PhosphoThr Peptide Binding Globally Rigidifies Much of the FHA Domain from Arabidopsis Receptor Kinase-Associated Protein Phosphatase<sup>,</sup>

Ding, Zhaofeng; Lee, § Gui-in; Liang, Xiaogan; Gallazzi, Fabio; Arunima, A.; Doren, Steven R. Van

doi:10.1021/bi050414a

Cited by 22 publications

(39 citation statements)

References 82 publications

(193 reference statements)

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“…The average rigidity of the backbone on the fast timescale is increased with pThr peptide bound 26. In fact, sites of binding-enhanced rigidity are observed with the β-sandwich in all four of the β-hairpins (those with blue coloration in Figure 5) 26. The nanosecond fluctuations enriched in its loops are quenched once the phosphopeptide is bound.…”

Section: Dynamics and Energetics Of Pthr Peptide Bindingmentioning

confidence: 98%

“…This swaps strands 9–11 into a β-sandwich with strands 1–7 from the other chain. In KI-FHA, β-strand 8 lacks measurable structural stability 32 and is mobile on the millisec scale 26. If low stability and mobility of β-strand 8 generalize to other FHA domains, it could account for β-strand 8 being malleable enough to straighten out in crystals of segment-swapped CHFr.…”

Section: Other Proposed Protein-binding Sitesmentioning

confidence: 99%

“…The nanosecond fluctuations enriched in its loops are quenched once the phosphopeptide is bound. Perhaps the binding-increased rigidity of KI-FHA reflects the favorable enthalpy of association 18 that might result from improved internal packing and hydrogen bonding 26.…”

Section: Dynamics and Energetics Of Pthr Peptide Bindingmentioning

confidence: 99%

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Mechanistic Insights into Phosphoprotein-Binding FHA Domains

Liang

Doren

2008

Acc. Chem. Res.

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CONSPECTUS FHA domains are protein modules that switch signals in diverse biological pathways by monitoring the phosphorylation of threonine residues of target proteins. As part of the effort to gain insight into cellular avoidance of cancer, FHA domains involved in the cellular response to DNA damage have been especially well characterized. The complete protein where the FHA domain resides and the interaction partners determine the nature of the signaling. Thus, a key biochemical question is: how do FHA domains pick out their partners from among thousands of alternatives in the cell? This Account discusses the structure, affinity, and specificity of FHA domains and the formation of their functional structure. Although FHA domains share sequence identity at only five loop residues, they all fold into a β-sandwich of two β-sheets. The conserved Arg and Ser of the recognition loops recognize the phosphorylation of the Thr targeted. Side chains emanating from loops that join β-strand 4 with 5, 6 with 7, or 10 with 11 make specific contacts with amino acids of the ligand that tailor sequence preferences. Many FHA domains choose a partner in extended conformation, somewhat according to the residue three after the phosphoThr in sequence (pT+3 position). One group of FHA domains chooses a short carboxylate-containing side chain at pT+3. Another group chooses a long, branched aliphatic side chain. A third group prefers other hydrophobic or uncharged, polar side chains at pT+3. However, another FHA domain instead chooses on the basis of pT−2, pT−3, and pT+1 positions. An FHA domain from a marker of human cancer instead chooses a much longer protein fragment that adds a β-strand to its β-sheet and that presents hydrophobic residues from a novel helix to the usual recognition surface. This novel recognition site and more remote sites for the binding of other types of protein partners were predicted for the entire family of FHA domains by a bioinformatics approach. The phosphopeptide-dependent dynamics of an FHA domain, SH2 domain, and PTB domain suggest a common theme: rigid, preformed binding surfaces support van der Waals contacts that provide favorable binding enthalpy. Despite the lack of pronounced conformational changes in FHA domains linked to binding events, more subtle adjustments may be possible. In the one FHA domain tested, phosphoThr peptide binding is accompanied by increased flexibility just outside the binding site and increased rigidity across the β-sandwich. The folding of the same FHA domain progresses through near-native intermediates that stabilize the recognition loops in the center of the phosphoprotein-binding surface; this may promote rigidity in the interface and affinity for targets phosphorylated on threonine.

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Section: Dynamics and Energetics Of Pthr Peptide Bindingmentioning

confidence: 98%

Section: Other Proposed Protein-binding Sitesmentioning

confidence: 99%

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Mechanistic Insights into Phosphoprotein-Binding FHA Domains

Liang

Doren

2008

Acc. Chem. Res.

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“…In the structure, β2 can instead be grouped with β3 to form a green foldon since their side chains pack together in the interior. β2's lower sensitivity to denaturant than that of β1 seems to correlate with (i) the greater surface accessibility of 24% for β2 than the 11% of β1 and (ii) slightly greater flexibility in β2 (S 2 = 0.846 for His196) than in β1 (S 2 of 0.914) (Ding et al, 2005). The NHX results on OspA show that some of the strands on the edges of its β-sheets (β-strands 1, 4 and 21 for example) also have lower m-values and stability than their neighbors to the interior of the sheet 21 .…”

Section: Implications Of Decreased Nhx Stability Towards Edges Of β-Smentioning

confidence: 94%

Partially Unfolded Forms and Non-two-state Folding of a β-Sandwich: FHA Domain from Arabidopsis Receptor Kinase-associated Protein Phosphatase

Liang

Lee

Doren

2006

Journal of Molecular Biology

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FHA domains adopt a β-sandwich fold with 11 strands. The first evidence of partially unfolded forms of a β-sandwich is derived from native-state hydrogen exchange (NHX) of the FHA domain from Kinase-Associated Protein Phosphatase from Arabidopsis. The folding kinetics of this FHA domain indicate that EX2 behavior prevails at pH 6.3. In the chevron plot, rollover in the folding arm and bends in the unfolding arm suggest folding intermediates. NHX of this FHA domain suggests a core of six most stable β-strands and two loops, characterized by rare global unfolding events. Flanking this stable core are β-strands and recognition loops with less stability, termed subglobal motifs. These suggest partially unfolded forms (near-native intermediates) with two levels of stability. The spatial separation of the subglobal motifs on the flanks suggests possible parallelism in their folding as additional β-strands align with the stable core of six strands. Intermediates may contribute to differences in stabilities and m-values suggested by NHX or kinetics relative to chemical denaturation. Residual structure in the unfolded regime is suggested by superprotection of β-strand 6 and by GdmCl-dependence of adjustments in amide NMR spectra and residual optical signal. The global folding stability depends strongly on pH, with at least 3 kcal/mol more stability at pH 7.3 than at pH 6.3. This FHA domain is hypothesized to fold progressively with initial hydrophobic collapse of its stable 6-stranded core followed by addition of less stable flanking β-strands and ordering of recognition loops.

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“…23 Similarly, loop regions in the FHA domain of Ki67 have been shown to adopt a fixed structure in the presence of a binding partner. 15 NMR chemical shift changes have indicated a similar situation in NIPP1, where several loops are restructured upon phosphopeptide binding.…”

Section: The Pml1p Fha Domain Is Expanded By Noncanonical Elementsmentioning

confidence: 99%

Crystal Structure of the Pml1p Subunit of the Yeast Precursor mRNA Retention and Splicing Complex

Trowitzsch

Weber

Lührmann

et al. 2009

Journal of Molecular Biology

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The precursor mRNA retention and splicing (RES) complex mediates nuclear retention and enhances splicing of precursor mRNAs. The RES complex from yeast comprises three proteins, Snu17p, Bud13p and Pml1p. Snu17p acts as a central platform that concomitantly binds the Bud13p and Pml1p subunits via short peptide epitopes. As a step to decipher the molecular architecture of the RES complex, we have determined crystal structures of full-length Pml1p and N-terminally truncated Pml1p. The first 50 residues of full-length Pml1p, encompassing the Snu17p-binding region, are disordered, showing that Pml1p binds to Snu17p via an intrinsically unstructured region. The remainder of Pml1p folds as a forkhead-associated (FHA) domain, which is expanded by a number of noncanonical elements compared with known FHA domains from other proteins. An atypical N-terminal appendix runs across one beta-sheet and thereby stabilizes the domain as shown by deletion experiments. FHA domains are thought to constitute phosphopeptide-binding elements. Consistently, a sulfate ion was found at the putative phosphopeptide-binding loops of full-length Pml1p. The N-terminally truncated version of the protein lacked a similar phosphopeptide mimic but retained an almost identical structure. A long loop neighboring the putative phosphopeptide-binding site was disordered in both structures. Comparison with other FHA domain proteins suggests that this loop adopts a defined conformation upon ligand binding and thereby confers ligand specificity. Our results show that in the RES complex, an FHA domain of Pml1p is flexibly tethered via an unstructured N-terminal region to Snu17p.

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PhosphoThr Peptide Binding Globally Rigidifies Much of the FHA Domain from Arabidopsis Receptor Kinase-Associated Protein Phosphatase^,

Cited by 22 publications

References 82 publications

Mechanistic Insights into Phosphoprotein-Binding FHA Domains

Mechanistic Insights into Phosphoprotein-Binding FHA Domains

Partially Unfolded Forms and Non-two-state Folding of a β-Sandwich: FHA Domain from Arabidopsis Receptor Kinase-associated Protein Phosphatase

Crystal Structure of the Pml1p Subunit of the Yeast Precursor mRNA Retention and Splicing Complex

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PhosphoThr Peptide Binding Globally Rigidifies Much of the FHA Domain from Arabidopsis Receptor Kinase-Associated Protein Phosphatase,

Cited by 22 publications

References 82 publications

Mechanistic Insights into Phosphoprotein-Binding FHA Domains

Mechanistic Insights into Phosphoprotein-Binding FHA Domains

Partially Unfolded Forms and Non-two-state Folding of a β-Sandwich: FHA Domain from Arabidopsis Receptor Kinase-associated Protein Phosphatase

Crystal Structure of the Pml1p Subunit of the Yeast Precursor mRNA Retention and Splicing Complex

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PhosphoThr Peptide Binding Globally Rigidifies Much of the FHA Domain from Arabidopsis Receptor Kinase-Associated Protein Phosphatase^,