The evolution of imprinting in plants: beyond the seed

Plant Reproduction ◽

10.1007/s00497-021-00410-7 ◽

2021 ◽

Author(s):

Sean A. Montgomery ◽

Frédéric Berger

Keyword(s):

Gene Expression ◽

Sexual Reproduction ◽

Genomic Imprinting ◽

Flowering Plants ◽

Land Plants ◽

Imprinted Gene ◽

Selective Pressures ◽

Experimental Support ◽

Evolutionary Origins ◽

Additional Support

AbstractGenomic imprinting results in the biased expression of alleles depending on if the allele was inherited from the mother or the father. Despite the prevalence of sexual reproduction across eukaryotes, imprinting is only found in placental mammals, flowering plants, and some insects, suggesting independent evolutionary origins. Numerous hypotheses have been proposed to explain the selective pressures that favour the innovation of imprinted gene expression and each differs in their experimental support and predictions. Due to the lack of investigation of imprinting in land plants, other than angiosperms with triploid endosperm, we do not know whether imprinting occurs in species lacking endosperm and with embryos developing on maternal plants. Here, we discuss the potential for uncovering additional examples of imprinting in land plants and how these observations may provide additional support for one or more existing imprinting hypotheses.

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DNA demethylase ROS1 negatively regulates the imprinting of DOGL4 and seed dormancy in Arabidopsis thaliana

Proceedings of the National Academy of Sciences ◽

10.1073/pnas.1812847115 ◽

2018 ◽

Vol 115 (42) ◽

pp. E9962-E9970 ◽

Cited By ~ 15

Author(s):

Haifeng Zhu ◽

Wenxiang Xie ◽

Dachao Xu ◽

Daisuke Miki ◽

Kai Tang ◽

...

Keyword(s):

Gene Expression ◽

Seed Dormancy ◽

Genomic Imprinting ◽

Dna Demethylation ◽

Paternal Allele ◽

Maternal Allele ◽

Imprinted Gene ◽

Differential Gene ◽

Parent Of Origin ◽

Dna Demethylase

Genomic imprinting is a form of epigenetic regulation resulting in differential gene expression that reflects the parent of origin. In plants, imprinted gene expression predominantly occurs in the seed endosperm. Maternal-specific DNA demethylation by the DNA demethylase DME frequently underlies genomic imprinting in endosperm. Whether other more ubiquitously expressed DNA demethylases regulate imprinting is unknown. Here, we found that the DNA demethylase ROS1 regulates the imprinting of DOGL4. DOGL4 is expressed from the maternal allele in endosperm and displays preferential methylation and suppression of the paternal allele. We found that ROS1 negatively regulates imprinting by demethylating the paternal allele, preventing its hypermethylation and complete silencing. Furthermore, we found that DOGL4 negatively affects seed dormancy and response to the phytohormone abscisic acid and that ROS1 controls these processes by regulating DOGL4. Our results reveal roles for ROS1 in mitigating imprinted gene expression and regulating seed dormancy.

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Associations between imprinted gene expression in the placenta, human fetal growth and preeclampsia

Biology Letters ◽

10.1098/rsbl.2017.0643 ◽

2017 ◽

Vol 13 (11) ◽

pp. 20170643 ◽

Cited By ~ 8

Author(s):

Julian K. Christians ◽

Katherine Leavey ◽

Brian J. Cox

Keyword(s):

Gene Expression ◽

Genomic Imprinting ◽

Fetal Growth ◽

Placental Insufficiency ◽

Imprinted Genes ◽

Nutrient Allocation ◽

Imprinted Gene ◽

Expression Levels ◽

Kinship Theory ◽

Coordinated Regulation

Genomic imprinting is essential for normal placental and fetal growth. One theory to explain the evolution of imprinting is the kinship theory (KT), which predicts that genes that are paternally expressed will promote fetal growth, whereas maternally expressed genes will suppress growth. We investigated the expression of imprinted genes using microarray measurements of expression in term placentae. Correlations between birthweight and the expression levels of imprinted genes were more significant than for non-imprinted genes, but did not tend to be positive for paternally expressed genes and negative for maternally expressed genes. Imprinted genes were more dysregulated in preeclampsia (a disorder associated with placental insufficiency) than randomly selected genes, and we observed an excess of patterns of dysregulation in preeclampsia that would be expected to reduce nutrient allocation to the fetus, given the predictions of the KT. However, we found no evidence of coordinated regulation among these imprinted genes. A few imprinted genes have previously been shown to be associated with fetal growth and preeclampsia, and our results indicate that this is true for a broader set of imprinted genes.

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Sexual conflict and the alternation of haploid and diploid generations

Philosophical Transactions of the Royal Society B Biological Sciences ◽

10.1098/rstb.2005.1794 ◽

2006 ◽

Vol 361 (1466) ◽

pp. 335-343 ◽

Cited By ~ 34

Author(s):

David Haig ◽

Amity Wilczek

Keyword(s):

Mate Choice ◽

Sexual Reproduction ◽

Genomic Imprinting ◽

Segregation Distortion ◽

Asexual Reproduction ◽

Sexual Conflict ◽

Land Plants ◽

Maternal Genome ◽

Selective Forces ◽

Haploid Complement

Land plants possess a multicellular diploid stage (sporophyte) that begins development while attached to a multicellular haploid progenitor (gametophyte). Although the closest algal relatives of land plants lack a multicellular sporophyte, they do produce a zygote that grows while attached to the maternal gametophyte. The diploid offspring shares one haploid set of genes with the haploid mother that supplies it with resources and a paternal haploid complement that is not shared with the mother. Sexual conflict can arise within the diploid offspring because the offspring's maternal genome will be transmitted in its entirety to all other sexual and asexual offspring that the mother may produce, but the offspring's paternally derived genes may be absent from these other offspring. Thus, the selective forces favouring the evolution of genomic imprinting may have been present from the origin of modern land plants. In bryophytes, where gametophytes are long-lived and capable of multiple bouts of asexual and sexual reproduction, we predict strong sexual conflict over allocation to sporophytes. Female gametophytes of pteridophytes produce a single sporophyte and often lack means of asexual reproduction. Therefore, sexual conflict is predicted to be attenuated. Finally, we explore similarities among models of mate choice, offspring choice and segregation distortion.

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Molecular mechanisms of genomic imprinting and clinical implications for cancer

Expert Reviews in Molecular Medicine ◽

10.1017/s1462399410001717 ◽

2011 ◽

Vol 13 ◽

Cited By ~ 53

Author(s):

Santiago Uribe-Lewis ◽

Kathryn Woodfine ◽

Lovorka Stojic ◽

Adele Murrell

Keyword(s):

Gene Expression ◽

Genomic Imprinting ◽

Noncoding Rna ◽

Molecular Mechanisms ◽

Expression Patterns ◽

Early Event ◽

Imprinted Genes ◽

Epigenetic Changes ◽

Imprinted Gene ◽

Growth Loss

Genomic imprinting is an epigenetic marking of genes in the parental germline that ensures the stable transmission of monoallelic gene expression patterns in a parent-of-origin-specific manner. Epigenetic marking systems are thus able to regulate gene activity independently of the underlying DNA sequence. Several imprinted gene products regulate cell proliferation and fetal growth; loss of their imprinted state, which effectively alters their dosage, might promote or suppress tumourigenic processes. Conversely, global epigenetic changes that underlie tumourigenesis might affect imprinted gene expression. Here, we review imprinted genes with regard to their roles in epigenetic predisposition to cancer, and discuss acquired epigenetic changes (DNA methylation, histone modifications and chromatin conformation) either as a result of cancer or as an early event in neoplasia. We also address recent work showing the potential role of noncoding RNA in modifying chromatin and affecting imprinted gene expression, and summarise the effects of loss of imprinting in cancer with regard to the roles that imprinted genes play in regulating growth signalling cascades. Finally, we speculate on the clinical applications of epigenetic drugs in cancer.

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Molecular basis of adaptive evolution of sperm motility involved in in vivo fertilization of terrestrial animals

Impact ◽

10.21820/23987073.2020.6.73 ◽

2020 ◽

Vol 2020 (6) ◽

pp. 73-75

Author(s):

Akihiko Watanabe

Keyword(s):

Sexual Reproduction ◽

Sperm Motility ◽

Asexual Reproduction ◽

Acrosome Reaction ◽

Sperm Morphology ◽

Adaptive Potential ◽

Selective Pressures ◽

The Face ◽

Genetic Profiles

One of the unifying traits of life on this planet is reproduction, or life's ability to make copies of itself. The mode of reproduction has evolved over time, having almost certainly begun with simple asexual reproduction when the ancestral single celled organism divided into two. Since these beginnings' life has tried out numerous strategies, and perhaps one of the most important and successful has been sexual reproduction. This form of reproduction relies on the union of gametes, otherwise known as sperm and egg. Evolutionarily, sexual reproduction allows for greater adaptive potential because the genes of two unique individuals have a chance to recombine and mix in order to produce a new individual. Unlike asexual reproduction which produces genetically-identical clones of the parent individual, sex produces offspring with novel genes and combinations of genes. Therefore, in the face of new selective pressures there is a higher chance that one of these novel genetic profiles will produce an adaptation that is advantageous in the new circumstances. Dr Akihiko Watanabe is a reproductive biologist based in the Department of Biology, Faculty of Science Yamagata University in Japan, he is currently working on three research projects; a comparative study on the signalling pathways for inducing sperm motility and acrosome reaction in amphibians, the mechanism behind the adaptive modification of sperm morphology and motility, and the origin of sperm motility initiating substance (SMIS).

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Changes in genomic imprinting and gene expression associated with transformation in a model of human osteosarcoma

Experimental and Molecular Pathology ◽

10.1016/j.yexmp.2008.03.013 ◽

2008 ◽

Vol 84 (3) ◽

pp. 234-239 ◽

Cited By ~ 45

Author(s):

Yi Li ◽

Gang Meng ◽

Qiao-nan Guo

Keyword(s):

Gene Expression ◽

Genomic Imprinting ◽

Human Osteosarcoma

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Genomic Imprinting of Dopa decarboxylase in Heart and Reciprocal Allelic Expression with Neighboring Grb10

Molecular and Cellular Biology ◽

10.1128/mcb.00862-07 ◽

2007 ◽

Vol 28 (1) ◽

pp. 386-396 ◽

Cited By ~ 28

Author(s):

Trevelyan R. Menheniott ◽

Kathryn Woodfine ◽

Reiner Schulz ◽

Andrew J. Wood ◽

David Monk ◽

...

Keyword(s):

Genomic Imprinting ◽

Promoter Region ◽

Germ Line ◽

Differential Methylation ◽

Dopa Decarboxylase ◽

Imprinted Genes ◽

Chromosome 11 ◽

Imprinted Gene ◽

Line Methylation ◽

Intron 1

ABSTRACT By combining a tissue-specific microarray screen with mouse uniparental duplications, we have identified a novel imprinted gene, Dopa decarboxylase (Ddc), on chromosome 11. Ddc_exon1a is a 2-kb transcript variant that initiates from an alternative first exon in intron 1 of the canonical Ddc transcript and is paternally expressed in trabecular cardiomyocytes of the embryonic and neonatal heart. Ddc displays tight conserved linkage with the maternally expressed and methylated Grb10 gene, suggesting that these reciprocally imprinted genes may be coordinately regulated. In Dnmt3L mutant embryos that lack maternal germ line methylation imprints, we show that Ddc is overexpressed and Grb10 is silenced. Their imprinting is therefore dependent on maternal germ line methylation, but the mechanism at Ddc does not appear to involve differential methylation of the Ddc_exon1a promoter region and may instead be provided by the oocyte mark at Grb10. Our analysis of Ddc redefines the imprinted Grb10 domain on mouse proximal chromosome 11 and identifies Ddc_exon1a as the first example of a heart-specific imprinted gene.

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Genomic imprinting and its role in ethiology of human hereditary diseases

Bulletin of Siberian Medicine ◽

10.20538/1682-0363-2004-3-8-17 ◽

2004 ◽

Vol 3 (3) ◽

pp. 8-17

Author(s):

S. A. Nazarenko

Keyword(s):

Gene Expression ◽

Genomic Imprinting ◽

Special Class ◽

Growth And Development ◽

Epigenetic Inheritance ◽

Hereditary Diseases ◽

Parental Origin ◽

Imprinted Genes ◽

Methylation Of Dna ◽

Differential Gene

Genomic imprinting is a form of non-Mendelian epigenetic inheritance that is defined by differential gene expression depending on its parental origin — maternal or paternal. It is known about 60 imprinted genes many of which effect significantly on the fetus growth and development. Methylation of DNA cytosine bases that defines the interaction of DNA and proteins identifying the modified bases and controls the gene expression through chromatin compacting-decompacting mechanism, is a main epigenetic genom modifier. Disturbances in monoallelic gene expression lead to the development of a special class of human hereditary diseases — genomic imprinting diseases.

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Optimal transcriptional regulation of cellular responses to sudden environmental shifts

10.1101/2020.09.14.297317 ◽

2020 ◽

Author(s):

Daniel Schultz ◽

Lev S. Tsimring

Keyword(s):

Gene Expression ◽

Gene Regulation ◽

Cell Response ◽

Cellular Responses ◽

Natural Systems ◽

Selective Pressures ◽

Regulatory Strategies ◽

Regulatory Strategy ◽

A Cell ◽

The Many

ABSTRACTCellular responses to sudden changes in their environment require prompt expression of the correct levels of the appropriate enzymes. These enzymes are typically regulated by transcription factors that sense the presence of inducers and control gene expression for the duration of the response. The specific choice of regulatory strategy depends on the characteristics of each cell response, with the pattern of gene expression dictated by parameters such as the affinity of the transcription factor to its binding sites and the strength of the promoters it regulates. Although much is known about how gene regulation determines the dynamics of cell responses, we still lack a framework to understand how the many different regulatory strategies evolved in natural systems relate to the constraints imposed by the selective pressures acting in each particular case. Here, we analyze a dynamical model of a cell response where expression of a transcriptionally repressed enzyme is induced by a sudden exposure to its substrate. We identify strategies of gene regulation that optimize the response for different types of selective pressures, which we define as a set of costs associated with substrate, enzyme and repressor intracellular concentrations during the response. We find that regulated responses happen within a defined region in the parameter space. While responses to costly (toxic) substrates favor the usage of strongly self-regulated repressors, responses where expression of enzyme is more costly than its substrate favor the usage of constitutively expressed repressors. There is only a very narrow range of selective pressures that would favor weakly self-regulated repressors. This framework can be used to infer which costs and benefits are most critical in the evolution of natural examples of cellular responses, and to predict how a response can optimize its regulation when transported to a new environment with different demands.

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Identification and evaluation of the novel genes for transcript normalization during female gametophyte development in sugarcane

PeerJ ◽

10.7717/peerj.12298 ◽

2021 ◽

Vol 9 ◽

pp. e12298

Author(s):

Maokai Yan ◽

Xingyue Jin ◽

Yanhui Liu ◽

Huihuang Chen ◽

Tao Ye ◽

...

Keyword(s):

Gene Expression ◽

Sexual Reproduction ◽

Reference Genes ◽

Female Gametophyte ◽

Developmental Stages ◽

Reproductive Organs ◽

The Novel ◽

Biofuel Feedstock ◽

Gametophyte Development ◽

Female Gametophyte Development

Background Sugarcane (Saccharum spontaneum L.), the major sugar and biofuel feedstock crop, is cultivated mainly by vegetative propagation worldwide due to the infertility of female reproductive organs resulting in the reduction of quality and output of sugar. Deciphering the gene expression profile during ovule development will improve our understanding of the complications underlying sexual reproduction in sugarcane. Optimal reference genes are essential for elucidating the expression pattern of a given gene by quantitative real-time PCR (qRT-PCR). Method In this study, based on transcriptome data obtained from sugarcane ovule, eighteen candidate reference genes were identified, cloned, and their expression levels were evaluated across five developmental stages ovule (AC, MMC, Meiosis, Mitosis, and Mature). Results Our results indicated that FAB2 and MOR1 were the most stably expressed genes during sugarcane female gametophyte development. Moreover, two genes, cell cycle-related genes REC8 and CDK, were selected, and their feasibility was validated. This study provides important insights into the female gametophyte development of sugarcane and reports novel reference genes for gene expression research on sugarcane sexual reproduction.

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