Your search keyword '"Geoffrey M. Duyk"' showing total 31 results

1. A Phenotype-Sensitizing Apoe-Deficient Genetic Background Reveals Novel Atherosclerosis Predisposition Loci in the Mouse

Author

T J McBride, Pei Shu, Jan L. Breslow, Geoffrey M. Duyk, S Whiteing, Deborah L. Nagle, Hayes M. Dansky, Jonathan D. Smith, Natalie Roy, Judith Barrios, M Donavan, Karen J. Moore, Jill Montagno, and John S. Smutko

Subjects

Male, Apolipoprotein E, Arteriosclerosis, Locus (genetics), Biology, Quantitative trait locus, Lesion, Mice, chemistry.chemical_compound, Apolipoproteins E, Quantitative Trait, Heritable, Gene Frequency, Inbred strain, Genetics, medicine, Animals, Genetic Predisposition to Disease, Cholesterol, Lipids, Phenotype, Mice, Inbred C57BL, chemistry, Female, medicine.symptom, Research Article, Lipoprotein

Abstract

Therapeutic intervention for atherosclerosis has predominantly concentrated on regulating cholesterol levels; however, these therapeutics are not efficacious for all patients, suggesting that other factors are involved. This study was initiated to identify mechanisms that regulate atherosclerosis predisposition in mice other than cholesterol level regulation. To do so we performed quantitative trait locus analysis using two inbred strains that each carry the atherosclerosis phenotype-sensitizing Apoe deficiency and that have been shown to have widely disparate predilection to atherosclerotic lesion formation. One highly significant locus on chromosome 10 (LOD = 7.8) accounted for 19% of the variance in lesion area independent of cholesterol. Two additional suggestive loci were identified on chromosomes 14 (LOD = 3.2) and 19 (LOD = 3.2), each accounting for 7–8% of the lesion variance. In all, five statistically significant and suggestive loci affecting lesion size but not lipoprotein levels were identified. Many of these were recapitulated in an independent confirmatory cross. In summary, two independently performed crosses between C57BL/6 and FVB/N Apoe-deficient mice have revealed several previously unreported atherosclerosis susceptibility loci that are distinct from loci linked to lipoprotein levels.

Published

2002

2. Characterization of Alu Repeats That Are Associated with Trinucleotide and Tetranucleotide Repeat Microsatellites

Author

Julie M. Gastier, Jacqueline C. Pulido, Val C. Sheffield, Tom Brody, Kenneth H. Buetow, Geoffrey M. Duyk, Jeffrey C. Murray, and Chandri N. Yandava

Subjects

Genetics, Subfamily, Genome, Human, Repetitive Sequences, Chromosome Mapping, Alu element, Biology, Genome, Homology (biology), Mice, Genetic marker, Animals, Humans, Microsatellite, Multiplex, Chromosomes, Artificial, Yeast, Genetics (clinical), Microsatellite Repeats, Repetitive Sequences, Nucleic Acid

Abstract

The association of subclasses of Alu repetitive elements with various classes of trinucleotide and tetranucleotide microsatellites was characterized as a first step toward advancing our understanding of the evolution of microsatellite repeats. In addition, information regarding the association of specific classes of microsatellites with families of Alu elements was used to facilitate the development of genetic markers. Sequences containingAlu repeats were eliminated because unique primers could not be designed. Various classes of microsatellites are associated with different classes of Alu repeats. Very abundant and poly(A)-rich microsatellite classes (ATA, AATA) are frequently associated with an evolutionarily older subclass of Alurepeats, AluSx, whereas most of GATA and CA microsatellites are associated with a recent Alu subfamily, AluY. Our observations support all three possible mechanisms for the association of Alu repeats to microsatellites. Primers designed using a set of sequences from a particular microsatellite class showed higher homology with more sequences of that class than probes designed for other classes. We developed an efficient method of prescreening GGAA and ATA microsatellite clones for Alu repeats with probes designed in this study. We also showed that Alu probes labeled in a single reaction (multiplex labeling) could be used efficiently for prescreening of GGAA clones. Sequencing of these prescreened GGAA microsatellites revealed only 5% Alu repeats. Prescreening with primers designed for ATA microsatellite class resulted in the reduction of the loss of markers from ∼50% to 10%. The newAlu probes that were designed have also proved to be useful inAlu–Alu fingerprinting.

Published

1997

3. Novel Mutations and a Mutational Hotspot in the M0DY3 Gene

Author

M Alexandra Glucksmann, Markku Lehto, Olga Tayber, Susan Scotti, Lucy Berkemeier, Jacqueline C Pulido, Ye Wu, Waan-Jeng Nir, Lei Fang, Paul Markel, Kevin D. Munnelly, Jill Goranson, Marju Orho, Brian M Young, Jennifer L Whitacre, Cheryl McMenimen, Michael Wantman, Tlinamija Tuomi, James Warram, Carol M Forsblom, Martin Carlsson, James Rosenzweig, Giulia Kennedy, Geoffrey M Duyk, Andrzej S Krolewski, Leif C Groop, and Jeffrey D Thomas

Subjects

Genetics, Exon, Glucokinase, Endocrinology, Diabetes and Metabolism, Internal Medicine, Hepatocyte Nuclear Factor 1-Beta, Missense mutation, Locus (genetics), Insertion, TCF4, Biology, Gene

Abstract

Maturity-onset diabetes of the young 3 (MODY3) is a type of NIDDM caused by mutations in the transcription factor hepatocyte nuclear factor-la (HNF-la) located on chromosome 12q. We have identified four novel HNF-la missense mutations in M0DY3 families. In four additional and unrelated families, we observed an identical insertion mutation that had occurred in a polycytidine tract in exon 4. Among those families, one exhibited a de novo mutation at this location. We propose that instability of this sequence represents a general mutational mechanism in M0DY3. We observed no HNFla mutations among 86 unrelated late-onset diabetic patients with relative insulin deficiency. Hence mutations in this gene appear to be most strongly associated with early-onset diabetes. Diabetes 46:1081-1086,1997 MODY. The MODY1 locus, on chromosome 20q, was shown to be linked in a single extended family (2). M0DY1 was recently shown to be caused by mutations in the transcription factor hepatocyte nuclear factor-la (HNF4a) (3). MODY2, located on chromosome 7p (4), is caused by mutations in the glucokinase gene (5). MODY3 was mapped to chromosome 12q (6) and is known to be caused by mutations in another transcription factor, HNF-la (7). Although the relative prevalence of these MODY subtypes varies regionally (8-10), families linked to chromosome 12q are the most frequently described. The glucokinase defects in MODY2 interfere with glucose uptake, resulting in hyperglycemia (5). Although the mechanism of hyperglycemia in MODY1 and MODY3 is not yet understood, phenotypic characterization of these families has shown a deficient insulin secretion response to glucose (11-13). We report here the characterization of the MODY3 gene

Published

1997

4. Identification and mutation analysis of the complete gene for Chediak–Higashi syndrome

Author

Deborah L. Nagle, Karen J. Moore, Barry J. Dussault, Peer Bork, Richard A. Spritz, Elizabeth A. Woolf, Geoffrey M. Duyk, Mohammad A. Karim, Donald J. Misumi, Charles M. Perou, Lisa Holmgren, Sonja H. McGrail, and Raymond E. Boissy

Subjects

Genetics, integumentary system, Chédiak–Higashi syndrome, Alternative splicing, Biology, medicine.disease, Inclusion bodies, Gene mapping, hemic and lymphatic diseases, Lysosomal trafficking regulator, medicine, Vacuolar Sorting Protein VPS15, medicine.symptom, Gene, Hypopigmentation

Abstract

Chediak-Higashi syndrome (CHS) is a rare, autosomal recessive disorder characterized by hypopigmentation, severe immunologic deficiency with neutropenia and lack of natural killer (NK) cells, a bleeding tendency and neurologic abnormalities. Most patients die in childhood. The CHS hallmark is the occurrence of giant inclusion bodies and organelles in a variety of cell types, and protein sorting defects into these organelles. Similar abnormalities occur in the beige mouse, the proposed model for human CHS. Two groups have recently reported the identification of the beige gene, however the two cDNAs were not at all similar. Here we describe the sequence of a human cDNA homologous to mouse beige, identify pathologic mutations and clarify the discrepancies of the previous reports. Analysis of the CHS polypeptide demonstrates that its modular architecture is similar to the yeast vacuolar sorting protein, VPS15.

Published

1996

5. Sets of short tandem repeat polymorphisms for efficient linkage screening of the human genome

Author

Val C. Sheffield, James L. Weber, Geoffrey M. Duyk, and Jan Dubovsky

Subjects

Chromosomes, Human, Pair 14, Genetic Markers, Male, Linkage (software), Genetics, Polymorphism, Genetic, Genetic Linkage, Genome, Human, General Medicine, Biology, Polymerase Chain Reaction, Genome, Loss of heterozygosity, Gene mapping, Genetic linkage, Genetic marker, Humans, Microsatellite, Female, Human genome, Molecular Biology, Genetics (clinical), Repetitive Sequences, Nucleic Acid

Abstract

For the purpose of initial screening of the human genome in linkage mapping, two overlapping sets of high quality short tandem repeat polymorphisms (STRPs) which span the autosomes have been assembled. The higher density set contains a total of 363 markers with an average heterozygosity of 79% and an average sex-equal genetic distance between markers of 10.5 cM. The lower density set, which is a subset of the other, contains 156 markers with an average heterozygosity of 80% and an average spacing of 26.5 cM. Tri- and tetranucleotide STRPs comprised 47 and 63%, respectively, of the markers within the higher and lower density sets. Markers within the screening sets were selected to have maximum quality, where quality was defined as a blend of high informativeness, strong amplification under standard PCR conditions, low amplification background, and ease in scoring. The screening sets along with combinations of STRPs which can be amplified and electrophoresed simultaneously are available electronically through anonymous ftp.

Published

1995

6. A collection of tri- and tetranucleotide repeat markers used to generate high quality, high resolution human genome-wide linkage maps

Author

John Zhong, Jeffrey C. Murray, Anne McClain, Thomas R. Businga, Titia Scherpler, Dee Ann Even, Jacqueline C. Pulido, Kenneth H. Buetow, James L. Weber, John Gilliam, Geoffrey M. Duyk, Chandri N. Yandava, Kerry Wiles, John S. Beck, Sara L.F. Sunden, Gretel Mattes, Julie M. Gastier, and Val C. Sheffield

Subjects

Genetic Markers, Genotype, Genetic Linkage, Computational biology, Biology, Polymerase Chain Reaction, Genome, Tandem repeat, Gene mapping, Genetic linkage, Genetics, Chromosomes, Human, Humans, Family, Molecular Biology, Genotyping, Genetics (clinical), DNA Primers, Repetitive Sequences, Nucleic Acid, Linkage (software), Polymorphism, Genetic, Base Sequence, Genome, Human, Genetic Carrier Screening, Chromosome Mapping, General Medicine, Microsatellite, Human genome

Abstract

We report a collection of tri- and tetranucleotide repeat sequence polymorphic markers used to construct genome-wide human linkage maps. Using a strategy of marker selection to create libraries highly enriched for the presence of specific tandem repeat elements, we have developed over 2000 high heterozygosity, easy-to-use tri- and tetranucleotide short tandem repeat polymorphisms (STRPs). To date, over 1300 of these markers have been genotyped on the CEPH reference families. Additional STRPs were assigned to chromosomes using human monochromosomal somatic cell hybrids. The linkage maps constructed with these markers have been integrated with other CEPH genotypes into a comprehensive high density linkage map. These STRPs have been shown to be robust for genotyping in a variety of laboratories using a variety of methods. The high quality of these STRPs makes them ideal candidates for use in genome-wide linkage searches. The integration of these markers with physical mapping reagents and other genetic markers will create a resource for moving from genome-wide linkage searches to rapid sublocalization of disease loci.

Published

1995

7. MATS: a rapid and efficient method for the development of microsatellite markers from YACs

Author

Jacqueline C. Pulido, Hong Chen, and Geoffrey M. Duyk

Subjects

Genetic Markers, Yeast artificial chromosome, Positional cloning, Molecular Sequence Data, Restriction Mapping, Saccharomyces cerevisiae, DNA, Satellite, Molecular cloning, Gene mutation, Biology, Polymerase Chain Reaction, Gene mapping, Genetics, Cloning, Molecular, DNA, Fungal, Chromosomes, Artificial, Yeast, DNA Primers, Gene Library, Sequence Tagged Sites, Base Sequence, Contig, Genetic Techniques, Suppression subtractive hybridization, Microsatellite, Oligonucleotide Probes

Abstract

In this report, we describe the successful application of a rapid and efficient procedure, based on subtractive hybridization and PCR amplification, for generating microsatellite-based markers directly from yeast artificial chromosomes (YACs). This strategy, termed MATS (marker addition through subtraction), exploits the fact that the only difference between a yeast host strain harboring a YAC and the host strain alone is the artificial chromosome. Given the low complexity of the yeast genome and relatively large target size presented by a YAC, only a single round of subtraction is required before amplification of the target sequences (YAC) and cloning into a plasmid vector for further analysis. Several key steps have been designed to achieve optimal subtraction and to obtain preferential amplification and recovery of the target sequences. Methods for efficient construction of small insert libraries and rapid, nonradioactive screening have also been integrated into the protocol. Using a 750-kb YAC as a target, we identified a minimum of 14 unique microsatellite containing clones, leading to the development of 12 polymorphic STSs (sequence-tagged sites). These new markers will facilitate the genetic localization of targeted locus and allow the accurate ordering by STS content mapping of a cloned contig spanning the interval. In addition to the utility of this approach in positional cloning, this strategy may provide an approach for filling gaps in the emerging genetic maps.

Published

1995

8. Specific isolation of 3′-terminal exons of human genes by exon trapping

Author

Geoffrey M. Duyk, J.T. den Dunnen, G.J.B. van Ommen, and Nicole A. Datson

Subjects

RNA Splicing, Molecular Sequence Data, Biology, Transfection, Exon shuffling, Polymerase Chain Reaction, Cell Line, Exon, Exon trapping, Gene cluster, Genetics, Humans, Cloning, Molecular, Gene, Base Sequence, Nucleic acid sequence, Nucleic Acid Hybridization, Exons, Cosmids, Molecular biology, Globins, genomic DNA, Tandem exon duplication, Poly A, Chromosomes, Human, Pair 16

Abstract

Exon trapping is a method to functionally clone expressed sequences from genomic DNA. We have previously developed the vector system pETV-SD2, which contains only a splice donor site (SD) followed by a LacZ gene, allowing trapping of internal exons of human genes by blue-white selection. We now describe the adaptation of the same system for the efficient trapping of 3'-terminal exons, by using different RT-PCR primers in a 3' RACE reaction. The addition of a T7 promoter to the RT-PCR products derived from pETV-SD2 allows their amplification in an isothermic amplification reaction called NASBA (nucleic acid sequence-based amplification reaction) and results in a strong signal from amplified 3' exons in addition to a great reduction of non-specific background. As a test for the system, 3' exon trapping was performed using a cosmid containing the alpha-globin gene cluster on chromosome 16. The 3'-terminal exons of the human alpha 1-, zeta 2-, and theta-globin genes were trapped, as well as a correctly spliced and polyadenylated sequence in the 3' flanking region of the alpha 1-globin gene. This exon appears to belong to a previously unidentified gene within the alpha-globin gene cluster. This 3' exon trapping strategy should facilitate the cloning of genes from large genomic regions.

Published

1994

9. Linkage of Bardet–Biedl syndrome to chromosome 16q and evidence for non–allelic genetic heterogeneity

Author

Geoffrey M. Duyk, Anne E. Kwitek-Black, Khalil Elbedour, Ruti Parvari, Chandra Naidu Yandava, Val C. Sheffield, Rivka Carmi, Edwin M. Stone, and Kenneth H. Buetow

Subjects

Male, BBS2, congenital, hereditary, and neonatal diseases and abnormalities, Genetic Linkage, BBS5, Locus (genetics), Biology, Bardet–Biedl syndrome, Intellectual Disability, Genetics, medicine, Humans, Obesity, Allele, Polydactyly, Genetic heterogeneity, Hypogonadism, Homozygote, Chromosome Mapping, Disease gene identification, medicine.disease, Pedigree, Female, Lod Score, Chromosomes, Human, Pair 16, Retinitis Pigmentosa

Abstract

Bardet-Biedl syndrome is an autosomal recessive disorder characterized by mental retardation, obesity, retinitis pigmentosa, polydactyly and hypogonadism. Other findings include hypertension, diabetes mellitus and renal and cardiovascular anomalies. We have performed a genome-wide search for linkage in a large inbred Bedouin family. Pairwise analysis established linkage with the locus D16S408 with no recombination and a lod score of 4.2. A multilocus lod score of 5.3 was observed. By demonstrating homozygosity, in all affected individuals, for the same allele of marker D16S408, further support for linkage is found, and the utility of homozygosity mapping using inbred families is demonstrated. In a second family, linkage was excluded at this locus, suggesting non-allelic genetic heterogeneity in this disorder.

Published

1993

10. Traces of her workings

Author

Julie M. Gastier, Geoffrey M. Duyk, and Robert F. Mueller

Subjects

Genetics, Art history, Biology

Published

1992

11. Identification of a germ-line mutation in the p53 gene in a patient with an intracranial ependymoma

Author

Val C. Sheffield, Laleh Daneshvar, Andrew K. Metzger, Philip H. Cogen, Geoffrey M. Duyk, and Michael S. B. Edwards

Subjects

Male, Ependymoma, Molecular Sequence Data, Biology, Gene mutation, medicine.disease_cause, Malignancy, Polymerase Chain Reaction, Cancer syndrome, Germline mutation, Sequence Homology, Nucleic Acid, Leukocytes, medicine, Animals, Humans, Genes, Tumor Suppressor, Amino Acid Sequence, Codon, Genetics, Mutation, Multidisciplinary, Base Sequence, Brain Neoplasms, Retinoblastoma, DNA, Neoplasm, medicine.disease, Pedigree, Child, Preschool, Cancer research, Female, Tumor Suppressor Protein p53, Oligonucleotide Probes, Carcinogenesis, Polymorphism, Restriction Fragment Length, Research Article

Abstract

We detected a germ-line mutation of the p53 gene in a patient with a malignant ependymoma of the posterior fossa. This mutation, which was found at codon 242, resulted in an amino acid substitution in a highly conserved site of exon 7 of the p53 gene; the same mutation was found in both the germ-line and the tumor tissue. This is the most common region of previously described somatic p53 mutations in tumor specimens and of the germ-line p53 mutations in patients with the Li-Fraumeni cancer syndrome. Evaluation of the patient's family revealed several direct maternal and paternal relatives who had died at a young age from different types of cancer. The association of a germ-line p53 mutation with an intracranial malignancy and a strong family history of cancer suggests that p53 gene mutations predispose a person to malignancy and, like retinoblastoma mutations, may be inherited.

Published

1991

12. The knockout mouse project

Author

Thomas F. Vogt, Wolfgang Wurst, Harald von Melchner, Alexandra L. Joyner, Brian Zambrowicz, Francis Stewart, Terry Magnuson, William C. Skarnes, Harold E. Varmus, Susan M. Dymecki, Philippe Soriano, Mario R. Capecchi, Jonathan D. Pollock, Allan Bradley, Mark W. Moore, William F. Dove, J.T. Eppig, Stephen G. Young, Arthur T. Sands, Richard P. Woychik, Lyuba Varticovski, Allen D. Roses, Jay Snoddy, D. Stewart, Geoff Hicks, Nathaniel Heintz, Francis S. Collins, James F. Battey, Brian Seed, Christopher P. Austin, Franziska B. Grieder, Thomas R. Insel, George D. Yancopoulos, Geoffrey M. Duyk, Bruce Stillman, Andras Nagy, Beverly H. Koller, Maja Bucan, Kevin C K Lloyd, Jan A. Witkowski, and Inder M. Verma

Subjects

Genetics, Mice, Knockout, Genetic Research, Biology, Phenotype, Article, International Knockout Mouse Consortium, Mice, Gene trapping, Knockout mouse, Database construction, Animals, Research Embryo Creation, Gene knockout, Alleles

Abstract

Mouse knockout technology provides a powerful means of elucidating gene function in vivo, and a publicly available genome-wide collection of mouse knockouts would be significantly enabling for biomedical discovery. To date, published knockouts exist for only about 10% of mouse genes. Furthermore, many of these are limited in utility because they have not been made or phenotyped in standardized ways, and many are not freely available to researchers. It is time to harness new technologies and efficiencies of production to mount a high-throughput international effort to produce and phenotype knockouts for all mouse genes, and place these resources into the public domain.

Published

2004

13. Construction of Small-Insert Libraries Enriched for Short Tandem Repeat Sequences by Marker Selection

Author

Jacqueline C. Pulido and Geoffrey M. Duyk

Subjects

Genetics, chemistry.chemical_compound, chemistry, Oligonucleotide, Phagemid, DNA replication, Genomic library, Biology, Primer (molecular biology), DNA, Primer extension, Insert (molecular biology)

Abstract

These protocols construct a representative small-insert genomic DNA library in a phagemid vector. First, size-selected DNA fragments are ligated into a phagemid vector. In the second protocol, the resulting small-insert phagemid library is propagated in a bacterial strain combining mutations at the dut and ung loci, which permit incorporation of uracil in place of thymidine during DNA replication. Infection of the phagemid library with M13 helper phage permits recovery of this library as single-stranded DNA (ssDNA). Finally, this uracil-substituted ssDNA is used as a template for primer extension using an oligonucleotide whose sequence corresponds to the STR class of interest [e.g., (GATA)10] as primer. The products of this primer-extension reaction are transformed into an E. coli strain maintaining wild-type genes at the dut and ung loci. Under these conditions, uracil-substituted ssDNA will be restricted from growing by the host-encoded uracil-N-glycosylase, while the primer-extended products are capable of replicating.

Published

2001

14. A genetic screen for mutations that disrupt an auditory response in Drosophila melanogaster

Author

Geoffrey M. Duyk, Norbert Perrimon, and Daniel F. Eberl

Subjects

Auditory perception, Genetics, Mutation, Multidisciplinary, biology, Behavior, Animal, media_common.quotation_subject, Mutant, Mutagenesis (molecular biology technique), Genes, Insect, Biological Sciences, biology.organism_classification, medicine.disease_cause, Phenotype, Courtship, Drosophila melanogaster, medicine, Auditory Perception, Animals, media_common, Genetic screen

Abstract

Hearing is one of the last sensory modalities to be subjected to genetic analysis in Drosophila melanogaster . We describe a behavioral assay for auditory function involving courtship among groups of males triggered by the pulse component of the courtship song. In a mutagenesis screen for mutations that disrupt the auditory response, we have recovered 15 mutations that either reduce or abolish this response. Mutant audiograms indicate that seven mutants reduced the amplitude of the response at all intensities. Another seven abolished the response altogether. The other mutant, 5L3 , responded only at high sound intensities, indicating that the threshold was shifted in this mutant. Six mutants were characterized in greater detail. 5L3 had a general courtship defect; courtship of females by 5L3 males also was affected strongly. 5P1 males courted females normally but had reduced success at copulation. 5P1 and 5N18 showed a significant decrement in olfactory response, indicating that the defects in these mutations are not specific to the auditory pathway. Two other mutants, 5M8 and 5N30 , produced amotile sperm although in 5N30 this phenotype was genetically separable from the auditory phenotype. Finally, a new adult circling behavior phenotype, the pirouette phenotype, associated with massive neurodegeneration in the brain, was discovered in two mutants, 5G10 and 5N18 . This study provides the basis for a genetic and molecular dissection of auditory mechanosensation and auditory behavior.

Published

1997

15. Identification of the murine beige gene by YAC complementation and positional cloning

Author

Liangtao Li, Karen J. Moore, Barry J. Dussault, Charles M. Perou, Monica J. Justice, Thomas H. Brody, Elizabeth A. Woolf, Lisa Holmgren, Cheryl A. Monroe, Robert J. Pryor, Sonja H. McGrail, Deborah L. Nagle, Donald J. Misumi, Jerry Kaplan, and Geoffrey M. Duyk

Subjects

Positional cloning, Sequence analysis, Mutant, Molecular Sequence Data, Vesicular Transport Proteins, Mice, Inbred Strains, Biology, Homology (biology), Mice, hemic and lymphatic diseases, Genetics, Animals, Humans, Amino Acid Sequence, Cloning, Molecular, Peptide sequence, Gene, Chromosomes, Artificial, Yeast, Base Sequence, Sequence Homology, Amino Acid, Genetic Complementation Test, Nucleic acid sequence, Intracellular Signaling Peptides and Proteins, Chromosome Mapping, Proteins, Sequence Analysis, DNA, Mice, Mutant Strains, Complementation, Protein Biosynthesis, Mutation, Chediak-Higashi Syndrome

Abstract

The beige mutation is a murine autosomal recessive disorder, resulting in hypopigmentation, bleeding and immune cell dysfunction. The gene defective in beige is thought to be a homologue of the gene for the human disorder Chediak-Higashi syndrome. We have identified the murine beige gene by in vitro complementation and positional cloning, and confirmed its identification by defining mutations in two independent mutant alleles. The sequence of the beige gene message shows strong nucleotide homology to multiple human ESTs, one or more of which may be associated with the Chediak-Higashi syndrome gene. The amino acid sequence of the Beige protein revealed a novel protein with significant amino acid homology to orphan proteins identified in Saccharomyces cerevisiae, Caenorhabditis elegans and humans.

Published

1996

16. Development of a screening set for new (CAG/CTG)n dynamic mutations

Author

Kenneth H. Buetow, Thomas R. Businga, Julie M. Gastier, Thomas Brody, Shanak Maitra, Jeffrey C. Murray, Xintong Hu, Val C. Sheffield, Geoffrey M. Duyk, Sara L.F. Sunden, Thomas J. Hudson, Mark S. Boguski, and Jacqueline C. Pulido

Subjects

musculoskeletal diseases, Male, congenital, hereditary, and neonatal diseases and abnormalities, Genotype, Minisatellite Repeats, Biology, Sequence-tagged site, Gene mapping, Trinucleotide Repeats, Genetics, Chromosomes, Human, Humans, Cloning, Molecular, Sequence Tagged Sites, Polymorphism, Genetic, Base Sequence, Genetic Diseases, Inborn, Chromosome, Chromosome Mapping, Molecular biology, nervous system diseases, Genetic marker, Mutation, Cosmid, Microsatellite, Female, Trinucleotide repeat expansion

Abstract

The expansion of a (CAG/CTG) n triplet repeat has been found to be associated with at least seven genetic diseases, suggesting that this mechanism of disease may be fairly common. To accelerate the discovery of new loci containing (CAG/CTG) n triplet expansions, we have isolated numerous genomic clones containing this class of repeats. We have developed 338 sequence-tagged sites (STSs) containing (CAG/CTG) n repeat sequences. Two hundred ninety-nine STSs were unambiguously assigned to chromosomes, and 89 of the total were assigned to YACs. The 141 STSs that were developed based on (CAG/CTG) n repeats of at least seven units were genotyped on four reference CEPH individuals to estimate their polymorphic quality.

Published

1996

17. Structural motifs of the PKD1 protein

Author

M.A. Glücksmann-Kuis, Stephen T. Reeders, Michael C. Schneider, M. Pohlschmidt, Geoffrey M. Duyk, C. Löhning, Peer Bork, and Anna-Maria Frischauf

Subjects

Genetics, Transplantation, TRPP Cation Channels, PKD1, Structural gene, Proteins, Biology, medicine.disease, Polycystic Kidney, Autosomal Dominant, Gene product, Complete sequence, Structure-Activity Relationship, Genes, Nephrology, Polycystic kidney disease, medicine, Gene family, Humans, Structural motif, Gene

Abstract

The complete sequence of the polycystic kidney disease gene (PKD1) and its transcript have been described. The predicted protein is not a member of a previously described gene family, but contains several structural motifs that are present in proteins of known function. Most of these domains are present in the extracellular parts of proteins involved in interactions with other proteins and carbohydrates. The PKD1 gene product also contains potential trans- membrane sequences. The molecule is likely to be involved in cell-cell or cell-matrix interactions, which is consistent with the different manifestations of polycystic kidney disease.

Published

1996

18. Survey of trinucleotide repeats in the human genome: assessment of their utility as genetic markers

Author

Jacqueline C. Pulido, Val C. Sheffield, James L. Weber, Julie M. Gastier, Jeffrey C. Murray, Sara L.F. Sunden, Kenneth H. Buetow, Thomas Brody, Thomas J. Hudson, and Geoffrey M. Duyk

Subjects

Genetic Markers, Molecular Sequence Data, Biology, Polymerase Chain Reaction, Loss of heterozygosity, Sequence-tagged site, Gene mapping, Tandem repeat, Terminology as Topic, Genetics, Chromosomes, Human, Humans, Molecular Biology, Genetics (clinical), DNA Primers, Repetitive Sequences, Nucleic Acid, Sequence Tagged Sites, Polymorphism, Genetic, Base Sequence, Genome, Human, Chromosome Mapping, General Medicine, Genetic marker, Microsatellite, Human genome, Trinucleotide repeat expansion

Abstract

Genetic markers based upon PCR amplification of short tandem repeat-containing sequence tagged sites (STSs) have become the standard for genetic mapping. We have completed a survey based on the direct isolation of representative members of each of the 10 trinucleotide repeat classes to determine their relative abundance, repeat size distribution, and general utility as genetic markers. Trinucleotide repeats, depending on the repeat class, are one to two orders of magnitude less frequent than (AC) n repeats. The average size of trinucleotide repeats sequenced was less than 15 repeat units in length, and only three of the STSs developed for this study demonstrated more than 25 repeats units. The (AAT) n class of repeats are the most abundant and also the most frequently polymorphic. Other classes of trinucleotide repeat classes observed to be frequently polymorphic include (AAC) n , (ACT) n , (ATC) n and (AAG) n ; however, the relative abundance of these classes is less than that observed for the (AAT) n class of repeats. Based upon this initial survey, we have initiated saturation cloning of the (AAT) n class of repeats. At the time of submission of this manuscript, we have developed, as part of the Cooperative Human Linkage Center (CHLC), more than 415 new high heterozygosity (AAT) n genetic markers (more than two alleles in four individuals) and 200 new low heterozygosity (AAT) n STSs from this larger screening effort combined with the initial survey.

Published

1995

19. cDNA cloning, tissue distribution, and chromosomal localization of Ocp2, a gene encoding a putative transcription-associated factor predominantly expressed in the auditory organs

Author

David P. Corey, Karen B. Avraham, Nancy A. Jenkins, Isolde Thalmann, Joe C. Adams, Neal G. Copeland, Geoffrey M. Duyk, Hong Chen, David R. Beier, and Rudi Thalmann

Subjects

Male, DNA, Complementary, Guinea Pigs, Molecular Sequence Data, RNA polymerase II, Biology, Polymerase Chain Reaction, Antibodies, Mice, Transcription (biology), Gene expression, otorhinolaryngologic diseases, Genetics, Transcriptional regulation, medicine, Animals, Tissue Distribution, Amino Acid Sequence, RNA, Messenger, Cloning, Molecular, Transcription factor, Organ of Corti, S-Phase Kinase-Associated Proteins, DNA Primers, Messenger RNA, Base Sequence, cDNA library, Chromosome Mapping, Molecular biology, Immunohistochemistry, medicine.anatomical_structure, biology.protein, sense organs, Transcription Factors

Abstract

We report the cloning of the Ocp2 gene encoding OCP-II from a guinea pig organ-of-Corti cDNA library. The predicted open reading frame encodes a protein of 163 amino acids with an estimated molecular mass of 18.6 kDa. A homology search revealed that Ocp2 shares significant sequence similarity with p15, a subunit of transcription factor SIII that regulates the activity of the RNA polymerase II elongation complex. The Ocp2 messenger RNA is expressed abundantly in the cochlea while not significantly in any other tissues examined, including brain, eye, heart, intestine, kidney, liver, lung, thigh muscle, and testis, demonstrating that the expression of this gene may be restricted to auditory organs. A polyclonal antiserum was raised against the N-terminal region of OCP-II. Immunohistochemical staining of paraffin-embedded sections of the cochlea showed that OCP-II is localized abundantly in nonsensory cells in the organ of Corti; in addition, it was also detected, at a lower concentration, in vestibular sensory organs, as well as auditory and vestibular brain stem nuclei. The Ocp2 gene was mapped to mouse chromosome 4 as well as 11. Our results suggest that OCP-II may be involved in transcription regulation for the development or maintenance of specialized functions of the inner ear.

Published

1995

20. Human genetic map. Genome maps V. Wall chart

Author

Kenneth H. Buetow, Susan Ludwigsen, Titia Scherpbier-Heddema, John Quillen, Jeffrey C. Murray, Val C. Sheffield, Geoffrey M. Duyk, James L. Weber, Jean Weissenbach, Gabor Gyapay, Colette Dib, Alain Vignal, Ray White, Norisada Matsunami, Steven Gerken, Roberta Mells, Hans Albertsen, Kenneth Ward, Rosemarie Plaetke, Shannon Odelberg, David Ward, Patricia Bray-Ward, Joan Menninger, Jonathan Lieman, Trushna Desai, and Amy Banks

Subjects

Genetic Markers, Multidisciplinary, Chart, Evolutionary biology, Genetic marker, Genome, Human, Human Genome Project, Chromosome Mapping, Chromosomes, Human, Humans, Genome project, Biology, Genome

Published

1994

21. Identification of a Bardet-Biedl syndrome locus on chromosome 3 and evaluation of an efficient approach to homozygosity mapping

Author

Sara L.F. Sunden, Geoffrey M. Duyk, Khalil Elbedour, Val C. Sheffield, Rivka Carmi, Edwin M. Stone, Tatiana Rokhlina, Darryl Y. Nishimura, and Anne E. Kwitek-Black

Subjects

BBS2, Male, congenital, hereditary, and neonatal diseases and abnormalities, Genetic Linkage, Locus (genetics), Biology, Chromosome 16, Bardet–Biedl syndrome, Locus heterogeneity, Genetics, medicine, Humans, Molecular Biology, Genetics (clinical), Laurence-Moon Syndrome, Polydactyly, Homozygote, Chromosome Mapping, Infant, General Medicine, DNA, Disease gene identification, medicine.disease, nervous system diseases, Pedigree, Chromosome 3, Evaluation Studies as Topic, Female, Chromosomes, Human, Pair 3

Abstract

Bardet-Biedl syndrome is an autosomal recessive disorder characterized by mental retardation, obesity, retinitis pigmentosa, polydactyly and hypogonadism. Individuals with this disorder also have an increased incidence of hypertension, diabetes mellitus, and renal and cardiac anomalies. We previously identified a locus on chromosome 16 causing this disorder, and provided evidence that Bardet-Biedl syndrome is hetero-geneous. In this study, we identify another Bardet-Biedl syndrome locus on chromosome 3 and confirm the non-allelic heterogeneity of this disorder in Bedouin populations. In addition, we demonstrate the feasibility of using pooled DNA samples from members of large kindreds as an efficient approach to homozygosity mapping

Published

1994

22. A trinucleotide repeat polymorphism in XT00444 (D13S635E)

Author

C N Yandava, Geoffrey M. Duyk, Hugh Watkins, and V Meyers

Subjects

Genetics, Polymorphism, Genetic, Base Sequence, Chromosomes, Human, Pair 13, Molecular Sequence Data, Gene Expression, Rodentia, General Medicine, Biology, Hybrid Cells, Polymerase Chain Reaction, Gene mapping, Oligodeoxyribonucleotides, Genetic marker, Microsatellite, Animals, Humans, Trinucleotide repeat expansion, Molecular Biology, Allele frequency, Gene, Genetics (clinical), Alleles, Repetitive Sequences, Nucleic Acid

Published

1994

23. Integrated human genome-wide maps constructed using the CEPH reference panel

Author

Geoffrey M. Duyk, James L. Weber, Kenneth H. Buetow, Susan Ludwigsen, T. Scherpbier-Heddema, Val C. Sheffield, Jeffrey C. Murray, and Zhenyuan Wang

Subjects

Genetics, Linkage (software), Genetic Markers, Information Services, Male, Polymorphism, Genetic, Databases, Factual, Genome, Human, High resolution, Chromosome Mapping, Biology, Polymerase Chain Reaction, Pedigree, Set (abstract data type), Gene mapping, Chromosomes, Human, Humans, Human genome, Female, France, Genotyping, Cartography, Algorithms

Abstract

High resolution linkage maps have proven to be invaluable tools in genetic investigations. We have assembled a collection of genetic maps constructed from primary data collected from investigators performing genotyping using the Centre Etude Polymorphism Humain (CEPH) reference pedigree panel. These maps were constructed using a rigorous, semi-automated map construction algorithm that evaluates the integrity of the maps during construction. Two classes of maps were produced: a high confidence "skeletal" set composed of 544 PCR based markers, and a more highly annotated "framework" set containing maps of 1,123 markers. Genetic map locations within the framework maps are provided for an additional 1,758 loci without statistically unique interval assignments.

Published

1994

24. An Exon Trapping System Providing Size Selection of Spliced Clones and Facilitating Direct Cloning

Author

Gert-Jan B. van Ommen, Nicole A. Datson, Johan T. den Dunnen, L. A. J. Blonden, and Geoffrey M. Duyk

Subjects

clone (Java method), Yeast artificial chromosome, Genetics, Cloning, genomic DNA, chemistry.chemical_compound, Exon trapping, chemistry, Cosmid, RNA, Biology, Molecular biology, DNA

Abstract

Exon trapping is a method to functionally clone expressed sequences from genomic DNA. We have developed an exon trapping procedure based on the use of vector pETVSD2. Cosmid DNA is partially digested and cloned in pETV-SD2. DNA of an entire library of subclones is introduced into COS-1 cells and transiently expressed. RNA is isolated and vector-derived transcripts are amplified by RT-PCR. Cloning of the RT-PCR products, which contain a ColEI-origin of replication and a supF marker, is established by NotI digestion and intramolecular circularisation. Due to their shorter length, spliced clones are preferentially amplified and cloned.

Published

1994

25. A denaturing gradient gel electrophoresis assay for sensitive detection of p53 mutations

Author

Anne E. Kwitek, Geoffrey M. Duyk, Val C. Sheffield, Phillip H. Cogen, Andrew K. Metzger, and John S. Beck

Subjects

Gel electrophoresis, Genetics, Mutation, Tumor suppressor gene, Base Sequence, Sequence analysis, Point mutation, Molecular Sequence Data, Nucleic acid sequence, Biology, medicine.disease_cause, Genes, p53, Molecular biology, Electrophoresis, Gel, Pulsed-Field, medicine, Humans, Point Mutation, Gene, Genetics (clinical), Temperature gradient gel electrophoresis

Abstract

p53 is a tumor suppressor gene located on 17p, a region of the human genome frequently deleted in tumors. Mutation of the p53 gene is an important step leading to development of many forms of human cancer. To simplify the analysis of tumors for p53 point mutations, we describe a GC-clamped denaturing gradient gel assay for detecting single-base substitutions within highly conserved regions of the p53 gene. This assay allows for efficient screening of tumors for single-base substitutions within the p53 gene and can be used to facilitate sequence analysis of p53 point mutations.

Published

1993

26. Exon trapping: a genetic screen to identify candidate transcribed sequences in cloned mammalian genomic DNA

Author

David R. Cox, Richard M. Myers, Suwon Kim, and Geoffrey M. Duyk

Subjects

Cloning, Genetics, Genomic Library, Multidisciplinary, Base Sequence, RNA Splicing, Genetic Vectors, Molecular Sequence Data, Exons, Molecular cloning, Biology, Cell Line, genomic DNA, Exon, Exon trapping, HLA Antigens, RNA splicing, Humans, Genomic library, Cloning, Molecular, Gene, Research Article

Abstract

Identification and recovery of transcribed sequences from cloned mammalian genomic DNA remains an important problem in isolating genes on the basis of their chromosomal location. We have developed a strategy that facilitates the recovery of exons from random pieces of cloned genomic DNA. The basis of this "exon trapping" strategy is that, during a retroviral life cycle, genomic sequences of nonviral origin are correctly spliced and may be recovered as a cDNA copy of the introduced segment. By using this genetic assay for cis-acting sequences required for RNA splicing, we have screened approximately 20 kilobase pairs of cloned genomic DNA and have recovered all four predicted exons.

Published

1990

27. Selective cleavage in the avian retroviral long terminal repeat sequence by the endonuclease associated with the alpha beta form of avian reverse transcriptase

Author

Anna Marie Skalka, Jonathan Leis, Geoffrey M. Duyk, and Mathew Longiaru

Subjects

Macromolecular Substances, Base pair, viruses, DNA, Recombinant, EcoRI, Biology, Avian sarcoma virus, Deoxyribonuclease EcoRI, Substrate Specificity, chemistry.chemical_compound, Cloning Site, Cloning, Molecular, Repetitive Sequences, Nucleic Acid, Genetics, Endodeoxyribonucleases, Multidisciplinary, Nucleic acid sequence, RNA-Directed DNA Polymerase, DNA Restriction Enzymes, Molecular biology, Long terminal repeat, Avian Sarcoma Viruses, chemistry, biology.protein, DNA, Research Article

Abstract

M13 recombinant DNA clones containing a 350-base sequence derived from the EcoRI fragment of two tandemly linked Rous-associated virus 2 (RAV-2) long terminal repeat (LTR) sequences have been used to map reverse transcriptase-associated endonuclease (RT-endonuclease) cleavage sites by primer extension studies. Under appropriate conditions, the alpha beta form of RT-endonuclease (composed of both the alpha and beta subunits) purified from Avian sarcoma virus (Pr-C and B-77 strains) introduces a specific break in the inverted complementary repeat sequence found at the junction of the LTRs. The cleavage sites occur in the same nucleotide sequence in (-) and (+) DNA strands; together they have the potential of generating a 6-base-pair staggered overlap that spans the junction. This supports the notion that the enzyme is involved in viral DNA integration. Other RT-endonuclease sites were analyzed. A second site, which occurs in the lac region of the M13 vector DNA upstream from the unique EcoRI cloning site, bears no apparent sequence homology to the site at the junction of the LTRs. However, it also lies within an inverted complementary repeat and, as is the case for the site in the LTR, the break occurs to the 5' side of the axis of symmetry. Cleavage at this second site is suppressed when the vector contains the RAV-2 LTR insert. Thus, the viral LTR appears to exert a cis effect that can influence a region over 300 base pairs away.

Published

1983

28. Identification and Characterization of the Mouse Obesity Gene tubby: A Member of a Novel Gene Family

Author

Ye Wu, Nathan D Lakey, Thomas Brody, Karen J. Moore, Janice A. Culpepper, George A. Carlson, Lisa Holmgren, Geoffrey D Alperin, John Lee, Patrick W. Kleyn, Jim Deeds, Elizabeth A. Woolf, Don J Misumi, Lucy R Berkemeier, Olga Tayber, Chris Ebeling, Linda Baldini, Olga Charlat, Jacqueline C. Pulido, Pei Shu, M.Alexandra Glücksmann-Kuis, Geoffrey M. Duyk, Steve G. Kovats, Brenda Kennedy, Fiona Hawkins, Hong Chen, and Wei Fan

Subjects

Positional cloning, Molecular Sequence Data, Gene Expression, Mice, Obese, Tubby protein, Biology, Polymerase Chain Reaction, General Biochemistry, Genetics and Molecular Biology, Exon, Mice, Gene expression, Animals, Obesity, RNA, Messenger, Allele, Cloning, Molecular, Gene, In Situ Hybridization, Adaptor Proteins, Signal Transducing, Genetics, Brain Chemistry, Base Sequence, Sequence Homology, Amino Acid, Biochemistry, Genetics and Molecular Biology(all), Alternative splicing, Intron, Chromosome Mapping, Genetic Variation, Proteins, Exons, Molecular biology, Alternative Splicing, Mutation, Insulin Resistance

Abstract

The mutated gene responsible for the tubby obesity phenotype has been identified by positional cloning. A single base change within a splice donor site results in the incorrect retention of a single intron in the mature tub mRNA transcript. The consequence of this mutation is the substitution of the carboxy-terminal 44 amino acids with 24 intron-encoded amino acids. The normal transcript appears to be abundantly expressed in the hypothalamus, a region of the brain involved in body weight regulation. Variation in the relative abundance of alternative splice products is observed between inbred mouse strains and appears to correlate with an intron length polymorphism. This allele of tub is a candidate for a previously reported diet-induced obesity quantitative trait locus on mouse chromosome 7.

29. Evidence That the Diabetes Gene Encodes the Leptin Receptor: Identification of a Mutation in the Leptin Receptor Gene in db/db Mice

Author

Xun Weng, Janice A. Culpepper, Karen J More, Hong Chen, Roger E. Breitbart, Elizabeth A. Woolf, Louis A. Tartaglia, Nathan D Lakey, Stephen J Ellis, Olga Charlat, Jay P. Morgenstern, Robert I. Tepper, and Geoffrey M. Duyk

Subjects

Leptin, DNA, Complementary, Molecular Sequence Data, Mice, Obese, Mice, Inbred Strains, Receptors, Cell Surface, Biology, medicine.disease_cause, Polymerase Chain Reaction, General Biochemistry, Genetics and Molecular Biology, Exon, Mice, medicine, Animals, Humans, Point Mutation, Amino Acid Sequence, Obesity, Receptors, Cytokine, DNA Primers, Mutation, Leptin receptor, Base Sequence, Sequence Homology, Amino Acid, Biochemistry, Genetics and Molecular Biology(all), Point mutation, Alternative splicing, Proteins, Molecular biology, Intracellular signal transduction, Db/db Mouse, Alternative Splicing, Diabetes Mellitus, Type 1, Phenotype, Receptors, Leptin, Signal transduction, Carrier Proteins, Signal Transduction

Abstract

OB-R is a high affinity receptor for leptin, an important circulating signal for the regulation of body weight. We identified an alternatively spliced transcript that encodes a form of mouse OB-R with a long intracellular domain. db/db mice also produce this alternatively spliced transcript, but with a 106 nt insertion that prematurely terminates the intracellular domain. We further identified a G→T point mutation in the genomic OB-R sequence in db/db mice. This mutation generates a donor splice site that converts the 106 nt region to a novel exon retained in the OB-R transcript. We predict that the long intracellular domain form of OB-R is crucial for initiating intracellular signal transduction, and as a corollary, the inability to produce this form of OB-R leads to the severe obese phenotype found in db/db mice.

30. A comprehensive human linkage map with centimorgan density

Author

Jeffrey C. Murray, Kenneth H. Buetow, James L. Weber, Susan Ludwigsen, Titia Scherpbier-Heddema, Frank Manion, John Quillen, Val C. Sheffield, Sara Sunden, Geoffrey M. Duyk, Jean Weissenbach, Gabor Gyapay, Colette Dib, Jean Morrissette, G. Mark Lathrop, Alain Vignal, Ray White, Norisada Matsunami, Steven Gerken, Roberta Mells, Hans Albertsen, Rosemarie Plaetke, Shannon Odelberg, David Ward, Jean Dausset, Daniel Cohen, and Howard Cann

Subjects

Genetics, Centimorgan, Multidisciplinary, Gene mapping, Genetic marker, Genetic linkage, Microsatellite, Human genome, Computational biology, Biology, Genome, Complete linkage

Abstract

In the last few years there have been rapid advances in developing genetic maps for humans, greatly enhancing our ability to localize and identify genes for inherited disorders. Through the collaborative efforts of three large groups generating microsatellite markers and the efforts of the 110 CEPH collaborators, a comprehensive human linkage map is presented here. It consists of 5840 loci, of which 970 are uniquely ordered, covering 4000 centimorgans on the sex-averaged map. Of these loci, 3617 are polymerase chain reaction-formatted short tandem repeat polymorphisms, and another 427 are genes. The map has markers at an average density of 0.7 centimorgan, providing a resource for ready transference to physical maps and achieving one of the first goals of the Human Genome Project--a comprehensive, high-density genetic map.

31. Characterization of the MODY3 phenotype - Early-onset diabetes caused by an insulin secretion defect

Author

Thomas Brettin, Jeffrey Thomas, M Gullstrom, Andrew Kirby, B Isomaa, Mikko Lehtovirta, T Kanninen, L Sarelin, Melanie M. Mahtani, M. Lehto, E. Widen, Carol Forsblom, Eric S. Lander, Marja-Riitta Taskinen, R C Turner, Geoffrey M. Duyk, A Hyrkkö, Tiinamaija Tuomi, Leif Groop, Marju Orho, and Susan E. Manley

Subjects

Adult, Male, medicine.medical_specialty, endocrine system diseases, Genotype, medicine.medical_treatment, Glutamate decarboxylase, Biology, Maturity onset diabetes of the young, Insulin resistance, Internal medicine, Diabetes mellitus, Insulin Secretion, medicine, Humans, Insulin, Chromosome 12, Aged, Aged, 80 and over, Glucokinase, Genetic Carrier Screening, Haplotype, nutritional and metabolic diseases, General Medicine, Middle Aged, medicine.disease, Pedigree, Endocrinology, Phenotype, Diabetes Mellitus, Type 2, Haplotypes, Female, Lod Score, Research Article

Abstract

Maturity-onset diabetes of the young (MODY) type 3 is a dominantly inherited form of diabetes, which is often misdiagnosed as non-insulin-dependent diabetes mellitus (NIDDM) or insulin-dependent diabetes mellitus (IDDM). Phenotypic analysis of members from four large Finnish MODY3 kindreds (linked to chromosome 12q with a maximum lod score of 15) revealed a severe impairment in insulin secretion, which was present also in those normoglycemic family members who had inherited the MODY3 gene. In contrast to patients with NIDDM, MODY3 patients did not show any features of the insulin resistance syndrome. They could be discriminated from patients with IDDM by lack of glutamic acid decarboxylase antibodies (GAD-Ab). Taken together with our recent findings of linkage between this region on chromosome 12 and an insulin-deficient form of NIDDM (NIDDM2), the data suggest that mutations at the MODY3/NIDDM2 gene(s) result in a reduced insulin secretory response, that subsequently progresses to diabetes and underlines the importance of subphenotypic classification in studies of diabetes.