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Small mouse cholangiocytes proliferate in response to H1 histamine receptor stimulation by activation of the IP3/CaMK I/CREB pathway

机译：通过激活IP3 / CaMK I / CREB途径，小鼠小胆管细胞响应H1组胺受体刺激而增殖

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Cholangiopathies are characterized by the heterogeneous proliferation of different-sized cholangiocytes. Large cholangiocytes proliferate by a cAMP-dependent mechanism. The function of small cholangiocytes may depend on the activation of inositol trisphosphate (IP3)/Ca2+-dependent signaling pathways; however, data supporting this speculation are lacking. Four histamine receptors exist (HRH1, HRH2, HRH3, and HRH4). In several cells: 1) activation of HRH1 increases intracellular Ca2+ concentration levels; and 2) increased [Ca2+](i) levels are coupled with calmodulin-dependent stimulation of calmodulin-dependent protein kinase (CaMK) and activation of cAMP-response element binding protein (CREB). HRH1 agonists modulate small cholangiocyte proliferation by activation of IP3/Ca2+-dependent CaMK/CREB. We evaluated HRH1 expression in cholangiocytes. Small and large cholangiocytes were stimulated with histamine trifluoromethyl toluidide (HTMT dimaleate; HRH1 agonist) for 24-48 h with/without terfenadine, BAPTA/AM, or W7 before measuring proliferation. Expression of CaMK I, II, and IV was evaluated in small and large cholangiocytes. We measured IP3, Ca2+ and cAMP levels, phosphorylation of CaMK I, and activation of CREB (in the absence/presence of W7) in small cholangiocytes treated with HTMT dimaleate. CaMK I knockdown was performed in small cholangiocytes stimulated with HTMT dimaleate before measurement of proliferation and CREB activity. Small and large cholangiocytes express HRH1, CaMK I, and CaMK II. Small (but not large) cholangiocytes proliferate in response to HTMT dimaleate and are blocked by terfenadine (HRH1 antagonist), BAPTA/AM, and W7. In small cholangiocytes, HTMT dimaleate increased IP3/Ca2+ levels, CaMK I phosphorylation, and CREB activity. Gene knockdown of CaMK I ablated the effects of HTMT dimaleate on small cholangiocyte proliferation and CREB activation. The IP3/Ca2+/CaMK I/CREB pathway is important in the regulation of small cholangiocyte function.

机译：胆管病的特征是不同大小的胆管细胞的异质增殖。大型胆管细胞通过cAMP依赖性机制增殖。小胆管细胞的功能可能取决于肌醇三磷酸（IP3）/ Ca2 +依赖性信号传导途径的激活。但是，缺乏支持这种推测的数据。存在四种组胺受体（HRH1，HRH2，HRH3和HRH4）。在几个细胞中：1）HRH1的激活会增加细胞内Ca2 +的浓度水平； 2）增加的[Ca2 +]（i）水平与钙调蛋白依赖性蛋白激酶（CaMK）的钙调蛋白依赖性刺激和cAMP反应元件结合蛋白（CREB）的激活相结合。 HRH1激动剂通过激活IP3 / Ca2 +依赖性CaMK / CREB来调节小胆管细胞增殖。我们评估了胆管细胞中HRH1的表达。在测量增殖之前，用/不使用特非那定，BAPTA / AM或W7将组胺三氟甲基甲苯胺（HTMT双马来酸酯； HRH1激动剂）刺激大小胆管细胞24-48小时。在大小胆管细胞中评估了CaMK I，II和IV的表达。我们测量了HTMT双马来酸酯处理的小胆管细胞的IP3，Ca2 +和cAMP水平，CaMK I的磷酸化以及CREB的激活（在W7存在/不存在的情况下）。在测量增殖和CREB活性之前，先用HTMT双马来酸酯刺激的小胆管细胞进行CaMK I抑制。大小胆管细胞均表达HRH1，CaMK I和CaMK II。小（但不是大）胆管细胞响应HTMT dimaleate增殖，并被terfenadine（HRH1拮抗剂），BAPTA / AM和W7阻断。在小的胆管细胞中，HTMT双马来酸酯可增加IP3 / Ca2 +水平，CaMK I磷酸化和CREB活性。 CaMK I的基因敲低消除了HTMT双马来酸酯对小胆管细胞增殖和CREB活化的影响。 IP3 / Ca2 + / CaMK I / CREB通路在调节小胆管细胞功能中很重要。

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H. Francis; S. Glaser; S. Demorrow; Eugenio Gaudio; Y. Ueno; J. Venter; D.E. Dostal; Paolo Onori; Antonio Franchitto; M. Marzioni; S. Vaculin; B. Vaculin; K. Katki; M. Stutes; J. Savage; G. Alpini;
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年度 2008
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专利

1. Small mouse cholangiocytes proliferate in response to H1 histamine receptor stimulation by activation of the IP3/CaMK I/CREB pathway. [J] . Francis H, Glaser S, Demorrow S American Journal of Physiology . 2008,第2aPta1期

机译：通过激活IP3 / CaMK I / CREB途径，小鼠小胆管细胞响应H1组胺受体刺激而增殖。
2. Small mouse cholangiocytes proliferate in response to HI histamine receptor stimulation by activation of the IP3/CaMK I/CREB pathway [J] . Francis H, Glaser S, DeMorrow S, American Journal of Physiology . 2008,第2aPta1期

机译：小鼠胆管细胞通过IP3 / CAMK I / CREB途径的激活来响应HI组胺受体刺激响应于HI组胺受体刺激而增殖
3. Stimulation of histamine H1 receptor up-regulates histamine H1 receptor itself through activation of receptor gene transcription. [J] . Das AK, Yoshimura S, Mishima R, Journal of pharmacological sciences. . 2007,第4期

机译：组胺H1受体的刺激通过受体基因转录的激活而上调组胺H1受体本身。
4. Accumulation of Perfluorinated Compounds and Effects on Peroxisome Proliferators-Activated Receptor alpha-Cytochrome P450 4A Signaling Pathway in Baikal Seal(Pusa sibirica) [C] . Hiroshi Ishibashi, Hisato Iwata, Eun-Young Kim International Symposium Pioneering Studies of Young Scientists on Chemical Pollution and Environmental Changes . 2007

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5. Novel mechanisms of cardioprotection: Catecholamine release by natriuretic peptides: Characterization and prevention; activation of ALDH2 in mast cell mitochondria: Prevention of local angiotensin II formation; activation of histamine H3-receptors: Reduction of angiotensin AT1-receptor neuronal expression [D] . Chan, Noel Yan-ki 2012

机译：心脏保护的新机制：利钠肽释放儿茶酚胺：表征和预防；肥大细胞线粒体中ALDH2的激活：预防局部血管紧张素II的形成； H3受体的活化：降低血管紧张素AT1受体神经元表达
6. Small mouse cholangiocytes proliferate in response to H1 histamine receptor stimulation by activation of the IP3/CaMK I/CREB pathway [O] . Heather Francis, Shannon Glaser, Sharon DeMorrow, -1

机译：通过激活IP3 / CaMK I / CREB途径小鼠小胆管细胞响应H1组胺受体刺激而增殖
7. Small mouse cholangiocytes proliferate in response to H1 histamine receptor stimulation by activation of the IP3/CaMK I/CREB pathway [O] . Francis, Heather, Glaser, Shannon, DeMorrow, Sharon, 2008

机译：通过激活IP3 / CaMK I / CREB途径，小鼠小胆管细胞响应H1组胺受体刺激而增殖
8. Implication of Prostaglandins and Histamine H1 and H2 Receptors in Radiation-Induced Temperature Responses of Rats [R] . Kandasamy, S. B., Hunt, W. A., Mickley, G. A 1988

机译：前列腺素和组胺H1和H2受体在大鼠辐射诱导的温度反应中的意义

Small mouse cholangiocytes proliferate in response to H1 histamine receptor stimulation by activation of the IP3/CaMK I/CREB pathway

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