生的抗体的染色模式相同。因此,审稿人通常要求进行额外的鉴定。尽管我们关于毒蕈碱受体分布的研究中使用的亲和纯化抗体在切片上产生了选择性染色模式,但很少有抗体通过预吸收试验,并且在蛋白质印迹法中没有一个产生预期大小的条带。更重要的是,在野生型和基因敲除小鼠的切片或蛋白质印迹法中,没有一个抗体的染色模式显示出差异。由于这些抗体被用于迄今为止发表的大多数研究中,我们的发现对整个毒蕈碱受体家族现有形态学知识体系的有效性提出了质疑。我们制定了抗体规格数据表应满足的要求,并建议将免疫组织化学作为核心技术的期刊促进对抗体的消费者评级。“认证”抗体可以避免徒劳且昂贵的验证试验,并应成为商业供应商的标准。

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