oral calcium-based or other non-aluminum-containing phosphate binders and a low phosphate diet should be used to control serum phosphorus levels in patients undergoing dialysis. uncontrolled serum phosphorus exacerbates secondary hyperparathyroidism and can lessen the effectiveness of doxercalciferol injection in reducing blood pth levels. if hypercalcemia occurs after initiating doxercalciferol injection therapy, the dose of doxercalciferol injection and/or calcium-containing phosphate binders should be decreased. if hyperphosphatemia occurs after initiating doxercalciferol injection, the dose of doxercalciferol injection should be decreased and/or the dose of phosphate binders increased. (see dosing recommendations for doxercalciferol injection under dosage and administration .) magnesium-containing antacids and doxercalciferol injection should not be used concomitantly in patients on chronic renal dialysis because such use may lead to the development of hypermagnesemia. serious hypersensitivity reactions, including fatal outcome, have been reported post marketing in patients on hemodialysis following administration of doxercalciferol injection. hypersensitivity reactions include anaphylaxis with symptoms of angioedema (involving face, lips, tongue and airways), hypotension, unresponsiveness, chest discomfort, shortness of breath, and cardiopulmonary arrest. these reactions may occur separately or together. monitor patients receiving doxercalciferol injection upon initiation of treatment for hypersensitivity reactions. should a hypersensitivity reaction occur, discontinue doxercalciferol, monitor and treat if indicated (see contraindications ).

eases during doxercalciferol injection treatment underscore the importance of regular safety monitoring of serum calcium and phosphorus levels throughout treatment. patients with higher pre-treatment serum levels of calcium (> 10.5 mg/dl) or phosphorus (> 6.9 mg/dl) were more likely to experience hypercalcemia or hyperphosphatemia. therefore, doxercalciferol injection should not be given to patients with a recent history of hypercalcemia or hyperphosphatemia, or evidence of vitamin d toxicity. table 3: incidence rates of hypercalcemia and hyperphosphatemia in two phase 3 studies with doxercalciferol injection study hypercalcemia (per 100 patient weeks) hyperphosphatemia (per 100 patient weeks) washout (off treatment) open-label (treatment) washout (off treatment) open-label (treatment) study c 0.9 0.9 0.9 2.4 study d 0.3 1 1.2 3.7

er than 55 mg 2 /dl 2 is noted, the dose of doxercalciferol injection should be decreased or suspended and/or the dose of phosphate binders should be appropriately adjusted. if suspended, the drug should be restarted at a dose that is 1 mcg lower. dosing must be individualized and based on ipth levels with monitoring of serum calcium and serum phosphorus levels. table 5 presents a suggested approach in dose titration: table 5: initial dosing ipth level doxercalciferol injection dose > 400 pg/ml 4 mcg 3 times per week at the end of dialysis, or approximately every other day dose titration ipth level doxercalciferol injection dose decreased by < 50% and above 300 pg/ml increase by 1 mcg to 2 mcg at 8-week intervals as necessary decreased by > 50% and above 300 pg/ml maintain 150 to 300 pg/ml maintain < 100 pg/ml suspend for one week, then resume at a dose that is at least 1 mcg lower

iting 21.3 19.7 musculoskeletal system arthralgia 4.9 0.0 metabolic and nutritional edema 34.4 21.3 weight increase 4.9 0.0 nervous system dizziness 11.5 9.8 sleep disorder 3.3 0.0 respiratory system dyspnea 11.5 6.6 skin pruritus 8.2 6.6 a patient who reported the same medical term more than once was counted only once for that medical term. potential adverse effects of doxercalciferol injection are, in general, similar to those encountered with excessive vitamin d intake. the early and late signs and symptoms of vitamin d intoxication associated with hypercalcemia include: early weakness, headache, somnolence, nausea, vomiting, dry mouth, constipation, muscle pain, bone pain, metallic taste, and anorexia. late polyuria, polydipsia, anorexia, weight loss, nocturia, conjunctivitis (calcific), pancreatitis, photophobia, rhinorrhea, pruritus, hyperthermia, decreased libido, elevated blood urea nitrogen (bun), albuminuria, hypercholesterolemia, elevated serum aspartate transaminase (ast) and alanine transaminase (alt), ectopic calcification, hypertension, cardiac arrhythmias, sensory disturbances, dehydration, apathy, arrested growth, urinary tract infections, and, rarely, overt psychosis. postmarketing experience because these reactions are reported voluntarily from a population of uncertain size, it is not always possible to estimate their frequency or to establish a causal relationship to drug exposure. hypersensitivity reactions, including fatal outcome, have been reported in patients on hemodialysis following administration of doxercalciferol injection. hypersensitivity reactions include anaphylaxis with symptoms of angioedema (involving face, lips, tongue and airways), hypotension, unresponsiveness, chest discomfort, shortness of breath, cardiopulmonary arrest, pruritus and skin burning sensation (see warnings ). these reactions may occur separately or together.

itriol (1α,25-(oh) 2 d 3 ) and 1α,25-(oh) 2 d 2 regulate blood calcium at levels required for essential body functions. specifically, the biologically active vitamin d metabolites control the intestinal absorption of dietary calcium, the tubular reabsorption of calcium by the kidney and, in conjunction with parathyroid hormone (pth), the mobilization of calcium from the skeleton. they act directly on bone cells (osteoblasts) to stimulate skeletal growth, and on the parathyroid glands to suppress pth synthesis and secretion. these functions are mediated by the interaction of these biologically active metabolites with specific receptor proteins in the various target tissues. in uremic patients, deficient production of biologically active vitamin d metabolites (due to lack of or insufficient 25-hydroxyvitamin d-1-alpha-hydroxylase activity) leads to secondary hyperparathyroidism, which contributes to the development of metabolic bone disease in patients with renal failure. pharmacokinetics and metabolism after intravenous administration, doxercalciferol is activated by cyp 27 in the liver to form 1α,25-(oh) 2 d 2 (major metabolite) and 1α,24-dihydroxyvitamin d 2 (minor metabolite). activation of doxercalciferol does not require the involvement of the kidneys. peak blood levels of 1α,25-(oh) 2 d 2 are reached at 8 +/- 5.9 hours (mean +/- sd) after a single intravenous dose of 5 mcg of doxercalciferol. the mean elimination half-life of 1α,25-(oh) 2 d 2 after an oral dose is approximately 32 to 37 hours with a range of up to 96 hours. the mean elimination half-life in patients with end stage renal disease (esrd) and in healthy volunteers appears to be similar following an oral dose. hemodialysis causes a temporary increase in 1α,25-(oh) 2 d 2 mean concentrations presumably due to volume contraction. 1α,25-(oh) 2 d 2 is not removed from blood during hemodialysis. clinical studies the safety and effectiveness of doxercalciferol injection were evaluated in two open-label, single-arm, multi-centered clinical studies (study c and study d) in a total of 70 patients with chronic kidney disease on hemodialysis (stage 5 ckd). patients in study c were an average age of 54 years (range: 23 to 73), were 50% male, and were 61% african-american, 25% caucasian, and 14% hispanic, and had been on hemodialysis for an average of 65 months. patients in study d were an average age of 51 years (range: 28 to 76), were 48% male, and 100% african-american and had been on hemodialysis for an average of 61 months. this group of 70 of the 138 patients who had been treated with doxercalciferol capsules in prior clinical studies (study a and study b) received doxercalciferol injection in an open-label fashion for 12 weeks following an 8-week washout (control) period. dosing of doxercalciferol injection was initiated at the rate of 4 mcg administered at the end of each dialysis session (3 times weekly) for a total of 12 mcg per week. the dosage of doxercalciferol was adjusted in an attempt to achieve ipth levels within a targeted range of 150 to 300 pg/ml. the dosage was increased by 2 mcg per dialysis session after 8 weeks of treatment if the ipth levels remained above 300 pg/ml and were greater than 50% of baseline levels. the maximum dosage was limited to 18 mcg per week. if at any time during the trial ipth fell below 150 pg/ml, doxercalciferol injection was immediately suspended and restarted at a lower dosage the following week. results fifty-two of the 70 patients who were treated with doxercalciferol injection achieved ipth levels ≤ 300 pg/ml. forty-one of these patients exhibited plasma ipth levels ≤ 300 pg/ml on at least three occasions. thirty-six patients had plasma ipth levels < 150 pg/ml on at least one occasion during study participation. mean weekly doses in study c ranged from 8.9 mcg to 12.5 mcg. in study d, the mean weekly doses ranged from 9.1 mcg to 11.6 mcg. decreases in plasma ipth from baseline values were calculated using as baseline the average of the last three values obtained during the 8-week washout period and are displayed in the table below. plasma ipth levels were measured weekly during the 12-week study. table 1: ipth summary data for patients receiving doxercalciferol injection ipth level study c (n = 28) study d (n = 42) combined protocols (n = 70) baseline (mean of weeks -2, -1 and 0) mean (se) 698 (60) 762 (65) 736 (46) median 562 648 634 on-treatment (week 12 values were carried forward for the two patients on study for 10 weeks ) mean (se) 406 (63) 426 (60) 418 (43) median 311 292 292 change from baseline treatment ipth minus baseline ipth mean (se) -292 (55) -336 (41) -318 (33) median -274 -315 -304 p-value wilcoxon one-sample test 0.004 0.001 < 0.001 in both studies, ipth levels increased progressively and significantly in 62.9% of patients during the 8-week washout (control) period during which no vitamin d derivatives were administered. in contrast, doxercalciferol injection treatment resulted in a clinically significant reduction (at least 30%) from baseline in mean ipth levels during the 12-week open-label treatment period in more than 92% of the 70 treated patients. table 2 shows the numbers of patients who achieved ipth levels below 300 pg/ml on one, two, or three or more non-consecutive occasions during the 12-week treatment period. thirty-seven of 70 patients (53%) had plasma ipth levels within the targeted range (150 to 300 pg/ml) during weeks 10 to 12. table 2: number of times ipth ≤ 300 pg/ml 1 2 ≥3 study c 3/28 0/28 16/28 study d 4/42 4/42 25/42

ysis session (3 times weekly) for a total of 12 mcg per week. the dosage of doxercalciferol was adjusted in an attempt to achieve ipth levels within a targeted range of 150 to 300 pg/ml. the dosage was increased by 2 mcg per dialysis session after 8 weeks of treatment if the ipth levels remained above 300 pg/ml and were greater than 50% of baseline levels. the maximum dosage was limited to 18 mcg per week. if at any time during the trial ipth fell below 150 pg/ml, doxercalciferol injection was immediately suspended and restarted at a lower dosage the following week. results fifty-two of the 70 patients who were treated with doxercalciferol injection achieved ipth levels ≤ 300 pg/ml. forty-one of these patients exhibited plasma ipth levels ≤ 300 pg/ml on at least three occasions. thirty-six patients had plasma ipth levels < 150 pg/ml on at least one occasion during study participation. mean weekly doses in study c ranged from 8.9 mcg to 12.5 mcg. in study d, the mean weekly doses ranged from 9.1 mcg to 11.6 mcg. decreases in plasma ipth from baseline values were calculated using as baseline the average of the last three values obtained during the 8-week washout period and are displayed in the table below. plasma ipth levels were measured weekly during the 12-week study. table 1: ipth summary data for patients receiving doxercalciferol injection ipth level study c (n = 28) study d (n = 42) combined protocols (n = 70) baseline (mean of weeks -2, -1 and 0) mean (se) 698 (60) 762 (65) 736 (46) median 562 648 634 on-treatment (week 12 values were carried forward for the two patients on study for 10 weeks ) mean (se) 406 (63) 426 (60) 418 (43) median 311 292 292 change from baseline treatment ipth minus baseline ipth mean (se) -292 (55) -336 (41) -318 (33) median -274 -315 -304 p-value wilcoxon one-sample test 0.004 0.001 < 0.001 in both studies, ipth levels increased progressively and significantly in 62.9% of patients during the 8-week washout (control) period during which no vitamin d derivatives were administered. in contrast, doxercalciferol injection treatment resulted in a clinically significant reduction (at least 30%) from baseline in mean ipth levels during the 12-week open-label treatment period in more than 92% of the 70 treated patients. table 2 shows the numbers of patients who achieved ipth levels below 300 pg/ml on one, two, or three or more non-consecutive occasions during the 12-week treatment period. thirty-seven of 70 patients (53%) had plasma ipth levels within the targeted range (150 to 300 pg/ml) during weeks 10 to 12. table 2: number of times ipth ≤ 300 pg/ml 1 2 ≥3 study c 3/28 0/28 16/28 study d 4/42 4/42 25/42