Desmopressin (Monograph)

Brand names: DDAVP, Minirin, Stimate
Drug class: Pituitary
ATC class: H01BA02
VA class: HS702
CAS number: 62357-86-2

Medically reviewed by Drugs.com on Jan 22, 2024. Written by ASHP.

Introduction

Synthetic polypeptide analog of arginine vasopressin (antidiuretic hormone [ADH]);¹⁰¹ ¹⁰² ¹¹¹ ¹¹² ¹¹⁴ ¹¹⁶ ¹¹⁷ ^a reduces urinary output and plasma osmolality and increases urine osmolality, as well as dose-dependent increases in plasma factor VIII (antihemophilic factor), plasminogen activator, and, to a lesser degree, factor VIII-related antigen and ristocetin cofactor activities.¹⁰¹ ¹⁰² ¹¹² ¹¹⁴ ¹¹⁷ ^a

Uses for Desmopressin

Diabetes Insipidus

Intranasally, orally, or parenterally for prevention or control of polydipsia, polyuria, and dehydration in diabetes insipidus caused by a deficiency of endogenous posterior pituitary ADH (neurohypophyseal diabetes insipidus).¹⁰¹ ¹⁰² ¹¹¹ ¹¹² ¹¹⁶ ¹¹⁷ ^a

Intranasal desmopressin considered drug of choice for chronic treatment of mild to severe neurohypophyseal diabetes insipidus, because of relatively long duration of action and relative lack of adverse effects.^a

Polyuria and Polydipsia

Intranasally, orally, or parenterally for management of temporary polyuria and polydipsia associated with trauma or surgery in the pituitary region.¹⁰¹ ¹⁰² ¹¹¹ ¹¹² ¹¹⁶ ¹¹⁷ ^a

Not effective in controlling polyuria caused by renal disease, nephrogenic diabetes insipidus, hypokalemia or hypercalcemia; variable efficacy in controlling polyuria secondary to administration of lithium.¹⁰¹ ¹⁰² ¹¹¹ ¹¹² ¹¹⁶ ¹¹⁷ ^a

Primary Nocturnal Enuresis

Orally for management of primary nocturnal enuresis.¹⁰³ ¹⁰⁵ ¹⁰⁶ ¹⁰⁷ ¹¹²

Used alone or as an adjunct to behavioral therapy and/or other nondrug measures; may be effective in some cases refractory to standard therapies (e.g., imipramine, enuresis alarms).¹⁰⁵ ¹⁰⁷ ¹¹²

Although some desmopressin intranasal preparations (i.e., solutions containing 0.1 mg/mL) initially received approval by FDA for treatment of primary nocturnal enuresis, this approval was withdrawn in 2007 because of the risk of serious hyponatremia that may result in seizures and death, particularly in children.¹⁰¹ ¹¹⁵ ¹¹⁷ (See Water Intoxication under Cautions.)

Treatment usually not indicated until a child reaches 6 years of age; condition will spontaneously remit in 15% of patients every year thereafter.¹⁰³ ¹⁰⁴ ¹⁰⁵ ¹⁰⁶

Rule out other possible etiologies (e.g., neurologic and/or spinal abnormalities, diabetes insipidus or diabetes mellitus, chronic renal failure, bacteriuria [especially in girls]) before initiation of drug therapy.¹⁰⁴ ¹⁰⁶

Hemophilia A

Generally indicated in patients with hemophilia A with factor VIII coagulant activity >5%;¹⁰⁰ ¹¹¹ ¹¹⁴ designated an orphan drug by FDA for this use.^a

Intranasally or parenterally for management of spontaneous or trauma-induced bleeding episodes (e.g., hemarthrosis, intramuscular hematoma, mucosal bleeding) in patients with mild hemophilia A.¹⁰⁰ ¹⁰⁸ ¹¹¹ ¹¹⁴

Intranasally or parenterally for maintenance of hemostasis during surgical procedures and postoperatively¹⁰⁰ ¹⁰⁸ ¹¹¹ ¹¹³ ¹¹⁴ ¹¹⁶ when administered 30 minutes prior to scheduled procedure.¹¹⁶

Not indicated for patients with hemophilia A with factor VIII coagulant activity ≤5%,¹⁰⁰ ¹¹¹ ¹¹⁴ ^a ¹¹⁶ hemophilia B,^a or patients with factor VIII antibodies.^a Use may be justified in patients with factor VIII coagulant activity between 2–5% in certain clinical situations; carefully monitor patient if drug is used in this situation.^a ¹¹¹ ¹¹⁶

Not effective in patients with severe hemophilia A.^a

von Willebrand Disease

Generally indicated in patients with mild to moderate classic von Willebrand disease (type 1) with factor VIII coagulant activity >5%;¹¹¹ ¹¹⁴ ¹¹⁶ designated an orphan drug by FDA for this use.^a

Parenterally for maintenance of hemostasis during surgical procedures and postoperatively^a when administered 30 minutes prior to scheduled procedure in patients with mild to moderate type 1 von Willebrand disease.¹¹¹ ¹¹⁶

Drug of choice for management of mild to moderate type 1 von Willebrand disease,¹⁰⁸ ¹⁰⁹ ¹¹⁰ especially in patients with plasma factor VIII activity >5%.¹⁰⁰ ¹¹¹ ¹¹⁴ ¹¹⁶

Patients with severe homozygous von Willebrand disease with factor VIII coagulant activity and factor VIII/von Willebrand antigen concentrations <1% least likely to respond; variable response in other patients depending on type of molecular defect associated with disease.¹¹¹ ¹¹⁶ ^a

Not indicated for patients with severe type 1 von Willebrand disease or when there is evidence of an abnormal molecular form of factor VIII antigen.¹¹¹ ¹¹⁴ ¹¹⁶ ^a

May be effective for management of bleeding in some, but not all, patients with type 2A, 2M, or 2N von Willebrand disease^{† [off-label]}.¹⁰⁸ ¹⁰⁹ ¹¹⁰ ¹¹⁸ ¹¹⁹ ¹²⁰

Usually not used in patients with type 2B von Willebrand disease^{† [off-label]} because of an increased risk of thromboembolic events and transient thrombocytopenia;¹⁰⁰ ¹¹⁰ ¹¹¹ ¹¹⁴ ¹¹⁸ ¹¹⁹ ¹²⁰ although, has been effectively used in some patients with type 2B von Willebrand disease^{† [off-label]}.¹¹⁰ ¹¹⁹

Not effective for management of bleeding in patients with type 3 von Willebrand disease^{† [off-label]}.¹¹⁰ ¹¹⁸ ¹¹⁹ ¹²⁰

Uremia

Has been used IV to increase factor VIII activity and reduce bleeding time in uremic patients^{† [off-label]} with prolonged bleeding times and hemorrhagic tendencies.^a Reduced bleeding time and normal hemostasis observed in some additional uremic patients who received IV drug before surgery or renal biopsy.^a

Diagnostic Uses

Has been used intranasally in adults and children to evaluate ability of kidneys to concentrate urine^†.^a

Sickle Cell Anemia

Has been used intranasally in a small number of patients with sickle cell anemia to induce hyponatremia resulting in decreased mean corpuscular hemoglobin concentrations and degree of sickling for the prevention and treatment of sickle cell crisis^†, but safety and efficacy not established.^a

Desmopressin Dosage and Administration

Administration

Administer intranasally, orally, or by sub-Q injection, direct IV injection, or slow IV infusion.¹⁰⁰ ¹⁰¹ ¹⁰² ¹¹¹ ¹¹² ¹¹⁴ ¹¹⁶ ¹¹⁷

Repeated administration every 12–24 hours may result in a gradual diminution of the increase in plasma factor VIII activity observed with a single dose; initial response reproducible when a period of 2–3 days or 1–6 weeks elapses between IV or intranasal administration, respectively.¹¹¹ ¹¹⁴ ¹¹⁶ ¹¹⁷ ^a

Intranasal Administration

Use intranasal preparations in children under adult supervision in order to monitor dose and fluid intake.¹⁰¹ ¹¹⁵ ¹¹⁷

Nasal solutions containing 0.1 mg of drug per mL used for treatment of diabetes insipidus;¹⁰¹ ¹⁰² ¹¹⁷ nasal solution containing 1.5 mg of drug per mL used for treatment of hemophilia A or von Willebrand disease.¹¹⁴

Administer nasal solutions containing 0.1 or 1.5 mg of drug per mL using the spray pump supplied by manufacturers;¹⁰¹ ¹¹⁴ alternatively, nasal solutions containing 0.1 mg/mL may be administered using a calibrated nasal tube supplied by manufacturers.¹⁰¹ ¹⁰² ¹¹⁷

Intranasal spray pump provided by manufacturers delivers 0.1 mL of solution per actuation.¹⁰¹ ¹¹⁴ When administering nasal solution containing 0.1 mg/mL using the spray pump, each 0.1-mL spray delivers a dose of 10 mcg; administer the solution using a nasal tube if a dose other than a multiple of 10 mcg is required (e.g., in pediatric patients).¹⁰¹

Nasal tube has 4 graduation markings that measure 0.05, 0.1, 0.15, or 0.2 mL and may be used to administer 5, 10, 15, or 20 mcg, respectively.¹⁰² ¹¹⁷

When administering nasal solution containing 1.5 mg/mL using the spray pump, each 0.1-mL spray delivers a dose of 150 mcg; use parenteral therapy if a dose other than a multiple of 150 mcg is required.¹¹⁴

Administer a test dose of the nasal solution containing 1.5 mg/mL prior to initial use to establish appropriate patient response in coagulation profile.

Administer nasal solution intranasally according to the manufacturer’s instructions to ensure that drug is deposited high in nasal cavity and does not pass down the throat.^a

Generally not administered intranasally when changes in nasal mucosa (e.g., scarring, edema) may cause erratic, unreliable absorption of drug;¹⁰¹ ¹⁰² ¹¹⁴ ¹¹⁷ ^a do not use or discontinue drug until nasal problems resolve.¹⁰¹ ¹⁰² ¹¹⁴ ¹¹⁷ Consider using desmopressin injection.¹⁰¹ ¹⁰² ¹¹⁴ ¹¹⁷

Do not administer intranasally when nasal congestion and blockage, nasal discharge, atrophy of nasal mucosa, or severe atrophic rhinitis is present;¹⁰¹ ¹⁰² ¹¹¹ ¹¹⁴ ¹¹⁶ ¹¹⁷ however, patients with nasal congestion and blockage have often responded well to intranasal therapy.¹⁰¹ ¹⁰² ¹¹⁷

Intranasal therapy may be inappropriate when patient has impaired consciousness.¹⁰¹ ¹⁰² ¹¹¹ ¹¹⁴ ¹¹⁶ ¹¹⁷

Alternative route of administration may be needed when nasal packing is present or during recovery from surgery in patients who have undergone cranial surgical procedures (e.g., transsphenoidal hypophysectomy).¹⁰¹ ¹⁰² ¹¹⁶ ¹¹⁷ ¹¹¹

IV Administration

For solution and drug compatibility information, see Stability: Compatibility.

Monitor BP and pulse during infusion.^a

Dilution

Hemophilia A or von Willebrand disease, IV infusion: Dilute the appropriate dose in 10 or 50 mL of 0.9% sodium chloride injection for administration in children weighing ≤10 kg or in adults and children weighing >10 kg, respectively.^a

Rate of Administration

Hemophilia A or von Willebrand disease, IV infusion: Slowly infuse IV over 15–30 minutes.¹¹¹ ¹¹⁶ ^a

Dosage

Available as desmopressin acetate; dosage expressed in terms of salt.¹⁰² ¹¹¹ ¹¹⁴ ¹¹⁶ ¹¹⁷

Diabetes Insipidus or Polyuria and Polydipsia: Adjust dosage according individual requirements (e.g., diurnal pattern of response).¹⁰¹ ¹⁰² ¹¹¹ ¹¹² ¹¹⁶ ¹¹⁷ ^a Estimate response by both adequate duration of sleep and adequate, not excessive, water turnover.¹⁰¹ ¹⁰² ¹¹¹ ¹¹² ¹¹⁶ ¹¹⁷ ^a Adjust morning and evening doses separately for an adequate diurnal rhythm of water turnover.¹⁰¹ ¹⁰² ¹¹¹ ¹¹² ¹¹⁶ ¹¹⁷ ^a

Primary Nocturnal Enuresis: Adjust dosage according individual requirements and response.¹¹²

Hemophilia A or von Willebrand Disease: Determine need for additional doses of drug or use of blood products for hemostasis based on clinical response (determined by laboratory tests) and condition of patient.¹¹¹ ¹¹⁴ ¹¹⁶ ^a Consider tendency toward tachyphylaxis (decreasing responsiveness) to drug when doses are repeated more frequently than every 48 hours.¹¹¹ ¹¹⁴ ¹¹⁶ ^a

von Willebrand Disease: Recommended (by National Hemophilia Foundation’s Medical and Scientific Advisory Council [MASAC]) that drug be administered no more frequently than once every 24 hours and used for no more than 3 consecutive days, unless such therapy is recommended by a clinician with expertise in treatment of the disease.¹⁰⁹

Pediatric Patients

Diabetes Insipidus

Neurohypophyseal

Intranasal

Children 3 months to 12 years of age: Initially, ≤5 mcg (0.05 mL of a solution containing 0.1 mg/ml).¹⁰¹ ¹⁰² ¹¹⁷ ^a

Usual dosage range: 5–30 mcg (0.05–0.3 mL of a solution containing 0.1 mg/mL) daily given intranasally in a single evening dose or in 2 divided doses.¹⁰¹ ¹⁰² ¹¹⁷ ^a

Use lowest effective dosage; about 25–33% of children and adults controlled with a single daily dose.¹⁰¹ ¹⁰² ¹¹⁷ ^a

Restrict fluid intake.¹⁰¹ ¹¹⁷

Oral

Children ≥4 years of age: Initially, 0.05 mg twice daily; adjust subsequent dosage according to response.¹¹²

0.1–0.8 mg daily given in divided doses is optimal dosage range for most patients.¹¹²

Increase or decrease total daily dosage in the range of 0.1–1.2 mg divided into 2 or 3 daily doses as needed to obtain adequate antidiuresis.¹¹²

Initiate oral therapy 12 hours after the last intranasal dose in patients who previously received intranasal therapy.¹¹²

Restrict fluid intake.¹¹²

Children ≥12 years of age: Usually, 2–4 mcg daily by direct IV injection given in 2 divided doses.¹¹¹ ¹¹⁶ ^a

Generally, administer one-tenth of the maintenance intranasal dosage parenterally in patients being switched from intranasal to direct IV injection therapy.¹¹¹ ¹¹⁶ ^a

Use lowest effective dosage.^a During long-term use, patients rarely may develop tolerance to drug and require cautious increase in dosage to achieve an adequate therapeutic response.^a

Restrict fluid intake.¹¹⁶

Sub-Q

Children ≥12 years of age: Usually, 2–4 mcg daily by sub-Q injection given in 2 divided doses.¹¹¹ ¹¹⁶ ^a

Generally, administer one-tenth of the maintenance intranasal dosage parenterally in patients being switched from intranasal to sub-Q injection therapy.¹¹¹ ¹¹⁶ ^a

Use lowest effective dosage.^a During long-term use, patients rarely may develop tolerance to drug and require cautious increase in dosage to achieve an adequate therapeutic response.^a

Restrict fluid intake.¹¹⁶

Primary Nocturnal Enuresis

Oral

Children ≥6 years of age: Initially, 0.2 mg at bedtime; dose may be adjusted up to 0.6 mg to achieve desired response.¹¹² In children being switched from intranasal to oral therapy, initiate oral therapy the night following (24 hours after) the last intranasal dose.¹¹² Duration of therapy not established in pediatric patients responding to therapy; some experts have suggested it is reasonable to continue therapy for 3–6 months, and after 3–6 months, therapy can be withdrawn and the patient reevaluated.¹²¹ ¹²² ¹²³ ¹²⁴

Restrict fluid intake for a minimum of 1 hour before drug administration and continue fluid restriction until next morning or at least 8 hours after drug administration.¹¹² ¹¹⁵ Some experts recommend that not more than 240 mL of fluid be consumed by children on any night when drug is used.¹²¹

Interrupt drug therapy during episodes of fluid and/or electrolyte imbalance (e.g., systemic infections, fever, recurrent vomiting or diarrhea) and under conditions associated with increased water intake (e.g., extremely hot weather, vigorous exercise).¹¹² ¹¹⁵

Hemophilia A

Intranasal

Children 11 months to 12 years of age: Usually, 300 mcg (0.1 mL or 1 spray from the spray pump into each nostril of a solution containing 1.5 mg/mL).¹¹⁴ Dosage of 150 mcg (0.1 mL or 1 spray from the spray pump into a single nostril of a solution containing 1.5 mg/mL) may be sufficient in patients who weigh <50 kg.¹¹⁴ Administer 2 hours prior to surgery if using preoperatively.¹¹⁴

IV

Children ≥3 months of age: Usually, 0.3 mcg/kg by slow IV infusion; administer 30 minutes prior to scheduled procedure if using preoperatively.¹¹¹ ¹¹⁶ ^a

Restrict fluid intake.¹¹⁶

von Willebrand Disease

Type 1

Intranasal

Children ≥3 months of age: Usually, 0.3 mcg/kg by slow IV infusion; administer 30 minutes prior to scheduled procedure if using preoperatively.¹¹¹ ¹¹⁶ ^a

Restrict fluid intake.¹¹⁶

Diagnostic Uses†

Testing for Renal Urine Concentrating Capacity†

Intranasal

10 mcg (0.1 mL of a solution containing 0.1 mg of drug per mL) has been administered intranasally in nonfasting infants 1–12 weeks of age.^a ¹⁷

20 mcg (0.2 mL of a solution containing 0.1 mg of drug per mL) has been administered intranasally in nonfasting children 2–15 years of age.^a ¹⁷

Urine sample was collected in 1–5 hours and specific gravity of urine was determined.^a An average individual usually concentrates urine to a specific gravity of ≥1.020 under test conditions.^a

Adults

Diabetes Insipidus

Neurohypophyseal

Intranasal

10–40 mcg (0.1–0.4 mL or 1–4 sprays from the spray pump of a solution containing 0.1 mg/mL) given intranasally in 1–3 divided doses daily.¹⁰¹ ¹⁰² ¹¹⁷ ^a

Alternatively, 5–40 mcg (0.05–0.4 mL of a solution containing 0.1 mg/mL) has been recommended.^a

Most adults require 20 mcg daily administered in 2 divided doses in the morning and the evening.¹⁰¹ ¹⁰² ¹¹⁷ ^a

Use lowest effective dosage; about 25–33% of adults and children controlled with a single daily dose.¹⁰² ¹¹⁷ ^a

Restrict fluid intake.¹⁰¹ ¹¹⁷

Oral

Initially, 0.05 mg twice daily; adjust subsequent dosage according to response.¹¹²

0.1–0.8 mg daily given in divided doses is optimal dosage range for most patients.¹¹²

Increase or decrease total daily dosage in the range of 0.1–1.2 mg divided into 2 or 3 daily doses as needed to obtain adequate antidiuresis.¹¹²

Initiate oral therapy 12 hours after the last intranasal dose in patients who previously received intranasal therapy.¹¹²

Restrict fluid intake.¹¹²

Usually, 2–4 mcg daily by IV injection given in 2 divided doses.¹¹¹ ¹¹⁶ ^a

Generally, administer one-tenth of the maintenance intranasal dosage parenterally in patients being switched from intranasal to direct IV injection therapy.¹¹¹ ¹¹⁶ ^a

Use lowest effective dosage.^a During long-term use, patients rarely may develop tolerance to drug and require cautious increase in dosage to achieve an adequate therapeutic response.^a

Restrict fluid intake.¹¹⁶

Sub-Q

Usually, 2–4 mcg daily by sub-Q injection given in 2 divided doses.¹¹¹ ¹¹⁶ ^a

Generally, administer one-tenth of the maintenance intranasal dosage parenterally in patients being switched from intranasal to sub-Q injection therapy.¹¹¹ ¹¹⁶ ^a

Use lowest effective dosage.^a During long-term use, patients rarely may develop tolerance to drug and require cautious increase in dosage to achieve an adequate therapeutic response.^a

Restrict fluid intake.¹¹⁶

Primary Nocturnal Enuresis

Oral

Initially, 0.2 mg at bedtime; dose may be adjusted up to 0.6 mg to achieve desired response.¹¹² Initiate oral therapy the night following (24 hours after) the last intranasal dose in patients previously on intranasal therapy.¹¹²

Restrict fluid intake for a minimum of 1 hour before drug administration and continue fluid restriction until next morning or at least 8 hours after drug administration.¹¹² ¹¹⁵

Hemophilia A

Intranasal

Usually, 300 mcg (0.1 mL or 1 spray from the spray pump into each nostril of a solution containing 1.5 mg/mL).¹¹⁴ Dosage of 150 mcg (0.1 mL or 1 spray from the spray pump into a single nostril of a solution containing 1.5 mg/mL) may be sufficient in patients who weigh <50 kg.¹¹⁴ Administer 2 hours prior to surgery if using preoperatively.¹¹⁴

IV

Usually, 0.3 mcg/kg by slow IV infusion; administer 30 minutes prior to scheduled procedure if using preoperatively.¹¹¹ ¹¹⁶ ^a

Restrict fluid intake.¹¹⁶

von Willebrand Disease

Type 1

Intranasal

Usually, 0.3 mcg/kg by slow IV infusion; administer 30 minutes prior to scheduled procedure if using preoperatively.¹¹¹ ¹¹⁶ ^a

Restrict fluid intake.¹¹⁶

Diagnostic Uses†

Testing for Renal Urine Concentrating Capacity†

Intranasal

10–40 mcg (0.1–0.4 mL of a solution containing 0.1 mg of drug per mL) has been administered intranasally to fasting or nonfasting adults.^a ¹² ²² ²³

Urine sample was collected in 1–5 hours and specific gravity of urine was determined.^a Average individual usually concentrates urine to a specific gravity of ≥1.020 under test conditions.^a

Special Populations

Geriatric Patients

Select dosage with caution, usually initiating therapy at the low end of the dosing range because of age-related decreases in hepatic, renal, and/or cardiac function and concomitant disease and drug therapy.¹⁰¹ ¹¹² ¹¹⁶ ¹¹⁷ (See Geriatric Use under Cautions.)

Cautions for Desmopressin

Contraindications

Known hypersensitivity to desmopressin acetate or any ingredient in the formulation.¹⁰¹ ¹⁰² ¹¹¹ ¹¹² ¹¹⁴ ¹¹⁶ ¹¹⁷ ^a
Moderate to severe renal impairment (Cl_cr <50 mL/minute).¹⁰¹ ¹¹² ¹¹⁶ ¹¹⁷
Hyponatremia or a history of hyponatremia.¹⁰¹ ¹¹² ¹¹⁵ ¹¹⁶ ¹¹⁷

Warnings/Precautions

Warnings

Water Intoxication

In late 2007, FDA reported results of a review of 61 postmarketing cases of hyponatremic-related seizures associated with use of desmopressin.¹¹⁵ In 55 cases, sodium concentrations ranged from 104–130 mEq/L during the seizure event.¹¹⁵ Two of these 55 cases were fatal; both patients experienced hyponatremia and seizures.¹¹⁵ However, direct contribution of drug to fatalities not clear.¹¹⁵ Intranasal formulations were used in 36 cases; 25 of these cases involved pediatric patients (i.e., patients <17 years of age).¹¹⁵ Most commonly reported indication for use in the 25 pediatric patients was nocturnal enuresis.¹¹⁵ In 39 of the 61 cases, patients received at least one concomitant drug or disease that also may be associated with hyponatremia and/or seizures.¹¹⁵ As a result, use of intranasal preparations for treatment of primary nocturnal enuresis no longer is approved by FDA; other approved indications for individual intranasal preparations were not changed.¹¹⁵

Reserve intranasal preparations for situations in which oral therapy is not feasible.¹⁰¹ ¹¹⁷

Use with caution in patients at risk for water intoxication with hyponatremia.¹¹⁵

Hyponatremia reported very rarely during international postmarketing surveillance.¹⁰¹ ¹¹² ¹¹⁵ ¹¹⁶ ¹¹⁷ Desmopressin is a potent antidiuretic and use may result in water intoxication and/or hyponatremia; hyponatremia may be fatal unless properly diagnosed and treated.¹⁰¹ ¹¹² ¹¹⁶ ¹¹⁷ Fluid restriction recommended; careful medical supervision required.¹⁰¹ ¹¹² ¹¹⁵ ¹¹⁶ ¹¹⁷

Carefully adjust fluid intake downwards, particularly in pediatric and geriatric patients, to reduce the risk of potential water intoxication and hyponatremia.¹⁰¹ ¹¹² ¹¹⁶ ¹¹⁷ Observe all patients for signs and symptoms associated with hyponatremia (i.e., headache, nausea/vomiting, decreased serum sodium, weight gain, restlessness, fatigue, lethargy, disorientation, depressed reflexes, appetite loss, irritability, muscle weakness, spasms or cramps, abnormal mental status [e.g., hallucinations, decreased consciousness, confusion]); severe symptoms may include seizure, coma, and/or respiratory arrest.¹⁰¹ ¹¹² ¹¹⁵ ¹¹⁶ ¹¹⁷ Consider the possibility of a rare occurrence of a substantial decrease in plasma osmolality that may result in seizures, which may lead to coma.¹⁰¹ ¹⁰² ¹¹¹ ¹¹² ¹¹⁴ ¹¹⁶ ¹¹⁷

Use with caution in patients with habitual or psychogenic polydipsia and in patients who are receiving certain drugs (e.g., tricyclic antidepressants, SSRIs) as these patients may be more likely to drink excessive amounts of water resulting in an increased risk for hyponatremia.¹⁰¹ ¹¹² ¹¹⁵ ¹¹⁶ ¹¹⁷ (See Specific Drugs under Interactions.)

Type 2B von Willebrand Disease

Do not use in patients with type 2B or platelet-type (pseudo) von Willebrand disease^† because of the risk of platelet aggregation and thrombocytopenia.¹¹¹ ¹¹⁴ ¹¹⁶ ^a (See von Willebrand Disease under Uses.)

Sensitivity Reactions

Hypersensitivity Reactions

Severe allergic reactions reported rarely.¹⁰¹ ¹⁰² ¹¹¹ ¹¹² ¹¹⁴ ¹¹⁶ ¹¹⁷ Anaphylaxis reported rarely with IV and intranasal administration, including isolated cases of fatal anaphylaxis with IV administration.¹⁰¹ ¹⁰² ¹¹¹ ¹¹² ¹¹⁴ ¹¹⁶ ¹¹⁷

Not known whether antibodies to drug are produced after repeated administration.¹¹¹ ¹¹⁴ ¹¹⁶

General Precautions

Cardiovascular Effects

Changes in BP resulting in either a slight increase in BP, which may respond to dosage reduction, or a transient decrease in BP and a compensatory increase in heart rate reported infrequently.¹⁰¹ ¹⁰² ¹¹¹ ¹¹² ¹¹⁴ ¹¹⁶ ¹¹⁷ ^a

Thrombotic events (e.g., thrombosis, acute cerebrovascular thrombosis, acute MI) reported rarely in patients predisposed to thrombus formation; causal relationship to drug not determined.¹¹¹ ¹¹⁴ ¹¹⁶ ^a

Use with caution in patients with coronary artery insufficiency and/or hypertensive cardiovascular disease¹⁰¹ ¹⁰² ¹¹¹ ¹¹² ¹¹⁴ ¹¹⁶ ¹¹⁷ ^a or in patients predisposed to thrombus formation.¹¹¹ ¹¹⁴ ¹¹⁶ ^a

Diseases Associated with Fluid and Electrolyte Imbalances

Use with caution in patients with conditions associated with fluid and electrolyte imbalances (e.g., cystic fibrosis, heart failure, renal disorders); these patients are prone to hyponatremia.¹⁰¹ ¹⁰² ¹¹¹ ¹¹² ¹¹⁴ ¹¹⁶ ¹¹⁷ (See Water Intoxication under Cautions.)

Patient Monitoring

Diabetes Insipidus or Polyuria and Polydipsia Associated with Head Trauma or Surgery: Monitor urine volume and osmolality, and in some cases, plasma osmolality.¹⁰¹ ¹⁰² ¹¹¹ ¹¹² ¹¹⁶ ¹¹⁷ ^a

Primary Nocturnal Enuresis: Monitor serum electrolytes at least once if therapy is continued for >7 days.¹⁰¹ ¹⁰² ¹¹⁷ ^a

Hemophilia A: Monitor factor VIII and factor VIII/ristocetin cofactor (von Willebrand factor) activities, factor VIII antigen concentrations, and aPTT.¹¹¹ ¹¹⁴ ¹¹⁶ ^a Determine factor VIII coagulant activity prior to initiating therapy for hemostasis; do not rely upon drug if factor VIII coagulant activity is <5% of normal.¹¹¹ ¹¹⁴ ¹¹⁶ ^a

von Willebrand Disease: Monitor factor VIII and factor VIII/ristocetin cofactor activities and factor VIII/von Willebrand factor antigen concentrations to ensure an adequate response is being achieved; determination of skin bleeding time also may be useful.¹¹¹ ¹¹⁴ ¹¹⁶ ^a

Specific Populations

Pregnancy

Category B.¹⁰¹ ¹⁰² ¹¹¹ ¹¹² ¹¹⁴ ¹¹⁶ ¹¹⁷

Lactation

Not known whether drug is distributed into milk; use with caution.¹⁰¹ ¹⁰² ¹¹¹ ¹¹² ¹¹⁴ ¹¹⁶ ¹¹⁷ ^a

Pediatric Use

Carefully restrict fluid intake in pediatric patients to prevent possible hyponatremia and water intoxication.¹⁰¹ ¹⁰² ¹¹¹ ¹¹² ¹¹⁴ ¹¹⁶ ¹¹⁷ ^a (See Water Intoxication under Cautions.)

Intranasal therapy has no effect on growth hormone, prolactin, or LH concentrations in children.^a

Diabetes Insipidus:Desmopressin tablets have been used safely for up to 44 months in pediatric patients ≥4 years of age with diabetes insipidus.¹¹² In younger pediatric patients, adjust dosage according to individual need to prevent excessive decrease in plasma osmolality resulting in hyponatremia and possible seizures.¹¹²

Safety and efficacy of desmopressin injection not established in pediatric patients <12 years of age with diabetes insipidus.¹¹¹ ¹¹⁶ ^a

Carefully adjust dosage of oral therapy or nasal solution (containing 0.1 mg of drug per mL) according to individual needs and tolerance in pediatric patients with diabetes insipidus, with particular attention to the risk of an extreme decrease in plasma osmolality and resulting hyponatremia or seizures in young children.¹⁰¹ ¹⁰² ¹¹² ¹¹⁷ ^a

Occasional change in response to nasal solution containing 0.1 mg of drug per mL in pediatric patients with diabetes insipidus reported (e.g., decreased responsiveness, shortened duration of effect), usually after periods >6 months.¹⁰² ¹¹⁷ ^a No evidence that change in responsiveness results from development of binding antibodies; may result from local inactivation of peptide.¹⁰² ¹¹⁷ ^a

Intranasal drug preferred to vasopressin injection and oral antidiuretic agents (e.g., chlorpropamide) because of frequency of adverse effects of these agents in pediatric patients with diabetes insipidus.^a

Nocturnal Enuresis: Desmopressin tablets have been used safely for <6 months in pediatric patients ≥6 years of age with primary nocturnal enuresis.¹¹²

Interrupt therapy during acute intercurrent illness characterized by fluid and/or electrolyte imbalance (e.g., systemic infections, fever, recurrent vomiting or diarrhea) and under conditions associated with increased water intake (e.g., extremely hot weather, vigorous exercise).¹¹² ¹¹⁵

Hemophilia or von Willebrand Disease: Do not use the nasal solution containing 1.5 mg of drug per mL for the treatment of hemophilia A or von Willebrand disease in pediatric patients <11 months of age; safety and efficacy established in pediatric patients 11 months to 12 years of age.¹¹⁴

Do not use desmopressin injection for the management of hemophilia A or von Willebrand disease in pediatric patients <3 months of age.¹¹¹ ¹¹⁶ ^a

Geriatric Use

Carefully restrict fluid intake in geriatric patients to prevent possible hyponatremia and water intoxication.¹⁰¹ ¹¹² ¹¹⁴ ¹¹⁶ ¹¹⁷ (See Water Intoxication under Cautions.) Hyponatremia and fluid overload reported during postmarketing surveillance.¹¹⁴

Insufficient experience in patients ≥65 years of age to determine whether geriatric patients respond differently than younger patients.¹⁰¹ ¹¹² ¹¹⁴ ¹¹⁶ ¹¹⁷ Other reported clinical experience has not identified differences in response between geriatric patients and younger adults.¹⁰¹ ¹¹² ¹¹⁶ ¹¹⁷

Select dosage with caution because of age-related decreases in hepatic, renal, and/or cardiac function and concomitant disease and drug therapy.¹⁰¹ ¹¹² ¹¹⁶ ¹¹⁷ (See Geriatric Patients under Dosage and Administration.)

Substantially eliminated by kidneys; risk of toxic reactions may be greater in patients with impaired renal function.¹⁰¹ ¹¹² ¹¹⁶ ¹¹⁷ Monitor renal function and adjust dosage accordingly since geriatric patients are more likely to have decreased renal function.¹⁰¹ ¹¹² ¹¹⁶ ¹¹⁷

Renal Impairment

Contraindicated in patients with moderate to severe renal impairment (Cl_cr <50 mL/minute).¹⁰¹ ¹¹² ¹¹⁶ ¹¹⁷

Common Adverse Effects

With intranasal therapy, adverse effects may include transient headache,¹⁰¹ ¹⁰² ¹¹² ¹¹⁴ ¹¹⁷ ^a nausea,¹⁰¹ ¹⁰² ¹¹² ¹¹⁴ ¹¹⁷ ^a nasal congestion,¹⁰¹ ¹⁰² ¹¹⁴ ¹¹⁷ ^a rhinitis,¹⁰¹ ¹⁰² ¹¹⁴ ¹¹⁷ ^a flushing (e.g., facial),¹⁰¹ ¹⁰² ¹¹² ¹¹⁴ ¹¹⁷ ^a mild abdominal cramps or pain,¹⁰¹ ¹⁰² ¹¹² ¹¹⁴ ¹¹⁷ ^a epistaxis,¹⁰¹ ¹⁰² ¹¹⁴ ¹¹⁷ ^a sore throat,¹⁰¹ ¹⁰² ¹¹⁴ ¹¹⁷ ^a cough,¹⁰¹ ¹⁰² ¹¹⁴ ¹¹⁷ ^a upper respiratory infection,¹⁰¹ ¹⁰² ¹¹⁴ ¹¹⁷ ^a dizziness,¹⁰¹ ¹⁰² ¹¹⁴ ¹¹⁷ ^a conjunctivitis,¹⁰¹ ¹⁰² ¹¹⁷ ^a ocular edema,¹⁰¹ ¹⁰² ¹¹⁷ ^a lacrimation disorder,¹⁰¹ ¹⁰² ¹¹⁷ ^a itchy or light-sensitive eyes,¹¹⁴ asthenia,¹⁰¹ ¹⁰² ¹¹⁷ ^a chills,¹⁰¹ ¹⁰² ¹¹⁴ ¹¹⁷ ^a warm feeling,¹¹⁴ nostril pain,¹⁰¹ ¹⁰² ¹¹⁷ ^a vomiting,¹¹⁴ ^a GI disorder,¹⁰¹ ¹⁰² ¹¹⁷ ^a somnolence,¹¹⁴ ^a insomnia,¹¹⁴ ^a pain,¹¹⁴ ^a chest pain,¹¹⁴ ^a palpitations,¹¹⁴ ^a tachycardia,¹¹⁴ ^a dyspepsia,¹¹⁴ edema,¹¹⁴ agitation,¹¹⁴ ^a balanitis,¹¹⁴ ^a vulval pain,¹¹⁴ ^a increased BP,¹⁰¹ ¹⁰² ¹¹⁷ ^a hyponatremia,^a severe allergic reactions (including anaphylaxis),¹⁰¹ ¹⁰² ¹¹⁷ convulsion,^a coma.^a

With oral therapy, adverse effects may include increased AST,¹¹² headache,¹¹² abnormal thinking,¹¹² diarrhea,¹¹² edema-weight gain.¹¹²

With parenteral therapy, adverse effects may include transient headache,¹¹¹ ¹¹² ¹¹⁶ ^a nausea,¹¹² ¹¹⁴ ¹¹⁶ ^a mild abdominal cramps,¹¹² ¹¹⁴ ¹¹⁶ ^a vulval pain,¹¹⁴ ¹¹⁶ ^a injection site reactions (local erythema, swelling, burning or severe pain),¹¹⁴ ¹¹⁶ facial flushing,¹¹² ¹¹⁴ ¹¹⁶ ^a BP changes (increased BP; decreased BP with compensatory increased heart rate),¹¹⁶ ^a tachycardia,^a hyponatremia,¹¹⁶ ^a excessive water retention,^a water intoxication,¹¹⁴ ¹¹⁶ ^a severe allergic reactions (including anaphylaxis),¹¹⁶ ^a thrombotic events (acute cerebrovascular thrombosis, acute MI).¹¹⁴ ¹¹⁶ ^a

Drug Interactions

Drugs that Increase the Risk of Water Intoxication with Hyponatremia

Use with caution in patients receiving concomitant therapy with drugs that may increase the risk of water intoxication with hyponatremia.¹⁰¹ ¹¹² ¹¹⁵ ¹¹⁶ ¹¹⁷ (See Water Intoxication under Cautions.)

Specific Drugs

Drug	Interaction	Comments
Alcohol	Possible decreased antidiuretic response to desmopressin^a	Use with caution^a
Aminocaproic acid	Concomitant therapy has been used without adverse effects¹¹¹ ¹¹⁴ ¹¹⁶
Antidepressants, tricyclics (e.g., imipramine)	Hyponatremic seizures reported rarely in patients receiving desmopressin and imipramine during postmarketing surveillance¹⁰¹ ¹¹² ¹¹⁶ ¹¹⁷ Possible increased risk of water intoxication with hyponatremia.¹⁰¹ ¹¹² ¹¹⁵ ¹¹⁶ ¹¹⁷	Use with caution¹⁰¹ ¹¹² ¹¹⁵ ¹¹⁶ ¹¹⁷
Carbamazepine	Prior administration of carbamazepine decreased duration of action of desmopressin^a Possible increased risk of water intoxication with hyponatremia.¹⁰¹ ¹¹² ¹¹⁵ ¹¹⁶ ¹¹⁷	Use with caution¹⁰¹ ¹¹² ¹¹⁶ ¹¹⁷
Chlorpromazine	Possible increased risk of water intoxication with hyponatremia.¹⁰¹ ¹¹² ¹¹⁵ ¹¹⁶ ¹¹⁷	Use with caution¹⁰¹ ¹¹² ¹¹⁶ ¹¹⁷
Chlorpropamide	Possible potentiation of antidiuretic response^a
Clofibrate	Potentiation and prolongation of antidiuretic effect of desmopressin^a
Demeclocycline	Possible decreased antidiuretic response to desmopressin^a	Use with caution^a
Epinephrine	Large doses of epinephrine may decrease the antidiuretic response to desmopressin^a	Use with caution^a
Fludrocortisone	Possible potentiation of antidiuretic response^a
Heparin	Possible decreased antidiuretic response to desmopressin^a	Use with caution^a
Lamotrigine	Possible increased risk of water intoxication with hyponatremia.¹⁰¹ ¹¹² ¹¹⁵ ¹¹⁶ ¹¹⁷	Use with caution¹⁰¹ ¹¹² ¹¹⁶ ¹¹⁷
Lithium	Possible decreased antidiuretic response to desmopressin^a	Use with caution^a
NSAIAs	Possible increased risk of water intoxication with hyponatremia.¹⁰¹ ¹¹² ¹¹⁵ ¹¹⁶ ¹¹⁷	Use with caution¹⁰¹ ¹¹² ¹¹⁶ ¹¹⁷
Opiates	Possible increased risk of water intoxication with hyponatremia.¹⁰¹ ¹¹² ¹¹⁵ ¹¹⁶ ¹¹⁷	Use with caution¹⁰¹ ¹¹² ¹¹⁶ ¹¹⁷
Oxybutynin	Hyponatremic seizures reported rarely in patients receiving desmopressin and oxybutynin during postmarketing surveillance¹⁰¹ ¹¹² ¹¹⁶ ¹¹⁷
SSRIs	Possible increased risk of water intoxication with hyponatremia.¹⁰¹ ¹¹² ¹¹⁵ ¹¹⁶ ¹¹⁷	Use with caution¹⁰¹ ¹¹² ¹¹⁵ ¹¹⁶ ¹¹⁷
Urea	Possible potentiation of antidiuretic response^a
Vasopressor agents		Carefully monitor patient if desmopressin doses as large as 0.3 mcg/kg are used with other vasopressor agents¹⁰¹ ¹⁰² ¹¹¹ ¹¹² ¹¹⁴ ¹¹⁶ ¹¹⁷

Desmopressin Pharmacokinetics

Absorption

Bioavailability

About 10–20% of a dose is absorbed through nasal mucosa following intranasal administration.^a

Minimally absorbed from GI tract following oral administration; bioavailability is about 5% compared with intranasal administration and about 0.16% compared with IV administration of the drug.¹¹²

Peak plasma concentrations attained by 0.9 or 1.5 hours following oral or intranasal administration, respectively.¹¹²

Bioavailability of a nasal solution (containing 1.5 mg of drug per mL) is about 3.3–4.1%; peak plasma concentrations attained 40–45 minutes after a dose.¹¹⁴

Exact fraction of drug absorbed following sub-Q injection not quantitatively determined; bioavailability determined qualitatively using urine output data.¹¹¹ ¹¹⁶

Onset

Antidiuretic effects occur within 15–60 minutes or at 60 minutes and peak in 1–5 or 4–7 hours following intranasal or oral administration, respectively.^a ¹¹²

Increased plasma concentrations of factor VIII and von Willebrand factor evident within 30 minutes and peak at about 1.5 hours following intranasal administration of 150–450 mcg of drug (1–3 sprays of a solution containing 1.5 mg of drug per mL).¹¹⁴

Increased plasma factor VIII activity occurs within 15–30 minutes and peaks between 1.5–2 hours following IV infusion.¹¹¹ ¹¹⁶ ^a

Duration

Varies among patients with a specific dose.^a

Antidiuretic effects persist 5–21 hours and abruptly end over a period of 60–90 minutes following intranasal administration.^a

Special Populations

Nasal congestion reportedly does not interfere with efficacy of intranasal drug, however, increased dosage may be required.^a

Percentage increase of factor VIII concentrations in patients with mild hemophilia A and von Willebrand disease not substantially different from healthy individuals.¹¹¹ ¹¹⁴ ¹¹⁶

Distribution

Extent

Not known whether distributed into human milk ¹⁰¹ ¹⁰² ¹¹¹ ¹¹² ¹¹⁴ ¹¹⁶ ¹¹⁷ or crosses placenta.^a

Elimination

Metabolism

Metabolic fate not known.^a

Does not appear to be degraded by aminopeptidases or other peptidases that cleave oxytocin and endogenous vasopressin in the plasma during late pregnancy.^a

Elimination Route

Excreted principally in urine.¹⁰¹ ¹¹² ¹¹⁶ ¹¹⁷

Half-life

3.3–3.5 hours following intranasal administration of 150–450 mcg of drug (1–3 sprays of a solution containing 1.5 mg of drug per mL).¹¹⁴

1.5–2.5 hours (on average and independent of dosage) following oral administration.¹¹²

Biphasic; mean initial and terminal plasma half-life of 7.8 and 75.5 minutes (range: 0.4–4 hours), respectively, following IV or intranasal (solution containing 0.1 mg of drug per mL) administration.¹⁰¹ ¹⁰² ¹¹¹ ¹¹⁶ ¹¹⁷ ^a

Special Populations

Renal clearance of drug decreases with decreasing renal function.¹⁰¹ ¹¹² ¹¹⁶ ¹¹⁷ ¹²⁵ Terminal half-lives of desmopressin averaged 3.7, 4.8, 7.2, or 10 hours following administration of a single IV dose of 2 mcg of drug in individuals with normal renal function (average Cl_Cr of 103 mL/minute), mild renal impairment (average Cl_Cr of 72 mL/minute), moderate renal impairment (average Cl_Cr of 37 mL/minute), or severe renal impairment (average Cl_Cr of 16 mL/minute; not on dialysis), respectively.¹²⁵ (See Contraindications under Cautions.)

Stability

Storage

Intranasal

Solution

Commercially available nasal solutions preserved with benzalkonium chloride: Controlled room temperature (20–25°C, not to exceed 25°C);¹⁰¹ ¹¹⁴ store container in upright position.¹⁰¹

Commercially available nasal solutions preserved with chlorobutanol: 2–8°C; stable for 3 weeks at controlled room temperature (20–25°C).¹⁰² ¹¹⁷

Commercially available nasal solutions containing 1.5 mg of drug per mL: Discard 6 months after opening.¹¹⁴

Oral

Tablets

20–25°C; avoid exposure to excessive heat or light.¹¹²

Parenteral

Injection

2–8°C;¹⁰⁰ ¹¹¹ avoid freezing.¹¹¹ ¹¹⁶ ^a

Compatibility

Parenteral

Solution Compatibility

Compatible
Sodium chloride 0.9%¹¹¹ ¹¹⁶ ^a

Actions

Synthetic analog of arginine vasopressin (antidiuretic hormone [ADH]); vasopressin maintains serum osmolality within a normal range by increasing reabsorption of water by the collecting ducts in the kidneys resulting in increased urine osmolality and decreased urinary flow rate.¹⁰¹ ¹⁰² ¹¹¹ ¹¹² ¹¹⁴ ¹¹⁶ ¹¹⁷ ^a
Desmopressin has same effects on water reabsorption as does vasopressin in patients with neurohypophyseal diabetes insipidus.^a
Elicits a greater antidiuretic response, on a weight basis, than does arginine vasopressin.^a
Therapeutic doses do not directly affect urinary sodium or potassium excretion, or serum sodium, potassium, or creatinine concentrations.^a
Antidiuretic potency of IV administration is about 10 times that following intranasal administration.¹⁰¹ ¹⁰² ¹¹¹ ¹¹⁶ ¹¹⁷ ^a
Dose-dependent increases in plasma factor VIII (antihemophilic factor), plasminogen activator, and, to a lesser degree, factor VIII-related antigen and ristocetin cofactor activities.^a
Rapidly increases plasminogen activator activity following IV administration; however, clinically important fibrinolysis not reported to date.¹¹¹ ¹¹⁴ ¹¹⁶ ^a
Elicits a greater increase in plasma factor VIII activity, on a weight basis, than does arginine vasopressin in patients with hemophilia or type I von Willebrand disease.¹¹¹ ¹¹⁴ ¹¹⁶ ^a
Reduced smooth muscle contracting and vasopressor properties compared with vasopressin and lypressin (no longer commercially available in the US);¹⁰¹ ¹⁰² ¹¹¹ ¹¹² ¹¹⁴ ¹¹⁶ ¹¹⁷ ^a mean arterial pressure may increase as much as 15 mm Hg with intranasal doses of ≥40 mcg.^a
Usual intranasal doses do not cause skin pallor or severe smooth muscle or abdominal cramps, unlike vasopressin and lypressin.^a
Not reported to stimulate uterine contractions.^a
Does not stimulate adrenocorticotropic hormone release or increase plasma cortisol concentrations, unlike vasopressin.^a

Advice to Patients

Importance of discussing with patient and/or guardian the risk of potential water intoxication and/or hyponatremia, fluid restriction (particularly in pediatric and geriatric patients), and monitoring of fluid intake (particularly during acute intercurrent illness [e.g., systemic infections, fever, recurrent vomiting or diarrhea] and under conditions associated with increased water intake [e.g., extremely hot weather, vigorous exercise]).¹⁰¹ ¹¹² ¹¹⁵ ¹¹⁶ ¹¹⁷ Importance of promptly informing clinicians if the patient’s fluid intake changes or if symptoms of hyponatremia (e.g., nausea, vomiting, fatigue, muscle cramps or weakness) occur.¹¹⁵
Importance of instructing patients on proper use of nasal tube or spray pump in order to obtain optimum results.^a Importance of informing patients to consult patient instructions on nasal spray provided by the manufacturer before use.¹⁰¹ ¹¹⁴ Importance of administering intranasal preparations in children under adult supervision in order to monitor dose and fluid intake.¹⁰¹ ¹¹⁵ ¹¹⁷
Importance of informing patients that a bottle of nasal solution containing 0.1 mg of drug per mL accurately delivers 50 doses of 10 mcg of drug per dose.¹⁰¹ Discard any solution remaining after 50 doses, since the amount delivered thereafter may be substantially <10 mcg of drug.¹⁰¹ Do not attempt to transfer any remaining solution to another bottle.¹⁰¹
Importance of informing patients that a bottle of nasal solution containing 1.5 mg of drug per mL accurately delivers 25 doses of 150 mcg of drug per dose.¹¹⁴ Discard any solution remaining after 25 doses, since the amount delivered thereafter may be substantially <150 mcg of drug.¹¹⁴ Do not attempt to transfer any remaining solution to another bottle.¹¹⁴
Importance of patients receiving nasal solution containing 1.5 mg of drug per mL to inform clinicians if bleeding is not controlled.¹¹⁴
Importance of informing clinicians of existing or contemplated concomitant therapy, including prescription and OTC drugs (e.g., tricyclic antidepressants, SSRIs, chlorpromazine, opiates, NSAIAs, lamotrigine, carbamazepine), as well as any concomitant illnesses (e.g., hyponatremia, habitual or psychogenic polydipsia, cystic fibrosis, heart failure, renal disorders).¹⁰¹ ¹⁰² ¹¹¹ ¹¹² ¹¹⁴ ¹¹⁶ ¹¹⁷
Importance of women informing clinicians if they are or plan to become pregnant or plan to breast-feed.¹⁰¹ ¹⁰² ¹¹¹ ¹¹² ¹¹⁴ ¹¹⁶ ¹¹⁷
Importance of informing patients of other important precautionary information.¹⁰¹ ¹⁰² ¹¹¹ ¹¹² ¹¹⁴ ¹¹⁶ ¹¹⁷ (See Cautions.)

Preparations

Excipients in commercially available drug preparations may have clinically important effects in some individuals; consult specific product labeling for details.

Please refer to the ASHP Drug Shortages Resource Center for information on shortages of one or more of these preparations.

* available from one or more manufacturer, distributor, and/or repackager by generic (nonproprietary) name

Desmopressin Acetate
Routes	Dosage Forms	Strengths	Brand Names	Manufacturer
Nasal	Solution	0.1 mg/mL*	DDAVP Nasal Spray (with benzalkonium chloride; with spray pump)	Sanofi-Aventis
			DDAVP Rhinal Tube (with chlorobutanol; with 2 calibrated nasal tubes; refrigerate)	Sanofi-Aventis
			Desmopressin Acetate Nasal Spray (with chlorobutanol)	Apotex
			Desmopressin Acetate Rhinal Tube (with chlorobutanol; with 2 calibrated nasal tubes; refrigerate)	Ferring
			Minirin (with chlorobutanol)	Apotex
		1.5 mg/mL	Stimate Nasal Spray (with benzalkonium chloride; with spray pump)	CSL Behring
Oral	Tablets	0.1 mg*	DDAVP (with povidone)	Sanofi-Aventis
			Desmopressin Acetate Tablets	Apotex
		0.2 mg*	DDAVP (with povidone)	Sanofi-Aventis
			Desmopressin Acetate Tablets	Apotex
Parenteral	Injection	4 mcg/mL*	DDAVP (with chlorobutanol)	Sanofi-Aventis
			Desmopressin Acetate Injection (with chlorobutanol)	Ferring

† Off-label: Use is not currently included in the labeling approved by the US Food and Drug Administration.

References

Only references cited for selected revisions after 1984 are available electronically.

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17. Aronson AS, Svenningsen NW. DDAVP test for estimation of renal concentrating capacity in infants and children. Arch Dis Child. 1974; 49:654-9. http://www.pubmedcentral.nih.gov/picrender.fcgi?tool=pmcentrez&artid=1648998&blobtype=pdf http://www.ncbi.nlm.nih.gov/pubmed/4425527?dopt=AbstractPlus

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100. Rhone-Poulenc Rorer. DDAVP (desmopressin acetate) injection 4 mcg/mL prescribing information (dated 1997 Sep) and DDAVP (desmopressin acetate) injection 15 mcg/mL prescribing information (dated 1997 Nov). In: Physician’s desk reference. 53rd ed. Montvale, NJ: Medical Economics Company Inc; 1999:2582-4.

101. Sanofi-Aventis. DDAVP (desmopressin acetate) nasal spray prescribing information. Bridgewater, NJ; 2007 Jul.

102. Ferring Pharmaceuticals. Desmopressin acetate rhinal tube prescribing information. Tarrytown, NY; 1998 Aug.

103. Anon. Desmopressin for nocturnal enuresis. Med Lett Drugs Ther. 1990; 32:38-9. http://www.ncbi.nlm.nih.gov/pubmed/2182991?dopt=AbstractPlus

104. Voiding dysfunction: nocturnal enuresis. In: Lehrman RE, Vaughn VC III, eds. Nelson textbook of pediatrics. 12th ed. Philadelphia: WB Saunders Company; 1983:1160-1.

105. Klauber GT. Clinical efficacy and safety of desmopressin in the treatment of nocturnal enuresis. J Pediatr. 1989; 114(Suppl 4, Part 2):719-22. http://www.ncbi.nlm.nih.gov/pubmed/2647954?dopt=AbstractPlus

106. Rushton HG. Nocturnal enuresis: epidemiology, evaluation, and currently available treatment options. J Pediatr. 1989; 114(Suppl 4, Part 2):691-6. http://www.ncbi.nlm.nih.gov/pubmed/2647951?dopt=AbstractPlus

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114. CSL Behring. Stimate (desmopressin acetate) nasal spray 1.5 mg/mL prescribing information. King of Prussia, PA; 2007 Jul.

115. Food and Drug Administration (FDA). FDA alert for healthcare professionals on desmopressin acetate (marketed as DDAVP Nasal Spray, DDAVP Rhinal Tube, DDAVP, DDVP, Minirin, and Stimate Nasal Spray). From FDA website. Accessed 2007 Dec 4. http://www.fda.gov/Drugs/DrugSafety/PostmarketDrugSafetyInformationforPatientsandProviders/ucm125561.htm

116. Sanofi-Aventis. DDAVP (desmopressin acetate) injection 4 mcg/mL prescribing information. Bridgewater, NJ; 2007 Jul.

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119. Shord SS, Lindley CM. Coagulation products and their uses. Am J Health Syst Pharm. 2000; 57:1403-17; quiz 1418-20. http://www.ncbi.nlm.nih.gov/pubmed/10938981?dopt=AbstractPlus

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122. Fritz G, Rockney R, and the Work Group on Quality Issues and the American Academy of Child and Adolescent Psychiatry. AACP official action: practice parameter for the assessment and treatment of children and adolescents with enuresis. J Am Acad Child Adloesc Psychiatry. 2004; 43:1540-50.

123. Voiding dysfunction: nocturnal enuresis. In: Behrman RE, Kliegman RM, Jenson HB, eds. Nelson textbook of pediatrics. 17th ed. Philadelphia: WB Saunders Company; 2004:1809.

124. Thiedke CC. Nocturnal enuresis. Am Fam Physician. 2003; 67:1499-1506. http://www.ncbi.nlm.nih.gov/pubmed/12722850?dopt=AbstractPlus

125. Agersø H, Seiding Larsen L, Riis A et al. Pharmacokinetics and renal excretion of desmopressin after intravenous administration to healthy subjects and renally impaired patients. Br J Clin Pharmacol. 2004; 58:352-8.

a. AHFS Drug Information 2007. McEvoy GK, ed. Desmopressin Acetate. Bethesda, MD: American Society of Health-System Pharmacists; 2007: 3219-22.