How N,N-Dimethyltryptamine Works?: DMTs Biophysiological Hydrogen Bond with H2O Supporting Multicellular Life & Hyper Generalised Cellular Divergence, Intracellularly, Extracellularly & Transcytosis.

Originally published "Where did I Cum From? My First Fuck? Or was it Love at 1st Sight?... Whenever DMT & H2O Hooked-Up Marks Our Evolutionary Origin of Life!... Now What Kinda Cunts Would Tear Such a Devine Union Apart!?" which organically evolved to climax identifying the union between DMT and H2O as our earliest ancestors, and they’re actions supporting multicellular organisms. Therefore, this introduction has been added to acknowledge that and state its original intention was discussing available results of Universal Asylums Metabolic Implications of"Psychedelics / Forbidden Fruit" upon DRUG Saturation - Planning Document and considerations for clinical analysis of the stored blood serum samples which remains relevant for tracing evolution back to our earliest ancestral origin.

Since undertaking this experiment numerous extremely relevant scientific publications have been released in the area of opioids and immune systems. Although these include numerous fairly typical misconceptions due oppressive governance retarding scientific evolution skewing it’s perspectives by denying access to the most significant information. As interconnected commitments have lead to the identification of consistent overlaps of clear significance yet great complexity at this stage I will not be attempting to undertake thorough critique. Rather my intention is to start out by refining aspect of my original hypothesis whilst identifying some of the clearest parallels between scientific data and their relevance to this research design whilst identifying certain misconceptions. Although what I have identified as of greatest significance has potential for countless assays designs anticipated to evolve with my understanding as interconnected sets of research merge.

Maintaining it’s original form for historical purposes N,N-Dimethyltryptamine (DMT) & Other "Forbidden Fruit" - Central Nervous System Specific Nutrients. whilst the available results of experiments supports the hypothesis of DMT being an exogenous “Nutrient” or “Primary Metabolite” via the Central Nervous System (CNS) the term “specific” never was quite true to the hypothesis unless of course DMT is converted to something else prior to distribution. However, it would seem more likely that a little bit goes a long a way. According to Mishra, P (2022) Metabolism refers to a set of life-sustaining chemical reactions, including the uptake of nutrients, the subsequent conversion of nutrients into energy or building blocks for organism growth, and finally the clearance of redundant or toxic substances.

The available results of this experimental research provide evidence of Ayahausca, Psilocybin and Mescaline supporting Generalised Cellular Divergence of such Harmonious Efficiency that it was almost impossible to precipitate the slightest sign of Opioid withdrawal with the administration of Naloxone. Refining my original Hypothesis that DMT is a critical form of nutrition within its own class of “Primary Metabolites” I’m uncomfortable with my previously suggested prefix ‘Alpha’ due to it implying the top of a hierarchy or a constant requirement. Although certainly up there in significance I see commonalities between DMT and water which Popkin, BM, et al. (2010) confirms is also a critical nutrient 75/55% Baby to Elderly ratio and is essential for cellular homeostasis. Therefore, for DMT to support Generalised Cellular Divergence, Intracellularly, Extracellularly and Transcytosis of such Harmonious Efficiency as to prevent Naloxone precipitated Opioid withdrawal water is likely facilitates conductivity action(s) between DMT and Cells within such systems. Another recent unintended breakthrough lead to the identification of extremely relevant parallels of this research design and its potential value regarding viruses.

For the sake of an introductory spectrum it seems necessary to refer to this as a state of Hyper Cellular Divergence in contrast to Hypo Cellular Divergence extreme. The majority of human population have endured states of Hypo Cellular Divergence which emerged a significant time into and rapidly increased with the pace of the Neolithic Revolution (Pahwa R, 2023). According to Klani AK (2022) micronutirient deficiencies are the most prevelent type nutritional deficiencies in one or more nutrients that are essential for optimal health which can otherwise lead to disease and developmental failure. One of several consistently overlooked factors in such delay may have been due to the plausible and highly probable possibility of agriculture originally being inspired by demand for plants containing such nutrients. Which eventially evolved to such substances becoming forbidden then, and remaining forbidden now due to shit cunts.

Inflammation is frequently attributed to a range of variables from psychological stress across physiological ailments including viral infections and is to some extent considered a contributing factor associated with most forms of disease and illness. According to Rouse & Sehrawat (2010) "A balanced combination of pro-inflammatory and anti-inflammatory mechanisms would facilitate viral clearance and immunity to reinfection, with minimal damage to host tissues." DMT & similar substances are scientifically recognised to facilitate regulation of inflamitory systems & cellular proliferation (Szabo, et al 2014, Szabo, 2016 & Rudin et al 2023). Whilst at it's peak this could be considered hyper cellular divergence. However, once the backlog of maintenance is done it possible that "healthy" could become a more apropriate prefix on the uppoerend of the scale of cellular divergence.

Under conditions supportive of Healthy Cellular Divergence there is enough evidence to indicate symbiotic coevolutionary relationships between DNA and RNA of multicultural lifeforms such as humans and both DNA and RNA viruses, interconnected to complex metabolic processes collectively contributing to healthy epigenetic coevolutionary crosstalk on genetic and chromosomal levels. This is not to s that all viruses are good or bad as such symbiotic relationships are likely to include all kinds of intimate coevolutionary relationships across species. Kyriakou E, et al., (2023) recognises the interplay between endogenous and exogenous viruses with 8% of the human genome is occupied by ancient retroviral DNA. Coffin JM, (1997) describe the complexitities of multidirectional reverse transcript action between DNA in humans, birds and reptiles.

This becomes extrememly important considering 1000’s of years of intergenerational Hypo Cellular Divergence is likely to have drastically distorted Phenotypic Divergence in all kinds of critically serious manner. This includes retardation of immune functions within humans whilst hosts which is a double edge sword creating dysregulation of gene expression and rapid evolution of RNA viruses. Whilst this creates physiological vulnerability in Humans, it is rarely considered this also makes us more dangerous in terms of being primary culprits of cross species infection giving animals more viruses than they do us (Tan, C.C.S.,Et al,. 2024) despite scientific evidence indicating we have already contributed to the extinction of countless healthy species (Cowie RH, Et Al 2023).

However, this gets complicated due to Humans also forcing various animals into states of Hypo Cellular Divergence weather via domestication or ecological destruction (Marie V, et al 2023). In this sense restricting scientific research in this area knowing these potential benefits and risk to profit from spreading disease (Rathish B, 2024) be seen as the bioweaponisation of humans and others animals therefore making making Governments, the United Nations and World Health Organisation Terrorist Organisations by their own definitions.

Although I have refine the wording of the above which was published yesterday my ego was shattered tonight to stumble upon scientific publications as recent as this month directly related to DMT and gene expression such as by Nogueira, et al. (2024) which I’m am only so far able to access more than the abstract and sounds as if theres evidence but are unclear. I’d figured out most the above on my own via experience leading to increasingly advanced experiments which purely came by chance, experience and necessity.

These quotes from Szabo A (2012) “DMT has been found to activate the sigma-1 receptor (Sig-1R), an intracellular chaperone fulfilling an interface role between the endoplasmic reticulum (ER) and mitochondria”… and…"Based on these complex intracellular actions the Sig-1R has been conceptualized as a “pluripotent modulator” in living systems, as a controller of cell survival and differentiation” do a very good covering various aspects of what I’m trying to find the right language to accurately articulate. However, describing the intricacies of something with a primary role facilitating dynamic coevolution of so many varying components is difficult. I tripped out to learn that scientific fields such as virology and immunology were seperate, if I recall right and that is true the only reason I can think of is because someone wants to sell vaccines. Along these lines I cannot understand why Szabo hasn’t come to similar conclusions regarding DMT being a powerful form of energy. I’m also surprised he hasn’t challenged the unproven claim that of DMT(+) being alegedly “endogenous” too.

Until now I have mainly spoken to therapeutic actions in more general terms with occasional reference to receptor groups in previous publications due to a combination of speaking to a broader audience and investing time into understanding as much as possible about whatever happens to be of greatest priority at any give time. However, I have developed enough familiarity and understanding over countless hours studying the scientific literature cited throughout previous work to identify parallels of great significance in the interconnection between different sets of research. Plus I probably should have been working on this for the past couple of years basically took a year off life. Anyways in regards to this freezer full of blood serum...

My first encounter with or T cells specifically CD4+T helper cells Th1 and Th17 relation to DMT’s actions was via Szabo (2015) providing the first scientific evidence supported my conclusions from years of experience. Followed by Szabo, et al (2014) throwing Dendritic Cells into the mix riddled with technical terms between clear english such as “DMT emerges as a potent and promising candidate in novel therapies of peripheral and CNS autoimmune diseases (such as multiple sclerosis or amyotrophic lateral sclerosis) and cancer.” to warrant almost breaking my brain going over with a fine tooth comb motivated by pure insanity aka “love”. Before eventually stumbling upon Szabo (2016) which isn’t really any less technical but more condensed including similar therapeutic action like regulation of inflammation, cellular proliferation, anti viral and anti tumour. Oh, and of course ‘immunomodulation’ (Pahwa R, et al,. 2023) .

Recently another love story of great significance lead to scientific publications regarding CD4+T helper cells Th1 and Th17 and Dendritic cells which according to Liang (2016) are the most potent antigen-presenting cells and play a critical role in the innate and adaptive immune system. Whilst most articles describe opioids as immune-modulators despite some paying more attention to their dis-regulations which may have pros and cons under different conditions (Mikati 3023 & Sacerdote 2013) In human bone marrow, δopioid receptor mRNA express at a low level in immature dendritic cells, conversely, at a high level in mature dendritic cells which is an area of congestion which is particularly painful in a “regular” state. Whilst reoccurring patterns in congestion, mutation and dysfunction are likely to occur at any given point of intracellularly, extracellularly and transcytosis under similar hypo congested conditions. Tracing what complex processes are going on in there on a nanoscale during hyper cellular divergence it is tricky. un, ,Et al., (2023).

Cano & Lopera (2013) reckon "Antigen recognition by TCR induces the formation of several “TCR microclusters” that accompany the reorganization and approach of other membrane molecules and signaling proteins towards the contact zone with the DC. This contact zone between the T Cell and DC membranes is known as an immunological synapse and consists of a highly organized and dynamic molecular complex divided into three concentric zones known as the central, peripheral, and distal supramolecular activation clusters. The central region is composed of the TCR complex, co-stimulatory and co-inhibitory molecules, and co-receptors. These co-receptors are known as primary and secondary activation signals". The complex biophysiological composition of DMT and similar substances is the only form of nutrition capable of activating the full spectrum of such supramolecular activation clusters.

Basically all current science is biased by studies on systems in states of hypo cellular divergence considered as the normal standard. This has both pros and cons as whilst creates challenges based on skewed science shuch consistently heavily skewed results are of great advantage in understanding sickness and desease which have many crossover patterns. This reseach design has enormouse potential value in terms of the range of acute reapeatable symptoms. I also expect DMT supported hyper cellular divergence increases ones natural tolerance to exdogeous opiods whilst reducing the need for them which also offers a repeatable objective experimental treatment models. .

As for the extreme end of Hyper Cellular Divergence I’ve found once clear the more frequently consumed the less you need them and the less noticeable the effects. Although, depending what your system is fighting will vary the nature of any potential psychological experience along with physical purging in different forms. I have previously hypothesises that the Ayauhasca activates the appendix excretion toxins into the lower intestinal tract where they can be efficiently purged via the anus.

Whilst taking a piss I looked up the composition of water H2O. The wonders of technology. 2 hydrogen (H) atoms and 1 oxygen atom. I’m not familiar enough with the intricacies of cells, and even if I was fuck knows how to prove it but that’s the only possible way of completing the circuit(s) on 50-100 Trillion living cells (khan 2024) doing their best to work together to keep us alive. DMT was originally N,N-dimethyltryptaminium described as a major microspecies at pH 7.3 it is a conjugate acid of a N,N-Dimethyltryptamine. With a Hydrogen Bond Donor Count of 2. Synonyms: N,N-dimethyltryptaminium, CHEBI:193124 and AKOS001584151. Molecular Formula C12H17N2+ (PubChem, 2004). According to Anon 2023 “A hydrogen bond is an intermolecular force (IMF) that forms a special type of dipole-dipole attraction when a hydrogen atom bonded to a strongly electronegative atom exists in the vicinity of another electronegative atom with a lone pair of electrons. Intermolecular forces (IMFs) occur between molecules. Other examples include ordinary dipole-dipole interactions and dispersion forces. Hydrogen bonds are are generally stronger than ordinary dipole-dipole and dispersion forces, but weaker than true covalent and ionic bonds.”. DMT is also likely activate the hydrogen and oxygen atoms which I expect plays a significant role in the regulation of inflammatory systems and transcytosis across and between various forms of cellular tissue. Chronic inflammatory diseases are the most significant cause of death in the world. The World Health Organization (WHO) ranks chronic diseases as the greatest threat to human health (Pahwa R, et al,. 2023).

N,N-Dimethyltryptamine's biophysiological interactions with H2O at the primary catalyst in Facilitating Hyper Generalised Cellular Divergence, Intracellularly, Extracellularly and Transcytosis in Multicellular Life. However, this only scrapes the surface of how DMT works. This publication raised the question what the fuck is a major microspecies inspiring a brief look back in time with DMT/DMT+ "Major Microspecies" & Suspected "Universal Ancestor" at the Trunk of the Biological "Tree of Life"!? before proceeding with the deeper exploration of this subject DMT/DMT+ & H2O: Group II Introns, Reverse Transcriptases in Hydrolytic Splicing, Intracellular & Extracellular Divergence & Transcytosis, & Healthy Genetic Evolution... & International Bioterrorism!!!

References

1. Anon, 2023. Hydrogen Bonding. [Accessed July 16, 2024] Available at: https://chem.libretexts.org/@go/page/1660 

2. Barksdale, Bryan & Doss, Manoj & Fonzo, Gregory & Nemeroff, Charles. (2024). The mechanistic divide in psychedelic neuroscience: An unbridgeable gap?. Neurotherapeutics. 21. e00322. 10.1016/j.neurot.2024.e00322 .https://www.researchgate.net/publication/377711235_The_mechanistic_divide_in_psychedelic_neuroscience_An_unbridgeable_gap

3. Cano RLE, Lopera HDE. Introduction to T and B lymphocytes. In: Anaya JM, Shoenfeld Y, Rojas-Villarraga A, et al., editors. Autoimmunity: From Bench to Bedside [Internet]. Bogota (Colombia): El Rosario University Press; 2013 Jul 18. Chapter 5. Available from: https://www.ncbi.nlm.nih.gov/books/NBK459471/

4. Cowie RH, Bouchet P, Fontaine B. The Sixth Mass Extinction: fact, fiction or speculation? Biol Rev Camb Philos Soc. 2022 Apr;97(2):640-663. doi: 10.1111/brv.12816. Epub 2022 Jan 10. PMID: 35014169; PMCID: PMC9786292. https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9786292/

5. Coffin JM, Hughes SH, Varmus HE, editors. Retroviruses. Cold Spring Harbor (NY): Cold Spring Harbor Laboratory Press; 1997. The Place of Retroviruses in Biology. Available from: https://www.ncbi.nlm.nih.gov/books/NBK19382/

6. Khan YS, Farhana A. Histology, Cell. [Updated 2023 May 1]. In: StatPearls [Internet]. Treasure Island (FL): StatPearls Publishing; 2024 Jan-. Available from: https://www.ncbi.nlm.nih.gov/books/NBK554382/

7. Kiani AK, Dhuli K, Donato K, Aquilanti B, Velluti V, Matera G, Iaconelli A, Connelly ST, Bellinato F, Gisondi P, Bertelli M. Main nutritional deficiencies. J Prev Med Hyg. 2022 Oct 17;63(2 Suppl 3):E93-E101. doi: 10.15167/2421-4248/jpmh2022.63.2S3.2752. PMID: 36479498; PMCID: PMC9710417. https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9710417/
   

8. Kyriakou E, Magiorkinis G. Interplay between endogenous and exogenous human retroviruses. Trends Microbiol. 2023 Sep;31(9):933-946. doi: 10.1016/j.tim.2023.03.008. Epub 2023 Apr 4. PMID: 37019721. https://pubmed.ncbi.nlm.nih.gov/37019721/

9. Liang X, Liu R, Chen C, Ji F, Li T. Opioid System Modulates the Immune Function: A Review. Transl Perioper Pain Med. 2016;1(1):5-13. PMID: 26985446; PMCID: PMC4790459. https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4790459/

10. Marie V, Gordon ML. The (Re-)Emergence and Spread of Viral Zoonotic Disease: A Perfect Storm of Human Ingenuity and Stupidity. Viruses. 2023 Jul 27;15(8):1638. doi: 10.3390/v15081638. PMID: 37631981; PMCID: PMC10458268. https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10458268/

11. Mikati MO, Klein RS. Fragile-like regulatory T cells modulate opioid withdrawal in humans and mice. Immunity. 2023 Feb 14;56(2):237-239. doi: 10.1016/j.immuni.2023.01.021. PMID: 36792570; PMCID: PMC10867865. https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10867865/

12. Mishra P, Beura S, Ghosh R, Modak R. Nutritional Epigenetics: How Metabolism Epigenetically Controls Cellular Physiology, Gene Expression and Disease. Subcell Biochem. 2022;100:239-267. doi: 10.1007/978-3-031-07634-3_8. PMID: 36301497.https://pubmed.ncbi.nlm.nih.gov/36301497/

13. Nogueira, Margareth & Golbert, Daiane & Menezes, Richardson & Almeida, Raíssa & Galvão-Coelho, Nicole & Siroky, Andressa & Lima, Thiago & Peixoto, Helton & Leao, Katarina & Leao, Richardson. (2024). Serotonergic psychedelic 5-MeO-DMT alters plasticity-related gene expression and generates anxiolytic effects in stressed mice. Molecular Psychiatry. 1-11. 10.1038/s41380-024-02655-w. https://www.researchgate.net/publication/382025962_Serotonergic_psychedelic_5-MeO-DMT_alters_plasticity-related_gene_expression_and_generates_anxiolytic_effects_in_stressed_mice

14. Pahwa R, Goyal A, Jialal I. Chronic Inflammation. [Updated 2023 Aug 7]. In: StatPearls [Internet]. Treasure Island (FL): StatPearls Publishing; 2024 Jan-. Available from: https://www.ncbi.nlm.nih.gov/books/NBK493173/

15. Plein LM, Rittner HL. Opioids and the immune system - friend or foe. Br J Pharmacol. 2018 Jul;175(14):2717-2725. doi: 10.1111/bph.13750. Epub 2017 Mar 23. PMID: 28213891; PMCID: PMC6016673. https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6016673/

16. Popkin BM, D'Anci KE, Rosenberg IH. Water, hydration, and health. Nutr Rev. 2010 Aug;68(8):439-58. doi: 10.1111/j.1753-4887.2010.00304.x. PMID: 20646222; PMCID: PMC2908954. https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2908954/

17. PubChem [Internet]. Bethesda (MD): National Library of Medicine (US), National Center for Biotechnology Information; 2004-. PubChem Compound Summary for CID 4525689, N,N-dimethyltryptaminium; [cited 2024 July 16]. Available from: https://pubchem.ncbi.nlm.nih.gov/compound/N_N-dimethyltryptaminium

18. Rathish B, Pillay R, Wilson A, et al. Comprehensive Review of Bioterrorism. [Updated 2023 Mar 27]. In: StatPearls [Internet]. Treasure Island (FL): StatPearls Publishing; 2024 Jan-. Available from: https://www.ncbi.nlm.nih.gov/books/NBK570614/

19. Rouse BT, Sehrawat S. Immunity and immunopathology to viruses: what decides the outcome? Nat Rev Immunol. 2010 Jul;10(7):514-26. doi: 10.1038/nri2802. PMID: 20577268; PMCID: PMC3899649. https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3899649/

20. Rudin D, Areesanan A, Liechti ME, Gründemann C. Classic psychedelics do not affect T cell and monocyte immune responses. Front Psychiatry. 2023 Jan 20;14:1042440. doi: 10.3389/fpsyt.2023.1042440. PMID: 36741125; PMCID: PMC9895091. https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9895091/

21. Sacerdote P, Limiroli E, Gaspani L. Experimental Evidence for Immunomodulatory Effects of Opioids. In: Madame Curie Bioscience Database [Internet]. Austin (TX): Landes Bioscience; 2000-2013. https://www.ncbi.nlm.nih.gov/books/NBK6402/

22. Szabo A , Kovacs A , Riba J, Djurovic S, Rajnavolgyi E, Frecska E, The Endogenous Hallucinogen and Trace Amine N,N-Dimethyltryptamine (DMT) Displays Potent Protective Effects against Hypoxia via Sigma-1 Receptor Activation in Human Primary iPSC-Derived Cortical Neurons and Microglia-Like Immune Cells, Frontiers in Neuroscience, VOL 10, 2016, 10.3389/fnins.2016.00423, ISSN=1662-453X https://www.frontiersin.org/journals/neuroscience/articles/10.3389/fnins.2016.00423

23. Szabo A. Psychedelics and Immunomodulation: Novel Approaches and Therapeutic Opportunities. Front Immunol. 2015 Jul 14;6:358. doi: 10.3389/fimmu.2015.00358. PMID: 26236313; PMCID: PMC4500993.https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4500993/

24. Sun, L., Su, Y., Jiao, A. et al. T cells in health and disease. Sig Transduct Target Ther 8, 235 (2023). https://doi.org/10.1038/s41392-023-01471-y, https://www.nature.com/articles/s41392-023-01471-y#citeas

25. Szabo A, Kovacs A, Frecska E, Rajnavolgyi E. Psychedelic N,N-dimethyltryptamine and 5-methoxy-N,N-dimethyltryptamine modulate innate and adaptive inflammatory responses through the sigma-1 receptor of human monocyte-derived dendritic cells. PLoS One. 2014 Aug 29;9(8):e106533. doi: 10.1371/journal.pone.0106533. PMID: 25171370; PMCID: PMC4149582. https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4149582/

26. Szabo A, Frecska E. Dimethyltryptamine (DMT): a biochemical Swiss Army knife in neuroinflammation and neuroprotection? Neural Regen Res. 2016 Mar;11(3):396-7. doi: 10.4103/1673-5374.179041. PMID: 27127466; PMCID: PMC4828992. https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4828992/

27. Tan, C.C.S., van Dorp, L. & Balloux, F. The evolutionary drivers and correlates of viral host jumps. Nat Ecol Evol 8, 960–971 (2024). https://doi.org/10.1038/s41559-024-02353-4https://www.nature.com/articles/s41559-024-02353-4#citeas

28. Van Blerkom LM. Role of viruses in human evolution. Am J Phys Anthropol. 2003;Suppl 37(Suppl ):14-46. doi: 10.1002/ajpa.10384. PMID: 14666532; PMCID: PMC7159740. https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7159740/