Chromogranin A, an “On/Off” Switch Controlling Dense-Core Secretory Granule Biogenesis

We present evidence that regulation of dense-core secretory granule biogenesis and hormone secretion in endocrine cells is dependent on chromogranin A (CGA). Downregulation of CGA expression in a neuroendocrine cell line, PC12, by antisense RNAs led to profound loss of dense-core secretory granules,...

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Veröffentlicht in:Cell 2001-08, Vol.106 (4), p.499-509
Hauptverfasser: Kim, Taeyoon, Tao-Cheng, Jung-Hwa, Eiden, Lee E., Loh, Y.Peng
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Sprache:eng
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Zusammenfassung:We present evidence that regulation of dense-core secretory granule biogenesis and hormone secretion in endocrine cells is dependent on chromogranin A (CGA). Downregulation of CGA expression in a neuroendocrine cell line, PC12, by antisense RNAs led to profound loss of dense-core secretory granules, impairment of regulated secretion of a transfected prohormone, and reduction of secretory granule proteins. Transfection of bovine CGA into a CGA-deficient PC12 clone rescued the regulated secretory phenotype. Stable transfection of CGA into a CGA-deficient pituitary cell line, 6T3, lacking a regulated secretory pathway, restored regulated secretion. Overexpression of CGA induced dense-core granules, immunoreactive for CGA, in nonendocrine fibroblast CV-1 cells. We conclude that CGA is an “on/off” switch that alone is sufficient to drive dense-core secretory granule biogenesis and hormone sequestration in endocrine cells.
ISSN:0092-8674
1097-4172
DOI:10.1016/S0092-8674(01)00459-7