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Human Serum Amyloid A3 (SAA3) Protein Expressed as a Fusion Protein with SAA2 Binds the Oxidized Low Density Lipoprotein Receptor

机译:表达为与SAA2融合蛋白的人血清淀粉样蛋白A3(SAA3)蛋白与氧化型低密度脂蛋白受体结合

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摘要

Serum amyloid A3 (SAA3) possesses characteristics distinct from the other serum amyloid A isoforms, SAA1, SAA2, and SAA4. High density lipoprotein contains the latter three isoforms, but not SAA3. The expression of mouse SAA3 (mSAA3) is known to be up-regulated extrahepatically in inflammatory responses, and acts as an endogenous ligand for the toll-like receptor 4/MD-2 complex. We previously reported that mSAA3 plays an important role in facilitating tumor metastasis by attracting circulating tumor cells and enhancing hyperpermeability in the lungs. On the other hand, human SAA3 (hSAA3) has long been regarded as a pseudogene, which is in contrast to the abundant expression levels of the other isoforms. Although the nucleotide sequence of hSAA3 is very similar to that of the other SAAs, a single oligonucleotide insertion in exon 2 causes a frame-shift to generate a unique amino acid sequence. In the present study, we identified that hSAA3 was transcribed in the hSAA2-SAA3 fusion transcripts of several human cell lines. In the fusion transcript, hSAA2 exon 3 was connected to hSAA3 exon 1 or hSAA3 exon 2, located approximately 130kb downstream from hSAA2 exon 3 in the genome, which suggested that it is produced by alternative splicing. Furthermore, we succeeded in detecting and isolating hSAA3 protein for the first time by an immunoprecipitation-enzyme linked immune assay system using monoclonal and polyclonal antibodies that recognize the hSAA3 unique amino acid sequence. We also demonstrated that hSAA3 bound oxidized low density lipoprotein receptor (oxLDL receptor, LOX-1) and elevated the phosphorylation of ERK, the intracellular MAP-kinase signaling protein.
机译:血清淀粉样蛋白A3(SAA3)具有不同于其他血清淀粉样蛋白A亚型SAA1,SAA2和SAA4的特征。高密度脂蛋白包含后三种同工型,但不包含SAA3。已知小鼠SAA3(mSAA3)的表达在炎性反应中在肝外上调,并且充当toll样受体4 / MD-2复合体的内源性配体。我们以前曾报道过,mSAA3在吸引循环肿瘤细胞和增强肺部通透性方面,在促进肿瘤转移中起着重要作用。另一方面,长期以来,人SAA3(hSAA3)被视为假基因,这与其他同工型的丰富表达水平形成了鲜明对比。尽管hSAA3的核苷酸序列与其他SAA的核苷酸序列非常相似,但在外显子2中插入单个寡核苷酸会引起移码,从而产生独特的氨基酸序列。在本研究中,我们确定了hSAA3在几种人类细胞系的hSAA2-SAA3融合转录物中转录。在融合转录本中,hSAA2外显子3与基因组中hSAA2外显子3下游约130kb处的hSAA3外显子1或hSAA3外显子2连接,这表明它是通过选择性剪接产生的。此外,我们首次使用识别hSAA3独特氨基酸序列的单克隆和多克隆抗体,通过免疫沉淀-酶联免疫分析系统成功检测和分离了hSAA3蛋白。我们还证明了hSAA3结合了氧化的低密度脂蛋白受体(oxLDL受体,LOX-1)并提高了细胞内MAP激酶信号蛋白ERK的磷酸化。

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