基于生物场能量处理的测试配方对重要器官健康特异性生物标志物的影响

Ariadne Esmene Afaganis, M. Trivedi, A. Branton, Dahryn Trivedi, G. Nayak, M. Gangwar, S. Jana
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引用次数: 0

摘要

多器官功能障碍综合征或功能衰竭是反对医疗服务的主要问题之一,以维持正常的功能。本研究旨在探索生物场能量处理测试配方对骨骼、心脏、肝脏、肺和大脑等重要器官功能的影响,使用标准活性参数进行特定细胞检测。测试配方和细胞培养基分为两部分,一部分未经处理(UT),另一部分由加拿大著名的生物场能量治疗师Ariadne Esmene Afaganis远程进行生物场能量治疗,并标记为生物场治疗(BT)测试配方/培养基。对试验配方进行了细胞活力测试,数据表明试验配方对所有细胞系都是安全无毒的。各组细胞保护活性显示,未处理培养基(UT-Med) +生物场处理试验项目(BT-TI)组对人心脏成纤维细胞(HCF)细胞的保护活性在1µg/mL时显著提高94.4%,而在10µg/mL时,BT-Med + BT-TI组对人肝癌细胞(HepG2)的保护活性显著提高84.4%。1µg/mL UT-Med + BT-TI组对腺癌人肺泡基底上皮细胞(A549)的细胞保护作用较未处理组提高124%。在10µg/mL时,UT-Med + BT-TI组MG-63细胞ALP活性显著增加85.9%,而在石川细胞中,BT-Med + BT-TI组ALP活性在0.1µg/mL时,与未处理组相比,ALP活性最大增加59.2%。在1和10µg/mL浓度下,UT-Med + BT-TI组HCF(心脏)细胞的百分比保护(LDH活性降低)分别显著提高了53%和40.5%,而BT-Med + UT-TI组在0.1、1和10µg/mL浓度下的保护分别提高了68.5%、70.7%和16.8%,在0.1、1和10µg/mL浓度下,BT-Med + BT-TI组细胞保护分别提高了86.5%、62.5%和34.2%。在10µg/mL浓度下,UT-Med + BT-TI、BT-Med + UT-TI和BT-Med + BT-TI组对HepG2(肝)细胞的保护率(ALT活性降低)分别比未处理组高33.5%、63.2%和99.2%。与未处理组相比,UT-Med + BT-TI、BT-Med + UT-TI和BT-Med + BT-TI组A549(肺)细胞的细胞保护作用(SOD活性增加)百分比分别增加39.8%(10µg/mL)、44%(25.5µg/mL)和59.7%(25.5µg/mL)。与未治疗的人神经母细胞瘤细胞(SH-SY5Y)相比,UT-Med + BT-TI、BT-Med + UT-TI和BT-Med + BT-TI组血清素水平分别显著提高59.2%(0.1µg/mL)、190.3%(0.1µg/mL)和201%(1µg/mL)。然而,与MG-63细胞相比,UT-Med + BT-TI、BT-Med + UT-TI和BT-Med + BT-TI组维生素D受体(VDR)的相对定量(RQ)分别显著提高了159.1%(50µg/mL)、212.7%(1µg/mL)和278.3%(10µg/mL)。因此,目前的数据得出结论,在使用Biofield Energy处理的测试配方(the Trivedi Effect®)治疗后,在特定细胞系中使用各种标准生物标志物的整体多器官健康状况在骨骼、心脏、肝脏、肺和大脑的健康方面得到了显著改善。因此,它可以作为一种补充和替代治疗许多多器官疾病的方法,如冠状动脉疾病、心律失常、先天性心脏病、心肌病、肝硬化、肝癌、血色素沉着症、哮喘、慢性支气管炎、囊性纤维化、骨质疏松症等。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Impact of Biofield Energy Treatment Based Test Formulation on Vital Organ Health Specific Biomarkers Using Cell Line Study
Multiple organ dysfunction syndrome or failure is one of the major concerns against healthcare services in order to maintain the normal function. The present study aimed to explore the impact of the Biofield Energy Treated test formulation on the function of vital organs such as bones, heart, liver, lungs, and brain using standard activity parameters in specific cell-based assays. The test formulation and cells medium was divided into two parts, one untreated (UT) and other part received the Biofield Energy Treatment remotely by a renowned Biofield Energy Healer, Ariadne Esmene Afaganis, Canada and was labeled as the Biofield Treated (BT) test formulation/media. The test formulation was tested for cell viability, and the data suggested that the test formulation was found safe and non-toxic against all the cell lines. Cytoprotective activity among the experimental groups showed a significant improved activity by 94.4% at 1 µg/mL in untreated medium (UT-Med) + Biofield Treated Test Item (BT-TI) group in human cardiac fibroblasts cells (HCF) cells, while 84.4% at 10 µg/mL in BT-Med + BT-TI groups in human hepatoma cells (HepG2), and 124% increased cytoprotective action at 1 µg/mL in UT-Med + BT-TI group in adenocarcinomic human alveolar basal epithelial cells (A549) cells as compared with the untreated test group. ALP activity in MG-63 cells was significantly increased by 85.9% at 10 µg/mL in the UT-Med + BT-TI group, while in Ishikawa cells showed maximum increased ALP activity by 59.2% at 0.1 µg/mL in BT-Med + BT-TI groups as compared to the untreated group. The percent protection of HCF (heart) cells (decreased of LDH activity) was significantly increased by 53% and 40.5% at 1 and 10 µg/mL concentrations respectively, in UT-Med + BT-TI group, while BT-Med + UT-TI group showed increased protection by 68.5%, 70.7%, and 16.8% at 0.1, 1, and 10 µg/mL respectively, and 86.5%, 62.5%, and 34.2% improved cellular protection at 0.1, 1, and 10 µg/mL respectively, in BT-Med + BT-TI group as compared to the untreated test group. The percent protection of HepG2 (liver) cells (decreased of ALT activity) was reported by 33.5%, 63.2%, and 99.2% at 10 µg/mL in the UT-Med + BT-TI, BT-Med + UT-TI, and BT-Med + BT-TI groups, respectively compared to the untreated group. Cellular protection of A549 (lungs) cells (increased of SOD activity) in terms of percentage was increased by increased by 39.8% (at 10 µg/mL), 44% (at 25.5 µg/mL), and 59.7% (at 25.5 µg/mL) in the UT-Med + BT-TI, BT-Med + UT-TI, and BT-Med + BT-TI groups, respectively compared to untreated group. Serotonin level was significantly increased by 59.2% (at 0.1 µg/mL), 190.3% (at 0.1 µg/mL), and 201% (at 1 µg/mL) in the UT-Med + BT-TI, BT-Med + UT-TI, and BT-Med + BT-TI groups, respectively compared to untreated in human neuroblastoma cells (SH-SY5Y). However, the relative quantification (RQ) of vitamin D receptor (VDR) was significantly increased by 159.1% (at 50 µg/mL), 212.7% (at 1 µg/mL), and 278.3% (at 10 µg/mL) in the UT-Med + BT-TI, BT-Med + UT-TI, and BT-Med + BT-TI groups, respectively as compared to the untreated in MG-63 cells. Thus, the present data concluded that the overall multiple organ health using various standard biomarkers in specific cell lines were significantly improved with respect to health of bones, heart, liver, lungs, and brain after treatment with the Biofield Energy treated test formulation (The Trivedi Effect®). Thus, it can be used as a complementary and alternative therapy approach against many multiple organ disorders such as coronary artery disease, arrhythmias, congenital heart disease, cardiomyopathy, cirrhosis, liver cancer, hemochromatosis, asthma, chronic bronchitis, cystic fibrosis, osteoporosis, etc.
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