Your search keyword '"Diamond–Blackfan anemia"' showing total 12 results

1. Functionally impaired RPL8 variants associated with Diamond–Blackfan anemia and a Diamond–Blackfan anemia‐like phenotype.

Author

Lebaron, Simon, O'Donohue, Marie‐Françoise, Smith, Scott C., Engleman, Kendra L., Juusola, Jane, Safina, Nicole P., Thiffault, Isabelle, Saunders, Carol J., and Gleizes, Pierre‐Emmanuel

Abstract

Diamond–Blackfan anemia is a rare genetic disease characterized by erythroblastopenia and a large spectrum of developmental anomalies. The vast majority of the cases genetically described are linked to heterozygous pathogenic variants in more than 20 ribosomal protein genes. Here we report an atypical clinical case of DBA associated with a missense variant in RPL8, which encodes RPL8/uL2, a protein of the 60S large ribosomal subunit. RPL8 has been previously implicated as a candidate disease gene in one patient with DBA bearing another type of missense variant; however, evidence for pathogenicity was limited to computational tools. Using functional studies in lymphoblastoid cells as well as yeast models, we show that the RPL8 variants detected in these two patients encode functionally deficient proteins that affect ribosome production and are therefore likely pathogenic. We propose to include RPL8 in the list of DBA‐associated genes. [ABSTRACT FROM AUTHOR]

Published

2022

2. Expansion of germline RPS20 mutation phenotype to include Diamond–Blackfan anemia.

Author

Bhar, Saleh, Zhou, Fujun, Reineke, Lucas C., Morris, Danna K., Khincha, Payal P., Giri, Neelam, Mirabello, Lisa, Bergstrom, Katie, Lemon, Laramie D., Williams, Christopher L., Toh, Yukimatsu, Elghetany, M. Tarek, Lloyd, Richard E., Alter, Blanche P., Savage, Sharon A., and Bertuch, Alison A.

Abstract

Diamond–Blackfan anemia (DBA) is a ribosomopathy of variable expressivity and penetrance characterized by red cell aplasia, congenital anomalies, and predisposition to certain cancers, including early‐onset colorectal cancer (CRC). DBA is primarily caused by a dominant mutation of a ribosomal protein (RP) gene, although approximately 20% of patients remain genetically uncharacterized despite exome sequencing and copy number analysis. Although somatic loss‐of‐function mutations in RP genes have been reported in sporadic cancers, with the exceptions of 5q‐myelodysplastic syndrome (RPS14) and microsatellite unstable CRC (RPL22), these cancers are not enriched in DBA. Conversely, pathogenic variants in RPS20 were previously implicated in familial CRC; however, none of the reported individuals had classical DBA features. We describe two unrelated children with DBA lacking variants in known DBA genes who were found by exome sequencing to have de novo novel missense variants in RPS20. The variants affect the same amino acid but result in different substitutions and reduce the RPS20 protein level. Yeast models with mutation of the cognate residue resulted in defects in growth, ribosome biogenesis, and polysome formation. These findings expand the phenotypic spectrum of RPS20 mutation beyond familial CRC to include DBA, which itself is associated with increased risk of CRC. [ABSTRACT FROM AUTHOR]

Published

2020

3. A functional assay for the clinical annotation of genetic variants of uncertain significance in Diamond–Blackfan anemia.

Author

Aspesi, Anna, Betti, Marta, Sculco, Marika, Actis, Chiara, Olgasi, Cristina, Wlodarski, Marcin W., Vlachos, Adrianna, Lipton, Jeffrey M., Ramenghi, Ugo, Santoro, Claudio, Follenzi, Antonia, Ellis, Steven R., and Dianzani, Irma

Abstract

Abstract: Diamond–Blackfan anemia (DBA) is a rare genetic hypoplasia of erythroid progenitors characterized by mild to severe anemia and associated with congenital malformations. Clinical manifestations in DBA patients are quite variable and genetic testing has become a critical factor in establishing a diagnosis of DBA. The majority of DBA cases are due to heterozygous loss‐of‐function mutations in ribosomal protein (RP) genes. Causative mutations are fairly straightforward to identify in the case of large deletions and frameshift and nonsense mutations found early in a protein coding sequence, but diagnosis becomes more challenging in the case of missense mutations and small in‐frame indels. Our group recently characterized the phenotype of lymphoblastoid cell lines established from DBA patients with pathogenic lesions in RPS19 and observed that defective pre‐rRNA processing, a hallmark of the disease, was rescued by lentiviral vectors expressing wild‐type RPS19. Here, we use this complementation assay to determine whether RPS19 variants of unknown significance are capable of rescuing pre‐rRNA processing defects in these lymphoblastoid cells as a means of assessing the effects of these sequence changes on the function of the RPS19 protein. This approach will be useful in differentiating pathogenic mutations from benign polymorphisms in identifying causative genes in DBA patients. [ABSTRACT FROM AUTHOR]

Published

2018

4. Expansion of germline RPS20 mutation phenotype to include Diamond-Blackfan anemia

Author

Payal P. Khincha, Yukimatsu Toh, Lucas C. Reineke, Laramie D. Lemon, M. Tarek Elghetany, Katie Bergstrom, Fujun Zhou, Lisa Mirabello, Alison A. Bertuch, Christopher L. Williams, Richard E. Lloyd, Danna K. Morris, Saleh Bhar, Neelam Giri, Sharon A. Savage, and Blanche P. Alter

Subjects

Male, Ribosomal Proteins, Adolescent, Ribosomopathy, Copy number analysis, Penetrance, Biology, medicine.disease_cause, Germline, Article, 03 medical and health sciences, Exome Sequencing, Genetics, medicine, Missense mutation, Humans, Amino Acid Sequence, Diamond–Blackfan anemia, Child, Genetics (clinical), Exome sequencing, Germ-Line Mutation, 030304 developmental biology, Anemia, Diamond-Blackfan, 0303 health sciences, Mutation, 030305 genetics & heredity, Infant, Newborn, medicine.disease, Pedigree, Protein Structure, Tertiary, Female, Colorectal Neoplasms

Abstract

Diamond-Blackfan anemia (DBA) is a ribosomopathy of variable expressivity and penetrance characterized by red cell aplasia, congenital anomalies, and predisposition to certain cancers, including early-onset colorectal cancer (CRC). DBA is primarily caused by a dominant mutation of a ribosomal protein (RP) gene, although approximately 20% of patients remain genetically uncharacterized despite exome sequencing and copy number analysis. Although somatic loss-of-function mutations in RP genes have been reported in sporadic cancers, with the exceptions of 5q-myelodysplastic syndrome (RPS14) and microsatellite unstable CRC (RPL22), these cancers are not enriched in DBA. Conversely, pathogenic variants in RPS20 were previously implicated in familial CRC; however, none of the reported individuals had classical DBA features. We describe two unrelated children with DBA lacking variants in known DBA genes who were found by exome sequencing to have de novo novel missense variants in RPS20. The variants affect the same amino acid but result in different substitutions and reduce the RPS20 protein level. Yeast models with mutation of the cognate residue resulted in defects in growth, ribosome biogenesis, and polysome formation. These findings expand the phenotypic spectrum of RPS20 mutation beyond familial CRC to include DBA, which itself is associated with increased risk of CRC.

Published

2020

5. A functional assay for the clinical annotation of genetic variants of uncertain significance in Diamond–Blackfan anemia

Author

Irma Dianzani, Marika Sculco, Marta Betti, Antonia Follenzi, Adrianna Vlachos, Jeffrey M. Lipton, Steven R. Ellis, Chiara Actis, Cristina Olgasi, Marcin W. Wlodarski, Ugo Ramenghi, Anna Aspesi, and Claudio Santoro

Subjects

0301 basic medicine, Diamond–Blackfan anemia, Ribosomal Proteins, DNA, Complementary, RPS19, Nonsense mutation, Biology, medicine.disease_cause, functional assay, ribosomal protein, VUS, Genetics, Genetics (clinical), Frameshift mutation, Cell Line, 03 medical and health sciences, medicine, Missense mutation, Humans, Frameshift Mutation, Gene, Research Articles, Genetic testing, Anemia, Diamond-Blackfan, Mutation, medicine.diagnostic_test, Computational Biology, medicine.disease, Phenotype, 3. Good health, 030104 developmental biology, Codon, Nonsense, Research Article

Abstract

Diamond–Blackfan anemia (DBA) is a rare genetic hypoplasia of erythroid progenitors characterized by mild to severe anemia and associated with congenital malformations. Clinical manifestations in DBA patients are quite variable and genetic testing has become a critical factor in establishing a diagnosis of DBA. The majority of DBA cases are due to heterozygous loss‐of‐function mutations in ribosomal protein (RP) genes. Causative mutations are fairly straightforward to identify in the case of large deletions and frameshift and nonsense mutations found early in a protein coding sequence, but diagnosis becomes more challenging in the case of missense mutations and small in‐frame indels. Our group recently characterized the phenotype of lymphoblastoid cell lines established from DBA patients with pathogenic lesions in RPS19 and observed that defective pre‐rRNA processing, a hallmark of the disease, was rescued by lentiviral vectors expressing wild‐type RPS19. Here, we use this complementation assay to determine whether RPS19 variants of unknown significance are capable of rescuing pre‐rRNA processing defects in these lymphoblastoid cells as a means of assessing the effects of these sequence changes on the function of the RPS19 protein. This approach will be useful in differentiating pathogenic mutations from benign polymorphisms in identifying causative genes in DBA patients.

Published

2018

6. Frameshift mutation in p53 regulator RPL26 is associated with multiple physical abnormalities and a specific pre-ribosomal RNA processing defect in diamond-blackfan anemia.

Author

Gazda, Hanna T., Preti, Milena, Sheen, Mee Rie, O'Donohue, Marie-Françoise, Vlachos, Adrianna, Davies, Stella M., Kattamis, Antonis, Doherty, Leana, Landowski, Michael, Buros, Christopher, Ghazvinian, Roxanne, Sieff, Colin A., Newburger, Peter E., Niewiadomska, Edyta, Matysiak, Michal, Glader, Bertil, Atsidaftos, Eva, Lipton, Jeffrey M., Gleizes, Pierre-Emmanuel, and Beggs, Alan H.

Abstract

Diamond-Blackfan anemia (DBA) is an inherited form of pure red cell aplasia that usually presents in infancy or early childhood and is associated with congenital malformations in ∼30-50% of patients. DBA has been associated with mutations in nine ribosomal protein (RP) genes in about 53% of patients. We completed a large-scale screen of 79 RP genes by sequencing 16 RP genes ( RPL3, RPL7, RPL8, RPL10, RPL14, RPL17, RPL19, RPL23A, RPL26, RPL27, RPL35, RPL36A, RPL39, RPS4X, RPS4Y1, and RPS21) in 96 DBA probands. We identified a de novo two-nucleotide deletion in RPL26 in one proband associated with multiple severe physical abnormalities. This mutation gives rise to a remarkable ribosome biogenesis defect that affects maturation of both the small and the large subunits. We also found a deletion in RPL19 and missense mutations in RPL3 and RPL23A, which may be variants of unknown significance. Together with RPL5, RPL11, and RPS7, RPL26 is the fourth RP regulating p53 activity that is linked to DBA. Hum Mutat 33:1037-1044, 2012. © 2012 Wiley Periodicals, Inc. [ABSTRACT FROM AUTHOR]

Published

2012

7. Frameshift mutation in p53 regulatorRPL26is associated with multiple physical abnormalities and a specific pre-ribosomal RNA processing defect in diamond-blackfan anemia

Author

Leana Doherty, Adrianna Vlachos, Eva Atsidaftos, Antonis Kattamis, Stella M. Davies, Michał Matysiak, Christopher Buros, Alan H. Beggs, Edyta Niewiadomska, Colin A. Sieff, Jeffrrey M. Lipton, Milena Preti, Michael Landowski, Marie-Françoise O'Donohue, Roxanne Ghazvinian, Pierre-Emmanuel Gleizes, Mee Rie Sheen, Hanna T. Gazda, Bertil Glader, Peter E. Newburger, Laboratoire de biologie moléculaire eucaryote (LBME), Université Toulouse III - Paul Sabatier (UT3), Université Fédérale Toulouse Midi-Pyrénées-Université Fédérale Toulouse Midi-Pyrénées-Centre National de la Recherche Scientifique (CNRS)-Centre de Biologie Intégrative (CBI), Université Fédérale Toulouse Midi-Pyrénées-Université Fédérale Toulouse Midi-Pyrénées-Centre National de la Recherche Scientifique (CNRS)-Centre National de la Recherche Scientifique (CNRS), Division of Genetics and Program in Genomics, The Manton Center for Orphan Disease Research, Boston Children's Hospital, The Feinstein Institute for Medical Research, First department of Pediatrics, University of Athens School of Medicine, Laboratory of Human Genetics of Infectious Diseases, Cohen Children's Medical Center of New York, Hofstra University School of Medicine, Hofstra University [Hempstead], First Department of Paediatrics, Athens University, Thalassaemia Unit, and 'Aghia Sofia' Children's Hospital

Subjects

Ribosomal Proteins, Proband, Ribosomopathy, Ribosomal Protein L3, [SDV]Life Sciences [q-bio], Blotting, Western, Pure red cell aplasia, Biology, medicine.disease_cause, Article, Frameshift mutation, 03 medical and health sciences, 0302 clinical medicine, Ribosomal protein, Genetics, medicine, Humans, Missense mutation, Abnormalities, Multiple, [SDV.BBM]Life Sciences [q-bio]/Biochemistry, Molecular Biology, RNA, Small Interfering, Diamond–Blackfan anemia, Frameshift Mutation, ComputingMilieux_MISCELLANEOUS, Genetics (clinical), Anemia, Diamond-Blackfan, 030304 developmental biology, 0303 health sciences, Mutation, Blotting, Northern, medicine.disease, Molecular biology, 3. Good health, RNA, Ribosomal, 030220 oncology & carcinogenesis, Tumor Suppressor Protein p53, [SDV.MHEP]Life Sciences [q-bio]/Human health and pathology, HeLa Cells

Abstract

International audience; Diamond-Blackfan anemia (DBA) is an inherited form of pure red cell aplasia that usually presents in infancy or early childhood and is associated with congenital malformations in ∼30-50% of patients. DBA has been associated with mutations in nine ribosomal protein (RP) genes in about 53% of patients. We completed a large scale screen of 79 RP genes by sequencing 16 RP genes (RPL3, RPL7, RPL8, RPL10, RPL14, RPL17, RPL19, RPL23A, RPL26, RPL27, RPL35, RPL36A, RPL39, RPS4X, RPS4Y1, and RPS21) in 96 DBA probands. We identified a de novo two-nucleotide deletion in RPL26 in one proband associated with multiple severe physical abnormalities. This mutation gives rise to a remarkable ribosome biogenesis defect that affects maturation of both the small and the large subunits. We also found a deletion in RPL19 and missense mutations in RPL3 and RPL23A, which may be variants of unknown significance. Together with RPL5, RPL11, and RPS7, RPL26 is the fourth ribosomal protein regulating p53 activity that is linked to DBA.

Published

2012

8. Identification of mutations in the ribosomal protein L5 (RPL5) and ribosomal protein L11 (RPL11) genes in Czech patients with Diamond-Blackfan anemia

Author

Helena Handrkova, Zdena Cerna, Jan Stary, Dagmar Pospisilova, Jana Cmejlova, Kvetoslava Petrtylova, Jiri Petrak, Y. Jabali, Vladimír Mihál, and Radek Cmejla

Subjects

Adult, Male, Ribosomal Proteins, DNA Mutational Analysis, Biology, medicine.disease_cause, Ribosomal protein L5, Young Adult, Gene Frequency, Ribosomal protein, Large ribosomal subunit, Genetics, medicine, Humans, Registries, Diamond–Blackfan anemia, Child, education, Gene, Genetics (clinical), Aged, Anemia, Diamond-Blackfan, Czech Republic, Family Health, Mutation, education.field_of_study, Base Sequence, Infant, Aplasia, Ribosomal RNA, medicine.disease, Molecular biology, Female

Abstract

Diamond-Blackfan anemia (DBA) is a congenital red blood cell aplasia that is usually diagnosed during early infancy. Apart from defects in red blood cell maturation, the disorder is also associated with various physical anomalies in 40% of patients. Mutations in the ribosomal protein (RP) S19 are found in 25% of patients, while mutations in other proteins of the small ribosomal subunit--RPS17 and RPS24--have been found in a fraction of patients. Recently, mutations in RPL5, RPL11, and RPL35a of the large ribosomal subunit have also been reported in several DBA patients. Here, we present the identification of mutations in the RPL5 and RPL11 genes in patients from the Czech DBA Registry. Mutations in RPL5 were identified in eight patients from 6 out of 28 families (21.4%), and mutations in RPL11 in two patients from 2 out of 28 families (7.1%). Interestingly, all 10 patients with either an RPL5 or RPL11 mutation exhibited one or more physical anomalies; specifically, thumb anomalies (flat thenar) were always present, while no such anomaly was observed in seven patients with an RPS19 mutation. Moreover, 9 out of 10 patients with either an RPL5 or RPL11 mutation were born small for gestational age (SGA) compared to 3 out of 7 patients from the RPS19-mutated group. These observations may suggest that mutations, at least in RPL5, seem to generally have more profound impact on fetal development than mutations in RPS19. Since RPL5 and RPL11, together with RPL23, are also involved in the MDM2-mediated p53 pathway regulation, we also screened the RPL23 gene for mutations; however, no mutations were identified.

Published

2009

9. A new database for ribosomal protein genes which are mutated in Diamond-Blackfan Anemia

Author

Irma Dianzani, Ilenia Boria, Federica Avondo, Ugo Ramenghi, Anna Aspesi, Paola Quarello, Adriana Carando, Emanuela Garelli, and Maria Francesca Campagnoli

Subjects

Ribosomal Proteins, DNA Mutational Analysis, Biology, Gene mutation, computer.software_genre, medicine.disease_cause, Genome, User-Computer Interface, Ribosomal protein, hemic and lymphatic diseases, Genetics, medicine, Humans, Diamond–Blackfan anemia, Gene, Genetics (clinical), Anemia, Diamond-Blackfan, Mutation, Database, Genome, Human, Diamond Blackfan syndrome, Autosomal dominant trait, medicine.disease, Phenotype, ribosomal protein, Databases, Nucleic Acid, computer

Abstract

Mutations in ribosomal proteins RPS19, RPS24 and RPS17 have been reported in Diamond-Blackfan Anemia (DBA), an autosomal dominant disease characterised by pure red cell aplasia. DBA is the prototype of ribosomapathies: a protein synthesis defect in a tissue with a high cellular turnover is considered the cause of the erythroid progenitor failure. We have created the Diamond-Blackfan Anemia mutation database to curate and record DBA gene mutations, together with their functional consequences and clinical phenotypes. This locus-specific resource is open to future submissions and is available online (http://www.dbagenes.unito.it). It is founded on the Leiden Open (source) Variation Database (LOVD) system and includes data from sequence and structure analysis tools, genomic database resources and published reports. It lists all identified variants and background genomic information. Phenotypic data are accessed by selecting a particular mutation. The database includes 219 unique variants of which 86 are disease-causing mutations. The database will be supplemented with other DBA genes as soon as they are reported and their mutations are identified and it should be of assistance to clinicians and investigators involved in DBA research and care.

Published

2008

10. Nonsense-mediated and nonstop decay of ribosomal protein S19 mRNA in Diamond-Blackfan anemia

Author

Gil Tchernia, Emanuela Garelli, Irma Dianzani, Andrew Chatr-aryamontri, Mara Angelini, Ugo Ramenghi, and Fabrizio Loreni

Subjects

RPS19, DNA Mutational Analysis, Messenger, Nonsense-mediated decay, nonsense mutation, NonStop, medicine.disease_cause, fibroblast, Diamond-Blackfan anemia, Diamond-Blackfan, Complementary, genetic stability, Missense mutation, Northern, gene mutation, Diamond–Blackfan anemia, Cells, Cultured, Genetics (clinical), Anemia, Diamond-Blackfan, Genetics, Mutation, Cultured, messenger RNA, Blotting, Reverse Transcriptase Polymerase Chain Reaction, Settore BIO/11, allele, article, Anemia, gene expression regulation, RNA analysis, Nonsense mediated decay, Stop codon, unclassified drug, priority journal, Blackfan Diamond anemia, Codon, Terminator, Sequence Analysis, Ribosomal Proteins, DNA, Complementary, regulatory mechanism, congenital malformation, Cells, rare disease, Biology, Cell Line, ribosome protein, RNA degradation, Ribosomal protein S19, medicine, protein s19, stop codon, Humans, NMD, controlled study, RNA, Messenger, human, Terminator, Codon, Gene, Alleles, gene identification, DBA, nonstop decay, lymphoblastoid cell, gene deletion, human cell, missense mutation, congenital hypoplastic anemia, nucleotide sequence, Sequence Analysis, DNA, DNA, Blotting, Northern, medicine.disease, Molecular biology, protein analysis, Protein Biosynthesis, RNA, nonsense mediated decay, Gene Deletion

Abstract

Mutations in the ribosomal protein (RP)S19 gene have been found in about 25% of the cases of Diamond-Blackfan anemia (DBA), a rare congenital hypoplastic anemia that includes variable physical malformations. Various mutations have been identified in the RPS19 gene, but no investigations regarding the effect of these alterations on RPS19 mRNA levels have been performed. It is well established that mutated mRNA containing a premature stop codon (PTC) or lacking a stop codon can be rapidly degraded by specific mechanisms called nonsense mediated decay (NMD) and nonstop decay. To study the involvement of such mechanisms in DBA, we analyzed immortalized lymphoblastoid cells and primary fibroblasts from patients presenting different kinds of mutations in the RPS19 gene, generating allelic deletion, missense, nonsense, and nonstop messengers. We found that RPS19 mRNA levels are decreased in the cells with allelic deletion and, to a variable extent, also in all the cell lines with PTC or nonstop mutations. Further analysis showed that translation inhibition causes a stabilization of the mutated RPS19 mRNA. Our findings indicate that NMD and nonstop decay affect the expression of mutated RPS19 genes; this may help to clarify genotype-phenotype correlations in DBA.

Published

2004

11. RPS19 mutations in patients with Diamond-Blackfan anemia

Author

Irma Dianzani, Marta Armiraglio, Fabrizio Loreni, Emanuela Garelli, Pierre-Emmanuel Gleizes, Sébastien Fribourg, Paola Quarello, Adriana Carando, Ugo Ramenghi, Maria Francesca Campagnoli, Federica Avondo, Elisa Pavesi, Laboratoire de biologie moléculaire eucaryote (LBME), Université Toulouse III - Paul Sabatier (UT3), Université Fédérale Toulouse Midi-Pyrénées-Université Fédérale Toulouse Midi-Pyrénées-Centre National de la Recherche Scientifique (CNRS)-Centre de Biologie Intégrative (CBI), and Université Fédérale Toulouse Midi-Pyrénées-Université Fédérale Toulouse Midi-Pyrénées-Centre National de la Recherche Scientifique (CNRS)-Centre National de la Recherche Scientifique (CNRS)

Subjects

Ribosomal Proteins, Diamond-Blackfan anemia, ribosomal protein S19, erythropoiesis, ribosome biogenesis, Biology, medicine.disease_cause, Frameshift mutation, 03 medical and health sciences, 0302 clinical medicine, Ribosomal protein S19, hemic and lymphatic diseases, Genetics, medicine, Missense mutation, Humans, Erythropoiesis, [SDV.BBM]Life Sciences [q-bio]/Biochemistry, Molecular Biology, Diamond–Blackfan anemia, Gene, Genetics (clinical), 030304 developmental biology, Anemia, Diamond-Blackfan, 0303 health sciences, Mutation, Polymorphism, Genetic, Settore BIO/11, Ribosome biogenesis, medicine.disease, 3. Good health, Phenotype, 030220 oncology & carcinogenesis, Cancer research, Haploinsufficiency

Abstract

Diamond-Blackfan anemia (DBA) is an inherited disease characterized by pure erythroid aplasia. Thirty percent (30%) of patients display malformations, especially of the hands, face, heart, and urogenital tract. DBA has an autosomal dominant pattern of inheritance. De novo mutations are common and familial cases display wide clinical heterogeneity. Twenty-five percent (25%) of patients carry a mutation in the ribosomal protein (RP) S19 gene, whereas mutations in RPS24, RPS17, RPL35A, RPL11, and RPL5 are rare. These genes encode for structural proteins of the ribosome. A link between ribosomal functions and erythroid aplasia is apparent in DBA, but its etiology is not clear. Most authors agree that a defect in protein synthesis in a rapidly proliferating tissue, such as the erythroid bone marrow, may explain the defective erythropoiesis. A total of 77 RPS19 mutations have been described. Most are whole gene deletions, translocations, or truncating mutations (nonsense or frameshift), suggesting that haploinsufficiency is the basis of DBA pathology. A total of 22 missense mutations have also been described and several works have provided in vitro functional data for the mutant proteins. This review looks at the data on all these mutations, proposes a functional classification, and describes six new mutations. It is shown that patients with RPS19 mutations display a poorer response to steroids and a worse long-term prognosis compared to other DBA patients.

Published

2008

12. Ribosomal protein S17 gene (RPS17) is mutated in Diamond-Blackfan anemia

Author

Dagmar Pospisilova, Jiri Petrak, Jana Cmejlova, Radek Cmejla, and Helena Handrkova

Subjects

Genetics, Adult, Male, Ribosomal Proteins, Mutation, Ribosomopathy, Codon, Initiator, Biology, medicine.disease, medicine.disease_cause, Molecular biology, Ribosome Subunits, Small, Eukaryotic translation, Start codon, Ribosomal protein, Ribosomal protein S19, medicine, Humans, Diamond–Blackfan anemia, Gene, Genetics (clinical), Anemia, Diamond-Blackfan

Abstract

Diamond-Blackfan anemia (DBA) is a congenital erythroid aplasia characterized as a normochromic macrocytic anemia with a selective deficiency in red blood cell precursors in otherwise normocellular bone marrow. In 40% of DBA patients, various physical anomalies are also present. Currently two genes are associated with the DBA phenotype--the ribosomal protein (RP) S19 mutated in 25% of DBA patients and RPS24 mutated in approximately 1.4% of DBA patients. Here we report the identification of a mutation in yet another ribosomal protein, RPS17. The mutation affects the translation initiation start codon, changing T to G (c.2T>G), thus eliminating the natural start of RPS17 protein biosynthesis. RNA analysis revealed that the mutated allele was expressed, and the next downstream start codon located at position +158 should give rise to a short peptide of only four amino acids (Met-Ser-Arg-Ile). The mutation arose de novo, since all healthy family members carry the wild-type alleles. The identification of a mutation in the third RP of the small ribosomal subunit in DBA patients further supports the theory that impaired translation may be the main cause of DBA pathogenesis.

Published

2007