Your search keyword '"Raught B"' showing total 5,599 results

151. Integrative analysis of bulk and single-cell transcriptomic data reveals novel insights into lipid metabolism and prognostic factors in hepatocellular carcinoma.

Author

Qi, Feiyu, Zha, Guiming, Zhang, Yanfang, Liu, Sihua, Yang, Yuhang, Sun, Wanliang, Wang, Dongdong, Liu, Zhong, Lu, Zheng, and Zhang, Dengyong

Subjects

GENE expression, GENE regulatory networks, DISEASE risk factors, LIVER cells, DRUG analysis

Abstract

Hepatocellular carcinoma (HCC) is associated with high mortality rate. This study investigated the status of lipid metabolism-related genes in HCC. Bulk transcriptomic and single-cell sequencing data for HCC were retrieved from public databases. The single-cell sequencing data was subjected to dimensionality reduction, which facilitated the annotation of distinct cell subpopulations and marker gene expression analysis within each subpopulation. Genes associated with lipid metabolism in liver cells were identified, and a machine-learning model was developed using the bulk transcriptomic data randomly partitioned into training and validation sets. The efficacy of the model was validated using these two sets. A multifactorial Cox analysis on the model genes combined with clinical features, led to the identification of age, HMGCS2, HNRNPU, and RAN as independent prognostic factors, which were included in the nomogram model construction and validation. A weighted gene co-expression analysis of all genes of the bulk transcriptome samples revealed the correlation between gene modules and risk score. Genes with cor > 0.4 in the highest-expressing module were selected for Gene Ontology and Kyoto Encyclopedia of Genes and Genomes functional enrichment analysis. Immune-related analysis was conducted based on seven algorithms for immune cell infiltration prediction. For the genes in the nomogram model, the expression in clinical pathological factors was also analyzed. The drug sensitivity analysis offered a reference for the selection of targeting drugs. This investigation provides novel insights and a theoretical basis for the prognosis, treatment, and pharmaceutical advancements for patients diagnosed with HCC. [ABSTRACT FROM AUTHOR]

Published

2024

152. Ribosomal S6 kinase (RSK) plays a critical role in DNA damage response via the phosphorylation of histone lysine demethylase KDM4B.

Author

Wu, Wenwen, Zhu, Jing, Nihira, Naoe Taira, Togashi, Yukiko, Goda, Atsushi, Koike, Junki, Yamaguchi, Kiyoshi, Furukawa, Yoichi, Tomita, Takuya, Saeki, Yasushi, Johmura, Yoshikazu, Nakanishi, Makoto, Miyoshi, Yasuo, and Ohta, Tomohiko

Subjects

DNA repair, HISTONE demethylases, DOUBLE-strand DNA breaks, RNA interference, SMALL interfering RNA, ESTROGEN

Abstract

Background: Epigenetic dysregulation affecting oncogenic transcription and DNA damage response is a hallmark of cancer. The histone demethylase KDM4B, a factor regulating these processes, plays important roles in estrogen receptor-mediated transcription and DNA repair in breast cancer. However, how oncogenic phospho-signal transduction affects epigenetic regulation is not fully understood. Here we found that KDM4B phosphorylation by ribosomal S6 kinase (RSK), a downstream effector of the Ras/MAPK pathway, is critical for the function of KDM4B in response to DNA damage. Methods: KDM4B-knockout breast cancer cell lines were generated via CRISPR/Cas9-mediated gene editing. Re-expression of wild-type or phospho-site mutated KDM4B in knockout cells was performed by lentivirus-mediated gene transfer. Gene knockdown was achieved by RNA interference. DNA double-strand breaks (DSBs) were induced by ionizing radiation or laser-microirradiation. Protein accumulation at DSB sites was analyzed by immunofluorescence. KDM4B phosphorylation by RSK was assessed by in vitro and in vivo kinase assays. Gene and protein expression levels were analyzed by RT‒PCR and western blotting. The sensitivity of cells to ionizing radiation was examined by a clonogenic survival assay. Results: RSK phosphorylated KDM4B at Ser666, and inhibition of the phosphorylation by RSK depletion or RSK inhibitors abrogated KDM4B accumulation at the sites of DNA double-strand breaks (DSBs). DSB repair was significantly delayed in KDM4B-knockout cells or cells treated with RSK inhibitors. The replacement of endogenous KDM4B with the phosphomimetic mutant S666D restored KDM4B accumulation and DSB repair that had been inhibited by RSK inhibitors, suggesting a critical role for RSK at the specific serine residue of KDM4B in the effect of RSK inhibitors on DSB repair. As a consequence of these aberrant responses, inhibition of KDM4B phosphorylation increased the sensitivity of the cells to ionizing radiation. Conclusions: Overall, the present study uncovered a novel function of RSK on the DNA damage response, which provides an additional role of its inhibitor in cancer therapy. [ABSTRACT FROM AUTHOR]

Published

2024

153. H3K27me3 Loss in Central Nervous System Tumors: Diagnostic, Prognostic, and Therapeutic Implications.

Author

Angelico, Giuseppe, Mazzucchelli, Manuel, Attanasio, Giulio, Tinnirello, Giordana, Farina, Jessica, Zanelli, Magda, Palicelli, Andrea, Bisagni, Alessandra, Barbagallo, Giuseppe Maria Vincenzo, Certo, Francesco, Zizzo, Maurizio, Koufopoulos, Nektarios, Magro, Gaetano, Caltabiano, Rosario, and Broggi, Giuseppe

Subjects

PROTEIN metabolism, PROTEINS, CANCER invasiveness, GLIOMAS, EPIGENOMICS, TUMOR markers, CENTRAL nervous system tumors, DNA methylation, IMMUNOHISTOCHEMISTRY, GENE expression, GENES, HISTONES, MENINGIOMA, GENETIC mutation, PROGRESSION-free survival

Abstract

Simple Summary: This article herein presented explores the role of the epigenetic marker H3K27me3 in tumors of the Central Nervous System, highlighting its importance for diagnosis, prognosis, and treatment. H3K27me3 involves the trimethylation of lysine 27 on the histone H3 protein, which is essential for regulating gene activity and maintaining chromatin structure. A reduction in H3K27me3 levels is commonly seen in CNS tumors such as diffuse midline gliomas and meningiomas and is associated with more aggressive tumor behavior and a worse prognosis. This article emphasizes the utility of H3K27me3 loss in tumor diagnosis, prognosis, and the advancement of targeted therapies. Central nervous system (CNS) tumors represent a formidable clinical challenge due to their molecular complexity and varied prognostic outcomes. This review delves into the pivotal role of the epigenetic marker H3K27me3 in the development and treatment of CNS tumors. H3K27me3, specifically the trimethylation of lysine 27 on the histone H3 protein, plays a crucial role in regulating gene expression and maintaining chromatin architecture (e.g., in X-chromosome inactivation). Notably, a reduction in H3K27me3 levels, frequently tied to mutations in the H3 gene family such as H3F3A and HIST1H3B, is evident in diverse brain tumor variants, including the diffuse midline glioma characterized by the H3K27M mutation and certain pediatric high-grade gliomas. The loss of H3K27me3 has been linked to more aggressive behavior in meningiomas, with the trimethylation loss associated with significantly shorter recurrence-free survival (RFS) among grade 2 meningiomas, albeit not within grade 1 tumors. Pediatric posterior fossa ependymomas characterized by a lowered H3K27me3 and DNA hypomethylation exhibit poor prognosis, underscoring the prognostic significance of these epigenetic alterations in CNS tumors. Comprehending the role of H3K27me3 in CNS tumors is vital for advancing diagnostic tools and therapeutic interventions, with the goal of enhancing patient outcomes and quality of life. This review underscores the importance of ongoing investigations into H3K27me to refine and optimize management strategies for CNS tumors, paving the way for improved personalized medicine practices in oncology. [ABSTRACT FROM AUTHOR]

Published

2024

154. Chronic Low-Dose-Rate Radiation-Induced Persistent DNA Damage and miRNA/mRNA Expression Changes in Mouse Hippocampus and Blood.

Author

Wang, Hong, Lau, Salihah, Tan, Amanda, and Tang, Feng Ru

Subjects

GENE expression, DENTATE gyrus, IMMUNOSTAINING, ANIMAL behavior, DNA damage

Abstract

Our previous study demonstrated that the acute high-dose-rate (3.3 Gy/min) γ-ray irradiation (γ-irradiation) of postnatal day-3 (P3) mice with 5 Gy induced depression and drastic neuropathological changes in the dentate gyrus of the hippocampus of adult mice. The present study investigated the effects of chronic low-dose-rate (1.2 mGy/h) γ-irradiation from P3 to P180 with a cumulative dose of 5 Gy on animal behaviour, hippocampal cellular change, and miRNA and mRNA expression in the hippocampus and blood in female mice. The radiation exposure did not significantly affect the animal's body weight, and neuropsychiatric changes such as anxiety and depression were examined by neurobehavioural tests, including open field, light-dark box, elevated plus maze, tail suspension, and forced swim tests. Immunohistochemical staining did not detect any obvious loss of mature and immature neurons (NeuN and DCX) or any inflammatory glial response (IBA1, GFAP, and PDGFRα). Nevertheless, γH2AX foci in the stratum granulosum of the dentate gyrus were significantly increased, suggesting the chronic low-dose-rate irradiation induced persistent DNA damage foci in mice. miRNA sequencing and qRT-PCR indicated an increased expression of miR-448-3p and miR-361-5p but decreased expression of miR-193a-3p in the mouse hippocampus. Meanwhile, mRNA sequencing and qRT-PCR showed the changed expression of some genes, including Fli1, Hs3st5, and Eif4ebp2. Database searching by miRDB and TargetScan predicted that Fli1 and Hs3st5 are the targets of miR-448-3p, and Eif4ebp2 is the target of miR-361-5p. miRNA/mRNA sequencing and qRT-PCR results in blood showed the increased expression of miR-6967-3p and the decreased expression of its target S1pr5. The interactions of these miRNAs and mRNAs may be related to the chronic low-dose-rate radiation-induced persistent DNA damage. [ABSTRACT FROM AUTHOR]

Published

2024

155. Unraveling the roles and mechanisms of mitochondrial translation in normal and malignant hematopoiesis.

Author

Liu, Lianxuan, Shao, Mi, Huang, Yue, Qian, Pengxu, and Huang, He

Subjects

GENETIC translation, CELL physiology, HEMATOLOGIC malignancies, T cells, IMMUNOREGULATION

Abstract

Due to spatial and genomic independence, mitochondria possess a translational mechanism distinct from that of cytoplasmic translation. Several regulators participate in the modulation of mitochondrial translation. Mitochondrial translation is coordinated with cytoplasmic translation through stress responses. Importantly, the inhibition of mitochondrial translation leads to the inhibition of cytoplasmic translation and metabolic disruption. Therefore, defects in mitochondrial translation are closely related to the functions of hematopoietic cells and various immune cells. Finally, the inhibition of mitochondrial translation is a potential therapeutic target for treating multiple hematologic malignancies. Collectively, more in-depth insights into mitochondrial translation not only facilitate our understanding of its functions in hematopoiesis, but also provide a basis for the discovery of new treatments for hematological malignancies and the modulation of immune cell function. [ABSTRACT FROM AUTHOR]

Published

2024

156. Disordered regions of human eIF4B orchestrate a dynamic self-association landscape.

Author

Swain, Bikash Chandra, Sarkis, Pascale, Ung, Vanessa, Rousseau, Sabrina, Fernandez, Laurent, Meltonyan, Ani, Aho, V. Esperance, Mercadante, Davide, Mackereth, Cameron D., and Aznauryan, Mikayel

Subjects

STRESS granules, MOLECULAR spectroscopy, IONIC strength, CELL physiology, CONDENSED matter

Abstract

Eukaryotic translation initiation factor eIF4B is required for efficient cap-dependent translation, it is overexpressed in cancer cells, and may influence stress granule formation. Due to the high degree of intrinsic disorder, eIF4B is rarely observed in cryo-EM structures of translation complexes and only ever by its single structured RNA recognition motif domain, leaving the molecular details of its large intrinsically disordered region (IDR) unknown. By integrating experiments and simulations we demonstrate that eIF4B IDR orchestrates and fine-tunes an intricate transition from monomers to a condensed phase, in which large-size dynamic oligomers form before mesoscopic phase separation. Single-molecule spectroscopy combined with molecular simulations enabled us to characterize the conformational ensembles and underlying intra- and intermolecular dynamics across the oligomerization transition. The observed sensitivity to ionic strength and molecular crowding in the self-association landscape suggests potential regulation of eIF4B nanoscopic and mesoscopic behaviors such as driven by protein modifications, binding partners or changes to the cellular environment. This study reveals how the intrinsically disordered region of eIF4B governs its transition from monomers to oligomers and condensed droplets, providing key insights into how its self-association may be regulated to carry out its cellular functions. [ABSTRACT FROM AUTHOR]

Published

2024

157. Cellular SUMO-specific proteases regulate HAdV-C5 E1B-55K SUMOylation and virus-induced cell transformation.

Author

Wing-Hang Ip, Fiedler, Marie, Gornott, Britta, Morische, Malte, Bertzbach, Luca D., and Dobner, Thomas

Subjects

CELL transformation, VIRAL proteins, POST-translational modification, PROTEOLYTIC enzymes, ONCOGENES

Abstract

Various viral proteins are post-translationally modified by SUMO-conjugation during the human adenovirus (HAdV) replication cycle. This modification leads to diverse consequences for target proteins as it influences their intracellular localization or cell transformation capabilities. SUMOylated HAdV proteins include the multifunctional oncoprotein E1B-55K. Our previous research, along with that of others, has demonstrated a substantial influence of yet another adenoviral oncoprotein, E4orf6, on E1B-55K SUMOylation levels. Protein SUMOylation can be reversed by cellular sentrin/SUMO-specific proteases (SENPs). In this study, we investigated the interaction of E1B-55K with cellular SENPs to understand deSUMOylation activities and their consequences for cell transformation mediated by this adenoviral oncoprotein. We show that E1B-55K interacts with and is deSUMOylated by SENP 1, independently of E4orf6. Consistent with these results, we found that SENP 1 prevents E1A/E1Bdependent focus formation in rodent cells. We anticipate these findings to be the groundwork for future studies on adenovirus-host interactions, the mechanisms that underlie E1B-55K SUMOylation, as well as the role of this major adenoviral oncoprotein in HAdV-mediated cell transformation. [ABSTRACT FROM AUTHOR]

Published

2024

158. Exploiting Translation Machinery for Cancer Therapy: Translation Factors as Promising Targets.

Author

Sehrawat, Urmila

Subjects

SMALL molecules, PROTEIN synthesis, DRUG target, CANCER invasiveness, SCIENTIFIC community, GENETIC translation

Abstract

Eukaryotic protein translation has slowly gained the scientific community's attention for its advanced and powerful therapeutic potential. However, recent technical developments in studying ribosomes and global translation have revolutionized our understanding of this complex multistep process. These developments have improved and deepened the current knowledge of mRNA translation, sparking excitement and new possibilities in this field. Translation factors are crucial for maintaining protein synthesis homeostasis. Since actively proliferating cancer cells depend on protein synthesis, dysregulated protein translation is central to tumorigenesis. Translation factors and their abnormal expressions directly affect multiple oncogenes and tumor suppressors. Recently, small molecules have been used to target translation factors, resulting in translation inhibition in a gene-specific manner, opening the door for developing translation inhibitors that can lead to novel chemotherapeutic drugs for treating multiple cancer types caused by dysregulated translation machinery. This review comprehensively summarizes the involvement of translation factors in tumor progression and oncogenesis. Also, it sheds light on the evolution of translation factors as novel drug targets for developing future therapeutic drugs for treating cancer. [ABSTRACT FROM AUTHOR]

Published

2024

159. Global organization of phenylpropanoid and anthocyanin pathways revealed by proximity labeling of trans-cinnamic acid 4-hydroxylase in Petunia inflata petal protoplasts.

Author

Aravena-Calvo, Javiera, Busck-Mellor, Silas, and Laursen, Tomas

Subjects

PLANT enzymes, PHENYLPROPANOIDS, CINNAMIC acid, CARBON cycle, CYTOCHROME P-450

Abstract

The phenylpropanoid pathway is one of the main carbon sinks in plants, channeling phenylalanine towards thousands of products including monolignols, stilbenes, flavonoids and volatile compounds. The enzymatic steps involved in many of these pathways are well characterized, however the physical organization of these enzymes within the plant cell remains poorly understood. Proximity-dependent labeling allows untargeted determination of both direct and indirect protein interactions in vivo, and therefore stands as an attractive alternative to targeted binary assays for determining global proteinprotein interaction networks. We used TurboID-based proximity labeling to study protein interaction networks of the core phenylpropanoid and anthocyanin pathways in petunia. To do so, we coupled the endoplasmic reticulum (ER) membrane anchored cytochrome P450 cinnamic acid 4-hydroxylase (C4H, CYP73A412) from Petunia inflata to TurboID and expressed it in protoplasts derived from anthocyanin-rich petunia petals. We identified multiple soluble enzymes from the late anthocyanin pathway among enriched proteins, along with other C4H isoforms, and other ER membrane anchored CYPs. Several of these interactions were subsequently confirmed by bimolecular fluorescence complementation (BiFC). Our results suggest that C4H co-localizes with enzymes from the phenylpropanoid- and downstream anthocyanin pathways, supporting the idea that C4H may serve as ER anchoring points for downstream metabolic pathways. Moreover, this study demonstrates the feasibility of using protoplasts to perform global mapping of protein network for enzymes in their native cellular environment. [ABSTRACT FROM AUTHOR]

Published

2024

160. Late-life dietary folate restriction reduces biosynthesis without compromising healthspan in mice.

Author

Blank, Heidi M., Hammer, Staci E., Boatright, Laurel, Roberts, Courtney, Heyden, Katarina E., Nagarajan, Aravindh, Mitsuhiro Tsuchiya, Brun, Marcel, Johnson, Charles D., Stover, Patrick J., Sitcheran, Raquel, Kennedy, Brian K., Adams, L. Garry, Kaeberlein, Matt, Field, Martha S., Threadgill, David W., Andrews-Polymenis, Helene L., and Polymenis, Michael

Published

2024

161. PPM1G dephosphorylates eIF4E in control of mRNA translation and cell proliferation.

Author

Peng Wang, Zixian Li, Sung-Hoon Kim, Haijin Xu, Hao Huang, Chutong Yang, Snape, Abby, Jung-Hyun Choi, Bermudez, Sara, Boivin, Marie-Noelle, Ferry, Nicolas, Karamchandani, Jason, Nagar, Bhushan, and Sonenberg, Nahum

Published

2024

162. C/EBPβ deletion in macrophages impairs mammary gland alveolar budding during the estrous cycle.

Author

Rojo, Michelle D., Bandyopadhyay, Ishitri, Burke, Caitlin M., Sturtz, Alexa D., Phillips, Emily S., Matherne, Megan G., Embrey, Samuel J., LaRue, Rebecca, Yinjie Qiu, Schwertfeger, Kathryn L., and Machado, Heather L.

Published

2024

163. Dysfunction of Telomeric Cdc13-Stn1-Ten1 Simultaneously Activates DNA Damage and Spindle Checkpoints.

Author

Grandin, Nathalie and Charbonneau, Michel

Subjects

UBIQUITIN ligases, SPINDLE apparatus, DNA damage, CELL cycle, SEPTINS

Abstract

Telomeres, the ends of eukaryotic linear chromosomes, are composed of repeated DNA sequences and specialized proteins, with the conserved telomeric Cdc13/CTC1-Stn1-Ten1 (CST) complex providing chromosome stability via telomere end protection and the regulation of telomerase accessibility. In this study, SIZ1, coding for a SUMO E3 ligase, and TOP2 (a SUMO target for Siz1 and Siz2) were isolated as extragenic suppressors of Saccharomyces cerevisiae CST temperature-sensitive mutants. ten1-sz, stn1-sz and cdc13-sz mutants were isolated next due to being sensitive to intracellular Siz1 dosage. In parallel, strong negative genetic interactions between mutants of CST and septins were identified, with septins being noticeably sumoylated through the action of Siz1. The temperature-sensitive arrest in these new mutants of CST was dependent on the G2/M Mad2-mediated and Bub2-mediated spindle checkpoints as well as on the G2/M Mec1-mediated DNA damage checkpoint. Our data suggest the existence of yet unknown functions of the telomeric Cdc13-Stn1-Ten1 complex associated with mitotic spindle positioning and/or assembly that could be further elucidated by studying these new ten1-sz, stn1-sz and cdc13-sz mutants. [ABSTRACT FROM AUTHOR]

Published

2024

164. General control nonderepressible 2 (GCN2) as a therapeutic target in age-related diseases.

Author

Altintas, Ozlem and MacArthur, Michael R.

Subjects

ELDER care, PROTEIN kinases, CELLULAR signal transduction, NEURODEGENERATION, GENE expression, MOLECULAR structure, AMINO acids, INFLAMMATION, TUMORS, ACTIVE aging, LONGEVITY

Abstract

The function of General Control Nonderepressible 2 (GCN2), an evolutionaryconserved component of the integrated stress response (ISR), has been welldocumented across organisms from yeast to mammals. Recently GCN2 has also gained attention for its role in health and disease states. In this review, we provide a brief overview of GCN2, including its structure, activation mechanisms and interacting partners, and explore its potential significance as a therapeutic target in various age-related diseases including neurodegeneration, inflammatory disorders and cancer. Finally, we summarize the barriers to effectively targeting GCN2 for the treatment of disease and to promote a healthier aging process. [ABSTRACT FROM AUTHOR]

Published

2024

165. Dysfunction of Calcyphosine-Like gene impairs retinal angiogenesis through the MYC axis and is associated with familial exudative vitreoretinopathy.

Author

Wenjing Liu, Shujin Li, Mu Yang, Jie Ma1 Lu Liu, Ping Fei, Qianchun Xiang, Lulin Huang, Peiquan Zhao, Zhenglin Yang, and Xianjun Zhu

Published

2024

166. Anabolic deficits and divergent unfolded protein response underlie skeletal and cardiac muscle growth impairments in the Yoshida hepatoma tumor model of cancer cachexia.

Author

Belcher, Daniel J., Kim, Nina, Navarro‐Llinas, Blanca, Möller, Maria, López‐Soriano, Francisco J., Busquets, Silvia, and Nader, Gustavo A.

Subjects

UNFOLDED protein response, MYOCARDIUM, SKELETAL muscle, TRANSCRIPTION factors, WEIGHT loss

Abstract

Cancer cachexia manifests as whole body wasting, however, the precise mechanisms governing the alterations in skeletal muscle and cardiac anabolism have yet to be fully elucidated. In this study, we explored changes in anabolic processes in both skeletal and cardiac muscles in the Yoshida AH‐130 ascites hepatoma model of cancer cachexia. AH‐130 tumor‐bearing rats experienced significant losses in body weight, skeletal muscle, and heart mass. Skeletal and cardiac muscle loss was associated with decreased ribosomal (r)RNA, and hypophosphorylation of the eukaryotic factor 4E binding protein 1. Endoplasmic reticulum stress was evident by higher activating transcription factor mRNA in skeletal muscle and growth arrest and DNA damage‐inducible protein (GADD)34 mRNA in both skeletal and cardiac muscles. Tumors provoked an increase in tissue expression of interferon‐γ in the heart, while an increase in interleukin‐1β mRNA was apparent in both skeletal and cardiac muscles. We conclude that compromised skeletal muscle and heart mass in the Yoshida AH‐130 ascites hepatoma model involves a marked reduction translational capacity and efficiency. Furthermore, our observations suggest that endoplasmic reticulum stress and tissue production of pro‐inflammatory factors may play a role in the development of skeletal and cardiac muscle wasting. [ABSTRACT FROM AUTHOR]

Published

2024

167. MRD in Acute Leukemias: Lessons Learned from Acute Promyelocytic Leukemia.

Author

Kegyes, David, Thiagarajan, Praveena S., and Ghiaur, Gabriel

Subjects

TREATMENT of acute promyelocytic leukemia, BONE marrow, ACUTE promyelocytic leukemia, POLYMERASE chain reaction, CARCINOGENESIS, MOLECULAR biology, SEQUENCE analysis

Abstract

Simple Summary: We provide a historical perspective on the current concepts of minimal residual disease (MRD) and how it evolves from minimal residual disease to measurable residual disease. We aim to highlight the fundamental biology behind MRD—the overlap between leukemia stem cells and MRD, and the role of the bone marrow microenvironment in the persistence of MRD. We describe how our success in measuring and subsequently eliminating residual disease in acute promyelocytic leukemia will pave the way towards progress in other acute leukemias. Introduction: Advances in molecular biology, polymerase chain reaction (PCR), and next-generation sequencing (NGS) have transformed the concept of minimal residual disease (MRD) from a philosophical idea into a measurable reality. Current Treatment Paradigms and Lessons Learned from APL: Acute promyelocytic leukemia (APL) leads the way in this transformation, initially using PCR to detect MRD in patients in remission, and more recently, aiming to eliminate it entirely with modern treatment strategies. Along the way, we have gained valuable insights that, when applied to other forms of acute leukemia, hold the potential to significantly improve the outcomes of these challenging diseases. Does the BM Microenvironment Play a Role in MRD?: In this review, we explore the current use of MRD in the management of acute leukemia and delve into the biological processes that contribute to MRD persistence, including its overlap with leukemia stem cells and the role of the bone marrow microenvironment. [ABSTRACT FROM AUTHOR]

Published

2024

168. Quantitative mapping of proteasome interactomes and substrates using ProteasomeID.

Author

Bartolome, Aleksandar, Heiby, Julia C., Di Fraia, Domenico, Heinze, Ivonne, Knaudt, Hannah, Spaeth, Ellen, Omrani, Omid, Minetti, Alberto, Hofmann, Maleen, Kirkpatrick, Joanna M., Dau, Therese, and Ori, Alessandro

Published

2024

169. Answering open questions in biology using spatial genomics and structured methods.

Author

Jena, Siddhartha G., Verma, Archit, and Engelhardt, Barbara E.

Subjects

BIOLOGICAL systems, CYTOLOGY, CELL morphology, CONCEPTUAL models, BIOLOGICAL models

Abstract

Genomics methods have uncovered patterns in a range of biological systems, but obscure important aspects of cell behavior: the shapes, relative locations, movement, and interactions of cells in space. Spatial technologies that collect genomic or epigenomic data while preserving spatial information have begun to overcome these limitations. These new data promise a deeper understanding of the factors that affect cellular behavior, and in particular the ability to directly test existing theories about cell state and variation in the context of morphology, location, motility, and signaling that could not be tested before. Rapid advancements in resolution, ease-of-use, and scale of spatial genomics technologies to address these questions also require an updated toolkit of statistical methods with which to interrogate these data. We present a framework to respond to this new avenue of research: four open biological questions that can now be answered using spatial genomics data paired with methods for analysis. We outline spatial data modalities for each open question that may yield specific insights, discuss how conflicting theories may be tested by comparing the data to conceptual models of biological behavior, and highlight statistical and machine learning-based tools that may prove particularly helpful to recover biological understanding. [ABSTRACT FROM AUTHOR]

Published

2024

170. TP63 transcriptionally regulates SLC7A5 to suppress ferroptosis in head and neck squamous cell carcinoma.

Author

Zilong Chen, Haoxi Cai, Weiwei Ye, Junming Wu, Jing Liu, Yun Xie, Shiqiang Feng, Yuanpei Jin, Yunxia Lv, Hui Ye, Chengfu Cai, and Gengming Cai

Subjects

GENE regulatory networks, SQUAMOUS cell carcinoma, RNA sequencing, FLUORESCENT probes, TUMOR microenvironment

Abstract

Background: Most head and neck squamous cell carcinoma (HNSCC) patients are diagnosed at an advanced local stage. While immunotherapy has improved survival rates, only a minority of patients respond durably to targeted immunotherapies, posing substantial clinical challenges. We investigated the heterogeneity of the tumor microenvironment in HNSCC cohorts before and after immunotherapy by analyzing single-cell RNA sequencing (scRNA-seq) data and bulk RNA sequencing datasets retrieved from public databases. Methods: We constructed a single-cell transcriptome landscape of HNSCC patients before and after immunotherapy and analyzed the cellular composition, developmental trajectories, gene regulatory networks, and communication patterns of different cell type subpopulations. Additionally, we assessed the expression levels of relevant indicators in HNSCC cells via western blot, ELISA, and fluorescent probe techniques. Results: At the single-cell level, we identified a subpopulation of TP63+ SLC7A5+ HNSCC that exhibited a ferroptosis-resistant phenotype. This subpopulation suppresses ferroptosis in malignant cells through the transcriptional upregulation of SLC7A5 mediated by high TP63 expression, thereby promoting tumor growth and resistance to immunotherapy. The experimental results demonstrated that the overexpression of TP63 upregulated the expression of SLC7A5 and suppressed the concentrations of Fe2+ and ROS in HNSCC cells. By integrating bulk transcriptome data, we developed a clinical scoring model based on TP63 and SLC7A5, which are closely associated with tumor stage, revealing the significant prognostic efficacy of the TP63+ SLC7A5+ HNSCC-mediated ferroptosis mechanism in HNSCC patients. Conclusion: Our research elucidates the TME in HNSCC before and after immunotherapy, revealing a novel mechanism by which TP63+ SLC7A5+ HNSCC inhibits ferroptosis and enhances tumor resistance via TP63-induced SLC7A5 upregulation. These insights lay the foundation for the development of more effective treatments for HNSCC. [ABSTRACT FROM AUTHOR]

Published

2024

171. The Type III Effector XopL Xcc in Xanthomonas campestris pv. campestris Targets the Proton Pump Interactor 1 and Suppresses Innate Immunity in Arabidopsis.

Author

Huang, Jing, Dong, Yuru, Li, Nana, He, Yongqiang, and Zhou, Hao

Subjects

XANTHOMONAS campestris, ARABIDOPSIS thaliana, DISEASE resistance of plants, BACTERIAL diseases, CELL membranes

Abstract

Xanthomonas campestris pathovar campestris (Xcc) is a significant phytopathogen causing black rot disease in crucifers. Xcc injects a variety of type III effectors (T3Es) into the host cell to assist infection or propagation. A number of T3Es inhibit plant immunity, but the biochemical basis for a vast majority of them remains unknown. Previous research has revealed that the evolutionarily conserved XopL-family effector XopLXcc inhibits plant immunity, although the underlying mechanisms remain incompletely elucidated. In this study, we identified proton pump interactor (PPI1) as a specific virulence target of XopLXcc in Arabidopsis. Notably, the C-terminus of PPI1 and the Leucine-rich repeat (LRR) domains of XopLXcc are pivotal for facilitating this interaction. Our findings indicate that PPI1 plays a role in the immune response of Arabidopsis to Xcc. These results propose a model in which XopLXcc binds to PPI1, disrupting the early defense responses activated in Arabidopsis during Xcc infection and providing valuable insights into potential strategies for regulating plasma membrane (PM) H+-ATPase activity during infection. These novel insights enhance our understanding of the pathogenic mechanisms of T3Es and contribute to the development of effective strategies for controlling bacterial diseases. [ABSTRACT FROM AUTHOR]

Published

2024

172. Resident demand-oriented selection and spatial layout strategy for public sports facilities.

Author

Chen, Yu, He, Shaoyao, Zhang, Mengmiao, and Cai, Yan

Abstract

In response to elevated living standards and evolving recreational values, public sports facilities have become a focal point. This study, targeting the central districts of Yiyang City across 17 neighborhoods, integrates questionnaire surveys, in-depth interviews, and geographic information system analysis to address the diversified needs in sports infrastructure. It reveals a discrepancy characterised by uniform facility types and flawed layouts, notably in Heshan and Ziyang, that fail to satisfy the diversified demands of residents. Consequently, the research introduces a bottom-up strategy, emphasising the need for facility selections and spatial layouts informed by community needs. Furthermore, it highlights the importance of demographic factors such as age, income, and education in guiding facility placement strategies to accommodate a broad spectrum of users. By doing so, the study contributes a novel, resident-focused framework to the discourse on public sports facilities, promoting sustainable and inclusive urban sports environment development. [ABSTRACT FROM AUTHOR]

Published

2024

173. NEK6 dampens FOXO3 nuclear translocation to stabilize C-MYC and promotes subsequent de novo purine synthesis to support ovarian cancer chemoresistance.

Author

Liu, Jingchun, Wang, Haoyu, Wan, Huanzhi, Yang, Jiang, Gao, Likun, Wang, Zhi, Zhang, Xiaoyi, Han, Wuyue, Peng, Jiaxin, Yang, Lian, and Hong, Li

Published

2024

174. Translation of Overlapping Open Reading Frames Promoted by Type 2 IRESs in Avian Calicivirus Genomes.

Author

Arhab, Yani, Pestova, Tatyana V., and Hellen, Christopher U. T.

Subjects

HORIZONTAL gene transfer, CALICIVIRUSES, GENETIC code, GENOMES, RNA

Abstract

Caliciviruses have positive-sense RNA genomes, typically with short 5′-untranslated regions (5′UTRs) that precede the long open reading frame 1 (ORF1). Exceptionally, some avian caliciviruses have long 5′UTRs containing a picornavirus-like internal ribosomal entry site (IRES), which was likely acquired by horizontal gene transfer. Here, we identified numerous additional avian calicivirus genomes with IRESs, predominantly type 2, and determined that many of these genomes contain a ~200–300 codon-long ORF (designated ORF1*) that overlaps the 5′-terminal region of ORF1. The activity of representative type 2 IRESs from grey teal calicivirus (GTCV) and Caliciviridae sp. isolate yc-13 (RaCV1) was confirmed by in vitro translation. Toeprinting showed that in cell-free extracts and in vitro reconstituted reactions, ribosomal initiation complexes assembled on the ORF1* initiation codon and at one or two AUG codons in ORF1 at the 3′-border and/or downstream of the IRES. Initiation at all three sites required eIF4A and eIF4G, which bound to a conserved region of the IRES; initiation on the ORF1* and principal ORF1 initiation codons involved eIF1/eIF1A-dependent scanning from the IRES's 3′-border. Initiation on these IRESs was enhanced by the IRES trans-acting factors (ITAFs) Ebp1/ITAF45, which bound to the apical subdomain Id of the IRES, and PTB (GTCV) or PCBP2 (RaCV1). [ABSTRACT FROM AUTHOR]

Published

2024

175. Genetics, Pathophysiology, and Current Challenges in Von Hippel–Lindau Disease Therapeutics.

Author

Gómez-Virgilio, Laura, Velazquez-Paniagua, Mireya, Cuazozon-Ferrer, Lucero, Silva-Lucero, Maria-del-Carmen, Gutierrez-Malacara, Andres-Ivan, Padilla-Mendoza, Juan-Ramón, Borbolla-Vázquez, Jessica, Díaz-Hernández, Job-Alí, Jiménez-Orozco, Fausto-Alejandro, and Cardenas-Aguayo, Maria-del-Carmen

Subjects

THERAPEUTICS, TUMOR suppressor genes, GENETICS, DIAGNOSIS, GENETIC testing, VON Hippel-Lindau disease

Abstract

This review article focuses on von Hippel–Lindau (VHL) disease, a rare genetic disorder characterized by the development of tumors and cysts throughout the body. It discusses the following aspects of the disease. Genetics: VHL disease is caused by mutations in the VHL tumor suppressor gene located on chromosome 3. These mutations can be inherited or occur spontaneously. This article details the different types of mutations and their associated clinical features. Pathophysiology: The underlying cause of VHL disease is the loss of function of the VHL protein (pVHL). This protein normally regulates hypoxia-inducible factors (HIFs), which are involved in cell growth and survival. When pVHL is dysfunctional, HIF levels become elevated, leading to uncontrolled cell growth and tumor formation. Clinical Manifestations: VHL disease can affect various organs, including the brain, spinal cord, retina, kidneys, pancreas, and adrenal glands. Symptoms depend on the location and size of the tumors. Diagnosis: Diagnosis of VHL disease involves a combination of clinical criteria, imaging studies, and genetic testing. Treatment: Treatment options for VHL disease depend on the type and location of the tumors. Surgery is the mainstay of treatment, but other options like radiation therapy may also be used. Challenges: This article highlights the challenges in VHL disease management, including the lack of effective therapies for some tumor types and the need for better methods to monitor disease progression. In conclusion, we emphasize the importance of ongoing research to develop new and improved treatments for VHL disease. [ABSTRACT FROM AUTHOR]

Published

2024

176. Raw data for the identification of SUMOylated proteins in S. cerevisiae subjected to two types of osmotic shock, using affinity purification coupled with mass spectrometry.

Author

Srikumar T, Lewicki MC, and Raught B

Abstract

The small ubiquitin-related modifier (SUMO) "stress response" (SSR) is a poorly understood evolutionarily conserved phenomenon in which steady-state SUMO conjugate levels are dramatically increased in response to environmental stresses. Here we describe the data acquired using affinity-purification coupled with mass spectrometry to identify proteins that are SUMOylated in response to two different types of osmotic stress, 1 M sorbitol and 1 M KCl. The mass spectrometry dataset described here has been uploaded to the MassIVE repository with ID: MSV000078739, and consists of 32 raw MS files acquired in data-dependent mode on a Thermo Q-Exactive instrument. iProphet-processed MS/MS search results and associated SAINT scores are also included as a reference. These data are discussed and interpreted in "The S. cerevisiae SUMO stress response is a conjugation-deconjugation cycle that targets the transcription machinery", by Lewicki et al. in the Journal of Proteomics, 2014 [1].

Published

2014

177. BioID data of c-MYC interacting protein partners in cultured cells and xenograft tumors.

Author

Chan PK, Srikumar T, Dingar D, Kalkat M, Penn LZ, and Raught B

Abstract

BioID was performed using FlagBirA⁎ (the R118G biotin ligase mutant protein) and FlagBirA⁎-Myc in HEK293 T-REx cells maintained both under standard cell culture conditions and as mouse xenografts. The mass spectrometry dataset acquired in this study has been uploaded to the MassIVE repository with ID: MSV000078518, and consists of 28 ⁎.raw MS files acquired on an Orbitrap Velos instrument, collected in data-dependent mode. iProphet processed MS/MS search results are also included as a reference. This study has been published as "BioID identifies novel c-MYC interacting partners in cultured cells and xenograft tumors", by Dingar et al. in the Journal of Proteomics, 2014 [1].

Published

2014

178. Src promotes GTPase activity of Ras via tyrosine 32 phosphorylation.

Author

Bunda S, Heir P, Srikumar T, Cook JD, Burrell K, Kano Y, Lee JE, Zadeh G, Raught B, and Ohh M

Subjects

Amino Acid Sequence, Animals, Cell Line, GTP Phosphohydrolases chemistry, GTPase-Activating Proteins metabolism, Guanosine Triphosphate metabolism, Humans, Hydrolysis, Membrane Proteins chemistry, Mice, Models, Molecular, Molecular Sequence Data, Mutant Proteins metabolism, Phosphorylation, Protein Binding, raf Kinases metabolism, GTP Phosphohydrolases metabolism, Membrane Proteins metabolism, Phosphotyrosine metabolism, src-Family Kinases metabolism

Abstract

Mutations in Ras GTPase and various other components of the Ras signaling pathways are among the most common genetic alterations in human cancers and also have been identified in several familial developmental syndromes. Over the past few decades it has become clear that the activity or the oncogenic potential of Ras is dependent on the nonreceptor tyrosine kinase Src to promote the Ras/Raf/MAPK pathway essential for proliferation, differentiation, and survival of eukaryotic cells. However, no direct relationship between Ras and Src has been established. We show here that Src binds to and phosphorylates GTP-, but not GDP-, loaded Ras on a conserved Y32 residue within the switch I region in vitro and that in vivo, Ras-Y32 phosphorylation markedly reduces the binding to effector Raf and concomitantly increases binding to GTPase-activating proteins and the rate of GTP hydrolysis. These results suggest that, in the context of predetermined crystallographic structures, Ras-Y32 serves as an Src-dependent keystone regulatory residue that modulates Ras GTPase activity and ensures unidirectionality to the Ras GTPase cycle.

Published

2014

179. Proteomic analyses of CSF aimed at biomarker development for pediatric brain tumors.

Author

Samuel N, Remke M, Rutka JT, Raught B, and Malkin D

Subjects

Animals, Biomarkers cerebrospinal fluid, Child, Humans, Brain Neoplasms cerebrospinal fluid, Proteomics methods

Abstract

Primary brain tumors cumulatively represent the most common solid tumors of childhood and are the leading cause of cancer related death in this age group. Traditionally, molecular findings and histological analyses from biopsies of resected tumor tissue have been used for diagnosis and classification of these diseases. However, there is a dearth of useful biomarkers that have been validated and clinically implemented for pediatric brain tumors. Notably, diseases of the central nervous system (CNS) can be assayed through analysis of cerebrospinal fluid (CSF) and as such, CSF represents an appropriate medium to obtain liquid biopsies that can be informative for diagnosis, disease classification and risk stratification. Proteomic profiling of pediatric CNS malignancies has identified putative protein markers of disease, yet few effective biomarkers have been clinically validated or implemented. Advances in protein quantification techniques have made it possible to conduct such investigations rapidly and accurately through proteome-wide analyses. This review summarizes the current literature on proteomics in pediatric neuro-oncology and discusses the implications for clinical applications of proteomics research. We also outline strategies for translating effective CSF proteomic studies into clinical applications to optimize the care of this patient population.

Published

2014

180. RNF168 ubiquitylates 53BP1 and controls its response to DNA double-strand breaks.

Author

Bohgaki M, Bohgaki T, El Ghamrasni S, Srikumar T, Maire G, Panier S, Fradet-Turcotte A, Stewart GS, Raught B, Hakem A, and Hakem R

Subjects

Animals, DNA Repair genetics, Fibroblasts, HEK293 Cells, Humans, Intracellular Signaling Peptides and Proteins physiology, Mice, Tumor Suppressor p53-Binding Protein 1, DNA Breaks, Double-Stranded, DNA Repair physiology, Intracellular Signaling Peptides and Proteins metabolism, Ubiquitin-Protein Ligases metabolism, Ubiquitination physiology

Abstract

Defective signaling or repair of DNA double-strand breaks has been associated with developmental defects and human diseases. The E3 ligase RING finger 168 (RNF168), mutated in the human radiosensitivity, immunodeficiency, dysmorphic features, and learning difficulties syndrome, was shown to ubiquitylate H2A-type histones, and this ubiquitylation was proposed to facilitate the recruitment of p53-binding protein 1 (53BP1) to the sites of DNA double-strand breaks. In contrast to more upstream proteins signaling DNA double-strand breaks (e.g., RNF8), deficiency of RNF168 fully prevents both the initial recruitment to and retention of 53BP1 at sites of DNA damage; however, the mechanism for this difference has remained unclear. Here, we identify mechanisms that regulate 53BP1 recruitment to the sites of DNA double-strand breaks and provide evidence that RNF168 plays a central role in the regulation of 53BP1 functions. RNF168 mediates K63-linked ubiquitylation of 53BP1 which is required for the initial recruitment of 53BP1 to sites of DNA double-strand breaks and for its function in DNA damage repair, checkpoint activation, and genomic integrity. Our findings highlight the multistep roles of RNF168 in signaling DNA damage.

Published

2013

181. Hierarchical phosphorylation of the translation inhibitor 4E-BP1.

Author

Gingras, A C, Raught, B, Gygi, S P, Niedzwiecka, A, Miron, M, Burley, S K, Polakiewicz, R D, Wyslouch-Cieszynska, A, Aebersold, R, and Sonenberg, N

Abstract

In most instances, translation is regulated at the initiation phase, when a ribosome is recruited to the 5' end of an mRNA. The eIF4E-binding proteins (4E-BPs) interdict translation initiation by binding to the translation factor eIF4E, and preventing recruitment of the translation machinery to mRNA. The 4E-BPs inhibit translation in a reversible manner. Hypophosphorylated 4E-BPs interact avidly with eIF4E, whereas 4E-BP hyperphosphorylation, elicited by stimulation of cells with hormones, cytokines, or growth factors, results in an abrogation of eIF4E-binding activity. We reported previously that phosphorylation of 4E-BP1 on Thr 37 and Thr 46 is relatively insensitive to serum deprivation and rapamycin treatment, and that phosphorylation of these residues is required for the subsequent phosphorylation of a set of unidentified serum-responsive sites. Here, using mass spectrometry, we identify the serum-responsive, rapamycin-sensitive sites as Ser 65 and Thr 70. Utilizing a novel combination of two-dimensional isoelectric focusing/SDS-PAGE and Western blotting with phosphospecific antibodies, we also establish the order of 4E-BP1 phosphorylation in vivo; phosphorylation of Thr 37/Thr 46 is followed by Thr 70 phosphorylation, and Ser 65 is phosphorylated last. Finally, we show that phosphorylation of Ser 65 and Thr 70 alone is insufficient to block binding to eIF4E, indicating that a combination of phosphorylation events is necessary to dissociate 4E-BP1 from eIF4E.

Published

2001

182. Regulation of translation initiation by FRAP/mTOR.

Author

Gingras, A C, Raught, B, and Sonenberg, N

Published

2001

183. MYC phosphorylation at novel regulatory regions suppresses transforming activity.

Author

Wasylishen AR, Chan-Seng-Yue M, Bros C, Dingar D, Tu WB, Kalkat M, Chan PK, Mullen PJ, Huang L, Meyer N, Raught B, Boutros PC, and Penn LZ

Subjects

Apoptosis, Biomarkers, Tumor metabolism, Blotting, Western, Cell Adhesion, Cell Proliferation, Cell Transformation, Neoplastic genetics, Cells, Cultured, Chromatin Immunoprecipitation, Colony-Forming Units Assay, Epithelial Cells metabolism, Epithelial Cells pathology, Female, Gene Expression Profiling, Humans, Mammary Glands, Human metabolism, Neuroblastoma genetics, Neuroblastoma metabolism, Oligonucleotide Array Sequence Analysis, Oxygen Consumption, Phosphorylation, Proto-Oncogene Proteins c-myc genetics, RNA, Messenger genetics, Real-Time Polymerase Chain Reaction, Regulatory Sequences, Nucleic Acid, Reverse Transcriptase Polymerase Chain Reaction, Biomarkers, Tumor genetics, Cell Transformation, Neoplastic pathology, Gene Expression Regulation, Neoplastic, Mammary Glands, Human pathology, Mutation genetics, Neuroblastoma pathology, Proto-Oncogene Proteins c-myc metabolism

Abstract

Despite its central role in human cancer, MYC deregulation is insufficient by itself to transform cells. Because inherent mechanisms of neoplastic control prevent precancerous lesions from becoming fully malignant, identifying transforming alleles of MYC that bypass such controls may provide fundamental insights into tumorigenesis. To date, the only activated allele of MYC known is T58A, the study of which led to identification of the tumor suppressor FBXW7 and its regulator USP28 as a novel therapeutic target. In this study, we screened a panel of MYC phosphorylation mutants for their ability to promote anchorage-independent colony growth of human MCF10A mammary epithelial cells, identifying S71A/S81A and T343A/S344A/S347A/S348A as more potent oncogenic mutants compared with wild-type (WT) MYC. The increased cell-transforming activity of these mutants was confirmed in SH-EP neuroblastoma cells and in three-dimensional MCF10A acini. Mechanistic investigations initiated by a genome-wide mRNA expression analysis of MCF10A acini identified 158 genes regulated by the mutant MYC alleles, compared with only 112 genes regulated by both WT and mutant alleles. Transcriptional gain-of-function was a common feature of the mutant alleles, with many additional genes uniquely dysregulated by individual mutant. Our work identifies novel sites of negative regulation in MYC and thus new sites for its therapeutic attack.

Published

2013

184. The CRAPome: a contaminant repository for affinity purification-mass spectrometry data.

Author

Mellacheruvu D, Wright Z, Couzens AL, Lambert JP, St-Denis NA, Li T, Miteva YV, Hauri S, Sardiu ME, Low TY, Halim VA, Bagshaw RD, Hubner NC, Al-Hakim A, Bouchard A, Faubert D, Fermin D, Dunham WH, Goudreault M, Lin ZY, Badillo BG, Pawson T, Durocher D, Coulombe B, Aebersold R, Superti-Furga G, Colinge J, Heck AJ, Choi H, Gstaiger M, Mohammed S, Cristea IM, Bennett KL, Washburn MP, Raught B, Ewing RM, Gingras AC, and Nesvizhskii AI

Subjects

Databases, Factual, Humans, Chromatography, Affinity methods, Mass Spectrometry methods, Protein Interaction Mapping methods, Proteins analysis, Proteomics methods

Abstract

Affinity purification coupled with mass spectrometry (AP-MS) is a widely used approach for the identification of protein-protein interactions. However, for any given protein of interest, determining which of the identified polypeptides represent bona fide interactors versus those that are background contaminants (for example, proteins that interact with the solid-phase support, affinity reagent or epitope tag) is a challenging task. The standard approach is to identify nonspecific interactions using one or more negative-control purifications, but many small-scale AP-MS studies do not capture a complete, accurate background protein set when available controls are limited. Fortunately, negative controls are largely bait independent. Hence, aggregating negative controls from multiple AP-MS studies can increase coverage and improve the characterization of background associated with a given experimental protocol. Here we present the contaminant repository for affinity purification (the CRAPome) and describe its use for scoring protein-protein interactions. The repository (currently available for Homo sapiens and Saccharomyces cerevisiae) and computational tools are freely accessible at http://www.crapome.org/.

Published

2013

185. CEP120 and SPICE1 cooperate with CPAP in centriole elongation.

Author

Comartin D, Gupta GD, Fussner E, Coyaud É, Hasegan M, Archinti M, Cheung SW, Pinchev D, Lawo S, Raught B, Bazett-Jones DP, Lüders J, and Pelletier L

Subjects

Cell Cycle, Cell Cycle Proteins metabolism, Cell Line, Tumor, Centrioles ultrastructure, HeLa Cells, Humans, Microscopy, Immunoelectron, Microtubule-Associated Proteins metabolism, Microtubules ultrastructure, Cell Cycle Proteins genetics, Centrioles metabolism, Microtubule-Associated Proteins genetics, Microtubules metabolism

Abstract

Centrosomes organize microtubule (MT) arrays and are comprised of centrioles surrounded by ordered pericentriolar proteins. Centrioles are barrel-shaped structures composed of MTs, and as basal bodies they template the formation of cilia/flagella. Defects in centriole assembly can lead to ciliopathies and genome instability. The assembly of procentrioles requires a set of conserved proteins. It is initiated at the G1-to-S transition by PLK4 and CEP152, which help recruit SASS6 and STIL to the vicinity of the mother centriole to organize the cartwheel. Subsequently, CPAP promotes centriolar MT assembly and elongation in G2. While centriole integrity is maintained by CEP135 and POC1 through MT stabilization, centriole elongation requires POC5 and is restricted by CP110 and CEP97. How strict control of centriole length is achieved remains unclear. Here, we show that CEP120 and SPICE1 are required to localize CEP135 (but not SASS6, STIL, or CPAP) to procentrioles. CEP120 associates with SPICE1 and CPAP, and depletion of any of these proteins results in short procentrioles. Furthermore, CEP120 or CPAP overexpression results in excessive centriole elongation, a process dependent on CEP120, SPICE1, and CPAP. Our findings identify a shared function for these proteins in centriole length control., (Copyright © 2013 Elsevier Ltd. All rights reserved.)

Published

2013

186. The linear ubiquitin-specific deubiquitinase gumby regulates angiogenesis.

Author

Rivkin E, Almeida SM, Ceccarelli DF, Juang YC, MacLean TA, Srikumar T, Huang H, Dunham WH, Fukumura R, Xie G, Gondo Y, Raught B, Gingras AC, Sicheri F, and Cordes SP

Subjects

Adaptor Proteins, Signal Transducing metabolism, Alleles, Amino Acid Sequence, Animals, Base Sequence, Crystallography, X-Ray, Dishevelled Proteins, Embryo, Mammalian blood supply, Embryo, Mammalian embryology, Embryo, Mammalian metabolism, Endopeptidases deficiency, Endopeptidases genetics, Female, Gene Expression Profiling, HEK293 Cells, Humans, Mice, Models, Molecular, Molecular Sequence Data, Phenotype, Phosphoproteins metabolism, Protein Conformation, Ubiquitin-Protein Ligases metabolism, Wnt Signaling Pathway, Endopeptidases chemistry, Endopeptidases metabolism, Neovascularization, Physiologic genetics, Ubiquitin chemistry, Ubiquitin metabolism, Ubiquitination

Abstract

A complex interaction of signalling events, including the Wnt pathway, regulates sprouting of blood vessels from pre-existing vasculature during angiogenesis. Here we show that two distinct mutations in the (uro)chordate-specific gumby (also called Fam105b) gene cause an embryonic angiogenic phenotype in gumby mice. Gumby interacts with disheveled 2 (DVL2), is expressed in canonical Wnt-responsive endothelial cells and encodes an ovarian tumour domain class of deubiquitinase that specifically cleaves linear ubiquitin linkages. A crystal structure of gumby in complex with linear diubiquitin reveals how the identified mutations adversely affect substrate binding and catalytic function in line with the severity of their angiogenic phenotypes. Gumby interacts with HOIP (also called RNF31), a key component of the linear ubiquitin assembly complex, and decreases linear ubiquitination and activation of NF-κB-dependent transcription. This work provides support for the biological importance of linear (de)ubiquitination in angiogenesis, craniofacial and neural development and in modulating Wnt signalling.

Published

2013

187. A global S. cerevisiae small ubiquitin-related modifier (SUMO) system interactome.

Author

Srikumar T, Lewicki MC, and Raught B

Subjects

Cell Cycle genetics, Cysteine Endopeptidases genetics, Cysteine Endopeptidases metabolism, DNA, Ribosomal genetics, Endopeptidases genetics, Endopeptidases metabolism, Nuclear Pore Complex Proteins genetics, Nuclear Pore Complex Proteins metabolism, Protein Interaction Mapping, Saccharomyces cerevisiae metabolism, Saccharomyces cerevisiae Proteins genetics, Saccharomyces cerevisiae Proteins metabolism, Signal Transduction, Small Ubiquitin-Related Modifier Proteins metabolism, Ubiquitin genetics, Ubiquitin metabolism, Ubiquitin-Conjugating Enzymes genetics, Ubiquitin-Conjugating Enzymes metabolism, Ubiquitin-Protein Ligases genetics, Ubiquitin-Protein Ligases metabolism, Gene Expression Regulation, Fungal, Saccharomyces cerevisiae genetics, Small Ubiquitin-Related Modifier Proteins genetics, Transcriptome

Abstract

The small ubiquitin-related modifier (SUMO) system has been implicated in a number of biological functions, yet the individual components of the SUMO machinery involved in each of these activities were largely unknown. Here we report the first global SUMO system interactome. Using affinity purification coupled with mass spectrometry, we identify >450 protein-protein interactions surrounding the SUMO E2, Siz type E3s and SUMO-specific proteases in budding yeast. Exploiting this information-rich resource, we validate several Siz1- and Siz2-specific substrates, identify a nucleoporin required for proper Ulp1 localization, and uncover important new roles for Ubc9 and Ulp2 in the maintenance of ribosomal DNA.

Published

2013

188. Global analysis of SUMO chain function reveals multiple roles in chromatin regulation.

Author

Srikumar T, Lewicki MC, Costanzo M, Tkach JM, van Bakel H, Tsui K, Johnson ES, Brown GW, Andrews BJ, Boone C, Giaever G, Nislow C, and Raught B

Subjects

Chromatin genetics, Mutation, RNA, Fungal genetics, RNA, Fungal metabolism, RNA, Messenger genetics, RNA, Messenger metabolism, SUMO-1 Protein genetics, Saccharomyces cerevisiae genetics, Saccharomyces cerevisiae Proteins genetics, Saccharomyces cerevisiae Proteins metabolism, Small Ubiquitin-Related Modifier Proteins genetics, Small Ubiquitin-Related Modifier Proteins metabolism, Chromatin metabolism, SUMO-1 Protein metabolism, Saccharomyces cerevisiae metabolism, Sumoylation physiology

Abstract

Like ubiquitin, the small ubiquitin-related modifier (SUMO) proteins can form oligomeric "chains," but the biological functions of these superstructures are not well understood. Here, we created mutant yeast strains unable to synthesize SUMO chains (smt3(allR)) and subjected them to high-content microscopic screening, synthetic genetic array (SGA) analysis, and high-density transcript profiling to perform the first global analysis of SUMO chain function. This comprehensive assessment identified 144 proteins with altered localization or intensity in smt3(allR) cells, 149 synthetic genetic interactions, and 225 mRNA transcripts (primarily consisting of stress- and nutrient-response genes) that displayed a >1.5-fold increase in expression levels. This information-rich resource strongly implicates SUMO chains in the regulation of chromatin. Indeed, using several different approaches, we demonstrate that SUMO chains are required for the maintenance of normal higher-order chromatin structure and transcriptional repression of environmental stress response genes in budding yeast.

Published

2013

189. A strategy for modulation of enzymes in the ubiquitin system.

Author

Ernst A, Avvakumov G, Tong J, Fan Y, Zhao Y, Alberts P, Persaud A, Walker JR, Neculai AM, Neculai D, Vorobyov A, Garg P, Beatty L, Chan PK, Juang YC, Landry MC, Yeh C, Zeqiraj E, Karamboulas K, Allali-Hassani A, Vedadi M, Tyers M, Moffat J, Sicheri F, Pelletier L, Durocher D, Raught B, Rotin D, Yang J, Moran MF, Dhe-Paganon S, and Sidhu SS

Subjects

Amino Acid Sequence, Conserved Sequence, Drug Design, Endopeptidases chemistry, HEK293 Cells, Humans, Molecular Sequence Data, Protease Inhibitors chemistry, Protease Inhibitors pharmacology, Protein Conformation, Protein Structure, Secondary, Small Molecule Libraries, Ubiquitin chemistry, Ubiquitin genetics, Ubiquitin Thiolesterase chemistry, Ubiquitin-Conjugating Enzymes chemistry, Ubiquitin-Conjugating Enzymes metabolism, Ubiquitin-Protein Ligases chemistry, Ubiquitin-Protein Ligases metabolism, Combinatorial Chemistry Techniques, Endopeptidases metabolism, Protease Inhibitors isolation & purification, Ubiquitin metabolism, Ubiquitin Thiolesterase metabolism, Ubiquitination drug effects

Abstract

The ubiquitin system regulates virtually all aspects of cellular function. We report a method to target the myriad enzymes that govern ubiquitination of protein substrates. We used massively diverse combinatorial libraries of ubiquitin variants to develop inhibitors of four deubiquitinases (DUBs) and analyzed the DUB-inhibitor complexes with crystallography. We extended the selection strategy to the ubiquitin conjugating (E2) and ubiquitin ligase (E3) enzymes and found that ubiquitin variants can also enhance enzyme activity. Last, we showed that ubiquitin variants can bind selectively to ubiquitin-binding domains. Ubiquitin variants exhibit selective function in cells and thus enable orthogonal modulation of specific enzymatic steps in the ubiquitin system.

Published

2013

190. A pathogen type III effector with a novel E3 ubiquitin ligase architecture.

Author

Singer AU, Schulze S, Skarina T, Xu X, Cui H, Eschen-Lippold L, Egler M, Srikumar T, Raught B, Lee J, Scheel D, Savchenko A, and Bonas U

Subjects

Amino Acid Motifs, Amino Acid Sequence, Amino Acids genetics, Amino Acids metabolism, Bacterial Outer Membrane Proteins chemistry, Bacterial Proteins chemistry, Cell Death, Crystallization, Molecular Sequence Data, Mutation, Plant Diseases microbiology, Plant Immunity, Protein Sorting Signals, Protein Structure, Tertiary, Ubiquitin-Protein Ligases chemistry, Virulence, Virulence Factors chemistry, Xanthomonas campestris physiology, Bacterial Outer Membrane Proteins metabolism, Bacterial Proteins metabolism, Host-Pathogen Interactions immunology, Plant Diseases immunology, Ubiquitin-Protein Ligases metabolism, Virulence Factors metabolism, Xanthomonas campestris pathogenicity

Abstract

Type III effectors are virulence factors of Gram-negative bacterial pathogens delivered directly into host cells by the type III secretion nanomachine where they manipulate host cell processes such as the innate immunity and gene expression. Here, we show that the novel type III effector XopL from the model plant pathogen Xanthomonas campestris pv. vesicatoria exhibits E3 ubiquitin ligase activity in vitro and in planta, induces plant cell death and subverts plant immunity. E3 ligase activity is associated with the C-terminal region of XopL, which specifically interacts with plant E2 ubiquitin conjugating enzymes and mediates formation of predominantly K11-linked polyubiquitin chains. The crystal structure of the XopL C-terminal domain revealed a single domain with a novel fold, termed XL-box, not present in any previously characterized E3 ligase. Mutation of amino acids in the central cavity of the XL-box disrupts E3 ligase activity and prevents XopL-induced plant cell death. The lack of cysteine residues in the XL-box suggests the absence of thioester-linked ubiquitin-E3 ligase intermediates and a non-catalytic mechanism for XopL-mediated ubiquitination. The crystal structure of the N-terminal region of XopL confirmed the presence of a leucine-rich repeat (LRR) domain, which may serve as a protein-protein interaction module for ubiquitination target recognition. While the E3 ligase activity is required to provoke plant cell death, suppression of PAMP responses solely depends on the N-terminal LRR domain. Taken together, the unique structural fold of the E3 ubiquitin ligase domain within the Xanthomonas XopL is unprecedented and highlights the variation in bacterial pathogen effectors mimicking this eukaryote-specific activity.

Published

2013

191. The hGIDGID4 E3 ubiquitin ligase complex targets ARHGAP11A to regulate cell migration.

Author

Bagci, Halil, Winkler, Martin, Grädel, Benjamin, Uliana, Federico, Boulais, Jonathan, Mohamed, Weaam I., Park, Sophia L., Côté, Jean-François, Pertz, Olivier, and Peter, Matthias

Published

2024

192. Using ProHits to store, annotate, and analyze affinity purification-mass spectrometry (AP-MS) data.

Author

Liu G, Zhang J, Choi H, Lambert JP, Srikumar T, Larsen B, Nesvizhskii AI, Raught B, Tyers M, and Gingras AC

Subjects

Chromatography, Affinity methods, Databases, Protein, Mass Spectrometry methods, Proteins chemistry, Proteomics methods, Software

Abstract

Affinity purification coupled with mass spectrometry (AP-MS) is a robust technique used to identify protein-protein interactions. With recent improvements in sample preparation, and dramatic advances in MS instrumentation speed and sensitivity, this technique is becoming more widely used throughout the scientific community. To meet the needs of research groups both large and small, we have developed software solutions for tracking, scoring and analyzing AP-MS data. Here, we provide details for the installation and utilization of ProHits, a Laboratory Information Management System designed specifically for AP-MS interaction proteomics. This protocol explains: (i) how to install the complete ProHits system, including modules for the management of mass spectrometry files and the analysis of interaction data, and (ii) alternative options for the use of pre-existing search results in simpler versions of ProHits, including a virtual machine implementation of our ProHits Lite software. We also describe how to use the main features of the software to analyze AP-MS data.

Published

2012

193. Beyond hairballs: The use of quantitative mass spectrometry data to understand protein-protein interactions.

Author

Gingras AC and Raught B

Subjects

Animals, Cell Line, DNA, Complementary metabolism, Databases, Protein, Humans, Models, Biological, Open Reading Frames, Peptides chemistry, Proteins chemistry, Proteomics methods, Software, Computational Biology methods, Mass Spectrometry methods, Protein Interaction Mapping methods

Abstract

The past 10 years have witnessed a dramatic proliferation in the availability of protein interaction data. However, for interaction mapping based on affinity purification coupled with mass spectrometry (AP-MS), there is a wealth of information present in the datasets that often goes unrecorded in public repositories, and as such remains largely unexplored. Further, how this type of data is represented and used by bioinformaticians has not been well established. Here, we point out some common mistakes in how AP-MS data are handled, and describe how protein complex organization and interaction dynamics can be inferred using quantitative AP-MS approaches., (Copyright © 2012 Federation of European Biochemical Societies. Published by Elsevier B.V. All rights reserved.)

Published

2012

194. A human ubiquitin conjugating enzyme (E2)-HECT E3 ligase structure-function screen.

Author

Sheng Y, Hong JH, Doherty R, Srikumar T, Shloush J, Avvakumov GV, Walker JR, Xue S, Neculai D, Wan JW, Kim SK, Arrowsmith CH, Raught B, and Dhe-Paganon S

Subjects

Amino Acid Sequence, Blotting, Western, Catalytic Domain, Evolution, Molecular, Humans, Mass Spectrometry, Models, Molecular, Phylogeny, Protein Binding, Sequence Homology, Amino Acid, Static Electricity, Surface Properties, Ubiquitin metabolism, Ubiquitin-Conjugating Enzymes genetics, Ubiquitin-Conjugating Enzymes metabolism, Ubiquitin-Protein Ligases classification, Ubiquitin-Protein Ligases metabolism, Ubiquitination, Protein Structure, Tertiary, Ubiquitin chemistry, Ubiquitin-Conjugating Enzymes chemistry, Ubiquitin-Protein Ligases chemistry

Abstract

Here we describe a systematic structure-function analysis of the human ubiquitin (Ub) E2 conjugating proteins, consisting of the determination of 15 new high-resolution three-dimensional structures of E2 catalytic domains, and autoubiquitylation assays for 26 Ub-loading E2s screened against a panel of nine different HECT (homologous to E6-AP carboxyl terminus) E3 ligase domains. Integration of our structural and biochemical data revealed several E2 surface properties associated with Ub chain building activity; (1) net positive or neutral E2 charge, (2) an "acidic trough" located near the catalytic Cys, surrounded by an extensive basic region, and (3) similarity to the previously described HECT binding signature in UBE2L3 (UbcH7). Mass spectrometry was used to characterize the autoubiquitylation products of a number of functional E2-HECT pairs, and demonstrated that HECT domains from different subfamilies catalyze the formation of very different types of Ub chains, largely independent of the E2 in the reaction. Our data set represents the first comprehensive analysis of E2-HECT E3 interactions, and thus provides a framework for better understanding the molecular mechanisms of ubiquitylation.

Published

2012

195. Proteomic profiling of the human cytomegalovirus UL35 gene products reveals a role for UL35 in the DNA repair response.

Author

Salsman J, Jagannathan M, Paladino P, Chan PK, Dellaire G, Raught B, and Frappier L

Subjects

Carrier Proteins genetics, Carrier Proteins metabolism, Cell Cycle, Cell Line, Cytomegalovirus genetics, Cytomegalovirus Infections metabolism, Cytomegalovirus Infections physiopathology, Gene Expression Regulation, Viral, Host-Pathogen Interactions, Humans, Protein Binding, Protein Serine-Threonine Kinases, Ubiquitin Thiolesterase genetics, Ubiquitin Thiolesterase metabolism, Ubiquitin-Protein Ligases, Ubiquitin-Specific Peptidase 7, Viral Proteins genetics, Cytomegalovirus metabolism, Cytomegalovirus Infections genetics, Cytomegalovirus Infections virology, DNA Repair, Proteomics, Viral Proteins metabolism

Abstract

Human cytomegalovirus infections involve the extensive modification of host cell pathways, including cell cycle control, the regulation of the DNA damage response, and averting promyelocytic leukemia (PML)-mediated antiviral responses. The UL35 gene from human cytomegalovirus is important for viral gene expression and efficient replication and encodes two proteins, UL35 and UL35a, whose mechanism of action is not well understood. Here, affinity purification coupled with mass spectrometry was used to identify previously unknown human cellular targets of UL35 and UL35a. We demonstrate that both viral proteins interact with the ubiquitin-specific protease USP7, and that UL35 expression can alter USP7 subcellular localization. In addition, UL35 (but not UL35a) was found to associate with three components of the Cul4(DCAF1) E3 ubiquitin ligase complex (DCAF1, DDB1, and DDA1) previously shown to be targeted by the HIV-1 Vpr protein. The coimmunoprecipitation and immunofluorescence microscopy of DCAF1 mutants revealed that the C-terminal region of DCAF1 is required for association with UL35 and mediates the dramatic relocalization of DCAF1 to UL35 nuclear bodies, which also contain conjugated ubiquitin. As previously reported for the Vpr-DCAF1 interaction, UL35 (but not UL35a) expression resulted in the accumulation of cells in the G(2) phase of the cell cycle, which is typical of a DNA damage response, and activated the G(2) checkpoint in a DCAF1-dependent manner. In addition, UL35 (but not UL35a) induced γ-H2AX and 53BP1 foci, indicating the activation of DNA damage and repair responses. Therefore, the identified interactions suggest that UL35 can contribute to viral replication through the manipulation of host responses.

Published

2012

196. The SUMO-specific isopeptidase SENP2 associates dynamically with nuclear pore complexes through interactions with karyopherins and the Nup107-160 nucleoporin subcomplex.

Author

Goeres J, Chan PK, Mukhopadhyay D, Zhang H, Raught B, and Matunis MJ

Subjects

Active Transport, Cell Nucleus physiology, Amino Acid Motifs, Cysteine Endopeptidases genetics, HEK293 Cells, HeLa Cells, Humans, Karyopherins genetics, Multiprotein Complexes genetics, Multiprotein Complexes metabolism, Nuclear Localization Signals genetics, Nuclear Pore genetics, Nuclear Pore Complex Proteins genetics, Nuclear Proteins genetics, Protein Structure, Tertiary, SUMO-1 Protein genetics, SUMO-1 Protein metabolism, Cysteine Endopeptidases metabolism, Karyopherins metabolism, Nuclear Localization Signals metabolism, Nuclear Pore metabolism, Nuclear Pore Complex Proteins metabolism, Nuclear Proteins metabolism

Abstract

The association of small, ubiquitin-related modifier-specific isopeptidases (also known as sentrin-specific proteases, or SENPs) with nuclear pore complexes (NPCs) is conserved in eukaryotic organisms ranging from yeast to mammals. However, the functional significance of this association remains poorly understood, particularly in mammalian cells. In this study, we have characterized the molecular basis for interactions between SENP2 and NPCs in human cells. Using fluorescence recovery after photobleaching, we demonstrate that SENP2, although concentrated at the nuclear basket, is dynamically associated with NPCs. This association is mediated by multiple targeting elements within the N-terminus of SENP2 that function cooperatively to mediate NPC localization. One of these elements consists of a high-affinity nuclear localization signal that mediates indirect tethering to FG-repeat-containing nucleoporins through karyopherins. A second element mediates interactions with the Nup107-160 nucleoporin subcomplex. A third element consists of a nuclear export signal. Collectively, our findings reveal that SENP2 is tethered to NPCs through a complex interplay of interactions with nuclear import and export receptors and nucleoporins. Disruption of these interactions enhances SENP2 substrate accessibility, suggesting an important regulatory node in the SUMO pathway.

Published

2011

197. miRNA-mediated deadenylation is orchestrated by GW182 through two conserved motifs that interact with CCR4-NOT.

Author

Fabian MR, Cieplak MK, Frank F, Morita M, Green J, Srikumar T, Nagar B, Yamamoto T, Raught B, Duchaine TF, and Sonenberg N

Subjects

Amino Acid Motifs, Animals, Autoantigens chemistry, Autoantigens genetics, Carrier Proteins genetics, Carrier Proteins metabolism, Exoribonucleases genetics, Exoribonucleases metabolism, HeLa Cells, Humans, MicroRNAs genetics, Multiprotein Complexes chemistry, Protein Structure, Tertiary, RNA-Binding Proteins chemistry, RNA-Binding Proteins genetics, RNA-Induced Silencing Complex genetics, Transcription Factors chemistry, Transcription Factors genetics, Autoantigens metabolism, MicroRNAs metabolism, Multiprotein Complexes metabolism, RNA-Binding Proteins metabolism, RNA-Induced Silencing Complex metabolism, Transcription Factors metabolism

Abstract

miRNAs recruit the miRNA-induced silencing complex (miRISC), which includes Argonaute and GW182 as core proteins. GW182 proteins effect translational repression and deadenylation of target mRNAs. However, the molecular mechanisms of GW182-mediated repression remain obscure. We show here that human GW182 independently interacts with the PAN2-PAN3 and CCR4-NOT deadenylase complexes. Interaction of GW182 with CCR4-NOT is mediated by two newly discovered phylogenetically conserved motifs. Although either motif is sufficient to bind CCR4-NOT, only one of them can promote processive deadenylation of target mRNAs. Thus, GW182 serves as both a platform that recruits deadenylases and as a deadenylase coactivator that facilitates the removal of the poly(A) tail by CCR4-NOT.

Published

2011

198. The dynamics and mechanism of SUMO chain deconjugation by SUMO-specific proteases.

Author

Békés M, Prudden J, Srikumar T, Raught B, Boddy MN, and Salvesen GS

Subjects

HEK293 Cells, HeLa Cells, Humans, Peptide Hydrolases genetics, SUMO-1 Protein genetics, Schizosaccharomyces genetics, Schizosaccharomyces pombe Proteins genetics, Peptide Hydrolases metabolism, SUMO-1 Protein metabolism, Schizosaccharomyces metabolism, Schizosaccharomyces pombe Proteins metabolism, Sumoylation physiology

Abstract

SUMOylation of proteins is a cyclic process that requires both conjugation and deconjugation of SUMO moieties. Besides modification by a single SUMO, SUMO chains have also been observed, yet the dynamics of SUMO conjugation/deconjugation remain poorly understood. Using a non-deconjugatable form of SUMO we demonstrate the underappreciated existence of SUMO chains in vivo, we highlight the importance of SUMO deconjugation, and we demonstrate the highly dynamic nature of the SUMO system. We show that SUMO-specific proteases (SENPs) play a crucial role in the dynamics of SUMO chains in vivo by constant deconjugation. Preventing deSUMOylation in Schizosaccharomyces pombe results in slow growth and a sensitivity to replication stress, highlighting the biological requirement for deSUMOylation dynamics. Furthermore, we present the mechanism of SUMO chain deconjugation by SENPs, which occurs via a stochastic mechanism, resulting in cleavage anywhere within a chain. Our results offer mechanistic insights into the workings of deSUMOylating proteases and highlight their importance in the homeostasis of (poly)SUMO-modified substrates.

Published

2011

199. Structural and functional comparison of the RING domains of two p53 E3 ligases, Mdm2 and Pirh2.

Author

Shloush J, Vlassov JE, Engson I, Duan S, Saridakis V, Dhe-Paganon S, Raught B, Sheng Y, and Arrowsmith CH

Subjects

Binding Sites, Humans, Mutagenesis, Nuclear Magnetic Resonance, Biomolecular, Protein Multimerization, Proto-Oncogene Proteins c-mdm2 genetics, Proto-Oncogene Proteins c-mdm2 metabolism, RING Finger Domains, Structure-Activity Relationship, Tumor Suppressor Protein p53 genetics, Tumor Suppressor Protein p53 metabolism, Ubiquitin-Protein Ligases genetics, Ubiquitin-Protein Ligases metabolism, Proto-Oncogene Proteins c-mdm2 chemistry, Tumor Suppressor Protein p53 chemistry, Ubiquitin-Protein Ligases chemistry

Abstract

The tumor suppressor p53 maintains genome stability and prevents malignant transformation by promoting cell cycle arrest and apoptosis. Both Mdm2 and Pirh2 have been shown to ubiquitylate p53 through their RING domains, thereby targeting p53 for proteasomal degradation. Using structural and functional analyses, here we show that the Pirh2 RING domain differs from the Mdm2 RING domain in its oligomeric state, surface charge distribution, and zinc coordination scheme. Pirh2 also possesses weaker E3 ligase activity toward p53 and directs ubiquitin to different residues on p53. NMR and mutagenesis studies suggest that whereas Pirh2 and Mdm2 share a conserved E2 binding site, the seven C-terminal residues of the Mdm2 RING directly contribute to Mdm2 E3 ligase activity, a feature unique to Mdm2 and absent in the Pirh2 RING domain. This comprehensive analysis of the Pirh2 and Mdm2 RING domains provides structural and mechanistic insight into p53 regulation by its E3 ligases.

Published

2011

200. ProHits: integrated software for mass spectrometry-based interaction proteomics.

Author

Liu G, Zhang J, Larsen B, Stark C, Breitkreutz A, Lin ZY, Breitkreutz BJ, Ding Y, Colwill K, Pasculescu A, Pawson T, Wrana JL, Nesvizhskii AI, Raught B, Tyers M, and Gingras AC

Subjects

Databases, Protein, Protein Binding, Saccharomyces cerevisiae metabolism, Saccharomyces cerevisiae Proteins metabolism, Mass Spectrometry methods, Proteomics methods, Software

Published

2010