Dr. Tau Braun

@drtaubraun

Biological Warfare: How a Bat Reproductive Operating System Was Forced Into Humanity
Deep in the mountains of Yunnan Province, China, in the spring of 2012, six men walked into an abandoned copper mine to clear bat guano from the walls. Bat guano is the accumulated droppings of bats, a rich, dark, crumbly material that is absolutely loaded with fungal spores. Within days, they were fighting for their lives.
They developed high fever, dry cough, profound fatigue, and severe respiratory distress. CT scans showed diffuse ground-glass opacities throughout their lungs, hazy shadows caused by alveolar damage and surfactant breakdown. Blood tests revealed elevated D-dimer, coagulopathy, thrombocytopenia, and clear evidence of widespread microvascular injury. Three of the six miners died. The survivors endured months of debilitating illness that looked like a bizarre hybrid of severe pneumonia and systemic metabolic collapse.
Scientists later traced the source to horseshoe bats roosting in that very cave. In 2013, a team led by Shi Zhengli from the Wuhan Institute of Virology returned to the mine and collected samples. The researchers made multiple trips back to the same cave between 2012 and 2015, gathering hundreds of samples from the bats and the environment.
Among those samples was a previously unknown sequence they named RaTG13.
In the female horseshoe bat, RaTG13 is not a pathogen. It is an exquisitely evolved reproductive operating system. After mating, the female uses this sequence and its associated spike protein to construct a durable amyloid-rich copulatory plug that preserves sperm for many months. She downregulates her core metabolism into deep torpor. She deploys phospholipase A2, the same potent enzyme family found in snake venoms, together with neutrophil elastase to precisely remodel reproductive tissue and later dissolve the plug at exactly the right moment. She activates galectin-3-mediated immune tolerance to prevent rejection of the foreign material. And she maintains a persistent low-grade IFN-γ signal that orchestrates the entire program while providing low-energy antimicrobial defense.
The system has another sophisticated layer: the RaTG13 spike protein sequence is packaged into exosomes, small extracellular vesicles that function as mobile biological messengers. These exosomes are shared among females in the dense cave colony through grooming, close contact, and aerosolized air, creating a colony-wide synchronization of reproductive timing and hibernation. It is a form of chemical communication that allows the entire group to coordinate their mating cycles and torpor states.
Scientists added a highly optimized furin cleavage site, functioning as a master “on-switch,” to the same biological instruction manual. The resulting combination, now known as SARS-CoV-2, was then introduced to humans.

It uses two primary entry routes, each triggering distinct pathology.
Nasopharynx Entry: The sequence, frequently carried in exosomes, is inhaled and binds to the olfactory epithelium. It exploits ACE2 receptors densely expressed on olfactory sensory neurons and sustentacular cells (the supportive “nurse” cells that physically anchor, nourish, and help regenerate the smell-sensing neurons while also forming part of the blood-nasal barrier). Once inside, it listens for volatile organic compounds produced by the nasal fungal microbiome. When these chemical cues appear, furin cleaves the spike protein, activating the full program. Chemotaxis plays a central role: the sequence induces strong chemotactic signals that recruit specific T-cell populations into the nasopharynx and olfactory bulb, establishing a persistent reservoir of IFN-γ-producing cells. This produces the characteristic burning dry throat, anosmia, and persistent local IFN-γ production. A deep nasal swab can mechanically damage this fragile mucosa, creating a direct pathway for the sequence to leak into the bloodstream.
Endothelial Entry: Once the sequence enters the circulation, whether through nasopharyngeal leakage, swab-induced trauma, or direct injection via the Covid Vaccines, the furin cleavage site enables rapid activation on vascular endothelial cells. The prompt now deploys its full set of reproductive and hibernation mechanisms across the entire body. It drives the formation of persistent fibrin amyloid microclots (fibrinaloids) that are functionally analogous to the bat’s durable copulatory plug — both create a long-lasting, protease-resistant protein matrix that maintains its biological cargo over extended periods. These microclots spread throughout the microvasculature, causing strokes in the brain, myocarditis in the heart, and kidney injury in the renal capillaries, and these represent only some of the widespread pathology seen across multiple organ systems. The prompt also hijacks nicotinic acetylcholine receptors, disrupting autonomic signaling and forcing cells into a sustained low-metabolic torpor state.
At the heart of both routes is persistent low-grade IFN-γ. In the bat, this signal is a carefully regulated coordinator that maintains immune tolerance, keeps the remodeling enzymes active at low levels, sustains the torpor state, and provides antimicrobial cover without wasting energy. In humans, because there is no seasonal off-switch, IFN-γ remains chronically elevated at low-to-moderate levels. It locks the entire system in place: reinforcing galectin-3 immune tolerance, sustaining amyloid microclot formation, suppressing mitochondrial function, and preventing the body from ever clearing the prompt.
The body is not fighting an infection. It is faithfully executing a bat’s reproductive maintenance program in a species that lacks any off-switch, any seasonal cue to exit torpor, and any biological context for the instructions it is following.
Because this system was never designed to run indefinitely, the damage accumulates relentlessly across major organs. In the lungs, ongoing phospholipase A2 and neutrophil elastase activity erodes surfactant and alveolar architecture. In the heart, microvascular occlusion and metabolic suppression lead to myocarditis and arrhythmias. In the brain, microclots and nicotinic receptor dysregulation cause strokes, cognitive and autonomic dysfunction. In the kidneys, capillary blockage and chronic inflammation drive progressive renal failure. The liver, spleen, and gastrointestinal tract suffer similar microvascular and metabolic insults. Persistent immune tolerance creates an environment that promotes cancer.
A reproductive strategy refined over millions of years for a small bat species has been unleashed in humans, where it functions as a devastating, self-perpetuating physiological trap. The body begins to dry up, crumble, and waste away.
It is vital that we truly understand what this sequence is really doing inside human beings. Only by recognizing that SARS-CoV-2 and its derivatives are running a misplaced bat reproductive hibernation maintenance program, complete with amyloid plugs, torpor metabolism, immune tolerance, and persistent IFN-gamma orchestration, can we develop mitigation strategies and treatments that actually match the underlying pathology instead of fighting the wrong battle. Until that biological reality is acknowledged, we will continue to apply mismatched solutions to a system that was never designed to run in our species.

Image Source: https://doi.org/10.1007/s00435-019-00467-z

Special Acknowledgement for investigating RaTG13 Steve Massey @stevenemassey
and Monali C. Rahalkar @MonaRahalkar

Note: This article was revised for accuracy regarding the functional analogy between bat copulatory plugs and human fibrin amyloid microclots. In a future article, I will illuminate the microclots and the rubbery calamari-like structures, and detail the underlying mechanisms.

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