← Tier board·File·#048·Evidence reviewed Jun 2026Tweet
01 · the file

Thymosin Beta 4.

D
Research-use-onlyThymic & immune-modulating peptides
DThymosin Beta 4Verdict: Mostly animal evidenceHuman evidence: limitedStatus: Research-use-onlyReceiptsCalculatorReferences
💡 Explain this simply
What this is

Thymosin Beta 4 is a research compound in the thymic & immune-modulating peptides.

Why people care

It draws interest for thymic & immune-modulating peptides.

What's actually supported

D-tier evidence: human evidence is limited; most support is preclinical.

What's not proven

General anti-aging / longevity; Human injury recovery; Muscle growth or fat loss claims.

What to be cautious about

Interesting on paper, but not a clinically proven option. The internet narrative is stronger than the human evidence.

What to compare next

Before you decide, compare Thymosin Beta 4 with Thymosin Alpha 1, Tb 500, Ll 37. See all →

Research-onlyAnimal-data heavySafety unclearRegulatory friction high
What it is

Thymosin Beta 4 is a research compound in the thymic & immune-modulating peptides.

What it does

Promoting new blood-vessel formation and repair signalling.

Why people use it

It draws interest for thymic & immune-modulating peptides.

Does it work?

D-tier evidence: human evidence is limited; most support is preclinical.

Bottom lineThymosin Beta 4 is D-tier: scientifically interesting in preclinical models, but human evidence is minimal and the online narrative tends to run ahead of it.
What the published evidence shows

A small actin-sequestering peptide (the parent of the TB-500 fragment) studied for tissue repair, wound healing, angiogenesis, and cardiac/corneal regeneration. Evidence is largely animal models and small early-phase trials; it is not an approved drug.

[1]Thymosin β4 accelerates wound healingJ Invest Dermatol, 1999 (PMID 10469335)

Verified citations resolve to PubMed / FDA. See how we score.

Thymosin Beta 4: the research file

What it is

Thymosin beta-4 (Tβ4) is a small, naturally occurring 43-amino-acid acidic peptide found in nearly all mammalian cells and in high concentrations in platelets, wound fluid, and many tissues. It is the principal member of the beta-thymosin family and is one of the most abundant actin-binding proteins in the cytoplasm. The injectable "research peptide" TB-500 is widely marketed as thymosin beta-4, but it is typically a synthetic fragment or analog of the parent molecule rather than the full-length, naturally sequenced peptide; the two are not strictly interchangeable.

How it works

Tβ4's best-characterized molecular function is sequestering monomeric (G-)actin: it binds G-actin in a roughly 1:1 ratio, buffers the pool of unpolymerized actin, and thereby regulates cytoskeletal assembly, cell migration, and motility. Beyond this structural role, Tβ4 has been reported to upregulate cell-survival signaling — notably activation of integrin-linked kinase (ILK) and the Akt pathway in cardiac cells — and to influence angiogenesis, inflammation, and the actin-binding protein laminin/myosin machinery during tissue remodeling. It also has downstream effects attributed to its N-terminal tetrapeptide (Ac-SDKP), a cleavage product with antifibrotic and anti-inflammatory activity. These mechanisms are largely defined in cell-culture and animal systems.

What the evidence shows

The strongest human clinical data come from ophthalmology: the full-length peptide as RGN-259 (0.1% Tβ4 ophthalmic solution, RegeneRx/regional partners) was studied in a randomized, placebo-controlled, double-masked Phase III trial in neurotrophic keratopathy (Int J Mol Sci 2022, PMID 36613994), and in the ARISE-1/-2/-3 Phase III dry-eye program, where ARISE-3 missed its co-primary endpoints but showed significant improvement in some pre-specified secondary sign/symptom measures with a clean safety profile. Most other applications remain preclinical: the landmark cardiac work (Bock-Marquette et al., Nature 2004, PMID 15565145) showed Tβ4 promoted cardiomyocyte migration, survival, and improved cardiac function after injury in mice via ILK/Akt, and dermal/corneal wound-healing benefits are documented in animal models (e.g., Sosne et al., Exp Eye Res 2002, PMID 11950239). There is no FDA-approved Tβ4 product and no robust human evidence for the systemic "tissue repair," tendon/muscle recovery, or anti-aging uses for which TB-500 is informally promoted; that gap between animal data and proven human benefit is substantial.

Safety considerations

In the controlled ophthalmic trials, topical Tβ4 (RGN-259) was generally well tolerated with a safety profile comparable to placebo, but those data are limited to eye-drop administration and do not establish the safety of systemic injection. For injectable TB-500 sold as a research chemical, there are essentially no published controlled human safety data: long-term effects, immunogenicity, and risks are not characterized in humans. A specific theoretical concern is Tβ4's role in cell migration and angiogenesis, which has prompted caution about effects on tumor growth or metastasis; some preclinical studies link elevated Tβ4 to more aggressive tumor behavior. Material sold outside regulated channels also carries contamination, mislabeling, and dosing-uncertainty risks. No doses or protocols are provided here.

Regulatory status

Thymosin beta-4 is not FDA-approved for any indication; the full-length peptide (RGN-259) is investigational, completed Phase III trials in eye disease, and has held orphan-drug designation but no marketing approval, while injectable TB-500 is sold only as a research-use/unapproved compound. It is prohibited in sport at all times by WADA under section S2 (peptide hormones, growth factors, related substances and mimetics).

Key facts
  • 43-amino-acid endogenous peptide; the major member of the beta-thymosin family and one of the most abundant intracellular actin-sequestering proteins
  • Found in high concentrations in platelets and wound fluid, implicating it in natural tissue repair
  • Full-length Tβ4 (RGN-259) reached Phase III human trials in ophthalmology (neurotrophic keratopathy and dry eye), unlike most claimed uses
  • The popular injectable 'TB-500' is generally a synthetic fragment/analog, not necessarily identical to natural full-length thymosin beta-4
  • Cardiac, dermal, and CNS repair claims rest largely on animal and cell studies, not confirmed human outcomes
  • Banned by WADA in and out of competition (S2); no FDA-approved product exists
Sources
  1. [1]Thymosin beta4 activates integrin-linked kinase and promotes cardiac cell migration, survival and cardiac repairNature, 2004, PMID 15565145
  2. [2]0.1% RGN-259 (Thymosin ß4) Ophthalmic Solution Promotes Healing and Improves Comfort in Neurotrophic Keratopathy Patients in a Randomized, Placebo-Controlled, Double-Masked Phase III Clinical TrialInternational Journal of Molecular Sciences, 2022, PMID 36613994
  3. [3]Thymosin β4: a multi-functional regenerative peptide. Basic properties and clinical applicationsExpert Opinion on Biological Therapy, 2012, PMID 22074294
  4. [4]Thymosin beta 4 promotes corneal wound healing and decreases inflammation in vivo following alkali injuryExperimental Eye Research, 2002, PMID 11950239
Evidence maturity
Anecdote
Mechanism
Animal
Early human
Clinical trials
Approved use

Currently sits at Early humanSome early human evidence exists but isn't definitive.

Online hypeLowvsActual evidenceEarlyGapBalanced

Jargon, decoded: · ·

02 · benefits people research this for

Areas this compound is studied or discussed for — not guaranteed effects.

Healing / tissue repair
Evidence: Early human evidence
Status: Research-use-only
Caution: Response, eligibility, and tolerability still vary.
Key facts
  • Thymosin beta-4 (Tβ4) is the full natural actin-binding peptide; the research chemical TB-500 is a synthetic fragment of it.
  • It is studied for tissue repair, corneal/wound healing, and cardiac repair, including some human trials.
Tβ4 vs. TB-500. Tβ4 is the complete natural peptide studied in formal trials; TB-500 is a synthetic fragment sold as a research chemical. Related, not identical.
Safety & status
  • Investigational; not an approved therapy.
  • Human efficacy for popular recovery claims is not established.
03 · evidence receipts

Marketing claim vs what the data actually shows. Tap a row for detail.

Claim audit for Thymosin Beta 4 is in progress — common claims will be checked against sources here. Meanwhile, the real source corpus is in References.

04 · stack fit

Stack fit

Decision clarity: Unknown

Not enough indexed evidence to assess.

Best fitResearch interest in thymic & immune-modulating peptides and angiogenesis & tissue repair.
Not a good fit forAnyone expecting proven human outcomes — the human evidence isn't there yet.
Evidence confidenceMedium
Risk profileUnclear
Regulatory frictionHigh
Hype riskMedium

Stack verdict: Interesting on paper, but not a clinically proven option. The internet narrative is stronger than the human evidence.

Not proven for

Thymosin Beta 4 is not established for:

General anti-aging / longevityHuman injury recoveryMuscle growth or fat loss claimsDisease treatmentAny use as a proven therapy

Tier ranking

D

A weighted evidence score of 40/100 places thymosin-beta-4 in D tier — based on published evidence, not popularity.

Weighted evidence score 40/100

Why not C: held back by human evidence, safety clarity, regulatory clarity, practical relevance.

Why not F: supported by preclinical depth.

What would move it up: Larger controlled human trials, clearer long-term safety, replicated findings, and regulatory progress.

What would move it down: Failed confirmatory trials, new safety signals, or evidence that popular claims don't translate.

Hype vs evidence (shown separately — does not affect the tier)
Internet hype: LowEvidence strength: EarlyRisk of overstatement: Medium
05 · safety / status
Evidence gap alert. Most support comes from animal, cell, or early research — high-quality human clinical evidence is limited.
Regulatory alert. This compound is not FDA-approved for the uses commonly discussed online.
Safety alert. Long-term human safety is not well established. Quality and purity from non-pharmaceutical sources is an additional risk.
Can it legally be used?Research-use-only
EMA / internationalVerify by region
Sport (WADA)Check the current WADA prohibited list
Known side effectsNot well characterized in humans
Biggest unknownsLong-term safety, broad off-label use, rare events
Main cautionResearch-only; human evidence limited; sourcing & purity risk
What we know
  • Thymosin Beta 4 is not FDA-approved for human use; it is discussed in a research context.
  • It belongs to the Thymic & immune-modulating peptides class.
  • Its principal mechanism is characterized in the literature.
What we don't know
  • Whether observed effects reliably translate to humans at large.
  • Long-term safety in healthy users, and full drug-interaction risk.
  • Optimal studied parameters outside any approved indication.
  • Claim-by-claim verdicts — these are authored against verified sources and shown when complete.
  • Quality and purity of material from non-pharmaceutical sources.
Caution if you're researching
Competitive sports (anti-doping)Autoimmune conditionsCancer-related pathwaysResearch-only compoundsDiabetes / glucose regulationPregnancy / fertility

This is not medical advice. These are areas where professional guidance and better evidence matter most.

06 · compare before you decide

See it next to its closest alternatives.

Thymosin Beta 4 vs Thymosin Alpha 1Thymosin Beta 4 vs Tb 500Thymosin Beta 4 vs Ll 37Thymosin Beta 4 vs KpvBuild a comparison →
07 · the read

Full brief

A deeper, chapter-by-chapter research briefing. Tap any chapter to expand.

In this brief
  1. What it is
  2. The Angiogenesis & tissue repair mechanism
  3. The preclinical evidence lane
  4. Why Early, and not higher or lower
  5. Proven lane vs speculative lane
  6. What people report
  7. Regulatory status
  8. What changed recently
01What it is

Simple takeaway: Thymosin Beta 4 is a research compound in the thymic & immune-modulating peptides.

Peptides associated with thymic function and immune signalling, plus antimicrobial host-defense peptides. It is not approved for human use; it is discussed here in a research context only.

02The Angiogenesis & tissue repair mechanism

Simple takeaway: Promoting new blood-vessel formation and repair signalling.

Several repair peptides are studied for effects on angiogenesis (new blood-vessel growth) and tissue/gut protection — largely in animal models. The translation of these repair signals to reliable human benefit remains unproven for most compounds in this group.

What this does not prove. A characterized mechanism explains how an effect could occur — it does not prove the effect reliably occurs in humans.
03The preclinical evidence lane

Simple takeaway: Support is mainly preclinical; 0 registered trials and 0 sources indexed.

The most defensible evidence comes from animal and mechanistic models. Human clinical evidence is limited.

What this does not prove. Preclinical or early-stage evidence does not establish reliable human outcomes.
04Why Early, and not higher or lower

Simple takeaway: Composite maturity 2.3/5.

What holds it back: human evidence, safety clarity, regulatory clarity, practical relevance. What supports its placement: preclinical depth. Stronger human trials, clearer long-term safety data, and regulatory progress would move it up; a safety signal or failure to replicate would move it down.

05Proven lane vs speculative lane

Simple takeaway: The research interest is real; most popular claims remain speculative.

What's supported is the preclinical/mechanistic research. What's speculative is the broad human benefit frequently claimed online, which the indexed human evidence does not establish.

06What people report

Simple takeaway: Community reports are not clinical evidence.

Online reports can surface expectation patterns and possible safety signals, but they are shaped by placebo effects, selection bias, confounders, and uncertain product quality and sourcing. We don't treat anecdotes as proof and we don't publish dosing or protocols.

What this does not prove. Anecdotes cannot establish efficacy or safety.
07Regulatory status

Simple takeaway: Research-use-only

Not approved by the FDA for human use; studied in research contexts. Regulatory status can change and differs by country; several peptides are also prohibited in sport (WADA). Verify current status before relying on it.

08What changed recently

Simple takeaway: No major evidence-changing update was identified in this review window.

The current profile reflects the existing body of indexed evidence. Material changes — new trials, approvals, or safety findings — are noted here when an editor logs them.

0 of 8 brief sections read
08 · community call

How the community sees this vs the evidence.

Your call on D-tier?

Evidence tier is D. Do you agree?

Community votes reflect user perception, not scientific proof — the evidence tier comes from our Research Maturity Index. Aggregate community sentiment will appear here once enough votes are collected.

Aggregate community sentiment will appear here once enough votes are in — we don't show invented numbers.

09 · follow updates
Follow updates on Thymosin Beta 4

Get notified when new studies, safety updates, regulatory changes, or the tier ranking change.

· New human study· Safety update· Regulatory change· Tier change· New claim check
10 · FAQ

FAQs

Is Thymosin Beta 4 FDA-approved?

No. Thymosin Beta 4 is not FDA-approved for the uses commonly discussed online. Not approved by the FDA for human use; studied in research contexts.

What is Thymosin Beta 4 studied for?

Thymosin Beta 4 is studied mainly for healing. Peptides associated with thymic function and immune signalling, plus antimicrobial host-defense peptides.

What does the research say about Thymosin Beta 4?

Mostly animal evidence. Human data is limited; most support comes from preclinical research.

Is Thymosin Beta 4 safe?

Long-term human safety is not well established for Thymosin Beta 4. Quality and purity from non-pharmaceutical sources is an added risk.

🧮 Reconstitution calculator (educational)

Educational reconstitution math from your own values — not medical advice or a dose recommendation. Open the full calculator →

Medication (optional — 30+ in library)
Peptide in vial (mg)
Reconstitution water (mL)
Target amount per draw
Syringe
Draw to
10
units
Volume to draw
0.1
mL
At this amount
20
draws / vial
After one draw
4.75
mg left
Syringe · draw to 10 of 100 units
0
10
20
30
40
50
60
70
80
90
100

Each unit on a 100u · 1.0 mL syringe ≈ 25 mcg of this solution.

Concentration
2.5
mg / mL
Concentration
2,500
mcg / mL
Per U-100 unit
25
mcg / unit
Show the math
5 mg × 1000 = 5,000 mcg in the vial
2 mL × 100 = 200 U-100 units of liquid
5,000 mcg ÷ 200 units = 25 mcg per unit
250 mcg ÷ 25 mcg/unit = 10 units
10 units ÷ 100 = 0.1 mL
5,000 mcg ÷ 250 mcg = 20 draws per vial
Compare reconstitution volumes (5mg vial)
Water
mcg / unit
units for 250mcg
1 mL505
2 mL2510
2.5 mL2012.5
3 mL16.6715
5 mL1025

More water → lower concentration → more units for the same amount.

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Keep exploring
Compare nextThymosin Beta 4 vs Thymosin Alpha 1See the evidence side by side.Outcome pathHealing / tissue repairWhere Thymosin Beta 4 sits vs. the alternatives.ToolConcentration calculatorHow vial size & water change concentration.
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Class
Thymic & immune-modulating peptides
Mechanisms
Researched for
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