Conformational Flexibility Tunes the Propensity of Transthyretin to Form Fibrils Through Non‐Native Intermediate States

Das, Jitendra K.; Mall, Shyam S.; Bej, Aritra; Mukherjee, Sujoy

doi:10.1002/anie.201407323

Cited by 26 publications

(36 citation statements)

References 27 publications

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“…However, a notable difference was observed in strand D. The short strand with little flexibility in WT TTR undergoes substantial conformational fluctuations in the pathogenic mutants. 60 These NMR results are largely consistent with our biophysical studies that showed the amyloidogenic states of the TTR variants are less stable than that of WT TTR. In addition, our solid-state NMR results reveal that amyloid states of WT and two mutant forms of TTR adopt a similar native-like CBEF and AGH β-sheet structure, but different DA substructures were observed in the mutant amyloids.…”

Section: Discussionsupporting

confidence: 90%

“…In addition, previous relaxation dispersion NMR experiments of the monomeric and tetrameric TTR showed that CBEF β-sheet remains stable while the other β-sheet (DAGH) undergoing extensive conformational fluctuations on millisecond time scales associated with misfolding and amyloid formation. 60,63 These NMR results suggest that DAGH β-sheet may be involved in intermolecular associations. Indeed, recent mechanistic studies of TTR aggregation showed that intermolecular interactions between strands H play a key role in TTR amyloid formation, and strand A has a strong aggregation propensity.…”

Section: Discussionmentioning

confidence: 76%

“…Recent relaxation NMR experiments identified flexible regions undergoing conformational fluctuations that might be linked to the dissociation of the TTR tetramer to aggregation-prone monomers. 60 The pathogenic mutations (V30M and L55P) were shown to induce more extensive conformational fluctuations of the same flexible regions as those observed for WT TTR. However, a notable difference was observed in strand D. The short strand with little flexibility in WT TTR undergoes substantial conformational fluctuations in the pathogenic mutants.…”

Section: Discussionmentioning

confidence: 78%

“…The longer side chain of methionine than that of valine may crash with other side chains in strands D and A, inducing a structural change in the DA substructure, as was suggested by the previous relaxation dispersion NMR experiments. 60 In the stronger amyloidogenic mutant L55P, the distance between residues P55 and M13 is higher (6.5 Å) even in the native state, in comparison to the native WT tetrameric TTR (5 Å), as shown in Supplementary Figure S5. The strand D is also more disordered in the more amyloidogenic mutant L55P TTR, which is consistent with our mass spectra-based analysis that showed the amyloidogenic state of the mutant is less stable than that of WT TTR.…”

Section: Discussionmentioning

confidence: 92%

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Pathogenic Mutations Induce Partial Structural Changes in the Native β-Sheet Structure of Transthyretin and Accelerate Aggregation

Lim

Dasari

et al. 2017

Biochemistry

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Amyloid formation of natively folded proteins involves global and/or local unfolding of the native state to form aggregation-prone intermediates. Here we report solid-state NMR structural studies of amyloid derived from wild-type (WT) and more aggressive mutant forms of transthyretin (TTR) to investigate the structural changes associated with effective TTR aggregation. We employed selective 13C-labeling schemes to investigate structural features of β-structured core regions in amyloid states of WT and two mutant forms (V30M and L55P) of TTR. Analyses of the 13C-13C correlation solid-state NMR spectra revealed that WT TTR aggregates contain an amyloid core consisting of native-like CBEF and DAGH β-sheet structures and the mutant TTR amyloids adopt a similar amyloid core structure with native-like CBEF and AGH β-structures. However, the V30M mutant amyloid was shown to have a different DA β-structure. In addition, strand D is more disordered even in the native state of L55P TTR, indicating that the pathogenic mutations affect the DA β-structure, leading to more effective amyloid formation. The NMR results are consistent with our mass spectrometry-based thermodynamic analyses that showed the amyloidogenic precursor states of WT and mutant TTRs adopt folded structures, but the mutant precursor states are less stable than that of WT TTR. Analyses of the oxidation rate of methionine sidechain also revealed that the sidechain of residue Met-30 pointing between strands D and A is not protected from the oxidation in V30M mutant, while protected in the native state, supporting that the DA β-structure might be disrupted in V30M mutant amyloid.

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Section: Discussionsupporting

confidence: 90%

Section: Discussionmentioning

confidence: 76%

Section: Discussionmentioning

confidence: 78%

Section: Discussionmentioning

confidence: 92%

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Pathogenic Mutations Induce Partial Structural Changes in the Native β-Sheet Structure of Transthyretin and Accelerate Aggregation

Lim

Dasari

et al. 2017

Biochemistry

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“…Relaxationsmessungen des Proteinrückgrats zeigten, dass im Vergleich zu M‐TTR eine geringere Zahl an T119M‐M‐TTR‐Resten 15 N‐Relaxationsdispersion aufweist . Zudem verringert der Einbau der T119M‐Mutation in das Wildtyp‐TTR die Konformationsdynamik innerhalb des tetrameren Zustands . Um darüber hinaus gehende Einblicke in Unterschiede der internen Dynamik zwischen dem monomeren T119M‐M‐TTR und Wildtyp‐TTR zu gewinnen, schätzen wir auf Basis der experimentellen chemischen Verschiebungen und unter Zuhilfenahme des Programms TALOS‐N die Ordnungsparameter des Proteinrückgrats ab.…”

Section: Figureunclassified

Struktur eines monomeren Transthyretin mit der klinisch wichtigen T119M‐Mutation

2016

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Mutationen im Protein Transthyretin kçnnen Transthyretin-Amyloidose hervorrufen sowie Individuen davor schützen.W enig ist jedoch über die strukturelle Basis pathogener und klinisch schützender Transthyretin-Mutanten bekannt. Hier berichten wir über die Lçsungsstruktur eines Transthyretin-Monomers,d as die klinischw ichtigeT 119M-Mutation trägt. Die Struktur offenbart eine nichtnative Anordnung, die sich von allen bekannten Transthyretin-Strukturen unterscheidet, und unterstreicht die Bedeutung von Lçsungsstudien mit hoher Auflçsung, um molekulare Prozesse zu verstehen, die zu Amyloid-Erkrankungen führen.

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Structure of Monomeric Transthyretin Carrying the Clinically Important T119M Mutation

2016

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Mutations in the protein transthyretin can cause as well as protect individuals from transthyretin amyloidosis, an incurable fatal inherited disease. Little is known, however, about the structural basis of pathogenic and clinically protective transthyretin mutants. Here we determined the solution structure of a transthyretin monomer that carries the clinically important T119M mutation. The structure displays a non-native arrangement that is distinct from all known structures of transthyretin and highlights the importance of high-resolution studies in solution for understanding molecular processes that lead to amyloid diseases.

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Conformational Flexibility Tunes the Propensity of Transthyretin to Form Fibrils Through Non‐Native Intermediate States

Cited by 26 publications

References 27 publications

Pathogenic Mutations Induce Partial Structural Changes in the Native β-Sheet Structure of Transthyretin and Accelerate Aggregation

Pathogenic Mutations Induce Partial Structural Changes in the Native β-Sheet Structure of Transthyretin and Accelerate Aggregation

Struktur eines monomeren Transthyretin mit der klinisch wichtigen T119M‐Mutation

Structure of Monomeric Transthyretin Carrying the Clinically Important T119M Mutation

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