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  • Manufactured by: GlaxoSmithKline

Buy Albuterol - 100 tabs each contains 4 mg Albuterol Sulphate

For strength athletes, bodybuilders and others who are seeking to improve performance or their physical appearance, albuterol offers numerous benefits. For the most part, it is most often considered a “fat burner” in the bodybuilding community. This is due to the ability of the drug to stimulate fat cells, increase lypolysis, decrease appetite, increase body temperature, as well as increasing basal metabolic rate, among other things (1). All of these factors, when combined with proper diet and training, would obviously help to increase the rate of fat loss in users. However the use of albuterol is not limited to simply fat loss. There is evidence that it can help to dramatically improve athletic performance as well as helping to contribute to anabolism.

There's pretty compelling evidence that shows albuterol is just about as effective as clenbuterol at increasing anabolism, with one exception: Albuterol is effective at "clinically safe" doses (in man), and clenbuterol is not. In other words, in order to achieve an anabolic effect from clenbuterol, you need to exceed its safety limits (which is not necessarily dangerous or undesirable for us healthy bodybuilder types).

On the other hand, albuterol, at clinically safe doses, increases whole-body protein content in rats by 20% in just three weeks! So it really does increase protein synthesis. Furthermore, there are several studies that show albuterol is effective at significantly increasing power output and muscular endurance in man. Additionally, albuterol is heart healthy, prevents muscle catabolism, and is a pretty darn good asthma medicine to boot. By all indications, albuterol should be effective for at least three to four weeks at increasing muscle mass before you need a week off from use. And from a personal experience, this bears out as well. I've had reasonably good success with albuterol, and I suggest anyone who has access to the drug to give it a try. I recommend starting with 2mg a day then up to 16 mg a day, taken in either two doses spaced 8-10 hours apart, or four doses spaced about four hours apart. Go on cycles of 3-4 weeks on, one week off. Be careful about stacking other adrenergic agonists, like ephedra, with albuterol. If you can tolerate the combination, go for it, but test it out first. The half-life of albuterol is about five hours, so if the doses are too frequent, there's a cumulative effect that could get the better of you, sending your heart into an arrhythmia that rivals the tempo of a hummingbird's wings. Just be aware that there are enormous tolerance differences between people. So start out slowly with minimal doses until you get a handle on how your body reacts to these compounds. And regarding aspirin, bag the idea of using it for anything other than pain control. Stacking it with stimulants is out of date and actually counterproductive.

So now that it has been established that albuterol has significantly less potential damaging side effects then clenbuterol, the differences in their efficiency in terms of lypolysis and performance enhancement can be explored. Since the primary difference between the two compounds is their half lives, it is obvious that if single doses of the separate drugs were given, clenbuterol would have a much longer lasting effect on the user and the effects of the drug would be active for a longer period of time. However this benefit of clenbuterol is circumvented simply by spacing the dosages administered of albuterol to much shorter periods of time. This requires much more frequent dosing, but this inconvenience may be well worth the fact that the effects of the drug cease much more quickly once administration of it is stopped.

Side Effects/Risks

Like all beta agonists, albuterol has major stimulant effects on users. This can lead to side effects such as an increase in blood pressure, increased heart rate an/or palpitations, insomnia, tremors, and increased sweating due to the thermogenic effects of the drug, among others (4). Of course the onset and severity of these side effects will vary from one user to another. It is recommended, as is the case with most drugs, that users begin administering relatively small doses of the compound to determine their tolerance level for it. The user then can slowly increase his or her dosages until they find one which provides them with the desired effects, while not producing side effects that the user would find intolerable.

Another aspect of albuterol use is its apparent effect of decreasing the levels of the amino acid taurine in the serum and the heart of users (6), as mentioned previously. This is a similar trait of other beta agonists. Many users will supplement with taurine to counteract this effect. It is believed that when the body is depleted of taurine, muscle cramps are more likely to occur, although there is no real scientific research that supports this assertion.

It should also be noted that there are some studies which have indicated that beta agonists, of which albuterol is one, can impair cardiovascular endurance and/or performance. However they have also been shown to help increase performance. Obviously like all situations where contradictory research exists, users will have to experiment with the drug themselves and see exactly how they react to the compound.

Heart damage, as indicated earlier, is often a worry among users because of animal studies indicating that it occurs in animals given clenbuterol. Due to the similarity of the compounds, there may be some concern among users that these negative effects that have been associated with clenbuterol use and its impact on the heart may also occur with the administration of albuterol. However there is little evidence that this is an issue. For the most part the scientific research has found no link between albuterol use and detrimental changes in the heart. This may be true for a number of reasons. First, the studies that indicated that clenbuterol caused cardiac hypertrophy and necrosis were conducted with animals. This is important because animals have a larger number of beta 2 receptors then humans.

The lack of heart damage attributable to albuterol use may also be due to the shorter half life of the drug relative to clenbuterol. This possible explanation is theoretical in nature, as no research has been conducted on the subject, but could be a contributing factor. However, the main point to be made is that there is no evidence that albuterol could be directly linked to potential heart damage in a user. For the most part, when used in a cautious manner, albuterol is a very safe drug to utilize.

Medical Abstract

Strength training and albuterol in facioscapulohumeral muscular dystrophy.

BACKGROUND: In animals and healthy volunteers beta2-adrenergic agonists increase muscle strength and mass, in particular when combined with strength training. In patients with facioscapulohumeral muscular dystrophy (FSHD) albuterol may exert anabolic effects. The authors evaluated the effect of strength training and albuterol on muscle strength and volume in FSHD. METHODS: Sixty-five patients were randomized to strength training of elbow flexors and ankle dorsiflexors or non-training. After 26 weeks albuterol (sustained-release, 8 mg BID) was added in a randomized, double-blind, placebo-controlled design. Primary outcome was maximum voluntary isometric strength (MVIC) at 52 weeks. Secondary outcomes comprised dynamic strength and muscle volume. RESULTS: Training and albuterol were well tolerated. Training of elbow flexors did not result in a significant effect on MVIC, but dynamic strength improved significantly. Elbow flexor MVIC strength increased significantly in albuterol vs placebo treated patients. Ankle dorsiflexor strength decreased in all groups. Eleven out of twelve non-trained muscles in the albuterol group showed a positive effect on MVIC compared to the placebo group (p < 0.05 in seven muscle groups). Muscle volume decreased in the placebo-treated, and increased in the albuterol-treated patients. No synergistic or antagonistic effects were observed between training and albuterol. CONCLUSIONS: In FSHD strength training and albuterol appear safe interventions with limited positive effect on muscle strength and volume. Consequences of prolonged use are presently unclear, which precludes routine prescription.

Salbutamol has been proven just as efficient as clenbutrol and in fact has been proven anabolic even in humans, while clenbuterol has been proven anabolic in animals only. "
Journal of Sport Medicine 1997 Dec
Clarkson PM, Thompson HS
Department of Exercise Science, School of Public Health and Health Sciences, University of Massachusetts, Amherst, USA.

"Salbutamol (2.7 ppm) fed to pigs between weaning and slaughter increased ADG (5%), dressing percentage (2%) and cross-sectional area of the longissimus (LD) muscle (14%). In fatter, White-line-sired pigs, but not in leaner, Meat-line-sired animals, it reduced backfat thickness (25%)." (This means increased muscle mass by 14% and fat decrease by 25%)
Journal Animal Science 1990 Jan
Warriss PD, Brown SN, Rolph TP, Kestin SC.
AFRC Institute of Food Research, Bristol Laboratory, Langford, UK.

"The data demonstrate that the chronic administration of therapeutic levels of salbutamol increases maximal anaerobic power in man, irrespective of the subjects' training status"
International Sports Medicine 2005 Sep
Le Panse B, Collomp K, Portier H, Lecoq AM, Jaffre C, Beaupied H, Richard O, Benhamou L, De Ceaurriz J, Courteix D.
LPM-IPROS, Faculte des Sports, Orleans, France.

"..in response to salbutamol administration (DeltaAIx-Salb) were determined before and after weight reduction. After a 12-week weight reduction program, the average weight loss was 7.96 +/- 3.47 kg, with losses of 21.88 +/- 20.39 cm2 in visceral fat areas.."
Yonsei Med J. 2005 Aug
Park SH, Shim KW.
Department of Cardiology and Ewha Medical Research Institute

"The beta-adrenergic system is involved in the control of energy metabolism and expenditure...The beta2-AR was stimulated with two doses of salbutamol...the findings support a role for this polymorphism in the development and maintenance of overweight and obesity"
Journal of Clinical Endocrinology Metabolism 2005 Apr.
Park SH, Shim KW.
Department of Cardiology and Ewha Medical Research Institute

"Isoproterenol and salbutamol elicited strong lipolytic responses in adipocytes isolated from horse and pony subcutaneous adipose tissue..."
Comp Biochem Physiology 2003 Oct
Carrington EF, Desautels M, Naylor JM.

University of Saskatchewan, Western College of Veterinary Medicine

"A 65-year-old Kenyan Asian developed rapidly progressive multiple symmetrical lipomatosis over 8 years.... A clinical trial of oral salbutamol, a beta 2-agonist, was performed with significant therapeutic effect. The body fat mass showed a reversal of the rapid progression while on the treatment, associated with an increase in the resting metabolic rate."
Clinical Endocrinology 1987 Nov
Leung NW, Gaer J, Beggs D, Kark AE, Holloway B, Peters TJ.
Division of Clinical Cell Biology, MRC Clinical Research Centre, Harrow, Middlesex, UK

"...Furthermore, continuous infusion of salbutamol (1.15 mg.kg body wt-1.day-1) via miniosmotic pumps did cause significant increases in muscle mass, protein..."
American Journal of Physiology
Choo JJ, Horan MA, Little RA, Rothwell NJ.
Department of Physiological Sciences, University of Manchester Medical School, United Kingdom
"Eight normal male subjects received single oral doses of BRL 35135 (8 mg) or the selective beta 2-adrenoceptor agonist salbutamol (8 mg)... BRL 35135 and salbutamol produced a significant fall in serum potassium concentration compared with placebo, in keeping with beta 2-adrenoceptor stimulation...A significant increase in basal metabolic rate occurred with both BRL 35135 and salbutamol. In the case of salbutamol, this effect appeared to be mediated solely by beta 2-adrenoceptors."
Clinical Science (London)
Wheeldon NM, McDevitt DG, McFarlane LC, Lipworth BJ.
Department of Clinical Pharmacology, Ninewells Hospital and Medical School, Dundee, Scotland, U.K.

"One group of animals (T-I) was fed salbutamol at a dose of 2 mg x kg-1 diet x day-1 for 38 days, while in another group (T-II) the beta-adrenergic agonist was discontinued in the diet 5 days before slaughter on the 43rd day. The semitendinosus muscle protein content increased (p < 0.05), while fat and collagen content decreased (p < 0.05) in the T-I group. These differences were not apparent in the group from which salbutamol was withdrawn. The data show that salbutamol is able to increase muscle content at the expense of fat stores in productive animals..."
An. Nutrition & Metabolism
del Barrio AS, Garcia-Calonge MA, Fernandez-Quintela A, Simon E, Portillo MP, Astiasaran I, Martinez JA.
Department of Nutrition and Food Science, University of Pais Vasco, Vitoria, Spain.

This product was added to our catalog on Monday 20 August, 2007.

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