Evidence-based Path to Newborn Screening for Duchenne Muscular Dystrophy

Overview

Journal Ann Neurol

Specialty Neurology

Date 2012 Mar 28

PMID 22451200

Citations 410

Authors

Jerry R Mendell

Chris Shilling

Nancy D Leslie

Kevin M Flanigan

Roula Al-Dahhak

Julie Gastier-Foster

Kelley Kneile

Diane M Dunn

Brett Duval

Alexander Aoyagi

Cindy Hamil

Maha Mahmoud

Kandice Roush

Lauren Bird

Chelsea Rankin

Heather Lilly

Natalie Street

Ram Chandrasekar

Robert B Weiss

Affiliations

Soon will be listed here.

Abstract

Objective: Creatine kinase (CK) levels are increased on dried blood spots in newborns related to the birthing process. As a marker for newborn screening, CK in Duchenne muscular dystrophy (DMD) results in false-positive testing. In this report, we introduce a 2-tier system using the dried blood spot to first assess CK with follow-up DMD gene testing.

Methods: A fluorometric assay based upon the enzymatic transphosphorylation of adenosine diphosphate to adenosine triphosphate was used to measure CK activity. Preliminary studies established a population-based range of CK in newborns using 30,547 deidentified anonymous dried blood spot samples. Mutation analysis used genomic DNA extracted from the dried blood spot followed by whole genome amplification with assessment of single-/multiexon deletions/duplications in the DMD gene using multiplex ligation-dependent probe amplification.

Results: DMD gene mutations (all exonic deletions) were found in 6 of 37,649 newborn male subjects, all of whom had CK levels>2,000U/l. In 3 newborns with CK>2,000U/l in whom DMD gene abnormalities were not found, we identified limb-girdle muscular dystrophy gene mutations affecting DYSF, SGCB, and FKRP.

Interpretation: A 2-tier system of analysis for newborn screening for DMD has been established. This path for newborn screening fits our health care system, minimizes false-positive testing, and uses predetermined levels of CK on dried blood spots to predict DMD gene mutations.

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