Diagnosis of lysosomal storage disorders: evaluation of lysosome-associated membrane protein LAMP-1 as a diagnostic marker

Author:

Meikle Peter J,Brooks Doug A,Ravenscroft Elaine M,Yan Miao,Williams Ruth E1,Jaunzems Alvis E1,Chataway Timothy K,Karageorgos Litsa E,Davey Richard C,Boulter Christine D,Carlsson Sven R2,Hopwood John J

Affiliation:

1. Lysosomal Diseases Research Unit, Departments of Chemical Pathology and Histopathology, Women’s and Children’s Hospital, 72 King William Rd., North Adelaide, South Australia, 5006, Australia

2. Department of Medical Biochemistry and Biophysics, Umea University, Umea, S-901 87, Sweden

Abstract

AbstractEarly diagnosis of lysosomal storage disorders (LSDs), before the onset of irreversible pathologies, will be a key factor in the development of effective therapies for many of these disorders. Newborn screening offers a potential mechanism for the early detection of these disorders. From studies of both normal and LSD-affected human skin fibroblasts we identified the lysosome-associated membrane protein LAMP-1 as a potential diagnostic marker. We have developed a sensitive method for the quantification of this protein with a time-resolved fluorescence immunoassay. A soluble form of LAMP-1 was observed in plasma samples, and determination of 152 unaffected individuals gave a median value of 303 μg/L with the 5th and 95th percentile at 175 and 448 μg/L respectively. Plasma samples from 320 LSD-affected individuals representing 25 different disorders were assayed. We observed that 17 of the 25 disorder groups tested had >88% of individuals above the 95th percentile of the control population, with 12 groups having 100% above the 95th percentile. Overall, 72% of patients had LAMP-1 concentrations above the 95th percentile of the unpartitioned control population. We suggest that LAMP-1 may be a useful marker in newborn screening for LSDs.

Publisher

Oxford University Press (OUP)

Subject

Biochemistry (medical),Clinical Biochemistry

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