hSSB1 and hSSB2 Form Similar Multiprotein Complexes That Participate in DNA Damage Response

Li, Yongjiang; Bolderson, Emma; Kumar, Rakesh; Muniandy, Parameswary A.; Xue, Yutong; Richard, Derek J.; Seidman, Michael M.; Pandita, Tej K.; Khanna, Kum Kum; Wang, Weidong

doi:10.1074/jbc.c109.039586

Cited by 104 publications

(177 citation statements)

References 29 publications

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“…In mSSB1 ∆/∆ MEFs, mSSB1 protein was undetectable, confirming that we successfully generated a mSSB1-null allele ( Figure 1B and 1C). The localization of mSSB2 to IR-induced DNA damage foci was not affected upon mSSB1 deletion, in agreement with previous reports [17,18,20] (Figure 1C). Interestingly, mSSB2 protein level was upregulated in the absence of mSSB1 ( Figure 1B).…”

Section: Mssb1 Deletion Results In Increased Chromosomal Aberrationssupporting

confidence: 82%

“…Previous studies suggest that hSSB1 and hSSB2 both form complexes with INTS3 and possess overlapping functions in the DNA damage response (DDR) [17,18]. The elevated expression of mSSB2 observed when mSSB1 is deleted ( Figures 1C, 2B, 2C and 3F) suggests that upregulation of mSSB2 likely compensates for mSSB1 loss, thereby complicating the analysis of mSSB1 function.…”

Section: Increased Chromatid Fusions In Mssb1-null Mefsmentioning

confidence: 83%

“…siRNA knockdown experiments suggest that INTS3 links hSSB1/2 and C9orf80 into heterotrimeric complexes [17,18,20]. As INTS3 controls the levels of hSSB1 through transcriptional regulation [20], it is unclear whether hSSB1 is able to localize to damaged DNA independent of INTS3.…”

Section: Localization Of Mssb1 To Damaged Dna Requires Both Interactimentioning

confidence: 99%

“…Notably, long trains of end-to-end fused chromosomes, a hallmark of TRF2 loss, were rarely observed in the setting of mSSB1 deficiency. As activation of the ATM kinase is negatively impacted when hSSB1 is depleted [17,18,20], we monitored the Chk2 phosphorylation status in mSSB1 ∆/∆ MEFs treated with shTRF2. Chk2 phosphorylation in mSSB1 ∆/∆ MEFs appears similar to that observed in WT MEFs, although this analysis is complicated by the fact that mSSB2 levels increased following mSSB1 deletion and therefore any decline in Chk2 phosphorylation due to mSSB1 loss will not be evident ( Figure 2B).…”

Section: Mssb1 and Mssb2 Localize To Telomeres And Participate In Thementioning

confidence: 99%

“…Telomeres consist of TTAGGG repetitive sequences that terminate in a 3′ ss G-rich overhang, and invasion of the 3′ end into duplex regions of the telomere is postulated to be important to protect DNA ends from being recognized by RPA, which would INTS3 and C9orf80, termed sensor of ssDNA complex 1 and 2 (SOSS1/2) [17][18][19][20]. Although RPA recruitment to damaged DNA requires both CtIP and the MRN complex, localization of SOSS1 to damaged DNA in S/ G2 phase requires only MRN [17].…”

Section: Introductionmentioning

confidence: 99%

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Single strand DNA binding proteins 1 and 2 protect newly replicated telomeres

Deng

Lei

et al. 2013

Cell Res

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Human single-strand (ss) DNA binding proteins 1 and 2 (hSSB1 and 2) are components of the hSSB1/2-INTS3-C9orf80 heterotrimeric protein complex shown to participate in DNA damage response and maintenance of genome stability. However, their roles at telomeres remain unknown. Here, we generated murine SSB1 conditional knockout mice and cells and found that mSSB1 plays a critical role in telomere end protection. Both mSSB1 and mSSB2 localize to a subset of telomeres and are required to repair TRF2-deficient telomeres. Deletion of mSSB1 resulted in increased chromatid-type fusions involving both leading-and lagging-strand telomeric DNA, suggesting that it is required for the protection of G-overhangs. mSSB1's interaction with INTS3 is required for its localization to damaged DNA. mSSB1 interacts with Pot1a, but not Pot1b, and its association with telomeric ssDNA requires Pot1a. mSSB1 ∆/∆ mice die at birth with developmental abnormalities, while mice with the hypomorphic mSSB1 F/F allele are born alive and display increased sensitivity to ionizing radiation (IR). Our results suggest that mSSB1 is required to maintain genome stability, and document a previously unrecognized role for mSSB1/2 in the protection of newly replicated leading-and lagging-strand telomeres.

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Section: Mssb1 Deletion Results In Increased Chromosomal Aberrationssupporting

confidence: 82%

Section: Increased Chromatid Fusions In Mssb1-null Mefsmentioning

confidence: 83%

Section: Localization Of Mssb1 To Damaged Dna Requires Both Interactimentioning

confidence: 99%

Section: Mssb1 and Mssb2 Localize To Telomeres And Participate In Thementioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Single strand DNA binding proteins 1 and 2 protect newly replicated telomeres

Deng

Lei

et al. 2013

Cell Res

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DNA‐dependent phase separation by human SSB2 (NABP1/OBFC2A) protein points to adaptations to eukaryotic genome repair processes

Kovács,

Harami,

Pálinkás

et al. 2024

Protein Science

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Single‐stranded DNA binding proteins (SSBs) are ubiquitous across all domains of life and play essential roles via stabilizing and protecting single‐stranded (ss) DNA as well as organizing multiprotein complexes during DNA replication, recombination, and repair. Two mammalian SSB paralogs (hSSB1 and hSSB2 in humans) were recently identified and shown to be involved in various genome maintenance processes. Following our recent discovery of the liquid–liquid phase separation (LLPS) propensity of Escherichia coli (Ec) SSB, here we show that hSSB2 also forms LLPS condensates under physiologically relevant ionic conditions. Similar to that seen for EcSSB, we demonstrate the essential contribution of hSSB2's C‐terminal intrinsically disordered region (IDR) to condensate formation, and the selective enrichment of various genome metabolic proteins in hSSB2 condensates. However, in contrast to EcSSB‐driven LLPS that is inhibited by ssDNA binding, hSSB2 phase separation requires single‐stranded nucleic acid binding, and is especially facilitated by ssDNA. Our results reveal an evolutionarily conserved role for SSB‐mediated LLPS in the spatiotemporal organization of genome maintenance complexes. At the same time, differential LLPS features of EcSSB and hSSB2 point to functional adaptations to prokaryotic versus eukaryotic genome metabolic contexts.

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The structural details of the interaction of single‐stranded DNA binding protein hSSB2 (NABP1/OBFC2A) with UV‐damaged DNA

et al. 2019

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Single-stranded DNA-binding proteins (SSBs) are required for all known DNA metabolic events such as DNA replication, recombination and repair. While a wealth of structural and functional data is available on the essential human SSB, hSSB1 (NABP2/OBFC2B), the close homolog hSSB2 (NABP1/OBFC2A) remains relatively uncharacterized. Both SSBs possess a well-structured OB (oligonucleotide/oligosaccharide-binding) domain that is able to recognize single-stranded DNA (ssDNA) followed by a flexible carboxyltail implicated in the interaction with other proteins. Despite the high sequence similarity of the OB domain, several recent studies have revealed distinct functional differences between hSSB1 and hSSB2. In this study, we show that hSSB2 is able to recognize cyclobutane pyrimidine dimers (CPD) that form in cellular DNA as a consequence of UV damage. Using a combination of biolayer interferometry and NMR, we determine the molecular details of the binding of the OB domain of hSSB2 to CPD-containing ssDNA, confirming the role of four key aromatic residues in hSSB2 (W59, Y78, W82, and Y89) that are also conserved in hSSB1. Our structural data thus demonstrate that ssDNA recognition by the OB fold of hSSB2 is highly similar to hSSB1, indicating that one SSB may be able to replace the other in any initial ssDNA binding event. However, any subsequent recruitment of other repair proteins most likely depends on the divergent carboxyl-tail and as such is likely to be different between hSSB1 and hSSB2.

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hSSB1 and hSSB2 Form Similar Multiprotein Complexes That Participate in DNA Damage Response

Cited by 104 publications

References 29 publications

Single strand DNA binding proteins 1 and 2 protect newly replicated telomeres

Single strand DNA binding proteins 1 and 2 protect newly replicated telomeres

DNA‐dependent phase separation by human SSB2 (NABP1/OBFC2A) protein points to adaptations to eukaryotic genome repair processes

The structural details of the interaction of single‐stranded DNA binding protein hSSB2 (NABP1/OBFC2A) with UV‐damaged DNA

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