Immunoreactive Levels of α-ketoglutarate Dehydrogenase Subunits in Friedreich's Ataxia and Spinocerebellar Ataxia Type 1

Frank Mastrogiacomo , Jacques LaMarche , Slobodan Dožić , Gordon Lindsay , Lucien Bettendorff , Yves Robitaille , Lawrence Schut , Stephen J. Kish
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引用次数: 37

Abstract

Enzyme activities of α-ketoglutarate dehydrogenase complex (αKGDHC) and one of its constituent subunits, dihydrolipoamide dehydrogenase (E3), are reported to be reduced in non-CNS tissues of some patients with Friedreich's ataxia (FA); however, the results are highly confliicting. To determine whether an enzyme abnormality occurs in brain, we measured immunoreactive levels of the three αKGDHC subunits, namely, α-ketoglutarate dehydrogenase (E1), dihydro-lipoamide succinyltransferase (E2) and E3 in postmortem frontal, occipital and cerebellar cortices of 18 control subjects, 9 patients with FA and, for comparison, 12 patients with spinocerebellar ataxia type 1 (SCA1). Decreased (−20 to −31%) levels of E3 were observed in all three examined areas of the patients with FA with the changes statistically significant in cerebellar and frontal cortices. The E3 reduction could be explained by a loss of αKGDHC or other dehydrogenase complexes (e.g. pyruvate dehydrogenase complex) which utilize this subunit. In SCA1, enzyme changes were limited to E2 in cerebellar (−26%) and frontal (−19%) cortices. Although the E3 and E2 reductions are only slight, and may represent secondary events, the changes in this key Krebs cycle enzyme could exacerbate degenerative processes in both of the spinocerebellar ataxia disorders.

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Friedreich共济失调和1型棘角肌共济失调患者α-酮戊二酸脱氢酶亚单位的免疫反应水平
据报道,在一些弗里德里希共济失调(FA)患者的非中枢神经系统组织中,α-酮戊二酸脱氢酶复合物(αKGDHC)及其组成亚基之一二氢硫酰胺脱氢酶(E3)的酶活性降低;然而,这些结果是高度一致的。为了确定大脑中是否发生酶异常,我们测量了18名对照受试者、9名FA患者和12名脊髓小脑共济失调1型(SCA1)患者死后额叶、枕叶和小脑皮质中三种αKGDHC亚基的免疫反应水平,即α-酮戊二酸脱氢酶(E1)、二氢硫酰胺琥珀酰转移酶(E2)和E3。在FA患者的所有三个检查区域都观察到E3水平下降(−20%至−31%),小脑和额叶皮质的变化具有统计学意义。E3的减少可以通过αKGDHC或利用该亚基的其他脱氢酶复合物(例如丙酮酸脱氢酶复合物)的损失来解释。在SCA1中,小脑皮层(-26%)和额叶皮层(-19%)的酶变化仅限于E2。尽管E3和E2的减少只是轻微的,并且可能代表次要事件,但这种关键的Krebs循环酶的变化可能会加剧这两种脊髓小脑共济失调疾病的退行性过程。
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