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钠离子依赖型无机磷酸盐转运蛋白 SLC34A1(NaPi-IIa)在小鼠脑中未定位:组织特异性抗原交叉反应的一个案例。

The sodium-dependent inorganic phosphate transporter SLC34A1 (NaPi-IIa) is not localized in the mouse brain: a case of tissue-specific antigenic cross-reactivity.

机构信息

Department of Anatomy and Centre for Molecular Biology and Neuroscience, University of Oslo, Oslo, Norway.

出版信息

J Histochem Cytochem. 2011 Sep;59(9):807-12. doi: 10.1369/0022155411411713. Epub 2011 May 23.

Abstract

The sodium-dependent inorganic phosphate transporter NaPi-IIa is expressed in the kidney. Here, the authors used a polyclonal antiserum raised against NaPi-IIa- and NaPi-IIa-deficient mice to characterize its expression in nervous tissue. Western blots showed that a NaPi-IIa immunoreactive band (90 kDa) was only present in wild-type kidney membranes and not in kidney knockout or wild-type brain membranes. In the water-soluble fraction of wild-type and knockout brains, another band (50 kDa) was observed; this band was not detected in the kidney. Light and electron microscopic immunohistochemistry using the NaPi-IIa antibodies showed immunolabeling of kidney tubules in wild-type but not knockout mice. In the brain, labeling of presynaptic nerve terminals was present also in NaPi-IIa-deficient mice. This labeling pattern was also produced by the NaPi-IIa preimmune serum. The authors conclude that the polyclonal antiserum is specific toward NaPi-IIa in the kidney, but in the brain, immunolabeling is caused by a cross-reaction of the antiserum with an unknown cytosolic protein that is not present in the kidney. This tissue-specific cross-reactivity highlights a potential pitfall when validating antibody specificity using knockout mouse-derived tissue other than the specific tissue of interest and underlines the utility of specificity testing using preimmune sera.

摘要

钠依赖性无机磷酸盐转运蛋白 NaPi-IIa 在肾脏中表达。在这里,作者使用针对 NaPi-IIa 和 NaPi-IIa 缺陷型小鼠的多克隆抗血清来研究其在神经组织中的表达。Western blot 显示,NaPi-IIa 免疫反应性条带(90 kDa)仅存在于野生型肾脏膜中,而不存在于肾脏敲除或野生型脑组织中。在野生型和敲除型脑组织的水溶性部分中,还观察到另一条带(50 kDa);这条带在肾脏中未检测到。使用 NaPi-IIa 抗体进行的光和电子显微镜免疫组织化学显示,在野生型肾脏中存在免疫标记,而在敲除型肾脏中不存在。在大脑中,也在 NaPi-IIa 缺陷型小鼠中观察到突触前神经末梢的标记。这种标记模式也由 NaPi-IIa 预免疫血清产生。作者得出结论,多克隆抗血清在肾脏中针对 NaPi-IIa 是特异性的,但在大脑中,免疫标记是由抗血清与在肾脏中不存在的未知细胞质蛋白的交叉反应引起的。这种组织特异性交叉反应强调了在使用除感兴趣的特定组织以外的敲除小鼠衍生组织验证抗体特异性时存在潜在的陷阱,并强调了使用预免疫血清进行特异性测试的实用性。

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