Growth Hormone Deficiency Calculator- Free GHD Assessment and GH Stimulation Test Interpreter Tool

Growth Hormone Deficiency Calculator – Free GHD Assessment and GH Stimulation Test Interpreter Tool | Super-Calculator.com

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Growth Hormone Deficiency Calculator

Assess growth hormone deficiency probability using GH stimulation test results with BMI-adjusted diagnostic cutoffs, IGF-1 standard deviation score evaluation, reference range bar visualization, and a clinical decision tree algorithm based on Endocrine Society, AACE, and GH Research Society guidelines. This comprehensive GHD assessment tool supports interpretation of insulin tolerance test (ITT), glucagon stimulation test, GHRH-arginine test, macimorelin test, and clonidine stimulation test results for both pediatric and adult patients.

Important Medical Disclaimer

This calculator is provided for informational and educational purposes only. It is not intended to replace professional medical advice, diagnosis, or treatment. Always consult with a qualified healthcare professional before making any medical decisions. The results from this calculator should be used as a reference guide only and not as the sole basis for clinical decisions.

Patient Age Group

Body Mass Index (kg/m2)25.0

Pituitary or Hypothalamic Disease History

Number of Other Pituitary Hormone Deficiencies

Structural Abnormality on Pituitary MRI

IGF-1 Standard Deviation Score (SDS)-1.5

GH Stimulation Test Type

Peak Growth Hormone Response (ng/mL)2.5

Growth Hormone Stimulation Test Diagnostic Protocol:

The GH stimulation test measures peak growth hormone response to pharmacological stimulation. Diagnostic cutoffs are test-specific and BMI-adjusted for adults. The insulin tolerance test (ITT) uses a cutoff of 3-5 ng/mL. The glucagon stimulation test uses BMI-dependent cutoffs: 3 ng/mL for BMI below 30 and 1 ng/mL for BMI 30 or above. The GHRH-arginine test uses three BMI tiers: 11 ng/mL (BMI under 25), 8 ng/mL (BMI 25-30), and 4.2 ng/mL (BMI over 30). Macimorelin uses a fixed cutoff of 2.8 ng/mL. Children use a standard cutoff of 10 ng/mL regardless of test type. Results should be interpreted alongside IGF-1 SDS, clinical history, pituitary hormone status, and MRI findings per Endocrine Society and AACE guidelines.

Overall GHD Probability

High (82%)

Stimulation Test Used

Glucagon

BMI-Adjusted GH Cutoff

3.0 ng/mL

Peak GH Classification

Deficient

IGF-1 SDS Classification

Low-Normal

Peak Growth Hormone Level on Diagnostic Reference Range

Deficient

Normal

Robust

2.5 ng/mL

Cutoff: 3.0

03.0102030

IGF-1 Standard Deviation Score on Diagnostic Reference Range

Low (below -2)

Low-Norm

Normal

High

-1.5 SDS

-5-2-10+2+3

Peak Growth Hormone Level

2.5 ng/mL – Below Cutoff

IGF-1 Standard Deviation Score

-1.5 SDS – Low-Normal

Pituitary Hormone Deficiencies

2 – Moderate Risk

Structural MRI Abnormality

Present

Clinical Recommendation: Findings suggest high probability of GHD. Consider endocrine referral for comprehensive evaluation and potential GH replacement therapy.

GHD Diagnostic Decision Algorithm

STEP 1: Does the patient have 3 or more other pituitary hormone deficiencies AND structural pituitary abnormality?

YES

STEP 2A: Is IGF-1 SDS below -2.0?

YES

GHD HIGHLY LIKELY
Stimulation testing may not be required
(greater than 95% probability)

PROCEED TO GH STIMULATION TEST
High pretest probability
One test may suffice

STEP 2B: GH Stimulation Test Result?
(Peak GH vs BMI-adjusted cutoff)

Below Cutoff

GHD LIKELY
Consider second test if isolated GHD
One test sufficient with 1-2 other deficiencies

Above Cutoff

GHD UNLIKELY
Consider alternative diagnoses
Repeat if clinical suspicion persists

Stimulation Test Type	BMI Category	Peak GH Cutoff (ng/mL)	Notes
Insulin Tolerance Test (ITT)	All BMI (adults)	3.0 – 5.0	Reference standard; contraindicated in seizures, cardiovascular disease
Glucagon Stimulation Test	BMI below 25	3.0	Most commonly used alternative; 4-hour test
Glucagon Stimulation Test	BMI 25-30 (high pretest)	3.0	High pretest probability
Glucagon Stimulation Test	BMI 25-30 (low pretest)	1.0	Low pretest probability
Glucagon Stimulation Test	BMI 30 or above	1.0	Obesity suppresses GH response
GHRH-Arginine Test	BMI below 25	11.0	May be falsely normal in hypothalamic GHD
GHRH-Arginine Test	BMI 25-30	8.0	GHRH availability may be limited
GHRH-Arginine Test	BMI 30 or above	4.2	Lowest cutoff for obese patients
Macimorelin Oral Test	All BMI (adults)	2.8	Oral administration; 90-minute test
Clonidine Stimulation Test	Pediatric	10.0	First-line in many pediatric centers
Pediatric Standard (all tests)	All BMI (children)	10.0	Two failed tests required for diagnosis

Important Medical Disclaimer

About This Growth Hormone Deficiency Calculator

This growth hormone deficiency calculator is designed for healthcare professionals, medical students, patients, and caregivers seeking to understand how key diagnostic parameters contribute to the assessment of GHD probability. The tool evaluates peak growth hormone levels from stimulation tests, IGF-1 standard deviation scores, the number of concurrent pituitary hormone deficiencies, structural MRI findings, and patient demographics to generate a comprehensive GHD probability estimate.

The calculator interprets GH stimulation test results using BMI-adjusted diagnostic cutoffs established by the Endocrine Society, the American Association of Clinical Endocrinologists (AACE), and the Growth Hormone Research Society. It supports five major stimulation test types: the insulin tolerance test (ITT), glucagon stimulation test, GHRH-arginine test, macimorelin oral test, and clonidine stimulation test, each with their specific diagnostic thresholds and clinical considerations.

The reference range bar visualization displays where peak GH and IGF-1 SDS values fall relative to established diagnostic zones, while the clinical decision tree algorithm guides users through the stepwise diagnostic approach recommended by international endocrine guidelines. The tool dynamically adjusts cutoff values based on patient BMI and selected test type, providing clinically relevant interpretation for each individual assessment scenario.

Growth Hormone Deficiency Calculator: Complete Guide to GHD Assessment, Diagnosis, and Stimulation Test Interpretation

Growth hormone deficiency (GHD) is a clinical syndrome characterized by insufficient secretion of growth hormone (GH) from the anterior pituitary gland, affecting approximately 1 in 4,000 to 1 in 10,000 children and 2 to 3 per 10,000 adults worldwide. Whether presenting as childhood-onset GHD causing short stature and delayed growth, or adult-onset GHD resulting in metabolic changes and reduced quality of life, accurate diagnosis requires a systematic evaluation combining clinical assessment, biochemical testing, and imaging studies. This comprehensive calculator helps healthcare professionals and patients understand how key diagnostic parameters interact in the evaluation of suspected growth hormone deficiency.

Understanding Growth Hormone and Its Physiological Role

Growth hormone is a 191-amino acid polypeptide secreted by somatotroph cells in the anterior pituitary gland. Its secretion follows a pulsatile pattern, primarily regulated by two hypothalamic hormones: growth hormone-releasing hormone (GHRH), which stimulates secretion, and somatostatin, which inhibits it. The largest and most predictable GH pulse occurs approximately one hour after the onset of deep sleep, though secretion is also stimulated by exercise, fasting, stress, and certain amino acids.

GH exerts its biological effects both directly and indirectly through insulin-like growth factor 1 (IGF-1), which is primarily produced by the liver. IGF-1 mediates most of the growth-promoting effects of GH and provides a negative feedback signal to the hypothalamus and pituitary. Because GH secretion is pulsatile and highly variable, random GH measurements are unreliable for diagnostic purposes. Instead, clinicians rely on IGF-1 levels, which remain relatively stable throughout the day, and provocative stimulation tests that challenge the pituitary to secrete GH in response to pharmacological agents.

Causes and Classification of Growth Hormone Deficiency

GHD can be classified by onset (childhood versus adult), etiology (congenital versus acquired), and severity (isolated versus combined with other pituitary hormone deficiencies). Childhood-onset GHD is most commonly idiopathic and hypothalamic in origin. Congenital causes include genetic mutations affecting the GH1 gene, GHRH receptor abnormalities, and central nervous system malformations such as septo-optic dysplasia and pituitary stalk interruption syndrome. Acquired causes in children include cranial irradiation, brain tumors (particularly craniopharyngiomas), meningitis, histiocytosis, and traumatic brain injury.

Adult-onset GHD is most commonly caused by hypothalamic-pituitary tumors and their treatment through surgery or radiation therapy. Pituitary adenomas are the most frequent cause, followed by craniopharyngiomas, which together account for approximately 57% of cases. Less common causes include traumatic brain injury, subarachnoid hemorrhage, vascular events, infiltrative diseases, infections, and autoimmune conditions. Importantly, GH is typically the first anterior pituitary hormone to be affected by pathological insults. Consequently, patients with multiple pituitary hormone deficiencies have a very high probability of concurrent GHD.

Key Point: GH is the Most Vulnerable Pituitary Hormone

Growth hormone is usually the first anterior pituitary hormone lost following hypothalamic-pituitary damage. Patients with three or more additional pituitary hormone deficiencies, a low IGF-1 level (less than -2 SDS), and structural pituitary abnormalities have a greater than 95% probability of GHD and may not require formal stimulation testing.

Clinical Features of Growth Hormone Deficiency

In children, the hallmark features of GHD include diminished height velocity and short stature, typically manifesting as height below the 3rd percentile or more than 2 standard deviations below the mean for age and sex. Growth deceleration, with a height velocity below the 25th percentile, is often the earliest clinical indicator. Other features may include delayed bone age relative to chronological age, increased truncal adiposity, mid-facial hypoplasia (in severe or congenital cases), micropenis in male neonates, and neonatal hypoglycemia. Children with combined pituitary hormone deficiencies may also present with signs of thyroid hormone, cortisol, or gonadotropin deficiency.

In adults, the clinical syndrome of GHD is more subtle and nonspecific. Features include decreased lean body mass, increased central adiposity, reduced exercise capacity, decreased bone mineral density, dyslipidemia with elevated LDL cholesterol, decreased quality of life characterized by fatigue and reduced psychological well-being, and an increased predisposition to cardiovascular disease. Because these symptoms are nonspecific, diagnostic workup for adult GHD should generally only be undertaken when there is reasonable clinical suspicion, such as a history of childhood GHD, structural hypothalamic-pituitary disease, or evidence of other pituitary hormone deficiencies.

Diagnostic Approach: When to Test for GHD

The decision to pursue evaluation for GHD should be guided by clinical context and probability of disease. In children, the GH Research Society consensus guidelines recommend evaluation when specific auxological criteria are met, including severe short stature (height below -3 SDS), height more than 1.5 SDS below the mid-parental height, height below -2 SDS combined with a growth velocity below the 25th percentile, or a decrease in height SDS of more than 0.5 over one year. Evaluation is also indicated in children with known risk factors such as prior cranial irradiation, other pituitary hormone deficiencies, or suggestive radiological findings.

In adults, the Endocrine Society recommends evaluation for patients with structural hypothalamic-pituitary disease, those who have undergone surgery or irradiation in the hypothalamic-pituitary region, patients with traumatic brain injury, and those with evidence of other pituitary hormone deficiencies. Idiopathic adult-onset GHD is extremely rare, and stringent criteria are necessary for this diagnosis, typically requiring two failed stimulation tests along with a low IGF-1 level. Patients with childhood-onset GHD should be retested after achieving adult height, unless they have known genetic mutations, embryopathic lesions, or irreversible structural damage causing multiple hormone deficiencies.

GH Stimulation Test Diagnostic Criteria

Peak GH less than 10 ng/mL (children) = GH Deficient
Peak GH less than 3-5 ng/mL (adults, test-dependent) = Severe GHD

The currently accepted peak GH cutoff for children is 10 ng/mL (micrograms per liter). For adults, cutoffs vary by test type and BMI: ITT uses 3-5 ng/mL, glucagon test uses 1-3 ng/mL (BMI-dependent), GHRH-arginine uses 4-11 ng/mL (BMI-dependent), and macimorelin uses 2.8 ng/mL. Two separate stimulation tests are recommended for children; adults with high pretest probability may require only one.

Growth Hormone Stimulation Tests: Types and Interpretation

Because random GH levels are unreliable due to the pulsatile nature of GH secretion, provocative stimulation tests are the cornerstone of biochemical diagnosis. These tests involve administering a pharmacological agent that stimulates pituitary GH release, followed by serial blood sampling to measure the peak GH response. The choice of stimulation test depends on the clinical context, patient characteristics, contraindications, and local availability.

The insulin tolerance test (ITT) has long been considered the reference standard for diagnosing GHD in both children and adults. It involves intravenous administration of regular insulin (0.1 U/kg) to induce hypoglycemia (blood glucose below 40 mg/dL or 2.2 mmol/L), which is a potent stimulus for GH release. A peak GH response below 3 ng/mL in adults (or below 5 ng/mL by some criteria) confirms severe GHD. However, the ITT is contraindicated in elderly patients, those with a history of seizures, cardiovascular disease, or cerebrovascular disease, and requires close medical supervision with continuous monitoring.

The glucagon stimulation test (GST) has become the most commonly used alternative, owing to its safety profile, reproducibility, and lack of influence by hypothalamic etiology. Intramuscular glucagon is administered at a dose of 1 mg (1.5 mg for patients weighing more than 90 kg), with GH levels measured at baseline and every 30 minutes for 4 hours. Diagnostic cutoffs are BMI-dependent: a peak GH below 3 ng/mL for patients with BMI below 30 kg/m2, and below 1 ng/mL for patients with BMI of 30 kg/m2 or greater.

GHRH-Arginine Test Cutoffs (BMI-Adjusted)

BMI less than 25: Peak GH less than 11.0 ng/mL = GH Deficient
BMI 25-30: Peak GH less than 8.0 ng/mL = GH Deficient
BMI greater than 30: Peak GH less than 4.2 ng/mL = GH Deficient

The GHRH-arginine test involves intravenous GHRH (1 mcg/kg) plus arginine (0.5 g/kg, maximum 30 g). However, it may yield falsely normal results in patients with hypothalamic causes of GHD (such as post-irradiation), because GHRH can still stimulate a functioning pituitary. Use alternative tests in these patients.

The Role of IGF-1 in GHD Diagnosis

Serum IGF-1 is the principal biochemical surrogate marker of GH secretion. Unlike GH, IGF-1 levels remain relatively stable throughout the day without significant pulsatile variation, making a single measurement clinically useful. IGF-1 levels should be interpreted relative to age- and sex-specific reference ranges, typically expressed as standard deviation scores (SDS). An IGF-1 SDS below -2 is considered low and suggestive of GHD, while an IGF-1 SDS below 0 in the appropriate clinical context may also raise suspicion.

However, IGF-1 levels have important limitations in GHD diagnosis. A normal IGF-1 does not exclude GHD, as overlap exists between GH-deficient and GH-sufficient populations, particularly in children with idiopathic GHD. Conversely, low IGF-1 levels can occur in conditions other than GHD, including malnutrition, chronic liver disease, poorly controlled diabetes, hypothyroidism, and the use of oral estrogens. For these reasons, IGF-1 measurement should not be used in isolation for diagnosis but rather integrated with clinical assessment, auxological data, and stimulation test results.

IGF binding protein 3 (IGFBP-3) is the major carrier protein for IGF-1 in the circulation and is also GH-dependent. While IGFBP-3 can provide supplementary diagnostic information, it has similar limitations to IGF-1 and is less widely used in current clinical practice. The combination of IGF-1 and IGFBP-3 measurements may improve diagnostic accuracy compared with either test alone, particularly in younger children where IGF-1 levels are physiologically low.

Key Point: IGF-1 Cannot Confirm or Exclude GHD Alone

A low IGF-1 (below -2 SDS) increases the likelihood of GHD but is not diagnostic in isolation. A normal IGF-1 does not rule out GHD, particularly in children with idiopathic GHD. IGF-1 must always be interpreted alongside clinical findings, growth data, and stimulation test results for accurate diagnosis.

Macimorelin: The Oral Diagnostic Test

Macimorelin is an orally administered ghrelin agonist approved by regulatory agencies for the diagnosis of adult GHD. It stimulates GH secretion through the ghrelin receptor (GHS-R1a) pathway, which is distinct from the GHRH pathway. The test is straightforward: after an overnight fast, patients ingest a single dose of macimorelin (0.5 mg/kg dissolved in water), and GH levels are measured at baseline, 30, 45, 60, and 90 minutes.

A peak GH level below 2.8 ng/mL confirms GHD with good sensitivity and specificity. Macimorelin offers several advantages over traditional stimulation tests, including oral administration, a shorter testing duration, fewer adverse effects, and no risk of hypoglycemia. However, it should not be used in patients taking strong CYP3A4 inhibitors, and its diagnostic performance may be affected by recent GH therapy. Availability and cost considerations may also limit its use in some clinical settings.

Pediatric Considerations in GHD Diagnosis

The diagnosis of GHD in children requires special consideration due to the age-dependent nature of GH secretion and the influence of pubertal status on test results. The currently agreed-upon peak GH cutoff for pediatric stimulation tests is 10 ng/mL, though proposed values of 5, 7, and 10 ng/mL exist on a continuum without definitive evidence supporting any single threshold. Two separate stimulation tests failing to produce an adequate GH response are typically required for diagnosis, except in specific circumstances where the pretest probability is very high.

Sex steroid priming before stimulation testing remains controversial. Some experts advocate for estrogen or testosterone priming in prepubertal children to reduce false-positive results, particularly in those with constitutional delay of growth and puberty. Without priming, prepubertal children may have falsely low GH responses, leading to overdiagnosis of GHD. However, standardized protocols for sex steroid priming are not universally established.

For neonates, stimulation testing is not required if all three of the following criteria are met: documented hypoglycemia, a serum GH level of 5 ng/mL or less, and either a deficiency in another pituitary hormone or ectopic posterior pituitary with pituitary hypoplasia and an abnormal stalk. In older children with established genetic causes, irreversible structural lesions, or panhypopituitarism with low IGF-1, repeated stimulation testing is generally unnecessary.

Transition Period: Retesting from Childhood to Adulthood

Patients diagnosed with childhood-onset GHD face a critical transition period when they reach adult height. Because a significant proportion of children with idiopathic isolated GHD will have normal GH secretion when retested as adults, retesting is recommended after completion of linear growth. Testing should be performed at least one month after discontinuing GH therapy to allow recovery of the hypothalamic-pituitary-GH axis.

Retesting is generally not required for patients with documented genetic or congenital causes of GHD, irreversible hypothalamic-pituitary structural abnormalities, or multiple pituitary hormone deficiencies with low IGF-1 levels. For those requiring retesting, adult diagnostic criteria and cutoff values should be applied, as pediatric cutoffs of 10 ng/mL would be overly stringent for adult assessment. The ITT and macimorelin are the preferred tests for transition patients.

Height Velocity Standard Deviation Score (SDS)

Height Velocity SDS = (Observed HV - Mean HV for Age/Sex) / SD of HV for Age/Sex

Height velocity (HV) is the rate of growth measured in centimeters per year. A height velocity SDS below -1 suggests subnormal growth, below -2 indicates significantly reduced growth velocity. This is one of the most sensitive clinical indicators of GHD in children, though it must be interpreted alongside bone age and pubertal status.

Body Mass Index and Its Impact on GH Testing

Obesity and elevated BMI significantly affect GH secretion and stimulation test results. Elevated free fatty acid levels in individuals with obesity cause a reversible suppression of GH secretion, leading to lower peak GH values on stimulation testing. This effect can produce false-positive diagnoses of GHD in obese individuals. For this reason, BMI-adjusted cutoff values are used for certain tests, particularly the GHRH-arginine test and the glucagon stimulation test.

With the glucagon stimulation test, the recommended cutoffs are peak GH below 3 ng/mL for patients with BMI below 25 or BMI 25 to 30 with high pretest probability, and peak GH below 1 ng/mL for patients with BMI of 30 or greater or BMI 25 to 30 with low pretest probability. Similarly, the GHRH-arginine test uses cutoffs of 11 ng/mL for BMI below 25, 8 ng/mL for BMI 25 to 30, and 4.2 ng/mL for BMI above 30. BMI-adjusted reference intervals have not been established for pediatric patients.

Imaging in GHD Assessment

Magnetic resonance imaging (MRI) of the hypothalamic-pituitary region plays an important role in the diagnostic evaluation of GHD. In children, MRI may reveal congenital abnormalities such as anterior pituitary hypoplasia, ectopic posterior pituitary bright spot, pituitary stalk interruption syndrome, or developmental cysts. It may also identify acquired lesions such as tumors, particularly craniopharyngiomas. The presence of structural pituitary abnormalities suggests a higher likelihood of persistent GHD requiring ongoing treatment.

In adults, MRI is essential to identify the underlying etiology, such as pituitary adenomas, craniopharyngiomas, or evidence of prior surgery or radiation. The imaging findings help guide decisions about the need for stimulation testing, the type of test to use, and the expected likelihood of GHD. Patients with normal pituitary MRI and idiopathic GHD require more stringent diagnostic criteria than those with obvious structural abnormalities.

GH Replacement Therapy Considerations

Once GHD is confirmed, recombinant human GH (rhGH) therapy is the standard treatment for both children and adults. In children, the primary goal is to promote linear growth and achieve a normal adult height. Dosing is typically weight-based, starting at 0.16 to 0.24 mg/kg per week divided into daily subcutaneous injections. The dose is adjusted based on growth response, IGF-1 levels, and side effects.

In adults, GH replacement addresses the metabolic and quality-of-life consequences of GHD. Treatment typically begins at a low dose (0.1 to 0.2 mg daily for younger adults, 0.1 mg daily for older adults) and is titrated based on clinical response, IGF-1 levels maintained within the age-adjusted reference range, and side effects. Common adverse effects include fluid retention, arthralgia, myalgia, and paresthesias, which are usually dose-related and resolve with dose reduction. Long-acting GH preparations that allow weekly or less frequent dosing are becoming available, potentially improving adherence and convenience.

Key Point: Monitoring During GH Therapy

During the dose adjustment period, IGF-1 levels should be monitored monthly or bimonthly. The target is to maintain IGF-1 within the age-adjusted normal range, ideally in the upper half. Once a maintenance dose is established, IGF-1 should be monitored approximately twice per year along with clinical assessment for response and side effects.

Alternative and Regional Diagnostic Approaches

While this calculator follows internationally recognized diagnostic criteria, it is worth noting that some regions and institutions use alternative or supplementary assessment tools. The clonidine stimulation test is commonly used as a first-line test in many pediatric centers, though it has lower sensitivity compared with arginine or insulin-based tests. The levodopa (L-DOPA) stimulation test is another option, though it similarly has limitations in specificity.

Spontaneous nocturnal GH secretion profiling, where blood samples are collected every 20 to 30 minutes overnight, can provide complementary information to stimulation testing. Studies suggest that combining nocturnal profiling with a single stimulation test may reduce the risk of overdiagnosing GHD compared with relying on stimulation testing alone. However, this approach is labor-intensive, costly, and not widely available in routine clinical practice.

Limitations and Caveats in GH Testing

Several important factors can confound the interpretation of GH stimulation test results. Assay heterogeneity remains a significant challenge, as different immunoassays can yield substantially different GH values for the same sample due to variations in antibody specificity, calibration standards, and cross-reactivity with GH isoforms and binding proteins. This means that cutoff values established with one assay may not be directly applicable to another.

Other confounding factors include patient age (GH secretion declines with aging), sex (estrogen enhances GH secretion), pubertal status (GH secretion increases two- to three-fold during mid-puberty), nutritional status (malnutrition suppresses IGF-1 production), concurrent medications (glucocorticoids suppress GH secretion; estrogens lower IGF-1 through hepatic effects), and body composition (obesity suppresses GH responses). Additionally, patients should be adequately replaced with other deficient hormones before GH testing, as untreated hypothyroidism or cortisol deficiency can affect test results.

Global Application and Population Considerations

Growth hormone deficiency has been studied across diverse populations worldwide, and diagnostic approaches are broadly similar across international guidelines from the Endocrine Society, the American Association of Clinical Endocrinologists (AACE), the GH Research Society, and the European Society of Endocrinology. However, some studies suggest that GH stimulation test cutoffs established primarily in Western populations may not be equally applicable across all ethnic groups.

For example, some data indicate that the Framingham-derived reference ranges may not perfectly translate to East Asian or South Asian populations. Healthcare providers should be aware of population-specific considerations when interpreting test results and should use locally validated reference ranges for IGF-1 when available. The assay-specific nature of GH and IGF-1 measurements further reinforces the importance of using the same laboratory and assay method for longitudinal follow-up of individual patients.

Quality of Life Assessment in Adult GHD

The QoL-AGHDA (Quality of Life Assessment of Growth Hormone Deficiency in Adults) questionnaire is a validated tool specifically designed to assess quality of life in adults with GHD. It consists of 25 yes/no questions covering dimensions such as energy, emotional reactions, social isolation, and perceived health. Higher scores indicate worse quality of life. While not part of the biochemical diagnostic workup, the QoL-AGHDA can help guide treatment decisions and monitor therapeutic response.

Other assessments used in clinical practice include measures of body composition (waist circumference, body fat percentage), bone mineral density (DEXA scan), lipid profiles, fasting glucose and insulin levels, and cardiovascular risk assessment. These comprehensive evaluations help establish the clinical impact of GHD and the potential benefits of replacement therapy for individual patients.

IGF-1 Standard Deviation Score (SDS) Interpretation

IGF-1 SDS below -2.0: Strongly suggestive of GHD
IGF-1 SDS -2.0 to -1.0: Possibly suggestive of GHD
IGF-1 SDS -1.0 to 0: Low-normal, consider clinical context
IGF-1 SDS above 0: GHD less likely (but not excluded)

IGF-1 SDS expresses the patient's IGF-1 level relative to the age- and sex-matched reference population. Values are assay-specific and should be calculated using the reference ranges provided by the laboratory performing the measurement. Low IGF-1 increases the pretest probability of GHD but cannot confirm or exclude the diagnosis alone.

Frequently Asked Questions

What is growth hormone deficiency?

Growth hormone deficiency (GHD) is a medical condition in which the pituitary gland does not produce sufficient growth hormone. In children, this leads to slow growth and short stature. In adults, it causes metabolic abnormalities including increased body fat, decreased muscle mass, reduced bone density, and impaired quality of life. GHD can be congenital or acquired, and may occur in isolation or alongside other pituitary hormone deficiencies.

How is growth hormone deficiency diagnosed?

Diagnosis involves a combination of clinical assessment, biochemical testing, and imaging. For children, evaluation of growth patterns, height velocity, and bone age are foundational. For both children and adults, IGF-1 measurement provides screening information, followed by GH stimulation tests to confirm the diagnosis. MRI of the hypothalamic-pituitary region helps identify structural causes. In children, two failed stimulation tests are typically required; in adults with high pretest probability, one test may suffice.

What is a GH stimulation test?

A GH stimulation test is a provocative diagnostic procedure in which a pharmacological agent is administered to stimulate the pituitary gland to release growth hormone. Blood samples are drawn at timed intervals to measure the peak GH response. Common stimulating agents include insulin (ITT), glucagon, arginine combined with GHRH, clonidine, levodopa, and macimorelin. Each test has specific protocols, advantages, limitations, and diagnostic cutoff values.

What peak GH level indicates deficiency in children?

The currently agreed-upon peak GH cutoff for diagnosing GHD in children is 10 ng/mL (micrograms per liter). A peak GH response below this threshold on two separate stimulation tests is considered diagnostic. Some experts consider values between 5 and 8 ng/mL equivocal, and only values above 8 or 10 ng/mL as truly normal. The choice of cutoff remains somewhat controversial, and results should be interpreted alongside clinical findings and other investigations.

What peak GH level indicates deficiency in adults?

For adults, the diagnostic cutoffs are lower and vary by test type. With the insulin tolerance test, a peak GH below 3 to 5 ng/mL confirms severe GHD. The glucagon stimulation test uses BMI-adjusted cutoffs of 3 ng/mL (BMI below 30) or 1 ng/mL (BMI 30 or above). The GHRH-arginine test uses cutoffs of 11, 8, or 4.2 ng/mL depending on BMI category. The macimorelin test uses a cutoff of 2.8 ng/mL regardless of BMI.

What is IGF-1 and why is it measured?

Insulin-like growth factor 1 (IGF-1) is a hormone primarily produced by the liver in response to GH stimulation. It mediates many of the growth-promoting effects of GH and remains relatively stable throughout the day, unlike pulsatile GH. IGF-1 levels reflect overall GH activity and are measured as part of the initial screening for GHD. Results are expressed as standard deviation scores (SDS) relative to age- and sex-matched reference populations.

Can a normal IGF-1 level exclude growth hormone deficiency?

No, a normal IGF-1 level cannot definitively exclude GHD. There is significant overlap between IGF-1 levels in GH-deficient and GH-sufficient individuals, particularly in children with idiopathic isolated GHD. Up to 30 to 40% of children with confirmed GHD may have IGF-1 levels within the normal range. Conversely, low IGF-1 can occur in conditions other than GHD. IGF-1 should always be interpreted in conjunction with clinical and auxological data.

Why does BMI affect GH stimulation test results?

Obesity causes a reversible suppression of GH secretion through multiple mechanisms, including elevated free fatty acids, hyperinsulinemia, and altered somatostatin tone. This means that obese individuals may have falsely low peak GH responses on stimulation testing, potentially leading to overdiagnosis of GHD. To account for this, BMI-adjusted diagnostic cutoffs are used for certain tests, with lower thresholds applied to patients with higher BMI.

What is the insulin tolerance test?

The insulin tolerance test (ITT) is considered the reference standard for diagnosing GHD. It involves intravenous administration of regular insulin (0.1 U/kg) to induce hypoglycemia (blood glucose below 40 mg/dL). This hypoglycemic stress triggers a counter-regulatory response that includes GH release. Blood samples for GH are drawn at 0, 15, 30, 60, 90, and 120 minutes. The test requires close medical supervision and is contraindicated in patients with seizure disorders, cardiovascular disease, or elderly patients.

What is the glucagon stimulation test?

The glucagon stimulation test (GST) is a widely used alternative to the ITT for diagnosing GHD in adults. Intramuscular glucagon is administered at a dose of 1 mg (1.5 mg for patients over 90 kg), and blood samples for GH are collected every 30 minutes for 4 hours. GH typically peaks at 90 to 120 minutes. The GST is generally well-tolerated, with nausea being the most common side effect. It has good reproducibility and is not affected by hypothalamic causes of GHD.

What is macimorelin and how does it work?

Macimorelin is an oral ghrelin receptor agonist approved for diagnosing adult GHD. Unlike traditional stimulation tests that require injections and prolonged monitoring, macimorelin is taken by mouth after an overnight fast. It stimulates GH release through the ghrelin pathway. Blood samples are drawn at 30, 45, 60, and 90 minutes. A peak GH below 2.8 ng/mL is diagnostic of GHD. The test is well-tolerated with a favorable safety profile and shorter duration than most alternatives.

How many stimulation tests are needed for diagnosis?

In children, two separate stimulation tests with subnormal GH responses are typically required for diagnosis. In adults, one stimulation test may be sufficient if the pretest probability is high (such as patients with structural pituitary disease and other hormone deficiencies). For adults with suspected idiopathic GHD (which is very rare), two stimulation tests are recommended. Certain high-risk patients with three or more pituitary hormone deficiencies and low IGF-1 may not require stimulation testing at all.

What factors can cause false results on GH stimulation tests?

Multiple factors can affect test accuracy. False-positive results (falsely diagnosing GHD) can occur with obesity, poorly controlled hypothyroidism, untreated cortisol deficiency, use of glucocorticoids, prepubertal status without sex steroid priming, and recent spontaneous GH pulse before testing (refractory period). False-negative results (missing true GHD) can occur with the GHRH-arginine test in patients with hypothalamic-origin GHD, as GHRH can directly stimulate a functioning pituitary. Assay variability also contributes to discordant results.

What is IGFBP-3 and what role does it play in diagnosis?

Insulin-like growth factor binding protein 3 (IGFBP-3) is the major carrier protein for IGF-1 in the blood and is also GH-dependent. Measuring IGFBP-3 can supplement IGF-1 data, particularly in younger children where IGF-1 reference ranges are less well established. Like IGF-1, IGFBP-3 has limited sensitivity and specificity when used alone. It tends to have better diagnostic utility in combination with IGF-1, especially for children under 3 years of age where IGF-1 levels are physiologically very low.

What is the difference between childhood-onset and adult-onset GHD?

Childhood-onset GHD primarily presents with impaired linear growth and short stature, and is most commonly idiopathic. Adult-onset GHD is usually caused by pituitary tumors or their treatment and presents with nonspecific metabolic symptoms. Diagnostic criteria differ: children use a peak GH cutoff of 10 ng/mL, while adults use lower, test-specific cutoffs. Childhood-onset patients who received GH therapy should be retested in the transition period to determine ongoing need for adult GH replacement.

Does GH deficiency need to be retested after childhood?

Yes, patients with childhood-onset GHD should be retested after achieving adult height, unless they have proven genetic mutations, embryopathic lesions causing multiple hormone deficits, or irreversible structural damage. Testing should occur at least one month after stopping GH therapy. Many patients with idiopathic isolated GHD will have normal GH secretion when retested as adults, indicating their childhood GHD was transient, possibly related to constitutional delay.

What is the role of brain MRI in GHD assessment?

Brain MRI, specifically focused on the hypothalamic-pituitary region, is essential in the evaluation of GHD. It helps identify structural abnormalities such as pituitary hypoplasia, ectopic posterior pituitary, stalk interruption syndrome, tumors, and post-surgical changes. The presence of structural abnormalities increases the pretest probability of GHD and may affect decisions about whether stimulation testing is needed. Findings of a normal pituitary on MRI in the context of failed stimulation tests suggest idiopathic GHD.

How does growth hormone deficiency affect bone health?

GH and IGF-1 play important roles in bone metabolism and maintaining bone mineral density. Adults with untreated GHD have reduced bone mineral density and an increased risk of osteoporosis and fractures. GH replacement therapy has been shown to improve bone mineral density over long-term treatment, though the full effect may take several years to manifest. Bone density monitoring with DEXA scanning is recommended as part of comprehensive GHD management.

Can GH deficiency be temporary?

Yes, GHD can be transient in certain situations. Many children diagnosed with idiopathic isolated GHD will have normal GH secretion when retested after achieving adult height, indicating their deficiency was not permanent. Transient GHD can also occur in the context of constitutional delay of growth and puberty, where the delay in pubertal hormones affects GH secretion. However, GHD caused by structural lesions, genetic mutations, or damage from surgery or radiation is typically permanent.

What are the side effects of GH stimulation tests?

Side effects vary by test type. The ITT can cause significant hypoglycemia requiring glucose rescue, and carries risks for patients with cardiovascular or seizure disorders. The glucagon test commonly causes nausea, and less frequently vomiting or headache. The GHRH-arginine test may cause facial flushing, nausea, or taste disturbance. Clonidine can cause drowsiness and hypotension. Macimorelin is generally well-tolerated, with dysgeusia (taste disturbance) being the most common side effect. All tests should be performed under appropriate medical supervision.

What is height velocity and why is it important?

Height velocity is the rate at which a child grows, measured in centimeters per year. It is one of the most sensitive indicators of GHD in children. Normal height velocity varies by age and pubertal stage, typically ranging from 5 to 7 cm per year in prepubertal children. A height velocity below the 25th percentile for age and sex, or a decline of more than 0.5 standard deviations in height SDS over one year, warrants further evaluation. Accurate measurement requires at least 6 months between height measurements, preferably 12 months.

How does puberty affect GH testing?

Puberty significantly influences GH secretion. During mid-puberty, pulsatile GH secretion increases two- to three-fold compared with prepubertal levels. This means that prepubertal children may have lower GH responses on stimulation testing, potentially leading to false-positive GHD diagnoses. Some experts advocate sex steroid priming (administering estrogen or testosterone briefly before testing) in prepubertal children to reduce this confounding effect, though this practice is not universally standardized.

What is the prevalence of growth hormone deficiency?

The prevalence of isolated GHD in children is estimated at approximately 1 in 4,000 to 1 in 10,000. When combined with other pituitary hormone deficiencies (multiple pituitary hormone deficiency or MPHD), the overall prevalence of hypopituitarism is approximately 2 to 3 per 10,000 in the adult population. The incidence of adult-onset GHD depends on the underlying cause and is highest in patients with pituitary tumors, particularly after surgical or radiation treatment.

Can growth hormone deficiency be inherited?

Yes, GHD can have genetic causes. Mutations in the GH1 gene (encoding growth hormone), the GHRHR gene (encoding the GHRH receptor), and genes involved in pituitary development such as PROP1, PIT1, HESX1, LHX3, LHX4, and SOX3 can cause inherited forms of GHD. These genetic forms may present as isolated GHD or as part of combined pituitary hormone deficiency syndromes. Genetic testing is increasingly available but is not yet routinely performed in all clinical settings.

What is the difference between GH deficiency and GH insensitivity?

GH deficiency involves insufficient production of growth hormone by the pituitary gland, while GH insensitivity (also called Laron syndrome) involves normal or elevated GH levels but defective GH receptors or downstream signaling. In GH insensitivity, IGF-1 levels are low despite normal or high GH levels, and patients do not respond to exogenous GH therapy. These conditions are distinguished by measuring both GH and IGF-1 levels, and by assessing the response to GH stimulation and GH therapy.

How long does growth hormone treatment last?

In children with GHD, treatment typically continues until adult height is achieved, growth plates have closed, or a satisfactory growth outcome has been reached. After this, retesting determines whether treatment should continue into adulthood. For adults with confirmed persistent GHD, treatment is generally lifelong, though ongoing assessment of benefits versus risks should be performed. Treatment may be discontinued if the patient no longer wishes to continue, if side effects are intolerable, or if the diagnosis is reconsidered upon retesting.

Does this calculator replace professional medical evaluation?

No, this calculator is designed for educational and informational purposes only. Growth hormone deficiency is a complex diagnosis that requires integration of clinical assessment, auxological data, multiple biochemical tests, imaging studies, and expert clinical judgment. This tool can help users understand how different diagnostic parameters relate to GHD probability, but it cannot replace the comprehensive evaluation performed by a qualified endocrinologist or pediatric endocrinologist. Always consult a healthcare professional for medical decisions.

What units are used for measuring growth hormone levels?

Growth hormone is most commonly measured in ng/mL (nanograms per milliliter) or mcg/L (micrograms per liter), which are equivalent (1 ng/mL = 1 mcg/L). Some older literature may use mU/L (milli-international units per liter), where the conversion factor depends on the GH standard used. The international standard for GH is the WHO 98/574 recombinant 22-kDa GH preparation. Different assays may report slightly different values for the same sample, making it important to use consistent assay methods for follow-up measurements.

How accurate are GH stimulation tests?

GH stimulation tests have significant limitations in accuracy. Studies show that the ITT has sensitivity of about 96% and specificity of 92% for diagnosing severe adult GHD. However, in children, the reproducibility of stimulation tests is poor, with studies showing that up to 30 to 50% of children who fail an initial test will pass on repeat testing. This highlights the importance of using stimulation tests as one component of a comprehensive diagnostic evaluation, rather than relying on them in isolation.

What is bone age and how does it relate to GHD?

Bone age refers to the maturation of the skeletal system as assessed by an X-ray of the left hand and wrist, compared with standardized reference atlases (Greulich-Pyle or Tanner-Whitehouse methods). In children with GHD, bone age is typically delayed relative to chronological age, often by 2 or more years. Delayed bone age reflects reduced exposure to GH and sex steroids and indicates remaining growth potential. It is an important component of the diagnostic evaluation and helps distinguish GHD from other causes of short stature.

Can adults develop growth hormone deficiency?

Yes, adults can develop GHD at any age. Adult-onset GHD most commonly results from pituitary tumors (especially nonfunctioning adenomas), craniopharyngiomas, pituitary surgery, cranial irradiation, traumatic brain injury, or subarachnoid hemorrhage. It can also continue from childhood-onset GHD. The clinical presentation in adults is different from children, involving metabolic changes rather than growth impairment. An estimated 2 to 3 per 10,000 adults are affected by GHD requiring treatment.

What is the cost of GH stimulation testing?

The cost varies significantly by region, healthcare system, and test type. The ITT and glucagon tests are relatively inexpensive in terms of the stimulating agents, but require clinical supervision and multiple blood draws. The GHRH-arginine test is limited by the availability (and sometimes high cost) of GHRH. Macimorelin, while convenient, may have higher drug acquisition costs. Total costs also include laboratory fees for GH measurement at multiple time points, nursing supervision, and facility charges. Insurance coverage varies by country and healthcare system.

How does this calculator assess GHD probability?

This calculator integrates multiple clinical and biochemical parameters to provide an estimated probability of GHD. It considers patient demographics (age, sex, BMI), clinical risk factors (number of other pituitary deficiencies, history of pituitary disease or treatment), IGF-1 SDS, and stimulation test results with appropriate test-specific and BMI-adjusted cutoffs. The assessment is based on published clinical guidelines from the Endocrine Society, AACE, and GH Research Society. Results are categorized as low, moderate, or high probability to guide further clinical decision-making.

Should other hormones be checked before GH testing?

Yes, it is essential that other pituitary hormone deficiencies be adequately treated before GH testing. Untreated hypothyroidism suppresses both GH secretion and IGF-1 production, potentially leading to falsely low results. Similarly, untreated cortisol deficiency can affect GH test responses. Patients should have their thyroid function, cortisol, and other relevant hormones assessed and adequately replaced before undergoing GH stimulation tests. This ensures that any measured GH deficit reflects true GHD rather than a secondary effect of other hormonal imbalances.

What are the long-term benefits of treating GHD in adults?

Long-term GH replacement in adults with confirmed GHD has been shown to improve body composition (reducing visceral fat and increasing lean body mass), increase bone mineral density over several years, improve lipid profiles (reducing LDL cholesterol), enhance exercise capacity and muscle strength, and improve quality of life including energy levels and psychological well-being. Some studies suggest potential cardiovascular benefits, though definitive evidence for reduced cardiovascular mortality is still being evaluated. The benefits must be weighed against the costs and commitment of daily injections, though long-acting formulations are improving convenience.

Conclusion

Growth hormone deficiency assessment requires a thoughtful, systematic approach that integrates clinical history, physical examination, auxological data, biochemical testing, and imaging. No single test or measurement can confirm or exclude GHD in isolation. This calculator serves as an educational tool to help users understand the diagnostic framework and how different parameters contribute to the overall assessment of GHD probability. The appropriate interpretation of stimulation test results requires attention to the specific test used, patient BMI, age, pubertal status, and the clinical context. Healthcare professionals should use their clinical judgment in conjunction with established guidelines when making diagnostic and therapeutic decisions regarding growth hormone deficiency.