Neuronal Developmental Marker FORSE-1 Identifies a Putative Progenitor of the Pulmonary Neuroendocrine Cell Lineage During Lung Development

Journal of Histochemistry and Cytochemistry

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ARTICLE

Neuronal Developmental Marker FORSE-1 Identifies a Putative Progenitor of the Pulmonary Neuroendocrine Cell Lineage During Lung Development

Jie Pan^a, Herman Yeger^a, and Ernest Cutz^a
^a Department of Paediatric Laboratory Medicine and Research Institute and Laboratory Medicine and Pathobiology, Hospital for Sick Children and University of Toronto, Toronto, Ontario, Canada

Correspondence to: Herman Yeger, Dept. of Paediatric Laboratory Medicine, The Hospital for Sick Children, 555 University Avenue, Toronto, Ontario M5G 1X8, Canada. E-mail: hermie@sickkids.on.ca

The FORSE-1 (forebrain-surface-embryonic) monoclonal antibody(MAb) recognizes a carbohydrate cell surface epitope relatedto the Lewis-X (LeX) and stage-specific embryonic antigens (SSEAs).In the developing CNS, the FORSE-1 epitope is believed to serveas a marker of progenitor cells. We studied the expression ofthe FORSE-1 epitope in pulmonary neuroendocrine cells (PNECs)and related neuroepithelial bodies (NEBs), cell types implicatedin paracrine regulation of lung development. We used dual immunolabelingto identify PNECs/NEBs in tissue sections from developing rabbitfetal lungs and corresponding primary lung cell cultures. Duringthe early stage (E16), the FORSE-1 MAb labeled primitive airwayepithelium, whereas serotonin (5HT) immunoreactivity, a markerof PNEC/NEB differentiation, was negative. After E18, FORSE-1labeling became restricted to PNECs and NEBs, identified byco-expression with 5HT, then decreased coincident with an increasein 5HT. Expression of the FORSE-1 epitope correlated inverselywith 5HT expression in PNEC/NEB cells. FORSE-1 immunoreactivitycorrelated with cell proliferation assessed by BrdU labeling.Downregulation of the FORSE-1 epitope correlated with maturationof PNECs/NEBs. The presence of few FORSE-1/5HT-positive cellsin postnatal lung suggests retention of progenitors. The FORSE-1epitope was associated with a high molecular weight (286 kD)glycoprotein that decreased with increasing gestational age,as demonstrated by immunoblotting. Overall expression of SSEA-1,-3, and -4 antigens was similar to FORSE-1/5HT, although theformer was preferentially localized to neurite-like processes.Because the role of the FORSE-1 epitope in the CNS probablyinvolves cell adhesion and differentiation, we propose a similarfunction in developing lung. The demonstration of LeX/SSEA antigenexpression in the PNEC/NEB cell lineage underscores the importanceof these cells in developing lung. Furthermore, the FORSE-1antigen may identify committed progenitors of the PNEC/NEB cellsystem. (J Histochem Cytochem 50:1567–1578, 2002)

Key Words: FORSE-1, stage-specific embryonic, antigens, Lewis antigens,pulmonary neuroendocrine, cells, neuroepithelial bodies, neuroendocrinedifferentiation, lung development

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