Diagnostic amyloid proteomics: experience of the UK National Amyloidosis Centre

Author:

Canetti Diana1,Rendell Nigel B.1,Gilbertson Janet A.1,Botcher Nicola1,Nocerino Paola1,Blanco Angel1,Di Vagno Lucia1,Rowczenio Dorota1,Verona Guglielmo1,Mangione P. Patrizia12,Bellotti Vittorio12,Hawkins Philip N.1,Gillmore Julian D.1,Taylor Graham W.1

Affiliation:

1. Wolfson Drug Discovery Unit and National Amyloidosis Centre, Centre for Amyloidosis and Acute Phase Proteins, Division of Medicine , University College London , London , UK

2. Department of Molecular Medicine, Institute of Biochemistry , University of Pavia , Pavia , Italy

Abstract

Abstract Systemic amyloidosis is a serious disease which is caused when normal circulating proteins misfold and aggregate extracellularly as insoluble fibrillary deposits throughout the body. This commonly results in cardiac, renal and neurological damage. The tissue target, progression and outcome of the disease depends on the type of protein forming the fibril deposit, and its correct identification is central to determining therapy. Proteomics is now used routinely in our centre to type amyloid; over the past 7 years we have examined over 2000 clinical samples. Proteomics results are linked directly to our patient database using a simple algorithm to automatically highlight the most likely amyloidogenic protein. Whilst the approach has proved very successful, we have encountered a number of challenges, including poor sample recovery, limited enzymatic digestion, the presence of multiple amyloidogenic proteins and the identification of pathogenic variants. Our proteomics procedures and approaches to resolving difficult issues are outlined.

Publisher

Walter de Gruyter GmbH

Subject

Biochemistry, medical,Clinical Biochemistry,General Medicine

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