Automated docking with protein flexibility in the design of femtomolar "click Chemistry" inhibitors of acetylcholinesterase

Garrett M. Morris; Luke G. Green; Zoran Radić; Palmer Taylor; K. Barry Sharpless; Arthur J. Olson; Flavio Grynszpan

doi:10.1021/ci300545a

Automated docking with protein flexibility in the design of femtomolar "click Chemistry" inhibitors of acetylcholinesterase

Garrett M. Morris, Luke G. Green, Zoran Radić, Palmer Taylor, K. Barry Sharpless, Arthur J. Olson, Flavio Grynszpan

מדעי הכימיה

פרסום מחקרי: פרסום בכתב עת › מאמר › ביקורת עמיתים

38 ציטוטים ‏(Scopus)

תקציר

The use of computer-aided structure-based drug design prior to synthesis has proven to be generally valuable in suggesting improved binding analogues of existing ligands.(1) Here we describe the application of the program AutoDock(2) to the design of a focused library that was used in the "click chemistry in-situ" generation of the most potent noncovalent inhibitor of the native enzyme acetylcholinesterase (AChE) yet developed (K_d = ∼100 fM).(3) AutoDock version 3.0.5 has been widely distributed and successfully used to predict bound conformations of flexible ligands. Here, we also used a version of AutoDock which permits additional conformational flexibility in selected amino acid side chains of the target protein.

שפה מקורית	אנגלית
עמודים (מ-עד)	898-906
מספר עמודים	9
כתב עת	Journal of Chemical Information and Modeling
כרך	53
מספר גיליון	4
מזהי עצם דיגיטלי (DOIs)	https://doi.org/10.1021/ci300545a
סטטוס פרסום	פורסם - 22 אפר׳ 2013

גישה למסמך

10.1021/ci300545a

קבצים וקישורים אחרים

Link to publication in Scopus

פורמט ציטוט ביבליוגרפי

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title = "Automated docking with protein flexibility in the design of femtomolar {"}click Chemistry{"} inhibitors of acetylcholinesterase",

abstract = "The use of computer-aided structure-based drug design prior to synthesis has proven to be generally valuable in suggesting improved binding analogues of existing ligands.(1) Here we describe the application of the program AutoDock(2) to the design of a focused library that was used in the {"}click chemistry in-situ{"} generation of the most potent noncovalent inhibitor of the native enzyme acetylcholinesterase (AChE) yet developed (Kd = ∼100 fM).(3) AutoDock version 3.0.5 has been widely distributed and successfully used to predict bound conformations of flexible ligands. Here, we also used a version of AutoDock which permits additional conformational flexibility in selected amino acid side chains of the target protein.",

author = "Morris, {Garrett M.} and Green, {Luke G.} and Zoran Radi{\'c} and Palmer Taylor and Sharpless, {K. Barry} and Olson, {Arthur J.} and Flavio Grynszpan",

year = "2013",

month = apr,

day = "22",

doi = "10.1021/ci300545a",

language = "אנגלית",

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journal = "Journal of Chemical Information and Modeling",

issn = "1549-9596",

publisher = "American Chemical Society",

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}

Automated docking with protein flexibility in the design of femtomolar "click Chemistry" inhibitors of acetylcholinesterase. / Morris, Garrett M.; Green, Luke G.; Radić, Zoran et al.
ב-: Journal of Chemical Information and Modeling, כרך 53, מס' 4, 22.04.2013, עמוד 898-906.

פרסום מחקרי: פרסום בכתב עת › מאמר › ביקורת עמיתים

TY - JOUR

T1 - Automated docking with protein flexibility in the design of femtomolar "click Chemistry" inhibitors of acetylcholinesterase

AU - Morris, Garrett M.

AU - Green, Luke G.

AU - Radić, Zoran

AU - Taylor, Palmer

AU - Sharpless, K. Barry

AU - Olson, Arthur J.

AU - Grynszpan, Flavio

PY - 2013/4/22

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AB - The use of computer-aided structure-based drug design prior to synthesis has proven to be generally valuable in suggesting improved binding analogues of existing ligands.(1) Here we describe the application of the program AutoDock(2) to the design of a focused library that was used in the "click chemistry in-situ" generation of the most potent noncovalent inhibitor of the native enzyme acetylcholinesterase (AChE) yet developed (Kd = ∼100 fM).(3) AutoDock version 3.0.5 has been widely distributed and successfully used to predict bound conformations of flexible ligands. Here, we also used a version of AutoDock which permits additional conformational flexibility in selected amino acid side chains of the target protein.

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Automated docking with protein flexibility in the design of femtomolar "click Chemistry" inhibitors of acetylcholinesterase

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