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Hot Rox
Extreme
5x Faster Fat Loss
Thermogenic Fat-Loss Phenomenon Makes Ephedra
Obsolete!
If you want maximum fat-burning effects to work continually,
around the clock (24/7), Hot Rox is the perfect supplement for
you!
Hot Rox:
* Ramps up lipolysis, releasing fat from adipocytes more rapidly
than ephedra-based products to the point of no contest.
* Minimizes lipogenesis (fat creation) via increased CAMP and T3.
* Maximizes and sustains metabolism around the clock, turning fat
into heat energy, through two powerful mechanisms: Fueling
the TCA cycle Stimulating mitochondrial uncoupling
* Provides an inexhaustible supply of the weak-link substrate
oxaloacetate and thus keeps the TCA cycle primed for sustained,
maximum fat burn.
* Elevates and maintains not only the increased production of T3,
but the peripheral conversion of T4 into T3 as well, without
suppressing TSH (natural thyroid production).
* Preserves or even promotes muscle-mass gains.
Bottom line, Hot Rox makes ephedra and the current crop of
fat-loss supplements obsolete!
This is definitely not an overstatement.
What makes the Hot Rox our invention so valuable and unique? First
of all, Hot Rox is far more effective at burning off body fat than
anything that's ever been on the market. Furthermore, unlike
ephedra-based formulas, Hot rox is safe and it doesn't
down-regulate beta-receptor sites and become ineffective over
time.
And get this... Hot Rox also increases protein synthesis and
the natural production of anabolic substrates (in both men and
women). In other words, Hot Rox may actually help to preserve or
even build muscle mass.
Even better yet, all of these metabolic benefits are sustained,
around the clock, week after week, as long as you continue to take
the formula.
We honestly believe that we've developed the fat-loss phenomenon
that everyone's been hoping for. Ever since the ripped look's
become the passionate desire of every body-conscious individual,
there's been a quest for a fat burner that, in addition to
continuously melting off adipose tissue, would help to preserve -
even promote - muscle-mass gains.
And we've done it! Not only that, Hot Rox is far more effective
than any of us involved with the project ever dreamed possible.
The name of our fat-loss phenomenon is Hot Rox and there's no
doubt in our minds that, after reading what follows, you'll be a
believer, too.
What's the Big Deal with Ephedra, Anyway?
Why is everyone so focused on adrenergic compounds, like ephedra?
A better thermogenic mousetrap should've replaced them years ago.
Unfortunately, instead of being innovative, supplement companies
became complacent, relying heavily upon the jitter-buzz factor to
sell their products.
Think about it... If ephedra-based products were all that
effective, why are you reading this article? How many bottles of
fat-loss supplements have you purchased in the last five years,
anyway? If you're like most of us, you've spent a small fortune
and you're still not as lean as you want to be.
I don't know why this isn't obvious to everyone, but adrenergic
compounds, in and of themselves, aren't all that powerful. In
fact, ephedrine, in the absence of caffeine, is barely even worth
considering as a fat-loss agent. Furthermore, if you attempt to
keep ephedrine levels continuously elevated (24/7), which is
what's required for optimal fat loss, beta receptors eventually
down-regulate, making ephedra even less effective.
Rapid Fat Loss, A Mission of 2 Tasks
The first thing to understand about fat loss is that almost
everyone has the science backward. They hope that by burning
energy, say on a Stairmaster, it will somehow suck the fat right
out of their blurred abs or other problem areas. This simply isn't
true. There is no pipeline through which muscle can pull fat from
adipocytes. There must be ample supplies of fatty acids in the
bloodstream to use as fuel or the muscle burns itself!
People also hope that cutting calories will guarantee fat loss.
This also isn't true. Again, energy-burning or energy deficits
won't suck fat from the fat cells. The energy can and often will
come from glycogen or muscle protein. And most important, caloric
reduction slows the metabolism and can actually interfere with fat
release!
Once this occurs, you're in a physiological nightmare: a state
that not only makes it nearly impossible to lose any additional
body fat, but you also begin to lose muscle mass as well, leaving
you skinny-fat.
Triggering lipolysis is the crucial first step, but you must also
support the burn. If not, it's perfectly plausible to stimulate
lipolysis only to have the fat redistributed back into adipocytes.
What a waste of time!
If your goal is to get as lean as possible while maintaining or
even gaining muscle mass, in addition to managing caloric intake,
you must successfully accomplish two and only two critical tasks.
Everything else is subordinate to these:
1. Support rapid lipolysis (fat release) while simultaneously
minimizing lipogenesis (fat creation).
2. Keep the TCA* cycle primed for maximum, aerobic-metabolic burn.
*Note: The TCA (tricarboxylic acid) cycle is also known as the
Krebs cycle or aerobic metabolism.
TASK 1 - Release the Fat Hounds! Lipolysis Up, Lipogenesis Down
Simply put, the goal here is to get fat cells to release fat (lipolysis)
faster than they create fat from dietary calories (lipogenesis).
If you want to induce lipolysis, you have to increase cAMP (cyclic
adenosine monophosphate). Cyclic AMP is responsible for triggering
the cellular processes for lipid metabolism. In other words, it's
the chief gatekeeper for stimulating lipolysis and slowing
lipogenesis.
Ramping up cAMP within fat cells activates protein kinase, which
in turn activates hormone-sensitive lipase, the enzyme that breaks
down the fat in adipocytes. This causes fatty acids and glycerol
to be released into the bloodstream.
High sensitivity to hormone-sensitive lipase depends upon ample
thyroid hormone being present. If T3 levels are low, lipase
activity won't increase as it should. In contrast, increased cAMP
in combination with high T3 levels will send lipolysis rates
through the roof.
Cyclic AMP can be stimulated directly by increasing
adenylate-cyclase activity. Adrenergic compounds (endogenous or
exogenous) can also indirectly increase cAMP by activating
adenylate cyclase when binding beta receptors. The adrenoreceptor
route, as mentioned before, has its limitations.
Additionally, both increased cAMP and high T3 levels decrease
lipoprotein lipase activity, which is an enzyme responsible for
lipogenesis. So in addition to stimulating lipolysis, cAMP and T3,
as a team, put the kibosh on lipogenesis as well.
This double-whammy effect that cAMP and T3 deliver is very
powerful, priming the body for the burn.
TASK 2 - Prime the TCA Cycle Ignition and Burn
When lipolysis outraces lipogenesis and releases fatty acids into
the blood, they diffuse into all cells of the body to be used as
fuel. Upon entering a cell, fatty acids are actively transported,
via carnitine acyltransferase, into mitochondria, which act as
cellular power plants. Once in the mitochondria, the fatty acid is
converted into fatty acid-CoA. Next, the fatty acid-CoA is broken
down further, two carbons at a time, into acetyl-CoA. This is the
ñfatî that fuels aerobic metabolism through the TCA (tricarboxylic
acid) cycle. In other words, when you think of burning off body
fat, the ñfatî being consumed is actually acetyl-CoA.
This is when T3 plays another huge role. T3 produces thermogenic
malic enzyme, which is the intermediary required to produce
oxaloacetate. And oxaloacetate, in combination with acetyl-CoA,
fuels the TCA cycle. For maximum thermogenesis, via the TCA cycle,
oxaloacetate needs to be present in ample amounts or the entire
process falls apart.
This is a weak link in the TCA cycle and requires exogenous
support through nutritional means if you want to maintain
continuous and rapid fat loss. (Just how you do that through
nutritional means is something I'll go over later.)
Additionally, T3 increases UCP3 uncoupling protein, which can have
profound effects on fat loss. In fat cells, uncoupling
dramatically increases lipolysis. And in other tissues, like in
muscle, uncoupling increases metabolic rate, thus supporting the
burn. The net effect is faster fat release from adipocytes,
followed by faster fat burning due to an overall-increased
metabolic rate.
The Whole Fat-Loss Enchilada
Bottom line, if you ramp up and sustain high cAMP and T3 levels,
you've done all that's required for maximum, continual fat
metabolism. In essence, you've achieved what's tantamount to
thermogenic nuclear war.
(Managing food intake is, of course, also required; hopefully
that's obvious.)
So how do we formulate a supplement that sustains
non-beta-receptor-mediated cAMP and increased T3 levels without
causing down-regulation?
Well, we have the answer. Specifically, we've developed a series
of compounds that when combined, produces a more profound effect
than our greatest expectations. In fact, at this point, we can't
imagine anything better.
The horsepower that fuels HOT-ROX is comprised of two novel
compounds and their synergists. The big daddy, which is also the
real magic behind our formula, is called A7-E™.
A7-E was designed by Bill Roberts and is best described as a
thyroid supercharger. It's completely new to the industry; it has
a patent filed on it; and it's so powerful on its own as a
fat-loss agent that there's no contest when compared to anything
else that's currently on the market.
A7-E launches us right smack dab in the middle of a new fat-loss
era!
A7-E™ - Rev Up and Potentiate Thyroid Activities
The most challenging task was finding a way to boost T3 levels
without suppressing TSH. From the scientific literature, there are
two groups of compounds that when taken together in relatively
high dosages, would do the trick nicely:
3,17-dihydroxy-delta-5-etiocholane-7-one (A7-D) supported by
guggulsterones.
Once converted into the active species, A7-D has been shown to
increase T3 in humans by as much as 30% without suppressing TSH!
Additionally, and to a much greater degree, A7-D increases
thermogenic malic enzyme. Remember, malic enzyme is the compound
responsible for producing oxaloacetate, which fuels the TCA cycle.
Guggulsterones, on the other hand, increase the peripheral
conversion of T4 into T3, making it the ideal complement to A7-D.
Increasing the peripheral conversion of T3 is very important
because the thyroid only produces 20% of the body's T3. Most of
the remaining 80% is derived from T4 through a conversion process
that occurs in various target tissues, like skeletal muscle, for
example.
On the surface, A7-D and guggulsterones appear to be great choices
for the HOT ROX formula. Unfortunately, however, both have
inherent problems which needed fixing if we were to achieve the
desired magnitude of effect. In other words, we wanted to improve
the wow factor by a bunch.
In essence, the bioavailability of A7-D isn't high enough and the
active life is far too short. So to improve both bioavailability
and length of active life, Bill engineered A7-D into a carbonate
ester, called 3,17-dihydroxy-delta-5-etiocholane-7-one
diethylcarbonate, or A7-E.
A7-E, due to its superior rate of conversion, its longer active
life, and its increased bioavailability, is the premier fat-loss
compound of our time. In and of itself, it's a very powerful and
effective fat-loss agent. But we didn't stop there...
We wanted a synergist for A7-E. All of our research pointed to one
obvious candidate - guggulsterone - because it increases the
peripheral conversion of T4 into T3, further supporting the
actions of A7-E. The problem, however, is guggulsterones are not
available in a pure state. They're found in a plant called
Commiphora mukul, which contains only small amounts of
guggulsterone Z and E.
Unfortunately, a good Commiphora mukul extract is only 2.5%
active, and that alone makes using an herbal extract unfeasible.
Additionally, it's very difficult to get consistent raw material,
making accurate dosing literally impossible. And if these weren't
big enough problems, there are other constituents in the plant
material that cause rather severe allergic reactions in a
significant portion of the population.
Our only solution was to produce 100% pure guggulsterones,
preferably with a 2:1 ratio between Z and E. And that's just what
we did. We included two parts purified guggulsterone Z to one part
purified guggulsterone E in our HOT-ROX formula.
So to recap, A7-E has the incredible ability to stimulate the
production of T3 and thermogenic malic enzyme; and pure
guggulsterones further enhance (synergize) these activities by
facilitating the peripheral conversion of T4 into T3.
SCLAREMAX™ The King of Cyclic AMP
The second novel compound in HOT-ROX is called Sclaremax.
Sclaremax is a diterpenoidal lactone found in a plant called
Salvia sclarea. It's known to be an extremely potent adenylate
cyclase activator, very similar to that of the diterpene
derivative, forskolin. In fact, cyclic AMP assays indicate
Sclaremax either equals or exceeds the actions of forskolin, but
with a much longer active life.
Additionally, like forskolin, Sclaremax stimulates adenylate
cyclase independently of beta-2 receptors, which means it has no
limitations because it won't down-regulate and it has a higher
maximal effect. In other words, the more you take, the greater the
effect - day after day after day...
So Sclaremax essentially mimics or acts like TSH - activating
adenylate cyclase in the membrane of thyroid cells, which in turn
elevates cyclic AMP and eventually leads to thyroid hormones being
released. It may also enhance the cyclic AMP response to TSH in
thyroid cells as well.
And because Sclaremax produces an accumulation of cyclic AMP, it
will also increase nitrogen retention. This means that it will
help preserve or even build lean-body mass (muscle) while
increasing lipolysis.
Another huge bonus in comparison to ephedra and other beta
agonists is that Sclaremax doesn't interact with beta-1
adrenoreceptors. In fact, Sclaremax, in very high doses, exhibits
a vasodilatory effect
Some other benefits of Sclaremax include its antithrombotic and
antidepressant effects, as well as its stimulating effect on
luteinizing hormone, via cyclic AMP, resulting in the production
of additional Testosterone (in males).
To synergize the effects of Sclaremax, we included the
methylxanthine caffeine. Caffeine is a potent competitive
inhibitor of phosphodiesterase enzyme, which is responsible for
the inactivation of cyclic AMP.
In comparison to caffeine, Sclaremax increases the formation of
cyclic AMP, whereas caffeine acts to prevent its degradation. In
other words, caffeine potentiates the effects of Sclaremax, thus
increasing the magnitude of cyclic AMP accumulation.
And since Sclaremax and caffeine increase cyclic AMP, but via
different mechanisms and not through the beta receptor, a
combination produces a powerful, synergistic effect on lipolysis.
So you can see that, even though A7-E, Sclaremax, guggulsterones,
and caffeine have discrete roles in the fat-loss process, they
also potentiate one another's activities, making the combination
extremely powerful.
We also wanted to utilize compounds in our formula that elevate
mood and suppress hunger, especially for carbohydrates. To do
this, we included ample amounts of acetyl-L-tyrosine and
5-hydroxy-L-tryptophan to maximize brain levels of norepinephrine,
dopamine, and serotonin, all of which tend to decrease while
following a calorie-restricted diet.
Maintaining high levels of norepinephrine, dopamine, and serotonin
will not only elevate mood and suppress appetite, but:
* Decrease fat storage
* Stimulate oxygen consumption
* Increase resting energy expenditure
* Decrease insulin levels
HOT ROX™ Isn't for Everyone
If you're not going to take fat loss seriously and be disciplined
with your diet, please don't buy the supplement. I don't care what
you take or what you do in the way of exercise, if you eat half a
smorgasbord every day you're gonna' get fatter.
On the other hand, if you're really committed to doing your part,
incorporating sound training and dietary guidelines, we promise
that HOT ROX will be the most effective fat-loss agent you've ever
used. It's expensive relative to other products on the market; but
when you compare its effects, HOT ROX is more than just a bargain
- it's a steal!
Just remember how much you've spent on fat-burners over the years
and see where that's gotten you. E-Nuff said
In Summary, HOT ROX:
* Ramps up lipolysis, releasing fat from adipocytes more rapidly
than ephedra-based products to the point of no contest.
* Minimizes lipogenesis (fat creation) via increased cAMP and T3.
* Maximizes and sustains metabolism around the clock, turning fat
into heat energy, through two powerful mechanisms: Fueling the TCA
cycle Stimulating mitochondrial uncoupling
* Provides an inexhaustible supply of the weak-link substrate
oxaloacetate and thus keeps the TCA cycle primed for sustained,
maximum fat burn.
* Elevates and maintains not only the increased production of T3,
but the peripheral conversion of T4 into T3 as well, without
suppressing TSH (natural thyroid production).
* Preserves or even promotes muscle-mass gains. So if you want
maximum fat-burning effects to work continually, around the clock
(24/7), HOT-ROX is the perfect supplement for you!
HOT ROX Fat-Loss Phenomenon
Bill Roberts, Cy Willson, and I believe that HOT-ROX represents
our best work to date. In summary, it's the first and only
designer fat-loss formulation ever to produce a rate and magnitude
of fat loss that makes being ripped attainable and maintainable
for most individuals.
With just A7-E alone, we've effectively made all ephedra-based
products and their weaker siblings obsolete. And when combining
Sclaremax and all of the synergists with A7-E, there's a
potentiation effect that will blow you away. In addition to
melting off fat like never before, you'll notice that you feel
either curiously warm or downright hot!
So if you want to wage thermogenic war against all those pesky
adipocytes - thus allowing you to attain and maintain the level of
leanness that you've been struggling so long to achieve - HOT ROX
is the only supplement that provides these nuclear weapons.
Bottom line, HOT ROX is the most powerful and most-effective
sports supplement ever developed for fat loss, period! Outrageous
and emphatic statement? You betcha, and it's true!
HOT ROX is truly a fat-loss phenomenon!
| Supplement
Facts: |
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Serving Size 2
caps |
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Servings Per Container 55 |
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Amount Per Serving |
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% DV |
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Hot-Rox™ Formula:
A7-E™ Super-Thermogenic Gel™ 20/700 (3,17-dihydroxy-delta-5-etiocholane-7- one diethylcarbonate, Sclaremax™
[proprietary, liquid sclareolide], GZ™ 100 [proprietary guggulsterone]), caffeine |
950mg |
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Calories |
120.00 |
0% |
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Calicum (calcium
chloride) |
55.00 mg |
4% |
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Sodium (sodium
chloride) |
51.00 mg |
3% |
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Potassium
(potassium chloride) |
38.00 mg |
4% |
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Plasma-Blast™ (Plasma Expanding
Complex) |
33.60 g |
0% |
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Creatine glycerol ester |
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** |
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D-Mannitol |
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** |
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Lime Juice (fruit) |
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** |
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HydraMax™ (Hyper Hydrating Complex) |
2.50 g |
0% |
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L-Taurine |
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** |
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L-Glutamine |
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** |
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WI-32™ (Workout Intensity Complex) |
1.70 g |
0% |
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L-Tyrosine |
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** |
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Phosphatidylcholine |
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** |
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White willow extract (Salix alba)
(bark) |
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** |
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| ** Daily Value (DV) not
established |
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Other Ingredients:
lauroyl macrogol-32 glycerides, gelatin, FD&C red #40, FD&C yellow #6,
titanium dioxide.
Directions: As a dietary supplement, take one or two capsules
in the morning prior to
breakfast and one or two capsules six hours later, each time on an
empty stomach with
8 oz. of water. If you haven't used this supplement previously,
begin by taking one
capsule twice per day for three days prior to increasing the dose.
Do not exceed four
capsules in any 24-hour period. FOR BEST RESULTS, USE CONTINUOUSLY
FOR A
MINIMUM OF ONE MONTH.
Warnings: Consult your physician before using this or any dietary
supplement. Do not
take
if you are pregnant or breast feeding, elderly or under the age of
18, chronically ill, or
taking
any prescription or over-the-counter medicine, including but not
limited to
antidepressants (such as MAO inhibitors), stimulants, allergy
medications, and medications
for
high blood pressure or other cardiovascular conditions. Discontinue
use if you
experience dizziness, headache, nausea, or heart palpitations. If
you have trouble
sleeping, do not take within 6 hours of bedtime. KEEP OUT OF REACH
OF CHILDREN.
Before beginning any program of weight loss, consult your health care
practitioner.
These statements have not been evaluted by the FDA. This product is
not intended to
diagnose, treat, cure or prevent any disease.
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