66365-41-1

Upstream product

• 592-87-0 lead(II) thiocyanate 
• 603-35-0 triphenylphosphine 

Downstream Products

• 72411-06-4 1-sec-Butyl-1-phenyl-3-phenylacetyl-thiourea 
• 71808-89-4 2-Thiocyanato-3-methyl-2-cyclohexenon 
• 71808-90-7 2-Thiocyanato-3,5,5-trimethyl-2-cyclohexenon 
• 68267-50-5 1-cyclohexyl-1-methylthiourea 
• 72411-05-3 1-Ethyl-1-phenyl-3-phenylacetyl-thiourea 
• 3955-58-6 N-ethyl-N-phenylthiourea 
• 72411-02-0 N-phenyl-N'-phenylacetyl-thiourea 
• 21257-55-6 N-hexanoyl-N'-phenyl-thiourea 
• 72411-03-1 N‐(phenylcarbamothioyl)cyclohexanecarboxamide 
• 53393-11-6 1-benzyl-1-methylthiourea 
• 68315-07-1 C₂₇H₂₅N₂PS 
• 72411-00-8 1-Benzyl-3-cyclohexanecarbonyl-1-methyl-thiourea 
• 72411-04-2 1-Methyl-1-phenyl-3-phenylacetyl-thiourea 
• 4104-75-0 1-methyl-1-phenylthiourea 

Relevant academic research and scientific papers

Synthesis, structure elucidation, DNA-PK and PI3K and anti-cancer activity of 8- and 6-aryl-substituted-1-3-benzoxazines

The synthesis of 6-aryl, 8- aryl, and 8-aryl-6-chloro-2-morpholino-1,3-benzoxazines with potent activity against PI3K and DNA-PK is described. Synthesis of thirty one analogues was facilitated by an improved synthesis of 3-bromo-2-hydroxybenzoic acid 13 by de-sulphonation of 3-bromo-2-hydroxy-5-sulfobenzoic acid 12 en route to 2-methylthio-substituted-benzoxazine intermediates 17-19. From this series, compound 20k (LTURM34) (dibenzo[b,d]thiophen-4-yl) (IC50 = 0.034 μM) was identified as a specific DNA-PK inhibitor, 170 fold more selective for DNA-PK activity compared to PI3K activity. Other compounds of the series show markedly altered selectivity for various PI3K isoforms including compound 20i (8-(naphthalen-1-yl) a potent and quite selective PI3Kδ inhibitor (IC50 = 0.64 μM). Finally, nine compounds were evaluated and showed antiproliferative activity against an NCI panel of cancer cell lines. Compound 20i (8-(naphthalen-1-yl) showed strong anti-proliferative activity against A498 renal cancer cells that warrants further investigation.

Functionalization of quinazolin-4-ones part 1: Synthesis of novel 7-substituted-2-thioxo quinazolin-4-ones from 4-substituted-2-aminobenzoic acids and PPh3(SCN)2

4-(Nitro, amino, acetylamino)-2-aminobenzoic acid were allowed to react with PPh3(SCN)2 and gave the crossholding 7-nitro, 7-acetylamino- and 7-amino-2-thioxo quinazolin-4-ones respectively. The nature of the substituent at position 4 of the 2-aminobenzoic acids has significant influence on the outcome of the cyclisation reaction with PPh 3(SCN)2. Similarly, the nature of the substituent at position 7 of the 2-substituted quinazolin-4-ones significantly affected the ease with which alkylation reactions could be performed. The alkylation selectivity of the 7- substiuted-2-thioxo quinazolin-4-ones was found to depend on the nature of the alkyl halide and the nature of the substituent at position 2.