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Y-P30/皮抑素的表达分析及Y-P30肽的特性研究

Analysis of Y-P30/Dermcidin expression and properties of the Y-P30 peptide.

作者信息

Mikhaylova Marina, Schumacher Anne, Borutzki Corinna, Neumann Janine R, Macharadze Tamar, El-Mousleh Tarek, Wahle Petra, Zenclussen Ana C, Kreutz Michael R

机构信息

RG Neuroplasticity, Leibniz-Institute for Neurobiology, Magdeburg 39118, Germany.

出版信息

BMC Res Notes. 2014 Jun 26;7:400. doi: 10.1186/1756-0500-7-400.

Abstract

BACKGROUND

The survival promoting peptide Y-P30 has a variety of neuritogenic and neuroprotective effects in vitro and in vivo. In previous work we reported the expression of Y-P30/dermcidin in maternal peripheral blood mononuclear cells (PBMCs) and the transport of the protein to the fetal brain. In this study we analyzed hormonal regulation of Y-P30 in human immune cells and expression of Y-P30 in the placenta. We further studied the stability and secretion of the Y-P30 peptide.

RESULTS

We found indications that Y-P30 might be produced in human placenta. The Y-P30 mRNA was rarely found in isolated human PBMCs and alpha-feto-protein, human chorionic gonadotropin as well as estradiol combined with progesterone could not induce Y-P30 expression. Y-P30 was found to be extraordinarily stable; therefore, contamination with the peptide and the Y-P30/Dermcidin precursor mRNA is a serious concern in experiments looking at the expression of Y-P30/Dermcidin. In cultured cell lines and primary neurons we found that Y-P30 could be released, but neuronal uptake of Y-P30 was not observed.

CONCLUSIONS

Our data suggest that a source of Y-P30 apart from eccrine glands might be the placenta. The peptide can be secreted together with the signaling peptide and it might reach the fetal brain where it can exert its neuritogenic functions by binding to neuronal membranes.

摘要

背景

促生存肽Y-P30在体外和体内具有多种促神经突生长和神经保护作用。在之前的研究中,我们报道了Y-P30/皮肤杀菌肽在母体外周血单个核细胞(PBMC)中的表达以及该蛋白向胎儿脑内的转运。在本研究中,我们分析了人类免疫细胞中Y-P30的激素调节以及Y-P30在胎盘中的表达。我们还进一步研究了Y-P30肽的稳定性和分泌情况。

结果

我们发现有迹象表明Y-P30可能在人胎盘中产生。在分离出的人类PBMC中很少发现Y-P30 mRNA,并且甲胎蛋白、人绒毛膜促性腺激素以及雌二醇与孕酮联合使用均不能诱导Y-P30表达。发现Y-P30极其稳定;因此,在研究Y-P30/皮肤杀菌肽表达的实验中,肽和Y-P30/皮肤杀菌肽前体mRNA的污染是一个严重问题。在培养的细胞系和原代神经元中,我们发现Y-P30可以释放,但未观察到Y-P30被神经元摄取。

结论

我们的数据表明,除了外分泌腺之外,Y-P30的一个来源可能是胎盘。该肽可以与信号肽一起分泌,并且可能到达胎儿脑内,在那里它可以通过与神经元膜结合发挥其促神经突生长功能。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f2a0/4082292/92e87caf6b2e/1756-0500-7-400-1.jpg

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