astaxanthin

虾青素
  • 文章类型: Journal Article
    干眼症(DED)是临床常见的眼病。DED的关键发病机制是高渗透压激活角膜上皮细胞和免疫细胞中的氧化应激信号通路,因此,产生炎症分子。干眼的复杂病理变化仍需阐明以促进治疗。在这项研究中,我们发现虾青素(AST)可以通过SLC7A11/GPX4途径预防DED。用AST治疗后,SLC7A11/GPX4通路在DED体内和体外均呈正激活,伴有自噬增强和铁凋亡降低。在高渗透压诱导的DED角膜上皮细胞中,AST增加铁蛋白的表达,促进铁的储存,减少Fe2+过载。它增加了谷胱甘肽(GSH)和GPX4,清除了活性氧(ROS)和脂质过氧化物,拯救了线粒体结构以防止铁中毒。此外,铁抑制素-1(Fer-1)抑制铁凋亡,铁螯合剂去铁胺甲磺酸盐(DFO),或AST可以激活健康的自噬通量。此外,在干眼症小鼠模型中,AST上调SLC7A11和GPX4并抑制铁凋亡。总结一下,我们发现AST可以通过增强SLC7A11/GPX4途径来改善DED,主要影响氧化应激,自噬,和铁性过程。
    Dry eye disease (DED) is a common eye disease in clinical practice. The crucial pathogenesis of DED is that hyperosmolarity activates oxidative stress signaling pathways in corneal epithelial and immune cells and, thus, produces inflammatory molecules. The complex pathological changes in the dry eye still need to be elucidated to facilitate treatment. In this study, we found that astaxanthin (AST) can protect against DED through the SLC7A11/GPX4 pathway. After treatment with AST, the SLC7A11/GPX4 pathway was positively activated in DED both in vivo and in vitro, accompanied by enhanced autophagy and decreased ferroptosis. In hyperosmolarity-induced DED corneal epithelial cells, AST increased the expression of ferritin to promote iron storage and reduce Fe2+ overload. It increased glutathione (GSH) and GPX4, scavenged reactive oxygen species (ROS) and lipid peroxide, and rescued the mitochondrial structure to prevent ferroptosis. Furthermore, inhibition of ferroptosis by ferrostatin-1 (Fer-1), iron chelator deferoxamine mesylate (DFO), or AST could activate healthy autophagic flux. In addition, in a dry eye mouse model, AST upregulated SLC7A11 and GPX4 and inhibited ferroptosis. To summarize, we found that AST can ameliorate DED by reinforcing the SLC7A11/GPX4 pathway, which mainly affects oxidative stress, autophagy, and ferroptosis processes.
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  • 文章类型: Journal Article
    湖水红球菌(Girod-Chantrans)Rostafinski(Chlorophyta)是虾青素最丰富的微藻来源。来自H.lacustris的天然虾青素已被广泛研究并用于世界范围内的商业生产。在这项研究中,我们检查了11种抗生素(硫酸双氢链霉素,新霉素,氯霉素,青霉素,链霉素,氨苄青霉素,卡那霉素,庆大霉素,潮霉素B,四环素,和巴龙霉素)对生物质干重的影响,增长,使用Jaworski\的无氮源培养基,以及H.lacustris的虾青素产量。在氨苄青霉素的存在下,H.lacustris中的虾青素含量得到了提高(0.25g/L,0.5g/L,1g/L),氯霉素(0.25g/L),和青霉素(0.25g/L,0.5g/L,1g/L)与第15天的对照相比。与对照相比,添加青霉素(0.5g/L)在第15天获得虾青素含量的最大增加(6.69倍)。同样,在第15天,对于添加青霉素(0.5g/L)生长的H.lacustris培养物,细胞数量也是最高的。
    Haematococcus lacustris (Girod-Chantrans) Rostafinski (Chlorophyta) is the richest microalgal source of astaxanthin. Natural astaxanthin from H. lacustris has been widely studied and used for commercial production worldwide. In this study, we examined the effects of 11 antibiotics (dihydrostreptomycin sulphate, neomycin, chloramphenicol, penicillin, streptomycin, ampicillin, kanamycin, gentamycin, hygromycin B, tetracycline, and paromomycin) on the biomass dry weight, growth, and astaxanthin yield of H. lacustris using Jaworski\'s medium without a nitrogen source. Astaxanthin content in H. lacustris was improved in the presence of ampicillin (0.25 g/L, 0.5 g/L, 1 g/L), chloramphenicol (0.25 g/L), and penicillin (0.25 g/L, 0.5 g/L, 1 g/L) in comparison to the control on day 15. The greatest increase in astaxanthin content on day 15 (6.69-fold) was obtained with the addition of penicillin (0.5 g/L) in comparison to the control. Similarly, on day 15, the cell numbers were also the highest for the H. lacustris culture grown with the addition of penicillin (0.5 g/L).
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  • 文章类型: Journal Article
    这项在大鼠佐剂性关节炎中进行的体内研究旨在促进对虾青素的治疗特性的理解,以便在单一疗法和标准RA治疗中治疗类风湿关节炎(RA)。甲氨蝶呤(MTX),联合治疗。主要目标是阐明虾青素的全部治疗潜力,评估其剂量依赖性,并比较其与其他类胡萝卜素如β-胡萝卜素和β-隐黄质(KXAN)的单药治疗效果。此外,使用不同来源的虾青素引起的治疗活性的潜在差异,合成(ASYN)与分离自Blakesleatrispora(ASTAP),使用单向方差分析(Tukey-Kramer事后检验)进行评估。KXAN在单药治疗中降低血浆MMP-9水平最有效,明显优于MTX,减少后爪肿胀。ASTAP和ASYN的作用差异已在各种生物特征中观察到,抗炎,和抗氧化参数。在与MTX的联合治疗中,ASYN+MTX组合被证明是更好的。这些发现,特别是KXAN和ASYNMTX的显着抗关节炎作用,可能是进一步临床前研究的基础。
    This in vivo study performed in rat adjuvant arthritis aims to advance the understanding of astaxanthin\'s therapeutic properties for the possible treatment of rheumatoid arthritis (RA) in monotherapy and along with the standard RA treatment, methotrexate (MTX), in combination therapy. The main goal was to elucidate astaxanthin\'s full therapeutic potential, evaluate its dose dependency, and compare its effects in monotherapy with other carotenoids such as β-carotene and β-cryptoxanthin (KXAN). Moreover, potential differences in therapeutic activity caused by using different sources of astaxanthin, synthetic (ASYN) versus isolated from Blakeslea trispora (ASTAP), were evaluated using one-way ANOVA (Tukey-Kramer post hoc test). KXAN was the most effective in reducing plasma MMP-9 levels in monotherapy, significantly better than MTX, and in reducing hind paw swelling. The differences in the action of ASTAP and ASYN have been observed across various biometric, anti-inflammatory, and antioxidative parameters. In combined therapy with MTX, the ASYN + MTX combination proved to be better. These findings, especially the significant anti-arthritic effect of KXAN and ASYN + MTX, could be the basis for further preclinical studies.
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  • 文章类型: Journal Article
    本研究旨在评估口服虾青素(ATX)对3岁阿拉伯赛马炎症标志物的影响。尽管在啮齿动物模型和人类运动员中观察到的ATX具有公认的抗氧化和抗炎特性,对马受试者的影响仍然未知。这项研究涉及一项对照试验,14匹马接受ATX(6匹马)或安慰剂(8匹马)。监控了四个月的比赛训练。炎性细胞因子:TNFα,IFNγ,IL-6、IL-10和前列腺素E(PGE),每月进行测量,以评估ATX对炎症反应的影响。结果表明,在研究过程中,ATX和对照组之间的测量参数没有显着差异。然而,在两组中观察到TNFα和IFNγ水平的显着时间依赖性下降(p=0.001),这表明定期训练自然会调节炎症反应。此外,在研究的早期阶段,TNFα和IFNγ之间存在正相关(p<0.001),在后期阶段,IL-6和IL-10之间存在正相关(p=0.008)。血液学参数保持稳定并在参考范围内,表明补充ATX没有不良反应。性能指标,包括完成和获胜的比赛数量,两组之间没有显着差异,表明ATX在研究条件下没有提高运动表现。总的来说,而ATX补充既不影响细胞因子水平也不影响阿拉伯赛马的性能,常规训练的天然抗炎作用是明显的.需要进一步的研究来探索不同条件下补充ATX的潜在益处。例如患有亚临床炎症或不同训练方案的马,充分阐明其在马运动医学中的作用和应用。
    This study aimed to evaluate the oral supplementation of astaxanthin (ATX) on inflammatory markers in 3-year-old Arabian racehorses. Despite the recognized antioxidant and anti-inflammatory properties of ATX observed in vitro in rodent models and in human athletes, the effects in equine subjects remain unknown. This study involved a controlled trial with 14 horses receiving either ATX (six horses) or a placebo (eight horses), monitored over four months of race training. Inflammatory cytokines: TNFα, IFNγ, IL-6, IL-10, and prostaglandin E (PGE), were measured monthly to assess the impact of ATX on the inflammatory response. The results indicated no significant differences in measured parameters between the ATX and the control group during the study. However, a significant time-dependent decrease in TNFα and IFNγ levels (p = 0.001) was observed in both groups, suggesting that regular training naturally modulates inflammatory responses. Moreover, positive correlations were noted between TNFα and IFNγ (p < 0.001) in the early phase of the study and between IL-6 and IL-10 (p = 0.008) in the later phase. Hematological parameters remained stable and within reference ranges, indicating no adverse effects of ATX supplementation. Performance metrics, including the number of races completed and wins, showed no significant differences between groups, suggesting that ATX did not enhance athletic performance under the study conditions. Overall, while ATX supplementation affected neither cytokine levels nor performance in Arabian racehorses, the natural anti-inflammatory effects of regular training were evident. Further research is needed to explore potential benefits of ATX supplementation under different conditions, such as in horses with subclinical inflammation or varying training regimens, to fully clarify its role and applications in equine sports medicine.
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  • 文章类型: Journal Article
    胸腺,动物的中央淋巴器官,作为T细胞发育的位点,分化和成熟,对适应性免疫至关重要。胸腺对于维持组织稳态以防止肿瘤和组织损伤至关重要。过度活跃或延长的免疫应答可导致来自增加的活性氧的产生的氧化应激。热应激诱导氧化应激并压倒天然抗氧化剂防御机制。本研究的目的是研究虾青素对热诱导的鸡胸腺氧化应激和细胞凋亡的保护特性。通过比较三组之间的生长性能和基因信号通路:热中性,热应力,和虾青素的热应激。热中性温度为21-22°C,热应力温度为32-35℃。两个热应激组都经历了生长性能下降,而虾青素治疗组的下降幅度略小。NF-kB的上调激活了炎症反应和抗氧化防御系统,NFE2L2,PPARα,细胞保护能力,与热中性组相比,热应激期间的凋亡基因途径。然而,表达水平在热中性和热应激与抗氧化剂组之间没有显着差异,提示虾青素可以减轻炎症和氧化应激损伤。
    The thymus, a central lymphoid organ in animals, serves as the site for T cell development, differentiation and maturation, vital to adaptive immunity. The thymus is critical for maintaining tissue homeostasis to protect against tumors and tissue damage. An overactive or prolonged immune response can lead to oxidative stress from increased production of reactive oxygen species. Heat stress induces oxidative stress and overwhelms the natural antioxidant defense mechanisms. This study\'s objectives were to investigate the protective properties of astaxanthin against heat-induced oxidative stress and apoptosis in the chicken thymus, by comparing the growth performance and gene signaling pathways among three groups: thermal neutral, heat stress, and heat stress with astaxanthin. The thermal neutral temperature was 21-22 °C, and the heat stress temperature was 32-35 °C. Both heat stress groups experienced reduced growth performance, while the astaxanthin-treated group showed a slightly lesser decline. The inflammatory response and antioxidant defense system were activated by the upregulation of the NF-kB, NFE2L2, PPARα, cytoprotective capacity, and apoptotic gene pathways during heat stress compared to the thermal neutral group. However, expression levels showed no significant differences between the thermal neutral and heat stress with antioxidant groups, suggesting that astaxanthin may mitigate inflammation and oxidative stress damage.
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  • 文章类型: Journal Article
    虾青素,酮-类胡萝卜素,已知具有有效的抗氧化性能。本研究旨在探讨虾青素对人中性粒细胞的抗炎作用及其机制。体外研究了虾青素对脂多糖(LPS)刺激的人中性粒细胞的影响。从健康志愿者中分离嗜中性粒细胞,并在存在和不存在虾青素的情况下用LPS刺激。我们评估了细胞因子的产生,通过丝裂原活化蛋白激酶(MAPKs)和核因子κB(NF-κB)激活信号通路,和凋亡。在不同浓度下评估虾青素的影响,并对预处理和共处理方案进行了测试。结果表明,虾青素显着降低了LPS刺激的中性粒细胞中促炎细胞因子TNF-α和IL-1β的产生。能有效抑制ERK1/2MAPK的磷酸化,不显著影响p38MAPK或NF-κB途径。此外,虾青素促进中性粒细胞凋亡,对抗LPS的细胞凋亡延缓作用。这些效果在预处理中更为明显。总之,虾青素通过减少细胞因子的产生和增强细胞凋亡,同时选择性调节细胞内信号通路,对中性粒细胞的炎症反应具有保护作用。虾青素显示出作为治疗严重炎症状态的治疗剂的显著潜力。
    Astaxanthin, a keto-carotenoid, is known to have potent antioxidant properties. This study aims to investigate the anti-inflammatory effect of astaxanthin and its mechanism in human neutrophils. The effects of astaxanthin on lipopolysaccharide (LPS)-stimulated human neutrophils were investigated in vitro. Neutrophils were isolated from healthy volunteers and stimulated with LPS in the presence and absence of astaxanthin. We assessed cytokine production, signaling pathway activation via mitogen-activated protein kinases (MAPKs) and nuclear factor kappa B (NF-κB), and apoptosis. Astaxanthin\'s impact was evaluated at different concentrations, and both pretreatment and cotreatment protocols were tested. The results demonstrated that astaxanthin significantly reduced the production of pro-inflammatory cytokines TNF-α and IL-1β in LPS-stimulated neutrophils. It effectively inhibited the phosphorylation of ERK1/2 MAPK, without notably affecting p38 MAPK or NF-κB pathways. Furthermore, astaxanthin promoted apoptosis in neutrophils, counteracting the apoptosis-delaying effects of LPS. These effects were more pronounced with pretreatment. In conclusion, astaxanthin has protective effects on inflammatory responses in neutrophils by reducing cytokine production and enhancing apoptosis while selectively modulating intracellular signaling pathways. Astaxanthin demonstrates significant potential as a therapeutic agent in the management of severe inflammatory conditions.
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  • 文章类型: Journal Article
    甲氨蝶呤(MTX),抗代谢剂,被广泛用于急性淋巴细胞白血病的治疗,尽管它与显著的器官功能障碍有关。虾青素(AST)是一种天然类胡萝卜素,最近已成为一种有前途的抗肿瘤和抗炎剂。在这项研究中,我们旨在评估虾青素和低剂量甲氨蝶呤联合治疗急性淋巴细胞白血病细胞系的有效性.二氢叶酸还原酶(DHFR)的表达,胸苷酸合成酶(TYMS),凋亡,使用qRT-PCR研究抗凋亡和炎症基因。进行流式细胞术用于细胞周期定量评估。克隆形成试验用于评估AST处理后的NALM6细胞增殖能力,MTX,和共同治疗。为了比较各组的抗氧化性能,进行了三价铁离子还原抗氧化能力测定。在MTX的存在下观察到生存力降低,AST,和他们的联合治疗。单独的AST和与MTX的组合均导致细胞周期停滞以及DHFR和TYMS表达的降低。而MTX,AST,它们的组合可以降低STAT3和BCL-XL基因的表达,它们可以作为BAX和CASP3,TNFα表达的正调节因子,IL6AST和MTX共处理抑制了集落形成能力。FRAP测定还显示AST和AST+MTX增加了抗氧化能力。我们的数据表明,AST可以提高MTX的治疗效果,其联合治疗可被认为是治疗急性淋巴细胞白血病的有希望的策略。
    Methotrexate (MTX), an antimetabolite agent, is widely used for acute lymphoblastic leukemia treatment, despite its association with significant organ dysfunction. Astaxanthin (AST) is a natural carotenoid which has recently been emerged as a promising anti-tumor and anti-inflammatory agent. In this study, we aimed to evaluate the effectiveness of astaxanthin and low-dose methotrexate co-treatment in acute lymphoblastic leukemia cell line. The expression of Dihydrofolate reductase (DHFR), Thymidylate synthase (TYMS), apoptotic, anti-apoptotic as well as inflammatory genes was investigated using qRT-PCR. Flow cytometry was performed for cell cycle quantitative evaluation. Clonogenic assay was used to assess NALM6 cells proliferation capacity following treatment with AST, MTX, and co-treatment. To compare the antioxidant property of each group, the ferric ion reducing anti-oxidant power assay was performed. A reduction in viability was observed in the presence of MTX, AST, and their combined treatment. Both AST alone and in combination with MTX caused cell cycle arrest and a reduction in the expression of DHFR and TYMS. While MTX, AST, and their combination could reduce STAT3 and BCL-XL gene expression, they could act as positive regulators for the expression of BAX and CASP3, TNFα, and IL6. AST and MTX co-treatment inhibited the colony formation ability. FRAP assay also revealed that AST and AST+MTX increased the antioxidant capacity. Our data suggests that AST can improve MTX treatment efficacy and their combination therapy can be considered as a promising strategy for the management of acute lymphoblastic leukemia.
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  • 文章类型: Journal Article
    背景:氧化应激(OS)在女性生殖和生育能力中起着有害的作用。一些研究探索了各种饮食干预和抗氧化剂补充剂,如虾青素(AST),减轻OS对女性生育能力的不利影响。在一些动物和临床研究中已经显示了AST对女性生育力和生殖器官氧化还原状态的改善作用。
    目的:目前对动物和临床研究的系统评价和荟萃分析的主要目的是全面概述目前关于AST对女性生育力和生殖结局的影响的证据。AST对氧化还原状态的影响,生殖器官炎症和凋亡标志物作为次要结局.
    方法:我们系统地搜索了电子数据库,包括PubMed,Scopus,和WebofScience,直到2024年1月1日,使用与AST相关的指定搜索词,女性生殖性能,和不孕症,考虑到在人类或动物模型中比较口服AST补充剂与安慰剂或对照的介入研究的文献中发现的不同同义词。
    方法:两名独立的评审员提取了有关研究特征的数据,结果,和偏见的风险。我们使用随机效应模型汇总了结果,并评估了异质性和证据质量。我们描述性地报告了动物模型的数据,因为meta分析是不可能的.
    方法:临床试验的荟萃分析表明,AST可显著提高卵泡液中卵母细胞成熟率(MD:8.40,95%CI:4.57~12.23,I2:0%)和总抗氧化能力水平(MD:0.04,95%CI:0.02~0.06,I2:0%)。其他ART和妊娠结局和氧化还原状态标志物没有显示出统计学上的显着变化。动物研究报道了AST对氧化还原状态的改善作用,炎症,凋亡,和卵巢组织形态学。
    结论:本系统综述显示,补充AST可以通过提高卵母细胞质量和降低生殖器官OS来改善辅助生殖技术的结果。然而,证据受到异质性的限制,偏见的风险,纳入研究的样本量较小。
    BACKGROUND: Oxidative stress (OS) plays a harmful role in female reproduction and fertility. Several studies explored various dietary interventions and antioxidant supplements, such as astaxanthin (AST), to mitigate the adverse effects of OS on female fertility. Ameliorative effects of AST on female fertility and the redox status of reproductive organs have been shown in several animal and clinical studies.
    OBJECTIVE: The main objective of present systematic review and meta-analysis of both animal and clinical studies was to provide a comprehensive overview of the current evidence on the effects of AST on female fertility and reproductive outcomes. The effect of AST on redox status, inflammatory and apoptotic markers in reproductive organs were included as the secondary outcomes.
    METHODS: We systematically searched electronic databases including PubMed, Scopus, and Web of Science, until January 1, 2024, using specified search terms related to AST, female reproductive performance, and infertility, considering the diverse synonyms found in the literature for interventional studies that compared oral AST supplementation with placebo or control in human or animal models.
    METHODS: Two independent reviewers extracted data on study characteristics, outcomes, and risk of bias. We pooled the results using random-effects models and assessed the heterogeneity and quality of evidence. We descriptively reported the data from animal models, as meta-analysis was not possible.
    METHODS: The meta-analysis of clinical trials showed that AST significantly increased the oocyte maturation rate (MD: 8.40, 95% CI: 4.57 to 12.23, I2: 0%) and the total antioxidant capacity levels in the follicular fluid (MD: 0.04, 95% CI: 0.02 to 0.06, I2: 0%). The other ART and pregnancy outcomes and redox status markers did not show statistically significant changes. The animal studies reported ameliorative effects of AST on redox status, inflammation, apoptosis, and ovarian tissue histomorphology.
    CONCLUSIONS: This systematic review shows that AST supplementation may improve assisted reproductive technology outcomes by enhancing oocyte quality and reducing OS in the reproductive organs. However, the evidence is limited by the heterogeneity, risk of bias, and small sample size of the included studies.
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  • 文章类型: Journal Article
    雨生红球藻中虾青素的生物合成是由能量驱动的。然而,鞭毛介导的能量消耗运动过程对虾青素积累的影响尚未得到很好的研究。在这项研究中,表征了虾青素和NADPH含量的概况,以及有或没有pH休克引起的鞭毛的光合参数。结果表明,细胞形态无明显改变,除了在pH休克治疗组中观察到的鞭毛损失。相比之下,鞭毛去除组中的虾青素含量为62.9%,在4、8和12h分别比对照高62.8%和91.1%,分别。同时,Y(II)增加和Y(NO)减少表明缺乏鞭毛运动过程的细胞可能会分配更多的能量用于虾青素的生物合成。NADPH分析证实了这一发现,这表明鞭毛去除细胞中的水平更高。这些结果为缺乏运动的细胞中的能量重新分配提供了对虾青素积累的潜在机制的初步见解。
    Astaxanthin biosynthesis in Haematococcus pluvialis is driven by energy. However, the effect of the flagella-mediated energy-consuming movement process on astaxanthin accumulation has not been well studied. In this study, the profiles of astaxanthin and NADPH contents in combination with the photosynthetic parameters with or without flagella enabled by pH shock were characterized. The results demonstrated that there was no significant alteration in cell morphology, with the exception of the loss of flagella observed in the pH shock treatment group. In contrast, the astaxanthin content in the flagella removal groups was 62.9%, 62.8% and 91.1% higher than that of the control at 4, 8 and 12 h, respectively. Simultaneously, the increased Y(II) and decreased Y(NO) suggest that cells lacking the flagellar movement process may allocate more energy towards astaxanthin biosynthesis. This finding was verified by NADPH analysis, which revealed higher levels in flagella removal cells. These results provide preliminary insights into the underlying mechanism of astaxanthin accumulation enabled by energy reassignment in movement-lacking cells.
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  • 文章类型: Journal Article
    背景:心力衰竭是一种慢性和进行性疾病,其中心肌无法泵送足够的血液和氧气来满足身体的需要。氧化应激和炎症是心力衰竭发展和进展的关键因素。虾青素,类胡萝卜素,具有很强的抗炎和抗氧化作用,可以保护心血管系统。一项研究将评估虾青素补充剂对炎症状态的影响,氧化应激,血脂谱,尿酸水平,内皮功能,生活质量,和心力衰竭患者的疾病症状。
    方法:本研究是一项为期8周的双盲对照随机临床试验,其中心力衰竭患者被随机分为两组:干预(每天1粒含有20毫克虾青素的胶囊,n=40)和安慰剂(每天含20毫克麦芽糖糊精的胶囊,n=40)将被分割。在干预的开始和结束时,尿酸,血脂谱,氧化应激指数,炎症标志物,血压,一氧化氮,人体测量因素将被测量,和测量生活质量的问卷,疲劳强度,呼吸急促,食欲就完成了.采用SPSS22版软件进行统计分析。
    结论:全球对天然和功能性食品越来越感兴趣。这项RCT有助于扩大对虾青素在心力衰竭患者中的潜在益处的研究,包括它的抗氧化剂,降脂,和抗炎作用。
    背景:伊朗临床试验注册IRCT20200429047235N3。2024年3月26日注册。
    BACKGROUND: Heart failure is a chronic and progressive disease where the heart muscle is unable to pump enough blood and oxygen to meet the body\'s needs. Oxidative stress and inflammation are key elements in the development and progression of heart failure. Astaxanthin, a carotenoid, has strong anti-inflammatory and antioxidant effects that may protect the cardiovascular system. A study will evaluate the effect of astaxanthin supplementation on inflammatory status, oxidative stress, lipid profile, uric acid levels, endothelial function, quality of life, and disease symptoms in people with heart failure.
    METHODS: The current study is a double-blind controlled randomized clinical trial for 8 weeks, in which people with heart failure were randomly assigned to two groups: intervention (one capsule containing 20 mg of astaxanthin per day, n = 40) and placebo (one capsule containing 20 mg of maltodextrin per day, n = 40) will be divided. At the beginning and end of the intervention, uric acid, lipid profile, oxidative stress indices, inflammatory markers, blood pressure, nitric oxide, and anthropometric factors will be measured, and questionnaires measuring quality of life, fatigue intensity, shortness of breath, and appetite will be completed. SPSS version 22 software will be used for statistical analysis.
    CONCLUSIONS: There is a growing global interest in natural and functional food products. This RCT contributes to the expanding body of research on the potential benefits of astaxanthin in heart failure patients, including its antioxidant, lipid-lowering, and anti-inflammatory effects.
    BACKGROUND: Iranian Registry of Clinical Trials IRCT20200429047235N3. Registered on 26 March 2024.
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