Literature DB >> 17637338

FASTDXL: a generalized screen to trap disulfide-stabilized complexes for use in structural studies.

Jacob E Corn1, James M Berger.   

Abstract

Structural studies of macromolecular complexes have produced extraordinary insights into a wide variety of biological processes. Unfortunately, as structural biologists pursue larger and more challenging assemblies, weakly stable and/or nonspecific interactions can become significant roadblocks to structure determination. We have developed a rapid and effective pool-based screen, termed FASTDXL (focused array screening technique for disulfide X-linking), to produce and identify disulfide-stabilized protein-nucleic acid assemblies. A significant strength of FASTDXL is that it can take advantage of prior structural knowledge about molecular interactions, but does not necessarily rely upon it. A detailed application of the approach to the difficult problem of trapping a bacterial primase-ssDNA complex is described, validating the method as a route toward obtaining diffracting crystals suitable for structure determination.

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Year:  2007        PMID: 17637338      PMCID: PMC2041450          DOI: 10.1016/j.str.2007.05.006

Source DB:  PubMed          Journal:  Structure        ISSN: 0969-2126            Impact factor:   5.006


  15 in total

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  7 in total

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Journal:  Protein Sci       Date:  2018-12-22       Impact factor: 6.725

3.  Enforced presentation of an extrahelical guanine to the lesion recognition pocket of human 8-oxoguanine glycosylase, hOGG1.

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5.  Structural model of the p14/SF3b155 · branch duplex complex.

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6.  Protein engineering of the quaternary sulfiredoxin.peroxiredoxin enzyme.substrate complex reveals the molecular basis for cysteine sulfinic acid phosphorylation.

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7.  Binding mechanism of metal⋅NTP substrates and stringent-response alarmones to bacterial DnaG-type primases.

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  7 in total

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