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• W2077247175 abstract "Abstract Here we report the synthesis of a number of compounds structurally related to arginine methyltransferase inhibitor 1 (AMI‐1). The structural alterations that we made included: 1) the substitution of the sulfonic groups with the bioisosteric carboxylic groups; 2) the replacement of the ureidic function with a bis‐amidic moiety; 3) the introduction of a N‐containing basic moiety; and 4) the positional isomerization of the aminohydroxynaphthoic moiety. We have assessed the biological activity of these compounds against a panel of arginine methyltransferases (fungal RmtA, hPRMT1, hCARM1, hPRMT3, hPRMT6) and a lysine methyltransferase (SET7/9) using histone and nonhistone proteins as substrates. Molecular modeling studies for a deep binding‐mode analysis of test compounds were also performed. The bis‐carboxylic acid derivatives 1 b and 7 b emerged as the most effective PRMT inhibitors, both in vitro and in vivo, being comparable or even better than the reference compound (AMI‐1) and practically inactive against the lysine methyltransferase SET7/9." @default.
• W2077247175 created "2016-06-24" @default.
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• W2077247175 date "2010-02-19" @default.
• W2077247175 modified "2023-10-17" @default.
• W2077247175 title "Design, Synthesis and Biological Evaluation of Carboxy Analogues of Arginine Methyltransferase Inhibitor 1 (AMI-1)" @default.
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• W2077247175 doi "https://doi.org/10.1002/cmdc.200900459" @default.
• W2077247175 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/20091730" @default.
• W2077247175 hasPublicationYear "2010" @default.
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