Origin, functional role, and clinical impact of fanconi anemia fanca mutations

Maria Castella; Roser Pujol; Elsa Callén; Juan P. Trujillo; José A. Casado; Hans Gille; Francis P. Lach; Arleen D. Auerbach; Detlev Schindler; Javier Benítez; Beatriz Porto; Teresa Ferro; Munoz Arturo; Julián Sevilla; Luis Madero; Elena Cela; Cristina Beléndez; Cristina Díaz De Heredia; Teresa Olivé; José Sánchez De Toledo; Isabel Badell; Montserrat Torrent; Jesús Estella; Ángeles Dasí; Antonia Rodríguez-Villa; Pedro Gémez; José Barbot; María Tapia; Antonio Molinés; Ángela Figuera; Juan A. Bueren; Jordi Surrallés

doi:10.1182/blood-2010-08-299917

Origin, functional role, and clinical impact of fanconi anemia fanca mutations

Maria Castella, Roser Pujol, Elsa Callén, Juan P. Trujillo, José A. Casado, Hans Gille, Francis P. Lach, Arleen D. Auerbach, Detlev Schindler, Javier Benítez, Beatriz Porto, Teresa Ferro, Munoz Arturo, Julián Sevilla, Luis Madero, Elena Cela, Cristina Beléndez, Cristina Díaz De Heredia, Teresa Olivé, José Sánchez De ToledoIsabel Badell, Montserrat Torrent, Jesús Estella, Ángeles Dasí, Antonia Rodríguez-Villa, Pedro Gémez, José Barbot, María Tapia, Antonio Molinés, Ángela Figuera, Juan A. Bueren, Jordi Surrallés

Producció científica: Contribució a revista › Article › Recerca › Avaluat per experts

109 Cites (Scopus)

Resum

Fanconi anemia is characterized by congenital abnormalities, bone marrow failure, and cancer predisposition. To investigate the origin, functional role, and clinical impact of FANCA mutations, we determined a FANCA mutational spectrum with 130 pathogenic alleles. Some of these mutations were further characterized for their distribution in populations, mode of emergence, or functional consequences at cellular and clinical level. The world most frequent FANCA mutation is not the result of a mutational "hot-spot" but results from worldwide dissemination of an ancestral Indo-European mutation. We provide molecular evidence that total absence of FANCA in humans does not reduce embryonic viability, as the observed frequency of mutation carriers in the Gypsy population equals the expected by Hardy-Weinberg equilibrium. We also prove that long distance Alu-Alu recombination can cause Fanconi anemia by originating large interstitial deletions involving FANCA and 2 adjacent genes. Finally, we show that all missense mutations studied lead to an altered FANCA protein that is unable to relocate to the nucleus and activate the FA/BRCA pathway. This may explain the observed lack of correlation between type of FANCA mutation and cellular phenotype or clinical severity in terms of age of onset of hematologic disease or number of malformations.

Idioma original	Anglès
Pàgines (de-a)	3759-3769
Revista	Blood
Volum	117
DOIs	https://doi.org/10.1182/blood-2010-08-299917
Estat de la publicació	Publicada - 7 d’abr. 2011

SDG de les Nacions Unides

Aquest resultat contribueix als següents objectius de desenvolupament sostenible.

Accés al document

10.1182/blood-2010-08-299917

Com citar-ho

Castella, M., Pujol, R., Callén, E., Trujillo, J. P., Casado, J. A., Gille, H., Lach, F. P., Auerbach, A. D., Schindler, D., Benítez, J., Porto, B., Ferro, T., Arturo, M., Sevilla, J., Madero, L., Cela, E., Beléndez, C., De Heredia, C. D., Olivé, T., ... Surrallés, J. (2011). Origin, functional role, and clinical impact of fanconi anemia fanca mutations. Blood, 117, 3759-3769. https://doi.org/10.1182/blood-2010-08-299917

@article{8c31db4dcbc945299e9e3d13c3f928c1,

title = "Origin, functional role, and clinical impact of fanconi anemia fanca mutations",

abstract = "Fanconi anemia is characterized by congenital abnormalities, bone marrow failure, and cancer predisposition. To investigate the origin, functional role, and clinical impact of FANCA mutations, we determined a FANCA mutational spectrum with 130 pathogenic alleles. Some of these mutations were further characterized for their distribution in populations, mode of emergence, or functional consequences at cellular and clinical level. The world most frequent FANCA mutation is not the result of a mutational {"}hot-spot{"} but results from worldwide dissemination of an ancestral Indo-European mutation. We provide molecular evidence that total absence of FANCA in humans does not reduce embryonic viability, as the observed frequency of mutation carriers in the Gypsy population equals the expected by Hardy-Weinberg equilibrium. We also prove that long distance Alu-Alu recombination can cause Fanconi anemia by originating large interstitial deletions involving FANCA and 2 adjacent genes. Finally, we show that all missense mutations studied lead to an altered FANCA protein that is unable to relocate to the nucleus and activate the FA/BRCA pathway. This may explain the observed lack of correlation between type of FANCA mutation and cellular phenotype or clinical severity in terms of age of onset of hematologic disease or number of malformations.",

author = "Maria Castella and Roser Pujol and Elsa Call{\'e}n and Trujillo, {Juan P.} and Casado, {Jos{\'e} A.} and Hans Gille and Lach, {Francis P.} and Auerbach, {Arleen D.} and Detlev Schindler and Javier Ben{\'i}tez and Beatriz Porto and Teresa Ferro and Munoz Arturo and Juli{\'a}n Sevilla and Luis Madero and Elena Cela and Cristina Bel{\'e}ndez and {De Heredia}, {Cristina D{\'i}az} and Teresa Oliv{\'e} and {De Toledo}, {Jos{\'e} S{\'a}nchez} and Isabel Badell and Montserrat Torrent and Jes{\'u}s Estella and {\'A}ngeles Das{\'i} and Antonia Rodr{\'i}guez-Villa and Pedro G{\'e}mez and Jos{\'e} Barbot and Mar{\'i}a Tapia and Antonio Molin{\'e}s and {\'A}ngela Figuera and Bueren, {Juan A.} and Jordi Surrall{\'e}s",

year = "2011",

month = apr,

day = "7",

doi = "10.1182/blood-2010-08-299917",

language = "English",

volume = "117",

pages = "3759--3769",

journal = "Blood",

issn = "0006-4971",

}

Castella, M, Pujol, R, Callén, E, Trujillo, JP, Casado, JA, Gille, H, Lach, FP, Auerbach, AD, Schindler, D, Benítez, J, Porto, B, Ferro, T, Arturo, M, Sevilla, J, Madero, L, Cela, E, Beléndez, C, De Heredia, CD, Olivé, T, De Toledo, JS, Badell, I, Torrent, M, Estella, J, Dasí, Á, Rodríguez-Villa, A, Gémez, P, Barbot, J, Tapia, M, Molinés, A, Figuera, Á, Bueren, JA & Surrallés, J 2011, 'Origin, functional role, and clinical impact of fanconi anemia fanca mutations', Blood, vol. 117, pàg. 3759-3769. https://doi.org/10.1182/blood-2010-08-299917

TY - JOUR

T1 - Origin, functional role, and clinical impact of fanconi anemia fanca mutations

AU - Castella, Maria

AU - Pujol, Roser

AU - Callén, Elsa

AU - Trujillo, Juan P.

AU - Casado, José A.

AU - Gille, Hans

AU - Lach, Francis P.

AU - Auerbach, Arleen D.

AU - Schindler, Detlev

AU - Benítez, Javier

AU - Porto, Beatriz

AU - Ferro, Teresa

AU - Arturo, Munoz

AU - Sevilla, Julián

AU - Madero, Luis

AU - Cela, Elena

AU - Beléndez, Cristina

AU - De Heredia, Cristina Díaz

AU - Olivé, Teresa

AU - De Toledo, José Sánchez

AU - Badell, Isabel

AU - Torrent, Montserrat

AU - Estella, Jesús

AU - Dasí, Ángeles

AU - Rodríguez-Villa, Antonia

AU - Gémez, Pedro

AU - Barbot, José

AU - Tapia, María

AU - Molinés, Antonio

AU - Figuera, Ángela

AU - Bueren, Juan A.

AU - Surrallés, Jordi

PY - 2011/4/7

Y1 - 2011/4/7

N2 - Fanconi anemia is characterized by congenital abnormalities, bone marrow failure, and cancer predisposition. To investigate the origin, functional role, and clinical impact of FANCA mutations, we determined a FANCA mutational spectrum with 130 pathogenic alleles. Some of these mutations were further characterized for their distribution in populations, mode of emergence, or functional consequences at cellular and clinical level. The world most frequent FANCA mutation is not the result of a mutational "hot-spot" but results from worldwide dissemination of an ancestral Indo-European mutation. We provide molecular evidence that total absence of FANCA in humans does not reduce embryonic viability, as the observed frequency of mutation carriers in the Gypsy population equals the expected by Hardy-Weinberg equilibrium. We also prove that long distance Alu-Alu recombination can cause Fanconi anemia by originating large interstitial deletions involving FANCA and 2 adjacent genes. Finally, we show that all missense mutations studied lead to an altered FANCA protein that is unable to relocate to the nucleus and activate the FA/BRCA pathway. This may explain the observed lack of correlation between type of FANCA mutation and cellular phenotype or clinical severity in terms of age of onset of hematologic disease or number of malformations.

AB - Fanconi anemia is characterized by congenital abnormalities, bone marrow failure, and cancer predisposition. To investigate the origin, functional role, and clinical impact of FANCA mutations, we determined a FANCA mutational spectrum with 130 pathogenic alleles. Some of these mutations were further characterized for their distribution in populations, mode of emergence, or functional consequences at cellular and clinical level. The world most frequent FANCA mutation is not the result of a mutational "hot-spot" but results from worldwide dissemination of an ancestral Indo-European mutation. We provide molecular evidence that total absence of FANCA in humans does not reduce embryonic viability, as the observed frequency of mutation carriers in the Gypsy population equals the expected by Hardy-Weinberg equilibrium. We also prove that long distance Alu-Alu recombination can cause Fanconi anemia by originating large interstitial deletions involving FANCA and 2 adjacent genes. Finally, we show that all missense mutations studied lead to an altered FANCA protein that is unable to relocate to the nucleus and activate the FA/BRCA pathway. This may explain the observed lack of correlation between type of FANCA mutation and cellular phenotype or clinical severity in terms of age of onset of hematologic disease or number of malformations.

U2 - 10.1182/blood-2010-08-299917

DO - 10.1182/blood-2010-08-299917

M3 - Article

SN - 0006-4971

VL - 117

SP - 3759

EP - 3769

JO - Blood

JF - Blood

ER -

Origin, functional role, and clinical impact of fanconi anemia fanca mutations

Resum

SDG de les Nacions Unides

Accés al document

Fingerprint

Com citar-ho