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Peptide Thymosin Beta 4

dragonfire101

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Anybody look into Thymosin Beta 4 yet. It can protect and regenerate damaged tissues of all sorts.

This would be excellent for a wide variety of bodybuilding needs such as helping prevent myocardial-infarction, improve tendon-muscle repair, nerve regeneration, and improve hair growth for us who don't like the shaved look.

It been around for at least 10 years just wondering why nothing ever came from it.
 
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Anybody look into Thymosin Beta 4 yet. It can protect and regenerate damaged tissues of all sorts.

This would be excellent for a wide variety of bodybuilding needs such as helping prevent myocardial-infarction, improve tendon-muscle repair, nerve regeneration, and improve hair growth for us who don't like the shaved look.

It been around for at least 10 years just wondering why nothing ever came from it.

Any studies you can point me to? I would like to read more about this.
 
Nice find, DF! Here's some reading:

Biological activities of thymosin β4
The archetypical β-thymosin is β4 (product in humans of the TMSB4X gene), which is a major cellular constituent in many tissues. Its intracellular concentration may reach as high as 0.5 mM.[13] Following Thymosin α1, β4 was the second of the biologically active peptides from Thymosin Fraction 5 to be completely sequenced and synthesized.[14]

[edit]Actin binding
Thymosin β4 was initially perceived as a thymic hormone. However this changed when it was discovered that it forms a 1:1 complex with G (globular) actin, and is present at high concentration in a wide range of mammalian cell types.[15] When appropriate, G-actin monomers polymerize to form F (filamentous) actin which together with other proteins that bind to actin comprise cellular microfilaments. Formation by G-actin of the complex with β-thymosin (= "sequestration") opposes this.

Due to its profusion in the cytosol and its ability to bind G-actin but not F-actin, thymosin β4 is regarded as the principal actin-sequestering protein in many cell types. Thymosin β4 functions like a buffer for monomeric actin as represented in the following reaction:[16]

F-actin ↔ G-actin + Thymosin β4 ↔ G-actin/Thymosin β4

Release of G-actin monomers from thymosin β4 occurs as part of the mechanism that drives actin polymerization in the normal function of the cytoskeleton in cell morphology and cell motility.

The sequence lkktet, which starts at residue 17 of the 43-aminoacid sequence of thymosin beta-4, and is strongly conserved between all β-thymosins, together with a similar sequence in WH2 domains, is frequently referred to as "the actin-binding motif" of these proteins, although modelling based on X-ray crystallography has shown that essentially the entire length of the β-thymosin sequence interacts with actin in the actin-thymosin complex.[17]

[edit]"Moonlighting"
In addition to its intracellular role as the major actin-sequestering molecule in cells of many multicellular animals, thymosin β4 shows a remarkably diverse range of effects when present in the fluid surrounding animal tissue cells. Taken together, these effects suggest that thymosin has a general role in tissue regeneration. This has suggested a variety of possible therapeutic applications, and several have now been extended to animal models and human clinical trials.

It is considered unlikely that thymosin β4 exerts all these effects via intracellular sequestration of G-actin. This would require its uptake by cells, and moreover, in most cases the cells affected already have substantial intracellular concentrations.

The diverse activities related to tissue repair may depend on interactions with receptors quite distinct from actin and possessing extracellular ligand-binding domains. Such multi-tasking by, or "partner promiscuity" of, proteins has been referred to as protein moonlighting.[18] Proteins such as thymosins which lack stable folded structure in aqueous solution, are known as intrinsically unstructured proteins (IUPs). Because IUPs acquire specific folded structures only on binding to their partner proteins, they offer special possibilities for interaction with multiple partners.[19] A candidate extracellular receptor of high affinity for thymosin β4 is the β subunit of cell surface-located ATP synthase, which would allow extracellular thymosin to signal via a purinergic receptor.[20]

Some of the multiple activities of thymosin β4 unrelated to actin may be mediated by a tetrapeptide enzymically-cleaved from its N-terminus, N-acetyl-ser-asp-lys-pro, brand names Seraspenide or Goralatide, best known as an inhibitor of the proliferation of haematopoietic (blood-cell precursor) stem cells of bone marrow.

[edit]Tissue regeneration
Work with cell cultures and experiments with animals have shown that administration of thymosin β4 can promote migration of cells, formation of blood vessels, maturation of stem cells, survival of various cell types and lowering of the production of pro-inflammatory cytokines. These multiple properties have provided the impetus for a world-wide series of on-going clinical trials of potential effectiveness of thymosin β4 in promoting repair of wounds in skin, cornea and heart.[21]

Such tissue-regenerating properties of thymosin β4 may ultimately contribute to repair of human heart muscle damaged by heart disease and heart attack. In mice, administration of thymosin β4 has been shown to stimulate formation of new heart muscle cells from otherwise inactive precursor cells present in the outer lining of adult hearts,[22] to induce migration of these cells into heart muscle[23] and recruit new blood vessels within the muscle.[24]

[edit]Anti-inflammatory role for sulfoxide
In 1999 researchers in Glasgow University found that an oxidised derivative of thymosin β4 (the sulfoxide, in which an oxygen atom is added to the methionine near the N-terminus) exerted several potentially anti-inflammatory effects on neutrophil leucocytes. It promoted their dispersion from a focus, inhibited their response to a small peptide (F-Met-Leu-Phe) which attracts them to sites of bacterial infection and lowered their adhesion to endothelial cells. (Adhesion to endothelial cells of blood vessel walls is pre-requisite for these cells to leave the bloodstream and invade infected tissue). A possible anti-inflammatory role for the β4 sulfoxide was supported by the group's finding that it counteracted artificially-induced inflammation in mice.

The group had first identified the thymosin sulfoxide as an active factor in culture fluid of cells responding to treatment with a steroid hormone, suggesting that its formation might form part of the mechanism by which steroids exert anti-inflammatory effects. Extracellular thymosin β4 would be readily oxidised to the sulfoxide in vivo at sites of inflammation, by the respiratory burst.[25]

[edit]Terminal deoxynucleotidyl transferase
Thymosin β4 induces the activity of the enzyme terminal deoxynucleotidyl transferase in populations of thymocytes (thymus-derived lymphocytes). This suggests that the peptide may contribute to the maturation of these cells.[14]

[edit]Clinical applications
Thymosin β4 is currently in multicenter trials in the United States and Europe in patients with bed sores, ulcers caused by venostasis, and Epidermolysis bullosa simplex. It is also about to enter clinical trials in diabetic patients who have been subjected to vitrectomy and in patients who have experienced heart attacks (myocardial infarction).

Levels of human thymosin β15 in urine have shown promise as a diagnostic marker for prostate cancer which is sensitive to potential aggressivenes of the tumour [26]
 
thank you for posting that bionic.
 
My pleasure, Tom.


The group had first identified the thymosin sulfoxide as an active factor in culture fluid of cells responding to treatment with a steroid hormone, suggesting that its formation might form part of the mechanism by which steroids exert anti-inflammatory effects. Extracellular thymosin β4 would be readily oxidised to the sulfoxide in vivo at sites of inflammation, by the respiratory burst.[25]

This quote (at least in my simple mind) shows that people who use steroids may already be benefitting from this peptide.
 
Last edited:
Ann N Y Acad Sci. 2007 Sep;1112:161-70. Epub 2007 Jun 28.
Thymosin beta4 is cardioprotective after myocardial infarction.
Srivastava D, Saxena A, Michael Dimaio J, Bock-Marquette I.
Source

Gladstone Institute of Cardiovascular Disease, 1650 Owens Street, San Francisco, CA 94158, USA. [email protected]
Abstract

Heart disease is a leading cause of death in newborns and in adults. Efforts to promote cardiac repair by introduction or recruitment of exogenous stem cells hold promise but typically involve isolation and introduction of autologous or donor progenitor cells. We have found that the G-actin-sequestering peptide thymosin beta4 promotes myocardial and endothelial cell migration in the embryonic heart and retains this property in postnatal cardiomyocytes. Survival of embryonic and postnatal cardiomyocytes in culture was also enhanced by thymosin beta4. We found that thymosin beta4 formed a functional complex with PINCH and integrin-linked kinase (ILK), resulting in activation of the survival kinase Akt/PKB, which was necessary for thymosin beta4's effects on cardiomyocytes. After coronary artery ligation in mice, thymosin beta4 treatment resulted in upregulation of ILK and Akt activity in the heart, enhanced early myocyte survival, and improved cardiac function. These findings suggest that thymosin beta4 promotes cardiomyocyte and endothelial migration, survival, and repair and may be a novel therapeutic target in the setting of acute myocardial damage.
 
Ann N Y Acad Sci. 2010 Apr;1194:105-11.

Thymosin beta4: a key factor for protective effects of eEPCs in acute and chronic ischemia.

Hinkel R, Bock-Marquette I, Hatzopoulos AK, Kupatt C.
Source

Internal Medicine I, Klinikum Grosshadern, Ludwig Maximilians University, Munich, Germany.
Erratum in

Ann N Y Acad Sci. 2010 Sep;1205(1):284. Hazopoulos, Antonis K [corrected to Hatzopoulos, Antonis K].

Abstract

Acute myocardial infarction is still one of the leading causes of death in the industrial nations. Even after successful revascularization, myocardial ischemia results in a loss of cardiomyocytes and scar formation. Embryonic EPCs (eEPCs), retroinfused into the ischemic region of the pig heart, provided rapid paracrine benefit to acute and chronic ischemia in a PI-3K/Akt-dependent manner. In a model of acute myocardial ischemia, infarct size and loss of regional myocardial function decreased after eEPC application, unless cell pre-treatment with thymosin beta4 shRNA was performed. Thymosin beta4 peptide retroinfusion mimicked the eEPC-derived improvement of infarct size and myocardial function. In chronic ischemia (rabbit model), eEPCs retroinfused into the ischemic hindlimb enhanced capillary density, collateral growth, and perfusion. Therapeutic neovascularization was absent when thymosin beta4 shRNA was introduced into eEPCs before application. In conclusion, eEPCs are capable of acute and chronic ischemia protection in a thymosin beta4 dependent manner.

PMID:
20536456
[PubMed - indexed for MEDLINE]
 
Over-expression of thymosin beta 4 promotes abnormal tooth development and stimulation of hair growth.

Int J Dev Biol. 2010;54(1):135-40.
Over-expression of thymosin beta 4 promotes abnormal tooth development and stimulation of hair growth.

Cha HJ, Philp D, Lee SH, Moon HS, Kleinman HK, Nakamura T.

Department of Parasitology and Genetics, College of Medicine, Kosin University, Busan, South Korea. [email protected]

Thymosin beta 4 has multi-functional roles in cell physiology. It accelerates wound healing, hair growth and angiogenesis, and increases laminin-5 expression in corneal epithelium. Furthermore, thymosin beta 4 stimulates tumor growth and metastasis by induction of cell migration and vascular endothelial growth factor-mediated angiogenesis. Using a construct on the skin-specific keratin-5 promoter, we have developed thymosin beta 4 over-expressing transgenic mice to further study its functional roles. Thymosin beta 4 in adult skin and in embryonic stages of the transgenic mouse was analyzed by both Western blot and immunohistochemistry. The over-expression of thymosin beta 4 was observed especially around hair follicles and in the teeth in the transgenic mice. We examined the phenotype of the thymosin beta 4 over-expressing mice. Hair growth was accelerated. In addition, the transgenic mice had abnormally-shaped white teeth and dull incisors. We found that the expression of laminin-5 was up-regulated in the skin of the transgenic mice. We conclude that thymosin beta 4 has an important physiological role in hair growth and in tooth development.

__
 
Ann N Y Acad Sci. 2010 Apr;1194:118-24.
Thymosin beta4 enhances repair by organizing connective tissue and preventing the appearance of myofibroblasts.
Ehrlich HP, Hazard SW 3rd.
Source

Division of Plastic Surgery, Pennsylvania State University College of Medicine, Hershey, Pennsylvania, USA. [email protected]
Abstract

Incisional wounds in rats treated locally with thymosin beta4 (Tbeta4) healed with minimal scaring and without loss in wound breaking strength. Treated wounds were significantly narrower in width. Polarized light microscopy treated wounds had superior organized collagen fibers, displaying a red birefringence, which is consistent with mature connective tissue. Control incisions had randomly organized collagen fibers, displaying green birefringence that is consistent with immature connective tissue. Immunohistology treated wounds had few myofibroblasts and fibroblasts with alpha smooth muscle actin (SMA) stained stress fibers. Polyvinyl alcohol sponge implants placed in subcutaneous pockets received either carrier or 100 microg of Tbeta4 on days 2, 3, and 4. On day 14, treated implants revealed longer, thicker collagen fiber bundles with intense yellow-red birefringence by polarized light microscopy. In controls, fine, thin collagen fiber bundles were arranged in random arrays with predominantly green birefringence. Controls contained mostly myofibroblasts, while few myofibroblasts appeared in Tbeta4 treated implants. Electron microscopy confirmed both cell types and the degree of collagen fiber bundle organization. Our results demonstrate that Tbeta4 treated wounds appear to mature earlier and heal with minimal scaring.

PMID:
20536458
[PubMed - indexed for MEDLINE]
 
J Biochem. 2011 Jan;149(1):43-8. Epub 2010 Sep 29.
Muscle injury-induced thymosin β4 acts as a chemoattractant for myoblasts.
Tokura Y, Nakayama Y, Fukada S, Nara N, Yamamoto H, Matsuda R, Hara T.
Source

Stem Cell Project Group, The Tokyo Metropolitan Institute of Medical Science, Tokyo Metropolitan Organization for Medical Research, 2-1-6 Kamikitazawa, Setagaya-ku, Tokyo 156-8506, Japan.
Abstract

Thymosin β4 (Tβ4) is a major intracellular G-actin-sequestering peptide. There is increasing evidence to support important extracellular functions of Tβ4 related to angiogenesis, wound healing and cardiovascular regeneration. We investigated the expression of 'Tβ4' and 'thymosin β10', a closely related peptide, during skeletal muscle regeneration in mice and chemotactic responses of myoblasts to these peptides. The mRNA levels of 'Tβ4' and 'thymosin β10' were up-regulated in the early stage of regenerating muscle fibres and inflammatory haematopoietic cells in the injured skeletal muscles of mice. We found that both Tβ4 and its sulphoxized form significantly accelerated wound closure and increased the chemotaxis of C2C12 myoblastic cells. Furthermore, we showed that primary myoblasts and myocytes derived from muscle satellite cells of adult mice were chemoattracted to sulphoxized form of Tβ4. These data indicate that muscle injury enhances the local production of Tβ4, thereby promoting the migration of myoblasts to facilitate skeletal muscle regeneration.

PMID:
20880960
[PubMed - indexed for MEDLINE]
 
Thymosin Beta 4 review

Hi guys , I'am new to the forum .I was looking for feedback on Thymosin beta 4 .

Especially on strength and muscle mass.Not interested so much into healing aspect .Seems like most people report only healing aspectand not on strength and mass. .I feel great .I'am natural bodybuilder, Roids free . Only use Ipamorelin natural peptide very conservative amount of 100 mg twice a day .

I just ordered Thymosin beta 4 10 mg / 7 vials .

My statistics .

6 feet tall
220
arms - 18 "
bench press max - 485 Raw
9% body fat

I train mostly upper body . Maybe I"am just a half bodybuilder, LOL

I will be taking 10 mg every week for 6 weeks , then 1 a month if effective


It is very pricey .This is why I thought my brothers in iron deserve honest no BS review .

I'll inform you on my strength improvements and size .
 
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this kills my all the time!!!! some smuck claiming to be natural but yet will take anything other than steroids and thinks he is natural!!!! can you tell me how the hell are you natural?

natural means you take nothing!!!! so if you cant do what you're doing with just food then you arent natural!!!!






Hi guys , I'am new to the forum .I was looking for feedback on Thymosin beta 4 .

Especially on strength and muscle mass.Not interested so much into healing aspect .Seems like most people report only healing aspectand not on strength and mass. .I feel great .I'am natural bodybuilder, Roids free . Only use Ipamorelin natural peptide very conservative amount of 100 mg twice a day .

I just ordered Thymosin beta 4 10 mg / 7 vials .

My statistics .

6 feet tall
220
arms - 18 "
bench press max - 485 Raw
9% body fat

I train mostly upper body . Maybe I"am just a half bodybuilder, LOL

I will be taking 10 mg every week for 6 weeks , then 1 a month if effective


It is very pricey .This is why I thought my brothers in iron deserve honest no BS review .

I'll inform you on my strength improvements and size .
 
If it was so damn awesome, don't you think it would cost more than what it does?
 
I'm sorry Phil. I'm just feeling a little "down" on myself and my lack of progress today.


You have been here a while, dont you think you should be bigger than you are now? What does price have to do with anything?
 
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sounds good, and so far the logs show some benefits... but IMO not worth any possible risk.
 

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