DISCLAIMER:

This information was gathered from sources including textbooks, medical journals, and pharmaceutical
reports, as well as interviews with athletes, steroid dealers, and medical experts. the author
assumes any liability for the information presented in this text. This blog is not intended to provide medical
advice. The purpose of this reference blog is only to provide a compendium of information for the reader, for entertainment purposes only. None of the information in this blog is meant to be applied.

get results with steroids now

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welcome to our blog, we wish you enjoy a great body and healthy life

Thursday, September 15, 2011

Read this page only if you are considering using steroids or you've used steroids before, but not gotten the results you wanted...

"YES! Discover How To Safely And Effectively Use Anabolic Steroids And Finally Get The Massive, Shredded, Muscle Gains You've Always Wanted... In As Little As 40 Days!"

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And How You Can:

  • Experience large strength gains
  • Enhance your health
  • Have a shredded, "good looking guy" muscular body
  • Build quickness and stamina
  • Have an impressive ripped physique that makes guys jealous and girls swoon


Dear Muscle Hungry Friend,

If you want to cut through the crap... the complicated scientific explanations that no one can understand, the media bullshit, the lies from athletes or champions, past and present, andget real, hard hitting, 100% useful steroids knowledge, explained in easy-to-understand terms, then this will be the most important letter you will ever read...

You see, I was just like you. I desperately wanted to get bigger, but I couldn't find any good information on how to. Sure, I heard the gym talk and the media coverage about steroids, but I had no idea how to separate fact from fiction.

In fact, looking back, I can confidently tell you that 90% of what we've heard about steroids is complete BS!

And now that I've been studying for such a long time, I'm stone-cold positive that...

I Can Teach You How To Get Huge - Fast!

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I know this because not only have I done it for myself, but I've taught others too.

See, it started when I wanted to gain some weight. I've been an athlete my entire life, and I tried to do weightlifting in order to build muscle and get to my 'ideal' bodyweight.

Now, I was well aware that building quality lean muscle mass is hard as hell, but I tried for YEARS, and still couldn't get over 150 pounds... even though my 'ideal' weight was 180.

See the problem?

30 lbs is a hell of a lot of weight to try and gain, even over a long period of time, especially considering that I am your classic ectomorph (hard gainer) and I couldn't gain weight to save my life. Sure, I could get stronger. But I couldn't gain any mass.

At best I hovered around 150 to 155 lbs, and sure I had great muscle definition, but I was stillSMALL!

This is the point where I finally got fed up and started looking around at the various alternatives to help me reach my weightlifting goals.

I spoke with professional bodybuilders, trainers, coaches, and even a doctor or two and I bought every book I could find on the subject.

During my quest for information, I was lucky enough to meet a highly respected bodybuilding coach (name withheld at his request) who has trained some of the top bodybuilding and fitness competitors in the world.

To make a long story short, he agreed to advise me in the use of steroids and help me plan out and implement a cycle to achieve my goals.

And the results were astonishing.

In Only 6 Weeks, I Gained An Amazing 24 lbs Of Lean Muscle, Lost 2" Off My Waist, Went Up 3 Suit Sizes In My Shoulders And Stripped Off 5% Of My Body Fat!

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Here, I'll prove it:

fdfd

steroids

Here were my stats prior to starting my steroid cycle and workout program:

  • 5' 9" Tall
  • 32" Waist
  • 39" Shoulder to Shoulder
  • Biceps: Small
  • 153 Lbs
  • 14% Body Fat

After six weeks of intensive workouts, strict diet, plenty of rest and of course steroids, the results were nothing short of astonishing:

  • 5' 9" Tall (to bad steroids can't make you grow)
  • 30" Waist
  • 42" Shoulder to Shoulder
  • 15.5" Biceps
  • 177 Lbs
  • 9% Body Fat
  • And My Strength Nearly Doubled

I seriously couldn't believe it. I'd heard about stories like that before, but I never thought it could happen to me.

And I wasn't the only one.

See What Other People Experienced:

I know, talk is cheap. Especially when it comes to steroids. So here's what some others said: click here




The thing is,

Gaining Weight With Steroids Can Be Safe - IF You Know What You're Doing

But the fact is, you can't go in blindly. You need to know...

check Exactly how to avoid negative side effects... even after several cycles of steroid use

The substance you MUST use if you want to combat the side effect of excess water intake (This just might surprise you.)

The precise diet cycle you need to be on for maximum muscle gains and optimum fat loss (80% of ste.....(TO READ MORE CLICK HERE )

Thursday, April 28, 2011

testosterone/oxymetholone cycle (MASS)

testosterone/oxymetholone cycle (MASS)

Products: 20 mL 200 mg/mL testosterone (enanthate or cypionate)
100 tablets 50 mg oxymetholone

All Weeks: Liver Support: Liver Stabil, Liv-52, or Essentiale Forte (label recommended dosage).
Cholesterol Support: Lipid Stabil (3 caps/day) and Fish Oil (4g/day).
Estrogen Support: tamoxifen (20-40 mg/day).

Comments: A combination of testosterone and oxymetholone is generally regarded as the most potent 2-drug stack for gaining raw muscle mass. Both drugs will present significant estrogenicity, and will be likely to induce gynecomastia quickly unless an estrogen maintenance drug such as tamoxifen is used. Inexperienced steroid users have been known to gain over 25-30 pounds on a cycle such as this. Water retention will be very high with this stack, however, and a rapid loss of water weight (possibly up to 10 pounds or more) is expected soon after the cycle is discontinued.

week------------------testosterone-------------------------oxymetholone
1-----------------------200mg
2-----------------------400mg
3-----------------------400mg----------------------------------50mg/day
4-----------------------400mg----------------------------------50mg/day
5-----------------------400mg---------------------------------100mg/day
6-----------------------500mg---------------------------------100mg/day
7-----------------------500mg---------------------------------100mg/day
8-----------------------500mg---------------------------------100mg/day
9-----------------------500mg---------------------------------100mg/day
10----------------------200mg---------------------------------100mg/day

Wednesday, April 27, 2011

fish oil, recommended dosage for athletes


Fish oil
is a primary source of omega-3 fatty acids. These "healthy" fatty acids offer a number of benefits. If you don't enjoy fish or are unable to eat much of it, you can take fish oil capsules. Fish oil in dietary supplement form can provide the same benefits as eating fish if taken in proper dosages. Speak to your doctor before beginning a dietary supplement regimen of any type, and always read the dosage directions on supplement bottles.

Function of fish oil

Fish oil contains docosahexaenoic acid, or DHA, and eicosapentaenoic acid, or EPA, which have been specifically linked to a reduced risk of heart attacks. The acids also help correct abnormal heart rhythms, or arrhythmia, and lower the risk of stroke if you have cardiovascular disease. Fish oil can help slow the buildup of plaque in the arteries and encourage lower blood pressure . Taking fish oil supplements is helpful if you only eat fish that is fried. Frying fish eliminates fish oil's benefits.

Dosageof fish oil

Fish oil is considered safe for adults, including pregnant and breastfeeding women. According to MedlinePlus, you should not take more that 3 g of fish oil per day if you are healthy. Certain conditions may require a higher dosage. For instance, doctors may recommend you take 1 to 4 g of fish oil daily if you have high triglycerides. If you have rheumatoid arthritis, you should take 3.8 g per day of EPA. Up to 5.1 g of fish oil is the recommended dose to help prevent miscarriages in women with anti-phospholipid antibody syndrome. If you have a condition, speak to your doctor to determine if fish oil is appropriate for you to take

Side Effectof fish oil::

Taking more than the recommended dosage can lead to potentially dangerous side effects. Too much fish oil can increase your risk of bleeding. The acids in fish oil can keep blood from clotting, which can impede a wound from healing. Your immune system may also be adversely affected by fish oil doses that are too high and make you more susceptible to illness. A weakened immune system is especially dangerous for the elderly and people suffering from an immune deficiency disease.

Cautions

Fish oil capsules can be made with oil from various fish species. Certain species, including king mackerel, farm-raised salmon and shark, have a risk of containing mercury and other environmental contaminants. Use caution when taking fish oil if you also take birth control pills. The drugs in birth control can impede the fish oil from helping lower your triglyceride levels. You should also be cautious if you take medication for high blood pressure. Fish oil can promote low blood pressure. Coupled with your medication, the fish oil can force your blood pressure too low.
reference: livingstrong.com

Tuesday, April 26, 2011

deca/dianabol cycle 2 (MASS)

deca/dianabol cycle 2 (MASS)

Products: 20 mL 200 mg/mL nandrolone decanoate
-200 tablets 5 mg methandrostenolone
All Weeks: Liver Support: Liver Stabil, Liv-52, or Essentiale Forte (label recommended dosage).
- Cholesterol Support: Lipid Stabil (3 caps/day) and Fish Oil (4g/day).
- Estrogen Support: tamoxifen (20-40 mg/day).
Comments: A more popular manifestation of the Deca/Dianabol Cycle, with more commonly accepted dosages for a moderately experienced steroid user. Incidences of side effects are expected to be higher at these dosages, although overall this stack is likely to be less problematic than a combination of testosterone and oxymetholone.

week-----------------nandrolone----------------------methandrostenolone
1------------------------400mg
2------------------------400mg
3------------------------400mg-----------------------------10mg/day
4------------------------400mg-----------------------------10mg/day
5------------------------400mg-----------------------------20mg/day
6------------------------400mg-----------------------------20mg/day
7------------------------400mg-----------------------------20mg/day
8------------------------400mg-----------------------------20mg/day
9------------------------400mg-----------------------------20mg/day
10-----------------------400mg-----------------------------20mg/day

deca/dianabol cycle 1(MASS)

deca/dianabol cycle 1(MASS)

Products: 10 mL 200 mg/mL nandrolone decanoate
100 tablets 5 mg methandrostenolone

All Weeks: Liver Support: Liver Stabil, Liv-52, or Essentiale Forte (label recommended dosage).
Cholesterol Support: Lipid Stabil (3 caps/day) and Fish Oil (4g/day).
Estrogen Support: tamoxifen (20-40 mg/day).

Comments:This is an extremely old and widely repeated steroid combination, based on the predominantly anabolic steroid nandrolone decanoate. Methandrostenolone serves as the androgenic component of this stack, and is added durring 3 week, which is a time that side effects of reduced androgenicity (with the exclusive use of nandrolone decanoate) are commonly noticed, such as loss of libido and sexual dysfunction.The doses used in this cycle are not high by most bodybuilding standards, but are sufficient to impart a noticeable increase in muscle size and strength.

week---------------nandrolone-----------------methandrostenolone
1------------------------200mg
2------------------------200mg
3------------------------200mg-------------------------10mg/day
4------------------------200mg-------------------------10mg/day
5------------------------300mg-------------------------10mg/day
6------------------------300mg-------------------------15mg/day
7------------------------300mg-------------------------15mg/day
8------------------------300mg-------------------------15mg/day

stanozolol cycle 2 (LEAN MASS/CUTTING)

stanozolol cycle 2 (LEAN MASS/CUTTING)

Products: 200 tablets 5 mg stanozolol

All Weeks: Liver Support: Liver Stabil, Liv-52, or Essentiale Forte (label recommended dosage).
Cholesterol Support: Lipid Stabil (3 caps/day) and Fish Oil (4g/day).
Comments: This is a stronger version of a cutting/lean mass building cycle utilizing stanozolol. The dosage used here is substantially higher than the first stanozolol cycle, a fact that makes this cycle more properly suited for bodybuilding purposes than Stanozolol Cycle #1. Cardiovascular and hepatic strain will be I more notable, and visible side effects more pronounced, than the first cycle. There should be no need to addition an estrogen maintenance drug.
week----------------------stanozolol
1---------------------------20mg/day
2---------------------------20mg/day
3---------------------------25mg/day
4---------------------------25mg/day
5---------------------------25mg/day
6---------------------------25mg/day

stanozolol cycle 1(LEAN MASS/CUTTING)

stanozolol cycle 1(LEAN MASS/CUTTING)

Products: 200 tablets 2mg Stanozolol

All Weeks: Liver Support: liver Stabil, Liv-52, or Essentiale Forte (label recommended dosage).
Cholesterol Support: Lipid Stabil (3 caps/day) and Fish Oil (4g/day).

Comments: This is a common first-cycle for an athlete looking for performance improvements or a bodybuilder looking for a lean mass or cutting steroid. This cycle was more common when stanozolol was widely available in 2 mg tablets. Such preparations are now uncommon except in Europe. The dosage used here is low by bodybuilding standards, although similar cycles have been the backbone programs for many athletic competitors, especially during the 1970s and 80's. Significant visible adverse reactions are unlikely at this dosage.

WEEK----------------------STANOZOLOL
1------------------------------8mg/day
2------------------------------8mg/day
3------------------------------10mg/day
4------------------------------10mg/day
5------------------------------10mg/day
6------------------------------10mg/day

Sunday, April 24, 2011

The Truth about Steroids


Why steroids are so powerful and so dangerous if abused


Steroids are natural substances with many different effects in the human body, which begin over several days. The primary use of steroids in health care is to reduce inflammation and other disease symptoms. Steroid inhalers have an important role in reducing deaths from asthma, local steroid injections are useful in treating painful joints and ligaments. Steroid creams are used extensively to treat eczema and other inflammatory skin conditions. Steroids make the whole immune system less active, which can be very useful in illnesses where there is an immune component - a huge number. Steroids are the ultimate anti-inflammatory drugs.

However steroid use in medicine is limited by very serious side effects in the body as a whole. That is why steroids tend to be used sparingly in local preparations such as sprays and creams, which ensure maximum steroid dose where it is needed, and minimum levels in the blood stream.


Steroid use in medicine and health care


Steroid skin creams for example cause thinning and weakness of the skin, while steroids also cause calcium to leak out of bones so that they weaken and fracture spontaneously. Steroids also make people feel very hungry and cause blood sugar to rise. People on steroids can gain weight and often develop a typical "moon face" as well as getting diabetes.

Another serious steroid problem is that we all need aggressive immune systems to fight infections and cancers, but steroids knock that out. People on high doses of steroids for medical reasons can die from chest infections and cancers of many kinds. We see these patterns in those who receive organ transplants, who need often need huge doses of steroids to stop the body from destroying the donated tissue. Cancers often develop, which shows us how important our white cells are in keeping us cancer-free, and how often all of us develop cancer in our daily lives. Most of us may have two or three tiny cancers inside us at any time. Taking high dose steroids makes it more likely one of these will develop rapidly.

People on high dose steroids are immune-deficient in every way so that many organisms that rarely cause problems can overgrow, totally upsetting the normal balance of mircobes in the body. An example is candida yeast which can grow rapidly in the mouth causing painful thrush.



Effects of steroids on brain and cancer


Steroids also affect the brain, and high doses can make people feel happy, euphoric, hyped-up, with disturbance of sleep and even serious psychiatric illness such as mania, very aggressive behavior and psychosis (delusions, pananoia, loss of touch with reality). If steroid users are also taking other drugs which affect mood or brain function, these side-effects can be far more common.

Steroids are really useful in the care of those with advanced cancer when short life expectancy from their condition means physicians are far more relaxed about long term side-effects.

Brain tumours often respond dramatically to steroids. The reason is that the brain is contained in a bony box inside the skull and pressure can build up inside the head, resulting in headaches, sickness, drowsiness and other problems. Brain scans often show that a tunour the size of a wallnut can be surrounded by a big immune reaction, with brain swelling and inflammation. Steroids reduce the additional swelling, often reversing symptoms and buying time - maybe a few weeks. The underlying cancer continues to grow and if the person finally begins to deteriorate death often follows rapidly as the steroid dose is reduced.

So steroids are really powerful, with wide ranges of actions, producing dramatic effects ranging from pain relief to mood elevation, and if it were not for the very serious side effects they would be used even more often.

The body becomes dependent on steroids and when used in health care, most physicians reduce dosage gradually, even though they may start in an acute illness with a very high dose.



Why do people abuse steroids?


So why on earth would anyone who is perfectly healthy want to take steroids? The reason is that one particular type, anabolic steroids, have another side effect which is to stimulate muscle growth. Sadly for the sports enthusiast, this effect only works well if steroid level in the body as a whole is quite high, and that guarantees problems with side effects.

Taking steroids won't increase muscle bulk without exercise but the normal response to exercise is exaggerated.

Often you will find underlying psychological reasons why people abuse steroids in muscle building. Some studies suggest up to 25% have been physically or sexually abused as children or attacked as adults and are highly motivated to make themselves powerful and resistant to future attack. Others have a body image problem similar to anorexia nervosa, so that they see a weak and feeble body in the mirror - muscle dysmorphia. In some, steroid abuse is just a part of a wider picture of risk-taking.



Anabolic and Androgenic steroids


Steroids can be divided into two types: anabolic and androgenic, but the distinction in some ways is artificial. Anabolic steroids mainly affect metabolism, immunity and muscle, while androgenic steroids have strong masculinisation effects on women and sometimes feminisation effects on men. But all anabolic steroids will increase masculine characteristics such as thick facial hair if the dose used is significant.

Steroid cycling is a regular pattern of steroid use and non-use by athletes or body builders, the aim being to get maximum action with minimum side-effects, often by using a wide variety of different steroid preparations at the same time (stacking), and perhaps to avoid detection by timing non-use to coincide with major competitions where steroids testing may be imposed.

Some steroid abuses use pyramidding - starting with low doses and building up over days or weeks to a peak dose and then tailing off.



Anabolic steroid side effects


Typical problems you will find in people who abuse anabolic steroids include liver tumors and cancer, jaundice (yellow skin from liver failure), retention of fluid, high blood pressure, heart attacks and strokes, increases in LDL (dangerous form of cholesterol), kidney cancer, acne and trembling.

Men may find their testes shrink, sperm count falls with increase of infertility, their hair falls out, breasts start to develop, and prostate cancer becomes more likely. More than half of body-builder sterod abusers will typically experience enlarged breasts and shrunken male organs.

Women can start looking like men: growing beards, going bald, voice breaking - while their menstrual cycle changes or stops, and the clitoris enlarges.

Steroid abuse is particularly risky for teenagers, because it forces the body rapidly to adulthood, bones stop growing - permanently - and they reach puberty early.

Adolescents--growth halted prematurely through premature skeletal maturation and accelerated puberty changes.

And of course, steroid injecting carries all the other risks associated with other injecting drug use, such as infection with HIV, and hepatitis B or hepatitis C.



How many people abuse steroids?

Some surveys suggest that 2.5% of high school pupils in the US will have taken illegal steroids at some time. This is particularly worrying considering the very high risks of steroid abuse in those under the age of 18.

source:globalchange.com

Saturday, April 23, 2011

Oxymetholone Post Cycle


Oxymetholone Post Cycle Therapy | Anadrol Post Cycle Therapy

Oxymetholone is the strongest and in the same time most effective oral steroid. First thing I want to underline is that Oxymetholone is 17-alkylated and it affects liver so better to use Liv52 during and after cycle.
If you can’t find Liv52 use Milk Thistle. Important thing here is to protect liver.

Also for the same reason I would not recommend using Oxymetholone longer than 6 weeks.

Now regarding post cycle therapy. Actually this will vary from case to case in dependency from other steroids used in combination with Oxymetholone.

I guess many of you will use it in combination with testosterone and in this case Oxymetholone Post Cycle Therapy would be next:


HCG used each fourth week at 250IU per week.

Nolvadex used 4 weeks after cycle at 20mg/day

source: steroidscycle.net

oxymetholone cycle 2(MASS)

oxymetholone cycle 2(MASS)

Products: 100 tablets 50 mg oxymetholone

All Weeks: Liver Support: Liver Stabil, Liv-52, or Essentiale Forte (label recommended dosage).
Cholesterol Support: Lipid Stabil (3 caps/day) and Fish Oil (4g/day).
Estrogen Support: tamoxifen (20-40 mg/day).
Comments: This is a more popular version of the oxymetholone only cycle. The doses here are more common with experienced steroid users, and more than sufficient to promote strong mass and strength increases. Side effects may be more noticeable than the lower dose cycle, of course, which may necessitate a higher dose of tamoxifen.

week---------------oxymetholone
1---------------------50mg/day
2---------------------50mg/day
3---------------------100mg/day
4---------------------100mg/day
5---------------------100mg/day
6---------------------100mg/day
7---------------------100mg/day
8---------------------100mg/day

oxymetholone cycle 1 (MASS)

oxymetholone cycle 1 (MASS)

Products: 50 tablets 50 mg oxymetholone

All Weeks: Liver Support: Liver Stabil, Liv-52, or Essentiale Forte (label recommended dosage).
Cholesterol Support: Lipid Stabil (3 caps/day) and Fish Oil (4g/day).
Estrogen Support: tamoxifen (20-40 mg/day).

Comments: Oxymetholone is commonly regarded as the most potent mass building steroid available. It is also prone to causing both strong estrogenic and androgenic side effects. A steroid novice may gain 15-20 pounds or more on this cycle, although a significant amount of this will be water retention, which will subside soon after drug discontinuance. Oxymetholone is also known for inducing strong cardiovascular and hepatic stress. While this drug may be more convenient to use than an injectable testosterone, it is not regarded as a safe alternative. Repeated use of c-17 alpha alkylated orals like this should be limited.

week-----------------oxymetholone
1-----------------------50mg/day
2-----------------------50mg/day
3-----------------------50mg/day
4-----------------------75mg/day
5-----------------------75mg/day
6-----------------------75mg/day

sustanon 250 cycle (MASS)

sustanon 250 cycle (MASS)

Products: 15 mL 250 mg/mL Sustanon (testosterone blend)

All Weeks: Cholesterol Support: Lipid Stabil (3 caps/day) and Fish Oil (4g/day).
Estrogen Support: tamoxifen (20-40 mg/day) or anastrozole (.5-1 mg/day).

Comments: This mass building program is similar to the other testosterone cycles, but utilizes Sustanon 250, a form of blended testosterone more widely used in Europe and other regions outside the u.S.The total steroid dosage of this cycle is 3,750 mg, extremely close to the amount used in testosterone cycle #2. A similar level of cardiovascular strain and visible side effects are expected.

week---------------sustanon
1-------------------250mg
2-------------------250mg
3-------------------500mg
4-------------------500mg
5-------------------500mg
6-------------------500mg
7-------------------500mg
8-------------------500mg
9-------------------250mg

testosterone cycle :2(MASS)

testosterone cycle :2(MASS)

Products: 20 mL 200 mg/mL Testosterone (enanthate or cypionate)

All Weeks: Cholesterol Support: Lipid Stabil (3 caps/day) and Fish Oil (4g/day).
Estrogen Support: tamoxifen (20-40 mg/day) or anastrozole (.5-1 mg/day).

Comments: This cycle is a common follow up to the first testosterone only cycle, with a higher dosage and 3 week longer duration of intake. The total testosterone dosage given is double in comparison, and is likely to produce more pronounced estrogenic and androgenic side effects. Cardiovascular strain may be slightly higher than the first cycle, but should remain substantially lower than cycles with oral AAS. Testosterone is arguably the safest, and at the same time one of the most effective, muscle-building steroids available.The exclusive repeated use of a cycle like this would be advised over more adventurous cycling/stacking if possible.

week---------------------testosterone
1---------------------------200mg
2---------------------------400mg
3---------------------------400mg
4---------------------------400mg
5---------------------------400mg
6---------------------------500mg
7---------------------------500mg
8---------------------------500mg
9---------------------------500mg
10--------------------------200mg

testosterone cycle :1(MASS)

testosterone cycle :1(MASS)

Products: 10 mL 200 mg/mL Testosterone (enanthate or cypionate)

All Weeks: Cholesterol Support: Lipid Stabil (3 caps/day) and Fish Oil (4 g/day).
Estrogen Support: tamoxifen (20-40 mg/day) or anastrozole (.5 mg/day).

Comments: This mass building cycle is likely to yield simi,lar quantitative results as an early Dianabol cycle, but is favored over the oral for its lower cardiovascular and hepatic strain.The doses used are expected to cause mild shifts in the HDL/LDL cholesterol ratio, but not the substantial changes normally seen with oral anabolic steroids. This sample cycle is likely to present the least amount of health side effects of al listed in this section.
week-----------------testosterone
1-----------------------200mg
2-----------------------200mg
3-----------------------300mg
4-----------------------300mg
5-----------------------300mg
6-----------------------350mg
7-----------------------350mg

dianabol cycle :2(MASS)

dianabol cycle :2(MASS)

Products: 200 tablets 5 mg Methandrostenolone

All Weeks: Liver Support: Liver Stabil, Liv-52, or Essentiale Forte (label recommended dosage).
Cholesterol Support: Lipid Stabil (3 caps/day) and Fish Oil (4g/day).
Estrogen Support: tamoxifen (20-40 mg/day).

Comments: This is a common follow up to the first Dianabol cycle, utilizing a slightly higher dose and longer duration of intake.The dosages used here are more common for bodybuilding purposes. A slightly greater intensity of adverse reactions is likely.

week-------------------methandrostenolone
1---------------------------20mg/day
2---------------------------20mg/day
3---------------------------25mg/day
4---------------------------25mg/day
5---------------------------25mg/day
6---------------------------25mg/day

dianabol cycle :1(MASS)

dianabol cycle :1(MASS)

Products:100 tablets 5 mg Methandrostenolone

All Weeks:
Liver Support: Liver Stabil, Liv-52, or Essentiale Forte (label recommended dosage).
Cholesterol Support: Lipid Stabil (3 caps/day) and Fish Oil (4 g/day).
Estrogen Support: tamoxifen (10-20 mg/day).

Comments:
This is a very common first cycle for building muscle mass, and utilizes a single standard bottle of methandrostenolone. This cycle is likely to produce very noticeable muscle growth in a first-time steroid user, often in excess of 8-1 Olbs of weight gain.This is usually not accompanied by significant visible side effects such as gynecomastia and water retention. Although this is considered a beginner's cycle, methandrostenolone is a c-17 alpha alkylated oral steroid, and presents significant cardiovascular and liver toxicity. The repeated use of such drugs should be limited.

week----------------------
methandrostenolone
1 ------------------------------10MG/DAY
2 ------------------------------10MG/DAY
3 ------------------------------15MG/DAY
4 ------------------------------15MG/DAY
5 ------------------------------ 20MG/DAY

Friday, April 15, 2011

Stacking steroids


As individuals become more experienced with anabolic/androgenic steroid use they may begin experimenting with the use of more than one steroid at a time. This practice is referred to as stacking. Stacking is most common with advanced bodybuilders who find that at a certain level of physical development they begin hitting plateaus that are difficult to break with a previous single-agent approach. In many cases, however, it may simply be the greater cumulative steroid dosage that is necessary for the resumed progress. Stacking usually involves the combination of a more androgenic steroid with one or more primarily anabolic agents. On the anabolic side, common steroids of choice include boldenone, methenolone, nandrolone, oxandrolone, and stanozolol. Testosterone, oxymetholone, or methandrostenolone will serves as the androgenic base of most stacks .

The reasons for stacking androgenic and anabolic steroids together in this manner are two fold. On the one hand, high doses of testosterone, oxymetholone, or methandrostenolone are prone to producing strong androgenic and estrogenic side effects. Stacking first became very popular during the 1960s, a time when effective estrogen maintenance drugs were not widely availabl~.An anabolic-androgen stack allowed the use of a higher total steroid dosage than would be tolerable with a single androgen. Anabolic-androgen pairing also appears to offer efficacy advantages over the use of primarily anabolic agents alone, even when they are taken in higher doses. This conflicts with the original expectations for "anabolic" steroids, which were specifically designed to emphasize muscle-building properties, but is repeatedly noticed by users. The reason the basic androgenic steroids are more anabolically productive is not fully understood, but is believed to involve the interplay of estrogenic hormones, androgenic stimulation in the central nervous system, and potentially other unidentified synergisms necessary for optimal muscle growth.

Today, the availability of drugs that can reduce estrogenic activity makes the continued use of single agent cycles based on a strong androgen like testosterone enanthate or cypionate much more viable than it was decades ago, Side effects like gynecomastia and water retention car· now be effectively minimized with anti-estrogens 01 aromatase inhibitors, even when taking higher doses Individuals should be aware that stacking is, likewise, noi a necessary practice. It is likely to remain commonl) applicable in competitive bodybuilding circles, however or when an individual is sure they have progressed as fal as they possibly can with a single-agent approach Otherwise, for many athletes and recreationa bodybuilders, the periodic use of a single steroid will bE . more than sufficient to maintain optimal levels of musclE mass and performance, and it may never be necessary tc deviate from this approach.

Steroid Cycles


Anabolic/androgenic steroids are not medically approved to promote excessive muscle mass gains (bodybuilding) or improve athletic performance. Aside from early experimentation on athletes by a handful of sports physicians, an extensive effort to study the physique-and performance-enhancing properties of these drugs, specifically with an eye on developing strategies for using them to maximize benefits and minimize adverse effects, has not been undertaken by the medical community. Because of this, illicit users have been left to develop their own protocols for administering these drugs. The result has been a large variety of different approaches to using these agents, some safer or more effective than ,others. While it would not be possible to comprehensively evaluate all known approaches, this section will discuss some of the most fundamental and time-proven methods for using AAS

Steroid Selection
When first considering what steroid(s) to use, one will notice there are many different medications that fall under the category of anabolic/androgenic steroids. This has been the result of many years of development, where specific patients and needs are addressed with drugs that have specific characteristics. For example, some drugs are considered milder (less androgenic), and produce fewer side effects in women and children. Others are more androgenic, which makes them better at supporting sexual functioning in men. Some are injectable medications, and others made for oral administration. There are limits to this diversity, however. All AAS drugs activate the same cellular receptor, and as such share similar protein anabolizing properties. In other words, while different AAS drugs may have some differing properties, if your objective is to gain muscle mass and strength, this could be accomplished with virtually any one of the commercially available agents.

While all AAS drugs may be capable of improving muscle mass, strength, and performance, it would not be correct to say there are no advantages to choosing one agent over another for a particular purpose. Most fundamentally, the quantity and quality of muscle gained may be different from one agent to another. In a general sense, AAS that are also estrogenic tend to be more effective at promoting increases in total muscle size.These steroids also tend to produce visible water (and sometimes fat) retention, however, and are generally favored when raw size is more important than muscle definition. Drugs with low or no significant estrogenicity tend to produce less dramatic size gains in comparison, but the quality is higher, with greater visible muscularity and definition. In reviewing the most popular AAS drugs, we can separate them into these two main categories as follows.

Mass (Bulking):
Methandrostenolone -Oral
Oxymetholone -Oral
Testosterone (cypionate, enanthate) -Injectable

Lean Mass:
Boldenone undecylenate -Injectable
Methenolone enanthate -Injectable
Nandrolone decanoate -Injectable
Oxandrolone -Oral
Stanozolol -Oral

The early stages of AAS use usually involve cycles with a single anabolic/androgenic steroid. Building muscle mass is the most common goal, and usually entails the use of one of the more androgenic substances such as testosterone, methandrostenolone, or oxymetholone. Those looking for lean mass often find favor in such anabolic staples as nandrolone decanoate, oxandrolone, or stanozolol. First time users rarely welcome injecting anabolic/androgenic steroids, and will usually choose an oral compound for the sake of convenience. Methandrostenolone is the most co-mmon choice for mass building, and is almost universally regarded as highly effective and only moderately problematic (in terms of estrogenic or androgenic side effects). Stanozolol is the oral anabolic steroid most often preferred for improving lean mass or athletic performance.

The potential for adverse reactions should also be considered when choosing a steroid to use, especially if AAS use is to be regularly repeated. For example, the listed oral medications present greater strain on the cardiovascular system, and are also liver toxic. For these reasons, the injectable medications listed are actually preferred for safety (testosterone most of all). Potential cosmetic side effects may also be taken into account. For example, men with a strong sensitivity to gynecomastia sometimes prefer non-estrogenic drugs such as methenolone, stanozolol, or oxandrolone. Individuals worried about hair loss, on the other hand, may isolate their use to predominantly anabolic drugs, such as nandrolone, methenolone, and oxandrolone. A detailed review of personal goals, health status, and potential side effects of each drug is advised before committing to any AAS regimen.

Dosage
The dosage used is important in determining the level of
benefit received. Anabolic/androgenic steroids tend to be
most efficient at promoting muscle gains when taken at a
moderately supratherapeutic dosage level. Below this
(therapeutic), potential anabolic benefits are often counterbalanced, at least to some extent, by the suppression of endogenous testosterone. At very high doses (excessive supratherapeutic), smaller incremental gains are noticed (diminishing returns). In the case of testosterone enanthate or cypionate, for example, a dosage of 100 mg per week is considered therapeutic, and is generally insufficient for noticing strong anabolic benefits. When the dosage is in the 200-600 mg per week range, however, the drug is highly efficient at supporting muscle growth (moderate supratherapeutic). Above this range, a greater level of muscle gain may be noticed, but the amount will be small in comparison to the dosage increase. Below are some commonly recommended dosages for the steroids listed earlier.

-Boldenone undecylenate: 200-400 mg/wk
-Methandrostenolone: 10-30 mg/day
-Methenolone enanthate: 200-400 mg/wk
-Nandrolone decanoate: 200-400 mg/wk
-Oxandrolone: 10-30 mg/day
-Oxymetholone: 50-1 00 mg/day
-Stanozolol: 10-30 mg/day
-Testosterone (cypionate, enanthate): 200600 mg/wk

There are additional considerations other than the cost effectiveness of a particular dosage. To begin with, high doses of anabolic/androgenic steroids tend to produce stronger negative cosmetic, psychological, and physical side effects. In light of diminishing returns, the tradeoff between results and adverse reactions becomes less and less favorable. Gains made on lower doses also tend to be better retained after steroid discontinuance than those resulting from excessive intake. It is generally not realistic to expect that rapid double-digit weight gains induced by massive dosing will remain long after a cycle is over. Slower steadier gains are advised. It is also very important' to remember that higher doses aren't always what are needed to achieve greater gains. An individual more focused on his or her training and diet will often make better gains on lower dosages of AAS than a less dedicated individual taking higher doses. With this understanding, AAS should only be considered when alii other variables ,of training and diet have been addressed, and always limited to the minimum dosage necessary td achieve the next realistic training/performance goal.

Duration (Cycling)
The administration of anabolic/androgenic steroids at a given dosage will typically produce noticeable increases in muscle size and strength for approximately 6-8 weeks. After this point, the rate of new muscle gain typically slows significantly. A plateau may be reached soon after, where all forward momentum has ceased. To continue making significant progress beyond this point can entail escalating dosages, which is likely to coincide with a greater incidence of adverse reactions and diminishing anabolic returns. Even without dosage escalation, negative health changes are already likely to be apparent, and should be corrected fairly quickly. The practice of extended or continuous steroid administration is discouraged for these reasons. It is generally recommended to use AAS drugs for no longer than 8 weeks at a time (10-12 weeks at the maximum), followed by an equal or longer period of abstinence before another steroid regimen is initiated. This pattern of rotating between "on" and "off" periods is referred to as cycling.

off-Cycle(Recovery, Bridging, and Tapering)
The period immediately following steroid cession can involve a state of hypogonadism (low androgen levels), and as a result protein catabolism. In an effort to minimize muscle loss, the objective here is usually on restoring natural testosterone production, maintaining an optimal level of muscle stimulation, and remaining dedicated to proper nutrition. A hormonal recovery program is usually initiated, which may involve the use of HCG, tamoxifen, and clomiphene (see PCT: Post Cycle Therapy). A substantial off-cycle period is also advised, involving abstinence from anabolic/androgenic steroids for at least 8-12 weeks. Some AAS abusers have difficulties with complete drug abstinence, and will initiate "bridging" routines between full-dose cycles. This may involve the periodic low-dose administration of an injectable steroid, such as 200 mg of testosterone enanthate or methenolone enanthate every 2-3 weeks. Such practice is discouraged, however, as it can interfere with hormonal recovery, and prevent a return to metabolic homeostasis.

When concluding a cycle, some steroid users also follow a practice of first slowly reducing their dosages (tapering). This tapering may proceed for a 3-4 week period, and will involve an even stepping down of the dose each week until the point of drug discontinuance. It is unknown, however, if such tapering offers any tangible value. This practice has never been evaluated in a clinical setting, and is not widely recommended with steroid medications as it is with some other drugs such as thyroid hormones or antidepressants. Virtually every high-dose AAS administration study can also be found to end at the maximum dosage, with no time allotted to tapering. One flaw in the logic of using a tapering program is that they are ostensibly designed to aid hormone recovery. Recovery is not possible, however, while supraphysiological levels of androgens are present, and such levels are usually found during all weeks of a normal (nonmedical) steroid taper. Individuals remain cautioned that dosage tapering is not a proven way to reduce postcycle muscle catabolism.

Friday, April 8, 2011

The Endocrinology of Muscle Growth


The road to anabolic insight must include a biological understanding of what muscle growth actually entails. Often simplified by the term "protein synthesis': muscle growth is actually a highly complex process involving much more than just building proteins from amino acids. Muscle hypertrophy, the correct scientific term for the way we adult humans build skeletal muscle, actually requires the fusion of new cells (called satellite cells) with existing muscle fibers. Since this discovery of satellite cells in 1961, a great deal of research into the mechanisms of muscle hypertrophy has been undertaken. Scientists have come to understand that unlike normal muscle cells, these satellite cells can be regenerated throughout adult life. Furthermore, they serve not as functional units of their own, but provide some of the necessary components to repair and rebuild damaged muscle cells. These satellite cells are normally dormant, and sit resting in small indentations on the outer surface of the muscle fibers, waiting for something to trigger them into activation.

Injury or trauma will provide the stimulus necessary to activate satellite cells. Once activated, they will begin to divide, multiply, and form into myoblasts (myoblasts are essentially donor cells that express myogenic genes). This stage of hypertrophy is often referred to as satellite cell proliferation. The myoblasts will then fuse with existing muscle fibers, donating their nuclei. This stage of the process is usually called differentiation. Skeletal muscle cells are multinucleated, which means they possess many nuclei. Increasing the number of nuclei allows the cell to regulate more cytoplasm, which allows more actin and myosin, the two dominant contractile proteins in skeletal muscle, to be produced. This increases the overall cell size and protein content of the muscle cell. Incidentally, the number of nuclei in relation to cross-sectional area also helps to determine the fiber type of the cell, namely slow twitch (aerobic) or fast twitch (anaerobic)326 327. It is important to note that we are not increasing muscle cell number with muscle hypertrophy. We are only increasing cell size and protein content, even though we are using satellite cells to help accomplish this. It is possible for myoblasts to fuse together and actually form new muscle fibers.This is called muscle hyperplasia,and equates to the legitimate growth of new muscle tissue. This is, however, not the primary mechanism of muscle growth in adult life.

Monday, April 4, 2011

side sffects ;Testicular Atrophy


Anabolic/androgenic steroids may produce atrophy (shrinkage) of the testicles. Testosterone is synthesized and secreted by the Leydig cells in the testes. Its release is regulated by the hypothalamic-pituitary-testicular axis, a system that is very sensitive to sex steroids.When anabolic steroids are administered, the HPTA will recognize the elevated hormone levels, and respond by reducing the synthesis of testosterone. If the testes are not given ample stimulation, over time they will atrophy, a process that can involve both a loss of testicular volume and shape. This atrophy mayor may not be obvious to the individual. In some cases, the testes will appear normal even though their functioning is insufficient. In other cases, shrinkage is very apparent. Visible testicular atrophy is one of the most common side effects of steroid abuse, appearing in more than 50% of all anabolic/androgenic steroid abusers.

Although testicular atrophy is very common in frequency, it is also regarded as a temporary reversible side effect.296 The gonads, by their nature, will vary in size under hormonal influence. Atrophy should not produce permanent damage. Note, however, that it can be a somewhat persistent issue. It may take many weeks or months of sufficient LH stimulation after steroid discontinuance for original testicular volume to be restored. Likewise, testicular atrophy is usually the root cause of prolonged post-cycle hypogonadism. In extreme cases, full recovery can take more than 12 months, and may even require medical intervention. A post-cycle recovery program inclusive of HCG (which mimics luteinizing hormone activity) may be used to minimize this recovery phase.297 This drug is also frequently effective for maintaining testicular mass when used on a periodic basis during steroid administration.29B HCG must be used with caution, however, as overuse may cause desensitization of the testes to LH,299 complicating HPTA recovery.

Some of the more potent anabolic/androgenic steroids, including testosterone, nandrolone, trenbolone, and oxymetholone, appear to be more suppressive of testosterone release than many other AAS drugs.This may be explained in part by the additional estrogenic or progestational activity inherent in these steroids, as estrogens and progestins both also provide negative feedback inhibition of testosterone release.30o 301 It is important to note, however, that all anabolic/androgenic steroids are capable of suppressing testosterone secretion. This includes primarily anabolic compounds such as methenolone and oxandrolone, which are normally regarded as milder in this regard. While these compounds may be less inhibitive of testosterone synthesis under some therapeutic conditions, when taken in the supratherapeutic doses necessary for physique-or performance-enhancement, significant atrophy and suppression are common, and distinctions less pronounced.

side sffects :Prostate Cancer


Prostate cancer is dependent on androgens. This disease will not develop if androgens are eliminated from the body at a young age (as with castration), and abatement of androgenic activity in patients with active disease is regarded as a standard path of treatment. A complete picture of the involvement of androgens, however, remains unclear. Studies show there is no association between the testosterone level and likelihood of developing prostate cancer.273 On the same note, the administration of exogenous testosterone during androgen replacement therapy seems to have no effect on the risk for developing this disease. A review of the: available medical literature also does not support an increased risk of prostate cancer in steroid abusers,275 which typically endure excessive levels of androgenic: stimulation. The present model suggests that while' testosterone is a necessary component of prostate cancer/' it does not appear to be a direct trigger for its onset

New diagnoses of prostate cancer are sometimes reported during testosterone replacement therapy anq steroid abuse. Such reports may be the result of a previously undiagnosed condition or unrelate~ development of this disease, with androgen stimulation assisting the tumor growth rate. Many forms of prostatE cancer possess functional androgen receptors, and arJ highly androgen responsive. As such, they can bJ stimulated to grow under the influence of testosterone 01 other anabolic/androgenic steroids. Given this effect, AA~ drugs are usually contraindicated in patients with ~ history of prostate cancer. While steroid administratio~l appears unlikely to cause prostate cancer,

side effects :Libido/Sexual Dysfunction



Anabolic/androgenic steroids may alter sexual desire and functioning. The nature of this alteration, however, can vary depending on individual circumstances.Testosterone is the primary male sex steroid, and is responsible for increasing sexual desire and supporting many male reproductive-system functions.264 Since all anabolic/androgenic steroids influence the same primary receptor as testosterone, abuse of these drugs (characterized by high levels of stimulation) is usually linked to strong increases in sexual desire, as well as copulation and orgasm frequency.265 The effect of steroid abuse on erectile function is more variable. In many cases, a significant increase in the frequency and duration of erections is noted. In other instances, however, periodic issues with having or maintaining erections are reported, even when steroid levels are high and libido is significantly increased. Sexual issues are also common after steroid discontinuance, when endogenous androgen levels are low.

Studies with dihydrotestosterone and aromatase inhibition demonstrate that estrogen is not necessary for the support of male libido and sexual functioning.266 Many non-aromatizable steroids are, therefore, capable of sustaining male sexual functioning given the right level of androgenic stimulation. Difficulties remain possible in many instances, however, especially when primarily anabolic compounds such as methenolone, nandrolone, oxandrolone, and stanozolol are used alone. These drugs many not provide sufficient androgenicity to compensate for the suppression of endogenous testosterone.267 Given the diverse nature in which sex steroids influence human psychology, the existence of other influencing factors during steroid abuse cannot be excluded, including estrogenic activity.268 The addition or substitution of testosterone during a cycle is usually regarded as the most reliable way to correct issues with male sexual interest and functioning, as it supplements the full spectrum of sex steroid activity.

Priallism:
In very rare instances, anabolic/androgenic steroids have been linked to priapism.269 270 271 This is a condition characterized by the development of an erection that will not return to its flaccid state within four hours. Priapism is a potentially very serious condition, which can require medical or surgical intervention. If left untreated, priapism can lead to permanent penile damage, erectile dysfunction, or even gangrene, which may necessitate removal of the penis. When priapism is linked to steroid use, testosterone is usually responsible. Furthermore, this condition appears to be more frequent in younger patients undergoing treatment for hypogonadism. This may be due in part to a rapid increase in androgenicity, in a male reproductive system that has not yet been exposed to high levels of stimulation. Priapism is very unlikely to develop in adult steroid abusers.

Friday, April 1, 2011

Psycological side sffects


The effects of anabolic/androgenic steroids on human psychology are complex, controversial, and not fully understood. What is known for certain is that sex steroids influence human psychology. They play a role in an individual's general mood, alertness, aggression, sense of well-being, and many other facets of our psychological state.There are known psychological differences between men and women because of differences in sex steroid levels, and, likewise, altering hormone levels with the administration of exogenous steroids may influence human psychology. The exact strength of this association, however, remains the subject of much research and speculation. In reviewing some of the more substantial data that has been presented thus far, we find a better (though incomplete) understanding of the effects of AAS in several key areas of psychological health.

Aggression
Men tend to be more aggressive than women, a characteristic that has been partly attributed to higher androgen levels. Physiologically, androgens are known to act on the amygdala and hypothalamus, areas of the brain involved in human aggression. They also affect the orbitofrontal cortex, an area involved with impulse control.231 Steroid abusers commonly report increases in aggression (irritability and bad temper) when taking anabolic/androgenic steroids. In fact, among the illicit steroid-using community, these drugs are often differentiated from one another with regard to their aggression-promoting properties. Many athletes in explosive strength sports even specifically favor highly androgenic drugs such as testosterone, methyltestosterone, and fluoxymestero'ne due to their perceived greater abilities to support aggression and the competitive drive.232 Whil~ some association between steroid use and aggression is understood, the magnitude of this association remains the subject of much debate.

The psychological effects of escalating dosages of testosterone esters have been examined in a number of placebo-controlled studies. At therapeutic levels, no adverse psychological effects are apparent. If anything, testosterone replacement therapy tends to improve mood and sense of well-being. When used at a contraceptive dosage (200 mg per week), again, no significant psychological effects are seen.233 234 As the dosage reaches a moderate supratherapeutic range (300 mg per week), psychological side effects such as aggression began to appear in some subjects, but these reports remain mild and infrequent.235 At a dosage of 500 to 600 mg per week (5 to 6 times the therapeutic level), mild increases in aggression and irritability are frequently reported. Approximately 50/0 of subbbbjes displayed manic or hypomanic behavior in reaaaacn to this much testosterone, although the vast mmcrity of people still exhibited minor or no psychological ange.

Dependency Addiction
Anabolic/androgenic steroids are considered to be drugs of abuse. Although there is no universally accepted definition for this, abuse is commonly described as the continued use of a substance in spite of adverse consequences. Given the negative health consequences that are associated with supratherapeutic doses of AAS drugs, this cl.assification is a difficult one to dispute. Drugs of abuse are very often also drugs of dependency, which in this context describes an impaired ability to control the use of a substance. There has been a longstanding debate over whether or not anabolic steroids also fit the definition of drugs of dependency. Furthermore, among those that support the notion of an anabolic steroid dependency, there is a split with regard to the nature of this dependency (psychological or physical).

Physical dependency is usually regarded as the most serious form of drug dependency, although both types can be very extreme and troubling depending on the situation. Physical dependency is defined as the need to administer a substance in order for the body to function normally. A physical dependency is usually characterized by drug tolerance, and withdrawal symptoms if the drug is discontinued abruptly. The most well known examples of drugs of physical dependency are opiates such as morphine, hydrocodone, oxycodone, and heroin. Opiates can be very difficult drugs for dependant individuals to quit using, since stopping their use tends to produce extreme withdrawal symptoms including physical pain, sweating, tremors, changes in heart rate and blood pressure, and intense cravings for the drug. The physical symptoms may last for days to weeks after the drug is discontinued, while the psychological symptoms can persist for months longer.

Anabolic/androgenic steroid abuse could be associated with many of the DSM-IV criteria necessary for a diagnosis of both psychological and physical drug dependency. For instance, it is not uncommon for someone to take the drugs in higher doses or for longer periods of time then they had initially planned (criteria #1). Many abusers also have a desire to cut down on their use of these drugs, but concerns over lost muscle size, strength, or performance may prevent this decision (criteria #2). Individuals often continue to abuse steroids in spite of negative health consequences (criteria #5). Steroid abuse is also associated with a diminishing level of effect and escalating dosages (criteria #6). Lastly, steroid discontinuance has been associated with withdrawal symptoms (criteria #7), including reduced sex drive, fatigue, depression, insomnia, suicidal thoughts, restlessness, lack of interest, dissatisfaction with body image, headaches, anorexia, and a desire to take more steroids.

The physical benefits of anabolic/androgenic steroids complicate the matter of drug dependency a great deal. Unlike narcotics, the main motivator behind the use of steroids is their positive effect on muscle and performance. With this in mind, steroid addiction could actually be a misdiagnosis for muscle dysmorphia in many cases. This is a psychological disorder characterized by persistent feelings of physical inadequacy in spite of extreme muscular development. Steroid abuse (often extreme) is highly common in muscle dysmorphics, along with compulsive resistance training.243 But steroid abuse is regarded as a symptom of this disorder, not a cause. In a similar sense, the physique-, strength-, and performanceimproving qualities of anabolic/androgenic steroids could be driving much or all of the abuse. An analogy would be the so-called addiction to chocolate. Some individuals develop tangible psychological issues surrounding the consumption of chocolate, with uncontrolled binging and negative social and health consequences. But we do not regard chocolate itself as a substance that causes dependency. There is some evidence that the reinforcing qualities of steroid use go beyond an attraction to their physical benefits. Lab animals such as mice and hamsters will repeatedly self-administer testosterone and other anabolic/androgenic steroids for example, an effect that cannot be caused by a perception of physical change.245 Testosterone is also known to interact with the mesolimbic dopamine system, which is common with other drugs of abuse.246 247 Studies additionally suggest that anabolic/androgenic steroids influence dopamine transporter density and increase sensitivity of the brain reward system.248 Steroids are known to influence psychology, and abusers commonly report an increased sense of well ness, vitality, and confidence when taking AAS drugs. Some speculate this is due in part to an inherent psychoactive effect. Further research is needed to determine if anabolic/androgenic steroids are actually mild psychoactive drugs.

Depression/Suicide
Anabolic/androgenic steroids abuse may be associated with bouts of depression. This is most common after the administration of AAS drugs has been discontinued, especially following high doses or long cycles. During the time that steroids are being administered, natural hormone production is diminished because the body recognizes the excess hormone levels. When the steroid drugs are abruptly discontinued, however, the body can enter a state of temporary hypogonadism (low androgen levels). This may be associated with a number of psychological symptoms including depression, insomnia, and loss of interest.This condition is usually referred to as anabolic steroid withdrawal depression, and can persist for weeks or even months as the body slowly resumes normal hormone production The most common method of addressing anabolic steroid withdrawal depression in men is preemptively, with the implementation of an aggressive post-cycle hormone recovery program. These programs are typically based on the combined use of HCG (human chorionic gonadotropin) and anti-estrogenic drugs such as tamoxifen and clomiphene. They are used together in a way that can stimulate and sensitize the hypothalamic pituitary testicular axis, allowing natural hormone production to return more quickly. Alternately or concurrently, fluoxetine (or other antidepressant medications) may help alleviate symptoms of depression following steroid withdrawal, especially when this depression is prolonged or severe.251 These drugs must be used with caution, however, as they also have been linked with increased thoughts of suicide in some patients Although less common,depression is sometimes reported during the active administration of anabolic/androgenic steroids. This may be caused by an imbalance of sex steroid levels, particularly with regard to relative androgenicity or estrogenicity. In more cases than not, it' will involve a situation where sufficient androgenicity is' not present, usually when primarily anabolic drugs are', being taken alone. Given the diverse nature in which seXi' steroids interact with human psychology, however, it isi difficult to clearly outline the parameters necessary fo~ this type of depression to develop. Further confusing the issue is the fact that this depression can involve eitheri elevated or suppressed levels of certain sex steroids. Th~i addition of testosterone to an anabolic steroid cycle! causing depression may alleviate the problem in man(but not all) instances,as it can provide both supplemental' androgenic and estrogenic action.
Suicide has been linked to anabolic/steroid abuse in rare instances.253 Such reports are usually case studies, involving individuals that were believed to be psychologically stable before abusing AAS, and who committed suicide during or after use of the drugs. It is known that depression is a common complaint during anabolic steroid withdrawal. It is also known that a small percentage of users are especially sensitive to the psychological effects of anabolic/androgenic steroids,and notice dramatic mood swings, manic behavior, and/or severe depression with their use. It is unknown why these individuals have such extreme reactions, while the vast majority of users notice only mild or moderate changes to their psychological state. Further research is needed to identify and understand these individuals. Readers are cautioned that adverse psychological effects, including severe depression and suicidal thoughts, have been associated with steroid abuse in a small minority of users. Beyond this, there is no compelling evidence suggesting that anabolic/androgenic steroid abuse will lead to suicide in otherwise mentally stable users.

Insomnia
Anabolic/androgenic steroid use may be associated with insomnia. This adverse reaction appears to be related to an imbalance of hormone levels, and has been noticed during both excess and insufficient hormonal states. For example, insomnia is a common complaint among men suffering from low androgen levels (hypogonadism).254 It is also frequently reported by steroid abusers during the post-cycle refractory period, when endogenous androgen levels are also low due to steroid-induced suppression.255 At the same time, this side effect is also seen during active AAS administration,256 when androgen levels are very high. The full etiology of steroid-related insomnia is not fully understood, although increased cortisol or diminished estrogen is commonly blamed.257 258 Given the complex interactions between sex steroids and the human psyche, it is difficult to predict how and when this adverse reaction will appear. While insomnia may be frequently reported among steroid users, this side effect rarely reaches a clinically significant level.

safe steroids use