An investigation into the MMP1 gene promoter region polymorphism - 1607 2G with recessive dystrophic epidermolysis bullosa disease severity in northeastern Mexican patients

Background Recessive dystrophic epidermolysis bullosa (RDEB) is a severe genetic skin blistering disorder caused by mutations in the gene COL7A1 encoding type VII collagen. Most of the patients' clinical severity depends in part on the nature and location of the mutations, ranging from the mild...

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Published inInternational journal of dermatology Vol. 53; no. 8; pp. 985 - 990
Main Authors Garza-Gómez, Jorge, Cerda-Flores, Ricardo M., Gómez-Flores, Minerva, Salas-Alanís, Julio C., Ocampo-Candiani, Jorge, Martínez-Garza, Laura E., South, Andrew P., Gallardo-Blanco, Hugo L.
Format Journal Article
LanguageEnglish
Published England Blackwell Publishing Ltd 01.08.2014
Subjects
Adolescent
Adult
Case-Control Studies
Child
Child, Preschool
Epidermolysis Bullosa Dystrophica - genetics
Gene Frequency
Genotype
Humans
Matrix Metalloproteinase 1 - genetics
Mexico
Middle Aged
Polymorphism, Single Nucleotide
Promoter Regions, Genetic
Severity of Illness Index
Young Adult
Mexico
Online AccessGet full text
ISSN0011-9059
1365-4632
1365-4632
DOI10.1111/ijd.12499

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Abstract Background Recessive dystrophic epidermolysis bullosa (RDEB) is a severe genetic skin blistering disorder caused by mutations in the gene COL7A1 encoding type VII collagen. Most of the patients' clinical severity depends in part on the nature and location of the mutations, ranging from the mild form described as RDEBother‐generalized (RDEB‐O) to the more aggressive phenotype described as RDEBsevere‐generalized (RDEB‐sev gen). However, interfamilial and interindividual differences in subjects with identical COL7A1 mutations suggest the presence of modifier elements, which may influence severity. There is a single nucleotide polymorphism (SNP) at the promoter of the MMP1 gene‐encoding matrix metalloproteinase type 1, which has been studied as a genetic disease modifier in different patient cohorts with different findings. Methods We tested the SNP in 30 patients with RDEB and 130 controls whose four grandparents were born in northeastern Mexico. Patients were clinically classified as RDEB‐sev gen and RDEB‐O by three dermatologists. The SNPStats, RXC, and SPSS software were used to perform statistical testing. Results The allele frequencies for 2G were 0.607, 0.562, and 0.642 for RDEB‐O, RDEB‐sev gen, and the control group, respectively. When the genotype frequencies were compared, there was no significant difference between RDEB‐sev gen (OR = 0.38, CI 95% 0.12–1.21), RDEB‐O (OR = 1.03, CI 95% 0.21–4.96), and the control group. Conclusion We found no significant association in relation to the severity of the study subjects and the SNP at the promoter of the MMP1 gene.
AbstractList Recessive dystrophic epidermolysis bullosa (RDEB) is a severe genetic skin blistering disorder caused by mutations in the gene COL7A1 encoding type VII collagen. Most of the patients' clinical severity depends in part on the nature and location of the mutations, ranging from the mild form described as RDEBother-generalized (RDEB-O) to the more aggressive phenotype described as RDEBsevere-generalized (RDEB-sev gen). However, interfamilial and interindividual differences in subjects with identical COL7A1 mutations suggest the presence of modifier elements, which may influence severity. There is a single nucleotide polymorphism (SNP) at the promoter of the MMP1 gene-encoding matrix metalloproteinase type 1, which has been studied as a genetic disease modifier in different patient cohorts with different findings.BACKGROUNDRecessive dystrophic epidermolysis bullosa (RDEB) is a severe genetic skin blistering disorder caused by mutations in the gene COL7A1 encoding type VII collagen. Most of the patients' clinical severity depends in part on the nature and location of the mutations, ranging from the mild form described as RDEBother-generalized (RDEB-O) to the more aggressive phenotype described as RDEBsevere-generalized (RDEB-sev gen). However, interfamilial and interindividual differences in subjects with identical COL7A1 mutations suggest the presence of modifier elements, which may influence severity. There is a single nucleotide polymorphism (SNP) at the promoter of the MMP1 gene-encoding matrix metalloproteinase type 1, which has been studied as a genetic disease modifier in different patient cohorts with different findings.We tested the SNP in 30 patients with RDEB and 130 controls whose four grandparents were born in northeastern Mexico. Patients were clinically classified as RDEB-sev gen and RDEB-O by three dermatologists. The SNPStats, RXC, and SPSS software were used to perform statistical testing.METHODSWe tested the SNP in 30 patients with RDEB and 130 controls whose four grandparents were born in northeastern Mexico. Patients were clinically classified as RDEB-sev gen and RDEB-O by three dermatologists. The SNPStats, RXC, and SPSS software were used to perform statistical testing.The allele frequencies for 2G were 0.607, 0.562, and 0.642 for RDEB-O, RDEB-sev gen, and the control group, respectively. When the genotype frequencies were compared, there was no significant difference between RDEB-sev gen (OR = 0.38, CI 95% 0.12-1.21), RDEB-O (OR = 1.03, CI 95% 0.21-4.96), and the control group.RESULTSThe allele frequencies for 2G were 0.607, 0.562, and 0.642 for RDEB-O, RDEB-sev gen, and the control group, respectively. When the genotype frequencies were compared, there was no significant difference between RDEB-sev gen (OR = 0.38, CI 95% 0.12-1.21), RDEB-O (OR = 1.03, CI 95% 0.21-4.96), and the control group.We found no significant association in relation to the severity of the study subjects and the SNP at the promoter of the MMP1 gene.CONCLUSIONWe found no significant association in relation to the severity of the study subjects and the SNP at the promoter of the MMP1 gene.
Background Recessive dystrophic epidermolysis bullosa (RDEB) is a severe genetic skin blistering disorder caused by mutations in the gene COL7A1 encoding type VII collagen. Most of the patients' clinical severity depends in part on the nature and location of the mutations, ranging from the mild form described as RDEBother‐generalized (RDEB‐O) to the more aggressive phenotype described as RDEBsevere‐generalized (RDEB‐sev gen). However, interfamilial and interindividual differences in subjects with identical COL7A1 mutations suggest the presence of modifier elements, which may influence severity. There is a single nucleotide polymorphism (SNP) at the promoter of the MMP1 gene‐encoding matrix metalloproteinase type 1, which has been studied as a genetic disease modifier in different patient cohorts with different findings. Methods We tested the SNP in 30 patients with RDEB and 130 controls whose four grandparents were born in northeastern Mexico. Patients were clinically classified as RDEB‐sev gen and RDEB‐O by three dermatologists. The SNPStats, RXC, and SPSS software were used to perform statistical testing. Results The allele frequencies for 2G were 0.607, 0.562, and 0.642 for RDEB‐O, RDEB‐sev gen, and the control group, respectively. When the genotype frequencies were compared, there was no significant difference between RDEB‐sev gen (OR = 0.38, CI 95% 0.12–1.21), RDEB‐O (OR = 1.03, CI 95% 0.21–4.96), and the control group. Conclusion We found no significant association in relation to the severity of the study subjects and the SNP at the promoter of the MMP1 gene.
Recessive dystrophic epidermolysis bullosa (RDEB) is a severe genetic skin blistering disorder caused by mutations in the gene COL7A1 encoding type VII collagen. Most of the patients' clinical severity depends in part on the nature and location of the mutations, ranging from the mild form described as RDEBother-generalized (RDEB-O) to the more aggressive phenotype described as RDEBsevere-generalized (RDEB-sev gen). However, interfamilial and interindividual differences in subjects with identical COL7A1 mutations suggest the presence of modifier elements, which may influence severity. There is a single nucleotide polymorphism (SNP) at the promoter of the MMP1 gene-encoding matrix metalloproteinase type 1, which has been studied as a genetic disease modifier in different patient cohorts with different findings. We tested the SNP in 30 patients with RDEB and 130 controls whose four grandparents were born in northeastern Mexico. Patients were clinically classified as RDEB-sev gen and RDEB-O by three dermatologists. The SNPStats, RXC, and SPSS software were used to perform statistical testing. The allele frequencies for 2G were 0.607, 0.562, and 0.642 for RDEB-O, RDEB-sev gen, and the control group, respectively. When the genotype frequencies were compared, there was no significant difference between RDEB-sev gen (OR = 0.38, CI 95% 0.12-1.21), RDEB-O (OR = 1.03, CI 95% 0.21-4.96), and the control group. We found no significant association in relation to the severity of the study subjects and the SNP at the promoter of the MMP1 gene.
Recessive dystrophic epidermolysis bullosa (RDEB) is a severe genetic skin blistering disorder caused by mutations in the gene COL7A1 encoding type VII collagen. Most of the patients' clinical severity depends in part on the nature and location of the mutations, ranging from the mild form described as RDEBother-generalized (RDEB-O) to the more aggressive phenotype described as RDEBsevere-generalized (RDEB-sev gen). However, interfamilial and interindividual differences in subjects with identical COL7A1 mutations suggest the presence of modifier elements, which may influence severity. There is a single nucleotide polymorphism (SNP) at the promoter of the MMP1 gene-encoding matrix metalloproteinase type 1, which has been studied as a genetic disease modifier in different patient cohorts with different findings. We tested the SNP in 30 patients with RDEB and 130 controls whose four grandparents were born in northeastern Mexico. Patients were clinically classified as RDEB-sev gen and RDEB-O by three dermatologists. The SNPStats, RXC, and SPSS software were used to perform statistical testing. The allele frequencies for 2G were 0.607, 0.562, and 0.642 for RDEB-O, RDEB-sev gen, and the control group, respectively. When the genotype frequencies were compared, there was no significant difference between RDEB-sev gen (OR = 0.38, CI 95% 0.12-1.21), RDEB-O (OR = 1.03, CI 95% 0.21-4.96), and the control group. We found no significant association in relation to the severity of the study subjects and the SNP at the promoter of the MMP1 gene.
Author South, Andrew P.
Garza-Gómez, Jorge
Salas-Alanís, Julio C.
Ocampo-Candiani, Jorge
Martínez-Garza, Laura E.
Gallardo-Blanco, Hugo L.
Cerda-Flores, Ricardo M.
Gómez-Flores, Minerva
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Snippet Background Recessive dystrophic epidermolysis bullosa (RDEB) is a severe genetic skin blistering disorder caused by mutations in the gene COL7A1 encoding type...
Recessive dystrophic epidermolysis bullosa (RDEB) is a severe genetic skin blistering disorder caused by mutations in the gene COL7A1 encoding type VII...
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pubmed
wiley
istex
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SubjectTerms Adolescent
Adult
Case-Control Studies
Child
Child, Preschool
Epidermolysis Bullosa Dystrophica - genetics
Gene Frequency
Genotype
Humans
Matrix Metalloproteinase 1 - genetics
Mexico
Middle Aged
Polymorphism, Single Nucleotide
Promoter Regions, Genetic
Severity of Illness Index
Young Adult
Title An investigation into the MMP1 gene promoter region polymorphism - 1607 2G with recessive dystrophic epidermolysis bullosa disease severity in northeastern Mexican patients
URI https://api.istex.fr/ark:/67375/WNG-T2921L7G-L/fulltext.pdf
https://onlinelibrary.wiley.com/doi/abs/10.1111%2Fijd.12499
https://www.ncbi.nlm.nih.gov/pubmed/24899116
https://www.proquest.com/docview/1547532080
https://www.proquest.com/docview/1639988842
Volume 53
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