POS-1 promotes endo-mesoderm development by inhibiting the cytoplasmic polyadenylation of neg-1 mRNA

Ahmed Elewa; Masaki Shirayama; Ebru Kaymak; Paul Francis Harrison; David R Powell; Zhuo Du; Christopher D Chute; Hannah Woolf; Dongni Yi; Takao Ishidate; Jagan Srinivasan; Zhirong Bao; Traude H Beilharz; Sean P Ryder; Craig C Mello

doi:10.1016/j.devcel.2015.05.024

POS-1 promotes endo-mesoderm development by inhibiting the cytoplasmic polyadenylation of neg-1 mRNA

Ahmed Elewa
, Masaki Shirayama
, Ebru Kaymak
, Paul Francis Harrison
, David R Powell
, Zhuo Du
, Christopher D Chute
, Hannah Woolf
, Dongni Yi
, Takao Ishidate
, Jagan Srinivasan
, Zhirong Bao
, Traude H Beilharz
, Sean P Ryder
, Craig C Mello

Research output: Contribution to journal › Article › Research › peer-review

18 Citations (Scopus)

Abstract

The regulation of mRNA translation is of fundamental importance in biological mechanisms ranging from embryonic axis specification to the formation of long-term memory. POS-1 is one of several CCCH zinc-finger RNA-binding proteins that regulate cell fate specification during C. elegans embryogenesis. Paradoxically, pos-1 mutants exhibit striking defects in endo-mesoderm development but have wild-type distributions of SKN-1, a key determinant of endo-mesoderm fates. RNAi screens for pos-1 suppressors identified genes encoding the cytoplasmic poly(A)-polymerase homolog GLD-2, the Bicaudal-C homolog GLD-3, and the protein NEG-1. We show that NEG-1 localizes in anterior nuclei, where it negatively regulates endo-mesoderm fates. In posterior cells, POS-1 binds the neg-1 3 UTR to oppose GLD-2 and GLD-3 activities that promote NEG-1 expression and cytoplasmic lengthening of the neg-1 mRNA poly(A) tail. Our findings uncover an intricate series of post-transcriptional regulatory interactions that, together, achieve precise spatial expression of endo-mesoderm fates in C. elegans embryos.

Original language	English
Pages (from-to)	108 - 118
Number of pages	11
Journal	Developmental Cell
Volume	34
Issue number	1
DOIs	https://doi.org/10.1016/j.devcel.2015.05.024
Publication status	Published - 2015

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Elewa, A., Shirayama, M., Kaymak, E., Harrison, P. F., Powell, D. R., Du, Z., Chute, C. D., Woolf, H., Yi, D., Ishidate, T., Srinivasan, J., Bao, Z., Beilharz, T. H., Ryder, S. P., & Mello, C. C. (2015). POS-1 promotes endo-mesoderm development by inhibiting the cytoplasmic polyadenylation of neg-1 mRNA. Developmental Cell, 34(1), 108 - 118. https://doi.org/10.1016/j.devcel.2015.05.024

@article{4f60ee0575714043bdc50bec673d83c2,

title = "POS-1 promotes endo-mesoderm development by inhibiting the cytoplasmic polyadenylation of neg-1 mRNA",

abstract = "The regulation of mRNA translation is of fundamental importance in biological mechanisms ranging from embryonic axis specification to the formation of long-term memory. POS-1 is one of several CCCH zinc-finger RNA-binding proteins that regulate cell fate specification during C. elegans embryogenesis. Paradoxically, pos-1 mutants exhibit striking defects in endo-mesoderm development but have wild-type distributions of SKN-1, a key determinant of endo-mesoderm fates. RNAi screens for pos-1 suppressors identified genes encoding the cytoplasmic poly(A)-polymerase homolog GLD-2, the Bicaudal-C homolog GLD-3, and the protein NEG-1. We show that NEG-1 localizes in anterior nuclei, where it negatively regulates endo-mesoderm fates. In posterior cells, POS-1 binds the neg-1 3 UTR to oppose GLD-2 and GLD-3 activities that promote NEG-1 expression and cytoplasmic lengthening of the neg-1 mRNA poly(A) tail. Our findings uncover an intricate series of post-transcriptional regulatory interactions that, together, achieve precise spatial expression of endo-mesoderm fates in C. elegans embryos.",

author = "Ahmed Elewa and Masaki Shirayama and Ebru Kaymak and Harrison, \{Paul Francis\} and Powell, \{David R\} and Zhuo Du and Chute, \{Christopher D\} and Hannah Woolf and Dongni Yi and Takao Ishidate and Jagan Srinivasan and Zhirong Bao and Beilharz, \{Traude H\} and Ryder, \{Sean P\} and Mello, \{Craig C\}",

year = "2015",

doi = "10.1016/j.devcel.2015.05.024",

language = "English",

volume = "34",

pages = "108 -- 118",

journal = "Developmental Cell",

issn = "1534-5807",

publisher = "Cell Press",

number = "1",

}

Elewa, A, Shirayama, M, Kaymak, E, Harrison, PF , Powell, DR, Du, Z, Chute, CD, Woolf, H, Yi, D, Ishidate, T, Srinivasan, J, Bao, Z, Beilharz, TH, Ryder, SP & Mello, CC 2015, 'POS-1 promotes endo-mesoderm development by inhibiting the cytoplasmic polyadenylation of neg-1 mRNA', Developmental Cell, vol. 34, no. 1, pp. 108 - 118. https://doi.org/10.1016/j.devcel.2015.05.024

TY - JOUR

T1 - POS-1 promotes endo-mesoderm development by inhibiting the cytoplasmic polyadenylation of neg-1 mRNA

AU - Elewa, Ahmed

AU - Shirayama, Masaki

AU - Kaymak, Ebru

AU - Harrison, Paul Francis

AU - Powell, David R

AU - Du, Zhuo

AU - Chute, Christopher D

AU - Woolf, Hannah

AU - Yi, Dongni

AU - Ishidate, Takao

AU - Srinivasan, Jagan

AU - Bao, Zhirong

AU - Beilharz, Traude H

AU - Ryder, Sean P

AU - Mello, Craig C

PY - 2015

Y1 - 2015

N2 - The regulation of mRNA translation is of fundamental importance in biological mechanisms ranging from embryonic axis specification to the formation of long-term memory. POS-1 is one of several CCCH zinc-finger RNA-binding proteins that regulate cell fate specification during C. elegans embryogenesis. Paradoxically, pos-1 mutants exhibit striking defects in endo-mesoderm development but have wild-type distributions of SKN-1, a key determinant of endo-mesoderm fates. RNAi screens for pos-1 suppressors identified genes encoding the cytoplasmic poly(A)-polymerase homolog GLD-2, the Bicaudal-C homolog GLD-3, and the protein NEG-1. We show that NEG-1 localizes in anterior nuclei, where it negatively regulates endo-mesoderm fates. In posterior cells, POS-1 binds the neg-1 3 UTR to oppose GLD-2 and GLD-3 activities that promote NEG-1 expression and cytoplasmic lengthening of the neg-1 mRNA poly(A) tail. Our findings uncover an intricate series of post-transcriptional regulatory interactions that, together, achieve precise spatial expression of endo-mesoderm fates in C. elegans embryos.

AB - The regulation of mRNA translation is of fundamental importance in biological mechanisms ranging from embryonic axis specification to the formation of long-term memory. POS-1 is one of several CCCH zinc-finger RNA-binding proteins that regulate cell fate specification during C. elegans embryogenesis. Paradoxically, pos-1 mutants exhibit striking defects in endo-mesoderm development but have wild-type distributions of SKN-1, a key determinant of endo-mesoderm fates. RNAi screens for pos-1 suppressors identified genes encoding the cytoplasmic poly(A)-polymerase homolog GLD-2, the Bicaudal-C homolog GLD-3, and the protein NEG-1. We show that NEG-1 localizes in anterior nuclei, where it negatively regulates endo-mesoderm fates. In posterior cells, POS-1 binds the neg-1 3 UTR to oppose GLD-2 and GLD-3 activities that promote NEG-1 expression and cytoplasmic lengthening of the neg-1 mRNA poly(A) tail. Our findings uncover an intricate series of post-transcriptional regulatory interactions that, together, achieve precise spatial expression of endo-mesoderm fates in C. elegans embryos.

UR - http://www.sciencedirect.com/science/article/pii/S1534580715003603

U2 - 10.1016/j.devcel.2015.05.024

DO - 10.1016/j.devcel.2015.05.024

M3 - Article

SN - 1534-5807

VL - 34

SP - 108

EP - 118

JO - Developmental Cell

JF - Developmental Cell

IS - 1

ER -

POS-1 promotes endo-mesoderm development by inhibiting the cytoplasmic polyadenylation of neg-1 mRNA

Abstract

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