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7-硝基吲唑与A/J和C57BL/6J小鼠品系的缺氧后通气行为

7-nitroindazole and posthypoxic ventilatory behavior in the A/J and C57BL/6J mouse strains.

作者信息

Price Edwin R, Han Fang, Dick Thomas E, Strohl Kingman P

机构信息

Department of Medicine, Case Western Reserve University, Cleveland, OH 44106, USA.

出版信息

J Appl Physiol (1985). 2003 Sep;95(3):1097-104. doi: 10.1152/japplphysiol.00166.2003.

Abstract

Periodic breathing (PB) is a fundamental breathing pattern in many common cardiopulmonary illnesses. The finding of PB in C57BL/6J (B6) mice was previously ascribed to strain differences in posthypoxic ventilatory and frequency decline in the B6 mice (Han F, Subramanian S, Price ER, Nadeau J, and Strohl KP. J Appl Physiol 92: 1133-1140, 2002). We tested whether the induction of posthypoxic frequency decline in A/J mice, through administration of a neuronal nitric oxide synthase blocker [7-nitroindazole (7-NI); 60 mg/kg], would cause A/J mice to exhibit PB and/or alter PB expression in the B6 strain. Recordings of ventilatory behavior by the plethysmography method were made when unanesthetized B6 (n = 10) or A/J (n = 6) animals were reoxygenated with 100% O2 or room air after exposure to 8% O2. Before undergoing gas challenges, mice were given an intraperitoneal injection of either peanut oil alone (vehicle) or 7-NI suspended in peanut oil. Compared with vehicle, both strains of mice exhibited posthypoxic frequency decline and the absence of short-term potentiation with 7-NI administration. B6 mice continued to exhibit posthypoxic PB; however, the PB was characterized by longer cycle and apnea length. In contrast, A/J mice did not show increased tendency toward posthypoxic PB with 7-NI. We conclude that 7-NI further differentiates the A/J and B6 strains in terms of PB and that strain-related differences in posthypoxic frequency decline are not primary determinants of this strain difference in the occurrence of PB. Metabolism was not associated with either the expression of posthypoxic ventilatory decline or PB. Furthermore, neuronal nitric oxide may be an organizing feature in the presence, length, and/or cycle length of apnea in the susceptible strain.

摘要

周期性呼吸(PB)是许多常见心肺疾病中的一种基本呼吸模式。先前在C57BL/6J(B6)小鼠中发现的PB被归因于B6小鼠低氧后通气和频率下降的品系差异(Han F,Subramanian S,Price ER,Nadeau J和Strohl KP。《应用生理学杂志》92:1133 - 1140,2002年)。我们测试了通过给予神经元型一氧化氮合酶阻滞剂[7 - 硝基吲唑(7 - NI);60毫克/千克]诱导A/J小鼠低氧后频率下降是否会导致A/J小鼠出现PB和/或改变B6品系中PB的表达。当未麻醉的B6(n = 10)或A/J(n = 6)动物在暴露于8%氧气后用100%氧气或室内空气复氧时,通过体积描记法记录通气行为。在进行气体挑战之前,给小鼠腹腔注射单独的花生油(载体)或悬浮在花生油中的7 - NI。与载体相比,两种品系的小鼠在给予7 - NI后均表现出低氧后频率下降且无短期增强。B6小鼠继续表现出低氧后PB;然而,PB的特征是周期和呼吸暂停长度更长。相比之下,A/J小鼠在给予7 - NI后未表现出低氧后PB增加的趋势。我们得出结论,7 - NI在PB方面进一步区分了A/J和B6品系,并且低氧后频率下降的品系相关差异不是该品系在PB发生上差异的主要决定因素。代谢与低氧后通气下降或PB的表达均无关。此外,神经元型一氧化氮可能是易感品系中呼吸暂停的存在、长度和/或周期长度的一个组织特征。

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