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10.1021/acs.jmedchem.5b00571

http://scihub22266oqcxt.onion/10.1021/acs.jmedchem.5b00571
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C4624220!4624220!26177091
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suck abstract from ncbi


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pmid26177091      J+Med+Chem 2015 ; 58 (15): 6002-17
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  • Design, Synthesis and Characterization of 3-(Benzylidene)indolin-2-one Derivatives as Ligands for ?-Synuclein Fibrils #MMPMID26177091
  • Chu W; Zhou D; Gaba V; Liu J; Li S; Peng X; Xu J; Dhavale D; Bagchi DP; d?Avignon A; Shakerdge NB; Bacskai BJ; Tu Z; Kotzbauer PT; Mach RH
  • J Med Chem 2015[Aug]; 58 (15): 6002-17 PMID26177091show ga
  • A series of 3-(benzilidine)indolin-2-one derivatives were synthesized and evaluated for their in vitro binding to alpha synuclein (?-syn), beta amyloid (A?), and tau fibrils. Compounds with a single double bond in the 3-position had only a modest affinity for ?-syn and no selectivity for ?-syn versus A? or tau fibrils. Homologation to the corresponding diene analogs yielded a mixture of Z,E and E,E isomers; substitution of the indoline nitrogen with an N-benzyl group resulted in increased binding to ?-syn and reasonable selectivity for ?-syn versus A? and tau. Introduction of a para-nitro group into the benzene ring of the diene enabled separation of the Z,E and E,E isomers and led to the identification of the Z,E configuration as the more active regioisomer. The data described here provide key structural information in the design of probes which bind preferentially to ?-syn versus A? or tau fibrils.
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