对大鼠的蛋白质组学分析揭示了重度抑郁症与饮食锌缺乏之间的共同机制。

Proteomics analysis in rats reveals convergent mechanisms between major depressive disorder and dietary zinc deficiency.

作者信息

Gąsior Łukasz, Pochwat Bartłomiej, Zaręba-Kozioł Monika, Włodarczyk Jakub, Grabrucker Andreas Martin, Szewczyk Bernadeta

机构信息

Maj Institute of Pharmacology, Department of Neurobiology, Polish Academy of Sciences, Smętna 12, Kraków, 31-343, Poland.

Laboratory of Cell Biophysics, Nencki Institute of Experimental Biology, Polish Academy of Sciences, Ludwika Pasteura 3, Warsaw, 02-093, Poland.

出版信息

Pharmacol Rep. 2025 Feb;77(1):145-157. doi: 10.1007/s43440-024-00681-7. Epub 2024 Dec 3.

DOI:10.1007/s43440-024-00681-7

PMID:39623245

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11743416/

Abstract

BACKGROUND

Preclinical and clinical studies have shown that dietary zinc deficiency can lead to symptoms similar to those observed in major depressive disorder (MDD). However, the underlying molecular mechanisms remain unclear. To investigate these mechanisms, we examined proteomic changes in the prefrontal cortex (PFC) and hippocampus (HP) of rats, two critical brain regions implicated in the pathophysiology of depression.

METHODS

Rats were fed diets either adequate in zinc (ZnA, 50 mg Zn/kg) or deficient in zinc (ZnD, <3 mg/kg) for four weeks. High-throughput proteomic analysis was used to detect changes in protein expression, supplemented by enzyme activity assay for mitochondrial complexes I and IV, examining their functional impacts.

RESULTS

ZnD led to significant alterations in protein expression related to zinc transport and mitochondrial function. Proteomic analysis revealed changes in zinc transporter family members such as Slc30a1 (6.64 log2FC), Slc30a3 (-2.32 log2FC), Slc30a4 (2.87 log2FC), Slc30a5 (5.90 log2FC), Slc30a6 (1.50 log2FC), and Slc30a7 (2.17 log2FC) in the PFC, and Slc30a3 (-1.02 log2FC), Slc30a5 (-1.04 log2FC), and Slc30a7 (1.08 log2FC) in the HP of rats subjected to ZnD. Furthermore, ZnD significantly affected essential mitochondrial activity proteins, including Atp5pb (3.25 log2FC), Cox2 (2.28 log2FC), Atp5me (2.04 log2FC), Cyc1 (2.30 log2FC), Cox4i1 (1.23 log2FC), Cox7c (1.63 log2FC), and Cisd1 (1.55 log2FC), with a pronounced decrease in complex I activity in the PFC.

CONCLUSIONS

Our study demonstrates that ZnD leads to significant proteomic changes in the PFC and HP of rats. Specifically, ZnD alters the expression of zinc transporter proteins and proteins critical for mitochondrial function. The significant decrease in complex I activity in the PFC further underscores the impact of ZnD on mitochondrial function. These results highlight the molecular mechanisms by which ZnD can influence brain function and contribute to symptoms similar to those observed in depression.

摘要

背景

临床前和临床研究表明，饮食中锌缺乏可导致与重度抑郁症（MDD）中观察到的症状相似的症状。然而，潜在的分子机制仍不清楚。为了研究这些机制，我们检测了大鼠前额叶皮质（PFC）和海马体（HP）的蛋白质组变化，这两个关键脑区与抑郁症的病理生理学有关。

方法

将大鼠喂食锌充足（ZnA，50毫克锌/千克）或锌缺乏（ZnD，<3毫克/千克）的饮食四周。采用高通量蛋白质组分析检测蛋白质表达变化，并通过线粒体复合物I和IV的酶活性测定进行补充，以研究它们的功能影响。

结果

ZnD导致与锌转运和线粒体功能相关的蛋白质表达发生显著改变。蛋白质组分析显示，在ZnD处理的大鼠的PFC中，锌转运蛋白家族成员如Slc30a1（6.64 log2FC）、Slc30a3（-2.32 log2FC）、Slc30a4（2.87 log2FC）、Slc30a5（5.90 log2FC）、Slc30a6（1.50 log2FC）和Slc30a7（2.17 log2FC）发生变化，在HP中，Slc30a3（-1.02 log2FC）、Slc30a5（-1.04 log2FC）和Slc30a7（1.08 log2FC）发生变化。此外，ZnD显著影响重要的线粒体活性蛋白，包括Atp5pb（3.25 log2FC）、Cox2（2.28 log2FC）、Atp5me（2.04 log2FC）、Cyc1（2.30 log2FC）、Cox4i1（1.23 log2FC）、Cox7c（1.63 log2FC）和Cisd1（1.55 log2FC），PFC中的复合物I活性明显降低。