A specialized processing body that is temporally and asymmetrically regulated during the cell cycle in <i>Saccharomyces cerevisiae </i>

Gill, Tina; Aulds, Jason; Schmitt, Michael N.

doi:10.1083/jcb.200512025

Cited by 54 publications

(51 citation statements)

References 31 publications

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“…First, RNase MRP was shown to cleave the 59 UTR of the CLB2 (Cyclin B2) mRNA (Gill et al 2004). (RNase MRP, generally a nucleolar enzyme, was shown to transiently accumulate in a discrete cytoplasmic spot where it co-localizes with the CLB2 mRNA [Gill et al 2006]). In vitro cleavage assays performed on the 59 UTR of CLB2 mRNA confirm previously reported (Gill et al 2004) RNase MRP cleavage at sites that are consistent with the identified consensus (Supplemental Fig.…”

Section: Cleavage Of Known Rnase Mrp Substratesmentioning

confidence: 99%

Substrate recognition by ribonucleoprotein ribonuclease MRP

Esakova

Perederina²,

Quan

et al. 2010

RNA

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The ribonucleoprotein complex ribonuclease (RNase) MRP is a site-specific endoribonuclease essential for the survival of the eukaryotic cell. RNase MRP closely resembles RNase P (a universal endoribonuclease responsible for the maturation of the 59 ends of tRNA) but recognizes distinct substrates including pre-rRNA and mRNA. Here we report the results of an in vitro selection of Saccharomyces cerevisiae RNase MRP substrates starting from a pool of random sequences. The results indicate that RNase MRP cleaves single-stranded RNA and is sensitive to sequences in the immediate vicinity of the cleavage site requiring a cytosine at the position +4 relative to the cleavage site. Structural implications of the differences in substrate recognition by RNases P and MRP are discussed.

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Section: Cleavage Of Known Rnase Mrp Substratesmentioning

confidence: 99%

Substrate recognition by ribonucleoprotein ribonuclease MRP

Esakova

Perederina²,

Quan

et al. 2010

RNA

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“…RNase MRP is also implicated in messenger RNA (mRNA) degradation and cell cycle progression at the end of mitosis. It processes the 5′-UTR of the cyclin B2 (CLB2) mRNA and regulates the completion of mitosis [8,9].…”

Section: The Function Of Rnase Mrpmentioning

confidence: 99%

RNase MRP RNA and human genetic diseases

Martin

2006

Cell Res

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“…Yeast RNase MRP is also involved in the regulation of the cell cycle by cleaving the 59 UTR of cyclin B2 mRNA (Cai et al 1999(Cai et al , 2002Gill et al 2006). Defects in RNase MRP function result in a variety of recessive pleiotropic diseases typically characterized by dwarfism (Ridanpaa et al 2001;Thiel et al 2005;Martin and Li 2007;Glazov et al 2011); the mechanisms responsible for the development of these diseases are not known.…”

Section: Introductionmentioning

confidence: 99%

“…RNase MRP is essential for the viability of eukaryotes (Schmitt and Clayton 1992;Schneider et al 2010). Though it was originally identified as a mitochondrial enzyme, the vast majority of RNase MRP is found in the nucleolus and, transiently, in the cytoplasm (Chang and Clayton 1987a;Karwan et al 1991;Gill et al 2006, and references therein). Mitochondrial RNase MRP has a distinct protein composition which is yet to be fully characterized (Lu et al 2010) and will not be discussed in this study.…”

Section: Introductionmentioning

confidence: 99%

Interactions of a Pop5/Rpp1 heterodimer with the catalytic domain of RNase MRP

Perederina

Khanova

Quan

et al. 2011

RNA

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Ribonuclease (RNase) MRP is a multicomponent ribonucleoprotein complex closely related to RNase P. RNase MRP and eukaryotic RNase P share most of their protein components, as well as multiple features of their catalytic RNA moieties, but have distinct substrate specificities. While RNase P is practically universally found in all three domains of life, RNase MRP is essential in eukaryotes. The structural organizations of eukaryotic RNase P and RNase MRP are poorly understood. Here, we show that Pop5 and Rpp1, protein components found in both RNase P and RNase MRP, form a heterodimer that binds directly to the conserved area of the putative catalytic domain of RNase MRP RNA. The Pop5/Rpp1 binding site corresponds to the protein binding site in bacterial RNase P RNA. Structural and evolutionary roles of the Pop5/Rpp1 heterodimer in RNases P and MRP are discussed.

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A specialized processing body that is temporally and asymmetrically regulated during the cell cycle in Saccharomyces cerevisiae

Cited by 54 publications

References 31 publications

Substrate recognition by ribonucleoprotein ribonuclease MRP

Substrate recognition by ribonucleoprotein ribonuclease MRP

RNase MRP RNA and human genetic diseases

Interactions of a Pop5/Rpp1 heterodimer with the catalytic domain of RNase MRP

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