INV SUPERIOR JUBILADO
SEILICOVICH Adriana
artículos
Título:
Dopamine-induced apoptosis of lactotropes is mediated by the short isoform of D2 receptor
Autor/es:
D. B. RADL; J. FERRARIS; V. BOTI; A. SEILICOVICH; D.K.SARKAR; D. PISERA
Revista:
PLOS ONE
Editorial:
PUBLIC LIBRARY SCIENCE
Referencias:
Año: 2011 vol. 6 p. 18097 - 18097
ISSN:
1932-6203
Resumen:
Dopamine, through D2 receptor (D2R), is the major regulator of lactotrope function in the anterior pituitary gland. Both D2R
isoforms, long (D2L) and short (D2S), are expressed in lactotropes. Although both isoforms can transduce dopamine signal,
they differ in the mechanism that leads to cell response. The administration of D2R agonists, such as cabergoline, is the
main pharmacological treatment for prolactinomas, but resistance to these drugs exists, which has been associated with
alterations in D2R expression. We previously reported that dopamine and cabergoline induce apoptosis of lactotropes in
primary culture in an estrogen-dependent manner. In this study we used an in vivo model to confirm the permissive action
of estradiol in the apoptosis of anterior pituitary cells induced by D2R agonists. Administration of cabergoline to female rats
induced apoptosis, measured by Annexin-V staining, in anterior pituitary gland from estradiol-treated rats but not from
ovariectomized rats. To evaluate the participation of D2R isoforms in the apoptosis induced by dopamine we used
lactotrope-derived PR1 cells stably transfected with expression vectors encoding D2L or D2S receptors. In the presence of
estradiol, dopamine induced apoptosis, determined by ELISA and TUNEL assay, only in PR1-D2S cells. To study the role of
p38 MAPK in apoptosis induced by D2R activation, anterior pituitary cells from primary culture or PR1-D2S were incubated
with an inhibitor of the p38 MAPK pathway (SB203850). SB203580 blocked the apoptotic effect of D2R activation in
lactotropes from primary cultures and PR1-D2S cells. Dopamine also induced p38 MAPK phosphorylation, determined by
western blot, in PR1-D2S cells and estradiol enhanced this effect. These data suggest that, in the presence of estradiol, D2R
agonists induce apoptosis of lactotropes by their interaction with D2S receptors and that p38 MAPK is involved in this
process.