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slo的一种蛋白激酶A调节的剪接异构体的出现与控制生殖行为的神经元的成熟有关。

The appearance of a protein kinase A-regulated splice isoform of slo is associated with the maturation of neurons that control reproductive behavior.

作者信息

Zhang Yalan, Joiner William J, Bhattacharjee Arin, Rassendren Francois, Magoski Neil S, Kaczmarek Leonard K

机构信息

Department of Pharmacology, Yale University School of Medicine, New Haven, Connecticut 06520, USA.

出版信息

J Biol Chem. 2004 Dec 10;279(50):52324-30. doi: 10.1074/jbc.M408543200. Epub 2004 Sep 16.

Abstract

In response to brief synaptic stimulation that activates protein kinase A (PKA), the bag cell neurons of Aplysia trigger the onset of reproductive behaviors by generating a prolonged afterdischarge. In juvenile animals, such afterdischarges are inhibited by a high density of Ca2+ -activated K+ (BK) channels, encoded by the slo gene. An increase in this current also follows an afterdischarge in mature animals, contributing to a subsequent refractory state that limits reproductive behaviors. Using a bag cell cDNA library, we have isolated two alternative transcripts of the slo gene, differing in the presence (slo-a) or absence (slo-b) of a consensus phosphorylation site for PKA. Expression of either isoform in Chinese hamster ovary cells produced Ca2+ - and voltage-dependent channels with macroscopic and unitary properties matching those in bag cell neurons. The isoforms differed, however, in their response to application of the catalytic subunit of PKA, which reduced the open probability of Slo-a, an effect that was reversed by a PKA inhibitor. In contrast, PKA had no effect on Slo-b. By immunocytochemistry, we determined that the PKA-regulated Slo-a subunit is present in adult, but not juvenile, bag cell neurons. Patch clamp recordings from adult and juvenile bag cell neurons confirmed that PKA decreases BK channel activity only in adults. Our findings suggest that a change in the identity of Slo isoforms expressed during development allows mature neurons to generate afterdischarges that are required for reproduction.

摘要

作为对激活蛋白激酶A(PKA)的短暂突触刺激的反应,海兔的袋状细胞神经元通过产生长时间的后放电来触发生殖行为的开始。在幼年动物中,这种后放电受到由slo基因编码的高密度Ca2+激活K+(BK)通道的抑制。在成熟动物中,这种电流的增加也伴随着后放电,导致随后的不应期状态,从而限制生殖行为。利用袋状细胞cDNA文库,我们分离出了slo基因的两种可变转录本,它们在是否存在PKA的共有磷酸化位点上有所不同(slo-a存在,slo-b不存在)。在中国仓鼠卵巢细胞中表达任何一种同工型都会产生Ca2+和电压依赖性通道,其宏观和单通道特性与袋状细胞神经元中的通道相匹配。然而,这两种同工型对PKA催化亚基的应用反应不同,PKA催化亚基降低了Slo-a的开放概率,这种效应可被PKA抑制剂逆转。相比之下,PKA对Slo-b没有影响。通过免疫细胞化学,我们确定PKA调节的Slo-a亚基存在于成年袋状细胞神经元中,而不存在于幼年袋状细胞神经元中。对成年和幼年袋状细胞神经元的膜片钳记录证实,PKA仅在成年动物中降低BK通道活性。我们的研究结果表明,发育过程中表达的Slo同工型身份的变化使成熟神经元能够产生繁殖所需的后放电。

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