Preventive Health Checkup That Actually Predicts How You'll Age — Delhi NCR

A standard yearly checkup measures what's easy to measure. It usually misses the things that actually predict long-term risk — insulin resistance, vascular inflammation, lipoprotein subfractions, body composition, and cardiovascular fitness. We build preventive checkups around those — not the generic panel that gets printed the same way for everyone.

Metabolic Medicine • Preventive Health

hs-CRP, ApoB, fasting insulin, HOMA-IR, Lp(a) — the biomarkers that predict long-term risk years before standard panels catch anything.

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Medically reviewed by Dr. Gagandeep Singh, MBBS · Last reviewed May 16, 2026

Beyond the Annual Checkup — Biomarkers That Actually Predict How You'll Age

“Preventive health” in India usually means an annual package: a long blood panel, an ECG, an ultrasound, a stress test, a printed report with any abnormal values highlighted, and a ten-minute conversation with whichever doctor has the slot.

That model catches some things. It misses most of the things that actually predict how you’ll age.

Most chronic disease in adults — type 2 diabetes, cardiovascular disease, dementia, frailty, metabolic syndrome — doesn’t arrive overnight. It builds quietly through years of insulin resistance, visceral fat accumulation, vascular inflammation, declining muscle mass, and metabolic drift that standard checkup panels routinely don’t look for. By the time a routine test reveals the disease, the underlying biology has been maturing for a decade.

At Redial Clinic in Green Park Extension, New Delhi, our preventive health program is built around the biomarkers and measurements that actually predict long-term risk — not the ones that are cheapest to print on a checkup report.

Modern biomarker panel: Fasting insulin, HOMA-IR, hs-CRP, ApoB, Lp(a), body composition, VO2max — not just glucose and basic lipids.
Early detection window: These markers shift years before fasting glucose or HbA1c — the window where intervention is most effective.
Interpretation, not just results: A proper clinical conversation, not a highlighted printout handed over in 10 minutes.
Ongoing relationship: Same clinician tracking your trajectory over years, not rotating through a hospital department.
Action-oriented: Every assessment produces a plan you can actually act on — not a report to file in a drawer.

What a modern preventive health checkup should actually include

A truly preventive health checkup goes well beyond fasting glucose, basic lipids, and an ECG. It includes markers of insulin resistance (fasting insulin, HOMA-IR), advanced cardiovascular risk (ApoB, lipoprotein(a), hs-CRP), body composition (visceral fat, muscle mass, not just BMI), cardiovascular fitness (VO2max or equivalent), metabolic function (HbA1c, liver markers, kidney markers including urine albumin), and age-appropriate cancer screening. The purpose is to detect biology well before it becomes disease — not to confirm disease after it has already arrived.

A reasonable modern preventive panel includes:

Glycaemic: fasting glucose, HbA1c, fasting insulin, HOMA-IR
Lipids (advanced): full lipid profile, plus ApoB (single best lipid marker for cardiovascular risk), plus lipoprotein(a) at least once in a lifetime
Inflammation: high-sensitivity C-reactive protein (hs-CRP)
Liver: ALT, AST, GGT, with attention to markers suggesting fatty liver
Kidney: serum creatinine, eGFR, urine albumin-to-creatinine ratio
Thyroid: TSH, with reflex T3/T4 where indicated
Nutritional status: vitamin D, vitamin B12 (particularly in vegetarians and long-term metformin users), iron studies where indicated
Body composition: waist circumference, BMI (interpreted with ICMR thresholds), muscle mass and visceral fat where measurement is available
Cardiovascular fitness: VO2max, resting heart rate, heart rate recovery — where feasible
Cancer screening: age- and risk-appropriate, discussed and arranged based on personal and family history

What is hs-CRP and why should it be in every preventive panel?

High-sensitivity C-reactive protein (hs-CRP) is a blood marker of low-grade systemic inflammation. Elevated hs-CRP is independently associated with increased risk of cardiovascular events, diabetes, and overall mortality — even in people whose cholesterol and glucose look fine. It is inexpensive, widely available, and profoundly underused in Indian preventive checkups. An hs-CRP below 1.0 mg/L suggests low cardiovascular risk; 1.0–3.0 mg/L is intermediate; above 3.0 mg/L is elevated and warrants clinical attention.

Why it matters:

Chronic low-grade inflammation is a quiet driver of atherosclerosis, diabetes progression, and long-term metabolic disease — often present long before conventional markers change
Elevated hs-CRP in an otherwise ‘normal’ panel identifies risk that LDL cholesterol and fasting glucose miss
hs-CRP is modifiable — body composition improvement, metabolic health, sleep, and specific anti-inflammatory interventions move the number in the right direction
A single elevated hs-CRP should be repeated before drawing conclusions — acute illness and recent infection transiently raise it. The pattern matters more than one reading.

Fasting insulin and HOMA-IR — the tests most checkups skip

Fasting insulin measures the level of circulating insulin after an overnight fast; HOMA-IR is a calculated index combining fasting insulin and fasting glucose to estimate insulin resistance. Together, they detect insulin resistance years before fasting glucose or HbA1c rise into diabetic ranges — the window where intervention is most effective. These tests are inexpensive, widely available, and genuinely underused in Indian preventive checkups that focus on glucose alone.

The clinical picture that emerges from running fasting insulin in a preventive panel:

Normal fasting insulin is typically <10 µU/mL; ideally 2–6 µU/mL in metabolically healthy adults. Many Indian patients with ‘normal’ glucose have fasting insulin 2–3 times this upper limit — significant insulin resistance that standard screening misses entirely.
HOMA-IR below 1.0 suggests good insulin sensitivity; 1.0–2.0 is reasonable; above 2.5 suggests meaningful insulin resistance warranting intervention.
Rising fasting insulin precedes rising HbA1c by years — sometimes a decade. Early detection reshapes the preventive trajectory.
Insulin resistance reversibility is best in the pre-diabetic window — which is precisely the window these tests identify.

ApoB — the single best lipid marker for cardiovascular risk

Apolipoprotein B (ApoB) measures the total number of atherogenic particles in the blood — LDL, VLDL, IDL, and lipoprotein(a) combined. Modern cardiovascular risk assessment increasingly recognises ApoB as a more accurate predictor of atherosclerotic disease than LDL cholesterol alone, particularly in patients with metabolic syndrome, diabetes, or mixed dyslipidaemia. It captures risk that LDL-C can miss.

Why ApoB deserves to be in modern preventive panels:

LDL cholesterol measures the mass of cholesterol inside LDL particles; ApoB counts the particles themselves. When particle number and cholesterol content don’t match (common in insulin resistance, diabetes, metabolic syndrome), LDL-C understates risk.
Treatment decisions increasingly use ApoB as a target — many guidelines now recommend ApoB goals for higher-risk patients
ApoB is not routinely run in standard Indian checkups despite being inexpensive and widely available
Lipoprotein(a) — genetically determined, unmodifiable through lifestyle — should also be measured at least once in a lifetime; combined with ApoB, it gives a comprehensive lipid risk picture

Body composition and fitness — the measurements that outperform BMI

BMI is a crude population-level metric that routinely misclassifies individual risk — particularly in South Asian patients whose visceral fat concentration at lower BMIs produces early metabolic disease. Body composition (muscle mass, visceral fat, waist circumference) and cardiovascular fitness (VO2max or equivalent) predict long-term health outcomes substantially better than BMI alone. A preventive assessment that ignores body composition and fitness is missing some of the most important signals available.

What body composition reveals

Two adults at the same weight can have very different metabolic pictures. Waist circumference (≥90 cm for Indian men, ≥80 cm for Indian women indicates elevated risk), visceral fat percentage, and muscle mass relative to fat mass all contribute to long-term risk in ways that BMI alone does not capture. Low muscle mass — particularly in adults over 50 — is an underappreciated risk factor for frailty, insulin resistance, and reduced lifespan.

What cardiovascular fitness reveals

VO2max — maximum oxygen uptake capacity — is one of the strongest predictors of all-cause mortality available in clinical medicine. A person with low VO2max has substantially higher long-term risk than a person with high VO2max, independent of weight, smoking, or traditional risk factors. Improving fitness is one of the highest-leverage modifications available. Even rough fitness assessment (heart rate recovery, functional capacity testing) tells you something the standard checkup ignores entirely.

Biological age — useful concept, overhyped marketing

Biological age refers to an estimate of how old your body is physiologically, based on biomarkers, rather than how old the calendar says you are. Several biological age calculators and DNA methylation tests exist, with varying levels of scientific validation. The concept is useful as a framing for preventive care; the specific commercial ‘biological age’ tests vary widely in quality and clinical utility. We take the concept seriously without over-paying for fashionable tests that don’t change management decisions.

Our honest position:

The idea that biomarkers can estimate physiological age is valid and increasingly supported by research
Practical biological age — insulin sensitivity, body composition, cardiovascular fitness, inflammation, metabolic health — is strongly predicted by a careful preventive panel, whether or not a commercial ‘biological age’ calculator is involved
Some commercial biological-age tests (epigenetic clocks, telomere length assays) are interesting but expensive, and many don’t change management decisions in ways that justify the cost
We discuss biological age testing honestly with interested patients — what’s useful, what’s hype — and include it where it adds real value, not because it’s trending

The nutrition gap most Indian adults don't know they have

The biggest nutritional threat to healthy aging in India is not overeating — it is protein undernutrition. Most Indian adults over 45 eat a diet adequate in calories but severely inadequate in protein. A standard dal-roti lunch gives 12–15 grams of protein. The same meal needs 25–30 grams to preserve muscle and satisfy hunger properly. This gap, repeated across three meals every day for decades, is a primary driver of sarcopenia — the gradual loss of muscle mass and strength — and the metabolic fragility that follows.

Sarcopenia is not inevitable, but it is normal when protein is consistently insufficient. Its consequences extend well beyond feeling physically weaker: muscle tissue is metabolically active, and losing it accelerates insulin resistance, cognitive slowing, and bone density loss. After the age of 50, the body becomes progressively less efficient at using dietary protein for muscle synthesis — which means protein needs actually increase with age, not decrease. A 60-year-old needs more protein per kilogram of body weight than a 30-year-old to achieve the same muscle-building response.

The practical translation: dal is a side dish. Eggs, paneer, curd, fish, and chicken are the proteins that fill the gap — all familiar, all affordable, all available in a Delhi kitchen. We plan for a real protein source at every meal, specifically, rather than assuming the background diet covers it.

Anti-inflammatory eating is the second lever for healthy aging. Chronic low-grade inflammation — measured by markers like hs-CRP — accelerates nearly every age-related disease process. The anti-inflammatory kitchen is not complicated: ghee rather than refined seed oils, turmeric generously in daily cooking, fatty fish regularly, abundant vegetables especially the green leafy ones, and minimising ultra-processed food and packaged snacks.

Gut health matters increasingly as we age. Stomach acid reduces, gut motility slows, and the microbiome changes in ways that affect digestion, immunity, and even mood. Curd daily, fermented foods where they suit the patient, and adequate fibre from dal and vegetables are the practical tools. The Indian kitchen already has these. The question is whether they are being used consistently.

Vitamin D is near-universally deficient in Delhi patients, regardless of how much time they spend outdoors — melanin, indoor lifestyle, and air pollution together make sun-based vitamin D synthesis unreliable in this population. Testing and correcting this is one of the first things we do. Low vitamin D worsens insulin resistance, muscle strength, bone density, and immune function — it is not a minor nutritional detail.

Who this program is for — and who it is not for

This program is designed for

Adults 30+ who want a proper, structured picture of their long-term health risk — and a real plan to act on it
People with strong family history of diabetes, cardiovascular disease, or metabolic conditions
People who have been doing 'yearly checkups' for years and want something genuinely more useful
People currently healthy on standard tests but intuitively aware that something may be brewing — weight creep, declining fitness, family-history worry
People who want specific modern biomarkers (hs-CRP, ApoB, fasting insulin, HOMA-IR, Lp(a)) in their assessment — and a clinician who knows what to do with the results
Adults serious about staying metabolically and cardiovascularly healthy into later life, not just 'catching things early'

This program is not designed for

One-off checkup packages where the patient wants a printed report and no ongoing conversation
People seeking advanced genetic testing, epigenetic clocks, or expensive fashionable biomarkers that don't change management
People looking for supplement recommendations as their primary health strategy
People with acute medical problems — those belong in specialist or emergency care first

How the program works

The program runs in three phases. First, a comprehensive baseline assessment that includes the full modern preventive panel, body composition, fitness evaluation, and detailed history-taking. Second, an individualised plan addressing whatever the assessment reveals — emerging insulin resistance, early inflammation, body composition, fitness gaps, nutrition, sleep, stress. Third, structured follow-up — typically 6–12 month review cycles with retests of relevant markers and plan adjustments.

Phase 1: Comprehensive baseline

Full modern preventive panel (glycaemic, lipid including ApoB and Lp(a), inflammation including hs-CRP, liver, kidney, thyroid, nutritional), body composition, waist circumference, fitness assessment where feasible, and a detailed conversation about personal and family history, lifestyle, sleep, stress, diet, and current medications or supplements.

Phase 2: Individualised plan

Based on your biomarker results, we identify the specific levers most worth pulling for your biology: protein adequacy at every meal to prevent muscle loss, cooking fat and inflammation corrections, movement priorities, sleep and stress interventions, targeted supplements where evidence supports them, and specialist referrals where warranted. Calibrated to your actual life, not a generic template.

Phase 3: Structured follow-up

Preventive health is not a one-off service. Typical follow-up runs at 6 or 12 month intervals depending on what the baseline showed, with retests of the markers most relevant to your picture and plan adjustments based on what changed. Major life transitions — job change, pregnancy, new medication, significant weight change — often warrant earlier review.

Why this differs from standard hospital checkup packages

Hospital checkup packages are optimised for volume, consistency, and throughput — the same panel is run for most patients, with results reviewed in a short standardised consultation. Our preventive program is built for depth, interpretation, and individualisation — a longer assessment, modern biomarkers most packages skip, and a working relationship with a clinician who will be looking at the data with you over time. Both have a role. The differences matter more than marketing language implies.

Scope: we run the markers that actually predict risk (hs-CRP, ApoB, fasting insulin, HOMA-IR, Lp(a), body composition) — standard packages usually don’t
Interpretation: results are reviewed in a proper clinical conversation, not handed over with highlighted abnormalities
Continuity: the same clinician follows your trajectory over years, not rotating through a hospital department
Action orientation: the assessment produces a plan you can actually act on, not a report to file in a drawer
Honest scope: we are not a substitute for cardiology, oncology, or specialist care where indicated — we coordinate referrals where they are needed

If your annual checkup has been giving you a highlighted report and no plan, and you suspect the markers that actually matter aren’t being looked at — you’re probably right.

A checkup designed around what predicts risk will give you genuinely actionable information about how you’re going to age. Book a preventive health assessment with Dr. Gagandeep Singh at Redial Clinic, Green Park Extension, New Delhi.

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Frequently Asked Questions

Is this an 'executive health checkup' package?

It is a preventive health assessment, not a packaged product. Hospital-chain ‘executive checkup’ packages are optimised for throughput and deliver a standardised panel in a few hours. Our preventive program runs deeper — different (and more) biomarkers, longer clinical conversation, and ongoing follow-up. Both models are legitimate for different needs. If you want a quick annual snapshot, a hospital package may suit you. If you want a serious picture of your long-term trajectory with an ongoing clinician relationship, this is designed for that.

What is hs-CRP and why should I know mine?

hs-CRP (high-sensitivity C-reactive protein) is a blood marker of low-grade inflammation in your body. Elevated hs-CRP independently predicts higher risk of cardiovascular events, type 2 diabetes, and overall mortality — often identifying risk that cholesterol and glucose alone miss. It is inexpensive and widely available. A single value should be interpreted in context (recent infections or illness raise it temporarily); the pattern over repeat tests matters more than one reading.

What is HOMA-IR and why run fasting insulin?

Fasting insulin measures the insulin level in your blood after an overnight fast; HOMA-IR is a calculated index combining fasting insulin and fasting glucose to estimate insulin resistance. These tests detect insulin resistance — the underlying driver of type 2 diabetes — years before it shows up on fasting glucose or HbA1c. They are among the highest-value preventive tests available and are routinely skipped by standard checkup panels. Normal fasting insulin is under 10 µU/mL; ideally 2–6 in metabolically healthy adults.

What is ApoB and how does it differ from LDL cholesterol?

LDL cholesterol measures the mass of cholesterol inside LDL particles. ApoB (apolipoprotein B) counts the total number of atherogenic particles in the blood — LDL plus VLDL, IDL, and lipoprotein(a). When particle number and cholesterol content don’t match — common in insulin resistance, diabetes, and metabolic syndrome — LDL-C understates the real risk. Modern cardiovascular medicine increasingly uses ApoB as a more accurate marker.

How often should I do a preventive health checkup?

For most adults 30+, a comprehensive baseline followed by annual or biannual follow-up is reasonable, adjusted based on what the baseline reveals. If initial results show emerging insulin resistance, elevated hs-CRP, or significant risk factors, shorter intervals (every 6 months) may make sense during the active intervention phase. Once markers are stable and in a healthy range, 12–24 month intervals often suffice.

I'm only 30 — do I really need this?

Probably yes, particularly if you have any family history of diabetes, cardiovascular disease, or metabolic conditions. The specific biomarkers we focus on (insulin resistance, inflammation, advanced lipids) begin shifting in your 20s and 30s for many people — especially in South Asian populations. Early identification means that small, sustainable corrections now can substantially alter your 40s, 50s, and 60s. Waiting until something is ‘wrong’ means waiting until much of the upstream biology has already matured.

What if my results are all normal?

That’s genuinely good news, and the useful thing about the modern panel is that it tells you normal in a more complete sense than standard checkups do. You still get the benefit of baseline data for future comparison, and a detailed conversation about what to maintain — rather than just ‘all clear, see you next year.’ Many patients with normal results value the plan for staying that way more than they value any finding.

Is this program covered by insurance?

Preventive health programs in India are generally not bundled for insurance reimbursement, though specific diagnostic tests may be reimbursable depending on your policy. We provide itemised invoicing to support any claims you may file. Costs are discussed transparently at initial assessment; the biomarker panel is reasonable relative to hospital executive packages, and the clinician time is the meaningful value.

References

Ridker PM et al., "Rosuvastatin to Prevent Vascular Events in Men and Women with Elevated C-Reactive Protein" (JUPITER trial), New England Journal of Medicine, 2008. https://doi.org/10.1056/NEJMoa0807646
Sniderman AD et al., "Apolipoprotein B Particles and Cardiovascular Disease: A Narrative Review," JAMA Cardiology, 2019. https://doi.org/10.1001/jamacardio.2019.3780
Mach F et al., "2019 ESC/EAS Guidelines for the management of dyslipidaemias," European Heart Journal, 2020. https://doi.org/10.1093/eurheartj/ehz455
Anjana RM et al., "Metabolic non-communicable disease health report of India: the ICMR-INDIAB national cross-sectional study (ICMR-INDIAB-17)," Lancet Diabetes & Endocrinology, 2023. https://doi.org/10.1016/S2213-8587(23)00119-5
Ross R et al., "Importance of Assessing Cardiorespiratory Fitness in Clinical Practice: A Case for Fitness as a Clinical Vital Sign," Circulation, 2016. https://doi.org/10.1161/CIR.0000000000000461

Written by: Dr. Gagandeep Singh, MBBS

Medically reviewed by: Dr. Gagandeep Singh, MBBS

Last updated: May 16, 2026

This page is for informational purposes only and does not constitute medical advice. Outcomes vary depending on diagnosis, baseline severity, adherence, and overall medical context. Medication changes, if any, are made only under medical supervision. Always consult a qualified healthcare professional before changing your treatment plan.

Redial Clinic, Green Park Extension, New Delhi