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使用放射性标记的(+)-S-145对人和豚鼠鼻黏膜中血栓素A2受体进行表征和定位

Characterization and localization of thromboxane A2 receptor in human and guinea-pig nasal mucosa using radiolabelled (+)-S-145.

作者信息

Arimura A, Miwa M, Hasegawa H, Kishino J, Notoya M, Yasui K, Komori M, Iwata S

机构信息

Discovery Research Laboratories II, Toyonaka, Osaka, Japan.

出版信息

Br J Pharmacol. 1998 Jun;124(4):795-803. doi: 10.1038/sj.bjp.0701904.

Abstract
  1. TxA2 receptor (TP-receptor) antagonists such as S-1452 and Bay u 3405 have been shown to be effective in alleviating nasal blockage in patients with allergic rhinitis as well as guinea-pig allergic rhinitis models. The present study was conducted to examine the existence and localization of the TP-receptor in human and guinea-pig nasal mucosa by in vitro receptor binding autoradiography using radiolabelled (+)-S-145, which is a potent and specific TP-receptor antagonist with an extremely slow dissociation rate. 2. We ascertained the binding specificity of [3H]-(+ )-S-145 in human and guinea-pig platelet membranes by comparing the ability of four TP-receptor ligands of U-46619, (+)-S-145, I-(+)-S-145 and Bay u 3405 to displace the specific binding of [3H]-(+)-S-145 and [3H]-U-46619. The rank order of potency (Ki) for the displacement was correlated highly with that determined from [3H]-U-46619 binding to the same preparations. 3. Quantitative autoradiography using a radioluminographic imaging plate system, in which the radioactivity of [3H]-(+)-S-145 is expressed as photostimulated luminescence (PSL) per area (mm2), revealed that specific binding of [3H]-(+)-S-145 to human and guinea-pig nasal mucosa was saturable. Scatchard analysis showed about three fold higher affinity and two fold greater maximal binding to the nasal mucosa of humans than that of guinea-pigs: the KD and Bmax values in human mucosa were 2.82+/-0.35 nM and 6.47+/-0.33 PSL mm(-2) and those in guinea-pig mucosa were 8.23+/-1.93 nM and 3.37+/-0.66 PSL mm(-2), respectively. 4. Specific [3H]-(+)-S-145 binding to cryostat sections of human and guinea-pig nasal mucosa was displaced by another TP-receptor antagonist, Bay u 3405, and a TP-receptor agonist, U-46619. The order of potency (Ki value: nM) was (+)-S-145 (2.5) > Bay u 3405 (15.4) > > U-46619 (359.6) in human nasal mucosa and (+)-S-145 (22.8) > U-46619 (49.8) approximately Bay u 3405 (62.1) in guinea-pig nasal mucosa. These rank orders showed rather good correlation with those obtained for the respective platelet membranes. 5. Autoradiographs of human nasal mucosa demonstrated that specific [125I]-(+)-S-145 binding sites mainly exist on the smooth muscle layers of venous sinusoids and arterioles in the lamina propria, with few or no binding sites in the epithelium and nasal gland. 6. We concluded that radiolabelled (+)-S-145 can be used as a TP-receptor ligand for autoradiographic study, and that the TP-receptor is exclusively located on smooth muscle layers of venous sinusoids and arterioles in the nasal mucosa. The potent vasoconstrictive activity of TxA2 may cause reduction of local blood flow followed by mucosal oedema probably through mechanisms of vascular injury such as ischaemia-reperfusion.
摘要
  1. 血栓素A2受体(TP受体)拮抗剂,如S - 1452和Bay u 3405,已被证明在缓解过敏性鼻炎患者以及豚鼠过敏性鼻炎模型的鼻阻塞方面有效。本研究旨在通过使用放射性标记的(+)-S - 145进行体外受体结合放射自显影,来检测TP受体在人和豚鼠鼻黏膜中的存在及定位,(+)-S - 145是一种强效且特异性的TP受体拮抗剂,其解离速率极慢。2. 通过比较U - 46619、(+)-S - 145、I -(+)-S - 145和Bay u 3405这四种TP受体配体取代[3H] -(+)-S - 145和[3H] - U - 46619特异性结合的能力,我们确定了[3H] -(+)-S - 145在人和豚鼠血小板膜中的结合特异性。取代效力(Ki)的排序与从[3H] - U - 46619与相同制剂结合所确定的排序高度相关。3. 使用放射性发光成像板系统进行定量放射自显影,其中[3H] -(+)-S - 145的放射性以每面积(mm2)的光刺激发光(PSL)表示,结果显示[3H] -(+)-S - 145与人及豚鼠鼻黏膜的特异性结合是可饱和的。Scatchard分析表明,人鼻黏膜对其亲和力约高3倍,最大结合量约大2倍:人黏膜中的KD和Bmax值分别为2.82±0.35 nM和6.47±0.33 PSL mm(-2),豚鼠黏膜中的分别为8.23±1.93 nM和3.37±0.66 PSL mm(-2)。4. 另一种TP受体拮抗剂Bay u 3405和一种TP受体激动剂U - 46619可取代[3H] -(+)-S - 145与人及豚鼠鼻黏膜冰冻切片的特异性结合。效力排序(Ki值:nM)在人鼻黏膜中为(+)-S - 145(2.5)>Bay u 3405(15.4)>>U - 46619(359.6),在豚鼠鼻黏膜中为(+)-S - 145(22.8)>U - 46619(49.8)≈Bay u 3405(62.1)。这些排序与各自血小板膜的排序显示出相当好的相关性。5. 人鼻黏膜的放射自显影片表明,特异性[125I] -(+)-S - 145结合位点主要存在于固有层静脉窦和小动脉的平滑肌层,上皮和鼻腺中几乎没有或不存在结合位点。6. 我们得出结论,放射性标记的(+)-S - 145可作为TP受体配体用于放射自显影研究,且TP受体仅位于鼻黏膜静脉窦和小动脉的平滑肌层。血栓素A2的强效血管收缩活性可能通过诸如缺血再灌注等血管损伤机制导致局部血流减少,进而引起黏膜水肿。

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