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通过血清靶向代谢组学分析对唐氏综合征相关代谢及氧化/亚硝化应激改变与生理性年龄相关变化进行生化鉴别。

Biochemical Discrimination of the Down Syndrome-Related Metabolic and Oxidative/Nitrosative Stress Alterations from the Physiologic Age-Related Changes through the Targeted Metabolomic Analysis of Serum.

作者信息

Lazzarino Giacomo, Amorini Angela M, Mangione Renata, Saab Miriam Wissam, Di Stasio Enrico, Di Rosa Michelino, Tavazzi Barbara, Lazzarino Giuseppe, Onder Graziano, Carfì Angelo

机构信息

UniCamillus-Saint Camillus International University of Health Sciences, Via di Sant'Alessandro 8, 00131 Rome, Italy.

Department of Biomedical and Biotechnological Sciences, Division of Medical Biochemistry, University of Catania, Via S. Sofia 97, 95123 Catania, Italy.

出版信息

Antioxidants (Basel). 2022 Jun 20;11(6):1208. doi: 10.3390/antiox11061208.

Abstract

Down Syndrome (DS) is a neurodevelopmental disorder that is characterized by an accelerated aging process, frequently associated with the development of Alzheimer's disease (AD). Previous studies evidenced that DS patients have various metabolic anomalies, easily measurable in their serum samples, although values that were found in DS patients were compared with those of age-matched non-DS patients, thus hampering to discriminate the physiologic age-related changes of serum metabolites from those that are truly caused by the pathologic processes associated with DS. In the present study we performed a targeted metabolomic evaluation of serum samples from DS patients without dementia of two age classes (Younger DS Patients, YDSP, aging 20-40 years; Aged DS Patients, ADSP, aging 41-60 years), comparing the results with those that were obtained in two age classes of non-DS patients (Younger non-DS Patients, YnonDSP, aging 30-60 years; Aged-nonDS Patients, AnonDSP, aging 75-90 years). Of the 36 compounds assayed, 30 had significantly different concentrations in Pooled non-DS Patients (PnonDSP), compared to Pooled DS Patients (PDSP). Age categorization revealed that 11/30 compounds were significantly different in AnonDSP, compared to YnonDSP, indicating physiologic, age-related changes of their circulating concentrations. A comparison between YDSP and ADSP showed that 19/30 metabolites had significantly different values from those found in the corresponding classes of non-DS patients, strongly suggesting pathologic, DS-associated alterations of their serum levels. Twelve compounds selectively and specifically discriminated PnonDSP from PDSP, whilst only three discriminated YDSP from ADSP. The results allowed to determine, for the first time and to the best of our knowledge, the true, age-independent alterations of metabolism that are measurable in serum and attributable only to DS. These findings may be of high relevance for better strategies (pharmacological, nutritional) aiming to specifically target the dysmetabolism and decreased antioxidant defenses that are associated with DS.

摘要

唐氏综合征(DS)是一种神经发育障碍,其特征是衰老过程加速,常与阿尔茨海默病(AD)的发展相关。先前的研究表明,DS患者存在各种代谢异常,在其血清样本中易于检测到,尽管将DS患者的检测值与年龄匹配的非DS患者进行了比较,但这妨碍了区分血清代谢物与年龄相关的生理变化和由与DS相关的病理过程真正引起的变化。在本研究中,我们对两个年龄组(年轻DS患者,20 - 40岁;老年DS患者,41 - 60岁)无痴呆的DS患者的血清样本进行了靶向代谢组学评估,并将结果与两个年龄组的非DS患者(年轻非DS患者,30 - 60岁;老年非DS患者,75 - 90岁)的结果进行比较。在所检测的36种化合物中,与合并的DS患者(PDSP)相比,合并的非DS患者(PnonDSP)中有30种化合物的浓度存在显著差异。年龄分类显示,与年轻非DS患者相比,老年非DS患者中11/30的化合物存在显著差异,表明其循环浓度存在与年龄相关的生理变化。年轻DS患者和老年DS患者之间的比较表明,19/30的代谢物与相应非DS患者组中的值存在显著差异,强烈提示其血清水平存在与DS相关的病理改变。12种化合物能够选择性且特异性地区分PnonDSP与PDSP,而只有3种化合物能够区分年轻DS患者与老年DS患者。据我们所知,这些结果首次确定了血清中可测量的、仅归因于DS的与年龄无关的真正代谢改变。这些发现对于旨在特异性针对与DS相关的代谢紊乱和抗氧化防御降低的更好策略(药物、营养)可能具有高度相关性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1a81/9219806/ca3a9f1dd280/antioxidants-11-01208-g001.jpg

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