nutrition care

营养护理
  • 文章类型: Journal Article
    新的发现强调了精神疾病与肠道微生物群的营养和生态失调的关联。但是潜在的机制,特别是在精神分裂症(SZ),仍未澄清。
    我们通过对肠道宏基因组进行测序,对SZ患者进行了病例对照研究(病例与对照=100:52);测量粪便和血浆非靶向代谢组;包括短,medium-,和长链脂肪酸;和靶向代谢物,以及每日食物摄入量的记录细节。
    宏基因组分析发现,SZ患者肠道中糖酶分解物种的富集和碳水化合物分解代谢途径和酶的丰度降低,但与蛋白质摄入量显着减少相比,肽酶的丰度增加。粪便代谢组分析发现许多蛋白质分解代谢产物的浓度增加,包括氨基酸(AA),尿素,支链短链脂肪酸,SZ患者的芳香族AAs的各种含氮衍生物。蛋白质合成,以宏基因组中丰富的AA-生物合成途径和氨酰-tRNA转移酶为代表,显著下降。基于其丰度的诊断随机森林模型的AUC(曲线下面积)达到85%和91%,分别。粪便中AA发酵酶和产物的水平与精神症状的严重程度均呈正相关。
    我们的发现揭示了SZ患者肠道微生物组明显的菌群失调,在健康条件下,微生物代谢主要由蛋白质发酵和碳水化合物发酵和蛋白质合成。肠道微生物的异常大量营养素代谢突出了营养护理的重要性以及在SZ中开发微生物群靶向疗法的潜力。
    Emerging findings highlighted the associations of mental illness to nutrition and dysbiosis in the intestinal microbiota, but the underlying mechanisms, especially in schizophrenia (SZ), remain unclarified.
    We conducted a case-control study of SZ patients (case to control=100:52) by performing sequencing of the gut metagenome; measurement of fecal and plasma non-targeted metabolome; including short-, medium-, and long-chain fatty acids; and targeted metabolites, along with recorded details of daily intakes of food.
    The metagenome analysis uncovered enrichment of asaccharolytic species and reduced abundance of carbohydrate catabolism pathways and enzymes in the gut of SZ patients, but increased abundance of peptidases in contrast to their significantly reduced protein intake. Fecal metabolome analysis identified increased concentrations of many protein catabolism products, including amino acids (AAs), urea, branched short-chain fatty acids, and various nitrogenous derivates of aromatic AAs in SZ patients. Protein synthesis, represented by the abundance of AA-biosynthesis pathways and aminoacyl-tRNA transferases in metagenome, was significantly decreased. The AUCs (area under the curve) of the diagnostic random forest models based on their abundance achieved 85% and 91%, respectively. The fecal levels of AA-fermentative enzymes and products uniformly showed positive correlations with the severity of psychiatric symptoms.
    Our findings revealed apparent dysbiosis in the intestinal microbiome of SZ patients, where microbial metabolism is dominated by protein fermentation and shift from carbohydrate fermentation and protein synthesis in healthy conditions. The aberrant macronutrient metabolism by gut microbes highlights the importance of nutrition care and the potential for developing microbiota-targeted therapeutics in SZ.
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