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If environmental elements are responsible for lack of sleep, the patient must be taught tips on how to appropriate them or compensate for them. All patients ought to be endorsed about sleep health (also often known as sleep hygiene). In any given yr, about 30% of Americans expertise intermittent insomnia, and about 10% expertise persistent insomnia. In the United States, the direct costs of insomnia complete about $16 billion a year, including the costs of testing, prescriber visits, and hypnotic medicine. This will assist condition your brain to see the bed room as a place the place sleep occurs. Patients who snore heavily and those with respiratory issues have decreased respiratory reserve, which could be further compromised by the respiratory-depressant actions of hypnotics. When hypnotics are employed, care should be taken to prevent drug-dependency insomnia, a situation that may lead to inappropriate prolongation of therapy. Drug-dependency insomnia is a selected downside with older hypnotics (eg, barbiturates), and develops as follows: 1. Upon cessation of therapy, a gentle withdrawal syndrome happens and disrupts sleep. Failing to recognize that the lack to sleep is a manifestation of drug withdrawal, the patient becomes satisfied that insomnia has returned and resumes drug use. Continued drug use leads to heightened physical dependence, making it much more difficult to withdraw medicine with out producing another episode of drugdependency insomnia. That is, they should be used in the lowest efficient dosage for the shortest time required. Major Hypnotics Used for Treatment Insomnia could be treated with prescribed drugs, nonprescription medicine, and alternative medicines. Among the prescription drugs, benzodiazepines and the benzodiazepine-like medication (zolpidem, zaleplon, and eszopiclone) are drugs of selection. Nonprescription drugs and alternative medicines are much much less efficient than the first-choice drugs, and hence must be reserved for people whose insomnia is mild. As proven in Table 34�5, hypnotic medication differ with respect to onset and length of action, and hence differ in their applications. Drugs corresponding to flurazepam, which have both a rapid onset and lengthy duration, are good for sufferers with both types of sleep issues. Cognitive and behavioral interventions embrace sleep restriction, management of the bed room setting, progressive leisure, and schooling about sleep hygiene. The American Academy of Sleep Medicine considers these interventions both effective and dependable, and therefore recommends them as first-line remedy for chronic insomnia, even if drug therapy is also employed. Hence, before resorting to medication, we should implement nondrug measures, and we should always treat any pathology that will underlie inadequate sleep. The affected person must be reassessed regularly to decide if drug remedy remains to be wanted. Interruption will allow tolerance to decline, thereby restoring responsiveness to therapy. Benzodiazepines Benzodiazepines are medication of first choice for short-term treatment of insomnia. These brokers are safe and efficient and lack the undesirable properties that typify barbiturates and different older hypnotics. Benzodiazepines have a low abuse potential, cause minimal tolerance and bodily dependence, current a minimal threat of suicide, and endure few interactions with different medication. Benzodiazepines have multiple desirable results on sleep: they lower the interval to sleep onset, decrease the variety of awakenings, and enhance whole sleeping time. With most benzodiazepines, tolerance to hypnotic actions develops slowly, allowing them to be used nightly for a number of weeks without a noticeable loss in hypnotic effects. Two agents-triazolam [Halcion] and flurazepam-can be thought of prototypes of the benzodiazepines used to promote sleep.

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If essential, bivalirudin may be infused for as a lot as 20 extra hours at a price of zero. In medical trials, argatroban reduced growth of new thrombosis and permitted restoration of platelet counts. Allergic reactions (dyspnea, cough, rash), which develop in 10% of sufferers, happen virtually solely in these receiving either thrombolytic drugs (eg, alteplase) or distinction media for coronary angioplasty. Argatroban has a brief half-life (about forty five minutes) owing to speedy metabolism by the liver. Unlike fondaparinux, which acts indirectly (see above), rivaroxaban binds directly with the lively center of factor Xa, and thereby inhibits manufacturing of thrombin. Rivaroxaban has Desirudin Desirudin [Iprivask] is a direct thrombin inhibitor much like bivalirudin. Rivaroxaban was a minimum of as efficient as warfarin, and carried the same risk of major hemorrhagic occasions of all kinds-but had a lower threat for intracranial bleeds and deadly bleeds. Rivaroxaban ought to be discontinued no much less than 18 hours before eradicating an epidural catheter; once the catheter is out, one other 6 hours should elapse before rivaroxaban is restarted. If a traumatic puncture occurs, rivaroxaban should be delayed for at least 24 hours. Anticoagulant-related spinal/epidural hematoma is mentioned additional above (see Adverse Effects under Heparin). Pharmacokinetics Rivaroxaban is run orally, and bioavailability is high (80% to 90%). Rivaroxaban is eradicated within the urine (36% as unchanged drug) and feces (7% as unchanged drug), with a half-life of 5 to 9 hours. In sufferers with renal impairment or hepatic impairment, rivaroxaban ranges might accumulate. The risk of hemorrhagic stroke and other major bleeds is significantly decrease with rivaroxaban. However we can prevent additional absorption of ingested rivaroxaban with activated charcoal (see Chapter 109). Because rivaroxaban is very protein sure, dialysis is unlikely to take away it from the blood. Like all different anticoagulants, rivaroxaban poses a risk of spinal or epidural hematoma in sufferers undergoing spinal puncture or epidural anesthesia. Concurrent use with antiplatelet drugs and fibrinolytics must be accomplished with warning. Renal impairment can delay excretion of rivaroxaban, and might thereby increase the danger of bleeding. Accordingly, rivaroxaban should be averted in patients with extreme renal impairment, indicated by a CrCl beneath 30 mL/min. In sufferers with average renal impairment (CrCl 30 to 50 mL/min), rivaroxaban should be used with caution. In medical trials, rivaroxaban ranges and anticoagulation had been extreme in sufferers with reasonable hepatic impairment. The drug will increase the risk of pregnancy-related hemorrhage, and will have detrimental results on the fetus. When pregnant rabbits got excessive doses (10 mg/kg or more) during organogenesis, rivaroxaban elevated fetal resorption, decreased fetal weight, and decreased the number of reside fetuses. However, dosing of rats and rabbits early in being pregnant was not related to gross fetal malformations. Preparations, Dosage, and Administration Rivaroxaban [Xarelto] is provided in tablets (10, 15, and 20 mg). The beneficial dosage is 10 mg as quickly as a day, with or with out food, starting 6 to 10 hours after knee or hip alternative surgery. Treatment length is 12 days following knee replacement and 35 days following hip replacement.

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Once-weekly dosing, which is simply as efficient as once-daily dosing, is feasible because alendronate undergoes incorporation into bone, the place it stays and acts for years. As with different bisphosphonates, benefits derive from inhibiting osteoclastmediated resorption of bone. The commonest opposed results are arthralgia, diarrhea, headache, rash, nausea, and a flu-like syndrome. Like alendronate, risedronate poses a significant danger of esophagitis, and a very small risk of atypical femoral fractures. Dosages are as follows: � � � � Postmenopausal osteoporosis, for prevention or remedy (Actonel or Atelvia)-With Actonel, 5 mg as quickly as day by day, 35 mg once weekly, or a hundred and fifty mg as quickly as a month. If needed, a second 2-month course can be given, supplied a minimal of 2 months have elapsed since completing the primary course. Drugs Affecting Calcium Levels and Bone Mineralization of the drug is sure to serum proteins, primarily albumin. Like alendronate, tiludronate poses a risk of esophagitis, ocular problems, musculoskeletal pain, and presumably esophageal most cancers. Other unwanted side effects include chest pain, edema, paresthesias, hyperparathyroidism, vomiting, and flatulence. In addition, etidronate causes faulty mineralization of newly fashioned bone (osteomalacia), and can thereby improve the chance of fractures. To maximize absorption, sufferers ought to wait 2 hours earlier than ingesting meals, antacids high in metals (eg, calcium, iron, magnesium, aluminum), and vitamins that comprise mineral supplements. Treatment can be repeated, but not till ninety days have elapsed since completing the prior course. The dosage for preventing heterotopic ossification in sufferers undergoing complete hip replacement is 20 mg/kg every day for 1 month before surgical procedure and for three months after. For heterotopic ossification caused by spinal wire harm, the dose is 20 mg/kg/day for two weeks, then 10 mg/kg/day for 10 weeks for a complete therapy interval of 12 weeks. Following absorption, ibandronate undergoes speedy binding to bone or excretion in the urine. As with different bisphosphonates, bivalent cations (eg, calcium, magnesium, iron) can significantly decrease absorption. Accordingly, ibandronate ought to be injected slowly-over an interval of 15 to 30 seconds. The dosage for prevention and treatment of osteoporosis is 150 mg as quickly as a month, taken on the identical day each month. Patients ought to swallow tablets entire with a full glass of water, whereas standing or sitting upright. For 60 minutes after dosing, sufferers should remain upright, and should not eat or drink something, including medications and dietary supplements. Kidney perform must be decided earlier than every dose and, if severe renal impairment is detected, the dose ought to be withheld. In addition, the drug is used off-label to stop bone loss, fractures, and different skeletal-related events in sufferers receiving any of a selection of therapies that create a danger of bone loss. Like different bisphosphonates, zoledronate undergoes incorporation into bone, the place it stays for years. When osteoclasts ingest the drug, it inhibits their exercise, stopping bone resorption. In one research, zoledronate normalized serum calcium in 88% of sufferers within 10 days of a single infusion. Specifically, onset is faster, period is longer, and, maybe most significantly, infusion time is shorter (15 minutes vs. For administration of postmenopausal osteoporosis, zoledronate differs from all other bisphosphonates in that dosing is completed just every year or once every 2 years. Compared with placebo therapy, once-yearly zoledronate decreases the Tiludronate Actions and Uses. The drug decreases abnormal bone progress and, unlike etidronate, does so with out interfering with bone mineralization.

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Like other dihydropyridines, clevidipine may cause hypotension and reflex tachycardia. In blood vessels, calcium entry causes vasoconstriction, and therefore calcium channel blockade causes vasodilation. In the heart, calcium channels are coupled to beta1 receptors, activation of which enhances calcium entry. As a end result, calcium channel blockade and beta blockade have identical results on cardiac function. Tachycardia is most intense with immediaterelease formulations, and much much less intense with sustained-release formulations. Beta blockers can be utilized to suppress reflex tachycardia brought on by nifedipine and other dihydropyridines. In toxic doses, nifedipine and other dihydropyridines may cause cardiosuppression, similar to verapamil and diltiazem. Immediate-release nifedipine has been related to increased mortality in sufferers with myocardial infarction and unstable angina, though a causal relationship has not been established. The National Heart, Lung, and Blood Institute recommends that immediate-release nifedipine, particularly in higher doses, be used with great caution, if at all. Baseline Data For all patients, determine blood strain and pulse price, and obtain laboratory evaluations of liver and kidney perform. For sufferers with angina pectoris, obtain baseline data on the frequency and severity of anginal assaults. Use with warning in patients with heart failure or liver impairment and in sufferers taking digoxin or beta blockers. Verapamil and diltiazem may be used for angina pectoris and essential hypertension. Verapamil may be used with digoxin to control ventricular fee in sufferers with atrial fibrillation and atrial flutter. Instruct sufferers to swallow sustained-release patients to self-monitor their blood stress and to maintain a blood strain document. Inform sufferers about indicators of edema (swelling in ankles or feet) and instruct them to notify the prescriber if these occur. Advise patients that constipation can be minimized Minimizing Adverse Interactions Digoxin. If hypotension or bradycardia is detected, withhold medication and notify the prescriber. Intravenous remedy with verapamil or diltiazem is reserved for cardiac dysrhythmias. Ongoing Evaluation and Interventions Evaluating Therapeutic Effects Angina Pectoris. Keep an ongoing record of anginal assaults, noting the time and depth of every assault and the probably precipitating event. Teach outpatients to chart the Managing Acute Toxicity Remove unabsorbed drug with gastric lavage followed by activated charcoal. For most patients, the aim is to scale back systolic/ diastolic strain to a price under 130/80 mm Hg. Teach time, depth, and circumstances of their assaults, and to notify the prescriber if assaults increase. Administration Instruct patients to swallow sustained-release formulations complete, without crushing or chewing. Ongoing Evaluation and Interventions Evaluating Therapeutic Effects See nursing implications for Verapamil and Diltiazem. Inform patients about signs of edema and instruct them to notify the prescriber if these occur. Undesired results associated to selective dilation of arterioles and veins are discussed below. Therapeutic implications of selective dilation are mentioned in Chapters 47, 48, 51, 53, and 107.

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Children 2 to 12 years old, and children 13 years and older who weigh lower than 50 kg-15 mg/kg every 6 hours or 12. As a end result, the results of aspirin persist until cells could make extra cyclooxygenase. Because platelets are unable to synthesize new cyclooxygenase, the antiplatelet effects of a single dose of aspirin persist for the lifetime of the platelet (about eight days). Antiinflammatory doses of aspirin are a lot higher than analgesic or antipyretic doses. Aspirin is a useful drug for rheumatoid arthritis and other chronic inflammatory situations. The danger of aspirin-induced gastric ulcers may be lowered by (1) testing for and eliminating H. When taken for major prevention, the benefits of aspirin have to be weighed towards the potential for hurt. Because of its antiplatelet actions, high-dose aspirin should be discontinued 1 week before elective surgery or parturition. In most cases, low-dose aspirin taken to protect against thrombosis may be continued. Because of its antiplatelet actions, aspirin can improve the risk of bleeding in patients taking warfarin, heparin, and different anticoagulants. By impairing renal perform, aspirin could cause sodium and water retention, edema, and elevation of blood strain. However, opposed outcomes are likely only in sufferers with extra danger components: superior age, preexisting renal dysfunction, hypovolemia, hypertension, hepatic cirrhosis, or heart failure. Long-term aspirin use could result in renal papillary necrosis and other types of renal injury. Use of aspirin throughout labor and delivery can suppress spontaneous uterine contractions, induce untimely closure of the ductus arteriosus, and intensify uterine bleeding. Aspirin can cause hypersensitivity reactions, particularly in adults with asthma, rhinitis, and nasal polyps. Hepatic necrosis from acetaminophen overdose results from accumulation of a poisonous metabolite. Risk is elevated by undernourishment, alcohol consumption, and preexisting liver disease. Chronic alcohol consumption increases the chance of liver damage from acetaminophen overdose, but in all probability not from therapeutic doses. Two main mechanisms are involved: induction of cytochrome P450 (which will increase manufacturing of the toxic metabolite of acetaminophen) and depletion of glutathione stores (which reduces cleansing of the metabolite). Acetaminophen might improve the risk of warfarin-induced bleeding by inhibiting the metabolism of warfarin. Ongoing Evaluation and Interventions Minimizing Adverse Effects Gastrointestinal Effects. Aspirin promotes bleeding by causing irreversible suppression of platelet aggregation. Specifically, low-dose aspirin should be discontinued in � Patients thought of at low risk of a cardiovascular occasion who require noncardiac surgery. Dosing ought to cease 7 to 10 days earlier than surgical procedure, and can resume 24 hours after the process. Exercise caution when utilizing aspirin in conjunction with warfarin, heparin, and different anticoagulants. Avoid aspirin in sufferers with bleeding problems (eg, hemophilia, vitamin K deficiency, hypoprothrombinemia). The nonacetylated salicylates-sodium salicylate, magnesium salicylate, and salsalate-have minimal effects on platelet aggregation. Accordingly, these drugs are most popular to be used in surgical patients and patients with bleeding issues. Monitor high-risk patients for indications of renal impairment (reduced urine output, weight gain despite diuretic remedy, speedy elevation of serum creatinine and blood urea nitrogen). Hypersensitivity reactions are most probably in adults with a history of bronchial asthma, rhinitis, and nasal polyps. If a severe hypersensitivity response happens, parenteral epinephrine is the treatment of alternative. Educate patients about manifestations of salicylism withheld until symptoms subside, after which remedy can resume however at a slightly lowered dosage.

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Accordingly, ladies must carefully weigh the dangers and advantages before selecting this drug. Table 75�6 reveals the methods during which estrogen and raloxifene are alike and different. Preparations, Dosage, and Administration Raloxifene [Evista] is available in 60-mg oral tablets. Women taking raloxifene to prevent or treat postmenopausal osteoporosis should ensure adequate consumption of calcium and vitamin D. The drug has two actions: It (1) will increase bone resorption by osteoclasts, and (2) will increase bone deposition by osteoblasts. The internet effect-resorption or deposition-depends on how the drug is run. Adverse effects included nausea, headache, arthralgias, again ache, and leg cramps. Temporary will increase in serum ranges of calcium, magnesium, and uric acid may happen. To date, cancer has only occurred in animal research and has not been detected in people. Teriparatide [Forteo] is supplied in particular prefilled pen injectors that comprise 600 mcg/2. For all indications, the really helpful dosage is 20 mcg as soon as every day by subQ injection into the anterior thigh or abdomen. Each pen can be used up to 28 days after the first injection, after which it ought to be discarded, even when some drug remains. Patients ought to store the pens cold-2�C to 8�C (36�F to 46�F)-but not frozen, and will take them out of the chilly solely to make an injection. The value for each syringe (a 28-day supply) is over $1500, so therapy prices may be very costly. Dosage is way larger in patients with bone metastases than in patients with osteoporosis, and hence unwanted side effects are more severe in patients with bone metastases. Denosumab was tested in a 3-year examine that enrolled 7868 postmenopausal ladies with osteoporosis. Compared with the ladies who received placebo injections, those who got denosumab had 68% fewer vertebral fractures, 40% fewer hip fractures, and 20% fewer fractures at other sites (wrist, leg, or shoulder). Taken together, these knowledge counsel that denosumab is equal to bisphosphonates for treating postmenopausal osteoporosis. Efficacy was evaluated by comparing denosumab with zoledronate (a bisphosphonate) in three double-blind trials that enrolled 5723 sufferers. One trial enrolled patients with breast cancer, one enrolled patients with prostate cancer, and one enrolled patients with other cancers, together with a number of myeloma, kidney cancer, small cell lung most cancers, and non�small cell lung most cancers. With monthly injections (as used for most cancers patients), denosumab ranges attain plateau in 6 months. Adverse Effects In postmenopausal women with osteoporosis, the most common opposed results are back pain, ache in the extremities, musculoskeletal pain, hypercholesterolemia, and urinary bladder infection. In most cancers patients with bone metastases, the most typical antagonistic results are fatigue, hypophosphatemia, and nausea. Denosumab can exacerbate preexisting hypocalcemia, presumably by reducing osteoclast activity. The threat of hypocalcemia is elevated in patients with impaired renal perform (including those on dialysis) and sufferers with different danger factors (eg, a historical past of hypoparathyroidism, thyroid surgical procedure, malabsorption syndromes, or excision of the small intestine). The manufacturer recommends monitoring ranges of calcium, magnesium, and phosphorus on this at-risk group. Denosumab increases the risk of serious infections, though the absolute danger is low. In clinical trials, some sufferers developed endocarditis, serious pores and skin infections, and infections of the stomach, urinary tract, and ear. Patients who develop signs of extreme infection should seek instant medical attention.

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Atorvastatin/Amlodipine [Caduet] Atorvastatin and amlodipine (a calcium channel blocker) are available in fixed-dose mixture tablets under the trade name Caduet. This is the primary single product indicated for dyslipidemia mixed with hypertension and/ or angina. The combination has one benefit over taking every drug individually: fewer drugs to swallow. Dosage is individualized on the premise of therapeutic response and tolerance of opposed results. The pharmacology of amlodipine and different calcium channel blockers is mentioned in Chapter forty five. Simvastatin and extended-release niacin can be found in fixed-dose combos offered as Simcor. The most common unwanted effects of Simcor, whatever the dose, are flushing, pruritus, and headache. Simcor tablets can be found in five simvastatin/niacin strengths: 20/500 mg, 40/500, 20/750 mg, 20/1000 mg, and 40/1000 mg. Dosing with a low-fat snack is recommended to scale back the incidence and severity of niacin-related abdomen upset. If needed and tolerated, the daily niacin dose may be steadily elevated to 2000 mg (with 40 mg of simvastatin). Simvastatin/Sitagliptin [Juvisync] Simvastatin and sitagliptin (a drug for reducing blood glucose) can be found in fixed-dose mixtures bought as Juvisync. This is the first single product indicated for dyslipidemia mixed with diabetes. Major adverse results of sitagliptin are pancreatitis and hypersensitivity reactions. Juvisync tablets include 50 or a hundred mg of sitagliptin plus both 10, 20, or 40 mg of simvastatin. Ezetimibe and atorvastatin can be found in fixeddose combos sold as Liptruzet. The product has two indications: major (familial and nonfamilial) hyperlipidemia and blended hyperlipidemia. Liptruzet is available in four ezetimibe/atorvastatin strengths: 10/10 mg, 10/20 mg, 10/40 mg, and 10/80 mg. The beneficial preliminary dosage is 10/10 mg or 10/20 mg as soon as a day with or with out meals. Simvastatin and ezetimibe are available in fixeddose combination tablets sold as Vytorin. Following its approval in 2004, the product rapidly grew to become considered one of our "top 10" most-prescribed medication. Because ezetimibe has a unique mechanism of action than simvastatin, the mixture can decrease ldl cholesterol more successfully than simvastatin alone. With this mixture, the dose of simvastatin required to effectively decrease cholesterol could also be lower than the dose required when simvastatin is used alone. Additional benefits of the mixture are convenience (take just one capsule instead of two) and lowered cost (the combination costs lower than both drugs bought separately). Despite the benefits of Vytorin, some authorities are concerned that the mixture may be less helpful than simvastatin alone. Unfortunately, current studies have revealed that consuming fish oil supplies no advantage in prevention of heart illness in high-risk populations. Two good sources are the Benecol brand of margarine, and delicate spreads sold under the trade name Promise. Both compounds are long-chain, omega-3 polyunsaturated fatty acids, with a methyl group at one finish and a carboxyl group at the other. Benefits of decrease doses (850 mg to 1 gm) could outcome from decreasing platelet aggregation; decreasing thrombosis (by effects on platelets and the vascular endothelium); lowering irritation (which could assist stabilize atherosclerotic plaques); and lowering blood stress and cardiac dysrhythmias. As the evidence is so new regarding lack of benefit in primary prevention of coronary heart illness, the American Heart Association still recommends eating no much less than two servings of fish a week. Methylmercury can cause coronary heart illness as nicely as neurologic harm, manifesting as tremor, numbness, tingling, altered imaginative and prescient, and impaired concentration.

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Yasmin, 64 years: To decrease blood loss during childbirth and elective surgery, high-dose aspirin must be discontinued a minimum of 1 week before these procedures. The pharmacology of amlodipine and different calcium channel blockers is discussed in Chapter 45.

Georg, 44 years: Since preeclampsia can deteriorate rapidly, with grave penalties for the patient and fetus, immediate supply is really helpful. With improved analysis and care, many hospitalizations could be prevented, high quality of life could be improved, and life expectancy might be prolonged.

Oelk, 30 years: If carbohydrate consumption is simply too nice or too small with respect to insulin dosage, hyperglycemia or hypoglycemia will outcome. To accomplish this, the drug is formulated in a capsule that contains protecting enteric-coated granules.

Flint, 29 years: However, correct symptomatic therapy can improve consolation and cut back or stop some crippling effects. As with B12 deficiency, the most prominent consequence of folate deficiency is megaloblastic anemia.

Treslott, 52 years: Effects start 2 hours after the primary dose, and plateau after 3 to 7 days of treatment. In solution, every molecule of aminophylline dissociates to yield two molecules of theophylline.

Thorek, 41 years: Achieving glucose management requires diligence on the part of the mom and her prescriber. Symptoms embody continual cough, excessive sputum manufacturing, wheezing, dyspnea, and poor train tolerance.

Hatlod, 25 years: Hence, they differ from the heparin-like anticoagulants, which inhibit thrombin indirectly (by enhancing the activity of antithrombin). The capsules may be swallowed intact, or their contents could also be dissolved in water and swallowed instantly.

Vandorn, 28 years: Patients should be knowledgeable about signs of liver injury-abdominal pain, fatigue, darkish urine, and jaundice-and suggested to report them instantly. The raw materials that allow elevated gluconeogenesis are the amino acids and fatty acids produced by metabolic breakdown of proteins and fats.

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