Introduction:
This article presents a theoretical analysis of the safe form and dosage of the
amygdalin derivative. By making a precise socio-anthropological analysis of the life of the ancient people of
Botra (Hunza people, Burusho/Brusho people), a hypothesis has been postulated through a number of modern
quantum-mechanical, molecular-topological and bio analytical checks, and has also been confirmed by two
proofs.
Methods:
The proposed hypothesis underwent theoretical and logical analysis to confirm and/or reject it. The
methodological scheme was: determining the optimal chemical formula, determination of the pharmaceutical
molecular form and determination of the drug dose.
Results:
A convenient, harmless, form of amygdalin derivative is available that has the same biological and
chemical activity and could be used in conservative clinical oncology. The article also presents a theoretical
comparative analysis of biochemical reactivity in in vivo and in vitro media, by which we also determine the
recommended dosage for patient administration. A comparative analysis of the data, obtained in published clinical
studies of amygdalin, is presented, summarizing a scheme of the anti-tumor activity of the proposed molecular
form.
Conclusion:
The hydrolyzed to amide / carboxylic acid cyano / nitrile glycosides are potential drugs. Their
biological activity remains unchanged, but their toxicity is many times lower than unmodified native molecules.
We claim that this study we have conducted on amygdalin / dhurrin-derived amide is the only study on this
molecular form. Other substances in these groups with pronounced biological activity (including anti-tumor) are
the hydrolyzed nitrile groups by Prunasin, Lucumin, Vicianin, Sambunigrin, Dhurrin, Taxiphyllin, Zierin,
Preteacin, p-Glucosyloxymandelonitrile, Linamarin, Lotaustralin, Acaciapetalin, Triglochinin, Dejdaclin, Tetraphyllin
A, Tetrallin B, Gynocardin etc., to their amide/carboxylic acid.
5,6-Dihydroxyindole-2-carboxylic acid is incorporated in mammalian melanin
