首页> 美国卫生研究院文献>Journal of Lipid Research >Coexpression of novel furin-resistant LPL variants with lipase maturation factor 1 enhances LPL secretion and activity
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Coexpression of novel furin-resistant LPL variants with lipase maturation factor 1 enhances LPL secretion and activity

机译:新型抗弗林蛋白酶的LPL变体与脂肪酶成熟因子1的共表达增强LPL的分泌和活性

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摘要

LPL is a secreted enzyme that hydrolyzes triglycerides from circulating lipoproteins. Individuals lacking LPL suffer from severe hypertriglyceridemia, a risk factor for acute pancreatitis. One potential treatment is to administer recombinant LPL as a protein therapeutic. However, use of LPL as a protein therapeutic is limited because it is an unstable enzyme that is difficult to produce in large quantities. Furthermore, these considerations also limit structural and biochemical studies that are needed for large-scale drug discovery efforts. We demonstrate that the yield of purified LPL can be dramatically enhanced by coexpressing its maturation factor, LMF1, and by introducing novel mutations into the LPL sequence to render it resistant to proteolytic cleavage by furin. One of these mutations introduces a motif for addition of an linked glycan to the furin-recognition site. Furin-resistant LPL has previously been reported, but is not commonly used. We show that our modifications do not adversely alter LPL’s enzymatic activity, stability, or in vivo function. Together, these data show that furin-resistant LPL is a useful reagent for both biochemical and biomedical studies.
机译:LPL是一种分泌的酶,可以水解循环脂蛋白中的甘油三酸酯。缺乏LPL的人患有严重的高甘油三酸酯血症,这是急性胰腺炎的危险因素。一种潜在的治疗方法是将重组LPL用作蛋白质治疗剂。但是,LPL作为蛋白质治疗剂的用途受到限制,因为它是一种不稳定的酶,难以大量生产。此外,这些考虑因素还限制了大规模药物发现工作所需的结构和生化研究。我们证明,通过共表达其成熟因子LMF1,并通过向LPL序列中引入新的突变以使其对弗林蛋白酶的蛋白水解切割具有抗性,可以显着提高纯化LPL的产量。这些突变之一引入了将连接的聚糖添加至弗林蛋白酶识别位点的基序。耐弗林蛋白酶的LPL已有报道,但并不常用。我们证明我们的修饰不会不利地改变LPL的酶活性,稳定性或体内功能。总之,这些数据表明耐弗林蛋白酶的LPL对于生化和生物医学研究都是有用的试剂。

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