✦ LIBER ✦

Developmental regulation of human truncated nerve growth factor receptor

✍ Scribed by Dr Peter S. DiStefano; Margaret Clagett-Dame; Diane M. Chelsea; Rebekah Loy

Publisher: John Wiley and Sons
Year: 1991
Tongue: English
Weight: 739 KB
Volume: 29
Category: Article
ISSN: 0364-5134
DOI: 10.1002/ana.410290105

No coin nor oath required. For personal study only.

✦ Synopsis

Monoclonal antibodies (designated XIFl and IIIG5) recognizing distinct epitopes of the human truncated nerve growth factor receptor (NGF-Rt) were used in a two-site radiometric immunosorbent assay to monitor levels of NGF-Rt in human urine as a function of age. Urine samples were collected from 70 neurologically normal subjects ranging in age from 1 month to 68 years. By using this sensitive two-site radiometric immunosorbent assay, NGF-Rt levels were found to be highest in urine from 1-month old subjects. By 2.5 months, NGF-Rt values were half of those seen at 1 month and decreased more gradually between 0.5 and 15 years. Between 15 and 68 years, urine NGF-Rt levels were relatively constant at 5% of 1-month values. No evidence for diurnal variation of adult NGF-Rt was apparent. Pregnant women in their third trimester showed significantly elevated urine NGF-Rt values compared with agematched normals. Affinity labeling of NGF-Rt with lZ5I-NGF followed by immunoprecipitation with ME20.4-IgG and gel autoradiography indicated that neonatal urine contained high amounts of truncated receptor (Mr = 50 kd); decreasingly lower amounts of NGF-Rt were observed on gel autoradiograms with development, indicating that the two-site radiometric immunosorbent assay correlated well with the affinity labeling technique for measuring NGF-Rt. NGF-Rt in urines from I-month-old and 36-year-old subjects showed no differences in affinities for NGF or for the monoclonal antibody IIIG5. These data show that NGF-Rt is developmentally regulated in human urine, and are discussed in relation to the development and maturation of the peripheral nervous system. The results obtained in this study establish the basis for studying NGF-Rt regulation during the course of abnormal development, regeneration, and neurodegeneration.

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