Diabetes Insipidus - Hyperexcision

Last updated: March 22, 2026

Diabetes insipidus is an inability to concentrate urine due to a lack of antidiuretic hormone (ADH) or insensitivity to ADH in the kidneys.

Classification of diabetes inspidus

Classification	Description	Causes
Central diabetes insipidus	Reduced secretion of ADH by the posterior pituitary gland	Idiopathic, tumours, head injury, pituitary surgery, encephalitis, meningitis, Wolfram syndrome (DIDMOAD), mutations in arginine vasopressin-neurophysin II gene (AVP-NPII)
Nephrogenic diabetes insipidus	The kidneys are insensitive to ADH	Lithium, hypercalcaemia, hypokalaemia, kidney disease, mutation in vasopressin-2 receptor, mutation in aquaporin-2 gene
Gestational diabetes inspidus	Occurs in pregnancy	Increased vasopressinase degrades ADH; increased prostaglandins make the kidneys less sensitive to ADH
Dipsogenic diabetes insipidus	Excessive drinking due to impaired thirst mechanism (unquenchable thirst)	Chronic meningitis, multiple sclerosis

Signs and symptoms
- Polydipsia
- Polyuria
- Nocturia
- Dehydration
- Focal neurological deficits due to a space-occupying lesion
Physical examination
- Dry mucous membranes
- Poor skin turgor
- Prolonged capillary refill time
- Tachycardia
- Orthostatic hypotension
- Palpable distended bladder
Differentials
- Diabetes mellitus
- Psychogenic polydipsia
- Diuretic overuse
- Urinary tract infection
- Hypercalcaemia
- Cushing’s syndrome
Investigations
- 24-hour urine collection
  - Dilute urine
- Plasma osmolality
  - Normal plasma osmolality is 285 – 295 mOsmol/kg
- Urine and serum osmolality for the urine to plasma (U:P) osmolality ratio
  - Dilute urine with U:P < 2
- Blood glucose to rule out diabetes
- Serum calcium to rule out hypercalcemia
- UECs
  - Hypenatremia
  - Dilutional hyponatremia may be present in primary polydipsia
- 8-hour water deprivation test: evaluates the kidneys’ ability to concentrate urine. Stage 1 involves fluid deprivation and measuring serum and urine osmolality to evaluate the kidney’s concentrating ability. Stage 2 involves administering desmopressin to differentiate cranial from nephrogenic diabetes insipidus.
  - Urine osmolality > 600 mOsmol/kg in stage 1 with a U: P ratio> 2 for normal concentrating ability
  - Urine concentrates less than normal in primary polydipsia
  - Urine osmolality is increased to > 600 mOsmol/kg after desmopressin
  - No increase in urine osmolality after desmopressin in nephrogenic diabetes insipidus
- Serum copeptin – copeptin is a surrogate marker for ADH (it is produced in equimolar amounts from its precursor)
  - Low copeptin in central diabetes insipidus
  - High copeptin in nephrogenic diabetes insipidus
Treatment
- Correct any underlying causes
- A low-solute diet to reduce osmotic load
- Adequate fluid intake
- Avoid rapid correction of hypernatremia
- Desmopressin for central diabetes insipidus
- Thiazide diuretics (endroflumethiazide) or NSAIDs can be used for nephrogenic diabetes insipidus
  - Prostaglandins locally inhibit the action of ADH
Emergency treatment
- Urgent UECs, serum and urine osmolality
- Monitor serum Na+, urine output and fluid balance
- Intravenous fluids to maintain urine output and to correct hypernatremia
- Trial of desmopressin

Interpretation of the water deprivation test

Diagnosis	Serum osmolality (mOsm/kg)	Urine osmolality (mOsm/kg)	Urine osmolality after desmopressin given (mOsm/kg)
Normal	285-295	>600	Not completed as normal results
Dipsogenic diabetes inspipidus	<300	400-600	No change
Cranial diabetic insipidus	>300	<300	Urine concentrates following desmopressin administration
Nephrogenic diabetes insipidus	>300	< 300	No change following desmopressin

Reference Intervals ›

Biochemistry

ACTH	P: <80 ng/L
ALT	P: 5–35 U/L
Albumin	P: 35–50 g/L
Aldosterone	P: 100–500 pmol/L
Alk. phosphatase	P: 30–130 U/L
α-Amylase	P: 0–180 IU/dL
α-Fetoprotein	S: <10 kU/L
Angiotensin II	P: 5–35 pmol/L
ADH	P: 0.9–4.6 pmol/L
AST	P: 5–35 U/L
Bicarbonate	P: 24–30 mmol/L
Bilirubin	P: 3–17 μmol/L
BNP	P: <50 ng/L
CRP	P: <10 mg/L
Calcitonin	P: <0.1 mcg/L
Calcium (ionized)	P: 1.0–1.25 mmol/L
Calcium (total)	P: 2.12–2.60 mmol/L
Chloride	P: 95–105 mmol/L
Cholesterol	P: <5.0 mmol/L
VLDL	P: 0.128–0.645 mmol/L
LDL	P: <2.0 mmol/L
HDL	P: 0.9–1.93 mmol/L
Cortisol AM	P: 450–700 nmol/L
Cortisol Midnight	P: 80–280 nmol/L
CK ♂	P: 25–195 U/L
CK ♀	P: 25–170 U/L
Creatinine	P: 70–100 μmol/L
Ferritin	P: 12–200 mcg/L
Folate	S: 2.1 mcg/L
FSH	P: 2–8 U/L ♂; >25 menopause
GGT ♂	P: 11–51 U/L
GGT ♀	P: 7–33 U/L
Glucose (fasting)	P: 3.5–5.5 mmol/L
Growth hormone	P: <20 mu/L
HbA1C (DCCT)	B: 4–6%
HbA1C (IFCC)	B: 20–42 mmol/mol
Iron ♂	S: 14–31 μmol/L
Iron ♀	S: 11–30 μmol/L
Lactate (venous)	P: 0.6–2.4 mmol/L
Lactate (arterial)	P: 0.6–1.8 mmol/L
LDH	P: 70–250 U/L
LH	P: 3–16 U/L
Magnesium	P: 0.75–1.05 mmol/L
Osmolality	P: 278–305 mosmol/kg
PTH	P: 0.8–8.5 pmol/L
Potassium	P: 3.5–5.3 mmol/L
Prolactin ♂	P: <450 U/L
Prolactin ♀	P: <600 U/L
PSA	P: 0–4 mcg/mL
Protein (total)	P: 60–80 g/L
Red cell folate	B: 0.36–1.44 μmol/L
Renin (erect)	P: 2.8–4.5 pmol/mL/h
Renin (recumbent)	P: 1.1–2.7 pmol/mL/h
Sodium	P: 135–145 mmol/L
TBG	P: 7–17 mg/L
TSH	P: 0.5–4.2 mU/L
T4	P: 70–140 nmol/L
Free T4	P: 9–22 pmol/L
TIBC	S: 54–75 μmol/L
Triglycerides	P: 0.50–2.3 mmol/L
T3	P: 1.2–3.0 nmol/L
Troponin T	P: <0.1 mcg/L
Urate ♂	P: 210–480 μmol/L
Urate ♀	P: 150–390 μmol/L
Urea	P: 2.5–6.7 mmol/L
Vitamin B12	S: 0.13–0.68 nmol/L
Vitamin D	S: 50 nmol/L

Arterial Blood Gases

pH	7.35–7.45
PaCO₂	4.7–6.0 kPa
PaO₂	>10.6 kPa
Base excess	±2 mmol/L

Urine

Cortisol (free)	<280 nmol/24h
Hydroxyindole acetic acid	16–73 μmol/24h
Hydroxymethylmandelic acid	16–48 μmol/24h
Metanephrines	0.03–0.69 μmol/mmol cr.
Osmolality	350–1000 mosmol/kg
17-Oxogenic steroids ♂	28–30 μmol/24h
17-Oxogenic steroids ♀	21–66 μmol/24h
17-Oxosteroids ♂	17–76 μmol/24h
17-Oxosteroids ♀	14–59 μmol/24h
Phosphate (inorganic)	15–50 mmol/24h
Potassium	14–120 mmol/24h
Protein	<150 mg/24h
Protein/creatinine ratio	<3 mg/mmol
Sodium	100–250 mmol/24h

Haematology

WCC	4.0–11.0 ×10⁹/L
RBC ♂	4.5–6.5 ×10¹²/L
RBC ♀	3.9–5.6 ×10¹²/L
Hb ♂	130–180 g/L
Hb ♀	115–160 g/L
PCV ♂	0.4–0.54 L/L
PCV ♀	0.37–0.47 L/L
MCV	76–96 fL
MCH	27–32 pg
MCHC	300–360 g/L
RDW	11.6–14.6%
Neutrophils	2.0–7.5 ×10⁹/L (40–75%)
Lymphocytes	1.0–4.5 ×10⁹/L (20–45%)
Eosinophils	0.04–0.44 ×10⁹/L (1–6%)
Basophils	0–0.10 ×10⁹/L (0–1%)
Monocytes	0.2–0.8 ×10⁹/L (2–10%)
Platelets	150–400 ×10⁹/L
Reticulocytes	0.8–2.0% / 25–100 ×10⁹/L
Prothrombin time	10–14 s
APTT	35–45 s

Paediatric

Pulse Rate (bpm)
Neonate	140–160
Infant <1yr	120–140
1–5 years	110–130
5–12 years	80–120
>12 years	70–100
Respiratory Rate (tachypnoea)
0–2 months	≥60/min
2–12 months	≥50/min
1–5 years	≥40/min
>5 years	≥30/min
Blood Pressure (mmHg)
Term	65/45
1 year	75/50
4 years	85/60
8 years	95/65
10 years	100/70
Weight Formulas
3–12 months	(a + 9)/2 kg
1–6 years	2a + 8 kg
>6 years	(7a − 5)/2 kg
Haemoglobin (g/dL)
Term newborn	13–20
1 month	11–18
2 months	10–15
1–2 years	10–13
>2 years	11–14
MUAC (6 months–5 years)
Obese	>17.5 cm
Normal	13.5–17.4 cm
At risk	12.5–13.4 cm
Moderate malnutrition	11.5–12.4 cm
Severe malnutrition	<11.5 cm
Developmental Milestones
Social smile	1.5 months
Head control	4 months
Sits unsupported	7 months
Crawls	10 months
Stands unsupported	10–12 months
Walks	12–13 months
Talks	18 months
CSF WBC (/mm³)
Term newborn	0–25
>2 weeks	0–5

Calculator ›

Post DiscussionCancel Reply