Monday, April 1, 2019
Causes of Cardiovascular Disease | Literature Review
Causes of Cardiovascular unhealthiness Literature Review2 Abstract3 Introduction 3.1 Cardiovascular distemperCardiovascular complaint (CVD) is the broad shed light on of diseases that involves the heart or/and blood vessels. CVD includes coronary thrombosis arteria disease, heart valve disease, arrhythmia, heart failure, hypertension, endocarditis, diseases of the aorta, disorders of the peripheral vascular system, and congenital heart disease 1. However, atherosclerosis accounts for the major give away of CVD (up to xx%), and sometimes CVD is mis hightail iting used as a synonym for atherosclerosis REF. Be ingest atherosclerosis is the underlying disease of several CVD, part of patients, where one diagnosis of CVD became manifest, may present with further co-morbidities, especially separate diagnosis of CVD argon common. However, the portion of patients with co-morbidities is depending on the baseline disease 2-4. For example 40-60% of patients with peripheral arterial infirmity ( roam) similarly present coronary artery disease (CAD) and noetic artery disease, but just now 10-30% of patients with CAD have withal drift (Figure 1) 2, 4. kick upstairs, the severity of cardiovascular co-morbidities correlates well with each other5-7.CVD is today liable for ca. 30% of all finales worldwide 8, while heart disease and stroke atomic number 18 the leading causes of mortality and disability in developed countries 9. Although the mortality grade of CVD has a considerable variation across countries (xx% in xx to xx% in xx) 10, a common trend of increase rates has been ascertained worldwide. Before 1900, infectious diseases and malnutrition were the well-nigh(prenominal) common causes of termination throughout the world, and CVD was responsible for The economic burden and the public health costs ar generally driven by CVD. In terms of combined morbidity and mortality, 148 one thousand million Disability-Adjusted Life-Years (DALYs) were lost w orldwide (2002), which represents nigh 10% of all lost DALYs REF. In 2008, CVD costs about 192 billion Euros a year alone in the European Union, which firmnesss in a per capita cost of 391 Euros 13.3.1.1 coronary artery diseaseAtherosclerosis is the most frequent and important pattern of Arteriosclerosis, other classs of Arteriosclerosis be Mnckeberg medial calcific sclerosis and Arteriolosclerosis, which vary in pathophysiological and clinical demonstration 14. As describe above (3.1), atherosclerosis is the leading cause of death (up to 30%) in developed countries and represents the major portion of CVD.Atherosclerosis (literal line of credit from Greek athero = gruel or paste sclerosis = hardness) is delimit as thickening and loss of rubber bandity of arterial fence ins and describes a cognitive process, where avoirdupois weightty substances, cholesterol, cubicleular waste products, calcium and fibrin building up in the inner line drive of arteries 14. These intimal lesions be called atheromas, atheromatous or fibrofatty plaques, which lead into an obstruction of vascular lumens and weakness the underlying media. Even deep down a given arterial bed, lesions or stenoses due to atherosclerosis tend to occur focally, typically in certain predisposed regions.3.1.1.1 Pathogenesis of AtherosclerosisDue to overwhelming importance of atherosclerosis, abundant efforts have been spent to discover its cause over the last hardly a(prenominal) decades. Today, the up-to-dately accepted concept, so called the response to reproach hypothesis, considers atherosclerosis to be a chronic instigative response of the arterial fence in initiated by injury to the endothelium 15. Further more(prenominal) than, lesion initiation and progression be sustained by interaction betwixt lipoproteins, macroph suppurates, T-lymph cells, and the normal cellular constituents of the arterial wall. This process of underdeveloped atherosclerosis, which typically lasts ov er a period of many years commonly many decades, toilet be split into several consecutive steps, as illustrated in Figure 2 REF. Parallel, a morphological change is spy inside the artery wall, where fatty streak represents the initial morphological lesion, regular(a) so the pathogenesis has started quite earlier with a chronic endothelial injury REF.Figure 2 Illustration of the Pathogenesis and Morphological Development of Atherosclerosis. SMC Smooth vigour Cell 6 m thick histology slices of coronary arteries stained with Movats pentachrome. A pathological intimal thickening with a fatty streak B pathological intimal thickening with a macroph shape up infiltration C proterozoic fibroatheroma with neoangiogenesis D fibroatheroma with thin thready cap and a healed snatch E late fibroatheroma with a sheet calcification. * demarks necrotic scores. Histology performed by CVPath Laboratory, Maryland, MD.The below describe steps of the pathogenesis of atherosclerosis shouldnt be en seen as a separated processes. They be interconnected and occur parallel. Further, several mechanism of vicious circles atomic number 18 described REF. However, the stratification into the flowe six steps helps to understand the complex pathogenesis and represents the current understanding(1) Chronic Endothelia InjuryAs the earliest step in the pathogenesis of atherosclerosis, endothelial activation and chronic injury, also known as endothelial disfunction, have been described 16. The following actors contributed in different extent to endothelial dysfunction and argon partly known as traditional assay parts for atherosclerosis 17 advancing age, dyslipidemia, hypertension, increase levels angiotensin, insulin resistance and diabetes, smoking, estrogen deficiency. Several biochemical pathways have been described for those factors increasing the endothelial dysfunction. Other factors like hyperhomocysteinemia, assertable infection and especially low or oscillatory shear tens e are still discussed whether they signifi batchtly contribute to endothelial dysfunction 18-22. The phe nonypical features of endothelial dysfunction are described as the cut downd vasodilator and increased vasoconstrictor capacity, an enhanced leukocyte trammel, an increase of pro-thrombotic and decrease of fibrinolytic activity, and an increase in out ontogenesis-promoting.(2) Accommodation and Oxidation of LipoproteinsIn addition and due the endothelial dysfunction lipoproteins, especially low density lipoprotein (LDL), sequestered from plasma in the extracellular space of the arterial intima. Beside the extent of endothelial dysfunction, this process is depending on the assiduousness of LDL in the blood circulation 23. Even so several mechanisms have been proposed for transport of LDL into the arterial intima including vesicular ferrying through endothelial cells, passive sieving through endothelial-cell pores, passage amongst cells, its not finally understand. However, n oticeable evidence exist, that the accommodation of LDL in the arterial intima is not only a passive meat by a leaking vascular endothelium REF. actuate of the lipoproteins that have entered the arterial wall stay there and are modify subsequently. Especially the registration of the lipoproteins has a trapping function for die selbigen 24. The most common modification is the oxidation of lipoproteins, giving rise to hydroperoxides, lysophospholipids, oxysterols, and aldehydic disruption products of fatty acids and phospholipids. But further modification like fusion of lipoproteins, proteolysis, lipolytic humiliation and glycation are well known 25.Such modified lipoproteins or particles of the modification process have incitive potential and trigger a topical anesthetic incitive response responsible for signaling subsequent steps in the atherogenesis. It includes a further increased endothelial dysfunction, which may cause a vicious circle of LDL accumulation, and activation of various cell types 24, 26, 27.(3) Migration of Monocytes and chemise into Macrophages/Foam CellsMore important, the unhealthy response induces migration of leukocytes such(prenominal) as monocytes or lymphocytes into the lesion. Leukocytes are attracted by chemoattractant factors including modified lipoprotein particles themselves and chemoattractant cytokines depicted by the smaller spheres, such as the chemokine monocyte chemoattractant protein-1, interleukin 1 (IL-1) or tumor necrosis factor of import (TNF-) produced by vascular wall cells in response to the inflammatory process REF. The activated arterial endothelial cells express a number of adhesion molecules and receptors on their show, which participate in the recruitment of leukocytes from the blood to the nascent lesion REF.Macrophages are a key p forge in atherogenesis 27. They develop from recruited monocytes, which migrated as described above into the lesion. In the mediator bear on process of maturation, those macrophages become lipid-laden coruscate cells by uptake of lipoprotein particles through receptor-mediated endocytosis REF. The accumulation of lipid in the macrophages results in the apoptosis and necrosis, which lead first to a boosted expression and secretion of inflammatory cytokines and second to a rout of their lipid excess into a necrotic lipid-core REF. Macrophages further produce enzymes, such as metalloproteinases, that degrade the extracellular intercellular substance and lead to instability of plaques REF.(4) Adhesion of platelets and Release of SMC activating factorsThe inflammatory process, especially triggered by the necrosis of the foam cells, microscopic b slide byes in endothelial oneness may occur. Platelets adhere to such places of limited endothelial denudation owing to exposure of the thrombogenic extracellular matrix of the underlying basement membrane and form microthrombi. Although most of the arterial mural microthrombi resolve without any clinical ma nifestation, they lead indirectly to lesion progression by pro-fibrotic stimulation REF. The platelets, activated by adhesion, release numerous factors that promote a fibrotic response, including platelet-derived growth factor (PDGF), fibroblast growth factor (FGF), insulin-like growth factor 1 (IGF-1), and transforming growth factor alpha (TGF-) 28-30. Thrombin itself generates fibrin that has a pro-fibrotic stimulus 28.(5) Migration and Proliferation of SMCsThe pro-fibrotic response includes first the migration of SMC from the media of the arterial wall, through the internal elastic membrane, and the accumulation within the expanding intima of the arterial wall. Second, stimulate the proliferation of SMC, which is responsible to form the pouch of the advanced lesion. Another part of the advanced lesions is an increased extracellular matrix. TGF- and other mediators stimulate the interstitial collagen production by SMC. These mediators may arise not only from neighboring endotheli al cells or leukocytes (a paracrine pathway) but also from the similar cell that responds to the factor (an autocrine pathway). Together, these alterations in quiet-muscle cells, signaled by these mediators acting at on the spur of the moment distances, can accelerate work shift of the early lesion (fatty streak) into a more fibrous SMC and extracellular matrix-rich plaque.(6) Enhanced accumulation of lipids, collagen and proteoglycansThe formation of a complex atherosclerotic lesion is characteristic by an extent remodeling process. Further foam cells within the expanding intimal lesion perish, while they phagocytose more and more lipids. The fibrotic cap between the so arisen lipid-rich necrotic core and the vascular lumen may vary in oppressiveness and admits the classification of thin cap fibroatheroma, which correlates with a higher risk for vivid luminal thrombosis REF. The production of extracellular matrix, as well plaque ontogenesis and complication can be stimulated by diverse growth factors or cytokines like IL-1 or TNF-, and can be inhibited by other cytokines (e.g. interferon alpha (IFN-)) REF.As atherosclerotic plaques advance, they show intimal arterial calcification REF. The akin proteins, which can be found in bone, are also localize in atherosclerotic lesions, e.g., osteocalcin, osteopontin, and bone morphogenetic proteins 31. Both, passive and active models are discussed for the development calcification 32. SMC can, promoted by several cytokines (e.g. transcription core binding factor 1), acquire osteoblast-like characteristics and secrete bone matrix 33.These examples illustrate how the pathogenesis of atherosclerosis involves a complex mix of mediators that in the balance determines the characteristics of particular lesions REF.3.1.1.2 The Role of upheavalThe grapheme of inflammation is central, while those inflammatory mechanisms mediate initiation, progression, and the complications of atherosclerotic lesions 26, 34. by means of the inflammatory process, arterial endothelial cells begin to express on their bob up selective adhesion molecules that bind various classes of leukocytes, especially monocyte and T lymphocyte which are found in early human and experimental atheroma REF. by and by monocytes adhere to the endothelium, they can first migrate in the intima, largely stimulated by chemokines and second transform into macrophages and avidly engulf lipoproteins, largely oxidise LDL REF. Although the phagocytosis of potentially harmful lipid particles by macrophages and subsequently the transformation into foam cells has an initially protective, this process involves further expression and secretion of inflammatory chemokines like Interleukin (IL)-1, Monocyte Chemotactic Protein (MCP)-1 or Tumor Necrosis Factor (TNF)-. Those enhance the inflammatory reaction and enable the further migration of leukocytes into the lesion REF. Macrophages also produce toxic atomic number 8 species that cause additiona l oxidation of the LDL in the lesions, and they elaborate growth factors that may contribute to SMC proliferation REF. Similary, T lymphocytes (both CD4+ and CD8+) are also recruited to the intima by chemo-attractants. Cross-talk between macrophages and T cells induces a chronic inflammatory state regarding cellular and humoral immune activation characteristics.This state of a chronic inflammation leads also to the next observed steps in the development and progression of atherosclerosis. Thus, it stimulates the migration and proliferation of smooth muscle cells (SMC), as well the proliferation of vascular endothelial cells in the lesion. finished fibrogenic mediators, released from activated leukocytes and inherent arterial cells, the replication of SMCs is getting enhanced and contributes to expanding upon by these cells of a dense extracellular matrix characteristic of the more advanced atherosclerotic lesion.3.1.1.3 Vasa Vasorum and Neo-AngiogenesisThe vasa vasorum of the aor ta is as a plexus in the wall of artery of microvessels, which are functional endarteries 35, 36. They either get down from major branches, originate from the main lumen of the aorta or drain in concomitant veins 37. These vessels allow the humoral communication between intravascular lumen, vessel wall and adventitial layer of large arteries including oxygen and nutrients tack REF.Several studies demonstrated that hypoxia 38, cytokines (e.g. vascular endothelial growth factor) 39, 40, pro-angiogenic factors (e.g. hypertension or hypercholesterolemia) stimulate the growth of the vasa vasorum 41. Those increased microvascular mesh topology may contribute to inflammation and lesion complications in several ways. First, the vasa vasorum provides an abundant surface area for leukocytes trafficking and may serve as the portal of entry and wall socket of white blood cells from the established atheroma.Microvessels in the plaques may also cede foci for intraplaque phlebotomise. Like t he neovessels in the diabetic retina, microvessels in the atheroma may be crumbly and prone to rupture and can produce focal hemorrhage. Such a vascular leak leads to thrombosis in situ and thrombin generation from prothrombin. In addition to its role in blood coagulation, thrombin can modulate many aspects of vascular cell function, as described above. Atherosclerotic plaques matter-of-factly contain fibrin and hemosiderin, an indication that episodes of intraplaque hemorrhage contribute to plaque complications.Multiple and frequently competing signals regulate these various cellular events. Increasingly, we appreciate links between atherogenic risk factors, inflammation, and the altered behavior of intrinsic vascular wall cells and infiltrating leukocytes that underlie the complex pathogenesis of these lesions.The present data head that vasa vasorum neoangiogenesis and atherosclerosis are seemingly inseparably linked, triggered and perpetuated by inflammatory reactions within the vascular wall.3.1.1.4 Risk Factors for Development of AtherosclerosisLocal shear seek In the coronary circulation, for example, the proximal left anterior come down coronary artery exhibits a particular predilection for developing atherosclerotic disease. Likewise, atherosclerosis preferentially affects the proximal portions of the renal arteries and, in the extracranial circulation to the brain, the carotid bifurcation. Indeed, atherosclerotic lesions oft form at branching points of arteries, regions of disturbed blood flow.Age, Gender, HTN, HLP, DM, Smoking, Race/Ethnicity,3.1.1.5 Atherosclerosis of the AortaIn the characteristic distribution of atherosclerotic plaques in humans the abdominal muscle aorta (Fig. 11-8) is usually much more involved than the pectoral aorta, and lesions tend to be much more prominent around the origins (ostia) of major branches. In descending order (after the lower abdominal aorta), the most heavily involved vessels are the coronary arterie s, the popliteal arteries, the internal carotid arteries, and the vessels of the circle of Willis. Vessels of the upper extremities are usually spared, as are the mesenteric and renal arteries, except at their ostia. Nevertheless, in an individual case, the severity of atherosclerosis in one artery does not predict the severity in another. In an individual, and indeed within a particular artery, lesions at various stages often coexist.2009_Dijk_The natural accounting of aortic atherosclerosis_A systematic histopathological evaluation of the peri-renal region.pdf3.1.2 fringy Arterial DiseasePeripheral Arterial Disease (PAD) is caused by atherosclerosis and represents the most common cause of lower extremity ischemic syndromes in developed countries 42. Symptoms of PAD are variable including pain, ache, hair loss, thickened nails, smooth and shiny uncase, reduced skin temperature, cramp, muscle atrophy, or a sense of fatigue in the muscles. Because of the disagreement of symptoms, the diagnosis of PDA is frequently missed 43. In addition, the major part of patients with PAD is asymptomatic REF.Beside these diagnostic challenges, PAD affects a large and increasing numbers of patients worldwide. Round 30 million people are morbid in worldwide, but of those only 10 million patients are presenting with symptoms 44. Further, the preponderance is increasing with age 6, 45, while the prevalence is 10% at the age of 60 years 46.Association to mortality3.1.2.1 Pathogenesis of Peripheral Artery DiseaseThe leading cause of PAD is atherosclerosis, especially in older patients (40 years) and at the lower extremities 42. Other, but rare causes of PAD include embolism, vasculitis, fibromuscular dysplasia, entrapment, and trauma.Atherosclerotic lesions, which are segmental and cause stenosis, are usually localized to large and medium-sized vessels. The pathology of these lesions is base on atherosclerotic plaques development, as described above (xxx). The primary sites o f closeness are the abdominal aorta and iliac arteries (30% of symptomatic patients), the femoral and popliteal arteries (80-90%), and the more distal arteries (40-50%) REF. Atherosclerotic lesions have been predominantly observed at arterial branch points. These may be explained by altered shear filtrate REF. However, the involvement of the distal and smaller arteries is more common in remote individuals and patients with diabetes mellitus REF.3.1.2.2 Risk Factors for Peripheral Arterial DiseaseWhile atherosclerosis is the major underlying condition of PAD, the risk factors for PAD are essentially the resembling as those for other form of atherosclerosis (like e.g. CAD), see Table 1 47-50. However, the risk factors smoking and diabetes may have even greater final result for PAD as compared for CAD 51.Risk FactorsIncreased risk for PADHypercholesterolemia1- to 2-fold (low)Homocysteinemia1- to 3-fold (moderate)Hypertension1- to 3-fold (moderate)Smoking (current and past)2- to 4- fold (high)Diabetes mellitus2- to 4-fold (high)Table 1 Risk Factors for Peripheral Arterial Disease3.1.2.3 Clinical Presentation of Peripheral Artery DiseasePAD affects more often the lower extremities (xx times more often than upper extremities) REF. The most common symptom of PAD is intermittent claudication, which is defined as presence of pain, ache, cramp, numbness, or a sense of fatigue in the muscles. Those symptoms occur during exercise and are relieved by consist, as result of the increased muscle ischemia during exercise caused by obstruction to arterial flow.Patients with PAD in the lower extremities resulting in ischemia may undulate in presentation from no symptoms to limb-threatening gangrene. Two major classifications base on the clinical presentations are established, the Fontaine and the Rutherford classification.While the more simple Fontaine classification consists of quartet stages (Table 2) 52, the Rutherford classification has four grades (0- cardinal) and seven categories (0-6). well patients are classified into Rutherford division 0. Any patient with claudicants are stratified into Rutherford grade I and divided into three categories based on the severity of the symptoms. If patients have pain at rest, they belong to Rutherford grade II and category 4. Any patient with waver paper loss are classified into Rutherford grade III and categories 5 and 6, based on the significance of the create from raw stuff loss 4. These two clinical classifications can be translated into each other according to Table 2.Fontaine salmagundiRutherford ClassificationStageClinicalGradeCategoryClinicalIAsymptomatic00AsymptomaticIIaMild claudicationI1Mild claudicationIIbModerate to severe claudicationI2Moderate claudicationI3Severe claudicationIIIIschemic rest painII4Ischemic rest painIVUlceration or gangreneIII5Minor tissue lossIII6Major tissue lossTable 2 Classification of Peripheral Arterial Disease based on the Fontaine Classification in Comparison t he Rutherford ClassificationIn the Framingham Offspring determine, the prevalence of PAD was determined in 1554 males and 1759 females from 1995 to 1998.55 The mean age was 59 years. PAD, defined as an ankle-brachial (blood pressure) index (ABI) of ABI Severity of PADThe mendelevium also queried the participant about symptoms of intermittent claudication using a standardized questionnaire 53.3.2 Local adipose create from raw stuff Depots 3.2.1 Variability of fat create from raw material 3.2.1.1 Anatomy and MorphologySACK Epicardial, mesenteric, and omental fat all share the same origin from the splanchnopleuric mesoderm associated with the gut.11Pericardial fat (pericardial adipose tissue PAT) is defined as epicardial fat in all these possible locations plus paracardial fat.14 Paracardial fat is situated on the external surface of the parietal pericardium within the mediastinum and has instead been termed mediastinal fat.15Paracardial fat originates from the primitive thoraci c mesenchyme, which splits to form the parietal (fibrous) pericardium and the outer thoracic wall.16 Epicardial adipose tissue is supplied by branches of the coronary arteries, whereas paracardial fat is supplied from different sources including the pericardiacophrenic artery, a branch of the internal mammary.17 Lipolysis and lipogenesis have not been measured directly in human epicardial fat. Based on approximately 2-fold higher rates of lipolysis and lipogenesis in guineapig epicardial fat than other fat depots, Marchington et al18,19 proposed that EAT serves to capture and store intravascular renounce fatty acid (FFA) to protect cardiomyocytes from exposure to excessive coronary arterial FFA concentrations during increased energy intake and, at other times, to release FFA as an immediate ATP source for the myocardium during periods of need. Epicardial fat and the myocardium are contiguous. Islands of mature adipocytes are more frequent within the subepicardial myocardium of the RV than the LV13 and may act as more readily available, direct sources of FFA for cardiomyocytes.The thickness of the wall of the right atrium is about 2 mm the left atrium, 3 to 5 mm the RV, 3 to 5 mm and the LV, 13 to 15 mm.20 Possibly, FFAs could diffusebidirectionally in interstitial swimming across concentration gradients from epicardial fat into the atrial and RV walls where EAT predominates and depravity versa, but this process in the LV wall can be questioned because the diffusion distance is much longer.Peri-vascular adipose tissue is defined as any adipocytes, which are located close to the vascular wall and has the mishap to secret their biomarkers into the vasa vasora of the wall (see 3.2.1.2).3.2.1.2 Secretion of Biomarkers by Adipose TissueAdipose tissue is known to have more functions than lipid storing. Adipose tissue secrets biomarkers and serves as an endocrine organ. Beside hormones, it secrets also different inflammatory cytokines and chemokines. The amount of adipose tissue were associated to xxx, xxx, xxx (FRAMINGHAM?). Especially peri-vascular adipose tissue like epicardial or visceral adipose tissue demonstrated higher expression of inflammatory biomarkers compared to other adipose tissue depots in the body REF.Beside the systemic effect of the secreted cytokines and chemokines, also a local effect/paracrine is hypothesied. Biomarkers secreted of peri-vascular adipose tissue reach over the vasa vasora of the major arteries their adventitia, media, and intima. Therefore it might be involved in the inflammatory process of atherosclerotic plaque. Further, a local effect can be thought by direct diffusion.3.2.2 Association of Adipose Tissue to Cardiovascular Disease 3.2.2.1 Atherosclerosis 3.2.2.2 Peripheral Arterial Disease 3.2.3 In-Vivo Assessmentof Adipose Tissue 3.2.3.1 Traditional Measures* BMI and WC 543.2.3.2 Imaging-based Assessment* dual energy X-ray absorptiometry (DXA) 55* charismatic resonance imaging (MRI) 56, 57* ultrasound 58* multi-detector computed tomography (MDCT) 59, 603.3 Framingham Heart battleground 3.3.1 historic Origin of the Framingham Heart StudyInfectious diseases were prior to World contend II the major burden for public health. But through a greater microbiological knowledge and improved sanitation, the morbidity and mortality of infectious disease decreased continuously. When penicillin was introduced in 1942, a dramatic reduction was made in the prevalence and incidence of infectious diseases, especially by controlling terabit and pneumococcal pneumonia REF.Replacing infectious diseases, public health was challenged by a mounting epidemic of CVD starting in the 1940s. With World War II over the alarming rise of CVD became increasingly evident. In the United States, 30% of all men developed CVD before reaching the age sixty. The prevalence of CVD was twice of cancer by 1950 and had become the leading cause of death REF. Even so the available statistic data from around the world was often crude and inaccurate, it clearly demonstrated a worldwide atherosclerotic CVD problem.moreover there was no known treatment to prolong life and to reduce mortality. Added to these distresses was the fact that little was known about etiology, pathogenesis and epidemiology of CVD.The big gap between the enormous public health burden of CVD on the one site and the little understanding of this disease on the other site increased drastically the need for action. At this time, some believed a primary antifertility blast was more promising than a search for cures Dawber, Thomas R. (1980), The Framingham Study The Epidemiology of Atherosclerotic Disease, Cambridge, Mass. Harvard University Press., while the secrets of the etiology of CVD and subsequently for treatment were not organism uncovered by basic laboratory and clinical research. Some of these prevention-minded individuals in use(p) positions of influence and were able to translate their beliefs into actions.The key was to develop a impediment approach, where first of all the characteristics of the host and environment, which lead to the early appearance of the disease, had to be determined. In particular, preventable or modifiable predisposing factors had to be identified. If a practical preventive approach was developed, the hope was that doctors and public health officials would adopt it and so have a widespread impact on the reduction of CVD-based morbidity and mortality.Accordingly to the preventive approach, the Framingham Heart Study was designed given the pluck to identify these modifiable characteristics of host and environment for CVD.3.3.2 Initiation of the Framingham Heart StudyBy the mid 1940s several striking studies were conducted with an examples epidemiological approach in the fields of nutritional imbalance, metabolic disorders, occupational hazards, accidents, cancer and run-down fever under principle investigators (PI) Drs. Dawber, Meadors and Moore REF, Dawber, Meadors and M oore 1951. In common, an association between the raft and the disease could be identified with-out knowledge of the precise etiology.One of those studies was performed by Dr. John Snow in 1936. He demonstrated that cut-ting off the water supply from contaminated wells, despite incomplete knowledge of the pathogenesis of the disease, stopped cholera. He observed on the one hand the source of the water supply and on the other hand the time and place where the disease occurred. He sufficiently pinpointed based on his observations the major environmental factor for cholera. Further investi
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