Abstract

We investigate the processes involved in communication along and between homologous chromosomes during meiosis, the specialized cell cycle that underlies gamete formation for sexual reproduction. Importantly, defects in meiosis underlie human infertility and several genetic diseases, notably Downs Syndrome. Proposed research addresses three broad areas. I. We investigate how chromosomal events can occur in an evenly-spaced pattern without direct genetic specification of position. In particular, such patterning is exhibited by meiotic crossovers, manifested originally in the genetic phenomenon of crossover interference and subsequently by cytological analyses of crossover-correlated structures along elongated mid-prophase chromosomes and later as points of connections between homologs along partially compacted diplotene chromosomes (chiasmata). We are using imaging, proteomics, genetics, mathematical simulations, and laser nanosurgery to address three questions: (A) What molecules are involved in interference? (B) What are the biological implications of this patterning? (C) Does communication occur by redistribution of mechanical stress, as we have proposed? II. We investigate homologous chromosome pairing, a central universal feature of the meiotic program, again by three entry points. (A) We have developed a uniquely powerful system for 3D tracking of homologously-pairing FROS foci in living meiotic yeast cells, with images collected densely over the entire time period of meiosis. This system is poised to address recombination-dependent and -independent pairing and the nature and roles of motion during the pairing period. (B) Meiotic homolog pairing involves both avoidance and active elimination of entanglements (interlocks). By tracking chromosome paths in Sordaria, we can now answer two key questions. (i) What is the mechanism of interlock resolution (by TopoII or by telomere-led movement)? (ii) Does the classical bouquet stage mediate initial homolog contact for pairing or is it involved primarily in ensuring regular topological relationships? (C) Our evidence suggests that repeat-induced point mutation (RIP) in Neurospora crassa involves recombination-independent DNA/DNA pairing. As a second approach to DSB-independent pairing, we are searching for functions required for RIP. III. Meiotic recombination occurs in close physical and functional interaction with chromosome structural axes and, once it forms between axes, the synaptonemal complex (SC). In Sordaria, we will extend recent findings which: (A) begin to elucidate a molecular pathway of events at the critical mid-prophase transition when SC is installed; (B) suggest a new idea for how chromatid axes become exchanged at sites of DNA crossovers; and reveal that breast cancer-related BRCA2 has diverse roles for chromosomes beyond those attributable to its canonical role as a Rad51 mediator. Finally, to open an entirely new window onto the meiotic process, we will develop a system for identification and analysis of Sordaria meiotic non-coding RNAs.

Public Health Relevance

Meiosis is the specialized cellular program that yields gametes for sexual reproduction. Interactions between homologous chromosomes lie at the heart of the meiotic program and our research addresses three aspects of this inter-homolog interaction program. Certain defects in this program result in chromosome mis-segregation, which, in turn, accounts for many important genetic diseases. Other defects result in sterility. Advances in fundamental understanding of meiotic inter-homolog interactions will ultimately have implications for diagnosis and, hopefully treatment of diverse reproductive defects.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM044794-28
Application #
9321140
Study Section
Molecular Genetics A Study Section (MGA)
Program Officer
Reddy, Michael K
Project Start
1990-07-01
Project End
2019-06-30
Budget Start
2017-07-01
Budget End
2018-06-30
Support Year
28
Fiscal Year
2017
Total Cost
Indirect Cost

  Institution

Name
Harvard University
Department
Microbiology/Immun/Virology
Type
Schools of Arts and Sciences
DUNS #
082359691
City
Cambridge
State
MA
Country
United States
Zip Code
02138

  Publications

Gutu, Andrian; Chang, Frederick; O'Shea, Erin K (2018) Dynamical localization of a thylakoid membrane binding protein is required for acquisition of photosynthetic competency. Mol Microbiol 108:16-31
Mazur, Alexey K; Gladyshev, Eugene (2018) Partition of Repeat-Induced Point Mutations Reveals Structural Aspects of Homologous DNA-DNA Pairing. Biophys J 115:605-615
White, Martin A; Wang, Shunxin; Zhang, Liangran et al. (2017) Quantitative Modeling and Automated Analysis of Meiotic Recombination. Methods Mol Biol 1471:305-323
Manhart, Carol M; Ni, Xiaodan; White, Martin A et al. (2017) The mismatch repair and meiotic recombination endonuclease Mlh1-Mlh3 is activated by polymer formation and can cleave DNA substrates in trans. PLoS Biol 15:e2001164
Gladyshev, Eugene (2017) Repeat-Induced Point Mutation and Other Genome Defense Mechanisms in Fungi. Microbiol Spectr 5:
Wang, Shunxin; Kleckner, Nancy; Zhang, Liangran (2017) Crossover maturation inefficiency and aneuploidy in human female meiosis. Cell Cycle 16:1017-1019
Gladyshev, Eugene; Kleckner, Nancy (2017) Recombination-independent recognition of DNA homology for repeat-induced point mutation. Curr Genet 63:389-400
Gladyshev, Eugene; Kleckner, Nancy (2017) DNA sequence homology induces cytosine-to-thymine mutation by a heterochromatin-related pathway in Neurospora. Nat Genet 49:887-894
Tessé, Sophie; Bourbon, Henri-Marc; Debuchy, Robert et al. (2017) Asy2/Mer2: an evolutionarily conserved mediator of meiotic recombination, pairing, and global chromosome compaction. Genes Dev 31:1880-1893
Wang, Shunxin; Hassold, Terry; Hunt, Patricia et al. (2017) Inefficient Crossover Maturation Underlies Elevated Aneuploidy in Human Female Meiosis. Cell 168:977-989.e17

Showing the most recent 10 out of 62 publications