- Supports increases in natural testosterone*
- May elevate luteinizing hormone levels*
- Aromatase enzyme inhibitor*
- May increase lean body mass*
- May increase strength*
- 30 servings per container
Out of stock
Testro Core™ is packed with over 10 efficaciously dosed, research backed natural testosterone enhancers designed to promote all things males in you. This powerful formula helps support increases in circulating testosterone while also blocking the body’s production of estrogen. Low testosterone levels can wreak havoc on your body and can cause undesirable side-effects such as fatigue, loss of muscle mass/strength, an increase in body fat, and low libido. Regardless if these low levels are due to normal aging, excess weight, stress, or other variables it is vital that steps be taken to maintain or increase this anabolic hormone’s levels in the body when below a normal range. When you really want help increasing your body’s natural testosterone levels, you want proven ingredients that enhance testosterone safely and effectively. The comprehensive ingredient profile found in Testro Core™ will assist in maximizing natural testosterone output and promote a superior muscle building environment.
- 1000mg Tribulus Terrestris – One study found men supplementing with Tribulus for 60 days were able to increase testosterone by 16.3%.
- 500mg Fenugreek Extract – Supports increases in circulating testosterone.
- 250mg Horny Goat Weed Extract – Shown in one study to increase testosterone levels by 3x over a 7-day period compared to a control group.
- 100mg Polygonum Cuspidatum – In a study published in 2008 polygonum was found to increase blood testosterone correlation by 51.6%.
- 100mg Maca Extract – Helps block the body’s production of estrogen while boosting testosterone levels.
Boron is what is known as a trace mineral. This means that our bodies benefit from it as a vital nutrient, but only in very, very small trace amounts.
• Boron has been implicated in increasing free testosterone and serum DHT levels.
• At the same time boron acts as an anti-estrogen and decreases sex hormone binding globulin (SHBG).
• A study conducted by Naghii et al. (2011) found men who supplemented with boron for 7 consecutive days increased free testosterone and dihydrotestosterone (DHT) levels by 28% and 10% respectively, while also decreasing free estrogen levels by 39%.
Zinc is vital for several important physiological roles in the body and is needed for many enzymatic reactions including those necessary to stimulate muscle protein synthesis.
• Zinc deficiency has been linked to low IGF-1 Levels and Growth Hormone.
• Zinc also supports optimal testosterone levels and may increase testosterone at rest and after exercise.
• A 2006 study by Killic et al. found wrestlers who supplemented with Zinc for 4 weeks were able preserve circulating testosterone and thyroid hormone concentrations, which declined in placebo due to the exhaustive workload.
Magnesium is an essential mineral and electrolyte. It is involved in protein synthesis, ATP formation, metabolism of carbohydrates and fats, and bone strength.
• Magnesium deficiencies are the second most common deficiency in developed countries. A lack of magnesium will raise blood pressure and reduce insulin sensitivity.
• Increases in free and total testosterone have been noted in sedentary and athletic populations when supplementing with magnesium supplementation. It also acts as a muscle relaxer and may improve aerobic performance.
• Brilla et al. (1992) discovered 26 untrained subjects who participated in a 7 week strength training program in conjunction with magnesium supplementation were able to increase testosterone relative to baseline.
B6 is a water soluble vitamin that is important to various metabolic reactions that occur in the body. It is also a coenzyme for protein metabolism and nervous and immune system function.
• B6 is also involved in the synthesis of hormones and red blood cells.
• Vitamin B6 may have some benefits with regard to increasing the rate of synthesis of testosterone.
• B6 may also be able to increase levels of growth hormone.
Tribulus is an herb that is mostly recommended for male health including virility and vitality, and specifically more catered towards cardiovascular and urogenital health.
• It is a common supplement for its libido enhancing properties and testosterone boosting properties.
• The theory behind tribulus is it elevates luteinizing hormone, which in turn sends instructions to the testes causing them to make testosterone.
• Sellandi et al. (2012) found in men supplementing with tribulus for 60 days were able to increase testosterone by 16.3%.
Trigonella foenum-graecum, commonly known as fenugreek, is a popular herb in Arabic regions and India. It has traditionally been used to enhance libido and masculinity.
• Fenugreek has been shown to increase testosterone in healthy males, which is thought to be due to a backlog of testosterone conversion into DHT via inhibiting the 5-alpha reductase enzyme.
• Fenugreek has also been used to alleviate blood sugar metabolism problems like diabetes.
• A human study done by Wilborn et al. (2010) noted that fenugreek supplementation led to increases in testosterone and bio-available testosterone, while also decreasing body fat.
Increases L-Dopamine which stimulates testosterone synthesis and growth hormone secretions.
Horny Goat Weed Extract:
Horny goat weed that is often used as an erectile aid and aphrodisiac.
• It seems to have the mechanisms to increase testosterone, but no human studies exist on the subject matter.
• Horny goat weed was shown in one rat study to increase testosterone levels by 3x over a 7-day period compared to a control group.
DIM is a molecule that consists of two indole groups attached to a methane group. It is commonly found in broccoli and hold promise as an aromatase inhibitor.
• DIM has potent effects on estrogen metabolism and is able to keep the body relatively balanced by preventing either drastic increases or decreases in estrogen.
• DIM can both inhibit the aromatase enzyme (and prevent conversion of testosterone into estrogen) and it can act on more potent forms of estrogen and convert them into less potent forms; this conversion reduces the overall effects of estrogen in the body.
White Button Mushroom:
White button mushroom can be used to drive down estrogen levels via inhibiting the aromatase enzyme.
• Researchers at Beckman Research Institute, found out that that an extract prepared from white button mushrooms decreased the activity of aromatase enzyme and estrogen levels in a dose dependent manner.
Maca 4:1 Extract:
Maca is a plant in the broccoli family. Maca has traditionally been used as an aphrodisiac.
• Men supplementing with maca have been known to experience an increase in sperm production. Maca also appears to be a potent suppressor of prostate hypertrophy.
• Preliminary research also suggests maca can protect the brain from damage, improve bone health, and even improve cognitive ability in healthy people.
Polygonum Cuspidatum (20% Resveratrol):
Resveratrol is a member of a group of plant compounds called polyphenols.
• Resveratrol may increase testosterone levels in the blood and may be an agonist for androgen receptors.
• Research suggests that Resveratrol may have an anti-aromatase effect on testosterone, meaning that it does not get converted into estrogen at the same rate.
• In one study published in 2008 in the Archives of Pharmacal Research, Resveratrol was found to increase blood testosterone correlation by 51.6% in mice.
Q: What is the best way to take Testro Core?
A: As a dietary supplement take one serving 1 to 2 times daily.
Q: When is the best time to take Testro Core?
A: For optimal results take 15 minutes prior to working out.
Q: Do natural testosterone boosters really work?
A: Yes..dependent upon the right ingredients being used. The ingredients in Testro Core have been confirmed by research to boost natural testosterone levels for varying periods of time.
Q: Do I need to take a testosterone enhancer?
A: It may be beneficial to take a testosterone enhancer if you are older (40+), have low levels of testosterone, or are an athlete that needs a temporary boost to work through a hard training cycle.
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2. Naghii, M. R., Mofid, M., Asgari, A. R., Hedayati, M., & Daneshpour, M. S. (2011). Comparative effects of daily and weekly boron supplementation on plasma steroid hormones and proinflammatory cytokines. Journal of Trace Elements in Medicine and Biology, 25(1), 54-58.
1. Brilla, L. R., & Conte, V. (2000). Effects of a novel zinc-magnesium formulation on hormones and strength. J Exerc Physiol Online, 3(4), 26-36.
2. Kilic, M., Baltaci, A. K., Gunay, M., Gökbel, H., Okudan, N., & Cicioglu, I. (2005). The effect of exhaustion exercise on thyroid hormones and testosterone levels of elite athletes receiving oral zinc. Neuro endocrinology letters, 27(1-2), 247-252.
3. Kilic, M. (2007). Effect of fatiguing bicycle exercise on thyroid hormone and testosterone levels in sedentary males supplemented with oral zinc. Neuro endocrinology letters, 28(5), 681-685.
4. Jalali, G. R., Roozbeh, J., Mohammadzadeh, A., Sharifian, M., Sagheb, M. M., Jahromi, A. H., … & Afshariani, R. (2010). Impact of oral zinc therapy on the level of sex hormones in male patients on hemodialysis. Renal failure,32(4), 417-419.
5. Netter, A., Nahoul, K., & Hartoma, R. (1981). Effect of zinc administration on plasma testosterone, dihydrotestosterone, and sperm count. Archives of andrology, 7(1), 69-73.
6. Tupe, R. P., & Chiplonkar, S. A. (2009). Zinc supplementation improved cognitive performance and taste acuity in Indian adolescent girls. Journal of the American College of Nutrition, 28(4), 388-396.
7. Prasad, A. S., Beck, F. W., Bao, B., Fitzgerald, J. T., Snell, D. C., Steinberg, J. D., & Cardozo, L. J. (2007). Zinc supplementation decreases incidence of infections in the elderly: effect of zinc on generation of cytokines and oxidative stress. The American journal of clinical nutrition,85(3), 837-844.
1. Cinar, V., Polat, Y., Baltaci, A. K., & Mogulkoc, R. (2011). Effects of magnesium supplementation on testosterone levels of athletes and sedentary subjects at rest and after exhaustion. Biological trace element research, 140(1), 18-23.
2. van der Plas, A. A., Schilder, J. C., Marinus, J., & van Hilten, J. J. (2013). An explanatory study evaluating the muscle relaxant effects of intramuscular magnesium sulphate for dystonia in complex regional pain syndrome. The Journal of Pain, 14(11), 1341-1348.
3. Hatzistavri, L. S., Sarafidis, P. A., Georgianos, P. I., Tziolas, I. M., Aroditis, C. P., Zebekakis, P. E., … & Lasaridis, A. N. (2009). Oral magnesium supplementation reduces ambulatory blood pressure in patients with mild hypertension. American journal of hypertension, 22(10), 1070-1075.
4. Golf, S. W., Bender, S., & Grüttner, J. (1998). On the significance of magnesium in extreme physical stress. Cardiovascular Drugs and Therapy,12(2), 197-202.
5. Carpenter, T. O., DeLucia, M. C., Zhang, J. H., Bejnerowicz, G., Tartamella, L., Dziura, J., … & Cohen, D. (2006). A randomized controlled study of effects of dietary magnesium oxide supplementation on bone mineral content in healthy girls. The Journal of Clinical Endocrinology & Metabolism, 91(12), 4866-4872.
6. Held, K., Antonijevic, I. A., Künzel, H., Uhr, M., Wetter, T. C., Golly, I. C., … & Murck, H. (2002). Oral Mg (2+) supplementation reverses age-related neuroendocrine and sleep EEG changes in humans. Pharmacopsychiatry,35(4), 135-143.
7. Brilla, L. R., & Haley, T. F. (1992). Effect of magnesium supplementation on strength training in humans. Journal of the American College of Nutrition,11(3), 326-329.
1. Czaja, J., Lebiedzinska, A., Marszall, M., & Szefer, P. (2011). Evaluation for magnesium and vitamin B6 supplementation among Polish elite athletes.Roczniki Państwowego Zakładu Higieny, 62(4).
2. Manore, M. M. (2000). Effect of physical activity on thiamine, riboflavin, and vitamin B-6 requirements. The American journal of clinical nutrition, 72(2), 598s-606s.
1. Brown, G. A., Vukovich, M. D., Sharp, R. L., Reifenrath, T. A., Parsons, K. A., & King, D. S. (1999). Effect of oral DHEA on serum testosterone and adaptations to resistance training in young men. Journal of Applied Physiology, 87(6), 2274-2283.
2. Brown, G. A., Vukovich, M. D., Martini, E. R., Kohut, M. L., Franke, W. D., Jackson, D. A., & King, D. S. (2001). Effects of androstenedione-herbal supplementation on serum sex hormone concentrations in 30-to 59-year-old men. International journal for vitamin and nutrition research, 71(5), 293-301.
3. Brown, G. A., Vukovich, M. D., Martini, E. R., Kohut, M. L., Franke, W. D., Jackson, D. A., & King, D. S. (2001). Endocrine and lipid responses to chronic androstenediol-herbal supplementation in 30 to 58 year old men.Journal of the American College of Nutrition, 20(5), 520-528.
4. Sellandi, T. M., Thakar, A. B., & Baghel, M. S. (2012). Clinical study of Tribulus terrestris Linn. in Oligozoospermia: A double blind study. Ayu, 33(3), 356.
5. Dimitrov, M., Georgiev, P., & Vitanov, S. (1986). [Use of tribestan on rams with sexual disorders]. Veterinarno-meditsinski nauki, 24(5), 102-110.
1. Chevassus, H., Molinier, N., Costa, F., Galtier, F., Renard, E., & Petit, P. (2009). A fenugreek seed extract selectively reduces spontaneous fat consumption in healthy volunteers. European journal of clinical pharmacology, 65(12), 1175-1178.
2. Wilborn, C., Taylor, L., Poole, C., Foster, C., Willoughby, D., & Kreider, R. (2010). Effects of a Purported Aromatase and 5 α-Reductase Inhibitor on Hormone Profiles in College-Age Men. International journal of sport nutrition,20(6), 457.
3. Steels, E., Rao, A., & Vitetta, L. (2011). Physiological Aspects of Male Libido Enhanced by Standardized Trigonella foenum‐graecum Extract and Mineral Formulation. Phytotherapy Research, 25(9), 1294-1300.
4. Kochhar, A., & Nagi, M. (2005). Effect of supplementation of traditional medicinal plants on blood glucose in non-insulin-dependent diabetics: a pilot study. Journal of medicinal food, 8(4), 545-549.
5. Gupta, A., Gupta, R., & Lal, B. (2001). Effect of Trigonella foenum-graecum (fenugreek) seeds on glycaemic control and insulin resistance in type 2 diabetes mellitus: a double blind placebo controlled study. The Journal of the Association of Physicians of India, 49, 1057-1061.
Maca 4:1 Extract:
1. Brooks, N. A., Wilcox, G., Walker, K. Z., Ashton, J. F., Cox, M. B., & Stojanovska, L. (2008). Beneficial effects of Lepidium meyenii (Maca) on psychological symptoms and measures of sexual dysfunction in postmenopausal women are not related to estrogen or androgen content.Menopause, 15(6), 1157-1162.
2. Gonzales, G. F., Cordova, A., Vega, K., Chung, A., Villena, A., Góñez, C., & Castillo, S. (2002). Effect of Lepidium meyenii (MACA) on sexual desire and its absent relationship with serum testosterone levels in adult healthy men.andrologia, 34(6), 367-372.
3. Zenico, T., Cicero, A. F. G., Valmorri, L., Mercuriali, M., & Bercovich, E. (2009). Subjective effects of Lepidium meyenii (Maca) extract on well‐being and sexual performances in patients with mild erectile dysfunction: a randomised, double‐blind clinical trial. Andrologia, 41(2), 95-99.
4. Dording, C. M., Fisher, L., Papakostas, G., Farabaugh, A., Sonawalla, S., Fava, M., & Mischoulon, D. (2008). A Double‐Blind, Randomized, Pilot Dose‐Finding Study of Maca Root (L. Meyenii) for the Management of SSRI‐Induced Sexual Dysfunction. CNS Neuroscience & Therapeutics, 14(3), 182-191.
Horny Goat Weed Extract:
1. Zhang, Z. B., & Yang, Q. T. (2006). The testosterone mimetic properties of icariin. Asian journal of andrology, 8(5), 601-605.
1. Lo, R., & Matthews, J. (2010). A New Class of Estrogen Receptor Beta–Selective Activators. Molecular interventions, 10(3), 133.
2. Leong, H., Riby, J. E., Firestone, G. L., & Bjeldanes, L. F. (2004). Potent ligand-independent estrogen receptor activation by 3, 3′-diindolylmethane is mediated by cross talk between the protein kinase A and mitogen-activated protein kinase signaling pathways. Molecular Endocrinology, 18(2), 291-302.
3. Leong, H., Firestone, G. L., & Bjeldanes, L. F. (2001). Cytostatic effects of 3, 3′-diindolylmethane in human endometrial cancer cells result from an estrogen receptor-mediated increase in transforming growth factor-α expression. Carcinogenesis, 22(11), 1809-1817.
4. Sanderson, J. T., Slobbe, L., Lansbergen, G. W., Safe, S., & Van den Berg, M. (2001). 2, 3, 7, 8-Tetrachlorodibenzo-p-dioxin and diindolylmethanes differentially induce cytochrome P450 1A1, 1B1, and 19 in H295R human adrenocortical carcinoma cells. Toxicological sciences, 61(1), 40-48.
5. Safe, S., Wang, F., Porter, W., Duan, R., & McDougal, A. (1998). Ah receptor agonists as endocrine disruptors: antiestrogenic activity and mechanisms. Toxicology letters, 102, 343-347.
White Button Mushroom:
1. Chen, S., Oh, S. R., Phung, S., Hur, G., Ye, J. J., Kwok, S. L., … & Williams, D. (2006). Anti-aromatase activity of phytochemicals in white button mushrooms (Agaricus bisporus). Cancer research, 66(24), 12026-12034.
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