首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Microsomal and cytosolic fractions of guinea pig hepatocytes contain 100-kilodalton GTP-binding proteins reactive with antisera against alpha subunits of stimulatory and inhibitory heterotrimeric GTP-binding proteins.
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Microsomal and cytosolic fractions of guinea pig hepatocytes contain 100-kilodalton GTP-binding proteins reactive with antisera against alpha subunits of stimulatory and inhibitory heterotrimeric GTP-binding proteins.

机译:豚鼠肝细胞的微粒体和胞质级分包含100公斤的GTP结合蛋白可与抗血清反应对抗刺激性和抑制性异三聚GTP结合蛋白的α亚基。

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摘要

Guinea pig hepatocytes fractionated by differential centrifugation into plasma membrane-enriched, microsomal, and cytosolic fractions were examined for their content of alpha and beta subunits of heterotrimeric GTP-binding proteins (G proteins) involved in signal transduction. alpha subunits of stimulatory (Gs) and inhibitory (Gi) proteins were detected by immunoblots with antisera reactive with the carboxyl-terminal decapeptide regions of these proteins. Unexpectedly, antisera (including immunopurified) to the alpha subunit but not the beta subunit reacted with a band of 100-kDa proteins in both the microsomal and cytosolic fractions. The immunoreactive 100-kDa proteins are not substrates for ADP-ribosylation catalyzed by pertussis toxin, cholera toxin, or diptheria toxin. Protease digests of the 100-kDa proteins yielded immunoreactive peptides that are distinctly different from those obtained from protease digests of alpha subunits of heterotrimeric G proteins. The 100-kDa protein(s) reactive with antisera to Gi alpha subunit bind to GTP-agarose but not to ATP-agarose. It is concluded that the immunoreactive 100-kDa proteins in microsomal and cytosolic fractions are structurally distinct G proteins from those linked to receptors in the plasma membrane and other G proteins such as elongation factor 2. Conceivably, the 100-kDa proteins represent a new class of G proteins.
机译:通过差速离心将豚鼠肝细胞分为富含血浆膜的微粒体和胞质组分,检查它们参与信号转导的异三聚体GTP结合蛋白(G蛋白)的α和β亚基含量。刺激性(Gs)和抑制性(Gi)蛋白的α亚基通过具有与这些蛋白的羧基末端十肽区域反应性的抗血清的免疫印迹进行检测。出乎意料的是,针对α亚基的抗血清(包括免疫纯化)而非β亚基与微粒体和胞质级分中的100 kDa蛋白带反应。免疫反应性100 kDa蛋白不是百日咳毒素,霍乱毒素或白喉毒素催化的ADP-核糖基化的底物。 100 kDa蛋白的蛋白酶消化产生的免疫反应性肽与异源三聚体G蛋白的α亚基的蛋白酶消化获得的肽明显不同。与抗血清对Gi alpha亚基反应的100 kDa蛋白与GTP-琼脂糖结合,但不与ATP-琼脂糖结合。结论是,微粒体和胞质组分中具有免疫反应性的100 kDa蛋白是结构上不同于与质膜受体和其他G蛋白(例如延伸因子2)相连的G蛋白。可以想象,100 kDa蛋白代表了一个新类别G蛋白。

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