Identification of microdeletions spanning the Diamond-Blackfan anemia locus on 19q13 and evidence for genetic heterogeneity

Peter Gustavsson; Emanuela Garelli; Natalia Draptchinskaia; Sarah Ball; Thiébaut Noël Willig; Dimitri Tentler; Irma Dianzani; Hope H. Punnett; Frank E. Shafer; Holger Cario; Ugo Ramenghi; Anders Glomstein; Rudolf A. Pfeiffer; Andy Goringe; Nancy F. Olivieri; Elizabeth Smibert; Gil Tchernia; Göran Elinder; Niklas Dahl

doi:10.1086/302100

Identification of microdeletions spanning the Diamond-Blackfan anemia locus on 19q13 and evidence for genetic heterogeneity

Peter Gustavsson, Emanuela Garelli, Natalia Draptchinskaia, Sarah Ball, Thiébaut Noël Willig, Dimitri Tentler, Irma Dianzani, Hope H. Punnett, Frank E. Shafer, Holger Cario, Ugo Ramenghi, Anders Glomstein, Rudolf A. Pfeiffer, Andy Goringe, Nancy F. Olivieri, Elizabeth Smibert, Gil Tchernia, Göran Elinder, Niklas Dahl

Risultato della ricerca: Contributo su rivista › Articolo in rivista › peer review

Abstract

Diamond-Blackfan anemia (DBA) is a rare pure red-cell hypoplasia of unknown etiology and pathogenesis. A major DBA locus has previously been localized to chromosome 19q13.2. Samples from additional families have been collected to identify key recombinations, microdeletions, and the possibility of heterogeneity for the disorder. In total, 29 multiplex DBA families and 50 families that comprise sporadic DBA cases have been analyzed with polymorphic 19q13 markers, including a newly identified short-tandem repeat in the critical gene region. The results from DNA analysis of 29 multiplex families revealed that 26 of these were consistent with a DBA gene on 19q localized to within a 4.1-cM interval restricted by loci D19S200 and D19S178; however, in three multiplex families, the DBA candidate region on 19q13 was excluded from the segregation of marker alleles. Our results suggest genetic heterogeneity for DBA, and we show that a gene region on chromosome 19q segregates with the disease in the majority of familial cases. Among the 50 families comprising sporadic DBA cases, we identified two novel and overlapping microdeletions on chromosome 19q13. In combination, the three known microdeletions associated with DBA restrict the critical gene region to ~1 Mb. The results indicate that a proportion of sporadic DBA cases are caused by deletions in the 19q13 region.

Lingua originale	Inglese
pagine (da-a)	1388-1395
Numero di pagine	8
Rivista	American Journal of Human Genetics
Volume	63
Numero di pubblicazione	5
DOI	https://doi.org/10.1086/302100
Stato di pubblicazione	Pubblicato - 1998
Pubblicato esternamente	Sì

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10.1086/302100

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Gustavsson, P., Garelli, E., Draptchinskaia, N., Ball, S., Willig, T. N., Tentler, D., Dianzani, I., Punnett, H. H., Shafer, F. E., Cario, H., Ramenghi, U., Glomstein, A., Pfeiffer, R. A., Goringe, A., Olivieri, N. F., Smibert, E., Tchernia, G., Elinder, G., & Dahl, N. (1998). Identification of microdeletions spanning the Diamond-Blackfan anemia locus on 19q13 and evidence for genetic heterogeneity. American Journal of Human Genetics, 63(5), 1388-1395. https://doi.org/10.1086/302100

@article{80eb392482684c14b777a60309198b96,

title = "Identification of microdeletions spanning the Diamond-Blackfan anemia locus on 19q13 and evidence for genetic heterogeneity",

abstract = "Diamond-Blackfan anemia (DBA) is a rare pure red-cell hypoplasia of unknown etiology and pathogenesis. A major DBA locus has previously been localized to chromosome 19q13.2. Samples from additional families have been collected to identify key recombinations, microdeletions, and the possibility of heterogeneity for the disorder. In total, 29 multiplex DBA families and 50 families that comprise sporadic DBA cases have been analyzed with polymorphic 19q13 markers, including a newly identified short-tandem repeat in the critical gene region. The results from DNA analysis of 29 multiplex families revealed that 26 of these were consistent with a DBA gene on 19q localized to within a 4.1-cM interval restricted by loci D19S200 and D19S178; however, in three multiplex families, the DBA candidate region on 19q13 was excluded from the segregation of marker alleles. Our results suggest genetic heterogeneity for DBA, and we show that a gene region on chromosome 19q segregates with the disease in the majority of familial cases. Among the 50 families comprising sporadic DBA cases, we identified two novel and overlapping microdeletions on chromosome 19q13. In combination, the three known microdeletions associated with DBA restrict the critical gene region to \textasciitilde{}1 Mb. The results indicate that a proportion of sporadic DBA cases are caused by deletions in the 19q13 region.",

author = "Peter Gustavsson and Emanuela Garelli and Natalia Draptchinskaia and Sarah Ball and Willig, \{Thi{\'e}baut No{\"e}l\} and Dimitri Tentler and Irma Dianzani and Punnett, \{Hope H.\} and Shafer, \{Frank E.\} and Holger Cario and Ugo Ramenghi and Anders Glomstein and Pfeiffer, \{Rudolf A.\} and Andy Goringe and Olivieri, \{Nancy F.\} and Elizabeth Smibert and Gil Tchernia and G{\"o}ran Elinder and Niklas Dahl",

note = "Funding Information: We thank Laurie Gordon at Lawrence Livermore National Laboratory. We also thank the DBA working groups, the European Society of Pediatric Hematology and Immunology, and all of the families who cooperated in this study. This study was supported by grants from the Children's Cancer Foundation of Sweden, the Swedish Medical Research Council, Torsten och Ragnar S{\"o}derberg's Foundation, Lundberg's Research Foundation, Ronald McDonald's Fund for Children, S{\"a}vstaholm Society, the DBA Foundation, Selanders Foundation, and L{\"a}ndells Foundation. We also would like to thank Telethon-Italy (grant E.619), U.K. DBA Registry support came from the Max Reinhart Charitable Trust, Direction de la Recherche Clinique (grant CRC 950183), Assistance Publique-H{\^o}pitaux de Paris, Association Fran{\c c}aise contre les Myopathies, and G{\'e}n{\'e}thon. ",

year = "1998",

doi = "10.1086/302100",

language = "English",

volume = "63",

pages = "1388--1395",

journal = "American Journal of Human Genetics",

issn = "0002-9297",

publisher = "Cell Press",

number = "5",

}

Gustavsson, P, Garelli, E, Draptchinskaia, N, Ball, S, Willig, TN, Tentler, D, Dianzani, I, Punnett, HH, Shafer, FE, Cario, H, Ramenghi, U, Glomstein, A, Pfeiffer, RA, Goringe, A, Olivieri, NF, Smibert, E, Tchernia, G, Elinder, G & Dahl, N 1998, 'Identification of microdeletions spanning the Diamond-Blackfan anemia locus on 19q13 and evidence for genetic heterogeneity', American Journal of Human Genetics, vol. 63, n. 5, pagg. 1388-1395. https://doi.org/10.1086/302100

TY - JOUR

T1 - Identification of microdeletions spanning the Diamond-Blackfan anemia locus on 19q13 and evidence for genetic heterogeneity

AU - Gustavsson, Peter

AU - Garelli, Emanuela

AU - Draptchinskaia, Natalia

AU - Ball, Sarah

AU - Willig, Thiébaut Noël

AU - Tentler, Dimitri

AU - Dianzani, Irma

AU - Punnett, Hope H.

AU - Shafer, Frank E.

AU - Cario, Holger

AU - Ramenghi, Ugo

AU - Glomstein, Anders

AU - Pfeiffer, Rudolf A.

AU - Goringe, Andy

AU - Olivieri, Nancy F.

AU - Smibert, Elizabeth

AU - Tchernia, Gil

AU - Elinder, Göran

AU - Dahl, Niklas

N1 - Funding Information: We thank Laurie Gordon at Lawrence Livermore National Laboratory. We also thank the DBA working groups, the European Society of Pediatric Hematology and Immunology, and all of the families who cooperated in this study. This study was supported by grants from the Children's Cancer Foundation of Sweden, the Swedish Medical Research Council, Torsten och Ragnar Söderberg's Foundation, Lundberg's Research Foundation, Ronald McDonald's Fund for Children, Sävstaholm Society, the DBA Foundation, Selanders Foundation, and Ländells Foundation. We also would like to thank Telethon-Italy (grant E.619), U.K. DBA Registry support came from the Max Reinhart Charitable Trust, Direction de la Recherche Clinique (grant CRC 950183), Assistance Publique-Hôpitaux de Paris, Association Française contre les Myopathies, and Généthon.

PY - 1998

Y1 - 1998

N2 - Diamond-Blackfan anemia (DBA) is a rare pure red-cell hypoplasia of unknown etiology and pathogenesis. A major DBA locus has previously been localized to chromosome 19q13.2. Samples from additional families have been collected to identify key recombinations, microdeletions, and the possibility of heterogeneity for the disorder. In total, 29 multiplex DBA families and 50 families that comprise sporadic DBA cases have been analyzed with polymorphic 19q13 markers, including a newly identified short-tandem repeat in the critical gene region. The results from DNA analysis of 29 multiplex families revealed that 26 of these were consistent with a DBA gene on 19q localized to within a 4.1-cM interval restricted by loci D19S200 and D19S178; however, in three multiplex families, the DBA candidate region on 19q13 was excluded from the segregation of marker alleles. Our results suggest genetic heterogeneity for DBA, and we show that a gene region on chromosome 19q segregates with the disease in the majority of familial cases. Among the 50 families comprising sporadic DBA cases, we identified two novel and overlapping microdeletions on chromosome 19q13. In combination, the three known microdeletions associated with DBA restrict the critical gene region to ~1 Mb. The results indicate that a proportion of sporadic DBA cases are caused by deletions in the 19q13 region.

AB - Diamond-Blackfan anemia (DBA) is a rare pure red-cell hypoplasia of unknown etiology and pathogenesis. A major DBA locus has previously been localized to chromosome 19q13.2. Samples from additional families have been collected to identify key recombinations, microdeletions, and the possibility of heterogeneity for the disorder. In total, 29 multiplex DBA families and 50 families that comprise sporadic DBA cases have been analyzed with polymorphic 19q13 markers, including a newly identified short-tandem repeat in the critical gene region. The results from DNA analysis of 29 multiplex families revealed that 26 of these were consistent with a DBA gene on 19q localized to within a 4.1-cM interval restricted by loci D19S200 and D19S178; however, in three multiplex families, the DBA candidate region on 19q13 was excluded from the segregation of marker alleles. Our results suggest genetic heterogeneity for DBA, and we show that a gene region on chromosome 19q segregates with the disease in the majority of familial cases. Among the 50 families comprising sporadic DBA cases, we identified two novel and overlapping microdeletions on chromosome 19q13. In combination, the three known microdeletions associated with DBA restrict the critical gene region to ~1 Mb. The results indicate that a proportion of sporadic DBA cases are caused by deletions in the 19q13 region.

UR - http://www.scopus.com/inward/record.url?scp=0032231651&partnerID=8YFLogxK

U2 - 10.1086/302100

DO - 10.1086/302100

M3 - Article

SN - 0002-9297

VL - 63

SP - 1388

EP - 1395

JO - American Journal of Human Genetics

JF - American Journal of Human Genetics

IS - 5

ER -

Identification of microdeletions spanning the Diamond-Blackfan anemia locus on 19q13 and evidence for genetic heterogeneity

Abstract

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