The objective of the current experiment was to evaluate the effect of biofield energy treatment on the isotopic abundance ratio of PM+1/PM (2H/1H or 13C/12C or 15N/14N) in indole using the gas chromatography-mass spectrometry (GC-MS). The sample of organic compound indole was divided into two parts - one part was designated as a control sample (untreated), and another part was considered as biofield energy treated sample, which was subjected to Mr. Trivedi’s biofield energy treatment (The Trivedi Effect®). The biofield energy treated indole sample was analyzed at different time intervals and were symbolized as T1, T2, T3, and T4 to understand the effect of the biofield energy on isotopic abundance ratio with respect to the time. From the GC-MS spectra, the presence of the molecular ion peak C8H7N+ (m/z 117) along with major fragmented peaks C7H6+ (m/z 90), C7H5+ (m/z 89), C5H3+ (m/z 63), C4H2+ (m/z 50), C3H3+ (m/z 39), and C2H4 (m/z 28) were observed in both control and biofield treated samples. Only, the relative peak intensities of the fragmented ions in the biofield treated indole was notably changed as compared to the control sample with respect to the time. The isotopic abundance ratio analysis of indole using GC-MS revealed that the isotopic abundance ratio of PM+1/PM in the biofield energy treated indole at T1 and T2 was significantly decreased by 44.28 and 28.18% as compared to the control sample. On the contrary, the isotopic abundance ratio of PM+1/PM in the biofield energy treated sample at T3 and T4, was significantly increased by 41.22 and 180.88%, respectively as compared to the control sample. Overall, the isotopic abundance ratio of PM+1/PM (2H/1H or 13C/12C or 15N/14N) was significantly altered in the biofield energy treated indole as compared to the control with respect to the time. The biofield treated indole with the altered isotopic abundance ratio might have altered the physicochemical properties and rate of reaction. This biofield energy treated indole might be more useful as a chemical intermediate in the production of pharmaceuticals, chemicals, plastics, dyes, and perfumes.
Comments: 8 Pages.
[v1] 2016-09-01 00:52:55
Unique-IP document downloads: 20 times
Vixra.org is a pre-print repository rather than a journal. Articles hosted may not yet have been verified by peer-review and should be treated as preliminary. In particular, anything that appears to include financial or legal advice or proposed medical treatments should be treated with due caution. Vixra.org will not be responsible for any consequences of actions that result from any form of use of any documents on this website.
Add your own feedback and questions here:
You are equally welcome to be positive or negative about any paper but please be polite. If you are being critical you must mention at least one specific error, otherwise your comment will be deleted as unhelpful.