Sex chromosome complement interacts with gonadal hormones in determining regional-specific neuroactive steroid levels in plasma, hippocampus, and hypothalamus. A study using the four core genotype mouse model

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS ACS Applied Bio Materials Pub Date : 2024-03-28 DOI:10.1016/j.jsbmb.2024.106514
Lucia Cioffi , Daniela Grassi , Silvia Diviccaro , Donatella Caruso , Daniel Pinto-Benito , Maria-Angeles Arevalo , Luis Miguel Garcia-Segura , Roberto Cosimo Melcangi , Silvia Giatti
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Abstract

An important aspect of the neuromodulatory and neuroprotective actions exerted by neuroactive steroids is that they are sex-specific, as determined by the sexually dimorphic levels of these molecules in plasma and the nervous tissue. Thus, the identification of the factors that generate the sex-dimorphic levels of neuroactive steroids may be crucial from a neuroprotectant perspective. The main driver for sex determination in mammals is the SRY gene and the subsequent presence of a specific gonad: testes for males and ovaries for females, thus producing hormonal compounds, primarily androgens and estrogens, respectively. Nowadays, it is well established that despite the relevance of gonads, other factors control sexual features, and, among them, sex chromosome complement is highly relevant. In this study, neuroactive steroids were evaluated by liquid chromatography-tandem mass spectrometry in the hypothalamus, the hippocampus, and plasma of the four core genotype mouse model, to determine the relative contribution of sex chromosome complement and gonads in determining their sex dimorphic levels. The data obtained reveal that although gonads are the main contributing factor for sex differences in neuroactive steroid levels, the levels of some neuroactive steroids, including testosterone, are also influenced in brain and plasma by tissue-specific actions of sex chromosomes. The data presented here adds a new piece to the puzzle of steroid level regulation, which may be useful in designing sex-specific neuroprotective approaches to pathological conditions affecting the nervous system.

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性染色体互补与性腺激素相互作用,决定血浆、海马和下丘脑中区域特异性神经活性类固醇水平。一项利用四核心基因型小鼠模型进行的研究。
神经活性类固醇所发挥的神经调节和神经保护作用的一个重要方面是它们具有性别特异性,这是由血浆和神经组织中这些分子的性别二态水平所决定的。因此,从神经保护剂的角度来看,确定产生神经活性类固醇性别二态水平的因素可能至关重要。哺乳动物性别决定的主要驱动力是 SRY 基因和随后特定性腺的存在:雄性睾丸和雌性卵巢,从而分别产生激素化合物,主要是雄激素和雌激素。如今,尽管性腺与性特征有关,但其他因素也控制着性特征,其中性染色体互补性与性特征密切相关。本研究采用液相色谱-串联质谱法对四种核心基因型小鼠下丘脑、海马和血浆中的神经活性类固醇进行了评估,以确定性染色体互补和性腺在决定其性别二态性水平方面的相对贡献。获得的数据显示,虽然性腺是造成神经活性类固醇水平性别差异的主要因素,但包括睾酮在内的一些神经活性类固醇的水平在大脑和血浆中也受到性染色体组织特异性作用的影响。
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来源期刊
ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
CiteScore
9.40
自引率
2.10%
发文量
464
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