Characterization of a Blood Spot Creatine Kinase Skeletal Muscle Isoform Immunoassay for High-Throughput Newborn Screening of Duchenne Muscular Dystrophy

Moat, Stuart; Korpimäki, Teemu; Furu, Petra; Hakala, Harri; Polari, Hanna; Meriö, Liisa; Mäkinen, Pauliina; Weeks, Ian

doi:10.1373/clinchem.2016.268425

Cited by 36 publications

(41 citation statements)

References 21 publications

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“…Currently, the recommended uniform screening panel encompasses 34 conditions. The HHS Secretary's Advisory Committee on Heritable Disorders in Newborns and Children is tasked with overseeing the process 5 of adding emerging conditions 6,7 to the recommended panel. The most recent additions are acid α-glucosidase (GAA) deficiency (Pompe disease), 8 α-L-iduronidase (IDUA) deficiency (MPS I), 9 and X-linked adrenoleukodystrophy.…”

Section: Introductionmentioning

confidence: 99%

Precision newborn screening for lysosomal disorders

Baerg

Stoway

Hart

et al. 2018

Genetics in Medicine

103

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Section: Introductionmentioning

confidence: 99%

Precision newborn screening for lysosomal disorders

Baerg

Stoway

Hart

et al. 2018

Genetics in Medicine

103

View full text Add to dashboard Cite

“…8,34,35 It is also possible to begin exploring whether the Cre/Crn ratio alone, the (Cre/Crn)/GAA ratio, or additional permutations of ratios could be relevant to the expansion of the biochemical phenotype of other conditions with prominent skeletal and cardiac myopathy and consequent elevation of creatinine phosphokinase, for example, very long chain fatty acid oxidation disorders 36 and particularly DMD and related disorders. 37 For proof of concept, preliminary testing of blood spotted on filter paper from residual clinical samples of genotyped DMD patients showed consistent elevations of the Cre/Crn ratio ( Figure 3; age 3-11 years, N = 10, range 6.42-8.99; age 25-39 years, N = 10, range 4.71-10.44; controls of age 21-60 years, N = 11, range 2.55-4.96; see Table 1 for neonatal reference percentiles). As a next step we are seeking neonatal/infantile blood spot specimens of DMD patients to evaluate whether one or more permutations of ratios integrating creatine and creatinine could be used as a second-tier test or even as an alternative primary test for newborn screening of DMD and related disorders.…”

Section: Discussionmentioning

confidence: 99%

Moonlighting newborn screening markers: the incidental discovery of a second-tier test for Pompe disease

Tortorelli

Eckerman

Orsini

et al. 2018

Genetics in Medicine

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“…For example, one classic widely used clinical blood ( plasma) biomarker for DMD is the enzyme creatine kinase (CK; Box 1), which is elevated in patients and in rodent and dog DMD models, but can be highly variable (reviewed by Dowling et al, 2019;Hathout et al, 2014;Szigyarto and Spitali, 2018). Nevertheless, increased CK levels, specifically the MM muscle form measured by immunoassay in dried bloodspots, are now being used for newborn DMD screening (Moat et al, 2017).…”

Section: Overview Of Molecular Biomarkers Especially For Myonecrosismentioning

confidence: 99%

Biomarkers for Duchenne muscular dystrophy: myonecrosis, inflammation and oxidative stress

et al. 2020

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Duchenne muscular dystrophy (DMD) is a lethal, X-linked disease that causes severe loss of muscle mass and function in young children. Promising therapies for DMD are being developed, but the long lead times required when using clinical outcome measures are hindering progress. This progress would be facilitated by robust molecular biomarkers in biofluids, such as blood and urine, which could be used to monitor disease progression and severity, as well as to determine optimal drug dosing before a full clinical trial. Many candidate DMD biomarkers have been identified, but there have been few follow-up studies to validate them. This Review describes the promising biomarkers for dystrophic muscle that have been identified in muscle, mainly using animal models. We strongly focus on myonecrosis and the associated inflammation and oxidative stress in DMD muscle, as the lack of dystrophin causes repeated bouts of myonecrosis, which are the key events that initiate the resultant severe dystropathology. We discuss the early events of intrinsic myonecrosis, along with early regeneration in the context of histological and other measures that are used to quantify its incidence. Molecular biomarkers linked to the closely associated events of inflammation and oxidative damage are discussed, with a focus on research related to protein thiol oxidation and to neutrophils. We summarise data linked to myonecrosis in muscle, blood and urine of dystrophic animal species, and discuss the challenge of translating such biomarkers to the clinic for DMD patients, especially to enhance the success of clinical trials.

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Characterization of a Blood Spot Creatine Kinase Skeletal Muscle Isoform Immunoassay for High-Throughput Newborn Screening of Duchenne Muscular Dystrophy

Abstract: CK-MM can be reliably quantified in blood spots. The development of this CK-MM assay on a commercial immunoassay analyzer would enable standardized and high-throughput newborn blood spot screening of DMD.

Cited by 36 publications

References 21 publications

Precision newborn screening for lysosomal disorders

Precision newborn screening for lysosomal disorders

Moonlighting newborn screening markers: the incidental discovery of a second-tier test for Pompe disease

Biomarkers for Duchenne muscular dystrophy: myonecrosis, inflammation and oxidative stress

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