Molecular analysis and genotype-phenotype correlation of Diamond-Blackfan anemia

被引:28
作者
Arbiv, O. A. [1 ]
Cuvelier, G. [2 ]
Klaassen, R. J. [3 ]
Fernandez, C. V. [4 ]
Robitaille, N. [5 ]
Steele, M. [6 ]
Breakey, V. [7 ]
Abish, S. [8 ]
Wu, J. [9 ]
Sinha, R. [10 ]
Silva, M. [11 ]
Goodyear, L. [12 ]
Jardine, L. [13 ]
Lipton, J. H. [14 ]
Corriveau-Bourque, C. [15 ]
Brossard, J. [16 ]
Michon, B. [17 ]
Ghemlas, I. [1 ,18 ]
Waespe, N. [1 ,19 ]
Zlateska, B. [1 ,19 ]
Sung, L. [20 ,21 ]
Cada, M. [19 ]
Dror, Y. [1 ,19 ,22 ]
机构
[1] Hosp Sick Children, Res Inst, Program Genet & Genome Biol, Toronto, ON, Canada
[2] CancerCare Manitoba, Div Haematol Oncol, Winnipeg, MB, Canada
[3] Childrens Hosp Eastern Ontario, Div Haematol Oncol, Ottawa, ON, Canada
[4] IWK Hlth Ctr, Div Haematol Oncol, Halifax, NS, Canada
[5] CHU St Justine, Div Haematol Oncol, Montreal, PQ, Canada
[6] Alberta Childrens Prov Gen Hosp, Div Haematol Oncol, Calgary, AB, Canada
[7] McMaster Childrens Hosp, Div Haematol Oncol, Hamilton, ON, Canada
[8] Montreal Childrens Hosp, Div Haematol Oncol, Montreal, PQ, Canada
[9] British Columbia Childrens Hosp, Div Haematol Oncol, Vancouver, BC, Canada
[10] Univ Saskatchewan, Div Haematol Oncol, Saskatoon, SK, Canada
[11] Queens Univ, Div Haematol Oncol, Kingston, ON, Canada
[12] Janeway Child Hlth Ctr, Div Haematol Oncol, St John, NF, Canada
[13] Childrens Hosp Western Ontario, Div Haematol Oncol, London, ON, Canada
[14] Princess Margaret Hosp, Dept Haematol & Internal Med, Toronto, ON, Canada
[15] Univ Alberta, Hlth Sci Ctr, Div Haematol Oncol, Edmonton, AB, Canada
[16] Ctr Y Sante LEstrie Fleur, Div Haematol Oncol, Sherbrooke, PQ, Canada
[17] CHU Laval, Div Haematol Oncol, Quebec City, PQ, Canada
[18] King Faisal Specialist Hosp & Res Ctr, Div Haematol Oncol, Riyadh, Saudi Arabia
[19] Hosp Sick Children, Dept Paediat, Div Haematol Oncol, Marrow Failure & Myelodysplasia Program,Haematol, Toronto, ON, Canada
[20] Hosp Sick Children, Res Inst, Program Child Hlth & Evaluat Med, Toronto, ON, Canada
[21] Hosp Sick Children, Dept Paediat, Div Haematol Oncol, Lymphoma Leukemia Sect, Toronto, ON, Canada
[22] Univ Toronto, Inst Med Sci, Toronto, ON, Canada
关键词
anemia; Diamond-Blackfan anemia; genetics; genotype-phenotype correlation; inherited bone marrow failure syndromes; physical malformations; MARROW FAILURE SYNDROMES; STEM-CELL TRANSPLANTATION; RIBOSOMAL-PROTEIN L5; GENETIC-ANALYSIS; RPL11; GENES; MUTATIONS; REGISTRY; UPDATE; IDENTIFICATION; DISEASE;
D O I
10.1111/cge.13158
中图分类号
Q3 [遗传学];
学科分类号
071007 ; 090102 ;
摘要
Diamond-Blackfan anemia (DBA) features hypoplastic anemia and congenital malformations, largely caused by mutations in various ribosomal proteins. The aim of this study was to characterize the spectrum of genetic lesions causing DBA and identify genotypes that correlate with phenotypes of clinical significance. Seventy-four patients with DBA from across Canada were included. Nucleotide-level mutations or large deletions were identified in 10 ribosomal genes in 45 cases. The RPS19 mutation group was associated with higher requirement for chronic treatment for anemia than other DBA groups. Patients with RPS19 mutations, however, were more likely to maintain long-term corticosteroid response without requirement for further chronic transfusions. Conversely, patients with RPL11 mutations were less likely to need chronic treatment. Birth defects, including cardiac, skeletal, hand, cleft lip or palate and genitourinary malformations, also varied among the various genetic groups. Patients with RPS19 mutations had the fewest number of defects, while patients with RPL5 had the greatest number of birth defects. This is the first study to show differences between DBA genetic groups with regards to treatment. Previously unreported differences in the rate and types of birth defects were also identified. These data allow better patient counseling, a more personalized monitoring plan, and may also suggest differential functions of DBA genes on ribosome and extra-ribosomal functions.
引用
收藏
页码:320 / 328
页数:9
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