J. Med. Chem.
 1990
DOI: 10.1021/jm00170a005
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Purine derivatives as competitive inhibitors of human erythrocyte membrane phosphatidylinositol 4-kinase

R. C. Young1,
Martin Jones2,
Kevin J. Milliner3
et al.

Abstract: The possibility of deriving a potent, cell-penetrating inhibitor of human erythrocyte PI 4-kinase, competitive with respect to ATP, has been investigated in a series of purine derivatives and analogues. The purine nucleus is not essential for binding to the ATP site but offers the advantage of synthetic accessibility to its derivatives. The optimum substitution pattern in purine was found to be an electron-releasing substituent in the 6-position (e.g. amino, as in adenine, 1) and a compact, lipophilic group in… Show more

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Cited by 38 publications
(14 citation statements)
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“…In early 90's, several purine and 7-deazapurine derivatives from both natural and synthetic sources (e.g., 9-cyclohexyladenine or echiguanine A) were identified as inhibitors of PI4K from human erythrocytes [115][116][117][118][119] which was subsequently identified as PI4K IIα [120]. An ATP analog was also found to inhibit PI4K class II enzyme from sheep brain with potency comparable to that of adenosine [121].…”
Section: Inhibitors Of Pi4ks and Their Potential In Human Medicinementioning
confidence: 99%

Phosphatidylinositol 4-kinases: Function, structure, and inhibition

Bouřa
1
,
Nencka
2
2015
Experimental Cell Research
130
2
107
0
1
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“…In early 90's, several purine and 7-deazapurine derivatives from both natural and synthetic sources (e.g., 9-cyclohexyladenine or echiguanine A) were identified as inhibitors of PI4K from human erythrocytes [115][116][117][118][119] which was subsequently identified as PI4K IIα [120]. An ATP analog was also found to inhibit PI4K class II enzyme from sheep brain with potency comparable to that of adenosine [121].…”
Section: Inhibitors Of Pi4ks and Their Potential In Human Medicinementioning
confidence: 99%

Phosphatidylinositol 4-kinases: Function, structure, and inhibition

Bouřa
1
,
Nencka
2
2015
Experimental Cell Research
130
2
107
0
1
View full textAdd to dashboardCite
“…The next step involved ring-closure, which was carried out on three different ways. Compounds 8 − 11 were prepared by ring closure of the appropriate carboxylic acids and 3,4-diaminoquinoline ( 6 ) in polyphosphoric acid . Compounds 12 and 13 were prepared by ring-closure of 2-furoyl chloride and hexanoyl chloride, respectively, with 3,4-diaminoquinoline ( 6 ) .…”
Section: Resultsmentioning
confidence: 99%
“…Compounds 8-11 were prepared by ring closure of the appropriate carboxylic acids and 3,4-diaminoquinoline (6) in polyphosphoric acid. 21 Compounds 12 and 13 were prepared by ring-closure of 2-furoyl chloride and hexanoyl chloride, respectively, with 3,4-diaminoquinoline (6). 22 Compound 7 was prepared by ring-closure of 3,4-diaminoquinoline (6) with formic acid in trimethylorthoformate.…”
Section: Resultsmentioning
confidence: 99%

Structure−Activity Relationships of New 1H-Imidazo[4,5-c]quinolin-4-amine Derivatives as Allosteric Enhancers of the A3 Adenosine Receptor

Göblyös
1
,
Gao
2
,
Brussee
3
et al. 2006
J. Med. Chem.
51
4
78
0
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“…43 Our switchable 5-nitrosopyrimidines might thus mimic two different purine derivatives depending on the orientation of the nitroso group. For example, form A of compound 6e (Figure 6) resembles 2amino-9-phenyladenine, which can act as a phosphatidylinositol-kinase inhibitor, 44 whereas form B of the same compound resembles 2-amino-6-phenylaminopurine, which can act as a cytokinin-receptor activator. 45 Theoretically, one compound may hence target two different metabolic pathways.…”
Section: ■ Conclusionmentioning
confidence: 99%

A Switchable Intramolecular Hydrogen Bond in Polysubstituted 5-Nitrosopyrimidines

Procházková
1
,
Čechová
2
,
Janeba
3
et al. 2013
J. Org. Chem.
14
4
7
0
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