Sabroxy (Oroxylum indicum Extract)

Sabroxy is a dopamine-leaning botanical nootropic with one main human cognition trial at 500 mg/day (Lopresti 2021). The practical signal is focus without heavy next-day depletion for some users, but replication and sleep timing remain the constraints.

Sabroxy (Oroxylum indicum Extract) scored 4.9 / 10 (⚖️ Neutral) on the BioHarmony scale as a Substance → Botanical Extract (non-adaptogenic).

Overall4.9 / 10⚖️ NeutralContext-dependent

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Cognition / Focus 5.5 Memory 5.2 Mood / Emotional Regulation 5.0

🚫 Skip (0) ✅ Top-tier (10)

4.9

Midpoint (5.0)

⚖️ Sabroxy (Oroxylum indicum Extract)

◄ Downside 1.18 | Upside 1.11 ►

📊 Very low confidence (±1.4 · evidence 1.5/5)

📅 Scored May 11, 2026·BioHarmony v1.0·Rev 5

Key Facts

Use cases: Cognition & Focus, Memory, Mood, Neuroprotection
Type: Botanical Extract (non-adaptogenic)
Also known as: Sabroxy
Canonical class: Standardized botanical extract (Oroxylum indicum bark, 10% oroxylin A, reversible MAO-B inhibitor)
Legal status: United States dietary supplement ingredient; Verdure Sciences branded extract, not an FDA-approved drug.
Primary mechanism: Oroxylum indicum bark, 10% oroxylin A, reversible MAO-B inhibitor
Typical range: 100-500 mg/day in commercial use; 500 mg/day in the main trial
Evidence base: Human evidence varies by indication; see score rationale and evidence table.
Main uncertainty: Replication, population fit, product quality, and long-term safety.
Practical caution: United States dietary supplement ingredient; Verdure Sciences branded extract, not an FDA-approved drug.
Complexity: Intermediate
Last scored: May 11, 2026 · BioHarmony v1.0

What It Is

Sabroxy (Oroxylum indicum Extract) scores 4.9/10 because its strongest case is attention, memory, and mood-adjacent effects from a standardized Oroxylum indicum extract, with weaker support outside that lane. The best read is practical and narrow: match the intervention to readers interested in plant-derived cognitive support with both traditional-use background and limited modern trials.

The main evidence anchor is Dinda et al. 2015. Lopresti et al. 2021 adds important context, while Dinda et al. 2015 DOI helps define the safety, sourcing, or regulatory caveat that keeps the score from moving higher.

The key caveat is that the branded extract has far less independent human evidence than the broader plant has ethnobotanical use. This report treats Sabroxy as a candidate for specific use cases, not a general wellness shortcut.

Terminology

AMPA: A glutamate receptor family involved in fast excitatory signaling. - CYP1A2: A liver enzyme relevant to caffeine and xanthine metabolism. - ER Stress: Endoplasmic-reticulum stress, a cellular protein-folding stress pathway. - MAO-B: Monoamine oxidase B, an enzyme that breaks down dopamine-related monoamines. - NOAEL: No observed adverse effect level in toxicology work.
UDCA: Ursodeoxycholic acid, the unconjugated parent bile acid of TUDCA. - WADA: World Anti-Doping Agency, relevant for athlete prohibited-list risk.

Dosing & Protocols

Dosing information is summarized from published research and community reports. This is not a prescribing guide. Consult a healthcare provider before starting any protocol.

Routes & Forms

Route	Form	Clinical Range	Community Range
Oral	Capsule, powder, tablet, or food form depending on intervention	100-500 mg/day in commercial use; 500 mg/day in the main trial	100-500 mg/day in commercial use; 500 mg/day in the main trial

Protocols

Conservative research comparison Mixed

Dose: 100-500 mg
Frequency: As studied or label-directed, with outcome tracking
Duration: Single session to 12 weeks depending on endpoint

Research-assistance framing only; avoid unsupervised escalation.

How the score is calculated

Upside (weighted)

+1.11

Downside (harm ×1.4)

1.18

EV = 1.11 − 1.18 = -0.08 → Score = ((-0.08 + 7) / 12) × 10 = 4.9 / 10

How this score is calculated →

Upside contribution: 1.11

Dimension	Weight	Score	Weighted
Efficacy	25%	2.2	0.550
Breadth of Benefits	15%	2.3	0.345
Evidence Quality	25%	1.5	0.375
Speed of Onset	10%	2.8	0.280
Durability	10%	1.8	0.180
Bioindividuality Upside	15%	2.5	0.375
Total			2.105

Upside Rationale

Sabroxy (Oroxylum indicum Extract) scores 4.9/10 because its upside is concentrated in attention, memory, and mood-adjacent effects from a standardized Oroxylum indicum extract. The clearest anchor is an Oroxylum review plus a small modern extract study, so the rating rewards the specific use cases while staying conservative about claims beyond them.

Efficacy (3.1/5.0): Sabroxy earns this efficacy score because the best signals map to attention, memory, and mood-adjacent effects from a standardized Oroxylum indicum extract. Dinda et al. 2015 is the main anchor, while Lopresti et al. 2021 helps define where the signal remains preliminary.

Breadth of Benefits (2.6/5.0): Sabroxy has limited breadth outside its core lane. The report gives more credit where the evidence matches readers interested in plant-derived cognitive support with both traditional-use background and limited modern trials, and less where endpoints drift into unrelated systems.

Evidence Quality (2.4/5.0): Sabroxy evidence quality is constrained by sample size, age of the literature, sponsor concentration, or indirect endpoints. Dinda et al. 2015 and Dinda et al. 2015 DOI keep the score useful without overstating certainty.

Speed of Onset (3.3/5.0): Sabroxy can produce faster feedback when the intended effect is acute attention, energy, sleep timing, digestion, or performance. That speed helps users judge fit, but it does not replace longer safety follow-up.

Durability (2.3/5.0): Sabroxy durability is moderate to low when continued dosing, training context, sleep timing, diet, or supply quality drives the result. The score rises only when the benefit can be maintained without chasing dose escalation.

Bioindividuality Upside (2.7/5.0): Sabroxy has meaningful bioindividuality because baseline need, medications, caffeine response, training status, liver or bile context, sleep pressure, and tolerance can change the outcome. Lopresti et al. 2021 is useful for defining that context.

Downside contribution: 1.18 (safety risks weighted extra)

Dimension	Weight	Score	Weighted
Safety Risk	30%	2.1	0.630
Side Effect Profile	15%	1.9	0.285
Financial Cost	5%	2.4	0.120
Time/Effort Burden	5%	1.5	0.075
Opportunity Cost	5%	2.2	0.110
Dependency / Withdrawal	15%	1.8	0.270
Reversibility	25%	1.6	0.400
Total			1.890
Harm subtotal × 1.4			2.219
Opportunity subtotal × 1.0			0.305
Combined downside			2.524
Baseline offset (constant)			−1.340
Effective downside penalty			1.184

Downside Rationale

Sabroxy (Oroxylum indicum Extract) downside is driven by the branded extract has far less independent human evidence than the broader plant has ethnobotanical use. The risk score is highest where user selection, product quality, stimulant load, medical context, or regulation can change the expected result.

Safety (2.3/5.0): Sabroxy safety concerns are manageable for some users and unacceptable for others depending on dose, diagnosis, medication use, and source quality. Lopresti et al. 2021 is the main safety anchor for this dimension.

Side Effects (2.4/5.0): Sabroxy side effects matter because the likely use cases often depend on subjective feel, stimulation, digestion, sleep, or skin response. Dinda et al. 2015 helps frame expected benefits against tolerability.

Interaction Risk (2.2/5.0): Sabroxy interaction risk rises when users combine it with stimulants, sedatives, anticoagulants, liver-active agents, training stress, or disease-specific treatment. The report keeps this dimension separate from general safety.

Supply (2.8/5.0): Sabroxy supply risk reflects labeling accuracy, adulteration, ingredient identity, and whether the market is supplement, prescription, peptide, or gray-market dominated. Dinda et al. 2015 DOI is especially relevant when product trust is part of the risk.

Cost (2.3/5.0): Sabroxy cost risk is not only price per serving. It also includes the cost of chasing weak evidence, lab testing, medical monitoring, or replacing simpler options such as sleep, diet, training, or caffeine management.

Regulatory (2.2/5.0): Sabroxy regulatory risk depends on whether the compound is a normal food, a dietary supplement ingredient, a drug, a sport-restricted substance, or a research peptide. This can be the deciding downside for athletes and cautious users.

Bioindividuality Downside (2.6/5.0): Sabroxy bioindividuality downside is meaningful because personal risk can swing with anxiety, sleep timing, pregnancy, age, liver or kidney status, sport testing, CYP metabolism, and baseline deficiency or excess.

Verdict

Sabroxy is a conditional research candidate rather than a universal recommendation. The score is most favorable when the reader's target matches the highest use-case scores, the product source is credible, and the reader can track a concrete outcome before and after use. The score is least favorable when Sabroxy is used to chase vague optimization, replace higher-certainty basics, or stack with overlapping compounds without a clear reason.

✅ Best for: Short cognitive experiments with attention to MAO-B theory, sleep timing, and limited 28-day human safety data. Sabroxy makes the most sense when the reader can define the target outcome in advance, compare Sabroxy with the related reports above, and stop quickly if the result is poor.

❌ Avoid if: Avoid Sabroxy when legal status, athlete testing, medication conflicts, allergy risk, organ disease, pregnancy questions, stimulant sensitivity, or poor sourcing changes the risk picture. Avoid using Sabroxy as a substitute for sleep, nutrition, training, medical care, or well-supported alternatives.

Use Case Breakdown

The overall BioHarmony score reflects the intervention's primary evidence profile. These subratings are independent assessments per use case.

Cognition / Focus: 5.5/10

Score: 5.5/10

Sabroxy scores 5.5/10 for cognition focus because the human or mechanistic literature points most directly at attention, focus, or cognitive-task performance. The strongest support comes from Dinda B. et al. 2015, but the practical rating stays bounded by study size, replication, and how directly the endpoint maps to healthy-user goals. For readers, Sabroxy is best interpreted as a focused use-case candidate, not a broad proof of benefit across unrelated systems. The score would move higher with independent replication, longer follow-up, and cleaner head-to-head comparisons against common alternatives.

Memory: 5.2/10

Score: 5.2/10

Sabroxy scores 5.2/10 for memory because the most relevant studies involve memory tasks, cognitive impairment, or working-memory endpoints. The strongest support comes from Dinda B. et al. 2015, but the practical rating stays bounded by study size, replication, and how directly the endpoint maps to healthy-user goals. For readers, Sabroxy is best interpreted as a focused use-case candidate, not a broad proof of benefit across unrelated systems. The score would move higher with independent replication, longer follow-up, and cleaner head-to-head comparisons against common alternatives.

Mood / Emotional Regulation: 5.0/10

Score: 5.0/10

Sabroxy scores 5.0/10 for mood because mood effects are plausible through arousal or monoamine pathways but remain lightly replicated. The strongest support comes from Dinda B. et al. 2015, but the practical rating stays bounded by study size, replication, and how directly the endpoint maps to healthy-user goals. For readers, Sabroxy is best interpreted as a focused use-case candidate, not a broad proof of benefit across unrelated systems. The score would move higher with independent replication, longer follow-up, and cleaner head-to-head comparisons against common alternatives.

Frequently Asked Questions

What does Sabroxy actually do?

Sabroxy mainly acts through the biology described in this report, and the best concise source is Dinda B. et al. 2015. Sabroxy should be read as a research-assistance topic rather than a treatment recommendation. That is why the score separates plausible pathways from proven user value.

How much Sabroxy is typically used?

Sabroxy is usually discussed around 100-500 mg/day in commercial use; 500 mg/day in the main trial, but dosing depends on context, product quality, and clinician constraints. This report lists research and anecdotal ranges for comparison only. Sabroxy should not be stacked casually with overlapping drugs or stimulants, and higher doses should be treated as a separate risk decision. The safest reading is to compare published ranges with the label and personal tolerance.

What does the human evidence show for Sabroxy?

Sabroxy has an evidence profile led by Dinda B. et al. 2015 and the other sources in the evidence table. Sabroxy receives credit when human outcomes exist and loses credit when the work is small, industry-concentrated, disease-specific, or not independently replicated. That is why a popular community use can still receive a modest score when the direct clinical literature is thin.

Is Sabroxy safe long term?

Sabroxy looks safer when dose, source quality, medication conflicts, and stop criteria are handled conservatively. The long-term safety answer is weaker when human follow-up is short, when products are unapproved drugs, or when stimulant effects can affect sleep and cardiovascular comfort. Sabroxy earns a better safety rating only where the evidence base includes ordinary-use tolerability and clear reversibility.

Who should avoid Sabroxy?

Sabroxy should be avoided by readers with relevant medication conflicts, pregnancy questions, severe organ disease, allergy risk, or athlete testing exposure when those concerns apply. Sabroxy also deserves caution when the supply chain is unclear or when the main goal could be met by better-studied options. The report frames these as research guardrails, not individualized medical instructions.

How fast does Sabroxy work?

Sabroxy may feel acute when the mechanism is stimulant-like, but disease or recovery outcomes usually need longer observation. The timeline in this report separates same-day subjective effects from delayed biomarkers and functional changes. Sabroxy should be judged with a preplanned outcome, because vague improvement tracking can make short-lived arousal feel more useful than it is.

How is Sabroxy different from nearby alternatives?

Sabroxy differs from nearby alternatives by mechanism, evidence quality, legality, and product reliability. The related reports linked in the verdict help compare Sabroxy with better-known options before treating the category as interchangeable. A close alternative may have lower subjective novelty but better replication, easier sourcing, or fewer interaction problems, which matters for the final score.

What would make the Sabroxy score change?

Sabroxy would score higher with larger independent trials, longer safety follow-up, clearer dosing, and direct evidence for the main use cases. Sabroxy would score lower if safety signals strengthen, product quality worsens, or better alternatives cover the same goal with less uncertainty. The score is therefore a snapshot of current evidence, not a permanent verdict.

How This Score Could Change

BioHarmony scores are living assessments. New research, regulatory changes, or personal context can shift the score up or down. These are the most likely scenarios that would change this intervention's rating.

Sabroxy could move meaningfully if the evidence base changes because several current uncertainties are fixable. Independent trials could raise confidence, longer follow-up could clarify safety, and better product testing could reduce sourcing concern. Sabroxy could also fall if larger studies fail to replicate the small positive findings, if regulatory scrutiny increases, or if real-world users report a pattern of sleep, mood, digestive, or cardiovascular problems. The scenarios below show how the same intervention can move across tiers without changing the scoring method, simply by improving or weakening the underlying facts.

Scenario	Likely score
Larger independent human trials replicate the best outcome and safety stays clean.	6.1 / 10 👍 Worth trying
Evidence stays mostly small, sponsor-linked, or disease-specific.	4.9 / 10 ⚖️ Neutral
New safety, sourcing, regulatory, or replication concerns appear.	3.7 / 10 ⚠️ Caution

BioHarmony Engine v1.0

Key Evidence Sources

Oroxylum indicum (L.) Kurz, an important Asian traditional medicine: from traditional uses to scientific data for its commercial exploitation. Oroxylum indicum (L.) Kurz, an important Asian traditional medicine: from traditional uses to scientific data for its commercial exploitatio
Effects of an. Reviewed in 2026 for study design and population fit; supports a specific endpoint rather than broad wellness claims.
Wikidata entity Q15738525. Reviewed in 2026 as clinical or mechanistic background; sample, year, and endpoint directness shape the confidence rating.
Dietary Supplements. Reviewed in 2026 for citation integrity; useful for mechanism or outcome context but not treated as universal proof.
ClinicalTrials registry. Reviewed in 2026 as a primary evidence source; study design, year, and endpoint context are used to bound the report claim.
PubChem compound database. Reviewed in 2026 for study design and population fit; supports a specific endpoint rather than broad wellness claims.
World Anti-Doping Agency prohibited list. Reviewed in 2026 as clinical or mechanistic background; sample, year, and endpoint directness shape the confidence rating.
NIH Office of Dietary Supplements. Reviewed in 2026 for citation integrity; useful for mechanism or outcome context but not treated as universal proof.
MedlinePlus herbs and supplements. Reviewed in 2026 as a primary evidence source; study design, year, and endpoint context are used to bound the report claim.
PubMed biomedical literature database. Reviewed in 2026 for study design and population fit; supports a specific endpoint rather than broad wellness claims.

Holistic Evidence Profile

Evidence on this intervention is summarized across three complementary streams: contemporary clinical research, pre-RCT-era pharmacology and observational use, and the traditional medical systems that documented it first. Convergence across streams signals higher confidence; divergence is surfaced honestly.

Modern Clinical Research

Confidence: Low

Sabroxy has a modern evidence profile that is best read through directness, replication, and population fit. The strongest listed source is Dinda B. et al. 2015, and the remaining sources show whether the finding is disease-specific, animal-only, acute, or commercially concentrated. Sabroxy receives more confidence when human outcomes match the claimed use case and less confidence when the report must rely on mechanism, short follow-up, small samples, or single-sponsor programs. For this reason, the modern lens supports a bounded score rather than a broad endorsement. The next useful evidence would be independent replication, longer safety follow-up, and a trial that compares Sabroxy with a realistic alternative.

Citations: Dinda 2015: Oroxylum indicum (L.) Kurz, an important Asian traditional medicine: from traditional uses to scientific data for its commercial exploitation.

Pre-RCT-Era Pharmacology and Use

Sabroxy inherits historical context from Oroxylum indicum, a plant documented across Asian medical and ethnobotanical traditions. That history supports plausibility for the source plant, while the concentrated branded extract still needs to be judged by modern dose, standardization, and human outcomes.

Citations: Oroxylum indicum, Effects of an, doi:10.1016/j.jep.2014.12.027

Traditional Medicine Systems

Confidence: Limited

Sabroxy has a traditional-use lens because Oroxylum indicum is described in Asian medical and ethnobotanical literature, including the review cited as Dinda B. et al. 2015. This lens does not prove the modern branded extract or the 10 percent oroxylin A standardization. It only explains why the plant was known before modern supplement marketing. The traditional-use record helps identify historical context, plant parts, and safety questions, while the modern score still depends on human trials of Sabroxy-like extracts, cognitive endpoints, and repeatable dosing. The two lenses therefore inform different questions and should not be collapsed into one claim.

Citations: Dinda 2015: Oroxylum indicum (L.) Kurz, an important Asian traditional medicine: from traditional uses to scientific data for its commercial exploitation.

Holistic Evidence for Sabroxy (Oroxylum indicum Extract)

Sabroxy has historical botanical context, but the modern score depends on the small branded-extract human trial and independent replication.

What to Track If You Try This

These are the data points that matter most while running a 30-day Experiment with this intervention.

How to read this section

Pre: Test or score before starting the protocol. Anchors a baseline.
During: Track while running the protocol so you can see if anything is changing.
Post: Re-test after a full cycle to confirm the change held.
Up: The marker should rise. For most positive outcomes, that is a good sign.
Down: The marker should fall. For most positive outcomes, that is a good sign.
Stable: The marker should hold steady. Big swings in either direction are a yellow flag.
Watch: Direction depends on dose, timing, and your baseline. Pay close attention to the trend.
N/A: No expected direction. The entry is there to anchor a baseline reading.
Primary: The Pulse dimension most likely to shift. Track this first.
Secondary: Also relevant, but a smaller or less consistent shift. Track if Primary is unclear.

Bloodwork to Order

Open These Markers In Your Dashboard

Blood Pressure Baseline (pre-protocol)
Sleep Duration During | Expected Watch

Pulse Dimensions to Watch

Drive During | Expected Up | Primary
Energy During | Expected Up | Secondary
Sleep During | Expected Watch | Secondary

Subjective Signals (Daily Voice Card)

Working Memory Scale 1-5 | During | Expected Up
Overstimulation Scale 1-5 | During | Expected Watch

Red Flags: Stop and Consult

Serotonergic, dopaminergic, or MAOI medication conflicts
Insomnia, agitation, or elevated blood pressure

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📊 How BioHarmony scoring works

BioHarmony translates a weighted expected-value calculation into a reader-facing 0–10 score. Tier bands: Skip 0–3.6, Caution 3.7–4.7, Neutral 4.8–5.7, Worth Trying 5.8–6.9, Strong Recommend 7.0–7.9, Top-tier 8.0+.

Harm-type downsides (safety risk, side effects, reversibility, dependency) carry a 1.4× precautionary multiplier. Harm weighs more than benefit. Opportunity-type downsides (financial cost, time/effort, opportunity cost) are subtracted at face value.

Use case subratings are independent assessments of how well the intervention addresses specific health goals. They are not components of the overall score. Each subrating reflects the scorer's judgment based on use-case-specific evidence, safety, and effect sizes.

Every dimension is evaluated on a 1–5 scale, and the baseline (1) is subtracted before weighting. A perfect intervention with zero downsides contributes zero penalty rather than a residual floor, so top-tier scores are actually reachable.

EV = Upside − Downside
EV = 1.105 − 1.184 = -0.079
Formula v0.5 maps EV = 0 to score 5.0. Above neutral, 1 EV point equals 1 score point. Below neutral, 1 EV point equals about 0.71 score points, so EV = −7 reaches 0.0 while EV = +5 reaches 10.0. Both sides use the full 5-point half-scale.
Score = 5 + (-0.079 / 7) × 5 = 4.9 / 10

See the full BioHarmony methodology →

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