Restoration of nuclear-import failure caused by triple A syndrome and oxidative stress.

[triple a syndrome]

Triple A syndrome is an autosomal recessive neurological disease , mimicking motor neuron disease , and is caused by mutant ALADIN , a nuclear-pore complex component . We recently discovered that the pathogenesis involved impaired nuclear import of DNA repair proteins , including DNA ligase I and the cerebellar ataxia causative protein aprataxin . Such impairment was overcome by fusing classical nuclear localization signal (NLS ) and 137 -aa downstream sequence of XRCC 1 , designated stretched NLS (stNLS ). We report here that the minimum essential sequence of stNLS (mstNLS ) is residues 239 -276 , downsized by more than 100 aa . mstNLS enabled efficient nuclear import of DNA repair proteins in patient fibroblasts , functioned under oxidative stress , and reduced oxidative-stress-induced cell death , more effectively than stNLS . The stress-tolerability of mstNLS was also exerted in control fibroblasts and neuroblastoma cells . These findings may help develop treatments for currently intractable triple A syndrome and other oxidative-stress-related neurological diseases , and contribute to nuclear compartmentalization study .

Diseases
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Diseases presenting "impaired nuclear import of dna repair proteins" symptom

triple a syndrome

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