Feel the Difference On Day 1

Finally, A Vitality Boosting Formula That Delivers

13 Powerful Ingredients Shown to Boost Male Vitality Up to 166% Higher Than Actual Testosterone Replacements ...By Restoring Your Mitochondria... The "Power Plants" Of Every Cell In The Body.

Cellular Level2
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Supercharge

Blood Flow

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Restore

Vitality

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Build 

Muscle

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Burn

Fat

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Enhance

Cognition

What Real Men Are Saying About Mito Male

Gold Stars

" If I could have only one supplement, Mito Male would be the one! At 63-years old, lifting for 30+ years, I know what works and Mito Male works! "

dr.rich

- Dr. Richard Schuttler

Verified Review

Gold Stars

“It really fires me up. Just turned 66, look and act 46. Now my workouts in the gym are just simply "shock and awe", they can't believe what they are seeing.”

man2

- Wayne H.

Verified Review

Gold Stars

“It has helped me tremendously. I feel so much better. I was in a bad way and it gave me back my life.”

khazad

-Gene N.

Verified Review

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MITOCHONDRIA

The Key to Feeling Young

If you’re a man over 35, yesterday’s T- Boosters simply won’t cut it. Research is showing that declining T levels are merely a symptom of a bigger problem that begins in the “powerplant” of your cells – the mitochondria.

Mitochondria produce the energy that every single cell in your body needs to survive. Muscle cells, heart cells, even the Leydig cells that produce hormones – all rely on your mitochondria to operate efficiently

Unfortunately, it’s estimated that the energy producing power of your mitochondria drops by 50% or more after you hit 40. And this sharp decline is linked to a whole host of problems we associate with aging … including low T, declining energy, muscle loss, memory loss, and poor circulation.

Mitochondrial Power

battery

Turning Back The Clock

On Male Aging

The best way to restore the energy, vitality, and body of a man’s youth is by rejuvenating and optimizing  his mitochondria.

And my biogenesis technology is a simple, proven, three-step process that not only helps  restore these mighty mitos to their former glory…

But also helps generate new mitochondria with fresh energy enhancing power!

3 Phases FOR RESTORING Male Vitality At The Cellular Level

Phase 1

Supercharge
Mitochondria

You need to get old, broken down mitochondria pumping out precious energy again. That means making sure they’re getting the proper raw materials that get turned into fuel for the rest of the body.

Phase 2

Protect
Mitochondria

Environmental threats aren’t going anywhere, even with  a good diet and exercise. Which is why we must make sure our mitochondria are shielded from outside threats to keep them running at 100%

Phase 3

Restore Old Mitochondria

Because we lose mitochondria as we age, it’s crucial to generate NEW ones in addition to repairing the ones we already have.  This is like adding a new “energy engine” to help your body push harder so every cell is working harder and faster than ever before. 

Mito Male Delivers On All Three Phases

…in one great tasting elixir. Simply mix one scoop a day in your favorite beverage to help restore the cellular power of youth for: all day, natural energy, a strong, muscular physique, gushing blood flow, and alpha male vitality and confidence.

PHASE 1

Supercharge Mitochondria

You need to get old, broken down mitochondria pumping out precious energy again. That means making sure they’re getting the proper raw materials that get turned into fuel for the rest of the body.

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Ingredient

What It Does

Mito Male Scientific References

1. Cavallini, G., Caracciolo, S., Vitali, G., Modenini, F., & Biagiotti, G. (2004). Carnitine versus androgen administration in the treatment of sexual dysfunction, depressed mood, and fatigue associated with male aging. Urology, 63(4), 641-646. doi:10.1016/j.urology.2003.11.009

2. Malaguarnera, M., Cammalleri, L., Gargante, M. P., Vacante, M., Colonna, V., & Motta, M. (2007). L-Carnitine treatment reduces severity of physical and mental fatigue and increases cognitive functions in centenarians: A randomized and controlled clinical trial. The American Journal of Clinical Nutrition, 86(6), 1738-1744. doi:10.1093/ajcn/86.5.1738

3. Karlic, H., & Lohninger, A. (2004). Supplementation of l-carnitine in athletes: Does it make sense? Nutrition, 20(7-8), 709-715. doi:10.1016/j.nut.2004.04.003


4. Samimi, M., Jamilian, M., Ebrahimi, F. A., Rahimi, M., Tajbakhsh, B., & Asemi, Z. (2016). Oral carnitine supplementation reduces body weight and insulin resistance in women with polycystic ovary syndrome: A randomized, double-blind, placebo-controlled trial. Clinical Endocrinology,84(6), 851-857. doi:10.1111/cen.13003


5. Sahlin, K. (2011). Boosting fat burning with carnitine: An old friend comes out from the shadow. The Journal of Physiology, 589(7), 1509-1510. doi:10.1113/jphysiol.2011.205815


6. Soczynska, J. K., Kennedy, S. H., Chow, C. S., Woldeyohannes, H. O., Konarski, J. Z., & Mcintyre, R. S. (2008). Acetyl-L-carnitine and α-lipoic acid: Possible neurotherapeutic agents for mood disorders? Expert Opinion on Investigational Drugs, 17(6), 827-843. doi:10.1517/13543784.17.6.827


7. Miyagawa, T., Kawamura, H., Obuchi, M., Ikesaki, A., Ozaki, A., Tokunaga, K., . . . Honda, M. (2013). Effects of Oral L-Carnitine Administration in Narcolepsy Patients: A Randomized, Double-Blind, Cross-Over and Placebo-Controlled Trial. PLoS ONE,8(1). doi:10.1371/journal.pone.0053707


8. Cristofano, A., Sapere, N., Marca, G. L., Angiolillo, A., Vitale, M., Corbi, G., . . . Costanzo, A. D. (2016). Serum Levels of Acyl-Carnitines along the Continuum from Normal to Alzheimers Dementia. Plos One, 11(5). doi:10.1371/journal.pone.0155694

. Fillit, H., & Hill, J. (2004). The Economic Benefits of Acetylcholinesterase Inhibitors for Patients with Alzheimer Disease and Associated Dementias. Alzheimer Disease & Associated Disorders,18. doi:10.1097/01.wad.0000127492.65032.d3


10. Miyata, M., Yoshihisa, A., Yamauchi, H., Owada, T., Sato, T., Suzuki, S., . . . Takeishi, Y. (2014). Impact of sleep-disordered breathing on myocardial damage and metabolism in patients with chronic heart failure. Heart and Vessels, 30(3), 318-324. doi:10.1007/s00380-014-0479-6


11. Lango, R. (2001). Influence of ?-carnitine and its derivatives on myocardial metabolism and function in ischemic heart disease and during cardiopulmonary bypass. Cardiovascular Research, 51(1), 21-29. doi:10.1016/s0008-6363(01)00313-3


12. Vescovo, G., Ravara, B., Gobbo, V., Sandri, M., Angelini, A., Barbera, M. D., . . . Libera, L. D. (2002). L-Carnitine: A potential treatment for blocking apoptosis and preventing skeletal muscle myopathy in heart failure. American Journal of Physiology-Cell Physiology, 283(3). doi:10.1152/ajpcell.00046.2002


13. Shadboorestan, A., Shokrzadeh, M., Ahangar, N., Abdollahi, M., Omidi, M., & Payam, S. S. (2013). The chemoprotective effects of l-carnitine against genotoxicity induced by diazinon in rat blood lymphocyte. Toxicology and Industrial Health,31(12), 1334-1340. doi:10.1177/0748233713491811


14. Chowanadisai, W., Bauerly, K. A., Tchaparian, E., Wong, A., Cortopassi, G. A., & Rucker, R. B. (2009). Pyrroloquinoline Quinone Stimulates Mitochondrial Biogenesis through cAMP Response Element-binding Protein Phosphorylation and Increased PGC-1α Expression. Journal of Biological Chemistry,285(1), 142-152. doi:10.1074/jbc.m109.030130


15. Chowanadisai, W., Bauerly, K. A., Tchaparian, E., Wong, A., Cortopassi, G. A., & Rucker, R. B. (2009). Pyrroloquinoline Quinone Stimulates Mitochondrial Biogenesis through cAMP Response Element-binding Protein Phosphorylation and Increased PGC-1α Expression. Journal of Biological Chemistry, 285(1), 142-152. doi:10.1074/jbc.m109.030130


16. Stites TE, Mitchell AE, Rucker RB. Physiological importance of quinoenzymes and the O-quinone family of cofactors. J Nutr. 2000 Apr;130(4):719-27
17. Steinberg, F., Stites, T. E., Anderson, P., Storms, D., Chan, I., Eghbali, S., & Rucker, R. (2003). Pyrroloquinoline Quinone Improves Growth and Reproductive Performance in Mice Fed Chemically Defined Diets. Experimental Biology and Medicine, 228(2), 160-166. doi:10.1177/153537020322800205


18. Biswas, T. K., Pandit, S., Mondal, S., Biswas, S. K., Jana, U., Ghosh, T., . . . Auddy, B. (2010). Clinical evaluation of spermatogenic activity of processed Shilajit in oligospermia. Andrologia,42(1), 48-56. doi:10.1111/j.1439-0272.2009.00956.x


19. Surapaneni, D. K., Adapa, S. R., Preeti, K., Teja, G. R., Veeraragavan, M., & Krishnamurthy, S. (2012). Shilajit attenuates behavioral symptoms of chronic fatigue syndrome by modulating the hypothalamic–pituitary–adrenal axis and mitochondrial bioenergetics in rats. Journal of Ethnopharmacology, 143(1), 91-99. doi:10.1016/j.jep.2012.06.002


20. Chang, C. S., Choi, J. B., Kim, H. J., & Park, S. B. (2011). Correlation Between Serum Testosterone Level and Concentrations of Copper and Zinc in Hair Tissue. Biological Trace Element Research,144(1-3), 264-271. doi:10.1007/s12011-011-9085-y


21. Plasma Steroid-Binding Proteins in Tumour Diseases. (1984). Molecular Aspects of Medicine, 371-380. doi:10.1016/b978-0-08-033239-0.50032-6

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