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Department of Pathology and Cell Biology, Faculty of Medicine, University of Montréal, Montréal, Québec, Canada H3T 1J4
Address all correspondence and requests for reprints to: Dr. María L. Vitale, Département Pathologie et Biologie Cellulaire, Faculté de Médecine, Université de Montréal, 2900 boulevard Édouard-Montpetit, Montréal, Quebéc, Canada H3T 1J4. E-mail: vitalem{at}ere.umontreal.ca
The participation of the actin cytoskeleton in the control of PRL
secretion by dopamine (DA) is not yet fully understood. Recently, we
demonstrated that DA induces cortical actin assembly and stabilization
in anterior pituitary PRL-secreting cells (lactotropes) that can be
linked to DA-induced inhibition of PRL secretion. Here we show that DA
prevents cell flattening and the formation of cytoplasmic actin cables
in cultured rat lactotropes. The effects of DA were reversible,
mediated by D2 receptors, exclusive to lactotropes, and independent of
other anterior pituitary cells present in the cultures. Because cAMP
and Ca2+ mediate DA-induced inhibition of PRL secretion and
synthesis, we investigated whether morphological responses to DA were
dependent on these second messengers. Either inhibition of protein
kinase A activity with the specific inhibitor KT5720 or blockade of
Ca2+ channels with nifedipine inhibited cell flattening and
induced cytoplasmic actin filament breakdown. Nifedipine was as
effective as DA, but KT5720 was less effective than DA. Increased
intracellular cAMP levels provoked cell flattening, which was blocked
by nifedipine and KT5720, but not by DA. The results suggest that
Ca2+-dependent pathways control cell shape in most
lactotropes; however, in a subpopulation of lactotropes, cAMP-dependent
pathways may also contribute to DA morphological responses. Next, we
studied the participation of the Rho family of guanosine
triphosphatases, which is known to regulate the dynamics of actin
filaments. Inactivation of Rho by C3 exoenzyme induced cytoplasmic
actin cable disassembly and lactotrope rounding up. No additive effects
were observed among Rho-, cAMP-, and Ca2+-dependent
pathways. However, C3-induced morphological responses were blocked by
increased cAMP levels, suggesting that Rho-dependent steps are upstream
cAMP-dependent steps. DA-induced actin cytoskeleton reorganization in
lactotropes may involve modifications in the expression and
localization of actin-binding proteins. DA increased expression of the
actin anchoring proteins talin and 
-actinin, but not of vinculin. DA
enhanced association of talin to cell membranes. Increased
talin-membrane interaction may be implicated in DA-induced maintenance
of a round phenotype in lactotrope cells.
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