The most common findings in patients with diabetes insipidus are polydipsia, polyuria, and nocturia.

Polyuria is defined as urine output more than 3 L/day in adults or 2 L/m2 in children. In children, symptoms can be nonspecific, and they may present with severe dehydration, constipation, vomiting, fevers, irritability, failure to thrive, and growth retardation. In patients with central nervous system (CNS) tumors, headaches, and visual defects may present in addition to the classic symptoms.

Additional symptoms in patients with diabetes insipidus may include weakness, lethargy, fatigue, and myalgias.

In mentally ill patients, extreme thirst is a good indicator of the problem.

The differentials for polyuria should include primary polydipsia and uncontrolled diabetes mellitus.

Calculate the plasma osmolality: 2[Na+] + [Glucose]/18 + [BUN]/2.8

Calculate the total 24-hour urine volume to confirm polyuria. Obtain baseline values of plasma electrolytes, random serum, and urine osmolality.[8][9][10][11]

To differentiate central and nephrogenic diabetes insipidus, perform a water deprivation test and desmopressin (DDAVP) trial. Typically a 7-hour deprivation test is adequate to diagnose diabetes insipidus. Primary polydipsia may require longer dehydration periods.

In adults, the water restriction test should be discontinued when one of the following is reached:

• Urine osmolality reaches normal reference range
• Urine osmolality stable on two to three consecutive hourly measurements, even with rising plasma osmolality
• Plasma osmolality greater than 295 mosmol/kg to 300 mosmol/kg
• Plasma Na greater than 145 mEq

In newborns and young infants, if nephrogenic diabetes insipidus is suspected the diagnostic test of choice is DDAVP (1 mcg subcutaneously or intravenously over 20 minutes, maximum dose of 0.4 mcg/kg).

In children, the water deprivation test should be closely monitored. If one of the following endpoints are reached discontinue the trial:

• Urine osmolality reaches normal reference range
• Plasma osmolality greater than 295 mosmol/kg to 300 mosmol/kg
• Plasma sodium greater than 145 meq/L
• Loss of 5% of body weight or signs of volume depletion

The water deprivation trial is most accurate when DDAVP is not given. After water deprivation, studies have demonstrated DDAVP can increase urine osmolality greater than 100% incomplete central diabetes insipidus and up to 50% in partial central diabetes insipidus.

In cases of nephrogenic diabetes insipidus, water deprivation suboptimally increases urine osmolality. DDAVP minimally increases urine osmolality in partial nephrogenic diabetes insipidus, with no increase in urine osmolality in complete nephrogenic diabetes insipidus.

Central diabetes insipidus is diagnosed when there is evidence of plasma hyperosmolality (greater than 300 mosm/l), urine hyperosmolality (less than 300 mosm/l or urine/plasma osmolality less than 1), with polyuria (urinary volume greater than 4 mL/kg/hr to 5 mL/kg/hr for two consecutive hours after surgery).

Copeptin and AQP2 have also been utilized to differentiate nephrogenic and central diabetes insipidus. In central diabetes insipidus, AQP2 increases with DDAVP administration. On the contrary, in patients with nephrogenic diabetes insipidus, the AQP2 excretion does not increase after DDAVP administration.

When suspecting a structural cause of diabetes insipidus, MRI imaging can identify malformations of the posterior pituitary.

DDAVP, an ADH analog, can be administered orally, intranasally, subcutaneously, or intravenously. In adults, the dose is ten mcg by nasal insufflation or 4 mcg subcutaneously or intravenously. In newborns or very young infants, the dose is one mcg subcutaneously or intravenously over 20 minutes with a maximum dose of 0.4 mcg/kg.

It is essential to replete fluid losses in diabetes insipidus, as some patients may have thirst impairment and will not respond adequately to water intake.[12][13][14]

Central Diabetes Insipidus

The preferred therapy is DDAVP. Typically, therapy is maintained for the duration of central diabetes insipidus, which varies depending on the cause. The minimum dose should be administered to control polyuria adequately.

It is important to monitor for hyponatremia, as water retention can lead to sodium concentration changes that may cause brain injury. The patients and families should be educated to observe for symptoms of nausea, vomiting, lethargy, headaches, confusion, seizures, and coma.

Other treatment options for central diabetes insipidus include low-solute diet (low salt, low protein), thiazide diuretics, chlorpropamide, carbamazepine, and non-steroidal anti-inflammatory drugs (NSAID).

DDAVP is considered safe the pregnancy.

Nephrogenic Diabetes Insipidus

The first step is correct the underlying cause. If possible, discontinue the offending agent such as lithium.

Low-solute diet may decrease the urine output. The lower amount of total solutes ingested, the lower the urine volume that will be excreted.

Thiazide diuretics may be used in conjunction with dietary changes. The mechanism of administering a diuretic in the setting of polyuria is to promote the reduction of urine volume, which triggers the endogenous release of aldosterone. By having less water delivered distally, there would be less water loss in the collecting tubule, where ADH targets its effects.

Other treatment options include DDAVP and NSAIDs. NSAIDs inhibit prostaglandin synthesis, which has antagonistic the effects of ADH.

• Hypercalcemia
• Hypokalemia
• Sickle cell anemia
• Histiocytosis
• Diabetes mellitus

The prognosis for most patients with DI is excellent as long as the underlying primary cause can be treated. Lithium discontinuation can restore normal kidney function but in some patients, the nephrogenic DI may be permanent. 

As long as the individual has access to water, the mortality can be avoided. However, in children and the elderly, the condition can lead to cardiovascular collapse, fever, and hypernatremia.

Patients should be warned about traveling and be prepared to manage diarrhea and vomiting so as to avoid dehydration. The patient should have easy access to water and should avoid traveling to hot destinations where medical care may not always be available.

Patients with significant electrolyte abnormalities should be closely monitored and admitted to the hospital.

There are many causes of DI and the disorder is best managed by an interprofessional team that includes the primary care provider, nurse practitioner, internist, and a pharmacist. Patient education is key.

The key is to hydrate and replace the electrolytes and then manage the primary condition causing DI. The pharmacist should keep track of all medications that can cause DI and make the appropriate recommendations to the clinician.

The nurse should educate the patient on traveling to hot destinations because dehydration can result in exacerbating the symptoms. If possible travel should be avoided until the condition is treated. 

In post-operative patients, the specific gravity of the urine should be monitored before administering desmopressin. In addition, blood should be drawn regularly and levels of electrolytes monitored.

Outcome

The outlook for patients with DI depends on the cause. For benign causes, the prognosis is good, but if the cause if a malignancy, then the prognosis is guarded.[15][5]