Your search keyword '"Yingyong Chinthammitr"' showing total 3 results

1. Iron overload in the Asian community

Author

Somdet Srichairatanakool, Alison T. Merryweather-Clarke, Carole McKeown, David J. Weatherall, Chanin Limwongse, Isaac Wilson-Morkeh, William G. Newman, David Oleesky, Nasaim Khan, Vip Viprakasit, Anuja Premawardhena, Phyu Wai, H. Janaka de Silva, John Hudson, Anthony J. Robins, Andrew Chilton, Gurvinder S Banait, Anuradha S Dassanayake, Maurice Jackson, Chun Yu Lok, Kathryn J. H. Robson, Yingyong Chinthammitr, and Rousseau Gama

Subjects

Adult, Male, Asia, Iron Overload, Adolescent, Genotype, Thalassemia, Molecular Sequence Data, Immunology, Ferroportin, Biochemistry, Consanguinity, Young Adult, Asian People, Hepcidins, Hepcidin, medicine, Humans, Amino Acid Sequence, Child, Hemochromatosis Protein, Cation Transport Proteins, Hemochromatosis, Hemojuvelin, Genetics, Sequence Homology, Amino Acid, biology, business.industry, Histocompatibility Antigens Class I, Membrane Proteins, Cell Biology, Hematology, Middle Aged, medicine.disease, Juvenile hemochromatosis, Pedigree, Phenotype, Hereditary hemochromatosis, Mutation, biology.protein, Female, HAMP, business, Antimicrobial Cationic Peptides

Abstract

Hereditary hemochromatosis is an iron overload disorder that can lead to the impairment of multiple organs and is caused by mutations in one or more different genes. Type 1 hemochromatosis is the most common form of the disease and results from mutations in the HFE gene. Juvenile hemochromatosis (JH) is the most severe form, usually caused by mutations in hemojuvelin (HJV) or hepcidin (HAMP). The autosomal dominant form of the disease, type 4, is due to mutations in the SLC40A1 gene, which encodes for ferroportin (FPN). Hereditary hemochromatosis is commonly found in populations of European origin. By contrast, hemochromatosis in Asia is rare and less well understood and can be masked by the presence of iron deficiency and secondary iron overload from thalassemia. Here, we provide a comprehensive report of hemochromatosis in a group of patients of Asian origin. We have identified novel mutations in HJV, HAMP, and SLC40A1 in countries not normally associated with hereditary hemochromatosis (Pakistan, Bangladesh, Sri Lanka, and Thailand). Our family studies show a high degree of consanguinity, highlighting the increased risk of iron overload in many countries of the developing world and in countries in which there are large immigrant populations from these regions.

Published

2009

2. In vitro functional analysis of human ferroportin (FPN) and hemochromatosis-associated FPN mutations

Author

Yingyong Chinthammitr, Hal Drakesmith, Alison T. Merryweather-Clarke, Kathryn J. H. Robson, Jon P. Edwards, Diana Cowley, Emma Sweetland, Vip Viprakasit, Lisa Schimanski, J Bastin, and Alain Townsend

Subjects

Iron, Immunology, Ferroportin, Intracellular Space, medicine.disease_cause, Biochemistry, Cell Line, Antigens, CD, Receptors, Transferrin, medicine, Humans, Cation Transport Proteins, Hemochromatosis, Mutation, biology, Transferrin saturation, Iron Deficiencies, Cell Biology, Hematology, Iron deficiency, medicine.disease, Cell biology, Ferritin, Phenotype, Ferritins, biology.protein, Haploinsufficiency, Intracellular, Protein Binding

Abstract

Type IV hemochromatosis is associated with dominant mutations in the SLC40A1 gene encoding ferroportin (FPN). Known as the “ferroportin disease,” this condition is typically characterized by high serum ferritin, reduced transferrin saturation, and macrophage iron loading. Previously FPN expression in vitro has been shown to cause iron deficiency in human cell lines and mediate iron export from Xenopus oocytes. We confirm these findings by showing that expression of human FPN in a human cell line results in an iron deficiency because of a 3-fold increased export of iron. We show that FPN mutations A77D, V162Δ, and G490D that are associated with a typical pattern of disease in vivo cause a loss of iron export function in vitro but do not physically or functionally impede wild-type FPN. These mutants may, therefore, lead to disease by haploinsufficiency. By contrast the variants Y64N, N144D, N144H, Q248H, and C326Y, which can be associated with greater transferrin saturation and more prominent iron deposition in liver parenchyma in vivo, retained iron export function in vitro. Because FPN is a target for negative feedback in iron homeostasis, we postulate that the latter group of mutants may resist inhibition, resulting in a permanently “turned on” iron exporter.

Published

2005

3. Molecular Diagnosis of the First Ferroportin Mutation (C326Y) in the Far East Causing a Dominant Form of Inherited Iron Overload

Author

Alison T. Merryweather-Clarke, Chanin Limwongse, Kathryn J. H. Robson, Vip Viprakasit, Yingyong Chinthammitr, Lisa Schimanski, Alain Townsend, Somdet Srichairatanakool, and Hal Drakesmith

Subjects

chemistry.chemical_classification, Genetics, Mutation, biology, Immunology, Ferroportin, Transferrin receptor, Cell Biology, Hematology, Compound heterozygosity, medicine.disease, medicine.disease_cause, Biochemistry, Molecular biology, chemistry, Hepcidin, Transferrin, biology.protein, medicine, Hemochromatosis, Hemojuvelin

Abstract

Genetic hemochromatosis (HH) is a common inherited disorder in populations of European origin in which different types of genetic hemochromatosis (type 1–4) have been characterized. Most hemochromatosis-type 1 patients are homozygotes or compound heterozygotes for two HFE mutations C282Y and H63D. Studies of several non-HFE iron overload families led to identification of mutations in hemojuvelin and hepcidin (juvenile form-HFE2A and B), transferrin receptor 2 (HFE3) and ferroportin (HFE4) as a cause of different forms of hemochromatosis. In the Far East, inherited hemochromatosis has rarely been reported and may have been misdiagnosed due to the high prevalence of secondary iron loading from hemoglobin disorders. This report describes, for the first time, non-HFE iron overload in patients from Southeast Asia. The affected Thai family presented with a distinctive clinical phenotype including macrocytosis and elevated transferrin saturation (>95%), increased non-transferrin bound iron (NTBI) as well as raised serum ferritin and marked hepatic hemochromatosis. Our patients tolerated therapeutic phlebotomy well. DNAs from peripheral blood leukocytes were firstly analyzed for three common HFE mutations (C282Y, H63D and IVS5+1 G→A). Subsequently, we screened all coding sequences, promoters and exon/intron boundaries of the HFE, HAMP, TfR2, HJV and SLC40A1 genes using denaturing high performance liquid chromatography (DHPLC). The entire coding region and splice sites of these genes were amplified and directly sequenced. We identified a novel mutation (C326Y) in ferroportin (SLC40A1, IREG-1, MTP-1), a membrane iron transport protein due to a G→A substitution at nucleotide 1281 in exon 7. This mutation was confirmed by restriction fragment length polymorphism (RFLP) analysis using Sfa NI. Six hundred Thai and two hundred Vietnamese chromosomes were analyzed for the C326Y mutation by RFLP analysis and it was not detected in any of the healthy controls studied. This result suggested that the G→A substitution is not a common polymorphism and is likely to be the causative mutation for the phenotype in this family. Previous reported mutations of ferroportin, including A77D and V162del, which lead to type IV hemochromatosis, were characterized by increased serum ferritin despite normal transferrin saturation, in contrast to our patients’ phenotype. These autosomal dominant mutants are postulated to lead to disease due to loss of iron exporting function. Preliminary in vivo assay using transient transfection of wild-type and ferroportin mutants in HeLa or 293T cells revealed, as expected, a loss of function and diminished surface membrane localisation in A77D and V162del mutants. Surprisingly, the C326Y mutant was indistinguishable from wt ferroportin in both iron status of the cell and protein localization suggesting different pathophysiology leading to iron overload in our patients.

Published

2004