Your search keyword '"Lim, Kim-Chew"' showing total 57 results

51. Compound loss of function of nuclear receptors Tr2and Tr4leads to induction of murine embryonic β-type globin genes

Author

Cui, Shuaiying, Tanabe, Osamu, Sierant, Michael, Shi, Lihong, Campbell, Andrew, Lim, Kim-Chew, and Engel, James Douglas

Abstract

The orphan nuclear receptors TR2 and TR4 have been shown to play key roles in repressing the embryonic and fetal globin genes in erythroid cells. However, combined germline inactivation of Tr2and Tr4leads to periimplantation lethal demise in inbred mice. Hence, we have previously been unable to examine the consequences of their dual loss of function in adult definitive erythroid cells. To circumvent this issue, we generated conditional null mutants in both genes and performed gene inactivation in vitro in adult bone marrow cells. Compound Tr2/Tr4loss of function led to induced expression of the embryonic εy and βh1 globins (murine counterparts of the human ε- and γ-globin genes). Additionally, TR2/TR4 function is required for terminal erythroid cell maturation. Loss of TR2/TR4 abolished their occupancy on the εy and βh1 gene promoters, and concurrently impaired co-occupancy by interacting corepressors. These data strongly support the hypothesis that the TR2/TR4 core complex is an adult stage-specific, gene-selective repressor of the embryonic globin genes. Detailed mechanistic understanding of the roles of TR2/TR4 and their cofactors in embryonic and fetal globin gene repression may ultimately enhance the discovery of novel therapeutic agents that can effectively inhibit their transcriptional activity and be safely applied to the treatment of β-globinopathies.

Published

2015

52. Structure and regulation of the chicken erythroid δ-aminolevulinate synthase gene

Author

Lim, Kim-Chew, primary, Ishihara, Hajime, additional, Riddle, Robert D., additional, Yang, Zhuoying, additional, Andrews, Nancy, additional, Yamamoto, Masayuki, additional, and Engel, James Douglas, additional

Published

1994

53. Expression of the chicken GATA factor family during early erythroid development and differentiation

Author

Leonard, Mark W., Lim, Kim-Chew, and Engel, James Douglas

Abstract

The DNA motif WGATAR has been identified within transcriptional regulatory domains of globin and other erythroid-specific genes and the activator proteins that bind to this regulatory element, the GATA factors, belong to a multi-gene family that is expressed in chicken erythroid cells. Here we show that, as in chickens, multiple members of the GATA factor family are expressed in human and murine erythroid cells. During the early stages of chicken embryogenesis (well before blood island formation), each of the GATA family members is transcribed with a unique temporal and spatial pattern. In the primitive erythroid lineage, tran-scription of the embryonic -globin gene parallels GATA-1 expression while the switch to -globin transcription in definitive erythroid cells is directly preceded by a pronounced increase in GATA-3 accumulation. The timing and pattern of expression of these different mRNAs during avian erythroid development and differentiation suggests that temporally regulated changes in GATA factor expression are required for vertebrate hematopoiesis.

Published

1993

54. Regulation and function of transcription factor GATA-1 during red blood cell differentiation

Author

Briegel, Karoline, Bartunek, Petr, Stengl, Gabi, Lim, Kim-Chew, Beug, Hartmut, Engel, James Douglas, and Zenke, Martin

Abstract

The tissue-specific transcription factor GATA-1 is a key regulator of red blood cell differentiation. One seemingly contradictory aspect of GATA-1 function is that, while it is abundant in erythroid progenitor cells prior to the onset of overt differentiation, it does not significantly activate known GATA-1 target genes in those cells. To investigate the mechanisms underlying GATA-1 function during the transition from early to late erythropoiesis, we have examined its expression and activity in normal avian erythroid progenitor cells before and after induction of differentiation. In these primary progenitor cells, GATA-1 protein was predominantly located in the cytoplasm, while induction of differentiation caused its rapid relocalization to the nucleus, suggesting that nuclear translocation constitutes an important regulatory step in GATA-1 activation. As an alternative way of addressing the same question, we also ectopically expressed a GATA-1/estrogen receptor fusion protein (GATA-1/ER) in red blood cell progenitors, where nuclear translocation of, and transcriptional activation by, this hybrid factor are conditionally controlled by estrogen. We found that hormone-activated GATA-1/ER protein accelerated red blood cell differentiation, and concomitantly suppressed cell proliferation. These phenotypic effects were accompanied by a simultaneous suppression of c-myb and GATA-2 transcription, two genes thought to be involved in the proliferative capacity of hematopoietic progenitor cells. Thus, GATA-1 appears to promote differentiation in committed erythroid progenitor cells both by inducing differentiation-specific genes and by simultaneously suppressing genes involved in cell proliferation.

Published

1996

55. Structure and regulation of the chicken erythroid {delta}-aminolevulinate synthase gene

Author

Lim, Kim-Chew, Ishihara, Hajime, Riddle, Robert D., Yang, Zhuoying, Andrews, Nancy, Yamamoto, Masayuki, and Engel, James Douglas

Abstract

Erythroid cells regulate heme biosynthesis in a manner that is distinct from all other cell types. While heme negatively regulates the synthesis of the housekeeping δ-amlnolevullnate synthase (ALAS-N) in all non-erythrold cells, the expression of an erythroid-speclfic isozyme (ALAS-E) is developmentally regulated in red blood cells. As a first step towards understanding the molecular basis for the transcrlptional regulation of ALAS-E during erythropolesis, we cloned and characterized the chicken ALAS-E locus. This gene spans 18 kbp and is composed of eleven exons. The intron/exon structure of erythroid ALAS was found to be conserved among several vertebrate species. Direct RNA sequencing identified a 5′ untranslated region that is derived from two contiguous exons and is predicted to form a very stable stem-loop structure that bears resemblance to the ferrltln iron-responsive element. Tissue-specific expression of the ALAS-E gene was analyzed by transient transfectlon assays in hematopoietlc cells of both erythroid and non-erythroid origins. These experiments identified distal (−784 to −505 bp) and proximal (−155 to +21 bp) promoter elements which are required for high level, erythroid-speclfic transcription.

Published

1994

56. GATA-3 is required for early T lineage progenitor development.

Author

Hosoya T, Kuroha T, Moriguchi T, Cummings D, Maillard I, Lim KC, and Engel JD

Subjects

Animals, Liver embryology, Mice, Mice, Inbred C57BL, Thymus Gland embryology, Cell Lineage, GATA3 Transcription Factor physiology, Hematopoietic Stem Cells physiology, Lymphopoiesis, T-Lymphocytes physiology

Abstract

Most T lymphocytes appear to arise from very rare early T lineage progenitors (ETPs) in the thymus, but the transcriptional programs that specify ETP generation are not completely known. The transcription factor GATA-3 is required for the development of T lymphocytes at multiple late differentiation steps as well as for the development of thymic natural killer cells. However, a role for GATA-3 before the double-negative (DN) 3 stage of T cell development has to date been obscured both by the developmental heterogeneity of DN1 thymocytes and the paucity of ETPs. We provide multiple lines of in vivo evidence through the analysis of T cell development in Gata3 hypomorphic mutant embryos, in irradiated mice reconstituted with Gata3 mutant hematopoietic cells, and in mice conditionally ablated for the Gata3 gene to show that GATA-3 is required for ETP generation. We further show that Gata3 loss does not affect hematopoietic stem cells or multipotent hematopoietic progenitors. Finally, we demonstrate that Gata3 mutant lymphoid progenitors exhibit neither increased apoptosis nor diminished cell-cycle progression. Thus, GATA-3 is required for the cell-autonomous development of the earliest characterized thymic T cell progenitors.

Published

2009

57. Genomic organization and sequence variation of the human integrin subunit alpha8 gene (ITGA8).

Author

Ekwa-Ekoka C, Diaz GA, Carlson C, Hasegawa T, Samudrala R, Lim KC, Yabu JM, Levy B, and Schnapp LM

Subjects

Base Sequence, Chromosome Mapping, Chromosomes, Human, Pair 10, DNA metabolism, DNA, Complementary metabolism, Databases, Genetic, Exons, Genetic Variation, Genotype, Humans, Immunohistochemistry, In Situ Hybridization, Fluorescence, Kidney metabolism, Linkage Disequilibrium, Lung metabolism, Models, Genetic, Models, Molecular, Molecular Sequence Data, Polymorphism, Genetic, Polymorphism, Single Nucleotide, Protein Conformation, Protein Structure, Secondary, Sequence Homology, Amino Acid, Genome, Integrin alpha Chains genetics, Integrin alpha Chains metabolism

Abstract

The integrin alpha8 is highly expressed during kidney and lung development. alpha8-deficient mice display abnormal renal development suggesting that alpha8 plays a critical role in organogenesis. Therefore, it would be of considerable interest to understand the genomic structure, localization and sequence variation of the alpha8 gene. Using FISH and genomic database analysis, we show that alpha8 gene maps to chromosome 10p13 and consists of >200 kbp organized into 30 exons. Examination of 47 individuals from two different ethnic groups (European and African descent) identified 286 varying sites. The diversity of alpha8 is comparable to that of other regions within the human genome. Eight of the varying sites were located in the coding regions: six resulted in nonsynonymous substitutions of which two lead to non-conservative changes in protein. None of the sites showed significant deviation from Hardy-Weinberg equilibrium. We mapped the coding region single nucleotide polymorphisms (SNPs) onto a model of the predicted alpha8 structure and found all the SNPs were located in the "calf" of the extracellular domain. In the European population, the linkage disequilibrium statistic D' showed three blocks of relatively non-recombinant regions in the alpha8 gene while the African population showed more evidence of recombination. The observed patterns of the linkage disequilibrium statistic R2 suggest that a large number of sites will need to be genotyped to ensure coverage of the entire gene for genetic association studies. Identification of the sequence variation will allow genetic association studies of alpha8 in kidney and lung disease.

Published

2004