Your search keyword '"Wang-Ting Hsieh"' showing total 27 results

1. The beneficial effects of commensal E. coli for colon epithelial cell recovery are related with Formyl peptide receptor 2 (Fpr2) in epithelial cells

Author

Keqiang Chen, John McCulloch, Rodrigo Das Neves, Gisele Rodrigues, Wang-Ting Hsieh, Wanghua Gong, Teizo Yoshimura, Jiaqiang Huang, Colm O’hUigin, Simone Difilippantonio, Matthew McCollum, Georgette Jones, Scott K. Durum, Giorgio Trinchieri, and Ji Ming Wang

Subjects

Commensal E. coli, Fpr2 −/− mice, Germ-free mice, Colitis, Regeneration, Diseases of the digestive system. Gastroenterology, RC799-869

Abstract

Abstract Background Formyl peptide receptor 2 (Fpr2) plays a crucial role in colon homeostasis and microbiota balance. Commensal E. coli is known to promote the regeneration of damaged colon epithelial cells. The aim of the study was to investigate the connection between E. coli and Fpr2 in the recovery of colon epithelial cells. Results The deficiency of Fpr2 was associated with impaired integrity of the colon mucosa and an imbalance of microbiota, characterized by the enrichment of Proteobacteria in the colon. Two serotypes of E. coli, O22:H8 and O91:H21, were identified in the mouse colon through complete genome sequencing. E. coli O22:H8 was found to be prevalent in the gut of mice and exhibited lower virulence compared to O91:H21. Germ-free (GF) mice that were pre-orally inoculated with E. coli O22:H8 showed reduced susceptibility to chemically induced colitis, increased proliferation of epithelial cells, and improved mouse survival. Following infection with E. coli O22:H8, the expression of Fpr2 in colon epithelial cells was upregulated, and the products derived from E. coli O22:H8 induced migration and proliferation of colon epithelial cells through Fpr2. Fpr2 deficiency increased susceptibility to chemically induced colitis, delayed the repair of damaged colon epithelial cells, and heightened inflammatory responses. Additionally, the population of E. coli was observed to increase in the colons of Fpr2 −/− mice with colitis. Conclusion Commensal E. coli O22:H8 stimulated the upregulation of Fpr2 expression in colon epithelial cells, and the products from E. coli induced migration and proliferation of colon epithelial cells through Fpr2. Fpr2 deficiency led to an increased E. coli population in the colon and delayed recovery of damaged colon epithelial cells in mice with colitis. Therefore, Fpr2 is essential for the effects of commensal E. coli on colon epithelial cell recovery.

Published

2023

2. Correction: The beneficial effects of commensal E. coli for colon epithelial cell recovery are related with Formyl peptide receptor 2 (Fpr2) in epithelial cells

Author

Keqiang Chen, John McCulloch, Rodrigo Das Neves, Gisele Rodrigues, Wang-Ting Hsieh, Wanghua Gong, Teizo Yoshimura, Jiaqiang Huang, Colm O’hUigin, Simone Diflippantonio, Matthew McCollum, Georgette Jones, Scott K. Durum, Giorgio Trinchieri, and Ji Ming Wang

Subjects

Diseases of the digestive system. Gastroenterology, RC799-869

Published

2023

3. Table S2 from T-Cell Deletion of MyD88 Connects IL17 and IκBζ to RAS Oncogenesis

Author

Stuart H. Yuspa, Giorgio Trinchieri, Maxwell Lee, Howard Yang, Asra Khan, Wang-Ting Hsieh, Lyudmila Lyakh, C. Andrew Stewart, Ren-Ming Dai, Loretta Smith, Megan Karwan, Laurie G. Kostecka, Jin-Qiu Chen, Amalia Sweet, Michelle J. Pan, Luowei Li, Shruti Naik, Mary Klosterman, Aleksandra M. Michalowski, Rosalba Salcedo, and Christophe Cataisson

Abstract

Supplemental table 2: List of genes from RNA profiling, the expression of which is significantly affected (by at least 1.5-fold change and FDR

Published

2023

4. Data from T-Cell Deletion of MyD88 Connects IL17 and IκBζ to RAS Oncogenesis

Author

Stuart H. Yuspa, Giorgio Trinchieri, Maxwell Lee, Howard Yang, Asra Khan, Wang-Ting Hsieh, Lyudmila Lyakh, C. Andrew Stewart, Ren-Ming Dai, Loretta Smith, Megan Karwan, Laurie G. Kostecka, Jin-Qiu Chen, Amalia Sweet, Michelle J. Pan, Luowei Li, Shruti Naik, Mary Klosterman, Aleksandra M. Michalowski, Rosalba Salcedo, and Christophe Cataisson

Abstract

Cancer development requires a favorable tissue microenvironment. By deleting Myd88 in keratinocytes or specific bone marrow subpopulations in oncogenic RAS-mediated skin carcinogenesis, we show that IL17 from infiltrating T cells and IκBζ signaling in keratinocytes are essential to produce a permissive microenvironment and tumor formation. Both normal and RAS-transformed keratinocytes respond to tumor promoters by activating canonical NF-κB and IκBζ signaling, releasing specific cytokines and chemokines that attract Th17 cells through MyD88-dependent signaling in T cells. The release of IL17 into the microenvironment elevates IκBζ in normal and RAS-transformed keratinocytes. Activation of IκBζ signaling is required for the expression of specific promoting factors induced by IL17 in normal keratinocytes and constitutively expressed in RAS-initiated keratinocytes. Deletion of Nfkbiz in keratinocytes impairs RAS-mediated benign tumor formation. Transcriptional profiling and gene set enrichment analysis of IκBζ−deficient RAS-initiated keratinocytes indicate that IκBζ signaling is common for RAS transformation of multiple epithelial cancers. Probing The Cancer Genome Atlas datasets using this transcriptional profile indicates that reduction of IκBζ signaling during cancer progression associates with poor prognosis in RAS-driven human cancers.Implications:The paradox that elevation of IκBζ and stimulation of IκBζ signaling through tumor extrinsic factors is required for RAS-mediated benign tumor formation while relative IκBζ expression is reduced in advanced cancers with poor prognosis implies that tumor cells switch from microenvironmental dependency early in carcinogenesis to cell-autonomous pathways during cancer progression.

Published

2023

5. Combined_supplemental_materials-Edmondson_et_al - Naturally Acquired Mouse Kidney Parvovirus Infection Produces a Persistent Interstitial Nephritis in Immunocompetent Laboratory Mice

Author

Edmondson, Elijah F., Wang-Ting Hsieh, Kramer, Josh A., Breed, Matthew W., Roelke-Parker, Melody E., Stephens-Devalle, Julie, Pate, Nathan M., Bassel, Laura L., Hollingshead, Melinda G., Baktiar O. Karim, Butcher, Donna O., Warner, Andrew C., Nagashima, Kunio, and Gulani, Jatinder

Subjects

70706 Veterinary Medicine, FOS: Clinical medicine, FOS: Veterinary sciences, 111599 Pharmacology and Pharmaceutical Sciences not elsewhere classified

Abstract

Combined_supplemental_materials-Edmondson_et_al for Naturally Acquired Mouse Kidney Parvovirus Infection Produces a Persistent Interstitial Nephritis in Immunocompetent Laboratory Mice by Elijah F. Edmondson, Wang-Ting Hsieh, Josh A. Kramer, Matthew W. Breed, Melody E. Roelke-Parker, Julie Stephens-Devalle, Nathan M. Pate, Laura L. Bassel, Melinda G. Hollingshead, Baktiar O. Karim, Donna O. Butcher, Andrew C. Warner, Kunio Nagashima and Jatinder Gulani in Veterinary Pathology

Published

2020

6. T-Cell Deletion of MyD88 Connects IL17 and IκBζ to RAS Oncogenesis

Author

Maxwell P. Lee, Stuart H. Yuspa, Christophe Cataisson, Megan Karwan, Ren-Ming Dai, Aleksandra M. Michalowski, Luowei Li, Lyudmila A. Lyakh, C. Andrew Stewart, Howard H. Yang, Amalia Sweet, Wang-Ting Hsieh, Mary Klosterman, Shruti Naik, Asra Khan, Michelle Pan, Rosalba Salcedo, Jin-Qiu Chen, Loretta Smith, Giorgio Trinchieri, and Laurie G. Kostecka

Subjects

0301 basic medicine, Keratinocytes, Cancer Research, Chemokine, Skin Neoplasms, Carcinogenesis, T cell, T-Lymphocytes, Biology, medicine.disease_cause, Article, 03 medical and health sciences, Mice, 0302 clinical medicine, medicine, Tumor Microenvironment, Animals, Humans, Neoplasms, Glandular and Epithelial, Molecular Biology, Adaptor Proteins, Signal Transducing, Regulation of gene expression, Mice, Knockout, Receptors, Interleukin-1 Type I, Tumor microenvironment, Interleukin-17, NF-kappa B, Signal transducing adaptor protein, Gene Expression Regulation, Neoplastic, Mice, Inbred C57BL, 030104 developmental biology, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Myeloid Differentiation Factor 88, Cancer research, biology.protein, ras Proteins, Female, Bone marrow, Signal transduction, Signal Transduction

Abstract

Cancer development requires a favorable tissue microenvironment. By deleting Myd88 in keratinocytes or specific bone marrow subpopulations in oncogenic RAS-mediated skin carcinogenesis, we show that IL17 from infiltrating T cells and IκBζ signaling in keratinocytes are essential to produce a permissive microenvironment and tumor formation. Both normal and RAS-transformed keratinocytes respond to tumor promoters by activating canonical NF-κB and IκBζ signaling, releasing specific cytokines and chemokines that attract Th17 cells through MyD88-dependent signaling in T cells. The release of IL17 into the microenvironment elevates IκBζ in normal and RAS-transformed keratinocytes. Activation of IκBζ signaling is required for the expression of specific promoting factors induced by IL17 in normal keratinocytes and constitutively expressed in RAS-initiated keratinocytes. Deletion of Nfkbiz in keratinocytes impairs RAS-mediated benign tumor formation. Transcriptional profiling and gene set enrichment analysis of IκBζ−deficient RAS-initiated keratinocytes indicate that IκBζ signaling is common for RAS transformation of multiple epithelial cancers. Probing The Cancer Genome Atlas datasets using this transcriptional profile indicates that reduction of IκBζ signaling during cancer progression associates with poor prognosis in RAS-driven human cancers. Implications: The paradox that elevation of IκBζ and stimulation of IκBζ signaling through tumor extrinsic factors is required for RAS-mediated benign tumor formation while relative IκBζ expression is reduced in advanced cancers with poor prognosis implies that tumor cells switch from microenvironmental dependency early in carcinogenesis to cell-autonomous pathways during cancer progression.

Published

2019

7. Correction of chromosomal point mutations in human cells with bifunctional oligonucleotides

Author

Yuri Khripine, Jilan Liu, Vivian Chih Wei Chen, Kenneth W. Culver, Alexander Khorlin, Yentram Huyen, and Wang-Ting Hsieh

Subjects

Adenosine Deaminase, Mutant, Oligonucleotides, Biomedical Engineering, Bioengineering, Biology, medicine.disease_cause, Applied Microbiology and Biotechnology, chemistry.chemical_compound, medicine, Chromosomes, Human, Humans, Point Mutation, Gene, Cell Line, Transformed, Mutation, Base Sequence, Oligonucleotide, Point mutation, Transfection, Genes, p53, Molecular biology, chemistry, Molecular Medicine, DNA, Biotechnology, Heteroduplex

Abstract

A sequence-specific genomic delivery system for the correction of chromosomal mutations was designed by incorporating two different binding domains into a single-stranded oligonucleotide. A repair domain (RD) contained the native sequence of the target region. A third strand-forming domain (TFD) was designed to form a triplex by Hoogsteen interactions. The design was based upon the premise that the RD will rapidly form a heteroduplex that is anchored synergistically by the TFD. Deoxyoligonucleotides were designed to form triplexes in the human adenosine deaminase (ADA) and p53 genes adjacent to known point mutations. Transfection of ADA-deficient human lymphocytes corrected the mutant sequence in 1-2% of cells. Neither the RD or TFD individually corrected the mutation. Transfection of p53 mutant human glioblastoma cells corrected the mutation and induced apoptosis in 7.5% of cells.

Published

1999

8. Genetic linkage mapping for a susceptibility locus to bipolar illness: Chromosomes 2,3,4,7,9,10p,11p,22, and Xpter

Author

John I. Nurnberger, D. Y. Rollins, Susan J. Donohue, Jeffrey C. Murray, Diane Coffman, Raji P. Grewal, J.L. Barrick, David C. Klein, Sevilla D. Detera-Wadleigh, Lynn R. Goldin, David Muniec, Kate Mills, Jason Sanders, Elliot S. Gershon, Wang-Ting Hsieh, Gordon Turner, Juliet J. Guroff, and Wade H. Berrettini

Subjects

Male, Bipolar Disorder, X Chromosome, Genotype, Genetic Linkage, Chromosomes, Human, Pair 22, Pseudoautosomal region, Locus (genetics), Pedigree chart, Gene mutation, Biology, Polymerase Chain Reaction, Gene mapping, Genetic linkage, Genetic model, Chromosomes, Human, Humans, Genetics (clinical), Genetics, Chromosomes, Human, Pair 10, Chromosomes, Human, Pair 11, Chromosome Mapping, Penetrance, Pedigree, Blotting, Southern, Chromosomes, Human, Pair 2, Female, Chromosomes, Human, Pair 3, Chromosomes, Human, Pair 4, Lod Score, Chromosomes, Human, Pair 9, Chromosomes, Human, Pair 7

Abstract

We are conducting a genome search for a predisposing locus to bipolar (manic-depressive) illness by genotyping 21 moderate-sized pedigrees. We report linkage data derived from screening marker loci on chromosomes 2, 3, 4, 7, 9, 10p, 11p, 22, and the pseudoautosomal region at Xpter. To analyze for linkage, two-point marker to illness lod scores were calculated under a dominant model with either 85% or 50% maximum penetrance and a recessive model with 85% maximum penetrance, and two affection status models. Under the dominant high penetrance model the cumulative lod scores in the pedigree series were less than -2 at {theta} = 0.01 in 134 of 142 loci examined, indicating that if the disease is genetically homogeneous, linkage could be excluded in these marker regions. Similar results were obtained using the other genetic models. Heterogeneity analysis was conducted when indicated, but no evidence for linkage was found. In the course of mapping we found a positive total lod score greater than +3 at the D7S78 locus at {theta} = 0.01 under a dominant, 50% penetrance model. The lod scores for additional markers within the D7S78 region failed to support the initial finding, implying that this was a spurious positive. Analysis withmore » affected pedigree member method for COL1A2 and D7S78 showed no significance for linkage, but for PLANH1, at the weighting functions f(p)=1 and f(p)=1/sqrt(p), borderline P values of 0.036 and 0.047 were obtained. We also detected new polymorphisms at the mineralo-corticoid receptor (MLR) and calmodulin II (CALMII) genes. These genes were genetically mapped and under affection status model 2 and a dominant, high penetrance mode of transmission the lod scores of {le}2 at {theta} = 0.01 were found. 39 refs., 2 figs., 12 tabs.« less

Published

1994

9. Genomic Screening for Genes Predisposing to Bipolar Disease

Author

Nina Harris, Henry Choi, Thomas N. Ferraro, Wade H. Berrettini, Lynn R. Goldin, Wang-Ting Hsieh, Eric Kron, Juliet G. Guroff, Sevilla D. Detera-Wadleigh, M.R. Hoehe, Diane Kazuba, David Muniec, Elliot S. Gershon, John I. Nurnberger, Maria Martinez, and Robert C. Alexander

Subjects

Genetics, Genomic screening, Psychiatry and Mental health, Bipolar disease, Biology, Gene, Biological Psychiatry, Genetics (clinical)

Published

1992

10. The human kininogen gene (KNG) mapped to chromosome 3q26-qter by analysis of somatic cell hybrids using the polymerase chain reaction

Author

David I. Smith, Dunne Fong, and Wang Ting Hsieh

Subjects

Somatic cell, Molecular Sequence Data, Hybrid Cells, In Vitro Techniques, Biology, Polymerase Chain Reaction, law.invention, Gene mapping, law, Cricetinae, Genetics, Animals, Humans, Deletion mapping, Gene, Genetics (clinical), Polymerase chain reaction, Electrophoresis, Agar Gel, Kininogen, Base Sequence, Kininogens, Chromosome Mapping, Chromosome, Molecular biology, Chromosome 3, Chromosomes, Human, Pair 3, circulatory and respiratory physiology

Abstract

Kinins, peptide products of kininogens, may be involved in hypertensive and diabetic diseases, and inflammatory disorders. The human kininogen gene (KNG) has been mapped to chromosome 3, using a panel of human-hamster somatic cell hybrids by polymerase chain reaction of hybrid DNA with gene-specific primers. KNG was further assigned to 3q26-3qter, using DNA from a second panel of chromosome 3 deletion mapping cell hybrids.

Published

1991

11. Mapping of the gene for human cysteine proteinase inhibitor stefin A, STF1, to chromosome 3cen-q21

Author

William Golembieski, Bonnie F. Sloane, David I. Smith, Wang Ting Hsieh, and Dunne Fong

Subjects

Genetics, Base Sequence, biology, Molecular Sequence Data, Chromosome Mapping, Chromosome, Cysteine Proteinase Inhibitors, Hybrid Cells, Cystatins, Polymerase Chain Reaction, Molecular biology, Gene mapping, Cystatin C, Chromosome 3, Cricetinae, Cystatin A, Centromere, biology.protein, Animals, Humans, Deletion mapping, Chromosomes, Human, Pair 3, Chromosome 20

Abstract

The gene for the human cysteine proteinase inhibitor stefin A (STF1), alias cystatin A, has been mapped to chromosome 3, using the polymerase chain reaction to specifically amplify the human stefin A sequence in human-hamster hybrid DNA. STF1 is further sublocalized to regions between centromere and 3q21 using a deletion mapping panel for this chromosome. This assignment shows that stefin A is not syntenic with cystatin C which has been localized to chromosome 20.

Published

1991

12. A linkage study of bipolar illness

Author

Thomas N. Ferraro, Elliot S. Gershon, Wade H. Berrettini, Sevilla D. Detera-Wadleigh, Juliet J. Guroff, Diane Kazuba, Wang-Ting Hsieh, Margret R. Hoehe, David Muniec, Lynn R. Goldin, Henry Choi, and John I. Nurnberger

Subjects

Genetic Markers, Male, Bipolar Disorder, Genotype, Genetic Linkage, Pedigree chart, Biology, Arts and Humanities (miscellaneous), Gene mapping, Chromosome 18, Risk Factors, medicine, Humans, Genetic Predisposition to Disease, Bipolar disorder, Linkage (software), Genetics, Models, Genetic, Autosomal dominant trait, medicine.disease, Penetrance, Pedigree, Psychiatry and Mental health, Genetic marker, Female, Lod Score, Chromosomes, Human, Pair 18

Abstract

Although genetic epidemiological studies of bipolar (BP) illness are consistent with a heritable component, inherited risk factors remain unknown. The goal of the present study is to describe the localization of BP susceptibility loci through linkage strategies, including a genome-wide search.A linkage study of 22 BP families has been performed. These BP families include almost 400 persons, 173 of whom have been diagnosed as having BP I, schizoaffective, BP II with major depression, or recurrent unipolar illness. Using an autosomal dominant disease model with 85% or 50% age-dependent penetrance, and a recessive model with 85% penetrance, linkage analyses were performed assuming a narrow (BP and schizoaffective) or a broad (BP, schizoaffective, or unipolar) definition of the BP spectrum. Affected sibling pairs and affected pedigree member analyses were performed when positive lod scores were observed in multiple pedigrees. The present article describes linkage analysis of 310 DNA markers on chromosomes 1, 5p, 6, 8, 10q, 11q, and 12 to 18.None of the loci examined disclosed compelling evidence for linkage using lod score analyses. Model-independent analysis by multilocus affected pedigree member method in the pericentromeric chromosome 18 region disclosed statistically significant evidence (P.0001) for a BP susceptibility gene in this region. Multilocus analysis by affected sibling pair method also disclosed evidence for linkage (P.00008).Our results imply that a BP susceptibility gene exists near the centromere of chromosome 18. Confirmation of this finding (by independent investigators studying different pedigrees) has been published, suggesting that a valid BP disease linkage may have been discovered.

Published

1997

13. Real-time detection of DNA hybridization and melting on oligonucleotide arrays by using optical wave guides

Author

Joanell V. Hoijer, Ronald C. Gamble, John D. Baldeschwieler, Cynthia Jou, Tomas Theriault, Julian Gordon, Don I. Stimpson, and Wang-Ting Hsieh

Subjects

Materials science, Light, Molecular Sequence Data, Biotin, Nucleic Acid Denaturation, Soaps, Signal, DNA sequencing, Structure-Activity Relationship, Optics, Human Genome Project, Humans, Scattering, Radiation, A-DNA, Detection limit, Multidisciplinary, Base Sequence, Oligonucleotide, business.industry, DNA–DNA hybridization, Nucleic Acid Hybridization, DNA, Molecular biology, Oligodeoxyribonucleotides, Thermodynamics, Human genome, Glass, DNA microarray, business, Caltech Library Services, Research Article

Abstract

The challenge of the Human Genome Project is to increase the rate of DNA sequence acquisition by two orders of magnitude to complete sequencing of the human genome by the year 2000. The present work describes a rapid detection method using a two-dimensional optical wave guide that allows measurement of real-time binding or melting of a light-scattering label on a DNA array. A particulate label on the target DNA acts as a light-scattering source when illuminated by the evanescent wave of the wave guide and only the label bound to the surface generates a signal. Imaging/visual examination of the scattered light permits interrogation of the entire array simultaneously. Hybridization specificity is equivalent to that obtained with a conventional system using autoradiography. Wave guide melting curves are consistent with those obtained in the liquid phase and single-base discrimination is facile. Dilution experiments showed an apparent lower limit of detection at 0.4 nM oligonucleotide. This performance is comparable to the best currently known fluorescence-based systems. In addition, wave guide detection allows manipulation of hybridization stringency during detection and thereby reduces DNA chip complexity. It is anticipated that this methodology will provide a powerful tool for diagnostic applications that require rapid cost-effective detection of variations from known sequences.

Published

1995

14. Confirmation of the human cathepsin B gene (CTSB) assignment to chromosome 8

Author

Joan C. Menninger, Marion M. Chan, Wang-Ting Hsieh, Dunne Fong, and David C. Ward

Subjects

medicine.diagnostic_test, Base Sequence, Molecular Sequence Data, Chromosome, Nucleic Acid Hybridization, Cathepsin F, Biology, Hybrid Cells, Molecular biology, Polymerase Chain Reaction, Cathepsin B, Fluorescence, Nucleic acid thermodynamics, Gene mapping, Genetics, medicine, Cosmid, Humans, Cloning, Molecular, Metaphase, Genetics (clinical), Fluorescence in situ hybridization, Chromosomes, Human, Pair 8

Abstract

Human cathepsin B gene (CTSB) has been mapped to two locations: 8p22 and 13q14. Here we confirm the chromosome 8 assignment by three independent methods: (1) analysis of human-hamster somatic cell hybrid DNA by polymerase chain reaction; (2) comparison of hybridization signals to cathepsin B in interphase nuclei of normal fibroblasts and fibroblasts with a chromosome 8 deletion; and (3) fluorescence in situ hybridization to metaphase spreads using cathepsin B cosmid clones. Our results indicate that human CTSB is located at 8p22-p23.1.

Published

1992

15. Genetic mapping of the Gs-alpha subunit gene (GNAS1) to the distal long arm of chromosome 20 using a polymorphism detected by denaturing gradient gel electrophoresis

Author

Allen M. Spiegel, M.R. Hoehe, Lee S. Weinstein, Wang Ting Hsieh, Maria Martinez, Qiuhe Cao, Pablo V. Gejman, and Elliot S. Gershon

Subjects

Male, Base Sequence, Molecular Sequence Data, Chromosomes, Human, Pair 20, DNA, Biology, Molecular biology, Electrophoresis, chemistry.chemical_compound, Gene mapping, chemistry, Genetic marker, GTP-Binding Proteins, Genetics, Humans, Electrophoresis, Polyacrylamide Gel, Female, Chromosome 20, Gene, Polyacrylamide gel electrophoresis, Temperature gradient gel electrophoresis, Polymorphism, Restriction Fragment Length

Published

1991

16. A NotI RFLP in the human alpha2-C4 adrenergic receptor locus (ADRA2RL2) detected by PFGE

Author

J.L. Barrick, Wang-Ting Hsieh, M.R. Hoehe, and Elliot S. Gershon

Subjects

Genetics, Electrophoresis, Agar Gel, Adrenergic receptor, Chromosome Mapping, Locus (genetics), Biology, Receptors, Adrenergic, alpha, Molecular biology, Gene mapping, Genetic marker, Pulsed-field gel electrophoresis, Humans, Alpha-2 adrenergic receptor, Restriction fragment length polymorphism, Chromosomes, Human, Pair 4, Deoxyribonucleases, Type II Site-Specific, Allele frequency, Polymorphism, Restriction Fragment Length

Published

1991

17. Manic depressive illness not linked to factor IX region in an independent series of pedigrees

Author

Pablo V. Gejman, Sevilla D. Detera-Wadleigh, Wade H. Berrettini, Maria Martinez, Lynn R. Goldin, Wang-Ting Hsieh, Joel Gelernter, and Elliot S. Gershon

Subjects

Genetics, Male, congenital, hereditary, and neonatal diseases and abnormalities, Bipolar Disorder, X Chromosome, Genetic Linkage, Pedigree chart, Locus (genetics), Biology, Xq28, Pedigree, Factor IX, Phenotype, Manic-depressive illness, medicine, Humans, Female, Lod Score, Polymorphism, Restriction Fragment Length, Lod scores, medicine.drug

Abstract

We studied seven informative kindreds segregating for manic depressive illness (MDI), consistent with X-chromosome transmission of the trait (families do not show affective disease in both a father and a son), using markers mapped to the region of Xq27–Xq28. The lod scores were consistently below -2 in the region extending from about 10 cM centromeric from the Factor IX locus (F9) to the colorblindness region. This study does not replicate previous reports of linkage of MDI to Factor IX (Xq27) and colorblindness region (Xq28) chromosomal markers in other kindreds.

Published

1990

18. A two-allele Pstl RFLP for the alpha-1C adrenergic receptor gene (ADRA1C)

Author

Debra A. Schwinn, Margret R. Hoehe, Wade H. Berrettini, and Wang-Ting Hsieh

Subjects

Genetics, General Medicine, Receptors, Adrenergic, alpha, Alpha-1C Adrenergic Receptor, Biology, α1 adrenergic receptor, Molecular biology, Gene mapping, Genetic marker, Humans, Allele, Restriction fragment length polymorphism, Deoxyribonucleases, Type II Site-Specific, Molecular Biology, Allele frequency, Gene, Alleles, Polymorphism, Restriction Fragment Length, Genetics (clinical), Chromosomes, Human, Pair 8

Published

1992

19. HindIII identifies a two allele DNA polymorphism of the human cannabinoid receptor gene (CNR)

Author

Wade H. Berrettini, L. Caenazzo, Elliot S. Gershon, M.R. Hoehe, Tom I. Bonner, and Wang-Ting Hsieh

Subjects

Genetics, biology, Receptors, Drug, medicine.medical_treatment, Nucleic Acid Hybridization, Deoxyribonuclease HindIII, HindIII, Molecular biology, Introns, White People, Gene mapping, medicine, biology.protein, Humans, Chromosomes, Human, Pair 6, Cannabinoid, Restriction fragment length polymorphism, Allele, Receptors, Cannabinoid, Gene, Allele frequency, Polymorphism, Restriction Fragment Length

Published

1991

20. A Pstl DNA polymorphism in the human stefin A gene (STF 1)

Author

Wade H. Berrettini, Joan L. Barrick, Wang ting Hsieh, Dunne Fong, and Marion M. Chan

Subjects

Genetics, Hybridization probe, DNA, Biology, Cystatins, Molecular biology, chemistry.chemical_compound, Gene mapping, chemistry, Genetic marker, Cystatin A, Humans, Chromosomes, Human, Pair 3, Restriction fragment length polymorphism, DNA Probes, Deoxyribonucleases, Type II Site-Specific, Molecular probe, Gene, Polymorphism, Restriction Fragment Length

Published

1991

21. A Taql DNA polymorphism in the human cathepsin B gene (CTSB)

Author

Dunne Fong, Mary Smith, Peter E. Barker, and Wang ting Hsieh

Subjects

Genetics, Cathepsin E, Cathepsin F, Biology, Molecular biology, Cathepsin B, chemistry.chemical_compound, Genes, Gene mapping, chemistry, Genetic marker, Humans, Restriction fragment length polymorphism, Deoxyribonucleases, Type II Site-Specific, Gene, Polymorphism, Restriction Fragment Length, DNA, Chromosomes, Human, Pair 8

Published

1990

22. Isolation of a cDNA clone for the human lysosomal proteinase cathepsin B

Author

Robert D. Wells, Dunne Fong, Wang-Ting Hsieh, David H. Calhoun, and Benjamin Lee

Subjects

Cathepsin D, Cathepsin E, Cathepsin F, Biology, Cathepsin A, Cathepsin B, Cathepsin O, Cathepsin H, Endopeptidases, Humans, Amino Acid Sequence, Peptide sequence, Multidisciplinary, Base Sequence, Calpain, Nucleic Acid Hybridization, DNA, Cathepsins, Molecular biology, Isoenzymes, Cysteine Endopeptidases, Liver, Biochemistry, Lysosomes, Research Article

Abstract

The cysteine proteinase cathepsin B is one member of the lysosomal acid hydrolases. Based on the peptide sequence of rat liver cathepsin B, an oligonucleotide mixture containing 128 different 17-mers was synthesized and used as a probe to screen adult and fetal human liver cDNA libraries. A recombinant clone with a 1540-nucleotide insert was identified from the fetal library, and DNA sequence analysis confirmed that this clone encodes human cathepsin B. The clone, designated pCB-1, has sequences for 81% of the coding region (for amino acid residues 50-252) together with approximately equal to 880 nucleotides of the 3' untranslated region of the mRNA. The DNA sequence also shows that the predicted carboxyl terminus of the coding sequence is longer than the mature protein by 6 amino acid residues. Southern blot analysis of restriction enzyme digests of human placental DNA revealed a simple pattern of hybridizing fragments using the cathepsin B coding sequence as probe. The result suggests that there is a single copy of cathepsin B gene per haploid genome.

Published

1986

23. Lactose repressor protein modified with dansyl chloride: activity effects and fluorescence properties

Author

Kathleen S. Matthews and Wang Ting Hsieh

Subjects

Isopropyl Thiogalactoside, Operator (biology), Stereochemistry, Repressor, Lac repressor, Biochemistry, Chloride, chemistry.chemical_compound, Escherichia coli, polycyclic compounds, medicine, Carbon Radioisotopes, Dansyl Compounds, Chemistry, Dansyl chloride, Chemical modification, DNA, Repressor Proteins, Kinetics, Spectrometry, Fluorescence, Monomer, Reagent, bacteria, Protein Binding, Transcription Factors, medicine.drug

Abstract

Chemical modification using 5-(dimethylamino)naphthalene-1-sulfonyl chloride (dansyl chloride) has been used to explore the importance of lysine residues involved in the binding activities of the lactose repressor and to introduce a fluorescent probe into the protein. Dansyl chloride modification of lac repressor resulted in loss of operator DNA binding at low molar ratios of reagent/monomer. Loss of nonspecific DNA binding was observed only at higher molar ratios, while isopropyl beta-D-thiogalactoside binding was not affected at any of the reagent levels studied. Lysine residues were the only modified amino acids detected. Protection of lysines-33 and -37 from modification by the presence of nonspecific DNA correlated with maintenance of operator DNA binding activity, and reaction of lysine-37 paralleled operator binding activity loss. Energy transfer between dansyl incorporated in the core region of the repressor protein and tryptophan-201 was observed, with an approximate distance of 23 A calculated between these two moieties.

Published

1985

24. Left-Handed DNA in Vivo

Author

Jacquelynn E. Larson, John A. Blaho, Adam Jaworski, Robert D. Wells, and Wang-Ting Hsieh

Subjects

Site-Specific DNA-Methyltransferase (Adenine-Specific), EcoRI, medicine.disease_cause, chemistry.chemical_compound, Plasmid, In vivo, Escherichia coli, medicine, Cloning, Molecular, Gene, Multidisciplinary, biology, DNA, Superhelical, DNA, Methyltransferases, Methylation, Molecular biology, Kinetics, Biochemistry, chemistry, Helix, biology.protein, Nucleic Acid Conformation, Plasmids

Abstract

Left-handed DNA is shown to exist and elicit a biological response in Escherichia coli. A plasmid encoding the gene for a temperature-sensitive Eco RI methylase (MEco RI) was cotransformed with different plasmids containing inserts that had varying capacities to form left-handed helices or cruciforms with a target Eco RI site in the center or at the ends of the inserts. Inhibition of methylation in vivo was found for the stable inserts with the longest left-handed (presumably Z) helices. In vitro methylation with the purified MEco RI agreed with the results in vivo. Supercoil-induced changes in the structure of the primary helix in vitro provided confirmation that left-handed helices were responsible for this behavior. The presence in vivo of left-handed inserts elicits specific deletions and plasmid incompatibilities in certain instances.

Published

1987

25. Unusual DNA Structures and the Probes Used for their Detection

Author

Jeffery C. Hanvey, Janusz Klysik, Robert D. Wells, Wang-Ting Hsieh, Sorour Amirhaeri, Wolfgang Zacharias, David A. Collier, Michael J. McLean, John A. Blaho, Adam Jaworski, Franz Wohlrab, and Jacquelynn E. Larson

Subjects

Cloning, Circular dichroism, biology, Oligonucleotide, DNA sequencing, Restriction fragment, law.invention, chemistry.chemical_compound, chemistry, Biochemistry, law, Mung Bean Nuclease, biology.protein, Recombinant DNA, DNA

Abstract

A veritable explosion in our knowledge of unusual DNA structures has occurred in recent years. Our enhanced knowledge about specific DNA sequences via DNA sequencing and cloning has been a contributory factor. Furthermore, the establishment of diverse types of methods for the detection and analysis of unusual DNA structures has also been important. For example, in the early days of left-handed Z-DNA (1979–1982), the only techniques available were x-ray diffraction on short oligonucleotides, circular dichroism, phosphorus NMR, and laser Raman spectroscopy. Today, at least 15 different types of physical, enzymatic, immunological, chemical, and spectroscopic methods are available. Studies have been conducted on recombinant plasraids, short synthetic oligonucleotides, as well as purified restriction fragments.

Published

1988

26. In vivo existence of left-handed DNA

Author

Adam Jaworski, Robert D. Wells, Wolfgang Zacharias, Wang-Ting Hsieh, John A. Blaho, and Jacquelynn E. Larson

Subjects

DNA, Bacterial, Site-Specific DNA-Methyltransferase (Adenine-Specific), EcoRI, DNA, Recombinant, Molecular cloning, Methylation, Z-DNA, chemistry.chemical_compound, Plasmid, Bacterial Proteins, In vivo, Genetics, biology, Base Sequence, General Medicine, DNA, Molecular biology, Kinetics, Biochemistry, chemistry, biology.protein, DNA supercoil, Nucleic Acid Conformation, Plasmids

Abstract

A genetic-biochemical assay has been developed to investigate the in vivo existence and consequences of unusual DNA structures. Left-handed DNA was shown to exist in living Escherichia coli . The Eco RI methyl-transferase gene (temperature-sensitive) was cloned to serve as a probe for perturbed GAATTC sites in vivo. This plasmid was cotransformed with different plasmids containing inserts that had varying capacities to form left-handed helices or cruciforms with a target EcoRI site in the center or at the ends of the inserts. Inhibition of methylation in vivo was found for the stable inserts with the longest left-handed helices. In vitro methylation with the purified M · Eco RI enzyme agreed with the in vivo results.

Published

1988

27. Detection of Cache Valley Virus in Biologics Manufactured in CHO Cells.

Author

Nims, Raymond W., Dusing, Sandra K., Wang-Ting Hsieh, Lovatt, Archie, Reid, C. Gordon, Onions, David, and Milne, Euan W.

Subjects

VIRAL disease diagnosis, BUNYAVIRUSES, BIOLOGICALS, INFECTION

Abstract

The article describes the detection of Cache valley virus (CVV) found in Chinese hamster ovary cell-derived biologics. This type of virus is a member of the Bunyaviridae family that infects livestock across North America and is conceived to enter the biologics production processes through contaminated fetal bovine serum used in the cell growth medium. The infections caused by this virus can be detected during production through the use of process monitoring and in vitro virus screening.

Published

2008