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Combined treatment with a selective PDE10A inhibitor TAK‐063 and either haloperidol or olanzapine at subeffective doses produces potent antipsychotic‐like effects without affecting plasma prolactin levels and cataleptic responses in rodents

机译：亚有效剂量的选择性PDE10A抑制剂TAK-063与氟哌啶醇或奥氮平的联合治疗可产生有效的抗精神病样作用而不会影响啮齿动物的血浆催乳素水平和抗氧化反应

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Activation of indirect pathway medium spiny neurons (MSNs) via promotion of cAMP production is the principal mechanism of action of current antipsychotics with dopamine D2 receptor antagonism. TAK‐063 [1‐[2‐fluoro‐4‐(1H‐pyrazol‐1‐yl)phenyl]‐5‐methoxy‐3‐(1‐phenyl‐1H‐pyrazol‐5‐yl)pyridazin‐4(1H)‐one] is a novel phosphodiesterase 10A inhibitor that activates both direct and indirect pathway MSNs through increasing both cAMP and cGMP levels by inhibition of their degradation. The activation of indirect pathway MSNs through the distinct mechanism of action of these drugs raises the possibility of augmented pharmacological effects by combination therapy. In this study, we evaluated the potential of combination therapy with TAK‐063 and current antipsychotics, such as haloperidol or olanzapine after oral administration. Combined treatment with TAK‐063 and either haloperidol or olanzapine produced a significant increase in phosphorylation of glutamate receptor subunit 1 in the rat striatum. An electrophysiological study using rat corticostriatal slices showed that TAK‐063 enhanced N‐methyl‐D‐aspartic acid receptor‐mediated synaptic responses in both direct and indirect pathway MSNs to a similar extent. Further evaluation using pathway‐specific markers revealed that coadministration of TAK‐063 with haloperidol or olanzapine additively activated the indirect pathway, but not the direct pathway. Combined treatment with TAK‐063 and either haloperidol or olanzapine at subeffective doses produced significant effects on methamphetamine‐ or MK‐801‐induced hyperactivity in rats and MK‐801‐induced deficits in prepulse inhibition in mice. TAK‐063 at 0.1 mg/kg did not affect plasma prolactin levels and cataleptic response from antipsychotics in rats. Thus, style="fixed-case">TAK‐063 may produce augmented antipsychotic‐like activities in combination with antipsychotics without effects on plasma prolactin levels and cataleptic responses in rodents.

机译：通过促进cAMP产生来激活间接途径中棘神经元（MSNs）是当前抗精神病药与多巴胺D2受体拮抗作用的主要作用机理。 TAK‐063 [1- [2-氟-4-（1H-吡唑-1-基）苯基] -5-甲氧基-3-（1-苯基-1H-吡唑-5-基）哒嗪-4（1H） [‐one]是一种新型磷酸二酯酶10A抑制剂，可通过抑制cAMP和cGMP的降解来提高其直接和间接途径，从而激活MSN。通过这些药物独特的作用机制激活间接途径MSNs，增加了通过联合疗法增强药理作用的可能性。在这项研究中，我们评估了口服TAK-063和目前的抗精神病药物（如氟哌啶醇或奥氮平）联合治疗的可能性。 TAK-063与氟哌啶醇或奥氮平的联合治疗可显着增加大鼠纹状体中谷氨酸受体亚基1的磷酸化。使用大鼠皮质窦口切片的电生理研究表明，TAK-063在直接和间接途径MSN中均增强了N-甲基-D-天冬氨酸受体介导的突触反应。使用途径特异性标记物进行的进一步评估显示，TAK-063与氟哌啶醇或奥氮平的共同给药可加性激活间接途径，而不是直接途径。联合使用TAK‐063和氟哌啶醇或奥氮平的亚有效剂量联合治疗可对大鼠甲基苯丙胺或MK‐801过度活跃产生显着影响，并在小鼠中由MK‐801诱导的前冲抑制缺陷。 0.1 mg / kg的TAK-063不会影响血浆催乳素水平和抗精神病药对大鼠的抗感性反应。因此， style =“ fixed-case”> TAK -063与抗精神病药联合使用可产生增强的抗精神病药样活性，而不会影响啮齿动物的血浆催乳素水平和抗氧化反应。

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期刊名称 Pharmacology Research Perspectives
作者
Kazunori Suzuki; Akina Harada; Hirobumi Suzuki; Clizia Capuani; Annarosa Ugolini; Mauro Corsi; Haruhide Kimura;
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作者单位

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年(卷),期 2018(6),1
年度 2018
页码 e00372
总页数 12
原文格式 PDF
正文语种
中图分类药学;
关键词
antipsychotics medium spiny neuron phosphodiesterase 10A schizophrenia TAK‐063;

机译：抗精神病药;中棘神经元;磷酸二酯酶10A;精神分裂症;TAK-063;

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外文文献

1. Combined treatment with a selective PDE10A inhibitor TAK‐063 and either haloperidol or olanzapine at subeffective doses produces potent antipsychotic‐like effects without affecting plasma prolactin levels and cataleptic responses in rodents [J] . Kazunori Suzuki, Akina Harada, Hirobumi Suzuki, Pharmacology Research & Perspectives . 2018,第1期

机译：亚有效剂量的选择性PDE10A抑制剂TAK-063与氟哌啶醇或奥氮平的联合治疗可产生有效的抗精神病样作用，而不会影响啮齿动物的血浆催乳素水平和抗氧化反应
2. In Vivo Pharmacological Characterization of TAK-063, a Potent and Selective Phosphodiesterase 10A Inhibitor with Antipsychotic-Like Activity in Rodents [J] . Kazunori Suzuki, Akina Harada, Eri Shiraishi, The Journal of Pharmacology and Experimental Therapeutics: Official Publication of the American Society for Pharmacology and Experimental Therapeutics . 2015,第3期

机译：TAK-063，一种具有抗精神病活性的啮齿类动物的有效和选择性磷酸二酯酶10A抑制剂的体内药理学表征
3. The PDE10A inhibitor MP-10 and haloperidol produce distinct gene expression profiles in the striatum and influence cataleptic behavior in rodents [J] . Gentzel Renee C., Toolan Dawn, Roberts Rhonda, Neuropharmacology . 2015,第Null期

机译：PDE10A抑制剂MP-10和氟哌啶醇在纹状体中产生不同的基因表达谱，并影响啮齿动物的镇静行为
4. S223. COMBINED TREATMENT WITH A SELECTIVE PDE10A INHIBITOR TAK-063 AND ANTIPSYCHOTICS AT SUBEFFECTIVE DOSES PRODUCES POTENT ANTIPSYCHOTIC-LIKE EFFECTS WITHOUT EXACERBATING SIDE EFFECTS PROFILE IN RODENTS [O] . Kazunori Suzuki, Akina Harada, Hirobumi Suzuki, 2018

机译：S223。在选择性剂量下联合使用选择性PDE10A抑制剂TAK-063和止痛药联合治疗可产生强效的类似止痛药的功效而不会在啮齿动物中引起副作用
5. TAK-063, a PDE10A Inhibitor with Balanced Activation of Direct and Indirect Pathways, Provides Potent Antipsychotic-Like Effects in Multiple Paradigms [O] . Kazunori Suzuki, Akina Harada, Hirobumi Suzuki, 2016

机译：TAK-063，PDE10A抑制剂具有平衡的直接和间接途径的激活，提供多种范式的有效的抗精神病效果

Combined treatment with a selective PDE10A inhibitor TAK‐063 and either haloperidol or olanzapine at subeffective doses produces potent antipsychotic‐like effects without affecting plasma prolactin levels and cataleptic responses in rodents

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