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Test Suspension Cycle Info
Test Suspension is the most powerful water based oral testosterone stimulating preparation commercially “available”. Many users report of dramatic muscle growth, hardness, increased strength, improved mood and enhanced energy levels. Test Suspension contains the active ingredient of Supratestin Depot™, which is a refined proprietary composite of pro-testosterone agents that may greatly promote heightened testosterone blood levels after oral administration. Use of omifen at the cycles completion is recommended to restore the hypothalmic/testicular axis to normal levels.
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Muscle gains with “suspension” are being reported unusually high yet extremely solid. Suspension has virtually no capacity to aromitize into estrogen, which may prevent side effects such as water retention and bloating. Suspension has an extremely high affinity to bind to multiple types of myocytic steroid receptors. Due to this action, strength increases are reported extraordinary. Powerlifters and strength athletes seeking higher lifting totals may optimally use Test Suspension in their cycles. Needless to say, many lifting records may be broken as a result of using of this product.
Suspension has a special applicator, which is used to draw out the desired dose. It is orally administered and held in the mouth for 60-180 seconds before swallowing. This specialized oral infusion testosterone assimilation system enhances absorption and will promote enhanced digestion to a large degree. This product pushes the boundaries of OTC performance enhancement technology with its incredible ergogenic efficacy and delivery method. Test Suspension is an extremely potent and highly recommended multi-purpose anabolic agent.
Testosterone suspension
Testosterone suspension is an injectable preparation containing testosterone (no ester), usually in a water base. Among bodybuilders, “suspension” is known to be an extremely potent mass agent. It is often said to be the most powerful injectable steroid available, producing very rapid muscle mass and strength. This is largely due to the swift action of the drug. When using a slow-acting oil-based steroid-like Sustanon® 250, it can take weeks before a peak testosterone level is reached. With the suspension, it is just a matter of hours. This will usually result in the athlete starting to notice size and strength gains by the end of the first week. By the time the athlete is 30 days into a suspension cycle, the length it will usually take for Sustanon® 250 to really begin working consistently, the mass gains are already (generally) very extreme.
Testosterone suspension Uses
Testosterone suspension is available in select human and veterinary drug markets. Composition and dosage may vary by country and manufacturer but usually contain 50 mg/ml or 100 mg/ml of steroid mixed in a water-based solution. Testosterone has low water solubility, so the steroid will noticeably separate from a water-based solution when a vial or ampule is left to sit. A quick shake will temporarily place the drug back into suspension so that the withdrawn dosage should always be consistent.
Structural Characteristics
Testosterone suspension contains (free) testosterone in a water-based suspension, although oils are sometimes also used as carriers. Without esterification, testosterone has a short half-life in the body. Testosterone suspension may require a minimum of 2-3 injections per week to maintain consistent hormone elevations. When calculating dose, especially when moving from one testosterone preparation to another, it is also important to remember that testosterone suspension contains more active testosterone per milligram than its esterified derivatives. For example, when the ester’s weight is taken into account, 100 mg of testosterone enanthate actually only provides 72 mg of raw testosterone.
Estrogenic – Side Effects
Testosterone is readily aromatized in the body to estradiol (estrogen). The aromatase (estrogen synthetase) enzyme is responsible for this metabolism of testosterone. Elevated estrogen levels can cause side effects such as increased water retention, body fat gain, and gynecomastia. Testosterone is considered a moderately estrogenic steroid. An anti-estrogen such as clomiphene citrate or tamoxifen citrate may be necessary to prevent estrogenic side effects. One may alternately use an aromatase inhibitor like Arimidex® (anastrozole), which more efficiently controls estrogen by preventing its synthesis. Aromatase inhibitors can be quite expensive compared to anti-estrogens, however, and may also negatively affect blood lipids.
Estrogenic side effects will occur in a dose-dependent manner. Higher doses (above normal therapeutic levels) of testosterone are more likely to require an anti-estrogen or aromatase inhibitor’s concurrent use. Since water retention and loss of muscle definition are common with higher testosterone doses, this drug is usually considered a poor choice for dieting or cutting training phases. Its moderate estrogenicity makes it more ideal for bulking phases, where the added water retention will support raw strength and muscle size and help foster a stronger anabolic environment.
Androgenic – Side Effects
Testosterone is the primary male androgen, responsible for maintaining secondary male sexual characteristics. Elevated testosterone levels are likely to produce androgenic side effects, including oily skin, acne, and body/facial hair growth. Men with a genetic predisposition for hair loss (androgenetic alopecia) may notice accelerated male pattern balding. Those concerned about hair loss may find a more comfortable nandrolone decanoate option, a comparably less androgenic steroid. Women are warned of the potential virilizing effects of anabolic/androgenic steroids, especially with strong androgen testosterone. These may include deepening of the voice, menstrual irregularities, skin texture changes, facial hair growth, and clitoral enlargement.
In androgen-responsive target tissues such as the skin, scalp, and prostate, testosterone’s high relative androgenicity is dependant on its reduction to dihydrotestosterone (DHT). The 5-alpha reductase enzyme is responsible for this metabolism of testosterone. The concurrent use of a 5-alpha reductase inhibitor such as finasteride or dutasteride will interfere with testosterone action’s site-specific potentiation, lowering testosterone drugs’ tendency to produce androgenic side effects. It is important to remember that anabolic and androgenic effects are both mediated via the cytosolic androgen receptor. Complete separation of testosterone’s anabolic and androgenic properties is impossible, even with total 5-alpha reductase inhibition.
Hepatotoxicity – Side Effects
Testosterone does not have hepatotoxic effects; liver toxicity is unlikely. One study examined the potential for hepatotoxicity with high testosterone doses by administering 400 mg of the hormone per day (2,800 mg per week) to a group of male subjects. The steroid was taken orally to reach higher peak concentrations in hepatic tissues compared to intramuscular injections. The hormone was given daily for 20 days and produced no significant changes in liver enzyme values, including serum albumin, bilirubin, alanine-amino-transferase, and alkaline phosphatases.426
Cardiovascular – Side Effects
Anabolic/androgenic steroids can have deleterious effects on serum cholesterol. This includes a tendency to reduce HDL (good) cholesterol values and increase LDL (bad) cholesterol values, which may shift the HDL to LDL balance in a direction that favors greater risk of arteriosclerosis. The relative impact of an anabolic/androgenic steroid on serum lipids is dependant on the dose, route of administration (oral vs. injectable), type of steroid (aromatizable or non-aromatizable), and level of resistance to hepatic metabolism. Anabolic/androgenic steroids may also adversely affect blood pressure and triglycerides, reduce endothelial relaxation, and support left ventricular hypertrophy, potentially increasing the risk of cardiovascular disease and myocardial infarction. Testosterone tends to have a much less dramatic impact on cardiovascular risk factors than synthetic steroids. This is partly due to its openness to metabolism by the liver, which allows it to have less effect on the hepatic management of cholesterol. The aromatization of testosterone to estradiol also helps to mitigate the negative effects of androgens on serum lipids. In one study, 280 mg per week of testosterone ester (enanthate) had a slight but not statistically significant effect on HDL cholesterol after 12 weeks, but when taken with an aromatase inhibitor a strong (25%) decrease was seen.427Studies using 300 mg of testosterone ester (enanthate) per week for 20 weeks without an aromatase inhibitor demonstrated only a 13% decrease in HDL cholesterol, while at 600 mg the reduction reached 21%.428 The negative impact of aromatase inhibition should be considered before a drug is added to testosterone therapy.
Due to estrogen’s positive influence on serum lipids, tamoxifen citrate or clomiphene citrate are preferred to aromatase inhibitors for those concerned with cardiovascular health, as they offer a partial estrogenic effect in the liver. This allows them to potentially improve lipid profiles and offset some of the negative effects of androgens. With doses of 600 mg or less of testosterone per week, the lipid profile’s impact tends to be noticeable but not dramatic, making an anti-estrogen (for cardioprotective purposes) perhaps unnecessary. Doses of 600 mg or less per week have also failed to produce statistically significant changes in LDL/VLDL cholesterol, triglycerides, apolipoprotein B/C-III, C-reactive protein, and insulin sensitivity, all indicating a relatively weak impact on cardiovascular risk factors.429 When used in moderate doses, injectable testosterone esters are usually considered the safest of all anabolic/androgenic steroids.
To help reduce cardiovascular strain, it is advised to maintain an active cardiovascular exercise program and minimize the intake of saturated fats, cholesterol, and simple carbohydrates at all times during active AAS administration. Supplementing with fish oils (4 grams per day) and a natural cholesterol/antioxidant formula such as Lipid Stabil or a product with comparable ingredients is also recommended.
Testosterone Suppression – Side Effects
All anabolic/androgenic steroids, when taken in doses sufficient to promote muscle gain, are expected to suppress endogenous testosterone production. Testosterone is the primary male androgen and offers strong negative feedback on endogenous testosterone production. Testosterone-based drugs will, likewise, have a strong effect on the hypothalamic regulation of natural steroid hormones. Testosterone levels should return to normal within 1-4 months of drug secession without the intervention of testosterone-stimulating substances. Note that prolonged hypogonadotrophic hypogonadism can develop secondary to steroid abuse, necessitating medical intervention.
The above side effects are not inclusive. For a more detailed discussion of potential side effects, see the book’s Steroid Side Effects section.
General Administration
Testosterone suspension contains undissolved testosterone particles, which form a short-acting repository in the muscle following injection. Depending on the particles’ size and other agents present, testosterone suspension injections may result in local irritation, pain, and redness. Veterinary testosterone suspensions may use large particles that require a needle as large as 21 gauge for injection, for example, and can be very uncomfortable to use. Modern testosterone suspension preparations made for human use often contain microcrystalline steroid particles. These crystals are highly refined and are too small to see with the naked eye. This design provides significantly more patient comfort than less refined products and is generally well tolerated.
Male Administration
To treat androgen insufficiency, the prescribing guidelines for testosterone suspension recommend a dose of 25-50 mg, which is given 2-3 times per week. When used for muscle-building purposes, testosterone suspension is often administered at a dose of 100-200 mg per injection, given every 2nd or 3rd day. Athletes looking to achieve an extremely rapid bulk gain will inject as much as 100 mg daily. In most cases, this higher dose can be amazing, the user seeming to inflate with bloated muscle mass in a concise period of time. Back when they were being manufactured, the U.S. 30 mL vials (100 mg/mL) were always the most sought after for this procedure, as each would run the cycle for about a month. Although this drug does require a frequent injection schedule, a well-refined suspension should pass through a needle as fine as 27 gauge (insulin). This allows the user more available injection sites, hitting the smaller muscle groups such as the deltoid, triceps, and calves.
Those looking for only a potent mass agent are often extremely happy with the results provided by testosterone suspension; this product certainly has a strong reputation for performing. But those athletes who want not just quantity but quality are likely to be disappointed, as the muscle mass gain is not going to be a hard, dense one. In fact, the user will often have to contend with excessive fat and water-weight gains when building their physique with this drug and will often seek the benefit of cutting agents soon afterward to clean up the look of muscularity. Alternatively, one could use a smaller dosage of testosterone suspension, which would allow for less estrogen buildup. One could stack it with any of a variety of other less or non-aromatizable steroids, depending on the desired goals in such a scenario.
Women Administration
Testosterone suspension is rarely used with women in clinical medicine. When applied, it is most often used as a secondary treatment for inoperable breast cancer. Doses given for this application may reach 100 mg three times per week, a level well into the threshold likely to cause strong virilizing side effects. Testosterone suspension is not recommended for women for physique- or performance-enhancing purposes due to its strong androgenic nature and tendency to produce virilizing side effects.
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