Diamond-Blackfan anaemia: genetic homogeneity for a gene on chromosome 19q13 restricted to 1.8 Mb

Gustavsson, Peter; Willig, Thiébaut-Noël; Haeringen, Arie van; Tchernia, Gil; Dianzani, Irma; Donnér, Mikael; Elinder, Göran; Renter, Jan-Inge; Nilsson, Per‐Gunnar; Gordon, Laurie; Skeppner, Gunnar; Veer-Korthof, Lisbeth van't; Kreuger, Anders; Dahl, Niklas

doi:10.1038/ng0897-368

Cited by 89 publications

(74 citation statements)

References 14 publications

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“…This gene is located at chromosome 19q13.2 and encodes a protein belonging to the small subunit of the ribosome. 9,10 Haploinsufficiency of the RPS19 gene product has been demonstrated in a subset of cases 11 and appears to be sufficient to cause DBA. The RPS19 protein plays an important role in 18S rRNA maturation and small ribosomal subunit synthesis in human cells.…”

Section: Introductionmentioning

confidence: 99%

Mutations in the ribosomal protein genes in Japanese patients with Diamond-Blackfan anemia

et al. 2010

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BackgroundDiamond-Blackfan anemia is a rare, clinically heterogeneous, congenital red cell aplasia: 40% of patients have congenital abnormalities. Recent studies have shown that in western countries, the disease is associated with heterozygous mutations in the ribosomal protein (RP) genes in about 50% of patients. There have been no studies to determine the incidence of these mutations in Asian patients with Diamond-Blackfan anemia. Design and MethodsWe screened 49 Japanese patients with Diamond-Blackfan anemia (45 probands) for mutations in the six known genes associated with Diamond-Blackfan anemia: RPS19, RPS24, RPS17, RPL5, RPL11, and RPL35A. RPS14 was also examined due to its implied involvement in 5q-syndrome. ResultsMutations in RPS19, RPL5, RPL11 and RPS17 were identified in five, four, two and one of the probands, respectively. In total, 12 (27%) of the Japanese Diamond-Blackfan anemia patients had mutations in ribosomal protein genes. No mutations were detected in RPS14, RPS24 or RPL35A. All patients with RPS19 and RPL5 mutations had physical abnormalities. Remarkably, cleft palate was seen in two patients with RPL5 mutations, and thumb anomalies were seen in six patients with an RPS19 or RPL5 mutation. In contrast, a small-for-date phenotype was seen in five patients without an RPL5 mutation. ConclusionsWe observed a slightly lower frequency of mutations in the ribosomal protein genes in patients with Diamond-Blackfan anemia compared to the frequency reported in western countries. Genotype-phenotype data suggest an association between anomalies and RPS19 mutations, and a negative association between small-for-date phenotype and RPL5 mutations.Key words: protein genes, Diamond-Blackfan anemia, RPL5 mutation. DiamondBlackfan anemia. Haematologica 2010;95(8):1293-1299. doi:10.3324/haematol.2009 This is an open-access paper. Citation: Konno Y, Toki T, Tandai S, Xu G, Wang RN, Terui K, Ohga S, Hara T, Hama A, Kojima S, Hasegawa D, Kosaka Y, Yanagisawa R, Koike K, Kanai R, Imai T, Hongo T, Park M-J, Sugita K, and Ito E. Mutations in the ribosomal protein genes in Japanese patients with Mutations in the ribosomal protein genes in Japanese patients with Diamond-Blackfan anemia

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Section: Introductionmentioning

confidence: 99%

Mutations in the ribosomal protein genes in Japanese patients with Diamond-Blackfan anemia

et al. 2010

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“…WNTs signal via frizzled receptors to activate intracellular signaling pathways that lead to the stabilization of β-catenin (the socalled canonical pathway), or they stimulate various β-catenin-independent signals, like Ca 2+ influx or JNK activation (the noncanonical pathway) (1). Secreted frizzled-related proteins (SFRPs) containing cysteine-rich domains related to those of frizzled receptors negatively regulate WNT signaling by neutralizing WNTs extracellularly (2). WNT signaling has previously been reported to play an important role in adipocyte differentiation.…”

Section: Lighting the Fat Furnace Without Sfrp5mentioning

confidence: 99%

What’s in a name?

Weiss¹,

Mason²

2012

J. Clin. Invest.

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“…Although most cases of DBA are sporadic (approximately 75%), both dominant and autosomal recessive patterns of inheritance have been implicated in the remaining 25% of cases 30,36 -38 with dominant inheritance being more common. 39 In 1997, Gustavsson et al, 39 examined chromosome 19 for linkage to DBA after identifying a DBA patient with a balanced reciprocal translocation (X;19) (p21; q13). 39 (The X chromosome was excluded from consideration based on the observed autosomal transmission of DBA.)…”

Section: Ribosomal Protein Diseasesmentioning

confidence: 99%

“…39 In 1997, Gustavsson et al, 39 examined chromosome 19 for linkage to DBA after identifying a DBA patient with a balanced reciprocal translocation (X;19) (p21; q13). 39 (The X chromosome was excluded from consideration based on the observed autosomal transmission of DBA.) Subsequently, the region surrounding the (X;19) (p21; q13) translocation break point was cloned and sequenced allowing the identification of cytoplasmic ribosomal protein S19 (RPS19) as the gene disrupted by the translocation.…”

Section: Ribosomal Protein Diseasesmentioning

confidence: 99%

Mitochondrial ribosomal proteins: Candidate genes for mitochondrial disease

Sylvester

Fischel‐Ghodsian

Mougey

et al. 2004

Genetics in Medicine

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Most of the energy requirement for cell growth, differentiation, and development is met by the mitochondria in the form of ATP produced by the process of oxidative phosphorylation. Human mitochondrial DNA encodes a total of 13 proteins, all of which are essential for oxidative phosphorylation. The mRNAs for these proteins are translated on mitochondrial ribosomes. Recently, the genes for human mitochondrial ribosomal proteins (MRPs) have been identified. In this review, we summarize their refined chromosomal location. It is well known that mutations in the mitochondrial translation system, i.e., ribosomal RNA and transfer RNA cause various pathologies. In this review, we suggest possible associations between clinical conditions and MRPs based on coincidence of genetic map data and chromosomal location. These MRPs may be candidate genes for the clinical condition or may act as modifiers of existing known gene mutations (mt-tRNA, mt-rRNA, etc.). Genet Med 2004:6(2):73-80.

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Diamond-Blackfan anaemia: genetic homogeneity for a gene on chromosome 19q13 restricted to 1.8 Mb

Cited by 89 publications

References 14 publications

Mutations in the ribosomal protein genes in Japanese patients with Diamond-Blackfan anemia

Mutations in the ribosomal protein genes in Japanese patients with Diamond-Blackfan anemia

What’s in a name?

Mitochondrial ribosomal proteins: Candidate genes for mitochondrial disease

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