脊髓P2X 4受体在大鼠慢性吗啡耐受形成中的作用

Role of Spinal P2x4 Receptor In Process of Chronic Morphine Tolerance in Rats

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摘要【目的】观察慢性吗啡耐受大鼠脊髓背角 P2X4受体（P2X4R）的表达以及鞘内注射嘌呤受体拮抗剂TNP‐ATP（P2X1‐4R抑制剂）和 PPADS（P2X1‐3，5‐7 R 抑制剂）对慢性吗啡耐受大鼠的影响。【方法】60只成年雄性SD 大鼠，随机分为4组（ n ＝15）：对照组（C组）、吗啡组（M组）、吗啡＋ TNP‐ATP 组（T组）和吗啡＋ PPADS 组（P 组）。对照组：大鼠鞘内注射生理盐水（20μL）；M 组：大鼠鞘内注入吗啡10μg （10μL ）和生理盐水10μL ；T组：大鼠鞘内注入 TNP‐ATP 10 nmol（10μL ），半小时后注入吗啡10μg （10μL）；P 组：大鼠经鞘内置管并注入PPADS 10 nmol（10μL），半小时后注入吗啡10μg（10μL），2次／日，连续7 d 。每只大鼠于术前测定基础热痛阈，各组每次给药后测量大鼠热痛阈，d1、d3、d7最后一次测量痛阈后处死5只大鼠取脊髓背角，采用免疫组化检测 P2X4受体表达。【结果】M 组在 d1、d3的热痛阈显著高于 C 组（ P ＜0．05），随着吗啡注药天数增加，M 组热痛阈逐渐下降，d5、d7与 C 组的差异无统计学意义（ P ＞0．05）。与M组比较，P组各时点热痛阈无明显差异，但 T组热痛阈虽然也呈下降趋势，但明显缓于 M 组，T 组 d5、d7的热痛阈高于M组，差异有统计学意义（ P ＜0．05）。与 C 组比较，M组和P组在给药 d1、d3、d7大鼠脊髓背角 P2X4R表达上调（ P ＜0．05）。鞘内注射 TNP‐ATP 组P2X4R表达明显低于M组和P组（ P ＜0．05）。【结论】鞘内给予 TNP‐ATP 能够延缓大鼠慢性吗啡耐受的形成，其机制可能与其抑制P2X4R的表达有关。 [Objective] To observe the changes of P2X4 receptor in spinal dorsal horn and explore the effect of TNP‐ATP （P2X1‐4 R inhibitor）and PPADS（P2X1‐3 ,5‐7 R inhibitor）intrathecally administered in chronic morphine tolerance rats .[Methods] A total of 60 male adult Sprague‐Dawley rats were randomly divided into four groups （ n = 15 each） of control ？ ,morphine （M） ;TNP‐ATP ＋ morphine （T） and PPADS ＋ morphine （P） .The animals received intrathecal injec‐tions of morphine 10 μg（10 μL）and saline 10 μL twice daily for 7 days （T1 - T7 ） in group M while an equal volume of sa‐line in group C .Groups T and P received intrathecal injections of 10 nmol（10 μL） TNP‐ATP and PPADS respectively for 7 days 30 min before the same treatment in group M .We assessed basic mechanical and thermal pain threshold at 2 days pre‐operation .Pain threshold to a thermal nociceptive stimulus was measured 30 min after dosing at T 1 - 7 in each group . Five rats in each group were sacrificed after last dosing at 1st ,3th ,7th days and spinal cord dorsal horn removed for de‐tecting the expression of P2X4 R by immunohistochemistry .[Results] Thermal pain threshold of group M was significant‐ly higher than that of group C at day 1 and 3 （ P 〈 0 .05） ,but decreased gradually afterwards with morphine dosing .And no significant difference existed between groups M and C at Day 5 and 7 （ P 〉 0 .05） .The difference was not significantly different between groups M and P （ P 〉 0 .05） .Thermal pain threshold of group T decreased more slowly than that of group M .Thermal pain threshold of group T was higher than that of group M ,especially during 5 and 7d （ P 〈 0 .05） .The expression of P2X4 R in groups M and P was obviously higher than that of group C at day 1 ,3 and 7 . The expression of P2X4 R significantly decreased in group T after an intrathecal dose of TNP‐ATP compared with groups M and P （ P 〈 0 .05） .[Conclusion] Intrathecal TNP‐ATP attenuates morphine

作者董良曾金曹健斌陈丽红黄一丹韦晓林

机构地区广西壮族自治区柳州市人民医院麻醉科广西壮族自治区柳州市人民医院胸外科

出处《医学临床研究》 CAS 2015年第6期1056-1059,共4页 Journal of Clinical Research

基金广西卫生厅自筹课题（Z2014411）

关键词受体嘌呤能P2 脊髓吗啡药物耐受性 Receptors, Purinergic P2 Spinal Cord Morphine Drug Tolerance

分类号 R971.2 [医药卫生—药品]

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脊髓P2X 4受体在大鼠慢性吗啡耐受形成中的作用

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