作为一种无铁多营养复合物的功能,诱导奖赏缺乏中的稳态生物学参数:促进血红蛋白化、有氧代谢、病毒免疫能力和神经炎症调节。

Kenneth Blum, Bernard W Downs, Manashi Bagchi, Steve Kushner, Bruce S Morrison, Jeffrey Galvin, Kourtney Randsdorp, Justin Randsdorp, Rajendra D Badgaiyan, Eric R Braverman, Debasis Bagchi
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引用次数: 3

摘要

背景:世界范围内一种常见的神经疾病是奖赏缺乏综合征(RDS),它会导致物质和非物质成瘾行为,必须通过整合中枢神经系统和外周神经系统的生物学方法来对抗。血红蛋白的完整性是决定整体健康功能的关键因素。营养补充疗法应该是恢复血液健康特性的基本策略。我们的实验室设计了一种独特的无铁VMP35配方,用于使用专有的Prodosome®吸收技术恢复贫血细胞中的铁依赖性血红蛋白。该配方含有一系列富含生物类黄酮的纳米乳化植物成分,增强结缔组织的结构完整性,增强免疫能力、细胞有氧代谢,并增强对炎症事件的有效调节。我们讨论了强大与脆弱免疫的复杂方面以及相应的炎症反应,以更深入地理解免疫行为和事件的各种和过于复杂的后遗症。VMP35的作用是通过高度可吸收的营养/营养基因组补充介导的,从而改善系统的功能行为。事实上,不含铁的VMP35促进了“系统生物学方法”,该方法可以恢复血红蛋白状态,逆转无氧缺氧,提高免疫反应能力,并调节全身和神经炎症后遗症的适当和可控激活。在这些致病情况下,缺铁性贫血被误解了,并提出了一个新的疾病学术语,慢性贫血综合征。还详细解释了还原论与系统生物学方法的比较治疗原理。方法:详细介绍了新型治疗性无铁VMP35液体营养品在将铁依赖性血红蛋白恢复为红细胞、增强细胞形态、活力和免疫能力方面的疗效,从而减少延长炎症后遗症的需要。结果:这一点在IRB先前批准的多受试者人体研究中得到了证实。此外,最近的两项案例研究报告了VMP35营养补充疗法对经历过近乎致命事件的受试者的显著恢复益处,这证实了本文中解释的发现。结论:这种新型的无铁VMP35调节一系列稳态生物学参数,如增强血红蛋白分泌、有氧代谢、病毒免疫能力和炎症调节。进一步的研究,检验运动成绩的机制和有益影响,正在进行中。重要的是,在这些困难的免疫挑战时期,调节一系列稳态免疫和炎症功能障碍等同于改善人群结果。试验注册:在纽约Path基金会的机构审查委员会(IRB)的指导下,对总共38名受试者进行了临床调查(2013年4月25日第13-009号)。这两项病例研究分别在宾夕法尼亚州兰开斯特的兰开斯特综合医院和美国宾夕法尼亚州费城的杰斐逊大学医院进行。这两项研究都是回顾性登记的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Induction of homeostatic biological parameters in reward deficiency as a function of an iron-free multi-nutrient complex: Promoting hemoglobinization, aerobic metabolism, viral immuno-competence, and neuroinflammatory regulation.

Induction of homeostatic biological parameters in reward deficiency as a function of an iron-free multi-nutrient complex: Promoting hemoglobinization, aerobic metabolism, viral immuno-competence, and neuroinflammatory regulation.

Induction of homeostatic biological parameters in reward deficiency as a function of an iron-free multi-nutrient complex: Promoting hemoglobinization, aerobic metabolism, viral immuno-competence, and neuroinflammatory regulation.

Induction of homeostatic biological parameters in reward deficiency as a function of an iron-free multi-nutrient complex: Promoting hemoglobinization, aerobic metabolism, viral immuno-competence, and neuroinflammatory regulation.

Background: A common neurological condition worldwide is Reward Deficiency Syndrome (RDS) leading to both substance and non-substance addictive behaviors, that must be combatted by integrating both central nervous system and peripheral nervous system biological approaches. Integrity of hemoglobin is a crucial determining factor for the overall health functions. Nutrient repletion therapy should be a fundamental strategy to restore the healthy properties of blood. A unique patent-pending iron-free VMP35 formulation was engineered by our laboratory to restore iron-dependent hemoglobin in anemic cells using a proprietary Prodosome® absorption technology. This formulation, containing an array of nano-emulsified botanical ingredients rich in bioflavonoids, strengthens the structural integrity of connective tissues, and potentiates immune competence, cellular aerobic metabolism, and enhances efficient regulation of inflammatory events. We discuss the intricate aspects of strong vs. fragile immunity and consequential inflammatory responses to convey a deeper understanding of the varied and overly complex sequela of immunological behaviors and events. The effect of the VMP35 is mediated through highly absorbable nutritional/nutrigenomic repletion enabling improvements in the systemic set of functional behaviors. In fact, the iron-free VMP35 facilitates a "Systems Biology Approach" which restores hemoglobin status, reverses anaerobic hypoxia, improves competent immune responsivity, and regulates appropriate and controlled activation of general and neuro-inflammatory sequela. Under these pathogenic circumstances, iron-deficiency anemia has been misconceptualized, and a new nosological term, Chronic Anemia Syndrome, is proposed. The comparative therapeutic rationale of Reductionist vs. Systems Biology approaches is also explained in detail.

Methods: The efficacy of the novel therapeutic iron-free VMP35 liquid nutraceutical is detailed in restoring iron-dependent hemoglobin to RBCs and boosting cellular morphology, viability, and immune competence, thereby reducing the need for prolonging inflammatory sequela.

Results: This was demonstrated in a previous IRB approved multi-subject human study. In addition, two recent case studies report dramatic restorative benefits of nutrient repletion therapy of the VMP35 on subjects having experienced near-fatal events, which confirmed the findings explained in this manuscript.

Conclusions: This novel iron-free VMP35 modulates an array of homeostatic biological parameters such as enhanced hemoglobinization, aerobic metabolism, viral immuno-competence, and inflammatory regulation. Further research, examining mechanistic and beneficial effects in athletic performance, is in progress. Importantly, during these troubled immune challenging times, modulating an array of homeostatic immunological and inflammatory dysfunctions are tantamount to improved population outcomes.

Trial registration: The Clinical investigation in a total of 38 subjects was conducted under an Institutional Review Board (IRB) from the Path Foundation in New York, NY (#13-009 April 25, 2013). The two case studies were done at Lancaster General Hospital, Lancaster, PA, and Jefferson University Hospital, Philadelphia, PA, USA. Both studies were retrospectively registered.

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