Your search keyword '"Mark G. Carter"' showing total 18 results

1. Established Preblastocyst- and Blastocyst-Derived ES Cell Lines Have Highly Similar Gene Expression Profiles, Despite Their Differing Requirements for Derivation Culture Conditions

Author

Mark G. Carter, Ren-He Xu, Chul Kim, Ge Lin, Joonghoon Park, Xiuchun Cindy Tian, and Tomokazu Amano

Subjects

Male, Green Fluorescent Proteins, Karyotype, Cell, Cell Culture Techniques, Embryonic Development, Biology, Morula, Cell Line, Mice, medicine, Animals, Blastocyst, Zona pellucida, Embryonic Stem Cells, Gene Expression Profiling, Embryogenesis, Teratoma, Embryo, Original Articles, Cell Biology, Molecular biology, Embryonic stem cell, Culture Media, Mice, Inbred C57BL, Gene expression profiling, medicine.anatomical_structure, Mice, Inbred DBA, Cell culture, Mice, Inbred CBA, Female, Octamer Transcription Factor-3, Developmental Biology, Biotechnology

Abstract

The efficiency of embryonic stem (ES) cell derivation relies on an optimized culture medium and techniques for treating preimplantation stage embryos. Recently, ES cell derivation from the preblastocyst developmental stage was reported by removing the zona pellucida from embryos of the most efficient strain for ES cell derivation (129Sv) during early preimplantation. Here, we showed that ES cells can be efficiently derived and maintained in a modified medium (MEMα), from preblastocysts of a low-efficiency mouse strain (a hybrid consisting of 50% B6, 25% CBA, and 25% DBA). Preblastocyst-derived ES cell lines were normal in terms of pluripotency-related protein expression, and chromosome number. Also, preblastocyst-derived ES cell lines from various culture conditions showed pluripotency in vivo through teratoma analysis. Interestingly, ES cell lines produced from preblastocysts and blastocysts, regardless of the derivation culture conditions, are nearly indistinguishable by their global gene expression profiles.

Published

2012

2. Single-cell transcript analysis of human embryonic stem cells

Author

Nathalie Boucher, Jason D. Gibson, Craig E. Nelson, Mark G. Carter, Kelly A. Holbrook, and Caroline M. Jakuba

Subjects

Cell type, Transcription, Genetic, Reverse Transcriptase Polymerase Chain Reaction, Gene Expression Profiling, Cellular differentiation, Biophysics, Cell Differentiation, Bone Morphogenetic Protein 4, Biology, Biochemistry, Embryonic stem cell, Molecular biology, Chromatin, Activins, Transcriptome, Gene expression profiling, medicine.anatomical_structure, embryonic structures, medicine, Humans, RNA, Endoderm, Stem cell, Embryonic Stem Cells

Abstract

We demonstrate the qualitative and quantitative power of single-cell transcript analysis to characterize transcriptome dynamics in human embryonic stem cells (hESC's). Single-cell analysis can systematically determine unique cellular profiles for use in cell sorting and identification, show the potential to augment standing models of cellular differentiation, and elucidate the behavior of stem cells exiting pluripotency. Using single-cell analysis of H9 hESC's differentiating under three culture conditions, we revealed transient expression of mesendodermal markers in all three protocols, followed by increasingly stable expression of embryonic endoderm and extra-embryonic endoderm markers. Our single-cell profiles reveal mixed populations of cell types, with both transcriptional and temporal heterogeneity marking differentiation under all conditions. Interestingly, we also observe extensive and prolonged co-expression of markers regulating both pluripotency and lineage differentiation in all culture conditions, and we find that pluripotency marker transcripts remain detectable in the majority of cells for many days. Finally, we show that cells derived from undifferentiated hESC colonies display consistent gene expression profiles characterized by three cohorts of transcripts: uniform, absent and sporadically detected messages, and that a striking correlation exists between genes' membership in these cohorts and their hESC promoter chromatin state, with bivalent promoters dominating the sporadic transcripts.

Published

2009

3. Beneficial Effect of Young Oocytes for Rabbit Somatic Cell Nuclear Transfer

Author

Xiangzhong Yang, Shaorong Gao, Mark G. Carter, X. Cindy Tian, Li-Ying Sung, Jie Xu, Y. Eugene Chen, Fuliang Du, Jifeng Zhang, Chingli He, S.A. Chaubal, and Rafael A. Fissore

Subjects

Mitogen-Activated Protein Kinase Kinases, Nuclear Transfer Techniques, Donor cell, Cell fusion, Metaphase ii, Cloning, Organism, Maturation-Promoting Factor, Age Factors, Embryo, Biology, Original Papers, Molecular biology, medicine.anatomical_structure, embryonic structures, Oocytes, medicine, Animals, Somatic cell nuclear transfer, Rabbits, Blastocyst, Cellular Senescence, Developmental Biology, Biotechnology

Abstract

This study was designed to examine the effect of the age of rabbit oocytes on the developmental potential of cloned embryos. The metaphase II oocytes used for nuclear transfer (NT) were collected at 10, 12, 14, and 16 h post-hCG injection (hpi). The total number of oocytes collected per donor (21.4–23.7) at 12 to 16 hpi was similar, but significantly higher than that collected at 10 hpi (16.2). Additionally, a significant improvement in blastocyst development was achieved with embryos generated by electrically mediated cell fusion (56.0%), compared to those from nuclear injection (13.1 %) (Experiment 1). Markedly higher blastocyst development (45.8–54.5%) was also achieved with oocytes collected at 10–12 hpi than from those collected 14–16 hpi (8.3–14.3%) (Experiment 2). In Experiment 3, the blastocyst rates of NT embryos derived from oocytes harvested 12 hpi (39.2–42.8 %) were significantly higher than from those collected at 16 hpi (6.8–8.4 %) (p

Published

2009

4. Global gene expression analysis identifies molecular pathways distinguishing blastocyst dormancy and activation

Author

Haibin Wang, Minoru S.H. Ko, Sudhansu K. Dey, Takiko Daikoku, Hiromichi Matsumoto, Toshio Hamatani, and Mark G. Carter

Subjects

Male, Cytoplasm, Cell signaling, DNA, Complementary, Mice, Inbred Strains, Biology, Mice, Pregnancy, medicine, Animals, Calcium Signaling, Blastocyst, reproductive and urinary physiology, Oligonucleotide Array Sequence Analysis, Cell Nucleus, Multidisciplinary, Epidermal Growth Factor, urogenital system, Cell Cycle, Estrogen secretion, Gene Expression Regulation, Developmental, Embryo, Biological Sciences, Cell cycle, Molecular biology, Chromatin, Cell biology, medicine.anatomical_structure, embryonic structures, Carbohydrate Metabolism, Intercellular Signaling Peptides and Proteins, Dormancy, Female, Embryonic diapause, Energy Metabolism, Cell Adhesion Molecules, Blastocyst growth, Heparin-binding EGF-like Growth Factor

Abstract

Delayed implantation (embryonic diapause) occurs when the embryo at the blastocyst stage achieves a state of suspended animation. During this period, blastocyst growth is very slow, with minimal or no cell division. Nearly 100 mammals in seven different orders undergo delayed implantation, but the underlying molecular mechanisms that direct this process remain largely unknown. In mice, ovariectomy before preimplantation ovarian estrogen secretion on day 4 of pregnancy initiates blastocyst dormancy, which normally lasts for 1–2 weeks by continued progesterone treatment, although blastocyst survival decreases with time. An estrogen injection rapidly activates blastocysts and initiates their implantation in the progesterone-primed uterus. Using this model, here we show that among ≈20,000 genes examined, only 229 are differentially expressed between dormant and activated blastocysts. The major functional categories of altered genes include the cell cycle, cell signaling, and energy metabolic pathways, particularly highlighting the importance of heparin-binding epidermal growth factor-like signaling in blastocyst–uterine crosstalk in implantation. The results provide evidence that the two different physiological states of the blastocyst, dormancy and activation, are molecularly distinguishable in a global perspective and underscore the importance of specific molecular pathways in these processes. This study has identified candidate genes that provide a scope for in-depth analysis of their functions and an opportunity for examining their relevance to blastocyst dormancy and activation in numerous other species for which microarray analysis is not available or possible due to very limited availability of blastocysts.

Published

2004

5. Mice deficient in the candidate tumor suppressor gene Hic1 exhibit developmental defects of structures affected in the Miller-Dieker syndrome

Author

Joseph L. Mankowski, Xiaobei Zeng, Margaret A. Johns, David M. Donovan, Li Zhou, M. Christine Zink, Mark G. Carter, and Stephen B. Baylin

Subjects

Candidate gene, Tumor suppressor gene, Kruppel-Like Transcription Factors, Biology, Exencephaly, medicine.disease_cause, Mice, Genetics, medicine, Animals, Humans, Abnormalities, Multiple, Genes, Tumor Suppressor, Molecular Biology, Gene, Genetics (clinical), Acrania, Mutation, Miller–Dieker syndrome, Reverse Transcriptase Polymerase Chain Reaction, Syndrome, General Medicine, Embryo, Mammalian, medicine.disease, Candidate Tumor Suppressor Gene, Blotting, Southern, Transcription Factors

Abstract

HIC1 is a candidate tumor suppressor gene which is frequently hypermethylated in human tumors, and its location within the Miller-Dieker syndrome's critical deletion region at chromosome 17p13.3 makes it a candidate gene for involvement in this gene deletion syndrome. To study the function of murine Hic1 in development, we have created Hic1 -deficient mice. These animals die perinatally and exhibit varying combinations of gross developmental defects throughout the second half of development, including acrania, exencephaly, cleft palate, limb abnormalities and omphalocele. These findings demonstrate a role for Hic1 in the development of structures affected in the Miller-Dieker syndrome, and provide functional evidence to strengthen its candidacy as a gene involved in this disorder.

Published

2000

6. Stem Cells and Nuclear Reprogramming

Author

Shinn-Chih Wu, Perng-Chih Shen, Mark G. Carter, Fuliang Du, and Giorgio A. Presicce

Subjects

lcsh:Internal medicine, Cell type, Article Subject, Cellular differentiation, Cell Biology, Biology, Embryonic stem cell, Cell biology, Editorial, Epigenetics, Stem cell, lcsh:RC31-1245, Induced pluripotent stem cell, Molecular Biology, Reprogramming, Adult stem cell

Abstract

Stem cells are found in all multicellular organisms, including two broadly defined cell types: embryonic stem cells (ESC) (C. Y. Cheong and T. Lufkin; and N. Lifantseva et al.) that are derived from the inner cell mass of blastocyst-stage embryos and adult stem cells that are present in adult tissues (C. M. Teven et al., R. Chung et al., and A. C. Wilber et al.). Nuclear reprogramming refers to the erasure and remodeling of epigenetic marks, which is a part of normal mammalian development. This reprogramming is likely required for totipotency of the newly formed embryo and erasure of acquired epigenetic changes (Felici). Advances in stem cells including induced pluripotent stem (IPS) cells (D. Dey and G. R. D. Evans; and P. Noisa and R. Parnpai) and nuclear reprogramming (C. M. Teven et al.) will provide new insights into the mechanisms of cellular differentiation, during embryonic development (N. Lifantsevaa et al.) as well as in adult tissues (C. M. Teven et al.), and their pluripotency (A. C. Wilber et al.), which may lead to cell-based therapies (R. Eggenschwiler et al.) for several human diseases (R. Chung et al.). Fuliang Du Mark G. Carter Giorgio A. Presicce Shinn-Chih Wu Perng-Chih Shen

Published

2011

7. An in situ hybridization-based screen for heterogeneously expressed genes in mouse ES cells

Author

Nabeebi Shaik, Carole A. Stagg, Lioudmila V. Sharova, Kazuhiro Aiba, Minoru S.H. Ko, Geppino Falco, Toshiyuki Yoshikawa, Mark G. Carter, Uwem C. Bassey, Carter, Mark G., Stagg, Carole A., Falco, Geppino, Yoshikawa, Toshiyuki, Bassey, Uwem C., Aiba, Kazuhiro, Sharova, Lioudmila V., Shaik, Nabeebi, and Ko, Minoru S. H.

Subjects

Homeobox protein NANOG, Whsc2, Cellular differentiation, Rex1, Rest, Pluripotent stem cell, Pa2g4, Mice, Inbred Strains, In situ hybridization, Oct4, Biology, Nanog, Article, Fscn1, Cell Line, E2f2, Mice, Rhox9, Gene expression, Genetics, Animals, ES cell, Atf4, Esrrb, Molecular Biology, Gene, EC cell, Embryonic Stem Cells, In Situ Hybridization, Krt8, Pgc7, Gene Expression Profiling, Zscan4, EndoA, Zfp42, Dppa3, Molecular biology, Homogeneous gene expression, Stella, Nelfa, Oct3/4, Gene expression profiling, Cell culture, Heterogeneous gene expression, Pou5f1, Transcription Factors, Developmental Biology

Abstract

We previously reported that Zscan4 showed heterogeneous expression patterns in mouse embryonic stem (ES) cells. To identify genes that show similar expression patterns, we carried out high-throughput in situ hybridization assays on ES cell cultures for 244 genes. Most of the genes are involved in transcriptional regulation, and were selected using microarray-based comparisons of gene expression profiles in ES and embryonal carcinoma (EC) cells versus differentiated cell types. Pou5f1 (Oct4, Oct3/4) and Krt8 (EndoA) were used as controls. Hybridization signals were detected on ES cell colonies for 147 genes (60%). The majority (136 genes) of them showed relatively homogeneous expression in ES cell colonies. However, we found that two genes unequivocally showed Zscan4-like spotted expression pattern (spot-in-colony pattern; Whsc2 and Rhox9). We also found that nine genes showed relatively heterogeneous expression pattern (mosaic-in-colony pattern: Zfp42/Rex1, Rest, Atf4, Pa2g4, E2f2, Nanog, Dppa3/Pgc7/Stella, Esrrb, and Fscn1). Among these genes, Zfp42/Rex1 showed unequivocally heterogeneous expression in individual ES cells prepared by the CytoSpin. These results show the presence of different types or states of cells within ES cell cultures otherwise thought to be undifferentiated and homogeneous, suggesting a previously unappreciated complexity in ES cell cultures.

Published

2008

8. Defining a developmental path to neural fate by global expression profiling of mouse embryonic stem cells and adult neural stem/progenitor cells

Author

Minoru S.H. Ko, Chiara Foroni, Mark G. Carter, Kazuhiro Aiba, Alexei A. Sharov, Angelo L. Vescovi, Aiba, K, Sharov, A, Carter, M, Foroni, C, Vescovi, A, and Ko, M

Subjects

Cellular differentiation, Embryoid body, Biology, Microarray, Mice, Neurosphere, Animals, Oligonucleotide Array Sequence Analysis, Neurons, Principal Component Analysis, Gene Expression Profiling, Multipotent Stem Cells, Cell Differentiation, Cell Biology, Neural stem, Molecular biology, Neural stem cell, Cell biology, Neuroepithelial cell, Endothelial stem cell, Embryonic stem cell, Progenitor cell, Molecular Medicine, Stem cell, Neural differentiation, Totipotent Stem Cells, Neural commitment, Developmental Biology, Adult stem cell

Abstract

To understand global features of gene expression changes during in vitro neural differentiation, we carried out the microarray analysis of embryonic stem cells (ESCs), embryonal carcinoma cells, and adult neural stem/progenitor (NS) cells. Expression profiling of ESCs during differentiation in monolayer culture revealed three distinct phases: undifferentiated ESCs, primitive ectoderm-like cells, and neural progenitor cells. Principal component (PC) analysis revealed that these cells were aligned on PC1 over the course of 6 days. This PC1 represents approximately 4,000 genes, the expression of which increased with neural commitment/differentiation. Furthermore, NS cells derived from adult brain and their differentiated cells were positioned along this PC axis further away from undifferentiated ESCs than embryonic stem–derived neural progenitors. We suggest that this PC1 defines a path to neural fate, providing a scale for the degree of commitment/differentiation.

Published

2005

9. Gene expression changes at metamorphosis induced by thyroid hormone in Xenopus laevis tadpoles

Author

Minoru S.H. Ko, Mark G. Carter, Donald D. Brown, Yu Lan Piao, Alexei A. Sharov, Liquan Cai, and Biswajit Das

Subjects

Tail, Thyroid Hormones, Transcription, Genetic, Brain ventricle proliferation, Xenopus, Cell cycle, Xenopus laevis, Transcriptional regulation, Transcription (biology), Gene expression, medicine, Animals, Limb growth, Fibroblast, Gene, Molecular Biology, Tadpole, Mitochondrial electron transport chain, biology, Metamorphosis, Gene Expression Profiling, Proteolytic enzymes, Metamorphosis, Biological, Brain, Gene Expression Regulation, Developmental, Cell Biology, biology.organism_classification, Molecular biology, Hindlimb, Gene expression profiling, Thyroid hormone, medicine.anatomical_structure, Larva, Tail resorption, Developmental Biology

Abstract

Thyroid hormone (TH) controlled gene expression profiles have been studied in the tail, hind limb and brain tissues during TH-induced and spontaneous Xenopus laevis metamorphosis. Amplified cRNA probes mixed with a universal standard were hybridized to a set of 21,807-sense strand 60-mer oligonucleotides on each slide representing the entries in X. laevis UniGene Build 48. Most of the up-regulated genes in hind limb and brain are the same. This reflects in part the fact that the initial response to TH induction in both tissues is cell proliferation. A large number of up-regulated genes in the limb and brain programs encode common components of the cell cycle, DNA and RNA metabolism, transcription and translation. Notch is one of the few genes that is differentially expressed exclusively in the brain in the first 48 h of TH induction studied in these experiments. The TH-induced gene expression changes in the tail are different from the limb and brain programs. Distinct muscle and fibroblast programs were identified in the tail. Dying muscle fibers in tail (marked by active caspase-3) up-regulate a group of genes that include proteolytic enzymes. At the climax of metamorphosis, tail muscle down-regulates more than half of the genes that encode the glycolytic enzymes in the cytoplasm and the tricarboxylic acid pathway and all five complexes of the electron transport system in mitochondria. These changes in gene expression precede the activation of caspase-3. Some of these same energy metabolism-related genes are up-regulated in the limb and brain programs by TH. A prominent feature of the tail fibroblasts is the down-regulation of several collagen and other extra cellular matrix genes and the up-regulation of hydrolytic enzymes that are responsible for dissolving the notochord and resorbing the tail.

Published

2005

10. High-throughput screen for genes predominantly expressed in the ICM of mouse blastocysts by whole mount in situ hybridization

Author

Mark G. Carter, Minoru S.H. Ko, Yulan Piao, Yuxia Wang, Toshiyuki Yoshikawa, Ilya G. Goldberg, Ryo Matoba, and Jinhui Zhong

Subjects

Candidate gene, In situ hybridization, Biology, In Vitro Techniques, Article, Mice, Genetics, medicine, Inner cell mass, Animals, Blastocyst, Genetic Testing, Molecular Biology, Gene, In Situ Hybridization, Computational Biology, Gene Expression Regulation, Developmental, Embryo, Genomics, Molecular biology, Embryonic stem cell, medicine.anatomical_structure, embryonic structures, Stem cell, Developmental Biology

Abstract

Mammalian preimplantation embryos provide an excellent opportunity to study temporal and spatial gene expression in whole mount in situ hybridization (WISH). However, large-scale studies are made difficult by the size of the embryos ( approximately 60mum diameter) and their fragility. We have developed a chamber system that allows parallel processing of embryos without the aid of a microscope. We first selected 91 candidate genes that were transcription factors highly expressed in blastocysts, and more highly expressed in embryonic (ES) than in trophoblast (TS) stem cells. We then used the WISH to identify 48 genes expressed predominantly in the inner cell mass (ICM) and to follow several of these genes in all seven preimplantation stages. The ICM-predominant expressions of these genes suggest their involvement in the pluripotency of embryonic cells. This system provides a useful tool to a systematic genome-scale analysis of preimplantation embryos.

Published

2005

11. Age-associated alteration of gene expression patterns in mouse oocytes

Author

Vincent VanBuren, Hidenori Akutsu, Alexei A. Sharov, Dawood B. Dudekula, Mark G. Carter, Geppino Falco, Toshio Hamatani, Minoru S.H. Ko, Carole A. Stagg, Hamatani, Toshio, Falco, Geppino, Carter, Mark G., Akutsu, Hidenori, Stagg, Carole A., Sharov, Alexei A., Dudekula, Dawood B., Vanburen, Vincent, and Ko, Minoru S. H.

Subjects

Oocyte, Aging, Biology, Andrology, Mice, Gene expression, Genetics, medicine, Gene family, Animals, Humans, Molecular Biology, Gene, Metaphase, Genetics (clinical), Phylogeny, Oligonucleotide Array Sequence Analysis, Animal, Oligonucleotide Array Sequence Analysi, Gene Expression Profiling, Biomarker, General Medicine, Chromatin, Gene expression profiling, Mice, Inbred C57BL, medicine.anatomical_structure, DNA methylation, Oocytes, Female, Biomarkers, Human

Abstract

Decreasing oocyte competence with maternal aging is a major factor in human infertility. To investigate the age-dependent molecular changes in a mouse model, we compared the expression profiles of metaphase II oocytes collected from 5- to 6-week-old mice with those collected from 42- to 45-week-old mice using the NIA 22K 60-mer oligo microarray. Among approximately 11 000 genes whose transcripts were detected in oocytes, about 5% (530) showed statistically significant expression changes, excluding the possibility of global decline in transcript abundance. Consistent with the generally accepted view of aging, the differentially expressed genes included ones involved in mitochondrial function and oxidative stress. However, the expression of other genes involved in chromatin structure, DNA methylation, genome stability and RNA helicases was also altered, suggesting the existence of additional mechanisms for aging. Among the transcripts decreased with aging, we identified and characterized a group of new oocyte-specific genes, members of the human NACHT, leucine-rich repeat and PYD-containing (NALP) gene family. These results have implications for aging research as well as for clinical ooplasmic donation to rejuvenate aging oocytes. © Oxford University Press 2004; all rights reserved.

Published

2004

12. Klotho gene variation and expression in 20 inbred mouse strains

Author

Clair A. Francomano, Harry C. Dietz, Mark G. Carter, Alexei A. Sharov, Arsun Bektas, and Shepherd H. Schurman

Subjects

Gene isoform, Arteriosclerosis, Molecular Sequence Data, Mice, Inbred Strains, Biology, urologic and male genital diseases, Kidney, Exon, Mice, Inbred strain, Genetic variation, Genetics, Animals, Humans, Klotho, Gene, Hearing Disorders, Klotho Proteins, Glucuronidase, chemistry.chemical_classification, Base Sequence, Cell Membrane, Kidney metabolism, Genetic Variation, Membrane Proteins, Aging, Premature, Molecular biology, Amino acid, chemistry, Amino Acid Substitution

Abstract

A defect in klotho gene expression in the mouse results in a syndrome that resembles human aging, with greatly shortened lifespan, arteriosclerosis, and defective hearing. In an effort to find functional murine variants of klotho, we sequenced the gene and examined renal expression of the secreted and membrane-bound Klotho isoforms from 16 laboratory-derived and 4 wild-derived inbred strains. Among the laboratory-derived strains, no sequence variation was found in any of the exons or intron-exon boundaries. Among the wild-derived strains, we found 45 sequence variants with six resulting in amino acid substitutions. One wild-derived strain, SPRET/Ei, had four amino acid substitutions and higher levels of the membrane form and total klotho mRNA. In addition, the membrane to secreted klotho expression ratio was elevated in three wild-derived strains with amino acid substitutions. Interestingly, SPRET/Ei mice have longer lifespans, decreased atherosclerosis risk factors, and better hearing than almost all other mouse strains.

Published

2004

13. In Situ-Synthesized Novel Microarray Optimized for Mouse Stem Cell and Early Developmental Expression Profiling

Author

Mark G. Carter, Pius M. Brzoska, Naomi T. Ko, Condie E. Carmack, Dawood B. Dudekula, Alexei A. Sharov, Toshio Hamatani, Yong Qian, Minoru S.H. Ko, S. Stuart Hwang, and Kazuhiro Aiba

Subjects

Chemical compound microarray, Microarray, Placenta, Oligonucleotides, Computational biology, Biology, Polymerase Chain Reaction, Sensitivity and Specificity, Mice, Complementary DNA, Genetics, Animals, Genetics (clinical), In Situ Hybridization, Oligonucleotide Array Sequence Analysis, cDNA library, Oligonucleotide, Gene Expression Profiling, Stem Cells, RNA, Gene Expression Regulation, Developmental, Embryo, Mammalian, Molecular biology, Resources, Gene expression profiling, Mice, Inbred C57BL, Multigene Family, Female, DNA microarray

Abstract

Applications of microarray technologies to mouse embryology/genetics have been limited, due to the nonavailability of microarrays containing large numbers of embryonic genes and the gap between microgram quantities of RNA required by typical microarray methods and the miniscule amounts of tissue available to researchers. To overcome these problems, we have developed a microarray platform containing in situ-synthesized 60-mer oligonucleotide probes representing approximately 22,000 unique mouse transcripts, assembled primarily from sequences of stem cell and embryo cDNA libraries. We have optimized RNA labeling protocols and experimental designs to use as little as 2 ng total RNA reliably and reproducibly. At least 98% of the probes contained in the microarray correspond to clones in our publicly available collections, making cDNAs readily available for further experimentation on genes of interest. These characteristics, combined with the ability to profile very small samples, make this system a resource for stem cell and embryogenomics research.[Supplemental material is available online atwww.genome.org and at the NIA Mouse cDNA Project Web site,http://lgsun.grc.nia.nih.gov/cDNA/cDNA.html.]

Published

2003

14. Transgenic animal bioreactors: A new line of defense against chemical weapons?

Author

Xiangzhong Yang and Mark G. Carter

Subjects

Cloning, Cell type, Multidisciplinary, Transgene, Mice, Transgenic, Biological Sciences, Biology, Molecular biology, Recombinant Proteins, Genetically modified organism, law.invention, Cell biology, Animals, Genetically Modified, Gene product, Transgenesis, Mice, Bioreactors, law, Butyrylcholinesterase, Gene expression, Recombinant DNA, Animals, Cloning, Molecular

Abstract

Dangerous organophosphorus (OP) compounds have been used as insecticides in agriculture and in chemical warfare. Because exposure to OP could create a danger for humans in the future, butyrylcholinesterase (BChE) has been developed for prophylaxis to these chemicals. Because it is impractical to obtain sufficient quantities of plasma BChE to treat humans exposed to OP agents, the production of recombinant BChE (rBChE) in milk of transgenic animals was investigated. Transgenic mice and goats were generated with human BChE cDNA under control of the goat β-casein promoter. Milk from transgenic animals contained 0.1–5 g/liter of active rBChE. The plasma half-life of PEGylated, goat-derived, purified rBChE in guinea pigs was 7-fold longer than non-PEGylated dimers. The rBChE from transgenic mice was inhibited by nerve agents at a 1:1 molar ratio. Transgenic goats produced active rBChE in milk sufficient for prophylaxis of humans at risk for exposure to OP agents.

Published

2007

15. 42 EFFECTS OF TRICHOSTATIN A TREATMENT ON GENE EXPRESSION OF CLONED MOUSE 2-CELL AND BLASTOCYST STAGE EMBRYOS

Author

L-Y. Sung, Xiangzhong Yang, Sadie L. Marjani, H. Shen, Mark G. Carter, L. Wang, K. Inoue, T. Cheng, H. Yu, Sandra L. Rodriguez-Zas, and Xiuchun Cindy Tian

Subjects

Genetics, Cloning, Embryo culture, Embryo, Reproductive technology, Biology, Embryonic stem cell, Andrology, Endocrinology, medicine.anatomical_structure, Trichostatin A, Reproductive Medicine, embryonic structures, medicine, Somatic cell nuclear transfer, Animal Science and Zoology, Blastocyst, Molecular Biology, Developmental Biology, Biotechnology, medicine.drug

Abstract

Trichostatin A (TSA) is a potent inhibitor of histone deacetylases and has been shown to improve cloned embryo pre-implantation and term development. We examined the effects of TSA treatment on cloned mouse embryonic gene expression using microarrays. Cloned mouse embryos were generated using long-term haematopoietic stem cells (LT-HSC) and terminally differentiated granulocytes (Gr-1) as nuclear donors, which have been shown to have significantly different cloning efficiencies (Sung et al. 2006 Nat. Gen. 38, 1323–1328). Late 2-cell and blastocyst stage cloned embryos and control, BDF1 in vivo and IVF embryos (n = 10 from each embryo type and stage, except LT-HSC blastocysts, where n = 5) were snap frozen in liquid nitrogen. Total RNA was isolated from individual embryos and amplified using the TargetAmp 2 round Aminoallyl aRNA amplification kit (Epicentre Biotechnologies, Madison, WI, USA). Amplified RNA from each embryo and a standard reference was labelled with Cy3 or Cy5 and hybridized to the mouse exonic evidence based oligonucleotide (MEEBO) microarray allowing for the interrogation of ~25 000 genes. After Loess normalization, ANOVA with false discovery rate (P

Published

2014

16. 278 Jak/Stat3 SIGNALING PROMOTES SOMATIC CELL REPROGRAMMING BY EPIGENETIC REGULATION

Author

Mark G. Carter, Xiuchun Cindy Tian, Y. Luo, Zongliang Jiang, and Y. Tang

Subjects

Homeobox protein NANOG, Rex1, Biology, Embryonic stem cell, Molecular biology, Cell biology, Endocrinology, DNA demethylation, Reproductive Medicine, embryonic structures, Genetics, Animal Science and Zoology, Epigenetics, Induced pluripotent stem cell, Molecular Biology, Leukemia inhibitory factor, Reprogramming, Developmental Biology, Biotechnology

Abstract

Although leukemia inhibitory factor (LIF) maintains the ground state pluripotency of mouse embryonic stem cells and induced pluripotent stem cells (iPSC) by activating the Janus kinase/signal transducer and activator of transcription 3 (Jak/Stat3) pathway, the mechanism remains unclear. Stat3 has only been shown to promote complete reprogramming of epiblast and neural stem cells, and the partially reprogrammed cells (pre-iPSC). We investigated if and how Jak/Stat3 activation promotes reprogramming of terminally differentiated mouse embryonic fibroblasts (MEF). We demonstrated that activated Stat3 not only promotes but is essential for the pluripotency establishment in MEF cell reprogramming. We further demonstrated that, during reprogramming, inhibiting Jak/Stat3 activity blocks demethylation of Oct4 and Nanog regulatory DNA sequences in induced cells, which are marked by suppressed endogenous pluripotent gene expression. These are correlated with significant upregulation of DNA methyltransferase (Dnmt) 1 and histone deacetylases (HDAC) expression, as well as the increased expression of lysine-specific histone demethylase 2 and methyl-CpG binding protein 2. Inhibiting Jak/Stat3 also blocks the expression of Dnmt3L, which is correlated with the failure of retroviral transgene silencing. Furthermore, Dnmt or HDAC inhibitor but not overexpression of Nanog rescues the reprogramming arrested by Jak/Stat3 inhibition or LIF deprivation. Finally, we demonstrated that LIF/Stat3 signal also represents the prerequisite for complete reprogramming of pre-iPSC. We conclude that Jak/Stat3 activity plays a fundamental role in promoting the establishment of pluripotency at the epigenetic level, by facilitating DNA demethylation/de novo methylation and open-chromatin formation during late stage reprogramming.

Published

2013

17. Dissecting Oct3/4-Regulated Gene Networks in Embryonic Stem Cells by Expression Profiling

Author

Hitoshi Niwa, Minoru S.H. Ko, Alexei A. Sharov, Shinji Masui, Mark G. Carter, Satoshi Ohtsuka, and Ryo Matoba

Subjects

Cellular differentiation, lcsh:Medicine, Biology, Mice, 03 medical and health sciences, 0302 clinical medicine, Proto-Oncogene Proteins, Gene expression, Animals, Gene Regulatory Networks, RNA, Small Interfering, lcsh:Science, Promoter Regions, Genetic, Molecular Biology, Transcription factor, Embryonic Stem Cells, Oligonucleotide Array Sequence Analysis, 030304 developmental biology, Regulation of gene expression, 0303 health sciences, Binding Sites, Computational Biology/Systems Biology, Multidisciplinary, Base Sequence, POU domain, Gene Expression Profiling, Genetics and Genomics/Gene Therapy, lcsh:R, Cell Differentiation, Promoter, DNA, Cell Biology, Molecular biology, Gene expression profiling, 030220 oncology & carcinogenesis, lcsh:Q, DNA microarray, Octamer Transcription Factor-3, Proto-Oncogene Proteins c-akt, Research Article, Developmental Biology

Abstract

POU transcription factor Pou5f1 (Oct3/4) is required to maintain ES cells in an undifferentiated state. Here we show that global expression profiling of Oct3/4-manipulated ES cells delineates the downstream target genes of Oct3/4. Combined with data from genome-wide chromatin-immunoprecipitation (ChIP) assays, this analysis identifies not only primary downstream targets of Oct3/4, but also secondary or tertiary targets. Furthermore, the analysis also reveals that downstream target genes are regulated either positively or negatively by Oct3/4. Identification of a group of genes that show both activation and repression depending on Oct3/4 expression levels provides a possible mechanism for the requirement of appropriate Oct3/4 expression to maintain undifferentiated ES cells. As a proof-of-principle study, one of the downstream genes, Tcl1, has been analyzed in detail. We show that Oct3/4 binds to the promoter region of Tcl1 and activates its transcription. We also show that Tcl1 is involved in the regulation of proliferation, but not differentiation, in ES cells. These findings suggest that the global expression profiling of gene-manipulated ES cells can help to delineate the structure and dynamics of gene regulatory networks.

Published

2006

18. Dynamics of global gene expression changes during mouse preimplantation development

Author

Alexei A. Sharov, Mark G. Carter, Minoru S.H. Ko, and Toshio Hamatani

Subjects

DNA Replication, Transcriptional Activation, Transcription, Genetic, Zygote, Pair-rule gene, Gene regulatory network, Biology, Morula, General Biochemistry, Genetics and Molecular Biology, Mice, Transcription (biology), Gene expression, Animals, Molecular Biology, Gene, Genetics, Regulation of gene expression, Gene Expression Regulation, Developmental, Cell Differentiation, Cell Biology, DNA Fingerprinting, Cell biology, Gene expression profiling, RNA, Messenger, Stored, Blastocyst, Protein Biosynthesis, Maternal to zygotic transition, Developmental Biology

Abstract

Understanding preimplantation development is important both for basic reproductive biology and for practical applications including regenerative medicine and livestock breeding. Global expression profiles revealed and characterized the distinctive patterns of maternal RNA degradation and zygotic gene activation, including two major transient waves of de novo transcription. The first wave corresponds to zygotic genome activation (ZGA); the second wave, named mid-preimplantation gene activation (MGA), precedes the dynamic morphological and functional changes from the morula to blastocyst stage. Further expression profiling of embryos treated with inhibitors of transcription, translation, and DNA replication revealed that the translation of maternal RNAs is required for the initiation of ZGA. We propose a cascade of gene activation from maternal RNA/protein sets to ZGA gene sets and thence to MGA gene sets. The large number of genes identified as involved in each phase is a first step toward analysis of the complex gene regulatory networks.