The familial mediterranean fever protein interacts and colocalizes with a putative Golgi transporter.

X. Chen, Y. Bykhovskaya, N. Tidow, M. Hamon, Z. Bercovitz, O. Spirina, N. Fischel‐Ghodsian
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引用次数: 24

Abstract

The biological function of pyrin, the protein mutated in Familial Mediterranean Fever (FMF), has not been elucidated. Based on sequence homology, a transcription factor activity was proposed for this neutrophil-specific protein. In a yeast two-hybrid assay, neither transcription activation activity nor any self interaction was detected for pyrin. Screening of an expression cDNA library of peripheral blood leukocytes using as bait the carboxyl portion of pyrin (amino acids 557-781), which contains most of the FMF mutations, led to the identification of P/M-IP1 (pyrin/marenostrin interacting protein 1). A splice variant of P/M-IP1, GTC-90, had previously been described as a component of the 13S hetero-oligomeric protein complex that stimulates in vitro Golgi transport. We have now shown that P/M-IP1 colocalizes with pyrin in the perinuclear cytoplasm of Cos-7 cells and that the interaction between these two proteins is impaired by FMF causing mutations in pyrin. These data suggest that, at some stage of its functional pathway, pyrin resides in the cytoplasm and might be involved in, or impacted by, cellular protein sorting by the Golgi apparatus. The data also imply that P/M-IP1 may be involved in the abnormal inflammatory response that occurs in patients with FMF.
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家族性地中海热蛋白与假定的高尔基转运蛋白相互作用并共定位。
家族性地中海热(FMF)突变蛋白pyrin的生物学功能尚未阐明。基于序列同源性,提出了该中性粒细胞特异性蛋白的转录因子活性。在酵母双杂交实验中,既没有转录激活活性,也没有检测到pyrin的任何自相互作用。筛选含有大多数FMF突变的pyrin羧基部分(557-781氨基酸)的外周血白细胞表达cDNA文库,鉴定出P/M-IP1 (pyrin/marenostrin相互作用蛋白1)。P/M-IP1的一个剪接变体GTC-90,之前被描述为13S异聚寡聚蛋白复合物的一个组成部分,刺激体外高尔基转运。我们现在已经证明,在Cos-7细胞的核周细胞质中,P/M-IP1与pyrin共定位,并且这两种蛋白之间的相互作用被FMF引起的pyrin突变破坏。这些数据表明,在其功能途径的某些阶段,pyrin驻留在细胞质中,并可能参与或受高尔基体细胞蛋白质分选的影响。这些数据还表明,P/M-IP1可能参与了FMF患者发生的异常炎症反应。
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