| الوصف: |
Gaucher disease, the most common lysosomal storage disorder, is caused by mutations in the GBA gene which codes for the enzyme glucocerebrosidase (GCase) resulting in its deficiency. GCase deficiency results in the accumulation of its substrate glucosylceramide (GlcCer) within the lysosomes leading to various severities of hepatosplenomegaly, bone disease and neurodegeneration. For most forms of Gaucher disease, the mutations in the GBA gene cause the enzyme to misfold but retain catalytic activity. However, the misfolded mutant enzyme is recognized and degraded by the endoplasmic reticulum-associated degradation (ERAD) pathway prior to delivery into the lysosome. Symptoms begin to show in patients when the function of the defective enzyme drops below 10-20% residual enzyme activity. There are currently three therapeutic approaches to treat Gaucher disease: enzyme replacement therapy (ERT), substrate reduction therapy (SRT), and a relatively recent addition, enzyme enhancement therapy (EET) through the use of pharmacological chaperones. Many pharmacological chaperones are competitive inhibitors that are capable of enhancing lysosomal GCase activity by stabilizing the folded conformation of GCase enabling it to bypass the ERAD pathway. Once the mutant enzyme enters the lysosome, high levels of GlcCer can outcompete the competitive inhibitor binding to the enzyme, thus partially restoring the hydrolytic pathway. For this thesis, a series of alkylated aminocyclitol derivatives have been synthesized and evaluated as competitive inhibitors of GCase with the intent of discovering specific and efficient pharmacological chaperones for Gaucher disease. Importantly, we have discovered that N,O-alklyated inosamines are potent inhibitors of GCase and therefore are lead compounds as a potential new EET for the treatment of Gaucher Disease. Based on the potency of the alkylated inosamines as reversible inhibitors, we designed and synthesized several alkylated conduritol aziridine inhibitors to be used as mechanism-based ... |
