Publication | Open Access
Lactonase Activity and Lipoprotein‐Phospholipase A<sub>2</sub> as Possible Novel Serum Biomarkers for the Differential Diagnosis of Autism Spectrum Disorders and Rett Syndrome: Results from a Pilot Study
22
Citations
33
References
2017
Year
Rett syndrome (RTT) and autism spectrum disorders (ASDs) are not merely expression of brain dysfunction but also reflect the perturbation of physiological/metabolic homeostasis. Accordingly, both disorders appear to be associated with increased vulnerability to toxicants produced by redox imbalance, inflammation, and pollution, and impairment of systemic-detoxifying agents could play a role in the exacerbation of these detrimental processes. To check this hypothesis, the activities of two mechanistically related blood-based enzymes, paraoxonase-1 (arylesterase, paraoxonase, and lactonase), and lipoprotein-associated phospholipase A<sub>2</sub> (Lp-PLA<sub>2</sub>) were measured in the serum of 79 ASD and 95 RTT patients, and 77 controls. Lactonase and Lp-PLA<sub>2</sub> showed a similar trend characterized by significantly lower levels of both activities in ASD compared to controls and RTT (<i>p</i> < 0.001 for all pairwise comparisons). Noteworthy, receiving operator curve (ROC) analysis revealed that lactonase and, mostly, Lp-PLA<sub>2</sub> were able to discriminate between ASD and controls (lactonase: area under curve, AUC = 0.660; Lp-PLA<sub>2</sub>, AUC = 0.780), and, considering only females, between ASD and RTT (lactonase, AUC = 0.714; Lp-PLA<sub>2</sub>, AUC = 0.881). These results suggest that lactonase and, especially, Lp-PLA<sub>2</sub> activities might represent novel candidate biomarkers for ASD.
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