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生长抑素及相关肽对兔海马CA1区影响的进一步研究。

Further studies of the effects of somatostatin and related peptides in area CA1 of rabbit hippocampus.

作者信息

Scharfman H E, Schwartzkroin P A

机构信息

Department of Neurological Surgery, University of Washington, Seattle 98195.

出版信息

Cell Mol Neurobiol. 1988 Dec;8(4):411-29. doi: 10.1007/BF00711226.

Abstract
  1. In slice studies of mature and immature CA1 hippocampal pyramidal cells from rabbit, somatostatin 14 (SS14), the related peptide somatostatin 28(1-12) [SS(1-12)], and the synthetic analogue of somatostatin 14, SMS-201995 (SMS), had similar effects. When pressure-ejected onto cell somata, these peptides elicited depolarizations, often accompanied by action potential discharge. When applied to dendrites, the peptides produced depolarizations or hyperpolarizations. 2. When a large amount of one of the three somatostatin-related (SS) peptides was applied to the slice at some distance from the impaled cell, hyperpolarizations were observed that were not always blocked by tetrodotoxin (TTX) or low Ca2+. Since SS peptides were also found to depolarize interneurons in area CA1, it seems likely that the hyperpolarizations that were blocked by TTX or low Ca2+ were mediated via excitation of interneurons that in turn hyperpolarized pyramidal cells. 3. All SS peptides also had long-lasting effects on CA1 pyramidal cells that led to spontaneous firing of action potentials and an increase in the number of action potentials discharged in response to a given depolarizing current pulse; the spontaneous discharge effect was blocked by TTX or low Ca2+ plus Mn2+ and, thus, appeared to have a presynaptic mechanism. However, the increase in discharge in response to a constant depolarizing current pulse was not dependent on intact synaptic transmission and, therefore, was attributable to a direct postsynaptic effect of the SS peptides.
摘要
  1. 在对来自兔的成熟和未成熟CA1海马锥体细胞的切片研究中,生长抑素14(SS14)、相关肽生长抑素28(1-12)[SS(1-12)]以及生长抑素14的合成类似物SMS-201995(SMS)具有相似的作用。当通过压力喷射到细胞体上时,这些肽引发去极化,常常伴有动作电位发放。当应用于树突时,这些肽产生去极化或超极化。2. 当将三种生长抑素相关(SS)肽之一大量应用于距刺入细胞一定距离的切片时,观察到超极化,这种超极化并不总是被河豚毒素(TTX)或低钙所阻断。由于还发现SS肽可使CA1区的中间神经元去极化,因此似乎被TTX或低钙阻断的超极化是通过中间神经元的兴奋介导的,进而使锥体细胞超极化。3. 所有SS肽对CA1锥体细胞也有持久作用,导致动作电位的自发发放以及对给定去极化电流脉冲发放的动作电位数量增加;自发发放效应被TTX或低钙加锰阻断,因此似乎有一个突触前机制。然而,对恒定去极化电流脉冲的发放增加并不依赖于完整的突触传递,因此可归因于SS肽的直接突触后效应。

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本文引用的文献

1
PATHWAY OF POSTSYNAPTIC INHIBITION IN THE HIPPOCAMPUS.海马体中突触后抑制的通路。
J Neurophysiol. 1964 Jul;27:608-19. doi: 10.1152/jn.1964.27.4.608.
4

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