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The effect of thrombolytric drugs on cardiac enzymes, Creatine Phospho kinase and Creatine Kinase -MB, in myocardial Infarction”
“The effect of thrombolytric drugs on cardiac enzymes, Creatine Phospho kinase and Creatine Kinase -MB, in myocardial Infarction”.
MYOCARDIAL INFARCTION
Myocardial infarction refers to a dynamic process by which one or more regions of the heart muscle experience a severe and prolonged decrease in oxygen supply because of insufficient coronary blood of subsequently, necrosis or death to the myocardial tissue occurs.
The onset of the myocardial infarction process may be sudden or gradual and the progression of the event to complete takes approximately 3 to 6 hours.
PREVALENCE
Myocardial infarction is the leading cause of death in the United States (US) as well as in most industrialized nations throughout the world. Approximately 800,000 people in the US are affected and in spite of a better awareness of presenting symptoms, 250,000 die prior to presentation to a hospital.4 The survival rate for US patients hospitalized with MI is approximately 90% to 95%. This represents a significant improvement in survival and is related to improvements in emergency medical response and treatment strategies.
In general, MI can occur at any age, but its incidence rises with age. The actual incidence is dependent upon predisposing risk factors for atherosclerosis, which are discussed below. Approximately 50% of all MI’s in the US occur in people younger than 65 years of age. However, in the future, as demographics shift and the mean age of the population increases, a larger percentage of patients presenting with MI will be older than 65 years.
Men are more susceptible than women, but the risk is more in female than in male after menopause.
CORONARY ARTERIES
The coronary arteries supply the capillaries of the myocardium with blood
The right coronary artery (RCA) supplies the right atrium and ventricle, the inferior portion of the left ventricle, the posterior septal wall and the SA and AV nodes
The left coronary artery (LCA) consists of two major branchiate left anterior descending (LAD) and the circumflex (LCX).
The LAD artery supplies below the anterior wall of the left ventricle, anterior ventricular septum and the apex of the left ventricle.
The LCX artery supplies blood to the lateral and posterior surfaces of the left ventricle.
CARDIAC ENZYMES
Levels of cardiac markers rise overtime. Hence, enzymes are drawn in a serial pattern usually on admission and over 6-24 hrs until 3 samples are obtained.
Enzymes commonly evaluated include CK, CKMB, LDH, TroponinT & I.
CK-MB ratio indicates the extent of damage of the cardiac muscle. The more the ratio, the more the damage of the cardiac muscle. Troponins are preferred markers of myocardial injury or they are very cardiac specific & are thought to rise before permanent injury develops.
Increased troponin concentrations should not be used by themselves to rule out a heart attack. Troponin will remain high for 1–2 weeks following MI allowing easy diagnosis if patient presents late with an old MI as other CE’s will not be raised unless reinfarction occurs.
Elevation of Cardiac Enzymes in Myocardial Infarction
Enzyme Rises in Peaks in Normalizes in Normal Value CKMB ratio
CK 12 hrs 16-30hrs 3-5 days 35-232IU/L
CKMB 4-8 hrs 24 hrs 72 hrs < 51IU/L <6%
Troponin I 3-6 hrs 20 hrs 14 days 0.0-0.4 ng/ml
Troponin T 2-4 hrs 8-12 hrs 14 days 0.0-0.1 ng/ml
LDH 12 hrs 12-24 hrs 10 days 100-190 IU/L
PATHOPHYSIOLOGY
The most common sites of MI are in the left ventricle, the chamber of heart which has the greatest work load. Tissue changes that occur in the myocardium are related to the extent to which the cells have been deprived of oxygen. Total deprivation results in an area of infarction in which the cells die and the tissue become necrotic.
Necrosis in this area is evident with in 5 to 6 hours after the occlusion. In response to this necrosis the body increases its products of leukocytes, which aid in the removal of dead cells. As collateral circulation enlarges, it brings fibroblasts, which form a connective tissue scar with in the area of infarction. Usually, the formation of fibrous scar tissue is complete with in 2 to 3 months.
Immediately surrounding the area of infarction is a less seriously damaged area of injury. It may deteriorate and thus extend the area of infarction or with adequate collateral circulation; it may regain its function with in 2 weeks.
The outer most area of damage is the zone of ischemia which borders the area of injury. The cells in this area are weakened by decreased oxygen supply, but function can return usually with in 2 to 3 weeks after the onset of occlusion.
RISK FACTORS
There are two types of risk factors for heart attack, including
- Inherited factors
- Acquired factors
Inherited factors
These are risk factors you are born with that cannot be changed, but can be improved with medical management and life style changes. Following are most at risk-
- persons with inherited hypertension
- persons with inherited low levels of HDL or high levels of LDL
- persons with a family history of heart disease aging men and women
- persons with diabetes mellitus [ type 1 diabetes ]
- women, after the onset of menopause- generally, men are at risk, at an earlier age than women, but after the onset women are equally at risk
Acquired factors
These are risk factors that are caused by activities that we choose to include in our lives that can be managed through life style changes and clinical care. Following are most at risk-
- Persons with acquired hypertension
- persons with acquired low level of HDL or high level of LDL
- cigarette smokers
- people who are under a lot of stress
- individual who lives a sedentary life
- persons overweight by 30 % or more
TYPE OF MYOCARDIAL INFARCTION
1. Different degrees of damage occurs to the heart muscle-
Zone of necrosis: death to the heart muscle caused by extensive and complete oxygen deprivation that is, irreversible damage
Zone of injury: region of heart muscle surrounding the area of necrosis; inflamed and injured, but still viable if adequate oxygen can be restored.
Zone of ischemia: region of the heart muscle surrounding the area of injury, which is ischemic and viable; not endangered unless extension of the infarction occurs.
2. According to the layers of the heart muscle involved, MI can be classified as-
Transmural or Q wave infarction; area of necrosis occurs throughout the thickness of the heart muscle. Subendocardial or non transmural infarction; area of necrosis is confined to the innermost layer of the heart muscle.
3. Location of the MI is identified as location of the damaged heart muscle within the left ventricle inferior, anterior, lateral and posterior-
Left ventricle is the most common and dangerous location for MI, as it is the main pumping chamber of the heart
Right ventricular infarction commonly occurs I junction with damage to the inferior and or posterior wall of the left ventricle
4. Region of the heart muscle that becomes damaged determine by the coronary artery that becomes obstructed
Left main coronary artery
Circumflex branch
Anterior ascending branch
Great cardiac vein
Middle cardiac vein
Right cardiac vein
CLINICAL MANIFESTATIONS
1) Chest pain
- not relieved by the rest over sublingual vasodilator therapy
- severe steady sub sternal chest pain of a crushing and squeezing nature
- may radiate to the arms, neck, jaw and shoulders
- continuous more than 15 minutes
- may produce anxiety and fear
2) Diaphoresis
3) Hypertension or hypotension
4) Bradycardia or tachycardia
5) Palpitation, severe anxiety, dyspnea
6) Disorientation, confusion and restlessness
7) Fainting, marked weakness
8) Nausea, vomiting, hiccoughs
9) Atypical symptoms such as epigastric pain abdominal distress, dull aching or tingling sensation, shortness of breath, extensive fatigue
DIGNOSTIC EVALUATION
1. ECG changes
Generally occur within 2 – 12 hours, but may take 72 – 96 hours.
Necrotic, injured and ischemic tissue alter ventricular depolarization and repolarization
ST segment depression and T wave inversion indicate a pattern of ischemia
ST elevation indicates an injury pattern
- Anterior small V3 – V4 leads
- Anterior extensive V2 – V5 leads
- Anteroseptal V1- V3 leads
- Posterior V1 – V2 leads, progressive R wave and ST depression
- Anterolateral V4 – V6, I, Avl leads
- Apical V5 – V6 leads
- Inferior lead ii, iii and avf [ reciprocal ]
2. Elevation of serum enzymes and isoenzymes:
Enzymes are drawn in a serial pattern usually on admission and every 6 – 24 hours until 3 samples are obtained. Enzyme activity then is correlated to the extent of heart muscle damage
Enzymes commonly evaluated include are CK, LDH, CK-MB, AST, Troponin I, Troponin T. [Fig.4 ]
LDH 2 is normally greater than LDH 1 except when the heart muscle is damaged a reversal occurs
3. Other findings:
White blood cell count and sedimentation rate elevates due to inflammatory process associated with damaged heart muscle.
Radionuclide imaging allows recognition of areas of decreased perfusion
Position emission tomography determines the presence of reversible heart muscle injury and irreversible or necrotic tissue, extends to which the injured heart muscle has responded to treatment also can be determined
MANAGEMENT
Therapy is aimed at the protection of ischemic and injured heart tissue to preserve muscle function, reduce the infarct size, and prevent death. Innovative modalities provide early restoration of coronary blood flow , and the use of pharmacologic agents improve oxygen supply and demand, reduce and/or prevent disarrhythmias, and inhibit the progression of coronary artery disease.
1. Opiate analgesic therapy: Morphine is used to relieve pain, improve cardiac hemodynamics by reducing preload and after load and to relieve anxiety.
Meperidine [Demerol] is useful for pain management in those patients contraindicated to morphine or sensitivity to respiratory depression.
2. Anxiolytic agents: Benzodiazepines are used with analgesics when anxiety complicates chest pain and its relief
3. Antiplatelet agents: Aspirin interfere with the function of the enzyme cyclooxygenase and inhibits the formation of thromboxane A2. Within minutes aspirin prevents additional platelet activation and interferes with platelet adhesion and cohesion
Other antiplatelet agents are, Clopidogrel, Ticlopidine, Dipyridamole, these agents, specifically Clopidogrel may be useful for patients who have a true allergy to aspirin and some times can be used with combination with Aspirin.
4. Supplemental oxygen: Supplemental oxygen should be administered. The rationale for use is the assurance that erythrocytes will be saturated to maximum carrying capacity. Because MI impairs the circulatory function of the heart, oxygen extraction by the heart and by other tissue may be diminished.
5. Nitrates: Intravenous Nitrates should be administered in MI, persistent ischemia, hypertension or large anterior wall MI. Nitrates are metabolized to nitric oxide in the vascular endothelium. Nitric oxide relaxes vascular smooth muscle and dilates the blood vessel lumen. Vasodilatation reduces both cardiac preload and after load, and decreases the myocardial oxygen requirements. Vasodilatation of the coronary arteries improves the blood flow through the partially obstructed vessels as well as through collateral vessels. When administered sublingually or intravenously, Nitroglycerin has a rapid onset of action.
6. Beta adrenergic blocking agents: Beta blockers are recommended within 12 hours of MI symptoms and are continued indefinitely. Beta blockers decrease the rate and force of myocardial contraction and decreases overall myocardial oxygen demand. During the acute phase of MI beta blockers may be initiated intravenously
7. Heparin: Unfractionated Heparin: intravenous unfractionated Heparin is recommended who undergo percutaneous revascularization. It is also recommended in patients who receive fibrinolytic therapy and non selective fibrinolytic agents such as urokinase, streptokinase and anistreplace. Heparin inhibits the additional formation and propagation of thrombi, effective when administered intravenous or subcutaneously.
Low-molecular-weight-Heparin: can be administered to MI clients not treated with fibrinolytic therapy
8. Fibrinolytic or Thrombolytic agents: Fibrinolytic therapy is indicated with ST segment elevation. Plasminogen activators restore coronary vessels by dissolving obstructing thrombus. The plasminogen activators have been shown to restore coronary blood flow in 50% to 80% of MI patients. The successful use of fibrinolytic agents provides a definite survival benefit that is maintained for years. Reteplase has been shown to produce slightly higher 60- and 90-minute angiographic patency rates than accelerated alteplase, while adverse-event rates were equal.
However, the better early patency rate did not translate into any survival advantage at 30 days follow-up. The most critical variable in achieving successful fibrinolysis is time from symptom onset to drug administration. A fibrinolytic is most effective when the “door-to-needle” time is 30 minutes or less.
9. Angiotensin converting enzyme inhibitors: Oral ACEI are recommended within the first 24 hours of the onset of the MI symptoms, decreases myocardial after load through vasodilatation.
10. Anti dysarrhythmic agents: Lidocaine decreases ventricular irritability, which commonly occurs post MI.
11. Calcium channel blockers: Improves the balance between the oxygen supply and demand by decreasing heart rate, blood pressure and dilating coronary vessels.
Diltiazem has been shown to decrease the incidence of reinfarction in patients with non-Q-Wave MIs.
12. Percutaneous Coronary Intervention [Fig-15]: Mechanical opening of the coronary vessel can be performed during an evolving infarction. A balloon tipped catheter is introduced through a guide wire into a coronary vessel with a non calcified atheromatous lesion. The balloon of the catheter is the inflated, causing disruption of the intima and changes in the atheroma. The result is an increase in the diameter of the lumen of the coronary vessel and improvement of blood flow below the lesion.
Percutaneous coronary intervention is an alternative therapy to fibrinolysis Restoration of coronary blood flow in a MI can be accomplished mechanically by percutaneous coronary intervention (PCI). Mechanical revascularization by PCI is used as a primary therapy as an alternative to fibrinolysis when fibrinolysis is not clearly indicated or contraindicated. PCI can successfully restore coronary blood flow in 90% to 95% of MI patients.
13. Surgical Revascularization: Emergent or urgent coronary artery bypass graft surgery is warranted in the setting of failed percutaneous intervention in patients with hemodynamic instability and coronary anatomy amenable to surgical grafting. Surgical revascularization is also indicated in the setting of mechanical complications of MI such as ventricular septal defect, free wall rupture, or acute mitral regurgitation. Restoration of coronary blood flow with emergency Coronary Artery Bypass Grafting (CABG) can limit myocardial injury and cell death if it is performed within 2 or 3 hours of symptom onset. Emergency CABG carries a higher risk of perioperative morbidity (bleeding and MI extension) and mortality than elective CABG. The risk of operative mortality during emergency CABG is increased in patients, who are in cardiogenic shock, those with previous CABG surgery, and with multi-vessel disease. On the other hand, urgent CABG confers a survival benefit in patients with recurrent ischemia post-MI whose coronary anatomy is unsuitable for complete revascularization with PCI. Elective CABG improves survival in post-MI patients who have left main artery disease, three-vessel disease, or two-vessel disease that is not amenable to PCI. The timing of elective CABG post-MI is controversial, but retrospective studies indicate that when CABG is performed as early as 3 to 7 days post-MI, operative mortality is equivalent to CABG performed on non-MI patients.
14. Cardiac Stress Testing: Cardiac stress testing post-MI has established value in risk stratification and assessment of functional capacity. Stress testing is not recommended within several days post-MI. Only sub-maximal stress tests should be performed in stable patients 4 to 7 days after MI. Exercise testing identifies patients with residual ischemia for additional efforts at revascularization. Exercise testing also provides prognostic information and acts as a guide for post-MI exercise prescription and cardiac rehabilitation.
15. Lipid Management: All post-MI patients should be on an American Heart Association Step II diet (< 200 mg cholesterol/day, < 7% of total calories from saturated fats). Post-MI patients with LDL-cholesterol levels > 100 mg/dL on a Step II diet are recommended to be on drug therapy to lower LDL-cholesterol levels < 100 mg/dL. Post-MI patients with HDL-cholesterol levels < 35 mg/dL on a Step II diet are recommended to participate in a regular exercise program and on drug therapy designed to increase HDL-cholesterol levels.4 Recent data indicate the all MI patients should be on statin therapy, regardless of lipid levels or diet
16. Long-term Medications: Most oral medications instituted in the hospital at the time of MI will be continued long-term. Therapy with aspirin and beta-blockade is continued indefinitely in all patients. ACEI is continued indefinitely in patients with congestive heart failure, left ventricular dysfunction (ejection fraction < 0.40), hypertension, or diabetes. A lipid-lowering agent, specifically a statin, in addition to dietary modification is continued indefinitely
17. Cardiac Rehabilitation: Cardiac rehabilitation provides a venue for continued education, re-enforcement of lifestyle modification, and adherence to a comprehensive prescription of therapies for recovery from MI, which includes exercise training. Participation in cardiac rehabilitation programs post-MI is associated with a decrease in subsequent cardiac morbidity and mortality. Other benefits include improvement in quality of life, functional capacity and social support. A minority of post-MI patients actually participate in formal cardiac rehabilitation programs due to either lack of structured programs, physician referrals, low patient motivation, non-compliance, or financial constraints.
NEED FOR THE STUDY
Reperfusion therapy, within which we include thrombolytic therapy and percutaneous coronary intervention (PCI), which includes angioplasty and stent placement, is the greatest advance in the treatment of acute myocardial infarction
Studies have shown that many patients with AMI who are eligible for reperfusion therapy do not receive it. Moreover, of those who do receive it, the time to administration of thrombolytic therapy, or “door-to-needle time” is often delayed, jeopardizing myocardium and leading to greater morbidity and mortality.
Clinical criteria and simple ECG parameters have limited value for the non-invasive diagnosis of myocardial reperfusion. Other methods, such as ST segment monitoring and kinetic analysis of biochemical markers, may also be value of in early identification of IRA {Infarct Related Artery}, total CK activity, CK-MB isoenzymes appear to be the most promising biochemical markers.
In addition, the thresholds suggested for the diagnosis of reperfusion were generally derived from “time-to-peak” values. This rules out early diagnosis because peak CK plasma values are reached, on averages 9 -+ 6 hours after thrombolysis.
Determination of plasma total and MB CK concentration provides accuracy superior to any other currently available method for the diagnosis of acute MI.
In addition to providing precise diagnosis of acute MI, quantitative MB CK assays can also be used to obtain an accurate estimate of infarct size. In recent years, accuracy in the diagnosis of acute MI has assumed even greater importance, since the choice and timing of a variety of diagnostic and therapeutic options following coronary care unit admission hinge on whether infarction has occurred. Furthermore, the advent of thrombolytic therapy of acute MI has emphasized the need for more sensitive biochemical markers of necrosis in the first hours. The eventual realization that the reestablishment of blood flow was the dominant mechanism for the diminution of infarct size led to a therapeutic approach dominated by thrombolysis and more literally by the use of interventions to open vessels and maintain them open.
The key observation is that benefit by the use of a drug could be demonstrated if the drug was given prior to the period of ischemia.
Nevertheless, the greatest benefit in the management of patients with myocardial infarction ha unquestionably been the reestablishment of blood flow as early as possible after occlusion
The aim of this study is to determine the reperfusion of injury exacerbated by thrombolytic drugs in Myocardial Infarction through the process of elevation of cardiac enzymes which peaks and comes to normal levels within 24 hours, preventing prolonged injury and ischemia of myocardial tissue.
However, the aim was to evaluate prospectively biochemical markers for the diagnosis of coronary patency early after IV thrombolysis for Acute Myocardial Infarction.
STATEMENT OF THE PROBLEM
“The effect of thrombolytric drugs on cardiac enzymes, Creatine Phospho kinase and Creatine Kinase -MB, in myocardial Infarction”.
OBJECTIVES
- To evaluate the effect of thrombolytic drugs on cardiac enzymes.
- To compare the effect of thrombolytic drugs and non thrombolytic drugs on cardiac enzymes
- To determine the importance of thrombolytics for a patient with myocardial infarction
- To suggest teaching guidelines to public regarding early seeking of medical help at the onset of chest pain.
OPERATIONAL DEFIITIONS
Effect: Result or produce a result
Thrombolytic drugs: medications used to dissolve blood clots
CPK: A cardiac isoenzyme which releases into the blood in high levels when an injury occurs to the heart. It is also known as Creatine Kinase or Creatine Phophokinase.
CK-MB: It is also a cardiac isoenzyme releases into the blood from the heart muscle during an injury of the heart
Myocardial infarction: Necrosis of a region of the myocardium caused by an interruption in the supply of blood to the heart, usually as a result of occlusion of a coronary artery.
HYPOTHESIS
“Thrombolytic agents has effect on fall in peak levels on cardiac enzymes, CK and CK-MB”
LIMITATIONS
Coronary care unit: The data of this research is applicable in the settings of coronary care unit.
Age: Clients are selected only between 35 to 65 yrs of age.
Myocardial infarction: This is also applicable to the clients who were admitted in the hospital within 6 hours of the onset of the chest pain with myocardial infarction who received Inj. Metalyse.
Acute coronary syndrome: The clients who are admitted after 6 hours of the onset of the chest pain with acute coronary syndrome are included in the control group.
METHODOLOGY:
This study was done by an experimental method of research design in the settings of Coronary Care Unit in Dubai Hospital, U.A.E. A consecutive series of patients receiving IV Metalyse [ Tenecteplase ] for MI from May 2006 to November 2006 were included in this study.
RESEARCH DESIGN:
This study uses the comparative design.
THE SETTINGS:
This study was conducted in patients irrespective of age, sex and nationality, who were admitted in Coronary Care Unit through Emergency Department in Dubai Hospital, U.A.E.
SAMPLE SIZE:
This study included 60 clients, men and women, irrespective of nationalities, between 35 years to 65 years of age. Among 60 clients 30 were taken as experimental group and another 30 considered as control group.
SAMPLING TECHNIQUE:
The samples are selected as convenient sample, into two groups, the experimental and control groups. The clients who received thrombolytic agents within 6 hours of the onset of the chest pain are selected as an experimental group, and the clients who were presented late after 6 hours of the onset of the chest pain and not received thrombolytics, are selected as control group. All patients treated had the diagnosis of myocardial infarction confirmed by subsequent elevation of both Creatine Kinase [CK] and CK-MB isoenzymes levels. IV Metalyse is administered at a dose of 6000 units to 9000 units according to the weight of the patients. Patients with acute MI who were admitted to CCU more than 6 hours of onset of pain were also included.
DATA COLLECTION PROCEDURE:
Data for the study is collected by an instrument, which consists of 22 items including sample number, age, and sex. Religion, nationality, occupation, food habits, life style onset of chest pain, date and time of admission, signs and symptoms, vital signs, type of MI, protocol of thrombolytic therapy, levels of cardiac enzymes, post thrombolytic treatment, drugs received and date of discharge.
Study reveals that, majority of the clients who had MI was from the Indian subcontinents, constituting 63.3 % and the minority constituting just 1.6 %, from Great Briton and Turkey. 3.3 % of the clients were Egyptians and Syrians. Bangladeshis comprised, 6.6 % and Pakistanis were about 21.6 %. Only 9.9 % of the clients who had MI were Dubai Nationals. Among them 46.6% of the clients were aged between 46 – 55 years and 41.6 % of the clients were between 36 – 45 years and the remaining 11.6 % of the clients are between 56 – 65 years of age.
36.2 % of the clients had acute coronary syndrome and were not given thrombolytics. Remaining of the clients was with true MI and most of them were thrombolysed. However, all clients have undergone coronary angioplasty. Out of these clients only one client had normal coronary vessels, two were with mild coronary stenosis for conservative medical treatment and 4 clients with major triple vessel block were posted for CABG. Rest of the clients was treated with Percutaneous Coronary Angioplasty to LAD [50%], RCA [21.6%] and Circumflex [13.5%].
It is also evident from the study that most of the Indians are affected with MI and the major contributing factors are smoking, stress and lack of knowledge about the disease condition.
Based on Chi-Square deviation the association between normalization of cardiac enzymes levels in the study groups are as follows-
In Experimental group, 30 clients have received Inj. Metalyse . among them except 4 clients, remaining 26 clients reports seen that cardiac enzymes are normalized within 24 hours after the admission and administration of thrombolytic agent.
In control group, 30 clients blood reports for normalization of cardiac enzymes were anlysed, where we found 27 clients reports shown the higher levels of cardiac enzymes after 24 hours of the admission.
- Critical Value 14.56, P value < 0.05 and Null hypothesis rejected
Inj. Metalyse has a good effect on the cardiac muscle provided with Critical Value- 14.56, Probability Value- < 0.05, as evidenced by fall in peak levels of cardiac enzymes CK and CK-MB within 24 hours after received thrombolytic agent.
DISCUSSION
Tenecteplase [ Metalyse] is a recombinant fibrin-specific plasminogen activator. It binds to the fibrin component of the thrombus and selectively converts thrombus-bound plasminogen to plasmin, which degrades the fibrin matrix of the thrombus. Tenecteplase is cleared from the circulation by binding to specific receptors in the liver followed by catabolism to small peptides.
After single intravenous bolus injection of tenecteplase in patients with acute myocardial infarction, tenecteplase antigen exhibits biphasic elimination from plasma. There is no dose dependence of tenecteplase clearance in the therapeutic dose range.
The initial dominant half-life is 24+_5.5 [mean=/-SD] min. the terminal half-life is 129+_87 minutes, and plasma clearance is 119+_49 ml/min
The main finding of this study is the early peaking of the total CPK level and CK-MB
isoenzymes have identified with successful reperfusion after Metalyse therapy. The peak CPK levels reached in 12 hours and CK-MB levels were shifted in 6 hours. The study reveals that the cardiac enzymes levels peaked and normalized within 24 hours time in the experimental group who received Thrombolytic agents within 6 hours of the onset of the chest pain. Where as it took 3- 5 days for the enzyme levels to peak for clients in the control group, who did not receive thrombolytic agents due to late arrival to the hospital, resulting in more damage to the myocardium.
Thus, it is evident that the extent of injury to the myocardium as well as the oxygen demand is less in the experimental group of the clients.
Finally, it may be used as a surrogate end point for angiographic demonstration of
patency in future clinical studies of reperfusion therapy. Diagnostic performance improved when the analysis was restricted to patients treated >6 hours after the onset of symptoms.
CONCLUSION
Clinical studies of fibrinolytic therapy in myocardial infarction show, that early thrombolytic treatment starting within 6 hours of the onset of the chest pain, significantly decreases the risk of further damage of the myocardium and oxygen demand, by the process of fall in peak levels of cardiac enzyme levels within 24 hours.
Inj. Metalyse has early peaking of cardiac enzymes in experimental group reflect the Infarction Related Artery opened, the clot has dissolved by Inj. Metalyse which means we have good thrombolytic effect, that is why we have early peaking levels.
Early identification of patients with persistent occlusion after thrombolyis during
Acute Myocardial Infarction also is important because it can pave the way for rescue interventions such as rescue Percutaneous Transluminal Coronary Angioplasty or repeated thrombolysis.
NURSING IMPLICATIONS:
SERVICE
Determine intensity of client’s angina
Observe for signs and symptoms
Place patient in a comfortable position
Administer oxygen if required
Obtain vital signs every 15 minutes for 2 hours, every half an hour for one hour and
every hour for two hours then as required
Obtain a 12 lead ECG
Monitor for relief of pain
Monitor patient’s response to drug therapy
Institute continuous cardiac monitoring and observe for- reperfusion, arrhythmias, rhythm changes, bradycardia and tachycardia
Interpret rhythm strips
Watch for complaints of headache with use of nitrates
Watch for recurrences of pain. Reinforce the importance of notifying nursing staff whenever pain is experienced.
Administer medications to relieve patient’s anxiety as directed such as sedatives and tranquilizers
Provide complete bed rest for 24 hours
Determine level of activity that precipitated anginal pain occurs.
Identify specific activities patient may engage in that are below the level at which anginal pain occurs
Prepare for the diagnostic and treatment procedures such as coronary angiogram and PTCA [ Percutaneous Transluminal Coronary Angioplasty]
EDUCATION
Counsel on risk factors and life style changes such as-
Methods of stress reduction such as biofeedback and relaxation techniques
Low fat and low cholesterol diet
Avoid excessive caffeine intake
Do not use diet pills, nasal decongestants
Follow up visits to control diabetes and hypertension
Educate patient and family members regarding-
Prevention of recurrence of pain
Regular use of medications
Hazards of smoking
Prevention of other contributing factors
Regular follow up
Importance of dietary modifications
Avoiding activities which cause anginal pain such as sudden exertion, walking against the wind, extremes of temperature, emotionally stressful situations, refraining from engaging in physical activity for 2 hours after meals, reduce weight etc.
Appropriate use of medications
Side effects of medications
ADMINISTARTION
Lead interdisciplinary intervention programs
Education of nursing students and staff
Provide in-service nursing education
Maintenance of records and reports
Maintenance of statistics
Making of policies and procedures
Supervision and evaluation of staff performance
Recommendations for further study
A majority of post MI patients actually not participating in formal cardiac rehabilitation programs due to either lack of structured programs, physician
referrals, low patient motivation, non compliance and financial constraints.
Cardiac rehabilitation provides a venue for continued education, reinforcement
of life style modification and adherence to comprehensive prescriptions of
therapies for recovery for MI, which includes exercise training.
Participation in cardiac rehabilitation programs, post MI with a decrease in
subsequent cardiac morbidity and mortality.
Adequate education in the hospitals and work places on causative and contributing factors, preventive measures of heart attacks and re heart attacks, is necessary.
All forms of reperfusion, depending on local facilities, need to be available to patients. Protocols must be written and agreed for the strategy of reperfusion to be applied within a network. Early diagnosis of ST Elevation Myocardial Infarction is essential and is best achieved by rapid ECG recording and interpretation at first medical contact, wherever this contact takes place.
About the Author
Pushpa Latha, MSN, Vinayaka Missions University, Selam, Madras, India E-Mail keerthiraksha@yahoo.co.in Ph- 00971504277926
Metal Forming FAQ
A metal M react beside nitrogen to form a compound have the formula M3N.?
The metal M would have to be a part of the 1st group of the broken up table, as the metals there have a valency of 1, i.e, they own one valence electron in their valence shells. Na/K/Li or any other group 1 metal (1+) N…
A metal M react beside phosphorus ( P4) to form a compound have the formula M3P.?
A metal M reacts with phosphorus ( P4) to form a compound have the formula M3P. 19.50 g of the metal produce 24.65 g of the compound. Calculate the molar mass of the metal. Enter a numeric answer only, no units. i enjoy no…
A metal M react beside S to form a compound next to formula M2S3.if 3.12gm of M react next to 2.88g of S.What is M?
Assuming S is monotonic sulfur and not a more natural allotrope (e.g., S4): Equation: 2M + 3S = M2S3 A. Moles of S 2.88g S ( 1mol / 32.07g) = .0898 mol S B. Moles…
A metal M react next to sulfur to form a compound have the formula M2S.?
A metal M reacts with sulfur to form a compound have the formula M2S. 19.54 g of the metal produce 23.21 g of the compound. Calculate the molar mass of the metal. calculate the mass of sulfur (since we know its molar mass) 23.21 g…
A metal whose 2+ ions form blue aqueous soloution i devise copper & a metal legendary 4 conductivity&malleability
this is 4 a chemistry scavenger hunt i can’t seem to find this one Yes, you are looking for some “Copper.” Source(s): http://www.copper.org/resources/properti?? +2 ions being blue is copper (dissolve it contained by Nitric acid, if you want to find out)….
A metal, M forms two oxides M3O and M2O. If the percent by mass of M contained by M3O is 65.0% what is the perce?
hey guys i just need some lend a hand on this chem. question, if anyone can help soon greatly appreciated. Thanks “> M is an nonexistent metal with rather amazing properties; oxidation states of +1…
A metal, M, forms an oxide beside the formula M2O within which the mass percentage of the metal is 94.32%. The chem?
A metal, M, forms an oxide with the formula M2O in which the mass percentage of the metal is 94.32%. The chemical symbol for the factor, M, is “> % mass of O = 100-94.32= 5.68% No. of…
A metal, M, forms an oxide near the formula M2O contained by which the mass percentage of the metal is 96.54%.?
the chemical symbol for the element, M, is ?? The atomic mass of 0xygen is 16 of 100 grams, 3.46 is oxygen, 48.27 is M1, 48.27 is M2 so the ratio of the atomic weights is 48.27/3.46 = 13.95…
A metal, M, forms an oxide next to the formula M2O contained by which the mass percentage of the metal is 93.36%.?
The chemical symbol for the element, M, is ______. mass of metal in 100g = 93.36 mass of oxygen surrounded by the oxide = 6.64 g moles of oxygen = 6.64/16 =0.415 moles moles of the metal =…
A metal, M, forms an oxide w/ the formula M2O surrounded by which the mass percentage of the metal is 93.10%. The?
28. A metal, M, forms an oxide with the formula M2O in which the mass percentage of the metal is 93.10%. The chemical symbol for the thing, M, is the answer is Ag gold Source(s): solved for hmk…
A unshakable metal M forms two chlorides?
Compound A: 85.2% M 14.8% Cl Compound B: 65.8% M 34.2% Cl a) Show that these compounds are consistent with the law of Multiple Proportions. b) Write down several sets of formulas for compounds A and B that are consistent near the percent composition data. c)Assume that the atomic weight of Cl is…
A(n) ____________ bond is formed by the attraction between positively charged metal ions and the _____
metal negetively charged metal ions Source(s): my science textbook cheating on your homework? ionic, negatively charged non-metallic ions
Active metals resembling sodium counter near cold sea, setting free hydrogen and forming a(n) ______ solution.?
Red hot iron reacts with steam forming hydrogen and _______. Basic, or alkaline Iron oxide (rust) Basic or alkaline solutions 2Na + H2O–>2NaOH +H2 Fe +H2O—>H2 + Fe(OH)2 iron hydroxide
Al react next to MnO2 to form Mn metal and aluminum oxide. A mixture of the 2 reactants is 67.2% mole percent Al?
Find the theoretical yield (in grams) of manganese from the hostile response of 290 of this mixture. “> Al= 67.2% therefore Mn is 32.8% 32.8%*290= 95.12gm yield of aluminium
Alkaline mud metals form compounds by..?
a. gaining electrons b. gaining protons c. losing neutrons d. losing electrons d. Metals LOVE to supply up electrons. d. losing electrons hope this helps :] the answer is d. metals are certain to give or donate electronssince they are more electropositive than non metals
All of the group IVA elements can form four covalent bonds to other non metals. All but carbon can ……….
All of the group IVA elements can form four covalent bonds to other non metals. All but carbon can form additional compounds with more than four bonds. What precincts carbon in this ability? 1Carbon typically forms pi bonds within only…
Aluminium is outstandingly reactive and the metal vigorously forms an oxide blanket, on the other hand the metal shines why?
the oxide forms a thin layer that protects the metal underneath by slowing further oxidation, but given some time it will lose its attraction the aluminium oxide layer is bright and white. so aluminium shines in desk light although it…
Aluminum is a group 3A metal. Which ion does Al typically form?
Al3??Al3+ Al5??Al5+ Al 3+ elements in group 3 have 3 electrons within their outer electron shells, so when ions are formed, the atoms lose 3 electrons. this gives them a charge of +3. they lose these electrons so that they have full outer shells. they become…
Aluminum metal react beside chlorine gas to form solid aluminum trichloride. What mass of chlorine gas is call for?
the raction is 2Al + 3Cl2 >>2 AlCl3 the ratio between Al and Cl2 is 2 : 3 moles Al = mass / molar mass moles Cl2 needed = moles Al x 3 / 2 multiply by 70.906 g/mol to find…
Aluminum metal react beside solid copper(II) oxide to form copper metal and solid aluminum oxide……………
write the equation (balanced with whole numbers) representing this repercussion and show any necessary calculations to find the enthalpy regulation for two moles of aluminum reacting. Is this endothermic or exothermic reaction equation: 2 Al(s) + 3 CuO(s) ??AlO(s) + 3 Cu(s) According to…
Aluminum metal react next to aqueous iron(III) oxide to form aqueous aluminum oxide and iron metal.?
What is the stoichiometric coefficient for aluminum when the chemical equation is balanced using the lowest, whole-numbered coefficients? You had the answer correct within your previous question of this question: Fe2O3 + 2Al -> 2Fe + Al2O3 + Heat It requires 2 Aluminum’s. This…
Aluminum metal react next to dilute hydrochloric sharp, HCl, to form hydrogen gas and a solution of aluminum..?
chloride, AlCl3. What volume of hydrogen at STP will be produced when 35.0 grams of aluminum reacts with HCl? First, write the hanging equation: 2Al + 6HCl –> 2AlCl3 + 3H2. Then look up the atomic weight of aluminum. It’s 26.98. (Since…
An analysis shows that 5.90 g of a titanium metal combines beside oxygen to form 9.84 g of titanium oxide.?
an analysis shows that 5.90 g of a titanium metal combines with oxygen to form 9.84 g of titanium oxide. what is the empirical formula of the compound? “> well…. 5.9/47.9=0.123mols of Ti 9.84-5.9=3.94g of O2 so 3.94/16=0.246mols of O2…
An unknown metal forms 2 different compounds near oxyge?
When a 5.5 g sample of the metal combines with oxygen below conditions that form oxide A, 6.99 g of product are formed. When a second 5.5g sample of the metal is combined with oxygen below conditions that form oxide B, 7.74 g of product are formed. Oxygen’s equivalent weight is…
Any musicians who similar to folk / viking / power metal and want to form a group?
Any musicians in the hawkesbury , NSW, australia, Wanna form a viking / folk / power metal band? i play guitar and im 16. Way too far dude, try purevolume though, it’s righteous for recruiting. But I’ll support it LONG LIVE BEER, BEARDS,…
Any other form of orthodontic spacing bar metal band?
I just got my metal band today, on my back molars and they’re driving me nuts. I can’t chew because my top tooth is hitting the bracket welded to the bottom metal trimming on the right side and the metal is buggin’ the **** out of my fillings. It’s like chewing…
Anyhow…Stumbled Across on the other hand ANOTHER Melodic Metal Band form Finland….?
called Wasara….. Might not be for everyone, but I enjoyed it: http://www.youtube.com/watch?v=HNKpWOctt?? http://www.youtube.com/watch?v=5OoH01UTk?? Music Q: Favorite Finnish Metal Band? Bonus Music Q: More Insane Metal Talent: Finland or Sweden? Bonus Bonus Q: What the heck is in the water over nearby, anyhow? are Fins and Swedes…
Are covalent bonds formed beside metals or nonmetals?
When metals react with eachother, do they form covalent bonds? I know when a metal and nonmetal act in response, it is ionic. When is it polar/non-polar covalent? when nonmetals react with respectively other, they form covalent bonds. a bond can be polar covalent if there’s a slight difference in electronegativity or…
Are in attendance any metals that can form covalent bonds?
I know that metals can form ionic and metallic bonds. Can they form covalent bonds? Yes; Covalent bonding includes copious kinds of interactions, including -bonding, -bonding, metal-metal bonding, agostic interactions, and three-center two-electron bonds. NO! Covalent bonding does not necessarily require the two atoms be of one and the same…
Are in attendance any simulation & analysis softwares available for sheet metal forming?
Yes, I use “Autodesk(R) Inventor”. there are commands allows to design sheet metal parts surrounded by a sheet metal mode. Beside the commands for the simulation and load analysis. This software is nice I close to it. It’s easy and fast to cram it, but needs some…
More Metal Formingquestions please visit : MachineryFAQ.com
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Transdermal Technology A New Sexual Enhancement Delivery System
Transdermal technology claims it is the key to a new and exciting breakthrough in men’s sexual health. Companies such as those who manufacture Prosolution Gel have many promises. Many guys suffer from lack of sexual performance form one time or another for many different reasons. The problems include:-
-Problems achieving an erection.
-The erection doesn’t quite become stiff enough.
-Unable to control the penis to achieve satisfaction for the man or his partner.
-Unable to keep the erection throughout the duration of the sexual act.
-Premature ejaculation.
-Little feeling leading to a poor climax.
Transdermal science claims to allow a fast-acting formula that delivers natural ingredients and nutrients directly to the penis for a feeling of fuller, thicker and firmer erections, plus longer lasting erections, improved sexual stamina and the prevention of premature ejaculation how do they back up these claims.
The Science
The way an erection works is the there are two chambers in the genitals that fill with blood during arousal. They fill with up to eight to ten times as much blood than that of a normal penis. This blood stays in the penis until the release through orgasm.
Men can run into problems at any stage of the erection from arousal though performance to the end of the climax cycle. Booze, stress, tiredness, worry, anxiety or other physical problems can interrupt at any time. For many guys the first sign of trouble can distract causing a snowball effect that can ruin the experience entirely.
Many guys who even go through and complete a sexual experience to the point of orgasm can still have an unfulfilled experience feel that they could have had a better and more rewarding experience which will lead to a better experience for the man and his partner.
Transdermal technology enables you to deliver erection and performance boosting ingredients directly to the penis. The active ingredients go to work in immediately to give you a thicker, bigger erection that last much longer than usual by bringing more blood to the penis during arousal is the first key to a better erection. Transdermal science incorporates the power of L-Arginine to increase nitric oxide in the area around your genitals – and nitric oxide helps to open blood vessels to allow you to pump up the chambers of the penis to their absolute maximum.
A Better Finish
The application of Transdermal science delivers a blast of Vitamin C and other nutrients work directly onto your penis by using a gel. This nutrient than allows you to keep you hard for longer that they claim to result it a better climax
In Conclusion
Transdermal technology may help in improving your sex life by allowing you to be able deliver the natural ingredients to help directly where needed through application of a gel or cream given. It must be noted however that before using a substance on your manhood that you research the product carefully and read testimonials.
The science behind direct application has been used for a number of years in medicine for use to help rashes or aid healing of cuts or burns. This technology can be translated to the penis and the fact there is a growing market must mean that many men are getting results with this technology.
About the Author
The new Prosolution Gel is the first and most succesful sexaul enhancement gel. Holly contributes to what is the average size of a penis a great male masturabtion resource.
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Bulk Up Your Muscles With Protein Smoothie Recipes
If you’ve been thinking of building up some muscle, you need to be serious about your exercise program and of course, your food choices. If you really want to get buff, you would want to increase your protein intake. Drinking protein-packed smoothies is a great way to promote muscular gains.
One of the best things about smoothies is it’s very versatile. You can add ingredients with high level of protein like eggs, tofu and protein powder to make sure you are getting the necessary protein required by your muscles to bulk up and get ripped.
I want to share with you some of my tried-and-tested protein smoothie recipes. These drinks are perfect any time of the day, but I personally prefer drinking them for breakfast and right after an intense workout.
CHOCO PROTEIN POWERCHARGE
This chocolate smoothie is not just packed with protein, it’s very delicious too.
What you need:
Two tablespoons chocolate milk syrup
Two cups of non-fat milk or milk substitute
Half a teaspoon dry chocolate pudding mix
One fourth cup peanut butter
One medium banana
One cup crushed ice
One tablespoon whey protein powder
Blend in all ingredients thoroughly until smooth.
STRENGTH THROUGH SOY
Personally, I would say this is the perfect protein smoothie for breakfast. One glass will boost your energy with soy protein, fiber, monounsaturated fats, vitamins, omega 3 fats and antioxidants!
What you need:
One cup orange juice
Half a cup soy milk
Half a cup nonfat plain yogurt
One medium banana
One half apple
One kiwi peeled
Half a cup mixed berries (frozen)
Half a cup tofu
Three tablespoons unsalted natural peanut butter
Two tablespoons aloe vera juice
Two tablespoons flaxseed oil
Combine all the fruits with orange juice in a blender. Blend until smooth. Add soy milk, tofu, yougurt, peanut butter, aloe vera juice and flaxseed oil. Blend well until smooth.
FRUITY FUEL
This is a wonderful recipe if you prefer your protein drink fruity. This also has a high concentration of fibers and antioxidants.
What you need:
One medium banana, cut
Two tablespoons whey protein powder
Three large strawberries
One fourth cup blueberries
Half a cup non-fat or skimmed milk
Half a cup crushed ice
Half a cup nonfat plain yogurt
First, blend in the banana with the milk, yogurt, ice and whey protein powder. Add the berries and blend thoroughly until smooth.
You can always make your own combinations. After all, diversity is the key to success. Make these recipes as a regular part of your muscle training program and I’m sure you’ll see positive results.
If you want to discover new protein-rich smoothie recipes as well as other delicious and nutritious smoothies, you will surely enjoy this recipe collection called “Sensational Smoothies: Drink Your Way To Health Deliciously”. This awesome ebook showcases over 180 recipes for smoothies that will keep you interested in this healthy habit. Find out more about it here: http://www.sensationalsmoothies.com
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ABB Performance Pure Pro 50 Shake, Milk Chocolate, 14.5-Ounce Bottles (Pack of 12) $42.35 Pure Pro 50 comes on strong with 50 grams of protein from milk and whey. Nothing comes close for convenience, taste and muscle-building support. A superior resealable aluminum bottle further distinguishes this potent potion from the pack. It keeps your protein cooler longer while providing an easy way to save some for later. Work Pure Pro 50 into your workout routine and experience ABB superiority… |
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Tension 101
The Basics
Imagine a car that’s idling too fast. It’s revved up and working hard but nothing useful is happening. The motor’s burning more fuel, creating more pollution and experiencing added wear and tear.
Well, it’s kind of the same with muscle tension. It doesn’t help you move and it certainly doesn’t make your muscles stronger. So really your muscles are working hard but not doing anything useful or accomplishing anything.
In fact, muscle tension causes a lot of wear and tear on your body. It strains tendons (which hold your muscles to your bones). It pulls joints tighter together (leading to grinding/crunching sounds and worn out cartilage). It limits your movement, interferes with your co-ordination and may even make you more accident-prone.
Tension also burns up the fuel in your muscles (which makes you feel tired) and creates toxic waste products called “metabolites” (the equivalent of car exhaust) which fatigue your muscles and make them feel sore and achy.
Why Control Tension
• You’ll feel more comfortable.
• You’ll prevent problems.
• You just know that tension isn’t good.
2 Causes Of Tension
1. Stress is one of the major sources of muscle tension. When under stress, you become like a turtle trying to pull its head into its shell. So your shoulder muscles might simply tighten up or they might round forward and lift up as your head pulls back. And if your stress level is high, you may actually notice your shoulders around your ears.
2. Just sitting or staying still for periods of time causes your muscles to tighten up. By remaining “static”, you’re basically training your muscles to lock your back or neck in a certain posture. Then when you begin to move, your muscles remain tense in an effort to maintain your position. Plus it takes some time for your muscles to realize that they can let go and relax. So the longer you sit without moving, the more you train your muscles to lock into position and the longer it takes to release them.
Key Tension Areas
Simply based on the way tension is created, the areas most vulnerable to tension are your neck, shoulders and back. Although tension can develop in any muscle in your body, these are the areas that are most commonly affected.
Tenderness And Tension
One of the best indicators of tension is tenderness, which is the discomfort you feel when you press on a muscle.
Blood vessels normally deliver oxygen and nutrients to a muscle and flush away waste products. But, when your muscles are tense, they’re essentially squeezing their own blood vessels.
So now, the muscles are working hard and creating lots of waste that’s not being washed out of the muscle. And as these “metabolites” (i.e. waste) begin to accumulate, they start to irritate pain nerves.
If the tension is significant, you’ll actually start to feel achy. If the tension is less severe, the nerves become sensitive and any added stimulus, like a squeeze to the muscle, can cause discomfort.
1 Easy Way To Relieve Tension
Massage can play an important role in helping you deal with your tension and your massage professional, like a mechanic, can adjust how fast your “muscle motors” are idling.
Basically, massage does two things:
First, it helps induce a relaxation response. This reduces the common defensive reactions in your body, including that “turtle-in-the-shell” action of your neck muscles. Relaxation also causes your brain and nervous system to slow down, which in turn lowers the tension level of all the muscles in your body.
Second, massage pulls and stretches, which physically releases the muscle. In addition, the sensations that your muscles feel, both conscious and subconscious, give your brain information about the level of tension that exists in your muscles. This helps your nervous system adjust your muscles to a normal level of tone.
Remember too that the effect of a massage on tension is almost instantaneous. You feel the tension leaving your body immediately. You don’t have to wait days or weeks to see results.
Also, regular massage both reduces your tension and trains your muscles to maintain a lower level of tension.
And when your muscles are healthy and relaxed, they won’t be tender and you won’t feel any discomfort, even when you’re receiving a massage.
1 Easy Way To Prevent Tension
One of the areas most likely to get tense is the shoulders.
(In the nearly 8 years that I’ve been doing chair massage, the shoulders are still the Number 1 area people ask to have massaged because they’re experiencing tension there.)
The muscle that makes up the shoulders is called the trapezius, often referred to as the “traps”. It’s an easy name to remember because this is the muscle that “traps” a lot of tension.
The good news is you can help prevent tension from building up in this muscle.
If you’re sitting or standing still for any significant period of time, be sure to move this muscle through a full range of motion, at least once in a while.
Something you can try is the “20/20 Rule”:
For every 20 minutes that you are inactive, spend 20 seconds moving.
This helps ensure that your muscles don’t have the chance to lock into any particular position.
Use the two simple exercises in this article to bring your “traps” through a full range of motion and keep your muscles relaxed and tension-free.
Download your exercise illustrations here: http://www.bodyworkbiz.com/courses/downloads/illustrations/s7937ks9.zip
If you have specific health concerns, consult your medical doctor. The information in this article is educational only and is not intended to replace the advice of your personal health care provider(s).
This article may be freely reprinted or distributed in its entirety in any e-zine, newsletter, blog or website. The author’s name, bio and website links must remain intact and be included with every production.
About the Author
Chris Simon is a Certified Chair Massage Practitioner specializing in relaxation massage for muscle tension and stress. He’s been providing on-site chair massage to people in their homes and employees at their workplaces in Hamilton and throughout Ontario since 1999. Visit his website at http://www.hamilton-massage.com to learn more.
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Relax into Stretch: Instant Flexibility Through Mastering Muscle Tension [VHS] … |
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The Healing Power of Nature: Visual Therapy for Stress Reduction & Wellness [VHS] “Views” of nature have powerful healing potential and can play an important role in helping to reduce everyday tension and stress. This videotape was created specifically as “visual therapy” to help promote relaxation and general wellness. Research has shown that long-term exposure to images of nature, such as these, can has lower blood pressure, ease muscle tension, reduce anxiety and create a mo… |
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Work Station Workout – Ergo Exercises for Computer Users $28.95 Certified Professional Ergonomist and Workplace Consultant, Dr. Michael O’Neill points out each high stress area and explains what each exercise will do to help combat the day-to-day strain of life at the computer. Work Station Workout is here to help with 33 simple, easy-to-use exercises that you can do at your computer – or virtually anywhere – to help ease tension, strengthen key muscles and re… |
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Village Naturals Therapy Muscle Relief Natural Lotion 16 fl oz $7.95 Let Village Naturals TherapyTM Muscle Relief Lotion make a house call. Massage away muscle aches and pains while aromatherapy vapors help you feel better. Our deep penetrating therapeutic formula is enriched with vitamins and skin softening ingredients that will help improve skin circulation and appearance. Relax and feel your aches melt away with ingredients extracted from natural sources. This p… |
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Harder Erections – If You Want A Harder Erection Get More Nitric Oxide Naturally!
Penis Enlagrement Exercises and topics on
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If you are a regular guy there would be times that you would wonder as to How to enlarge my penis which means that there are lots of people who want such info. There are many reasons why people want to know about how to get a larger penile size as they feel that this can help them in enjoying more pleasurable sexual relations.
If you have been wondering ‘how do I enlarge my penis’ then you’ve come to the right place. I want to outline exactly what does and what does not work for penis male enlargement.
Today is the generation when we live in major medical breakthroughs that give us the answers to our medically-problematic questions. Those questions include life-threatening queries about cancer heart problems stress-related problems and particularly to men sex improvement and penis male enlargement devices. We have seen it all commonly with the introduction of pills into our lives like male enlarging pills and male pills that deals with erectile early dysfunction. Particularly for the younger generation penis male enlargement devices and programs are considered options for sex performance.
Exercises happen to the safest and easiest methods of ensuring natural penis male enlargement. These exercises can make your penis grow by up to 3 inches and the best part is that you can do them easily at home.
The first thing we have to pay attention to is our diet hormonal and cardiovascular systems. The point being is that our bodies must be healthy if we’re going to grow our penis to any significant degree. Secondly using specific herbs and supplements really does help add inches.
Do you feel your confidence level ebbing away because of your small penis size? Do you think you can’t please your girl because you feel somewhat lacking in size? You’re certainly not alone! Let’s face it. Close to 8 in 10 men are in the same boat as you feeling small insecure and embarrassed about their manhood. But if you think that you can safely make your penis bigger with the myriad of costly male enhancement products on the market think again. Most if not all of them will not give you any real sizeable improvements in your penis.
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Maxoderm HFR – Nitric Oxide Topical Gel, 4 oz,(Barmensen Labs) $37.00 Maxoderm HFR Gel is the only topical Nitric Oxide formula scientifically engineered with VasoTran Auctum, our patent pending delivery matrix guaranteed to maximize results. Maxoderm HFR Gel helps stimulate your Hard Flex Ratio (HFR), which measures muscle contraction efficiency at the pinnacle of muscle tension. The greater your HFR, the greater your muscle load and output, resulting in increased … |
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Dorian Yates Approved Pro-NOx Topical Cream, 2-Ounce Bottles $22.50 Targeted nitric oxide generator. Nitric oxide pump contains arginine AKG and L-Arginine. Delivers nitric oxide directly to the muscle. Super pumps when stacked. Manufactured in USA…. |
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HFR Nitric Oxide Gel Topical Cell Volumizer for Men (4oz) HFR is a radically innovative topical cell volumizer, formulated as a Nitric Oxide training gel, which combines targeted delivery and vasodilation. Containing patent pending VasoTran Edurus, the only Nitric Oxide delivery system that targets muscles directly, HFR provides athletes with maximum absorption starting with your very first training session…. |
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Technology-based NOx̳ and SO emission rates for the electric utility sector: Final report (Topical report) … |
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Build Muscle Mass Fast – Seven Benefits Of Nitric Oxide Supplements
In 1998, three scientists won the Nobel Prize in Physiology or Medicine for their discovery of the gas nitric oxide. This gas is extraordinarily valuable in controlling blood circulation and in brain, lung, kidney, liver and other essential organ regulation. There are also numerous tissues that profit from the gas, regulating many bodily functions.
This great vertical jump training program teaches you every thing you need to know so as to quickly increase your vertical jump! Click on on the follwoing link to check it out: Jump Manual Review
1. Blood pressure and clotting control Through the aid of nitric oxide, blood pressure may be reduced while both blood flow and blood vessel diameter are enhanced and blood clot formation is improved. Endothelial cells assist the controlling and relaxing of blood vessels, and this is further improved through the utilization of the gas. Studies suggest that nitric oxide supplements enlarge blood vessels, keep the heart from harm and boost the provision of oxygen to the body.
2. Vitamin-enhanced The supplementation is loaded with B-sitosterol, ursolic acid, glycosides, plant sterols and anthraquinones, as well as potassium, calcium, zinc, vitamin A and C, and iron.
3. Immune system protection The immune system is also helped, since the immune cells usually discharge nitric oxide to destroy bacteria as well as parasitic and viral infections. The assembly of the blood cells in the bone marrow is improved with nitric oxide supplements, while the number of immune-boosting “Killer T-Cells” is enhanced. Quite valuable in the muscle recovery of the entire body, these supplements are also believed to contribute to the cutback in tumor growth, and can develop immune response hostile to cancerous cells.
4. Pain relief A superb doctor for both rheumatism and inflammation, the supplementation relieves pain. Additionally, because it facilitates the decrease of inflammation, it is helpful for bodybuilders since it aids in muscle pain reduction accompanying extreme stress.
5. Fast muscle gain For those of you looking to gain muscle mass fast, these supplements help to widen the blood channels that lead to skeletal muscles. Therefore, people using this supplement often put on lean muscle mass faster and gain improved endurance. A good choice for bodybuilders, nitric oxide improves blood flow, making it more feasible for the blood to distribute more nutrients to the muscles, increasing their size.
6. Improve body functioning Accountable for the communication of messages between nerve cells, this gas is linked with the processes of memory, sleeping, and learning. These nutritional supplements stimulate the brain and moderate many functions that vary from behavior to gastrointestinal movements. Research claims that nitric oxide is an excellent supplement credited with changes for the better of the performance of numerous systems of the body.
7. Sexual response increase This nutritional supplement will also assist in stimulating, repairing, and amplifying sexual response. Actually, one of the results of Viagraa is escalating the quantity of nitric oxide in the body because it prolongs and intensifies the phase of stimulation.
Caution Nitric oxide supplements usually have the amino acid arginine-alpha-ketoglutarate, in which overdose could occur. Too much of this amino acid could cause diarrhea, queasiness, and weakness. The consumption of this supplementation has no cut-and-dry dosage that must be obeyed. To find the ideal dosage for yourself, use tolerance mapping. Take insignificant dosages for seven days and observe its benefits and side effects; then boost the dosage until you see the most benefits with the least side effects.
Now that you’ve got some ideas about ways to improve your vertical jump, would you like more tips for how to jump higher? Are you a dedicated athlete with a desire to excel at your sport? Do you want to use the best and most effective vertical jump training system to greatly increase your jump height? If yes, then you need to join Jacob Hiller’s Jump Manual Program.
Click here ==> The Jump Manual, to read more about this Vertical Jump Training Program, and how it ranks with other Popular Vertical Jump Training Systems out there.
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Related articles: Jacob Hiller’s Jumping Manual On ESPN, Free Vertical Jump Training Tips
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Article By Jacob Hiller: Jacob Hiller is the creator of a bestselling vertical jump program “The Jump Manual”, and he is considered one of the world’s foremost authorities on vertical jump training. Click on the following link to visit his website: Jacob Hiller’s Jump Manual
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Designs For Health – Amino Acid Synergy – 120 Vcaps $24.00 Designs For Health – Amino Acid Synergy – 120 Vcaps… |
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1Fast400 Arginine Alpha Ketoglutarate 2:1, AAKG 2:1, 1000-Grams $59.99 Information Coming SoonPacking Information:Each powder is put into a 4oz HDPE container, Heat Sealed, and labeled with dosing based off 1/4 tsp. Some items may be hygroscopic and may clump during shipment. This does not effect the efficacy of the product, but just the texture. Available for immediate shipment (subject to stock level). ORDER Today!… |
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APOLLO FITNESS ESSENTIALS REJUVENATE AMINO ACID SUPPLEMENT, 120 CAPSULES $29.99 REJUVENATE is useful as a general supplement to diets that are insufficient in quality protein, for athletes that require additional amino acids to maintain or achieve greater lean body mass, for patients who are cachexic form chronic illness or GI malabsorption, for individuals who are in catabolic states due to stress or illness, for those recovering from surgery or tissue trauma, for people wan… |
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Sprint Triathlon Training
Sprint triathlon are often the stepping stone for many triathletes to get involoved in the sport. Sprints are also races that you can do more often through out the year VS an Ironman. The coaches at the rock star triathlon Academy have put togeather some things you can do to enhance your sprint triathlon training.
1. Avoid Your Facebook Ironman Friends. If you just got back from an explosive 2 mile run, then log-in to your social network to find that yourfriend just slogged out 12 miles, you may be discouraged. It is very important, however, for you to realize that the individual who is training for Ironman is actually making themselves slower when it comes to sprint triathlon training. So don’t be discouraged that you’re not “fit enough”. For sprint triathlon training, you should pursue speed, and not slow endurance.
2. Consider Nutrition Supplementation. There are many nutrition supplements that can assist you with explosiveness, power, speed and recovery. A few of the tried and true aids that are easily accessible to enhance your sprint triathlon training include: creatine, nitric oxide, CoQ10, branched chain amino acids and glutamine. Don’t be afraid of supplements! All those listed here have been researched many times and found to be both safe and effective.
3. Include Overspeed Training. Despite popular belief, overspeed training does not mean that you go out and swim, bike or run faster than you normally would during your sprint triathlon training. Instead, this term refers to neuromuscular training – teaching your muscles how to contract quickly and repetitively. For swimming, this could include practicing with a metronome. For running, you can include treadmill efforts at a pace that makes your legs turn over faster than they would while running outside. And for cycling, you can simply choose an easy gear and perform fast spins at 100+ revolutions per minute.
4. Do Plyometrics. Jumping, hopping, bounding and leaping exercises, also known as “plyometrics” can significantly enhance your sprint triathlon training performance by teaching your muscles to recover quickly between contractions and also produce faster and more forceful efforts. An example of plyometrics would include perform a series of 3×10 jumps up onto a bench or box before you go out for run, or chest passing a medicine ball against a wall for 8 explosive reps. Doing a single plyometric session at least once per week for eight weeks leading up to your sprint triathlon will make you a quicker athlete.
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http://www.rockstartriathlete.com Sprint Triathlon Training Ideas from the guys at the Rock Star Triathlete Academy
Get free advice on how to train for a sprint triathlon right here http://rockstartriathlete.com