Pharmacological chaperones increase residual β-galactocerebrosidase activity in fibroblasts from Krabbe patients.

[krabbe disease]

Krabbe disease or globoid cell leukodystrophy is a degenerative , lysosomal storage disease resulting from the deficiency of β-galactocerebrosidase activity . This enzyme catalyzes the lysosomal hydrolysis of galactocerebroside and psychosine . Krabbe disease is inherited as an autosomal recessive trait , and many of the 70 disease-causing mutations identified in the GALC gene are associated with protein misfolding . Recent studies have shown that enzyme inhibitors can sometimes translocate misfolded polypeptides to their appropriate target organelle bypassing the normal cellular quality control machinery and resulting in enhanced activity . In search for pharmacological chaperones that could rescue the β-galactocerebrosidase activity , we investigated the effect of α-Lobeline or 3 ',4 ',7 -trihydroxyisoflavone on several patient-derived fibroblast cell lines carrying missense mutations , rather than on transduced cell lines . Incubation of these cell lines with α-lobeline or 3 ',4 ',7 -trihydroxyisoflavone leads to an increase of β-galacocerebrosidase activity in p .G 553 R + p .G 553 R , in p .E 130 K + p .N 295 T and in p .G 57 S + p .G 57 S mutant forms over the critical threshold . The low but sustained expression of β-galactocerebrosidase induced by these compounds is a promising result ; in fact , it is known that residual enzyme activity of only 15 -20 % is sufficient for clinical efficacy . The molecular interaction of the two chaperones with β-galactocerebrosidase is also supported by in silico analysis . Collectively , our combined in silico-in vitro approach indicate α-lobeline and 3 ',4 ',7 -trihydroxyisoflavone as two potential pharmacological chaperones for the treatment or improvement of quality of life in selected Krabbe disease patients .