Abstract

Gene regulation, a fundamental process in biology, is typically investigated at the level of transcription, yet there is a growing recognition of consequential post-transcriptional control of gene expression. In animals, microRNAs (miRNAs) and other small RNAs direct much of post-transcriptional regulation. MicroRNAs are regulatory RNAs that repress gene expression by interacting with messenger RNAs (mRNAs). In humans, miRNAs contribute to most biological pathways, and mutations perturbing miRNAs are implicated in disease. The unifying theme of all small RNA pathways is the silencing complex, which contains a small RNA and an Argonaute protein, the core proteins ofthe silencing complex. We have recently discovered two novel roles for an individual Argonaute protein, AG04, in male gametogenesis in mice. Ago4 is required for both the correct timing of entry into meiosis, a specialized form of cell division in the germline, and, for silencing ofthe sex chromosomes in meiosis, which is essential to the male germline. These are the first specific biological functions attributed to Ago4. Moreover, our data suggests that Ago3 shares some of these Ago4 functions. Because AGO proteins always function with small RNAs, our data directly implicate small RNAs in the regulation of meiotic entry and meiotic silencing. Our major goals for this proposal are to identify the small RNAs that participate in meiotic entry and meiotic silencing, and, to define their regulatory targets.
Our first aim i s to use high-throughput sequencing to identify the small RNAs and mRNAs expressed at different times of germline development in mice. To gain insights into gene regulation in the germline, we will also perform sequencing of mouse strains deficient in Ago3, Ago4, or both. In our second aim, we will use the sequencing data from aim I, together with computational approaches, to determine the mRNA targets of germline small RNAs. In our final aim, we will explore the biological significance of specific regulatory events in germline function and development using transgenic mice. Because meiotic entry and meiotic silencing are fundamental processes in germline biology, our studies will contribute to a better understanding of human reproductive biology and health.

Public Health Relevance

Small RNAs contribute to the regulation of most mammalian genes, thereby playing critical roles in human development;moreover, mutations that perturb small RNA function contribute to many human diseases. Argonaute proteins are pivotal to the function of all small RNAs, and together with our collaborators, we have recently discovered important roles for one argonaute, AG04, in the normal functioning ofthe male germline in mammals.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Specialized Center (P50)
Project #
1P50HD076210-01A1
Application #
8705107
Study Section
Special Emphasis Panel (ZHD1)
Project Start
Project End
Budget Start
2014-04-14
Budget End
2015-03-31
Support Year
1
Fiscal Year
2014
Total Cost
Indirect Cost

  Institution

Name
Cornell University
Department
Type
DUNS #
City
Ithaca
State
NY
Country
United States
Zip Code
14850

  Publications

Sones, Jennifer L; Merriam, Audrey A; Seffens, Angelina et al. (2018) Angiogenic factor imbalance precedes complement deposition in placentae of the BPH/5 model of preeclampsia. FASEB J 32:2574-2586
Singh, D; Paduch, D A; Schlegel, P N et al. (2017) The production of glial cell line-derived neurotrophic factor by human sertoli cells is substantially reduced in sertoli cell-only testes. Hum Reprod 32:1108-1117
Hilz, Stephanie; Fogarty, Elizabeth A; Modzelewski, Andrew J et al. (2017) Transcriptome profiling of the developing male germ line identifies the miR-29 family as a global regulator during meiosis. RNA Biol 14:219-235
Gray, Stephen; Cohen, Paula E (2016) Control of Meiotic Crossovers: From Double-Strand Break Formation to Designation. Annu Rev Genet 50:175-210
Wang, Jocelyn; Wissink, Erin M; Watson, Neva B et al. (2016) Fetal and adult progenitors give rise to unique populations of CD8+ T cells. Blood 128:3073-3082
Hilz, Stephanie; Modzelewski, Andrew J; Cohen, Paula E et al. (2016) The roles of microRNAs and siRNAs in mammalian spermatogenesis. Development 143:3061-73
Geissler, Rene; Simkin, Alfred; Floss, Doreen et al. (2016) A widespread sequence-specific mRNA decay pathway mediated by hnRNPs A1 and A2/B1. Genes Dev 30:1070-85
Flesken-Nikitin, Andrea; Harlan, Blaine A; Nikitin, Alexander Yu (2016) Transplantation Into the Mouse Ovarian Fat Pad. J Vis Exp :
Wissink, Erin M; Smith, Norah L; Spektor, Roman et al. (2015) MicroRNAs and Their Targets Are Differentially Regulated in Adult and Neonatal Mouse CD8+ T Cells. Genetics 201:1017-30
Modzelewski, Andrew J; Hilz, Stephanie; Crate, Elizabeth A et al. (2015) Dgcr8 and Dicer are essential for sex chromosome integrity during meiosis in males. J Cell Sci 128:2314-27

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