Structural bases of GM1 gangliosidosis and Morquio B disease.

[gm1 gangliosidosis]

Allelic mutations of the lysosomal beta -galactosidase gene cause heterogeneous clinical phenotypes , such as GM 1 gangliosidosis and Morquio B disease , the former being further classified into three variants , namely infantile , juvenile and adult forms ; and heterogeneous biochemical phenotypes were shown in these forms . We tried to elucidate the bases of these diseases from a structural viewpoint . We first constructed a three -dimensional structural model of human beta -galactosidase by means of homology modeling . The human beta -galactosidase consists of three domains , such as , a TIM barrel fold domain , which functions as a catalytic domain , and two galactose-binding domain-like fold domains . We then constructed structural models of representative mutant beta -galactosidase proteins (G 123 R , R 201 C , I 51 T and Y 83 H ) and predicted the structural change associated with each phenotype by calculating the number of affected atoms , determining the root-mean-square deviation and the solvent-accessible surface area , and by color imaging . The results show that there is a good correlation between the structural changes caused by amino-acid substitutions in the beta -galactosidase molecule , as well as biochemical and clinical phenotypes in these representative cases . Protein structural study is useful for elucidating the bases of these diseases .

Diseases
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Diseases presenting "heterogeneous biochemical phenotypes" symptom

gm1 gangliosidosis

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