Association and regulation of the BLM helicase by the telomere proteins TRF1 and TRF2

Lillard-Wetherell, Kate; Machwe, Amrita; Langland, Gregory T.; Combs, Kelly A.; Behbehani, Gregory K.; Schonberg, Steven; German, James; Turchi, John J.; Orren, David K.; Groden, Joanna

doi:10.1093/hmg/ddh193

Cited by 144 publications

(152 citation statements)

References 47 publications

Supporting

Mentioning

144

Contrasting

Unclassified

Order By: Relevance

“…It is noteworthy that PML bodies that contain DNA in ALT cells, also called APBs, not only contain Smc5/6 (Potts and Yu 2007) but also require Smc5/6-dependent SUMOylation of the shelterin complex, an event thought to mediate the recruitment of telomere repeats to APBs (Potts and Yu 2007). Moreover, BLM has been implicated in ALT pathways, localizes to APBs, and interacts with the shelterin subunits TRF1 and TRF2 (Stavropoulos et al 2002;Lillard-Wetherell et al 2004;Zimmermann et al 2014), and its overexpression promotes increased telomeric HR and longer telomeres (Stavropoulos et al 2002). It is tempting to speculate that Smc5/6 might promote telomeric recombination in ALT cells by coordinating recruitment of telomeres and BLM to APBs and activating the prorecombinogetic role of BLM in a manner analogous to what we demonstrated here for Sgs1.…”

Section: Discussionmentioning

confidence: 99%

Sgs1's roles in DNA end resection, HJ dissolution, and crossover suppression require a two-step SUMO regulation dependent on Smc5/6

et al. 2016

View full text Add to dashboard Cite

The RecQ helicase Sgs1 plays critical roles during DNA repair by homologous recombination, from end resection to Holliday junction (HJ) dissolution. Sgs1 has both pro-and anti-recombinogenic roles, and therefore its activity must be tightly regulated. However, the controls involved in recruitment and activation of Sgs1 at damaged sites are unknown. Here we show a two-step role for Smc5/6 in recruiting and activating Sgs1 through SUMOylation. First, auto-SUMOylation of Smc5/6 subunits leads to recruitment of Sgs1 as part of the STR (Sgs1-Top3-Rmi1) complex, mediated by two SUMO-interacting motifs (SIMs) on Sgs1 that specifically recognize SUMOylated Smc5/6. Second, Smc5/6-dependent SUMOylation of Sgs1 and Top3 is required for the efficient function of STR. Sgs1 mutants impaired in recognition of SUMOylated Smc5/6 (sgs1-SIMΔ) or SUMO-dead alleles (sgs1-KR) exhibit unprocessed HJs at damaged replication forks, increased crossover frequencies during double-strand break repair, and severe impairment in DNA end resection. Smc5/6 is a key regulator of Sgs1's recombination functions.

show abstract

Section: Discussionmentioning

confidence: 99%

Sgs1's roles in DNA end resection, HJ dissolution, and crossover suppression require a two-step SUMO regulation dependent on Smc5/6

et al. 2016

View full text Add to dashboard Cite

show abstract

“…Other studies have also shown that the C-terminal fragment of BLM, encompassing the RQC and HRDC domains, is necessary for the interaction with the telomere-associated protein, TRF2, which stimulates BLM-mediated unwinding of two telomere substrates in vitro; a 3Ј-overhang and a telomere D-loop structure (Lillard-Wetherell et al, 2004). Collectively, these studies indicate that the HRDC domain plays an important role both in conferring some specific enzymatic activities to the individual RecQ enzymes and in DNA structure-specific recognition.…”

Section: The Helicase-and-rnased-like-c-terminal Domainmentioning

confidence: 99%

RecQ helicases: Multiple structures for multiple functions?

Vindigni

Hickson

2009

HFSP Journal

View full text Add to dashboard Cite

“…It has been shown that TRF1 counts and controls the length of telomere repeats, probably through its interaction with TIN2, Tankyrase, PINX1, TPP1, and POT1 (7,9,12,15,(17)(18)(19)(20)(21)(22)(23)(24). In comparison, TRF2 has an essential role in end protection and the telomeric recruitment of several proteins, including the BRCA1 Cterminal domain-containing protein RAP1, the nucleotide excision repair protein ERCC1͞XPF, BLM, and the DNA repair MRN complex (24)(25)(26)(27)(28)(29)(30)(31). Because of their abilities to interact with multiple proteins, TRF1 and TRF2 are by definition hubs of protein-protein interaction at the telomeres (32).…”

mentioning

confidence: 99%

A critical role for TPP1 and TIN2 interaction in high-order telomeric complex assembly

O’Connor

Safari

Xin

et al. 2006

Proc. Natl. Acad. Sci. U.S.A.

219

234

View full text Add to dashboard Cite

Mammalian telomeric proteins function through dynamic interactions with each other and telomere DNA. We previously reported the formation of a high-molecular-mass telomeric complex (the mammalian telosome) that contains the six core proteins TRF1, TRF2, RAP1, TIN2, POT1, and TPP1 (formerly named PTOP͞PIP1͞ TINT1) and mediates telomere end-capping and length control. In this report, we sought to elucidate the mechanism of six-protein complex (or shelterin) formation and the function of this complex. Through reconstitution experiments, we demonstrate here that TIN2 and TPP1 are key components in mediating the six-protein complex assembly. We demonstrate that not only TIN2 but also TPP1 are required to bridge the TRF1 and TRF2 subcomplexes. Specifically, TPP1 helps to stabilize the TRF1-TIN2-TRF2 interaction and promote six-protein complex formation. Consistent with this model, overexpression of TPP1 enhanced TIN2-TRF2 association. Conversely, knocking down TPP1 reduced the ability of endogenous TRF1 to associate with the TRF2 complex. Our results suggest that coordinated interactions among TPP1, TIN2, TRF1, and TRF2 may ensure robust assembly of the telosome, telomere targeting of its subunits, and, ultimately, regulated telomere maintenance.protein complex ͉ telomere ͉ telosome M ammalian telomeres are regulated by the telomerase and telomeric proteins (1-6). Among the telomere-associated proteins important for mammalian telomere homeostasis, POT1 is likely the major regulator of telomere length control (7-9). POT1 binds the 3Ј G-rich telomere overhangs through its oligonucleotide-binding folds (7, 10, 11) and may regulate telomerase access (12)(13)(14). The telomere recruitment of POT1 thus constitutes an important step in telomere end-capping and length control. Recently, a new telomeric protein TPP1 (previously PTOP͞PIP1͞TINT1) was identified as a regulator of POT1 (9,15,16). The telomeric targeting of POT1 depends on its interaction with TPP1 (9). It remains to be determined how TPP1 interacts with other telomeric proteins and whether TPP1 has any function other than targeting POT1.In contrast to POT1, TRF1 and TRF2 directly bind doublestranded telomere DNA and interact with a number of proteins to maintain telomere structure and length (1-5). It has been shown that TRF1 counts and controls the length of telomere repeats, probably through its interaction with TIN2, Tankyrase, PINX1, TPP1, and POT1 (7,9,12,15,(17)(18)(19)(20)(21)(22)(23)(24). In comparison, TRF2 has an essential role in end protection and the telomeric recruitment of several proteins, including the BRCA1 Cterminal domain-containing protein RAP1, the nucleotide excision repair protein ERCC1͞XPF, BLM, and the DNA repair MRN complex (24-31). Because of their abilities to interact with multiple proteins, TRF1 and TRF2 are by definition hubs of protein-protein interaction at the telomeres (32). Recent studies have established multiple pairwise interactions among the six telomeric proteins (TRF1, TRF2, RAP1, TIN2, POT1, and TPP1), including the asso...

show abstract

Association and regulation of the BLM helicase by the telomere proteins TRF1 and TRF2

Cited by 144 publications

References 47 publications

Sgs1's roles in DNA end resection, HJ dissolution, and crossover suppression require a two-step SUMO regulation dependent on Smc5/6

Sgs1's roles in DNA end resection, HJ dissolution, and crossover suppression require a two-step SUMO regulation dependent on Smc5/6

RecQ helicases: Multiple structures for multiple functions?

A critical role for TPP1 and TIN2 interaction in high-order telomeric complex assembly

Contact Info

Product

Resources

About