Identification of novel bile acids as biomarkers for the early diagnosis of Niemann-Pick C disease.

Francesca Mazzacuva,Nariyasu Mano,Peter T Clayton,Masamitsu Maekawa,Kevin Mills,Paul Gissen,Frances Platt,Forbes D Porter,Danielle Te Vruchte,Philippa Mills,Takashi Iida,Stephane Camuzeaux,Elena‐Raluca Nicoli,Christopher Wassif

doi:10.1002/1873-3468.12196

Identification of novel bile acids as biomarkers for the early diagnosis of Niemann-Pick C disease.

Francesca Mazzacuva, Nariyasu Mano + Show 12 more

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https://doi.org/10.1002/1873-3468.12196

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Journal: FEBS Letters	Publication Date: May 27, 2016
Citations: 87	License type: CC BY-NC-ND 4.0

Affiliation: University College London, Tohoku University Hospital, Great Ormond Street Hospital, University of Oxford, Eunice Kennedy Shriver National Institute of Child Health and Human Development, National Institutes of Health, Nihon University

#Niemann‐Pick C #Bile Acids In Biological Fluids + Show 8 more

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Abstract

This article describes a rapid UPLC‐MS/MS method to quantitate novel bile acids in biological fluids and the evaluation of their diagnostic potential in Niemann‐Pick C (NPC). Two new compounds, NPCBA1 (3β‐hydroxy,7β‐N‐acetylglucosaminyl‐5‐cholenoic acid) and NPCBA2 (probably 3β,5α,6β‐trihydroxycholanoyl‐glycine), were observed to accumulate preferentially in NPC patients: median plasma concentrations of NPCBA1 and NPCBA2 were 40‐ and 10‐fold higher in patients than in controls. However, NPCBA1 concentrations were normal in some patients because they carried a common mutation inactivating the GlcNAc transferase required for the synthesis of this bile acid. NPCBA2, not containing a GlcNAc moiety, is thus a better NPC biomarker.

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