inidine, terfenadine) should therefore be used with caution.

ize or rate of growth, were not shown in clinical trials performed with octreotide acetate injection; these trials were not optimally designed to detect such effects. carcinoid tumors octreotide acetate is indicated for the symptomatic treatment of patients with metastatic carcinoid tumors where it suppresses or inhibits the severe diarrhea and flushing episodes associated with the disease. octreotide acetate studies were not designed to show an effect on the size, rate of growth, or development of metastases. vasoactive intestinal peptide tumors (vipomas) octreotide acetate is indicated for the treatment of the profuse watery diarrhea associated with vip-secreting tumors. octreotide acetate studies were not designed to show an effect on the size, rate of growth, or development of metastases.

c hepatitis, or pancreatitis during octreotide acetate therapy or following its withdrawal. one patient developed ascending cholangitis during octreotide acetate therapy and died. there have been postmarketing reports of cholelithiasis (gallstones) resulting in complications requiring cholecystectomy. if complications of cholelithiasis are suspected, discontinue octreotide acetate and treat appropriately. complete atrioventricular block patients who receive octreotide acetate injection intravenously may be at increased risk for higher degree atrioventricular blocks. in postmarketing reports, complete atrioventricular block was reported in patients receiving intravenous octreotide acetate during surgical procedures. in majority of patients, octreotide acetate was given at higher than recommended doses and/or as a continuous intravenous infusion. the safety of continuous intravenous infusion has not been established in patients receiving octreotide acetate for the approved indications. consider cardiac monitoring in patients receiving octreotide acetate intravenously.

de acetate is stable in sterile isotonic saline solutions or sterile solutions of dextrose 5% in water for 24 hours. it may be diluted in volumes of 50 to 200 ml and infused intravenously over 15 to 30 minutes or administered by iv push over 3 minutes. in emergency situations (e.g., carcinoid crisis), it may be given by rapid bolus. the initial dosage is usually 50 mcg administered twice or 3 times daily. upward dose titration is frequently required. dosage information for patients with specific tumors follows. acromegaly dosage may be initiated at 50 mcg 3 times a day. beginning with this low dose may permit adaptation to adverse gastrointestinal effects for patients who will require higher doses. insulin growth factor-1 (igf-1; somatomedin c) levels every 2 weeks can be used to guide titration. alternatively, multiple growth hormone (gh) levels at 0 to 8 hours after octreotide acetate injection administration permit more rapid titration of dose. the goal is to achieve gh levels less than 5 ng/ml or igf-1 (somatomedin c) levels less than 1.9 unit/ml in males and less than 2.2 unit/ml in females. the dose most commonly found to be effective is 100 mcg 3 times a day, but some patients require up to 500 mcg 3 times a day for maximum effectiveness. doses greater than 300 mcg/day seldom result in additional biochemical benefit, and if an increase in dose fails to provide additional benefit, the dose should be reduced. igf-1 (somatomedin c) or gh levels should be reevaluated at 6-month intervals. octreotide acetate should be withdrawn yearly for approximately 4 weeks from patients who have received irradiation to assess disease activity. if gh or igf-1 (somatomedin c) levels increase and signs and symptoms recur, octreotide acetate therapy may be resumed. carcinoid tumors the suggested daily dosage of octreotide acetate during the first 2 weeks of therapy ranges from 100 to 600 mcg/day in 2 to 4 divided doses (mean daily dosage is 300 mcg). in the clinical studies, the median daily maintenance dosage was approximately 450 mcg, but clinical and biochemical benefits were obtained in some patients with as little as 50 mcg, while others required doses up to 1,500 mcg/day. however, experience with doses above 750 mcg/day is limited. vipomas daily dosages of 200 to 300 mcg in 2 to 4 divided doses are recommended during the initial 2 weeks of therapy (range, 150 to 750 mcg) to control symptoms of the disease. on an individual basis, dosage may be adjusted to achieve a therapeutic response, but usually doses above 450 mcg/day are not required.

reated with 300 mcg/day than in those treated with 750 mcg/day. vomiting, flatulence, abnormal stools, abdominal distention, and constipation were each seen in less than 10% of patients. in rare instances, gastrointestinal side effects may resemble acute intestinal obstruction, with progressive abdominal distension, severe epigastric pain, abdominal tenderness, and guarding. hypo/hyperglycemia hypoglycemia and hyperglycemia occurred in 3% and 16% of acromegalic patients, respectively, but only in about 1.5% of other patients. symptoms of hypoglycemia were noted in approximately 2% of patients. hypothyroidism in acromegalics, biochemical hypothyroidism alone occurred in 12% while goiter occurred in 6% during octreotide acetate therapy (see precautions - general ) . in patients without acromegaly, hypothyroidism has only been reported in several isolated patients and goiter has not been reported. other adverse events pain on injection was reported in 7.7%, headache in 6% and dizziness in 5%. pancreatitis was also observed (see warnings and precautions ) . other adverse events 1% to 4% other events (relationship to drug not established), each observed in 1% to 4% of patients, included fatigue, weakness, pruritus, joint pain, backache, urinary tract infection, cold symptoms, flu symptoms, injection site hematoma, bruise, edema, flushing, blurred vision, pollakiuria, fat malabsorption, hair loss, visual disturbance, and depression. other adverse events less than 1% events reported in less than 1% of patients and for which relationship to octreotide acetate injection is not established are listed: gastrointestinal (gi): hepatitis, jaundice, increase in liver enzymes, gi bleeding, hemorrhoids, appendicitis, gastric/peptic ulcer, gallbladder polyp; integumentary: rash, cellulitis, petechiae, urticaria, basal cell carcinoma; musculoskeletal: arthritis, joint effusion, muscle pain, raynaud's phenomenon; cardiovascular: chest pain, shortness of breath, thrombophlebitis, ischemia, congestive heart failure, hypertension, hypertensive reaction, palpitations, orthostatic bp decrease, tachycardia; cns: anxiety, libido decrease, syncope, tremor, seizure, vertigo, bell's palsy, paranoia, pituitary apoplexy, increased intraocular pressure, amnesia, hearing loss, neuritis; respiratory: pneumonia, pulmonary nodule, status asthmaticus; endocrine: galactorrhea, hypoadrenalism, diabetes insipidus, gynecomastia, amenorrhea, polymenorrhea, oligomenorrhea, vaginitis; urogenital: nephrolithiasis, hematuria; hematologic: anemia, iron deficiency, epistaxis; miscellaneous: otitis, allergic reaction, increased ck, weight loss. evaluation of 20 patients treated for at least 6 months has failed to demonstrate titers of antibodies exceeding background levels. however, antibody titers to octreotide acetate were subsequently reported in 3 patients and resulted in prolonged duration of drug action in 2 patients. anaphylactoid reactions, including anaphylactic shock, have been reported in several patients receiving octreotide acetate. postmarketing experience the following adverse reactions have been identified during the postapproval use of octreotide acetate. because these reactions are reported voluntarily from a population of uncertain size, it is not always possible to reliably estimate their frequency or establish a causal relationship to drug exposure. hepatobiliary: cholelithiasis, cholecystitis, cholangitis and pancreatitis, which have sometimes required cholecystectomy gastrointestinal: intestinal obstruction hematologic : thrombocytopenia

inidine, terfenadine) should therefore be used with caution.

n octreotide concentration after 6 doses of 40 mg octreotide acetate for injectable suspension administered by intramuscular (im) injection every 4 weeks was approximately 3 ng/ml. steady-state concentrations was achieved after 3 injections of a 40-mg dose. mean bmi increased 0.1 kg/m 2 in octreotide acetate for injectable suspension-treated subjects compared to 0 kg/m 2 in saline control-treated subjects. efficacy was not demonstrated. diarrhea occurred in 11 of 30 (37%) patients treated with octreotide acetate for injectable suspension. no unexpected adverse events were observed. however, with octreotide acetate for injectable suspension at 40 mg once a month, the incidence of new cholelithiasis in this pediatric population (33%) was higher than that seen in other adult indications such as acromegaly (22%) or malignant carcinoid syndrome (24%), where octreotide acetate for injectable suspension was 10 to 30 mg once a month.

he incidence of gallstone or biliary sludge formation was markedly increased (see warnings ) . octreotide suppresses secretion of thyroid stimulating hormone (tsh). pharmacokinetics after subcutaneous injection, octreotide is absorbed rapidly and completely from the injection site. peak concentrations of 5.2 ng/ml (100-mcg dose) were reached 0.4 hours after dosing. using a specific radioimmunoassay, intravenous (iv) and subcutaneous doses were found to be bioequivalent. peak concentrations and area under the curve (auc) values were dose proportional after iv single doses up to 200 mcg and subcutaneous single doses up to 500 mcg and after subcutaneous multiple doses up to 500 mcg 3 times a day (1,500 mcg/day). in healthy volunteers, the distribution of octreotide from plasma was rapid (tα 1/2 = 0.2 h), the volume of distribution (v dss ) was estimated to be 13.6 l, and the total body clearance ranged from 7 l/hr to 10 l/hr. in blood, the distribution into the erythrocytes was found to be negligible and about 65% was bound in the plasma in a concentration-independent manner. binding was mainly to lipoprotein and, to a lesser extent, to albumin. the elimination of octreotide from plasma had an apparent half-life of 1.7 to 1.9 hours compared with 1 to 3 minutes with the natural hormone. the duration of action of octreotide acetate injection is variable but extends up to 12 hours depending upon the type of tumor. about 32% of the dose is excreted unchanged into the urine. in an elderly population, dose adjustments may be necessary due to a significant increase in the half-life (46%) and a significant decrease in the clearance (26%) of the drug. in patients with acromegaly, the pharmacokinetics differs somewhat from those in healthy volunteers. a mean peak concentration of 2.8 ng/ml (100-mcg dose) was reached in 0.7 hours after subcutaneous dosing. the volume of distribution (v dss ) was estimated to be 21.6 ± 8.5 l, and the total body clearance was increased to 18 l/h. the mean percent of the drug bound was 41.2%. the disposition and elimination half-lives were similar to normals. in patients with renal impairment, the elimination of octreotide from plasma was prolonged and total body clearance reduced. in mild renal impairment (cl cr 40 to 60 ml/min), octreotide t 1/2 was 2.4 hours and total body clearance was 8.8 l/hr, in moderate impairment (cl cr 10 to 39 ml/min) t 1/2 was 3 hours and total body clearance 7.3 l/hr, and in severely renally impaired patients not requiring dialysis (cl cr <10 ml/min) t 1/2 was 3.1 hours and total body clearance was 7.6 l/hr. in patients with severe renal failure requiring dialysis, total body clearance was reduced to about half that found in healthy subjects (from approximately 10 l/hr to 4.5 l/hr). patients with liver cirrhosis showed prolonged elimination of drug, with octreotide t 1/2 increasing to 3.7 hr and total body clearance decreasing to 5.9 l/hr, whereas patients with fatty liver disease showed t 1/2 increased to 3.4 hr and total body clearance of 8.2 l/hr.

he elimination of octreotide from plasma had an apparent half-life of 1.7 to 1.9 hours compared with 1 to 3 minutes with the natural hormone. the duration of action of octreotide acetate injection is variable but extends up to 12 hours depending upon the type of tumor. about 32% of the dose is excreted unchanged into the urine. in an elderly population, dose adjustments may be necessary due to a significant increase in the half-life (46%) and a significant decrease in the clearance (26%) of the drug. in patients with acromegaly, the pharmacokinetics differs somewhat from those in healthy volunteers. a mean peak concentration of 2.8 ng/ml (100-mcg dose) was reached in 0.7 hours after subcutaneous dosing. the volume of distribution (v dss ) was estimated to be 21.6 ± 8.5 l, and the total body clearance was increased to 18 l/h. the mean percent of the drug bound was 41.2%. the disposition and elimination half-lives were similar to normals. in patients with renal impairment, the elimination of octreotide from plasma was prolonged and total body clearance reduced. in mild renal impairment (cl cr 40 to 60 ml/min), octreotide t 1/2 was 2.4 hours and total body clearance was 8.8 l/hr, in moderate impairment (cl cr 10 to 39 ml/min) t 1/2 was 3 hours and total body clearance 7.3 l/hr, and in severely renally impaired patients not requiring dialysis (cl cr <10 ml/min) t 1/2 was 3.1 hours and total body clearance was 7.6 l/hr. in patients with severe renal failure requiring dialysis, total body clearance was reduced to about half that found in healthy subjects (from approximately 10 l/hr to 4.5 l/hr). patients with liver cirrhosis showed prolonged elimination of drug, with octreotide t 1/2 increasing to 3.7 hr and total body clearance decreasing to 5.9 l/hr, whereas patients with fatty liver disease showed t 1/2 increased to 3.4 hr and total body clearance of 8.2 l/hr.

ate for up to 5 years. there was also a 15% incidence of uterine adenocarcinomas in the 1,250 mcg/kg/day females compared to 7% in the saline-control females and 0% in the vehicle-control females. the presence of endometritis coupled with the absence of corpora lutea, the reduction in mammary fibroadenomas, and the presence of uterine dilatation suggest that the uterine tumors were associated with estrogen dominance in the aged female rats which does not occur in humans. octreotide acetate did not impair fertility in rats at doses up to 1,000 mcg/kg/day, which represents 7x the human exposure based on body surface area. there are no adequate and well-controlled studies of octreotide use in pregnant women. reproduction studies have been performed in rats and rabbits at doses up to 16 times the highest recommended human dose based on body surface area and revealed no evidence of harm to the fetus due to octreotide. however, because animal reproduction studies are not always predictive of human response, this drug should be used during pregnancy only if clearly needed. in postmarketing data, a limited number of exposed pregnancies have been reported in patients with acromegaly. most women were exposed to octreotide during the first trimester of pregnancy at doses ranging from 100 to 300 mcg/day of octreotide acetate injection or 20 to 30 mg once a month of octreotide acetate for injectable suspension, however some women elected to continue octreotide therapy throughout pregnancy. in cases with a known outcome, no congenital malformations were reported.

light. at room temperature (20°c to 30°c or 70°f to 86°f), octreotide acetate injection is stable for 14 days if protected from light. the solution can be allowed to come to room temperature prior to administration. do not warm artificially. after initial use, multiple dose vials should be discarded within 14 days. single dose vials should be opened just prior to administration and the unused portion discarded. dispose unused product or waste properly. the container closure is not made with natural rubber latex. lake zurich, il 60047 www.fresenius-kabi.com/us 451028k revised: march 2022 fresenius kabi logo