A mutation in the 5′ untranslated region of the human α‐galactosidase A gene in high‐activity variants inhibits specific protein binding

Saifudeen, Zubaida; Desnick, Robert J.; Ehrlich, Melanie

doi:10.1016/0014-5793(95)00891-c

Cited by 10 publications

(14 citation statements)

References 26 publications

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“…One of the most common research applications of chimeric genetic reporter systems is in the analysis of cis-acting elements, like gene promoters; however, to the best of our knowledge, the functional consequences of the 5 0 UTR SNPs upon GLA gene expression have never been assayed in this manner. Overall, our results are consistent with the working hypothesis, based on observations in vivo that some of the minor 5 0 UTR SNPs alleles significantly affect aGal activity levels (Saifudeen et al 1995;Fitzmaurice et al 1997;Oliveira et al 2008a, b), and provide indirect evidence that the human GLA 5 0 UTR indeed contains sequences that are involved in the regulation of gene expression. These data also demonstrate, for the first time, that the 5 0 UTRdependent modulation of GLA gene expression may vary among different cell types.…”

Section: Discussionsupporting

confidence: 91%

“…Because they were neither translated nor part of the mRNA Kozak consensus sequence for translation initiation, they were regarded as biologically neutral, but subsequent studies showed that the c.-30A allele was associated with increased aGal activity in plasma (Saifudeen et al 1995) and the c.-10T allele with decreased aGal activity in leukocytes (Oliveira et al 2008a, b), as compared to the corresponding WT alleles. Since the GLA 5 0 UTR c.-10 and c.-30 positions are within binding sites respectively for the MDBP and the NFkB and Ets families of TF, the effect of those two nucleotide transitions upon aGal expression in vivo might be mediated by modulation of transcriptional activity.…”

Section: Discussionmentioning

confidence: 99%

“…ncbi.nlm.nih.gov/nuccore/NM_000169.2; National Library of Medicine, Bethesda, MD, USA). Three single nucleotide polymorphisms (SNPs) respectively identified by reference numbers rs2071225, rs3027585 and rs3027584 at the NCBI SNP database (dbSNP, http://www.ncbi.nlm.nih.gov/snp/), which result from cytosine-to-thymine (C>T) or adenineto-guanine (G>A) transitions at cDNA nucleotide positions c.-10(C>T), c.-12(G>A) and c.-30(G>A), counting backwards from the translation initiation codon, are relatively common in several ethnically different populations (Davies et al 1993;Saifudeen et al 1995;Wu et al 2011;Ferri et al 2012), including the Portuguese (Oliveira et al 2008a). The dbSNP lists three additional GLA 5 0 UTR SNPs, at positions c.-8(C>G), c.-18(T>C) and c.-105(A>G), respectively identified as rs371291716, rs545597063 and rs3027583, but these variants have never been reported in the Portuguese population.…”

Section: Introductionmentioning

confidence: 99%

“…Compared to the wild-type (WT) allele, the c.-30A allele is associated with increased plasma aGal activity (Saifudeen et al 1995;Fitzmaurice et al 1997), the c.-10T allele is associated with decreased activity of aGal in leukocytes (Oliveira et al 2008a, b) and the c.-44T allele might be associated with increased plasma aGal activity (Baptista et al 2010). Contrastingly, the SNP c.-12(G>A) seems to have no effect upon GLA gene expression (Oliveira et al 2008a).…”

Section: Introductionmentioning

confidence: 99%

“…Because the GLA 5 0 UTR contains a binding site for methylated DNA-binding protein (MDBP)/regulatory factor X (RFX) transcription factor family (Zhang et al 1990;Samac et al 1998), as well as partially overlapping binding motifs for the nuclear factor kappa-B (NFkB) and E-26 (Ets) transcriptional regulatory factors (Saifudeen et al 1995;Fitzmaurice et al 1997), it has been previously suggested that protein ligands to these sites might be involved in the regulation of GLA gene expression (Saifudeen et al 1995;Fitzmaurice et al 1997). Since the SNPs c.-10(C>T) and c.-30(G>A) involve nucleotides respectively located at each of those binding sites, they might act as polymorphic modulators of GLA gene expression, with possible clinical relevance particularly in males carrying GLA sequence variants associated with high REA.…”

Section: Introductionmentioning

confidence: 99%

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The Modulatory Effects of the Polymorphisms in GLA 5′-Untranslated Region Upon Gene Expression Are Cell-Type Specific

2015

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Lysosomal a-galactosidase A (aGal) is the enzyme deficient in Fabry disease (FD). The 5 0 -untranslated region (5 0 UTR) of the aGal gene (GLA) shows a remarkable degree of variation with three common single nucleotide polymorphisms at nucleotide positions c.-30G>A, c.-12G>A and c.-10C>T. We have recently identified in young Portuguese stroke patients a fourth polymorphism, at c.-44C>T, co-segregating in cis with the c.-12A allele. In vivo, the c.-30A allele is associated with higher enzyme activity in plasma, whereas c.-10T is associated with moderately decreased enzyme activity in leucocytes. Limited data suggest that c.-44T might be associated with increased plasma aGal activity. We have used a luciferase reporter system to experimentally assess the relative modulatory effects on gene expression of the different GLA 5 0 UTR polymorphisms, as compared to the wild-type sequence, in four different human cell lines. Group-wise, the relative luciferase expression patterns of the various GLA variant isoforms differed significantly in all four cell lines, as evaluated by non-parametric statistics, and were cell-type specific. Some of the post hoc pairwise statistical comparisons were also significant, but the observed effects of the GLA 5 0 UTR polymorphisms upon the luciferase transcriptional activity in vitro did not consistently replicate the in vivo observations. These data suggest that the GLA 5 0 UTR polymorphisms are possible modulators of the aGal expression. Further studies are needed to elucidate the biological and clinical implications of these observations, particularly to clarify the effect of these polymorphisms in individuals carrying GLA variants associated with high residual enzyme activity, with no or mild FD clinical phenotypes.

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Section: Discussionsupporting

confidence: 91%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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The Modulatory Effects of the Polymorphisms in GLA 5′-Untranslated Region Upon Gene Expression Are Cell-Type Specific

2015

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Effect of single‐nucleotide polymorphisms of the 5′ untranslated region of the human α‐galactosidase gene on enzyme activity, and their frequencies in Portuguese caucasians

Oliveira¹,

Ferreira²,

Barceló³

et al. 2008

J of Inher Metab Disea

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Mean α-Gal leukocyte activity was ∼ 25% higher in subjects with the g.1170C or CC genotype than in those with the alternative genotypes (p < 0.05). The frequency of the g.1170T allele in subjects with low α-Gal activity in dried blood spots was 4-fold higher (p < 0.05) than in the general population. As in hemizygotes, the g.1150A heterozygote identified in this study had plasma α-Gal activity more than 2-fold above the normal mean. The g.1168A allele did not affect enzyme activity. Surprisingly, females with the standard GLA exon 1 genotype had significantly higher plasma α-Gal activity than genetically comparable males.

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The g.1170C>T polymorphism of the 5′ untranslated region of the human alpha‐galactosidase gene is associated with decreased enzyme expression—Evidence from a family study

Oliveira

Ferreira

Reguenga

et al. 2008

J of Inher Metab Disea

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Subnormal leukocyte α-galactosidase (α-Gal) activity was found during evaluation of an adolescent male with cryptogenic cerebrovascular small-vessel disease. The only molecular abnormality found was the g.1170C>T single-nucleotide polymorphism (SNP) in the 5' untranslated region of exon 1 in the α-Gal gene (GLA). Historically, this polymorphism has been considered to be biologically neutral. To test the hypothesis that the g.1170T allele might be associated with lower α-Gal expression, we genotyped GLA exon 1 and measured leukocyte and plasma α-Gal in the parents, brother and sister of the index case. The g.1170T allele co-segregated with a subnormal leukocyte α-Gal activity in the three siblings. Although plasma enzyme activities were within the normal range in all five relatives, the ranking of their values suggested a dosage effect of the g.1170T allele. Western blotting assays of leukocyte protein extracts showed that the relative expression of α-Gal in both the patient and his sister was significantly lower than in sex-matched hemizygous or homozygous controls for the g.1170C allele, either normalized to the β-actin immunoblot expression or standardized to a known amount of recombinant human α-Gal. These family data, in combination with results from a recent GLA SNP screening study among healthy Portuguese individuals, suggest that the g.1170C>T SNP may be co-dominantly associated with a relatively decreased GLA expression at the transcription and/or translation level. Larger population studies are needed to confirm these findings and to test the hypothesis that the GLA g.1170C>T may contribute to the multifactorial risk of ischaemic small-vessel cerebrovascular disease.

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A mutation in the 5′ untranslated region of the human α‐galactosidase A gene in high‐activity variants inhibits specific protein binding

Cited by 10 publications

References 26 publications

The Modulatory Effects of the Polymorphisms in GLA 5′-Untranslated Region Upon Gene Expression Are Cell-Type Specific

The Modulatory Effects of the Polymorphisms in GLA 5′-Untranslated Region Upon Gene Expression Are Cell-Type Specific

Effect of single‐nucleotide polymorphisms of the 5′ untranslated region of the human α‐galactosidase gene on enzyme activity, and their frequencies in Portuguese caucasians

The g.1170C>T polymorphism of the 5′ untranslated region of the human alpha‐galactosidase gene is associated with decreased enzyme expression—Evidence from a family study

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