Prograf®
tacrolimus capsules
tacrolimus injection (for intravenous infusion only)
|
Prograf is available for oral administration as capsules (tacrolimus capsules) containing the equivalent of 0.5 mg, 1 mg or 5 mg of anhydrous tacrolimus. Inactive ingredients include lactose, hydroxypropyl methylcellulose, croscarmellose sodium, and magnesium stearate. The 0.5 mg capsule shell contains gelatin, titanium dioxide and ferric oxide, the 1 mg capsule shell contains gelatin and titanium dioxide, and the 5 mg capsule shell contains gelatin, titanium dioxide and ferric oxide.
Tacrolimus, previously known as FK506, is the active ingredient in
Prograf. Tacrolimus is a macrolide immunosuppressant produced by Streptomyces
tsukubaensis. Chemically, tacrolimus is designated as [3S-[3R*[E(1S*,3S*,4S*)],4S*,5R*,8S*,9E,12R*,14R*,15S*,16R*,18S*,19S*,26aR*]]-5,6,8,11,12,
13,14,15,16,17,18,19,24,25,26,26a-hexadecahydro-5, 19-dihydroxy-3-
[2-(4-hydroxy-3-methoxycyclohexyl) -1-methylethenyl]-14,
16-dimethoxy-4,10,12, 18-tetramethyl-8-(2-propenyl)-15,
19-epoxy-3H-pyrido[2,1-c][1,4] oxaazacyclotricosine-1,7,20,
21(4H,23H)-tetrone, monohydrate.
The chemical structure of tacrolimus is:
Tacrolimus has an empirical formula of C44H69NO12 ·H2O and a formula weight of 822.05. Tacrolimus appears as white crystals or crystalline powder. It is practically insoluble in water, freely soluble in ethanol, and very soluble in methanol and chloroform.
Tacrolimus prolongs the survival of the host and transplanted graft in animal transplant models of liver, kidney, heart, bone marrow, small bowel and pancreas, lung and trachea, skin, cornea, and limb.
Tacrolimus activity is primarily due to the parent drug. The pharmacokinetic parameters (mean±S.D.) of tacrolimus have been determined following intravenous (IV) and oral (PO) administration in healthy volunteers, kidney transplant and liver transplant patients. (See table below.)
| Population | N | Route (Dose) |
Parameters | |||||
| Cmax (ng/mL) |
Tmax (hr) |
AUC (ng·hr/mL) |
t½ (hr) |
Cl (L/hr/kg) |
V (L/kg) |
|||
| Healthy Volunteers |
8 | IV (0.025 mg/kg/4hr) |
— |
— |
598* ± 125 |
34.2 ± 7.7 |
0.040 ±0.009 |
1.91 ±0.31 |
| 16 | PO (5 mg) |
29.7 ±7.2 |
1.6 ±0.7 |
243** ±73 |
34.8 ±11.4 |
0.041† ±0.008 |
1.94† ±0.53 |
|
| Kidney Transplant Pts |
26 | IV (0.02 mg/kg/12hr) |
— |
— |
294*** ±262 |
18.8 ±16.7 |
0.083 ±0.050 |
1.41 ±0.66 |
| PO (0.2 mg/kg/day) |
19.2 ±10.3 |
3.0 | 203*** ±42 |
# | # | # | ||
| PO (0.3 mg/kg/day) |
24.2 ±15.8 |
1.5 | 288*** ±93 |
# | # | # | ||
| Liver Transplant Pts |
17 | IV (0.05 mg/kg/12 hr) |
— | — | 3300*** ±2130 |
11.7 ±3.9 |
0.053 ±0.017 |
0.85 ±0.30 |
| PO (0.3 mg/kg/day) |
68.5 ±30.0 |
2.3 ±1.5 |
519*** ±179 |
# | # | # | ||
Due to intersubject variability in tacrolimus pharmacokinetics, individualization of dosing regimen is necessary for optimal therapy. (See DOSAGE AND ADMINISTRATION). Pharmacokinetic data indicate that whole blood concentrations rather than plasma concentrations serve as the more appropriate sampling compartment to describe tacrolimus pharmacokinetics.
Absorption
Absorption of tacrolimus from the gastrointestinal tract after oral administration is incomplete and variable. The absolute bioavailability of tacrolimus was 17±10% in adult kidney transplant patients (N=26), 22±6% in adult liver transplant patients (N=17), and 18±5% in healthy volunteers (N=16).
Distribution
The plasma protein binding of tacrolimus is approximately 99% and is independent of concentration over a range of 5-50 ng/mL. Tacrolimus is bound mainly to albumin and alpha-1-acid glycoprotein, and has a high level of association with erythrocytes. The distribution of tacrolimus between whole blood and plasma depends on several factors, such as hematocrit, temperature at the time of plasma separation, drug concentration, and plasma protein concentration. In a U.S. study, the ratio of whole blood concentration to plasma concentration averaged 35 (range 12 to 67).
Metabolism
Tacrolimus is extensively metabolized by the mixed-function oxidase system, primarily the cytochrome P-450 system (CYP3A). A metabolic pathway leading to the formation of 8 possible metabolites has been proposed. Demethylation and hydroxylation were identified as the primary mechanisms of biotransformation in vitro. The major metabolite identified in incubations with human liver microsomes is 13-demethyl tacrolimus. In in vitro studies, a 31-demethyl metabolite has been reported to have the same activity as tacrolimus.
Excretion
The mean clearance following IV administration of tacrolimus is 0.040, 0.083 and 0.053 L/hr/kg in healthy volunteers, adult kidney transplant patients and adult liver transplant patients, respectively. In man, less than 1% of the dose administered is excreted unchanged in urine.
Special Populations
Pediatric
Pharmacokinetics of tacrolimus have been studied in liver transplantation patients, 0.7 to 13.2 years of age. Following IV administration of a 0.037 mg/kg/day dose to 12 pediatric patients, mean terminal half-life, volume of distribution and clearance were 11.5±3.8 hours, 2.6±2.1 L/kg and 0.138±0.071 L/hr/kg, respectively. Following oral administration to 9 patients, mean AUC and Cmax were 337±167 ng•hr/mL and 43.4±27.9 ng/mL, respectively. The absolute bioavailability was 31± 21%.
Renal and Hepatic Insufficiency
The mean pharmacokinetic parameters for tacrolimus following single administrations to patients with renal and hepatic impairment are given in the following table.
|
Population
(No. of Patients) |
Dose
|
AUC 0-t
(ng·hr/mL) |
t½
(hr) |
V
(L/kg) |
Cl
(L/hr/kg) |
|
Renal
Impairment (n=12) |
0.02
mg/kg/4hr IV |
393±123 (t = 60hr) |
26.3±9.2
|
1.07
±0.20 |
0.038
±0.014 |
|
Mild Hepatic
Impairment (n=6) |
0.02 |
367±107 (t=72hr) |
60.6±43.8
Range: 27.8 - 141 |
3.1
±1.6 |
0.042
±0.02 |
|
7.7 mg
PO |
488±320 (t = 72hr) |
66.1±44.8
Range: 29.5 - 138 |
3.7
±4.7* |
0.034
±0.019* |
|
|
Severe Hepatic
Impairment (n=6, IV) |
0.02
mg/kg/4hr IV (n=2) |
762±204
(t=120hr) |
198±158
Range: 81-436 |
3.9
±1.0 |
0.017
±0.013 |
|
0.01
mg/kg/8hr IV (n=4) |
289±117
(t=144hr) |
|
|
|
|
|
Severe Hepatic
Impairment (n=5, PO)†
|
8 mg PO
(n=1) |
658
(t=120hr) |
119±35
Range: 85-178 |
3.1
±3.4* |
0.016
±0.011* |
|
5mg PO
(n=4) |
533±156
(t=144hr) |
||||
|
4 mg PO
(n=1) |
| * corrected for bioavailability † 1 patient did not receive the PO dose |
Renal Insufficiency:
Tacrolimus pharmacokinetics following a single IV administration were determined in 12 patients (7 not on dialysis and 5 on dialysis, serum creatinine of 3.9±1.6 and 12.0±2.4 mg/dL, respectively) prior to their kidney transplant. The pharmacokinetic parameters obtained were similar for both groups.
Hepatic Insufficiency:
Tacrolimus pharmacokinetics have been determined in six patients with mild hepatic dysfunction (mean Pugh score: 6.2) following single IV and oral administrations. The mean clearance of tacrolimus in patients with mild hepatic dysfunction was not substantially different from that in normal volunteers (see previous table). Tacrolimus pharmacokinetics were studied in 6 patients with severe hepatic dysfunction (mean Pugh score: >10). The mean clearance was substantially lower in patients with severe hepatic dysfunction, irrespective of the route of administration.
Race
A formal study to evaluate the pharmacokinetic disposition of tacrolimus in Black transplant patients has not been conducted. However, a retrospective comparison of Black and Caucasian kidney transplant patients indicated that Black patients required higher tacrolimus doses to attain similar trough concentrations. (See DOSAGE AND ADMINISTRATION).
Gender
A formal study to evaluate the effect of gender on tacrolimus pharmacokinetics has not been conducted, however, there was no difference in dosing by gender in the kidney transplant trial. A retrospective comparison of pharmacokinetics in healthy volunteers, and in kidney and liver transplant patients indicated no gender-based differences.
The safety and efficacy of Prograf-based immunosuppression following orthotopic liver transplantation were assessed in two prospective, randomized, non-blinded multicenter studies. The active control groups were treated with a cyclosporine-based immunosuppressive regimen. Both studies used concomitant adrenal corticosteroids as part of the immunosuppressive regimens. These studies were designed to evaluate whether the two regimens were therapeutically equivalent, with patient and graft survival at 12 months following transplantation as the primary endpoints. The Prograf-based immunosuppressive regimen was found to be equivalent to the cyclosporine-based immunosuppressive regimens.
Prograf-based immunosuppression following kidney transplantation was assessed in a Phase III randomized, multicenter, non-blinded, prospective study. There were 412 kidney transplant patients enrolled at 19 clinical sites in the United States. Study therapy was initiated when renal function was stable as indicated by a serum creatinine < 4 mg/dL (median of 4 days after transplantation, range 1 to 14 days). Patients less than 6 years of age were excluded.
Prograf is indicated for the prophylaxis of organ rejection in patients receiving allogeneic liver or kidney transplants. It is recommended that Prograf be used concomitantly with adrenal corticosteroids. Because of the risk of anaphylaxis, Prograf injection should be reserved for patients unable to take Prograf capsules orally.
Prograf is contraindicated in patients with a hypersensitivity to tacrolimus. Prograf injection is contraindicated in patients with a hypersensitivity to HCO-60 (polyoxyl 60 hydrogenated castor oil).
(See boxed WARNING.)
Insulin-dependent post-transplant diabetes mellitus (PTDM) was reported in 20% of Prograf-treated kidney transplant patients without pretransplant history of diabetes millitus in the Phase III study below (See Tables Below). The median time to onset of PTDM was 68 days. Insulin dependence was reversible in 15% of these PTDM patients at one year and in 50% at two years post transplant. Black and Hispanic kidney transplant patients were at an increased risk of development of PTDM.
Incidence of Post Transplant Diabetes Mellitus
and Insulin Use at 2 years in Kidney Transplant Recipients in the Phase
III Study
|
Status of PTDM*
|
Prograf | CBIR |
| Patients without pretransplant history of diabetes mellitus. | 151 | 151 |
| New onset PTDM*, 1st Year | 30/151 (20%) | 6/151 (4%) |
| Still insulin dependent at one year in those
without prior history of diabetes. |
25/151(17%) | 5/151 (3%) |
| New onset PTDM* post 1 year | 1 | 0 |
| Patients with PTDM* at 2 years | 16/151 (11%) | 5/151 (3%) |
|
*use of insulin for 30 or more consecutive days, with < 5 day gap, without a prior history of insulin dependent diabetes mellitus or non insulin dependent diabetes mellitus. |
Development of Post Transplant Diabetes Mellitus by Race
and by Treatment Group during First Year Post Kidney Transplantation in the
Phase III Study
| Patient Race | Prograf | CBIR | ||
| No. of Patients at Risk |
Patients Who Developed PTDM* |
No. of Patients at Risk |
Patients Who Developed PTDM* |
|
| Black | 41 | 15 (37%) | 36 | 3 (8%) |
| Hispanic | 17 | 5 (29%) | 18 | 1 (6%) |
| Caucasian | 82 | 10 (12%) | 87 | 1 (1%) |
| Other | 11 | 0 (0%) | 10 | 1 (10%) |
| Total | 151 | 30 (20%) | 151 | 6 (4%) |
|
* use of insulin for 30 or more consecutive days, with < 5 day gap, without a prior history of insulin dependent diabetes mellitus or non insulin dependent diabetes mellitus. |
Insulin-dependent post-transplant diabetes mellitus was reported in 18% and 11% of Prograf-treated liver transplant patients and was reversible in 45% and 31% of these patients at one year post transplant, in the U.S. and European randomized studies, respectively (See Table below). Hyperglycemia was associated with the use of Prograf in 47% and 33% of liver transplant recipients in the U.S. and European randomized studies, respectively, and may require treatment (see ADVERSE REACTIONS).
Incidence of Post Transplant Diabetes Mellitus and Insulin Use
at One Year in Liver Transplant Recipients
| Status of PTDM* | US Study | European Study | ||
| Prograf | CBIR | Prograf | CBIR | |
| Patients at risk ** | 239 | 236 | 239 | 249 |
| New Onset PTDM* | 42 (18%) | 30 (13%) | 26 (11%) | 12(5%) |
| Patients still on insulin at 1 year | 23 (10%) | 19 (8%) | 18 (8%) | 6 (2%) |
*
**Patients without pretransplant history of diabetes mellitus.
Prograf can cause neurotoxicity and nephrotoxicity, particularly when used in high doses. Nephrotoxicity was reported in approximately 52% of kidney transplantation patients and in 40% and 36% of liver transplantation patients receiving Prograf in the U.S. and European randomized trials, respectively (see ADVERSE REACTIONS). More overt nephrotoxicity is seen early after transplantation, characterized by increasing serum creatinine and a decrease in urine output. Patients with impaired renal function should be monitored closely as the dosage of Prograf may need to be reduced. In patients with persistent elevations of serum creatinine who are unresponsive to dosage adjustments, consideration should be given to changing to another immunosuppressive therapy. Care should be taken in using tacrolimus with other nephrotoxic drugs. In particular, to avoid excess nephrotoxicity, Prograf should not be used simultaneously with cyclosporine. Prograf or cyclosporine should be discontinued at least 24 hours prior to initiating the other. In the presence of elevated Prograf or cyclosporine concentrations, dosing with the other drug usually should be further delayed.
Hypertension is a common adverse effect of Prograf therapy (see ADVERSE REACTIONS). Mild or moderate hypertension is more frequently reported than severe hypertension. Antihypertensive therapy may be required; the control of blood pressure can be accomplished with any of the common antihypertensive agents. Since tacrolimus may cause hyperkalemia, potassium-sparing diuretics should be avoided. While calcium-channel blocking agents can be effective in treating Prograf-associated hypertension, care should be taken since interference with tacrolimus metabolism may require a dosage reduction (see Drug Interactions).
For patients with renal insufficiency some evidence suggests that lower doses should be used (see CLINICAL PHARMACOLOGY and DOSAGE AND ADMINISTRATION).
Myocardial hypertrophy has been reported in association with the administration of Prograf, and is generally manifested by echocardiographically demonstrated concentric increases in left ventricular posterior wall and interventricular septum thickness. Hypertrophy has been observed in infants, children and adults. This condition appears reversible in most cases following dose reduction or discontinuance of therapy. In a group of 20 patients with pre- and post-treatment echocardiograms who showed evidence of myocardial hypertrophy, mean tacrolimus whole blood concentrations during the period prior to diagnosis of myocardial hypertrophy ranged from 11 to 53 ng/mL in infants (N=10, age 0.4 to 2 years), 4 to 46 ng/mL in children (N=7, age 2 to 15 years) and 11 to 24 ng/mL in adults (N=3, age 37 to 53 years).
Patients should be informed of the need for repeated appropriate laboratory tests while they are receiving Prograf. They should be given complete dosage instructions, advised of the potential risks during pregnancy, and informed of the increased risk of neoplasia. Patients should be informed that changes in dosage should not be undertaken without first consulting their physician.
Serum creatinine, potassium, and fasting glucose should be assessed regularly. Routine monitoring of metabolic and hematologic systems should be performed as clinically warranted.
Due to the potential for additive or synergistic impairment of renal function, care should be taken when administering Prograf with drugs that may be associated with renal dysfunction. These include, but are not limited to, aminoglycosides, amphotericin B, and cisplatin. Initial clinical experience with the co-administration of Prograf and cyclosporine resulted in additive/synergistic nephrotoxicity. Patients switched from cyclosporine to Prograf should receive the first Prograf dose no sooner than 24 hours after the last cyclosporine dose. Dosing may be further delayed in the presence of elevated cyclosporine levels.
Since tacrolimus is metabolized mainly by the CYP3A enzyme systems, substances known to inhibit these enzymes may decrease the metabolism or increase bioavailability of tacrolimus as indicated by increased whole blood or plasma concentrations. Drugs known to induce these enzyme systems may result in an increased metabolism of tacrolimus or decreased bioavailability as indicated by decreased whole blood or plasma concentrations. Monitoring of blood concentrations and appropriate dosage adjustments are essential when such drugs are used concomitantly.
| *Drugs That May Increase Tacrolimus Blood Concentrations: | ||||
| Calcium Channel Blockers |
Antifungal Agents |
Macrolide Antibiotics |
||
| diltiazem | clotrimazole | clarithromycin | ||
| nicardipine | fluconazole | erythromycin | ||
| nifedipine | itraconazole | troleandomycin | ||
| verapamil | ketoconazole | |||
| Gastrointestinal Prokinetic Agents |
Other Drugs |
|||
| cisapride | bromocriptine | |||
| metoclopramide | cimetidine | |||
| cyclosporine | ||||
| danazol | ||||
| ethinyl estradiol | ||||
| methylprednisolone | ||||
| omeprazole | ||||
| protease inhibitors | ||||
| nefazodone | ||||
| In a study of 6 normal volunteers, a significant increase
in tacrolimus oral bioavailability (14±5% vs. 30±8%) was observed
with concomitant ketoconazole administration (200 mg). The apparent oral
clearance of tacrolimus during ketoconazole administration was significantly
decreased compared to tacrolimus alone (0.430±0.129L/hr/kg vs. 0.148±0.043L/hr/kg).
Overall, IV clearance of tacrolimus was not significantly changed by ketoconazole
co-administration, although it was highly variable between patients. |
||||
| *Drugs That May Decrease Tacrolimus Blood Concentrations: | ||||
| Anticonvulsants | Antibiotics | Herbal Preparations | ||
| carbamazepine | rifabutin | St. John's Wort | ||
| phenobarbital | rifampin | |||
| phenytoin | ||||
*This table is not all inclusive.
St. John's Wort (Hypericum perforatum) induces CYP3A4 and P-glycoprotein. Since tacrolimus is a substrate for CYP3A4, there is the potential that the use of St. John's Wort in patients receiving Prograf could result in reduced tacrolimus levels.
In a study of 6 normal volunteers, a significant decrease in tacrolimus oral bioavailability (14±6% vs. 7±3%) was observed with concomitant rifampin administration (600 mg). In addition, there was a significant increase in tacrolimus clearance (0.036±0.008L/hr/kg vs. 0.053±0.010L/hr/kg) with concomitant rifampin administration.
Interaction studies with drugs used in HIV therapy have not been conducted. However, care should be exercised when drugs that are nephrotoxic (e.g., ganciclovir) or that are metabolized by CYP3A (e.g., ritonavir) are administered concomitantly with tacrolimus. Tacrolimus may effect the pharmacokinetics of other drugs (e.g. phenytoin) and increase their concentration. Grapefruit juice affects CYP3A-mediated metabolism and should be avoided (see DOSAGE AND ADMINISTRATION).
Immunosuppressants may affect vaccination. Therefore, during treatment with Prograf, vaccination may be less effective. The use of live vaccines should be avoided; live vaccines may include, but are not limited to measles, mumps, rubella, oral polio, BCG, yellow fever, and TY 21a typhoid.1
An increased incidence of malignancy is a recognized complication of immunosuppression in recipients of organ transplants. The most common forms of neoplasms are non-Hodgkin's lymphomas and carcinomas of the skin. As with other immunosuppressive therapies, the risk of malignancies in Prograf recipients may be higher than in the normal, healthy population. Lymphoproliferative disorders associated with Epstein-Barr Virus infection have been seen. It has been reported that reduction or discontinuation of immunosuppression may cause the lesions to regress.
In reproduction studies in rats and rabbits, adverse effects on the fetus were observed mainly at dose levels that were toxic to dams. Tacrolimus at oral doses of 0.32 and 1.0 mg/kg during organogenesis in rabbits was associated with maternal toxicity as well as an increase in incidence of abortions; these doses are equivalent to 0.5 - 1X and 1.6 - 3.3X the recommended clinical dose range (0.1 - 0.2 mg/kg) based on body surface area corrections. At the higher dose only, an increased incidence of malformations and developmental variations was also seen. Tacrolimus, at oral doses of 3.2 mg/kg during organogenesis in rats, was associated with maternal toxicity and caused an increase in late resorptions, decreased numbers of live births, and decreased pup weight and viability. Tacrolimus, given orally at 1.0 and 3.2 mg/kg (equivalent to 0.7 - 1.4X and 2.3 - 4.6X the recommended clinical dose range based on body surface area corrections) to pregnant rats after organogenesis and during lactation, was associated with reduced pup weights.
Since tacrolimus is excreted in human milk, nursing should be avoided.
Experience with Prograf in pediatric kidney transplant patients is limited. Successful liver transplants have been performed in pediatric patients (ages up to 16 years) using Prograf. The two randomized active-controlled trials of Prograf in primary liver transplantation included 56 pediatric patients. Thirty-one patients were randomized to Prograf-based and 25 to cyclosporine-based therapies. Additionally, a minimum of 122 pediatric patients were studied in an uncontrolled trial of tacrolimus in living related donor liver transplantation. Pediatric patients generally required higher doses of Prograf to maintain blood trough concentrations of tacrolimus similar to adult patients (see DOSAGE AND ADMINISTRATION).
The principal adverse reactions of Prograf are tremor, headache, diarrhea, hypertension, nausea, and renal dysfunction. These occur with oral and IV administration of Prograf and may respond to a reduction in dosing. Diarrhea was sometimes associated with other gastrointestinal complaints such as nausea and vomiting.
LIVER TRANSPLANTATION: ADVERSE EVENTS OCCURRING IN > 15% OF PROGRAF-TREATED PATIENTS
| U.S. STUDY (%) | EUROPEAN STUDY (%) | |||
| Prograf (N=250) |
CBIR (N=250) |
Prograf (N=264) |
CBIR (N=265) |
|
| Nervous System | ||||
| Headache (see WARNINGS) | 64 | 60 | 37 | 26 |
| Tremor (see WARNINGS) | 56 | 46 | 48 | 32 |
| Insomnia | 64 | 68 | 32 | 23 |
| Paresthesia | 40 | 30 | 17 | 17 |
| Gastrointestinal | ||||
| Diarrhea | 72 | 47 | 37 | 27 |
| Nausea | 46 | 37 | 32 | 27 |
| Constipation | 24 | 27 | 23 | 21 |
| LFT Abnormal | 36 | 30 | 6 | 5 |
| Anorexia | 34 | 24 | 7 | 5 |
| Vomiting | 27 | 15 | 14 | 11 |
| Cardiovascular | ||||
| Hypertension (see PRECAUTIONS) | 47 | 56 | 38 | 43 |
| Urogenital | ||||
| Kidney Function Abnormal (see WARNINGS) | 40 | 27 | 36 | 23 |
| Creatinine Increased (see WARNINGS) | 39 | 25 | 24 | 19 |
| BUN Increased (see WARNINGS) | 30 | 22 | 12 | 9 |
| Urinary Tract Infection | 16 | 18 | 21 | 19 |
| Oliguria | 18 | 15 | 19 | 12 |
| Metabolic and Nutritional | ||||
| Hyperkalemia (see WARNINGS) | 45 | 26 | 13 | 9 |
| Hypokalemia | 29 | 34 | 13 | 16 |
| Hyperglycemia (see WARNINGS) | 47 | 38 | 33 | 22 |
| Hypomagnesemia | 48 | 45 | 16 | 9 |
| Hemic and Lymphatic | ||||
| Anemia | 47 | 38 | 5 | 1 |
| Leukocytosis | 32 | 26 | 8 | 8 |
| Thrombocytopenia | 24 | 20 | 14 | 19 |
| Miscellaneous | ||||
| Abdominal Pain | 59 | 54 | 29 | 22 |
| Pain | 63 | 57 | 24 | 22 |
| Fever | 48 | 56 | 19 | 22 |
| Asthenia | 52 | 48 | 11 | 7 |
| Back Pain | 30 | 29 | 17 | 17 |
| Ascites | 27 | 22 | 7 | 8 |
| Peripheral Edema | 26 | 26 | 12 | 14 |
| Respiratory System | ||||
| Pleural Effusion | 30 | 32 | 36 | 35 |
| Atelectasis | 28 | 30 | 5 | 4 |
| Dyspnea | 29 | 23 | 5 | 4 |
| Skin and Appendages | ||||
| Pruritus | 36 | 20 | 15 | 7 |
| Rash | 24 | 19 | 10 | 4 |
Less frequently observed adverse reactions in both liver transplantation and kidney transplantation patients are described under the subsection Less Frequently Reported Adverse Reactions below.
The most common adverse reactions reported were infection, tremor, hypertension, decreased renal function, constipation, diarrhea, headache, abdominal pain and insomnia.
KIDNEY TRANSPLANTATION: ADVERSE EVENTS OCCURRING IN > 15% OF PROGRAF-TREATED PATIENTS
| Prograf (N=205) |
CBIR (N=207) |
|
| Nervous System | ||
| Tremor (see WARNINGS) | 54 | 34 |
| Headache (see WARNINGS) | 44 | 38 |
| Insomnia | 32 | 30 |
| Paresthesia | 23 | 16 |
| Dizziness | 19 | 16 |
| Gastrointestinal | ||
| Diarrhea | 44 | 41 |
| Nausea | 38 | 36 |
| Constipation | 35 | 43 |
| Vomiting | 29 | 23 |
| Dyspepsia | 28 | 20 |
| Cardiovascular | ||
| Hypertension (see PRECAUTIONS) | 50 | 52 |
| Chest Pain | 19 | 13 |
| Urogenital | ||
| Creatinine Increased (see WARNINGS) | 45 | 42 |
| Urinary Tract Infection | 34 | 35 |
| Metabolic and Nutritional | ||
| Hypophosphatemia | 49 | 53 |
| Hypomagnesemia | 34 | 17 |
| Hyperlipemia | 31 | 38 |
| Hyperkalemia (see WARNINGS) | 31 | 32 |
| Diabetes Mellitus (see WARNINGS) | 24 | 9 |
| Hypokalemia | 22 | 25 |
| Hyperglycemia (see WARNINGS) | 22 | 16 |
| Edema | 18 | 19 |
| Hemic and Lymphatic | ||
| Anemia | 30 | 24 |
| Leukopenia | 15 | 17 |
| Miscellaneous | ||
| Infection | 45 | 49 |
| Peripheral Edema | 36 | 48 |
| Asthenia | 34 | 30 |
| Abdominal Pain | 33 | 31 |
| Pain | 32 | 30 |
| Fever | 29 | 29 |
| Back Pain | 24 | 20 |
| Respiratory System | ||
| Dyspnea | 22 | 18 |
| Cough Increased | 18 | 15 |
| Musculoskeletal | ||
| Arthralgia | 25 | 24 |
| Skin | ||
| Rash | 17 | 12 |
| Pruritis | 15 | 7 |
Less frequently observed adverse reactions in both liver transplantion and kidney transplantation patients are described under the subsection Less Frequently Reported Adverse Reactions shown below.
The following adverse events were reported in the range of 3% to less than 15% incidence in either liver or kidney transplant recipients who were treated with tacrolimus in the Phase 3 comparative trials.
Post Marketing
The following have been reported: increased amylase including pancreatitis, hearing loss including deafness, leukoencephalopathy, thrombocytopenic purpura, hemolytic-uremia syndrome, acute renal failure, Stevens-Johnson syndrome, stomach ulcer, glycosuria, cardiac arrhythmia and gastroenteritis.
Limited overdosage experience is available. Acute overdosages of up to 30 times the intended dose have been reported. Almost all cases have been asymptomatic and all patients recovered with no sequelae. Occasionally, acute overdosage has been followed by adverse reactions consistent with those listed in the ADVERSE REACTIONS section except in one case where transient urticaria and lethargy were observed. Based on the poor aqueous solubility and extensive erythrocyte and plasma protein binding, it is anticipated that tacrolimus is not dialyzable to any significant extent; there is no experience with charcoal hemoperfusion. The oral use of activated charcoal has been reported in treating acute overdoses, but experience has not been sufficient to warrant recommending its use. General supportive measures and treatment of specific symptoms should be followed in all cases of overdosage.
NOTE: Anaphylactic reactions have occurred with injectables containing castor oil derivatives. See WARNINGS.
In patients unable to take oral Prograf capsules, therapy may be initiated with Prograf injection. The initial dose of Prograf should be administered no sooner than 6 hours after transplantation. The recommended starting dose of Prograf injection is 0.03-0.05 mg/kg/day as a continuous IV infusion. Adult patients should receive doses at the lower end of the dosing range. Concomitant adrenal corticosteroid therapy is recommended early post-transplantation. Continuous IV infusion of Prograf injection should be continued only until the patient can tolerate oral administration of Prograf capsules.
Prograf injection must be diluted with 0.9% Sodium Chloride Injection or 5% Dextrose Injection to a concentration between 0.004 mg/mL and 0.02 mg/mL prior to use. Diluted infusion solution should be stored in glass or polyethylene containers and should be discarded after 24 hours. The diluted infusion solution should not be stored in a PVC container due to decreased stability and the potential for extraction of phthalates. In situations where more dilute solutions are utilized (e.g., pediatric dosing, etc.), PVC-free tubing should likewise be used to minimize the potential for significant drug adsorption onto the tubing. Parenteral drug products should be inspected visually for particulate matter and discoloration prior to administration, whenever solution and container permit. Due to the chemical instability of tacrolimus in alkaline media, Prograf injection should not be mixed or co-infused with solutions of pH 9 or greater (e.g., ganciclovir or acyclovir).
Summary of Initial Oral Dosage Recommendations and Typical Whole Blood Trough Concentrations
| Patient Population | Recommended Initial Oral Dose* |
Typical Whole Blood Trough Concentrations |
| Adult kidney transplant patients | 0.2 mg/kg/day | month 1-3 : 7-20 ng/mL month 4-12 : 5-15 ng/mL |
| Adult liver transplant patients | 0.10-0.15 mg/kg/day | month 1-12 : 5-20 ng/mL |
| Pediatric liver transplant patients | 0.15-0.20 mg/kg/day | month 1-12 : 5-20 ng/mL |
*Note: two divided doses, q12h
It is recommended that patients initiate oral therapy with Prograf capsules if possible. If IV therapy is necessary, conversion from IV to oral Prograf is recommended as soon as oral therapy can be tolerated. This usually occurs within 2-3 days. The initial dose of Prograf should be administered no sooner than 6 hours after transplantation. In a patient receiving an IV infusion, the first dose of oral therapy should be given 8-12 hours after discontinuing the IV infusion. The recommended starting oral dose of Prograf capsules is 0.10-0.15 mg/kg/day administered in two divided daily doses every 12 hours. Co-administered grapefruit juice has been reported to increase tacrolimus blood trough concentrations in liver transplant patients. (See Drugs That May Alter Tacrolimus Concentrations.)
Dosage and typical tacrolimus whole blood trough concentrations are shown in the table above; blood concentration details are described in Blood Concentration Monitoring: Liver Transplantation below.
The recommended starting oral dose of Prograf is 0.2 mg/kg/day administered every 12 hours in two divided doses. The initial dose of Prograf may be administered within 24 hours of transplantation, but should be delayed until renal function has recovered (as indicated for example by a serum creatinine<4 mg/dL). Black patients may require higher doses to achieve comparable blood concentrations. Dosage and typical tacrolimus whole blood trough concentrations are shown in the table above; blood concentration details are described in Blood Concentration Monitoring: Kidney Transplantation below.
| Time After Transplant |
Caucasian n=114 |
Black n=56 |
||
| Dose (mg/kg) |
Trough Concentrations (ng/mL) |
Dose (mg/kg) |
Trough Concentrations (ng/mL) |
|
| Day 7 | 0.18 | 12.0 | 0.23 | 10.9 |
| Month 1 | 0.17 | 12.8 | 0.26 | 12.9 |
| Month 6 | 0.14 | 11.8 | 0.24 | 11.5 |
| Month 12 | 0.13 | 10.1 | 0.19 | 11.0 |
Pediatric liver transplantation patients without pre-existing renal or hepatic dysfunction have required and tolerated higher doses than adults to achieve similar blood concentrations. Therefore, it is recommended that therapy be initiated in pediatric patients at a starting IV dose of 0.03-0.05 mg/kg/day and a starting oral dose of 0.15-0.20 mg/kg/day. Dose adjustments may be required. Experience in pediatric kidney transplantation patients is limited.
Due to the reduced clearance and prolonged half-life, patients with severe hepatic impairment (Pugh > 10) may require lower doses of Prograf. Close monitoring of blood concentrations is warranted.
Due to the potential for nephrotoxicity, patients with renal or hepatic impairment should receive doses at the lowest value of the recommended IV and oral dosing ranges. Further reductions in dose below these ranges may be required. Prograf therapy usually should be delayed up to 48 hours or longer in patients with post-operative oliguria.
Prograf should not be used simultaneously with cyclosporine. Prograf or cyclosporine should be discontinued at least 24 hours before initiating the other. In the presence of elevated Prograf or cyclosporine concentrations, dosing with the other drug usually should be further delayed.
Monitoring of tacrolimus blood concentrations in conjunction with other laboratory and clinical parameters is considered an essential aid to patient management for the evaluation of rejection, toxicity, dose adjustments and compliance. Factors influencing frequency of monitoring include but are not limited to hepatic or renal dysfunction, the addition or discontinuation of potentially interacting drugs and the posttransplant time. Blood concentration monitoring is not a replacement for renal and liver function monitoring and tissue biopsies.
Although there is a lack of direct correlation between tacrolimus concentrations and drug efficacy, data from Phase II and III studies of liver transplant patients have shown an increasing incidence of adverse events with increasing trough blood concentrations. Most patients are stable when trough whole blood concentrations are maintained between 5 to 20 ng/mL. Long term posttransplant patients often are maintained at the low end of this target range.
Data from the Phase III study indicates that trough concentrations of tacrolimus in whole blood, as measured by IMx®, were most variable during the first week of dosing. During the first three months, 80% of the patients maintained trough concentrations between 7-20 ng/mL, and then between 5-15 ng/mL, through one-year.
Prograf injection (tacrolimus injection) 5mg (for IV infusion only)Supplied as a sterile solution in 1 mL ampules containing the equivalent of 5 mg of anhydrous tacrolimus per mL, in boxes of 10 ampules (NDC 0469-3016-01). Store and Dispense Made in Ireland |
Prograf capsules (tacrolimus capsules) 0.5 mgOblong, light yellow, branded with red "0.5 mg" on the
capsule cap and " Prograf capsules (tacrolimus capsules) 1 mg Oblong, white, branded with red "1 mg" on the capsule
cap and " Prograf capsules (tacrolimus capsules) 5mg Oblong, grayish/red, branded with white "5 mg" on the
capsule cap and " Store and Dispense Made in Japan |
Manufactured for:
Fujisawa Healthcare, Inc.
Deerfield, IL 60015-2548
Rx only
ZL40306
1. CDC: Recommendations of the Advisory Committee on Immunization Practices: Use of vaccines and immune globulins in persons with altered immunocompetence. MMWR 1993;42(RR-4):1-18.
607" on
the capsule body, supplied in 100-count plastic bottles (NDC 0469-0607-73) containing
the equivalent of 0.5 mg anhydrous tacrolimus.