High Throughput in-silico Screening against Flexible Protein Receptors

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We report results for the in-silico screening of a database of 10000 ﬂexible compounds against various crystal structures of the thymidine kinase receptor complexed with 10 known inhibitors. The ligands were docked with the stochastic tunneling method using a ﬁrst-principle based scoring function. Using a rigid receptor we ﬁnd large deviations in the rank of the known inhibitors depending on the choice of receptor conformation. We then performed a screen in which critical receptor sidechains were permitted to change conformation and found improved scores for those inhibitors that did not dock well in any of the previous screens. These data demonstrate that the failure to dock did not originate from deﬁciencies in the scoring function or the docking algorithm, but from the neglect of receptor degrees of freedom.

Holger Merlitz, Wolfgang Wenzel

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Applied Computing | Critical Receptor Sidechains | ICCSA 2004 | Scoring Function | Thymidine Kinase Receptor |

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Added	01 Jul 2010
Updated	01 Jul 2010
Type	Conference
Year	2004
Where	ICCSA
Authors	Holger Merlitz, Wolfgang Wenzel

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High Throughput in-silico Screening against Flexible Protein Receptors

Applied Computing | Critical Receptor Sidechains | ICCSA 2004 | Scoring Function | Thymidine Kinase Receptor |

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