TESTOLONE (RAD-140) – Solution, 600mg (20mg/mL)
SKU: 84240974619

TESTOLONE (RAD-140) – Solution, 600mg (20mg/mL)

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Description

TESTOLONE (RAD-140) – Solution, 600mg (20mg/mL)TESTOLONE (RAD 140) RAD 140 Effects on Animal Body Mass RAD 140 SARM, chemically known as (2 chloro 4 [[(1R,2S) 1 [5 (4 cyanophenyl) 1,3,4 oxadiazol 2 yl] 2 hydroxypropyl]amino] 3 methylbenzonitrile), also known as testolone, was originally synthesized by Radius Health Inc. in collaboration with researchers from the University of Illinois, Obiter Research, and Cambridge Major Laboratories. According to the initial study detailing the synthesis and

TESTOLONE (RAD-140)

RAD 140 Effects on Animal Body Mass

RAD 140 SARM, chemically known as (2-chloro-4-[[(1R,2S)-1-[5-(4-cyanophenyl)-1,3,4-oxadiazol-2-yl]-2-hydroxypropyl]amino]-3-methylbenzonitrile), also known as testolone, was originally synthesized by Radius Health Inc. in collaboration with researchers from the University of Illinois, Obiter Research, and Cambridge Major Laboratories.

According to the initial study detailing the synthesis and preliminary findings of the compound, RAD140 exhibits high stability (with a half-life of more than 2 hours) in incubations with rat and monkey microsomes. It also has a high affinity for the androgen receptor, with a Ki of 7 nM, approximately four times higher than that of testosterone itself. Simultaneously, the nearest hormone receptor activated by RAD140 was progesterone, at a level of 750 nM.

Early primate studies indicated that even at the lowest dose of 0.1 mg/kg, juvenile macaques gained an average of 10% body weight over a trial period of 28 days. This increase was primarily confirmed to be lean body mass, as indicated by DEXA scans conducted before and after the trial period. These results were, however, somewhat variable.

RAD 140 Effects on Neurons

In a study conducted by Jayaraman et al., castrated male rats were investigated to determine the neuroprotective effects of RAD 140 supplementation, with a view towards potential applications of SARMs against neurodegenerative diseases.

The rats were orally provided with 1 mg/kg of RAD 140 per day for two weeks. It was found that RAD140 was able to significantly reduce apoptosis caused by Aβ, apoptosis activator II, and hydrogen peroxide. This is attributed to the role that MAPK signaling plays in neuroprotection.

Aβ was by far the most potent trigger of apoptosis introduced to the rats. After 24 hours of exposure to Aβ, the number of viable neurons in the rats had decreased by 50%. However, when administered RAD 140 in a concentration-dependent manner, the viability of the neurons increased exponentially. The most effective concentration of RAD 140 was 100 nM, leading to approximately 90% neuron survival after Aβ exposure (Source).

In addition to measuring the neuroprotective effects against various forms of apoptosis, researchers also measured the effects RAD 140 had on kainate-induced neuron death. It was found that this form of neuron death was significantly reduced compared to a control group (Source).

Concentration
20mg/ml.

Half Life
16 hours.

DISCLAIMER
This material is sold for use in laboratory research only. Terms of sale apply. Not for human consumption, nor for medical, veterinary or domestic use. Please familiarize yourself with our DISCLAIMER before ordering.

 

Data Sheet

RAD140 (Testolone) – Solution, 600mg (20mg/mL)

Application Selective Androgen Receptor Modulator
CAS 1182367-47-0
Molar Mass 393.83 g/mol
 Chemical Formula C20H16ClN5O2
IUPAC Name 2-chloro-4-{[(1R,2S)-1-[5-(4-cyanophenyl)-1,3,4-oxadiazol-2-yl]-2-hydroxypropyl]amino}-3-methylbenzonitrile
Synonyms RAD140, RAD-140, Testolone
Storage Room temperature
Solubility Soluble in Ethanol, PEG400
Organoleptic Profile Clear Liquid
Physical Form Solution in PEG400
Specification 20mg/mL ±5%
Terms This material is sold for laboratory research use only. Terms of sale apply. Not for human consumption, nor medical, veterinary, or household uses. Please familiarize yourself with our Terms & Conditions prior to ordering.
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SKU: 84240974619

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J
John Matlock
Cuba, US
★★★★★ 5
It's How Wars End That Become Important Afterward
Format: Paperback
The twentiety century taught us a lot about wars and how they end. World War I showed us that making strong demands on the defeated (who didn't admit defeat to their own people) set the stage for the next big war. World War II was fought until the Unconditional Surrender of the Germans and Japanese. Something that thinkers still debate as having made them fight all that harder. VietNam was fought with no clear end in sight, and "another VietNam" entered our language. The first Gulf War was ended when Colin Powell and Bush II debated how to end the war. They stopped before they had to go in and see what the Sunni's, Shiite's and Kurds made of the power vacuum left by the removal of Saddam would have created. Bush II is learning about this now. This is the second revised edition of this book, originally published in 1971 and then updated in 1991 and now 2005 to reflect happenings in new wars. Still some of the old wars had interesting insights that I didn't know before, such as how Finland, originally on Germany's side against Russia, made a peace with Russia and kicked the Germans out before they became a Russian province. Great Book.
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Reviewed in the United States on April 6, 2005
C
César González Rouco
Omaha, US
★★★★★ 3
Complementary readings
Format: Paperback
There are already three good reviews so I will only suggest reading the following books instead of, or in addition to, this peculiar work: a) "War in human civilization" by Azar Gat; b) "War before Civilization. The Myth of the Peaceful Savage", by Lawrence Keeley; c) "How War Began" by Keith F. Otterbein; d) "War and Peace and War: The Rise and Fall of Empires" by Peter Turchin; and e) "War and the Law of Nations: A General History" by Stephen Neff.
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Reviewed in the United States on August 8, 2009
B
bjcefola
Belleville, US
★★★★★ 5
Excellent short-book analysis
Format: Paperback
This short book is an outstanding analysis of how nations end wars, or accept peace. Ikle shows how governments often prefer obviously self-destructive courses rather then compromise peace terms. The problem is most acute when factional interests dominate strategy rather then a rational unitary interest. In such a circumstance, factions that benefit from continuing the war will accuse those pursuing peace of treason. Sadly, there is no equivalent derogatory word in English for those who pursue war to the detriment of their country. The book was first written in 1971, and most of the examples are from the two world wars. The work is still extremely relevant, and at 130 pages it's well worth the time. Highly recommended as a first book to read on ending war.
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Reviewed in the United States on May 4, 2007
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Nick
Massapequa, US
★★★★★ 5
eye-opener
Format: Paperback
Great book
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Reviewed in the United States on April 23, 2026
A
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Atiqullah
Lexington, US
★★★★★ 5
Excellent everyday strategies
Format: Paperback
This helped me to get whatever I want
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Reviewed in the United States on September 5, 2024

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