Abstract

Synthesis of mRNAs in eukaryotic cells is a highly complex process, including, in addition to transcription itself, splicing and 3' end formation of mRNA precursors. My laboratory has studied the mechanisms and regulation of these processes for many years, and also shown how they are integrated with other cellular events such as DNA damage, and also how they function in differentiation and disease. This proposal combines our studies in these areas, and can be divided into the following three broad areas: 1) mRNA processing and disease. Studies examining the roles of several proteins implicated in RNA metabolism in cancer and neurodegenerative disease will be pursued. The role of RNA processing factors in cancer reflects two distinct mechanisms, overexpression of splicing regulatory proteins and mutation of genes encoding various splicing factors. With respect to the former, ongoing experiments stemming from studies elucidating the mechanism underlying deregulation of PKM alternative splicing (AS) in cancer will be pursued. Important questions include the generality of the mechanism, the importance of splicing factor overexpression to tumor development, and the identity of the critical regulated splicing events. Splicing factor mutations can cause MDS and certain leukemias, and ongoing studies are aimed at elucidating mechanisms by which mutations affect the function of several, e.g., SRSF2 and SF3B1, and how such defects lead to disease. With respect to neurodegenerative disease, work centers on how ALS-causing mutations in the RNA/DNA-binding protein TLS/FUS disrupt protein function; how the hexanucleotide repeat expansions in C9ORF72 form G-quadruplex structures that sequester hnRNP H, disrupt AS, and contribute to ALS; and how disease-causing mutations in the RNA/DNA helicase Senataxin affect its role in prevention of transcription-induced DNA damage. 2) mRNA processing and differentiation. Studies examining how changes in AS and alternative polyadenylation (APA) contribute to human embryonic stem cell pluripotency and differentiation will be pursued. How AS affects the function of the transcriptional regulator TCF3 and how this contributes to differentiation will be determined. The mechanism of the AS event, including how the splicing regulators are themselves regulated, will be investigated. Our unexpected finding that AS of transcripts encoding two PA factors, both subunits of CPSF and implicated in AAUAAA recognition, is altered during differentiation will be pursued. How the distinct isoforms affect APA, and differentiation, will be determined, as will the mechanism by which they influence PA site choice. 3) RNA processing and transcription. Experiments examining the function of the RNA pol II CTD, a unique domain consisting of 26-52 heptad repeats (consensus YSPTSPS), will be continued. For example, recent experiments establishing a role for P-Tyr1 residues in facilitating turnover of certain lncRNAs, and suggesting that this involves interaction with the RNA helicase Mtr4 and the PA machinery, will be pursued. These and other experiments will advance our understanding of the CTD code that links transcription and RNA processing.

Public Health Relevance

The experiments described in this proposal are designed to increase our understanding of the mechanisms and regulation of essential mRNA processing reactions, and how they are coupled to and affect other nuclear processes such as transcription. Recent studies have revealed that changes in these processes occur and have important consequences during development and disease, and our studies will provide considerable mechanistic insight into these important processes.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Unknown (R35)
Project #
5R35GM118136-04
Application #
9707595
Study Section
Special Emphasis Panel (ZGM1)
Program Officer
Bender, Michael T
Project Start
2016-06-08
Project End
2021-05-31
Budget Start
2019-06-01
Budget End
2020-05-31
Support Year
4
Fiscal Year
2019
Total Cost
Indirect Cost

  Institution

Name
Columbia University (N.Y.)
Department
Biology
Type
Graduate Schools
DUNS #
049179401
City
New York
State
NY
Country
United States
Zip Code
10027

  Publications

Conlon, Erin G; Fagegaltier, Delphine; Agius, Phaedra et al. (2018) Unexpected similarities between C9ORF72 and sporadic forms of ALS/FTD suggest a common disease mechanism. Elife 7:
Ogami, Koichi; Chen, Yaqiong; Manley, James L (2018) RNA surveillance by the nuclear RNA exosome: mechanisms and significance. Noncoding RNA 4:
Sun, Yadong; Zhang, Yixiao; Hamilton, Keith et al. (2018) Molecular basis for the recognition of the human AAUAAA polyadenylation signal. Proc Natl Acad Sci U S A 115:E1419-E1428
Yurko, Nathan M; Manley, James L (2018) The RNA polymerase II CTD ""orphan"" residues: Emerging insights into the functions of Tyr-1, Thr-4, and Ser-7. Transcription 9:30-40
Yamazaki, Takashi; Liu, Lizhi; Lazarev, Denis et al. (2018) TCF3 alternative splicing controlled by hnRNP H/F regulates E-cadherin expression and hESC pluripotency. Genes Dev 32:1161-1174
Richard, Patricia; Manley, James L (2017) R Loops and Links to Human Disease. J Mol Biol 429:3168-3180
Ogami, Koichi; Manley, James L (2017) Mtr4/ZFC3H1 protects polysomes through nuclear RNA surveillance. Cell Cycle 16:1999-2000
Liu, Xiaochuan; Hoque, Mainul; Larochelle, Marc et al. (2017) Comparative analysis of alternative polyadenylation in S. cerevisiae and S. pombe. Genome Res 27:1685-1695
Yurko, Nathan; Liu, Xiaochuan; Yamazaki, Takashi et al. (2017) MPK1/SLT2 Links Multiple Stress Responses with Gene Expression in Budding Yeast by Phosphorylating Tyr1 of the RNAP II CTD. Mol Cell 68:913-925.e3
Conlon, Erin G; Manley, James L (2017) RNA-binding proteins in neurodegeneration: mechanisms in aggregate. Genes Dev 31:1509-1528

Showing the most recent 10 out of 16 publications