Common Fibril Structures Imply Systemically Conserved Protein Misfolding Pathways In Vivo

Karthikeyan Annamalai; Falk Liberta; Marie Theres Vielberg; William Close; Hauke Lilie; Karl Heinz Gührs; Angelika Schierhorn; Rolf Koehler; Andreas Schmidt; Christian Haupt; Ute Hegenbart; Stefan Schönland; Matthias Schmidt; Michael Groll; Marcus Fändrich

doi:10.1002/anie.201701761

Common Fibril Structures Imply Systemically Conserved Protein Misfolding Pathways In Vivo

Karthikeyan Annamalai, Falk Liberta, Marie Theres Vielberg, William Close, Hauke Lilie, Karl Heinz Gührs, Angelika Schierhorn, Rolf Koehler, Andreas Schmidt, Christian Haupt, Ute Hegenbart, Stefan Schönland, Matthias Schmidt, Michael Groll, Marcus Fändrich

Lehrstuhl für Biochemie

Publikation: Beitrag in Fachzeitschrift › Artikel › Begutachtung

54 Zitate (Scopus)

Abstract

Systemic amyloidosis is caused by the misfolding of a circulating amyloid precursor protein and the deposition of amyloid fibrils in multiple organs. Chemical and biophysical analysis of amyloid fibrils from human AL and murine AA amyloidosis reveal the same fibril morphologies in different tissues or organs of one patient or diseased animal. The observed structural similarities concerned the fibril morphology, the fibril protein primary and secondary structures, the presence of post-translational modifications and, in case of the AL fibrils, the partially folded characteristics of the polypeptide chain within the fibril. Our data imply for both analyzed forms of amyloidosis that the pathways of protein misfolding are systemically conserved; that is, they follow the same rules irrespective of where inside one body fibrils are formed or accumulated.

Originalsprache	Englisch
Seiten (von - bis)	7510-7514
Seitenumfang	5
Fachzeitschrift	Angewandte Chemie International Edition in English
Jahrgang	56
Ausgabenummer	26
DOIs	https://doi.org/10.1002/anie.201701761
Publikationsstatus	Veröffentlicht - 19 Juni 2017

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10.1002/anie.201701761

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Annamalai, K., Liberta, F., Vielberg, M. T., Close, W., Lilie, H., Gührs, K. H., Schierhorn, A., Koehler, R., Schmidt, A., Haupt, C., Hegenbart, U., Schönland, S., Schmidt, M., Groll, M., & Fändrich, M. (2017). Common Fibril Structures Imply Systemically Conserved Protein Misfolding Pathways In Vivo. Angewandte Chemie International Edition in English, 56(26), 7510-7514. https://doi.org/10.1002/anie.201701761

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title = "Common Fibril Structures Imply Systemically Conserved Protein Misfolding Pathways In Vivo",

abstract = "Systemic amyloidosis is caused by the misfolding of a circulating amyloid precursor protein and the deposition of amyloid fibrils in multiple organs. Chemical and biophysical analysis of amyloid fibrils from human AL and murine AA amyloidosis reveal the same fibril morphologies in different tissues or organs of one patient or diseased animal. The observed structural similarities concerned the fibril morphology, the fibril protein primary and secondary structures, the presence of post-translational modifications and, in case of the AL fibrils, the partially folded characteristics of the polypeptide chain within the fibril. Our data imply for both analyzed forms of amyloidosis that the pathways of protein misfolding are systemically conserved; that is, they follow the same rules irrespective of where inside one body fibrils are formed or accumulated.",

keywords = "Alzheimer's disease, Parkinson's disease, conformational disease, prions, protein aggregation",

author = "Karthikeyan Annamalai and Falk Liberta and Vielberg, {Marie Theres} and William Close and Hauke Lilie and G{\"u}hrs, {Karl Heinz} and Angelika Schierhorn and Rolf Koehler and Andreas Schmidt and Christian Haupt and Ute Hegenbart and Stefan Sch{\"o}nland and Matthias Schmidt and Michael Groll and Marcus F{\"a}ndrich",

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year = "2017",

month = jun,

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doi = "10.1002/anie.201701761",

language = "English",

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Annamalai, K, Liberta, F, Vielberg, MT, Close, W, Lilie, H, Gührs, KH, Schierhorn, A, Koehler, R, Schmidt, A, Haupt, C, Hegenbart, U, Schönland, S, Schmidt, M, Groll, M & Fändrich, M 2017, 'Common Fibril Structures Imply Systemically Conserved Protein Misfolding Pathways In Vivo', Angewandte Chemie International Edition in English, Jg. 56, Nr. 26, S. 7510-7514. https://doi.org/10.1002/anie.201701761

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AU - Annamalai, Karthikeyan

AU - Liberta, Falk

AU - Vielberg, Marie Theres

AU - Close, William

AU - Lilie, Hauke

AU - Gührs, Karl Heinz

AU - Schierhorn, Angelika

AU - Koehler, Rolf

AU - Schmidt, Andreas

AU - Haupt, Christian

AU - Hegenbart, Ute

AU - Schönland, Stefan

AU - Schmidt, Matthias

AU - Groll, Michael

AU - Fändrich, Marcus

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N2 - Systemic amyloidosis is caused by the misfolding of a circulating amyloid precursor protein and the deposition of amyloid fibrils in multiple organs. Chemical and biophysical analysis of amyloid fibrils from human AL and murine AA amyloidosis reveal the same fibril morphologies in different tissues or organs of one patient or diseased animal. The observed structural similarities concerned the fibril morphology, the fibril protein primary and secondary structures, the presence of post-translational modifications and, in case of the AL fibrils, the partially folded characteristics of the polypeptide chain within the fibril. Our data imply for both analyzed forms of amyloidosis that the pathways of protein misfolding are systemically conserved; that is, they follow the same rules irrespective of where inside one body fibrils are formed or accumulated.

AB - Systemic amyloidosis is caused by the misfolding of a circulating amyloid precursor protein and the deposition of amyloid fibrils in multiple organs. Chemical and biophysical analysis of amyloid fibrils from human AL and murine AA amyloidosis reveal the same fibril morphologies in different tissues or organs of one patient or diseased animal. The observed structural similarities concerned the fibril morphology, the fibril protein primary and secondary structures, the presence of post-translational modifications and, in case of the AL fibrils, the partially folded characteristics of the polypeptide chain within the fibril. Our data imply for both analyzed forms of amyloidosis that the pathways of protein misfolding are systemically conserved; that is, they follow the same rules irrespective of where inside one body fibrils are formed or accumulated.

KW - Alzheimer's disease

KW - Parkinson's disease

KW - conformational disease

KW - prions

KW - protein aggregation

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Common Fibril Structures Imply Systemically Conserved Protein Misfolding Pathways In Vivo

Abstract

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