Laboratory Analysis

Increased urinary lead excretion after injection of EDTA is a recognized test for lead accumulation in the body.⁶ Urinary lead excretion was measured before and after EDTA infusion in 5 patients with atomic absorption spectroscopy,⁷ using the method of Roosels.⁸  In every case, a substantial increase in lead excretion was measured.  Simultaneously, urinary delta-amino levulinic acid (DALA) decreased.  DALA was measured in the Central Laboratories of the University Hospital of Zurich, according to the methods of Doss and Schmidt.⁹

   It is emphasized that the population studied and reported on in this paper was not exposed to any more lead or other environmental carcinogens than residents of most metropolitan areas throughout the world.

    Traffic flow past residences of the study subjects was 4000 vehicles per day in 1956, increasing to 8000 vehicles per day in 1968.  Of those, 7000 were passenger cars and 400 were diesel trucks.

    Environmental measurements of pollutants and carcinogens were made in the immediate and surrounding area of this study.  Tests were done at the Woods Hole Laboratories, Massachusetts, USA, using ultraviolet spectrophotography, mass-spectrography and chromatography.¹⁰   Soil tests adjacent to the highway where the study population lived showed the presence of polycyclic aromatic hydrocarbons, which are known carcinogens.  In more remote sections of the same city, levels of these pollutants were found to be approximately three times lower, inversely correlated with the distance from automobile traffic.  Further analyses showed the majority of measured carcinogens to be from automobile pollution.  Pollution immediately adjacent to the highway where the study population resided was at or only slightly above permissible levels allowed under public health and environmental regulations in the USA.

 

Discussion

Following preliminary communication of these data, the committee responsible for the surveillance of air quality in Switzerland scrutinized the results using a different statistical method.¹¹    They found a higher incidence of death from cancer in the untreated group than in the population of Switzerland as a whole.

The fact that an identical group treated with EDTA experienced a 90% reduction in cancer mortality, as well as a reduction in death from all causes was also confirmed.  The fact that the general mortality as well as cancer mortality was lower in treated than untreated individuals was also confirmed by Knutti and Schlatter.¹¹  Their proposed explanation was that treated patients might possibly have been more health conscious or under better medical care, but this does not seem an adequate explanation of the recorded facts.  Residents of less polluted areas experience a lower cancer mortality, despite the same level of medical care.

    Evidence presented in this paper indicated that (1) EDTA removes cancer causing or promoting substances, from the body, and (2) those substances are correlated with environmental pollution from vehicular traffic.

    The overall reduction of death from all causes and increased Longevity I the EDTA treated group shows that chelation therapy also reduces other common causes of mortality such as artherosclerosis and cardiovascular disease.  Except for cancer mortality, exact data are not available for statistical analysis.

    As early as 1961, it was reported from animal experiments that intravenous injections of EDTA could slow the growth of experimental carcinoma ¹².   A cancer-inhibiting effect has also been demonstrated for other chelating agents, including BAL, cystine, penicillamine and citric acid ^13-16.   Many tumor inhibiting medications, including 5-flouracil, possess metal-binding properties. ¹⁷

    Lead potentiates the carcinogenicity of aromatic hydrocarbons such as benzopyrene by five fold. 18 areas adjacent to heavily traveled highways are polluted with many other carcinogens, including polycyclic aromatic hydrocarbons, nitrosamines, epoxides, cadmium and asbestos, in addition to inorganic and tetraethyl lead.

    Since the data from this study were last reported,⁵ new research has linked cancer to free radical pathology. ^19-21.  EDTA removes transition elements, such as iron, which accelerate free radical pathology, including cancer.  Iron is an essential nutritional element but it is also know to accumulate with age.  Catalysis of lipid peroxidation by iron potentiates the cancer promoting substances.  EDTA increases the urinary excretion of unbound and freely catalytic iron 10 times more then it does lead.  There are many reasons why EDTA chelation therapy could act to prevent cancer.

    A recent publication by McDonagh, et al, ²² confirms improvement in a wide variety of symptoms, as first reported in this study population.2 Neurasthenic and nonspecific multi-organ symptoms improve significantly following EDTA chelation therapy, resulting in a marked improvement in the overall quality of life.

    Body stores of iron correlate with the risk of cancer.^23-25 and artherosclerosis. ²⁶ EDTA removes unbound and potentially toxic iron from the body much more effectively than lead, ²¹ which may account for the findings in this study.

    Large scale, double blind, controlled studies should be undertaken to fully document the many benefits observed in clinical practice following treatment with EDTA.   EDTA is an inexpensive and relatively safe substance to administer but he patent has expired and pharmaceutical companies have no incentive to fund such research. 

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