Abstract EN:

Lysosomal storage diseases are a group of 50 genetically inherited disorders that are characterized by a deficiency of one or more specific lysosomal enzymes which causes an accumulation of substrates inside the lysosome. Enzyme replacement therapy consists in the targeting of recombinant enzymes through the cation-independent mannose 6-phosphate receptor (CI-M6PR) transport. CI-M6PR allows the transport of enzymes carrying the M6P marker towards the lysosomes. The main drawback with the M6P recognition marker is its sensitivity to hydrolysis by phosphatases. Therefore, isosteric analogues of M6P functionalized at the anomeric position by different spacer arms were synthesized. The biological evaluation of these analogues revealed that they are stable in human serum and are recognized by CI-M6PR as well as the M6P itself. Additional studies on living cells showed that none of the prepared analogues is cytotoxic. The conjugation of AMFA-1 to the cathepsin D-KDEL low affinity mutant induced a 10-fold increase of its affinity for the CI-M6PR. The enzymatic activity of chemically modified cathepsin D-KDEL was found fully maintained.