17 research outputs found
Development of coronary stents using advanced results of materials science and technology
Stents are high tech endovascular implants. K&M Inc. is the single Eastern European stent
producer company. The market needs more biocompatible devices as the trend of the stent
development all the producers have to react. The other members of a R&D consortium is
research institutions deals with diamond-like and drug-eluting coatings for decade. These
biocompatible coatings can avoid the metallic stent surface to directly contact to the living
tissues. This way a biologically active drug connected to the surface can be delivered directly
to the diseased vessel wall. The Cardiovascular Institution has the clinical facility to test the
new products. This group of applicants is obliged to develop, test and put on the market the
new generation biocompatible coated stents
Examination of mechanical and medical application properties of coronary stents
The medical application properties of coronary stents describe their behaviour in the human vascular system from planting to functioning. However these properties have great importance to surgeons, not all of them have standardized examination methods. In our study we demonstrate three procedures, which can be used to examine stents, considering the referred properties, like flaring, trackability and MSA (metallic surface area). In the course of our research four stents were investigated, three made of tube and one made of wire, and the results were promising about the application of these methods described in the followings
Blocking the Increase of Intracellular Deuterium Concentration Prevents the Expression of Cancer-Related Genes, Tumor Development, and Tumor Recurrence in Cancer Patients
The possible role of the naturally occurring deuterium in the regulation of cell division was first described in the 1990s. To investigate the mechanism of influence of deuterium (D) on cell growth, expression of 236 cancer-related and 536 kinase genes were tested in deuterium-depleted (40 and 80 ppm) and deuterium-enriched (300 ppm) media compared to natural D level (150 ppm). Among genes with expression changes exceeding 30% and copy numbers over 30 (124 and 135 genes, respectively) 97.3% of them was upregulated at 300 ppm D-concentration. In mice exposed to chemical carcinogen, one-year survival data showed that deuterium-depleted water (DDW) with 30 ppm D as drinking water prevented tumor development. One quarter of the treated male mice survived 344 days, the females 334 days, while one quarter of the control mice survived only 188 and 156 days, respectively. In our human retrospective study 204 previously treated cancer patients with disease in remission, who consumed DDW, were followed. Cumulative follow-up time was 1024 years, and average follow-up time per patient, 5 years (median: 3.6 years). One hundred and fifty-six patients out of 204 (77.9%) did not relapse during their 803 years cumulative follow-up time. Median survival time (MST) was not calculable due to the extremely low death rate (11 cancer-related deaths, 5.4% of the study population). Importantly, 8 out of 11 deaths occurred several years after stopping DDW consumption, confirming that regular consumption of DDW can prevent recurrence of cancer. These findings point to the likely mechanism in which consumption of DDW keeps D-concentration below natural levels, preventing the D/H ratio from increasing to the threshold required for cell division. This in turn can serve as a key to reduce the relapse rate of cancer patients and/or to reduce cancer incidence in healthy populations
Blocking the Increase of Intracellular Deuterium Concentration Prevents the Expression of Cancer-Related Genes, Tumor Development, and Tumor Recurrence in Cancer Patients
The possible role of the naturally occurring deuterium in the regulation of cell division was first described in the 1990s. To investigate the mechanism of influence of deuterium (D) on cell growth, expression of 236 cancer-related and 536 kinase genes were tested in deuterium-depleted (40 and 80 ppm) and deuterium-enriched (300 ppm) media compared to natural D level (150 ppm). Among genes with expression changes exceeding 30% and copy numbers over 30 (124 and 135 genes, respectively) 97.3% of them was upregulated at 300 ppm D-concentration. In mice exposed to chemical carcinogen, one-year survival data showed that deuterium-depleted water (DDW) with 30 ppm D as drinking water prevented tumor development. One quarter of the treated male mice survived 344 days, the females 334 days, while one quarter of the control mice survived only 188 and 156 days, respectively. In our human retrospective study 204 previously treated cancer patients with disease in remission, who consumed DDW, were followed. Cumulative follow-up time was 1024 years, and average follow-up time per patient, 5 years (median: 3.6 years). One hundred and fifty-six patients out of 204 (77.9%) did not relapse during their 803 years cumulative follow-up time. Median survival time (MST) was not calculable due to the extremely low death rate (11 cancer-related deaths, 5.4% of the study population). Importantly, 8 out of 11 deaths occurred several years after stopping DDW consumption, confirming that regular consumption of DDW can prevent recurrence of cancer. These findings point to the likely mechanism in which consumption of DDW keeps D-concentration below natural levels, preventing the D/H ratio from increasing to the threshold required for cell division. This in turn can serve as a key to reduce the relapse rate of cancer patients and/or to reduce cancer incidence in healthy populations
Detection of nanobacteria-like particles in human atherosclerotic plaques
Recent and historical evidence is consistent with the view that atherosclerosis is an infectious disease or
microbial toxicosis impacted by genetics and behavior. Because small bacterial-like particles, also known
as nanobacteria have been detected in kidney stones, kidney and liver cyst fluids, and can form a calci-
um apatite coat we posited that this agent is present in calcified human atherosclerotic plaques. Carotid
and aortic atherosclerotic plaques and blood samples collected at autopsy were examined for nanobacte-
ria-like structures by light microscopy (hematoxylin-eosin and a calcium-specific von Kossa staining),
immuno-gold labeling for transmission electron microscopy (TEM) for specific nanobacterial antigens,
and propagation from homogenized, filtered specimens in culture medium. Nanobacterial antigens were
identified
in situ
by immuno-TEM in 9 of 14 plaque specimens, but none of the normal carotid or aortic
tissue (5 specimens). Nanobacteria-like particles were propagated from 26 of 42 sclerotic aorta and
carotid samples and were confirmed by dot immunoblot, light microscopy and TEM. [
3
H]L-aspartic acid
was incorporated into high molecular weight compounds of demineralized particles. PCR amplification
of 16S rDNA sequences from the particles was unsuccessful by traditional protocols. Identification of
nanobacteria-like particles at the lesion supports, but does not by itself prove the hypothesis that these
agents contribute to the pathogenesis of atherosclerosis, especially vascular calcifications
Blocking the increase of intracellular deuterium concentration prevents expression of cancer-related genes, tumor development, and tumor recurrence in cancer patients
The possible role of the naturally occurring deuterium in the regulation of cell division was first described in the 1990s. To investigate the mechanismof influence of deuterium (D) on cell growth, expression of 236 cancer-related and 536 kinase genes were tested in deuterium-depleted (40 and 80 ppm) and deuterium-enriched (300 ppm) media compared to natural D-level (150 ppm). Among genes with expression changes exceeding 30% and copy numbers over 30 (124 and 135 genes, respectively) 97.3% of them was upregulated at 300 ppm D-concentration. In mice exposed to chemical carcinogen, one-year survival data showed that deuterium-depleted water (DDW) with 30 ppm D as drinking water prevented tumor development. One quarter of the treated male mice survived 344 days, the females 334 days, while one quarter of the control mice survived only 188 and 156 days, respectively. In our human retrospective study 204 previously treated cancer patients with disease in remission, who consumed DDW, were followed. Cumulative follow-up time was 1024 years, and average follow-up time per patient, 5 years (median: 3.6 years). One hundred and fifty-six patients out of 204 (77.9%) did not relapse during their 803 years cumulative follow-up time. Median survival time (MST) was not calculable due to the extremely low death rate (11 cancer-related deaths, 5.4% of the study population). Importantly, 8 out of 11 deaths occurred several years after stopping DDW consumption, confirming that regular consumption of DDW can prevent recurrence of cancer. These findings point to the likely mechanism in which consumption of DDW keeps D-concentration below natural levels, preventing the D/H ratio from increasing to the threshold required for cell division. This in turn can serve as a key to reduce the relapse rate of cancer patients and/or to reduce cancer incidence in healthy populations