Excerpt for MIASMS- The Killer Bodyguards by , available in its entirety at Smashwords







MIASMS

Killer Bodyguards!



By

Chandran K C



Copyright 2018 Chandran K C

A Smashword Edition













Chapter 1. Redefining 'Miasms'

Homeopathic understanding and management of ‘chronic disease’ is based on the concept of ‘miasms’. Hahnemann has provided detailed explanations regarding three types of ‘miasms’ such as ‘psora’, ‘syphills’ and ‘sycosis’. Theory of  ‘miasms’ and chronic diseases were developed during later part of Hahnemann’s life, when he learned from his clinical experience that medicines selected on the basis of similarity of symptoms as he advocated earlier offered only temporary relief to the most patients.

According to his theory of ‘chronic diseases’, ‘psora’, the ‘miasm’ of suppressed ‘itch’, is the underlying primary cause of all chronic diseases other than those of ‘venereal’ origin. ‘Psora’ is said to be the greatest obstruction to cure. Other two miasms, ‘syphilis’ and ‘sycosis’ are considered to be miasms of venereal diseases, ‘syphilis’ and ‘gonorrhoea’ respectively. Hahnemann considered ‘psora’ to be the most important and universal ‘miasm’. According to his theory, unless this ‘miasm’ or ‘disease poison’ is eradicated with appropriate ‘anti-psoric’ drugs, permanent and lasting cure cannot be attained.

The primary forms of expression of ‘psora’ is considered to be the itching eruptions on skin, that of ‘syphilis’ un-healing tissue destructions like malignant ulcers, and that of ‘sycosis’ warts and condylomata.

Symptoms of primary ‘psora’ include the different types of itches and eruptions that appear on the skin. Hahnemann considered the ‘miasm of psora’ to be inherited through generations of human kind.

Now, let us try to analyze the concept of miasms and chronic diseases in the light of scientific understanding of molecular biology, ‘similia similibus curentur’ and ‘potentization’.

Human organism is constantly exposed to the attacks of various types of exogenous and endogenous foreign molecules and ions. They may bind to the complex native biological molecules, thereby deforming their configuration and making them incapable of participating in the normal bio-chemical interactions. As per scientific view, this phenomenon underlies the molecular basis of most pathological conditions.

If the pathological foreign molecules are of protein nature, native biological defense proteins having configurational affinity to these foreign proteins attaches to them, destroys and removes them from the organism as part of body’s defense mechanism.  During this defense process, some of the involved native protein molecules get configurationally deformed by the interaction with foreign molecules. Native protein molecules so deformed will be carrying the 3-D spacial impressions of the interacted foreign molecules on their periphery. These impressions exist as three dimensional pockets, having a configuration complementary to that of foreign proteins. These molecular imprinted proteins thus become incapacitated for their normal biological processes, and remain a burden in the organism. Antibodies actually belong to this class of such deformed globulin proteins, subjected to ‘molecular imprinting’ by foreign proteins.

Certain endogenic molecules and ions such as hormones, neuro-chemicals, and other metabolic byproducts such as super-oxides, when circulated in excess, may   also attach to various bio-molecules other than their natural targets, and induce configurational changes in them.


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