发酵木瓜制剂(FPP)调节聚集性神经退行性疾病危险因素中年受试者关键标志物的2年双盲RCT随访研究

Clinical Pharmacology & Biopharmaceutics Pub Date : 2017-01-01 Epub Date: 2017-05-18 DOI:10.4172/2167-065X.1000170
Francesco Marotta, Massimiliano Marcellino, Umberto Solimene, Biagio Cuffari, Hariom Yadav, Alexander N Khokhlov, Aldo Lorenzetti, Amelie Mantello, Joseph Cervi, Roberto Catanzaro
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引用次数: 3

摘要

近年来,许多研究报道了代谢综合征与神经退行性疾病之间的重要关系。越来越多的证据表明,遗传和环境风险因素(从饮食到生活方式到污染物)与固有的年龄相关的氧化性炎症变化的相互作用可能被提倡来解释神经退行性疾病的流行。近年来,在实验和临床研究中,一种特殊的发酵木瓜制剂(FPP)已被证明对多种慢性疾病和衰老机制中的许多氧化还原信号异常有显著影响。本研究的目的是评估FPP在伴有潜在神经退行性疾病聚集性危险因素的代谢性疾病患者中的应用。研究人群包括90名年龄在45-65岁之间的患者,他们患有即将发生的代谢综合征,之前被选为ApoE4基因型阴性。采用随机对照试验、双盲方法,一组服用FPP 4.5 g,每天2次(这是之前临床研究中最常用的剂量),另一组服用口服抗氧化鸡尾酒(反式白藜芦醇、硒、维生素E、维生素C)。治疗21个月后,在最后3个月的研究治疗中,选择添加一种重金属螯合剂,剂量为3g /每天。检测参数为:常规氧化LDL-胆固醇、抗氧化LDL、亲环蛋白a (CyPA)、纤溶酶原激活物抑制剂-1、CyPA基因表达。从这项研究中可以看出,与对照抗氧化剂不同,FPP显著降低了氧化ldl,并使抗Ox-LDL/Ox-LDL比率接近正常化(见sè)。此外,只有FPP降低了血浆亲环蛋白a水平和纤溶酶原激活物抑制剂(p
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A 2-year Double-Blind RCT Follow-up Study with Fermented Papaya Preparation (FPP) Modulating Key Markers in Middle-Age Subjects with Clustered Neurodegenerative Disease-Risk Factors.

In recent years a number of studies have reported the significant relationship between metabolic syndrome and neurodegenerative disease. There is accumulating evidence that the interplay of combined genetic and environmental risk factors (from diet to life style to pollutants) to intrinsic age-related oxi-inflammatory changes may be advocated for to explain the pandemic of neurodegenerative diseases. In recent years a specific Fermented Papaya Preparation (FPP) has been shown to significantly affect a number of redox signalling abnormalities in a variety of chronic diseases and as well in aging mechanisms either on experimental and on clinical ground. The aim of the present study was to evaluate FPP use in impending metabolic disease patients with potentially neurodegenerative disease clustered risk factors. The study population consisted of 90 patients aged 45-65 years old, with impending metabolic syndrome and previously selected as to be ApoE4 genotype negative. By applying a RCT, double-blind method, one group received FPP 4.5 g twice a day (the most common dosage utilized in prior clinical studies) while the other received an oral antioxidant cocktail (trans-resveratrol, selenium, vitamin E, vitamin C). Then, after 21 month treatment period, a selected heavy metal chelator was added at the dosage of 3 g/nocte for the final 3 months study treatment. The parameters tested were: routine tests oxidized LDL-cholesterol, anti-oxidised LDL, Cyclophilin-A (CyPA), plasminogen activator inhibitor-1 and CyPA gene expression. From this study it would appear that FPP, unlike the control antioxidant, significantly decreased oxidized-LDL and near normalizing the anti-Ox-LDL/Ox-LDL ratio (p<0.001) although unaffecting the lipid profile per sè. Moreover, only FPP decreased cyclophilin-A plasma level and plasminogen activator-inhibitor (p<0.01) together with downregulating cyclophilin-A gene expression (p<0.01). Insulin resistance was only mildly improved. Heavy metals gut clearance proved to be effectively enhanced by the chelator (p<0.01) and this was not affected by any of the nutraceuticals, nor it added any further benefit to the biological action of FPP.

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