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The application of diuretics induce an increased rate of wat
The application of diuretics induce an increased rate of water exiting brain cells encouraging the formation of increased intracellular polyphosphoric acid. In the absence of the diuretic water is retained in cells converting polyphosphoric tsa hdac synthesis to monophosphoric acid. The latter change decreases the hydroxylamine/hydrogen peroxide production and betaine formation. This effect is also enhanced by defective operation of the hypothalamus in controlling brain water content [34], [35], [36].
Lewy bodies and amyloid plaques
The formation of Lewy bodies and amyloid plaques associated with Parkinson’s and Alzheimer’s diseases are examples of protein polymerisation. Organic peroxides such as benzoyl peroxide are initiators of polymerisation. As shown active monatomic oxygen is produced in the brain and acts as a polymerisation agent. Entry into the cerebrospinal fluid induces polymerisation of proteins in this fluid and any associated tissue. This mechanism is supported by the observation that treatment using indole-3-propionic acid in the case of Alzheimer’s disease retards the formation of polymerised protein bodies [26]. This compound is derived by hydrolysis decomposition of tryptophan betaine. The transfer of indole-3-propionic acid into the brain cells involved therefore has the effect of slowing the formation of tryptophan which is one source of active oxygen leading to formation of amyloid plaques. Continuous treatment with indole-3-propionic acid would be expected to further slow tryptophan betaine formation ultimately causing a decrease of the activity of one of the sensory organs, for example hearing. In the case of Parkinson’s disease the high rate of production of hydrogen peroxide/hydroxylamine gives rise to leakage of a high concentration of monatomic oxygen into the cerebrospinal fluid from increased glucose/fructose decomposition producing Lewy bodies by protein polymerisation. This situation is further enhanced by the formation of glycine amino acid as described above. This compound is a component of proteins and additionally interferes with normal protein in the brain. Ultimately the excess of oxygen extends the distribution of Lewy bodies producing added physical interference with brain operations.
Conclusions
The above proposals also indicate that motor neuron disease and multiple sclerosis are also likely to be the result of the intermittent failure to produce hydrogen peroxide and hydroxylamine and/or the presence of excess metabolic iron which completely decomposes any of these compounds produced. Excess metabolic iron has been demonstrated to occur in cases of both diseases [37], [38], [39], [40], [41]. This condition is amplified by progressive or intermittent decrease of the metabolic intake of sulphate and nitrate required to form hydrogen peroxide and hydroxylamine and reduced sequestration of iron at high blood pH values (alkalosis).
Conflict of interest