- 1. Why Testosterone Matters: Beyond Muscle
- 2. The Modern Decline: A Population-Level Crisis
- 3. Testing: What to Measure and How to Interpret
- 4. Natural Optimization: The Foundation
- 5. Nutrition Factors: Building Blocks and Disruptors
- 6. Testosterone Replacement Therapy: When and How
- 7. The Controversy: Risks, Benefits, and Fertility
- 8. Other Androgens and SARMs: What Research Shows
- 9. Practical Framework for Evaluation and Action
This guide is for educational purposes. Testosterone is a controlled substance in most countries and requires medical supervision for therapeutic use. We do not provide dosing recommendations— that is the domain of qualified physicians. Our goal is to help you understand your hormonal health so you can have informed conversations with healthcare providers and make intelligent decisions about optimization.
1. Why Testosterone Matters: Beyond Muscle
When most people think of testosterone, they think of muscles and aggression. The reality is far more interesting. Testosterone is a master regulatory hormone that influences virtually every system in the male body—from your brain chemistry to your bone density, from your cardiovascular health to your capacity for creative thinking.
Understanding what testosterone actually does reveals why its optimization matters so much for men navigating the second half of life.
Cognitive Function
Testosterone directly affects brain function through androgen receptors distributed throughout the cerebral cortex, hippocampus, and amygdala.[1] The cognitive effects are substantial:
- Spatial reasoning — Men with higher testosterone consistently outperform on spatial tasks; low T is associated with spatial cognitive decline[2]
- Verbal memory — The relationship is U-shaped; both very low and supraphysiological levels impair verbal memory, with optimal function in the mid-normal range[3]
- Processing speed — Higher testosterone is associated with faster cognitive processing in aging men[4]
- Executive function — Planning, working memory, and cognitive flexibility all correlate with testosterone levels[5]
The Testosterone Trials, one of the largest studies on testosterone therapy in older men, found that treatment improved spatial memory and self-reported cognitive function, though effects on other domains were mixed.[6]
Mood and Psychological Well-being
The relationship between testosterone and mood is profound. Low testosterone is strongly associated with:
- Depression — Men with low T are 4× more likely to be diagnosed with clinical depression; testosterone replacement significantly improves depressive symptoms in hypogonadal men[7]
- Anxiety — Low testosterone increases anxiety sensitivity and reduces stress resilience[8]
- Irritability and mood swings — Often a symptom of declining T, frequently misattributed to "just getting older"
- Diminished sense of well-being — The subjective feeling of vitality and engagement with life
One of the most underrecognized symptoms of low testosterone is anhedonia—the diminished capacity to experience pleasure. Men describe losing interest in hobbies, feeling like "life has lost its color," or no longer being moved by things that once excited them. This is often dismissed as burnout or normal aging but can be a direct consequence of hormonal decline.
Motivation and Drive
Testosterone modulates the dopaminergic system, directly influencing motivation, reward sensitivity, and goal-directed behavior.[9] This manifests as:
- Ambition and competitive drive — Testosterone primes risk-taking and status-seeking behavior
- Initiative and energy — The willingness to start things and see them through
- Libido — Sexual desire is testosterone-dependent and often the first thing men notice declining
- General vitality — The subjective sense of energy and capability
Metabolic Health
Testosterone plays a central role in metabolic function:
- Body composition — T promotes muscle protein synthesis and inhibits fat storage; low T leads to increased visceral adiposity[10]
- Insulin sensitivity — Higher testosterone improves glucose metabolism; low T is associated with insulin resistance and type 2 diabetes risk[11]
- Lipid profiles — Complex relationship; generally, optimal T levels support healthy HDL and reduce harmful lipoproteins
- Bone density — Testosterone (and its conversion to estradiol) is critical for maintaining bone mineral density in men[12]
The relationship between testosterone and metabolic health is bidirectional: low testosterone promotes obesity and metabolic dysfunction, while obesity and metabolic dysfunction suppress testosterone production. This creates a vicious cycle that becomes increasingly difficult to break as it progresses.
Cardiovascular Health
The relationship between testosterone and cardiovascular health has been controversial, but recent large-scale evidence is clarifying the picture:
- Low testosterone is associated with increased cardiovascular mortality[13]
- The TRAVERSE trial (2023), the largest randomized trial of testosterone therapy to date, found no increased cardiovascular risk with treatment in men at elevated cardiac risk[14]
- Testosterone influences erythropoiesis (red blood cell production), vascular tone, and cardiac muscle function
2. The Modern Decline: A Population-Level Crisis
Something troubling is happening to male testosterone levels across the developed world. This isn't speculation—it's documented in multiple large-scale epidemiological studies spanning decades.
The Evidence
The Massachusetts Male Aging Study (MMAS), one of the most comprehensive longitudinal studies of male hormones, revealed a startling finding: testosterone levels declined by approximately 1.2% per year from 1987 to 2004, independent of age.[15] This means a 65-year-old man in 2004 had significantly lower testosterone than a 65-year-old man in 1987.
These findings have been replicated internationally:
- Danish study (2007) — Found similar generational declines in Danish men[16]
- Finnish study (2013) — Documented declining T levels across Finnish birth cohorts[17]
- Israeli study (2020) — Reported substantial decline in testosterone among Israeli men
- U.S. NHANES data — Confirmed population-level decline in American men
The scope of decline is substantial. Comparing same-age men across generations:
| Birth Year | Average T at Age 50 | % Decline vs 1940s |
|---|---|---|
| 1940s cohort | ~600 ng/dL | — |
| 1960s cohort | ~520 ng/dL | -13% |
| 1980s cohort | ~450 ng/dL | -25% |
| 2000s cohort | ~400 ng/dL (projected) | -33% |
Note: These are approximations based on multiple studies. Individual variation is substantial.
Potential Causes
The causes of this generational decline are likely multifactorial:
Obesity Epidemic
Obesity rates have skyrocketed over the same period. Adipose tissue contains aromatase, which converts testosterone to estradiol. More body fat = more aromatization = lower testosterone. Obesity alone, however, doesn't fully explain the decline—the trend persists even when controlling for BMI.[15]
Endocrine Disruptors
Our environment is saturated with chemicals that interfere with hormonal signaling:
- Phthalates — Found in plastics, personal care products; associated with lower testosterone and impaired testicular function[18]
- BPA and analogues — Plasticizers with estrogenic activity
- Pesticides — Many have anti-androgenic or estrogenic properties
- PFAS ("forever chemicals") — Persistent compounds linked to hormonal disruption
Lifestyle Factors
- Sleep deprivation — Modern sleep duration has declined; sleep restriction acutely lowers testosterone[19]
- Physical inactivity — Sedentary behavior suppresses T production
- Chronic stress — Sustained cortisol elevation inhibits the HPG axis
- Dietary changes — Increased processed food consumption, altered fat intake
Other Factors
- Increased rates of metabolic syndrome
- Medication use — Opioids, statins, and other common medications can suppress T
- Reduced smoking — Surprisingly, smoking increases testosterone (though the overall health tradeoff is obviously negative)
As population testosterone levels decline, so do laboratory "reference ranges." Many labs now consider 250-300 ng/dL the lower limit of "normal" because it reflects the statistical bottom of current populations. But a level that's statistically common in sick populations is not the same as biologically optimal. A man with 300 ng/dL may be told his testosterone is "normal" while experiencing all the symptoms of deficiency.
3. Testing: What to Measure and How to Interpret
Accurate assessment of testosterone status requires more than a single blood test. The endocrine system is complex, and understanding where a problem originates—if there is one—requires a comprehensive panel.
The Essential Panel
The total amount of testosterone in your blood, including both bound and unbound fractions. This is the starting point for any assessment.
Important Caveats
- Testosterone has diurnal variation—levels peak in early morning and can be 25-30% lower by afternoon
- Always test fasting in the morning for consistent, comparable results
- A single low reading should be confirmed with a repeat test
- Acute illness, poor sleep, and recent intense exercise can transiently lower T
Only 2-3% of total testosterone circulates unbound ("free")—this is the fraction that can directly enter cells and exert biological effects. The rest is bound to SHBG (~40-60%) or albumin (~40%).
Why It Matters
You can have "normal" total testosterone but low free testosterone if SHBG is elevated. Symptoms correlate more closely with free testosterone than total in many men.
The primary binding protein for testosterone. SHBG levels significantly affect how much testosterone is biologically available.
What Affects SHBG
| Increases SHBG | Decreases SHBG |
|---|---|
| Aging | Obesity |
| Hyperthyroidism | Hypothyroidism |
| Liver disease | Insulin resistance |
| Estrogen excess | High-dose androgens |
| Low calorie intake | Certain medications |
Estradiol is essential for male health—it's not just a "female hormone." Testosterone converts to estradiol via aromatase. Both too low and too high E2 cause problems.
E2 Too Low
- Joint pain and stiffness
- Low libido (paradoxically)
- Poor bone health
- Mood disturbances
E2 Too High
- Water retention and bloating
- Gynecomastia (breast tissue development)
- Emotional lability
- Erectile dysfunction
Important: Always request the sensitive estradiol test (LC-MS/MS method), not the standard immunoassay, which is designed for female ranges and unreliable in men.
Luteinizing hormone (LH) and follicle-stimulating hormone (FSH) are pituitary hormones that regulate testicular function. They help determine whether low testosterone is a primary (testicular) or secondary (pituitary/hypothalamic) problem.
Interpretation
| Testosterone | LH | Indicates |
|---|---|---|
| Low | High | Primary hypogonadism (testicular failure) |
| Low | Low/Normal | Secondary hypogonadism (pituitary/hypothalamic issue) |
| Normal | Normal | Normal HPG axis function |
Secondary hypogonadism may warrant further investigation (pituitary imaging) and is sometimes more amenable to treatment alternatives to TRT.
Additional Useful Markers
- Prolactin — Elevated prolactin suppresses testosterone; can indicate pituitary issues
- TSH and Free T4 — Thyroid function affects SHBG and general hormonal health
- Complete Blood Count — Baseline hematocrit is important before considering TRT
- Metabolic Panel — Liver and kidney function, fasting glucose
- PSA — Prostate-specific antigen, baseline before any testosterone therapy
- DHT — Dihydrotestosterone, the most potent androgen (optional but informative)
Total Testosterone Reference
Lab "normal" starts at ~264-300, but most men feel best in the 500-800 range. Symptoms often appear below 400 ng/dL even if labs say "normal."
4. Natural Optimization: The Foundation
Before considering any medical intervention, it's essential to optimize the foundational factors that influence testosterone production. These lifestyle modifications can meaningfully increase testosterone levels—in some cases by 20-30%—and improve overall health regardless of hormonal status.
Sleep: The Master Regulator
Sleep is the single most important factor for testosterone production. The majority of daily testosterone release occurs during sleep, particularly during REM cycles.[19]
Strong Evidence
A landmark University of Chicago study found that restricting sleep to 5 hours per night for one week reduced testosterone levels by 10-15% in healthy young men—equivalent to 10-15 years of aging.[20]
Sleep Optimization Protocol
- Duration: 7-9 hours per night, consistently
- Timing: Consistent bedtime and wake time, even on weekends
- Environment: Cool (65-68°F), completely dark, quiet
- Pre-sleep: No screens 1-2 hours before bed; blue light blocks melatonin
- No alcohol: Alcohol disrupts REM sleep and lowers overnight T production
- Address sleep apnea: Untreated sleep apnea devastates testosterone levels
If you snore heavily, wake up unrested despite adequate sleep time, or have been told you stop breathing at night, get evaluated for sleep apnea. Treatment with CPAP can substantially increase testosterone in affected men. This is one of the most underdiagnosed causes of low T.
Resistance Training: The Primary Exercise Intervention
Exercise influences testosterone, but not all exercise is equal. The evidence strongly favors resistance training over aerobic exercise for testosterone optimization.
Strong Evidence
- Resistance training acutely elevates testosterone post-workout[21]
- Long-term resistance training is associated with higher baseline testosterone[22]
- Compound movements (squats, deadlifts, rows, presses) produce larger hormonal responses than isolation exercises
- Higher volume and intensity correlate with greater testosterone response
Optimal Training Parameters
| Variable | Recommendation | Rationale |
|---|---|---|
| Frequency | 3-5 days/week | Sufficient stimulus with recovery |
| Exercise Selection | Compound movements | More muscle mass recruited = greater hormonal response |
| Intensity | 70-85% 1RM | Moderate-heavy loads optimal |
| Volume | Multiple sets (3-5) | Higher volume increases response |
| Rest Periods | 60-90 seconds | Shorter rest may enhance acute T response |
Endurance Exercise: The Nuance
While some aerobic exercise supports overall health, excessive endurance training can suppress testosterone through chronic cortisol elevation and energy deficit. Marathon runners and Ironman athletes often have lower testosterone than their sedentary peers. Keep cardio moderate and prioritize resistance training.
Body Composition: Breaking the Vicious Cycle
The relationship between body fat and testosterone creates a feedback loop:
- Excess body fat (especially visceral fat) contains aromatase, which converts testosterone to estrogen
- Lower testosterone promotes fat accumulation and makes fat loss harder
- Higher estrogen from aromatization further suppresses testosterone production
Strong Evidence
Studies show that weight loss in obese men can increase testosterone by 50-100+ ng/dL— sometimes bringing men from hypogonadal to normal range without medication.[23]
Target Body Composition
- Optimal body fat: 10-20% for most men
- Getting there: Moderate caloric deficit (500 cal/day), high protein (0.7-1g/lb bodyweight), resistance training
- Avoid extreme diets: Very low calorie diets tank testosterone acutely
Stress Management: Cortisol is the Enemy
Cortisol and testosterone have an inverse relationship. Chronic stress keeps cortisol elevated, which directly suppresses the hypothalamic-pituitary-gonadal (HPG) axis and inhibits testosterone production.[24]
Moderate Evidence
Practical Interventions
- Meditation/mindfulness: Even 10-15 minutes daily reduces cortisol
- Nature exposure: Time outdoors lowers stress hormones
- Social connection: Isolation is a chronic stressor
- Identify and address stressors: Work, relationships, financial stress
- Adaptogenic herbs: Ashwagandha has evidence for cortisol reduction (discussed below)
5. Nutrition Factors: Building Blocks and Disruptors
Essential Nutrients for Testosterone Production
Zinc is directly involved in testosterone synthesis and is concentrated in the prostate and testes. Zinc deficiency reliably lowers testosterone; supplementation in deficient individuals raises it.[25]
Strong Evidence (for correction of deficiency)
Food Sources
- Oysters (highest food source)
- Beef and lamb
- Pumpkin seeds
- Crab, lobster
Caution: Don't megadose zinc long-term—it can deplete copper. If supplementing >30mg daily, consider adding 2mg copper.
Vitamin D functions more like a hormone than a vitamin. Receptors exist in testicular tissue, and D status correlates with testosterone levels.[26]
Moderate Evidence
A year-long supplementation study in men with low vitamin D showed a ~25% increase in testosterone.[27] Effects are most pronounced in those starting deficient (below 30 ng/mL).
Test your levels: Vitamin D is one of the most common deficiencies in developed countries, especially at higher latitudes or for those who work indoors.
Testosterone is synthesized from cholesterol. Adequate dietary fat—particularly saturated and monounsaturated fat—supports hormonal production.
Moderate Evidence
- Very low-fat diets (<20% of calories) are associated with lower testosterone[28]
- Saturated fat intake positively correlates with testosterone in some studies
- Cholesterol restriction can reduce substrate for steroidogenesis
Recommendations
- Don't fear dietary fat—aim for 25-40% of calories from fat
- Include saturated fats (eggs, red meat, coconut oil) in moderation
- Emphasize monounsaturated fats (olive oil, avocados, nuts)
- Limit excessive polyunsaturated vegetable oils
Magnesium is involved in over 300 enzymatic reactions, including testosterone synthesis. Deficiency is common and associated with lower testosterone.[29]
Moderate Evidence
Supplements with Evidence
The best-studied herbal intervention for testosterone. Multiple randomized controlled trials show meaningful effects.[30]
Strong Evidence
Research Findings
- Studies show 10-40% increases in testosterone
- Significant cortisol reduction (mechanism may be indirect)
- Improved sperm parameters
- Enhanced exercise performance and recovery
Traditional Southeast Asian herb with growing research support for testosterone and male reproductive health.[31]
Moderate Evidence
Appears to work partly by reducing SHBG, increasing free testosterone. Also shows cortisol-lowering effects and improved stress resilience.
Avoiding Endocrine Disruptors
Minimizing exposure to xenoestrogens and anti-androgens may be as important as what you add to your regimen.
High-Priority Avoidances
- BPA and phthalates: Avoid plastic food containers, especially when heated; use glass or stainless steel
- Parabens: Common in personal care products; check labels
- Pesticide residues: Consider organic for the "dirty dozen" produce highest in pesticides
- Non-stick cookware: PFAS chemicals; use cast iron or stainless steel
- Fragrances: Often contain phthalates; use fragrance-free products
- Receipts: Thermal paper contains BPA; decline or wash hands after handling
Focus first on the big levers: sleep, exercise, body composition, stress. Then address nutrient deficiencies (test Vitamin D, consider zinc/magnesium). Endocrine disruptor avoidance and supplements like ashwagandha are the polish on top of this foundation.
6. Testosterone Replacement Therapy: When and How
When natural optimization isn't sufficient—or when there's a genuine medical condition causing hypogonadism—testosterone replacement therapy (TRT) becomes a consideration. Understanding when it's appropriate, what options exist, and what monitoring is required allows for informed decision-making.
TRT is prescription hormone therapy that requires physician oversight. We do not provide dosing recommendations. This section is educational—work with a qualified doctor (endocrinologist, urologist, or hormone-specialized physician) for treatment.
When TRT May Be Appropriate
The Endocrine Society guidelines recommend TRT for men with:[32]
- Consistently low testosterone — Two morning measurements below ~300 ng/dL (though many clinicians use higher thresholds)
- Symptoms of androgen deficiency — Low libido, erectile dysfunction, fatigue, depressed mood, reduced muscle mass, etc.
- No contraindications — See below
Contraindications
- Prostate or breast cancer (current or history)
- Polycythemia (elevated hematocrit >54%)
- Untreated severe sleep apnea
- Uncontrolled heart failure
- Desire for fertility in the near term (TRT suppresses sperm production)
- PSA >4 ng/mL without urological evaluation
TRT Modalities
Intramuscular or subcutaneous injections of testosterone esters. The gold standard for efficacy and cost-effectiveness.
Common Esters
| Ester | Half-Life | Typical Frequency |
|---|---|---|
| Testosterone Cypionate | ~8 days | 1-2x weekly |
| Testosterone Enanthate | ~7 days | 1-2x weekly |
| Testosterone Propionate | ~2 days | Every other day |
| Testosterone Undecanoate (Nebido) | ~20-30 days | Every 10-14 weeks |
Advantages
- Most effective at raising and maintaining testosterone levels
- Flexible dosing allows fine-tuning
- Most affordable option (generic cypionate/enanthate)
- Subcutaneous injection is painless with small needles
Disadvantages
- Requires self-injection or clinic visits
- Levels fluctuate between injections (less so with frequent dosing)
- Peak-trough variation can affect mood/energy in sensitive individuals
Modern protocol trend: More frequent, smaller injections (2-3x weekly subcutaneous) produce more stable levels with fewer side effects than traditional weekly or biweekly intramuscular injections.
Daily application of testosterone gel or cream to skin, typically shoulders, upper arms, or abdomen.
Common Products
- AndroGel, Testim (commercial gels)
- Compounded testosterone cream (often better absorption)
- Testosterone nasal gel (Natesto)
Advantages
- No injections
- More stable daily levels (mimics circadian rhythm better)
- Easy to adjust or discontinue
Disadvantages
- Transfer risk—can expose partners, children, pets to testosterone
- Variable absorption (some men are "poor absorbers")
- More expensive than injectable
- Daily application required
- May not achieve optimal levels in all men
Small pellets implanted under the skin (usually hip/buttock) that slowly release testosterone over 3-6 months.
Advantages
- Convenient—no daily/weekly action required
- Very stable levels
- No transfer risk
Disadvantages
- Requires minor surgical procedure for insertion
- Cannot easily adjust if levels are wrong
- Pellet extrusion (falling out) occurs in ~10% of cases
- More expensive
- Levels decline toward end of cycle
Adjunctive Medications
TRT often involves additional medications to manage specific effects:
hCG (Human Chorionic Gonadotropin)
- Mimics LH, maintains testicular function and size
- Preserves some fertility potential
- Often co-prescribed with TRT, especially in younger men
- Increases intratesticular testosterone
Aromatase Inhibitors (Anastrozole, etc.)
- Reduce conversion of testosterone to estradiol
- Used if estrogen rises too high on TRT
- Overuse can crash estrogen (problematic—see earlier section)
- Should be dosed conservatively based on labs, not prophylactically
Monitoring on TRT
| Marker | Frequency | Target/Concern |
|---|---|---|
| Total/Free Testosterone | 6-8 weeks, then q6-12 months | Optimal range; adjust protocol if needed |
| Estradiol (sensitive) | With testosterone | 20-35 pg/mL; avoid extremes |
| Hematocrit/Hemoglobin | Baseline, 3-6 months, then annually | Hematocrit <54%; donate blood if elevated |
| PSA | Baseline, 3-6 months, then annually | Monitor for significant increases |
| Lipid Panel | Annually | TRT can affect HDL/LDL |
| Metabolic Panel | Annually | Liver, kidney function, glucose |
7. The Controversy: Risks, Benefits, and Fertility
Testosterone therapy remains controversial in mainstream medicine, though the landscape has shifted significantly with recent large-scale evidence. Understanding the actual risk-benefit profile requires looking at real data rather than theoretical concerns.
Cardiovascular Risk: The Evolving Story
For years, TRT was associated with cardiovascular concern based on a few poorly-designed studies and theoretical considerations about hematocrit increases and potential prothrombotic effects.
The TRAVERSE trial (2023) was a game-changer—a randomized, placebo-controlled trial of over 5,200 men aged 45-80 with preexisting cardiovascular disease or high cardiac risk.[14]
- No increased cardiovascular events — Primary endpoint (cardiovascular death, MI, stroke) was not different between testosterone and placebo groups
- No excess mortality
- Higher incidence of atrial fibrillation and acute kidney injury in testosterone group (warrants monitoring)
- Improved sexual function, mood, physical function in testosterone group
Bottom line: In men with low testosterone and cardiovascular risk, TRT does not appear to increase major cardiovascular events over ~3 years of follow-up.
Prostate Risk
The prostate cancer concern stems from the androgen-dependence of prostate tissue. However, evidence does not support that TRT increases prostate cancer risk in men with normal prostate exams and PSA:[33]
- Multiple meta-analyses show no increased prostate cancer incidence with TRT
- Very high intratesticular testosterone doesn't increase cancer risk in young men
- The "saturation model" suggests androgen receptors are saturated at relatively low T levels; more T doesn't mean more prostate stimulation
- Monitoring PSA remains important; TRT in men with active prostate cancer is contraindicated
Fertility: The Critical Consideration
This is the most important practical consideration for younger men. TRT suppresses the HPG axis and dramatically reduces or eliminates sperm production.
Exogenous testosterone suppresses LH and FSH, which are required for spermatogenesis. Most men on TRT become azoospermic (zero sperm) or severely oligospermic. While often reversible upon discontinuation, recovery can take 6-18 months and isn't guaranteed.
Fertility-Preserving Options
- hCG — Maintains some testicular function; may preserve some fertility
- hCG monotherapy — Alternative to TRT that maintains fertility
- Clomiphene citrate (Clomid) — SERM that blocks estrogen feedback, increasing LH/FSH and natural testosterone; preserves fertility but less effective at raising T than TRT
- Enclomiphene — Active isomer of clomiphene with fewer side effects
- Sperm banking — If starting TRT, bank sperm first if future fertility is desired
Other Risks and Side Effects
- Erythrocytosis (elevated hematocrit) — Most common side effect; increases blood viscosity; managed with blood donation or dose adjustment
- Acne and oily skin — Androgen effect on sebaceous glands
- Hair loss — TRT can accelerate male pattern baldness in predisposed men
- Gynecomastia — If estrogen rises too high; preventable with monitoring
- Testicular atrophy — Testes shrink without LH stimulation; prevented with hCG
- Sleep apnea worsening — Possible in predisposed individuals
- Mood changes — Usually positive, but some men experience irritability, especially with unstable levels
8. Other Androgens and SARMs: What Research Shows
Beyond testosterone itself, various other compounds with androgenic or anabolic properties have entered the optimization space. Understanding what the research actually shows— versus marketing claims—is essential for informed decision-making.
DHEA (Dehydroepiandrosterone)
DHEA is a prohormone produced by the adrenal glands that serves as a precursor to both testosterone and estrogen.
Moderate Evidence
- Levels decline significantly with age (by age 70, ~10-20% of peak)
- Supplementation (25-100mg/day) raises DHEA-S levels reliably
- Effects on testosterone are modest and inconsistent[34]
- May have independent benefits for mood, cognition, and bone density
- Converts more to estrogen in some individuals
Practical view: DHEA is a reasonable adjunct for men over 50 with low DHEA-S levels. Don't expect dramatic testosterone increases; effects are subtle.
SARMs (Selective Androgen Receptor Modulators)
SARMs were developed to provide anabolic effects (muscle, bone) without the full androgenic profile of testosterone (prostate stimulation, hair loss, etc.). They remain experimental with no approved medical uses.
SARMs are investigational drugs, not supplements. They are not approved by any regulatory agency. Products sold as SARMs are frequently mislabeled, underdosed, or contaminated. Long-term safety data in humans does not exist.
Common SARMs
| Compound | Primary Effect | Research Status |
|---|---|---|
| Ostarine (MK-2866) | Muscle preservation, mild anabolic | Phase 2 trials completed; development paused |
| LGD-4033 (Ligandrol) | Stronger anabolic, lean mass | Phase 1 trials; suppresses endogenous T |
| RAD-140 (Testolone) | Strong anabolic, neuroprotective claims | Preclinical; very suppressive |
| MK-677 (Ibutamoren) | GH secretagogue (not actually a SARM) | Phase 2; increases GH, hunger, water retention |
What Research Actually Shows
- They do build muscle — Phase 2 data shows statistically significant lean mass increases[35]
- They do suppress testosterone — All SARMs suppress endogenous T to varying degrees; "no PCT needed" is false
- Selectivity is incomplete — Effects on lipids (HDL suppression), liver enzymes have been observed[36]
- Long-term safety is unknown — No multi-year human data exists
- Quality control is nonexistent — Studies of "SARMs" sold online find frequent misrepresentation[37]
Bottom line: SARMs are not a "safer alternative to steroids." They suppress natural testosterone, have unknown long-term risks, and come with quality control concerns. For most men seeking optimization, legal alternatives (TRT if appropriate, natural optimization) make more sense.
Anabolic Steroids
Traditional anabolic steroids (nandrolone, trenbolone, etc.) are outside the scope of optimization and health-focused discussion. These are controlled substances with well-documented risk profiles including:
- Severe HPTA suppression
- Cardiovascular stress (LVH, lipid disruption)
- Liver toxicity (oral steroids)
- Psychological effects
- Legal consequences
If you're considering supraphysiological androgens for physique purposes, that's a different decision framework than health optimization. Be honest about goals and accept the risk profile.
9. Practical Framework for Evaluation and Action
Bringing everything together, here's a systematic approach for any man concerned about his testosterone status and overall hormonal health.
Low libido? Fatigue? Brain fog? Mood changes? Loss of motivation? Difficulty building muscle despite training? Morning erections diminished? These symptoms don't diagnose low T but warrant investigation.
Morning, fasting blood draw. Include: Total T, Free T, SHBG, Estradiol (sensitive), LH, FSH, CBC, metabolic panel, lipids, PSA (if 40+), thyroid (TSH, free T4), Vitamin D, prolactin. Repeat if low.
Sleep 7-9 hours consistently. Resistance train 3-5x/week. Lose excess body fat. Manage stress. Address nutrient deficiencies (Vitamin D, zinc, magnesium). Consider ashwagandha. Minimize endocrine disruptors.
Did levels improve? Do symptoms remain? Many men see 100-200 ng/dL increases from lifestyle alone. If still symptomatic with suboptimal levels, proceed to medical evaluation.
Work with a physician (endocrinologist, urologist, or hormone specialist). Discuss TRT candidacy. Consider alternatives (clomiphene, hCG) if fertility is a concern. Rule out secondary causes (pituitary issues).
Follow-up labs at 6-8 weeks. Adjust protocol based on levels, symptoms, and side effects. Monitor hematocrit, estradiol, PSA. Maintain lifestyle factors— TRT amplifies good habits but doesn't replace them.
When to Act vs. When to Accept
Not every man needs TRT. Some perspective:
- If you're 35 with a testosterone of 650 ng/dL and no symptoms, you don't have a problem—don't create one
- If you're 45 with testosterone of 350 ng/dL, significant symptoms, and lifestyle is already optimized, medical intervention is reasonable
- Age-related decline is real but not inevitable at the rates we're seeing. Much of what's attributed to "normal aging" is actually lifestyle and environmental
- Optimization ≠ supraphysiological levels. The goal is healthy function, not maximum testosterone
Finding the Right Provider
Not all physicians understand testosterone therapy. Look for:
- Willingness to look at the full picture — Not just total T, but free T, SHBG, symptoms
- Modern protocols — Frequent injections, attention to E2 management, hCG consideration
- Not dismissive — "Your levels are normal" when you're at 320 ng/dL with symptoms is inadequate
- Not a pill mill — Jumps to TRT without lifestyle discussion or proper workup is a red flag too
Options include endocrinologists, urologists with andrology interest, anti-aging/longevity medicine physicians, and some progressive primary care providers. Telehealth hormone clinics have expanded access but quality varies—do due diligence.
Testosterone optimization isn't about chasing numbers—it's about vitality, function, and quality of life. The goal is to feel strong, clear-headed, motivated, and capable well into your later decades. For some men, that requires medical intervention. For many, it requires sleeping better, training harder, eating smarter, and reducing exposure to the modern factors suppressing our hormones. Know your numbers, optimize what you can control, and make informed decisions about the rest.
References
- Simerly RB, et al. Distribution of androgen and estrogen receptor mRNA-containing cells in the rat brain. J Comp Neurol. 1990;294(1):76-95.
- Cherrier MM, et al. Testosterone supplementation improves spatial and verbal memory in healthy older men. Neurology. 2001;57(1):80-8.
- Wolf OT, Kirschbaum C. Endogenous estradiol and testosterone levels are associated with cognitive performance in older women and men. Horm Behav. 2002;41(3):259-66.
- Muller M, et al. Endogenous sex hormones and cognitive function in aging men. J Clin Endocrinol Metab. 2005;90(5):2618-23.
- Janowsky JS. The role of androgens in cognition and brain aging in men. Neuroscience. 2006;138(3):1015-20.
- Snyder PJ, et al. Effects of testosterone treatment in older men. N Engl J Med. 2016;374(7):611-624.
- Shores MM, et al. Low serum testosterone and mortality in male veterans. Arch Intern Med. 2006;166(15):1660-5.
- McHenry J, et al. Sex differences in anxiety and depression: role of testosterone. Front Neuroendocrinol. 2014;35(1):42-57.
- Hermans EJ, et al. Testosterone administration reduces lying in men. PLoS One. 2010;5(7):e11356.
- Kelly DM, Jones TH. Testosterone: a metabolic hormone in health and disease. J Endocrinol. 2013;217(3):R25-45.
- Grossmann M. Low testosterone in men with type 2 diabetes: significance and treatment. J Clin Endocrinol Metab. 2011;96(8):2341-53.
- Khosla S, et al. Relationship of serum sex steroid levels and bone turnover markers with bone mineral density in men. J Clin Endocrinol Metab. 1998;83(7):2266-74.
- Araujo AB, et al. Endogenous testosterone and mortality in men: a systematic review and meta-analysis. J Clin Endocrinol Metab. 2011;96(10):3007-19.
- Lincoff AM, et al. Cardiovascular safety of testosterone-replacement therapy. N Engl J Med. 2023;389(2):107-117.
- Travison TG, et al. A population-level decline in serum testosterone levels in American men. J Clin Endocrinol Metab. 2007;92(1):196-202.
- Andersson AM, et al. Secular decline in male testosterone and sex hormone binding globulin serum levels in Danish population surveys. J Clin Endocrinol Metab. 2007;92(12):4696-705.
- Perheentupa A, et al. A cohort effect on serum testosterone levels in Finnish men. Eur J Endocrinol. 2013;168(2):227-33.
- Swan SH, et al. Semen quality in relation to biomarkers of pesticide exposure. Environ Health Perspect. 2003;111(12):1478-84.
- Luboshitzky R, et al. Disruption of the nocturnal testosterone rhythm by sleep fragmentation in normal men. J Clin Endocrinol Metab. 2001;86(3):1134-9.
- Leproult R, Van Cauter E. Effect of 1 week of sleep restriction on testosterone levels in young healthy men. JAMA. 2011;305(21):2173-4.
- Kraemer WJ, Ratamess NA. Hormonal responses and adaptations to resistance exercise and training. Sports Med. 2005;35(4):339-61.
- Vingren JL, et al. Testosterone physiology in resistance exercise and training. Sports Med. 2010;40(12):1037-53.
- Corona G, et al. Body weight loss reverts obesity-associated hypogonadotropic hypogonadism: a systematic review and meta-analysis. Eur J Endocrinol. 2013;168(6):829-43.
- Cumming DC, et al. Reproductive hormone increases in response to acute exercise in men. Med Sci Sports Exerc. 1986;18(4):369-73.
- Prasad AS, et al. Zinc status and serum testosterone levels of healthy adults. Nutrition. 1996;12(5):344-8.
- Wehr E, et al. Association of vitamin D status with serum androgen levels in men. Clin Endocrinol (Oxf). 2010;73(2):243-8.
- Pilz S, et al. Effect of vitamin D supplementation on testosterone levels in men. Horm Metab Res. 2011;43(3):223-5.
- Whittaker J, Wu K. Low-fat diets and testosterone in men: Systematic review and meta-analysis of intervention studies. J Steroid Biochem Mol Biol. 2021;210:105878.
- Maggio M, et al. The interplay between magnesium and testosterone in modulating physical function in men. Int J Endocrinol. 2014;2014:525249.
- Lopresti AL, et al. A randomized, double-blind, placebo-controlled, crossover study examining the hormonal and vitality effects of ashwagandha in aging, overweight males. Am J Mens Health. 2019;13(2):1557988319835985.
- Talbott SM, et al. Effect of Tongkat Ali on stress hormones and psychological mood state in moderately stressed subjects. J Int Soc Sports Nutr. 2013;10(1):28.
- Bhasin S, et al. Testosterone therapy in men with hypogonadism: an Endocrine Society clinical practice guideline. J Clin Endocrinol Metab. 2018;103(5):1715-1744.
- Boyle P, et al. Endogenous and exogenous testosterone and the risk of prostate cancer and increased prostate-specific antigen. BJU Int. 2016;118(5):672-89.
- Morales A, et al. Adding to the controversy: pitfalls in the diagnosis of testosterone deficiency syndromes with questionnaires and biochemistry. Aging Male. 2007;10(2):57-65.
- Dalton JT, et al. The selective androgen receptor modulator GTx-024 (enobosarm) improves lean body mass and physical function in healthy elderly men and postmenopausal women. J Cachexia Sarcopenia Muscle. 2011;2(3):153-161.
- Basaria S, et al. The safety, pharmacokinetics, and effects of LGD-4033, a novel nonsteroidal oral, selective androgen receptor modulator. J Gerontol A Biol Sci Med Sci. 2013;68(1):87-95.
- Van Wagoner RM, et al. Chemical composition and labeling of substances marketed as selective androgen receptor modulators and sold via the internet. JAMA. 2017;318(20):2004-2010.
- Travison TG, et al. Harmonized reference ranges for circulating testosterone levels in men of four cohort studies. J Clin Endocrinol Metab. 2017;102(4):1161-1173.
- Mulligan T, et al. Prevalence of hypogonadism in males aged at least 45 years: the HIM study. Int J Clin Pract. 2006;60(7):762-9.
- Corona G, et al. Testosterone replacement therapy and cardiovascular risk: a review. World J Mens Health. 2015;33(3):130-42.
- Traish AM, et al. Long-term testosterone therapy in hypogonadal men ameliorates elements of the metabolic syndrome. Int J Clin Pract. 2014;68(3):314-29.
- Wang C, et al. Investigation, treatment, and monitoring of late-onset hypogonadism in males. Int J Androl. 2009;32(1):1-10.
- Dhindsa S, et al. Testosterone concentrations in diabetic and nondiabetic obese men. Diabetes Care. 2010;33(6):1186-92.
- Nieschlag E, et al. Testosterone: action, deficiency, substitution. Cambridge University Press. 2012.
- Rastrelli G, et al. Testosterone replacement therapy for sexual symptoms. Sex Med Rev. 2019;7(3):464-475.
- Hackett G, et al. British Society for Sexual Medicine guidelines on adult testosterone deficiency, with statements for UK practice. J Sex Med. 2017;14(12):1504-1523.
- Calof OM, et al. Adverse events associated with testosterone replacement in middle-aged and older men: a meta-analysis. J Gerontol A Biol Sci Med Sci. 2005;60(11):1451-7.
- Swerdloff RS, et al. Long-term pharmacokinetics of transdermal testosterone gel in hypogonadal men. J Clin Endocrinol Metab. 2000;85(12):4500-10.
Questions about hormonal optimization? Join the discussion.
Enter the Soma Community