Your search keyword '"MUS81"' showing total 347 results

1. TDP1 phosphorylation by CDK1 in mitosis promotes MUS81-dependent repair of trapped Top1-DNA covalent complexes.

Author

Paul Chowdhuri, Srijita and Das, Benu Brata

Subjects

*CELLULAR control mechanisms, *DNA damage, *DNA topoisomerase I, *GENETIC transcription, *ANAPHASE, *DNA repair

Abstract

Topoisomerase 1 (Top1) controls DNA topology, relieves DNA supercoiling during replication and transcription, and is critical for mitotic progression to the G1 phase. Tyrosyl-DNA phosphodiesterase 1 (TDP1) mediates the removal of trapped Top1-DNA covalent complexes (Top1cc). Here, we identify CDK1-dependent phosphorylation of TDP1 at residue S61 during mitosis. A TDP1 variant defective for S61 phosphorylation (TDP1-S61A) is trapped on the mitotic chromosomes, triggering DNA damage and mitotic defects. Moreover, we show that Top1cc repair in mitosis occurs via a MUS81-dependent DNA repair mechanism. Replication stress induced by camptothecin or aphidicolin leads to TDP1-S61A enrichment at common fragile sites, which over-stimulates MUS81-dependent chromatid breaks, anaphase bridges, and micronuclei, ultimately culminating in the formation of 53BP1 nuclear bodies during G1 phase. Our findings provide new insights into the cell cycle-dependent regulation of TDP1 dynamics for the repair of trapped Top1-DNA covalent complexes during mitosis that prevents genomic instability following replication stress. Synopsis: Tyrosyl-DNA phosphodiesterase 1 (TDP1) supports repair of trapped Top1-DNA covalent complexes. This study shows that TDP1 is phosphorylated at its residue S61 by CDK1 during mitosis, countering DNA damage, mitotic abnormalities, and chromosomal instability upon replication stress. CDK1 phosphorylates TDP1 at S61 during mitosis. TDP1 defective for S61 phosphorylation (TDP1-S61A) is retained on the mitotic chromosomes, triggering DNA damage and mitotic defects. A MUS81-dependent pathway is predominantly responsible for mitotic clearing of trapped Top1-DNA covalent complexes. MUS81 depletion rescues chromosomal abnormalities in TDP1-S61A-expressing cells. Blocking CDK1-mediated TDP1 phosphorylation results in increased levels of DNA damage and genomic instability upon replication stress. [ABSTRACT FROM AUTHOR]

Published

2024

2. MUS81 cleaves TOP1-derived lesions and other DNA–protein cross-links

Author

Victoria Marini, Fedor Nikulenkov, Pounami Samadder, Sissel Juul, Birgitta R. Knudsen, and Lumir Krejci

Subjects

DNA-protein cross-links repair, MUS81, TDP1, Topoisomerase 1, Biology (General), QH301-705.5

Abstract

Abstract Background DNA-protein cross-links (DPCs) are one of the most deleterious DNA lesions, originating from various sources, including enzymatic activity. For instance, topoisomerases, which play a fundamental role in DNA metabolic processes such as replication and transcription, can be trapped and remain covalently bound to DNA in the presence of poisons or nearby DNA damage. Given the complexity of individual DPCs, numerous repair pathways have been described. The protein tyrosyl-DNA phosphodiesterase 1 (Tdp1) has been demonstrated to be responsible for removing topoisomerase 1 (Top1). Nevertheless, studies in budding yeast have indicated that alternative pathways involving Mus81, a structure-specific DNA endonuclease, could also remove Top1 and other DPCs. Results This study shows that MUS81 can efficiently cleave various DNA substrates modified by fluorescein, streptavidin or proteolytically processed topoisomerase. Furthermore, the inability of MUS81 to cleave substrates bearing native TOP1 suggests that TOP1 must be either dislodged or partially degraded prior to MUS81 cleavage. We demonstrated that MUS81 could cleave a model DPC in nuclear extracts and that depletion of TDP1 in MUS81-KO cells induces sensitivity to the TOP1 poison camptothecin (CPT) and affects cell proliferation. This sensitivity is only partially suppressed by TOP1 depletion, indicating that other DPCs might require the MUS81 activity for cell proliferation. Conclusions Our data indicate that MUS81 and TDP1 play independent roles in the repair of CPT-induced lesions, thus representing new therapeutic targets for cancer cell sensitisation in combination with TOP1 inhibitors.

Published

2023

3. MUS81 cleaves TOP1-derived lesions and other DNA–protein cross-links.

Author

Marini, Victoria, Nikulenkov, Fedor, Samadder, Pounami, Juul, Sissel, Knudsen, Birgitta R., and Krejci, Lumir

Subjects

*DNA topoisomerase I, *NUCLEAR models, *POISONS, *ENDONUCLEASES, *CELL proliferation, *CAMPTOTHECIN, *DRUG target, *DNA repair, *DNA damage

Abstract

Background: DNA-protein cross-links (DPCs) are one of the most deleterious DNA lesions, originating from various sources, including enzymatic activity. For instance, topoisomerases, which play a fundamental role in DNA metabolic processes such as replication and transcription, can be trapped and remain covalently bound to DNA in the presence of poisons or nearby DNA damage. Given the complexity of individual DPCs, numerous repair pathways have been described. The protein tyrosyl-DNA phosphodiesterase 1 (Tdp1) has been demonstrated to be responsible for removing topoisomerase 1 (Top1). Nevertheless, studies in budding yeast have indicated that alternative pathways involving Mus81, a structure-specific DNA endonuclease, could also remove Top1 and other DPCs. Results: This study shows that MUS81 can efficiently cleave various DNA substrates modified by fluorescein, streptavidin or proteolytically processed topoisomerase. Furthermore, the inability of MUS81 to cleave substrates bearing native TOP1 suggests that TOP1 must be either dislodged or partially degraded prior to MUS81 cleavage. We demonstrated that MUS81 could cleave a model DPC in nuclear extracts and that depletion of TDP1 in MUS81-KO cells induces sensitivity to the TOP1 poison camptothecin (CPT) and affects cell proliferation. This sensitivity is only partially suppressed by TOP1 depletion, indicating that other DPCs might require the MUS81 activity for cell proliferation. Conclusions: Our data indicate that MUS81 and TDP1 play independent roles in the repair of CPT-induced lesions, thus representing new therapeutic targets for cancer cell sensitisation in combination with TOP1 inhibitors. [ABSTRACT FROM AUTHOR]

Published

2023

4. The Control of the Crossover Localization in Allium.

Author

Kudryavtseva, Natalia, Ermolaev, Aleksey, Pivovarov, Anton, Simanovsky, Sergey, Odintsov, Sergey, and Khrustaleva, Ludmila

Subjects

*ALLIUM fistulosum, *ALLIUM, *ONIONS, *STEM cells, *IN situ hybridization

Abstract

Meiotic crossovers/chiasmata are not randomly distributed and strictly controlled. The mechanisms behind crossover (CO) patterning remain largely unknown. In Allium cepa, as in the vast majority of plants and animals, COs predominantly occur in the distal 2/3 of the chromosome arm, while in Allium fistulosum they are strictly localized in the proximal region. We investigated the factors that may contribute to the pattern of COs in A. cepa, A. fistulosum and their F 1 diploid (2n = 2x = 8C + 8F) and F 1 triploid (2n = 3x = 16F + 8C) hybrids. The genome structure of F 1 hybrids was confirmed using genomic in situ hybridization (GISH). The analysis of bivalents in the pollen mother cells (PMCs) of the F 1 triploid hybrid showed a significant shift in the localization of COs to the distal and interstitial regions. In F 1 diploid hybrid, the COs localization was predominantly the same as that of the A. cepa parent. We found no differences in the assembly and disassembly of ASY1 and ZYP1 in PMCs between A. cepa and A. fistulosum, while F 1 diploid hybrid showed a delay in chromosome pairing and a partial absence of synapsis in paired chromosomes. Immunolabeling of MLH1 (class I COs) and MUS81 (class II COs) proteins showed a significant difference in the class I/II CO ratio between A. fistulosum (50%:50%) and A. cepa (73%:27%). The MLH1:MUS81 ratio at the homeologous synapsis of F 1 diploid hybrid (70%:30%) was the most similar to that of the A. cepa parent. F 1 triploid hybrid at the A. fistulosum homologous synapsis showed a significant increase in MLH1:MUS81 ratio (60%:40%) compared to the A. fistulosum parent. The results suggest possible genetic control of CO localization. Other factors affecting the distribution of COs are discussed. [ABSTRACT FROM AUTHOR]

Published

2023

5. MUS81 is required for atypical recombination intermediate resolution but not crossover designation in rice.

Author

Mu, Na, Li, Yafei, Li, Sanhe, Shi, Wenqing, Shen, Yi, Yang, Han, Zhang, Fanfan, Tang, Ding, Du, Guijie, You, Aiqing, and Cheng, Zhukuan

Subjects

*GENETIC recombination, *MEIOSIS, *METHYL methanesulfonate, *DNA repair, *CROSSING over (Genetics), *CHROMOSOMES, *MITOSIS

Abstract

Summary: The endonuclease methyl methanesulfonate and UV‐sensitive protein 81 (MUS81) has been reported to participate in DNA repair during mitosis and meiosis. However, the exact meiotic function of MUS81 in rice remains unclear.Here, we use a combination of physiological, cytological, and genetic approaches to provide evidence that MUS81 functions in atypical recombination intermediate resolution rather than crossover designation in rice.Cytological and genetic analysis revealed that the total chiasma numbers in mus81 mutants were indistinguishable from wild‐type. The numbers of HEI10 foci (the sites of interference‐sensitive crossovers) in mus81 were also similar to that of wild‐type. Moreover, disruption of MUS81 in msh5 or msh4 msh5 background did not further decrease chiasmata frequency, suggesting that rice MUS81 did not function in crossover designation. Mutation of FANCM and ZEP1 could enhance recombination frequency. Unexpectedly, chromosome fragments and bridges were frequently observed in mus81 zep1 and mus81 fancm, illustrating that MUS81 may resolve atypical recombination intermediates.Taken together, our data suggest that MUS81 contributes little to crossover designation but plays a crucial role in the resolution of atypical meiotic intermediates by working together with other anti‐crossover factors. [ABSTRACT FROM AUTHOR]

Published

2023

6. Targeting MUS81 promotes the anticancer effect of WEE1 inhibitor and immune checkpoint blocking combination therapy via activating cGAS/STING signaling in gastric cancer cells

Author

Chengguo Li, Qian Shen, Peng Zhang, Tao Wang, Weizhen Liu, Ruidong Li, Xianxiong Ma, Xiangyu Zeng, Yuping Yin, and Kaixiong Tao

Subjects

MUS81, WEE1, Immune checkpoint blocking, cGAS/STING pathway, Gastric cancer, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Identification of genomic biomarkers to predict the anticancer effects of indicated drugs is considered a promising strategy for the development of precision medicine. DNA endonuclease MUS81 plays a pivotal role in various biological processes during malignant diseases, mainly in DNA damage repair and replication fork stability. Our previous study reported that MUS81 was highly expressed and linked to tumor metastasis in gastric cancer; however, its therapeutic value has not been fully elucidated. Methods Bioinformatics analysis was used to define MUS81-related differential genes, which were further validated in clinical tissue samples. Gain or loss of function MUS81 cell models were constructed to elucidate the effect and mechanism of MUS81 on WEE1 expression. Moreover, the antitumor effect of targeting MUS81 combined with WEE1 inhibitors was verified using in vivo and in vitro assays. Thereafter, the cGAS/STING pathway was evaluated, and the therapeutic value of MUS81 for immunotherapy of gastric cancer was determined. Results In this study, MUS81 negatively correlated with the expression of cell cycle checkpoint kinase WEE1. Furthermore, we identified that MUS81 regulated the ubiquitination of WEE1 via E-3 ligase β-TRCP in an enzymatic manner. In addition, MUS81 inhibition could sensitize the anticancer effect of the WEE1 inhibitor MK1775 in gastric cancer in vitro and in vivo. Interestingly, when MUS81 was targeted, it increased the accumulation of cytosolic DNA induced by MK1775 treatment and activated the DNA sensor STING-mediated innate immunity in the gastric cancer cells. Thus, the WEE1 inhibitor MK1775 specifically enhanced the anticancer effect of immune checkpoint blockade therapy in MUS81 deficient gastric cancer cells. Conclusions Our data provide rational evidence that targeting MUS81 could elevate the expression of WEE1 by regulating its ubiquitination and could activate the innate immune response, thereby enhancing the anticancer efficacy of WEE1 inhibitor and immune checkpoint blockade combination therapy in gastric cancer cells.

Published

2021

7. Comparative transcriptomic analysis of thermally stressed Arabidopsis thaliana meiotic recombination mutants

Author

Jiyue Huang, Hongkuan Wang, Yingxiang Wang, and Gregory P. Copenhaver

Subjects

Heat stress, Meiotic recombination, MUS81, MSH4, ASY1, RNA-Seq, Biotechnology, TP248.13-248.65, Genetics, QH426-470

Abstract

Abstract Background Meiosis is a specialized cell division that underpins sexual reproduction in most eukaryotes. During meiosis, interhomolog meiotic recombination facilitates accurate chromosome segregation and generates genetic diversity by shuffling parental alleles in the gametes. The frequency of meiotic recombination in Arabidopsis has a U-shaped curve in response to environmental temperature, and is dependent on the Type I, crossover (CO) interference-sensitive pathway. The mechanisms that modulate recombination frequency in response to temperature are not yet known. Results In this study, we compare the transcriptomes of thermally-stressed meiotic-stage anthers from msh4 and mus81 mutants that mediate the Type I and Type II meiotic recombination pathways, respectively. We show that heat stress reduces the number of expressed genes regardless of genotype. In addition, msh4 mutants have a distinct gene expression pattern compared to mus81 and wild type controls. Interestingly, ASY1, which encodes a HORMA domain protein that is a component of meiotic chromosome axes, is up-regulated in wild type and mus81 but not in msh4. In addition, SDS the meiosis-specific cyclin-like gene, DMC1 the meiosis-specific recombinase, SYN1/REC8 the meiosis-specific cohesion complex component, and SWI1 which functions in meiotic sister chromatid cohesion are up-regulated in all three genotypes. We also characterize 51 novel, previously unannotated transcripts, and show that their promoter regions are associated with A-rich meiotic recombination hotspot motifs. Conclusions Our transcriptomic analysis of msh4 and mus81 mutants enhances our understanding of how the Type I and Type II meiotic CO pathway respond to environmental temperature stress and might provide a strategy to manipulate recombination levels in plants.

Published

2021

8. The Control of the Crossover Localization in Allium

Author

Natalia Kudryavtseva, Aleksey Ermolaev, Anton Pivovarov, Sergey Simanovsky, Sergey Odintsov, and Ludmila Khrustaleva

Subjects

chiasmata localization, MUS81, MLH1, ASY1, ZYP1, Allium, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Meiotic crossovers/chiasmata are not randomly distributed and strictly controlled. The mechanisms behind crossover (CO) patterning remain largely unknown. In Allium cepa, as in the vast majority of plants and animals, COs predominantly occur in the distal 2/3 of the chromosome arm, while in Allium fistulosum they are strictly localized in the proximal region. We investigated the factors that may contribute to the pattern of COs in A. cepa, A. fistulosum and their F1 diploid (2n = 2x = 8C + 8F) and F1 triploid (2n = 3x = 16F + 8C) hybrids. The genome structure of F1 hybrids was confirmed using genomic in situ hybridization (GISH). The analysis of bivalents in the pollen mother cells (PMCs) of the F1 triploid hybrid showed a significant shift in the localization of COs to the distal and interstitial regions. In F1 diploid hybrid, the COs localization was predominantly the same as that of the A. cepa parent. We found no differences in the assembly and disassembly of ASY1 and ZYP1 in PMCs between A. cepa and A. fistulosum, while F1 diploid hybrid showed a delay in chromosome pairing and a partial absence of synapsis in paired chromosomes. Immunolabeling of MLH1 (class I COs) and MUS81 (class II COs) proteins showed a significant difference in the class I/II CO ratio between A. fistulosum (50%:50%) and A. cepa (73%:27%). The MLH1:MUS81 ratio at the homeologous synapsis of F1 diploid hybrid (70%:30%) was the most similar to that of the A. cepa parent. F1 triploid hybrid at the A. fistulosum homologous synapsis showed a significant increase in MLH1:MUS81 ratio (60%:40%) compared to the A. fistulosum parent. The results suggest possible genetic control of CO localization. Other factors affecting the distribution of COs are discussed.

Published

2023

9. MUS81 Inhibition Enhances the Anticancer Efficacy of Talazoparib by Impairing ATR/CHK1 Signaling Pathway in Gastric Cancer.

Author

Wang, Tao, Zhang, Peng, Li, Chengguo, Liu, Weizhen, Shen, Qian, Yang, Lei, Xie, Gengchen, Bai, Jie, Li, Ruidong, Tao, Kaixiong, and Yin, Yuping

Subjects

STOMACH cancer, ANTINEOPLASTIC agents, CELLULAR signal transduction, DNA repair, DNA damage

Abstract

MUS81 is a critical endonuclease involved in heterodimer formation with Eme1/Mms4 and an important DNA damage repair regulatory molecule. Our previous study suggested that MUS81 was overexpressed and its high expression was positively correlated with gastric cancer metastasis. However, the therapeutic potential of targeting MUS81 in gastric cancer requires further exploration. Therefore, in this study, the Cancer Genome Atlas (TCGA) data were analyzed and showed that MUS81 is a key regulator of cell cycle distribution and DNA damage repair in gastric cancer. In vitro and in vivo , MUS81 knockdown significantly enhanced the anticancer effect of the PARP inhibitor talazoparib. Mechanistically, MUS81 inhibition impaired the activation of the ATR/CHK1 cell cycle signaling pathway and promoted gastric cancer cells with talazoparib-induced DNA damage to continue mitosis. Moreover, addition of the bromodomain-containing protein 4 inhibitor AZD5153 increased the anticancer effect of talazoparib via MUS81 inhibition in gastric cancer cells, and this combination effect was largely impaired when MUS81 was knocked down. In conclusion, these data suggested that MUS81 regulated ATR/CHK1 activation, a key signaling pathway in the G2M checkpoint, and targeting MUS81 enhanced the antitumor efficacy of talazoparib. Therefore, AZD5153 combined with talazoparib may represent a promising therapeutic strategy for patients with MUS81 proficient gastric cancer. [ABSTRACT FROM AUTHOR]

Published

2022

10. MUS81 Inhibition Enhances the Anticancer Efficacy of Talazoparib by Impairing ATR/CHK1 Signaling Pathway in Gastric Cancer

Author

Tao Wang, Peng Zhang, Chengguo Li, Weizhen Liu, Qian Shen, Lei Yang, Gengchen Xie, Jie Bai, Ruidong Li, Kaixiong Tao, and Yuping Yin

Subjects

gastric cancer, MUS81, PARP inhibitor, BRD4 inhibitor, DNA damage, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

MUS81 is a critical endonuclease involved in heterodimer formation with Eme1/Mms4 and an important DNA damage repair regulatory molecule. Our previous study suggested that MUS81 was overexpressed and its high expression was positively correlated with gastric cancer metastasis. However, the therapeutic potential of targeting MUS81 in gastric cancer requires further exploration. Therefore, in this study, the Cancer Genome Atlas (TCGA) data were analyzed and showed that MUS81 is a key regulator of cell cycle distribution and DNA damage repair in gastric cancer. In vitro and in vivo, MUS81 knockdown significantly enhanced the anticancer effect of the PARP inhibitor talazoparib. Mechanistically, MUS81 inhibition impaired the activation of the ATR/CHK1 cell cycle signaling pathway and promoted gastric cancer cells with talazoparib-induced DNA damage to continue mitosis. Moreover, addition of the bromodomain-containing protein 4 inhibitor AZD5153 increased the anticancer effect of talazoparib via MUS81 inhibition in gastric cancer cells, and this combination effect was largely impaired when MUS81 was knocked down. In conclusion, these data suggested that MUS81 regulated ATR/CHK1 activation, a key signaling pathway in the G2M checkpoint, and targeting MUS81 enhanced the antitumor efficacy of talazoparib. Therefore, AZD5153 combined with talazoparib may represent a promising therapeutic strategy for patients with MUS81 proficient gastric cancer.

Published

2022

11. Targeting MUS81 promotes the anticancer effect of WEE1 inhibitor and immune checkpoint blocking combination therapy via activating cGAS/STING signaling in gastric cancer cells.

Author

Li, Chengguo, Shen, Qian, Zhang, Peng, Wang, Tao, Liu, Weizhen, Li, Ruidong, Ma, Xianxiong, Zeng, Xiangyu, Yin, Yuping, and Tao, Kaixiong

Subjects

*IMMUNE checkpoint inhibitors, *ANTINEOPLASTIC agents, *STOMACH cancer, *CANCER cells, *IMMUNE checkpoint proteins, *IPILIMUMAB

Abstract

Background: Identification of genomic biomarkers to predict the anticancer effects of indicated drugs is considered a promising strategy for the development of precision medicine. DNA endonuclease MUS81 plays a pivotal role in various biological processes during malignant diseases, mainly in DNA damage repair and replication fork stability. Our previous study reported that MUS81 was highly expressed and linked to tumor metastasis in gastric cancer; however, its therapeutic value has not been fully elucidated. Methods: Bioinformatics analysis was used to define MUS81-related differential genes, which were further validated in clinical tissue samples. Gain or loss of function MUS81 cell models were constructed to elucidate the effect and mechanism of MUS81 on WEE1 expression. Moreover, the antitumor effect of targeting MUS81 combined with WEE1 inhibitors was verified using in vivo and in vitro assays. Thereafter, the cGAS/STING pathway was evaluated, and the therapeutic value of MUS81 for immunotherapy of gastric cancer was determined. Results: In this study, MUS81 negatively correlated with the expression of cell cycle checkpoint kinase WEE1. Furthermore, we identified that MUS81 regulated the ubiquitination of WEE1 via E-3 ligase β-TRCP in an enzymatic manner. In addition, MUS81 inhibition could sensitize the anticancer effect of the WEE1 inhibitor MK1775 in gastric cancer in vitro and in vivo. Interestingly, when MUS81 was targeted, it increased the accumulation of cytosolic DNA induced by MK1775 treatment and activated the DNA sensor STING-mediated innate immunity in the gastric cancer cells. Thus, the WEE1 inhibitor MK1775 specifically enhanced the anticancer effect of immune checkpoint blockade therapy in MUS81 deficient gastric cancer cells. Conclusions: Our data provide rational evidence that targeting MUS81 could elevate the expression of WEE1 by regulating its ubiquitination and could activate the innate immune response, thereby enhancing the anticancer efficacy of WEE1 inhibitor and immune checkpoint blockade combination therapy in gastric cancer cells. [ABSTRACT FROM AUTHOR]

Published

2021

12. Valproic Acid Regulates HR and Cell Cycle Through MUS81-pRPA2 Pathway in Response to Hydroxyurea

Author

Benyu Su, David Lim, Zhujun Tian, Guochao Liu, Chenxia Ding, Zuchao Cai, Chen Chen, Fengmei Zhang, and Zhihui Feng

Subjects

breast cancer, VPA, HU, pRPA2, MUS81, cell cycle, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Breast cancer is the primary problem threatening women’s health. The combined application of valproic acid (VPA) and hydroxyurea (HU) has a synergistic effect on killing breast cancer cells, but the molecular mechanism remains elusive. Replication protein A2 phosphorylation (pRPA2), is essential for homologous recombination (HR) repair and cell cycle. Here we showed that in response to HU, the VPA significantly decreased the tumor cells survival, and promoted S-phase slippage, which was associated with the decrease of pCHK1 and WEE1/pCDK1-mediated checkpoint kinases phosphorylation pathway and inhibited pRPA2/Rad51-mediated HR repair pathway; the mutation of pRPA2 significantly diminished the above effect, indicating that VPA-caused HU sensitization was pRPA2 dependent. It was further found that VPA and HU combination treatment also resulted in the decrease of endonuclease MUS81. After MUS81 elimination, not only the level of pRPA2 was abolished in response to HU treatment, but also VPA-caused HU sensitization was significantly down-regulated through pRPA2-mediated checkpoint kinases phosphorylation and HR repair pathways. In addition, the VPA altered the tumor microenvironment and reduced tumor burden by recruiting macrophages to tumor sites; the Kaplan-Meier analysis showed that patients with high pRPA2 expression had significantly worse survival. Overall, our findings demonstrated that VPA influences HR repair and cell cycle through down-regulating MUS81-pRPA2 pathway in response to HU treatment.

Published

2021

13. Valproic Acid Regulates HR and Cell Cycle Through MUS81-pRPA2 Pathway in Response to Hydroxyurea.

Author

Su, Benyu, Lim, David, Tian, Zhujun, Liu, Guochao, Ding, Chenxia, Cai, Zuchao, Chen, Chen, Zhang, Fengmei, and Feng, Zhihui

Subjects

VALPROIC acid, CELL cycle, BREAST cancer, HYDROXYUREA, CELL survival

Abstract

Breast cancer is the primary problem threatening women's health. The combined application of valproic acid (VPA) and hydroxyurea (HU) has a synergistic effect on killing breast cancer cells, but the molecular mechanism remains elusive. Replication protein A2 phosphorylation (pRPA2), is essential for homologous recombination (HR) repair and cell cycle. Here we showed that in response to HU, the VPA significantly decreased the tumor cells survival, and promoted S-phase slippage, which was associated with the decrease of pCHK1 and WEE1/pCDK1-mediated checkpoint kinases phosphorylation pathway and inhibited pRPA2/Rad51-mediated HR repair pathway; the mutation of pRPA2 significantly diminished the above effect, indicating that VPA-caused HU sensitization was pRPA2 dependent. It was further found that VPA and HU combination treatment also resulted in the decrease of endonuclease MUS81. After MUS81 elimination, not only the level of pRPA2 was abolished in response to HU treatment, but also VPA-caused HU sensitization was significantly down-regulated through pRPA2-mediated checkpoint kinases phosphorylation and HR repair pathways. In addition, the VPA altered the tumor microenvironment and reduced tumor burden by recruiting macrophages to tumor sites; the Kaplan-Meier analysis showed that patients with high pRPA2 expression had significantly worse survival. Overall, our findings demonstrated that VPA influences HR repair and cell cycle through down-regulating MUS81-pRPA2 pathway in response to HU treatment. [ABSTRACT FROM AUTHOR]

Published

2021

14. Comparative transcriptomic analysis of thermally stressed Arabidopsis thaliana meiotic recombination mutants.

Author

Huang, Jiyue, Wang, Hongkuan, Wang, Yingxiang, and Copenhaver, Gregory P.

Subjects

*MEIOSIS, *STRAINS & stresses (Mechanics), *ARABIDOPSIS thaliana, *CHROMOSOME segregation, *GENES, *CELL division

Abstract

Background: Meiosis is a specialized cell division that underpins sexual reproduction in most eukaryotes. During meiosis, interhomolog meiotic recombination facilitates accurate chromosome segregation and generates genetic diversity by shuffling parental alleles in the gametes. The frequency of meiotic recombination in Arabidopsis has a U-shaped curve in response to environmental temperature, and is dependent on the Type I, crossover (CO) interference-sensitive pathway. The mechanisms that modulate recombination frequency in response to temperature are not yet known. Results: In this study, we compare the transcriptomes of thermally-stressed meiotic-stage anthers from msh4 and mus81 mutants that mediate the Type I and Type II meiotic recombination pathways, respectively. We show that heat stress reduces the number of expressed genes regardless of genotype. In addition, msh4 mutants have a distinct gene expression pattern compared to mus81 and wild type controls. Interestingly, ASY1, which encodes a HORMA domain protein that is a component of meiotic chromosome axes, is up-regulated in wild type and mus81 but not in msh4. In addition, SDS the meiosis-specific cyclin-like gene, DMC1 the meiosis-specific recombinase, SYN1/REC8 the meiosis-specific cohesion complex component, and SWI1 which functions in meiotic sister chromatid cohesion are up-regulated in all three genotypes. We also characterize 51 novel, previously unannotated transcripts, and show that their promoter regions are associated with A-rich meiotic recombination hotspot motifs. Conclusions: Our transcriptomic analysis of msh4 and mus81 mutants enhances our understanding of how the Type I and Type II meiotic CO pathway respond to environmental temperature stress and might provide a strategy to manipulate recombination levels in plants. [ABSTRACT FROM AUTHOR]

Published

2021

15. The cruciform DNA‐binding protein Crp1 stimulates the endonuclease activity of Mus81–Mms4 in Saccharomyces cerevisiae.

Author

Phung, Huong Thi Thu, Tran, Diem Hong, and Nguyen, Ta Xuan

Subjects

*DNA-binding proteins, *SACCHAROMYCES cerevisiae, *DNA replication, *ENDONUCLEASES, *DNA repair, *PROTEIN-protein interactions, *DNA

Abstract

The Saccharomyces cerevisiae Mus81–Mms4 complex is a highly conserved DNA structure‐specific endonuclease that plays essential roles in the processing of recombination intermediates that arise during the repair of stalled replication forks and double‐stranded breaks. To identify novel factors functioning conjointly with Mus81–Mms4, we performed a biochemical screen and found that Crp1, a cruciform DNA‐recognizing protein that specifically binds to DNA four‐way junction structures, could stimulate the Mus81–Mms4 endonuclease. The specific protein interaction between Mus81–Mms4 and Crp1 was responsible for the stimulation observed. Multicopy expression of Crp1 could partially rescue the sensitivity to DNA‐damaging agents of the sgs1∆mus81∆21‐24N mutant. Our results provide insight into the functional role and interaction of Crp1 with other proteins involved in DNA repair. [ABSTRACT FROM AUTHOR]

Published

2020

16. The possible function of Flp1 in homologous recombination repair in Saccharomyces cerevisiae

Author

Huong Thi Thu Phung, Hoa Luong Hieu Nguyen, and Dung Hoang Nguyen

Subjects

Flp1, genetic screening, homologous recombination repair, Mus81, Sgs1, Genetics, QH426-470

Abstract

Saccharomyces cerevisiae Mus81 is a structure-selective endonuclease which constitutes an alternative pathway in parallel with the helicase-topoisomerase Sgs1-Top3-Rmi1 complex to resolve a number of DNA intermediates during DNA replication, repair, and homologous recombination. Previously, it was showed that the N-terminal region of Mus81 was required for its in vivo function in a redundant manner with Sgs1; mus81Δ120N mutant that lacks the first 120 amino acid residues at the N-terminus exhibited synthetic lethality in combination with the loss of SGS1. In this study, the physiologically important role of the N-terminal region of Mus81 in processing toxic intermediates was further investigated. We examined the cellular defect of sgs1Δmus81Δ100N cells and observed that although viable, the cells became very sensitive to DNA damaging agents. A single-copy suppressor screening to seek for a factor(s) that could rescue the drug sensitivity of sgs1Δmus81Δ100N cells was performed and revealed that Flp1, a site-specific recombinase 1 encoded on the 2-micron plasmid was a suppressor. Moreover, Flp1 overexpression could partially suppress the drug sensitivity of mus81Δ cells at 37 °C. Our findings suggest a possible function of Flp1 in coordination with Mus81 and Sgs1 to jointly resolve the branched-DNA structures generated in cells attempting to repair DNA damages.

Published

2018

17. Homologous recombination and Mus81 promote replication completion in response to replication fork blockage.

Author

Pardo, Benjamin, Moriel‐Carretero, María, Vicat, Thibaud, Aguilera, Andrés, and Pasero, Philippe

Abstract

Impediments to DNA replication threaten genome stability. The homologous recombination (HR) pathway has been involved in the restart of blocked replication forks. Here, we used a method to increase yeast cell permeability in order to study at the molecular level the fate of replication forks blocked by DNA topoisomerase I poisoning by camptothecin (CPT). Our results indicate that Rad52 and Rad51 HR factors are required to complete DNA replication in response to CPT. Recombination events occurring during S phase do not generally lead to the restart of DNA synthesis but rather protect blocked forks until they merge with convergent forks. This fusion generates structures requiring their resolution by the Mus81 endonuclease in G2/M. At the global genome level, the multiplicity of replication origins in eukaryotic genomes and the fork protection mechanism provided by HR appear therefore to be essential to complete DNA replication in response to fork blockage. Synopsis: Camptothecin induces replication fork blockage. Homologous recombination is required to protect blocked forks until they merge with convergent forks. This fusion generates structures requiring their resolution by the Mus81 endonuclease in G2/M. Rad52 and Rad51 recombination factors are required to complete DNA replication in response to CPT‐induced DNA damage by protecting blocked forks.Recombination events induced by CPT during S phase do not globally lead to the restart of DNA synthesis by Pol32‐dependent BIR.Mus81 endonuclease is essential to promote the termination of blocked replication forks. [ABSTRACT FROM AUTHOR]

Published

2020

18. The Cdc14 Phosphatase Controls Resolution of Recombination Intermediates and Crossover Formation during Meiosis

Author

Paula Alonso-Ramos, David Álvarez-Melo, Katerina Strouhalova, Carolina Pascual-Silva, George B. Garside, Meret Arter, Teresa Bermejo, Rokas Grigaitis, Rahel Wettstein, Marta Fernández-Díaz, Joao Matos, Marco Geymonat, Pedro A. San-Segundo, and Jesús A. Carballo

Subjects

Cdc14, Yen1, Sgs1, Mus81, CDK1, Ndt80, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Meiotic defects derived from incorrect DNA repair during gametogenesis can lead to mutations, aneuploidies and infertility. The coordinated resolution of meiotic recombination intermediates is required for crossover formation, ultimately necessary for the accurate completion of both rounds of chromosome segregation. Numerous master kinases orchestrate the correct assembly and activity of the repair machinery. Although much less is known, the reversal of phosphorylation events in meiosis must also be key to coordinate the timing and functionality of repair enzymes. Cdc14 is a crucial phosphatase required for the dephosphorylation of multiple CDK1 targets in many eukaryotes. Mutations that inactivate this phosphatase lead to meiotic failure, but until now it was unknown if Cdc14 plays a direct role in meiotic recombination. Here, we show that the elimination of Cdc14 leads to severe defects in the processing and resolution of recombination intermediates, causing a drastic depletion in crossovers when other repair pathways are compromised. We also show that Cdc14 is required for the correct activity and localization of the Holliday Junction resolvase Yen1/GEN1. We reveal that Cdc14 regulates Yen1 activity from meiosis I onwards, and this function is essential for crossover resolution in the absence of other repair pathways. We also demonstrate that Cdc14 and Yen1 are required to safeguard sister chromatid segregation during the second meiotic division, a late action that is independent of the earlier role in crossover formation. Thus, this work uncovers previously undescribed functions of the evolutionary conserved Cdc14 phosphatase in the regulation of meiotic recombination.

Published

2021

19. MUS81 Participates in the Progression of Serous Ovarian Cancer Associated With Dysfunctional DNA Repair System

Author

Renquan Lu, Suhong Xie, Yanchun Wang, Hui Zheng, Hongqin Zhang, Minjie Deng, Weizhong Shi, Ailing Zhong, Miaomiao Chen, Meiqin Zhang, Xiaofeng Xu, Masood A. Shammas, and Lin Guo

Subjects

ovarian cancer, MUS81, DNA damage, homologous recombination (HR), chemotherapy, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Objective: Methyl methanesulfonate ultraviolet sensitive gene clone 81 (MUS81) is a structure-specific endonuclease that plays a pivotal role in the DNA repair system of cancer cells. In this study, we aim to elucidate the potential association between the dysfunction of MUS81 and the progression of Serous Ovarian Cancer (SOC).Methods: To investigate the association between MUS81 and prognosis of SOC, immunohistochemistry technology and qPCR were used to analyze the level of MUS81 expression, and transcriptional profile analysis and protein interaction screening chip were used to explore the MUS81 related signal pathways. Random amplified polymorphic DNA (RAPD) analysis, immunofluorescence and comet assays were further performed to evaluate genomic instability and DNA damage status of transduced SOC cells. Experiments both in vitro and in vivo were conducted to verify the impact of MUS81 silencing on chemotherapeutic drug sensitivity of SOC.Results: The overexpression of MUS81 in SOC tissues was related to poor clinical outcomes. The transcriptional chip data showed that MUS81 was involved in multiple pathways associated with DNA repair. Deficiency of MUS81 intensified the genome instability of SOC cells, promoted the emergence of DSBs and restrained the formation of RAD51 foci in SOC cells with exposure to UV. Furthermore, downregulation of MUS81 enhanced the sensitivity to Camptothecin and Olaparib in SOC cell lines and xenograft model.Conclusions: MUS81 is involved in the progression of SOC and inhibition of MUS81 could augment the susceptibility to chemotherapeutic agents. MUS81 might represent a novel molecular target for SOC chemotherapy.

Published

2019

20. SIN3A histone deacetylase action counteracts MUS81 to promote stalled fork stability.

Author

Muñoz S, Barroso S, Badra-Fajardo N, Marqueta-Gracia JJ, García-Rubio ML, Ubieto-Capella P, Méndez J, and Aguilera A

Subjects

Acetylation, Protein Processing, Post-Translational, DNA, Chromatin, Cell Cycle Proteins

Abstract

During genome duplication, replication forks (RFs) can be stalled by different obstacles or by depletion of replication factors or nucleotides. A limited number of histone post-translational modifications at stalled RFs are involved in RF protection and restart. Provided the recent observation that the SIN3A histone deacetylase complex reduces transcription-replication conflicts, we explore the role of the SIN3A complex in protecting RFs under stressed conditions. We observe that Sin3A protein is enriched at replicating DNA in the presence of hydroxyurea. In this situation, Sin3A-depleted cells show increased RF stalling, H3 acetylation, and DNA breaks at stalled RFs. Under Sin3A depletion, RF recovery is impaired, and DNA damage accumulates. Importantly, these effects are partially dependent on the MUS81 endonuclease, which promotes DNA breaks and MRE11-dependent DNA degradation of such breaks. We propose that chromatin deacetylation triggered by the SIN3A complex limits MUS81 cleavage of stalled RFs, promoting genome stability when DNA replication is challenged., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2024 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2024

21. MUS81 Participates in the Progression of Serous Ovarian Cancer Associated With Dysfunctional DNA Repair System.

Author

Lu, Renquan, Xie, Suhong, Wang, Yanchun, Zheng, Hui, Zhang, Hongqin, Deng, Minjie, Shi, Weizhong, Zhong, Ailing, Chen, Miaomiao, Zhang, Meiqin, Xu, Xiaofeng, Shammas, Masood A., and Guo, Lin

Subjects

DNA repair, OVARIAN cancer, ENDONUCLEASES, MOLECULAR cloning, METHYL methanesulfonate, DNA damage

Abstract

Objective: Methyl methanesulfonate ultraviolet sensitive gene clone 81 (MUS81) is a structure-specific endonuclease that plays a pivotal role in the DNA repair system of cancer cells. In this study, we aim to elucidate the potential association between the dysfunction of MUS81 and the progression of Serous Ovarian Cancer (SOC). Methods: To investigate the association between MUS81 and prognosis of SOC, immunohistochemistry technology and qPCR were used to analyze the level of MUS81 expression, and transcriptional profile analysis and protein interaction screening chip were used to explore the MUS81 related signal pathways. Random amplified polymorphic DNA (RAPD) analysis, immunofluorescence and comet assays were further performed to evaluate genomic instability and DNA damage status of transduced SOC cells. Experiments both in vitro and in vivo were conducted to verify the impact of MUS81 silencing on chemotherapeutic drug sensitivity of SOC. Results: The overexpression of MUS81 in SOC tissues was related to poor clinical outcomes. The transcriptional chip data showed that MUS81 was involved in multiple pathways associated with DNA repair. Deficiency of MUS81 intensified the genome instability of SOC cells, promoted the emergence of DSBs and restrained the formation of RAD51 foci in SOC cells with exposure to UV. Furthermore, downregulation of MUS81 enhanced the sensitivity to Camptothecin and Olaparib in SOC cell lines and xenograft model. Conclusions: MUS81 is involved in the progression of SOC and inhibition of MUS81 could augment the susceptibility to chemotherapeutic agents. MUS81 might represent a novel molecular target for SOC chemotherapy. [ABSTRACT FROM AUTHOR]

Published

2019

22. Meiotic Nuclear Oscillations Are Necessary to Avoid Excessive Chromosome Associations

Author

Mariola R. Chacón, Petrina Delivani, and Iva M. Tolić

Subjects

meiosis, meiotic prophase, chromosome pairing, recombination, double-strand breaks, chromosome missegregation, nuclear oscillations, horsetail movement, Rec25, Mus81, Biology (General), QH301-705.5

Abstract

Pairing of homologous chromosomes is a crucial step in meiosis, which in fission yeast depends on nuclear oscillations. However, how nuclear oscillations help pairing is unknown. Here, we show that homologous loci typically pair when the spindle pole body is at the cell pole and the nucleus is elongated, whereas they unpair when the spindle pole body is in the cell center and the nucleus is round. Inhibition of oscillations demonstrated that movement is required for initial pairing and that prolonged association of loci leads to mis-segregation. The double-strand break marker Rec25 accumulates in elongated nuclei, indicating that prolonged chromosome stretching triggers recombinatory pathways leading to mis-segregation. Mis-segregation is rescued by overexpression of the Holliday junction resolvase Mus81, suggesting that prolonged pairing results in irresolvable recombination intermediates. We conclude that nuclear oscillations exhibit a dual role, promoting initial pairing and restricting the time of chromosome associations to ensure proper segregation.

Published

2016

23. The Control of the Crossover Localization in Allium

Author

Natalia Kudryavtseva, Aleksey Ermolaev, Anton Pivovarov, Sergey Simanovsky, Sergey Odintsov, and Ludmila Khrustaleva

Subjects

Inorganic Chemistry, chiasmata localization, MUS81, MLH1, ASY1, ZYP1, Allium, GISH, Organic Chemistry, genetics, General Medicine, Physical and Theoretical Chemistry, Molecular Biology, Spectroscopy, Catalysis, Computer Science Applications

Abstract

Meiotic crossovers/chiasmata are not randomly distributed and strictly controlled. The mechanisms behind COs patterning remain largely unknown. In many species COs predominantly occur in the distal 2/3 of the chromosome arm and suppression of COs is observed in the proximal regions. The exceptions are some species, among which Allium fistulosum has strictly localized COs in the proximal region. The ability to manipulate the COs localization can be useful for onion breeding. We investigated the factors that may contribute to the pattern of COs in two closely related onion species A. cepa and A. fistulosum, which differ significantly in the localization of chiasmata, and their F1 diploid and triploid hybrids in pollen mother cells. We demonstrate a significant shift in the COs localization to the distal and interstitial region in F1 triploid hybrid, which has a complete diploid set of A. fistulosum chromosomes and haploid set of A. cepa chromosomes. This observation points to a possible genetic control of COs distribution. We did not find the differences in the assembly and disassembly of ASY1 and ZYP1 between A. cepa and A. fistulosum while the difference between parental species and their hybrids was observed. In diploid F1 hybrids at pachytene the chromosome pairing delay marked by ASY1 was revealed. Immunolocalization of MLH1, a marker for class I of the interference-dependent COs, and MUS81, a marker for class II of the interference-free COs, and mlh1/mus81 gene expression profiling in different stages of meiosis showed a spatiotemporal asymmetry among A. cepa, A. fistulosum and their diploid and triploid F1 hybrids. Our results support the hypothesis of genetic control of CO distribution as one of the players that affect meiotic recombination and exchange of genomic material.

Published

2022

24. A new class of ultrafine anaphase bridges generated by homologous recombination.

Author

Chan, Ying Wai and West, Stephen C.

Abstract

Ultrafine anaphase bridges (UFBs) are a potential source of genome instability that is a hallmark of cancer. UFBs can arise from DNA catenanes at centromeres/rDNA loci, late replication intermediates induced by replication stress, and DNA linkages at telomeres. Recently, it was reported that DNA intertwinements generated by homologous recombination give rise to a new class of UFBs, which have been termed homologous recombination ultrafine bridges (HR-UFBs). HR-UFBs are decorated with PICH and BLM in anaphase, and are subsequently converted to RPA-coated, single-stranded DNA bridges. Breakage of these sister chromatid entanglements leads to DNA damage that can be repaired by non-homologous end joining in the next cell cycle, but the potential consequences include DNA rearrangements, chromosome translocations and fusions. Visualisation of these HR-UFBs, and knowledge of how they arise, provides a molecular basis to explain how upregulation of homologous recombination or failure to resolve recombination intermediates leads to the development of chromosomal instability observed in certain cancers. [ABSTRACT FROM AUTHOR]

Published

2018

25. The possible function of Flp1 in homologous recombination repair in Saccharomyces cerevisiae.

Author

Phung, Huong Thi Thu, Nguyen, Hoa Luong Hieu, and Nguyen, Dung Hoang

Subjects

*SACCHAROMYCES cerevisiae, *HOMOLOGY (Biology), *HOMOLOGOUS recombination, *FUNGI

Abstract

Saccharomyces cerevisiae Mus81 is a structure-selective endonuclease which constitutes an alternative pathway in parallel with the helicase-topoisomerase Sgs1-Top3-Rmi1 complex to resolve a number of DNA intermediates during DNA replication, repair, and homologous recombination. Previously, it was showed that the N-terminal region of Mus81 was required for its in vivo function in a redundant manner with Sgs1; mus81Δ120N mutant that lacks the first 120 amino acid residues at the N-terminus exhibited synthetic lethality in combination with the loss of SGS1. In this study, the physiologically important role of the N-terminal region of Mus81 in processing toxic intermediates was further investigated. We examined the cellular defect of sgs1Δmus81Δ100N cells and observed that although viable, the cells became very sensitive to DNA damaging agents. A single-copy suppressor screening to seek for a factor(s) that could rescue the drug sensitivity of sgs1Δmus81Δ100N cells was performed and revealed that Flp1, a site-specific recombinase 1 encoded on the 2-micron plasmid was a suppressor. Moreover, Flp1 overexpression could partially suppress the drug sensitivity of mus81Δ cells at 37 °C. Our findings suggest a possible function of Flp1 in coordination with Mus81 and Sgs1 to jointly resolve the branched-DNA structures generated in cells attempting to repair DNA damages. [ABSTRACT FROM AUTHOR]

Published

2018

26. Genetic dissection of crossover mutants defines discrete intermediates in mouse meiosis.

Author

Premkumar, Tolkappiyan, Paniker, Lakshmi, Kang, Rhea, Biot, Mathilde, Humphrey, Ericka, Destain, Honorine, Ferranti, Isabella, Okulate, Iyinyeoluwa, Nguyen, Holly, Kilaru, Vindhya, Frasca, Melissa, Chakraborty, Parijat, and Cole, Francesca

Subjects

*MEIOSIS, *HOLLIDAY junctions, *CHROMOSOME segregation, *MICE, *DISSECTION

Abstract

Crossovers (COs), the exchange of homolog arms, are required for accurate chromosome segregation during meiosis. Studies in yeast have described the single-end invasion (SEI) intermediate: a stabilized 3′ end annealed with the homolog as the first detectible CO precursor. SEIs are thought to differentiate into double Holliday junctions (dHJs) that are resolved by MutLgamma (MLH1/MLH3) into COs. Currently, we lack knowledge of early steps of mammalian CO recombination or how intermediates are differentiated in any organism. Using comprehensive analysis of recombination in thirteen different genetic conditions with varying levels of compromised CO resolution, we infer CO precursors include asymmetric SEI-like intermediates and dHJs in mouse. In contrast to yeast, MLH3 is structurally required to differentiate CO precursors into dHJs. We verify conservation of aspects of meiotic recombination and show unique features in mouse, providing mechanistic insight into CO formation. [Display omitted] • Dissection of recombination in mouse spermatocytes defective for crossing over • EXO1 promotes MutLgamma endonuclease activity but is not fully required • Formation of single-end invasion-like and double Holliday junction intermediates • MLH3 plays a structural role to promote double Holliday junction formation Accurate chromosome segregation in meiosis requires crossovers, but we lack an understanding of how they form in mammals. Premkumar et al. dissect recombination in multiple crossover mutants to show unique and conserved mechanisms in mice. They find two distinct precursors and show that MLH3 is structurally required to form double Holliday junctions. [ABSTRACT FROM AUTHOR]

Published

2023

27. 53BP1 and BRCA1 control pathway choice for stalled replication restart

Author

Yixi Xu, Shaokai Ning, Zheng Wei, Ran Xu, Xinlin Xu, Mengtan Xing, Rong Guo, and Dongyi Xu

Subjects

BRCA1, 53BP1, RIF1, replication stress, stalled replication fork restart, MUS81, Medicine, Science, Biology (General), QH301-705.5

Abstract

The cellular pathways that restart stalled replication forks are essential for genome stability and tumor prevention. However, how many of these pathways exist in cells and how these pathways are selectively activated remain unclear. Here, we describe two major fork restart pathways, and demonstrate that their selection is governed by 53BP1 and BRCA1, which are known to control the pathway choice to repair double-strand DNA breaks (DSBs). Specifically, 53BP1 promotes a fork cleavage-free pathway, whereas BRCA1 facilitates a break-induced replication (BIR) pathway coupled with SLX-MUS complex-mediated fork cleavage. The defect in the first pathway, but not DSB repair, in a 53BP1 mutant is largely corrected by disrupting BRCA1, and vice versa. Moreover, PLK1 temporally regulates the switch of these two pathways through enhancing the assembly of the SLX-MUS complex. Our results reveal two distinct fork restart pathways, which are antagonistically controlled by 53BP1 and BRCA1 in a DSB repair-independent manner.

Published

2017

28. Inter-Fork Strand Annealing causes genomic deletions during the termination of DNA replication

Author

Carl A Morrow, Michael O Nguyen, Andrew Fower, Io Nam Wong, Fekret Osman, Claire Bryer, and Matthew C Whitby

Subjects

DNA replication, homologous recombination, Rad52, replication fork collapse, replication fork barrier, Mus81, Medicine, Science, Biology (General), QH301-705.5

Abstract

Problems that arise during DNA replication can drive genomic alterations that are instrumental in the development of cancers and many human genetic disorders. Replication fork barriers are a commonly encountered problem, which can cause fork collapse and act as hotspots for replication termination. Collapsed forks can be rescued by homologous recombination, which restarts replication. However, replication restart is relatively slow and, therefore, replication termination may frequently occur by an active fork converging on a collapsed fork. We find that this type of non-canonical fork convergence in fission yeast is prone to trigger deletions between repetitive DNA sequences via a mechanism we call Inter-Fork Strand Annealing (IFSA) that depends on the recombination proteins Rad52, Exo1 and Mus81, and is countered by the FANCM-related DNA helicase Fml1. Based on our findings, we propose that IFSA is a potential threat to genomic stability in eukaryotes.

Published

2017

29. Arsenic-induced sumoylation of Mus81 is involved in regulating genomic stability.

Author

Hu, Liyan, Yang, Feikun, Lu, Lou, and Dai, Wei

Abstract

Chronic environmental exposure to metal toxicants such as chromium and arsenic is closely related to the development of several types of common cancers. Genetic and epigenetic studies in the past decade reveal that post-translational modifications of histones play a role in metal carcinogenesis. However, exact molecular mechanisms of metal carcinogenesis remain to be elucidated. In this study we found that As2O3, an environmental metal toxicant, upregulated overall modifications of many cellular proteins by SUMO2/3. Sumoylated proteins from arsenic-treated cells constitutively expressing His6-SUMO2 were pulled down by Ni-IDA resin under denaturing conditions. Mass spectrometric analysis revealed over 100 proteins that were potentially modified by sumoylation. Mus81, a DNA endonuclease involved in homologous recombination repair, was among the identified proteins whose sumoylation was increased after treatment with As2O3.We further showed that K10 and K524 were 2 lysine residues essential for Mus81 sumoylation. Moreover, we demonstrated that Mus81 sumoylation is important for normal mitotic chromosome congression and that cells expressing SUMO-resistant Mus81 mutants displayed compromised DNA damage responses after exposure to metal toxins such as Cr(VI) and arsenic. [ABSTRACT FROM PUBLISHER]

Published

2017

30. A Mechanism for Controlled Breakage of Under-replicated Chromosomes during Mitosis.

Author

Duda, Heike, Arter, Meret, Gloggnitzer, Jiradet, Teloni, Federico, Wild, Philipp, Blanco, Miguel G., Altmeyer, Matthias, and Matos, Joao

Subjects

*CHROMOSOME segregation, *MITOSIS, *DNA replication, *NUCLEASES, *KINASES

Abstract

Summary While DNA replication and mitosis occur in a sequential manner, precisely how cells maintain their temporal separation and order remains elusive. Here, we unveil a double-negative feedback loop between replication intermediates and an M-phase-specific structure-selective endonuclease, MUS81-SLX4, which renders DNA replication and mitosis mutually exclusive. MUS81 nuclease is constitutively active throughout the cell cycle but requires association with SLX4 for efficient substrate targeting. To preclude toxic processing of replicating chromosomes, WEE1 kinase restrains CDK1 and PLK1-mediated MUS81-SLX4 assembly during S phase. Accordingly, WEE1 inhibition triggers widespread nucleolytic breakage of replication intermediates, halting DNA replication and leading to chromosome pulverization. Unexpectedly, premature entry into mitosis—licensed by unrestrained CDK1 activity during S phase—requires MUS81-SLX4, which inhibits DNA replication. This suggests that ongoing replication assists WEE1 in delaying entry into M phase and, indirectly, in preventing MUS81-SLX4 assembly. Conversely, MUS81-SLX4 activation during mitosis promotes targeted resolution of persistent replication intermediates, which safeguards chromosome segregation. [ABSTRACT FROM AUTHOR]

Published

2016

31. Small-molecule inhibitors identify the RAD52-ssDNA interaction as critical for recovery from replication stress and for survival of BRCA2 deficient cells

Author

Sarah R Hengel, Eva Malacaria, Laura Folly da Silva Constantino, Fletcher E Bain, Andrea Diaz, Brandon G Koch, Liping Yu, Meng Wu, Pietro Pichierri, M Ashley Spies, and Maria Spies

Subjects

RAD52, high throughput screening, small-molecule inhibitors, BRCA2, MUS81, DNA repair, Medicine, Science, Biology (General), QH301-705.5

Abstract

The DNA repair protein RAD52 is an emerging therapeutic target of high importance for BRCA-deficient tumors. Depletion of RAD52 is synthetically lethal with defects in tumor suppressors BRCA1, BRCA2 and PALB2. RAD52 also participates in the recovery of the stalled replication forks. Anticipating that ssDNA binding activity underlies the RAD52 cellular functions, we carried out a high throughput screening campaign to identify compounds that disrupt the RAD52-ssDNA interaction. Lead compounds were confirmed as RAD52 inhibitors in biochemical assays. Computational analysis predicted that these inhibitors bind within the ssDNA-binding groove of the RAD52 oligomeric ring. The nature of the inhibitor-RAD52 complex was validated through an in silico screening campaign, culminating in the discovery of an additional RAD52 inhibitor. Cellular studies with our inhibitors showed that the RAD52-ssDNA interaction enables its function at stalled replication forks, and that the inhibition of RAD52-ssDNA binding acts additively with BRCA2 or MUS81 depletion in cell killing.

Published

2016

32. The cruciform DNA‐binding protein Crp1 stimulates the endonuclease activity of Mus81–Mms4 inSaccharomyces cerevisiae

Author

Huong Thi Thu Phung, Diem Hong Tran, and Ta Xuan Nguyen

Subjects

Saccharomyces cerevisiae Proteins, Flap Endonucleases, DNA repair, Saccharomyces cerevisiae, Mutant, Biophysics, Biochemistry, DNA-binding protein, 03 medical and health sciences, Endonuclease, chemistry.chemical_compound, Protein Domains, Structural Biology, Gene Expression Regulation, Fungal, Genetics, Molecular Biology, 030304 developmental biology, DNA, Cruciform, 0303 health sciences, RecQ Helicases, biology, 030302 biochemistry & molecular biology, Cell Biology, Endonucleases, biology.organism_classification, MUS81, Cell biology, DNA-Binding Proteins, Enzyme Activation, Kinetics, chemistry, Cruciform, Mutation, biology.protein, Nucleic Acid Conformation, DNA, Protein Binding

Abstract

The Saccharomyces cerevisiae Mus81-Mms4 complex is a highly conserved DNA structure-specific endonuclease that plays essential roles in the processing of recombination intermediates that arise during the repair of stalled replication forks and double-stranded breaks. To identify novel factors functioning conjointly with Mus81-Mms4, we performed a biochemical screen and found that Crp1, a cruciform DNA-recognizing protein that specifically binds to DNA four-way junction structures, could stimulate the Mus81-Mms4 endonuclease. The specific protein interaction between Mus81-Mms4 and Crp1 was responsible for the stimulation observed. Multicopy expression of Crp1 could partially rescue the sensitivity to DNA-damaging agents of the sgs1∆mus81∆21-24N mutant. Our results provide insight into the functional role and interaction of Crp1 with other proteins involved in DNA repair.

Published

2020

33. The repair of topoisomerase 2 cleavage complexes in Arabidopsis

Author

Holger Puchta, Leonie Hacker, Janina Enderle, and Annika Dorn

Subjects

Life sciences, biology, Nuclease, Mutation, Mutant, Cell Biology, Plant Science, Biology, medicine.disease_cause, biology.organism_classification, MUS81, Cell biology, Methyl methanesulfonate, Focus on Cell Biology, chemistry.chemical_compound, chemistry, Arabidopsis, ddc:570, biology.protein, medicine, CRISPR, DNA

Abstract

DNA–protein crosslinks (DPCs) and DNA double-stranded breaks (DSBs), including those produced by stalled topoisomerase 2 cleavage complexes (TOP2ccs), must be repaired to ensure genome stability. The basic mechanisms of TOP2cc repair have been characterized in other eukaryotes, but we lack information for plants. Using CRISPR/Cas-induced mutants, we show that Arabidopsis thaliana has two main TOP2cc repair pathways: one is defined by TYROSYL-DNA-PHOSPHODIESTERASE 2 (TDP2), which hydrolyzes TOP2–DNA linkages, the other by the DNA-dependent protease WSS1A (a homolog of human SPARTAN/yeast weak suppressor of smt3 [Wss1]), which also functions in DPC repair. TDP1 and TDP2 function nonredundantly in TOP1cc repair, indicating that they act specifically on their respective stalled cleavage complexes. The nuclease METHYL METHANESULFONATE AND UV-SENSITIVE PROTEIN 81 (MUS81) plays a major role in global DPC repair and a minor role in TOP2cc repair. DSBs arise as intermediates of TOP2cc repair and are repaired by classical and alternative nonhomologous end joining (NHEJ) pathways. Double-mutant analysis indicates that “clean” DNA ends caused by TDP2 hydrolysis are mainly religated by classical NHEJ, which helps avoid mutation. In contrast, the mutagenic alternative NHEJ pathway mainly processes nonligateable DNA ends. Thus, TDP2 promotes maintenance of plant genome integrity by error-free repair of TOP2cc.

Published

2022

34. The alternative lengthening of telomeres mechanism jeopardizes telomere integrity if not properly restricted

Author

Silva, Bruno, Arora, Rajika, Azzalin, Claus Maria, and Repositório da Universidade de Lisboa

Subjects

Multidisciplinary, Humans, RNA, Long Noncoding, TERRA, Mus81, DNA, Telomere, Endonucleases, Telomerase, alternative lengthening of telomeres, telomere transcription

Abstract

A substantial number of human cancers are telomerase-negative and elongate physiologically damaged telomeres through a break-induced replication (BIR)-based mechanism known as alternative lengthening of telomeres (ALT). We recently demonstrated that inhibiting the transcription of the telomeric long noncoding RNA TERRA suppresses telomere damage and ALT features, indicating that telomere transcription is a main trigger of ALT activity. Here we show that experimentally increased TERRA transcription not only increases ALT features, as expected, but also causes rapid loss of telomeric DNA through a pathway that requires the endonuclease Mus81. Our data indicate that the ALT mechanism can endanger telomere integrity if not properly controlled and point to TERRA transcription as a uniquely versatile target for therapy., Proceedings of the National Academy of Sciences of the United States of America, 119 (39), ISSN:0027-8424, ISSN:1091-6490

Published

2022

35. Effect of GEN1 interference on the chemosensitivity of the breast cancer MCF-7 and SKBR3 cell lines.

Author

YUNLU WU, YING QIAN, GUOZHONG ZHOU, JUAN LV, QIUYUE YAN, and XUEJUN DONG

Subjects

*GENETICS of breast cancer, *CHEMORECEPTORS, *HOLLIDAY junctions, *FLUOROURACIL, *CANCER cells, *GENE expression, *REVERSE transcriptase polymerase chain reaction, BREAST cancer chemotherapy

Abstract

Chemotherapy is a notable method for the treatment of breast cancer. Numerous genes associated with the sensitivity of cancer to chemotherapy have been found. In recent years, evidence has suggested that a particular structure termed Holliday junction (HJ) plays a crucial role in cancer chemosensitivity. Targeting HJ resolvases, such as structure-specific endonuclease subunit SLX4 (Slx4) and MUS81 structure-specific endonuclease subunit (Mus81), significantly increases the chemosensitivity of tumor cells. Flap endonuclease GEN homolog 1 (GEN1) is a HJ resolvase that belongs to the Rad2/xeroderma pigmentosum complementation group G nuclease family. Whether GEN1 affects the chemosensitivity of tumor cells in a similar manner to Slx4 and Mus81 remains unknown. The aim of the present study was to determine the effect of GEN1 interference on the chemosensitivity of breast cancer cell lines. The investigation of the function of GEN1 was performed using MCF-7 and SKBR3 cells. Short hairpin RNA was used to suppress the expression of GEN1, and western blot analysis and reverse transcription-quantitative polymerase chain reaction were used to detect gene expression. In addition, a cell counting kit-8 assay was performed to detect the viability of cells and flow cytometry was performed to test apoptosis levels. Suppression of GEN1 in SKBR3 cells effectively increased the sensitivity to the chemotherapeutic drug 5-fluorouracil (5-FU), while MCF-7 cells showed no significant change in sensitivity following GEN1 suppression. However, when GEN1 was targeted in addition to Mus81, the MCF-7 cells also demonstrated a significantly increased sensitivity to 5-FU. In addition, when the level of Mus81 was low, GEN1 expression was increased under a low concentration of 5-FU. The present results suggest that GEN1 may play different roles in different breast cancer cell lines. The function of GEN1 may be affected by the level of Mus81 in the cell line. In addition, GEN1 interference may improve the sensitivity to chemotherapy induced by targeting Mus81 alone. [ABSTRACT FROM AUTHOR]

Published

2016

36. Mus81 knockdown improves chemosensitivity of hepatocellular carcinoma cells by inducing S-phase arrest and promoting apoptosis through CHK1 pathway.

Author

Wu, Fan, Chen, Wei‐Jia, Yan, Lun, Tan, Guo‐Qian, Li, Wei‐Tao, Zhu, Xuan‐Jin, Ge, Xiao‐Chuan, Liu, Jian‐Wei, and Wang, Bai‐Lin

Subjects

*CANCER cells, *LIVER cancer, *LIVER metastasis, *FIBROLAMELLAR hepatocellular carcinoma, *MITOMYCIN C, *FLUOROURACIL

Abstract

As a critical endonuclease in DNA repair, Mus81 is traditionally regarded as a tumor suppressor, but recently correlated with the sensitivity of mitomycin C and 5-fluorouracil in colon cancer and breast cancer cells. However, its role in chemosensitivity of other human malignancies still remains unknown. This study therefore aims to investigate the effects of Mus81 knockdown on the chemosensitivity of hepatocellular carcinoma ( HCC), a usually chemorefractory tumor, and explore the underlying mechanisms. Mus81 expression in HepG2 and Bel-7402 HCC cell lines was depleted by lentivirus-mediated short hairpin RNA and the elevated sensitivity of these Mus81-inhibited HCC cells to therapeutic agents, especially to epirubicin ( EPI), was evidenced by MTT assay and an HCC chemotherapy mouse model. Flow cytometric analysis also showed that Mus81 knockdown lead to an obvious S-phase arrest and an elevated apoptosis in EPI-treated HepG2 and Bel-7402 cells, which could be rescued by CHK1 inhibition. The activation of CHK1/ CDC25A/ CDK2 pathway was also demonstrated in Mus81-inhibited HepG2 cells and xenograft mouse tumors under EPI treatment. Meanwhile, the apoptosis of HepG2 cells in response to EPI was remarkably promoted by Mus81 knockdown through activating p53/Bax/Caspase-3 pathway under the controlling of CHK1. In addition, CHK2 inhibition slightly raised CHK1 activity, thereby enhancing the S-phase arrest and apoptosis induced by EPI in Mus81-suppressed HCC cells. In conclusion, Mus81 knockdown improves the chemosensitivity of HCC cells by inducing S-phase arrest and promoting apoptosis through CHK1 pathway, suggesting Mus81 as a novel therapeutic target for HCC. [ABSTRACT FROM AUTHOR]

Published

2016

37. The Cdc14 Phosphatase Controls Resolution of Recombination Intermediates and Crossover Formation during Meiosis

Author

Agencia Estatal de Investigación (España), Junta de Castilla y León, Federal Institute of Technology Zurich, Swiss National Science Foundation, Alonso-Ramos, Paula, Álvarez-Melo, David, Strouhalova, Katerina, Pascual-Silva, Carolina, Garside, George B., Arter, Meret, Bermejo, Teresa, Grigaitis, Rokas, Wettstein, Rahel, Fernández-Díaz, Marta, Matos, Joao, Geymonat, Marco, San-Segundo, Pedro A., Carballo, Jesús A., Agencia Estatal de Investigación (España), Junta de Castilla y León, Federal Institute of Technology Zurich, Swiss National Science Foundation, Alonso-Ramos, Paula, Álvarez-Melo, David, Strouhalova, Katerina, Pascual-Silva, Carolina, Garside, George B., Arter, Meret, Bermejo, Teresa, Grigaitis, Rokas, Wettstein, Rahel, Fernández-Díaz, Marta, Matos, Joao, Geymonat, Marco, San-Segundo, Pedro A., and Carballo, Jesús A.

Abstract

Meiotic defects derived from incorrect DNA repair during gametogenesis can lead to mutations, aneuploidies and infertility. The coordinated resolution of meiotic recombination intermediates is required for crossover formation, ultimately necessary for the accurate completion of both rounds of chromosome segregation. Numerous master kinases orchestrate the correct assembly and activity of the repair machinery. Although much less is known, the reversal of phosphorylation events in meiosis must also be key to coordinate the timing and functionality of repair enzymes. Cdc14 is a crucial phosphatase required for the dephosphorylation of multiple CDK1 targets in many eukaryotes. Mutations that inactivate this phosphatase lead to meiotic failure, but until now it was unknown if Cdc14 plays a direct role in meiotic recombination. Here, we show that the elimination of Cdc14 leads to severe defects in the processing and resolution of recombination intermediates, causing a drastic depletion in crossovers when other repair pathways are compromised. We also show that Cdc14 is required for the correct activity and localization of the Holliday Junction resolvase Yen1/GEN1. We reveal that Cdc14 regulates Yen1 activity from meiosis I onwards, and this function is essential for crossover resolution in the absence of other repair pathways. We also demonstrate that Cdc14 and Yen1 are required to safeguard sister chromatid segregation during the second meiotic division, a late action that is independent of the earlier role in crossover formation. Thus, this work uncovers previously undescribed functions of the evolutionary conserved Cdc14 phosphatase in the regulation of meiotic recombination.

Published

2021

38. Valproic Acid Regulates HR and Cell Cycle Through MUS81-pRPA2 Pathway in Response to Hydroxyurea

Author

Chenxia Ding, Zhihui Feng, Fengmei Zhang, Benyu Su, Zuchao Cai, Guochao Liu, Zhujun Tian, David Lim, and Chen Chen

Subjects

Cancer Research, breast cancer, HU, HR, medicine, RC254-282, Sensitization, Original Research, Tumor microenvironment, Valproic Acid, biology, Chemistry, Kinase, pRPA2, MUS81, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Cell cycle, Replication protein A2, Wee1, medicine.anatomical_structure, Oncology, Cancer research, biology.protein, Phosphorylation, cell cycle, lipids (amino acids, peptides, and proteins), VPA, medicine.drug

Abstract

Breast cancer is the primary problem threatening women’s health. The combined application of valproic acid (VPA) and hydroxyurea (HU) has a synergistic effect on killing breast cancer cells, but the molecular mechanism remains elusive. Replication protein A2 phosphorylation (pRPA2), is essential for homologous recombination (HR) repair and cell cycle. Here we showed that in response to HU, the VPA significantly decreased the tumor cells survival, and promoted S-phase slippage, which was associated with the decrease of pCHK1 and WEE1/pCDK1-mediated checkpoint kinases phosphorylation pathway and inhibited pRPA2/Rad51-mediated HR repair pathway; the mutation of pRPA2 significantly diminished the above effect, indicating that VPA-caused HU sensitization was pRPA2 dependent. It was further found that VPA and HU combination treatment also resulted in the decrease of endonuclease MUS81. After MUS81 elimination, not only the level of pRPA2 was abolished in response to HU treatment, but also VPA-caused HU sensitization was significantly down-regulated through pRPA2-mediated checkpoint kinases phosphorylation and HR repair pathways. In addition, the VPA altered the tumor microenvironment and reduced tumor burden by recruiting macrophages to tumor sites; the Kaplan-Meier analysis showed that patients with high pRPA2 expression had significantly worse survival. Overall, our findings demonstrated that VPA influences HR repair and cell cycle through down-regulating MUS81-pRPA2 pathway in response to HU treatment.

Published

2021

39. Inhibition of MUS81 by siRNA Reverses Resistance to Cisplatin in Human Ovarian Cancer Cell Lines

Author

Christopher N. Parris, Helen A. Foster, Hussein Al-Ali, Emma C. Bourton, Sheba Adam-Zahir, and Piers N. Plowman

Subjects

Cisplatin, Chemistry, Cell culture, medicine, Cancer research, Ovarian cancer, medicine.disease, MUS81, medicine.drug

Abstract

Bacground: Drugs that induce DNA interstrand crosslinks form the mainstay of anticancer treatments for different cancers. These drugs are used to treat ovarian cancer which is the most prevalent gynaecological cancer. Five-year survival rates are approximately 40% and the development of drug resistant disease is an important factor in treatment failure. Methods: In this study a comprehensive evaluation of the expression and function of the site-specific endonuclease MUS81 was conducted. Using quantitative real time PCR analysis and imaging flow cytometry we determined the mRNA and protein expression of MUS81 in three ovarian cancer cell lines and two immortalised human fibroblast cell lines which had been made resistant to cisplatin by chronic exposure. siRNA knockdown of MUS81 was employed to determine the effect on overall cell survival which was assessed using clonogenic assays. Results: In the five cisplatin-resistant cell lines we observed increased MUS81 mRNA expression. In addition MUS81 protein expression in the form of discrete nuclear foci in cells was observed in all cell lines following cisplatin exposure, there being significantly more foci in cisplatin resistant cell lines. siRNA knockdown of MUS81 significantly reduced both mRNA and protein levels in two cell lines (SK-OV-3 and MRC5-SV1 – wild-type and resistant) and critically re-sensitised cisplatin resistant cells to wild-type level, determined by clonogenic assay.Conclusion: MUS81 is central to the development of cisplatin resistance in ovarian cancer cell lines. Inhibition of MUS81 restored drug sensitivity to the cells. MUS81 may be a useful therapeutic target to overcome drug resistance in ovarian and other cancers.

Published

2021

40. Human MUS81: A Fence-Sitter in Cancer

Author

Sisi Chen, Xinwei Geng, Madiha Zahra Syeda, Zhengming Huang, Chao Zhang, and Songmin Ying

Subjects

chromosomal instability, DNA repair, Review, Gene mutation, Biology, DNA damage response, endonuclease, chemistry.chemical_compound, Endonuclease, Cell and Developmental Biology, Chromosome instability, medicine, Viability assay, human MUS81, lcsh:QH301-705.5, Cancer, Cell Biology, medicine.disease, MUS81, chemistry, lcsh:Biology (General), biology.protein, Cancer research, cancer therapy, DNA, Developmental Biology

Abstract

MUS81 complex, exhibiting endonuclease activity on specific DNA structures, plays an influential part in DNA repair. Research has proved that MUS81 is dispensable for embryonic development and cell viability in mammals. However, an intricate picture has emerged from studies in which discrepant gene mutations completely alter the role of MUS81 in human cancers. Here, we review the recent understanding of how MUS81 functions in tumors with distinct genetic backgrounds and discuss the potential therapeutic strategies targeting MUS81 in cancer.

Published

2021

41. Determinants for degradation of SAMHD1, Mus81 and induction of G2 arrest in HIV-1 Vpr and SIVagm Vpr.

Author

DePaula-Silva, Ana Beatriz, Cassiday, Patrick A., Chumley, Jeffrey, Bosque, Alberto, Monteiro-Filho, Carlos M.R., Mahon, Cathal S., Cone, Kelsey R., Krogan, Nevan, Elde, Nels C., and Planelles, Vicente

Subjects

*HIV, *BIODEGRADATION, *UBIQUITINATION, *LENTIVIRUSES, *AMINO acids, *MUTANT proteins

Abstract

Vpr and Vpx are a group of highly related accessory proteins from primate lentiviruses. Despite the high degree of amino acid homology within this group, these proteins can be highly divergent in their functions. In this work, we constructed chimeric and mutant proteins between HIV-1 and SIVagm Vpr in order to better understand the structure–function relationships. We tested these constructs for their abilities to induce G 2 arrest in human cells and to degrade agmSAMHD1 and Mus81. We found that the C-terminus of HIV-1 Vpr, when transferred onto SIVagm Vpr, provides the latter with the de novo ability to induce G 2 arrest in human cells. We confirmed that HIV-1 Vpr induces degradation of Mus81 although, surprisingly, degradation is independent and genetically separable from Vpr׳s ability to induce G 2 arrest. [ABSTRACT FROM AUTHOR]

Published

2015

42. Homologous recombination and Mus81 promote replication completion in response to replication fork blockage

Author

Universidad de Sevilla. Departamento de Genética, Pardo, Benjamín, Moriel Carretero, María, Vicat, Thibaud, Aguilera López, Andrés, Pasero, Philippe, Universidad de Sevilla. Departamento de Genética, Pardo, Benjamín, Moriel Carretero, María, Vicat, Thibaud, Aguilera López, Andrés, and Pasero, Philippe

Abstract

Impediments to DNA replication threaten genome stability. The homologous recombination (HR) pathway has been involved in the restart of blocked replication forks. Here, we used a method to increase yeast cell permeability in order to study at the molecular level the fate of replication forks blocked by DNA topoisomerase I poisoning by camptothecin (CPT). Our results indicate that Rad52 and Rad51 HR factors are required to complete DNA replication in response to CPT. Recombination events occurring during S phase do not generally lead to the restart of DNA synthesis but rather protect blocked forks until they merge with convergent forks. This fusion generates structures requiring their resolution by the Mus81 endonuclease in G2/M. At the global genome level, the multiplicity of replication origins in eukaryotic genomes and the fork protection mechanism provided by HR appear therefore to be essential to complete DNA replication in response to fork blockage.

Published

2020

43. Homologous recombination and Mus81 promote replication completion in response to replication fork blockage

Author

Agence Nationale de la Recherche (France), Ligue Nationale contre le Cancer (France), Institut National du Cancer (France), Ministerio de Economía y Competitividad (España), Junta de Andalucía, Fondation pour la Recherche Médicale, European Commission, Pardo, Benjamín, Moriel-Carretero, María, Vicat, Thibaud, Aguilera, Andrés, Pasero, Philippe, Agence Nationale de la Recherche (France), Ligue Nationale contre le Cancer (France), Institut National du Cancer (France), Ministerio de Economía y Competitividad (España), Junta de Andalucía, Fondation pour la Recherche Médicale, European Commission, Pardo, Benjamín, Moriel-Carretero, María, Vicat, Thibaud, Aguilera, Andrés, and Pasero, Philippe

Abstract

Impediments to DNA replication threaten genome stability. The homologous recombination (HR) pathway has been involved in the restart of blocked replication forks. Here, we used a method to increase yeast cell permeability in order to study at the molecular level the fate of replication forks blocked by DNA topoisomerase I poisoning by camptothecin (CPT). Our results indicate that Rad52 and Rad51 HR factors are required to complete DNA replication in response to CPT. Recombination events occurring during S phase do not generally lead to the restart of DNA synthesis but rather protect blocked forks until they merge with convergent forks. This fusion generates structures requiring their resolution by the Mus81 endonuclease in G2/M. At the global genome level, the multiplicity of replication origins in eukaryotic genomes and the fork protection mechanism provided by HR appear therefore to be essential to complete DNA replication in response to fork blockage.

Published

2020

44. Coordinated roles of SLX4 and MutSβ in DNA repair and the maintenance of genome stability

Author

Stephen C. West and Sarah J. Young

Subjects

XPF, DNA Repair, DNA repair, SMX nuclease, crosslinks, Biology, DNA damage response, Biochemistry, Article, Genomic Instability, Recombinases, 03 medical and health sciences, chemistry.chemical_compound, DNA Maintenance, Neoplasms, Animals, Humans, Protein Interaction Maps, Molecular Biology, 030304 developmental biology, Telomere-binding protein, 0303 health sciences, 030302 biochemistry & molecular biology, MUS81, telomeres, recombination, Telomere, Cell biology, chemistry, MutS Homolog 3 Protein, DNA mismatch repair, Trinucleotide repeat expansion, DNA, DNA Damage

Abstract

SLX4 provides a molecular scaffold for the assembly of multiple protein complexes required for the maintenance of genome stability. It is involved in the repair of DNA crosslinks, the resolution of recombination intermediates, the response to replication stress and the maintenance of telomere length. To carry out these diverse functions, SLX4 interacts with three structure-selective endonucleases, MUS81-EME1, SLX1 and XPF-ERCC1, as well as the telomere binding proteins TRF2, RTEL1 and SLX4IP. Recently, SLX4 was shown to interact with MutSβ, a heterodimeric protein involved in DNA mismatch repair, trinucleotide repeat instability, crosslink repair and recombination. Importantly, MutSβ promotes the pathogenic expansion of CAG/CTG trinucleotide repeats, which is causative of myotonic dystrophy and Huntington's disease. The colocalization and specific interaction of MutSβ with SLX4, together with their apparently overlapping functions, are suggestive of a common role in reactions that promote DNA maintenance and genome stability. This review will focus on the role of SLX4 in DNA repair, the interplay between MutSβ and SLX4, and detail how they cooperate to promote recombinational repair and DNA crosslink repair. Furthermore, we speculate that MutSβ and SLX4 may provide an alternative cellular mechanism that modulates trinucleotide instability.

Published

2021

45. ATRX and RECQ5 define distinct homologous recombination subpathways

Author

Ki Choi Chan, Amira Elbakry, Szilvia Juhász, and Markus Löbrich

Subjects

DNA repair synthesis, X-linked Nuclear Protein, DNA Repair, synthesis-dependent strand annealing, chemistry.chemical_compound, crossovers, Proliferating Cell Nuclear Antigen, Radiation, Ionizing, Homologous chromosome, Holliday junction, Humans, Sister chromatids, DNA Breaks, Double-Stranded, Homologous Recombination, ATRX, Cell Proliferation, DNA, Cruciform, Multidisciplinary, RecQ Helicases, sister chromatid exchanges, Holliday Junction Resolvases, Cell Biology, Biological Sciences, Chromatin Assembly and Disassembly, Endonucleases, MUS81, Chromatin, Cell biology, DNA-Binding Proteins, Holliday junctions, chemistry, Homologous recombination, DNA, Signal Transduction

Abstract

Significance Homologous recombination (HR) repairs DNA double-strand breaks by using a homologous template to retrieve sequence information lost at the break site. The broken DNA molecule first engages with the homologous donor molecule and is then separated from it to complete the process. Depending on the HR subpathways used, the separation step can lead to crossovers (COs) between the participating molecules. Such events can cause genomic alterations and eventually cancer if a donor molecule other than the identical sister chromatid is used. Here, we characterize two subpathways of HR with different propensities to form COs. We show the unexpected dominance of the CO-forming subpathway and characterize the processes involved in CO formation and subpathway choice in cancer and normal, untransformed cells., Homologous recombination (HR) is an important DNA double-strand break (DSB) repair pathway that copies sequence information lost at the break site from an undamaged homologous template. This involves the formation of a recombination structure that is processed to restore the original sequence but also harbors the potential for crossover (CO) formation between the participating molecules. Synthesis-dependent strand annealing (SDSA) is an HR subpathway that prevents CO formation and is thought to predominate in mammalian cells. The chromatin remodeler ATRX promotes an alternative HR subpathway that has the potential to form COs. Here, we show that ATRX-dependent HR outcompetes RECQ5-dependent SDSA for the repair of most two-ended DSBs in human cells and leads to the frequent formation of COs, assessed by measuring sister chromatid exchanges (SCEs). We provide evidence that subpathway choice is dependent on interaction of both ATRX and RECQ5 with proliferating cell nuclear antigen. We also show that the subpathway usage varies among different cancer cell lines and compare it to untransformed cells. We further observe HR intermediates arising as ionizing radiation (IR)-induced ultra-fine bridges only in cells expressing ATRX and lacking MUS81 and GEN1. Consistently, damage-induced MUS81 recruitment is only observed in ATRX-expressing cells. Cells lacking BLM show similar MUS81 recruitment and IR-induced SCE formation as control cells. Collectively, these results suggest that the ATRX pathway involves the formation of HR intermediates whose processing is entirely dependent on MUS81 and GEN1 and independent of BLM. We propose that the predominant ATRX-dependent HR subpathway forms joint molecules distinct from classical Holliday junctions.

Published

2021

46. Mus81-Eme1–dependent aberrant processing of DNA replication intermediates in mitosis impairs genome integrity

Author

Calzetta, Nicolás Luis, Besteiro, Marina Alejandra González, and Gottifredi, Vanesa

Subjects

DNA Replication, DNA damage, Chk1, Mitosis, Biology, Genomic Instability, purl.org/becyt/ford/1 [https], Chromosome segregation, 03 medical and health sciences, 0302 clinical medicine, Under-replicated DNA, Chromosomal Instability, Chromosome instability, Humans, Mus81, CHEK1, purl.org/becyt/ford/1.6 [https], Molecular Biology, Research Articles, 030304 developmental biology, 0303 health sciences, Endodeoxyribonucleases, Multidisciplinary, DNA synthesis, DNA replication, SciAdv r-articles, virus diseases, Cell Biology, DNA, Endonucleases, MUS81, female genital diseases and pregnancy complications, Cell biology, DNA-Binding Proteins, 030220 oncology & carcinogenesis, Research Article, DNA Damage

Abstract

The molecular scissors Mus81 fixes or ruins chromosomes depending on the availability of DNA precursors in mitosis., Chromosome instability (CIN) underpins cancer evolution and is associated with drug resistance and poor prognosis. Understanding the mechanistic basis of CIN is thus a priority. The structure-specific endonuclease Mus81-Eme1 is known to prevent CIN. Intriguingly, however, here we show that the aberrant processing of late replication intermediates by Mus81-Eme1 is a source of CIN. Upon depletion of checkpoint kinase 1 (Chk1), Mus81-Eme1 cleaves under-replicated DNA engaged in mitotic DNA synthesis, leading to chromosome segregation defects. Supplementing cells with nucleosides allows the completion of mitotic DNA synthesis, restraining Mus81-Eme1–dependent DNA damage in mitosis and the ensuing CIN. We found no correlation between CIN arising from nucleotide shortage in mitosis and cell death, which were selectively linked to DNA damage load in mitosis and S phase, respectively. Our findings imply the possibility of optimizing Chk1-directed therapies by inducing cell death while curtailing CIN, a common side effect of chemotherapy.

Published

2020

47. Inhibition of Mus81 by siRNA enhances sensitivity to 5-FU in breast carcinoma cell lines.

Author

Ying Qian, Yanning Liu, Qiuyue Yan, Juan Lv, Xiaoyan Ni, Yunlu Wu, and Xuejun Dong

Subjects

*CELL lines, *SMALL interfering RNA, *BREAST cancer, *GENOMES, *DNA repair, *FLUOROURACIL, *POLYMERASE chain reaction, *WESTERN immunoblotting

Abstract

Purpose: One of the most challenging aspects of breast carcinoma chemotherapy is the rapid acquirement of drug resistance. Improving the sensitivity to chemotherapeutic drugs is very important for successful treatment. Mus81 plays an important role in maintaining the stability of the genome and DNA repair. However, recent studies suggested that Mus81 expression levels correlate well with resistance to DNA-damaging drugs. The present study aimed to investigate the role of Mus81 on the chemosensitivity of breast carcinoma cells in response to 5-fluorouracil (5-FU), a chemotherapeutic drug that is widely used for treatment of breast malignancies. Methods: The expression of Mus81 in MCF-7 and T47D cells was suppressed by small interfering RNA (siRNA). mRNA and protein levels of Mus81 were analyzed by quantitative real-time polymerase chain reaction and Western blot. Cell viability and colony survival were determined by Cell Counting Kit-8 and plate colony formation assay, respectively. Cell cycle and apoptosis were detected by flow cytometry. Results: 5-FU inhibited the cell viability of MCF-7 and T47D cells in a concentration-dependent manner. We found that the Mus81-silenced MCF-7 and T47D cells exhibited decreased cell viability and clonogenic survival, but increased G2 accumulation, in response to 5-FU. In addition, Mus81 deficiency resulted in increased apoptosis and p53 expression in MCF-7 after 5-FU treatment. However, Mus81 deficiency did not affect the apoptosis of T47D cells with 5-FU. Conclusion: Taken together, our data suggest that Mus81 inhibition significantly increased the chemosensitivity of MCF-7 and T47D cells in response to 5-FU. Thus, Mus81 siRNA is potentially a useful adjuvant strategy for breast cancer chemotherapy. [ABSTRACT FROM AUTHOR]

Published

2014

48. Combined fluorescent and electron microscopic imaging unveils the specific properties of two classes of meiotic crossovers.

Author

Anderson, Lorinda K., Lohmiller, Leslie D., Xiaomin Tang, Hammond, D. Boyd, Javernick, Lauren, Shearer, Lindsay, Basu-Roy, Sayantani, Martin, Olivier C., and Falque, Matthieu

Subjects

*MEIOSIS, *HOMOLOGOUS chromosomes, *MEDICAL imaging systems, *ELECTRON microscopy, *OPTICAL microscopes, *PLANT breeding, TOMATO genetics

Abstract

Crossovers (COs) shuffle genetic information and allow balanced segregation of homologous chromosomes during the first division of meiosis. In several organisms, mutants demonstrate that two molecularly distinct pathways produce COs. One pathway produces class I COs that exhibit interference (lowered probability of nearby COs), and the other pathway produces class II COs with little or no interference. However, the relative contributions, genomic distributions, and interactions of these two pathways are essentially unknown in nonmutant organisms because marker segregation only indicates that a CO has occurred, not its class type. Here, we combine the efficiency of light microscopy for revealing cellular functions using fluorescent probes with the high resolution of electron microscopy to localize and characterize COs in the same sample of meiotic pachytene chromosomes from wild-type tomato. To our knowledge, for the first time, every CO along each chromosome can be identified by class to unveil specific characteristics of each pathway. We find that class I and II COs have different recombination profiles along chromosomes. In particular, class II COs, which represent about 18% of all COs, exhibit no interference and are disproportionately represented in pericentric heterochroma-tin, a feature potentially exploitable in plant breeding. Finally, our results demonstrate that the two pathways are not independent because there is interference between class I and II COs. [ABSTRACT FROM AUTHOR]

Published

2014

49. Crystal structures of the structure-selective nuclease Mus81- Eme1 bound to flap DNA substrates.

Author

Gwon, Gwang Hyeon, Jo, Aera, Baek, Kyuwon, Jin, Kyeong Sik, Fu, Yaoyao, Lee, Jong‐Bong, Kim, YoungChang, and Cho, Yunje

Subjects

*CRYSTAL structure, *BIOCHEMICAL substrates, *NUCLEASES, *MOLECULAR structure, *BIOLOGICAL transport

Abstract

The Mus81- Eme1 complex is a structure-selective endonuclease with a critical role in the resolution of recombination intermediates during DNA repair after interstrand cross-links, replication fork collapse, or double-strand breaks. To explain the molecular basis of 3′ flap substrate recognition and cleavage mechanism by Mus81-Eme1, we determined crystal structures of human Mus81- Eme1 bound to various flap DNA substrates. Mus81-Eme1 undergoes gross substrate-induced conformational changes that reveal two key features: (i) a hydrophobic wedge of Mus81 that separates pre- and post-nick duplex DNA and (ii) a '5′ end binding pocket' that hosts the 5′ nicked end of post-nick DNA. These features are crucial for comprehensive protein- DNA interaction, sharp bending of the 3′ flap DNA substrate, and incision strand placement at the active site. While Mus81- Eme1 unexpectedly shares several common features with members of the 5′ flap nuclease family, the combined structural, biochemical, and biophysical analyses explain why Mus81- Eme1 preferentially cleaves 3′ flap DNA substrates with 5′ nicked ends. [ABSTRACT FROM AUTHOR]

Published

2014

50. Expression Analysis of EEPD1 and MUS81 Genes in Breast Cancer

Author

Ali Zekri, Nemamali Azadi, Mansoor Khaledi, Ehsan Sohrabi, Hamed Afkhami, Ehsan Razmara, and Masoumeh Moslemi

Subjects

0301 basic medicine, Colorectal cancer, business.industry, Cancer, General Medicine, medicine.disease, medicine.disease_cause, MUS81, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Breast cancer, 030220 oncology & carcinogenesis, Gene expression, medicine, Cancer research, skin and connective tissue diseases, Micronucleus, Carcinogenesis, business, Gene

Abstract

Breast cancer is one of the chief causes of death and also the most common type of cancer among women worldwide...

Published

2020