Preclinical diagnosis and carrier detection in ataxia associated with abnormalities of lipoamide dehydrogenase

Abstract

To see whether kinetic assays of lipoamide dehydrogenase could be used for carrier detection or preclinical diagnosis, Michaelis-Menten constants (Km_L and Km_H) for the enzyme were determined in platelets from families with a form of recessive Friedreich ataxia and low activities of the enzyme. The Km_L of patients' enzyme was 132 ± 5 μM lipoamide (mean ± SEM) versus 56 ± 9 μM for controls (p < 0.001), and Km_H for the patients was 421 ± 19 μM versus 147 ± 14 μM for the controls (p < 0.001). The activity and Km values of one patient's enzyme were abnormal 1 year before neurologic signs appeared. The Km values for the enzymes of the six parents were also elevated (average Km_L, 105 ± 10 μM; average Km_H, 378 ± 47 μM, p < 0.02). The maximal activities of the parents' enzymes, relative to a mitochondrial marker, were intermediate between the mean maximal control activity and the mean activity for the affected offspring. The data suggest that the abnormalities of lipoamide dehydrogenase are inherited in a recessive pattern in these families.