First-episode mild depression in young adults is a pre-proatherogenic condition even in the absence of subclinical metabolic syndrome: lowered lecithin-cholesterol acyltransferase as a key factor.

Neuro endocrinology letters Pub Date : 2024-12-22

Michael Maes, Asara Vasupanrajit, Ketsupar Jirakran, Bo Zhou, Chavit Tunvirachaisakul, Abbas F Almulla

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Abstract

Background: Major depression is classified into distinct subtypes: simple (SDMD) and major dysmood disorder (MDMD). MDMD patients exhibit elevated atherogenicity and decreased reverse cholesterol transport (RCT). However, comprehensive data regarding lipid metabolism is absent in first episode (FE)-SDMD.

Aims: In this case-control study, plasma lipid levels, lecithin-cholesterol acyltransferase (LCAT), free cholesterol, apolipoprotein (Apo)A1, ApoB, and ApoE are compared between academic students with first episode SDMD (FE-SDMD) (n = 44) or SDMD (n = 64) and control students (n = 44), after excluding those with metabolic syndrome (MetS).

Results: LCAT is decreased, and free cholesterol and ApoE increased in subjects with SDMD and FE-SDMD as compared with controls. There were no significant alterations in high-density lipoprotein cholesterol (HDLc), ApoA1, RCT, ApoB and triglycerides in SDMD. LCAT, free cholesterol and atherogenicity indices are significantly associated with suicidal behaviors and the SDMD phenome. The effects of LCAT on those phenome features is completely mediated by free cholesterol and brooding. SDMD and FE-SDMD patients without signs of subclinical MetS show lowered LCAT and increased free cholesterol as compared with normal controls. There are significant interactions between the SDMD and FE-SDMD diagnosis and subclinical MetS, which result in decreased HDLc and RCT, and an increased ApoB/ApoA ratio.

Discussion: FE-SDMD and SDMD are pre-proatherogenic states, because of decreased LCAT, and increased free cholesterol and ApoE, and their intersections with subclinical MetS. These aberrations may drive atherogenicity, and activation of peripheral and central oxidative, neuro-immune, and degenerative pathways. Individuals with FE-SDMD should be screened and treated for increased atherogenicity risk by measuring free cholesterol and ApoE.

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即使在没有亚临床代谢综合征的情况下，年轻人的首发轻度抑郁症也是一种动脉粥样硬化前状态：卵磷脂-胆固醇酰基转移酶降低是一个关键因素。

背景：重度抑郁症可分为不同的亚型：单纯性（SDMD）和重度心境障碍（MDMD）。MDMD患者表现出动脉粥样硬化性升高和逆向胆固醇转运降低（RCT）。然而，关于首发(FE)-SDMD的脂质代谢的综合数据缺乏。目的：在本病例对照研究中，在排除代谢综合征（MetS）后，比较首发SDMD (FE-SDMD) （n = 44）或SDMD （n = 64）学生与对照学生（n = 44）的血脂水平、卵磷脂-胆固醇酰基转移酶（LCAT）、游离胆固醇、载脂蛋白（Apo）A1、ApoB和ApoE。结果：与对照组相比，SDMD和FE-SDMD患者LCAT降低，游离胆固醇和ApoE升高。SDMD患者的高密度脂蛋白胆固醇（HDLc）、ApoA1、RCT、ApoB和甘油三酯均无显著变化。LCAT、游离胆固醇和动脉粥样硬化指数与自杀行为和SDMD现象显著相关。LCAT对这些表型特征的影响完全是由游离胆固醇和忧郁介导的。与正常对照相比，无亚临床MetS症状的SDMD和FE-SDMD患者的LCAT降低，游离胆固醇升高。SDMD和FE-SDMD诊断与亚临床MetS之间存在显著的相互作用，导致HDLc和RCT降低，ApoB/ApoA比值升高。讨论：FE-SDMD和SDMD是动脉粥样硬化前的状态，因为LCAT降低，游离胆固醇和ApoE升高，它们与亚临床MetS有交叉。这些异常可能导致动脉粥样硬化，激活外周和中枢氧化、神经免疫和退行性通路。FE-SDMD患者应该通过检测游离胆固醇和载脂蛋白e来筛查和治疗动脉粥样硬化风险。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Neuro endocrinology letters

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