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2-amino-6-hydroxybenzonitrile is a chemical with a specific purpose. Lookchem provides you with multiple data and supplier information of this chemical.

859960-36-4

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859960-36-4 Usage

Physical state

pale yellow crystalline solid

Applications

building block in synthesis of pharmaceuticals and agrochemicals
Key intermediate in production of pramipexole, used to treat restless legs syndrome and Parkinson's disease
Key ingredient in synthesis of fungicides, herbicides, and insecticides

Toxicity

toxic if ingested or inhaled, can cause skin and eye irritation.

Check Digit Verification of cas no

The CAS Registry Mumber 859960-36-4 includes 9 digits separated into 3 groups by hyphens. The first part of the number,starting from the left, has 6 digits, 8,5,9,9,6 and 0 respectively; the second part has 2 digits, 3 and 6 respectively.
Calculate Digit Verification of CAS Registry Number 859960-36:
(8*8)+(7*5)+(6*9)+(5*9)+(4*6)+(3*0)+(2*3)+(1*6)=234
234 % 10 = 4
So 859960-36-4 is a valid CAS Registry Number.

859960-36-4Downstream Products

859960-36-4Relevant academic research and scientific papers

The discovery of 2-substituted phenol quinazolines as potent RET kinase inhibitors with improved KDR selectivity

Newton, Rebecca,Bowler, Katherine A.,Burns, Emily M.,Chapman, Philip J.,Fairweather, Emma E.,Fritzl, Samantha J.R.,Goldberg, Kristin M.,Hamilton, Niall M.,Holt, Sarah V.,Hopkins, Gemma V.,Jones, Stuart D.,Jordan, Allan M.,Lyons, Amanda J.,Nikki March,McDonald, Neil Q.,Maguire, Laura A.,Mould, Daniel P.,Purkiss, Andrew G.,Small, Helen F.,Stowell, Alexandra I.J.,Thomson, Graeme J.,Waddell, Ian D.,Waszkowycz, Bohdan,Watson, Amanda J.,Ogilvie, Donald J.

, p. 20 - 32 (2016)

Deregulation of the receptor tyrosine kinase RET has been implicated in medullary thyroid cancer, a small percentage of lung adenocarcinomas, endocrine-resistant breast cancer and pancreatic cancer. There are several clinically approved multi-kinase inhibitors that target RET as a secondary pharmacology but additional activities, most notably inhibition of KDR, lead to dose-limiting toxicities. There is, therefore, a clinical need for more specific RET kinase inhibitors. Herein we report our efforts towards identifying a potent and selective RET inhibitor using vandetanib 1 as the starting point for structure-based drug design. Phenolic anilinoquinazolines exemplified by 6 showed improved affinities towards RET but, unsurprisingly, suffered from high metabolic clearance. Efforts to mitigate the metabolic liability of the phenol led to the discovery that a flanking substituent not only improved the hepatocyte stability, but could also impart a significant gain in selectivity. This culminated in the identification of 36; a potent RET inhibitor with much improved selectivity against KDR.

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