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Human DJ-1 and its homologs are novel glyoxalases.

Human molecular genetics (2012-04-24)
Ju-young Lee, Jeeyeon Song, Kyu Kwon, Sumi Jang, Chayeon Kim, Kwanghee Baek, Jeongho Kim, Chankyu Park
RESUMEN

Human DJ-1 is a genetic cause of early-onset Parkinson's disease (PD), although its biochemical function is unknown. We report here that human DJ-1 and its homologs of the mouse and Caenorhabditis elegans are novel types of glyoxalase, converting glyoxal or methylglyoxal to glycolic or lactic acid, respectively, in the absence of glutathione. Purified DJ-1 proteins exhibit typical Michaelis-Menten kinetics, which were abolished completely in the mutants of essential catalytic residues, consisting of cysteine and glutamic acid. The presence of DJ-1 protected mouse embryonic fibroblast and dopaminergically derived SH-SY5Y cells from treatments of glyoxals. Likewise, C. elegans lacking cDJR-1.1, a DJ-1 homolog expressed primarily in the intestine, protected worms from glyoxal-induced death. Sub-lethal doses of glyoxals caused significant degeneration of the dopaminergic neurons in C. elegans lacking cDJR-1.2, another DJ-1 homolog expressed primarily in the head region, including neurons. Our findings that DJ-1 serves as scavengers for reactive carbonyl species may provide a new insight into the causation of PD.

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Sigma-Aldrich
Glyoxal solution, 40 wt. % in H2O
Sigma-Aldrich
Glyoxal solution, for molecular biology, BioReagent, ~40% in H2O (~8.8 M)