Update of the pompe disease mutation database with 60 novel GAA sequence variants and additional studies on the functional effect of 34 previously reported variants

Marian Kroos; Marianne Hoogeveen-Westerveld; Helen Michelakakis; Robert Pomponio; Ans Van der Ploeg; Dicky Halley; Arnold Reuser; Persephone Augoustides-Savvopoulou; Margreet Ausems; Jose Barcena Llona; Juan Bautista Lorite; Nadine van der Beek; Luisa Bonafe; Mario Cuk; Marc D'Hooghe; Baziel Engelen; A. Farouk; K. Fumic; E. Garcia-Delgado; Andreas Herzog; J. Hurst; Simon Jones; M. H. Kariminejad; Aynur Küçükçongar; W. Lissens; Allan Lund; Danielle Majoor-Krakauer; Shingo Kumamoto; E. Maravi; Suely Marie; Eugen Mengel; Irene Mavridou; E. Munteis Olivas; H. Najmabadi; Toshika Okumiya; Stojan Peric; Eduard Paschke; Barbara Plecko; Wim Robberecht; Piraye Serdaroglu; Mohammad Shboul; Mojca Zerjav Tansek; A. Tarnutzer; Vidosava Rakocevic Stojanovic; Anna Tylki-Szymanska; Maria Venâncio; Kristof Verhoeven

doi:10.1002/humu.22108

Update of the pompe disease mutation database with 60 novel GAA sequence variants and additional studies on the functional effect of 34 previously reported variants

Marian Kroos
, Marianne Hoogeveen-Westerveld
, Helen Michelakakis
, Robert Pomponio
, Ans Van der Ploeg
, Dicky Halley
, Arnold Reuser
, Persephone Augoustides-Savvopoulou
, Margreet Ausems
, Jose Barcena Llona
, Juan Bautista Lorite
, Nadine van der Beek
, Luisa Bonafe
, Mario Cuk
, Marc D'Hooghe
, Baziel Engelen
, A. Farouk
, K. Fumic
, E. Garcia-Delgado
, Andreas Herzog

J. Hurst, Simon Jones, M. H. Kariminejad, Aynur Küçükçongar, W. Lissens, Allan Lund, Danielle Majoor-Krakauer, Shingo Kumamoto, E. Maravi, Suely Marie, Eugen Mengel, Irene Mavridou, E. Munteis Olivas, H. Najmabadi, Toshika Okumiya, Stojan Peric, Eduard Paschke, Barbara Plecko, Wim Robberecht, Piraye Serdaroglu, Mohammad Shboul, Mojca Zerjav Tansek, A. Tarnutzer, Vidosava Rakocevic Stojanovic, Anna Tylki-Szymanska, Maria Venâncio, Kristof Verhoeven

College of Engineering and Information Technology

Erasmus University Rotterdam
Institute of Child Health
Genzyme Corporation
Hippokratioj General Hospital
Utrecht University
Hospital de Cruces
University Hospital Sagrado Corazon
University of Lausanne
University of Zagreb
General Hospital St. Jan
Radboud University Nijmegen
Hrraa Hospital Mecca
Hospital de Mostoles
Johannes Gutenberg University Mainz
Oxford University Hospitals NHS Foundation Trust
St Mary's Hospital
Kariminejad-Najmabadi Pathology and Genetics Center
Gazi University
University Hospital
University of Copenhagen
Kumamoto University
Hospital Universitario de Navarra
Universidade de São Paulo
Hospital del Mar
University of Belgrade
University of Graz
KU Leuven
Istanbul University
University of Ljubljana
University of Zurich
Children's Memorial Health Institute
Children's Hospital Carmona da Mota

Research output: Contribution to journal › Article › peer-review

66 Scopus citations

Abstract

Pompe disease is an autosomal recessive lysosomal glycogen storage disorder, characterized by progressive muscle weakness. Deficiency of acid α-glucosidase (EC; 3.2.1.20/3) can be caused by numerous pathogenic variants in the GAA gene. The Pompe Disease Mutation Database at aims to list all variants and their effect. This update reports on 94 variants. We examined 35 novel and 34 known mutations by site-directed mutagenesis and transient expression in COS-7 cells or HEK293T cells. Each of these mutations was given a severity rating using a previously published system, based on the level of acid α-glucosidase activity in medium and transfected cells and on the quantity and quality of the different molecular mass species in the posttranslational modification and transport of acid α-glucosidase. This approach enabled to classify 55 missense mutations as pathogenic and 13 as likely nonpathogenic. Based on their nature and the use of in silico analysis (Alamut® software), 12 of the additional 25 novel mutations were predicted to be pathogenic including 4 splicing mutations, 6 mutations leading to frameshift, and 2 point mutations causing stop codons. Seven of the additional mutations were considered nonpathogenic (4 silent and 3 occurring in intron regions), and 6 are still under investigation.

Original language	English
Pages (from-to)	1161-1165
Number of pages	5
Journal	Human Mutation
Volume	33
Issue number	8
DOIs	https://doi.org/10.1002/humu.22108
State	Published - Aug 2012

Keywords

α-glucosidase
Acid maltase
GAA
Glycogenosis
Lysosomal storage disorder
Pompe disease

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10.1002/humu.22108

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Kroos, M., Hoogeveen-Westerveld, M., Michelakakis, H., Pomponio, R., Van der Ploeg, A., Halley, D., Reuser, A., Augoustides-Savvopoulou, P., Ausems, M., Llona, J. B., Bautista Lorite, J., van der Beek, N., Bonafe, L., Cuk, M., D'Hooghe, M., Engelen, B., Farouk, A., Fumic, K., Garcia-Delgado, E., ... Verhoeven, K. (2012). Update of the pompe disease mutation database with 60 novel GAA sequence variants and additional studies on the functional effect of 34 previously reported variants. Human Mutation, 33(8), 1161-1165. https://doi.org/10.1002/humu.22108

@article{c9944ab5f59e4220a593d86ce318042f,

title = "Update of the pompe disease mutation database with 60 novel GAA sequence variants and additional studies on the functional effect of 34 previously reported variants",

abstract = "Pompe disease is an autosomal recessive lysosomal glycogen storage disorder, characterized by progressive muscle weakness. Deficiency of acid α-glucosidase (EC; 3.2.1.20/3) can be caused by numerous pathogenic variants in the GAA gene. The Pompe Disease Mutation Database at aims to list all variants and their effect. This update reports on 94 variants. We examined 35 novel and 34 known mutations by site-directed mutagenesis and transient expression in COS-7 cells or HEK293T cells. Each of these mutations was given a severity rating using a previously published system, based on the level of acid α-glucosidase activity in medium and transfected cells and on the quantity and quality of the different molecular mass species in the posttranslational modification and transport of acid α-glucosidase. This approach enabled to classify 55 missense mutations as pathogenic and 13 as likely nonpathogenic. Based on their nature and the use of in silico analysis (Alamut{\textregistered} software), 12 of the additional 25 novel mutations were predicted to be pathogenic including 4 splicing mutations, 6 mutations leading to frameshift, and 2 point mutations causing stop codons. Seven of the additional mutations were considered nonpathogenic (4 silent and 3 occurring in intron regions), and 6 are still under investigation.",

keywords = "α-glucosidase, Acid maltase, GAA, Glycogenosis, Lysosomal storage disorder, Pompe disease",

author = "Marian Kroos and Marianne Hoogeveen-Westerveld and Helen Michelakakis and Robert Pomponio and \{Van der Ploeg\}, Ans and Dicky Halley and Arnold Reuser and Persephone Augoustides-Savvopoulou and Margreet Ausems and Llona, \{Jose Barcena\} and \{Bautista Lorite\}, Juan and \{van der Beek\}, Nadine and Luisa Bonafe and Mario Cuk and Marc D'Hooghe and Baziel Engelen and A. Farouk and K. Fumic and E. Garcia-Delgado and Andreas Herzog and J. Hurst and Simon Jones and Kariminejad, \{M. H.\} and Aynur K{\"u}{\c c}{\"u}k{\c c}ongar and W. Lissens and Allan Lund and Danielle Majoor-Krakauer and Shingo Kumamoto and E. Maravi and Suely Marie and Eugen Mengel and Irene Mavridou and \{Munteis Olivas\}, E. and H. Najmabadi and Toshika Okumiya and Stojan Peric and Eduard Paschke and Barbara Plecko and Wim Robberecht and Piraye Serdaroglu and Mohammad Shboul and Tansek, \{Mojca Zerjav\} and A. Tarnutzer and Stojanovic, \{Vidosava Rakocevic\} and Anna Tylki-Szymanska and Maria Ven{\^a}ncio and Kristof Verhoeven",

year = "2012",

month = aug,

doi = "10.1002/humu.22108",

language = "English",

volume = "33",

pages = "1161--1165",

journal = "Human Mutation",

issn = "1059-7794",

publisher = "John Wiley and Sons Inc",

number = "8",

}

Kroos, M, Hoogeveen-Westerveld, M, Michelakakis, H, Pomponio, R, Van der Ploeg, A, Halley, D, Reuser, A, Augoustides-Savvopoulou, P, Ausems, M, Llona, JB, Bautista Lorite, J, van der Beek, N, Bonafe, L, Cuk, M, D'Hooghe, M, Engelen, B, Farouk, A, Fumic, K, Garcia-Delgado, E, Herzog, A, Hurst, J, Jones, S, Kariminejad, MH, Küçükçongar, A, Lissens, W, Lund, A, Majoor-Krakauer, D, Kumamoto, S, Maravi, E, Marie, S, Mengel, E, Mavridou, I, Munteis Olivas, E, Najmabadi, H, Okumiya, T, Peric, S, Paschke, E, Plecko, B, Robberecht, W, Serdaroglu, P, Shboul, M, Tansek, MZ, Tarnutzer, A, Stojanovic, VR, Tylki-Szymanska, A, Venâncio, M & Verhoeven, K 2012, 'Update of the pompe disease mutation database with 60 novel GAA sequence variants and additional studies on the functional effect of 34 previously reported variants', Human Mutation, vol. 33, no. 8, pp. 1161-1165. https://doi.org/10.1002/humu.22108

TY - JOUR

T1 - Update of the pompe disease mutation database with 60 novel GAA sequence variants and additional studies on the functional effect of 34 previously reported variants

AU - Kroos, Marian

AU - Hoogeveen-Westerveld, Marianne

AU - Michelakakis, Helen

AU - Pomponio, Robert

AU - Van der Ploeg, Ans

AU - Halley, Dicky

AU - Reuser, Arnold

AU - Augoustides-Savvopoulou, Persephone

AU - Ausems, Margreet

AU - Llona, Jose Barcena

AU - Bautista Lorite, Juan

AU - van der Beek, Nadine

AU - Bonafe, Luisa

AU - Cuk, Mario

AU - D'Hooghe, Marc

AU - Engelen, Baziel

AU - Farouk, A.

AU - Fumic, K.

AU - Garcia-Delgado, E.

AU - Herzog, Andreas

AU - Hurst, J.

AU - Jones, Simon

AU - Kariminejad, M. H.

AU - Küçükçongar, Aynur

AU - Lissens, W.

AU - Lund, Allan

AU - Majoor-Krakauer, Danielle

AU - Kumamoto, Shingo

AU - Maravi, E.

AU - Marie, Suely

AU - Mengel, Eugen

AU - Mavridou, Irene

AU - Munteis Olivas, E.

AU - Najmabadi, H.

AU - Okumiya, Toshika

AU - Peric, Stojan

AU - Paschke, Eduard

AU - Plecko, Barbara

AU - Robberecht, Wim

AU - Serdaroglu, Piraye

AU - Shboul, Mohammad

AU - Tansek, Mojca Zerjav

AU - Tarnutzer, A.

AU - Stojanovic, Vidosava Rakocevic

AU - Tylki-Szymanska, Anna

AU - Venâncio, Maria

AU - Verhoeven, Kristof

PY - 2012/8

Y1 - 2012/8

N2 - Pompe disease is an autosomal recessive lysosomal glycogen storage disorder, characterized by progressive muscle weakness. Deficiency of acid α-glucosidase (EC; 3.2.1.20/3) can be caused by numerous pathogenic variants in the GAA gene. The Pompe Disease Mutation Database at aims to list all variants and their effect. This update reports on 94 variants. We examined 35 novel and 34 known mutations by site-directed mutagenesis and transient expression in COS-7 cells or HEK293T cells. Each of these mutations was given a severity rating using a previously published system, based on the level of acid α-glucosidase activity in medium and transfected cells and on the quantity and quality of the different molecular mass species in the posttranslational modification and transport of acid α-glucosidase. This approach enabled to classify 55 missense mutations as pathogenic and 13 as likely nonpathogenic. Based on their nature and the use of in silico analysis (Alamut® software), 12 of the additional 25 novel mutations were predicted to be pathogenic including 4 splicing mutations, 6 mutations leading to frameshift, and 2 point mutations causing stop codons. Seven of the additional mutations were considered nonpathogenic (4 silent and 3 occurring in intron regions), and 6 are still under investigation.

AB - Pompe disease is an autosomal recessive lysosomal glycogen storage disorder, characterized by progressive muscle weakness. Deficiency of acid α-glucosidase (EC; 3.2.1.20/3) can be caused by numerous pathogenic variants in the GAA gene. The Pompe Disease Mutation Database at aims to list all variants and their effect. This update reports on 94 variants. We examined 35 novel and 34 known mutations by site-directed mutagenesis and transient expression in COS-7 cells or HEK293T cells. Each of these mutations was given a severity rating using a previously published system, based on the level of acid α-glucosidase activity in medium and transfected cells and on the quantity and quality of the different molecular mass species in the posttranslational modification and transport of acid α-glucosidase. This approach enabled to classify 55 missense mutations as pathogenic and 13 as likely nonpathogenic. Based on their nature and the use of in silico analysis (Alamut® software), 12 of the additional 25 novel mutations were predicted to be pathogenic including 4 splicing mutations, 6 mutations leading to frameshift, and 2 point mutations causing stop codons. Seven of the additional mutations were considered nonpathogenic (4 silent and 3 occurring in intron regions), and 6 are still under investigation.

KW - α-glucosidase

KW - Acid maltase

KW - GAA

KW - Glycogenosis

KW - Lysosomal storage disorder

KW - Pompe disease

UR - https://www.scopus.com/pages/publications/84863872592

U2 - 10.1002/humu.22108

DO - 10.1002/humu.22108

M3 - Article

C2 - 22644586

AN - SCOPUS:84863872592

SN - 1059-7794

VL - 33

SP - 1161

EP - 1165

JO - Human Mutation

JF - Human Mutation

IS - 8

ER -

Update of the pompe disease mutation database with 60 novel GAA sequence variants and additional studies on the functional effect of 34 previously reported variants

Abstract

Keywords

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