Brackett J C, Sims H F, Rinaldo P, Shapiro S, Powell C K, Bennett M J, Strauss A W
Department of Medicine, Washington University School of Medicine, St. Louis, Missouri, USA.
J Clin Invest. 1995 May;95(5):2076-82. doi: 10.1172/JCI117894.
Human trifunctional protein catalyzes three steps in mitochondrial beta-oxidation of fatty acids, including the long chain 3-hydroxyacyl-CoA dehydrogenase step. Deficiency of this heterocomplex, which contains 4 alpha and 4 beta subunits, causes sudden unexplained infant death, a Reye-like syndrome, cardiomyopathy, or skeletal myopathy. We determined the molecular basis of this deficiency in a patient with neonatal presentation and later sudden death using reverse transcription and PCR amplification of his alpha subunit mRNA. We demonstrated a universal deletion of exon 3 (71 bp) in his mRNA. This deletion causes a frameshift and very early premature termination. Amplification of genomic DNA demonstrated that the patient was a compound heterozygote with two different mutations in the 5' donor splice site following exon 3: a paternally inherited G to A transversion at the invariant position +1 and a maternally inherited A to G mutation at position +3. Both allelic mutations apparently cause exon 3 skipping, resulting in undetectable levels of alpha subunit protein, and complete loss of trifunctional protein. This is the initial molecular characterization of trifunctional protein deficiency.
人类三功能蛋白催化脂肪酸线粒体β-氧化过程中的三个步骤,包括长链3-羟酰基辅酶A脱氢酶步骤。这种由4个α亚基和4个β亚基组成的异源复合物的缺乏会导致不明原因的婴儿猝死、类瑞氏综合征、心肌病或骨骼肌病。我们使用逆转录和对患者α亚基mRNA进行PCR扩增的方法,确定了一名新生儿期发病并随后猝死患者这种缺乏症的分子基础。我们在其mRNA中证实了外显子3(71bp)的普遍缺失。这种缺失导致移码和非常早的提前终止。基因组DNA扩增表明该患者是复合杂合子,在外显子3后的5'供体剪接位点有两个不同的突变:父亲遗传的在不变位置+1处的G到A颠换和母亲遗传的在位置+3处的A到G突变。两个等位基因突变显然都导致外显子3跳跃,导致α亚基蛋白水平检测不到,以及三功能蛋白完全缺失。这是三功能蛋白缺乏症的首次分子特征描述。
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