Amyloidogenicity and Clinical Phenotype Associated with Five Novel Mutations in Apolipoprotein A-I
Dorota Rowczenio,Ahmet Dogan,Jason D. Theis,Julie A. Vrana,Helen J. Lachmann,Ashutosh D. Wechalekar,Janet A. Gilbertson,Toby Hunt,Simon D. J. Gibbs,Prayman T. Sattianayagam,JH Pinney,Philip N. Hawkins,Julian D. Gillmore +12 more
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TLDR
The clinical spectrum and outcome are reviewed in detail and support the need for sequencing of the apolipoprotein A-I gene among patients with apparent localized amyloidosis in whom IHC is nondiagnostic of the fibril protein, even in the absence of a family history of disease.Abstract:
The phenotype of hereditary apolipoprotein A-I amyloidosis is heterogeneous with some patients developing extensive visceral amyloid deposits and end-stage renal failure as young adults and others having only laryngeal and/or skin amyloid, which may be of little clinical consequence. Clinical management and prognosis of patients with systemic amyloidosis depend entirely on correct identification of the fibril protein, such that light chain amyloidosis (AL, previously referred to as "primary"), the most frequently diagnosed type, is treated with chemotherapy, which has absolutely no role in hereditary apolipoprotein A-I amyloidosis. We report five novel apolipoprotein A-I variants, four of which were amyloidogenic and one of which was incidental in a patient with systemic AL amyloidosis. Interestingly, only one of four patients with apolipoprotein A-I amyloidosis had a family history of similar disease. Laser microdissection and tandem mass spectrometry-based proteomics were used to confirm the amyloid fibril protein and, for the first time in apolipoprotein A-I amyloidosis, demonstrated that only mutated protein as opposed to wild-type apolipoprotein A-I was deposited as amyloid. The clinical spectrum and outcome of hereditary apolipoprotein A-I amyloidosis are reviewed in detail and support the need for sequencing of the apolipoprotein A-I gene among patients with apparent localized amyloidosis in whom IHC is nondiagnostic of the fibril protein, even in the absence of a family history of disease.read more
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Online registry for mutations in hereditary amyloidosis including nomenclature recommendations.
Dorota Rowczenio,Islam Noor,Julian D. Gillmore,Helen J. Lachmann,Carol J. Whelan,Philip N. Hawkins,Laura Obici,Per Westermark,Gilles Grateau,Ashutosh D. Wechalekar +9 more
TL;DR: An online registry of genes and mutations in hereditary amyloidosis including their associated clinical phenotypes is designed with support from the EU FP6 EURAMY project with a view to having a single free online portal for the collection and distribution of this information.
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Protein aggregation: mechanisms and functional consequences.
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Update on the molecular biology of dyslipidemias.
TL;DR: In most patients, dyslipidemias have a complex genetic etiology consisting of multiple genetic variants as established by genome wide association studies, and there is room for further characterization of genes influencing lipid levels.
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Systemic amyloidosis from A (AA) to T (ATTR): a review.
Eli Muchtar,Angela Dispenzieri,Hila Magen,Martha Grogan,Michelle L. Mauermann,Ellen D. McPhail,Paul J. Kurtin,Nelson Leung,Francis K. Buadi,D. Dingli,Shaji Kumar,Morie A. Gertz +11 more
TL;DR: Each type of systemic amyloidosis is reviewed to provide the practitioner with practical tools to improve diagnosis and management of these rare disorders.
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Protein aggregation and fibrillogenesis in cerebral and systemic amyloid disease
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