人睫状肌细胞对FP类前列腺素类似物的反应:磷酸肌醇水解、细胞内钙离子动员和丝裂原活化蛋白激酶激活。
Human ciliary muscle cell responses to FP-class prostaglandin analogs: phosphoinositide hydrolysis, intracellular Ca2+ mobilization and MAP kinase activation.
作者信息
Sharif Naj A, Crider Julie Y, Husain Shahid, Kaddour-Djebbar Ismail, Ansari Habib R, Abdel-Latif Ata A
机构信息
Molecular Pharmacology Unit, Alcon Research, Ltd., Fort Worth, TX 76134-2099, USA.
出版信息
J Ocul Pharmacol Ther. 2003 Oct;19(5):437-55. doi: 10.1089/108076803322473006.
Phospholipase C induced phosphoinositide (PI) turnover, intracellular Ca(2+) (Ca(2+)) mobilization and mitogen-activated protein (MAP) kinase activation by FP-class prostaglandin analogs was studied in normal human ciliary muscle (h-CM) cells. Agonist potencies obtained in the PI turnover assays were: travoprost acid ((+)-fluprostenol; EC(50) = 2.6 +/- 0.8 nM) > bimatoprost acid (EC(50) = 3.6 +/- 1.2 nM) > (+/-)-fluprostenol (EC(50) = 4.3 +/- 1.3 nM) >> prostaglandin F(2 alpha) (PGF(2 alpha)) (EC(50) = 134 +/- 17 nM) > latanoprost acid (EC(50) = 198 +/- 83 nM) > S-1033 (EC(50) = 2930 +/- 1420 nM) > unoprostone (EC(50) = 5590 +/- 1490 nM) > bimatoprost (EC(50) = 9600 +/- 1100 nM). Agonist potencies in h-CM cells correlated well with those previously obtained for the cloned human ciliary body-derived FP receptor (r = 0.96, p< 0.001) and that present on h-TM cells (r = 0.94, p< 0.0001). Travoprost acid, PGF(2 alpha) and unoprostone also stimulated Ca(2+) mobilization in h-CM cells with travoprost acid being the most potent agonist. MAP kinase activity was stimulated in the h-CM cells with the following rank order of activity (at 100 nM): travoprost acid > PGF(2 alpha) > latanoprost acid > PGD(2) > bimatoprost > latanoprost = bimatoprost acid = fluprostenol > PGE(2) = S-1033 > unoprostone > PGI(2). The PI turnover, Ca(2+) mobilization and MAP kinase activation induced by several of these agonists was blocked by the FP receptor antagonist, AL-8810 (11 beta-fluoro-15-epiindanyl PGF(2 alpha)) (e.g. K(i) = 5.7 microM versus PI turnover). These studies have characterized the biochemical and pharmacological properties of the native FP prostaglandin receptor present on h-CM cells using three signal transduction mechanism assays and a broad panel of FP-class agonist analogs (including free acids of bimatoprost, travoprost and latanoprost) and the FP receptor antagonist, AL-8810.
在正常人睫状肌(h-CM)细胞中研究了磷脂酶C诱导的磷酸肌醇(PI)周转、细胞内Ca(2+)(Ca(2+))动员以及FP类前列腺素类似物对丝裂原活化蛋白(MAP)激酶的激活作用。在PI周转试验中获得的激动剂效力顺序为:曲伏前列酸((+)-氟前列醇;EC(50) = 2.6 ± 0.8 nM)> 比马前列酸(EC(50) = 3.6 ± 1.2 nM)> (+/-)-氟前列醇(EC(50) = 4.3 ± 1.3 nM)>> 前列腺素F(2α)(PGF(2α))(EC(50) = 134 ± 17 nM)> 拉坦前列酸(EC(50) = 198 ± 83 nM)> S-1033(EC(50) = 2930 ± 1420 nM)> 乌诺前列酮(EC(50) = 5590 ± 1490 nM)> 比马前列素(EC(50) = 9600 ± 1100 nM)。h-CM细胞中的激动剂效力与先前在克隆的人睫状体来源的FP受体上获得的效力相关性良好(r = 0.96,p < 0.001),与h-TM细胞上的效力相关性也良好(r = 0.94,p < 0.0001)。曲伏前列酸、PGF(2α)和乌诺前列酮也刺激h-CM细胞中的Ca(2+)动员,其中曲伏前列酸是最有效的激动剂。h-CM细胞中的MAP激酶活性受到刺激,活性顺序如下(在100 nM时):曲伏前列酸 > PGF(2α) > 拉坦前列酸 > PGD(2) > 比马前列素 > 拉坦前列素 = 比马前列酸 = 氟前列醇 > PGE(2) = S-1033 > 乌诺前列酮 > PGI(2)。几种这些激动剂诱导的PI周转、Ca(2+)动员和MAP激酶激活被FP受体拮抗剂AL-8810(11β-氟-15-表吲哚基PGF(2α))阻断(例如,相对于PI周转,K(i) = 5.7 μM)。这些研究使用三种信号转导机制测定法以及一系列广泛的FP类激动剂类似物(包括比马前列素、曲伏前列素和拉坦前列素的游离酸)和FP受体拮抗剂AL-8810,对h-CM细胞上天然FP前列腺素受体的生化和药理学特性进行了表征。
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