Co‐existence of two functional mutations on the same allele of the human ferrochelatase gene in erythropoietic protoporphyria

Pierro, Elena Di; Brancaleoni, Valentina; Moriondo, Valeria; Besana, V.; Cappellini, Maria Domenica

doi:10.1111/j.1399-0004.2007.00733.x

Cited by 16 publications

(16 citation statements)

References 15 publications

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“…Thus, in pulmonary arterial hypertension, a disease caused by mutations in the bone morphogenetic protein receptor type 2 ( BMPR2 ) gene, the penetrance of the BMPR2 disease allele is dependent upon the level of expression of the wild-type BMPR2 allele (Hamid et al 2009a). Similarly, in erythropoietic protoporphyria, an autosomal dominant condition caused by mutations in the ferrochelatase ( FECH ) gene, the penetrance of the pathogenic FECH allele is influenced by the level of expression of the wild-type FECH allele (Gouya et al 1999; 2002; Di Pierro et al 2007). Other examples of autosomal dominant conditions where the degree of clinical penetrance is modulated by differential expression of the wild-type and mutant alleles include hereditary elliptocytosis ( SPTA1 , Wilmotte et al 1993), Marfan syndrome ( FBN1 , Hutchinson et al 2003), retinoblastoma ( RB1 , Taylor et al 2007), colorectal cancer ( APC , Yan et al 2002; TGFBR1 , Valle et al 2008) and breast and ovarian cancer ( BRCA1 , Ginolhac et al 2003).…”

Section: Influence Of the Gene Expression Level On Mutation Penetrancementioning

confidence: 99%

Where genotype is not predictive of phenotype: towards an understanding of the molecular basis of reduced penetrance in human inherited disease

et al. 2013

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Some individuals with a particular disease-causing mutation or genotype fail to express most if not all features of the disease in question, a phenomenon that is known as ‘reduced (or incomplete) penetrance’. Reduced penetrance is not uncommon; indeed, there are many known examples of ‘disease-causing mutations’ that fail to cause disease in at least a proportion of the individuals who carry them. Reduced penetrance may therefore explain not only why genetic diseases are occasionally transmitted through unaffected parents, but also why healthy individuals can harbour quite large numbers of potentially disadvantageous variants in their genomes without suffering any obvious ill effects. Reduced penetrance can be a function of the specific mutation(s) involved or of allele dosage. It may also result from differential allelic expression, copy number variation or the modulating influence of additional genetic variants in cis or in trans. The penetrance of some pathogenic genotypes is known to be age- and/or sex-dependent. Variable penetrance may also reflect the action of unlinked modifier genes, epigenetic changes or environmental factors. At least in some cases, complete penetrance appears to require the presence of one or more genetic variants at other loci. In this review, we summarize the evidence for reduced penetrance being a widespread phenomenon in human genetics and explore some of the molecular mechanisms that may help to explain this enigmatic characteristic of human inherited disease.

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Section: Influence Of the Gene Expression Level On Mutation Penetrancementioning

confidence: 99%

Where genotype is not predictive of phenotype: towards an understanding of the molecular basis of reduced penetrance in human inherited disease

et al. 2013

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“…In absence of the SNP, an individual with identical mutation in FECH is unaffected. 3,4 The effect of SNP at miRNA target site modulating posttranscriptional regulation has increasingly been reported. 22,23 Such cases could be examined for variations in penetrance of the associated mutations.…”

Section: Discussionmentioning

confidence: 99%

“…In erythropoietic protoporphyria (EPP), an autosomal dominant disorder of heme biosynthesis, the clinical phenotype results from coinheritance of a mutant allele and a low-expressed wild-type allele of FECH. 3,4 Brugada syndrome, a cardiac disorder, is inherited as an autosomal dominant mutation but shows incomplete penetrance. Poelzing et al reported that individuals carrying a H558R polymorphism in trans, on the normal allele of the gene, in addition to the disease causing R282H mutation in SCN5A are asymptomatic, suggesting that the H558R polymorphism overrides the effect of the mutant allele.…”

Section: Introductionmentioning

confidence: 99%

Modeling SNP mediated differential targeting of homologous 3′UTR by microRNA

et al. 2012

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We had previously proposed that the post-transcriptional regulation through microRNA as a mechanism for incomplete penetrance and variable expressivity, leads to lack of correlation between genotype and phenotype. Here we report the validation of miRNA-target interactions we predicted earlier and demonstrate the regulation of endogenous JAG1 by hsamiR-214 and hsa-miR-124, and TGFBR2 by hsa-miR-34b*, through luciferase activity of reporter constructs and also the expression levels of the endogenous genes. Using these targets, we have modeled the diploid state for miRNA target site with heterozygosity for the SNP and demonstrate the differential targeting of an otherwise identical 3'UTR. We show that SNP rs8708 (A . G) at the target site of hsa-miR-214 can relieve the repression while an SNP rs11466532 (C . T) enhances the repression of reporter expression by hsa-miR-34b*. We discuss the results in the light of its implications in the context of penetrance of dominant mutations in miRNA targeted genes, using JAG1 as an example. These observations imply that disease causing mutations in JAG1 linked to the SNP rs8708G will be poorly targeted by hsa-miR-214 when present against a normal allele of JAG1 with rs8708A and will show penetrance of JAG1 mutations as Alagille syndrome, while mutant JAG1 linked to rs8708A against rs8708G on the normal allele will show either no disease or much attenuated symptoms and hence exhibit incomplete penetrance.

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“…A wide heterogeneity of genetic defects has been reported although predominant mutations are more frequent than in acute porphyrias. Large deletions are really prevalent in chronic porphyrias mostly in EPP [50][51][52]. Although patients with gene defects causing truncated proteins might be more vulnerable to liver complications [53], no exact genotypephenotype correlation predicting liver damage has been reported.…”

Section: Clinical Presentation and Diagnosis Of Chronic Porphyriasmentioning

confidence: 99%

Porphyrias at a glance: diagnosis and treatment

et al. 2010

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Porphyrias are a group of eight rare inherited metabolic disorders of heme biosynthesis pathway. Porphyrias are still underdiagnosed, although examinations of urine and plasma are first-line tests for detecting excess of porphyrins or heme precursors in suspected patients. Diagnosis, particularly for the acute forms, is essential to avoid precipitating factors and the use of triggering drugs. Mutation screening of family members is recommended to identify presymptomatic carriers and to prevent acute attacks. The therapeutic approach should be appropriate regarding specific forms of porphyria and treatment should be started promptly.

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Co‐existence of two functional mutations on the same allele of the human ferrochelatase gene in erythropoietic protoporphyria

Cited by 16 publications

References 15 publications

Where genotype is not predictive of phenotype: towards an understanding of the molecular basis of reduced penetrance in human inherited disease

Where genotype is not predictive of phenotype: towards an understanding of the molecular basis of reduced penetrance in human inherited disease

Modeling SNP mediated differential targeting of homologous 3′UTR by microRNA

Porphyrias at a glance: diagnosis and treatment

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