Your search keyword '"Gametogenesis physiology"' showing total 11 results

1. Genetic evidence for Amh modulation of gonadotropin actions to control gonadal homeostasis and gametogenesis in zebrafish and its noncanonical signaling through Bmpr2a receptor.

Author

Zhang Z, Wu K, Ren Z, and Ge W

Subjects

Animals, Anti-Mullerian Hormone genetics, Bone Morphogenetic Protein Receptors, Type II genetics, Female, Germ Cells cytology, Gonadotropins genetics, Male, Zebrafish genetics, Zebrafish Proteins genetics, Anti-Mullerian Hormone metabolism, Bone Morphogenetic Protein Receptors, Type II metabolism, Gametogenesis physiology, Germ Cells metabolism, Gonadotropins metabolism, Signal Transduction physiology, Zebrafish metabolism, Zebrafish Proteins metabolism

Abstract

Anti-Müllerian hormone (Amh) plays an important role in gonadal function. Amh deficiency causes severe gonadal dysgenesis and dysfunction in zebrafish, with gonadal hypertrophy in both sexes. However, its mechanism of action remains unknown. Intriguingly, the Amh cognate type II receptor (Amhr2) is missing in the zebrafish genome, in sharp contrast to other species. Using a series of zebrafish mutants ( amh , fshb , fshr and lhcgr ), we provided unequivocal evidence for actions of Amh, via modulation of gonadotropin signaling, on both germ cell proliferation and differentiation. The gonadal hypertrophy in amh mutants was abolished in the absence of Fshr in females or Fshr/Lhcgr in males. Furthermore, we demonstrated that knockout of bmpr2a , but not bmpr2b , phenocopied all phenotypes of the amh mutant in both sexes, including gonadal hypertrophy, hyperproliferation of germ cells, retarded gametogenesis and reduced fshb expression. In summary, the present study provided comprehensive genetic evidence for an intimate interaction of gonadotropin and Amh pathways in gonadal homeostasis and gametogenesis and for Bmpr2a as the possible missing link for Amh signaling in zebrafish., Competing Interests: Competing interestsThe authors declare no competing or financial interests., (© 2020. Published by The Company of Biologists Ltd.)

Published

2020

2. Disruption of amylase genes by RNA interference affects reproduction in the Pacific oyster Crassostrea gigas.

Author

Huvet A, Béguel JP, Cavaleiro NP, Thomas Y, Quillien V, Boudry P, Alunno-Bruscia M, and Fabioux C

Subjects

Amylases metabolism, Animals, Crassostrea genetics, Female, Gametogenesis physiology, Gonads physiology, Male, Reproduction physiology, Amylases genetics, Crassostrea physiology, RNA Interference

Abstract

Feeding strategies and digestive capacities can have important implications for variation in energetic pathways associated with ecological and economically important traits, such as growth or reproduction in bivalve species. Here, we investigated the role of amylase in the digestive processes of Crassostrea gigas, using in vivo RNA interference. This approach also allowed us to investigate the relationship between energy intake by feeding and gametogenesis in oysters. Double-stranded (ds)RNA designed to target the two α-amylase genes A and B was injected in vivo into the visceral mass of oysters at two doses. These treatments caused significant reductions in mean mRNA levels of the amylase genes: -50.7% and -59% mRNA A, and -71.9% and -70.6% mRNA B in 15 and 75 µg dsRNA-injected oysters, respectively, relative to controls. Interestingly, reproductive knock-down phenotypes were observed for both sexes at 48 days post-injection, with a significant reduction of the gonad area (-22.5% relative to controls) and germ cell under-proliferation revealed by histology. In response to the higher dose of dsRNA, we also observed reductions in amylase activity (-53%) and absorption efficiency (-5%). Based on these data, dynamic energy budget modeling showed that the limitation of energy intake by feeding that was induced by injection of amylase dsRNA was insufficient to affect gonadic development at the level observed in the present study. This finding suggests that other driving mechanisms, such as endogenous hormonal modulation, might significantly change energy allocation to reproduction, and increase the maintenance rate in oysters in response to dsRNA injection., (© 2015. Published by The Company of Biologists Ltd.)

Published

2015

3. Plant germline formation: common concepts and developmental flexibility in sexual and asexual reproduction.

Author

Schmidt A, Schmid MW, and Grossniklaus U

Subjects

Cell Polarity physiology, Gametogenesis physiology, Reproduction physiology, Cell Lineage physiology, Epigenesis, Genetic physiology, Gene Expression Regulation, Developmental physiology, Gene Expression Regulation, Plant physiology, Germ Cells, Plant growth & development, Meiosis physiology, Plant Development physiology, Plants genetics

Abstract

The life cycle of flowering plants alternates between two heteromorphic generations: a diploid sporophytic generation and a haploid gametophytic generation. During the development of the plant reproductive lineages - the germlines - typically, single sporophytic (somatic) cells in the flower become committed to undergo meiosis. The resulting spores subsequently develop into highly polarized and differentiated haploid gametophytes that harbour the gametes. Recent studies have provided insights into the genetic basis and regulatory programs underlying cell specification and the acquisition of reproductive fate during both sexual reproduction and asexual (apomictic) reproduction. As we review here, these recent advances emphasize the importance of transcriptional, translational and post-transcriptional regulation, and the role of epigenetic regulatory pathways and hormonal activity., (© 2015. Published by The Company of Biologists Ltd.)

Published

2015

4. How to make a primordial germ cell.

Author

Magnúsdóttir E and Surani MA

Subjects

Animals, Cell Dedifferentiation, Cell Lineage, Embryonic Stem Cells cytology, Embryonic Stem Cells metabolism, Epigenesis, Genetic, Female, Gametogenesis genetics, Gametogenesis physiology, Gene Regulatory Networks, Germ Cells metabolism, Humans, Male, Mice, Pluripotent Stem Cells cytology, Pluripotent Stem Cells metabolism, Stem Cells metabolism, Germ Cells cytology, Stem Cells cytology

Abstract

Primordial germ cells (PGCs) are the precursors of sperm and eggs, which generate a new organism that is capable of creating endless new generations through germ cells. PGCs are specified during early mammalian postimplantation development, and are uniquely programmed for transmission of genetic and epigenetic information to subsequent generations. In this Primer, we summarise the establishment of the fundamental principles of PGC specification during early development and discuss how it is now possible to make mouse PGCs from pluripotent embryonic stem cells, and indeed somatic cells if they are first rendered pluripotent in culture.

Published

2014

5. Drosophila Myt1 is a Cdk1 inhibitory kinase that regulates multiple aspects of cell cycle behavior during gametogenesis.

Author

Jin Z, Homola EM, Goldbach P, Choi Y, Brill JA, and Campbell SD

Subjects

Amino Acid Sequence, Animals, Drosophila physiology, Drosophila Proteins genetics, Female, Male, Microscopy, Fluorescence, Molecular Sequence Data, Mutation genetics, Phosphorylation, Protein Kinases genetics, Sequence Alignment, Sequence Analysis, DNA, CDC2 Protein Kinase metabolism, Cell Cycle physiology, Cell Proliferation, Drosophila genetics, Drosophila Proteins metabolism, Gametogenesis physiology, Phenotype, Protein Kinases metabolism

Abstract

The metazoan Wee1-like kinases Wee1 and Myt1 regulate the essential mitotic regulator Cdk1 by inhibitory phosphorylation. This regulatory mechanism, which prevents Cdk1 from triggering premature mitotic events, is also induced during the DNA damage response and used to coordinate cell proliferation with crucial developmental events. Despite the previously demonstrated role for Myt1 regulation of Cdk1 during meiosis, relatively little is known of how Myt1 functions at other developmental stages. To address this issue, we have undertaken a functional analysis of Drosophila Myt1 that has revealed novel developmental roles for this conserved cell cycle regulator during gametogenesis. Notably, more proliferating cells were observed in myt1 mutant testes and ovaries than controls. This can partly be attributed to ectopic division of germline-associated somatic cells in myt1 mutants, suggesting that Myt1 serves a role in regulating exit from the cell cycle. Moreover, mitotic index measurements suggested that germline stem cells proliferate more rapidly, in myt1 mutant females. In addition, male myt1 germline cells occasionally undergo an extra mitotic division, resulting in meiotic cysts with twice the normal numbers of cells. Based on these observations, we propose that Myt1 serves unique Cdk1 regulatory functions required for efficient coupling of cell differentiation with cell cycle progression.

Published

2005

6. Genetic and molecular identification of genes required for female gametophyte development and function in Arabidopsis.

Author

Pagnussat GC, Yu HJ, Ngo QA, Rajani S, Mayalagu S, Johnson CS, Capron A, Xie LF, Ye D, and Sundaresan V

Subjects

Arabidopsis embryology, Fertilization genetics, Mutation genetics, Phenotype, Arabidopsis cytology, Arabidopsis genetics, Gametogenesis genetics, Gametogenesis physiology, Genes, Plant genetics

Abstract

The plant life cycle involves an alternation of generations between sporophyte and gametophyte. Currently, the genes and pathways involved in gametophytic development and function in flowering plants remain largely unknown. A large-scale mutant screen of Ds transposon insertion lines was employed to identify 130 mutants of Arabidopsis thaliana with defects in female gametophyte development and function. A wide variety of mutant phenotypes were observed, ranging from defects in different stages of early embryo sac development to mutants with apparently normal embryo sacs, but exhibiting defects in processes such as pollen tube guidance, fertilization or early embryo development. Unexpectedly, nearly half of the mutants isolated in this study were found to be primarily defective in post-fertilization processes dependent on the maternal allele, suggesting that genes expressed from the female gametophyte or the maternal genome play a major role in the early development of plant embryos. Sequence identification of the genes disrupted in the mutants revealed genes involved in protein degradation, cell death, signal transduction and transcriptional regulation required for embryo sac development, fertilization and early embryogenesis. These results provide a first comprehensive overview of the genes and gene products involved in female gametophyte development and function within a flowering plant.

Published

2005

7. cgh-1, a conserved predicted RNA helicase required for gametogenesis and protection from physiological germline apoptosis in C. elegans.

Author

Navarro RE, Shim EY, Kohara Y, Singson A, and Blackwell TK

Subjects

Amino Acid Sequence, Animals, Caenorhabditis elegans enzymology, Cell Survival, DEAD-box RNA Helicases, Disorders of Sex Development, Female, Fertility, Gametogenesis physiology, Germ Cells cytology, Germ Cells physiology, Humans, Male, Molecular Sequence Data, Oocytes cytology, RNA Helicases genetics, Apoptosis, Caenorhabditis elegans Proteins, Proto-Oncogene Proteins physiology, RNA Helicases physiology, RNA Nucleotidyltransferases physiology

Abstract

A high frequency of apoptosis is a conserved hallmark of oocyte development. In C. elegans, about half of all developing oocytes are normally killed by a physiological germline-specific apoptosis pathway, apparently so that they donate cytoplasm to the survivors. We have investigated the functions of CGH-1, the C. elegans ortholog of the predicted RNA helicase ste13/ME31B/RCK/p54, which is germline-associated in metazoans and required for sexual reproduction in yeast. We show that CGH-1 is expressed specifically in the germline and early embryo, and is localized to P granules and other possible mRNA-protein particles. cgh-1 is required for oocyte and sperm function. It is also needed to prevent the physiological germline apoptosis mechanism killing essentially all developing oocytes, making lack of cgh-1 function the first stimulus identified that can trigger this mechanism. We conclude that cgh-1 and its orthologs may perform conserved functions during gametogenesis, that in C. elegans certain aspects of oocyte development are monitored by the physiological germline apoptosis pathway, and that similar surveillance mechanisms may contribute to germline apoptosis in other species.

Published

2001

8. Parental methylation patterns of a transgenic locus in adult somatic tissues are imprinted during gametogenesis.

Author

Ueda T, Yamazaki K, Suzuki R, Fujimoto H, Sasaki H, Sakaki Y, and Higashinakagawa T

Subjects

Animals, Cloning, Molecular, Female, Gametogenesis genetics, Male, Metallothionein genetics, Mice, Mice, Transgenic genetics, Polymerase Chain Reaction, Prealbumin genetics, Promoter Regions, Genetic genetics, Gametogenesis physiology, Methylation, Mice, Transgenic physiology

Abstract

The methylation status of a mouse metallothionein-I/human transthyretin fusion gene was studied during gametogenesis in transgenic mice. In the adult tissues of this mouse line, the promoter region of the transgene on chromosome 11 is methylated when it is maternally inherited and undermethylated when it is paternally inherited. Germ cells from various developmental stages of gametogenesis were isolated, and their DNAs were assayed using methylation-sensitive restriction endonucleases and the polymerase chain reaction. Only low to nonexistent levels of transgene methylation were detected in germ cells from 14.5-day-old male and female fetuses irrespective of the parental origin of the transgene. This undermethylated state persisted in oocytes from newborn females as well as in testicular spermatogenic cells and sperm. By contrast, the transgene promoter was completely methylated in fully grown oocytes arrested at the first meiotic prophase. The endogenous metallothionein-I gene promoter, located on a different chromosome, remained undermethylated at all stages examined, consistent with previous findings reported for a typical CpG island. Taken together, the results suggest that parental-specific adult patterns of transgene methylation are established during gametogenesis.

Published

1992

9. The role of initial cells in maize anther morphogenesis.

Author

Dawe RK and Freeling M

Subjects

Microscopy, Electron, Scanning, Morphogenesis physiology, Zea mays ultrastructure, Gametogenesis physiology, Zea mays embryology

Abstract

The near absence of cell movement in plants makes clonal analysis a particularly informative method for reconstructing the early events of organ formation. We traced the patterns of cell division during maize anther development by inducing sector boundaries that preceded the earliest events of anther initiation. In doing this, we were able to estimate the smallest number of cells that are fated to form an anther, characteristic cell division patterns that occur during anther morphogenesis, and the relationship between the pre-existing symmetry of the initial cells and the final symmetry of the mature anther. Four general conclusions are made: (1) anthers are initiated from small groups of 12 or fewer cells in each of two floral meristematic layers; (2) the early growth of the anther is more like a shoot than a glume or leaf; (3) cell ancestry does not dictate basic structure and (4) the orientation of initial cells predicts the orientation of the four pollen-containing microsporangia, which define the axes of symmetry on the mature anther. The final point is discussed with other data, and an explanation involving a 'structural template' is invoked. The idea is that the orientation of initial cells within the floral meristem establishes an architectural pattern into which anther cells are recruited without regard to their cellular lineages. The structural template hypothesis may prove to be generally applicable to problems of pattern formation in plants.

Published

1992

10. The distribution of plasmodesmata and its relationship to morphogenesis in fern gametophytes.

Author

Tilney LG, Cooke TJ, Connelly PS, and Tilney MS

Subjects

Cell Division, Microscopy, Electron, Plants ultrastructure, Gametogenesis physiology, Plant Physiological Phenomena

Abstract

Fern (Onoclea sensibilis) gametophytes when grown in the dark form a linear file of cells (one-dimensional) called a protonema. In the light two-dimensional growth occurs which results in a heart-shaped prothallus one cell thick. The objective of this paper is to relate the most common pattern of cell division observed in developing gametophytes to the formation of the plasmodesmatal network. Since the prothalli are only two dimensional, we can easily determine from thin sections the total number and the density (number per unit surface area) of plasmodesmata at each developmental stage. As the prothallus grows the number of plasmodesmata increases 50-fold in the apical or meristematic cell. This number eventually reaches a plateau even though the density continues to increase with each new cell division. What is particularly striking is that both the number and density of plasmodesmata between adjacent cells is precisely determined. Furthermore, the pattern of plasmodesmata distribution is predictable so that (1) we can identify the apical meristematic cells by their plasmodesmata number, or density, as well as by their size, shape and location, (2) we can predict, again from plasmodesmata number, the location of a future wall of the apical cell prior to its actual formation, (3) we can show that the density of plasmodesmata in the triangular apical cell of the prothallus (14 plasmodesmata microns-2) is comparable to those reported for secretory glands which are known to have high rates of plasmodesmatal transport and (4) we can show that once the plasmodesmata have been formed during division, no subsequent change in the number of plasmodesmata occurs following cell plate formation.

Published

1990

11. Sex determination in the germ line of Drosophila depends on genetic signals and inductive somatic factors.

Author

Nöthiger R, Jonglez M, Leuthold M, Meier-Gerschwiler P, and Weber T

Subjects

Animals, Female, Gametogenesis genetics, Gene Expression Regulation genetics, Genotype, Germ Cells physiology, Germ Layers physiology, Gonads physiology, Male, Mutation, Phenotype, Drosophila genetics, Gametogenesis physiology, Sex Determination Analysis

Abstract

We have analyzed the mechanism of sex determination in the germ line of Drosophila by manipulating three parameters: (1) the ratio of X-chromosomes to sets of autosomes (X:A); (2) the state of activity of the gene Sex-lethal (Sxl), and (3) the sex of the gonadal soma. To this end, animals with a ratio of 2X:2A and 2X:3A were sexually transformed into pseudomales by mutations at the sex-determining genes Sxl (Sex-lethal), tra (transformer), tra-2 (transformer-2), or dsx (double-sex). Animals with the karyotype 2X;3A were also transformed into pseudofemales by the constitutive mutation SxlM1. The sexual phenotype of the gonads and of the germ cells was assessed by phase-contrast microscopy. Confirming the conclusions of Steinmann-Zwicky et al. (Cell 57, 157, 1989), we found that all three parameters affect sex determination in germ cells. In contrast to the soma in which sex determination is completely cell-autonomous, sex determination in the germ line has a non-autonomous component inasmuch as the sex of the soma can influence the sexual pathway of the germ cells. Somatic induction has a clear effect on 2X;2A germ cells that carry a Sxl+ allele. These cells, which form eggs in an ovary, can enter spermatogenesis in testes. Mutations that cause partial loss of function or gain of function of Sxl thwart somatic induction and, independently of the sex of the soma, dictate spermatogenesis or oogenesis, respectively. Somatic induction has a much weaker effect on 2X;3A germ cells. This ratio is essentially a male signal for germ cells which consistently enter spermatogenesis in testes, even when they carry SxlM1. In a female soma, however, SxlM1 enables the 2X;3A germ cells to form almost normal eggs. Our results show that sex determination in the germ line is more complex than in the soma. They provide further evidence that the state of Sxl, the key gene for sex determination and dosage compensation in the soma, also determines the sex of the germ cells, and that, in the germ line, the state of activity of Sxl is regulated not only by the X:A ratio, but also by somatic inductive stimuli.

Published

1989