Your search keyword '"Bottomley SS"' showing total 78 results

1. The phenotypic spectrum of germline YARS2 variants: from isolated sideroblastic anemia to mitochondrial myopathy, lactic acidosis and sideroblastic anemia 2

Author

Riley, LG, Heeney, MM, Rudinger-Thirion, J, Frugier, M, Campagna, DR, Zhou, R, Hale, GA, Hilliard, LM, Kaplan, JA, Kwiatkowski, JL, Sieff, CA, Steensma, DP, Rennings, AJ, Simons, A, Schaap, N, Roodenburg, RJ, Kleefstra, T, Arenillas, L, Fita-Torro, J, Ahmed, R, Abboud, M, Bechara, E, Farah, R, Tamminga, RYJ, Bottomley, SS, Sanchez, M, Huls, G, Swinkels, DW, Christodoulou, J, Fleming, MD, Riley, LG, Heeney, MM, Rudinger-Thirion, J, Frugier, M, Campagna, DR, Zhou, R, Hale, GA, Hilliard, LM, Kaplan, JA, Kwiatkowski, JL, Sieff, CA, Steensma, DP, Rennings, AJ, Simons, A, Schaap, N, Roodenburg, RJ, Kleefstra, T, Arenillas, L, Fita-Torro, J, Ahmed, R, Abboud, M, Bechara, E, Farah, R, Tamminga, RYJ, Bottomley, SS, Sanchez, M, Huls, G, Swinkels, DW, Christodoulou, J, and Fleming, MD

Abstract

YARS2 variants have previously been described in patients with myopathy, lactic acidosis and sideroblastic anemia 2 (MLASA2). YARS2 encodes the mitochondrial tyrosyl-tRNA synthetase, which is responsible for conjugating tyrosine to its cognate mt-tRNA for mitochondrial protein synthesis. Here we describe 14 individuals from 11 families presenting with sideroblastic anemia and YARS2 variants that we identified using a sideroblastic anemia gene panel or exome sequencing. The phenotype of these patients ranged from MLASA to isolated congenital sideroblastic anemia. As in previous cases, inter- and intra-familial phenotypic variability was observed, however, this report includes the first cases with isolated sideroblastic anemia and patients with biallelic YARS2 variants that have no clinically ascertainable phenotype. We identified ten novel YARS2 variants and three previously reported variants. In vitro amino-acylation assays of five novel missense variants showed that three had less effect on the catalytic activity of YARS2 than the most commonly reported variant, p.(Phe52Leu), associated with MLASA2, which may explain the milder phenotypes in patients with these variants. However, the other two missense variants had a more severe effect on YARS2 catalytic efficiency. Several patients carried the common YARS2 c.572 G>T, p.(Gly191Val) variant (minor allele frequency =0.1259) in trans with a rare deleterious YARS2 variant. We have previously shown that the p.(Gly191Val) variant reduces YARS2 catalytic activity. Consequently, we suggest that biallelic YARS2 variants, including severe loss-of-function alleles in trans of the common p.(Gly191Val) variant, should be considered as a cause of isolated congenital sideroblastic anemia, as well as the MLASA syndromic phenotype.

Published

2018

2. Acute leukemia in idiopathic sideroblastic anemia: response to combination chemotherapy

Author

Hussein, KK, Salem, Z, Bottomley, SS, and Livingston, RB

Abstract

Three patients with idiopathic sideroblastic anemia of variable duration developed acute leukemia. In two the leukemia was morphologically and histochemically myeloblastic, in one lymphoblastic. With combination chemotherapy remission was achieved in all three. The remission inductions were complicated by long periods of bone marrow suppression and the duration of remissions was brief (3, 2 and 3 months). Survival after diagnosis was 13, 10 and 9 mo, respectively. The ring sideroblast abnormality persisted during the leukemic and remission phases and transfusion requirements remained unaltered in the two patients with transfusion dependent anemia throughout their courses.

Published

1982

3. Sideroblastic anemia with markedly increased free erythrocyte protoporphyrin without dermal photosensitivity

Author

Romslo, I, Brun, A, Sandberg, S, Bottomley, SS, Hovding, G, and Talstad, I

Abstract

A patient with idiopathic sideroblastic anemia and atypical clinical and biochemical findings is described. He had a greatly increased erythrocyte and plasma protoporphyrin, but normal urine and fecal porphyrins. The erythrocyte protoporphyrin had a fluorescence spectrum typical of free protoporphyrin, but caused no photosensitivity. Bone marrow metal chelatase activity was normal. There were no clinical signs of liver disease. The abnormal porphyrin metabolism in this patient is not known though a number of explanations are discussed.

Published

1982

4. Bone marrow delta-aminolaevulinate synthase deficiency in a female with congenital sideroblastic anemia

Author

Buchanan, GR, Bottomley, SS, and Nitschke, R

Abstract

Heme biosynthesis was examined in erythroid tissue of a 4-yr-old girl with severe sideroblastic anemia since infancy, as documented by the presence of intramitochondrial deposits of iron in erythroblasts. Free red cell protoporphyrin, urinary porphyrins, and activities of erythrocyte porphobilinogen synthase, uroporphyrinogen 1 synthase, aspartate aminotransferase, and pyridoxine kinase were normal or increased. Bone marrow ferrochelatase activity was normal. Activity of bone marrow delta-aminolaevulinate (ALA) synthase was markedly reduced to 7 pmole ALA/10(6) erythroblasts/30 min (normal 127 +/- 29) but was enhanced fivefold by pyridoxal phosphate (normal 0%--25% increase). Therapy with oral pyridoxine and parenteral pyridoxal-5'-phosphate did not increase effective red cell production. The sideroblastic anemia in this patient appears to be related to a congenital defect in the initial step of heme biosynthesis.

Published

1980

5. Red Plasma Caused By Unique Anthraquinones

Author

UCL, Bottomley, SS., Lemli, J., Compernolle, F., UCL, Bottomley, SS., Lemli, J., and Compernolle, F.

Published

1986

6. Delta-aminolevulinic acid synthetase activity in normal human bone marrow and in patients with idiopathic sideroblastic anemia

Author

Bottomley Ss, Tanaka M, and Self J

Subjects

medicine.medical_specialty, Time Factors, Glycine, Human bone, In Vitro Techniques, Biochemistry, Bone Marrow, Internal medicine, Delta-aminolevulinic acid synthetase activity, Medicine, Humans, In patient, Ketoglutarate Dehydrogenase Complex, Carbon Radioisotopes, Edetic Acid, Aged, business.industry, Idiopathic sideroblastic anemia, Hydrogen-Ion Concentration, Middle Aged, Chromatography, Ion Exchange, Levulinic Acids, Anemia, Sideroblastic, Kinetics, Endocrinology, Pyridoxal Phosphate, business, 5-Aminolevulinate Synthetase

Published

1973

7. Book reviews.

Author

Negro F, Bergman RN, Katan MB, and Bottomley SS

Published

2005

8. Engineered bacterial lipoate protein ligase A (lplA) restores lipoylation in cell models of lipoylation deficiency.

Author

Bick N, Dreishpoon M, Perry A, Rogachevskaya A, Bottomley SS, Fleming MD, Ducamp S, and Tsvetkov P

Abstract

Protein lipoylation, a vital lysine posttranslational modification (PTM), plays a crucial role in the function of key mitochondrial TCA cycle enzymatic complexes. In eukaryotes, lipoyl PTM synthesis occurs exclusively through de novo pathways, relying on lipoyl synthesis/transfer enzymes, dependent upon mitochondrial fatty acid and Fe-S cluster biosynthesis. Dysregulation in any of these pathways leads to diminished cellular lipoylation. Efficient restoration of lipoylation in lipoylation deficiency cell states using either chemical or genetic approaches has been challenging due to pathway complexity and multiple upstream regulators. To address this challenge, we explored the possibility that a bacterial lipoate protein ligase (lplA) enzyme, that can salvage free lipoic acid bypassing the dependency on de novo synthesis, could be engineered to be functional in human cells. Overexpression of the engineered lplA in lipoylation null cells restored lipoylation levels, cellular respiration, and growth in low glucose conditions. Engineered lplA restored lipoylation in all tested lipoylation null cell models, mimicking defects in mitochondrial fatty acid synthesis (MECR KO), Fe-S cluster biosynthesis (BOLA3 KO), and specific lipoylation regulating enzymes (FDX1, LIAS and LIPT1 KOs). Furthermore, we describe a patient with a homozygous c.212C>T variant LIPT1 with a previously uncharacterized syndromic congenital sideroblastic anemia. K562 erythroleukemia cells engineered to harbor this missense LIPT1 allele recapitulate the lipoylation deficient phenotype and exhibit impaired proliferation in low glucose that is completely restored by engineered lplA. This synthetic approach offers a potential therapeutic strategy for treating lipoylation disorders., Competing Interests: Conflict-of-interest disclosure The authors declare no competing financial interests., (Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2024

9. SLC25A38 congenital sideroblastic anemia: Phenotypes and genotypes of 31 individuals from 24 families, including 11 novel mutations, and a review of the literature.

Author

Heeney MM, Berhe S, Campagna DR, Oved JH, Kurre P, Shaw PJ, Teo J, Shanap MA, Hassab HM, Glader BE, Shah S, Yoshimi A, Ameri A, Antin JH, Boudreaux J, Briones M, Dickerson KE, Fernandez CV, Farah R, Hasle H, Keel SB, Olson TS, Powers JM, Rose MJ, Shimamura A, Bottomley SS, and Fleming MD

Subjects

Child, Preschool, Female, Humans, Infant, Infant, Newborn, Male, Anemia, Sideroblastic congenital, Genotype, Mitochondrial Membrane Transport Proteins genetics, Mutation, Phenotype

Abstract

The congenital sideroblastic anemias (CSAs) are a heterogeneous group of inherited disorders of erythropoiesis characterized by pathologic deposits of iron in the mitochondria of developing erythroblasts. Mutations in the mitochondrial glycine carrier SLC25A38 cause the most common recessive form of CSA. Nonetheless, the disease is still rare, there being fewer than 70 reported families. Here we describe the clinical phenotype and genotypes of 31 individuals from 24 families, including 11 novel mutations. We also review the spectrum of reported mutations and genotypes associated with the disease, describe the unique localization of missense mutations in transmembrane domains and account for the presence of several alleles in different populations., (© 2021 Wiley Periodicals LLC.)

Published

2021

10. Mutations in the iron-sulfur cluster biogenesis protein HSCB cause congenital sideroblastic anemia.

Author

Crispin A, Guo C, Chen C, Campagna DR, Schmidt PJ, Lichtenstein D, Cao C, Sendamarai AK, Hildick-Smith GJ, Huston NC, Boudreaux J, Bottomley SS, Heeney MM, Paw BH, Fleming MD, and Ducamp S

Subjects

Adolescent, Anemia, Sideroblastic congenital, Anemia, Sideroblastic metabolism, Animals, Child, DNA Mutational Analysis, Female, Frameshift Mutation, Gene Knockdown Techniques, Humans, Iron-Sulfur Proteins deficiency, Iron-Sulfur Proteins genetics, K562 Cells, Male, Mice, Mice, Knockout, Molecular Chaperones metabolism, Pedigree, Polymorphism, Single Nucleotide, Promoter Regions, Genetic, Young Adult, Zebrafish, Anemia, Sideroblastic genetics, Molecular Chaperones genetics, Mutation

Abstract

The congenital sideroblastic anemias (CSAs) can be caused by primary defects in mitochondrial iron-sulfur (Fe-S) cluster biogenesis. HSCB (heat shock cognate B), which encodes a mitochondrial cochaperone, also known as HSC20 (heat shock cognate protein 20), is the partner of mitochondrial heat shock protein A9 (HSPA9). Together with glutaredoxin 5 (GLRX5), HSCB and HSPA9 facilitate the transfer of nascent 2-iron, 2-sulfur clusters to recipient mitochondrial proteins. Mutations in both HSPA9 and GLRX5 have previously been associated with CSA. Therefore, we hypothesized that mutations in HSCB could also cause CSA. We screened patients with genetically undefined CSA and identified a frameshift mutation and a rare promoter variant in HSCB in a female patient with non-syndromic CSA. We found that HSCB expression was decreased in patient-derived fibroblasts and K562 erythroleukemia cells engineered to have the patient-specific promoter variant. Furthermore, gene knockdown and deletion experiments performed in K562 cells, zebrafish, and mice demonstrate that loss of HSCB results in impaired Fe-S cluster biogenesis, a defect in RBC hemoglobinization, and the development of siderocytes and more broadly perturbs hematopoiesis in vivo. These results further affirm the involvement of Fe-S cluster biogenesis in erythropoiesis and hematopoiesis and define HSCB as a CSA gene.

Published

2020

11. The phenotypic spectrum of germline YARS2 variants: from isolated sideroblastic anemia to mitochondrial myopathy, lactic acidosis and sideroblastic anemia 2.

Author

Riley LG, Heeney MM, Rudinger-Thirion J, Frugier M, Campagna DR, Zhou R, Hale GA, Hilliard LM, Kaplan JA, Kwiatkowski JL, Sieff CA, Steensma DP, Rennings AJ, Simons A, Schaap N, Roodenburg RJ, Kleefstra T, Arenillas L, Fita-Torró J, Ahmed R, Abboud M, Bechara E, Farah R, Tamminga RYJ, Bottomley SS, Sanchez M, Huls G, Swinkels DW, Christodoulou J, and Fleming MD

Subjects

Acidosis, Lactic enzymology, Adolescent, Anemia, Sideroblastic enzymology, Female, Genetic Association Studies, Genetic Diseases, X-Linked enzymology, Humans, Infant, MELAS Syndrome enzymology, Male, Middle Aged, Mutation, Missense, Young Adult, Acidosis, Lactic genetics, Anemia, Sideroblastic genetics, Genetic Diseases, X-Linked genetics, Germ-Line Mutation, MELAS Syndrome genetics, Mitochondrial Proteins genetics, Tyrosine-tRNA Ligase genetics

Abstract

YARS2 variants have previously been described in patients with myopathy, lactic acidosis and sideroblastic anemia 2 (MLASA2). YARS2 encodes the mitochondrial tyrosyl-tRNA synthetase, which is responsible for conjugating tyrosine to its cognate mt-tRNA for mitochondrial protein synthesis. Here we describe 14 individuals from 11 families presenting with sideroblastic anemia and YARS2 variants that we identified using a sideroblastic anemia gene panel or exome sequencing. The phenotype of these patients ranged from MLASA to isolated congenital sideroblastic anemia. As in previous cases, inter- and intra-familial phenotypic variability was observed, however, this report includes the first cases with isolated sideroblastic anemia and patients with biallelic YARS2 variants that have no clinically ascertainable phenotype. We identified ten novel YARS2 variants and three previously reported variants. In vitro amino-acylation assays of five novel missense variants showed that three had less effect on the catalytic activity of YARS2 than the most commonly reported variant, p.(Phe52Leu), associated with MLASA2, which may explain the milder phenotypes in patients with these variants. However, the other two missense variants had a more severe effect on YARS2 catalytic efficiency. Several patients carried the common YARS2 c.572 G>T, p.(Gly191Val) variant (minor allele frequency =0.1259) in trans with a rare deleterious YARS2 variant. We have previously shown that the p.(Gly191Val) variant reduces YARS2 catalytic activity. Consequently, we suggest that biallelic YARS2 variants, including severe loss-of-function alleles in trans of the common p.(Gly191Val) variant, should be considered as a cause of isolated congenital sideroblastic anemia, as well as the MLASA syndromic phenotype., (Copyright© 2018 Ferrata Storti Foundation.)

Published

2018

12. Recurrent heteroplasmy for the MT-ATP6 p.Ser148Asn (m.8969G>A) mutation in patients with syndromic congenital sideroblastic anemia of variable clinical severity.

Author

Berhe S, Heeney MM, Campagna DR, Thompson JF, White EJ, Ross T, Peake RWA, Hanrahan JD, Rodriguez V, Renaud DL, Patnaik MS, Chang E, Bottomley SS, and Fleming MD

Subjects

Adolescent, Anemia, Sideroblastic metabolism, Anemia, Sideroblastic pathology, Child, DNA Mutational Analysis methods, Female, Genetic Association Studies, Genetic Diseases, X-Linked metabolism, Genetic Diseases, X-Linked pathology, Humans, Infant, Male, Mitochondrial Proton-Translocating ATPases metabolism, Point Mutation, Recurrence, Syndrome, Anemia, Sideroblastic genetics, DNA, Mitochondrial genetics, Genetic Diseases, X-Linked genetics, Mitochondrial Proton-Translocating ATPases genetics, Mutation, Missense

Published

2018

13. Reduced-toxicity allogeneic hematopoietic stem cell transplantation in congenital sideroblastic anemia.

Author

Kim MH, Shah S, Bottomley SS, and Shah NC

Abstract

The case of an infant girl with severe congenital sideroblastic anemia associated with a novel molecular defect in mitochondrial transporter SLC25A38 is presented. Her transfusion dependence was fully reversed following allogeneic hematopoietic stem cell transplantation using a modified reduced-intensity conditioning regimen, and she remains healthy 5 years posttransplant.

Published

2018

14. A recurring mutation in the respiratory complex 1 protein NDUFB11 is responsible for a novel form of X-linked sideroblastic anemia.

Author

Lichtenstein DA, Crispin AW, Sendamarai AK, Campagna DR, Schmitz-Abe K, Sousa CM, Kafina MD, Schmidt PJ, Niemeyer CM, Porter J, May A, Patnaik MM, Heeney MM, Kimmelman A, Bottomley SS, Paw BH, Markianos K, and Fleming MD

Subjects

Adolescent, Adult, Aged, Anemia, Sideroblastic metabolism, Anemia, Sideroblastic pathology, Child, Child, Preschool, Chromosomes, Human, X metabolism, Electron Transport Complex I metabolism, Female, Genetic Diseases, X-Linked metabolism, Humans, K562 Cells, Male, Middle Aged, Anemia, Sideroblastic genetics, Base Sequence, Chromosomes, Human, X genetics, Electron Transport Complex I genetics, Genetic Diseases, X-Linked genetics, Sequence Deletion

Abstract

The congenital sideroblastic anemias (CSAs) are a heterogeneous group of inherited blood disorders characterized by pathological mitochondrial iron deposition in erythroid precursors. Each known cause has been attributed to a mutation in a protein associated with heme biosynthesis, iron-sulfur cluster biogenesis, mitochondrial translation, or a component of the mitochondrial respiratory chain. Here, we describe a recurring mutation, c.276_278del, p.F93del, in NDUFB11, a mitochondrial respiratory complex I-associated protein encoded on the X chromosome, in 5 males with a variably syndromic, normocytic CSA. The p.F93del mutation results in respiratory insufficiency and loss of complex I stability and activity in patient-derived fibroblasts. Targeted introduction of this allele into K562 erythroleukemia cells results in a proliferation defect with minimal effect on erythroid differentiation potential, suggesting the mechanism of anemia in this disorder., (© 2016 by The American Society of Hematology.)

Published

2016

15. Congenital sideroblastic anemia due to mutations in the mitochondrial HSP70 homologue HSPA9.

Author

Schmitz-Abe K, Ciesielski SJ, Schmidt PJ, Campagna DR, Rahimov F, Schilke BA, Cuijpers M, Rieneck K, Lausen B, Linenberger ML, Sendamarai AK, Guo C, Hofmann I, Newburger PE, Matthews D, Shimamura A, Snijders PJ, Towne MC, Niemeyer CM, Watson HG, Dziegiel MH, Heeney MM, May A, Bottomley SS, Swinkels DW, Markianos K, Craig EA, and Fleming MD

Subjects

Adult, Aged, Base Sequence, DNA Mutational Analysis, Female, Genotype, Humans, Infant, Infant, Newborn, Male, Middle Aged, Molecular Sequence Data, Mutation, Oligonucleotide Array Sequence Analysis, Pedigree, Polymorphism, Single Nucleotide, Real-Time Polymerase Chain Reaction, Reverse Transcriptase Polymerase Chain Reaction, Young Adult, Anemia, Sideroblastic genetics, Genetic Diseases, X-Linked genetics, HSP70 Heat-Shock Proteins genetics, Mitochondrial Proteins genetics

Abstract

The congenital sideroblastic anemias (CSAs) are relatively uncommon diseases characterized by defects in mitochondrial heme synthesis, iron-sulfur (Fe-S) cluster biogenesis, or protein synthesis. Here we demonstrate that mutations in HSPA9, a mitochondrial HSP70 homolog located in the chromosome 5q deletion syndrome 5q33 critical deletion interval and involved in mitochondrial Fe-S biogenesis, result in CSA inherited as an autosomal recessive trait. In a fraction of patients with just 1 severe loss-of-function allele, expression of the clinical phenotype is associated with a common coding single nucleotide polymorphism in trans that correlates with reduced messenger RNA expression and results in a pseudodominant pattern of inheritance., (© 2015 by The American Society of Hematology.)

Published

2015

16. Mutations in TRNT1 cause congenital sideroblastic anemia with immunodeficiency, fevers, and developmental delay (SIFD).

Author

Chakraborty PK, Schmitz-Abe K, Kennedy EK, Mamady H, Naas T, Durie D, Campagna DR, Lau A, Sendamarai AK, Wiseman DH, May A, Jolles S, Connor P, Powell C, Heeney MM, Giardina PJ, Klaassen RJ, Kannengiesser C, Thuret I, Thompson AA, Marques L, Hughes S, Bonney DK, Bottomley SS, Wynn RF, Laxer RM, Minniti CP, Moppett J, Bordon V, Geraghty M, Joyce PB, Markianos K, Rudner AD, Holcik M, and Fleming MD

Subjects

Alleles, Anemia, Sideroblastic complications, Anemia, Sideroblastic enzymology, Developmental Disabilities genetics, Fever genetics, Genetic Diseases, X-Linked complications, Genetic Diseases, X-Linked enzymology, HEK293 Cells, Humans, Immunologic Deficiency Syndromes genetics, Anemia, Sideroblastic congenital, Anemia, Sideroblastic genetics, Developmental Disabilities complications, Fever complications, Genetic Diseases, X-Linked genetics, Immunologic Deficiency Syndromes complications, Mutation genetics, RNA Nucleotidyltransferases genetics

Abstract

Mutations in genes encoding proteins that are involved in mitochondrial heme synthesis, iron-sulfur cluster biogenesis, and mitochondrial protein synthesis have previously been implicated in the pathogenesis of the congenital sideroblastic anemias (CSAs). We recently described a syndromic form of CSA associated with B-cell immunodeficiency, periodic fevers, and developmental delay (SIFD). Here we demonstrate that SIFD is caused by biallelic mutations in TRNT1, the gene encoding the CCA-adding enzyme essential for maturation of both nuclear and mitochondrial transfer RNAs. Using budding yeast lacking the TRNT1 homolog, CCA1, we confirm that the patient-associated TRNT1 mutations result in partial loss of function of TRNT1 and lead to metabolic defects in both the mitochondria and cytosol, which can account for the phenotypic pleiotropy.

Published

2014

17. Sideroblastic anemia: diagnosis and management.

Author

Bottomley SS and Fleming MD

Subjects

Anemia, Sideroblastic complications, Disease Management, Humans, Iron Overload etiology, Anemia, Sideroblastic diagnosis, Anemia, Sideroblastic therapy

Abstract

Sideroblastic anemias (SAs) may be acquired or congenital and share the features of disrupted utilization of iron in the erythroblast, ineffective erythropoiesis, and variable systemic iron overload. Congenital forms can have associated syndromic features or be nonsyndromic, and many of them have mutations in genes encoding proteins involved in heme biosynthesis, iron-sulfur cluster biogenesis, or mitochondrial protein synthesis. The mechanism(s) for the acquired clonal SA is undefined and is under intense study. Precise diagnosis of these disorders rests on careful clinical and laboratory evaluation, including molecular analysis. Supportive treatments usually provide for a favorable prognosis and often for normal survival., (Copyright © 2014 Elsevier Inc. All rights reserved.)

Published

2014

18. X-linked sideroblastic anemia due to ALAS2 intron 1 enhancer element GATA-binding site mutations.

Author

Campagna DR, de Bie CI, Schmitz-Abe K, Sweeney M, Sendamarai AK, Schmidt PJ, Heeney MM, Yntema HG, Kannengiesser C, Grandchamp B, Niemeyer CM, Knoers NV, Swart S, Marron G, van Wijk R, Raymakers RA, May A, Markianos K, Bottomley SS, Swinkels DW, and Fleming MD

Subjects

Adult, Aged, Anemia, Sideroblastic blood, Binding Sites, Europe ethnology, Female, Genetic Diseases, X-Linked blood, Genotype, Humans, Male, Middle Aged, Pedigree, Young Adult, 5-Aminolevulinate Synthetase genetics, Anemia, Sideroblastic genetics, Enhancer Elements, Genetic genetics, GATA Transcription Factors metabolism, Genetic Diseases, X-Linked genetics, Introns genetics, Mutation

Abstract

X-linked sideroblastic anemia (XLSA) is the most common form of congenital sideroblastic anemia. In affected males, it is uniformly associated with partial loss-of-function missense mutations in the erythroid-specific heme biosynthesis protein 5-aminolevulinate synthase 2 (ALAS2). Here, we report five families with XLSA owing to mutations in a GATA transcription factor binding site located in a transcriptional enhancer element in intron 1 of the ALAS2 gene. As such, this study defines a new class of mutations that should be evaluated in patients undergoing genetic testing for a suspected diagnosis of XLSA., (Copyright © 2013 Wiley Periodicals, Inc.)

Published

2014

19. A novel syndrome of congenital sideroblastic anemia, B-cell immunodeficiency, periodic fevers, and developmental delay (SIFD).

Author

Wiseman DH, May A, Jolles S, Connor P, Powell C, Heeney MM, Giardina PJ, Klaassen RJ, Chakraborty P, Geraghty MT, Major-Cook N, Kannengiesser C, Thuret I, Thompson AA, Marques L, Hughes S, Bonney DK, Bottomley SS, Fleming MD, and Wynn RF

Subjects

Anemia, Sideroblastic blood, Anemia, Sideroblastic genetics, Developmental Disabilities blood, Developmental Disabilities genetics, Familial Mediterranean Fever blood, Familial Mediterranean Fever genetics, Female, Hearing Loss, Sensorineural blood, Hearing Loss, Sensorineural diagnosis, Hearing Loss, Sensorineural genetics, Humans, Immunologic Deficiency Syndromes blood, Immunologic Deficiency Syndromes genetics, Infant, Infant, Newborn, Male, Nervous System Diseases blood, Nervous System Diseases diagnosis, Nervous System Diseases genetics, Pedigree, Phenotype, Syndrome, Anemia, Sideroblastic diagnosis, B-Lymphocytes immunology, Developmental Disabilities diagnosis, Familial Mediterranean Fever diagnosis, Immunologic Deficiency Syndromes diagnosis

Abstract

Congenital sideroblastic anemias (CSAs) are a heterogeneous group of inherited disorders identified by pathological erythroid precursors with perinuclear mitochondrial iron deposition in bone marrow. An international collaborative group of physicians and laboratory scientists collated clinical information on cases of CSA lacking known causative mutations, identifying a clinical subgroup of CSA associated with B immunodeficiency, periodic fevers, and development delay. Twelve cases from 10 families were identified. Median age at presentation was 2 months. Anemia at diagnosis was sideroblastic, typically severe (median hemoglobin, 7.1 g/dL) and markedly microcytic (median mean corpuscular volume, 62.0 fL). Clinical course involved recurrent febrile illness and gastrointestinal disturbance, lacking an infective cause. Investigation revealed B-cell lymphopenia (CD19⁺ range, 0.016-0.22 × 10⁹/L) and panhypogammaglobulinemia in most cases. Children displayed developmental delay alongside variable neurodegeneration, seizures, cerebellar abnormalities, sensorineural deafness, and other multisystem features. Most required regular blood transfusion, iron chelation, and intravenous immunoglobulin replacement. Median survival was 48 months, with 7 deaths caused by cardiac or multiorgan failure. One child underwent bone marrow transplantation aged 9 months, with apparent cure of the hematologic and immunologic manifestations. We describe and define a novel CSA and B-cell immunodeficiency syndrome with additional features resembling a mitochondrial cytopathy. The molecular etiology is under investigation.

Published

2013

20. Sideroblastic anemia, iron overload, and ALAS2 R452S in African-American males: phenotype and genotype features of five unrelated patients.

Author

Lee PL, Reid TJ 3rd, Bottomley SS, and Barton JC

Subjects

Adult, Black or African American, Anemia, Sideroblastic ethnology, Child, Genetic Association Studies, Genetic Diseases, X-Linked, Humans, Male, Middle Aged, Polymorphism, Single Nucleotide, Severity of Illness Index, United States, 5-Aminolevulinate Synthetase genetics, Amino Acid Substitution, Anemia, Sideroblastic genetics, Iron Overload genetics

Published

2011

21. Systematic molecular genetic analysis of congenital sideroblastic anemia: evidence for genetic heterogeneity and identification of novel mutations.

Author

Bergmann AK, Campagna DR, McLoughlin EM, Agarwal S, Fleming MD, Bottomley SS, and Neufeld EJ

Subjects

5-Aminolevulinate Synthetase genetics, ATP-Binding Cassette Transporters genetics, Adolescent, Adult, Anemia, Sideroblastic congenital, Child, Child, Preschool, Female, Glutaredoxins genetics, Humans, Hydro-Lyases genetics, Infant, Male, Membrane Transport Proteins genetics, Middle Aged, Mitochondrial Membrane Transport Proteins genetics, United States epidemiology, Anemia, Sideroblastic epidemiology, Anemia, Sideroblastic genetics, Genetic Heterogeneity, Mutation

Abstract

Background: Sideroblastic anemias are heterogeneous congenital and acquired bone marrow disorders characterized by pathologic iron deposits in mitochondria of erythroid precursors. Among the congenital sideroblastic anemias (CSAs), the most common form is X-linked sideroblastic anemia, due to mutations in 5-aminolevulinate synthase (ALAS2). A novel autosomal recessive CSA, caused by mutations in the erythroid specific mitochondrial transporter SLC25A38, was recently defined. Other known etiologies include mutations in genes encoding the thiamine transporter SLC19A2, the RNA-modifying enzyme pseudouridine synthase 1 (PUS1), a mitochondrial ATP-binding cassette transporter (ABCB7), glutaredoxin 5 (GLRX5), as well as mitochondrial DNA deletions. Despite these known diverse causes, in a substantial portion of CSA cases a presumed genetic defect remains unknown., Procedure: In the context of the recent discovery of SLC25A38 as a major novel cause, we systematically analyzed a large cohort of previously unreported CSA patients. Sixty CSA probands (28 females, 32 males) were examined for ALAS2, SLC25A38, PUS1, GLRX5, and ABCB7 mutations. SLC19A2 and mitochondrial DNA were only analyzed if characteristic syndromic features were apparent., Results: Twelve probands had biallelic mutations in SLC25A38. Seven ALAS2 mutations were detected in eight sporadic CSA cases, two being novel. We also identified a novel homozygous null PUS1 mutation and novel mitochondrial DNA deletions in two patients with Pearson syndrome. No mutations were encountered in GLRX5, ABCB7, or SLC19A2., Conclusions: The remaining undefined probands (43%) can be grouped according to gender, family, and clinical characteristics, suggesting novel X-linked and autosomal recessive forms of CSA., ((c) 2009 Wiley-Liss, Inc.)

Published

2010

22. Mutations in mitochondrial carrier family gene SLC25A38 cause nonsyndromic autosomal recessive congenital sideroblastic anemia.

Author

Guernsey DL, Jiang H, Campagna DR, Evans SC, Ferguson M, Kellogg MD, Lachance M, Matsuoka M, Nightingale M, Rideout A, Saint-Amant L, Schmidt PJ, Orr A, Bottomley SS, Fleming MD, Ludman M, Dyack S, Fernandez CV, and Samuels ME

Subjects

Animals, Carrier State, Family, Fishes genetics, Heme biosynthesis, Humans, Phenotype, Yeasts genetics, Anemia, Sideroblastic genetics, Mitochondrial Membrane Transport Proteins genetics, Mutation

Abstract

The sideroblastic anemias are a heterogeneous group of congenital and acquired hematological disorders whose morphological hallmark is the presence of ringed sideroblasts--bone marrow erythroid precursors containing pathologic iron deposits within mitochondria. Here, by positional cloning, we define a previously unknown form of autosomal recessive nonsyndromic congenital sideroblastic anemia, associated with mutations in the gene encoding the erythroid specific mitochondrial carrier family protein SLC25A38, and demonstrate that SLC25A38 is important for the biosynthesis of heme in eukaryotes.

Published

2009

23. Copper deficiency after gastric surgery: a reason for caution.

Author

Prodan CI, Bottomley SS, Vincent AS, Cowan LD, Greenwood-Van Meerveld B, Holland NR, and Lind SE

Subjects

Adult, Aged, Aged, 80 and over, Ceruloplasmin metabolism, Copper administration & dosage, Dietary Supplements, Humans, Male, Middle Aged, Vitamin B 12 Deficiency blood, Copper deficiency, Gastrectomy adverse effects, Postoperative Complications blood

Abstract

Background: : Acquired copper deficiency in adults leads to hematological and neurological manifestations that mimic vitamin B12 deficiency. A significant number of patients with copper deficiency syndrome have a history of gastric surgery, often remote. We sought to determine whether copper deficiency is present in a population of individuals with longstanding partial gastric resection., Methods: : Serum copper, ceruloplasmin, and zinc levels were determined in 20 patients with a history of partial gastric resection and 50 controls, randomly selected from the Oklahoma City Veterans Affairs Medical Center electronic database., Results: : Hypocupremia and symptoms of copper deficiency were detected in patients with partial gastric resection in contrast to controls (3/20 versus 0/50, P = 0.02). Serum copper and ceruloplasmin levels were significantly lower in individuals with partial gastric resection than in controls (P = 0.04 and P = 0.001, respectively). The mean interval between gastric surgery and testing was 20.7 years., Conclusions: : Our results indicate that a significant number of individuals with longstanding history of partial gastric resection have undiagnosed hypocupremia. Screening for copper deficiency after gastric surgery may prevent the development of hematological and neurological complications in these patients.

Published

2009

24. Purification and characterization of sideroblasts from patients with acquired and hereditary sideroblastic anaemia.

Author

Martin FM, Prchal J, Nieva J, Saven A, Andrey J, Bethel K, Barton JC, Aripally G, Bottomley SS, and Friedman JS

Subjects

Aged, Aged, 80 and over, Bone Marrow Cells pathology, Cell Separation methods, Female, Humans, Male, Anemia, Sideroblastic pathology, Erythroblasts pathology

Published

2008

25. Analysis of mitochondrial DNA in 104 patients with myelodysplastic syndromes.

Author

Wulfert M, Küpper AC, Tapprich C, Bottomley SS, Bowen D, Germing U, Haas R, and Gattermann N

Subjects

Adult, Age Factors, Aged, Aged, 80 and over, Bone Marrow pathology, Chromatography, High Pressure Liquid methods, DNA Mutational Analysis, Disease Progression, Humans, Middle Aged, Mutation, Polymerase Chain Reaction methods, Sensitivity and Specificity, DNA, Mitochondrial genetics, Myelodysplastic Syndromes genetics

Abstract

Objective: To determine the frequency and spectrum of somatic mutations of mitochondrial DNA (mtDNA) in bone marrow of patients with myelodysplastic syndrome (MDS)., Materials and Methods: Analysis included 104 patients with MDS (24 refractory anemia, 32 refractory anemia with ringed sideroblasts, 34 refractory anemia with excess of blasts, 7 refractory anemia with excess of blasts in transformation to acute leukemia, and 7 chronic myelo-monocytic leukemia), 3 patients with acute myeloid leukemia from MDS, and 36 patients with myeloproliferative disease (23 chronic myeloid leukemia, 9 polycythemia vera, 4 idiopathic myelofibrosis). Mutation scanning was performed using heteroduplex analysis with denaturing high-performance liquid chromatography (dHPLC). The entire mitochondrial genome was amplified in 67 overlapping polymerase chain reaction fragments carefully optimized regarding DNA melting profiles. Abnormal dHPLC findings were confirmed by DNA sequencing., Results: Heteroplasmic mtDNA mutations, mostly transitions, were identified in 56% of MDS and 44% of myeloproliferative disorders patients. In MDS, mutation frequency increased with age and more-advanced disease. Mutational spectra showed no hot spots and were similar in different types of MDS. Heteroplasmic mutations generally did not represent known polymorphisms, and about half of them affected conserved amino acids or nucleotides. Mutations were less frequent in protein encoding genes (50 per 10(6) base pairs) than other mitochondrial genes (transfer RNAs, ribosomal RNAs, and control region; about 80 per 10(6) base pairs)., Conclusions: As mitochondria often show ultrastructural abnormalities in MDS, including pathological iron accumulation, mitochondrial dysfunction may contribute to MDS pathology. We found a high frequency of acquired mtDNA mutations in MDS. However, their functional importance remains unclear, considering that genotype correlates poorly with phenotype in mitochondrial diseases. The clonally expanded mtDNA mutations in MDS support the concept of age-related damage to mtDNA in hematopoietic stem cells.

Published

2008

26. A confusing case of confusion. Acute porphyrias.

Author

Jackson R, Toubia N, Dhaliwal G, Bottomley SS, and Bronze MS

Subjects

Acidosis, Lactic etiology, Acute Disease, Anticonvulsants administration & dosage, Brain diagnostic imaging, Brain pathology, Diagnosis, Differential, Diet, Reducing, Drug Combinations, Electroencephalography, Epilepsy, Tonic-Clonic cerebrospinal fluid, Epilepsy, Tonic-Clonic drug therapy, Epilepsy, Tonic-Clonic etiology, Estrogens, Conjugated (USP), Fatal Outcome, Female, Headache etiology, Hormone Replacement Therapy, Humans, Magnetic Resonance Imaging, Medroxyprogesterone Acetate, Middle Aged, Phenobarbital administration & dosage, Phenytoin administration & dosage, Porphyrias complications, Porphyrias urine, Spinal Puncture, Tomography, X-Ray Computed, Valproic Acid administration & dosage, Vomiting etiology, Weight Loss, Confusion etiology, Porphyrias diagnosis

Published

2008

27. Hypocupremia associated with prior vitamin B12 deficiency.

Author

Prodan CI, Bottomley SS, Vincent AS, Cowan LD, Holland NR, and Lind SE

Subjects

Aged, Aged, 80 and over, Case-Control Studies, Female, Humans, Male, Middle Aged, Neurodegenerative Diseases etiology, Pilot Projects, Vitamin B 12 blood, Ceruloplasmin analysis, Copper deficiency, Neurodegenerative Diseases blood, Vitamin B 12 Deficiency blood, Vitamin B 12 Deficiency complications

Abstract

Clinical similarities between vitamin B(12) and copper deficiencies prompted us to investigate if hypocupremia is present in patients receiving vitamin B(12) supplementation. Our pilot study results indicate that a significant number of elderly patients with prior diagnosis of vitamin B(12) deficiency have also undiagnosed hypocupremia.

Published

2007

28. Iron overload and prolonged ingestion of iron supplements: clinical features and mutation analysis of hemochromatosis-associated genes in four cases.

Author

Barton JC, Lee PL, West C, and Bottomley SS

Subjects

Adult, Aged, Drug Administration Schedule, Female, Genotype, Hemochromatosis diagnosis, Hemochromatosis Protein, Humans, Iron administration & dosage, Iron Overload chemically induced, Iron Overload genetics, Male, Mutation, Dietary Supplements adverse effects, Hemochromatosis chemically induced, Hemochromatosis genetics, Histocompatibility Antigens Class I genetics, Iron adverse effects, Iron Overload diagnosis, Membrane Proteins genetics

Abstract

We evaluated and treated four white adults (one man, three women) who had iron overload associated with daily ingestion of iron supplements for 7, 15, 35, and 61 years, respectively. We performed HFE mutation analysis to detect C282Y, H63D, and S65C in each patient; in two patients, HFE exons were sequenced. In two patients, direct sequencing was performed to detect coding region mutations of TFR2, HAMP, FPN1, HJV, and ALAS2. Patients 1-4 ingested 153, 547, 1,341, and 4,898 g of inorganic iron as supplements. Patient 1 had hemochromatosis, HFE C282Y homozygosity, and beta-thalassemia minor. Patient 2 had spherocytosis and no HFE coding region mutations. Patient 3 had no anemia, a normal HFE genotype, and no coding region mutations in HAMP, FPN1, HJV, or ALAS2; she was heterozygous for the TFR2 coding region mutation V583I (nt 1,747 G-->A, exon 15). Patient 4 had no anemia and no coding region mutations in HFE, TFR2, HAMP, FPN1, HJV, or ALAS2. Iron removed by phlebotomy was 32.4, 10.4, 15.2, and 4.0 g, respectively. There was a positive correlation of log(10) serum ferritin and the quantity of iron removed by phlebotomy (P = 0.0371). Estimated absorption of iron from supplements in patients 1-4 was 20.9%, 1.9%, 1.1%, and 0.08%. We conclude that the clinical phenotypes and hemochromatosis genotypes of adults who develop iron overload after ingesting iron supplements over long periods are heterogeneous. Therapeutic phlebotomy is feasible and effective, and would prevent complications of iron overload.

Published

2006

29. Relapsing hypocupraemic myelopathy requiring high-dose oral copper replacement.

Author

Prodan CI, Bottomley SS, Holland NR, and Lind SE

Subjects

Deficiency Diseases complications, Female, Humans, Middle Aged, Treatment Outcome, Copper deficiency, Copper therapeutic use, Spinal Cord Diseases drug therapy, Spinal Cord Diseases etiology

Abstract

Adult-onset copper deficiency with neurological manifestations is a newly recognised syndrome. Long-term oral copper replacement therapy has been the mainstay of treatment in the literature. A case of relapsing hypocupraemic myelopathy responsive to increased doses of copper replacement is reported. Standard doses of copper may not be sufficient for all patients.

Published

2006

30. X-linked sideroblastic anemia associated with a novel ALAS2 mutation and unfortunate skewed X-chromosome inactivation patterns.

Author

Aivado M, Gattermann N, Rong A, Giagounidis AA, Prall WC, Czibere A, Hildebrandt B, Haas R, and Bottomley SS

Subjects

Adolescent, Adult, Age Factors, Anemia, Sideroblastic diagnosis, Diagnosis, Differential, Erythroid Precursor Cells, Family Health, Female, Humans, Inheritance Patterns, 5-Aminolevulinate Synthetase genetics, Anemia, Sideroblastic genetics, Genetic Diseases, X-Linked, Mutation, X Chromosome Inactivation

Abstract

Historically X-linked sideroblastic anemia, with rare exceptions, was thought to be manifested only in males. Since the discovery of the erythroid-specific isoform of 5-aminolevulinate synthase (ALAS2) and the cloning of its gene (ALAS2) 15 years ago, mutation analysis has revealed that clinical expression of this X-linked disorder is prevalent in females as well. However, presence of the disease in both genders within affected kindreds appears to be very uncommon. We report a unique family with the disorder in three women who have had widely disparate clinical courses. The anemia is associated with a previously unrecognized ALAS2 mutation (Arg436Trp) and is unresponsive to pyridoxine. To clarify the varied clinical courses of the patients, X-chromosome inactivation patterns were examined in hematopoietic and non-hematopoietic cells. We observed inactivation patterns supporting the conclusions that one daughter has a mild phenotype at age 31 because of moderate constitutive skewed X-chromosome inactivation, another daughter with clinical onset at age 16 is severely affected due to extreme constitutive X-skewing, whereas the mother developed progressive anemia in the fifth decade as she acquired an age-related non-random X-inactivation in hematopoietic cells. In addition, we observed random X-inactivation in reticulocytes of all three women that contrasted with a markedly skewed inactivation pattern in bone marrow erythroid cells. This discordance is attributable to apoptosis of erythroid precursors derived from progenitor cells with an active X-chromosome bearing the ALAS2 mutation. The features of the disorder in this family are also instructive in regard to the differential diagnosis of sideroblastic anemias in women.

Published

2006

31. Congenital sideroblastic anemias.

Author

Bottomley SS

Subjects

Anemia, Sideroblastic classification, Anemia, Sideroblastic diagnosis, Anemia, Sideroblastic etiology, Humans, Iron Overload, Mitochondria metabolism, Splenectomy, Anemia, Sideroblastic congenital

Abstract

Congenital forms of sideroblastic anemia constitute a subset of uncommon disorders within the wider spectrum of sideroblastic anemias, all of which are diagnosed by the presence of pathologic iron deposits in erythroblast mitochondria. The congenital sideroblastic anemias are heterogeneous disorders; some arise from known molecular defects but others are diagnosed only by their clinical features. Elucidation of several of the underlying defects has advanced our understanding of heme biosynthesis and iron metabolism in the erythroid cell. With the details of the porphyrin synthetic pathway clarified, now the important frontier of research is investigation of the mechanisms of mitochondrial and cellular iron homeostasis and their relationship to the regulation of heme biosynthesis. Knowledge gained from efforts in this area of study may also provide new approaches to treatments, which remain largely supportive for most types of congenital sideroblastic anemia.

Published

2006

32. Myelopathy due to copper deficiency.

Author

Prodan CI, Holland NR, Wisdom PJ, and Bottomley SS

Subjects

Adult, Anemia blood, Anemia drug therapy, Copper blood, Copper therapeutic use, Female, Humans, Middle Aged, Neutropenia blood, Neutropenia drug therapy, Polyneuropathies blood, Polyneuropathies etiology, Spinal Cord Diseases blood, Zinc blood, Copper deficiency, Spinal Cord Diseases etiology

Published

2004

33. The major splice variant of human 5-aminolevulinate synthase-2 contributes significantly to erythroid heme biosynthesis.

Author

Cox TC, Sadlon TJ, Schwarz QP, Matthews CS, Wise PD, Cox LL, Bottomley SS, and May BK

Subjects

Alternative Splicing, Amino Acid Sequence, Animals, Base Sequence, COS Cells, Catalysis, Codon, Electrophoresis, Polyacrylamide Gel, Exons, Genetic Vectors, Green Fluorescent Proteins, Hemoglobins chemistry, Humans, Luminescent Proteins metabolism, Microscopy, Fluorescence, Mitochondria metabolism, Molecular Sequence Data, Polymerase Chain Reaction, Protein Isoforms, Protein Structure, Tertiary, RNA, Messenger metabolism, Reticulocytes metabolism, Ribonucleases metabolism, Subcellular Fractions metabolism, Succinate-CoA Ligases chemistry, Two-Hybrid System Techniques, 5-Aminolevulinate Synthetase biosynthesis, 5-Aminolevulinate Synthetase genetics, Erythrocytes metabolism, Heme biosynthesis

Abstract

The initial step of the heme biosynthetic pathway in erythroid cells is catalyzed by an erythroid-specific isoform of 5-aminolevulinate synthase-2 (ALAS2). Previously, an alternatively spliced mRNA isoform of ALAS2 was identified although the functional significance of the encoded protein was unknown. We sought to characterize the contribution of this ALAS2 isoform to overall erythroid heme biosynthesis. Here, we report the identification of three novel ALAS2 mRNA splice isoforms in addition to the previously described isoform lacking exon 4-derived sequence. Quantitation of these mRNAs using ribonuclease protection experiments revealed that the isoform without exon 4-derived sequence represents approximately 35-45% of total ALAS2 mRNA while the newly identified transcripts together represent approximately 15%. Despite the significant amounts of these three new transcripts, their features indicate that they are unlikely to substantially contribute to overall mitochondrial ALAS2 activity. In contrast, in vitro studies show that the major splice variant (lacking exon 4-encoded sequence) produces a functional enzyme, albeit with slightly reduced activity and with affinity for the ATP-specific, beta subunit of succinyl CoA synthase, comparable to that of mature ALAS2. It was also established that the first 49 amino acids of the ALAS2 pre-protein are necessary and sufficient for translocation across the mitochondrial inner membrane and that this process is not affected by the absence of exon 4-encoded sequence. We conclude that the major splice isoform of ALAS2 is functional in vivo and could significantly contribute to erythroid heme biosynthesis and hemoglobin formation.

Published

2004

34. 5-Aminolevulinic acid synthase: mechanism, mutations and medicine.

Author

Shoolingin-Jordan PM, Al-Daihan S, Alexeev D, Baxter RL, Bottomley SS, Kahari ID, Roy I, Sarwar M, Sawyer L, and Wang SF

Subjects

5-Aminolevulinate Synthetase chemistry, 5-Aminolevulinate Synthetase genetics, Erythroid Precursor Cells enzymology, Humans, Models, Molecular, Mutation, Rhodobacter sphaeroides enzymology, Structure-Activity Relationship, Substrate Specificity, 5-Aminolevulinate Synthetase metabolism

Abstract

5-Aminolevulinic acid synthase (ALAS), the first enzyme of the heme biosynthesis pathway, catalyses the pyridoxal 5'-phosphate-dependent condensation between glycine and succinyl-CoA to yield 5-aminolevulinic acid (5-amino-4-oxopentanoate). A three-dimensional structural model of Rhodobacter spheroides ALAS has been constructed and used to identify amino acid residues at the active site that are likely to be important for the recognition of glycine, the only amino acid substrate. Several residues have been investigated by site-directed mutagenesis and enzyme variants have been generated that are able to use alanine, serine or threonine. A three-dimensional structure model of 5-aminolevulinic acid synthase from human erythrocytes (ALAS 2) has also been constructed and used to map a range of naturally occurring human mutants that give rise to X-linked sideroblastic anemia. A number of these anemias respond favourably to vitamin B(6) (pyridoxine) therapy, whereas others are either partially responsive or completely refractory. Detailed investigations with selected human mutants have highlighted the importance of arginine-517 that is implicated in glycine carboxyl group binding.

Published

2003

35. CNS demyelination associated with copper deficiency and hyperzincemia.

Author

Prodan CI, Holland NR, Wisdom PJ, Burstein SA, and Bottomley SS

Subjects

Brain pathology, Demyelinating Diseases pathology, Female, Humans, Magnetic Resonance Imaging, Male, Middle Aged, Copper deficiency, Demyelinating Diseases blood, Demyelinating Diseases etiology, Zinc blood

Abstract

CNS demyelination is not a previously reported feature of acquired copper deficiency. The authors report two patients with idiopathic hypocupremia and hyperzincemia, hematologic changes of copper deficiency, and extensive CNS demyelination. Hematologic recovery followed copper supplementation, both initially and after relapse off copper therapy, while serum zinc levels remained high and the neurologic abnormalities only stabilized.

Published

2002

36. Iron deficiency due to excessive therapeutic phlebotomy in hemochromatosis.

Author

Barton JC and Bottomley SS

Subjects

Adult, Aged, Erythrocyte Indices, Female, Humans, Male, Middle Aged, Anemia, Iron-Deficiency etiology, Hemochromatosis therapy, Phlebotomy

Abstract

Thirteen adults (eight men, five women) with hemochromatosis had undergone routine iron depletion therapy but while on maintenance phlebotomies developed iron deficiency which persisted for 25 +/- 13 (mean +/- 1 SD) months before diagnosis. All had symptoms and signs of iron deficiency. Levels of transferrin saturation were 10% +/- 5% (1 SD), and serum ferritin concentrations were 8 +/- 3 ng/mL. Eleven had anemia; eight had hypochromia and microcytosis. Bone marrow specimens obtained in five patients revealed no stainable iron. Medical records indicated that parameters of body iron status were infrequently or incorrectly used for adjusting the frequency of phlebotomies. Two patients developed iron deficiency due to additional blood loss from esophageal varices and bilateral hip replacement, respectively. Ten of the patients were treated with ferrous sulfate, 325 mg daily, for 2-6 weeks when anemia was corrected. In patients who were not given iron, anemia and microcytosis recovered in 8-24 months. We conclude that (i) sustained iron deficiency in hemochromatosis patients should be prevented by monitoring hemoglobin levels and serum ferritin; and (ii) hemoglobin concentrations and values of mean corpuscular hemoglobin may be higher in iron-deficient persons with hemochromatosis than in individuals without hemochromatosis. Symptomatic iron deficiency in hemochromatosis patients may be treated safely with a brief course of ferrous sulfate. Recovery is slower when iron is not given. However, iron supplementation is unnecessary and not recommended for the mild, self-limited anemia and decreased serum iron and ferritin concentrations encountered after initial iron depletion therapy for hemochromatosis.

Published

2000

37. Acute intermittent porphyria: novel missense mutations in the human hydroxymethylbilane synthase gene.

Author

Ramdall RB, Cunha L, Astrin KH, Katz DR, Anderson KE, Glucksman M, Bottomley SS, and Desnick RJ

Subjects

Female, Gene Expression, Heme biosynthesis, Heme genetics, Humans, Hydroxymethylbilane Synthase metabolism, Male, Porphyria, Acute Intermittent enzymology, Amino Acid Substitution, Hydroxymethylbilane Synthase genetics, Mutation, Missense, Porphyria, Acute Intermittent genetics

Abstract

Purpose: To identify mutations in families with acute intermittent porphyria, an autosomal dominant inborn error of metabolism that results from the half-normal activity of the third enzyme in the heme biosynthetic pathway, hydroxymethylbilane synthase., Methods: Mutations were identified by direct solid phase sequencing., Results: Two novel missense mutations E80G and T78P and three previously reported mutations, R173W, G111R, and the splice site lesion, IVS1+1, were detected, each in an unrelated proband. The causality of the novel missense mutations was demonstrated by expression studies., Conclusion: These findings provide for the precise diagnosis of carriers in these families and further expand the molecular heterogeneity of AIP.

Published

2000

38. Secondary iron overload disorders.

Author

Bottomley SS

Subjects

Humans, Iron Overload etiology

Abstract

Diverse clinical disorders distinct from hereditary hemochromatosis are associated with accumulation of excess body iron in heterogeneous patterns and through various mechanisms. A deranged iron turnover somehow relates to the altered physiological barrier for iron absorption in several defined chronic anemias with ineffective erythropoiesis. Unexcretable excess iron acquired from transfusions provides a therapeutic challenge. Genetic defects of proteins essential for transport of iron into and out of cells (transferrin and ceruloplasmin) deprive the erythron of the metal and cause its accumulation in other vital organs. The hemochromatosis alleles predictably contribute to an iron burden from other causes, commonly facilitate the expression of porphyria cutanea tarda, and their clinical expression may be accelerated by hereditary hemolytic anemias. Even minimal iron excess in liver disease may contribute to the hepatocellular injury from factors such as alcohol and viruses. Uniquely localized siderosis occurs in the lung and kidney where iron cannot turn over and causes variable tissue damage. The most devastating iron overload disorder, neonatal hemochromatosis, is understood least of all.

Published

1998

39. Molecular defects of erythroid 5-aminolevulinate synthase in X-linked sideroblastic anemia.

Author

Bottomley SS, May BK, Cox TC, Cotter PD, and Bishop DF

Subjects

5-Aminolevulinate Synthetase blood, Amino Acid Sequence, Anemia, Sideroblastic diagnosis, Erythropoiesis, Genetic Linkage, Hemoglobins biosynthesis, Humans, Isoenzymes blood, Molecular Sequence Data, Point Mutation, Polymorphism, Genetic, X Chromosome, 5-Aminolevulinate Synthetase genetics, Anemia, Sideroblastic enzymology, Anemia, Sideroblastic genetics, Erythrocytes enzymology, Isoenzymes genetics

Abstract

The erythroid-specific isozyme of 5-aminolevulinate synthase (ALAS2), the first and rate-limiting enzyme of heme biosynthesis, is expressed concomitantly with the differentiation and maturation of the erythroid cell in order to accommodate generation of the large amounts of heme required for hemoglobin production. During the past few years the ALAS2 gene and its transcript have been characterized and the amino acid sequence of the enzyme deduced. The human genetic disorder X-linked sideroblastic anemia, previously postulated to be caused by defects of ALAS, has now been analyzed at the molecular and tissue-specific level. A heterogeneous group of point mutations in the catalytic domain of the ALAS2 enzyme has been found to cause the disorder. Impaired activity of recombinant mutant ALAS2 enzymes has also been demonstrated. Characterization of molecular defects in individuals with X-linked sideroblastic anemia has provided improved diagnosis for at-risk family members.

Published

1995

40. Molecular regulation of heme biosynthesis in higher vertebrates.

Author

May BK, Dogra SC, Sadlon TJ, Bhasker CR, Cox TC, and Bottomley SS

Subjects

5-Aminolevulinate Synthetase genetics, 5-Aminolevulinate Synthetase metabolism, Amino Acid Sequence, Anemia, Sideroblastic genetics, Anemia, Sideroblastic metabolism, Animals, Cytochrome P-450 Enzyme System biosynthesis, Erythrocytes enzymology, Erythropoiesis, Heme Oxygenase (Decyclizing) metabolism, Humans, Liver enzymology, Molecular Sequence Data, Porphyrias genetics, Porphyrias metabolism, Sequence Homology, Amino Acid, Transcription, Genetic, Vertebrates, 5-Aminolevulinate Synthetase biosynthesis, Gene Expression Regulation, Heme biosynthesis

Published

1995

41. X-linked pyridoxine-responsive sideroblastic anemia due to a Thr388-to-Ser substitution in erythroid 5-aminolevulinate synthase.

Author

Cox TC, Bottomley SS, Wiley JS, Bawden MJ, Matthews CS, and May BK

Subjects

Aged, Amino Acid Sequence, Anemia, Sideroblastic drug therapy, Anemia, Sideroblastic enzymology, Base Sequence, DNA, Complementary, Erythroblasts enzymology, Female, Genetic Linkage, Humans, Male, Molecular Sequence Data, Pedigree, Point Mutation, Pyridoxine therapeutic use, 5-Aminolevulinate Synthetase genetics, Anemia, Sideroblastic genetics, Isoenzymes genetics, X Chromosome

Abstract

Background: X-linked sideroblastic anemia is usually associated with reduced 5-aminolevulinate synthase activity in erythroid cells, and some cases are responsive to treatment with pyridoxine, the precursor to the cofactor of the enzyme. The recently identified gene for an erythroid-specific 5-aminolevulinate synthase isoenzyme and its localization to the X chromosome make it likely that one or more defects in this gene underlie the anemia., Methods: Using a polymorphic dinucleotide-repeat sequence in the erythroid 5-aminolevulinate synthase gene, we confirmed the linkage of this gene to the disorder in a family with X-linked pyridoxine-responsive sideroblastic anemia. We therefore sought evidence of a nucleotide-sequence abnormality in the erythroid 5-aminolevulinate synthase gene by analyzing enzymatically amplified DNA., Results: DNA-sequencing studies in two affected males and one carrier female in the kindred demonstrated a cytosine-to-guanine change at nucleotide 1215 (in exon 8). This change results in the substitution of serine for threonine at amino acid residue 388, near the lysine that binds the pyridoxal phosphate cofactor. In expression studies, the activity of the mutant enzyme was reduced relative to that of the wild type, and this reduction was comparable to that in erythroid cells of the proband during relapse of the anemia; the enzyme activity expressed in the presence of pyridoxine was comparable to that in the proband's marrow cells during remission. Although the affinity of the mutant enzyme for pyridoxal phosphate was not altered, the mutation appears to introduce a conformational change at the active site of the enzyme., Conclusions: We identified a point mutation resulting in an amino acid change near the pyridoxal phosphate-binding site of the erythroid 5-aminolevulinate synthase isoenzyme as the underlying defect in a kindred with X-linked pyridoxine-responsive sideroblastic anemia.

Published

1994

42. 5-Aminolevulinate synthase in sideroblastic anemias: mRNA and enzyme activity levels in bone marrow cells.

Author

Bottomley SS, Healy HM, Brandenburg MA, and May BK

Subjects

5-Aminolevulinate Synthetase physiology, Adult, Aged, Anemia, Sideroblastic blood, Anemia, Sideroblastic genetics, Blotting, Northern, Bone Marrow chemistry, DNA analysis, DNA genetics, Female, Genetic Linkage genetics, Globins analysis, Globins genetics, Glycophorins analysis, Glycophorins genetics, Humans, Isoenzymes genetics, Isoenzymes physiology, Male, Middle Aged, RNA, Messenger genetics, X Chromosome, 5-Aminolevulinate Synthetase analysis, 5-Aminolevulinate Synthetase genetics, Anemia, Sideroblastic enzymology, Bone Marrow enzymology, Bone Marrow pathology, Isoenzymes analysis, RNA, Messenger analysis

Abstract

To examine the role of 5-aminolevulinate synthase (ALAS) in the pathogenesis of sideroblastic anemias, levels of mRNAs for erythroid and housekeeping ALAS isozymes were examined, and total ALAS activity was assessed in bone marrow cells. In two patients with X-linked sideroblastic anemia the levels of mRNA for erythroid ALAS as well as for alpha and beta globin appear to be decreased while levels of mRNA for glycophorin A in both patients were the same as in normal individuals. However, amounts of housekeeping ALAS mRNA were increased two- to threefold in these patients. Total ALAS activity was also increased two- or threefold, perhaps reflecting increased transcription of the housekeeping gene in response to diminished cellular heme in erythroid cells and/or enhanced translation of the erythroid isoform in response to iron accumulation. In a third patient with X-linked sideroblastic anemia ALAS activity was low but increased to twice the normal value after pyridoxine administration, suggesting a structural defect of the enzyme. In a fourth patient, with isolated congenital, pyridoxine-responsive sideroblastic anemia, the erythroid ALAS mRNA was normal and a low enzyme activity was strikingly enhanced by pyridoxal-phosphate albeit to subnormal levels. In idiopathic acquired sideroblastic anemia, ALAS mRNA for both isozymes was normal and enzyme activity was slightly elevated. These observations thus reflect heterogeneous aberrations of erythroid heme synthesis in the various types of sideroblastic anemia and suggest that defects involving erythroid ALAS underlie at least some of them.

Published

1992

43. Human erythroid 5-aminolevulinate synthase. Gene structure and species-specific differences in alternative RNA splicing.

Author

Conboy JG, Cox TC, Bottomley SS, Bawden MJ, and May BK

Subjects

Amino Acid Sequence, Base Sequence, Exons, Humans, Introns, Molecular Sequence Data, Polymerase Chain Reaction, RNA, Messenger genetics, RNA, Messenger metabolism, Restriction Mapping, Species Specificity, 5-Aminolevulinate Synthetase genetics, Genes, Isoenzymes genetics, RNA Splicing, Reticulocytes enzymology

Abstract

Erythroid 5-aminolevulinate synthase (ALAS) is expressed exclusively in differentiating erythroid cells as the principal isoform of the enzyme to catalyze the first step of the heme biosynthetic pathway. The human gene encoding this isozyme was isolated from a cosmid library, and its structure was characterized with restriction mapping followed by sequencing of fragments. The gene is 22 kilobases long and has 11 exons. Exon 2 encodes the N-terminal signal sequence required for mitochondrial import, exons 3 and 4 encode a variable portion of the N-terminal end, and exons 5-11 the highly conserved C-terminal portion of the mature protein, respectively. Enzymatic amplification of human reticulocyte RNA using PCR techniques revealed two erythroid ALAS mRNA transcripts predicted to encode both the prototypical 64-kDa isoform as well as a novel smaller isoform with a deletion of 37 amino acids near the N terminus. The two mRNA isoforms are generated by alternative splicing of exon 4 and are expressed in fetal erythroid cells as well as at all stages of erythroid development tested, so that there is no evidence of differentiation-specific regulation of exon 4 splicing. However, striking species-specific differences were observed in that alternative splicing of exon 4 was found in man but not dog or mouse; also, the previously described alternative splicing within exon 3 in mouse was not observed in man. This transcript heterogeneity suggests the existence of erythroid ALAS protein isoforms with potentially distinct functional or regulatory roles. The occurrence of species-specific splicing in the least conserved region of the enzyme may reflect another mechanism of gene evolution in eukaryotes.

Published

1992

44. Sideroblastic anemia: death from iron overload.

Author

Bottomley SS

Subjects

Adult, Anemia, Sideroblastic complications, Anemia, Sideroblastic mortality, Hemochromatosis drug therapy, Humans, Iron administration & dosage, Iron adverse effects, Iron blood, Liver Cirrhosis complications, Liver Cirrhosis pathology, Male, Pyridoxine therapeutic use, Anemia, Sideroblastic genetics

Published

1991

45. Sideroblastic anemia.

Author

Bottomley SS

Subjects

Anemia, Sideroblastic diagnosis, Anemia, Sideroblastic genetics, Anemia, Sideroblastic pathology, Heme biosynthesis, Humans, Iron metabolism, Anemia, Sideroblastic etiology, Iron blood

Published

1991

46. Erythroid 5-aminolevulinate synthase is located on the X chromosome.

Author

Cox TC, Bawden MJ, Abraham NG, Bottomley SS, May BK, Baker E, Chen LZ, and Sutherland GR

Subjects

5-Aminolevulinate Synthetase blood, Anemia, Sideroblastic enzymology, Anemia, Sideroblastic genetics, Animals, Blotting, Southern, Chromosome Banding, Chromosome Mapping, DNA genetics, DNA Probes, Humans, Hybrid Cells, Karyotyping, Mice, Nucleic Acid Hybridization, 5-Aminolevulinate Synthetase genetics, Erythrocytes enzymology, X Chromosome

Abstract

The gene for erythroid 5-aminolevulinate synthase has been mapped to Xpter-Xq26 by Southern blot hybridization analysis of a mouse/human hybrid cell panel. In situ hybridization maps the gene to Xp21-Xq21, with the most likely location being on band Xp11.2. The mapping of the erythroid 5-amino-levulinate synthase gene to the X chromosome suggests that a defect in this gene may be the primary cause of X-linked sideroblastic anemia.

Published

1990

47. Experience with the red cell uroporphyrinogen synthase (URO-S) assay in kindreds with acute intermittent porphyria (AIP).

Author

Kreimer-Birnbaum M, Bonkowsky HL, and Bottomley SS

Subjects

Acute Disease, Clinical Enzyme Tests, Female, Genetic Carrier Screening, Humans, Male, Pedigree, Porphyrias genetics, Sex Factors, Ammonia-Lyases blood, Erythrocytes enzymology, Hydroxymethylbilane Synthase blood, Porphyrias diagnosis

Published

1980

48. Pure red cell aplasia associated with fenoprofen.

Author

Reitz CL and Bottomley SS

Subjects

Aged, Arthritis drug therapy, Fenoprofen administration & dosage, Humans, Male, Anemia, Aplastic chemically induced, Fenoprofen adverse effects, Phenylpropionates adverse effects

Abstract

A 69-year-old man developed pure red cell aplasia after taking fenoprofen for ten months. The erythroid defect fully reversed after the drug was discontinued and could not be attributed to the patient's previously treated lung carcinoma. This case represents the third example of erythroid aplasia associated with an anti-inflammatory agent and the first instance due to fenoprofen.

Published

1984

49. Bone marrow delta-aminolevulinic acid synthetase activity in experimental sideroblastic anemia.

Author

Tanaka M and Bottomley SS

Subjects

Anemia, Sideroblastic blood, Anemia, Sideroblastic chemically induced, Animals, Bone Marrow analysis, Bone Marrow Cells, Cycloserine, Disease Models, Animal, Female, Isoniazid, Pyridoxal Phosphate blood, 5-Aminolevulinate Synthetase metabolism, Anemia, Sideroblastic enzymology, Bone Marrow enzymology

Published

1974

50. Peripheral blood remission of hairy cell leukemia after transfusion hepatitis.

Author

Keefer MJ, Weber MJ, Bottomley SS, Solanki DL, and Hosty TA

Subjects

Aged, Blood Cell Count, Female, Granulocytes cytology, Hepatitis etiology, Hepatitis B transmission, Hepatitis C transmission, Humans, Leukemia, Hairy Cell blood, Leukemia, Hairy Cell complications, Male, Middle Aged, Remission Induction, Splenectomy, Erythrocyte Transfusion, Hepatitis transmission, Leukemia, Hairy Cell therapy, Transfusion Reaction

Abstract

Hairy cell leukemia is a chronic lymphoproliferative disorder characterized clinically by splenomegaly and cytopenias. Spontaneous remissions are rare and splenectomy is often performed when the blood counts worsen and cause symptoms. Three of our patients with hairy cell leukemia developed recurrent pancytopenia and transfusion-dependent anemia after splenectomy. Each subsequently acquired transfusion hepatitis and in two patients marked hematologic improvement was noted within 2 months. Complete peripheral blood remission occurred within 17 months in all patients although bone marrow infiltration with hairy cells persisted. One patient remains in remission for 12 years; the other two succumbed to infectious illnesses but with normal blood counts. The mechanism by which hepatitis virus induces hematologic recovery in patients with hairy cell leukemia is unknown but may involve augmentation of the interferon system.

Published

1987