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Prostaglandin E1 and dibutyryl cyclic AMP enhance platelet resistance to deformation.
Authors:D L Wang  Y N Chang  H T C Hsu  S Usami and S Chien
Institution:

a Institute of Biomedical Sciences, Academia Sinica, Taipei, Taiwan, ROC

b Departments of Applied Mechanics and Engineering Sciences (Bioengineering) and Medicine, University of California, San Diego, La Jolla, Calif, USA

Abstract:The effect of prostaglandin E1 (PGE1) on platelets is mediated through the PGE1 receptor and the consequent maintenance of the platelet's discoid shape. The effects of PGE1 and dibutyryl cAMP (dbcAMP) on the deformability of human platelets were studied. Deformability tests based upon the micropipette aspiration on the platelets were performed by using pipettes with radii (Rp) of 0.26-0.36 gm. The time course of the extension length (Dp, in μg) of the platelets in response to aspiration with a negative pressure (ΔP) of 5 cm H2 O (ΔP × Rp = 0.15 dynes/cm) was analyzed. PGE1 treatment (0.1 μM) resulted in a decrease of platelet deformability as compared with results obtained for apparently non-activated, control platelets. The deformation index, i.e., Dp/Rp (PGE1 -treated) / Dp/Rp (control), was significantly reduced to 0.90 ± 0.04. DbcAMP treatment also significantly decreased the deformability of platelets and this decrease was dbcAMP dose dependent. In contrast, colchicine- or cytochalasin D-treated platelets increased deformability. PGE1 -treated platelets had a higher cAMP]i than controls. Platelets treated with PGE1 or dbcAMP showed a reduced Ca2+]i increment induced by thrombin as compared to non-treated controls. These results indicate that PGE1 and dbcAMP treatment of platelets is accompanied by an enhancement of platelet resistance to deformation. The increased cAMP]i and low Ca2+]i after PGE1 treatment may limit the rearrangement of cytoskeleton and thus enhance platelet resistance to deformation.
Keywords:Author Keywords: Platelet deformability  Prostaglandin E1  cAMP
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