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Six-marker metabolic and adrenal panel to identify hormonal drivers of insulin resistance, weight dysfunction, and metabolic syndrome.
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A six-marker metabolic and hormone panel assessing fasting insulin, HbA1c, glucose, cortisol, DHEAS, and adiponectin.
Insulin resistance is not just a blood sugar problem — it is a hormonal condition with roots in adrenal function, sex hormone balance, and inflammatory signalling. The Insulin Resistance and Metabolic Hormone Panel maps these interconnections through six targeted markers.
Fasting insulin and HbA1c reveal the glycaemic burden and insulin secretory demand. Fasting glucose provides the acute reading that contextualises insulin sensitivity. Cortisol and dehydroepiandrosterone sulphate (DHEA-S) reflect the adrenal contribution to insulin resistance — elevated cortisol directly promotes gluconeogenesis and adipose accumulation, while the cortisol-to-dehydroepiandrosterone sulphate (DHEA-S) ratio is a sensitive indicator of chronic HPA axis stress. Adiponectin — a fat-cell hormone that is paradoxically low in obesity — is a powerful anti-inflammatory, insulin-sensitising marker whose decline predicts metabolic disease risk years before clinical diabetes appears.
This panel is relevant for people with weight gain they cannot explain through diet and lifestyle alone, those at elevated risk of type 2 diabetes, and anyone managing PCOS, fatigue, or adrenal dysfunction with a metabolic component. Venous draw required, fasted. GMC-physician reviewed results within 3 to 5 working days.
Understand what each marker measures, why it matters, and what the science says — not just a list of numbers.
Pancreatic hormone measured in the fasted state; elevated fasting insulin is the earliest biochemical indicator of insulin resistance.
Three-month average blood glucose; reflects chronic glycaemic load and risk of type 2 diabetes progression.
Immediate blood glucose in the fasted state; contextualises insulin level to calculate insulin sensitivity.
Primary stress hormone that promotes gluconeogenesis, fat storage, and insulin resistance when chronically elevated.
Adrenal androgen that counterbalances cortisol; the cortisol-to-dehydroepiandrosterone sulphate (DHEA-S) ratio reflects chronic adrenal stress burden.
Anti-inflammatory, insulin-sensitising hormone produced by fat cells; paradoxically low in obesity and a strong predictor of metabolic disease risk.
This panel is designed for adults who want a comprehensive, evidence-based picture of their metabolic health — not a GP referral panel.
People with unexplained weight gain, particularly around the abdomen
Those with a family history of type 2 diabetes or metabolic syndrome
Women with PCOS wanting to understand the metabolic dimension of their condition
Individuals experiencing chronic fatigue and stress with associated weight changes
Fasting insulin is not a standardised diagnostic test for insulin resistance and no universally agreed reference ranges exist; values must be interpreted alongside clinical features and fasting glucose. This panel does not include a glucose tolerance test (OGTT), which is the gold standard for diagnosing impaired glucose tolerance and type 2 diabetes. Adiponectin testing is not widely used in NHS routine practice and is an emerging biomarker; reference ranges should be interpreted in the context of the clinical picture. Cortisol in this panel is a single morning value and cannot replace dynamic adrenal testing for diagnosing adrenal insufficiency. Please discuss significantly abnormal results with your GP promptly.
From order to physician-reviewed report in as little as three working days.
Three options designed to fit your schedule, location, and preference — all producing a laboratory-standard sample.
Adults 18+ in mainland UK. Not suitable if you have had a transfusion in the last 3 months.
Order anytime; kit dispatched within 24 hours Mon–Fri.
Allow 24–48 hours for sample transit on top of lab processing time.
Adults 18+ within 20 miles of a serviced city centre.
Mon–Sun, 06:00–20:00. Next-day booking typical.
Sample reaches the lab within 24 hours of collection.
Adults 16+ with photo ID. Paediatric draws by appointment at selected sites.
Mon–Fri, with Saturday hours at most metropolitan locations.
Samples processed same-day at the receiving clinic.
Every test is processed in a UKAS ISO 15189-accredited laboratory, overseen by GMC-registered physicians, and governed by UK GDPR. No overseas processing, no offshore data.
Follow these guidelines to ensure accurate, reproducible results. Most markers are sensitive to recent food, exercise, and sleep.
Can't find your answer? Our clinical support team is available Monday to Friday, 9am–5pm.
Contact supportInsulin resistance occurs when cells in the muscles, liver, and fat tissue become less responsive to the insulin signal. The pancreas compensates by producing more insulin to maintain blood glucose control — a state of hyperinsulinaemia. Over time, this leads to progressively higher fasting insulin levels, rising blood glucose, increased fat storage (particularly visceral), systemic inflammation, and eventually impaired glucose tolerance or type 2 diabetes. Elevated fasting insulin is one of the earliest detectable markers — often appearing years before HbA1c becomes abnormal.
HOMA-IR (Homeostatic Model Assessment of Insulin Resistance) is a formula-based index calculated from fasting insulin and fasting glucose. It is widely used in research and increasingly in clinical practice as a practical measure of insulin resistance. Your Trupoint Health physician report will calculate and report your HOMA-IR score alongside an interpretation of what it means in your context. A score below 1.0 generally indicates good insulin sensitivity; above 2.0 suggests developing insulin resistance; above 2.9 is consistent with significant insulin resistance in most adult populations.
Adiponectin is produced by fat cells (adipocytes) and has powerful insulin-sensitising and anti-inflammatory effects. Paradoxically, people with more body fat (particularly visceral fat) have lower adiponectin levels — a finding that helps explain why visceral obesity drives metabolic disease even in people who appear otherwise healthy. Low adiponectin is an independent predictor of insulin resistance, type 2 diabetes, and cardiovascular disease — sometimes identifying risk years before standard markers become abnormal. Including adiponectin gives a forward-looking view of metabolic trajectory that fasting glucose and HbA1c alone do not provide.
Cortisol, the primary stress hormone, directly promotes gluconeogenesis (glucose production by the liver) and stimulates fat storage in the abdominal region. Chronically elevated cortisol drives up blood glucose and insulin demand, and reduces the sensitivity of cells to insulin over time. The cortisol-to-dehydroepiandrosterone sulphate (DHEA-S) ratio in this panel reflects this dynamic: a high cortisol with low dehydroepiandrosterone sulphate (DHEA-S) suggests chronic adrenal stress burden that may be contributing to the metabolic picture. Addressing cortisol excess through sleep, stress management, and appropriate support can be an important adjunct to standard metabolic interventions.
The most evidence-based interventions for improving insulin sensitivity include: resistance training (which increases muscle glucose uptake and GLUT4 expression); reducing refined carbohydrate and added sugar intake; increasing dietary fibre; improving sleep quality and duration (poor sleep acutely increases insulin resistance); losing even 5 to 10% of body weight if overweight; and intermittent fasting or time-restricted eating in appropriate individuals. Regular walking after meals has also been shown to substantially reduce postprandial glucose and insulin spikes. Monitoring your fasting insulin and HOMA-IR every 3 to 6 months is a useful way to track the metabolic impact of these changes.
Yes, particularly if fasting insulin, glucose, or HbA1c are outside the reference range. While this panel is a screening and monitoring tool rather than a diagnostic test, significantly elevated fasting insulin, impaired fasting glucose (6.1 to 6.9 mmol/L), or HbA1c in the pre-diabetic range (42 to 47 mmol/mol) are all findings that warrant a conversation with your GP. Your Trupoint Health physician report will provide clear guidance on whether and how urgently a GP consultation is recommended. Early identification and intervention at the pre-diabetes stage can prevent or delay progression to type 2 diabetes in the majority of cases.
