Kishore K. Rana scite author profile

Kishore K. Rana

4Publications

28Citation Statements Received

8Citation Statements Given

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Affiliations

Molecular Discovery (United Kingdom), GlaxoSmithKline (United Kingdom)

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Purine derivatives as competitive inhibitors of human erythrocyte membrane phosphatidylinositol 4-kinase

Young¹,

Jones²,

Milliner³

et al. 1990

J. Med. Chem.

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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 either the 8-position or, preferably, the 9-position, suggesting the importance of the N-1 lone pair and hydrophobic contributions of the 8- and 9-substituents to binding. The most potent inhibitor synthesized was 9-cyclohexyladenine (54), which has an apparent Ki value of 3.7 microM.

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Improved syntheses of inositol phospholipid analogues

Jones¹,

Rana²,

Ward³

et al. 1989

Tetrahedron Letters

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A Novel Preparation of 2‐Naphthyl and 5‐Benzo[B]thienyl Methanesulfonyl Chlorides.

Walker

Rana

2003

ChemInform

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A Novel Preparation of 2-Naphthyl and 5-Benzo[B]thienyl Methanesulfonyl Chlorides

Walker

Rana

2003

Synthetic Communications

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Kishore K. Rana

Purine derivatives as competitive inhibitors of human erythrocyte membrane phosphatidylinositol 4-kinase

Improved syntheses of inositol phospholipid analogues

A Novel Preparation of 2‐Naphthyl and 5‐Benzo[B]thienyl Methanesulfonyl Chlorides.

A Novel Preparation of 2-Naphthyl and 5-Benzo[B]thienyl Methanesulfonyl Chlorides

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