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Autor Tema: O Miostatin Blocker  (Pročitano 17523 puta)

Van mreže MARE 85

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« Odgovor #15 poslato: Maj 02, 2008, 02:02:37 posle podne »
Ma znam sumporni nego ko zna kakve posledice ostaju posle koriscenja ovog
WHERE THE MIND GOES,THE BODY WILL FOLLOW

Van mreže H2SO4

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« Odgovor #16 poslato: Maj 02, 2008, 02:03:53 posle podne »
marvel comics
matere mi matere,
kupicu ti dimije

Van mreže MARE 85

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« Odgovor #17 poslato: Maj 02, 2008, 02:22:50 posle podne »
Ha ha ha ma kako!
WHERE THE MIND GOES,THE BODY WILL FOLLOW

Van mreže left hook

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« Odgovor #18 poslato: Maj 03, 2008, 03:33:53 posle podne »

Van mreže chris.l

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« Odgovor #19 poslato: Maj 04, 2008, 12:42:28 posle podne »

Van mreže Kralj ist Back-Bakic

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« Odgovor #20 poslato: Jul 13, 2008, 08:41:31 posle podne »
A Phase I/II trial of MYO-029 in Adult
Subjects with Muscular Dystrophy
Kathryn R. Wagner, MD, PhD,1 James L. Fleckenstein, MD,2 Anthony A. Amato, MD,3
Richard J. Barohn, MD,4 Katharine Bushby, MD,5 Diana M. Escolar, MD,6 Kevin M. Flanigan, MD,7
Alan Pestronk, MD,8 Rabi Tawil, MD,9 Gil I. Wolfe, MD,10 Michelle Eagle, PhD, MSc, MCSP, SRP,5
Julaine M. Florence, PT, DPT,8 Wendy M. King, PT,11 Shree Pandya, MS, PT,9 Volker Straub, MD,5
Paul Juneau, MS,12 Kathleen Meyers, RN, BSN,13 Cristina Csimma, PharmD, MHP,14
Tracey Araujo, MSPharm,14 Robert Allen, MD,13 Stephanie A. Parsons, PhD,13 John M. Wozney, PhD,14
Edward R. LaVallie, PhD,14 and Jerry R. Mendell, MD11
Objective: Myostatin is an endogenous negative regulator of muscle growth and a novel target for muscle diseases. We conducted
a safety trial of a neutralizing antibody to myostatin, MYO-029, in adult muscular dystrophies (Becker muscular dystrophy,
facioscapulohumeral dystrophy, and limb-girdle muscular dystrophy).
Methods: This double-blind, placebo-controlled, multinational, randomized study included 116 subjects divided into sequential
dose-escalation cohorts, each receiving MYO-029 or placebo (Cohort 1 at 1mg/kg; Cohort 2 at 3mg/kg; Cohort 3 at 10mg/kg;
Cohort 4 at 30mg/kg). Safety and adverse events were assessed by reported signs and symptoms, as well as by physical examinations,
laboratory results, echocardiograms, electrocardiograms, and in subjects with facioscapulohumeral dystrophy, funduscopic
and audiometry examinations. Biological activity of MYO-029 was assessed through manual muscle testing, quantitative
muscle testing, timed function tests, subject-reported outcomes, magnetic resonance imaging studies, dual-energy radiographic
absorptiometry studies, and muscle biopsy.
Results: MYO-029 had good safety and tolerability with the exception of cutaneous hypersensitivity at the 10 and 30mg/kg
doses. There were no improvements noted in exploratory end points of muscle strength or function, but the study was not
powered to look for efficacy. Importantly, bioactivity of MYO-029 was supported by a trend in a limited number of subjects
toward increased muscle size using dual-energy radiographic absorptiometry and muscle histology.
Interpretation: This trial supports the hypothesis that systemic administration of myostatin inhibitors provides an adequate
safety margin for clinical studies. Further evaluation of more potent myostatin inhibitors for stimulating muscle growth in
muscular dystrophy should be considered.
Ann Neurol 2008;63:561–571
Muscular dystrophies are a diverse set of distinct, inherited
disorders that commonly manifest with progressive
skeletal muscle weakness and wasting. Despite
substantial progress in understanding the pathophysiological
basis of these diseases, no pharmacological therapies
have been identified that increase muscle
strength, other than corticosteroids, which provide a
modest benefit to some patients with these disorders.1
For muscular dystrophies that present in adulthood,
there have been only a few small clinical trials, and
none involved a novel therapeutic agent.2–6 This article
describes a clinical trial of a novel agent, an inhibitor
of myostatin, designed to increase muscle mass and
strength in several of the most common forms of adult
muscular dystrophy.
Myostatin, a member of the transforming growth
From the 1Departments of Neurology and Neuroscience, The Johns
Hopkins University School of Medicine, Baltimore, MD; 2Department
of Internal Medicine, University of Oklahoma College of
Medicine at Tulsa, Tulsa, OK; 3Department of Neurology, Brigham
and Women’s Hospital, Boston, MA; 4Department of Neurology,
University of Kansas Medical Center, Kansas City, KS; 5University
of Newcastle Upon Tyne, Institute of Human Genetics, Newcastle
Upon Tyne, United Kingdom; 6Children’s National Medical Center,
Research Center Genetic Medicine, Washington, DC; 7University
of Utah School of Medicine, Departments of Neurology, Human
Genetics, and Pathology, Salt Lake City, UT; 8Neuromuscular
Division, Washington University School of Medicine, St. Louis,
MO; 9Neuromuscular Disease Center, University of Rochester
Medical Center, Rochester, NY; 10University of Texas Southwestern
Medical Center, Dallas, TX; 11Department of Pediatrics and Neurology,
Columbus Children’s Research Institute, Ohio State University,
Columbus, OH; 12Senior Statistician, MMS Holdings, Inc.,
Canton, MI; 13Wyeth Research, Collegeville, PA; and 14Wyeth Research,
Cambridge, MA.
Received Oct 31, 2007, and in revised form Dec 18. Accepted for
publication Dec 21, 2007.
Current address for Dr Csimma: Clarus Ventures, Cambridge, MA.
Published online Mar 11, 2008, in Wiley InterScience
(www.interscience.wiley.com). DOI: 10.1002/ana.21338
Address correspondence to Dr Wagner, The Johns Hopkins University
School of Medicine, Department of Neurology, Meyer
5-119, 600 North Wolfe Street, Baltimore, MD 21287-7519.
E-mail: kwagner@jhmi.edu
ORIGINAL ARTICLES
© 2008 American Neurological Association 561
Published by Wiley-Liss, Inc., through Wiley Subscription Services
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Van mreže Kralj ist Back-Bakic

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« Odgovor #21 poslato: Avgust 10, 2008, 05:32:29 posle podne »
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Van mreže Kralj ist Back-Bakic

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« Odgovor #22 poslato: Avgust 11, 2008, 10:58:43 posle podne »
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Van mreže Polomac

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« Odgovor #23 poslato: April 26, 2009, 04:37:02 posle podne »

Van mreže The_Bulldog

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« Odgovor #24 poslato: Decembar 13, 2009, 03:19:32 pre podne »
Muscle Mutants
Eric Henderson, Ph.D.


What would happens if your muscles grew all the time? Well, you would be a giant “myoball” and live about 8 minutes. Cell death (apoptosis) and inhibition of cell growth is part of normal development and once you have grown to your adult size, your body really does not want to keep growing.

That is why we have to stress our bodies to get additional muscle growth. That is also why we need to vary our exercises to continually confuse your muscles and force them to continually grow to compensate for their ever changing environment

Now the fun begins. Let’s think of all the things working against us in terms of muscle growth.

Age: as a 51 year old I can tell you that my muscles do not want to grow a nanometer without extremely convincing reasons to do so. Lower testosterone, cross-linked muscle and support tissue. The battle is intense!

2. Oxidative stress: Again, compensating for all those free radicals I generate when working out gets tougher and tougher with age. Try The Feast, it works.

Myostatin and Follistatin. What? These are two proteins involved in the suppression of muscle growth. If you walk all day and your muscles responded accordingly your gluts and quads would be the size of a house! Myostatin and Follistatin are proteins that inhibit muscle growth. If you shut these proteins down you get incredible increases in native (non-exercise induced) muscle growth. The mouse on the bottom has had his myostatin/follistatin activity genetically decreased - compare him to the normal mouse on the top.

Now, theory time. Have you ever known those lucky guys in the gym who start out with great 6 packs and then after 2 weeks of lifting have giant pecs and biceps? Yeah, those guys (and girls) are likely to be, in my opinion, myostatin/follistatin mutants! That’s right folks, here come the X-man - the mutants are taking over. There is new evidence this is the case. In a study of racing dogs the best athletes were myostatin mutants!Wait! Before you freak out, remember that we are ALL mutants of one sort of another.

Now, for guys like me who are extremely hard gainers but follow all the “rules” (lots of health meals, intense workouts, rest, etc.) one likely explanation is that I am another form of myostatin/follistatin mutant. In my case, unfortunately, the myostatin/follistatin levels are likely to be abnormally high! That means, that as soon as I even think about lifting a weight, my body starts to shut down muscle growth.

Bummer!

So what do we do? Well, everything you can - short intense workouts, take lots of antioxidants (this enhances growth of muscle) and so on. But will we ever obtain the success of the genetically gifted? Not likely. Not with out gene therapy or buckets of cancer-inducing steroids. Still, even the skinniest myostatin mutant can make some progress. And it will not be long before someone comes up with a myostatin inhibitor that actually works (there are some on the market but they do not even come close to the Henderson A-list because they are essentially fractionated seaweed - stuff I could make in my lab in a day, but why, it does not work).

Why will this take so long? Consider this, anything that goes into your mouth goes through an acid wash that is designed and optimized over millions of years to break things down. So how the heck is a myostatin inhibitor going to get through your gut intact and with retention of biological activity - not likely!

It can happen (tylenol and a lot of other drugs work this way,for example) but it will be a long and tedious path to creating the ultimate myostatin inhibitor. And will it be legal, probably not.

So in the mean time, just work out hard, eat right and get rest. You will see improvements and you will find happiness! In the mean time I will try to figure out how to compensate for our many and varied genetic mutations - and let you know as soon as I come up with something!

Peace and Health,

Eric






Van mreže Stevcho

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« Odgovor #25 poslato: Decembar 13, 2009, 12:10:46 posle podne »
haha nabildovani pilici... lol
No curling in the squat rack!

Van mreže Remetik

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« Odgovor #26 poslato: Decembar 14, 2009, 02:52:25 pre podne »
Kakvi pilici, vidis da su neki misevi-pacovi!  :-X