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一种经过改良的类似微量血淋巴的溶液HL3.1,用于在正常和突变果蝇幼虫的神经肌肉接头处进行生理记录。

A modified minimal hemolymph-like solution, HL3.1, for physiological recordings at the neuromuscular junctions of normal and mutant Drosophila larvae.

作者信息

Feng Yanfei, Ueda Atsushi, Wu Chun-Fang

机构信息

Department of Biological Sciences, University of Iowa, Iowa City, IA 52242, USA.

出版信息

J Neurogenet. 2004 Apr-Jun;18(2):377-402. doi: 10.1080/01677060490894522.

Abstract

The hemolymph-like HL3 saline(Stewart et al., 1994)and standard saline(Jan & Jan, 1976)are two widely used bathing solutions for physiological recordings at the Drosophila larval neuromuscular junction. It has been established that longevity of larval preparations is better maintained in HL3 saline. However, HL3 can produce results that are inconsistent with previous findings in standard saline, particularly on temperature sensitivity and membrane excitability phenotypes. In wild-type larvae, the excitatory junctional potentials(EJPs)in standard saline(containing 4 mM Mg(2+)and 1.8 mM Ca(2+))were not blocked by a temperature increase up to 39-40 degrees C, consistent with unimpaired larval locomotion below these temperatures. However, in HL3 saline(containing 20 mM Mg(2+)and 1.5 mM Ca(2+)), EJPs were blocked at 30 degrees C. As for temperature-sensitive mutants nap(ts)and para(ts), the EJP-blocking temperatures were decreased from about 29 and 33 degrees C in standard saline to about 23 and 26 degrees C in HL3, respectively. Compound action potential recordings confirmed that segmental nerve action potentials were more readily blocked by a temperature increase in HL3 than in standard saline. Axonal excitability was suppressed in HL3 even at room temperatures, as evidenced by a lengthened refractory period in wild-type larvae. Similar suppression occurred for the hyper-excitable double mutant eag Sh, which maintained high-frequency spontaneous EJPs in standard saline but showed a rapidly declining EJP frequency in HL3. Application of HL3 saline also strongly suppressed the prolonged transmitter release following removal of repolarization mechanisms by K(+)channel blockers or by the eag Sh mutation previously described in standard saline. These discrepancies suggest that the high divalent cation content in HL3 may confer a surface charge screening effect to suppress nerve membrane excitability. We found that a minimal adjustment of the HL3 saline, decreasing the Mg(2+)ion concentration from 20 to 4 mM, was sufficient to resolve the discrepancies. While retaining the longevity of the larval neuromuscular preparation, the modified HL3 saline(HL3.1)restored the established wild-type EJP properties as well as phenotypes of several widely used temperature-sensitive and hyper-excitable mutants previously documented in standard saline.

摘要

类血淋巴HL3盐溶液(Stewart等人,1994年)和标准盐溶液(Jan和Jan,1976年)是果蝇幼虫神经肌肉接头处生理记录中广泛使用的两种浴液。已经确定,在HL3盐溶液中幼虫标本的寿命能得到更好的维持。然而,HL3可能会产生与先前在标准盐溶液中的发现不一致的结果,特别是在温度敏感性和膜兴奋性表型方面。在野生型幼虫中,标准盐溶液(含有4 mM Mg(2+)和1.8 mM Ca(2+))中的兴奋性接头电位(EJPs)在温度升高到39 - 40摄氏度时不会被阻断,这与在这些温度以下幼虫运动未受损害一致。然而,在HL3盐溶液(含有20 mM Mg(2+)和1.5 mM Ca(2+))中,EJPs在30摄氏度时就被阻断。至于温度敏感突变体nap(ts)和para(ts),EJP阻断温度分别从标准盐溶液中的约29和33摄氏度降至HL3中的约23和26摄氏度。复合动作电位记录证实,与标准盐溶液相比,HL3中节段神经动作电位更容易因温度升高而被阻断。即使在室温下,HL3中轴突兴奋性也受到抑制,野生型幼虫的不应期延长就证明了这一点。对于超兴奋性双突变体eag Sh也有类似的抑制情况,它在标准盐溶液中维持高频自发EJPs,但在HL3中EJP频率迅速下降。在标准盐溶液中,通过钾通道阻滞剂或先前描述的eag Sh突变去除复极化机制后,HL3盐溶液的应用也强烈抑制了延长的递质释放。这些差异表明,HL3中高含量的二价阳离子可能赋予表面电荷筛选效应以抑制神经膜兴奋性。我们发现,对HL3盐溶液进行最小程度的调整,将Mg(2+)离子浓度从20 mM降至4 mM,就足以解决这些差异。在保留幼虫神经肌肉标本寿命的同时,改良后的HL3盐溶液(HL3.1)恢复了已确定的野生型EJP特性以及先前在标准盐溶液中记录的几种广泛使用的温度敏感和超兴奋性突变体的表型。

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