Defining the Phenotype and Assessing Severity in Phosphoglucomutase-1 Deficiency

Sunnie Yan Wai Wong; Therese Gadomski; Tamas Kozicz; Eva Morava; Lesa J. Beamer; Tomas Honzik; Miski Mohamed; Eva Morava; Saskia B. Wortmann; Katja S. Brocke Holmefjord; Marit Mork; Francis Bowling; Jolanta Sykut-Cegielska; Dieter Koch; Amanda Ackermann; Charles A. Stanley; Daisy Rymen; Avraham Zeharia; Moeen Al-Sayed; Thomas Marquardt; Jaak Jaeken; Dirk Lefeber; Donald F. Conrad

doi:10.1016/j.jpeds.2016.04.021

Defining the Phenotype and Assessing Severity in Phosphoglucomutase-1 Deficiency

Sunnie Yan Wai Wong^*, Therese Gadomski, Tamas Kozicz, Eva Morava, Lesa J. Beamer, Tomas Honzik, Miski Mohamed, Eva Morava, Saskia B. Wortmann, Katja S. Brocke Holmefjord, Marit Mork, Francis Bowling, Jolanta Sykut-Cegielska, Dieter Koch, Amanda Ackermann, Charles A. Stanley, Daisy Rymen, Avraham Zeharia, Moeen Al-Sayed, Thomas MarquardtJaak Jaeken, Dirk Lefeber, Donald F. Conrad

^*Corresponding author for this work

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Abstract

Objective To define phenotypic groups and identify predictors of disease severity in patients with phosphoglucomutase-1 deficiency (PGM1-CDG). Study design We evaluated 27 patients with PGM1-CDG who were divided into 3 phenotypic groups, and group assignment was validated by a scoring system, the Tulane PGM1-CDG Rating Scale (TPCRS). This scale evaluates measurable clinical features of PGM1-CDG. We examined the relationship between genotype, enzyme activity, and TPCRS score by using regression analysis. Associations between the most common clinical features and disease severity were evaluated by principal component analysis. Results We found a statistically significant stratification of the TPCRS scores among the phenotypic groups (P <.001). Regression analysis showed that there is no significant correlation between genotype, enzyme activity, and TPCRS score. Principal component analysis identified 5 variables that contributed to 54% variance in the cohort and are predictive of disease severity: congenital malformation, cardiac involvement, endocrine deficiency, myopathy, and growth. Conclusions We established a scoring algorithm to reliably evaluate disease severity in patients with PGM1-CDG on the basis of their clinical history and presentation. We also identified 5 clinical features that are predictors of disease severity; 2 of these features can be evaluated by physical examination, without the need for specific diagnostic testing and thus allow for rapid assessment and initiation of therapy.

Original language	English
Pages (from-to)	130-136.e8
Journal	Journal of Pediatrics
Volume	175
DOIs	https://doi.org/10.1016/j.jpeds.2016.04.021
State	Published - 1 Aug 2016

Funding

Funders	Funder number
National Institutes of Health	1 U54 GM104940
National Institute of Mental Health	R01MH101810
National Institute of General Medical Sciences
Ministerstvo Zdravotnictví Ceské Republiky	MZ CR AZV 16-31932A
Všeobecná Fakultní Nemocnice v Praze	RVO-VFN 64165

Keywords

bifid uvula
cleft palate
coagulopathy
congenital disorder of glycosylation
congenital malformation
dilated cardiomyopathy
hepatopathy
hormonal deficiency
hypoglycemia
myopathy
small stature

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10.1016/j.jpeds.2016.04.021

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Wong, S. Y. W., Gadomski, T., Kozicz, T., Morava, E., Beamer, L. J., Honzik, T., Mohamed, M., Morava, E., Wortmann, S. B., Brocke Holmefjord, K. S., Mork, M., Bowling, F., Sykut-Cegielska, J., Koch, D., Ackermann, A., Stanley, C. A., Rymen, D., Zeharia, A., Al-Sayed, M., ... Conrad, D. F. (2016). Defining the Phenotype and Assessing Severity in Phosphoglucomutase-1 Deficiency. Journal of Pediatrics, 175, 130-136.e8. https://doi.org/10.1016/j.jpeds.2016.04.021

@article{35ce1a42b1724b36a6d2f4c988011442,

title = "Defining the Phenotype and Assessing Severity in Phosphoglucomutase-1 Deficiency",

abstract = "Objective To define phenotypic groups and identify predictors of disease severity in patients with phosphoglucomutase-1 deficiency (PGM1-CDG). Study design We evaluated 27 patients with PGM1-CDG who were divided into 3 phenotypic groups, and group assignment was validated by a scoring system, the Tulane PGM1-CDG Rating Scale (TPCRS). This scale evaluates measurable clinical features of PGM1-CDG. We examined the relationship between genotype, enzyme activity, and TPCRS score by using regression analysis. Associations between the most common clinical features and disease severity were evaluated by principal component analysis. Results We found a statistically significant stratification of the TPCRS scores among the phenotypic groups (P <.001). Regression analysis showed that there is no significant correlation between genotype, enzyme activity, and TPCRS score. Principal component analysis identified 5 variables that contributed to 54% variance in the cohort and are predictive of disease severity: congenital malformation, cardiac involvement, endocrine deficiency, myopathy, and growth. Conclusions We established a scoring algorithm to reliably evaluate disease severity in patients with PGM1-CDG on the basis of their clinical history and presentation. We also identified 5 clinical features that are predictors of disease severity; 2 of these features can be evaluated by physical examination, without the need for specific diagnostic testing and thus allow for rapid assessment and initiation of therapy.",

keywords = "bifid uvula, cleft palate, coagulopathy, congenital disorder of glycosylation, congenital malformation, dilated cardiomyopathy, hepatopathy, hormonal deficiency, hypoglycemia, myopathy, small stature",

author = "Wong, {Sunnie Yan Wai} and Therese Gadomski and Tamas Kozicz and Eva Morava and Beamer, {Lesa J.} and Tomas Honzik and Miski Mohamed and Eva Morava and Wortmann, {Saskia B.} and {Brocke Holmefjord}, {Katja S.} and Marit Mork and Francis Bowling and Jolanta Sykut-Cegielska and Dieter Koch and Amanda Ackermann and Stanley, {Charles A.} and Daisy Rymen and Avraham Zeharia and Moeen Al-Sayed and Thomas Marquardt and Jaak Jaeken and Dirk Lefeber and Conrad, {Donald F.}",

note = "Publisher Copyright: {\textcopyright} 2016 Elsevier Inc.",

year = "2016",

month = aug,

day = "1",

doi = "10.1016/j.jpeds.2016.04.021",

language = "אנגלית",

volume = "175",

pages = "130--136.e8",

journal = "Journal of Pediatrics",

issn = "0022-3476",

publisher = "Elsevier Inc.",

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Wong, SYW, Gadomski, T, Kozicz, T, Morava, E, Beamer, LJ, Honzik, T, Mohamed, M, Morava, E, Wortmann, SB, Brocke Holmefjord, KS, Mork, M, Bowling, F, Sykut-Cegielska, J, Koch, D, Ackermann, A, Stanley, CA, Rymen, D, Zeharia, A, Al-Sayed, M, Marquardt, T, Jaeken, J, Lefeber, D & Conrad, DF 2016, 'Defining the Phenotype and Assessing Severity in Phosphoglucomutase-1 Deficiency', Journal of Pediatrics, vol. 175, pp. 130-136.e8. https://doi.org/10.1016/j.jpeds.2016.04.021

TY - JOUR

T1 - Defining the Phenotype and Assessing Severity in Phosphoglucomutase-1 Deficiency

AU - Wong, Sunnie Yan Wai

AU - Gadomski, Therese

AU - Kozicz, Tamas

AU - Morava, Eva

AU - Beamer, Lesa J.

AU - Honzik, Tomas

AU - Mohamed, Miski

AU - Morava, Eva

AU - Wortmann, Saskia B.

AU - Brocke Holmefjord, Katja S.

AU - Mork, Marit

AU - Bowling, Francis

AU - Sykut-Cegielska, Jolanta

AU - Koch, Dieter

AU - Ackermann, Amanda

AU - Stanley, Charles A.

AU - Rymen, Daisy

AU - Zeharia, Avraham

AU - Al-Sayed, Moeen

AU - Marquardt, Thomas

AU - Jaeken, Jaak

AU - Lefeber, Dirk

AU - Conrad, Donald F.

PY - 2016/8/1

Y1 - 2016/8/1

N2 - Objective To define phenotypic groups and identify predictors of disease severity in patients with phosphoglucomutase-1 deficiency (PGM1-CDG). Study design We evaluated 27 patients with PGM1-CDG who were divided into 3 phenotypic groups, and group assignment was validated by a scoring system, the Tulane PGM1-CDG Rating Scale (TPCRS). This scale evaluates measurable clinical features of PGM1-CDG. We examined the relationship between genotype, enzyme activity, and TPCRS score by using regression analysis. Associations between the most common clinical features and disease severity were evaluated by principal component analysis. Results We found a statistically significant stratification of the TPCRS scores among the phenotypic groups (P <.001). Regression analysis showed that there is no significant correlation between genotype, enzyme activity, and TPCRS score. Principal component analysis identified 5 variables that contributed to 54% variance in the cohort and are predictive of disease severity: congenital malformation, cardiac involvement, endocrine deficiency, myopathy, and growth. Conclusions We established a scoring algorithm to reliably evaluate disease severity in patients with PGM1-CDG on the basis of their clinical history and presentation. We also identified 5 clinical features that are predictors of disease severity; 2 of these features can be evaluated by physical examination, without the need for specific diagnostic testing and thus allow for rapid assessment and initiation of therapy.

AB - Objective To define phenotypic groups and identify predictors of disease severity in patients with phosphoglucomutase-1 deficiency (PGM1-CDG). Study design We evaluated 27 patients with PGM1-CDG who were divided into 3 phenotypic groups, and group assignment was validated by a scoring system, the Tulane PGM1-CDG Rating Scale (TPCRS). This scale evaluates measurable clinical features of PGM1-CDG. We examined the relationship between genotype, enzyme activity, and TPCRS score by using regression analysis. Associations between the most common clinical features and disease severity were evaluated by principal component analysis. Results We found a statistically significant stratification of the TPCRS scores among the phenotypic groups (P <.001). Regression analysis showed that there is no significant correlation between genotype, enzyme activity, and TPCRS score. Principal component analysis identified 5 variables that contributed to 54% variance in the cohort and are predictive of disease severity: congenital malformation, cardiac involvement, endocrine deficiency, myopathy, and growth. Conclusions We established a scoring algorithm to reliably evaluate disease severity in patients with PGM1-CDG on the basis of their clinical history and presentation. We also identified 5 clinical features that are predictors of disease severity; 2 of these features can be evaluated by physical examination, without the need for specific diagnostic testing and thus allow for rapid assessment and initiation of therapy.

KW - bifid uvula

KW - cleft palate

KW - coagulopathy

KW - congenital disorder of glycosylation

KW - congenital malformation

KW - dilated cardiomyopathy

KW - hepatopathy

KW - hormonal deficiency

KW - hypoglycemia

KW - myopathy

KW - small stature

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U2 - 10.1016/j.jpeds.2016.04.021

DO - 10.1016/j.jpeds.2016.04.021

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C2 - 27206562

AN - SCOPUS:84971283620

SN - 0022-3476

VL - 175

SP - 130-136.e8

JO - Journal of Pediatrics

JF - Journal of Pediatrics

ER -

Defining the Phenotype and Assessing Severity in Phosphoglucomutase-1 Deficiency

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