Investigation of active crystal morphogenesis peptide sequences from peptide libraries by crystallization on peptide functionalized beads

Krattiger, Philipp; Nassif, Nadine; Völkel, Antje; Mastai, Yitzhak; Wennemers, Helma; Cölfen, Helmut

Investigation of active crystal morphogenesis peptide sequences from peptide libraries by crystallization on peptide functionalized beads

Dateien

12790.pdfGröße: 2.45 MBDownloads: 959

Datum

2010

Autor:innen

Krattiger, Philipp

Nassif, Nadine

Völkel, Antje

Mastai, Yitzhak

Wennemers, Helma

Cölfen, Helmut

Open Access-Veröffentlichung

Open Access Green

Sammlungen

Chemie

Publikationstyp

Zeitschriftenartikel

Publikationsstatus

Published

Erschienen in

Colloids and Surfaces A: Physicochemical and Engineering Aspects. 2010, 354(1-3), pp. 218-225. ISSN 0927-7757. Available under: doi: 10.1016/j.colsurfa.2009.09.031

Zusammenfassung

In this study, split-and-mix peptide libraries from one to four amino acids bound to functionalized beads were used to identify active morphogenesis peptides for the systems CaCO3 and dl-alanine. Density gradient ultracentrifugation was used to remove all beads without crystals as well as crystals homogeneously nucleated in solution. From the remaining fractions, beads were selected, which account for differences in crystal morphologies from the default crystal morphology on a micrometer scale and their amino acid sequence was analyzed. Our results show that multiple and different peptide sequences are found to be active in the morphogenesis of CaCO3 and dl-alanine. It was not possible to find a correlation, which connects active single amino acids with the sequences of di-, tri- and tetrapeptides. However, peptide charge was found to be important for morphogenesis. Peptides active in CaCO3 morphogenesis were enriched in basic amino acids while those active for dl-alanine morphogenesis contained more acidic amino acids. This can be explained by charge charge interactions of the crystallizing species with the countercharged peptide moieties. Tests for chiral separation for the dl-alanine system showed that with the applied oligopeptide libraries, no enantioselective crystallization was achieved to a significant extent. The presented combinatorial crystallization assay provides an easy tool for crystallization control, which can be used for the straightforward selection of interesting species under a light microscope. However, suitable staining techniques to identify individual beads with crystals, which are for example a pure enantiomer still need to be developed.

Fachgebiet (DDC)

540 Chemie

Schlagwörter

Split-and-mix peptide libraries, CaCO3, dl-Alanine, Morphogenesis, Crystallization control

Zitieren

ISO 690

KRATTIGER, Philipp, Nadine NASSIF, Antje VÖLKEL, Yitzhak MASTAI, Helma WENNEMERS, Helmut CÖLFEN, 2010. Investigation of active crystal morphogenesis peptide sequences from peptide libraries by crystallization on peptide functionalized beads. In: Colloids and Surfaces A: Physicochemical and Engineering Aspects. 2010, 354(1-3), pp. 218-225. ISSN 0927-7757. Available under: doi: 10.1016/j.colsurfa.2009.09.031

BibTex

@article{Krattiger2010Inves-10003,
  year={2010},
  doi={10.1016/j.colsurfa.2009.09.031},
  title={Investigation of active crystal morphogenesis peptide sequences from peptide libraries by crystallization on peptide functionalized beads},
  number={1-3},
  volume={354},
  issn={0927-7757},
  journal={Colloids and Surfaces A: Physicochemical and Engineering Aspects},
  pages={218--225},
  author={Krattiger, Philipp and Nassif, Nadine and Völkel, Antje and Mastai, Yitzhak and Wennemers, Helma and Cölfen, Helmut}
}

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Universitätsbibliographie

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