首页> 外文期刊>Journal of applied physiology >Discharge of the hypoglossal nerve cannot distinguish eupnea from gasping, as defined by phrenic discharge, in the in situ mouse.
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Discharge of the hypoglossal nerve cannot distinguish eupnea from gasping, as defined by phrenic discharge, in the in situ mouse.

机译:舌下神经的放电不能区分原位小鼠的气喘和gas气,如distinguish放电所定义。

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If normal, eupneic breathing fails, gasping is recruited. Serotonin was proposed as essential for gasping, based on findings using an in vitro mouse preparation. This preparation generates rhythmic activities of the hypoglossal nerve that are considered to be akin to both eupnea and gasping. In previous studies, gasping of in situ rat and mouse preparations continued unabated following blockers of receptors for serotonin. However, hypoglossal activity was not recorded in the mouse, and we hypothesized that its discharge during gasping might be dependent on serotonin. In the in situ mouse preparation, hypoglossal discharge had varying and inconsistent patterns during eupnea, discharging concomitant with the phrenic burst, at varying intervals between phrenic bursts, or was silent in some respiratory cycles. In eupnea, phrenic discharge was incrementing, whereas hypoglossal discharge was decrementing in 15 of 20 preparations. During ischemia-induced gasping, peak phrenic height was reached at 205 +/- 17 ms, compared with 282 +/- 27.9 ms after the start of the eupneic burst (P < 0.002). In contrast, rates of rise of hypoglossal discharge in gasping (peak at 233 +/- 25 ms) and eupnea (peak at 199 +/- 19.2 ms) were the same. The uncoupling of hypoglossal from phrenic discharge in eupnea was exacerbated by methysergide, an antagonist of serotonin receptors. These findings demonstrate that hypoglossal discharge alone cannot distinguish eupnea from gasping nor, in eupnea, can hypoglossal activity be used to differentiate neural inspiration from expiration. These findings have significant negative implications for conclusions drawn from the in vitro medullary slice of mouse.
机译:如果正常,正气道呼吸失败,则会抽气。根据体外小鼠制剂的发现,血清素被认为是喘气必不可少的。该制剂产生了舌下神经的节律性活动,被认为类似于呼吸道和喘息。在先前的研究中,在阻断5-羟色胺受体之后,原位大鼠和小鼠的准备工作仍在继续进行。但是,在小鼠中未记录到舌下活动,我们推测在喘气期间其放电可能取决于血清素。在原位小鼠制备中,舌下放电在气喘期间具有变化和不一致的模式,与爆发伴随放电,at爆发之间间隔不同,或者在某些呼吸周期中保持沉默。在正常情况下,20份制剂中有15份气分泌增加,而舌下分泌减少。在局部缺血引起的喘息期间,up气峰值的峰值达到205 +/- 17 ms,而紫癜爆发后的峰值为282 +/- 27.9 ms(P <0.002)。相比之下,喘气(峰值在233 +/- 25毫秒)和呼吸暂停(峰值在199 +/- 19.2毫秒)时舌下分泌增加的速率相同。 5-羟色胺受体拮抗药美塞麦肽加剧了通气时hypo分泌与e气的解偶联。这些发现表明,仅舌下排出不能将气喘与喘息区分开,在舌上也不能用舌下活动来区分呼气与神经兴奋。这些发现对从小鼠的体外髓质切片得出的结论具有重大的负面影响。

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