Telomerase RNA TLC1 Shuttling to the Cytoplasm Requires mRNA Export Factors and Is Important for Telomere Maintenance

Wu, Haijia; Becker, Daniel M.; Krebber, Heike

doi:10.1016/j.celrep.2014.08.021

Cited by 35 publications

(78 citation statements)

References 13 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…To challenge the current view that snRNA shuttling evolved only in higher eukaryotes, we systematically explored snRNA shuttling in S. cerevisiae. Due to the fact that Pol II transcripts such as mRNAs and the non-coding telomerase-RNA TLC1 require Mex67-Mtr2 and Xpo1/Crm1 for their nuclear export (Tutucci and Stutz, 2011;Wu et al, 2014), we investigated whether the shuttling of snRNAs would also be dependent on these factors. First, we analyzed potential export defects by fluorescence in situ hybridization (FISH) experiments in mutant forms of Xpo1, Mex67, and its interacting partners Dbp5/Rat8 and Nup159/ Rat7 (Tieg and Krebber, 2013).…”

Section: Results Snrnas Are Exported Into the Cytoplasm Via Xpo1 And mentioning

confidence: 99%

“…In human cells, CBC binds to PHAX (phosphorylated adaptor RNA export) that in turn recruits the RanGTPase driven exportin CRM1 (chromosome maintenance 1) for nuclear export (Kö hler and Hurt, 2007;Matera and Wang, 2014). In yeast, Pol II transcripts such as mRNAs and the non-coding telomerase-RNA TLC1 use Mex67-Mtr2 (TAP-p15 in human) and Xpo1/Crm1 for their nuclear export (Tutucci and Stutz, 2011;Wu et al, 2014). Interestingly, the current literature suggests that snRNAs do not shuttle in yeast (Olson and Siliciano, 2003;Murphy et al, 2004), although they undergo similar maturation steps as in human cells (Will and L€ uhrmann, 2001;Matera and Wang, 2014;Sloan et al, 2016;Vasianovich and Wellinger, 2017).…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Nuclear Pre-snRNA Export Is an Essential Quality Assurance Mechanism for Functional Spliceosomes

et al. 2019

Self Cite

View full text Add to dashboard Cite

show abstract

Section: Results Snrnas Are Exported Into the Cytoplasm Via Xpo1 And mentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Nuclear Pre-snRNA Export Is an Essential Quality Assurance Mechanism for Functional Spliceosomes

et al. 2019

Self Cite

View full text Add to dashboard Cite

show abstract

“…The biogenesis pathway of the RNA Pol II transcribed TLC1 RNA somewhat parallels that of pre-snRNAs, but in contrast, nuclear export of TLC1 involves two nuclear transport systems: Crm1 together with the Ran GTPase as well as the Mex67-Mtr2 heterodimer [199,200]. It is not yet know how Crm1 associates with TLC1, but it is likely that an unidentified export adaptor mediates this interaction.…”

Section: Accepted Manuscriptmentioning

confidence: 91%

“…It is not yet know how Crm1 associates with TLC1, but it is likely that an unidentified export adaptor mediates this interaction. Mutations in Mex67 cause nuclear accumulation of export-competent TLC1 RNAs but it appears that the concerted action of both Crm1 and Mex67-Mtr2 is necessary for efficient biogenesis of telomerase as telomere shortening is only observed in double mutants [200]. Once in the cytoplasm, the export machinery is released and the TLC1 RNA assembles with the reverse transcriptase Est2…”

Section: Accepted Manuscriptmentioning

confidence: 98%

Nucleocytoplasmic Transport of RNAs and RNA–Protein Complexes

Sloan

Gleizes

Bohnsack

2016

Journal of Molecular Biology

View full text Add to dashboard Cite

“…Telomerase RNA, as a template for nucleotide addition, is essential for the telomerase enzyme . To be fully functional, telomerase RNA has to be shuttled into the cytoplasm to form a complex with other associated proteins (TERT) . If telomerase RNA is blocked, the enzyme is inactivated.…”

Section: Introductionmentioning

confidence: 99%

Efficient Cytoplasmic Delivery of Antisense Probes Assisted by Cyclized‐Peptide‐Mediated Photoinduced Endosomal Escape

2019

View full text Add to dashboard Cite

Intracellular delivery and endosomal release of antisense oligonucleotides remain a significant challenge in the development of gene‐targeted therapeutics. Previously, noncovalently cyclized TAT peptide (Cyc‐TAT), in which the final ring‐closing step is accomplished by hybridization of two short complementary γPNA segments, has been proven more efficient than its linear analogues at entering cells. As Cyc‐TAT also readily accommodates a binding site, that is, an overhanging γPNA sequence, for codelivery of functional nucleic acid probes into cells, we were able to demonstrate that the overhang‐Cyc‐TAT penetrated into A549 cells when carrying an anti‐telomerase γPNA that specifically reduced telomerase activity by over 97 %. Herein, we report that the cyclized TAT(FAM) can escape endosomes much more efficiently than the linear TAT(FAM) after LED illumination (490 nm). Based on this observation, the endosomal release of overhang‐Cyc‐TAT(FAM)/anti‐telomerase γPNA complex can be greatly enhanced by photoactivation, thus shortening cell treatment time from 60 to 3 h, while keeping the same high efficiency in inhibiting telomerase activity inside A549 cells.

show abstract

Telomerase RNA TLC1 Shuttling to the Cytoplasm Requires mRNA Export Factors and Is Important for Telomere Maintenance

Cited by 35 publications

References 13 publications

Nuclear Pre-snRNA Export Is an Essential Quality Assurance Mechanism for Functional Spliceosomes

Nuclear Pre-snRNA Export Is an Essential Quality Assurance Mechanism for Functional Spliceosomes

Nucleocytoplasmic Transport of RNAs and RNA–Protein Complexes

Efficient Cytoplasmic Delivery of Antisense Probes Assisted by Cyclized‐Peptide‐Mediated Photoinduced Endosomal Escape

Contact Info

Product

Resources

About