This is the process.
Bacteria such as Haemophilus influenzae stick to the respiratory mucosa
Bacteria divide and colonise the mucosa (forming a microbiome)
Bacteria are coughed up in sputum
Sputum is swallowed, therefore bacteria are swallowed
Most bacteria are simply digested in the stomach
A small percentage make it through to the small intestine
These bacteria are taken up by immune lymphoid tissue in the wall of the small intestine called Peyer’s patches
Peyer’s patches recognise these bacteria as foreign
Peyer’s patches produce a form of T helper cell to combat the infection
These newly formed T cells migrate in the blood to the lungs, then into the lung mucosa
Here the new T helper cells ‘help’ the activation of immune responses such as the formation of more neutrophils
These neutrophils are phagocytic, they eat any foreign material, such as any bacteria and any virus. They are not fussy eaters; they eat any antigen.
The person now enjoys ‘learned innate immunity’
As bacteria and viruses are eaten and internally digested in the upper part of the lungs, they are dead, so cannot migrate down to infect the alveoli, the gaseous exchange structures.
As the alveoli are not infected, they do not become inflamed, therefore they do not fill up with inflammatory fluid leading to a consolidated pneumonia
As these thin-walled alveoli are not infected, the viruses and bacteria are not present, so do not migrate into the blood leading to systemic illness.
Therefore, in short, the person stays well
As the T cells are very powerful stimulants of immunity and inflammation, we do not want them hanging around for a long time, therefore they are short lived in the lungs
However, the neutrophils they have stimulated self-perpetuate over a longer period of time (probably about 10 months)
This means the upper airways are patrolled and protected for months after an episode of T cell stimulation
As the upper airways are kept clear of viruses and bacteria the lower airways are protected from descending infection
Therefore, infections such as influenza or covid may present as mild or even asymptomatic
Such a protected person is therefore able to ‘compartmentalise’ the infection in the upper airways, preventing it from descending to the lower alveoli
Physiologically, this system is protective but imperfect, for example a lot of the bacteria are digested in the stomach
This means some people will be well protected from severe disease after covid or influenza infection, while others are not
Giving an optimised strain of Haemophilus influenzae as an Immunobiotic can enhance the efficiency of this natural physiological system
The administered Haemophilus influenzae is killed, so cannot reproduce to cause disease
The administered Haemophilus influenzae is enteric coated, so it will be protected as it passes through the stomach, meaning it will reach the small intestine in large numbers
This will provide lots of stimulation to the Peyer’s patches
This is not a vaccination, it is an augmentation of a completely natural physiological system
A tablet could probably be taken before every winter as an OTC (over the counter medication)
Millions of acute exacerbations (going to the lungs) could be prevented
The tablet would cost very little as an OTC, it’s just dead bugs
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