Masi_2018_Clin.Chem_64_690

Reference

Title : Specific Substrate for the Assay of Lysosomal Acid Lipase - Masi_2018_Clin.Chem_64_690
Author(s) : Masi S , Chennamaneni N , Turecek F , Scott CR , Gelb MH
Ref : Clinical Chemistry , 64 :690 , 2018
Abstract :

BACKGROUND: Deficiency of lysosomal acid lipase (LAL) causes Wolman disease and cholesterol ester storage disease. With the recent introduction of enzyme replacement therapy to manage LAL deficiency comes the need for a reliable assay of LAL enzymatic activity that can be applied to dried blood spots (DBS). METHODS: We prepared and tested a library of analogs of palmitoyl 4-methylumbelifferyl esters to find a highly active and specific substrate for LAL in DBS. The LAL assay was optimized leading to both LC-MS/MS and fluorometric assay of LAL. We tested the new assay on DBS from healthy and LAL-deficient patients. RESULTS: The ester formed between palmitic acid and 4-propyl-8-methyl-7-hydroxycoumarin (P-PMHC) was found to be >98% selective for LAL in DBS based on the sensitivity of its activity to the LAL-specific inactivator Lalistat-2 and the fact that the activity was close to zero using DBS from patients previously shown to be LAL-deficient. Use of P-PMHC and heavy isotope-labeled internal standard with optimized assay conditions led to an approximately 2-fold increase in the specific activity of LAL compared with the previously reported LAL assay. Patients deficient in LAL were readily distinguished from normal persons with the new LAL assay using UPLC-MS/MS or fluorometric assay platforms. CONCLUSIONS: The new assay can measure LAL in DBS with a single measurement compared with the previous method involving 2 assays done in parallel.

PubMedSearch : Masi_2018_Clin.Chem_64_690
PubMedID: 29339442
Gene_locus related to this paper: human-LIPA

Related information

Inhibitor Lalistat-2
Substrate P-PMHC
Gene_locus human-LIPA

Citations formats

Masi S, Chennamaneni N, Turecek F, Scott CR, Gelb MH (2018)
Specific Substrate for the Assay of Lysosomal Acid Lipase
Clinical Chemistry 64 :690

Masi S, Chennamaneni N, Turecek F, Scott CR, Gelb MH (2018)
Clinical Chemistry 64 :690