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GENETICALLY ENGINEERED PROBIOTIC E. COLI NISSLE TO CONSUME AMINO ACIDS ASSOCIATED WITH ORPHAN METABOLIC DISEASES

机译:遗传工程化的肠埃希氏大肠杆菌(E. COLI NISSLE)食用与鸦片代谢性疾病相关的氨基酸

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Orphan metabolic diseases are rare genetic defects that interfere with metabolism due to ineffective or missing enzymes. Two of them, Phenylketonuria (PKU) and Maple Syrup Urine Disease (MSUD) are defined by accumulation of amino acids to toxic levels due to defective metabolism of protein break down products. PKU is caused by a defect in the gene encoding phenylalanine hydroxylase (PAH). MSUD is caused by a defect in a multi-enzyme complex found in mitochondria called branched chain a-ketoacid dehydrogenase "BCKDH". Without the activity of these enzymes, the amino acid phenylalanine (Phe) in the case of PKU or the branched-chain amino acids leucine (Leu), isoleucine and valine for MSUD build up to neurotoxic levels in the blood and brain, leading to neurological deficits. Current treatment options focus on dietary protein restriction, are insufficient and, unfortunately, can lead to a failure to thrive. Lifelong compliance with a prescription diet is also a concern. We have genetically engineered Nissle, a probiotic strain of E. coli, to reduce serum phenylalanine and leucine levels in patients with PKU or MSUD; preclinical data supporting the activity of these strains are described.
机译:孤儿代谢疾病是罕见的遗传缺陷,由于无效或缺失的酶而会干扰代谢。它们中的两个,苯丙酮酸尿症(PKU)和枫糖浆尿病(MSUD),是由于蛋白质分解产物代谢不良而将氨基酸积累到有毒水平而定义的。 PKU是由编码苯丙氨酸羟化酶(PAH)的基因缺陷引起的。 MSUD是由线粒体中一种称为支链α-酮酸脱氢酶“ BCKDH”的多酶复合物的缺陷引起的。没有这些酶的活性,对于PKU而言,氨基酸苯丙氨酸(Phe)或MSUD的支链氨基酸亮氨酸(Leu),异亮氨酸和缬氨酸在血液和大脑中积累至神经毒性水平,导致神经系统疾病赤字。当前的治疗选择集中在限制饮食中的蛋白质上,这是不足的,而且不幸的是,这可能会导致ive壮成长。终身遵守处方饮食也是一个问题。我们对大肠杆菌的益生菌Nissle进行了基因改造,以降低PKU或MSUD患者的血清苯丙氨酸和亮氨酸水平;描述了支持这些菌株活性的临床前数据。

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