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Return to: HGH/ IGF1/ SLIN & Peptides |
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#Post#: 6214-------------------------------------------------- |
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The Difference Between (ZPHC, CP, Spectrum) Vs Unlabeled HGH ? |
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Half Life Increased |
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By: Road2HardCoreIron Date: July 19, 2025, 9:33 pm |
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ZPHC, Canadalab, and Spectrum half-life. Half is increased up to |
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58 days once mixed. However, the bac water will start to lose |
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its potency after 28 days. It should be swapped for a new bac |
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water after 28 days. This process increases the release of hGH |
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in your system. Only top-of-the-line peptides are made using |
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this method. This is why they proudly produce such high dosages |
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of HGH. Anyone interested in trying these products should seek a |
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licensed doctor. Get your lab work and learn about what you are |
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prescribed. What products are included in the medication? The |
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pros and cons. I'm not a doctor. Nor do we offer this |
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medication. We are just messengers to ensure you make wise |
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decisions. |
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(Big Ronnie Coleman's recent issues with Sepsis) Should be |
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aware of and care about what goes into our bodies. Whether it |
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be due to back surgeries or other things. Everyone should know |
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we are allowing in our bodies and how and where it is produced. |
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Long-acting forms of growth hormone-releasing hormone and growth |
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hormone: effects in normal volunteers and adults with growth |
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hormone deficiency |
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David R Clemmons 1 |
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Background: Growth hormone (GH) replacement therapy in adults |
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and children has found broad acceptance by endocrinologists and |
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patients, but the need for daily injections remains a |
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significant barrier to more widespread use. LONG-ACTING |
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FORMULATIONS: Several approaches have been taken to develop |
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long-acting forms of GH and to extend the half-life of |
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GH-releasing factor. Each of these preparations has been tested |
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in experimental animal models and found to extend the half-life |
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of GH and GH-releasing hormone (GHRH) and to increase mean daily |
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GH levels. Frequent sampling following administration of |
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long-acting GHRH showed that the greatest increases occurred in |
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trough GH levels, which increased 7.8-fold. The extended GH |
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half-life and increased trough levels resulted in increases in |
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insulin-like growth factor I (IGF-I) levels, which increased |
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1.4- to 4.1-fold and extended the duration of the IGF-I increase |
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from 7 to 14 days. These increases in GH and IGF-I levels allow |
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these compounds to be administered much less frequently, and |
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several studies have shown that IGF-I levels can be maintained |
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in a therapeutically effective range with much less frequent GH |
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administration. |
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Safety: Complications other than those generally associated with |
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GH therapy include nodule formation and lipoatrophy at the |
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injection sites. One long-term study of a long-acting |
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formulation demonstrated that growth could be effectively |
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stimulated in GH-deficient children, but that the peak growth |
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velocity was only about 80% of that seen following daily |
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subcutaneous GH injections. Subcutaneous nodule formation in |
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some patients may have contributed to noncompliance and thus to |
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the difference in growth velocity. |
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Conclusions: Different types of GH and GHRH formulations have |
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been developed with extended half-lives. In general, these |
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preparations are pharmacokinetically and pharmacodynamically |
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effective, extend GH half-lives with longer sustained elevation |
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of IGF-I and permit much less frequent GH administration. Thus, |
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it may be possible to develop a therapeutically effective form |
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of GH for use in long-term treatment. The precise efficacy and |
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safety assessments to use in monitoring long-term GH |
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administration have not been definitively established. |
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