(๐Ÿ’ช Rapid muscle gain) Receptor Grade IGF-1 LR3 (100mcg) - Biotech Peptides

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Description

๐Ÿงฌ What is IGF-1 LR3?

IGF-1 LR3 (Long R3 IGF-1) is a modified version of IGF-1:

Its characteristics include:

Extended half-life (longer than natural IGF-1)
Stronger receptor binding affinity
Higher biological activity

โ€œReceptor Gradeโ€ is typically a marketing term meaning:
๐Ÿ‘‰ โ€œHigh-purity / strong receptor-binding versionโ€ (though not an official medical classification)

๐Ÿ’ช Why Does the Fitness Community Consider It โ€œPowerfulโ€?

Its core mechanism of action is:

โžก๏ธ Enhances cellular uptake of glucose and amino acids
โžก๏ธ Promotes protein synthesis
โžก๏ธ Accelerates muscle recovery

Therefore, it is marketed for:

๐Ÿ”ฅ Rapid muscle gain
๐Ÿ’ช Powerful recovery capabilities
๐Ÿ“ˆ Improved nutrient utilization efficiency
๐Ÿฉน Accelerated post-workout repair
๐Ÿง  Its relationship with GH (Growth Hormone)

Many people misunderstand:

HGH ย  ย IGF-1 LR3
Upstream hormone ย  ย Downstream signaling factor
Stimulates the liver to produce IGF-1 ย  ย Acts directly on tissues
Indirect action ย  ย More direct cellular action

๐Ÿ‘‰ Simply put:
GH is the โ€œconductor,โ€ and IGF-1 is the โ€œperformer.โ€

โšก What makes โ€œLR3โ€ special?

After modification, LR3:

Has a longer half-life (around 20+ hours)
Is less susceptible to inhibition by IGF-binding protein
Penetrates tissues more easily to exert its effects

Therefore, it is more โ€œpotentโ€ than natural IGF-1.

๐Ÿ’ช Common User Feedback (from forums)

Common observations in the fitness community:

Enhanced muscle โ€œfullnessโ€
Faster recovery
Stronger post-workout pump
Rapid weight gain (water/glycogen)
Improved nutrient utilization


Receptor Grade IGF-1 LR3 Peptide

Receptor Grade IGF-1 LR3 peptide is a research reagent examined in studies on cellular growth, IGF receptors, and IGF binding proteins. It contains an extended N-terminal structure of 13 amino acids and a replacement of the glutamic acid at residue 3. Additionally, the addition of arginine in the original sequence of recombinant IGF-1 (rhIGF-1), which ultimately leads to the formation of an 83 amino acid peptide. Hence, it is named IGF-1 Long R3.[1,2] It appears to be potentially more influential on cellular activities than rhIGF-1 due to an apparent significant improvement in its biological activity. This is since it exhibits a stronger affinity for the IGF receptor and lower affinity towards other proteins that may inactivate it. Moreover, the classification of Receptor Grade refers to the purity of the material, which is considered higher than the standard Media Grade IGF-1 LR3. Media grate IGF-1 LR3 is routinely studied in cell cultures and as a research reagent, at an economical cost, for studies where biological potency is not crucial. Receptor Grade IGF-1 LR3 is considered the reagent of choice to achieve optimum results when performing any animal study and cell-based assays. Growth of mammalian cells in the presence of low concentrations of Long R3 IGF-1 appears to result in better productivity than standard concentrations of insulin and/or standard IGF-1.[1] Researchers report that the peptide exhibited โ€œequivalent or better performance using two recombinant CHO cell lines.โ€ IGF-1 LR3 may be more capable of inducing the type 1 IGF receptor, potentially promoting an elevated level of intracellular signaling, cellular proliferation, and apoptosis inhibition.

Specifications

Molecular Formula: C400H625N111O115S9

Molecular Weight: 9117.5 g/mol

Sequence: MFPAMPLSSL FVNGPRTLCG AELVDALQFV CGDRGFYFNK PTGYGSSSRR APQTGIVDEC CFRSCDLRRL EMYCAPLKPA KSA

Receptor Grade IGF-1 LR3 Research

Receptor Grade IGF-1 LR3 and Biological Activity
The peptide appears to bring about a more pronounced but short-lived impact than IGF-1 through a potential resistance in the association of inactivating proteins such as IGF binding proteins (IGFBPs).[2] Insulin-like Growth Factor Binding Proteins (IGFBPs) are a category of proteins that may regulate the availability of Insulin-like Growth Factors (IGFs) within the bloodstream, possibly influencing their interactions with various tissues. It is conceivable that a decrease in the binding affinity of IGF-1 LR3 for IGFBPs might affect its bioavailability, potentially reducing its duration of action. Additionally, this weakened binding might alter how IGF-1 LR3 engages with targeted tissues in experimental settings. These changes could potentially enhance the potency of IGF-1 LR3, although possibly shortening its active duration. This suggests that the interactions between IGF-1 LR3 and IGFBPs might determine the functional outcomes of IGF-1 LR3 in specific experimental contexts. Consequently, this may result in IGF-1 LR3 being more potent but with a shorter duration of action compared to recombinant Insulin-like Growth Factor 1 (rhIGF-1). Studies in murine models indicate that IGF-1 LR3 may be cleared from the plasma faster, to be destributed more quickly into various tissue models as compared to IGF-1.[3] The investigation into the tissue distribution patterns of IGF-1 LR3 suggested it might localize differently from IGF-1. Notably, elevated levels of IGF-1 LR3 were observed in specific tissues, including the kidneys, ovaries, and adrenal glands in murine models. [1] This distinct localization pattern implies that organs primarily involved in metabolic and reproductive functions might have different abilities to absorb or retain IGF-1 LR3 compared to IGF-1. It is speculated that these observed differences might be due to IGF-1 LR3's reduced tendency to bind with IGF-binding proteins (IGFBPs). This reduced binding may affect its bioavailability and interactions with target tissues in experimental models. However, there is a hypothesis that a peptide with similar modifications, specifically the R3 modification found in IGF-1 LR3, may possess greater anabolic potential than regular IGF-1 despite a shorter duration of action. Further research is necessary to understand these mechanisms and their implications fully.[4]

Receptor Grade IGF-1 LR3 and Insulin-Like Growth Factor Receptor Interactions
Naturally produced IGF-1 hormones interact with at least two cell surface receptors: the IGF-1 receptor (IGF-1R) and the insulin receptor.[5] The researchers also note that โ€œIR and IGF1R act as identical portals to the regulation of gene expression, with differences between insulin and IGF-1 effects due to a modulation of the amplitude of the signal created by the specific ligand-receptor interaction.โ€ The IGF-1R is referred to as the โ€œphysiologicโ€ receptor due to its potential higher affinity (approximately 100 times higher) for IGF-1 as compared to the insulin receptor. The association of IGF-1 and IGF-1R apparently leads to changes in metabolism, prevention of cell death (apoptosis), promotion of cell growth (hypertrophy), differentiation and cell division (hyperplasia), normal development, and even malignant growth. IGF-1R has been researched for its involvement in diverse types of cancer, such as prostate, breast, and lung cancer.[6] IGF-1 also appears to stimulate insulin receptors and activate them, thereby promoting glucose uptake from the bloodstream by cells. IGF-1 displays a three-fold influence on muscle cells.

Receptor Grade IGF-1 LR3 and Muscle Cells
Preliminary research utilizing murine models suggests that IGF-1 LR3 might have significant anabolic (muscle-building) actions. Specifically, a study examined its impact on both normal mice and those experiencing catabolic (muscle-wasting) conditions induced by dexamethasone, a synthetic steroid.[7] The researchers noted that IGF-1 LR3 appeared to be roughly 2.5 times more potent than regular IGF-1 in producing anabolic actions. These observed actions included weight gain, an increase in the weight of internal organs (visceral organs), and possibly improved efficiency in converting feed into body mass. These findings were noted when the murine models were subjected to continuous exposure to IGF-1 LR3. Unfortunately, there are no studies investigating the direct potential of IGF-1 LR3 on muscle cells. Considering the similaritied between the two peptides, IGF-1 LR3 is expected to have similar actions on muscle cells as IGF-1.

Based on research, studies posit that IGF-1 may promote an increase in the number of muscle cells, also known as hyperplasia. Secondly, IGF-1 appears to influence the lifespan of satellite cells of the skeletal muscles.[8] Satellite cells appear to provide nutritional support to muscle cells, helping them to operate efficiently. IGF-1 may help to build muscle tissue by improving the lifespan of these cells. Finally, IGF-1 appears to promote the differentiation of myoblasts.[9] In other words, it may encourage the commitment of stem cell progeny from non-specific pluripotent stem cells to dedicated muscle tissue. To conclude, IGF-1 may improve muscle development by enhancing the rate at which generic stem cells are transformed into muscle cells.

Disclaimer: The products mentioned are not intended for human or animal consumption. Research chemicals are intended solely for laboratory experimentation and/or in-vitro testing. Bodily introduction of any sort is strictly prohibited by law. All purchases are limited to licensed researchers and/or qualified professionals. All information shared in this article is for educational purposes only.

ย 

References

  1. Thomas, James N., and Victor Fung. โ€œComparison of long R3 IGF-1 with insulin in the support of cell growth and recombinant protein expression in CHO cells.โ€ Animal Cell Technology. Butterworth-Heinemann, 1994. 91-95.
  2. Assefa, Biruhalem, et al. โ€œInsulin-like growth factor (IGF) binding protein-2, independently of IGF-1, induces GLUT-4 translocation and glucose uptake in 3T3-L1 adipocytes.โ€ Oxidative Medicine and Cellular Longevity 2017 (2017).
  3. Bastian SE, Walton PE, Wallace JC, Ballard FJ. Plasma clearance and tissue distribution of labelled insulin-like growth factor-I (IGF-I) and an analogue LR3IGF-I in pregnant rats. J Endocrinol. 1993 Aug;138(2):327-36. . PMID: 7693845.
  4. Elis S, Wu Y, Courtland HW, Cannata D, Sun H, Beth-On M, Liu C, Jasper H, Domenรฉ H, Karabatas L, Guida C, Basta-Pljakic J, Cardoso L, Rosen CJ, Frystyk J, Yakar S. Unbound (bioavailable) IGF1 enhances somatic growth. Dis Model Mech. 2011 Sep;4(5):649-58. . Epub 2011 May 31. PMID: 21628395; PMCID: PMC3180229.
  5. Boucher J, Tseng YH, Kahn CR. Insulin and insulin-like growth factor-1 receptors act as ligand-specific amplitude modulators of a common pathway regulating gene transcription. J Biol Chem. 2010 May 28;285(22):17235-45. . Epub 2010 Apr 1. PMID: 20360006; PMCID: PMC2878077.
  6. Shanmugalingam T, Bosco C, Ridley AJ, Van Hemelrijck M. Is there a role for IGF-1 in the development of second primary cancers? Cancer Med. 2016 Nov;5(11):3353-3367. . Epub 2016 Oct 13. PMID: 27734632; PMCID: PMC5119990.
  7. Tomas, F. M., Knowles, S. E., Owens, P. C., Chandler, C. S., Francis, G. L., Read, L. C., & Ballard, F. J. (1992). Insulin-like growth factor-I (IGF-I) and especially IGF-I variants are anabolic in dexamethasone-treated rats. The Biochemical journal, 282 ( Pt 1)(Pt 1), 91โ€“97.
  8. Yoshida T, Delafontaine P. Mechanisms of IGF-1-Mediated Regulation of Skeletal Muscle Hypertrophy and Atrophy. Cells. 2020 Aug 26;9(9):1970. . PMID: 32858949; PMCID: PMC7564605.
  9. Aboalola D, Han VKM. Different Effects of Insulin-Like Growth Factor-1 and Insulin-Like Growth Factor-2 on Myogenic Differentiation of Human Mesenchymal Stem Cells. Stem Cells Int. 2017;2017:8286248. . Epub 2017 Dec 14. PMID: 29387091; PMCID: PMC5745708.
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This product is strictly for research/laboratory use only. Human or animal use and/or consumption is strictly prohibited by law. Only qualified and licensed professionals should handle these products. Any information found on Biotech Peptides is strictly for educational purposes only. Refer to our for more details.


Dr. Usman (BSc, MBBS, MaRCP) completed his studies in medicine at the Royal College of Physicians, London. He is an avid researcher with more than 30 publications in internationally recognized peer-reviewed journals. Dr. Usman has worked as a researcher and a medical consultant for reputable pharmaceutical companies such as Johnson & Johnson and Sanofi.

Real Customer Reviews of Weight Loss Peptide

๐Ÿ”ฅ Real Customer Reviews of Weight Loss Peptide

๐Ÿ”ฅ Finally something that ACTUALLY works
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๐Ÿ• I stopped thinking about snacks 24/7
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๐Ÿ‘– Lost my baby weight faster than expected
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๐Ÿ‹๏ธ Lost fat without losing muscle
I wanted something to control cravings while staying lean in the gym. After 2 months my waist is down, abs are visible again, and workouts still feel strong.
๐Ÿฅน I finally feel in control again
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โ“ Frequently Asked Questions

Everything you need to know before getting started โœจ

Most customers report noticeable appetite control within the first 1โ€“2 weeks. Visible weight loss results are commonly seen within 4โ€“8 weeks depending on lifestyle, consistency, and metabolism.

One of the biggest benefits customers mention is reduced cravings and feeling full longer after meals. Many users naturally eat smaller portions without feeling deprived.

Most users describe the process as quick and manageable. The needles used are extremely small and designed for comfort and convenience at home.

Unlike traditional diet pills that rely on stimulants, peptide-based support is designed to help regulate appetite and eating behavior more naturally without the crash or jittery feeling.

Many of our customers felt frustrated after years of failed diets, supplements, and workout plans. This has helped users finally stay consistent by making portion control and cravings easier to manage.

Orders are typically processed within 24โ€“48 hours. Delivery times vary by country, but most customers receive their package within 5โ€“10 business days.

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