HGH

June 24th, 2010 meetsteroids.com

There are primarily two theories as to how GH exerts its growth promoting effects. The first theory is called the Dual Effector theory. The second theory is called the Somatomedin (“mediator of growth”) Hypothesis. Both theories are fairly strait forward. Let?s start with the Dual Effector theory.

The Dual Effector theory states that GH itself has anabolic effects directly on body tissues. This theory has been supported by studies looking at the effects of injecting GH directly into growth plates. Genetically altered strains of mice have also help to support this theory. When comparing mice that genetically over express GH and mice that over express insulin-like growth factor-1 (IGF-1), GH mice are larger. Those who support the dual effector theory site this evidence. Interestingly, when IGF-1 antiserum (it destroys IGF-1) is administered concomitantly with GH, all of the anabolic effects of GH are abolished. Clearly IGF-1 has got to be involved somewhere between the pituitary and the target tissue (i.e. muscle). The Somatomedin hypothesis clears things up somewhat.

The Somatomedin hypothesis states that GH exerts its growth promoting effects through IGF-1. More specifically, GH is first released from the pituitary and then travels to the liver and other peripheral tissues where it causes the synthesis and release of IGFs. IGFs work as endocrine growth factors, meaning that they travel in the blood to the target tissues after being released from cells that produced it, specifically the liver in this case. Many studies have been performed showing that animals that are GH deficient, systemic IGF-1 infusions lead to normal growth. Admittedly, the effects are similar to those observed after GH administration. In fact, additional studies have shown IGF-1 to be greatly inferior as an endocrine growth factor requiring almost 50 times the amount to exert that same effects of GH. Recently rhIGF-1 has become widely more available and is currently approved form the treatment of HIV associated wasting. This increased availability allowed testing of this hypothesis in humans. Studies in human subjects with GH insensitivity (Laron syndrome) have consistently validated the somatomedin hypothesis (Rank, 1995; Savage, 1993). These results indicate that although IGF-1 might be the mediator of GH effects, it’s not as simple as just getting the liver to release IGF-1.

So the main difference between these two theories is that the Dual effector theory states that GH doesn?t necessarily need IGF-1 to work, the Somatomedin hypothesis insists it does. In reality both theories are correct. It?s just that the Somatomedin hypothesis focuses on “circulating” IGF-1, the Dual Effector theory recognizes that although IGF-1 is still the active hormone, it doesn’t have to come from the blood (liver), it can be produced on location by the very cells that use it.

In summary, by combining the Dual Effector theory and the Somatomedin hypothesis there are three main mechanisms by which GH makes things grow. First, the effects of GH on bone formation and organ growth are mediated by the endocrine action of IGF-1. As stated in the Somatomedin hypothesis, GH, released from the pituitary, causes increased production and release of IGF-1 into the general circulation. IGF-1 then travels to target tissues such as bones, organs, and muscle to cause anabolic effects.

Second, GH regulates the activity of IGF-1 by increasing the production of binding proteins (specifically IGFBP-3 and another important protein called the acid-labile subunit) that increase the half-life of IGF-1 from minutes to hours. Circulating proteases then act to break up the binding protein/hormone complex thereby releasing the IGF-1 in a controlled fashion over time. GH may even cause target tissues to produce IGFBP-3 increasing its effectiveness locally.

Third, GH may influence the activity of IGF-1 on an autocrine/paracrine level. Autocrine means that a hormone has an effect on the cell that produced it, paracrine means to have an effect on the “cell(s)” next to it as well. This is a completely localized effect, not dependent on the blood stream to carry things where you want them. Muscle growth from weight training is the result of IGF-1 being produced by the muscle cells themselves, not the liver. In fact, IGF-1 form the liver is genetically different from IGF-1 produced in your muscles. This information should explain why using IGF-1 systemically (from the blood stream) has been a hit and miss proposition.

In order to sufficiently address the role of GH and IGF-1 in muscle growth, we need to explore the mechanism of not only IGF-1?s autocrine/paracrine actions, but also the mechanisms of muscle growth itself.

The ability of muscle tissue to constantly regenerate in response to activity makes it unique. Its ability to respond to physical/mechanical stimuli depends greatly on what are called satellite cells. Satellite cells are muscle precursor cells. You might think of them as “pro-muscle” cells. They are cells that reside on and around muscle cells. These cells sit dormant until called upon by growth factors such as IGF-1. Under the influence of IGF-1 these cells divide (proliferate) and genetically change (differentiation) into cells that have nuclei identical to those of muscle cells. These new satellite cells with muscle nuclei are critical if not mandatory to muscle growth.

Without the ability to increase the number of nuclei, a muscle cell will not grow larger and its ability to repair itself is limited. The explanation for this is quite simple. The nucleus of the cell is where all of the blue prints for new muscle proteins come from. The larger the muscle, the more nuclei you need to maintain protein synthesis. There is a “nuclear to volume” ratio that cannot be overridden. Whenever a muscle grows in response to mechanical overload (i.e. weight training) there is a positive correlation between the increase in the number of myonuclei and the increase in muscle cell’s cross sectional area (CSA). When satellite cells are prohibited from donating new nuclei, overloaded muscle will not grow. So you see, one important key to exercise induced muscle growth is the activation of satellite cells by growth factors such as IGF-1.

Few people realize that you can inject a muscle with IGF-1 and it will grow! Studies have shown that, when injected locally, IGF-1 increases satellite cell activity, muscle DNA content, muscle protein content, muscle weight and muscle cross sectional area.

Scientists are now figuring out the signaling pathway by which mechanical stimulation and IGF-1 activity leads to all of the above changes in satellite cells, muscle DNA content, muscle protein content, muscle weight and muscle cross sectional area just outlined above. This research is stemming from studies done to explain cardiac hypertrophy. It involves a muscle enzyme called calcineurin which is a phosphatase enzyme activated by high intracellular calcium ion concentrations (Dunn, 1999). Note that overloaded muscle is characterized by chronically elevated intracellular calcium ion concentrations. Other recent research has demonstrated that IGF-1 increases intracellular calcium ion concentrations leading to the activation of the calcineurin signaling pathway, and subsequent muscle fiber hypertrophy. I am by no means a geneticist so I hesitated even bringing this research up. To avoid confusion I will enlist the help of the people doing the research. The researchers involved in these studies have explained it this way, IGF-1 as well as activated calcineurin, induces expression of the transcription factor GATA-2, which accumulates in a subset of myocyte nuclei, where it associates with calcineurin and a specific dephosphorylated isoform of the transcription factor nuclear factor of activated T cells or NF-ATc1. Thus, IGF-1 induces calcineurin-mediated signaling and activation of GATA-2, a marker of skeletal muscle hypertrophy, which cooperates with selected NF-ATc isoforms to activate gene expression programs leading to increased contractile protein synthesis and muscle hypertrophy. Simple huh?

I’m not really sure why someone would choose to inject oil instead of IGF-1. Oil gives you lumps and causes your peers to make jokes about you behind your back. IGF-1 just makes the muscle grow and leaves people wondering how you brought up those lagging rear delts. There are primarily two theories as to how GH exerts its growth promoting effects. The first theory is called the Dual Effector theory. The second theory is called the Somatomedin (“mediator of growth”) Hypothesis. Both theories are fairly strait forward. Let?s start with the Dual Effector theory.

The Dual Effector theory states that GH itself has anabolic effects directly on body tissues. This theory has been supported by studies looking at the effects of injecting GH directly into growth plates. Genetically altered strains of mice have also help to support this theory. When comparing mice that genetically over express GH and mice that over express insulin-like growth factor-1 (IGF-1), GH mice are larger. Those who support the dual effector theory site this evidence. Interestingly, when IGF-1 antiserum (it destroys IGF-1) is administered concomitantly with GH, all of the anabolic effects of GH are abolished. Clearly IGF-1 has got to be involved somewhere between the pituitary and the target tissue (i.e. muscle). The Somatomedin hypothesis clears things up somewhat.

The Somatomedin hypothesis states that GH exerts its growth promoting effects through IGF-1. More specifically, GH is first released from the pituitary and then travels to the liver and other peripheral tissues where it causes the synthesis and release of IGFs. IGFs work as endocrine growth factors, meaning that they travel in the blood to the target tissues after being released from cells that produced it, specifically the liver in this case. Many studies have been performed showing that animals that are GH deficient, systemic IGF-1 infusions lead to normal growth. Admittedly, the effects are similar to those observed after GH administration. In fact, additional studies have shown IGF-1 to be greatly inferior as an endocrine growth factor requiring almost 50 times the amount to exert that same effects of GH. Recently rhIGF-1 has become widely more available and is currently approved form the treatment of HIV associated wasting. This increased availability allowed testing of this hypothesis in humans. Studies in human subjects with GH insensitivity (Laron syndrome) have consistently validated the somatomedin hypothesis (Rank, 1995; Savage, 1993). These results indicate that although IGF-1 might be the mediator of GH effects, it’s not as simple as just getting the liver to release IGF-1.

So the main difference between these two theories is that the Dual effector theory states that GH doesn?t necessarily need IGF-1 to work, the Somatomedin hypothesis insists it does. In reality both theories are correct. It?s just that the Somatomedin hypothesis focuses on “circulating” IGF-1, the Dual Effector theory recognizes that although IGF-1 is still the active hormone, it doesn’t have to come from the blood (liver), it can be produced on location by the very cells that use it.

In summary, by combining the Dual Effector theory and the Somatomedin hypothesis there are three main mechanisms by which GH makes things grow. First, the effects of GH on bone formation and organ growth are mediated by the endocrine action of IGF-1. As stated in the Somatomedin hypothesis, GH, released from the pituitary, causes increased production and release of IGF-1 into the general circulation. IGF-1 then travels to target tissues such as bones, organs, and muscle to cause anabolic effects.

Second, GH regulates the activity of IGF-1 by increasing the production of binding proteins (specifically IGFBP-3 and another important protein called the acid-labile subunit) that increase the half-life of IGF-1 from minutes to hours. Circulating proteases then act to break up the binding protein/hormone complex thereby releasing the IGF-1 in a controlled fashion over time. GH may even cause target tissues to produce IGFBP-3 increasing its effectiveness locally.

Third, GH may influence the activity of IGF-1 on an autocrine/paracrine level. Autocrine means that a hormone has an effect on the cell that produced it, paracrine means to have an effect on the “cell(s)” next to it as well. This is a completely localized effect, not dependent on the blood stream to carry things where you want them. Muscle growth from weight training is the result of IGF-1 being produced by the muscle cells themselves, not the liver. In fact, IGF-1 form the liver is genetically different from IGF-1 produced in your muscles. This information should explain why using IGF-1 systemically (from the blood stream) has been a hit and miss proposition.

In order to sufficiently address the role of GH and IGF-1 in muscle growth, we need to explore the mechanism of not only IGF-1?s autocrine/paracrine actions, but also the mechanisms of muscle growth itself.

The ability of muscle tissue to constantly regenerate in response to activity makes it unique. Its ability to respond to physical/mechanical stimuli depends greatly on what are called satellite cells. Satellite cells are muscle precursor cells. You might think of them as “pro-muscle” cells. They are cells that reside on and around muscle cells. These cells sit dormant until called upon by growth factors such as IGF-1. Under the influence of IGF-1 these cells divide (proliferate) and genetically change (differentiation) into cells that have nuclei identical to those of muscle cells. These new satellite cells with muscle nuclei are critical if not mandatory to muscle growth.

Without the ability to increase the number of nuclei, a muscle cell will not grow larger and its ability to repair itself is limited. The explanation for this is quite simple. The nucleus of the cell is where all of the blue prints for new muscle proteins come from. The larger the muscle, the more nuclei you need to maintain protein synthesis. There is a “nuclear to volume” ratio that cannot be overridden. Whenever a muscle grows in response to mechanical overload (i.e. weight training) there is a positive correlation between the increase in the number of myonuclei and the increase in muscle cell’s cross sectional area (CSA). When satellite cells are prohibited from donating new nuclei, overloaded muscle will not grow. So you see, one important key to exercise induced muscle growth is the activation of satellite cells by growth factors such as IGF-1.

Few people realize that you can inject a muscle with IGF-1 and it will grow! Studies have shown that, when injected locally, IGF-1 increases satellite cell activity, muscle DNA content, muscle protein content, muscle weight and muscle cross sectional area.

I’m not really sure why someone would choose to inject oil instead of IGF-1. Oil gives you lumps and causes your peers to make jokes about you behind your back. IGF-1 just makes the muscle grow and leaves people wondering how you brought up those lagging rear delts.

Scientists are now figuring out the signaling pathway by which mechanical stimulation and IGF-1 activity leads to all of the above changes in satellite cells, muscle DNA content, muscle protein content, muscle weight and muscle cross sectional area just outlined above. This research is stemming from studies done to explain cardiac hypertrophy. It involves a muscle enzyme called calcineurin which is a phosphatase enzyme activated by high intracellular calcium ion concentrations (Dunn, 1999). Note that overloaded muscle is characterized by chronically elevated intracellular calcium ion concentrations. Other recent research has demonstrated that IGF-1 increases intracellular calcium ion concentrations leading to the activation of the calcineurin signaling pathway, and subsequent muscle fiber hypertrophy. I am by no means a geneticist so I hesitated even bringing this research up. To avoid confusion I will enlist the help of the people doing the research. The researchers involved in these studies have explained it this way, IGF-1 as well as activated calcineurin, induces expression of the transcription factor GATA-2, which accumulates in a subset of myocyte nuclei, where it associates with calcineurin and a specific dephosphorylated isoform of the transcription factor nuclear factor of activated T cells or NF-ATc1. Thus, IGF-1 induces calcineurin-mediated signaling and activation of GATA-2, a marker of skeletal muscle hypertrophy, which cooperates with selected NF-ATc isoforms to activate gene expression programs leading to increased contractile protein synthesis and muscle hypertrophy. Simple huh?

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T3 Profile

June 22nd, 2010 meetsteroids.com

Cytomel is not an anabolic/androgenic steroid but a thyroid hormone. As a substance it contains synthetically manufactured liothyronine sodium which resembles the natural thyroid hormone tricodide-thyronine (L-T3). The thyroid of a healthy person usually produces two hormones, the better known L-thyroxine (L-T4) and the aforementioned L-triiodine-thyronine (L-T3). Since Cytomel is the synthetic equivalent of the latter hormone, it causes the same processes in the body as if the thyroid were to produce more of the hormone. It is interesting to note that L-T3 is clearly the stronger and more effective of these two hormones. This makes Cytomel more effective than the commercially available L-T4 compounds such as L-thyroxine or Synthroid. L-T3 has proven to be 4-5 times more biologically active and to take effect more quickly than L-thyroxine (L-T4).” In school medicine Cytomel is used to treat thyroid insufficiency (hypothyroidism). Among other secondary symptoms are obesity, metabolic disorders, and fatigue. Bodybuilders take advantage of these characteristics and stimulate their metabolism by taking Cytomel, which causes a faster conversion of carbohydrates, proteins, and fats. Body builders, of course, are especially interested in an increased lipolysis, which means increased fat burning. Competing body builders, in particular, use Cytomel during the weeks before a championship since it helps to maintain an extremely low fat content, without necessitating a hunger diet. Athletes who use low dosages of Cytomel report that by the simultaneous intake of steroids, the steroids become mote effective, most likely as the result of the faster conversion of protein.
To a great extent several body builders who are pictured in “muscle magazines” and display a hard and defined look in photos, eat fast food and iron this out by taking Cytomel. The over stimulated thyroid burns calories like a blast furnace. Nowadays, instead of Cytomel, athletes use Clenbuterol which is becoming more and more popular. Those who combine these two compounds will burn an enormous amount of fat. Cytomel is also popular among female body builders. Since women generally have slower metabolisms than men, it is extremely difficult for them to obtain the right form for a competition given today’s standards. A drastic reduction of food and calories below the 1000 calorie/day mark can often be avoided by taking Cytomel. Women, no doubt, are more prone to side effects than men but usually get along well with 50 mcg/day. A short-term intake of Cytomel in a reasonable dosage is certainly “healthier” than an extreme hunger diet.
As for the dosage, one should be very careful since Cytomel is a very strong and highly effective thyroid hormone. It is extremely important that one begins with a low dosage, increasing it slowly and evenly over the course of several days. Most athletes begin by taking one 25-mcg tablet per day and increasing this dosage every three to four days by one additional tablet. A dose higher than 100-mcg/ day is not necessary and not advisable. It is not recommended that the daily dose be taken all at once but broken down into three smaller individual doses so that they become more effective. It is also important that Cytomel not be taken for more than six weeks. At least two months of abstinence from the drug needs to follow. Those who take high dosages of Cytomel over a long period of time are at risk of developing a chronic thyroid insufficiency. As a consequence, the athlete might be forced to take thyroid medication for the rest of his life. It is also important that the dosage is reduced slowly and evenly by taking fewer tablets and not be ended abruptly. Those who plan to take Cytomel should first consult a physician in order to be sure that no thyroid hyperfunction exists.
Possible side effects are: heart palpitation, trembling, irregular heartbeat, heart oppression, agita-tion, shortness of breath, excretion of sugar through the urine, excessive perspiration, diarrhea, weight loss, psychic disorders, etc., as well as symptoms of hypersensitivity.” Our experience is that most symptoms consist of trembling of hands, nausea, headaches, high perspiration, and increased heartbeat. These negative side effects can often be eliminated by temporarily reducing the daily dosage. Those who use Cytomel over several weeks will experience a decrease in muscle mass. This can be avoided or delayed by simultaneously taking steroids. For the most part, since Cytomel also metabolizes protein, the athlete must eat a diet rich in protein.

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Winstrol Depot Profile

June 22nd, 2010 meetsteroids.com

Winstrol

(stanozolol)

Winstrol – Stanozolol is a very commonly used anabolic steroid for cutting cycles. While many people will attempt to use Dianabol or even Anadrol for cutting cycles, I´ve really never heard of anyone using Stanozolol for anything except a cutting cycle. It´s a bit of a one-trick-pony in this respect. Let me repeat that: Stanozolol is a cutting drug. Not many people will argue for its use in a bulking cycle. It´s certainly not a very effective compound for treating anemia (1) and thus, one could rightly assume that its role in bulking cycles is very limited. One novel use for Winstrol in any cycle (perhaps even bulking) would be to use it at a very limited dose, in order to lower SHBG. (2) One of the properties of Winstrol is it´s profound ability to lower SHBG much more than other steroids. A dose of .2mg/kg lowered SHBG significantly, which would in turn, raise the amount of free testosterone circulating in the body. As with 99% of steroids, however, it´s important to note that suppression of your natural hormonal levels will occur (though perhaps not to the extent that it will with many other steroids).(10) As with running virtually any compound, testosterone supplementation (i.e. running test in a cycle containing Winstrol) is warranted to avoid possible sexual dysfunction.

Winstrol & Stanozol Side Effects

Adding it to a heavy bulking cycle could be problematic, as Stanozolol is a 17aa compound, meaning that it´s been altered to endure the first pass through your liver without being destroyed. This makes it an orally active compound; so many people choose to take the pills which are available from both legitimate pharmaceutical companies as well as Underground Labs. Unfortunately, since it is 17aa, it is also liver toxic& in fact; Stanozolol has one of the worst hepatoxicity (mg for mg) of any steroid. This is the reason its addition to a bulking cycle could be problematic; generally a bulking cycle will be very heavy, dosage wise as well as toxicity-wise. It also has undesirable results on Cholesterol, and a mere 6mgs/day of Stanozolol can lower HDL by 33% and raise LDL by 29% (3). Cardiac Hypertrophy, even at lower doses could be a concern with Winstrol as well (4) Thus, many people limit their intake of Stanozolol to precontest or Summer-cutting types of cycles. It´s generally accepted that due to the toxicity issues of Stanozolol, its use should be limited to 6 weeks& as with anything though, many people have run it for up to 12 weeks with no problems.

Winstrol & Stanozol Use Effects

I ran Winstrol for about 3 months (12 weeks) at a dose of 100mgs Every Other Day (along with Test prop at 125mgs, every other day) and I suffered no ill-effects. My joints felt fine, and I can say that the only thing which was undesirable about that cycle was the injection pain. Generally, people report a “dry” and less lubricated feeling in their joints when on this drug (fluid retention is nil with Stanozolol), and also a “dry” overall look as regards contest prep. This could be due to a sort of “reverse-osmotic” effect…of course this is speculation, but people do look “dryer” on Winnie, and some even look dryer in the site they inject (more on this later). There are many conflicting reports on tendon strength and Stanozolol, even in medical journals. Some reports state that it weakens tendons, others that it strengthens them (and some speculation on the internet among many “guru´s” is that it strengthens them unevenly, leading to possible injury). For this reason, it may be best for athletes in explosive or high-impact sports to stay away from this drug. It has certainly been shown to be beneficial in some bone ailments induced by glucocorticoid induced stress (5) as well as having collagen producing properties (11), but with all of the anecdotal problems athletes have suffered with their joints while on Stanozolol, I simply can not recommend it with confidence to strength/speed athletes. I can say that personally, it was an effective compound for me and did not cause joint duress, but I can do without the discomfort of the shots, and have found other DHT based compounds to be far more effective (Masteron springs to mind).

As previously stated, this compound is unique, as it is available in both an oral form as well as an injectable form. Both forms contain the exact same compound, but injecting this compound (and yes, you can drink the injectable version, and no you shouldn´t) is superior to ingesting it orally in terms of nitrogen retention (6), and thus one would also imagine, for overall anabolism. Injecting it also has the advantage of avoiding the “first pass” through your liver, and thus places your liver under less stress.

Stanozolol (Winstrol) and Women

Stanozolol is also one of the few compounds that women can take safely, as it´s anabolic:androgenic ratio is quite skewed towards anabolism. It´s generally accepted that women can tolerate around 5-10mgs a day of this compound. Men, on the other hand can dose themselves in the .5-1.5mg/kg range. I find 100mgs injected every other Day to be sufficient, but of course, even with the injectable form, every day dosing is optimal. I tend to favor DHT based compounds, and have enjoyed great success with a Winstrol/Masteron/Testosterone cycle, but I suspect that replacing the Masteron in that cycle with Trenbolone would prove more beneficial for most bodybuilders seeking to get ripped.

Although the anabolic ratio of this product is very high as compared to its androgenic actions, not many people report huge weight gains off of Stanozolol. Also, interestingly, it has a relatively weak AR binding ability (7), which is quite unusual for a “cutting” steroid. Many of the effects of this drug, as relates to building muscle, are probably from its very high protein synthesizing ability (6) (8). In addition, since this compound is derived from DHT, it tends to promote a very nice, “quality” look to the user´s muscles, with little or no water retention. Winstrol does not aromatize at any rate and has even been speculated to have anti-progestenic properties (in at least some cases, where it may “block” that receptor) (9). If one were to run ancillary compounds with Stanozolol, perhaps Tamoxifen would be appropriate for it´s beneficial effects on blood lipids, but an anti-estrogen (in it´s classic sense) would be unwarranted; proper post cycle therapy is still needed, though.

Most underground labs produce Winstrol at very reasonable prices, in both an oral as well as injectable form. Unfortunately, production value differs vastly due to the varying size of the Stanozolol powder used to make the injectable version; the finer the powder, the smaller gauge needle it will fit through, and the easier the injection will be. Of course the opposite is also true& In any case, you should be paying under $100 for a 10ml bottle of 100mg/ml concentration, and roughly the same for 100 or so 10mg tablets

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Testosterone Enanthate. Profile.

June 20th, 2010 meetsteroids.com

Testosterone Enanthate is probably the most commonly used form of testosterone by both athletes and bodybuilders alike. Although I don´t have any hard statistics on this, I´d be willing to bet that this form of testosterone is the most commonly used form of testosterone on the black market today. It´s very effective for building muscle and strength, losing fat, and is cheap & readily available.

To understand exactly how Testosterone Enanthate (a.k.a. “test enth” or just “enth”) builds muscle and burns fat, first we´ll take a look at androgens and what they do in the body. You see, hormones are substances secreted by one cell, that has an effect on the functions of another cell. Testosterone is manufactured in the Leydig´s cells of the testes (in men). The adult male produces between 2.5 and 11mgs of Test per day.

Testosterone induces changes in shape, size and also can change the appearance and the number of muscle fibres(7). Androgens like testosterone can protect your hard earned muscle from the catabolic (muscle wasting) glucocorticoid hormones(8), thus inhibiting their ability to send a message to muscle cells to release stored protein. Remember, Testosterone sends a message to muscle cells to store more contractile protein (called actin and myosin); glucocorticoid hormones send the opposite message. In addition, Testosterone has the ability to increase erythropoiesis (red blood cell production) in your kidneys(9), and a higher Red Blood Cell (RBC) count may improve endurance via better oxygenated blood. More RBCs can also improve recovery from strenuous physical activity. Agression levels often rise dramatically with the use of exogenous testosterone (15).

All of these great benefits are to be had with the use of test enth alone, but realistically, it will be part of a cycle containing one or more other drugs. People who are bulking will probably choose Deca or Eq (possibly with Dbol as well) and those who are cutting will probably steer towards Eq and perhaps Trenbolone. Very often users will shoot this drug once or twice a week, but blood levels are still above baseline with this drug at around day eight (16).Common wisdom holds that the testosterone portion of any such cycle should be equal to or greater than any other injectable drug(s) portion (on a mg basis)…

Of course, the usual nasty side effects you can get from any form of injectable testosterone are possible with testosterone Enanthate (acne, hairloss, prostate enlargement, and shutting down your body´s own natural hormonal system, etc…) but they are very overstated or controllable in many instances.

A large percentage of those side effects occur from the body´s ability to turn testosterone into estrogen via a metabolic pathway mediated by the aromatase enzyme. This process, known as aromatization causes a portion of testosterone to be converted to estrogen. Aromatase Inhibitors (Arimidex and Letroaole, for example) can combat this very effectively, and are usually necessary with doses over ½ a gram per week.

you should be paying no more than $75 for a 10cc bottle of it, dosed at 200-250mgs/ml. Of course, as usual, prices fluctuate, but I´d recommend sticking with a reputable underground lab, rather then Organon, UpJohn, or one of the many other expensive (and often counterfeited) companies. This drug is relatively cheap to produce, as the raw materials are very inexpensive, and as such, should be reasonably cheap and especially since this drug should be a consideration for inclusion in any cycle.

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Dianabol Profile.

June 20th, 2010 meetsteroids.com

Dianabol

Dbol – Methandrostenolone

This was more or less the second Anabolic Steroid ever produced. The first, as we all know was Testosterone, which was produced in the early 1900´s and experimented with by Nazi´s in WW2, in an attempt to produce a better soldier.

Russian Dianabol and Team Sports History

Russian athletes in the 1953 World Championships as well as the Olympic games then used testosterone with great success. After that, John Zeigler, who was a doctor working with the US Weightlifting Team, began a cooperative project with Ciba to develop an equalizer for US atheletes. Flash forward to 1956 and enter Dianabol ; the original trade name for Ciba´s Methandrostenolone… but called “Dbol” by athletes. The original package insert said that 10mgs/day was enough to provide full androgen replacement for a man and Dr.Zeigler recommended that athletes take 5-10mgs/day. Incidentally, this is also the dose that Bodybuilders were reputed to take from then until roughly the 1970´s. Yeah, this was allegedly Arnold´s dose, Zane´s dose, etc… simply stacked with some testosterone. (For any trivia buffs out there, Dan Duchaine´s mail order steroid business operated under the name “The John Zeigler Fan Club”).

Dianabol Steroid Use

Enough with the history lesson, lets get into what this stuff is, and what it does. Well, first off, it´s usually found in pill form, though it can be found as an injectable also (Under the Trade name: Reforvit-B, which is 25mgs of methandrostenolone mixed with B-vitamins). It is a 17aa steroid, which means it has been altered at the 17th Carbon position, to survive its´ first pass through your liver, and make it into your blood stream. It´ll raise your blood pressure (4) and is also hepatoxic (Liver-Toxic), so be careful with it. Although I have known people to take up to 100mgs/day of this stuff and not suffer any ill-effects, and one study looked at that exact dose, and the people involved didn´t suffer any intolerable side effects ( 7). Lets examine this particular study a bit further, though:

In this study, done in the early 80´s, a very high dose of Dbol (100mgs/day for 6 weeks) decreased plasma testosterone to about 40% of it´s normal value, plasma GH went up about a third, LH dropped to about 80% of it´s original value, and FSH went down about a third also (these are all approximate numbers, for the sake of brevity, but you get the idea). Body fat did not go up significantly and Fat Free Mass went up anywhere between 2-7kgs (3.3kgs average gain). The researchers concluded that Dbol increases Fat Free Mass as well as increasing strength and performance. I can only agree, having found this to be the case for me when I did my first cycle (which was 6 weeks of dbol alone at 25mgs/day), I gained roughly 25lbs and kept nearly ½ of it. Since then, Dbol has always had a special place in my heart.

Dianabol Side Effects

As with many other 17aa steroids, Dianabol is also a very weak binder to the Androgen Receptor, so most of it´s effects are thought to be non-receptor mediated, and are attributable to other mechanisms (i.e. protein synthesis as indicated by the production of muscle tissue with very high levels of nitrogen, etc… which was indicated in the 100mg/day study). This also means it only has a modest aromatase activity (2).

How strong is Dbol? Well…on a mg for mg basis, most people agree that it´s stronger than A50…but the reason most people don´t get the same gains off of Dbol is that almost nobody takes equivalent doses (I mean…I´ve heard of people taking 150mgs of A50, but not Dbol, even though the dbol would probably provide more solid gains and be less toxic, I suspect).

So how do we incorporate this stuff into our AAS regimen? Clearly, the inclusion of Dbol at any point in a cycle would contribute to gains, however, I´d speculate that Dbol is most regularly used for 2 reasons:

  1. At the start of a cycle to “Kick Start” gains
  2. As a “Bridge” between cycles, to maintain gains

Lets examine these two uses.

Dianabol Cycle

In order to kick start a dianabol cycle, usually what you do is incorporate a fast acting oral like dianabol (or anadrol) and combine it with long acting injectables (such as Deca or Eq with some Testosterone). The reasoning here is that the oral (Dbol in this case) will give almost immediate results, while the injectable takes time to produce results. The end result is that you start seeing results within the first week of your cycle and continue up until the end with the injectables. This entails taking anywhere from 25-50mgs of dbol (although as little as 20mgs or as much as 100mgs have been reported) for 3-6 weeks at the start of a cycle (average time for a “Kick Start” is 4 weeks, though), and then ceasing their use as the injectables start to produce results.

In order to successfully bridge between cycles (and this means using a low dose of AAS, in this case dbol), you need to recover your natural hormonal levels to pre-cycle levels or to within acceptable parameters, and then you start your next cycle. The idea here is that you won´t lose any gains, but rather a low dose of an AAS will help you maintain them. Typically, you´d use around 10mgs/day of dbol and combine it with an aggressive Post-Cycle Therapy (PCT) course of Nolvadex (and/or Clomid) and HCG. This would give you full androgen replacement from the Dbol and a shot at recovering your natural hormonal levels via the other stuff you are taking. Remember, the 100mg/day dose of dbol in the study we looked at earlier did not suppress Test, LH, or FSH to a degree that would make recovery impossible and certainly not with 1/10th that dose in conjunction with an aggressive PCT.

All in all, this is a very good drug, and a potent tool for quick gains or retaining gains…when used properly and safely.

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Keto Diet broken down.

June 19th, 2010 meetsteroids.com

1. Choose a keto diet plan. Many keto plans are available, such as the Atkins and South Beach diets. Research ketogenic diets online and at the library or talk to a doctor or nutritionist. Ask your doctor to recommend a keto diet and find out why the recommendation is better than other keto plans.

  • Step 2

    Seek the advice of a nutritionist, knowledgeable of keto diets, to help you plan meals. The expert advice will help you get the correct amount of nutrients through your diet and give you ideas for food variety.

  • Step 3

    Select quality meat. Keto diets allow you to eat a large quantity of meat. Quality meat is fresh, hormone-free, little fat, has the right coloring and no odor. Choose a variety of meats from beef to fish. Eat fish whenever possible because of the high content of omega-3 fatty acids benefits your heart.

  • Step 4

    Limit the consumption of carbohydrates. Most ketogenic diets utilize a combination of carbohydrate elimination and low carbohydrate meal plans. Often, you induce ketosis by eliminating all carbohydrates for about two weeks and then slowly introduce a limited amount of carbohydrates back into your diet.

  • Step 5

    Eliminate sugar from your diet. Even small amounts of sugar can convince your body to start burning glucose for energy instead of fat. Sugar is avoided for maximum weight loss.

  • Step 6

    Drink plenty of water to encourage weight loss. Water assists your metabolism to burn more calories and helps prevent constipation.

  • Step 7

    Take vitamin supplements because the low carbohydrate and high protein focus of the diet can deprive you of certain essential vitamins. Get a multivitamin and supplements for calcium and B complex to balance nutrition.

  • Step 8

    Exercise regularly. You will lose fat faster on a keto diet if you exercise. Walk around the block, ride a bike, jog in the park or work out on the elliptical. Schedule some form of exercise into your daily routine to keep your heart healthy and lose weight.

  • Step 9

    Get enough sleep. You may be extra tired during the early stages of ketosis. Sleep 7 to 8 hours a night for maximum energy. Adequate rest will also assist your weight loss effortsr

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    Synthol.

    June 18th, 2010 meetsteroids.com

    This compound is a perfect example of the extremes that some bodybuilders will go to be the “biggest”. Not content to have 20 or 22-inch arms, bodybuilders found a way to push the limits up to the 27-inch barrier. Yes you read correctly there are freaks walking around now sporting thigh-sized arms from their shoulders!

    Synthol has its origins in the 1980′s when a drug called Esiclene was all the rage. For those who missed the 1980′s, Esiclene, was not used to build muscle mass like traditional steroids but instead was used as a quick fix to bring up weak bodyparts before a contest. The drug acted primarily by causing a localized swelling. Bodybuilders found it very useful in bringing up such small muscles as the calves, rear shoulders, and arms. The only drawbacks were that Esiclene was very painful to use and very short-lived.

    In the mid 1990′s a researcher took the next logical step and invented an oil-based compound that could be injected directly into the muscle.
    The initial name he chose was Synthol, but he later learned that this was already registered and trademarked by a pharmaceutical company. So he renamed his product Pump N’ Pose, but as with steroid trade names the first name stuck. It has now reached the point that Synthol is as well known as such bodybuilding compounds as creatine, Dianabol, and whey protein.

    Chemically the drug is composed of 85% medium-chain triglyceride oils (a fatty acid), 7.5% lidocaine (painkiller), and benzyl alcohol. The oil is injected straight into the muscle where it becomes trapped between the muscle fibers. With each injection, a larger volume of oil builds up, and the muscle swells up just like a balloon. It is estimated that about 30% of what is injected is broken down by the body while the remaining 70% breaks down slowly over three to five years. Users report incredible muscle pumps during training, but this could be a result of the extra pressure generated by the trapped oil.

    Is it safe?

    Although some bodybuilders consider Pump & Pose relatively safe to use, there are numerous health issues to consider. Injecting any amount of fatty-acid material intramuscularly can be dangerous. This is compounded by the fact that most bodybuilders have any medical training. It’s very easy to hit a major nerve and if you do hit one by accident you can easily cause permanent paralysis of muscle fibers in that area.

    The repeated injections cause other problems. As bodybuilders have discovered from long-term steroid use, sticking a needle into the same are results in the build up of painful scar tissue that may require surgery to remove. And it gets worse. Should you inject into a vein or artery by mistake the fatty acids could be carried to the lungs and cause a pulmonary embolism. They may also reach the heart and induce a heart attack. They might even make it to the brain and lead to stroke. As you might guess all three cases are potentially fatal. Oh and did we mention that if you strike a larger artery such as the femoral artery you could bleed to death in minutes!

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    Sarms S4

    June 17th, 2010 meetsteroids.com

    SARMS S-4 and bridging. Is This The Perfect Drug To Use In-Between Steroid Cycles?

    SARMS S-4 is the latest addition to the anabolic steroid using bodybuilder’s arsenal and it’s creating a storm of controversy. It may very well be most significant advancement in muscle development since the invention of Dianabol back in 1956. A bold statement for sure. But SARMS S-4 is truly an incredible compound with many applications, most significantly, as a viable anabolic enhancement to be used in-between steroid cycles which is also known as bridging (1).

    SARMS S-4 is not a steroid. It is the veritable “next step” beyond steroids. It’s a Selective Androgen Receptor Modulator, which essentially means it targets your androgen receptors in a way where they’re most beneficial for building muscle while avoiding the nasty side effects that go along with traditional androgenic steroids (2).

    Due to that elusive combination of good without the bad, SARMS S-4 has been hailed as the “Holy Grail of Muscle Growth.” It’s what all athletes have been waiting and wishing for. Think of it as pizza without calories, alcohol without the hangover and safe sex without condoms. Is that possible? Yes it is. But there are limitations. (Damn!) But rest assured, they’re minor. There is a catch – there always is. But in the case of SARMS S-4, the catch isn’t that bad.

    For one thing, SARMS S-4 will not work like mega doses of steroids. You would not be able to take huge dosages in order to gain massive size on the order of a gram of testosterone. Its benefits work within a specific dosage range (3). In that regard, SARMS S-4 is unique. A good comparison would be to aspirin, which will always lower a temperature from a fever, but no lower than 98.6. However, MORE aspirin will not improve the condition. There’s that “sweet spot” where it works its magic with virtually no risk. SARMS S-4 is like that. In controlled dosages, it’s a non toxic, non testosterone suppressive compound that works like steroids, but without the side effects(4). But beyond a certain dosage, it does not work much better. It has a sort of “built in safety net.” Using 50ml a day is an effective dosage with 100mls a day being the cut-off point to avoid any negative side effects.

    The potential and the possibilities are as compelling as they are enticing, but one area where SARMS S-4 is becoming increasingly popular is in the area of “bridging.”

    A “bridge” is essentially a description for using any compound that will maintain the gains of your last steroid cycle until you decide to start your next cycle, however many months later. How to best bridge has been a controversial topic for some time. In the past, bodybuilders have attempted to sustain the effects of a steroid cycle by using a milder , less suppressive steroid (such as Primobolin) in-between cycles.

    Another method of attempting a “bridge” was to use a short acting oral in the morning so that it would not be active past a four hour window. In this way, at least theoretically, you could recover over-night, resulting in your body managing to restore its natural hormonal balance. Unfortunately, neither game plan was especially successful for even a low dose of any steroid will cause suppression of your natural testosterone production and hinder recovery.

    That’s where SARMS S-4 fits in… Remember, SARMS S-4 is not a steroid. It works on an entirely different principle – that of being “selective” to muscle. And at 50 mls a day it has’s been shown to have no suppressive effects. (Unless dosing exceeds several months)(5). This makes SARMS S-4 the perfect choice to be used in-between cycles. You won’t make massive gains while on but you’ll hold onto your gains and still be in an “enhanced” state without fear of suppression. Not a bad deal.

    It would make far more sense to “bridge” using SARMS S-4 on its own, or with natural supplements in order for the body to maintain ultimate anabolism without suppression. As much as using a less suppressive steroid may seem to make sense, ANY steroid even in low dosages will suppress, delay recovery, and ultimately work against the process of recovering from a cycle. It will also minimize the results of the NEXT cycle since the receptors would not have had a chance to replenish(6) This is what makes SARMS S-4 superior for this purpose.

    Another similar method that’s becoming popular is to use SARMS S-4 as a “mini-cycle” in-between steroid cycles. In other words, once you finish your course of steroids and do a proper PCT and settle into being “natural”, after a while you can use SARMS S-4 daily for a 4 week run. In this way you can bump up gains, increase muscle density, improve lifts and burn fat – all without deregulating androgen receptors or compromising the HPTA. (Hypothalamic Pituitary Testicular Axis)(7). Never before has this been possible.

    A PCT following a SARMS S-4 cycle may not be necessary. Some OTC supplements may be all you need to get back to baseline. SARMS S-4 won’t aromatize so there’s no fear of developing gyno or other estrogen related conditions(8).

    SARMS S-4 has many uses and having an anabolic/androgenic advantages while off cycle may be the most significant of all.

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    Top 3 Proper Guidlines to Buying Steroids.

    June 15th, 2010 meetsteroids.com

    When first looking into a cycle, the first thing that one wants to think of is RESEARCH.  Before ever swallowing or injecting any Anabolic steroid you want to no what you are putting into your body and what side effects you could see. 

    1st.  You want to make sure you have reached your full potential atleast working out and following a diet for atleast a year or two.  Steroids will help but that is it, they are no magic pill.  If your diet isn’t in line and you are not working out hard and following a routine steroids are going to do nothing for you. 

    2. Finding a cycle for a begginer.  This is most important because alot of Begginers are going to want to go straight into oral only cycles and not realizing that in the end they are going to loose most if not all there gains.  I have seen it over and over again.  Injecting is the way to go.  And Having  Testosterone as the base of ever cycle is key to making and keeping gains.  Your first cycle is the best cycle you can use so use it properly. 

    3.Finding a legit source.  There are many many people out there just looking to rip you off.  Worse then that there are many underground labs selling fake and dirty steroids that can potentially hurt you and make you sick.   Searching and reading what and who other members use is easy but hard to find.  Make your way around the net and do not rush this.  Forums are your key. 

    These are the 3 main Keys to going about making your purchase and learning about what you are putting into your body.  If you find a great source they will take care of you.

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    Injection gone wrong. Abscess

    June 15th, 2010 meetsteroids.com

    Here you see, this gentleman purchased underground steroids and supplies and found himself in a horribly painful situation.  Not only did he not get the effect he wanted, his training was completely side-tracked for months as he had to recover from a horrific abscess that he ended up with after using the underground steroids.  This again points out some of the dangers with taking steroids when you are not under the care of a doctor, trainer, or physician’s assistant.  You never know what you are getting, you literally could be injecting anything into your body.  Worse yet, there is nothing you can do about it since you obtained the steroids illegally.  You can’t go to the police, you can’t sue the supplier, you cannot even worn others due to the fact that it could implicate you.  So again, before you reach for the needle or pill for that matter to get that edge that you are looking for take a look at these pictures and wait a couple of weeks.  If you still feel like this is something you want to do then find a legitimate supplier.  You must make sure you know what you are taking.

    Read threw the injection section to see a proper way of injecting.

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