Your search keyword '"Leonid Segal"' showing total 5 results

1. A Large Set of Finnish Affected Sibling Pair Families With Type 2 Diabetes Suggests Susceptibility Loci on Chromosomes 6, 11, and 14

Author

Richard M. Watanabe, Kerry R. Wiles, Kimberly Colby, Narisu Narisu, Julie A. Douglas, Leonid Segal, Tasha E. Fingerlin, Elizabeth R. Hauser, Pablo Hollstein, Kimberly F. Doheny, Victoria L. Magnuson, Kathleen M. Humphreys, Michael P. Epstein, Soumitra Ghosh, David Rha, Rachel Porter, Jason Tovar, Yong D. Suh, Jaakko Tuomilehto, William Hagopian, Francis S. Collins, Chun Li, Arun M. Unni, Carrie Pfahl, Laura J. Scott, Jason E. Hill, Anabelle Morales-Mena, George Lin, Thomas A. Buchanan, Konstantinos N. Lazaridis, Elizabeth W. Pugh, Peggy P. White, Roshni A. Kasad, Peter S. Chines, Anne U. Jackson, Kristin Patzkowski, Jessica Lambert, Michael R. Erdos, Heather M. Stringham, Timo T. Valle, Richard N. Bergman, Karen L. Mohlke, Kaisa Silander, Christian Welch, William L. Duren, and Michael Boehnke

Subjects

Genetic Markers, Male, Positional cloning, Endocrinology, Diabetes and Metabolism, 030209 endocrinology & metabolism, Biology, 03 medical and health sciences, 0302 clinical medicine, Internal Medicine, Humans, Family, Genetic Predisposition to Disease, Age of Onset, Sibling, Gene, Finland, Aged, DNA Primers, 030304 developmental biology, Chromosomes, Human, Pair 14, Linkage (software), Genetics, 0303 health sciences, Affected sibling, Base Sequence, Genome, Human, Chromosomes, Human, Pair 11, Siblings, Chromosome, Middle Aged, Diabetes Mellitus, Type 2, Genetic marker, Body Constitution, Chromosomes, Human, Pair 6, Female, Human genome

Abstract

The aim of the Finland-United States Investigation of NIDDM Genetics (FUSION) study is to identify genes that predispose to type 2 diabetes or are responsible for variability in diabetes-related traits via a positional cloning and positional candidate gene approach. In a previously published genome-wide scan of 478 Finnish affected sibling pair (ASP) families (FUSION 1), the strongest linkage results were on chromosomes 20 and 11. We now report a second genome-wide scan using an independent set of 242 Finnish ASP families (FUSION 2), a detailed analysis of the combined set of 737 FUSION 1 + 2 families (495 updated FUSION 1 families), and fine mapping of the regions of chromosomes 11 and 20. The strongest FUSION 2 linkage results were on chromosomes 6 (maximum logarithm of odds score [MLS] = 2.30 at 95 cM) and 14 (MLS = 1.80 at 57 cM). For the combined FUSION 1 + 2 families, three results were particularly notable: chromosome 11 (MLS = 2.98 at 82 cM), chromosome 14 (MLS = 2.74 at 58 cM), and chromosome 6 (MLS = 2.66 at 96 cM). We obtained smaller FUSION 1 + 2 MLSs on chromosomes X (MLS = 1.27 at 152 cM) and 20p (MLS = 1.21 at 20 cM). Among the 10 regions that showed nominally significant evidence for linkage in FUSION 1, four (on chromosomes 6, 11, 14, and X) also showed evidence for linkage in FUSION 2 and stronger evidence for linkage in the combined FUSION 1 + 2 sample.

Published

2004

2. The Finland–United States Investigation of Non–Insulin-Dependent Diabetes Mellitus Genetics (FUSION) Study. I. An Autosomal Genome Scan for Genes That Predispose to Type 2 Diabetes

Author

Alyson Witt, Ethan M. Lange, David Rha, William Hagopian, Edna H. Ross, James E. Balow, Catherine Te, Richard M. Watanabe, Heather M. Stringham, Francis S. Collins, Richard C. McEachin, Zarir E. Karanjawala, Elizabeth R. Hauser, William L. Duren, Michael Boehnke, Thomas A. Buchanan, Timo T. Valle, Tasha E. Fingerlin, Richard N. Bergman, Jillian Blaschak-Harvan, Chun Li, Liisa Toivanen, Julie I. Knapp, Victoria L. Magnuson, Gabriele Vidgren, Leonid Segal, Delphine S. Ally, Anjene Musick, Jennie Chang, Stella J. Nylund, Arun M. Unni, Shane A. Shapiro, Peggy P. White, Karen L. Mohlke, Michael P. Epstein, Elza Demirchyan, Ben Shurtleff, Kristina Kudelko, Jaakko Tuomilehto, Joseph B. Rayman, Michael R. Erdos, Hong Shi Kaleta, Eva Tuomilehto-Wolf, Christian Welch, Carl D. Langefeld, Julie A. Douglas, Tiffany Musick, Joyce Tannenbaum, Carrie Pfahl, Ravi Sharaf, Kimmo Kohtamäki, Alistair So, Colin Martin, Jason Tovar, Soumitra Ghosh, Rachel Porter, Peter S. Chines, Edward H. Trager, Johan G. Eriksson, Ray Whiten, Kaisa Silander, Anabelle Morales-Mena, Gunther Birznieks, and William Eldridge

Subjects

Genetics, 0303 health sciences, Autosome, Genome Scan, Chromosome, chemical and pharmacologic phenomena, 030209 endocrinology & metabolism, Locus (genetics), Biology, Quantitative trait locus, Genome, 03 medical and health sciences, 0302 clinical medicine, Microsatellite, Genetics(clinical), Chromosome 20, Genetics (clinical), 030304 developmental biology

Abstract

We performed a genome scan at an average resolution of 8 cM in 719 Finnish sib pairs with type 2 diabetes. Our strongest results are for chromosome 20, where we observe a weighted maximum LOD score (MLS) of 2.15 at map position 69.5 cM from pter and secondary weighted LOD-score peaks of 2.04 at 56.5 cM and 1.99 at 17.5 cM. Our next largest MLS is for chromosome 11 (MLS = 1.75 at 84.0 cM), followed by chromosomes 2 (MLS = 0.87 at 5.5 cM), 10 (MLS = 0.77 at 75.0 cM), and 6 (MLS = 0.61 at 112.5 cM), all under an additive model. When we condition on chromosome 2 at 8.5 cM, the MLS for chromosome 20 increases to 5.50 at 69.0 cM (P=.0014). An ordered-subsets analysis based on families with high or low diabetes-related quantitative traits yielded results that support the possible existence of disease-predisposing genes on chromosomes 6 and 10. Genomewide linkage-disequilibrium analysis using microsatellite marker data revealed strong evidence of association for D22S423 (P=.00007). Further analyses are being carried out to confirm and to refine the location of these putative diabetes-predisposing genes.

Published

2000

3. The Finland–United States Investigation of Non–Insulin-Dependent Diabetes Mellitus Genetics (FUSION) Study. II. An Autosomal Genome Scan for Diabetes-Related Quantitative-Trait Loci

Author

Richard C. McEachin, Gabriele Vidgren, William Hagopian, Tasha E. Fingerlin, Shane A. Shapiro, Christian Welch, Colin Martin, William L. Duren, Michael Boehnke, Johan G. Eriksson, Gunther Birznieks, William Eldridge, Ray Whiten, Liisa Toivanen, Julie A. Douglas, Zarir E. Karanjawala, Francis S. Collins, Thomas A. Buchanan, Soumitra Ghosh, Carl D. Langefeld, Anjene Musick, Jennie Chang, Stella J. Nylund, Timo T. Valle, Alistair So, Catherine Te, Chun Li, Leonid Segal, Karen L. Mohlke, Carrie Pfahl, Ravi Sharaf, Edna H. Ross, Rachel Porter, Richard M. Watanabe, Joseph B. Rayman, Eva Tuomilehto-Wolf, Elza Demirchyan, David Rha, Joyce Tannenbaum, Victoria L. Magnuson, Elizabeth R. Hauser, Michael P. Epstein, Kimmo Kohtamäki, Richard N. Bergman, Delphine S. Ally, Alyson Witt, Edward H. Trager, Ben Shurtleff, Kristina Kudelko, Jaakko Tuomilehto, Peggy P. White, Julie I. Knapp, Michael R. Erdos, Kaisa Silander, Peter S. Chines, Hong Shi Kaleta, James E. Balow, Christian Ehnholm, Heather M. Stringham, Arun M. Unni, Tiffany Musick, Jason Tovar, Jillian Blaschak-Harvan, Anabelle Morales-Mena, and Ethan M. Lange

Subjects

Blood Glucose, Male, Genetic Linkage, Matched-Pair Analysis, medicine.medical_treatment, chemical and pharmacologic phenomena, Locus (genetics), Type 2 diabetes, Quantitative trait locus, Biology, Body Mass Index, Nuclear Family, Quantitative Trait, Heritable, Sex Factors, Genetic linkage, Diabetes mellitus, Genetics, medicine, Chromosomes, Human, Humans, Insulin, Genetics(clinical), Genetic Predisposition to Disease, Genetic Testing, Finland, Genetics (clinical), Autosome, Genome, Human, Age Factors, Type 2 Diabetes Mellitus, Articles, Fasting, Middle Aged, medicine.disease, United States, Diabetes Mellitus, Type 2, Female

Abstract

Type 2 diabetes mellitus is a complex disorder encompassing multiple metabolic defects. We report results from an autosomal genome scan for type 2 diabetes-related quantitative traits in 580 Finnish families ascertained for an affected sibling pair and analyzed by the variance components-based quantitative-trait locus (QTL) linkage approach. We analyzed diabetic and nondiabetic subjects separately, because of the possible impact of disease on the traits of interest. In diabetic individuals, our strongest results were observed on chromosomes 3 (fasting C-peptide/glucose: maximum LOD score [MLS] = 3.13 at 53.0 cM) and 13 (body-mass index: MLS = 3.28 at 5.0 cM). In nondiabetic individuals, the strongest results were observed on chromosomes 10 (acute insulin response: MLS = 3.11 at 21.0 cM), 13 (2-h insulin: MLS = 2.86 at 65.5 cM), and 17 (fasting insulin/glucose ratio: MLS = 3.20 at 9.0 cM). In several cases, there was evidence for overlapping signals between diabetic and nondiabetic individuals; therefore we performed joint analyses. In these joint analyses, we observed strong signals for chromosomes 3 (body-mass index: MLS = 3.43 at 59.5 cM), 17 (empirical insulin-resistance index: MLS = 3.61 at 0.0 cM), and 19 (empirical insulin-resistance index: MLS = 2.80 at 74.5 cM). Integrating genome-scan results from the companion article by Ghosh et al., we identify several regions that may harbor susceptibility genes for type 2 diabetes in the Finnish population.

Published

2000

4. The Finland–United States Investigation of Non–Insulin‐Dependent Diabetes Mellitus Genetics (FUSION) Study. II. An Autosomal Genome Scan for Diabetes‐Related Quantitative‐Trait Loci

Author

Richard M. Watanabe, Soumitra Ghosh, Carl D. Langefeld, Timo T. Valle, Elizabeth R. Hauser, Victoria L. Magnuson, Karen L. Mohlke, Kaisa Silander, Delphine S. Ally, Peter Chines, Jillian Blaschak‐Harvan, Julie A. Douglas, William L. Duren, Michael P. Epstein, Tasha E. Fingerlin, Hong Shi Kaleta, Ethan M. Lange, Chun Li, Richard C. McEachin, Heather M. Stringham, Edward Trager, Peggy P. White, James Balow, Jr., Gunther Birznieks, Jennie Chang, William Eldridge, Michael R. Erdos, Zarir E. Karanjawala, Julie I. Knapp, Kristina Kudelko, Colin Martin, Anabelle Morales‐Mena, Anjene Musick, Tiffany Musick, Carrie Pfahl, Rachel Porter, Joseph B. Rayman, David Rha, Leonid Segal, Shane Shapiro, Ravi Sharaf, Ben Shurtleff, Alistair So, Joyce Tannenbaum, Catherine Te, Jason Tovar, Arun Unni, Christian Welch, Ray Whiten, Alyson Witt, Kimmo Kohtamaki, Christian Ehnholm, Johan Eriksson, Liisa Toivanen, Gabriele Vidgren, Stella J. Nylund, Eva Tuomilehto‐Wolf, Edna H. Ross, Elza Demirchyan, William A. Hagopian, Thomas A. Buchanan, Jaakko Tuomilehto, Richard N. Bergman, Francis S. Collins, and Michael Boehnke

Subjects

Genetics, Genetics (clinical)

Published

2000

5. Type 2 diabetes: evidence for linkage on chromosome 20 in 716 Finnish affected sib pairs

Author

Richard N. Bergman, Johan G. Eriksson, Gunther Birznieks, Eva Tuomilehto-Wolf, William Eldridge, Victoria L. Magnuson, Colin Martin, William Hagopian, Delphine S. Ally, Christian Ehnholm, Soumitra Ghosh, Alistair So, Rachel Porter, Jillian Blaschak-Harvan, Arun M. Unni, Michael R. Erdos, James E. Balow, Gabriele Vidgren, Michael Boehnke, Ben Shurtleff, Kimmo Kohtamäki, Kristina Kudelko, Jaakko Tuomilehto, Elizabeth R. Hauser, Anjene Musick, Jennie Chang, Thomas A. Buchanan, Carl D. Langefeld, Shane A. Shapiro, Ravi Sharaf, Hong-Shi Kaleta, Timo T. Valle, Francis S. Collins, Tuula Tenkula, Joyce Tannenbaum, Leonid Segal, Peter S. Chines, Catherine Te, Richard M. Watanabe, and Alyson Witt

Subjects

Adult, Blood Glucose, Genetic Markers, Male, Genetic Linkage, Chromosomes, Human, Pair 20, Quantitative trait locus, Biology, Nuclear Family, Centimorgan, Genetic linkage, Genetic variation, Odds Ratio, Humans, Point Mutation, Genetic Predisposition to Disease, Spouses, Finland, Polymorphism, Single-Stranded Conformational, Sequence Deletion, Genetics, Linkage (software), Multidisciplinary, Models, Genetic, Basic Helix-Loop-Helix Leucine Zipper Transcription Factors, Chromosome, Chromosome Mapping, Genetic Variation, Exons, Glucose Tolerance Test, Middle Aged, Biological Sciences, Phosphoproteins, Introns, DNA-Binding Proteins, Diabetes Mellitus, Type 2, Hepatocyte Nuclear Factor 4, Genetic marker, Female, Chromosome 20, Transcription Factors

Abstract

We are conducting a genome scan at an average resolution of 10 centimorgans (cM) for type 2 diabetes susceptibility genes in 716 affected sib pairs from 477 Finnish families. To date, our best evidence for linkage is on chromosome 20 with potentially separable peaks located on both the long and short arms. The unweighted multipoint maximum logarithm of odds score (MLS) was 3.08 on 20p (location, x̂ = 19.5 cM) under an additive model, whereas the weighted MLS was 2.06 on 20q ( x̂ = 57 cM, recurrence risk, λ̂ s = 1.25, P = 0.009). Weighted logarithm of odds scores of 2.00 ( x̂ = 69.5 cM, P = 0.010) and 1.92 ( x̂ = 18.5 cM, P = 0.013) were also observed. Ordered subset analyses based on sibships with extreme mean values of diabetes-related quantitative traits yielded sets of families who contributed disproportionately to the peaks. Two-hour glucose levels in offspring of diabetic individuals gave a MLS of 2.12 ( P = 0.0018) at 9.5 cM. Evidence from this and other studies suggests at least two diabetes-susceptibility genes on chromosome 20. We have also screened the gene for maturity-onset diabetes of the young 1, hepatic nuclear factor 4-a ( HNF-4 α) in 64 affected sibships with evidence for high chromosomal sharing at its location on chromosome 20q. We found no evidence that sequence changes in this gene accounted for the linkage results we observed.

Published

1999