Introduction
Background
Chronic kidney disease (CKD) is a worldwide public health problem and is now recognized as a common condition that is associated with an increased risk of cardiovascular disease and chronic renal failure (CRF).
The Kidney Disease Outcomes Quality Initiative (K/DOQI) of the National Kidney Foundation (NKF) defines chronic kidney disease as either kidney damage or a decreased kidney glomerular filtration rate (GFR) of less than 60 mL/min/1.73 m2 for 3 or more months. Whatever the underlying etiology, the destruction of renal mass with irreversible sclerosis and loss of nephrons leads to a progressive decline in GFR. The different stages of chronic kidney disease form a continuum in time; prior to February 2002, no uniform classification of the stages of chronic kidney disease existed. At that time, K/DOQI published a classification of the stages of chronic kidney disease, as follows:
* Stage 1: Kidney damage with normal or increased GFR (>90 mL/min/1.73 m2)
* Stage 2: Mild reduction in GFR (60-89 mL/min/1.73 m2)
* Stage 3: Moderate reduction in GFR (30-59 mL/min/1.73 m2)
* Stage 4: Severe reduction in GFR (15-29 mL/min/1.73 m2)
* Stage 5: Kidney failure (GFR <15 mL/min/1.73 m2 or dialysis)
In stage 1 and stage 2 chronic kidney disease, GFR alone does not clinch the diagnosis. Other markers of kidney damage, including abnormalities in the composition of blood or urine or abnormalities in imaging tests, should also be present in establishing a diagnosis of stage 1 and stage 2 chronic kidney disease.
The K/DOQI definition and the classification of chronic kidney disease allow better communication and intervention at the different stages.
Pathophysiology
Approximately 1 million nephrons are present in each kidney, each contributing to the total GFR. Regardless of the etiology of renal injury, with progressive destruction of nephrons, the kidney has an innate ability to maintain GFR by hyperfiltration and compensatory hypertrophy of the remaining healthy nephrons. This nephron adaptability allows for continued normal clearance of plasma solutes so that substances such as urea and creatinine start to show significant increases in plasma levels only after total GFR has decreased to 50%, when the renal reserve has been exhausted. The plasma creatinine value will approximately double with a 50% reduction in GFR. A rise in plasma creatinine from a baseline value of 0.6 mg/dL to 1.2 mg/dL in a patient, although still within the reference range, actually represents a loss of 50% of functioning nephron mass.
The residual nephron hyperfiltration and hypertrophy, although beneficial for the reasons noted, has been hypothesized to represent a major cause of progressive renal dysfunction. This is believed to occur because of increased glomerular capillary pressure, which damages the capillaries and leads initially to focal and segmental glomerulosclerosis and eventually to global glomerulosclerosis. This hypothesis has been based on studies of five-sixths nephrectomized rats, which develop lesions that are identical to those observed in humans with chronic kidney disease.
Factors other than the underlying disease process and glomerular hypertension that may cause progressive renal injury include the following:
* Systemic hypertension
* Acute insults from nephrotoxins or decreased perfusion
* Proteinuria
* Increased renal ammoniagenesis with interstitial injury
* Hyperlipidemia
* Hyperphosphatemia with calcium phosphate deposition
* Decreased levels of nitrous oxide
* Smoking
Frequency
United States
In the United States, there is a rising incidence and prevalence of kidney failure, with poor outcomes and high cost. Kidney disease is the ninth leading cause of death in the United States. Data from the United States Renal Data System (USRDS) indicated that there has been an increase of 104% in the prevalence of chronic renal failure (CRF) between the years 1990-2001. There is an even higher prevalence of the earlier stages of chronic kidney disease.
According to the Third National Health and Nutrition Examination Survey, it was estimated that 6.2 million people (ie, 3% of total US population) older than 12 years had a serum creatinine value above 1.5 mg/dL; 8 million people had a glomerular filtration rate (GFR) of less than 60 mL/min, the majority of them being in the Medicare senior population (5.9 million people). Therefore, for the first time, the US Surgeon General's mandate for America's citizenry, Healthy People 2010, contains a chapter focused on chronic kidney disease. The objectives of this chapter are to articulate goals and to provide strategies to reduce the incidence, morbidity, mortality, and health costs of chronic kidney disease in the United States. The burden of chronic kidney disease can be assessed by multiple criteria, all of which underscore the need for improved detection, treatment, and monitoring of clinical and fiscal outcomes. Reducing renal failure will require additional public health efforts, including effective preventive strategies and early detection and treatment of chronic kidney disease.
Because of the nonuniform definition of kidney disease prior to February 2002, among other factors, most patients with earlier stages of chronic kidney disease have not been recognized or adequately treated. The Third National Health and Examination Survey (NHANES III) estimated that the prevalence of chronic kidney disease in adults in the United States was 11% (19.2 million): 3.3% (5.9 million) had stage 1, 3% (5.3 million) had stage 2, 4.3% (7.6 million) had stage 3, 0.2% (400,000) had stage 4, and 0.2% (300,000) had stage 5.
Furthermore, the prevalence of chronic kidney disease stages 1-4 increased from 10% in 1988-1994 to 13.1% in 1999-2004. This increase is partially explained by the increase in the prevalence of diabetes and hypertension, the two most common causes of chronic kidney disease.
International
The incidence rates of end-stage renal disease (ESRD) have increased steadily internationally since 1989. The United States has the highest incident rate of ESRD, followed by Japan. Japan has the highest prevalence per million population, with the United States taking second place.
Mortality/Morbidity
Chronic kidney disease is a major cause of morbidity and mortality, particularly at the later stages. Although the diabetic population is at highest risk, in the United States, the general hemodialysis and peritoneal dialysis populations have 2 hospital admissions per patient per year; patients who have a renal transplant have an average of 1 hospital admission per year. The 5-year survival rate for a patient undergoing chronic dialysis in the United States is approximately 35%. This is approximately 25% in patients with diabetes. The most common cause of death in the dialysis population is cardiovascular disease.
Among patients with ESRD aged 65 years and older, the mortality rates are 6 times higher than in the general population. In 2003, over 69,000 dialysis patients enrolled in the ESRD program died (annual adjusted mortality rate of 210.7 per 1000 patient-years at risk for the dialysis population, which represents a 14% decrease since peaking at 244.5 per 1000 patient-years in 1988). The highest mortality rate is within the first 6 months of initiating dialysis, which then tends to improve over the next 6 months, before increasing gradually over the next 4 years.
The mortality rates associated with hemodialysis are striking and indicate that the life expectancy of patients entering into hemodialysis is markedly shortened. At every age, patients with ESRD on dialysis have significantly increased mortality when compared with nondialysis patients and individuals without kidney disease. At age 60 years, a healthy person can expect to live for more than 20 years, whereas the life expectancy of a 60-year-old patient starting hemodialysis is closer to 4 years.
Race
Chronic kidney disease affects all races, but, in the United States, a significantly higher incidence of ESRD exists in blacks as compared to whites; the incident rate for blacks is nearly 4 times that for whites.
Choi et al found that rates of end-stage renal disease among black patients exceeded those among white patients at all levels of baseline estimated glomerular filtration rate (eGFR).1 Similarly, mortality rates among black patients were equal to or higher than those among white patients at all levels of eGFR. Risk of end-stage renal disease among black patients was highest at an eGFR of 45-59 mL/min/1.73 m2 (hazard ratio, 3.08), as was the risk of mortality (hazard ratio, 1.32).
Sex
In NHANES III, the distribution of estimated GFRs for the chronic kidney disease stages was similar in both sexes. Nonetheless, the USRDS 2004 Annual Data Report reveals that the incident rate of ESRD cases is higher for males with 409 per million population in 2002 compared to 276 for females.
Age
Chronic kidney disease is found in persons of all ages. The normal annual mean decline in the GFR with age from the peak GFR (approximately 120 mL/min/1.73 m2) attained during the third decade of life is approximately 1 mL/min/y/1.73 m2, reaching a mean value of 70 mL/min/1.73 m2 at age 70 years. Nonetheless, in the United States, the highest incidence rate of ESRD occurs in patients older than 65 years. As per NHANES III data, the prevalence of chronic kidney disease was 37.8% among patients older than 70 years. Besides diabetes mellitus and hypertension, age is an independent major predictor of chronic kidney disease. The geriatric population is the most rapidly growing kidney failure (chronic kidney disease stage 5) population in the United States.
The biologic process of aging initiates various structural and functional changes within the kidney. Renal mass progressively declines with advancing age. Glomerulosclerosis leads to a decrease in renal weight. Histologic examination is notable for a decrease in glomerular number of as much as 30-50% by age 70 years.
Ischemic obsolescence of cortical glomeruli is predominant, with relative sparing of the renal medulla. Juxtamedullary glomeruli see a shunting of blood from the afferent to efferent arterioles, resulting in redistribution of blood flow favoring the renal medulla. These anatomical and functional changes in renal vasculature appear to contribute to an age-related decrease in renal blood flow. Renal hemodynamic measurements in aged human and animals suggest that altered functional response of the renal vasculature may be an underlying factor in diminished renal blood flow and increased filtration noted with progressive renal aging. The vasodilatory response is blunted in the elderly when compared to younger patients.
However, the vasoconstrictor response to intrarenal angiotensin is identical in both young and older human subjects. A blunted vasodilatory capacity with appropriate vasoconstrictor response may indicate that the aged kidney is in a state of vasodilatation to compensate for the underlying sclerotic damage.
Given the histologic evidence for nephronal senescence with age, a decline in the GFR is expected. However, a wide variation in the rate of decline in the GFR is reported because of measurement methods, race, gender, genetic variance, and other risk factors for renal dysfunction. Because of these anatomical and physiological changes, elderly patients with chronic kidney disease may behave differently, in terms of progression and response to pharmacological treatment, than younger patients.
Therefore, a serum creatinine value of 1.2 mg/dL in a 70-kg, 25-year-old man versus a 70-kg, 80-year-old man represents an eGFR of 74 mL/min/1.73m2 and 58 mL/min/1.73m2, respectively. What can appear as only mild renal impairment in a 70-kg, 80-year-old man with a pathologically elevated serum creatinine of 2 mg/dL actually represents severe renal impairment when the eGFR is calculated to be 32 mL/min/1.73m2. Therefore, an eGFR must be determined simply by using the Modification of Diet in Renal Disease (MDRD) equation (see Other Tests) in elderly people so that appropriate drug dosing adjustments can be made and nephrotoxins can be avoided in patients who have more extensive chronic kidney disease than would be suggested by the serum creatinine value alone.
Clinical
History
Patients with chronic kidney disease stages 1-3 (GFR >30 mL/min) are generally asymptomatic and do not experience clinically evident disturbances in water or electrolyte balance or endocrine/metabolic derangements. Generally, these disturbances clinically manifest with chronic kidney disease stages 4-5 (GFR <30 mL/min). Uremic manifestations in patients with chronic kidney disease stage 5 are believed to be primarily secondary to an accumulation of toxins, the identity of which is generally not known.
The ability to maintain potassium (K) excretion at near normal levels is generally maintained in chronic kidney disease patients as long as both aldosterone secretion and distal flow are maintained. Another defense against potassium retention in patients with chronic kidney disease is increased potassium excretion in the GI tract, which also is under control of aldosterone.
Therefore, hyperkalemia usually develops when the GFR falls to less than 20-25 mL/min because of the decreased ability of the kidneys to excrete potassium. It can be observed sooner in patients who ingest a potassium-rich diet or if serum aldosterone levels are low, such as in type IV renal tubular acidosis commonly observed in people with diabetes or with use of angiotensin-converting enzyme (ACE) inhibitors or nonsteroidal anti-inflammatory drugs (NSAIDs). Hyperkalemia in chronic kidney disease can be aggravated by an extracellular shift of potassium, such as that occurs in the setting of acidemia or from lack of insulin. Hypokalemia is uncommon but can develop among patients with very poor intake of potassium, gastrointestinal or urinary loss of potassium, diarrhea, or diuretic use.
Metabolic acidosis often is mixed, normal anion gap and increased anion gap, the latter observed generally with chronic kidney disease stage 5 but with the anion gap generally not higher than 20 mEq/L. In chronic kidney disease, the kidneys are unable to produce enough ammonia in the proximal tubules to excrete the endogenous acid into the urine in the form of ammonium.
In chronic kidney disease stage 5, accumulation of phosphates, sulphates, and other organic anions are the cause of the increase in anion gap. Metabolic acidosis has been shown to have deleterious effects on protein balance, leading to a negative nitrogen balance, increased protein degradation, increased essential amino acid oxidation, reduced albumin synthesis, and a lack of adaptation to a low protein diet. Hence, this is associated with protein-energy malnutrition, loss of lean body mass, and muscle weakness. The mechanism for reducing protein may include effects on ATP-dependent ubiquitin proteasomes and increased activity of branched chain keto acid dehydrogenases.
In the NHANES III prevalence study, hypoalbuminemia (a marker of protein-energy malnutrition and a powerful predictive marker of mortality in dialysis patients as well as in the general population) was independently associated with low bicarbonate as well as the inflammatory marker C reactive protein. Metabolic acidosis is a factor in the development of renal osteodystrophy, as bone acts as a buffer for excess acid, with resultant loss of mineral. Acidosis may interfere with vitamin D metabolism, and patients who are persistently more acidotic are more likely to have osteomalacia or low-turnover bone disease.
The evidence for the benefits and risks of correcting metabolic acidosis is very limited, with no randomized controlled trials in pre-ESRD patients, none in children, and only 3 small trials in dialysis patients. These trials suggest that there may be some beneficial effects on both protein metabolism and bone metabolism, but the trials were underpowered to provide robust evidence. Experts recommend alkali therapy to maintain the serum bicarbonate concentration above 22 mEq/L.
Inflammation and hemostasis may increase the risk of kidney function decline, but prospective studies are lacking. The Atherosclerosis Risk in Communities (ARIC) Study, a prospective observational cohort, observed markers of inflammation and hemostasis in 14,854 middle-aged adults.2 The risk for decreased kidney function associated with the inflammatory and hemostasis markers was examined, using data from 1787 cases of chronic kidney disease (CKD) that developed between 1987 and 2004.
After adjustments for various factors, such as demographics smoking, blood pressure, diabetes, lipid levels, prior myocardial infarction (MI), antihypertensive use, and alcohol use, the above study revealed that the risk for chronic kidney disease rose with increasing quartiles of white blood cell (WBC) count, fibrinogen, von Willebrand factor, and factor VIIIc. The investigators found a strong inverse association between serum albumin level and chronic kidney disease risk. The study's findings suggested that inflammation and hemostasis are antecedent pathways for chronic kidney disease.
Salt and water handling by the kidney is altered in patients with chronic kidney disease. Extracellular volume expansion and total-body volume overload results from failure of sodium and free water excretion. This generally becomes clinically manifested when the GFR falls to less than 10-15 mL/min, when compensatory mechanisms have become exhausted. As kidney function declines further, sodium retention and extracellular volume expansion lead to peripheral and, not uncommonly, pulmonary edema and hypertension. At a higher GFR, excess sodium and water intake could result in a similar picture if the ingested amounts of sodium and water exceed the available potential for compensatory excretion.
Normochromic normocytic anemia principally develops from decreased renal synthesis of erythropoietin, the hormone responsible for bone marrow stimulation for red blood cell (RBC) production. It starts early in the course of disease and becomes more severe as the GFR progressively decreases with the availability of less viable renal mass. No reticulocyte response occurs. RBC survival is decreased, and tendency of bleeding is increased from the uremia-induced platelet dysfunction. Other causes of anemia in chronic kidney disease patients include chronic blood loss, secondary hyperparathyroidism, inflammation, nutritional deficiency, and accumulation of inhibitors of erythropoiesis.
Anemia is associated with fatigue, reduced exercise capacity, impaired cognitive and immune function, and reduced quality of life. Anemia is also associated with the development of cardiovascular disease, the new onset of heart failure, or the development of more severe heart failure. Anemia is associated with increased cardiovascular mortality.
Renal bone disease is a common complication of chronic kidney disease and results in both skeletal complications (eg, abnormality of bone turnover, mineralization, linear growth) and extraskeletal complications (eg, vascular or soft tissue calcification). Different types of bone disease occur with chronic kidney disease, as follows: (1) high turnover bone disease due to high parathyroid hormone (PTH) levels; (2a) low turnover bone disease (adynamic bone disease); (2b) defective mineralization (osteomalacia); (3) mixed disease; and (4) beta-2-microglobulin associated bone disease.
Secondary hyperparathyroidism develops because of hyperphosphatemia, hypocalcemia, decreased renal synthesis of 1,25-dihydroxycholecalciferol (1,25-dihydroxyvitamin D, or calcitriol), intrinsic alteration in the parathyroid gland that give rises to increased PTH secretion as well as increased parathyroid growth, and skeletal resistance to PTH.
Calcium and calcitriol are primary feedback inhibitors; hyperphosphatemia is a stimulus to PTH synthesis and secretion.
Phosphate retention begins in early chronic kidney disease; when the GFR falls, less phosphate is filtered and excreted, but serum levels do not rise initially because of increased PTH secretion, which increases renal excretion. As the GFR falls toward chronic kidney disease stages 4-5, hyperphosphatemia develops from the inability of the kidneys to excrete the excess dietary intake. Hyperphosphatemia suppresses the renal hydroxylation of inactive 25-hydroxyvitamin D to calcitriol, so serum calcitriol levels are low when the GFR is less than 30 mL/min. Increased phosphate concentration also effects PTH concentration by its direct effect on parathyroid gland (posttranscriptional effect).
Hypocalcemia develops primarily from decreased intestinal calcium absorption because of low plasma calcitriol levels and possibly from calcium binding to elevated serum levels of phosphate.
Low serum calcitriol levels, hypocalcemia, and hyperphosphatemia have all been demonstrated to independently trigger PTH synthesis and secretion. As these stimuli persist in chronic kidney disease, particularly in the more advanced stages, PTH secretion becomes maladaptive and the parathyroid glands, which initially hypertrophy, become hyperplastic. The persistently elevated PTH levels exacerbate hyperphosphatemia from bone resorption of phosphate.
If serum levels of PTH remain elevated, a high bone turnover lesion, known as osteitis fibrosa, develops. This is one of several bone lesions, which as a group are commonly known as renal osteodystrophy. These lesions develop in patients with severe chronic kidney disease and are common in those with ESRD.
The prevalence of adynamic bone disease in the United States has increased, and it has been described before the initiation of dialysis in some cases. The pathogenesis of adynamic bone disease is not well defined, but several factors may contribute, including high calcium load, use of vitamin D sterols, increasing age, previous corticosteroid therapy, peritoneal dialysis, and increased level of N-terminally truncated PTH fragments. Low turnover osteomalacia in the setting of chronic kidney disease is associated with aluminum accumulation and is markedly less common. Dialysis-related amyloidosis from beta-2-microglobulin accumulation in patients who have required chronic dialysis for at least 8-10 years is another form of bone disease that manifests with cysts at the ends of long bones.
Other manifestations of uremia in ESRD, many of which are more likely in patients who are inadequately dialyzed, include the following:
* Pericarditis - Can be complicated by cardiac tamponade, possibly resulting in death.
* Encephalopathy - Can progress to coma and death
* Peripheral neuropathy
* Restless leg syndrome
* GI symptoms - Anorexia, nausea, vomiting, diarrhea
* Skin manifestations - Dry skin, pruritus, ecchymosis
* Fatigue, increased somnolence, failure to thrive
* Malnutrition
* Erectile dysfunction, decreased libido, amenorrhea
* Platelet dysfunction with tendency to bleeding
Physical
The physical examination often is not very helpful but may reveal findings characteristic of the condition underlying chronic kidney disease (eg, lupus, severe arteriosclerosis, hypertension) or complications of chronic kidney disease (eg, anemia, bleeding diathesis, pericarditis).
Causes
Causes include the following:
* Vascular disease - Renal artery stenosis, cytoplasmic pattern antineutrophil cytoplasmic antibody (C-ANCA)–positive and perinuclear pattern antineutrophil cytoplasmic antibody (P-ANCA)–positive vasculitides, antineutrophil cytoplasmic antibody (ANCA)–negative vasculitides, atheroemboli, hypertensive nephrosclerosis, renal vein thrombosis
* Primary glomerular disease - Membranous nephropathy, immunoglobulin A (IgA) nephropathy, focal and segmental glomerulosclerosis (FSGS), minimal change disease, membranoproliferative glomerulonephritis, rapidly progressive (crescentic) glomerulonephritis
* Secondary glomerular disease - Diabetes mellitus, systemic lupus erythematosus, rheumatoid arthritis, mixed connective tissue disease, scleroderma, Goodpasture syndrome, Wegener granulomatosis, mixed cryoglobulinemia, postinfectious glomerulonephritis, endocarditis, hepatitis B and C, syphilis, human immunodeficiency virus (HIV), parasitic infection, heroin use, gold, penicillamine, amyloidosis, light chain deposition disease, neoplasia, thrombotic thrombocytopenic purpura (TTP), hemolytic-uremic syndrome (HUS), Henoch-Schönlein purpura, Alport syndrome, reflux nephropathy
* Tubulointerstitial disease - Drugs (eg, sulfa, allopurinol), infection (viral, bacterial, parasitic), Sjögren syndrome, chronic hypokalemia, chronic hypercalcemia, sarcoidosis, multiple myeloma cast nephropathy, heavy metals, radiation nephritis, polycystic kidneys, cystinosis
* Urinary tract obstruction - Urolithiasis, benign prostatic hypertrophy, tumors, retroperitoneal fibrosis, urethral stricture, neurogenic bladderDifferential Diagnoses
Acute Renal Failure
Workup
Laboratory Studies
The following tests may be indicated:
* Serum electrolytes, BUN, and creatinine - The BUN and creatinine levels will be elevated in patients with chronic kidney disease. Hyperkalemia or low bicarbonate levels may be present in patients with chronic kidney disease.
* Serum calcium, phosphate, vitamin D, and intact parathyroid hormone (PTH) levels are obtained to look for evidence of renal bone disease.
* CBC count - Normochromic normocytic anemia is commonly seen in chronic kidney disease. Other underlying causes of anemia should be ruled out.
* Serum albumin - Patients may have hypoalbuminemia due to urinary protein loss or malnutrition.
* Lipid profile - A lipid profile should be performed in all patients with chronic kidney disease because of their increased risk of cardiovascular disease.
* Urinalysis - Dipstick proteinuria may suggest a glomerular or tubulointerstitial problem. The urine sediment finding of RBCs, RBC casts, suggests proliferative glomerulonephritis. Pyuria and/or WBC casts are suggestive of interstitial nephritis (particularly if eosinophiluria is present) or urinary tract infection.
* Spot urine collection for total protein-to-creatinine ratio allows reliable approximation (extrapolation) of total 24-hour urinary protein excretion. A value of greater than 2 g is considered to be within the glomerular range, and a value of greater than 3-3.5 g is within the nephrotic range; less than 2 is characteristic of tubulointerstitial problems.
* Twenty-four–hour urine collection for total protein and CrCl
In certain cases, the following tests may be ordered as part of the evaluation of patients with chronic kidney disease:
* Serum and urine protein electrophoresis to screen for a monoclonal protein possibly representing multiple myeloma
* Antinuclear antibodies (ANA), double-stranded DNA antibody levels to screen for systemic lupus erythematosus
* Serum complement levels - May be depressed with some glomerulonephritides
* C-ANCA and P-ANCA levels - Helpful if positive in diagnosis of Wegener granulomatosis and polyarteritis nodosa or microscopic polyangiitis, respectively
* Anti–glomerular basement membrane (anti-GBM) antibodies - Highly suggestive of underlying Goodpasture syndrome
* Hepatitis B and C, HIV, Venereal Disease Research Laboratory (VDRL) serology - Conditions associated with some glomerulonephritides
Imaging Studies
The following imaging studies may be indicated:
* Plain abdominal x-ray - Particularly useful to look for radio-opaque stones or nephrocalcinosis
* Intravenous pyelogram - Not commonly used because of potential for intravenous contrast renal toxicity; often used to diagnose renal stones
* Renal ultrasound - Small echogenic kidneys are observed in advanced renal failure. Kidneys usually are normal in size in advanced diabetic nephropathy, where affected kidneys initially are enlarged from hyperfiltration. Structural abnormalities, such as polycystic kidneys, also may be observed. This is a useful test to screen for hydronephrosis, which may not be observed in early obstruction, or involvement of the retroperitoneum with fibrosis, tumor, or diffuse adenopathy. Retrograde pyelogram may be indicated if a high index of clinical suspicion for obstruction exists despite a negative study finding.
* Renal radionuclide scan - Useful to screen for renal artery stenosis when performed with captopril administration but is unreliable for GFR of less than 30 cc/min; also quantitates differential renal contribution to total GFR
* CT scan - CT scan is useful to better define renal masses and cysts usually noted on ultrasound. Also, it is the most sensitive test for identifying renal stones. IV contrast-enhanced CT scans should be avoided in patients with renal impairment to avoid acute renal failure; this risk significantly increases in patients with moderate-to-severe chronic kidney disease. Dehydration also markedly increases this risk.
* MRI is very useful in patients who require a CT scan but who cannot receive intravenous contrast. It is reliable in the diagnosis of renal vein thrombosis, as are CT scan and renal venography. Magnetic resonance angiography also is becoming more useful for diagnosis of renal artery stenosis, although renal arteriography remains the criterion standard.
* Voiding cystourethrogram (VCUG) - Criterion standard for diagnosis of vesicoureteral reflux
Other Tests
The Cockcroft-Gault formula for estimating CrCl should be used routinely as a simple means to provide a reliable approximation of residual renal function in all patients with chronic kidney disease. The formulas are as follows:
* CrCl (male) = ([140-age] X weight in kg)/(serum creatinine X 72)
* CrCl (female) = CrCl (male) X 0.85
Alternatively, the Modification of Diet in Renal Disease (MDRD) Study equation could be used to calculate the GFR. This equation does not require a patient's weight.3
Procedures
Percutaneous renal biopsy is performed most often with ultrasound guidance and the use of a mechanical gun. It generally is indicated when renal impairment and/or proteinuria approaching the nephrotic range are present and the diagnosis is unclear after appropriate other workup. It is not indicated in the setting of small echogenic kidneys on ultrasound because these are severely scarred and represent chronic irreversible injury. The most common complication of this procedure is bleeding, which can be life threatening in a minority of occurrences.
Surgical open renal biopsy can be considered when the risk of renal bleeding is felt to be great, occasionally with solitary kidneys, or when percutaneous biopsy is technically difficult to perform.
Histologic Findings
Renal histology in chronic kidney disease reveals findings compatible with the underlying primary renal diagnosis and, generally, findings of segmental and globally sclerosed glomeruli and tubulointerstitial atrophy, often with tubulointerstitial mononuclear infiltrates.Treatment
Medical Care
The medical care of patients with chronic kidney disease should focus on the following:
Delaying or halting the progression of chronic kidney disease
Treatment of the underlying condition if possible is indicated.
Aggressive blood pressure control to target values per current guidelines is indicated. Systolic blood pressure control is considered more important and is also considered difficult to control in elderly patients with chronic kidney disease.
Use ACE inhibitors or angiotensin receptor blockers as tolerated, with close monitoring for renal deterioration and for hyperkalemia (avoid in advanced renal failure, bilateral renal artery stenosis [RAS], RAS in a solitary kidney). Data support the use of ACE inhibitors/angiotensin receptor blockers in diabetic kidney disease with or without proteinuria. However, in nondiabetic kidney disease, ACE inhibitors/angiotensin receptor blockers are effective in retarding the progression of disease among patients with proteinuria of less of than 500 mg/d.
Aggressive glycemic control per the American Diabetes Association (ADA) recommendations (target HbA1C <7%) is indicated.
Although the Modification of Diet in Renal Disease (MDRD) Study failed to show the effect of protein restriction in retardation of the progression of kidney disease, a meta-analysis suggests a beneficial role for protein restriction. The National Kidney Foundation (NKF) guidelines suggest that if a patient is started on protein restriction, the physician needs to closely monitor the patient's nutritional status. Predialysis low serum albumin is associated with a poor outcome among dialysis patients.
Treatment of hyperlipidemia to target levels per current guidelines is indicated.
Avoidance of nephrotoxins, including IV radiocontrast, nonsteroidal anti-inflammatory agents, and aminoglycosides is indicated.
Encourage smoking cessation, as smokers tend to reach ESRD earlier than nonsmokers.
De Brito-Ashurst et al studied whether bicarbonate supplementation preserves renal function in chronic kidney disease (CKD).4 Adult patients (n=134) with chronic kidney disease (ie, creatinine clearance [CrCl] 15-30 mL/min/1.73 m2 and serum bicarbonate 16-20 mmol/L) were randomly assigned to receive oral sodium bicarbonate supplementation or standard care for 2 years. A slower decline in CrCl was observed in the bicarbonate group than in the control group (1.88 vs 5.93 mL/min/1.73 m2; P <0.0001). Patients in the bicarbonate group were also less likely to experience rapid disease progression than were members of the control group (9% vs 45%; P <0.0001), and fewer patients who received bicarbonate supplementation developed ESRD (6.5% vs 33%; P <0.001). In addition to the benefits listed above, nutritional parameters improved with bicarbonate supplementation.
Treating the pathologic manifestations of chronic kidney disease
The following should be addressed:
* Anemia with erythropoietin, with the goal being 11-12 g/dL, as normalization of hemoglobin in patients with chronic kidney disease stages 4-5 has been associated with an increased risk of combined outcome. Before starting Epogen, iron stores should be checked, and the aim is to keep iron saturation at 30-50% and ferritin at 200-500.
* Hyperphosphatemia with dietary phosphate binders and dietary phosphate restriction
* Hypocalcemia with calcium supplements with or without calcitriol
* Hyperparathyroidism with calcitriol or vitamin D analogs
* Volume overload with loop diuretics or ultrafiltration
* Metabolic acidosis with oral alkali supplementation
* Uremic manifestations with chronic renal replacement therapy (hemodialysis, peritoneal dialysis, or renal transplantation): Indications include severe metabolic acidosis, hyperkalemia, pericarditis, encephalopathy, intractable volume overload, failure to thrive and malnutrition, peripheral neuropathy, intractable gastrointestinal symptoms, and the GFR less than 10 mL/min.
* Cardiovascular complications
Timely planning for chronic renal replacement therapy
Consider the following:
* Early education regarding natural disease progression, different dialytic modalities, renal transplantation, patient option to refuse or discontinue chronic dialysis
* Timely placement of permanent vascular access (arrange for surgical creation of primary arteriovenous fistula, if possible, and preferably at least 6 months in advance of anticipated date of dialysis)
* Timely elective peritoneal dialysis catheter insertion
* Timely referral for renal transplantation
Consultations
Consultations include the following:
* Early nephrology referral (decreases morbidity and mortality)
* Renal dietitian
* Vascular surgery for permanent vascular access
* General surgery for peritoneal catheter placement
* Referral to renal transplant center
Diet
Protein restriction early in chronic kidney disease as a means to delay a decline in the GFR is controversial; however, as the patient approaches chronic kidney disease stage 5, this is recommended to delay the onset of uremic symptoms. Patients with chronic kidney disease who already are predisposed to becoming malnourished are at higher risk for malnutrition with overly aggressive protein restriction. Malnutrition is a well-established predictor of increased morbidity and mortality in the ESRD population and must be avoided if possible.
Restriction of the following may also be indicated:
* Phosphate restriction starting early in chronic kidney disease
* Potassium restriction
* Sodium and water restriction as needed to avoid volume overload
See related CME at New Guidelines Address Nutritional Needs of Children With Chronic Kidney Disease.
Medication
Phosphate-lowering Agents
Hyperphosphatemia is treated with dietary phosphate binders and dietary phosphate restriction. Hypocalcemia is treated with calcium supplements and possibly calcitriol. Hyperparathyroidism is treated with calcitriol or vitamin D analogs.
A small trial (n=61) by Fishbane et al examined the effect of paricalcitol on protein excretion in patients with chronic kidney disease.5 In this double-blind, randomized study, more patients in the paricalcitol group achieved a 10% reduction in proteinuria than did members of the control group (57.1% vs 25.9%, respectively; P=0.03).
Calcium acetate (Calphron, PhosLo)
For treatment of hyperphosphatemia in chronic kidney disease. Combines with dietary phosphorus to form insoluble calcium phosphate, which is excreted in feces.
* Dosing
* Interactions
* Contraindications
* Precautions
Adult
1334 mg PO with each meal; increase to bring serum phosphate value to 6 mg/dL as long as hypercalcemia does not develop; may require as much as 2668 mg
Pediatric
Not established
* Dosing
* Interactions
* Contraindications
* Precautions
May increase effect of quinidine; may decrease effects of tetracyclines, atenolol, salicylates, iron salts, and fluoroquinolones; IV administration antagonizes effects of verapamil; large intakes of dietary fiber may decrease calcium absorption and levels
* Dosing
* Interactions
* Contraindications
* Precautions
Hypercalcemia; hypophosphatemia; renal calculi
* Dosing
* Interactions
* Contraindications
* Precautions
Pregnancy
C - Fetal risk revealed in studies in animals but not established or not studied in humans; may use if benefits outweigh risk to fetus
Precautions
Hypercalcemia or hypercalcuria may occur when therapeutic amounts are administered
Calcium carbonate (Caltrate, Oystercal)
For treatment of hyperphosphatemia or as a calcium supplement in chronic kidney disease. Successfully normalizes phosphate concentrations in patients with chronic kidney disease. Combines with dietary phosphate to form insoluble calcium phosphate, which is excreted in feces. Marketed in a variety of dosage forms and is relatively inexpensive.
* Dosing
* Interactions
* Contraindications
* Precautions
Adult
1-2 g PO divided bid/qid; with meals as a phosphorous binder; between meals as a calcium supplement
Pediatric
45-65 mg/kg/d PO divided qid
* Dosing
* Interactions
* Contraindications
* Precautions
May decrease effects of tetracyclines, atenolol, salicylates, iron salts, and fluoroquinolones; IV administration antagonizes effects of verapamil; large intakes of dietary fiber may decrease calcium absorption and levels
* Dosing
* Interactions
* Contraindications
* Precautions
Renal calculi; hypercalcemia; hypophosphatemia; digitalis toxicity
* Dosing
* Interactions
* Contraindications
* Precautions
Pregnancy
C - Fetal risk revealed in studies in animals but not established or not studied in humans; may use if benefits outweigh risk to fetus
Precautions
Hypercalcemia or hypercalcuria may occur when therapeutic amounts are administered
Calcitriol (Rocaltrol, Calcijex)
Used to suppress parathyroid production and secretion in secondary hyperparathyroidism and for treatment of hypocalcemia in chronic kidney disease by increasing intestinal calcium absorption.
* Dosing
* Interactions
* Contraindications
* Precautions
Adult
0.25 mcg PO qd/qod
0.5 mcg IV qd 3 times/wk
Increase at 4- to 8-wk intervals by 0.25-mcg/d to achieve target PTH level and to maintain serum calcium levels at 9-10 mg/dL
Pediatric
Initial: 15 ng/kg/d PO
Maintenance: 5-40 ng/kg/d PO
* Dosing
* Interactions
* Contraindications
* Precautions
Cholestyramine and colestipol decrease absorption; magnesium-containing antacids and thiazide diuretics can increase calcitriol effects
* Dosing
* Interactions
* Contraindications
* Precautions
Documented hypersensitivity; hypercalcemia; malabsorption syndrome
* Dosing
* Interactions
* Contraindications
* Precautions
Pregnancy
C - Fetal risk revealed in studies in animals but not established or not studied in humans; may use if benefits outweigh risk to fetus
Precautions
Adequate response to calcitriol in improving hypocalcemia depends on adequate dietary calcium intake; serum calcium phosphate product must not exceed 70 mg/dL to minimize metastatic tissue and blood vessel calcification; avoid hypercalcemia
Doxercalciferol (Hectorol)
A vitamin D analog (1-alpha-hydroxyergocalciferol) that does not require activation by the kidneys. Indicated for the treatment of secondary hyperparathyroidism in end-stage renal disease.
* Dosing
* Interactions
* Contraindications
* Precautions
Adult
10 mcg PO 3 times/wk at dialysis; adjust dose as needed to lower blood iPTH to 150-300 pg/mL; increase dose by 2.5 mcg/8 wk if iPTH is not lowered by 50% and fails to reach the target range; not to exceed 20 mcg/3 times/wk
Alternatively, 4 mcg IV 3 times/wk; may adjust dose by 1-2 mcg/8 wk to maintain iPTH levels
Pediatric
Not established
* Dosing
* Interactions
* Contraindications
* Precautions
Coadministration with drugs that impair absorption of fat soluble vitamins (eg, cholestyramine) may decrease doxercalciferol absorption; increases the risk of hypermagnesemia with magnesium-containing products (eg, antacids)
* Dosing
* Interactions
* Contraindications
* Precautions
Documented hypersensitivity; recent hypercalcemia or hyperphosphatemia
* Dosing
* Interactions
* Contraindications
* Precautions
Pregnancy
B - Fetal risk not confirmed in studies in humans but has been shown in some studies in animals
Precautions
May cause headache, malaise, dyspnea, or hypercalcemia; caution in renal osteodystrophy with hyperphosphatemia (potential for metastatic calcification)
Lanthanum carbonate (Fosrenal)
Noncalcium, nonaluminum phosphate binder indicated for reduction of high phosphorus levels in patients with end-stage renal disease. Directly binds dietary phosphorus in upper GI tract, thereby inhibiting phosphorus absorption.
* Dosing
* Interactions
* Contraindications
* Precautions
Adult
Initial: 250-500 mg PO tid pc (chewable tabs); adjust dose q2-3wk to target serum phosphorus level
Maintenance: 500-1000 mg PO tid pc
Pediatric
Not established
* Dosing
* Interactions
* Contraindications
* Precautions
Drugs known to interact with antacids (eg, alendronate, amprenavir, ciprofloxacin, itraconazole, tetracycline, thyroid hormones) should not be administered within 2 h
* Dosing
* Interactions
* Contraindications
* Precautions
Documented hypersensitivity; bowel obstruction; hypophosphatemia
* Dosing
* Interactions
* Contraindications
* Precautions
Pregnancy
C - Fetal risk revealed in studies in animals but not established or not studied in humans; may use if benefits outweigh risk to fetus
Precautions
Deposited into developing bone, including growth plate (long-term effects unknown); common adverse effects typically diminish over time but include headache, abdominal pain, nausea, diarrhea, constipation, and vomiting; in clinical trials, dialysis graft occlusion occurred more frequently than with placebo; caution with GI motility diseases (eg, Crohn disease, ulcerative colitis) or recent GI surgery
Sevelamer (Renagel)
Indicated for the reduction of serum phosphorous in patients with ESRD. Binds dietary phosphate in the intestine, thus inhibiting its absorption. In patients on hemodialysis, it decreases the frequency of hypercalcemic episodes relative to patients on calcium acetate treatment.
* Dosing
* Interactions
* Contraindications
* Precautions
Adult
Initial: 800-1600 mg PO tid with meals
Maintenance: Increase or decrease by 400-800 mg per meal q2wk to maintain serum phosphorous at 6 mg/dL or less
Pediatric
Not established
* Dosing
* Interactions
* Contraindications
* Precautions
None reported
* Dosing
* Interactions
* Contraindications
* Precautions
Documented hypersensitivity; bowel obstruction; hypophosphatemia
* Dosing
* Interactions
* Contraindications
* Precautions
Pregnancy
C - Fetal risk revealed in studies in animals but not established or not studied in humans; may use if benefits outweigh risk to fetus
Precautions
Caution in patients with dysphagia, severe GI tract motility disorders, or swallowing disorders; does not contain calcium or alkali supplementation (monitor serum calcium, bicarbonate, and chloride levels)
Paricalcitol (Zemplar)
For treatment of secondary hyperparathyroidism in ESRD. Reduces PTH levels, stimulates calcium and phosphorous absorption, and stimulates bone mineralization.
* Dosing
* Interactions
* Contraindications
* Precautions
Adult
0.04-0.1 mcg IV bolus 3 times/wk; adjust dose based on PTH levels
Pediatric
Not established
* Dosing
* Interactions
* Contraindications
* Precautions
Do not use phosphate or vitamin D-related compounds concomitantly with paricalcitol; caution if administered with digoxin (digitalis toxicity is potentiated by hypercalcemia)
* Dosing
* Interactions
* Contraindications
* Precautions
Documented hypersensitivity; hypercalcemia; vitamin D toxicity
* Dosing
* Interactions
* Contraindications
* Precautions
Pregnancy
C - Fetal risk revealed in studies in animals but not established or not studied in humans; may use if benefits outweigh risk to fetus
Precautions
Caution in breastfeeding; adverse effects include GI tract distress, dry mouth, lightheadedness, edema, chills, or fever
Growth Factors
Used to treat anemia of chronic kidney disease by stimulating RBC production.
Epoetin alfa (Epogen, Procrit)
Stimulates division and differentiation of committed erythroid progenitor cells. Induces release of reticulocytes from bone marrow into blood stream.
* Dosing
* Interactions
* Contraindications
* Precautions
Adult
50-150 U/kg IV/SC 3 times/wk
Pediatric
Not established
* Dosing
* Interactions
* Contraindications
* Precautions
None reported
* Dosing
* Interactions
* Contraindications
* Precautions
Documented hypersensitivity; uncontrolled hypertension
* Dosing
* Interactions
* Contraindications
* Precautions
Pregnancy
C - Fetal risk revealed in studies in animals but not established or not studied in humans; may use if benefits outweigh risk to fetus
Precautions
Caution in porphyria, hypertension, and history of seizures; decrease dose if hematocrit increase exceeds 4 U in any 2-wk period
Iron Salts
Nutritionally essential inorganic substances used to treat anemia.
Ferrous sulfate (Feosol, Feratab, Slow FE)
Used as a building block for hemoglobin synthesis in treating anemia of chronic kidney disease with erythropoietin.
* Dosing
* Interactions
* Contraindications
* Precautions
Adult
325 mg PO qd/tid
Pediatric
<15 kg: 5 mg/kg/d PO
15-30 kg: 160 mg PO qd
* Dosing
* Interactions
* Contraindications
* Precautions
Absorption is enhanced by ascorbic acid; interferes with tetracycline absorption; food and antacids impair absorption
* Dosing
* Interactions
* Contraindications
* Precautions
Documented hypersensitivity
* Dosing
* Interactions
* Contraindications
* Precautions
Pregnancy
A - Fetal risk not revealed in controlled studies in humans
Precautions
GI tract upset; iron toxicity is observed with ingestion of large amount and can be fatal, especially in children; parenteral (IV) administration may cause several reactions, including headaches, malaise, fever, generalized lymphadenopathy, arthralgia, and urticaria; can cause severe anaphylaxis; other reactions include phlebitis at infusion site
Iron dextran (DexFerrum, InFed)
Used to treat microcytic, hypochromic anemia resulting from iron deficiency when oral administration is unfeasible or ineffective.
Utilized to replenish iron stores in individuals on erythropoietin therapy who cannot take or tolerate oral iron supplementation.
A 0.5-mL (0.25 mL in children) test dose should be administered prior to starting therapy.
Available as 50 mg iron/mL (as dextran).
* Dosing
* Interactions
* Contraindications
* Precautions
Adult
>50 kg: 100 mg IV (2 mL); not to exceed 2 mL/d
Pediatric
5-10 kg: 50 mg IV (1 mL)
* Dosing
* Interactions
* Contraindications
* Precautions
Chloramphenicol-induced bone marrow toxicity may cause increased iron levels
* Dosing
* Interactions
* Contraindications
* Precautions
Documented hypersensitivity; anemias that are not involved with iron deficiency; hemochromatosis; hemolytic anemia; acute phase of infectious kidney disease
* Dosing
* Interactions
* Contraindications
* Precautions
Pregnancy
C - Fetal risk revealed in studies in animals but not established or not studied in humans; may use if benefits outweigh risk to fetus
Precautions
Monitor for allergic reactions (eg, flushing, hypotension, nausea)
Iron sucrose (Venofer)
Used to treat iron deficiency (in conjunction with erythropoietin) due to chronic hemodialysis. Iron deficiency is caused by blood loss during the dialysis procedure, increased erythropoiesis, and insufficient absorption of iron from the GI tract. Iron sucrose has shown a lower incidence of anaphylaxis than other parenteral iron products.
* Dosing
* Interactions
* Contraindications
* Precautions
Adult
5 mL (100 mg elemental iron) IV by slow injection or infusion during dialysis session; typically requires a minimum cumulative dose of 1000 mg of elemental iron over 10 consecutive dialysis sessions to achieve a favorable hemoglobin or hematocrit response; not to exceed 3 doses per wk
Pediatric
Not established
* Dosing
* Interactions
* Contraindications
* Precautions
Decreases bioavailability of orally administered iron
* Dosing
* Interactions
* Contraindications
* Precautions
Documented hypersensitivity; iron overload; anemia unrelated to iron deficiency
* Dosing
* Interactions
* Contraindications
* Precautions
Pregnancy
B - Fetal risk not confirmed in studies in humans but has been shown in some studies in animals
Precautions
May cause hypotension (related to IV administration rate or cumulative dose), cramps, headache, nausea, vomiting, diarrhea, or anaphylaxis
Ferric gluconate (Ferrlecit)
Replaces iron found in hemoglobin, myoglobin, and specific enzyme systems. Allows transportation of oxygen via hemoglobin.
* Dosing
* Interactions
* Contraindications
* Precautions
Adult
125 mg elemental iron/10 mL IV; may require cumulative dose of 1 g elemental iron to achieve favorable response in patients receiving hemodialysis
Pediatric
Not established
* Dosing
* Interactions
* Contraindications
* Precautions
Vitamin C may increase absorption of oral iron when administered concurrently; absorption of oral preparation of iron and tetracyclines decreased when administered concurrently; concurrent administration of H2 blockers or proton pump inhibitors may inhibit iron absorption
* Dosing
* Interactions
* Contraindications
* Precautions
Documented hypersensitivity; hemochromatosis; hemolytic anemia
* Dosing
* Interactions
* Contraindications
* Precautions
Pregnancy
B - Fetal risk not confirmed in studies in humans but has been shown in some studies in animals
Precautions
Flushing and transient hypotension may occur; may augment hemodialysis-induced hypotension
Ferumoxytol (Feraheme)
Indicated for iron replacement for iron deficiency anemia in adults with chronic kidney disease.
* Dosing
* Interactions
* Contraindications
* Precautions
Adult
510 mg IV once, then repeat 3-8 d later
May re-administer dose if iron deficiency anemia persists or reoccurs
Hemodialysis: Administer once blood pressure stable and patient has completed at least 1 h of hemodialysis
Pediatric
Not established
* Dosing
* Interactions
* Contraindications
* Precautions
May reduce absorption of concomitantly administered oral iron products
* Dosing
* Interactions
* Contraindications
* Precautions
Documented hypersensitivity; evidence of iron overload; anemia not caused by iron deficiency
* Dosing
* Interactions
* Contraindications
* Precautions
Pregnancy
C - Fetal risk revealed in studies in animals but not established or not studied in humans; may use if benefits outweigh risk to fetus
Precautions
Observe for signs and symptoms of hypersensitivity for at least 30 min following administration; may cause hypotension (monitor blood pressure during/following administration); monitor hematologic responses during therapy (do not administer if evidence of iron overload); can alter MRI studies
Common adverse effects (>2%) include diarrhea, nausea, dizziness, hypotension, constipation, and peripheral edema
Recombinant Human Erythropoietin
Stimulates development of erythroid progenitor cells.
Darbepoetin (Aranesp)
Erythropoiesis stimulating protein closely related to erythropoietin, a primary growth factor produced in kidney that stimulates development of erythroid progenitor cells. Mechanism of action is similar to that of endogenous erythropoietin, which interacts with stem cells to increase red cell production. Differs from epoetin alfa (recombinant human erythropoietin) in containing 5 N-linked oligosaccharide chains, whereas epoetin alfa contains 3. Has longer half-life than epoetin alfa (may be administered weekly or biweekly).
* Dosing
* Interactions
* Contraindications
* Precautions
Adult
0.45 mcg/kg IV/SC qwk initially; adjust dose (not to exceed 3 mcg/kg/wk) or frequency (eg, q2wk); to maintain target Hgb (not to exceed 12 g/dL); do not increase dose more frequently than qmo
Switching from epoetin alfa: Base dose on total weekly erythropoietin dose and frequency of administration
Pediatric
Not established
* Dosing
* Interactions
* Contraindications
* Precautions
None reported
* Dosing
* Interactions
* Contraindications
* Precautions
Documented hypersensitivity; uncontrolled hypertension
* Dosing
* Interactions
* Contraindications
* Precautions
Pregnancy
C - Fetal risk revealed in studies in animals but not established or not studied in humans; may use if benefits outweigh risk to fetus
Precautions
Elevation in Hgb > 1 g/dL/2wk increases risk of MI, neurologic events (eg, seizures, stroke) and exacerbations of hypertension, CHF, thrombosis, ischemia, and edema; adverse effects include infection, hypertension, hypotension, myalgia, headache, and diarrhea (some of adverse events may be due to chronic renal failure or dialysis); severe skin rash may occur (rare)
Calcimimetic Agents
These agents reduce parathyroid hormone levels.
Cinacalcet (Sensipar)
Directly lowers intact parathyroid hormone (iPTH) levels by increasing sensitivity of calcium sensing receptor on chief cell of parathyroid gland to extracellular calcium. Also results in concomitant serum calcium decrease. Indicated for secondary hyperparathyroidism in patients with chronic kidney disease on dialysis.
* Dosing
* Interactions
* Contraindications
* Precautions
Adult
30 mg PO qd initially; titrate upward slowly (no more frequent than q2-4wk intervals) by 30 mg increments to target iPTH of 150-300 pg/mL
Take with meals or immediately following; do not crush, chew or cut tablets
Pediatric
Not establishedFollow-up
Further Inpatient Care
Patients who develop potentially life-threatening complications of chronic kidney disease should be hospitalized and closely monitored.
Further Outpatient Care
Patients with chronic kidney disease should be referred to a nephrologist early in the course of their disease and have continued nephrologic follow-up until initiation of chronic renal replacement therapy.
A multidisciplinary approach to care, including involvement of the nephrologist, primary care physician, renal dietitian, nurse, and social worker, should be initiated early in the course of chronic kidney disease, with close patient follow-up.
Transfer
Patients with chronic kidney disease acutely presenting with indications for dialytic therapy should be transferred to a hospital center where acute dialysis can be performed.
Prognosis
Patients with chronic kidney disease generally progress to ESRD. The rate of progression depends on the underlying diagnosis, on the successful implementation of secondary preventative measures, and on the individual patient.
Patients on chronic dialysis have a high incidence of morbidity and mortality.
Patients with ESRD who undergo renal transplantation survive longer than those on chronic dialysis.
Patient Education
Patients with chronic kidney disease should be educated about the importance of compliance with secondary preventative measures, natural disease progression, prescribed medications (highlighting their potential benefits and adverse effects), avoidance of nephrotoxins, diet, chronic renal replacement modalities, including peritoneal dialysis, hemodialysis, and transplantation, and permanent vascular access options for hemodialysis.
For excellent patient education resources, visit eMedicine's Diabetes Center. Also, see eMedicine's patient education article Chronic Kidney Failure.
Miscellaneous
Medicolegal Pitfalls
Early diagnosis and treatment of the underlying cause or/and institution of secondary preventative measures in chronic kidney disease is imperative to try to delay, or possibly halt, progression. Early nephrologic referral is of extreme importance.
Timely initiation of chronic renal replacement therapy is imperative to prevent the uremic complications of chronic kidney disease that can lead to significant morbidity and death.
In chronic kidney disease, doses and intervals of drugs that are excreted or metabolized renally should be adjusted accordingly for the residual GFR. Some drugs are contraindicated in moderate-to-severe renal impairment because of potentially serious effects from drug or metabolite accumulation. Routine consultation of the appropriate references should be undertaken when prescribing any new drug to a patient with chronic kidney disease.
Special Concerns
Female patients with advanced chronic kidney disease commonly develop menstrual irregularities; women with ESRD are typically amenorrheic and infertile.
Pregnancy in chronic kidney disease can be associated with accelerated renal decline. In advanced chronic kidney disease and ESRD, pregnancy is associated with markedly decreased fetal survival.
Forty-five percent of patients with chronic kidney disease (CKD) have depressive symptoms at dialysis therapy initiation, as assessed using self-report scales. However, these scales may emphasize somatic symptoms, specifically, sleep disturbance, fatigue, and anorexia, that can coexist with chronic disease symptoms. Hedayati et al conducted a validation study to determine whether these scales could lead to overestimation of depression diagnosis.6 The study compared the Beck Depression Inventory (BDI) and the 16-item Quick Inventory of Depressive Symptomatology-Self Report (QIDS-SR(16)) with a gold-standard structured psychiatric interview in 272 patients with stage 2-5 chronic kidney disease who had not been treated with dialysis.
The above study's authors found the QIDS-SR(16) and the BDI to be effective screening tools, concluding that a score of 10 or 11, respectively, was the best cutoff score for identification of a major depressive episode in the study's patient population.
