首页> 美国卫生研究院文献>Biochemical Journal >Isoform I (mdr3) is the major form of P-glycoprotein expressed in mouse brain capillaries. Evidence for cross-reactivity of antibody C219 with an unrelated protein.
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Isoform I (mdr3) is the major form of P-glycoprotein expressed in mouse brain capillaries. Evidence for cross-reactivity of antibody C219 with an unrelated protein.

机译:异构体I(mdr3)是在小鼠脑毛细血管中表达的P-糖蛋白的主要形式。抗体C219与无关蛋白发生交叉反应的证据。

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摘要

P-glycoprotein (P-gp) is expressed in various non-cancerous tissues such as the endothelial cells of the blood-brain barrier. We used several monoclonal antibodies (mAbs) and isoform-specific polyclonal antibodies to establish which P-gp isoforms are expressed in isolated mouse brain capillaries. P-gp class I isoform was detected in capillaries with a Western immunoblotting procedure using a specific antiserum. No immunoreactivity was observed with either class II- or class III-specific antisera. Immunoreactivity was observed with mAb C219. However, this antibody detected two distinct immunoreactive proteins (155 and 190 kDa) in the isolated brain capillaries. These two proteins comigrated as a broad band when the samples were submitted to heat prior to gel electrophoresis. The glycoprotein nature of these two antigens was evaluated by their sensitivity to N-glycanase treatment. Following this treatment, the size of the proteins was reduced from 190 and 155 kDa to 180 and 120 kDa, respectively. Triton X-114 phase-partitioning studies showed that the 190 kDa immunoreactive protein was poorly solubilized by Triton X-114, while the 155 kDa protein was partitioned in the detergent-rich phase. In labelling experiments, only the 155 kDa protein was photolabelled with [125I]iodoarylazidoprazosin. These results show that a 190 kDa protein detected by antibody C219 is an antigen unrelated to the three P-gp isoforms presently known. Cross-reactivity of C219 with an unrelated protein emphasizes the fact that more than one antibody should be used in the assessment of P-gp expression in cell lines and tissues.
机译:P-糖蛋白(P-gp)在各种非癌性组织(如血脑屏障的内皮细胞)中表达。我们使用了几种单克隆抗体(mAb)和同工型特异性多克隆抗体来确定哪些P-gp同工型在分离的小鼠脑毛细血管中表达。使用特定的抗血清,采用Western免疫印迹方法在毛细血管中检测到P-gp I类同工型。 II类或III类特异性抗血清未观察到免疫反应性。用mAb C219观察到免疫反应性。但是,该抗体在分离的脑毛细血管中检测到两个不同的免疫反应蛋白(155和190 kDa)。当在凝胶电泳之前将样品加热时,这两种蛋白质会以宽谱带的形式出现。通过对N-聚糖酶处理的敏感性来评估这两种抗原的糖蛋白性质。经过这种处理,蛋白质的大小分别从190 kDa和155 kDa减小到180 kDa和120 kDa。 Triton X-114相分配研究表明190 kDa免疫反应蛋白被Triton X-114溶解的较弱,而155 kDa蛋白则分配在富含去污剂的相中。在标记实验中,只有155 kDa蛋白被[125I]碘代芳基叠氮基吡唑啉进行了光标记。这些结果表明,由抗体C219检测到的190kDa蛋白是与目前已知的三种P-gp同工型无关的抗原。 C219与无关蛋白的交叉反应性强调了这样一个事实,即在评估细胞系和组织中P-gp表达时应使用一种以上的抗体。

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