<i>HFE</i> gene polymorphism defined by sequence‐based typing of the Brazilian population and a standardized nomenclature for <i>HFE</i> allele sequences

Campos, Wagner Narciso de; Massaro, Juliana Doblas; Martinelli, A.L.C.; Halliwell, Jason A.; Marsh, S. G. E.; Mendes‐Junior, Celso T.; Donadi, Eduardo Antônio

doi:10.1111/tan.13097

Cited by 4 publications

(5 citation statements)

References 16 publications

(34 reference statements)

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“…The results regarding HFE alleles are presented in two forms: (1) as previously reported in the literature, including the single nucleotide polymorphism (SNP) reference number (rs), the usual SNP names (H63DC>G, C282YG>A, IVS2(+4)T>C and IVS4(-44)T>C) and new variation sites (Table 1); and (2) as the newly described official HFE allele nomenclature (Table 2)[10]. The location of the previously reported variation sites with respect to the nucleotide sequence that defined the new HFE nomenclature is illustrated in Figure 1.…”

Section: Resultsmentioning

confidence: 99%

“…The reconstruction of the meiotic phase generated nine alleles, included into four major allele groups ( HFE *001 to *004), as standardized by IMGT[10]. These allele groups encoded four distinct proteins (HFE*001 to *004) on the basis of polymorphic sites along the coding region, encompassing the H63DC>G (exon 2), IVS2(+4)T>C (intron 2), rs807209 (G>C intron 3), C282YG>A (exon 4) IVS4(-44)T>C (intron 4) and the new mutation (G>DEL at intron 5) (Table 2).…”

Section: Resultsmentioning

confidence: 99%

“…HFE nucleotide variations were retrieved from the NCBI (NC_000006.12) and Ensembl (ENSG00000010704) databases. Primer sequences, amplification conditions and allele nomenclature were defined as previously reported[10]. Sequencing was performed using an ABI 3500 sequencer (Applied Biosystems, Foster City, CA).…”

Section: Methodsmentioning

confidence: 99%

“…Structure of the HFE gene (ID# ENSG00000010704 - http://www.ensembl.org) at chromosome region 6p21.3, showing the reference number (rs) of variation sites (NCBI Data base - http://www.ncbi.nlm.nih.gov/snp), previously associated with iron disorders. Shaded grey areas indicate the sequenced gene regions and the respective pairs of primers, as previously described[10]. The combination of these variation sites, translated into the official nomenclature for HFE alleles is also shown in the bottom chart; i.e ., the combination of the triplet bases and respective encoded residues of the two most important mutations (H63DC>G and C282YG>A) that defined the four major HFE allele groups (mutated bases are shown in bold type).…”

Section: Methodsmentioning

confidence: 99%

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Comprehensive analysis ofHFEgene in hereditary hemochromatosis and in diseases associated with acquired iron overload

Campos

Massaro

Cançado

et al. 2019

WJH

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BACKGROUND Patients with hepatitis C virus (HCV) and hepatocellular carcinoma (HCC) may or not develop iron overload (IO), which is associated with worst prognosis, because can cause serious damage to organs. HFE gene controls the iron uptake from gut, particularly in patients with hereditary hemochromatosis (HH). AIM To identify associations between HFE coding region in patients exhibiting hereditary hemochromatosis and in diseases associated with acquired IO. METHODS We sequenced exons 2 to 5 and boundary introns of HFE gene, evaluating all polymorphic sites in patients presenting hereditary (hemochromatosis) or acquired iron overload HCV and HCC) and in healthy controls, using Sanger sequencing. We also determined the ensemble of extended haplotype in healthy control individuals, including several major histocompatibility complex loci, using sequence specific probes. Haplotype reconstruction was performed using the Arlequin and Phase softwares, and linkage disequilibrium (LD) between histocompatibility loci and HFE gene was performed using the Haploview software. RESULTS The HFE *003 allele was overrepresented ( f = 71%) and HFE *001 allele was underrepresented ( f = 14%) in HH patients compared to all groups. A strong linkage disequilibrium was observed among the H63D-G , IVS2(+4)-C and C282Y-G gene variants, particularly in HH; however, the mutation IVS2(+4)T>C was not directly associated with HH susceptibility. The HFE *001/ HFE *002 genotype conferred susceptibility to HCC in HCV patients exhibiting IO ( P = 0.02, OR = 14.14). Although HFE is telomeric to other histocompatibility genes, the H63D-G/IVS2(+4)-C ( P ≤ 0.00001/ P ≤ 0.0057) combination was in LD with HLA-B *44 allele group in healthy controls. No LD was observed between HFE alleles and other major histocompatibility loci. CONCLUSION A differential HFE association was observed for HH and for diseases associated with acquired IO (HCV, HCC). Since HFE is very distant from other histocompatibility loci, only weak associations were observed with these alleles.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

See 2 more Smart Citations

Comprehensive analysis ofHFEgene in hereditary hemochromatosis and in diseases associated with acquired iron overload

Campos

Massaro

Cançado

et al. 2019

WJH

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“…The 5' piece of exon 6 possesses a local stop codon and is accountable in encoding of the cytoplasmic tail. Hence, the whole-length of gene means only 6 exons [19]. The HFE protein holds 343 amino acids and possesses a peptide, a transmembrane region, binding region of an extracellular transferrin receptors (α1 and α2), a transmembrane segment, a short cytoplasmic tail, and an immunoglobulin-like α3 region [20] (Fig.…”

Section: Introductionmentioning

confidence: 99%

HFE Gene Mutations as Predisposing Factors for Childhood Acute Lymphoblastic Leukaemia in Iraqi Patients

Albandar,

Jabbar,

Ibrahim

et al. 2024

UTJsci

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Hemochromatosis is a prevalent hereditary disorder that causes excess iron to build up in the body to dangerous levels. Hereditary hemochromatosis, also known as HFE-related hemochromatosis is carried on by changes in the HFE gene. Investigating the gene mutations of the HFE gene is a way to explore the prevalence of this disease. This study aims to determine the association between hemochromatosis HFE gene mutations (C282Y and H63D) and childhood acute lymphoblastic leukaemia in patients at Basra Specialized Hospital for Children and AL-sadder Teaching Hospital in the Basra governance. QIAamp DNA and Blood Mini Kit were used to isolate and identify Human genomic DNA and detect mutations in the HFE gene using the DNA hybridization method. In this study, the absence of the C282Y mutations in both patients and the control group was identified. However, testing DNA-based hybridization experiments revealed low detection levels of the H63D (homozygous, heterozygous) mutations; in only 12.5% of patients. The H63D (only homozygous) mutations were present in 10% of the control group. The association between patients and the control group is considered statistically significant. The HFE gene mutations (C282Y and H63D), originate in acute lymphoblastic leukaemia in childhood, thus, this study recommends complementary investigations to illustrate this case in more detail with more cases of patients and discover the hidden agents underlying these mutations.

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Nomenclature for factors of the HLA system, update September 2017

Marsh¹

2017

Human Immunology

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HFE gene polymorphism defined by sequence‐based typing of the Brazilian population and a standardized nomenclature for HFE allele sequences

Cited by 4 publications

References 16 publications

Comprehensive analysis ofHFEgene in hereditary hemochromatosis and in diseases associated with acquired iron overload

Comprehensive analysis ofHFEgene in hereditary hemochromatosis and in diseases associated with acquired iron overload

HFE Gene Mutations as Predisposing Factors for Childhood Acute Lymphoblastic Leukaemia in Iraqi Patients

Nomenclature for factors of the HLA system, update September 2017

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