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Review
. 2019 Jan 21;14(1):20.
doi: 10.1186/s13023-018-0985-1.

Recommendations for patient screening in ultra-rare inherited metabolic diseases: what have we learned from Niemann-Pick disease type C?

María-Jesús Sobrido  1 Peter Bauer  2   3 Tom de Koning  4 Thomas Klopstock  5 Yann Nadjar  6 Marc C Patterson  7 Matthis Synofzik  8   9 Chris J Hendriksz  10
Affiliations
Review

Recommendations for patient screening in ultra-rare inherited metabolic diseases: what have we learned from Niemann-Pick disease type C?

María-Jesús Sobrido et al. Orphanet J Rare Dis. .

Abstract

Background: Rare and ultra-rare diseases (URDs) are often chronic and life-threatening conditions that have a profound impact on sufferers and their families, but many are notoriously difficult to detect. Niemann-Pick disease type C (NP-C) serves to illustrate the challenges, benefits and pitfalls associated with screening for ultra-rare inborn errors of metabolism (IEMs). A comprehensive, non-systematic review of published information from NP-C screening studies was conducted, focusing on diagnostic methods and study designs that have been employed to date. As a key part of this analysis, data from both successful studies (where cases were positively identified) and unsuccessful studies (where the chosen approach failed to identify any cases) were included alongside information from our own experiences gained from the planning and execution of screening for NP-C. On this basis, best-practice recommendations for ultra-rare IEM screening are provided. Twenty-six published screening studies were identified and categorised according to study design into four groups: 1) prospective patient cohort and family-based secondary screenings (18 studies); 2) analyses of archived 'biobank' materials (one study); 3) medical chart review and bioinformatics data mining (five studies); and 4) newborn screening (two studies). NPC1/NPC2 sequencing was the most common primary screening method (Sanger sequencing in eight studies and next-generation sequencing [gene panel or exome sequencing] in five studies), followed by biomarker analyses (usually oxysterols) and clinical surveillance.

Conclusions: Historically, screening for NP-C has been based on single-patient studies, small case series, and targeted cohorts, but the emergence of new diagnostic methods over the last 5-10 years has provided opportunities to screen for NP-C on a larger scale. Combining clinical, biomarker and genetic diagnostic methods represents the most effective way to identify NP-C cases, while reducing the likelihood of misdiagnosis. Our recommendations are intended as a guide for planning screening protocols for ultra-rare IEMs in general.

Keywords: Diagnosis; Niemann-Pick disease; Screening; Ultra-rare disease.

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Conflict of interest statement

Ethics approval and consent to participate

Not applicable.

Consent for publication

Not applicable.

Competing interests

PB has received travel expenses, research funding, and speaker honoraria from Actelion Pharmaceuticals Ltd. TdK has received research funding from Actelion Pharmaceuticals Ltd. TK has received research funding, travel expenses, presentation honoraria and consulting fees from Actelion Pharmaceuticals Ltd. YN has received speech honoraria from Actelion Pharmaceuticals Ltd. and Orphan Europe, as well as travel funding from Actelion Pharmaceuticals Ltd., Shire, and Genzyme. MCP has received research grants from the Peggy Furth Fund, the National Institutes of Health [NS 65768–01], the National MS Society, Orphazyme and Actelion Pharmaceuticals Ltd., and honoraria and consulting fees from Actelion Pharmaceuticals Ltd., Alexion, Amicus, Novartis, Orphazyme, Shire HGT, Stem Cells Inc., Vtesse; stock in IntraBio; stipend and royalties from Sage Publications (Journal of Child Neurology and Child Neurology Open) and royalties from Wolters-Kluwer (Up-To-Date). MJS has received a research grant, travel expenses and speaker honoraria from Actelion Pharmaceuticals Ltd., and is a co-founder and shareholder of Genomic Consulting. MS has received travel expenses, presentation honoraria and consulting fees from Actelion Pharmaceuticals Ltd. CJH, Director of FYMCA Medical Ltd., has received consultancy fees and travel expenses from Alexion, Amicus, Biomarin, Chiesi, Inventiva, Sanofi Genzyme, and Shire, and conducted paid research on behalf of Amicus, Biomarin, Sanofi Genzyme, and Shire.

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