Probing the self‐association, intermolecular contacts, and folding propensity of amelogenin

Ndao, Moise; Dutta, Kaushik; Bromley, Keith M.; Lakshminarayanan, Rajamani; Sun, Zhi; Rewari, Gita; Moradian‐Oldak, Janet; Evans, John Spencer

doi:10.1002/pro.603

Cited by 28 publications

(65 citation statements)

References 48 publications

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“…40 Based on the PPII propensity scale for individual amino acid residues, we previously reported that PPII is the dominant structure in the central region of amelogenin 33 and our solvent engineering studies confirmed that the Pro, Gln central domain is resistant to folding. 40 The rigidity in the central region and flexibility at the N- and C- termini may have important functional significance for amelogenin in vivo . 40 …”

Section: Amelogenin and Its Targetssupporting

confidence: 61%

“…40 The rigidity in the central region and flexibility at the N- and C- termini may have important functional significance for amelogenin in vivo . 40 …”

Section: Amelogenin and Its Targetsmentioning

confidence: 99%

“…(A) Amelogenin monomer in acidic solution; Reproduced with permission from ref 27. (B) In 70% TFE; Reproduced with permission from ref 40. (C) In 10% SDS; Reproduced with permission from ref 41.…”

Section: Figurementioning

confidence: 99%

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Amelogenin and enamel biomimetics

2015

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Mature tooth enamel is acellular and does not regenerate itself. Developing technologies that rebuild tooth enamel and preserve tooth structure is therefore of great interest. Considering the importance of amelogenin protein in dental enamel formation, its ability to control apatite mineralization in vitro, and its potential to be applied in fabrication of future bio-inspired dental material this review focuses on two major subjects: amelogenin and enamel biomimetics. We review the most recent findings on amelogenin secondary and tertiary structural properties with a focus on its interactions with different targets including other enamel proteins, apatite mineral, and phospholipids. Following a brief overview of enamel hierarchical structure and its mechanical properties we will present the state-of-the-art strategies in the biomimetic reconstruction of human enamel.

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Section: Amelogenin and Its Targetssupporting

confidence: 61%

“…40 The rigidity in the central region and flexibility at the N- and C- termini may have important functional significance for amelogenin in vivo . 40 …”

Section: Amelogenin and Its Targetsmentioning

confidence: 99%

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Amelogenin and enamel biomimetics

2015

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“…Mammals DMP1 4.0 CD, DLS, FTIR, SAXS (Gericke et al, 2010;He et al, 2003aHe et al, , 2003b DPP 2.8 CD, NMR, SAXS (Cross et al, 2005;Evans et al, 1994;Fujisawa & Kuboki, 1998;George & Hao, 2005;He et al, 2005b;Lee et al, 1977) BSP 4.1 CD, NMR, SAXS (Fisher et al, 2001;Tye et al, 2003Tye et al, , 2005Wuttke et al, 2001) OPN 4.4 CD, NMR, FTIR (Fisher et al, 2001;Gorski et al, 1995) amelogenin 6.6 CD, NMR (Buchko et al, 2010;Delak et al, 2009b;Ndao et al, 2011;Shaw et al, 2008) statherin 8.0 CD, NMR (Long et al, 2001;Naganagowda et al, 1998;Raj et al, 1992) lithostathine 5.7 CD (Gerbaud et al, 2000) Haliotis rufescens AP7 5.2 CD, NMR (Kim et al, 2004(Kim et al, , 2006aMichenfelder et al, 2003;Wustman et al, 2004) Atrina rigita Asprich 2.7-3.5 CD, NMR (Collino et al, 2006;Delak et al, 2009aDelak et al, , 2008Kim et al, 2008;Ndao et al, 2010) Procambrus clarkii CAP-1 3.9 CD (Inoue et al, 2007) Strongylocentrotus purpuratus SM50 10.8 CD, NMR (Xu & Evans, 1999;Zhang et al, 2000) PM27 8.1 CD, NMR Danio rerio Stm 4.1 CD, gel filtration (Kaplon et al, 2008(Kaplon et al, , 2009 Table 1. IDPs involved in biomineralization of calcium carbonate and phosphate for which a disordered structure has been confirmed...…”

Section: Protein Pi Methods Referencementioning

confidence: 99%

“…There is no well-defined, continuous region with an ordered structure, but some residual secondary structure was observed. In addition, amelogenin exists in at least two conformations (Buchko et al, 2010;Delak et al, 2009b;Ndao et al, 2011). Amelogenin can interact with other important proteins engaged in enamel formation (Bartlett et al, 2006).…”

Section: Enamel Proteinsmentioning

confidence: 99%

Intrinsically Disordered Proteins in Biomineralization

Wojtas¹,

Dobryszycki²,

Ożyhar³

2012

Advanced Topics in Biomineralization

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Structural adaptation of tooth enamel protein amelogenin in the presence of SDS micelles

et al. 2014

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Amelogenin, the major extracellular matrix protein of developing tooth enamel is intrinsically disordered. Through its interaction with other proteins and mineral, amelogenin assists enamel biomineralization by controlling the formation of highly organized enamel crystal arrays. We used circular dichroism (CD), dynamic light scattering (DLS), fluorescence and NMR spectroscopy to investigate the folding propensity of recombinant porcine amelogenin rP172 following its interaction with SDS, at levels above critical micelle concentration. The rP172-SDS complex formation was confirmed by DLS, while an increase in the structure moiety of rP172 was noted through CD and fluorescence experiments. Fluorescence quenching analyses performed on several rP172 mutants where all but one Trp was replaced by Tyr at different sequence regions confirmed that the interaction of amelogenin with SDS micelles occurs via the N-terminal region close to Trp25 where helical segments can be detected by NMR. NMR spectroscopy and structural refinement calculations using CS-Rosetta modelling confirm that the highly conserved N-terminal domain is prone to form helical structure when bound to SDS micelles. Our findings reported here reveal interactions leading to significant changes in the secondary structure of rP172 upon treatment with SDS. These interactions may reflect the physiological relevance of the flexible nature of amelogenin and its sequence specific helical propensity that might enable it to structurally adapt with charged and potential targets such as cell surface, mineral, and other proteins during enamel biomineralization.

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Probing the self‐association, intermolecular contacts, and folding propensity of amelogenin

Cited by 28 publications

References 48 publications

Amelogenin and enamel biomimetics

Amelogenin and enamel biomimetics

Intrinsically Disordered Proteins in Biomineralization

Structural adaptation of tooth enamel protein amelogenin in the presence of SDS micelles

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