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首页> 外文期刊>Journal of cell biology >Thermal stability of the helical structure of type IV collagen within basement membranes in situ: determination with a conformation-dependent monoclonal antibody.
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Thermal stability of the helical structure of type IV collagen within basement membranes in situ: determination with a conformation-dependent monoclonal antibody.

机译:基底膜内IV型胶原螺旋结构原位的热稳定性:用构象依赖性单克隆抗体测定。

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To examine the thermal stability of the helical structure of type IV collagen within basement membranes in situ, we have employed indirect immunofluorescence histochemistry performed at progressively higher temperatures using a conformation-dependent antibody, IV-IA8. We previously observed by competition enzyme-linked immunosorbent assay that, in neutral solution, the helical epitope to which this antibody binds undergoes thermal denaturation over the range of 37-40 degrees C. In the present study, we have reacted unfixed cryostat tissue sections with this antibody at successively higher temperatures. We have operationally defined denaturation as the point at which type IV-specific fluorescence is no longer detectable. Under these conditions, the in situ denaturation temperature of this epitope in most basement membranes is 50-55 degrees C. In capillaries and some other small blood vessels the fluorescent signal is still clearly detectable at 60 degrees C, the highest temperature at which we can confidently use this technique. We conclude that the stability of the helical structure of type IV collagen within a basement membrane is considerably greater than it is in solution, and that conformation-dependent monoclonal antibodies can be useful probes for investigations of molecular structure in situ.
机译:为了检查IV型胶原螺旋结构在基膜内原位的热稳定性,我们采用了间接免疫荧光组织化学,方法是使用构象依赖性抗体IV-IA8在逐渐升高的温度下进行。我们以前通过竞争酶联免疫吸附试验观察到,在中性溶液中,该抗体结合的螺旋表位在37-40摄氏度范围内发生热变性。在本研究中,我们使未固定的低温恒温器组织切片与此抗体在更高的温度下连续运行。我们已将变性定义为不再可检测到IV型荧光的点。在这些条件下,该表位在大多数基底膜中的原位变性温度为50-55摄氏度。在毛细管和其他一些小血管中,仍可以在60摄氏度(我们可以达到的最高温度)下清晰地检测到荧光信号。放心地使用这项技术。我们得出的结论是,基底膜中IV型胶原螺旋结构的稳定性比溶液中的稳定性要好得多,而且构象依赖性单克隆抗体可以作为用于原位分子结构研究的有用探针。

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