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细胞外 ATP 通过嘌呤能 P2X7 和腺苷 A1 受体在新生和慢性癫痫大鼠中差异影响癫痫样活动。

Extracellular ATP differentially affects epileptiform activity via purinergic P2X7 and adenosine A1 receptors in naive and chronic epileptic rats.

机构信息

Institute of Neurophysiology, Charité-Universitätsmedizin Berlin, Charitplatz 1, Berlin, Germany.

出版信息

Epilepsia. 2012 Nov;53(11):1978-86. doi: 10.1111/j.1528-1167.2012.03724.x. Epub 2012 Oct 25.

Abstract

PURPOSE

Adenosine is considered an endogenous anticonvulsant. However, much less is known about the putative effects of its precursor, ATP, on epilepsy. Therefore, we tested whether ATP and its receptors are able to modulate epileptiform activity in the medial entorhinal cortex of the rat.

METHODS

Recurrent epileptiform discharges (REDs) were induced by elevating extracellular potassium concentration combined with application of bicuculline in brain slices from naive and pilocarpine-treated chronic epileptic rats. Field potentials were recorded from layer V/VI of the medial entorhinal cortex.

KEY FINDINGS

REDs in slices from naive animals had a higher incidence and a shorter duration than in slices from chronic epileptic animals. Exogenous application of ATP reversibly reduced the incidence of REDs in naive and chronic epileptic slices via activation of adenosine A(1) receptors without discernible P2 receptor effects. This effect was stronger in slices from chronic epileptic rats. In slices from naive rats, the P2X7 receptor antagonist A 740003 slightly but significantly reduced the amplitude of slow field potentials of REDs. In slices from chronic epileptic rats, none of the P2 receptor antagonists affected the parameters of REDs.

SIGNIFICANCE

Our results suggest that endogenously released ATP differentially modulates REDs by activation of A(1) and P2X7 receptors. Although it has a minor proepileptic effect by direct activation of P2X7 receptors, its metabolite adenosine reduces the epileptiform activity via activation of A(1) receptors. The exact effect of ATP on neural activity depends on the actual activity of ectonucleotidases and the expression level of the purinergic receptors, which both alter during epileptogenesis. In addition, our data suggest that P2X7 receptor antagonists have a minor antiepileptic effect.

摘要

目的

腺苷被认为是一种内源性抗惊厥物质。然而,关于其前体 ATP 对癫痫的潜在作用,人们知之甚少。因此,我们测试了 ATP 及其受体是否能够调节大鼠内侧隔核的癫痫样活动。

方法

在来自未处理和匹鲁卡品处理的慢性癫痫大鼠的脑片中,通过升高细胞外钾浓度并应用荷包牡丹碱来诱导反复性癫痫样放电(REDs)。从内侧隔核的 V/VI 层记录场电位。

主要发现

与慢性癫痫动物的脑片相比,来自未处理动物的脑片中 REDs 的发生率更高,持续时间更短。外源性应用 ATP 通过激活腺苷 A1 受体可逆地降低了来自未处理和慢性癫痫脑片的 REDs 的发生率,而没有明显的 P2 受体作用。这种作用在慢性癫痫大鼠的脑片中更强。在来自未处理大鼠的脑片中,P2X7 受体拮抗剂 A 740003 略微但显著降低了 REDs 的慢场电位的振幅。在来自慢性癫痫大鼠的脑片中,没有一种 P2 受体拮抗剂影响 REDs 的参数。

意义

我们的结果表明,内源性释放的 ATP 通过激活 A1 和 P2X7 受体来差异调节 REDs。尽管它通过直接激活 P2X7 受体具有轻微的致痫作用,但它的代谢物腺苷通过激活 A1 受体来减少癫痫样活动。ATP 对神经活动的确切影响取决于外核苷酸酶的实际活性和嘌呤能受体的表达水平,这两者在癫痫发生过程中都会发生改变。此外,我们的数据表明 P2X7 受体拮抗剂的抗癫痫作用较小。

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