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Pleomorphism and Germ Theory Explained - Live Blood Online

The cells can change to different types, from fungus, bacterium, virus and more. Becham versus Pasteur.

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100% found this document useful (1 vote)
80 views10 pages

Pleomorphism and Germ Theory Explained - Live Blood Online

The cells can change to different types, from fungus, bacterium, virus and more. Becham versus Pasteur.

Uploaded by

Carl MacCord
Copyright
© © All Rights Reserved
We take content rights seriously. If you suspect this is your content, claim it here.
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Pleomorphism and Germ Theory Explained

Pleomorphism and germ theory


The accepted biological paradigm today, which has led to the development of the

pleomorphism and germ theory, is Monomorphism (Gr. mónos: single + morphē: form).

This paradigm, developed by Louis Pasteur and other scientists, states that all

microorganisms only have one possible form and do not have the ability to evolve into

different types of organisms.

The germ theory followed, which states that speci�c diseases are caused by infection

with speci�c microorganisms and are cured when the microorganisms have been

destroyed.

 
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This led to the development and widespread use


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of antibiotics, animal testing and
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many of the other atrocities of modern medicine.
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Pleomorphism, the polar opposite of Monomorphism, was developed by scientists like

Antoine Béchamp and Günther Enderlein and states that microorganisms have various

life cycles and stages of development that can range between viruses, bacteria, yeast

and fungi, depending on the type of microorganism and the environment it is presented

with.

What is interesting is that pleomorphism and its proponents has been entirely written

out of history books and encyclopedias and is not as much as mentioned, even for

historical interest, in universities and training institutions.

Antoine Béchamp

We

will

begin

our

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overview of theAbout
history of pleomorphism at theThe
beginning, with French scientist
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Antoine Béchamp (1816-1908).
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Béchamp was a Master of Pharmacy, Doctor of Science, Doctor of Medicine, Professor of


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Medical Chemistry and Pharmacy, Fellow and Professor of Physics and Toxicology,

Professor of Biological Chemistry and Dean of the Faculty of Medicine.

He was actively involved in his biological research at the same time as Louis Pasteur.

Ten years of experimentation led Béchamp to the conclusion that the tiny “molecular

granulations” that have been observed in the cells of plants and animals by other

researchers, were living elements.

He called them “microzymas” (small ferments), due to their ability to ferment sugar.

He continued his research over another 13 years, developing the Theory of Microzymas.

This theory states that the microzyma is an independently living element, found in all

living organisms and survives after the death of the organism. It functions to both build

and recycle the organism.

It is the builder and destroyer of cells; it precedes life at the cellular level and is the

foundation of all biological organization. In healthy conditions, the microzymas have a

bene�cial relationship with the organism and fermentation occurs normally.

However, microzymas are very sensitive to biological signals, responding to changes in

the terrain, especially pH. When the terrain becomes compromised, the microzymas

become what Béchamp called “morbidly evolved”, changing into microscopic forms

(bacteria) that contribute to the development of illness. Béchamp believed this

characteristic to be linked to the function of the microzymas to recycle the body upon

death.

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The change in About


the terrain is interpreted by the microzymas that the organism is already
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dead, which is a signal for them to change into the “morbidly evolved” forms capable of
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more vigorous fermentative breakdown.

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Béchamp was also able to show that compounds such as alcohol and acetic acid are

produced in the tissues of all organisms as a direct result of the fermentation activity of

the microzymas.

The difference between the two theories is quite clear:

Pasteur’s germ theory sees disease as being caused by external factors, whilst

Béchamp’s pleomorphic theory considers the internal environment as the most

important contributing factor.

Béchamp did not deny that the air carried germs, but maintained that they were not

primarily responsible, and certainly not necessary, for disease. They are only present

because of the compromised terrain. A good analogy was made by Rudolph Virchow: “…

mosquitoes seek the stagnant water, but do not cause the pool to become stagnant.”

Claude Bernard

A researcher worth mentioning, who preceded Antoine

Béchamp, was French physiologist Claude Bernard

(1813-1878).

He was one of the �rst scientists of his time to see that

disease is not simply determined by the germs involved

or the symptoms present. He believed disease to be a

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by the body’s internal environment, which he called the


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“Terrain”.
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The state of the terrain is determined by four factors, namely:


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1) its acid/alkaline balance;

2) its electric/magnetic charge;

3) its level of poisoning;

4) its nutritional status.

Royal Raymond Rife

During the 1920’s R.R. Rife was researching a method to

treat disease by destroying microorganisms through

radio frequency radiation. To help him determine the

correct frequency, he designed and built a most

incredible microscope (consisting of 5682 parts) that

used polarizing prisms to “stain” the organisms with

light. He then used a radio frequency beam ray to

destroy the organisms, which he used successfully to

cure many serious conditions, including polio, TB and

cancer.

He is relevant to the history of pleomorphism in that he was able to isolate a virus he

found in cancerous tissue and transform it into a fungus and then into a bacterium. He

was able to repeat this hundreds of times and showed that the pleomorphic
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development ofAbout
microorganisms goes beyond the bacterial level to the fungal stage.
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Günther EnderleinMicroscopes Blog  

German zoologist and bacteriologist Prof. Dr. Günther

Enderlein (1872-1968) is still considered by many as the

father of pleomorphism. He based his work on that of

Antoine Béchamp and conducted research for over 60

years, which led him to several remarkable discoveries.

He showed that the protit, not the cell, is the smallest

biological unit of life. Protits (Béchamp’s microzymas)

are small, living protein particles found in all the cells, blood and other �uids of all living

organisms. They can not be destroyed and survives after the death of the organism,

performing the function of decomposition.

He also found that the blood is not sterile and that it contains tiny life forms, capable of

evolving into more complex, pathogenic (disease-causing) organisms when conditions

are favourable.

Much of his discoveries he made because he was looking at live blood in dark�eld. This

helped himPrivacy
to see&that
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in healthy 

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working with the body in a symbiotic relationship. However, when presented with a
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disturbed environment, the protits are able to develop into more complex, pathogenic
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forms, including bacteria and fungi. The speci�c symptoms and forms of disease

depend on the level of development of the pathogenic


Microscopes Blog forms,
which is governed by the
state of the terrain.

Enderlein referred to all the possible developmental forms of the protits as the

Endobiont. He discovered that two microbes exist, and has always existed, in all

vertebrate mammals. These are Mucor racemosus Fresen, which he called the primary

parasite, and Aspergillus niger van Tieghem.

Mucor is found in the blood and other cells and when in its bene�cial, primitive stages,

it is responsible for the coagulation of blood. When in its pathogenic stages, Mucor

leads to congestion, cancer and many other degenerative diseases.

Aspergillus, in its primitive stages, is responsible for the regulation of the citric acid

cycle and calcium metabolism.

Enderlein believed that the infection of mammals with Aspergillus allowed for the

development of skeletal structures.

Aspergillus can be found in the bones, connective tissue and lymphatics. Pathogenic

phases of Aspergillus are responsible for para-tubercular diseases, connective tissue

disorders, arthritis and skin problems.

Enderlein showed that while exogenous microorganisms are monomorphic and

produce recognizable, communicable diseases, other non-communicable, chronic

diseases are caused by the pathogenic evolution of the pleomorphic Endobiont.

This evolution is governed by the state of the terrain, particularly the pH.

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The Anartatic Law of Interdependence states that the progressive development of


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microorganisms from the protit stages into their higher and highest stages requires a
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progressively descending pH.

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This process, once started, is then supported by the Endobiont itself, which produces

acid wastes from its metabolism of protein. Each microorganism produces a speci�c

organic acid: Aspergillus produces citric acid and Mucor produces lactic acid.

It is important to note that Enderlein described the evolution of Mucor and Aspergillus,

both of which �nd their culminant (highest stage of development) as a fungal organism.

Other organisms that may also be pleomorphic do not necessarily have their

culminants in the fungal phase, but rather in the bacterial phase (e.g. Staphylococcus

aureus).

Gaston Naessens

Quebec scientist Gaston Naessens, who is currently

involved in research, has also contributed greatly to

pleomorphism. He designed a special microscope,

called the “Somatoscope”, which enables him to

observe changes in living tissue at very high

magni�cation and resolution.

He, like Enderlein and Béchamp, discovered small

living particles, which he called “somatids”. He has identi�ed two somatid cycles: the

microcycle and the macrocycle. Only the microcycle occurs in health and consists of

only three stages, where all three forms are symbiotic. The macrocycle occurs in

disease and consists


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The culminant fungal phases of Mucor racemosus and Aspergillus niger only occupy
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the blood after death as it requires an acidic environment.
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There are transitional mycelial phases that can however be observed in the blood.
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These phases represent the highest phase of Mucor’s development in the living host and

their presence is indicative of severe conditions.

By Elizabeth Clemons | November 3rd, 2017

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