Your search keyword '"Raff A"' showing total 125 results

1. A role for Noggin in the development of oligodendrocyte precursor cells

Author

Kondo, Toru and Raff, Martin C.

Subjects

Astrocytes -- Research, Developmental biology -- Research, Biological sciences

Abstract

Oligodendrocyte precursor cells (OPCs) can be differentiated in culture into either oligodendrocytes or type-2 astrocytes (2As), depending on the culture conditions. Whereas oligodendrocyte development can occur in the absence of inducing signals, 2A development apparently cannot. Fetal calf serum (FCS) and bone morphogenetic proteins (BMPs) are powerful inducers of 2A development in culture, but there is no compelling evidence that OPCs develop into astrocytes in vivo. We show here that BMPs are made by glial cells in the developing rat optic nerve, raising the question of why 2As do not normally develop in the optic nerve. We demonstrate that the BMP antagonist Noggin is strongly expressed by both OPCs and type-1 astrocytes in the developing optic nerve. We also show that depletion of Noggin by a small interference RNA inhibits OPC proliferation and induces 2A differentiation in the presence of a low, non-2A-inducing concentration of FCS. By contrast, enforced expression of Noggin in OPCs blocks FCS-induced 2A differentiation. These findings suggest that BMPs in FCS are largely responsible for the 2A-inducing activity of FCS and that Noggin may normally inhibit the formation of 2As in the developing CNS. Keywords: Optic nerve; Oligodendrocyte precursor cells (OPCs); Type-1 astrocytes (1As); Type-2 astrocytes (2As); BMP4; Noggin

Published

2004

2. Pattern formation in a pentameral animal: induction of early adult rudiment development in sea urchins

Author

Minsuk, Sharon B. and Raff, Rudolf A.

Subjects

Biological sciences

Abstract

We investigated adult rudiment induction in the direct-developing sea urchin Heliocidaris erythrogramma microsurgically. After removal of the archenteron (which includes presumptive coelomic mesoderm as well as presumptive endoderm) from late gastrulae, larval ectoderm develops properly but obvious rudiments (tube feet, nervous system, and adult skeleton) fail to form, indicating that coelomic mesoderm, endoderm, or both are required for induction of adult development. Recombination of ectoderm and archenteron rescues development. Implanted endoderm alone or left coelom alone each regenerate the full complement of archenteron derivatives; thus, they are uninformative as to the relative inductive potential of the two regions. However, in isolated ectoderm, more limited regeneration gives rise to larvae containing no archenteron derivatives at all, endoderm only, or both endoderm and left coelom. Adult nervous system begins to develop only in the latter, indicating that left coelom is required for the inductive signal. Isolated ectoderm develops a vestibule (the precursor of adult ectoderm) and correctly regulates vestibular expression of the ectodermal territory marker HeET-1, indicating that the early phase of vestibule development occurs autonomously; only later development requires the inductive signal. Another ectodermal marker, HEARS, is regulated properly in the larval ectoderm region, but not in the vestibule. HEARS regulation thus represents an early response to the inducing signal. We compare HEARS expression in H. erythrogramma with that in indirect developers and discuss its implications for modularity in the evolution of developmental mode. Key Words: induction; signaling; mesoderm; coelom; hydrocoel; vestibule; rudiment; modularity; skeletal patterning.

Published

2002

3. Posttranscriptional regulation of p18 and p27 Cdk inhibitor proteins and the timing of oligodendrocyte differentiation

Author

Tokumoto, Yasuhito M., Apperly, James A., Gao, Fen-Biao, and Raff, Martin C.

Subjects

Genetic transcription -- Regulation, Enzyme inhibitors -- Physiological aspects, Gene expression -- Physiological aspects, Cell proliferation -- Analysis, Biological sciences

Abstract

A cell-intrinsic timer helps control when rodent oligodendrocyte precursor cells (OPCs) exit the cell cycle and terminally differentiate when cultured in platelet-derived growth factor (PDGF) and thyroid hormone (TH). There is evidence that the cyclin-dependent kinase inhibitor (CKI) p27/Kip1 (p27) is a component of this TH-regulated timer, as it increases as OPCs proliferate and is required for the timer to operate accurately. Here, we provide evidence that another CKI, p18/INK (p18), may also be a component of the timer: it increases as OPCs proliferate, and its overexpression in OPCs accelerates the timer, causing the cells to differentiate prematurely. We also show that the overexpression of p27 accelerates the timer and that the increases in both p27 and p18 that occur in proliferating OPCs are controlled posttranscriptionally. By contrast, we show that the overexpression of either p18 or p27 in OPCs proliferating in PDGF and the absence of TH greatly slows the cell cycle but fails to accelerate the spontaneous differentiation that normally occurs independently of TH. Key Words: oligodendrocytes; p18; p27; Cdk inhibitor.

Published

2002

4. An Intrinsic Timer That Controls Cell-Cycle Withdrawal in Cultured Cardiac Myocytes

Author

Burton, P.B.J., Raff, M.C., Kerr, P., Yacoub, M.H., and Barton, P.J.R.

Subjects

Cell cycle -- Research, Cell differentiation -- Research, Muscle cells -- Research, Biological sciences

Abstract

Developing cardiac myocytes divide a limited number of times before they stop and terminally differentiate, but the mechanism that stops their division is unknown. To help study the stopping mechanism, we defined conditions under which embryonic rat cardiac myocytes cultured in serum-free medium proliferate and exit the cell cycle on a schedule that closely resembles that seen in vivo. The culture medium contains FGF-1 and FGF-2, which stimulate cell proliferation, and thyroid hormone, which seems to be necessary for stable cell-cycle exit. Time-lapse video recording shows that the cells within a clone tend to divide a similar number of times before they stop, whereas cells in different clones divide a variable number of times before they stop. Cells cultured at 33 degrees C divide more slowly but stop dividing at around the same time as cells cultured at 37 degrees C, having undergone fewer divisions. Together, these findings suggest that an intrinsic timer helps control when cardiac myocytes withdraw from the cell cycle and that the timer does not operate by simply counting cell divisions. We provide evidence that the cyclin-dependent kinase inhibitors p18 and p27 may be part of the timer and that thyroid hormone may help developing cardiac myocytes stably withdraw from the cell cycle.

Published

1999

5. An Analysis of the Early Events When Oligodendrocyte Precursor Cells Are Triggered to Differentiate by Thyroid Hormone, Retinoic Acid, or PDGF Withdrawal

Author

Tokumoto, Yasuhito M., Durand, Beatrice, and Raff, Martin C.

Subjects

Cell differentiation -- Research, Thyroid hormones -- Physiological aspects, Biological sciences

Abstract

Oligodendrocyte precursor cells withdraw from the cell cycle and terminally differentiate after a limited number of cell divisions. The timing of cell-cycle withdrawal and differentiation is controlled by an intrinsic timer, which consists of a timing component that measures elapsed time and an effector component that arrests the cell cycle and initiates differentiation. The effector component can be triggered by either thyroid hormone (TH) or retinoic acid (RA). In this study we investigate how TH and RA act to trigger differentiation. We show the following: (1) Synthetic retinoids that can inhibit AP-1 transcription factors but do not activate gene transcription cannot trigger the effector mechanism, suggesting that TH and RA do not act only by inhibiting AP-1 activity as previously suggested. (2) Both TH and RA induce a transcriptionally dependent antigenic change in purified precursor cells within 2-4 h. (3) Unexpectedly, even before they differentiate, the precursor cells express ceramide galactosyltransferase (CGT), the enzyme that catalyzes the final step in the synthesis of galactocerebroside, an early marker of oligodendrocyte differentiation. (4) Neither TH nor RA directly activates the transcription of the CGT gene, a number of immediate early genes, or the genes that encode any of the known cyclin-dependent kinase inhibitors. (5) The withdrawal of the mitogen platelet-derived growth factor (PDGF), but not TH or RA treatment, causes a rapid decrease in c-fos, NGFI-A/Krox-24, and cyclin D2 mRNA, even though all three treatments trigger cell-cycle arrest and differentiation. (6) PDGF withdrawal and TH treatment, but not RA treatment, induce an increase in cyclin D3 mRNA within 4 h. Thus, we have not found any early changes in gene expression that occur with all three treatments that trigger oligodendrocyte differentiation.

Published

1999

6. Cell-intrinsic timers and thyroid hormone regulate the probability of cell-cycle withdrawal and differentiation of oligodendrocyte precursor cells

Author

Gao, Fen-Biao, Apperly, James, and Raff, Martin

Subjects

Cell cycle -- Research, Thyroid hormones -- Research, Biological sciences

Abstract

During vertebrate development many types of precursor cells divide a limited number of times before they stop dividing and terminally differentiate. It is unclear what causes the cells to stop dividing when they do. We have been studying this problem in the oligodendrocyte cell lineage, which is responsible for myelination in the vertebrate central nervous system. Here we show for the first time that in clonal cultures of oligodendrocyte precursor cells purified from embryonic day 18 (E18) rat optic nerves the first oligodendrocytes develop within 3-4 days, equivalent to the time they first differentiate in the nerve, and that this timely differentiation depends on the presence of thyroid hormone. These findings suggest that a cell-intrinsic, thyroid-hormone-regulated timer determines when the first oligodendrocytes develop. Whereas the first oligodendrocytes develop asynchronously within clones, the vast majority develop after the first week in culture and do so more synchronously within clones. We show that [Beta]1 thyroid hormone receptors in the precursor cells increase in clonal cultures in the absence of thyroid hormone in parallel with the increasing sensitivity of the cells to the cell-cycle-arresting activity of thyroid hormone; moreover, the increase in [Beta]1 receptors, like the timer itself, is accelerated at 33 [degrees] C compared to 37 [degrees] C, suggesting that the increase in receptors may be part of the intrinsic timer. Finally, we show that the precursor cells do not divide indefinitely when stimulated to divide extensively in the absence of thyroid hormone but, instead, eventually stop dividing and either die or differentiate.

Published

1998

7. Continuous observation of multipotential retinal progenitor cells in clonal density culture

Author

Jensen, Abbie M. and Raff, Martin C.

Subjects

Stem cells -- Research, Vertebrates -- Research, Neurons -- Research, Mice -- Research, Biological sciences

Abstract

All neural cell types in the vertebrate retina, except astrocytes, have been shown to develop from multipotential progenitor cells. It is not known, however, to what extent the progenitor cells are heterogeneous in their developmental potential or to what extent cell-cell interactions versus cell-autonomous factors influence the types of cells they become. To address these issues we developed a clonal-density cell culture system where mouse retinal progenitor cells can survive, divide, and differentiate. We followed the development of clones both by continuous time-lapse video microscopy and by daily microscopic observation. We show that even when cultured at clonal density in a homogeneous general environment, where they cannot contact cells outside their own clone, the retinal progenitor cells vary in proliferative capacity, cell cycle time, and in the cell types that they generate. In addition, we show that under these conditions single progenitor cells can generate both neurons and glia, in which case the neurons almost always develop before glial cells, as is the case in vivo.

Published

1997

8. Mechanisms of evolutionary changes in timing, spatial expression, and mRNA processing in the msp130 gene in a direct-developing sea urchin, Heliocidaris erythrogramma

Author

Klueg, Kristin M., Harkey, Michael A., and Raff, Rudolf A.

Subjects

Messenger RNA -- Research, Sea urchins -- Genetic aspects, Cytoskeleton -- Research, Biological sciences

Published

1997

9. Genetic analysis of the Drosophila beta3-tubulin gene demonstrates that the microtubule cytoskeleton in the cells of the visceral mesoderm is required for morphogenesis of the midgut endoderm

Author

Dettman, Robert W., Turner, F. Rudolf, and Raff, Elizabeth C.

Subjects

Tubulins -- Genetic aspects, Mutation (Biology) -- Genetic aspects, Cytoskeleton -- Genetic aspects, Morphogenesis -- Genetic aspects, Drosophila -- Genetic aspects, Developmental biology -- Genetic aspects, Biological sciences

Abstract

We have investigated the cellular basis for lethality of mutant alleles of the Drosophila melanogaster [Beta]3-tubulin gene, [Beta]Tub60D. Lethal [Beta]3 mutations can be grouped into two classes: the most severe mutations (Class I alleles) cause death during the first larval instar, while weaker alleles (Class II) cause death in later larval stages or in early pupal development. Since [Beta]3 is not expressed during larval development, lethality of the Class I mutations must reflect essential functions of [Beta]3 in embryogenesis. [Beta]3-tubulin is zygotically expressed during midembryogenesis in the developing mesoderm, and the major site of [Beta]3 accumulation is in the developing muscles during myogenesis. We show that the embryonic pattern of [Beta]3 expression, including accumulation in the developing musculature, is conserved in other Drosophila species. However, we found that loss of [Beta]3 function does not cause discernible defects in either the ultrastructure or function of the larval muscle. Thus [Beta]3-tubulin is dispensable in its highest site of accumulation. Rather, the essential site of function of [Beta]3 in embryos is in cells of the visceral mesoderm. Lethality of Class I alleles is caused by defects in midgut morphogenesis and failure of gut function. Although the folding pattern is irregular and the gut is smaller than normal, a complete folded gut forms in mutant larvae, and the visceral muscle functions normally to move food through the gut. However, mutant larvae cannot absorb nutrients across the gut wall. Thus loss of [Beta]3 function in the mesoderm results in defects in the underlying endodermally derived layer of the gut. Our data provide an assay for cellular interactions between mesoderm and endodermal tissues and reveal a role for the microtubule cytoskeleton of the visceral mesodermal cells in differentiation of the endodermal cell layer of the larval gut.

Published

1996

10. Resynthesizing evolutionary and developmental biology

Author

Gilbert, Scott F., Opitz, John M., and Raff, Rudolf A.

Subjects

Evolution -- Research, Developmental biology -- Research, Embryology -- Analysis, Homology (Biology) -- Analysis, Biological sciences

Published

1996

11. Structure, expression, and extracellular targeting of PM27, a skeletal protein associated specifically with growth of the sea urchin larval spicule

Author

Harkey, Michael A., Klueg, Kristin, Sheppard, Paul, and Raff, Rudolf A.

Subjects

Sea urchins -- Research, Gene expression -- Analysis, Skeleton -- Growth, Biological sciences

Abstract

The PM27 gene is involved in the growth of spicules in the sea urchin larva. This gene encodes a 27 kDa protein whose N-terminus is similar to other fiber-forming proteins and whose C-terminus is similar to C-class lectins. The protein is expressed in the primary mesenchyme cells in the growing tip of the spicule.

Published

1995

12. Tissue-specific microtubule functions in Drosophila spermatogenesis require the beta2-tubulin isotype-specific carboxy terminus

Author

Fackenthal, James D., Turner, F. Rudolf, and Raff, Elizabeth C.

Subjects

Tubulins -- Genetic aspects, Spermatogenesis -- Research, Biological sciences

Abstract

Researchers have identified the degree to which a beta-tubulin isoform without its carboxy terminus can integrate into operational suprastructures by producing two early-stop-codon variants of the gene for the testis-specific beta-tubulin (beta 2) in Drosophila melanogaster. The carboxy terminus of beta 2-tubulin is essential for the alignment of microtubule suprastructures in spermatogenesis.

Published

1993

13. The SpEGF III gene encodes a member of the fibropellins: EGF repeat-containingproteins that form the apical lamina of the sea urchin embryo

Author

Bisgrove, Brent W. and Raff, Rudolf A.

Subjects

Sea urchin embryo -- Genetic aspects, Epidermal growth factor -- Research, Biological sciences

Abstract

Researchers discovered a gene in the sea urchin Strongylocentrotus purpuratus that encodes a protein with multiple epidermal growth factor (EGF)-like patterns. The SpEGF III DNA sequence predicts a 570 amino acid protein with a complex domain structure similar to that of fibropellins, which are protein products of the SpEGF I gene. The timing of the accumulation of SpEGF III protein coincides with a rise in the structural complexity of the apical lamina, and with the developmental period when the lamina is crucial to gastrulation.

Published

1993

14. Role of Thyroid Hormone Receptors in Timing Oligodendrocyte Differentiation

Author

Billon, Nathalie, Tokumoto, Yasuhito, Forrest, Douglas, and Raff, Martin

Subjects

Thyroid hormones -- Physiological aspects, Dendrites -- Physiological aspects, Hormone receptors -- Physiological aspects, Cell differentiation -- Analysis, Biological sciences

Abstract

The timing of oligodendrocyte differentiation is thought to depend on both intracellular mechanisms and extracellular signals. Thyroid hormone (TH) helps control this timing both in vitro and in vivo, but it is still uncertain how it does so. TH acts through nuclear receptors that are encoded by two genes, TR[Alpha] and TR[Beta]. Previous studies suggested that TR[Beta] receptors may mediate the effect of TH on oligodendrocyte precursor cells (OPCs). Consistent with this possibility, we show here that overexpression of TR[Beta]1 promotes precocious oligodendrocyte differentiation, whereas expression of two dominant-negative forms of TR[Beta]1 greatly delays differentiation. Surprisingly, however, we find that postnatal TR[Beta]--/--mice have a normal number of oligodendrocytes in their optic nerves and that TR[Beta]--/-- OPCs stop dividing and differentiate normally in response to TH in vitro. Moreover, we find that OPCs do not express TR[Beta]1 or TR[Beta]2 mRNAs, whereas they do express TR[Alpha]1 and TR[Alpha]2 mRNAs. These findings suggest that [Alpha] receptors mediate the effect of TH on the timing of oligodendrocyte differentiation. We also show that TR[Alpha]2 mRNA, which encodes a dominant-negative form of TR[Alpha], decreases as OPCs proliferate in vitro and in vivo. This decrease may help control when oligodendrocyte precursors differentiate.

Published

2001

15. A role for Noggin in the development of oligodendrocyte precursor cells

Author

Martin Raff and Toru Kondo

Subjects

animal structures, Oligodendrocyte precursor cells (OPCs), Optic nerve, Enzyme-Linked Immunosorbent Assay, Type-2 astrocytes (2As), BMP4, Ciliary neurotrophic factor, Bone morphogenetic protein, Rats, Sprague-Dawley, Noggin, In vivo, Glial Fibrillary Acidic Protein, medicine, Animals, Receptors, Growth Factor, RNA, Messenger, Type-1 astrocytes (1As), Molecular Biology, DNA Primers, Messenger RNA, Base Sequence, biology, Neural tube, Proteins, Cell Differentiation, Bone Morphogenetic Protein Receptors, Cell Biology, Immunohistochemistry, Oligodendrocyte, Rats, Cell biology, Oligodendroglia, medicine.anatomical_structure, embryonic structures, Immunology, biology.protein, lipids (amino acids, peptides, and proteins), Carrier Proteins, Developmental Biology

Abstract

Oligodendrocyte precursor cells (OPCs) can be differentiated in culture into either oligodendrocytes or type-2 astrocytes (2As), depending on the culture conditions. Whereas oligodendrocyte development can occur in the absence of inducing signals, 2A development apparently cannot. Fetal calf serum (FCS) and bone morphogenetic proteins (BMPs) are powerful inducers of 2A development in culture, but there is no compelling evidence that OPCs develop into astrocytes in vivo. We show here that BMPs are made by glial cells in the developing rat optic nerve, raising the question of why 2As do not normally develop in the optic nerve. We demonstrate that the BMP antagonist Noggin is strongly expressed by both OPCs and type-1 astrocytes in the developing optic nerve. We also show that depletion of Noggin by a small interference RNA inhibits OPC proliferation and induces 2A differentiation in the presence of a low, non-2A-inducing concentration of FCS. By contrast, enforced expression of Noggin in OPCs blocks FCS-induced 2A differentiation. These findings suggest that BMPs in FCS are largely responsible for the 2A-inducing activity of FCS and that Noggin may normally inhibit the formation of 2As in the developing CNS.

Published

2004

16. A Transient Specialization of the Microtubule Cytoskeleton Is Required for Differentiation of the Drosophila Visual System

Author

Hoyle, Henry D., Turner, F. Rudolf, and Raff, Elizabeth C.

Subjects

Developmental biology -- Research, Embryology -- Research, Drosophila -- Research, Cell differentiation -- Research, Biological sciences

Abstract

Drosophila [Beta]3-tubulin is an essential isoform expressed during differentiation of many cell types in embryos and pupae. We report here that during pupal development transient [Beta]3 expression demarcates a unique subset of neurons in the developing adult visual system. [Beta]3 is coassembled into microtubules with [Beta]1, the sole [Beta]-tubulin isoform in the permanent microtubule cytoskeleton of the adult eye and brain. Examination of [Beta]3 mutant phenotypes showed that [Beta]3 is required for axonal patterning and connectivity and for spatial positioning within the optic lobe. Comparison of the phenotypes of [Beta]3 mutations with those that result from disruption of the Hedgehog signaling pathway shows that [Beta]3 functions early in the establishment of the adult visual system. Our data support the hypothesis that [Beta]3 confers specialized properties on the microtubules into which it is incorporated. Thus a transient specialization of the microtubule cytoskeleton during differentiation of a specific subset of the neurons has permanent consequences for later cell function. Key Words: Drosophila; microtubules, tubulin expression; retina; optic lobe.

Published

2000

17. Pattern Formation in a Pentameral Animal: Induction of Early Adult Rudiment Development in Sea Urchins

Author

Sharon B. Minsuk and Rudolf A. Raff

Subjects

Mesoderm, animal structures, Intra-embryonic coelom, Ectoderm, Histogenesis, Biology, Models, Biological, Bone and Bones, vestibule, medicine, Animals, Cell Lineage, Muscle, Skeletal, induction, Molecular Biology, modularity, In Situ Hybridization, rudiment, Bone Development, Microscopy, Confocal, coelom, Gene Expression Regulation, Developmental, Cell Biology, Anatomy, hydrocoel, Immunohistochemistry, Recombinant Proteins, medicine.anatomical_structure, Sea Urchins, embryonic structures, Coelom, Endoderm, signaling, Archenteron, skeletal patterning, Enterocoely, Signal Transduction, Developmental Biology

Abstract

We investigated adult rudiment induction in the direct-developing sea urchin Heliocidaris erythrogramma microsurgically. After removal of the archenteron (which includes presumptive coelomic mesoderm as well as presumptive endoderm) from late gastrulae, larval ectoderm develops properly but obvious rudiments (tube feet, nervous system, and adult skeleton) fail to form, indicating that coelomic mesoderm, endoderm, or both are required for induction of adult development. Recombination of ectoderm and archenteron rescues development. Implanted endoderm alone or left coelom alone each regenerate the full complement of archenteron derivatives; thus, they are uninformative as to the relative inductive potential of the two regions. However, in isolated ectoderm, more limited regeneration gives rise to larvae containing no archenteron derivatives at all, endoderm only, or both endoderm and left coelom. Adult nervous system begins to develop only in the latter, indicating that left coelom is required for the inductive signal. Isolated ectoderm develops a vestibule (the precursor of adult ectoderm) and correctly regulates vestibular expression of the ectodermal territory marker HeET-1, indicating that the early phase of vestibule development occurs autonomously; only later development requires the inductive signal. Another ectodermal marker, HeARS, is regulated properly in the larval ectoderm region, but not in the vestibule. HeARS regulation thus represents an early response to the inducing signal. We compare HeARS expression in H. erythrogramma with that in indirect developers and discuss its implications for modularity in the evolution of developmental mode.

Published

2002

18. A Transient Specialization of the Microtubule Cytoskeleton Is Required for Differentiation of the Drosophila Visual System

Author

Elizabeth C. Raff, F. Rudolf Turner, and Henry D. Hoyle

Subjects

Gene isoform, Cell type, retina, Embryo, Nonmammalian, Mutant, Biology, Eye, Animals, Genetically Modified, microtubules, Microtubule, Tubulin, medicine, Animals, Drosophila Proteins, Promoter Regions, Genetic, Ubiquitins, Molecular Biology, Cytoskeleton, Body Patterning, Retina, optic lobe, Optic Lobe, Nonmammalian, Pupa, Gene Expression Regulation, Developmental, Embryo, Cell Biology, Phenotype, Hedgehog signaling pathway, Axons, Cell biology, tubulin expression, medicine.anatomical_structure, Drosophila melanogaster, Mutagenesis, Larva, Insect Proteins, Drosophila, Developmental Biology

Abstract

Drosophila beta3-tubulin is an essential isoform expressed during differentiation of many cell types in embryos and pupae. We report here that during pupal development transient beta3 expression demarcates a unique subset of neurons in the developing adult visual system. beta3 is coassembled into microtubules with beta1, the sole beta-tubulin isoform in the permanent microtubule cytoskeleton of the adult eye and brain. Examination of beta3 mutant phenotypes showed that beta3 is required for axonal patterning and connectivity and for spatial positioning within the optic lobe. Comparison of the phenotypes of beta3 mutations with those that result from disruption of the Hedgehog signaling pathway shows that beta3 functions early in the establishment of the adult visual system. Our data support the hypothesis that beta3 confers specialized properties on the microtubules into which it is incorporated. Thus a transient specialization of the microtubule cytoskeleton during differentiation of a specific subset of the neurons has permanent consequences for later cell function.

Published

2000

19. An Analysis of the Early Events When Oligodendrocyte Precursor Cells Are Triggered to Differentiate by Thyroid Hormone, Retinoic Acid, or PDGF Withdrawal

Author

Béatrice Durand, Yasuhito M. Tokumoto, Martin Raff, MRC Laboratory Mol Cell Biol and Cell Biol, London, and University College of London [London] (UCL)

Subjects

immediate early genes, Cdk inhibitors, Retinoic acid, [SDV.BC.BC]Life Sciences [q-bio]/Cellular Biology/Subcellular Processes [q-bio.SC], Rats, Sprague-Dawley, chemistry.chemical_compound, 0302 clinical medicine, [SDV.BC.IC]Life Sciences [q-bio]/Cellular Biology/Cell Behavior [q-bio.CB], retinoic acid, Cells, Cultured, NGFI-A/Krox-24, Platelet-Derived Growth Factor, 0303 health sciences, biology, Effector, Stem Cells, Cell Differentiation, PDGF, Cyclin-Dependent Kinases, Oligodendroglia, Platelet-derived growth factor receptor, Signal Transduction, c-fos, Thyroid Hormones, D cyclins, ceramide galactosyltransferase, oligodendrocytes, Tretinoin, 03 medical and health sciences, Keratolytic Agents, Cyclin D2, Cyclin-dependent kinase, Cyclins, Precursor cell, Animals, Cyclin D3, Genes, Immediate-Early, Molecular Biology, 030304 developmental biology, Oligodendrocyte differentiation, Cell Biology, thyroid hormone, Rats, [SDV.BDD.EO]Life Sciences [q-bio]/Development Biology/Embryology and Organogenesis, Gene Expression Regulation, chemistry, biology.protein, Cancer research, 030217 neurology & neurosurgery, Developmental Biology

Abstract

International audience; Oligodendrocyte precursor cells withdraw from the cell cycle and terminally differentiate after a limited number of cell divisions. The timing of cell-cycle withdrawal and differentiation is controlled by an intrinsic timer, which consists of a timing component that measures elapsed time and an effector component that arrests the cell cycle and initiates differentiation. The effector component can be triggered by either thyroid hormone (TH) or retinoic acid (RA). In this study we investigate how TH and RA act to trigger differentiation. We show the following: (1) Synthetic retinoids that can inhibit AP-1 transcription factors but do not activate gene transcription cannot trigger the effector mechanism, suggesting that TH and RA do not act only by inhibiting AP-1 activity as previously suggested. (2) Both TH and RA induce a transcriptionally dependent antigenic change in purified precursor cells within 2-4 h. (3) Unexpectedly, even before they differentiate, the precursor cells express ceramide galactosyltransferase (CGT), the enzyme that catalyzes the final step in the synthesis of galactocerebroside, an early marker of oligodendrocyte differentiation. (4) Neither TH nor RA directly activates the transcription of the CGT gene, a number of immediate early genes, or the genes that encode any of the known cyclin-dependent kinase inhibitors. (5) The withdrawal of the mitogen platelet-derived growth factor (PDGF), but not TH or RA treatment, causes a rapid decrease in c-fos, NGFI-A/Krox-24, and cyclin D2 mRNA, even though all three treatments trigger cell-cycle arrest and differentiation. (6) PDGF withdrawal and TH treatment, but not RA treatment, induce an increase in cyclin D3 mRNA within 4 h. Thus, we have not found any early changes in gene expression that occur with all three treatments that trigger oligodendrocyte differentiation.

Published

1999

20. Apextrin, a Novel Extracellular Protein Associated with Larval Ectoderm Evolution in Heliocidaris erythrogramma

Author

Eric S. Haag, Rudolf A. Raff, Mary E. Andrews, and Belinda J. Sly

Subjects

Mesenchyme, Molecular Sequence Data, Ectoderm, Apical cell, 03 medical and health sciences, 0302 clinical medicine, biology.animal, medicine, Extracellular, Animals, Amino Acid Sequence, RNA, Messenger, Cloning, Molecular, Molecular Biology, Sea urchin, 030304 developmental biology, 0303 health sciences, Base Sequence, Sequence Homology, Amino Acid, biology, Proteins, Embryo, Cell Biology, Blastula, biology.organism_classification, Biological Evolution, Immunohistochemistry, Molecular biology, Recombinant Proteins, medicine.anatomical_structure, Larva, Sea Urchins, Heliocidaris, 030217 neurology & neurosurgery, Developmental Biology

Abstract

During the evolution of direct development in the sea urchin Heliocidaris erythrogramma major modifications occurred, which allowed the precocious formation of adult-specific structures and led to a novel larval body that surrounds these structures. The HeET-1 gene was isolated in a differential screen for transcripts enriched in the early embryos of H. erythrogramma relative to those of its indirect-developing congener, H. tuberculata. HeET-1 was unique among the three genes found in that no homologous transcript was detected in H. tuberculata total embryonic RNA blots. To verify this apparently extreme differential expression of the HeET-1 genes in Heliocidaris, we isolated the HeET-1 homologue from H. tuberculata genomic DNA and used it to probe blots of poly(A)+ RNA prepared from H. tuberculata embryos. It is expressed in H. tuberculata embryos at levels undetectable by this technique. The predicted amino acid sequence of HeET-1 suggested that it encodes a novel secreted protein. To assess the function of HeET-1, we raised polyclonal antisera to the HeET-1-encoded protein. We find that it is present in eggs in a type of secretory vesicle and that this maternal pool is gradually secreted after fertilization. As cells acquire apical–basal polarity in the blastula the protein becomes localized to the apical extracellular matrix, leading us to name the protein apextrin. The apical extracellular localization of apextrin is maintained in the columnar cells of the larval ectoderm until their internalization at metamorphosis. Ingressing mesenchyme cells rapidly endocytose apextrin upon leaving the vegetal plate. Comparison with fibropellin III, an apical lamina component, suggests that apextrin is an extracellular protein that is in tighter association with the plasma membrane than is the hyalin layer or apical lamina. We propose that apextrin is involved in apical cell adhesion and that its high level of expression may represent an adaptive cooption necessary for strengthening the large H. erythrogramma embryo.

Published

1999

21. Genetic Analysis of theDrosophilaβ3-Tubulin Gene Demonstrates That the Microtubule Cytoskeleton in the Cells of the Visceral Mesoderm Is Required for Morphogenesis of the Midgut Endoderm

Author

Robert W. Dettman, Elizabeth C. Raff, and F. Rudolf Turner

Subjects

Sarcomeres, Mesoderm, Embryo, Nonmammalian, animal structures, Mutant, Morphogenesis, Biology, Microtubules, Myofibrils, Species Specificity, Tubulin, medicine, Animals, Molecular Biology, Cytoskeleton, Genetics, Myogenesis, Muscles, Endoderm, Embryogenesis, fungi, Cell Differentiation, Embryo, Feeding Behavior, Cell Biology, Immunohistochemistry, Embryonic stem cell, Cell biology, Intestines, Microscopy, Electron, medicine.anatomical_structure, Larva, Drosophila, Genes, Lethal, Developmental Biology

Abstract

We have investigated the cellular basis for lethality of mutant alleles of the Drosophila melanogaster beta3-tubulin gene, betaTub60D. Lethal beta3 mutations can be grouped into two classes: the most severe mutations (Class I alleles) cause death during the first larval instar, while weaker alleles (Class II) cause death in later larval stages or in early pupal development. Since beta3 is not expressed during larval development, lethality of the Class I mutations must reflect essential functions of beta3 in embryogenesis. Beta3-tubulin is zygotically expressed during midembryogenesis in the developing mesoderm, and the major site of beta3 accumulation is in the developing muscles during myogenesis. We show that the embryonic pattern of beta3 expression, including accumulation in the developing musculature, is conserved in other Drosophila species. However, we found that loss of beta3 function does not cause discernible defects in either the ultrastructure or function of the larval muscle. Thus beta3-tubulin is dispensable in its highest site of accumulation. Rather, the essential site of function of beta3 in embryos is in cells of the visceral mesoderm. Lethality of Class I alleles is caused by defects in midgut morphogenesis and failure of gut function. Although the folding pattern is irregular and the gut is smaller than normal, a complete folded gut forms in mutant larvae, and the visceral muscle functions normally to move food through the gut. However, mutant larvae cannot absorb nutrients across the gut wall. Thus loss of beta3 function in the mesoderm results in defects in the underlying endodermally derived layer of the gut. Our data provide an assay for cellular interactions between mesoderm and endodermal tissues and reveal a role for the microtubule cytoskeleton of the visceral mesodermal cells in differentiation of the endodermal cell layer of the larval gut.

Published

1996

22. Tissue-Specific Microtubule Functions in Drosophila Spermatogenesis Require the β2-Tubulin Isotype-Specific Carboxy Terminus

Author

Elizabeth C. Raff, James D. Fackenthal, and F.R. Turner

Subjects

Male, Axoneme, Molecular Sequence Data, Microtubules, Tubulin, Microtubule, Drosophilidae, Animals, Amino Acid Sequence, Spermatogenesis, Molecular Biology, Gene, Alleles, chemistry.chemical_classification, Genetics, Base Sequence, biology, Cell Biology, biology.organism_classification, Null allele, Amino acid, Cell biology, Drosophila melanogaster, chemistry, biology.protein, Developmental Biology

Abstract

beta-Tubulins are encoded by members of multigene families and are generally highly conserved at the sequence level. The carboxyl terminal 15 amino acids are markedly more diverged than the rest of the sequence and constitute an "isotype defining region," which is conserved in corresponding beta-tubulin isoforms in different vertebrate species. It is thought that the carboxy terminus of beta-tubulin may not be required for assembly of microtubules per se, but it may be necessary for conferring properties on beta-tubulins required for isotype-specific functions. We have determined the extent to which a beta-tubulin isoform that lacks its carboxy terminus can assemble into functional suprastructures by generating two early-stop-codon variants of the gene for the testis-specific beta-tubulin (beta 2) in Drosophila melanogaster. We have also sequenced the null allele of this gene and discovered that it also contains an early-stop codon. By examining the products of these genes and the phenotypes they confer, we have determined that the beta-tubulin variants with large truncations (171 or 50 amino acids) do not accumulate to detectable levels and provide no beta-tubulin function. However, a small truncation missing only the terminal 15 amino acids is capable of being assembled into ultrastructurally normal looking microtubules in vivo, even though the truncated protein is less stable than wildtype beta 2. The functional failings of this truncated beta-tubulin are manifested in defective microtubule-based spermatogenic suprastructures, rather than at the level of assembly of individual microtubules. The most remarkable defect conferred by the truncated beta 2 is the failure of axonemes to assemble with proper organization, even though microtubules with presumptive axoneme identity are clearly present. We therefore demonstrate that the carboxy terminus of beta 2-tubulin is indeed required for organization of microtubule suprastructures in spermatogenesis. This observation supports the hypothesis that the variable carboxy terminus mediates isotype-specific microtubule-dependent functions.

Published

1993

23. Fibropellins, products of an EGF repeat-containing gene, form a unique extracellular matrix structure that surrounds the sea urchin embryo

Author

Brent W. Bisgrove, Rudolf A. Raff, and Mary E. Andrews

Subjects

Gene Expression, Cortical granule, Hyaline layer, Antibody Specificity, biology.animal, Botany, Gene expression, Animals, Molecular Biology, Sea urchin, Glycoproteins, chemistry.chemical_classification, Extracellular Matrix Proteins, Epidermal Growth Factor, biology, Cell Biology, biology.organism_classification, Blastula, Strongylocentrotus purpuratus, Fusion protein, Extracellular Matrix, Cell biology, Molecular Weight, Blastocyst, chemistry, Multigene Family, Sea Urchins, embryonic structures, Glycoprotein, Developmental Biology

Abstract

The sea urchin SpEGF I gene belongs to a growing family of developmentally important genes which encode proteins that contain repeated epidermal growth factor-like motifs. To characterize the embryonic expression of the protein products of this gene from Strongylocentrotus purpuratus , we generated polyclonal antisera from SpEGF I fusion proteins. These antibodies recognize two glycoproteins of 145 and 185 kDa, which we have named fibropellins. These proteins are present in unfertilized oocytes and throughout early development. The fibropellins are stored in cytoplasmic vesicles in the oocyte and are released soon after fertilization in a distinct secretory event following the exocytosis of cortical granule contents. Following secretion the proteins are localized in the basal surface of the hyaline layer. At the blastula stage the fibropellins become organized into distinct fibers which form a mesh-like network over the surface of the embryo. During subsequent development to the pluteus larva stage this network increases in overall morphological complexity and becomes regionally distinct. The molecular weights of the fibropellins and their pattern of embryonic localization indicate that these proteins form a component of the hyaline layer previously described as the apical lamina.

Published

1991

24. Novel origins of lineage founder cells in the direct-developing sea urchin Heliocidaris erythrogramma

Author

Rudolf A. Raff and Gregory A. Wray

Subjects

Blastomeres, Cell type, animal structures, Polarity in embryogenesis, Ectoderm, Cell fate determination, Nervous System, Mesoderm, biology.animal, medicine, Animals, Molecular Biology, Sea urchin, biology, Cell Differentiation, Cell Biology, Blastomere, Anatomy, biology.organism_classification, medicine.anatomical_structure, Evolutionary biology, Larva, Sea Urchins, embryonic structures, Endoderm, Heliocidaris, Digestive System, Cell Division, Developmental Biology

Abstract

The lineage and fate of each blastomere in the 32-cell embryo of the direct-developing sea urchin Heliocidaris erythrogramma have been traced by microinjection of tetramethylrhodamine-dextran. The results reveal substantive evolutionary modifications of the ancestral cell lineage pattern of indirect sea urchin development. Significant among these modifications are changes in the time and order of cell lineage segregation: vegetal ectodermal founder cells consistently arise earlier than during indirect development, while internal founder cells generally segregate later and in a different sequence. Modifications have also arisen in proportions of the embryo fated to become various cell types and larval structures. Ectodermal fates, particularly vestibular ectoderm, comprise a greater proportion of the total cellular volume in H. erythrogramma. Among internal cell types, coelom consumes more and endoderm less of the remaining cellular volume than during indirect sea urchin development. Evolutionary modifications are also apparent in the positional origin of larval cell types and structures in H. erythrogramma. These include an apparent tilt in the axis of prospective cell fate relative to the animal-vegetal axis as defined by cleavage planes. Together these evolutionary changes in the cell lineage of H. erythrogramma produce an accelerated loss of dorsoventral symmetry in cell fate relative to indirect development. The extent and diversity of rearrangements in its cell lineage indicate that the nonfeeding larva of H. erythrogramma is a highly modified, novel form rather than a degenerate pluteus larva. These same modifications underscore the evolutionarily flexible relationship between cell lineage, gene expression, and larval morphology in sea urchin development.

Published

1990

25. Corrigendum to 'A role for Noggin in the development of oligodendrocyte precursor cells' [Dev. Bio. 267 (2004) 242–251]

Author

Toru Kondo and Martin Raff

Subjects

Oligodendrocyte progenitor, Cell Biology, Noggin, Biology, Molecular Biology, Cell biology, Developmental Biology

Published

2004

26. Role of thyroid hormone receptors in timing oligodendrocyte differentiation

Author

Martin Raff, Douglas Forrest, Yasuhito M. Tokumoto, and Nathalie Billon

Subjects

medicine.medical_specialty, Thyroid Hormones, Cellular differentiation, Biology, Rats, Sprague-Dawley, Mice, Internal medicine, Precursor cell, medicine, Animals, RNA, Messenger, Receptor, Molecular Biology, DNA Primers, Thyroid hormone receptor, Receptors, Thyroid Hormone, Base Sequence, Oligodendrocyte differentiation, Cell Differentiation, Optic Nerve, Cell Biology, Immunohistochemistry, Oligodendrocyte, Cell biology, Rats, Mice, Inbred C57BL, Oligodendroglia, medicine.anatomical_structure, Endocrinology, Nuclear receptor, Developmental biology, Developmental Biology

Abstract

The timing of oligodendrocyte differentiation is thought to depend on both intracellular mechanisms and extracellular signals. Thyroid hormone (TH) helps control this timing both in vitro and in vivo, but it is still uncertain how it does so. TH acts through nuclear receptors that are encoded by two genes, TRalpha and TRbeta. Previous studies suggested that TRbeta receptors may mediate the effect of TH on oligodendrocyte precursor cells (OPCs). Consistent with this possibility, we show here that overexpression of TRbeta1 promotes precocious oligodendrocyte differentiation, whereas expression of two dominant-negative forms of TRbeta1 greatly delays differentiation. Surprisingly, however, we find that postnatal TRbeta-/- mice have a normal number of oligodendrocytes in their optic nerves and that TRbeta-/- OPCs stop dividing and differentiate normally in response to TH in vitro. Moreover, we find that OPCs do not express TRbeta1 or TRbeta2 mRNAs, whereas they do express TRalpha1 and TRalpha2 mRNAs. These findings suggest that alpha receptors mediate the effect of TH on the timing of oligodendrocyte differentiation. We also show that TRalpha2 mRNA, which encodes a dominant-negative form of TRalpha, decreases as OPCs proliferate in vitro and in vivo. This decrease may help control when oligodendrocyte precursors differentiate.

Published

2001

27. An intrinsic timer that controls cell-cycle withdrawal in cultured cardiac myocytes

Author

Magdi H. Yacoub, Paul B. J. Burton, P. Kerr, Martin Raff, and Paul J.R. Barton

Subjects

medicine.medical_specialty, Cell, Clone (cell biology), Cell Count, Cell Cycle Proteins, Biology, Fibroblast growth factor, Mice, Internal medicine, medicine, Myocyte, Animals, Cyclin-Dependent Kinase Inhibitor p18, Enzyme Inhibitors, Molecular Biology, timer, Cells, Cultured, Mice, Knockout, Microscopy, Video, Cell growth, Myocardium, Tumor Suppressor Proteins, Cell Cycle, Temperature, Cell Differentiation, Heart, Cell Biology, differentiation, Cell cycle, Embryonic stem cell, Immunohistochemistry, Cyclin-Dependent Kinases, Cell biology, culture, Clone Cells, Endocrinology, medicine.anatomical_structure, Triiodothyronine, Fibroblast Growth Factor 2, Carrier Proteins, Microtubule-Associated Proteins, Cell Division, Cyclin-Dependent Kinase Inhibitor p27, Developmental Biology, Hormone

Abstract

Developing cardiac myocytes divide a limited number of times before they stop and terminally differentiate, but the mechanism that stops their division is unknown. To help study the stopping mechanism, we defined conditions under which embryonic rat cardiac myocytes cultured in serum-free medium proliferate and exit the cell cycle on a schedule that closely resembles that seen in vivo. The culture medium contains FGF-1 and FGF-2, which stimulate cell proliferation, and thyroid hormone, which seems to be necessary for stable cell-cycle exit. Time-lapse video recording shows that the cells within a clone tend to divide a similar number of times before they stop, whereas cells in different clones divide a variable number of times before they stop. Cells cultured at 33 degrees C divide more slowly but stop dividing at around the same time as cells cultured at 37 degrees C, having undergone fewer divisions. Together, these findings suggest that an intrinsic timer helps control when cardiac myocytes withdraw from the cell cycle and that the timer does not operate by simply counting cell divisions. We provide evidence that the cyclin-dependent kinase inhibitors p18 and p27 may be part of the timer and that thyroid hormone may help developing cardiac myocytes stably withdraw from the cell cycle.

Published

2000

28. Cell-intrinsic timers and thyroid hormone regulate the probability of cell-cycle withdrawal and differentiation of oligodendrocyte precursor cells

Author

James A. Apperly, Fen-Biao Gao, and Martin Raff

Subjects

endocrine system, medicine.medical_specialty, Thyroid Hormones, medicine.medical_treatment, Biology, Rats, Sprague-Dawley, Internal medicine, Precursor cell, medicine, Animals, Humans, Receptor, Molecular Biology, Cells, Cultured, Thyroid hormone receptor, Microscopy, Confocal, Receptors, Thyroid Hormone, Growth factor, Stem Cells, Thyroid, Cell Cycle, Cell Differentiation, Optic Nerve, Cell Biology, Embryonic stem cell, Oligodendrocyte, Cell biology, Clone Cells, Rats, Oligodendroglia, medicine.anatomical_structure, Endocrinology, Hormone, Developmental Biology

Abstract

During vertebrate development many types of precursor cells divide a limited number of times before they stop dividing and terminally differentiate. It is unclear what causes the cells to stop dividing when they do. We have been studying this problem in the oligodendrocyte cell lineage, which is responsible for myelination in the vertebrate central nervous system. Here we show for the first time that in clonal cultures of oligodendrocyte precursor cells purified from embryonic day 18 (E18) rat optic nerves the first oligodendrocytes develop within 3-4 days, equivalent to the time they first differentiate in the nerve, and that this timely differentiation depends on the presence of thyroid hormone. These findings suggest that a cell-intrinsic, thyroid-hormone-regulated timer determines when the first oligodendrocytes develop. Whereas the first oligodendrocytes develop asynchronously within clones, the vast majority develop after the first week in culture and do so more synchronously within clones. We show that beta1 thyroid hormone receptors in the precursor cells increase in clonal cultures in the absence of thyroid hormone in parallel with the increasing sensitivity of the cells to the cell-cycle-arresting activity of thyroid hormone; moreover, the increase in beta1 receptors, like the timer itself, is accelerated at 33 degrees C compared to 37 degrees C, suggesting that the increase in receptors may be part of the intrinsic timer. Finally, we show that the precursor cells do not divide indefinitely when stimulated to divide extensively in the absence of thyroid hormone but, instead, eventually stop dividing and either die or differentiate.

Published

1998

29. Mechanisms of evolutionary changes in timing, spatial expression, and mRNA processing in the msp130 gene in a direct-developing sea urchin, Heliocidaris erythrogramma

Author

Rudolf A. Raff, Kristin M. Klueg, and Michael A. Harkey

Subjects

0106 biological sciences, Embryo, Nonmammalian, Time Factors, Transcription, Genetic, Mesenchyme, Recombinant Fusion Proteins, Biology, Ingression, 010603 evolutionary biology, 01 natural sciences, Mesoderm, 03 medical and health sciences, Transcription (biology), Genes, Reporter, biology.animal, medicine, Animals, RNA, Messenger, Promoter Regions, Genetic, Molecular Biology, Gene, Sea urchin, 030304 developmental biology, 0303 health sciences, Messenger RNA, Sea urchin skeletogenesis, Gene Expression Regulation, Developmental, Cell Biology, Anatomy, Biological Evolution, Cell biology, Alternative Splicing, medicine.anatomical_structure, Larva, Sea Urchins, Heterochrony, Developmental Biology

Abstract

Developmental processes associated with skeletogenesis differ in the direct-developing sea urchin Heliocidaris erythrogramma from that in Heliocidaris tuberculata and other indirect-developing species. In H. erythrogramma, the differences include ingression of a much higher number of mesenchyme cells, failure of the cells to form the typical ring pattern of cells prior to the onset of skeletogenesis, a significantly reduced larval skeleton, and a delay in timing of expression of the skeletogenic cell-restricted gene msp130. We report that the heterochronic change in msp130 expression is regulated at the level of transcription. By transient expression of reporter constructs containing msp130 promoter regions from direct- and indirect-developing species, we found that this evolutionary change in regulation is consistent with changes in the timing of action of trans -acting factors in skeletogenic mesenchyme cells. We further used these experiments to show that the H. erythrogramma promoter contains elements required for correct spatial expression in the primary mesenchyme cells of an indirect-developing host. We finally show that alternate processing of H. erythrogramma msp130 is thus far specific to this species and not an aspect of adult skeletogenesis.

Published

1997

30. Resynthesizing evolutionary and developmental biology

Author

Rudolf A. Raff, Scott F. Gilbert, and John M. Opitz

Subjects

Modern evolutionary synthesis, Population genetics, Cell Biology, Biology, Macroevolution, Morphogenetic field, Genome, Biological Evolution, Evolutionary biology, Evolutionary developmental biology, Genetics, Homeobox, Animals, Humans, Molecular Biology, Developmental biology, Developmental Biology

Abstract

A new and more robust evolutionary synthesis is emerging that attempts to explain macroevolution as well as microevolutionary events. This new synthesis emphasizes three morphological areas of biology that had been marginalized by the Modern Synthesis of genetics and evolution: embryology, macroevolution, and homology. The foundations for this new synthesis have been provided by new findings from developmental genetics and from the reinterpretation of the fossil record. In this nascent synthesis, macroevolutionary questions are not seen as being soluble by population genetics, and the developmental actions of genes involved with growth and cell specification are seen as being critical for the formation of higher taxa. In addition to discovering the remarkable homologies of homeobox genes and their domains of expression, developmental genetics has recently proposed homologies of process that supplement the older homologies of structure. Homologous developmental pathways, such those involving thewntgenes, are seen in numerous embryonic processes, and they are seen occurring in discrete regions, the morphogenetic fields. These fields (which exemplify the modular nature of developing embryos) are proposed to mediate between genotype and phenotype. Just as the cell (and not its genome) functions as the unit of organic structure and function, so the morphogenetic field (and not the genes or the cells) is seen as a major unit of ontogeny whose changes bring about changes in evolution.

Published

1996

31. The SpEGF III gene encodes a member of the fibropellins: EGF repeat-containing proteins that form the apical lamina of the sea urchin embryo

Author

Brent W. Bisgrove and Rudolf A. Raff

Subjects

Immunoprecipitation, Molecular Sequence Data, Complementary DNA, Gene expression, Animals, Amino Acid Sequence, RNA, Messenger, Molecular Biology, Peptide sequence, Genetics, Messenger RNA, Extracellular Matrix Proteins, biology, Base Sequence, Epidermal Growth Factor, Sequence Homology, Amino Acid, Cell Biology, DNA, biology.organism_classification, Blastula, Avidin, Strongylocentrotus purpuratus, Fusion protein, Cell biology, Extracellular Matrix, Sea Urchins, Developmental Biology

Abstract

We have identified a gene in the sea urchin Strongylocentrotus purpuratus that encodes a protein with multiple epidermal growth factor(EGF)-like motifs. The SpEGF III cDNA sequence predicts a 570 amino acid protein with a complex domain structure similar to that of the fibropellins--the protein products of the SpEGF I gene. A putative hydrophobic leader sequence is followed by an EGF-like motif, a domain similar to complement Cls, seven tandem EGF-like repeats, and a carboxy terminal domain similar to avidin. The 2.9-kb SpEGF III mRNA is expressed from a single copy gene. SpEGF III mRNA is present at low levels in unfertilized eggs and during early cleavage, then rapidly increases in abundance between late morula and mesenchyme blastula stages to maximal levels maintained through subsequent stages. Polyclonal antisera from SpEGF III fusion proteins reveal that the protein is a 100-kDa fibropellin which is present in unfertilized eggs but does not accumulate substantially until the mesenchyme blastula stage. The protein is localized to the apical lamina, a structurally complex component of the extracellular matrix that is made up of three major proteins, two of which are the differentially spliced products of SpEGF I. The size and localization of the SpEGF III protein, and the results of immunoprecipitation assays which reveal that it is tightly associated with the products of SpEGF I, indicate that it is the third major protein component of the apical lamina. The timing of SpEGF III protein accumulation is coincident with an increase in the structural complexity of the apical lamina, and with the developmental period when the apical lamina plays an important role in gastrulation.

Published

1993

32. The 'lecithotrophic' sea urchin Heliocidaris erythrogramma lacks typical yolk platelets and yolk glycoproteins

Author

Gregory A. Wray, William J. Lennarz, Leanne B. Scott, and Rudolf A. Raff

Subjects

animal structures, food.ingredient, Immunoelectron microscopy, Blotting, Western, Egg protein, food, Yolk, biology.animal, Animals, Pluteus, Molecular Biology, Sea urchin, Glycoproteins, Ovum, chemistry.chemical_classification, Organelles, Larva, biology, Embryogenesis, Egg Proteins, Cell Biology, Anatomy, biology.organism_classification, Biological Evolution, Cell biology, Molecular Weight, Microscopy, Electron, chemistry, Sea Urchins, embryonic structures, Glycoprotein, Developmental Biology

Abstract

The sea urchin Heliocidaris tuberculata undergoes typical development, forming an echinoid pluteus larva, whereas H. erythrogramma undergoes direct development via a highly modified, nonfeeding larva. Using a polyclonal antibody prepared against yolk glycoproteins from the typical developer Stronglyocentrotus purpuratus, we found that H. tuberculata contains cross-reactive proteins in abundance, but H. erythrogramma does not. In addition, we used immunoelectron microscopy to demonstrate that unfertilized eggs of H. tuberculata contain yolk platelets, but those of H. erythrogramma do not.

Published

1990

33. Corrigendum to “A role for Noggin in the development of oligodendrocyte precursor cells” [Dev. Bio. 267 (2004) 242–251]

Author

Kondo, Toru, primary and Raff, Martin C, additional

Published

2004

34. Apextrin, a novel extracellular protein associated with larval ectoderm evolution in Heliocidaris erythrogramma

Author

Haag, Eric S., Sly, Belinda J., Andrews, Mary E., and Raff, Rudolf A.

Subjects

Sea urchins -- Research, Developmental biology -- Research, Sea urchin embryo -- Genetic aspects, Biological sciences

Abstract

During the evolution of direct development in the sea urchin Heliocidaris erythrogramma major modifications occurred, which allowed the precocious formation of adult-specific structures and led to a novel larval body that surrounds these structures. The HeET-1 gene was isolated in a differential screen for transcripts enriched in the early embryos of H. erythrogramma relative to those of its indirect-developing congener, H. tuberculata. HeET-1 was unique among the three genes found in that no homologous transcript was detected in H. tuberculata total embryonic RNA blots. To verify this apparently extreme differential expression of the HeET-1 genes in Heliocidaris, we isolated the HeET-1 homologue from H. tuberculata genomic DNA and used it to probe blots of [poly(A).sup.+] RNA prepared from H. tuberculata embryos. It is expressed in H. tuberculata embryos at levels undetectable by this technique. The predicted amino acid sequence of HeET-1 suggested that it encodes a novel secreted protein. To assess the function of HeET-1, we raised polyclonal antisera to the HeET-1-encoded protein. We find that it is present in eggs in a type of secretory vesicle and that this maternal pool is gradually secreted after fertilization. As cells acquire apical-basal polarity in the blastula the protein becomes localized to the apical extracellular matrix, leading us to name the protein apextrin. The apical extracellular localization of apextrin is maintained in the columnar cells of the larval ectoderm until their internalization at metamorphosis. Ingressing mesenchyme cells rapidly endocytose apextrin upon leaving the vegetal plate. Comparison with fibropellin III, an apical lamina component, suggests that apextrin is an extracellular protein that is in tighter association with the plasma membrane than is the hyalin layer or apical lamina. We propose that apextrin is involved in apical cell adhesion and that its high level of expression may represent an adaptive cooption necessary for strengthening the large H. erythrogramma embryo.

Published

1999

35. Mechanisms of Evolutionary Changes in Timing, Spatial Expression, and mRNA Processing in themsp130Gene in a Direct-Developing Sea Urchin,Heliocidaris erythrogramma

Author

Klueg, Kristin M., primary, Harkey, Michael A., additional, and Raff, Rudolf A., additional

Published

1997

36. Genetic Analysis of theDrosophilaβ3-Tubulin Gene Demonstrates That the Microtubule Cytoskeleton in the Cells of the Visceral Mesoderm Is Required for Morphogenesis of the Midgut Endoderm

Author

Dettman, Robert W., primary, Turner, F.Rudolf, additional, and Raff, Elizabeth C., additional

Published

1996

37. Tissue-Specific Microtubule Functions in Drosophila Spermatogenesis Require the β2-Tubulin Isotype-Specific Carboxy Terminus

Author

Fackenthal, James D., primary, Turner, F.Rudolf, additional, and Raff, Elizabeth C., additional

Published

1993

38. The SpEGF III Gene Encodes a Member of the Fibropellins: EGF Repeat-Containing Proteins That Form the Apical Lamina of the Sea Urchin Embryo

Author

Bisgrove, Brent W., primary and Raff, Rudolf A., additional

Published

1993

39. Fibropellins, products of an EGF repeat-containing gene, form a unique extracellular matrix structure that surrounds the sea urchin embryo

Author

Bisgrove, Brent W., primary, Andrews, Mary E., additional, and Raff, Rudolf A., additional

Published

1991

40. The “lecithotrophic” sea urchin Heliocidaris erythrogramma lacks typical yolk platelets and yolk glycoproteins

Author

Scott, Leanne B., primary, Lennarz, William J., additional, Raff, Rudolf A., additional, and Wray, Gregory A., additional

Published

1990

41. Constraint, flexibility, and phylogenetic history in the evolution of direct development in sea urchins

Author

Rudolf A. Raff

Subjects

Larva, Embryo, Nonmammalian, animal structures, biology, Phylogenetic tree, Ecology, Cell Biology, biology.organism_classification, Biological Evolution, Phylogenetics, Evolutionary biology, Sea Urchins, biology.animal, embryonic structures, Animals, Juvenile, Female, Pluteus, Heliocidaris, Molecular Biology, Sea urchin, Heterochrony, Phylogeny, Ovum, Developmental Biology

Abstract

Development in sea urchins typically involves the production of an elaborate feeding larva, the pluteus, within which the juvenile sea urchin grows. However, a significant fraction of sea urchins have completely or partially eliminated the pluteus, and instead undergo direct development from a large egg. Direct development is achieved primarily by heterochrony, that is, by the abbreviation or elimination of larval developmental processes and the acceleration of processes involved in development of adult features. Direct development has evolved independently several times, and in several ways. These radically altered ontogenies offer remarkable opportunities for the study of the mechanisms by which early development undergoes evolutionary modification. The recent availability of monoclonal antibody and cDNA probes that recognize homologous cells in embryos of closely related typical and direct developing species makes possible an experimental analysis of the cellular and molecular bases for heterochronic changes in development.

Published

1987

42. Evolutionary modification of cell lineage in the direct-developing sea urchin Heliocidaris erythrogramma

Author

Rudolf A. Raff and Gregory A. Wray

Subjects

Blastomeres, Microinjections, Cell division, Zygote, Cleavage Stage, Ovum, Ectoderm, Cleavage (embryo), Culture Techniques, biology.animal, Botany, medicine, Animals, Pluteus, Molecular Biology, Sea urchin, Fluorescent Dyes, biology, Cell Differentiation, Embryo, Gastrula, Cell Biology, Blastomere, biology.organism_classification, Biological Evolution, Cell biology, medicine.anatomical_structure, Larva, Sea Urchins, Heliocidaris, Developmental Biology

Abstract

The sea urchin Heliocidaris erythrogramma undergoes direct development, bypassing the usual echinoid pluteus larva. We present an analysis of cell lineage in H. erythrogramma as part of a definition of the mechanistic basis for this evolutionary change in developmental mode. Microinjection of fluoresceinated tracer dye and surface marking with vital dye are used to follow larval fates of 2-cell, 8-cell, and 16-cell blastomeres, and to examine axial specification. The animal-vegetal axis and adult dorsoventral axis are basically unmodified in H. erythrogramma. Animal cell fates are very similar to those of typically developing species; however, vegetal cell fates in H. erythrogramma are substantially altered. Radial differences exist among vegetal blastomere fates in the 8-cell embryo: dorsal vegetal blastomeres contribute proportionately more descendants to ectodermal and fewer to mesodermal fates, while ventral vegetal blastomeres have a complementary bias in fates. In addition, vegetal cell fates are more variable than in typical developers. There are no cells in H. erythrogramma with fates comparable to those of the micromeres and macromeres of typically developing echinoids. Instead, all vegetal cells in the 16-cell embryo can contribute progeny to ectoderm and gut. Alterations have thus arisen in cleavage patterns and timing of cell lineage partitioning during the evolution of direct development in H. erythrogramma.

Published

1989

43. Protein synthesis as an early response to fertilization of the sea urchin egg: A model

Author

Rudolf A. Raff, Dennis E. Leister, Carolyn J. Huffman, John W. Brandis, and Arthur L. Koch

Subjects

Embryo, Nonmammalian, Kinetics, Biology, Models, Biological, Ribosome, Human fertilization, biology.animal, Protein biosynthesis, Animals, Molecular Biology, Sea urchin, Ovum, chemistry.chemical_classification, Messenger RNA, Computers, Proteins, Translation (biology), Cell Biology, Amino acid, Biochemistry, chemistry, Fertilization, Protein Biosynthesis, Sea Urchins, Female, Mathematics, Developmental Biology

Abstract

We have developed a quantitative computer model which simulates the rise in protein synthesis resulting from the fertilization of the sea urchin egg. The model predicts the kinetics of incorporation of radioactively labeled amino acids into proteins for the experimental situation in which the amino acid pool is labeled prior to fertilization. The computer model is used to examine the impact of changes in the values of major parameters such as the time of initiation of protein synthesis, the rate at which mRNA is unmasked, the ribosome transit time, and the rate of depletion of the labeled amino acid pool on the kinetics of amino acid incorporation. When experimentally determined values for these parameters are used the model predicts kinetics which closely approximate the kinetics actually observed in newly fertilized eggs. We suggest that the rate at which mRNA is made available for translation and a change in the elongation rate following fertilization control the rise in protein synthesis, and that both of these processes are initiated within 0–2 min following the initial fertilization event.

Published

1981

44. A test for masked message: The template activity of messenger ribonucleoprotein particles isolated from sea urchin eggs

Author

Elihu M. Young, Rudolf A. Raff, Nancy A. Jenkins, and John F. Kaumeyer

Subjects

Polysome, biology.animal, Botany, Centrifugation, Density Gradient, Protein biosynthesis, Animals, Centrifugation, RNA, Messenger, Molecular Biology, Sea urchin, Ovum, Messenger RNA, biology, Sodium, RNA, Cell Biology, biology.organism_classification, Messenger RNP, Nucleoproteins, Ribonucleoproteins, Echinoderm, Polyribosomes, Protein Biosynthesis, Sea Urchins, embryonic structures, Potassium, Biophysics, Female, Developmental Biology

Abstract

The hypothesis that the “masked message” of unfertilized eggs consists of nontranslatable mRNP particles was directly tested by in vitro translation of mRNPs in a system derived from wheat germ. Three classes of mRNPs were tested: particles prepared from sea urchin eggs in buffers containing 0.35 M K + , particles prepared from sea urchin eggs in 0.35 M Na + , and particles released with EDTA in 0.35 M K + from polysomes of sea urchin embryos cultured in the presence of actinomycin D. The mRNA content of particles was monitored by determination of poly(A) content. The wheat germ system used is quantitatively stimulated by addition of mRNA derived from eggs or from any of the classes of mRNPs used. Particles prepared from eggs with Na + or released from polysomes contain less protein than particles isolated from eggs in K + , and as expected these particles are fully translatable in vitro . Particles prepared from eggs in buffers containing 0.35 M K + produce little or no stimulation in the in vitro system. That this lack of translation represents in vivo masking is indicated by several considerations: (1) The nontranslatable particles were prepared in 0.35 M K + and 5 m M Mg 2+ , ion concentrations similar to those found in echinoderm eggs; (2) density and sedimentation rate characteristics of the particles are little changed by isolation; (3) RNA extracted from isolated particles is fully translatable; and (4) particles prepared from polysomes or under conditions which destabilize RNPs are translatable. These data support the masking hypothesis for the protein synthesis repression system of eggs.

Published

1978

45. Sea urchin primary mesenchyme cells: Relation of cell polarity to the epithelial-mesenchymal transformation

Author

Rudolf A. Raff and John A. Anstrom

Subjects

Cellular differentiation, Mesenchyme, Fluorescent Antibody Technique, Golgi Apparatus, Ingression, Biology, Microtubules, Mesoderm, symbols.namesake, Cell Movement, Cell polarity, Morphogenesis, medicine, Animals, Monensin, Molecular Biology, Cell Membrane, Blastocoel, Cell Differentiation, Epithelial Cells, Microtubule organizing center, Cell migration, Cell Biology, Anatomy, Golgi apparatus, Endocytosis, Cell biology, Microscopy, Electron, medicine.anatomical_structure, Sea Urchins, symbols, Developmental Biology

Abstract

In euechinoid sea urchin embryos, a subset of epithelial cells in the wall of the blastula become pulsatile, elongate, lose connections with their neighboring cells, and move into the blastocoel to form the primary mesenchyme cells. The Golgi apparatus and microtubule organizing center (MTOC) are located at the apical end of these epithelial cells. We show that as primary mesenchyme cells begin to move into the blastocoel, the Golgi apparatus and MTOC move to a new position adjacent to the apical side of the nucleus. They do not move to a position between the nucleus and the leading (i.e., basal) end of the cell as they do in cultured fibroblasts undergoing directed migration. In addition, we have inhibited the movement of membranous vesicles to the cell surface by incubating embryos in the ionophore monensin. We have used antibodies to msp130, a primary mesenchyme cell surface-specific glycoprotein, to demonstrate that monensin inhibits the movement of msp130-containing vesicles to the cell surface. Despite the inhibition of membrane shuttling by monensin, primary mesenchyme cells ingress on schedule and display normal cell-shape changes. We draw two conclusions from our data. First, the cellular elongation that characterizes ingression is not due to the local insertion of membrane at the leading (basal) end of the cell. Second, ingression does not depend upon establishment of the same cell polarity required for fibroblasts to carry out directed cell migration.

Published

1988

46. Astrocytes, ependymal cells, and oligodendrocytes develop on schedule in dissociated cell cultures of embryonic rat brain

Author

Perry P. Bartlett, Martin Raff, and Erika R. Abney

Subjects

Ependymal Cell, Galactosylceramides, Gestational Age, Nerve Tissue Proteins, Biology, Tetanus Toxin, Ependyma, Glial Fibrillary Acidic Protein, medicine, Animals, Cilia, Molecular Biology, Cells, Cultured, Gliogenesis, Glial fibrillary acidic protein, Brain, Cell Biology, Embryonic stem cell, Rats, Cell biology, Neuroepithelial cell, Oligodendroglia, medicine.anatomical_structure, Cell culture, Astrocytes, Immunology, biology.protein, Galactocerebroside, Neuroglia, Developmental Biology, Astrocyte

Abstract

We have used cell-type-specific markers to study the development of neurones and glial cells in dissociated cell cultures of 10-day embryonic rat brain. Tetanus-toxin-binding neurones and phagocytic macrophages with surface receptors for IgG were present from the beginning of such cultures. GFAP + astrocytes developed after 5–6 days, ependymal cells with beating cilia after 7–8 days, and galactocerebroside + oligodendrocytes after 13–14 days in culture. When cultures were prepared from 13-day embryonic brain, these glial cells developed 3 days earlier than they did in cultures of 10-day embryonic brain. When freshly isolated cell suspensions from brains of embryos at various ages were studied, we found that the development of specific neural cells in vivo precisely parallelled their development in vitro . Thus glial cells develop right on schedule in dissociated cell cultures suggesting that biological clocks are more important than positional information in gliogenesis after 10 days gestation. We demonstrate that rat neural antigen-2 (Ran-2) which is defined by a monoclonal antibody is expressed on astrocyte precursors.

Published

1981

47. Messenger ribonucleoprotein particles in developing sea urchin embryos

Author

Rudolf A. Raff and Elihu M. Young

Subjects

Messenger RNA, Transcription, Genetic, RNA, Cell Biology, Biology, Blastula, Molecular biology, Messenger RNP, chemistry.chemical_compound, Nucleoproteins, Ribonucleoproteins, chemistry, Puromycin, Transcription (biology), Polyribosomes, Sea Urchins, Polysome, Dactinomycin, Animals, RNA, Messenger, Poly A, Molecular Biology, Developmental Biology, Ribonucleoprotein

Abstract

Messenger RNA entering polysomes during early development of the sea urchin embryo consists of both oogenetic and newly transcribed sequences. Newly transcribed mRNA enters polysomes rapidly while oogenetic mRNA enters polysomes from a pool of stable, nontranslatable messenger ribonucleoprotein particles (mRNPs) derived from the unfertilized egg. Protein content may relate to differences in the regulation of newly transcribed and oogenetic mRNAs. Oogenetic poly(A) + mRNA was found to be present in both polysomal and subpolysomal fractions of cleavage stage and early blastula stage embryos. This mRNA was found to be present in subpolysomal mRNPs with a density of 1.45 g/cm 3 in Cs 2 SO 4 . Poly(A) + mRNPs released from polysomes of embryos cultured in the presence of actinomycin D sedimented in a broad peak centered at 55 S and contained RNA of 21 S. The density of these particles was sensitive to the method of release; puromycin-released mRNPs had a density of 1.45 g/cm 3 , while EDTA caused a shift in density to 1.55 g/cm 3 , indicating a partial loss of protein. The results with newly synthesized mRNAs contrast sharply. Newly transcribed mRNA in subpolysomal mRNPs had a density of 1.55–1.66 g/cm 3 , a density approaching that of deproteinized RNA. Messenger RNA released from polysomes either by EDTA or puromycin was examined to determine the possible existence of polysomal mRNPs. When [ 3 H]uridine-labeled mRNA was released from late cleavage stage embryo polysomes by either technique, and centrifuged on sucrose gradients, two broad peaks were found. One peak centered at 30 S contained 21 S mRNA while the other at 15 S contained 9 S histone mRNA. When these fractions were fixed with formaldehyde, they banded on Cs 2 SO 4 gradients at a density of 1.60–1.66 g/cm 3 , very similar to that of pure RNA. We conclude that the newly transcribed mRNA may be present in stable mRNPs containing up to 10% protein in either subpolysomal or polysomal fractions. These mRNPs are clearly distinguishable from the protein-rich mRNPs containing oogenetic mRNAs.

Published

1979

48. Polar lobe specific regulation of translation in embryos of Ilyanassa obsoleta

Author

Rudolf A. Raff and Kenneth M. Newrock

Subjects

Time Factors, Transcription, Genetic, Ilyanassa, Snails, Organogenesis, Tritium, Transcription (biology), Protein biosynthesis, Animals, Humans, Carbon Radioisotopes, RNA, Messenger, Molecular Biology, Ovum, Messenger RNA, biology, Ilyanassa obsoleta, RNA, Embryo, Cell Biology, Anatomy, biology.organism_classification, Centrifugation, Zonal, Cell biology, Microscopy, Electron, Germ Cells, RNA, Ribosomal, Protein Biosynthesis, Dactinomycin, Microscopy, Electron, Scanning, Electrophoresis, Polyacrylamide Gel, Female, Cell Division, Developmental Biology

Abstract

Comparisons of the patterns of synthesis of 14 C-labeled proteins of normal embryos of Ilyanassa with the patterns of synthesis of 3 H-labeled proteins of embryos from which the polar lobes had been removed at the trefoil stage were made by coelectrophoresis on polyacrylamide disc gels. Controls utilizing biochemical and morphological markers were performed to assure that normal and delobed embryos were developing at equivalent rates. The expression of significant differences in the patterns of protein synthesis were found between normal and delobed embryos, and these differences were not dependent upon concomitant RNA synthesis. These differences were observable as early as after only 24 hr of development, although organogenesis does not begin until much later in development. Therefore, the observed differences probably reflect determininative events. The results support the hypothesis that the developmental determinants of the polar lobe may include specific, preformed mRNA sequences, or specific regulators of translation.

Published

1975

49. Tracing the development of oligodendrocytes from precursor cells using monoclonal antibodies, fluorescence-activated cell sorting, and cell culture

Author

Martin Raff, Erika R. Abney, and Brenda P. Williams

Subjects

medicine.drug_class, Cell Separation, Biology, Monoclonal antibody, Epitopes, Tissue culture, Tetanus Toxin, Precursor cell, medicine, Animals, Molecular Biology, Cells, Cultured, Neurons, Antibodies, Monoclonal, Brain, Cell Differentiation, Optic Nerve, Rats, Inbred Strains, Complement System Proteins, Cell Biology, Cell sorting, Flow Cytometry, Embryonic stem cell, Rats, Cell biology, Oligodendroglia, Cell killing, Cell culture, Immunology, Immunologic Techniques, biology.protein, Antibody, Neuroglia, Developmental Biology

Abstract

We have used antibody and complement-mediated cell killing, fluorescence-activated cell sorting and tissue culture to study the development of rat oligodendrocytes. We show that (1) three ligands that bind to the majority of CNS neurons (the monoclonal antibodies A4 and A2B5 and tetanus toxin) also bind to immature oligodendrocytes and to precursor cells in 14-day embryonic rat brain that develop into oligodendrocytes in vitro; and (2) precursor cells in 17- to 18-day embryonic rat optic nerve can develop into oligodendrocytes in vitro in the absence of living neurons.

Published

1983

50. Translation of oogenetic mRNA in sea urchin eggs and early embryos

Author

Rudolf A. Raff and John W. Brandis

Subjects

Genetics, Zygote, Translational efficiency, Translation (biology), Cell Biology, Biology, biology.organism_classification, Strongylocentrotus purpuratus, Cell biology, Human fertilization, Polysome, biology.animal, embryonic structures, Protein biosynthesis, Molecular Biology, Sea urchin, Developmental Biology

Abstract

Two independent methods were used to measure the rate of ribosome transit along the average mRNA strand in both unfertilized eggs and zygotes of the sea urchin Strongylocentrotus purpuratus at 16.5°C. The first method provided a direct measurement of ribosome transit times for the synthesis of the weight-average newly released polypeptide (MW = 50,000 in eggs and zygotes). The second method yielded elongation rates for different size classes of nascent peptide chains, from which transit times were calculated. The transit time for unfertilized eggs (the average value based upon measurements made by both methods) is 43 min, which is shortened to 17 min within 30 min after fertilization. Translational efficiencies were calculated by dividing the number of ribosomes on an average-sized polysome by the average ribosome transit times. The translational efficiency for protein synthesis in unfertilized eggs is 0.23 polypeptides completed per mRNA strand per minute, which increases to 0.58 molecules completed per strand per minute in the zygote. These data indicate two- to threefold increase in translational efficiency shortly after fertilization.

Published

1978