DAdams91982
Board Sponsor
Nope... it is a 17aa methyl, therefore a ~99% bioavail rate. The LV only gives you the benefit of modulating the dosage precisely... albeit a huge factor when dealing with SD.
My take on Superdrol
- Thread starter nattydisaster
- Start date
Nope... it is a 17aa methyl, therefore a ~99% bioavail rate. The LV only gives you the benefit of modulating the dosage precisely... albeit a huge factor when dealing with SD.
dumbhick3
Member
You're probably right but I still wander...that LV technology is a bit hard to understand for me (SEEDS, oral, eso****eal, and stomach lining absorbtion, etc).
The only reason I think that the LV could in theory make the same dose slightly stronger than cap form is by rough analogy the fact that injectable winstrol is more potent than oral winstrol since it misses the first pass metabolism in the liver when injected. Both forms are near 100% bioavailable, but the first pass metabolism metabolizes some of that 100% dose so avoiding it means more active in your system at least with winstrol.
I doubt it is anything that dramatic with the LV (if anything at all), and really, I don't think it would be desirable or necessary to enhance the absorption of a dimethyl like superdrol since it is already so resilient to being broken down by the liver (much more than the single methyls). But it has been suggested that absorption of the LV starts in the mouth and the eso****us which to me seems like an avenue for some of the superdrol to avoid first pass hepatic biotransformation (I'm really speculating here).
What say you Trauma?
...RAZORBACK09
Member
Oh okay, I thought I had read that the absorption was 3-4 times more then the pills so I figured 10mg of LV would be maybe like a 30mg of pill.
I'm going to be running tren/SD together (3 weeks SD, 6 week tren) should I just run liver care for the 3 weeks or the whole cycle?
DAdams91982
Board Sponsor
You're probably right but I still wander...that LV technology is a bit hard to understand for me (SEEDS, oral, eso****eal, and stomach lining absorbtion, etc).
The only reason I think that the LV could in theory make the same dose slightly stronger than cap form is by rough analogy the fact that injectable winstrol is more potent than oral winstrol since it misses the first pass metabolism in the liver when injected. Both forms are near 100% bioavailable, but the first pass metabolism metabolizes some of that 100% dose so avoiding it means more active in your system at least with winstrol.
I doubt it is anything that dramatic with the LV (if anything at all), and really, I don't think it would be desirable or necessary to enhance the absorption of a dimethyl like superdrol since it is already so resilient to being broken down by the liver (much more than the single methyls). But it has been suggested that absorption of the LV starts in the mouth and the eso****us which to me seems like an avenue for some of the superdrol to avoid first pass hepatic biotransformation (I'm really speculating here).
What say you Trauma?
I think your knowledge about these are a bit skewed. the whole point of being methylated is the first liver pass, there is no skipping a first liver pass, the first time it goes through the liver is the first liver pass. Methylation prevents the breakdown on the first pass. No matter the point of absorbtion, the molecule enters the blood stream and goes through the liver.
As for winny, I have used both to test out that theory and seen the exact same effects, as have others who have used in the past. I speculate the winny theory is a placebo effect, IE: It's injects = stronger.
Dragon13
Active member
99%? Never heard that before. Reference?
DAdams91982
Board Sponsor
I did my research almost 5 years ago... here is a pretty comprehensive list of research.. knock yourself out.
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Dragon13
Active member
Uh, I've seen this page at Rx. NONE of the information there quotes 99% bioavailabilty, and NONE of those studies are even pertinent to the bioavailabilty of AAS.
If you don't have the source, just say so. In any event, absent data to the contrary, I am not quite on board wth ANY 17a- oral steroid being 99% bioavailable.
Trauma1
Legend
I can tell you Halodrol being labeled as "mild" is a misnomer. Again, this is where guys read anecdotal reports around the internet and take them as some kind of valid and substantiated reference; when in reality, you should take them for nothing more than an entertaining read.
I'm all about the science, not the hearsay.
- John
Trauma1
Legend
You're probably right but I still wander...that LV technology is a bit hard to understand for me (SEEDS, oral, eso****eal, and stomach lining absorbtion, etc).
The only reason I think that the LV could in theory make the same dose slightly stronger than cap form is by rough analogy the fact that injectable winstrol is more potent than oral winstrol since it misses the first pass metabolism in the liver when injected. Both forms are near 100% bioavailable, but the first pass metabolism metabolizes some of that 100% dose so avoiding it means more active in your system at least with winstrol.
I doubt it is anything that dramatic with the LV (if anything at all), and really, I don't think it would be desirable or necessary to enhance the absorption of a dimethyl like superdrol since it is already so resilient to being broken down by the liver (much more than the single methyls). But it has been suggested that absorption of the LV starts in the mouth and the eso****us which to me seems like an avenue for some of the superdrol to avoid first pass hepatic biotransformation (I'm really speculating here).
What say you Trauma?
I'll answer this tomorrow; my bed is calling me right now.
- John
fueledpassion
Well-known member
Yeah I read on one of Eric Potratz's articles on PP's website that it only takes about 3 days for near complete shutdown..( I think )
RAZORBACK09
Member
So if stacking with tren, should it be used first 3 weeks or last 3? I've gotten mixed reviews so I'm trying to figure it out before I go on cycle.
DAdams91982
Board Sponsor
Suit yourself. You can go ask Matt from DS though, he will definitely reconfirm my statement... since he is the master of methyls... he keeps all his research by his side, I on the otherhand could care less if someone believes me or not.
Although checking the A;A ratio of these methyls, and seeing that something as low as 2.5mg of SD can give results, that would have to tell you logically that every last mg will have to be absorbed... be that as it may, it is your right to disagree.
the GUNSHOW
Member
hey man how long of a cycle do you think some one can do at just 10mg?
younganabolic
Member
I think you should do it the last 3 weeks just because superdrol takes a while to kick in
p5sky
Well-known member
I noticed some nice strength gains on day 2 of 5mg. I have never run SD so that may have an effect of the compound. I mostly have noticed gains in shoulders and legs. Squats I have been able to push more wt at good reps at the end of my sets. I usually did 3 sets 225x8, then 245x6, 275x2/3. My 2nd day of SD was squat day and I EASILY did my 3x225x10, 245x8, 275x8, 305x2. Still more energy but did not want to push it and get hurt. Yesterday I did 2 sets of 315x3 PR!
dumbhick3
Member
Sledge is quite knowledgable in these things. I wouldn't waste his time
.But sometimes there is more to the picture than just near 100% bioavailability (just my opinion).
This is more what I was inferring with the winstrol analogy:
I think that most hepatic-metabolized injectables (IM/IV/SC) do miss the first pass hepatic biotransformation in the liver by being absorbed into the bloodstream first (thus exerting immediate effects at 100% of the injected dose before reaching the liver and being metabolized for the first time-the "second metabolism" according to the article below).
On the other hand, orals go straight from the stomach to the liver and then exert their effects (and undergo more extensive hepatic metabolism consequently). I am oversimplifying here and leaving out some details.
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Most ppl know what SHBG is (I hope
), but this article got me thinking. Winstrol is usually not run solo if you have much respect for your joints (ppl do it, but not too often).So could it be that oral winstrol seems as potent as injectable winstrol b/c the oral binds SHBG to a much greater degree than the injectable, and consequently, the other steroids that you are stacking the oral with benefits from lowered SHBG (and your own endogenous test for that matter since estrogen isn't going to be much of an issue with solo winstrol due its DHT-derivate AI-like effects)? This SHBG discussion is just a theory to try and explain oral vs inject winstrol subjective effects, though the above link has some interesting graphs and more commentary on the subject.
It's interesting that Anthony Roberts suggests that winstrol may have less than 100% bioavailability. If I didn't quote it above, I think it is somewhere in that article I linked to. By the way, I am not insinuating that he is an expert; maybe he is; I don't know honestly.
I guess another quasi-example would be morphine (I know; nothing like a steroid). It has very poor oral bioavailability and increasingly high bioavailability as you go from SC to IM to IV (the latter being 100%). It's not methylated (that would be codeine/methylmorphine, lol, and it still sux) as with the steroids being discussed, but the reason that morphine has such horrible oral bioavailability is due to the first pass hepatic metabolization which wipes out most of an oral dose of it, leaving about 10-15% or so to enter the bloodstream (rough guess). 17a-methylated steroids are much more resilient orally of course, though other methylations like 1a- and 3a- aren't necessarily so resilient. Also, with the morphine illustration again, the time to onset of effects is directly related to the route of administration and how fast 100% of it or 10% of it can reach the bloodstream, then opioid receptors, etc. And finally, the duration of effect of morphine is inversely related to how quickly it gets into the bloodstream.
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Much of this isn't directly applicable to methylated steroids, but it is interesting to speculate that IM winstrol could possibly be acting like a "mini-depot" injection for lack of a better word due to its avoidance of first pass metabolism and entering the bloodstream before reaching the liver, and still being very resilient when it gets there due to 17a-methylation, etc. The "mini-depot" idea could explain why EOD injections are often used interchangeably with ED tabs. Again, just more speculation.
You have used both of them and are obviously quite knowledgable, so I don't question your opinion (I respect it).
My opinion (and it is just an opinion) is that based on anecdotal feedback from friends, some of Seth Roberts' comments in Anabolic Pharmacology regarding oral vs inject winstrol, and the article above, I am still inclined to believe that the injectable winstrol is more potent than the oral version (and possibly even a bit less strenuous on the liver, though I haven't read anything to substantiate that).
So back to Superdrone LV (lol), it seems like Trauma's got some 'splaining to do to let us know if any of that superdrol LV dose could possibly go directly into the bloodstream and avoid the first pass "gut metabolism" that a cap of superdrol would undergo in full (of course, there is microdrol-sublingual right? anybody try that?).
I am going to go out on a limb to answer one recurring question and say (speculatively) that no, 10mg of superdrol lv does not equal 30mg of superdrol caps. If there is a difference in end effects, it would be smaller than that.
Good discussion; I am learning quite a bit along the way.
BigBlackGuy
Well-known member
I have talked to Bill Roberts in the past about his 2-on 4-off cycle method. Here is the case study for reference: (cant link without 50 posts) mesomorphosis. com/articles/pharmacology/steroid-case-study-01.htm
You can see they have blood tests done on the "lab rat". Suppression had not begun, nor had liver damage, when the two weeks were up. In some cases (I believe it is mentioned in the above link) that his HPTA was upregulated after the 2 weeks, some kind of rebound effect. The above link also does not mention Superdrol or any other Sdrol clone.
Can this method be applied to Superdrol? Sure. Will it work? Maybe. You have to know how your body responds.
In reference to Unreal's comments about 2 weeks not being magical, he is right. Maybe 1 week and 6 days. Maybe 2 weeks and a day. The point is that 2 weeks worked. It isn't magical, not exact, but in the case above, yes it did work. That is the point. Bill has certainly never said anything like that either. I don't know of anyone else who supports 2-on 4-off.
Also, what is this 2-on 2-off? Is that even a real thing? Or do people just want fast results so they warp Bill's work? Although he HAS mentioned it, I don't think he has ever done a study on it. His recommendation is a 1-3 ratio of on and off. So don't expect to be on for half the year and be suppression/sides free.
As a side note, why would Sdrol be more suppressive than something like dbol? If taken at the correct effectiveness to dosage ratio... I feel as though Sdrol wouldn't be extra suppressive.
Bottom line? People seem to be wanting results too quickly. There's always a factor missing when people say that training, diet, and recovery are the only parts of the equation when it comes to building muscle and getting stronger. That factor is time!
You can see they have blood tests done on the "lab rat". Suppression had not begun, nor had liver damage, when the two weeks were up. In some cases (I believe it is mentioned in the above link) that his HPTA was upregulated after the 2 weeks, some kind of rebound effect. The above link also does not mention Superdrol or any other Sdrol clone.
Can this method be applied to Superdrol? Sure. Will it work? Maybe. You have to know how your body responds.
In reference to Unreal's comments about 2 weeks not being magical, he is right. Maybe 1 week and 6 days. Maybe 2 weeks and a day. The point is that 2 weeks worked. It isn't magical, not exact, but in the case above, yes it did work. That is the point. Bill has certainly never said anything like that either. I don't know of anyone else who supports 2-on 4-off.
Also, what is this 2-on 2-off? Is that even a real thing? Or do people just want fast results so they warp Bill's work? Although he HAS mentioned it, I don't think he has ever done a study on it. His recommendation is a 1-3 ratio of on and off. So don't expect to be on for half the year and be suppression/sides free.
As a side note, why would Sdrol be more suppressive than something like dbol? If taken at the correct effectiveness to dosage ratio... I feel as though Sdrol wouldn't be extra suppressive.
Bottom line? People seem to be wanting results too quickly. There's always a factor missing when people say that training, diet, and recovery are the only parts of the equation when it comes to building muscle and getting stronger. That factor is time!
dumbhick3
Member
I don't know where the 2 on/2 off idea came from myself; it seems like a hormonal rollercoaster, but that's just my opinion.
Me and my nuts are tight, but I'd be most concerned about liver failure which I hear causes impotence and potentially death
.Interesting question. My guess is that since neither has appreciable effects on the PR, superdrol may be more suppressive due to its dimethylation, differences in A:A ratios of 400:20 versus 90-210:40-60 which seem to pan out in real life and not just on paper (not a scientific answer I know), and anecdotal feedback on sdrol. Also, d-bol provides more androgenic support than sdrol by itself and via its highly androgenic 5AR metabolite M1T (900-1600:200-300). Bridging with low doses of d-bol is also not unheard of, so between d-bol and sdrol, I'd say that d-bol has more androgenic support and similarity to test than sdrol (so kind of a quasi-HRT effect). I don't know if anyone has gotten intracycle bloodwork done on superdrol though. I'd like to see some hormone values at 2, 3, or 4 weeks on cycle.
Taking the high dose approach, it seems anecdotally at least that 30mg/day of superdrol would be more suppressive than 100mg/day of d-bol, but I'm just speculating and still not really answering your question very well.
Clin Sci (Lond). 1981 Apr;60(4):457-61
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BigBlackGuy
Well-known member
Agreed. I've only heard proposals for 2-on 2-off, never any that were completed. That's probably not a good sign.
Me and my nuts are tight, but I'd be most concerned about liver failure which I hear causes impotence and potentially death
I think the liver failure is over stated. If every bad thing I heard about a steroid were true, half of this forum would be dead, not to mention there are tons of horrible clones being produced, along with the general disdain from the roid "vets" for designers.
I didn't think about the ratio between Anabolic/Androgenic when I made the post. The ratio shows that Sdrol is going to better (anecdotally, of course) for retaining gains than Dbol, so if we talk strictly a Dbol only cycle (foolish, yes) or an Sdrol only cycle, Sdrol is probably going to come through. Of course, as you said Dbol is used generally for bridging, and it's rarely used alone.
True, I suppose it would have to be an issue of how long does it take to recover hormone levels compared to how well the gains last. If you do a dbol only cycle and gain 20 lbs, and recover fast, you might hold a decent amount of the gains. If you take sdrol and gain 20 pounds and dont recover quickly, even assuming sdrol is better for retaining gains innately, then you might not keep too much.