The Relationship of the −5, −8, and −24 Variant Alleles in African Americans to Triosephosphate Isomerase (TPI) Enzyme Activity and to TPI Deficiency
In 424 African-American and 75 white subjects, we found that the −5 (TPI 592 A→G), −8 (TPI 589 G→A), and −24 (TPI 573 T→G) variants in the triosephosphate isomerase (TPI) gene occurred frequently (41.0%) in the African-American subjects but did not occur in the whites. These data suggest that this s...
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| Published in | Blood Vol. 92; no. 8; pp. 2959 - 2962 |
|---|---|
| Main Authors | , , , , , , |
| Format | Journal Article |
| Language | English |
| Published |
Washington, DC
The Americain Society of Hematology
15.10.1998
|
| Subjects | |
| Online Access | Get full text |
| ISSN | 0006-4971 1528-0020 |
| DOI | 10.1182/blood.V92.8.2959 |
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| Abstract | In 424 African-American and 75 white subjects, we found that the −5 (TPI 592 A→G), −8 (TPI 589 G→A), and −24 (TPI 573 T→G) variants in the triosephosphate isomerase (TPI) gene occurred frequently (41.0%) in the African-American subjects but did not occur in the whites. These data suggest that this set of polymorphisms may turn out to be one of the higher-incidence molecular markers of African lineage, a surprising finding because others had reported that these nucleotide substitutions were restricted to a small subset of African Americans who had been characterized as TPI-deficiency heterozygotes. Additionally, we investigated the relationship of these variants to TPI-enzyme activity. Although the variant substitutions (occurring in three haplotypes: −5 alone, −5 −8, and −5 −8 −24) were associated with moderate reduction in enzyme activity, severe-deficiency heterozygotes could not be identified with certainty, and none of the haplotypes were restricted to subjects with marked reduction of enzyme activity. Three subjects were homozygous for the −5 −8 haplotype, a finding inconsistent with the putative role of this haplotype as the cause of a null variant incompatible with life in homozygotes. Despite these findings, the possibility remains that the −5 −8 or −5 −8 −24 haplotypes may in some instances contribute to compound heterozygosity and clinical TPI deficiency.
© 1998 by The American Society of Hematology. |
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| AbstractList | In 424 African-American and 75 white subjects, we found that the -5 (TPI 592 A-->G), -8 (TPI 589 G-->A), and -24 (TPI 573 T-->G) variants in the triosephosphate isomerase (TPI) gene occurred frequently (41.0%) in the African-American subjects but did not occur in the whites. These data suggest that this set of polymorphisms may turn out to be one of the higher-incidence molecular markers of African lineage, a surprising finding because others had reported that these nucleotide substitutions were restricted to a small subset of African Americans who had been characterized as TPI-deficiency heterozygotes. Additionally, we investigated the relationship of these variants to TPI-enzyme activity. Although the variant substitutions (occurring in three haplotypes: -5 alone, -5 -8, and -5 -8 -24) were associated with moderate reduction in enzyme activity, severe-deficiency heterozygotes could not be identified with certainty, and none of the haplotypes were restricted to subjects with marked reduction of enzyme activity. Three subjects were homozygous for the -5 -8 haplotype, a finding inconsistent with the putative role of this haplotype as the cause of a null variant incompatible with life in homozygotes. Despite these findings, the possibility remains that the -5 -8 or -5 -8 -24 haplotypes may in some instances contribute to compound heterozygosity and clinical TPI deficiency.In 424 African-American and 75 white subjects, we found that the -5 (TPI 592 A-->G), -8 (TPI 589 G-->A), and -24 (TPI 573 T-->G) variants in the triosephosphate isomerase (TPI) gene occurred frequently (41.0%) in the African-American subjects but did not occur in the whites. These data suggest that this set of polymorphisms may turn out to be one of the higher-incidence molecular markers of African lineage, a surprising finding because others had reported that these nucleotide substitutions were restricted to a small subset of African Americans who had been characterized as TPI-deficiency heterozygotes. Additionally, we investigated the relationship of these variants to TPI-enzyme activity. Although the variant substitutions (occurring in three haplotypes: -5 alone, -5 -8, and -5 -8 -24) were associated with moderate reduction in enzyme activity, severe-deficiency heterozygotes could not be identified with certainty, and none of the haplotypes were restricted to subjects with marked reduction of enzyme activity. Three subjects were homozygous for the -5 -8 haplotype, a finding inconsistent with the putative role of this haplotype as the cause of a null variant incompatible with life in homozygotes. Despite these findings, the possibility remains that the -5 -8 or -5 -8 -24 haplotypes may in some instances contribute to compound heterozygosity and clinical TPI deficiency. In 424 African-American and 75 white subjects, we found that the -5 (TPI 592 A-->G), -8 (TPI 589 G-->A), and -24 (TPI 573 T-->G) variants in the triosephosphate isomerase (TPI) gene occurred frequently (41.0%) in the African-American subjects but did not occur in the whites. These data suggest that this set of polymorphisms may turn out to be one of the higher-incidence molecular markers of African lineage, a surprising finding because others had reported that these nucleotide substitutions were restricted to a small subset of African Americans who had been characterized as TPI-deficiency heterozygotes. Additionally, we investigated the relationship of these variants to TPI-enzyme activity. Although the variant substitutions (occurring in three haplotypes: -5 alone, -5 -8, and -5 -8 -24) were associated with moderate reduction in enzyme activity, severe-deficiency heterozygotes could not be identified with certainty, and none of the haplotypes were restricted to subjects with marked reduction of enzyme activity. Three subjects were homozygous for the -5 -8 haplotype, a finding inconsistent with the putative role of this haplotype as the cause of a null variant incompatible with life in homozygotes. Despite these findings, the possibility remains that the -5 -8 or -5 -8 -24 haplotypes may in some instances contribute to compound heterozygosity and clinical TPI deficiency. In 424 African-American and 75 white subjects, we found that the −5 (TPI 592 A→G), −8 (TPI 589 G→A), and −24 (TPI 573 T→G) variants in the triosephosphate isomerase (TPI) gene occurred frequently (41.0%) in the African-American subjects but did not occur in the whites. These data suggest that this set of polymorphisms may turn out to be one of the higher-incidence molecular markers of African lineage, a surprising finding because others had reported that these nucleotide substitutions were restricted to a small subset of African Americans who had been characterized as TPI-deficiency heterozygotes. Additionally, we investigated the relationship of these variants to TPI-enzyme activity. Although the variant substitutions (occurring in three haplotypes: −5 alone, −5 −8, and −5 −8 −24) were associated with moderate reduction in enzyme activity, severe-deficiency heterozygotes could not be identified with certainty, and none of the haplotypes were restricted to subjects with marked reduction of enzyme activity. Three subjects were homozygous for the −5 −8 haplotype, a finding inconsistent with the putative role of this haplotype as the cause of a null variant incompatible with life in homozygotes. Despite these findings, the possibility remains that the −5 −8 or −5 −8 −24 haplotypes may in some instances contribute to compound heterozygosity and clinical TPI deficiency. © 1998 by The American Society of Hematology. |
| Author | Lin, James Singh, Satinder Yim, Catherine Beutler, Ernest Westwood, Beryl Schneider, Arthur Forman, Linda |
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| Cites_doi | 10.1002/ajh.2830500407 10.1093/genetics/123.4.837 10.1006/bcmd.1996.0011 10.1007/BF00291364 10.1016/0027-5107(95)00004-3 10.1056/NEJM196502042720503 10.1006/bcmd.1996.0019 10.1203/00006450-198211000-00012 |
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| Keywords | Human Nervous system diseases Intramolecular oxidoreductases Enzyme Transcription promoter Deficiency Genetic variant Negroid Metabolic diseases Hemopathy Enzymopathy Triose-phosphate isomerase Genetic disease Isomerases Enzymatic activity Race Genetics Black American Haplotype |
| Language | English |
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| References | Beutler (2020021220515254100_B10) 1984 Schneider (2020021220515254100_B1) 1965; 272 Schneider (2020021220515254100_B2) 1996; 22 Eber (2020021220515254100_B6) 1984; 67 Watanabe (2020021220515254100_B9) 1996; 58 Mohrenweiser (2020021220515254100_B4) 1982; 16 Zingg (2020021220515254100_B8) 1995; 328 Schneider (2020021220515254100_B11) 1995; 50 Satoh (2020021220515254100_B5) 1983; 35 Schneider (2020021220515254100_B3) 1996; 22 Merkle (2020021220515254100_B7) 1989; 123 |
| References_xml | – volume: 35 start-page: 656 year: 1983 ident: 2020021220515254100_B5 article-title: The frequency among Japanese of heterozygotes for deficiency variants of 11 enzymes. publication-title: Am J Hum Genet – volume: 50 start-page: 263 year: 1995 ident: 2020021220515254100_B11 article-title: Triosephosphate isomerase deficiency: Repetitive occurrence of point mutation in amino acid 104 in multiple apparently unrelated families. publication-title: Am J Hematol doi: 10.1002/ajh.2830500407 – year: 1984 ident: 2020021220515254100_B10 article-title: Red Cell Metabolism – volume: 123 start-page: 837 year: 1989 ident: 2020021220515254100_B7 article-title: Characterization of triosephosphate isomerase mutants with reduced enzyme activity in Mus musculus. publication-title: Genetics doi: 10.1093/genetics/123.4.837 – volume: 22 start-page: 82 year: 1996 ident: 2020021220515254100_B3 article-title: Hematologically important mutations: Triosephosphate isomerase. publication-title: Blood Cells Mol Dis doi: 10.1006/bcmd.1996.0011 – volume: 67 start-page: 336 year: 1984 ident: 2020021220515254100_B6 article-title: Prevalence of partial deficiency of red cell triosephosphate isomerase in Germany—A study of 3000 people. publication-title: Hum Genet doi: 10.1007/BF00291364 – volume: 328 start-page: 163 year: 1995 ident: 2020021220515254100_B8 article-title: Molecular analysis of four ENU-induced triosephosphate isomerase null mutants in Mus musculus. publication-title: Mutat Res doi: 10.1016/0027-5107(95)00004-3 – volume: 272 start-page: 229 year: 1965 ident: 2020021220515254100_B1 article-title: Hereditary hemolytic anemia with triosephosphate isomerase deficiency. publication-title: N Engl J Med doi: 10.1056/NEJM196502042720503 – volume: 22 start-page: 115 year: 1996 ident: 2020021220515254100_B2 article-title: The 1591C mutation in triosephosphate isomerase (TPI) deficiency. Tightly linked polymorphisms and a common haplotype in all known families. publication-title: Blood Cells Mol Dis doi: 10.1006/bcmd.1996.0019 – volume: 16 start-page: 960 year: 1982 ident: 2020021220515254100_B4 article-title: Elevated frequency of carriers for triosephosphate isomerase deficiency in newborn infants. publication-title: Pediatr Res doi: 10.1203/00006450-198211000-00012 – volume: 58 start-page: 308 year: 1996 ident: 2020021220515254100_B9 article-title: Molecular analysis of a series of alleles in humans with reduced activity at the triosephosphate isomerase locus. publication-title: Am J Hum Genet |
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| Snippet | In 424 African-American and 75 white subjects, we found that the −5 (TPI 592 A→G), −8 (TPI 589 G→A), and −24 (TPI 573 T→G) variants in the triosephosphate... In 424 African-American and 75 white subjects, we found that the -5 (TPI 592 A-->G), -8 (TPI 589 G-->A), and -24 (TPI 573 T-->G) variants in the... |
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| SubjectTerms | Alleles Biological and medical sciences Black or African American Black People - genetics Errors of metabolism Gene Frequency Haplotypes - genetics Heterozygote Humans Medical sciences Metabolic diseases Miscellaneous hereditary metabolic disorders Polymerase Chain Reaction Polymorphism, Genetic Polymorphism, Restriction Fragment Length Triose-Phosphate Isomerase - deficiency Triose-Phosphate Isomerase - genetics White People - genetics |
| Title | The Relationship of the −5, −8, and −24 Variant Alleles in African Americans to Triosephosphate Isomerase (TPI) Enzyme Activity and to TPI Deficiency |
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