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Tadalafil is a selective phosphodiesterase type 5 (PDE5) inhibitor that is commonly used to treat erectile dysfunction. PDE5 is an enzyme that regulates cGMP, a signalling pathway involved in various physiological processes. By selectively inhibiting PDE5, tadalafil prevents the degradation of cGMP. Increased accumulation of cGMP in penile tissues causes relaxation of vascular smooth muscles, thus enhancing blood flow and resulting in erection. PDE5 is expressed in various tissues, including lung, brain, kidney and cardiac myocytes.
Tadalafil was first approved in 2003 for erectile dysfunction and was marketed under the brand name, Cialis. Later, it got approved for pulmonary arterial hypertension (PAH) in 2009. Research shows that tadalafil might improve cardiovascular health and treat cancers. At Elements Sarms, liquid cialis for sale is limited to educational and research purposes.
From Pubchem
IUPAC Name:(2R,8R)-2-(1,3-benzodioxol-5-yl)-6-methyl-3,6,17-triazatetracyclo[8.7.0.03,8.011,16]heptadeca-1(10),11,13,15-tetraene-4,7-dioneSynonyms: Cialis, TadanafilMolecular Formula: C22H19N3O4Molecular Weight: 389.4 g/molCAS Number: 171596-29-5PubChem CID: 110635
Tadalafil was approved by the FDA after various clinical trials successfully demonstrated its efficacy. In a randomized double-blind placebo-controlled trial, 348 men with erectile dysfunction were randomly given 20 mg of tadalafil or placebo. Further, patients were randomized to two four-week treatment intervals during which they were asked to engage in sexual intercourse after 24 and 36 hours of dose administration. The results found that tadalafil significantly improved intercourse attempts with higher rates at both 36 hours (59.2%) and 24 hours (52.9%) post-dosing compared to placebo [1].
Research shows that daily tadalafil is more effective in improving erectile function than on-demand tadalafil [2]. A long-term efficacy study found that tadalafil at doses of 5mg, 10mg and 20mg daily for up to 18-24 months is generally well tolerated [3]. Moreover, the comparison studies revealed that tadalafil might be preferred over sildenafil because of its long duration of action [4].
Benign prostatic hyperplasia (BPH) is characterized by the proliferation of smooth and epithelial cells in the prostrate transition zone, resulting in prostate enlargement. The enlarged prostate can obstruct the urinary flow and cause lower urinary tract symptoms, like frequent urination, incomplete urination and dribbling. Various clinical trials indicate that tadalafil can improve lower urinary tract symptoms secondary to BPH in men with and without erectile dysfunction [5, 6].
Tadalafil might achieve this effect by upregulating NO/cGMP activity, resulting in reduced smooth muscle tension and cellular growth within the prostate and bladder. It more effectively relaxes prostatic tissue and influences afferent nerve activity than other PDE5 inhibitors. This mechanism enhances blood perfusion and reduces inflammation markers [7].
From NCBI
Besides regulating the levels of cGMP, PDE-5 inhibitors have been known to increase the levels of cAMP (cyclic adenosine monophosphate). cGMP and cAMP play a significant role in mediating various brain functions under various physiological and pathological conditions. One study found that tadalafil improves functional recovery in rat model of embolic stroke, which is attributed to enhanced levels of cGMP and increased angiogenesis [8].
Research on animal models found that tadalafil can alleviate the effect of injury to the spinal cord by increased nitric oxide (NO) and superoxide dismutase (SOD). NO acts as a retrograde transmitter and causes enhanced production of cGMP, while SOD neutralizes the superoxide radicals and reduces oxidative stress in the body. By increasing the production of NO and SOD, tadalafil might enhance the beneficial response to injury and mitigate the oxidative stress caused by spinal cord injury [9].
Research shows that tadalafil might exert a positive impact on diabetes. In diabetic patients, insulin resistance impairs the NO signalling pathway and obesity promotes inflammation. One study in diabetic rats found that 1mg/kg tadalafil administration for 28 days reduced fasting blood glucose and triglyceride levels. Further, it reduced the infarct size following ischemia-reperfusion injury and decreased the levels of inflammatory cytokines and chemokines [10].
In another study, diabetic mice treated with tadalafil every 48 hours for 8 weeks showed improved nerve conduction, thermal sensitivity, blood flow, vessel density, and nerve fiber density. Tadalafil also reversed diabetes-induced changes in axon diameter, myelin thickness, and protein levels related to nerve growth factors. These findings suggest that tadalafil enhances regional blood flow in sciatic nerve tissue, potentially improving nerve function and alleviating diabetic peripheral neuropathy [11].
Tadalafil is a phosphodiesterase type 5 inhibitor with a long half-life of 17 hours. FDA has approved it for the treatment of pulmonary arterial hypertension, erectile dysfunction and lower urinary tract symptoms secondary to benign prostatic hyperplasia. Further, it is being explored for its effect on Duchenne Muscular Dystrophy and Pancreatic cancer. If you are wondering where to buy tadalafil, Element Sarms offers the option to purchase cialis liquid of premium quality exclusively for research purposes. Only buy tadalafil if you are a qualified researcher.
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