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神经活性肽与加州海兔特定神经元中蛋白质分泌途径的关联:SCPA和SCPB在致密核心囊泡内容物及高尔基体反面的免疫定位

Association of neuroactive peptides with the protein secretory pathway in identified neurons of Aplysia californica: immunolocalization of SCPA and SCPB to the contents of dense-core vesicles and the trans face of the Golgi apparatus.

作者信息

Reed W, Weiss K R, Lloyd P E, Kupfermann I, Chen M, Bailey C H

机构信息

Center for Neurobiology and Behavior, Columbia University, New York, New York.

出版信息

J Comp Neurol. 1988 Jun 15;272(3):358-69. doi: 10.1002/cne.902720306.

DOI:10.1002/cne.902720306
PMID:3138290
Abstract

The subcellular distribution of two molluscan neuropeptides, the small cardioactive peptides A and B (SCPA and SCPB), has been determined in two identified Aplysia buccal ganglion neurons, B1 and B2. These neurons were previously shown to synthesize and release these neuropeptides. B1 and B2, identified by their size and location within the ganglion, were labeled by intrasomatic injection of an electron-dense particulate marker (ferritin or Imposil) permitting the unequivocal identification of their somata and proximal processes in thin sections. The somatic cytoplasm of both neurons had a conspicuous population of large dense-core vesicles along with a smaller number of compound vesicles and small lucent vesicles. All three vesicle types are found in the neurites within the neuropil and proximal axon in the esophageal nerve. Immunoreactivity was localized on the surface of thin sections by the indirect immunogold method. The primary antiserum was shown to recognize both SCPA and SCPB after the neuropeptides had been immobilized on protein-coated nitrocellulose membranes by means of glutaraldehyde, the primary fixative used to immobilize SCPA and SCPB in situ. SCP immunoreactivity was present in the lumens of the dense-core vesicles distributed throughout the cytoplasm of B1 and B2 and in dense-core regions of the Golgi apparatus in the somatic cytoplasm. Taken together with biochemical evidence that B1 and B2 synthesize and release SCPs, these data suggest that the neuropeptides are sequestered into the protein secretory pathway of B1 and B2, a distribution that supports the notion that the SCPs function physiologically as neurotransmitters or neuromodulators.

摘要

已在两种已鉴定的海兔口腔神经节神经元B1和B2中确定了两种软体动物神经肽——小促心肽A和B(SCPA和SCPB)的亚细胞分布。先前已证明这些神经元能合成并释放这些神经肽。通过神经节内的大小和位置鉴定出的B1和B2,通过体细胞内注射电子致密颗粒标记物(铁蛋白或Imposil)进行标记,从而能够在薄切片中明确识别它们的胞体和近端突起。两种神经元的体细胞胞质中都有大量明显的大致密核心囊泡,以及数量较少的复合囊泡和小透明囊泡。在神经纤维网内的神经突和食管神经的近端轴突中都发现了这三种囊泡类型。通过间接免疫金法将免疫反应定位在薄切片的表面。在神经肽通过戊二醛固定在蛋白包被的硝酸纤维素膜上后,已证明一抗能识别SCPA和SCPB,戊二醛是用于原位固定SCPA和SCPB的主要固定剂。SCP免疫反应存在于分布在B1和B2整个胞质中的致密核心囊泡的腔内,以及体细胞胞质中高尔基体的致密核心区域。结合生化证据表明B1和B2合成并释放SCPs,这些数据表明神经肽被隔离到B1和B2的蛋白质分泌途径中,这种分布支持了SCPs在生理上作为神经递质或神经调节剂发挥作用的观点。

相似文献

1
Association of neuroactive peptides with the protein secretory pathway in identified neurons of Aplysia californica: immunolocalization of SCPA and SCPB to the contents of dense-core vesicles and the trans face of the Golgi apparatus.神经活性肽与加州海兔特定神经元中蛋白质分泌途径的关联:SCPA和SCPB在致密核心囊泡内容物及高尔基体反面的免疫定位
J Comp Neurol. 1988 Jun 15;272(3):358-69. doi: 10.1002/cne.902720306.
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Biochemical and immunocytological localization of molluscan small cardioactive peptides in the nervous system of Aplysia californica.加州海兔神经系统中软体动物小的心脏活性肽的生化与免疫细胞定位
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Release of neuropeptides during intracellular stimulation of single identified Aplysia neurons in culture.
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Biochemical and morphological correlates of transmitter type in C2, an identified histaminergic neuron in Aplysia.海兔中已鉴定的组胺能神经元C2中神经递质类型的生化与形态学关联
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Morphology of two pairs of identified peptidergic neurons in the buccal ganglia of the mollusc Tritonia diomedea.
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Central peptidergic neurons regulate gut motility in Aplysia.中枢肽能神经元调节海兔的肠道蠕动。
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Modulation of peptide release from single identified Aplysia neurons in culture.培养的单个已鉴定的海兔神经元中肽释放的调节。
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Multiple neuropeptides in cholinergic motor neurons of Aplysia: evidence for modulation intrinsic to the motor circuit.海兔胆碱能运动神经元中的多种神经肽:运动回路内在调制的证据
Proc Natl Acad Sci U S A. 1987 May;84(10):3486-90. doi: 10.1073/pnas.84.10.3486.
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Modulation of calcium current and diverse K+ currents in identified Hermissenda neurons by small cardioactive peptide B.小活性心肽B对已鉴定的艾氏海兔神经元中钙电流和多种钾电流的调节作用
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Biochemical and immunocytological localization of the neuropeptides FMRFamide, SCPA, SCPB, to neurons involved in the regulation of feeding in Aplysia.神经肽FMRF酰胺、SCPA、SCPB在参与调控海兔摄食的神经元中的生化及免疫细胞定位。
J Neurosci. 1987 Apr;7(4):1123-32. doi: 10.1523/JNEUROSCI.07-04-01123.1987.

引用本文的文献

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Multifaceted Expression of Peptidergic Modulation in the Feeding System of Aplysia.多肽调制在海兔摄食系统中的多方面表现。
ACS Chem Neurosci. 2018 Aug 15;9(8):1917-1927. doi: 10.1021/acschemneuro.7b00447. Epub 2018 Jan 24.
2
Presynaptic target of Ca2+ action on neuropeptide and acetylcholine release in Aplysia californica.加州海兔中Ca2+对神经肽和乙酰胆碱释放作用的突触前靶点。
J Physiol. 2001 Sep 15;535(Pt 3):647-62. doi: 10.1111/j.1469-7793.2001.00647.x.
3
Peptide cotransmitter release from motorneuron B16 in aplysia californica: costorage, corelease, and functional implications.
加州海兔运动神经元B16中肽类共递质的释放:共储存、共同释放及其功能意义。
J Neurosci. 2000 Mar 1;20(5):2036-42. doi: 10.1523/JNEUROSCI.20-05-02036.2000.
4
The secretion of classical and peptide cotransmitters from a single presynaptic neuron involves a synaptobrevin-like molecule.单个突触前神经元分泌经典递质和肽类共递质涉及一种类似突触小泡蛋白的分子。
J Neurosci. 1997 Apr 1;17(7):2338-47. doi: 10.1523/JNEUROSCI.17-07-02338.1997.
5
Costorage and corelease of modulatory peptide cotransmitters with partially antagonistic actions on the accessory radula closer muscle of Aplysia californica.调节性肽共递质在加州海兔副齿舌闭肌上具有部分拮抗作用的共储存和共同释放
J Neurosci. 1996 Dec 15;16(24):8092-104. doi: 10.1523/JNEUROSCI.16-24-08092.1996.
6
Frequency-dependent release of peptide cotransmitters from identified cholinergic motor neurons in Aplysia.海兔中已鉴定的胆碱能运动神经元肽类共递质的频率依赖性释放。
Proc Natl Acad Sci U S A. 1989 Nov;86(22):9034-8. doi: 10.1073/pnas.86.22.9034.
7
Peptidergic motoneurons in the buccal ganglia of Aplysia californica: immunocytochemical, morphological, and physiological characterizations.加利福尼亚海兔颊神经节中的肽能运动神经元:免疫细胞化学、形态学及生理学特征
J Comp Physiol A. 1991 Mar;168(3):323-36. doi: 10.1007/BF00198352.