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Beastdrol Advice + PCT

Manuel

New member
Hi
im am 28 years old live in europe and working as an ICT MANAGER
ive been working out since i was 18/19 sometimes i took a break for 4/8 months due to fam problems
but most of the time i work out 4/5 times a week
lately 4 times a week monday/tuesday thursday/friday - wednesday / saterday and sunday is resting :P

i tryed alot of supps and mostly i use Brands like BSN / BPI or Muscletech. I KNow Most Is Advertise Scams Highly Priced Low Workings ;)

2/3 years ago i tryed steriods 4 week cycle oral just before summer started - can't remember what i used exactly but it did wonders for me my weigt was like 75 kilo (yes i am lean and no fam related muscular builds or sports history)
but after that cycle i went from 75 kilo to almost 90 almost no side effects only that i was a bit grumpy / short edged :P
i did eat more but not exactly a food plan,
just healthy things lots of meat and veggies also used vitamin pils and protien shakes and other stuff.

but because im in europe it can be expensive(Steriods), sow my friends braught me to the site MRsupps and i was surpised at the prices.

now my question is i wanna try Beastdrol the starter kit

Atm i have been resting from gym for 8 weeks now just started this week again
Wanted to try this Beastdrol in april.
weight atm is around 80kilo (yes lost a bit after cycle :P )
i eat 3/5 times a day still.
i don't use alcohol and i am a non smoker!

my work out is good i gues i got it from my trainer its a 4 day gym workout cycle
monday chest / tri ceps
tuesday back
wednesday rest
thursday biceps / schoulders
friday legs

now i wanna get big and ripped like when i used the oral cycle few years ago
do i get good results? and will they stay or go away few weeks after using cycle?

and with Beast can i still use Muscletech products cuz i have plenty still in my house
like neurocore, nitrotech, leukic caps,weightgainer, and bpi amino blox!!

if annyone has tested this or can tell me more on how to use or what better to stack with im all ears :)

My cycle shedule will be posted beneath this one!!!
 
I read alot about Beastdrol and other stuff!

But since everyone is reacting diffrent on supps i wonder what to take with and WHAT NOT

My cycle wud be this: And yes i asked around and ppl said its no problem to use some supps ON CYCLE
(this Shedule will be applyed end april/begin mei) sow that in juni/juli im done with it

1 Beastdrol
1 Forged Liver Support
1 Forged Post Cycle
1 Forged Joint Repair
1 Forma Stanzol (got one xtra bottle cuz i gonna use it on cycle aswell)

[/I][/B]also i will use these:
Mass Protein Bars Stack (This stack comes with 2 better protein bar packs
1 16 once high protein power butter (enough to make to batches of protein bars).
Better protein bars when made with 8oz power butter and 3/4ths cup Honey
Total calories 456
Total fat 10g
Sat fat 4g
trans fat 0g
total Carbohydrates 39g
total sugar 27g
protein 38g)

GEAR (2bottles =400 pills)
Unleashed \ Post Cycle Combo
HCGenerate
Need 2 Sleep (Only wanna use this if i cant get a good night sleep)

Big Blast (43% CFM Whey Isolate, 19% Dextrose, 15% Rilose, 10% Super Plasma Protein, 10% Whole Egg, 2% Creapure Creatine Monohydrate
1% L-Arginine Alpha Ketoglutarate Aminogen )

Then Comes The Multi Vitamin Section (** = Use Whole Year / * = Use Only While Doing Actualy Gym/Supp Cycle)
Flindal Multi Vitamin & Minerals (13 Vitamins & 14 Minerals in 1 pil) Dosage 1 a day ** 90 pils per sachet, got 5 of them
Flindal Omega 3 Forte (Fish fatty acids + Vitamin E) 1 cap a day 585mg a cap ** 90 caps per sachet, got 5 of them
Roter Chewable Vitamin C pils (Lactose and Glute Free / 70mg Vitamin C) 3 pils a day ** those are 400pils per bottle, got 3 of them
and some cranberry/magnesium pils


Then some supps i know most ppl argue about or disagree with me but i felt good using it and did help me a little bit as i may say
(but yeah i agree on marketing bs and some very high prices )

Alpha Amino Prototype 216 pils Brand Muscletech (Yeah I Kow Will be flamed for using M Products :P but i have these and more from M laying around sow i dun wanna trow it just away)

2x Nitro Tech Hardcore Pro Series Vanilla/Chocolate Muscletech
Leukic Hardcore Pro Series (1 bottle 180 caps) Muscletech
Neurocore (1 tub Pre work out supp) Muscletech
Nitro Amino FX (2x tub ) Muscletech
BLOX (Contains SAA=Silk Amino Acids ) 1 tub BPI
Anabolic Vitakic (2 bottles ) * 3-5 caps a day 150 caps per bottle Muscletech
100% Premium Mass Gainer (12 lb Chocolate ) Muscletech
100% Premium Whey (5lb Chocolate) Muscletech
and the last one
Lean Gain By Body & Fit Sportsnutrition 5kilo container chocolate milkshake this one i am using atm its an all time shaker ;P
100% Whey Gold Standard 2,5 kilo tub chocolate

Now i know this is much and shud have cost alot but NO i worked at a storage facillity near me where we stored many of these products before they go to body shops! almost all of this i got for a FEW BUCKS euro's that is as im from netherland!

And yes most is muscletech now you may think oh this kid fall for the hype or marketing bs i can honestly say NO i don't
then why i have sow much of M well it was the most common in oure fac together with bpi and bsn.
bsn made me puke almost on al products and yes i tryed tons of supps
bpi was decent by taste but didnt do a real noticeable effect
and last but not least MUSCLETECH omg the advertising makes me sick and its everywhere but yes ppl seem do dig it cant blame them for false hopes and empty pockets

Wel i used the whole chain of M supps alsow not a real diffrence in appearence but for me the tastes of some prod where awesome and as far as whey and mass it did some work for me hence why i have the mass and whey from M. And i did get it all almost for free!!!

But that aside my real question is again is this to much to use with my cycle ON and OFF Before and After?
i know beast does alot to the body sow i dun wanna encurrage myself or these prod to do more damage then neccesary
but if i can handle it and its ok, would adding these to my diet be beneficial as of gains and strength?

cycle would be done like this: I gym in the morning at around 11/12

1st week Beastdrol - 1 capsule 2 times a day spread out morning and night. i wanna build up tolerance in 1st week
2-5 Beastdrol - 1 capsule 3 times a day spread out morning, Noon, and night.
2-10 Forma Stanzol - starting 3 pumps for tolerance then raise to 5 pumps rubbed on your chest 2 times a day morning and night.
2-5 HCgenrate - 5 caps a day
1-4 Forged Joint Repair - 1 capsule 2 times a day morning and night. (Dunnow If I Really Need This?)
1-4 Forged Liver Support - 1 capsule 2 times a day morning and night.
4-8 Forged Post Cycle - 2 capsules 2 times a day morning and night.
4-8 Unleashed / Post Cycle - 3 caps a day (Dunnow If The Xtra Bottle Post Cycle Is Nesecery?)

Only got 1 bottle of beast sow i wont make a full 5 week cycle more like 4,5 cuz of 1st week tolerance!
if you think this is no good or not nesecery then please let me know

The Hype Supps as we call it wil be taken inbetween meals and gym vissits
diet consist of 3/5 meal times a day
note that i can eat alot of fast food :P i know thats not healthy
my metabolism is well very quick if i may say sow and works sometimes to great sow gaining is hard i can eat alot but weight goes up almost nothing i am current at 77 kilo and my goal is to be over 85kilo again i am very lean sow i wont need cutting my abs are good and noticable sow that wont be a problem i just wanna gain weight muscle and strenght!

this was a long speech but the more info the better the help they say
and yes i read allot on here but i want new and more experienced oppinions on how what not to take with Beast and such and what you surely need to take!

ty in advance Greeting Manuel. :D
 
the good thing is that you have done a lot of research... so you have a lot of things covered however you definitely have a few holes in your cycle... one thing is for sure, beast will shut you down, hard! so you need to add a serm to your pct... either torem or clomid... go to chemicalneed.com for those... i would also consider running transaderm alongside the beast to combat the lethargy and other sides that come along with it... beast is harsh, so you really want to make sure you prevent as many sides as you can... you are going to gain a lot of size off this, good dry size but how long you keep it is really up to you... you need to bust your a$$ after cycle and have a good plan for after your cycle is over... you can get a lot out of this cycle if done properly... generally 4 weeks is all you run of beast... most people can't take much more than that... so 5 would be the most i could see you doing and if you can handle it, by all means, go for it... im going to refrain from making any comments about your muscletech supps... if you have them and spent money on them, then i understand you wanting to use them, but if it were me, i would try to sell them and get top quality... just my thoughts... anyway, good luck with your cycle, you should log it if you have the time...
 
hey thnx for quick advice :)

yes i did years of research and reading alot of stuff before trying and still i need to ask alot so i can asure my self being covered ;)

I cant find transaderm thats why i wanted to put HCGenerate with Beast! and unleashed after.

But my mean concirn is the cycle itself is it good or bad idea to build up tolerance and run the rest with it and use supps alongside?
because i never tryed it and everyone says its a hard one i wanna do 2 pils first week then go to 3 pils a day till bottle is finished!
and as far as Muscletech supps go i got alot of them for almost no money i can sell them i guess or use idc lol i got lots of other brand name supps as i can get my hands on them easy and very very cheap :P

bc if i do use transaderm do i use it when i start Beast or?


i think torem shud be better since i did reasearch on clomid and nolva/Tamoxifen they had something to do with cancer and erectile funtions! i don't say there not working or very bad but its something to deepen youre mind in when using it alot ;)
Articles below:

Its an longggg article but its very helpfull and much info ;)


I am going to come back to this post later when I have more time. I have come to realise that there is no official Post Cycle Therapy or cookie cutter once size fits all pct for all cycles. Pct,pree pct,bridging for all different cycles is way more then something one cookie cutter official Post Cycle Therapy can cover.

So I will cover many different cycles,length of cycles,compounds used,what can be used on cycle,what can be used during cycle,what can be used for pct, methods of pre pct, methods of bridging and more. I think the members of ef diserve much more then a cookie cutter pct.

In the mean time if you need pct advice just send me a pm and I would be more then happy to help you.


First off I would like to say if you cant sit through something like this and read the whole thing. Then you really have no business taking these kinds od drugs in the first place. You also have no business making a comment on this thread ether. Thanks.

What Is Nolvadex/Tamoxifen?

Tamoxifen is considered as the antagonist of the estrogen receptor which again is primarily present in the breast tissue of the human body. It is interesting to note that certain breast cancer cells require that the estrogen levels need to grow with passing time. Ideally, Tamoxifen has been used as the standard endocrine for the treatment of early breast cancer patients. It is therefore used as an anti estrogen therapy and it is mainly given to postmenopausal women. The role of an estrogen is to bind as well as activate the estrogen receptors that are present in the breast cells of a human body. The role of Tamoxifen is to stop estrogen to bind with the receptor. Although it is metabolized into compounds that aid in the binding of estrogen receptors, Tamoxifen does not allow the estrogen receptors to get activated in the breast cells of the human body. Hence, the growth of breast cancer cells can be stopped by making use of this compound. Nonetheless, results vary from person to person and the use of Tamoxifen cannot be deduced as a permanent cure for breast cancer patients.

It is ideally a drug which is taken orally in the form of an edible tablet and it is known to interfere with the activity of the estrogen levels present in the breast tissue. It has been studied that unless the estrogen levels in the human body are kept under strict control, they can lead to breast cancer. Tamoxifen has primarily been used for the past 30 years for treating patients suffering from breast cancer. It has also been administered to patients who are in their early stages of breast cancer. Even patients whose breast cancer has spread to various parts of the body have been known to use Tamoxifen on a regular basis. It has been stated that this drug has the ability to stop cancer cells from spreading within the human body but ironically there is no substantial study which clearly backs this statement with the help of substantial proof. Nonetheless, owing to the hype that it has received via media, people who are having breast cancer or those women who run the risk of developing breast cancer have been known to take this medicine on a regular basis. Interestingly, it has also been seen that women who are suffering from ductul carcinoma in stu, which in turn is similar to invasive breast cancer, have also been known to administer this medicine on a regular basis.

In the past 20 years steroid users have been using nolvadex for a number of reasons. To ether help reduce bloat or gyno problems during a cycle or after a cycle to help recovery natural test production. In men, tamoxifen "nolvaldex" is sometimes used by steroid-taking, weight-training athletes.An alternative and highly similar compound is clomiphene citrate "clomid". These drugs are used as anti-estrogen therapy. In this regard, the drug is used for three purposes. The first purpose, is to reduce the effect of circulating estrogens even if Tamoxifen itself increase the circulating level of estrogens since they are not bound to the estrogen receptors. Abnormally high levels of estrogen in men, can be caused by taking highly aromatizing anabolic steroids e.g. Dianabol, Anadrol or Testosterone. In dosing with a dosing with 20 mg of Novaldex (Tamoxifen) for the duration of a steroid cycle, a reduction in water retention can be achieved. This prevents large fluctuations in water weight within the muscle.

Using Tamoxifen for the duration of a steroid cycle may or may not promote a preferable outcome for a weight training athlete, as the temporary increase in water weight within the muscle increases strength and allows larger weights to be used for the duration of the steroid cycle. Said water will dissipate once usage of steroids has ceased, and a dramatic loss in weight can be observed. Tamoxifen is also used to prevent estrogen related gynecomastia, resulting from elevated estrogenic levels. It can be taken as a preventative measure in small doses, or used at the onset of any symptoms e.g. nipple soreness/sensitivity. In the latter case, dosing reverses the affliction

However it Is now well known that well taking nolvadex serum level estrogen raises and yet another drug must be taken with it during cycle,during pct,or after pct to prevent estrogen rebound. (how retarded). Studies have of course shown the its use can cause a rise in lh and test production but at what cost? Many other factors must be taken into account.

All this is happening in complete ignorance as they are not aware that this medicine has certain side effects that can prove fatal in the longer run. At the same time robbing ones self of a better pct and cycle from using drugs like this.
Though I do feel its "ok" to use them "if you must" but use as little as you can and use support/pct sups to help alleviate the side effects and bad feelings one gets from these harsh drugs.

Where Was This drug Discovered?

Interestingly, this drug was discovered by AstraZeneca Pharmaceuticals which were earliest known as ICI pharmaceuticals. It is now sold under various trade names such as Nolvadex, Valodex and Istubal. Although it is sold under various names, it is primarily known and popularly termed as Tamoxifen. Although this drug is widely used in treating breast cancer patients, it also has adverse side effects which very few people are actually aware off.

Once praised for its benefits in preventing breast cancer recurrence, the lucrative pharmaceutical drug tamoxifen is now implicated in causing dangerous side-effects, including other types of cancers.

In the early 1970's, a shameful chapter closed on the widespread use of a known carcinogenic and endocrine-disrupting drug called DES (diethylstilboestrol), the first synthetic, non-steroidal estrogen drug. Against the advice of its creator, Sir Charles Dodd, between four and six million American and European women and 10,000 Australian women innocently used DES for the prevention of miscarriage and pregnancy complications.

In addition, DES became a popular though unproven drug for a variety of other conditions. It was used for the suppression of lactation, the treatment of acne, the treatment of certain types of breast and prostatic cancer, and as an inhibitor of growth in young girls, an estrogen replacement in menopause and a "morning after" pill.

It would take 30 years to accept what laboratory tests had indicated as early as 1938 — that DES was a highly dangerous and harmful drug. It was reported that, 20 years after taking DES, mothers had a 40 to 50 per cent greater risk of breast cancer than non-exposed mothers. In addition, the children of DES mothers showed a high incidence of reproductive abnormalities, miscarriages, vaginal cancer, testicular cancer, sterility and immune dysfunction. In fact, it is feared that repercussions of this drug will be felt for generations to come.

The irony of this entire debacle is that the medical establishment finally acknowledged that DES was useless in preventing miscarriages. Thus, DES, another disastrous experiment on women, was added to the long list of major medical blunders.

Out of this early research, a new drug appeared on the horizon which would be soon be heralded as a shining star in the war against the growing epidemic of breast cancer. In the late 1960's the pharmaceutical industry developed a drug called "tamoxifen". As a synthetic, non-steroidal compound with hormone-like effects (many of which are poorly understood), tamoxifen has a similar structure to DES. In fact, it was observed that tamoxifen caused the same abnormal changes seen in cells of women taking estradiol and DES. This similarity raised alarm bells for some.

Pierre Blais, well known as a drug researcher who was ejected from Canada's health protection bureaucracy when he spoke out about silicone breast implants, describes the story of tamoxifen as "the story of modern drug design which produces garbage drugs". He says, "Good drug design ceased, unfortunately, in the 1930s." Tamoxifen, Blais asserts, "...is a garbage drug that made it to the top of the scrap heap. It is a DES in the making."

Blais's dire predictions were ignored with the promise of a potential drug treatment for breast cancer. Tamoxifen was first approved by the US Food and Drug Administration (FDA) for use as a birth-control pill; however, it proved to induce rather than inhibit ovulation.(just goes to show how retarded they truly are) Although tamoxifen didn't work as a contraceptive, it was found to lower mammary cancer rates in animals. Animal studies showed that tamoxifen prevented estrogen from binding to receptor sites on breast tissue cells. Tamoxifen also reduced the incidence of breast cancer in rodents after administration of a breast-carcinogenic substance. This discovery provided the impetus to study its effects in treating human breast cancer.

Estrogen is the common link between most breast cancer risk factors, i.e., genetic, reproductive, dietary, lifestyle and environmental. It both stimulates the division of breast cells (healthy as well as cancerous) and, especially in its 'bad' form, increases the risk of breast cancer. Thus, hormonal drugs such as tamoxifen that block the effects of estrogen on the breast were expected to reduce the risk of breast cancer recurring in women treated for breast cancer.

Tamoxifen acts as a weak estrogen by competing for estrogen receptors much as phyto-estrogens do(I want you to keep this word PHYTO ESTROGENS IN MIND WE WILL COVER IT AGAIN LATER). Like phyto-estrogens, tamoxifen has mild estrogenic properties but is considered an anti-estrogen since it inhibits the activity of regular estrogens. More accurately, tamoxifen is an estrogen-blocker(Not a estrogen reducer)
HORMONAL EFFECTS OF TAMOXIFEN IN OLIGOSPERMIC MEN -- WILLIS et al. 73 (1): 171 -- Journal of Endocrinology

Yes the test shows over time that both lh and androgins were raised, but at the same time (serum level estrogen was tripled)and thus the reason many experence rebound gyno after its use.

Tamoxifen fights breast cancer by competing with estrogen for space on estrogen receptors in the tumor tissue. Every tamoxifen molecule that hooks onto an estrogen receptor prevents an estrogen molecule from linking up at the same site. Without a steady supply of estrogen, cells in an estrogen-receptor-positive (ER+) tumor do not thrive and the tumor's ability to spread is reduced.

However, tamoxifen exhibited two conflicting characteristics. It could act either as an anti-estrogen or as an estrogen. Therefore, while tamoxifen is anti-estrogenic to the breast, it also acts as an estrogen to the uterus and, to a lesser extent, the heart, blood vessels and bone. Moreover tamoxifen also acts as an estrogen in the liver thus causing the lowering of IGF-1
In This Issue -- 82 (21): 1661 -- JNCI Journal of the National Cancer Institute
http://cancerres.aacrjournals.org/cg.../49/7/1882.pdf
Effect of low dose tamoxifen on the insulin-like growth factor system in healthy women
Comparison of Tamoxifen and Testosterone Propionate in Male Rats: Differential Prevention of Orchidectomy Effects on Sex Organs, Bone Mass, Growth, and the Growth Hormone-IGF-I Axis -- Fitts et al. 25 (4): 523 -- Journal of Andrology

For people suffering from breast cancer I guess this would be a good thing. Since Lowering IGF would reduce the growth of everything. However this is not one any of the people using nolva for pct or on cycle use want now is it?

So, although it initially showed the tendency to counter breast cancer recurrence, it would soon be revealed that it also promoted particularly aggressive uterine and liver cancers, caused fatal blood clots and interfered with many other functions.

Doctors, however, were quick to jump on the tamoxifen bandwagon, turning a blind eye to its more injurious tendencies. Starting in the 1970's oncologists began using tamoxifen to treat women with cancer, often in combination with other drugs, radiation or surgery such as lumpectomy and mastectomy, with modest success. Like DES, tamoxifen's benefits were then extended for use as a preventive against osteoporosis and heart disease.

Today, doctors are treating about one million American breast cancer patients with tamoxifen, about 20 per cent of them for more than five years. As studies published in the New England Journal of Medicine in 1989 and the Journal of the National Cancer Institute in 1992 showed, women with breast cancer who took tamoxifen reduced their chances of developing cancer in the other breast (contralateral cancer) by about 30 to 50 per cent. These findings would later be challenged.

Tamoxifen is now recommended for all pre-menopausal women with hormone-positive cancers, as well as for most postmenopausal women with breast cancer and/or a growing number of women with hormone-negative cancers. Tamoxifen is currently used by more women with breast cancer than any other drug.

Tamoxifen (brand name Nolvadex) is now the most widely prescribed cancer medication in the world. It generated revenues of US $265 million in 1992. By 1995, worldwide sales of Nolvadex reached $400 million. (7) And at AUD $90 for one month's supply, it doesn't come cheap (the Australian Pharmaceutical Benefits Scheme covers $70).
Global sales of tamoxifen in 2001 were $1,024 million.[54] Since the expiration of the patent in 2002, it is now widely available as a generic drug around the world. Barr Labs Inc had challenged the patent (which in 1992 was ruled unenforcable) but later came to an agreement with Zeneca to licence the patent and sell tamoxifen at close to Zeneca's price.[55] As of 2004, tamoxifen was the world's largest selling hormonal drug on record and off record may be the number 1 selling drug in word of all time to date. So we are truly talking about billions in revenue world wide for drug companies,sources,ug's and more. Money is at the root of this drug and why its so heavily pushed on all forums by everyone. Its cheap to make and it brings in billions plain and simple.

These numbers are nothing compared to what this drug now makes for the drug companies,sources.ug's selling it. So you can bet your life they will make sure every test and study in the world is published to make sure its seen in a good light. This not even including its "off label use" Ie all us men using it for on cycle and pct. The use of the drug for this reason triples its sales and you can just emagen the amount of money its making. You do the math my friends!. At this very moment 500000000 sources and people with monitary ties to this drug are out there pushing like crazy to make sure you and everyone else keeps its use for pct alive. This is the #1 reason why we have not given up on this years ago.

Tamoxifen was developed by UK-based Imperial Chemical Industries (ICI), one of the world's largest multinational chemical corporations. Zeneca, an ICI subsidiary, is responsible for manufacturing and marketing the hormone and is now the world's largest cancer-drug company.
CARCINOGENENIC EFFECTS
It wasn't long before laboratory studies showed that tamoxifen acted as a carcinogen. It has been found that tamoxifen binds tightly and irreversibly to DNA, the genetic blueprint of a cell, causing a cancerous mutation to take place. Even Australia's conservative National Health and Medical Research Council (NHMRC) warned that no amount of tamoxifen is safe when it comes to carcinogenic effects.

In California there is a law called "Proposition 65" that requires the state to publish and maintain a list of all known carcinogens. In May 1995, the state's Carcinogen Identification Committee voted unanimously to add tamoxifen to its list.

When research is done on anti-cancer drugs (such as SERMs), the aim is to find a drug that prolongs life, with the least amount of acute side-effects. In other words, the goal isn’t so much about finding a cure, as it is finding something that can alleviate the symptoms and/or prolong life.

When it comes to steroid users so many are willing to forgo any and everything to get the one simple effect they desire (recovery). The popularity of these drugs stems from the popular advice to use these drugs for everything from testosterone recovery.***** tits,make your **** grow bigger, increase the amount of jiz you drop on a girls face, and everything in between. Advice on its use is handed out like candy and everyones got a sweat tooth for quick advice. Of course many "vets and so called know it alls" defend it to the death and it can do no wrong. Mainly do to not wanting to be wrong,habit,they got money involved with it, or just for the sake of argument.

“Its FDA approved for cancer treatment. It must be safe!”

It’s wrong to assume that an “FDA approved” drug has a proven safety profile. The FDA has continually issued stronger health warnings for tamoxifen over the years. For instance, in 1994 the FDA demanded that the tamoxifen manufacturer Zeneca (an ICI sub-division), issue warning letters to health care practitioners about the increased risk of endometrial and gastro-intestinal cancers with tamoxifen use. Zeneca also reported adverse effects similar to those seen with DES, such as reproductive abnormalities in the animals whose mothers received tamoxifen. (remember, DES was the original synthetic estrogen, and also an analog to tamoxifen)

A number of cancer researchers have pointed out the health risks too, such as Elwood et al (6) -

“[Tamoxifen], therefore, is not appropriate for use in the general population because of the known increased risk of endometrial cancer”


What Are Side Effects Of Temoxifen

You Can Get Blood Clots!

Have you any idea that a regular dosage of Tamoxifen can actually increase the chances of blood clots? Well, this is a true fact and can be fatal for those who are using this drug to get rid or avoid the chance of getting Gyno on cycle and or for pct. According to recent medical studies, it has been noticed that people who have been using Tamoxifen on a regular basis have had a substantial increase in terms of their blood clots. Hence, as compared to those people who are not using this drug, their chances of getting blood clots is relatively higher.

A blood clot can be defined as an internal body mechanism by which the cut can be stopped from bleeding excessively. The proteins present in your blood work along with the platelets and in a bid to form a clot. This is also termed as coagulation. In the event of an injury, this can prove to be really very effective as it would stop the flow of blood from your wound and thus save your life. Nonetheless, if the blood clots while it is moving through your body, it can prove fatal. This is also termed as hyper coagulation and it can prove very dangerous for the concerned individual. Tamoxifen has been known to cause hyper coagulation and hence, it needs to be taken under strict medical supervision.

When the study was conducted, it was ascertained that a relatively large number of people developed this conditions and although not many people using this drug were actually studied, those that were using it regularly, were in a shock to find out that it also led to blood clots.

Hence, although this drug is helpful to a certain extent, we need to also see that the extent of damage it can do to our body in terms of hazardous blood clots are much more and hence, you as a steroid user need to exercise caution and spend some quality time researching on this so called ‘wonder-drug’ before making it an eminent part of your daily routine and or pct.

One of the main reasons why a blood clot is considered dangerous is because this drug causes a clot inside the blood vessel which in turn is known as thrombus. What happens is that at times this blood clot can travel through your blood streams and get pushed into your lungs. When this happens, you can be rest assured that your life is in acute danger as this condition is life threatening. This condition is also known as pulmonary embolus. Similarly, a clot this clot can also block the blood vessels in the brain and this in turn may lead to a stroke. When this blood clot clocks the blood vessels of your heart, it stops the blood from rushing to your heart area thereby reducing the oxygen supply to that area. This in turn leads to cardiac arrest.

All the above mentioned conditions arising from blood clots, which in turn are caused from a regular intake of Tamoxifen, can prove to be life threatening for the concerned individual. Hence, even before you decide to take this medication on a regular basis, you need to exercise caution and be prepared to face the ill effects of this so called ‘wonder-drug’.



Increased susceptibility to gyno -

Tamoxifen is often used to combat gyno during cycle when “flare ups” occur. While tamoxifen may provide immediate inhibition of proliferation, and serve as valuable tool, it can actually increase future susceptibility to gyno.

This is caused by tamoxifen’s ability to up-regulate the progesterone receptor. (54-56) This can dramatically increase the chances of developing gyno in future cycles when utilizing progestin based anabolics such as Nandrolone (Deca) or Trenbolone (or any pro-hormone acting upon the progesterone receptor).

It is interesting to speculate. Is tamoxifen use directly related to the increased gyno occurrences seen with modern day steroid users?


You Can Develop Cataract!

Cataract can be defined as a thin white layer of membrane which blocks the passing light to the retina thereby clouding your vision. Although it is relatively painless, it does cloud your vision and can even blind you if it is not removed through the means of a surgical procedure. The retina is ideally a nerve layer which is located at the back of the eye socket and its main purpose is to direct the light which is entering the eye via the means of electromagnetic signals to the brain. Once the brain receives these nerve signals, it is passed on to the nervous system, after which you can transform your vision into clear moving pictures. If this thin layer of membrane is blocked owing to any reason, you would have problems with your vision.

While aging is looked on as the major cause behind cataract, it has recently been noticed that patients using Tamoxifen have been identified as ones susceptible to cataract on a regular basis. people who are aging and using this drug on a regular basis are on a higher risk of contracting cataract as compared to those who are not using Tamoxifen. The other eye problems that can be faced by individuals include scarring of the corneal area and abrupt retinal changes.

In case you are using this drug regularly and you have a cloudy, fuzzy or foggy vision, you need to get your eyesight checked with immediate effect. In case you are unable to withstand the glare of lamps and are unable to catch a glimpse of the morning sun, then again you need to get your eyes checked. This is so because, Temoxifen has a natural tendency to obstruct the normal eye vision and if you do suffer from this symptom, you may not be able to drive at night as the headlamps of the opposing vehicle may blind you momentarily.


In order to get rid of cataract that has been developed owing to a continuous intake of Temoxifen, you may need to undergo a corrective surgery. In case you want to delay a surgical procedure, you may want to light up your room with plenty of tubes and bulbs and keep your eyeglass up to date with the latest prescription. Ideally, the only known cure for cataract that has been a resultant of Temoxifen is a surgical procedure.

If you would like to avoid this problem, you would have to seek an alternative to Temoxifen at the earliest given opportunity.



Libido reduction & erectile dysfunction
Erectile dysfunction ow libido, and general impotence are typical complaints from men recently discontinuing steroids or HRT therapy, which is often combated by Clomid or Nolvadex, paradoxically so.

Regardless of any positive effects on fertility or testosterone levels, Clomid and Nolvadex use is highly correlated with erectile dysfunction, libido suppression, and even emotional disorders Research with male breast cancer patients has also reported decreased libido, and thrombosis associated with tamoxifen use. he thrombotic effect (blood vessel clogging) could explain the mechanism by which SERMs may inhibit erectile function, by reducing circulation to erectile tissue (as discussed before)


Nolva/clomid both raise shbg.
This is something I do not see a lot of people disusing so I I wanted to make it well know. Just do a web search on TAMOXIFEN,clomid or nolva raises shbg or any variation and you will get all the studies and prof you need.
Trait Anxiety and Tamoxifen Effects on Bone Mineral Density and Sex Hormone- Binding Globulin -- Cameron et al. 64 (4): 612 -- Psychosomatic Medicine
iHOP - Information Hyperlinked over Proteins [ SHBG ]
Sex Hormone Binding Globulin in Clinical Perspective; Acta Obstetricia et Gynecologica Scandinavica - 66(3):Pages 255-262 - Informa Healthcare
Wiley InterScience :: Session Cookies

2. Nolva lowers Igf-1 Again just a simple search on (TAMOXIFEN or nolva lowers IGF 1 and walla you got all the prof you need.

In This Issue -- 82 (21): 1661 -- JNCI Journal of the National Cancer Institute
http://cancerres.aacrjournals.org/cg.../49/7/1882.pdf
Effect of low dose tamoxifen on the insulin-like growth factor system in healthy women
Comparison of Tamoxifen and Testosterone Propionate in Male Rats: Differential Prevention of Orchidectomy Effects on Sex Organs, Bone Mass, Growth, and the Growth Hormone-IGF-I Axis -- Fitts et al. 25 (4): 523 -- Journal of Andrology


They can cause Major triglyceride and glucose problems and even to the point of Severe hypertriglyceridemia or also Pancreatitis

Severe hypertriglyceridemia caused by tamoxifen-tr... [Endocr J. 1997] - PubMed result
Tamoxifen-induced hypertriglyceridemia in association with diabetes mellitus - EM|consulte
SpringerLink - Journal Article
Capecitabine-Induced Severe Hypertriglyceridemia: Report of Two Cases -- Kurt et al. 40 (2): 328 -- The Annals of Pharmacotherapy
Elsevier: Article Locator
Estrogen and Triglycerides
http://annonc.oxfordjournals.org/cgi.../11/8/1067.pdf
WikiGenes - Hypertriglyceridemia


A word on clomiphene (Clomid) –

Clomiphene (Clomid) consists of two stereoisomers which possess radically different pharmacodynamics. Zuclomiphene has predominantly estrogenic effects and slow clearance while the enclomiphene isomer has predominately anti-estrogenic effects and quick clearance. his creates a divergent effects between estrogen blockage and estrogen stimulation and an acute imbalance once Clomid administration is discontinued. Bodybuilders will often complain of “estrogenic rebound” after stopping Clomid, which could be attributed to the lingering estrogenic isomer zuclomiphene as the anti-estrogenic enclomiphene has long cleared the system. (Recently, enclomiphene has been isolated by the pharmaceutical company Repros, for use in Androxal™.)

For all intents and purposes, tamoxifen is a superior SERM, simply for the fact that tamoxifen provides a purely anti-estrogenic isomer, whereas Clomid provides a mix of anti and pro estrogenic effects.

In regards to the health consequences about to be listed, it can be safely assumed that Clomid will share similar detrimental effects as tamoxifen, since it shares the same triphenylethylene backbone and carcinogenic tendencies.


One of the main reasons why people make use of Clomid is for the purpose of recovering their bodies after a steroid cycle In simple words, this drug is mainly used in the form of post cycle therapy. Clomid has the actual potential to stimulate the production of hypothalamus which in turn would release a particular kind of hormone called gonadotrophic hormones. This hormone has the natural ability to allow the human testicles to secrete testosterone, which in turn would bring the depleting levels of testosterone in the body to its permissible levels. When this is achieved, the human body would stop losing its muscle mass in a natural way. Reacovery of test production is the gaols at any cost is the common thought.


Its a known fact that both clomid and nolvadex cause some really messed up mood swings.
Clomid/nolva have been known to cause severe mood swings in users and it has apparently been noticed that anyone who has been making use of Clomid/nolva have suffered from such side effects on a regular basis. Many users have categorically complained that the use of Clomid has been considered as the worst side effect that they have suffered so far. A few features of mood swings may include a change in the usual behaviour, tearful behaviour, excessive depression, anxiety and extremely sensitive in nature. Stop acting like you don't know what I am talking about. We all know its true.


Liver cancer -

Originally, tamoxifen was accepted as being non-toxic to the human liver upon finding that tamoxifen did not cause noticeable liver damage (DNA adducts) during short-term test tube studies with human liver cells.

However, it became apparent that test tube research was largely flawed due to the low rate of metabolism in such a superficial environment. It was soon discovered that the hepatotoxic effects from tamoxifen stem from the metabolism and buildup of the a-hydroxytamoxifen and N-desmethyltamoxifen metabolites, which would only appear in an in vivo environment. Surely enough, the results from the original rat studies showing dramatic carcinogenic effects on the liver, soon correlated with human data when researchers found the same type of liver DNA adducts in tamoxifen patients.

More recent human research has reported tamoxifen treated women to have 3x the risk of developing fatty liver disease, which occurs as soon as 3 months into therapy at only 20mg/day. In some cases, the disease lasts up to 3 years, despite cessation of tamoxifen therapy. Five and ten year follow-ups with patients on long term tamoxifen therapy show cases of deadly hepatocellular carcinoma.

In 2002, a bizarre study examined the use of tamoxifen for hepatocellular carcinoma treatment in humans. It was assumed that since tamoxifen could inhibit proliferation of breast cancer, it could offer the same benefit for liver cancer. The devastating results could not have been more indicative of tamoxifen’s hepatotoxic nature, as the tamoxifen treatment significantly increased the rate of death, compared to the group not receiving tamoxifen.

Finally, in a case study reviewing tamoxifen induced liver disease; D.F Moffat et al made a profound statement –

“Hepatocellular carcinoma in tamoxifen treated patients may be under-reported since there may be reluctance to biopsy liver tumours which are assumed to be secondary carcinoma of the breast.” In other words, it appears that liver carcinomas from a large number of breast cancer patients on tamoxifen therapy have been misdiagnosed as an infection from the breast cancer itself.

Although tamoxifen induced liver cancer may take years to manifest in a healthy male, its damaging effects could easily be exaggerated by other popular hepatotoxic drugs, such as 17aa oral steroids.


The main reason for this Thread is not to say (never use them again) as I know the title would have one to believe ha ha its an attention getter title guys. But to make you well aware of the negative effects and the fact that we have advanced. Many new drugs and many new products have been effectively used in place of these harmful drugs. At the very least lowering the dosage amount and length at which they are used, and replacing the higher doses with other pct products or estrogen reducing products is the best way to go now.
 
alot to read i know :(

but heres my main question about the full cycle i made a few and wanted some profs who used it to look into and tell which is best:

Cycle 1
1-2 Beastdrol - 1 capsule 2 times a day spread out morning and night. i wanna build up tolerance in 1st week
2-4 Beastdrol - 1 capsule 3 times a day spread out morning, Noon, and night.
2-10 Forma Stanzol - starting 3 pumps for tolerance then raise to 5 pumps rubbed on your chest 2 times a day morning and night.
2-5 HCgenrate - 5 caps a day
1-4 Forged Joint Repair - 1 capsule 2 times a day morning and night. (Dunnow If I Really Need This?)
1-4 Forged Liver Support - 1 capsule 2 times a day morning and night.
4-8 Forged Post Cycle - 2 capsules 2 times a day morning and night.
4-8 Unleashed / Post Cycle - 3 caps a day (Dunnow If The Xtra Bottle Post Cycle Is Nesecery?)

Or
Cycle 2
2weeks prior to Beast - N2Guard untill 2 weeks after full cycle. (good idea or no??)
1-4 Beastdrol - 1capsule 3 times a day spread out morning, Noon, and night.
1-4 Forged Joint Repair - 1 capsule 2 times a day morning and night.
1-4 Forged Liver Support - 1 capsule 2 times a day morning and night.
1-4/5 HCGenerate 5 caps a day / or Transaderm or both???
4-8 Forged Post Cycle - 2 capsules 2 times a day morning and night.
4-8 Unleashed / Post Cycle - 3 caps a day (Dunnow If The Xtra Bottle Post Cycle Is Nesecery?)
4-8/10 Forma Stanzol - starting 3 pumps for tolerance then raise to 5 pumps rubbed on your chest 2 times a day morning and night.
4-8 Liquid Torem (Only wanna use if gyno is starting)

Or

Cycle 3
2weeks prior to Beast - N2Guard untill 2 weeks after full cycle. (good idea or no??)
1-2 Beastdrol - 1 capsule 2 times a day spread out morning and night. i wanna build up tolerance in 1st week
2-4 Beastdrol - 1 capsule 3 times a day spread out morning, Noon, and night.
1-4 Forged Joint Repair - 1 capsule 2 times a day morning and night.
1-4 Forged Liver Support - 1 capsule 2 times a day morning and night.
1-4/5 HCGenerate 5 caps a day / or Transaderm or both???
4-8 Forged Post Cycle - 2 capsules 2 times a day morning and night.
4-8 Unleashed / Post Cycle - 3 caps a day (Dunnow If The Xtra Bottle Post Cycle Is Nesecery?)
4-8/10 Forma Stanzol - starting 3 pumps for tolerance then raise to 5 pumps rubbed on your chest 2 times a day morning and night.
4-8 Liquid Torem (Only wanna use if gyno is starting)


Wich cycle wud be the best or did i forget annything or put to much up?

the change betweem them is small but cud do some diffrence thats why im asking and i put torem up instead of nolva/clomid!
 
i guess im confused as to why you would write you only want to use liquid torem if gyno is starting... you have to run a serm in your pct with beast bro... its as simple as that...

do beast 1-4... test your tolerance the first week and move on from there
you need to run n2guard through the cycle... you can preload for a week with hawthorne and milk thistle or n2guard itself...
TRANSADERM is what you want to run with this... run it 1-4
forma is excellent... you need to do 5 pumps a.m. and 5 p.m... you will be fine on tolerance...

pct
torem
unleashed
post cycle
daa
 
ok thats what i was afraid of :P

sow a serm is def needed ;) I will use liquid torem then and i will do the 3rd Cycle sheme then!!!
Made some small changes i think i got ALL COVVERED NOW :)

Cycle 3
1 week prior to Beast - N2Guard untill 1 week after full cycle.
1-2 Beastdrol - 1 capsule 2 times a day spread out morning and night. i wanna build up tolerance in 1st week
2-4 Beastdrol - 1 capsule 3 times a day spread out morning, Noon, and night.
1-4 Forged Joint Repair - 1 capsule 2 times a day morning and night.
1-4 Forged Liver Support - 1 capsule 2 times a day morning and night.
1-4 Transaderm
4-8 Forged Post Cycle - 2 capsules 2 times a day morning and night.
4-8 Unleashed / Post Cycle - 3 caps a day
4-8/10 Forma Stanzol - 5 pumps rubbed on your chest 2 times a day morning and night.
4-8 Liquid Torem Tapperd down
4-8 DAA ( anny specific type or will any D-Aspartic Acid do? )

Then what i got left is the HCGenerate? no use for it or?
 
I DONT WANNA B CONTROVERSIAL BUT I CAME ACROSS THIS ON ANOTHER FORUM
STATED FROM AN NEEDTOGETAAS OFFICIAL SPONSER AND HE WROTE THIS TO SOMEONE WHO WAS GON USE BEAST:


As far as furst cycles go you kind of went right for the most powerful oral steroid you could ever get lol. You skipped a few levels but at least you have the entire cycle planed out fine.

M friend I am the designer and creator of beastdrol and every other product you are also taking. I been in this industry doing what I do not for 5 times as long as everyone in this thread has even been around the forum. THOUSANDS!! Of people have ran the exact same cycle you are about to run some not as well laid out but almost every last one of them loved the cycle and the gains they got from it.

You have a great lay out and about the only thing I would add is Hcgenerate 3 caps am 2 caps pm during the cycle and that is about it. You will have a great cycle, you will recover just fine. If my words do not end up true than Ill refund you all of it my self.

YOU DO NOT NEED TO ADD A SERM TO PCT!!!!!!!!!!!!! Its only going to make you feel like crap and its not going to add a single thing to the pct. Most of the people telling you to do this are doing so simple because they have no Idea what forma-stanzol really is and what is in the product. Its a strong "drug" known as formastan or formally known as Lentaron I.M. Depot
Go ahead and look it up it was a suicidal or also known as ***8220;steroidal***8221; aromatase inhibitor that was made and sold by pharmaceutical companies for many years. Than it also has natural serms/phytoserms that work like a serm would too. On top of that 7,8 Benzo which will brake the blood brain barer and cause the release of gNRH..

With the added post cycle a fairly good natural test booster your pct will be just fine. I want you to run the cycle exactly how you have it laid out. If your not perfectly recovered after the pct than I will refund you for all of it and buy you everything you need for any other kind of pct you want to do.. But I know for a fact you will be fine... Enjoy and keep me posted.

And this was written by someone else

Quote:
Originally Posted by BarbellBeast View Post
Why not?

There's nothing wrong with a lower dose of SD as a first cycle.

Ya one could always use some Halo but to tell you the truth I didn't get much from the weaker orals.
Halo has no Androgenic affect..it's rated at zero but it's all 100%Anabolic.So if you feel tired...Halo is the one to perk ya up and the muscles will love it!

Quote:
Originally Posted by Needtogetaas View Post
YOU DO NOT NEED TO ADD A SERM TO PCT!!!!!!!!!!!!!
He's right.
Beastdrol will drop your estrogen to zero,with PCT or during it, it will maintain at least some Estrogen in your blood but not enough to give ya ***** tits.


no serm? HCGenerate or transaderm? makes me confused xD

i think i will just stick to my 3rd Cycle as i layed out above ;)
 
Also, since this is your first cycle, let YOUR body tell you if you need a SERM or not. Start with a SERM this time, if you feel like s*** the four weeks of PCT lower the doses or just don't use it next time. Those articles you posted were written by those who probably have a couple cycles under their belt...
 
Cycle 3 it is then :D

will order the things i dun have yet soon sow i can start edn april begin mai

i will keep ya'll updated on how its going :)
 
OP why not do three pills at once? I am currently on Beast and I take 3 pills 45 minutes before the gym and my pumps are great. I did one in the morning, one mid-day, and finally one at night for the first week. The three at once I like a lot more.
 
don't think my immune system will shutdown as im very healthy im practicly never sick!

but yes you never know but stil im going for 2 pils a day see how it goes then go up to 3 pils a day!

i ordered the serm sow i shud be good :)



and for mtsingh:
3 pils at once? lol sounds crazy but if you can take it please go on lol :P

im not gonna try that i might try 2 pills in the morning prior to workout and the 3rd in the evening!

but since this is my first time with Beast i think i stick to 3 pills spread out over the day :P

we'll see how it goes and maybe i can change/adjust the 2nd cycle if i decide to do another one :D
 
About keeping gains... yes you will keep gains with the PCT and support supps you are using. Any cycle support from NTBM will help keep gains very well
 
ok thats what i was afraid of :P

sow a serm is def needed ;) I will use liquid torem then and i will do the 3rd Cycle sheme then!!!
Made some small changes i think i got ALL COVVERED NOW :)

Cycle 3
1 week prior to Beast - N2Guard untill 1 week after full cycle.
1-2 Beastdrol - 1 capsule 2 times a day spread out morning and night. i wanna build up tolerance in 1st week
2-4 Beastdrol - 1 capsule 3 times a day spread out morning, Noon, and night.
1-4 Forged Joint Repair - 1 capsule 2 times a day morning and night.
1-4 Forged Liver Support - 1 capsule 2 times a day morning and night.
1-4 Transaderm
4-8 Forged Post Cycle - 2 capsules 2 times a day morning and night.
4-8 Unleashed / Post Cycle - 3 caps a day
4-8/10 Forma Stanzol - 5 pumps rubbed on your chest 2 times a day morning and night.
4-8 Liquid Torem Tapperd down
4-8 DAA ( anny specific type or will any D-Aspartic Acid do? )

Then what i got left is the HCGenerate? no use for it or?

I like the lay out. However like I said you can use this exact same lay out without the torem. These days we replace the plan DAA with D-spark though, Advancements and all ya know :wub:
 
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