Your search keyword '"CELL cycle proteins"' showing total 71,690 results

1. Adenovirus small E1A directs activation of Alu transcription at YAP/TEAD- and AP-1-bound enhancers through interactions with the EP400 chromatin remodeler.

Author

Cantarella, Simona, Vezzoli, Marco, Carnevali, Davide, Morselli, Marco, Zemke, Nathan, Montanini, Barbara, Daussy, Coralie, Wodrich, Harald, Teichmann, Martin, Pellegrini, Matteo, Berk, Arnold, Dieci, Giorgio, and Ferrari, Roberto

Subjects

Humans, Enhancer Elements, Genetic, Alu Elements, Transcription Factors, Adenovirus E1A Proteins, DNA-Binding Proteins, DNA Helicases, Transcription Factor AP-1, Chromatin Assembly and Disassembly, YAP-Signaling Proteins, Adaptor Proteins, Signal Transducing, Cell Cycle Proteins, Transcriptional Activation, Phosphoproteins, Cells, Cultured, Fibroblasts, Histones, Nuclear Proteins, Transcription Factors, TFIII

Abstract

Alu retrotransposons, which form the largest family of mobile DNA elements in the human genome, have recently come to attention as a potential source of regulatory novelties, most notably by participating in enhancer function. Even though Alu transcription by RNA polymerase III is subjected to tight epigenetic silencing, their expression has long been known to increase in response to various types of stress, including viral infection. Here we show that, in primary human fibroblasts, adenovirus small e1a triggered derepression of hundreds of individual Alus by promoting TFIIIB recruitment by Alu-bound TFIIIC. Epigenome profiling revealed an e1a-induced decrease of H3K27 acetylation and increase of H3K4 monomethylation at derepressed Alus, making them resemble poised enhancers. The enhancer nature of e1a-targeted Alus was confirmed by the enrichment, in their upstream regions, of the EP300/CBP acetyltransferase, EP400 chromatin remodeler and YAP1 and FOS transcription factors. The physical interaction of e1a with EP400 was critical for Alu derepression, which was abrogated upon EP400 ablation. Our data suggest that e1a targets a subset of enhancer Alus whose transcriptional activation, which requires EP400 and is mediated by the e1a-EP400 interaction, may participate in the manipulation of enhancer activity by adenoviruses.

Published

2024

2. Mck1-mediated proteolysis of CENP-A prevents mislocalization of CENP-A for chromosomal stability in Saccharomyces cerevisiae.

Author

Zhang, Tianyi, Au, Wei-Chun, Ohkuni, Kentaro, Shrestha, Roshan, Kaiser, Peter, and Basrai, Munira

Subjects

CENP-A, Cdc4, Cse4, Mck1, centromere, Saccharomyces cerevisiae Proteins, Saccharomyces cerevisiae, Chromosomal Instability, Proteolysis, Chromosomal Proteins, Non-Histone, Centromere Protein A, Phosphorylation, DNA-Binding Proteins, Cell Cycle Proteins, Centromere, F-Box Proteins, Ubiquitin-Protein Ligase Complexes, Ubiquitin-Protein Ligases

Abstract

Centromeric localization of evolutionarily conserved CENP-A (Cse4 in Saccharomyces cerevisiae) is essential for chromosomal stability. Mislocalization of overexpressed CENP-A to noncentromeric regions contributes to chromosomal instability in yeasts, flies, and humans. Overexpression and mislocalization of CENP-A observed in many cancers are associated with poor prognosis. Previous studies have shown that F-box proteins, Cdc4 and Met30 of the Skp, Cullin, F-box ubiquitin ligase cooperatively regulate proteolysis of Cse4 to prevent Cse4 mislocalization and chromosomal instability under normal physiological conditions. Mck1-mediated phosphorylation of Skp, Cullin, F-box-Cdc4 substrates such as Cdc6 and Rcn1 enhances the interaction of the substrates with Cdc4. Here, we report that Mck1 interacts with Cse4, and Mck1-mediated proteolysis of Cse4 prevents Cse4 mislocalization for chromosomal stability. Our results showed that mck1Δ strain overexpressing CSE4 (GAL-CSE4) exhibits lethality, defects in ubiquitin-mediated proteolysis of Cse4, mislocalization of Cse4, and reduced Cse4-Cdc4 interaction. Strain expressing GAL-cse4-3A with mutations in three potential Mck1 phosphorylation consensus sites (S10, S16, and T166) also exhibits growth defects, increased stability with mislocalization of Cse4-3A, chromosomal instability, and reduced interaction with Cdc4. Constitutive expression of histone H3 (Δ16H3) suppresses the chromosomal instability phenotype of GAL-cse4-3A strain, suggesting that the chromosomal instability phenotype is linked to Cse4-3A mislocalization. We conclude that Mck1 and its three potential phosphorylation sites on Cse4 promote Cse4-Cdc4 interaction and this contributes to ubiquitin-mediated proteolysis of Cse4 preventing its mislocalization and chromosomal instability. These studies advance our understanding of pathways that regulate cellular levels of CENP-A to prevent mislocalization of CENP-A in human cancers.

Published

2024

3. Cohesin prevents cross-domain gene coactivation

Author

Dong, Peng, Zhang, Shu, Gandin, Valentina, Xie, Liangqi, Wang, Lihua, Lemire, Andrew L, Li, Wenhong, Otsuna, Hideo, Kawase, Takashi, Lander, Arthur D, Chang, Howard Y, and Liu, Zhe J

Subjects

Biochemistry and Cell Biology, Bioinformatics and Computational Biology, Genetics, Biological Sciences, Biotechnology, Human Genome, 1.1 Normal biological development and functioning, Generic health relevance, Cohesins, Cell Cycle Proteins, Chromosomal Proteins, Non-Histone, Chromatin, Gene Expression Regulation, Promoter Regions, Genetic, Single-Cell Analysis, Saccharomyces cerevisiae, Transcriptome, Medical and Health Sciences, Developmental Biology, Agricultural biotechnology, Bioinformatics and computational biology

Abstract

The contrast between the disruption of genome topology after cohesin loss and the lack of downstream gene expression changes instigates intense debates regarding the structure-function relationship between genome and gene regulation. Here, by analyzing transcriptome and chromatin accessibility at the single-cell level, we discover that, instead of dictating population-wide gene expression levels, cohesin supplies a general function to neutralize stochastic coexpression tendencies of cis-linked genes in single cells. Notably, cohesin loss induces widespread gene coactivation and chromatin co-opening tens of million bases apart in cis. Spatial genome and protein imaging reveals that cohesin prevents gene co-bursting along the chromosome and blocks spatial mixing of transcriptional hubs. Single-molecule imaging shows that cohesin confines the exploration of diverse enhancer and core promoter binding transcriptional regulators. Together, these results support that cohesin arranges nuclear topology to control gene coexpression in single cells.

Published

2024

4. A Phase II Trial of the WEE1 Inhibitor Adavosertib in SETD2-Altered Advanced Solid Tumor Malignancies (NCI 10170).

Author

Maldonado, Edward, Rathmell, W, Shapiro, Geoffrey, Takebe, Naoko, Rodon, Jordi, Mahalingam, Devalingam, Trikalinos, Nikolaos, Kalebasty, Arash, Parikh, Mamta, Boerner, Scott, Balido, Celene, Krings, Gregor, Burns, Timothy, Bergsland, Emily, Munster, Pamela, Ashworth, Alan, LoRusso, Patricia, and Aggarwal, Rahul

Subjects

Humans, Middle Aged, Histone-Lysine N-Methyltransferase, Male, Aged, Female, Protein-Tyrosine Kinases, Cell Cycle Proteins, Pyrazoles, Neoplasms, Carcinoma, Renal Cell, Kidney Neoplasms, Pyrimidinones, Mutation

Abstract

UNLABELLED: We sought to evaluate the efficacy of WEE1 inhibitor adavosertib in patients with solid tumor malignancies (cohort A) and clear cell renal cell carcinoma (ccRCC; cohort B). NCT03284385 was a parallel cohort, Simon two-stage, phase II study of adavosertib (300 mg QDAY by mouth on days 1-5 and 8-12 of each 21-day cycle) in patients with solid tumor malignancies harboring a pathogenic SETD2 mutation. The primary endpoint was the objective response rate. Correlative assays evaluated the loss of H3K36me3 by IHC, a downstream consequence of SETD2 loss, in archival tumor tissue. Eighteen patients were enrolled (9/cohort). The median age was 60 years (range 45-74). The median duration of treatment was 1.28 months (range 0-24+). No objective responses were observed in either cohort; accrual was halted following stage 1. Minor tumor regressions were observed in 4/18 (22%) evaluable patients. Stable disease (SD) was the best overall response in 10/18 (56%) patients, including three patients with SD > 4 months. One patient with ccRCC remains on treatment for >24 months. The most common adverse events of any grade were nausea (59%), anemia (41%), diarrhea (41%), and neutropenia (41%). Nine patients (50%) experienced a Grade ≥3 adverse event. Of eight evaluable archival tissue samples, six (75%) had a loss of H3K36me3 by IHC. Adavosertib failed to exhibit objective responses in SETD2-altered ccRCC and other solid tumor malignancies although prolonged SD was observed in a subset of patients. Combination approaches may yield greater depth of tumor response. SIGNIFICANCE: WEE1 inhibition with adavosertib monotherapy demonstrated limited clinical activity in patients with SETD2-altered solid tumors despite compelling preclinical data indicating a synthetic lethal effect, which did not translate into robust tumor regression. Loss of the H3K36me3 trimethylation mark caused by SETD2-deficiency was confirmed in the majority of evaluable tumors. A subset of patients derived clinical benefit as manifested by minor tumor regressions and prolonged SD.

Published

2024

5. Multi-step control of homologous recombination via Mec1/ATR suppresses chromosomal rearrangements

Author

Xie, Bokun, Sanford, Ethan James, Hung, Shih-Hsun, Wagner, Mateusz, Heyer, Wolf-Dietrich, and Smolka, Marcus B

Subjects

Biochemistry and Cell Biology, Biological Sciences, Genetics, Prevention, Human Genome, Saccharomyces cerevisiae Proteins, Saccharomyces cerevisiae, Protein Serine-Threonine Kinases, Homologous Recombination, Intracellular Signaling Peptides and Proteins, Cell Cycle Proteins, Checkpoint Kinase 2, RecQ Helicases, Signal Transduction, Phosphorylation, Chromosome Aberrations, Gene Rearrangement, Mec1, Sgs1, Resection, Chromosomal Rearrangement, Information and Computing Sciences, Medical and Health Sciences, Developmental Biology, Biological sciences, Biomedical and clinical sciences

Abstract

The Mec1/ATR kinase is crucial for genome stability, yet the mechanism by which it prevents gross chromosomal rearrangements (GCRs) remains unknown. Here we find that in cells with deficient Mec1 signaling, GCRs accumulate due to the deregulation of multiple steps in homologous recombination (HR). Mec1 primarily suppresses GCRs through its role in activating the canonical checkpoint kinase Rad53, which ensures the proper control of DNA end resection. Upon loss of Rad53 signaling and resection control, Mec1 becomes hyperactivated and triggers a salvage pathway in which the Sgs1 helicase is recruited to sites of DNA lesions via the 911-Dpb11 scaffolds and phosphorylated by Mec1 to favor heteroduplex rejection and limit HR-driven GCR accumulation. Fusing an ssDNA recognition domain to Sgs1 bypasses the requirement of Mec1 signaling for GCR suppression and nearly eliminates D-loop formation, thus preventing non-allelic recombination events. We propose that Mec1 regulates multiple steps of HR to prevent GCRs while ensuring balanced HR usage when needed for promoting tolerance to replication stress.

Published

2024

6. Cadmium binding by the F-box domain induces p97-mediated SCF complex disassembly to activate stress response programs.

Author

Lauinger, Linda, Andronicos, Anna, Flick, Karin, Yu, Clinton, Durairaj, Geetha, Huang, Lan, and Kaiser, Peter

Subjects

Cadmium, Protein Binding, SKP Cullin F-Box Protein Ligases, Valosin Containing Protein, Saccharomyces cerevisiae, Stress, Physiological, F-Box Proteins, Saccharomyces cerevisiae Proteins, Ubiquitination, Protein Domains, Humans, S-Phase Kinase-Associated Proteins, Cell Cycle Proteins

Abstract

The F-box domain is a highly conserved structural motif that defines the largest class of ubiquitin ligases, Skp1/Cullin1/F-box protein (SCF) complexes. The only known function of the F-box motif is to form the protein interaction surface with Skp1. Here we show that the F-box domain can function as an environmental sensor. We demonstrate that the F-box domain of Met30 is a cadmium sensor that blocks the activity of the SCFMet30 ubiquitin ligase during cadmium stress. Several highly conserved cysteine residues within the Met30 F-box contribute to binding of cadmium with a KD of 8 µM. Binding induces a conformational change that allows for Met30 autoubiquitylation, which in turn leads to recruitment of the segregase Cdc48/p97/VCP followed by active SCFMet30 disassembly. The resulting inactivation of SCFMet30 protects cells from cadmium stress. Our results show that F-box domains participate in regulation of SCF ligases beyond formation of the Skp1 binding interface.

Published

2024

7. Hippo-YAP/TAZ signalling coordinates adipose plasticity and energy balance by uncoupling leptin expression from fat mass.

Author

Choi, Sungwoo, Kang, Ju-Gyeong, Tran, Yen, Jeong, Sun-Hye, Park, Kun-Young, Shin, Hyemi, Kim, Young, Park, Myungsun, Nahmgoong, Hahn, Seol, Taejun, Jeon, Haeyon, Kim, Yeongmin, Park, Sanghee, Kim, Hee-Joo, Kim, Min-Seob, Li, Xiaoxu, Bou Sleiman, Maroun, Lee, Eries, Choi, Jinhyuk, Eisenbarth, David, Lee, Sang, Cho, Suhyeon, Auwerx, Johan, Kim, Il-Young, Kim, Jae, Park, Jong-Eun, Lim, Dae-Sik, Suh, Jae, and Moore, David

Subjects

Animals, Leptin, Signal Transduction, Energy Metabolism, Protein Serine-Threonine Kinases, Mice, Adaptor Proteins, Signal Transducing, YAP-Signaling Proteins, Adipose Tissue, Adipocytes, Hippo Signaling Pathway, Cell Cycle Proteins, Transcription Factors, Transcriptional Coactivator with PDZ-Binding Motif Proteins, Phosphoproteins, Tumor Suppressor Proteins, Trans-Activators

Abstract

Adipose tissues serve as an energy reservoir and endocrine organ, yet the mechanisms that coordinate these functions remain elusive. Here, we show that the transcriptional coregulators, YAP and TAZ, uncouple fat mass from leptin levels and regulate adipocyte plasticity to maintain metabolic homeostasis. Activating YAP/TAZ signalling in adipocytes by deletion of the upstream regulators Lats1 and Lats2 results in a profound reduction in fat mass by converting mature adipocytes into delipidated progenitor-like cells, but does not cause lipodystrophy-related metabolic dysfunction, due to a paradoxical increase in circulating leptin levels. Mechanistically, we demonstrate that YAP/TAZ-TEAD signalling upregulates leptin expression by directly binding to an upstream enhancer site of the leptin gene. We further show that YAP/TAZ activity is associated with, and functionally required for, leptin regulation during fasting and refeeding. These results suggest that adipocyte Hippo-YAP/TAZ signalling constitutes a nexus for coordinating adipose tissue lipid storage capacity and systemic energy balance through the regulation of adipocyte plasticity and leptin gene transcription.

Published

2024

8. Ribosome subunit attrition and activation of the p53-MDM4 axis dominate the response of MLL-rearranged cancer cells to WDR5 WIN site inhibition.

Author

Howard, Gregory, Wang, Jing, Rose, Kristie, Jones, Camden, Patel, Purvi, Tsui, Tina, Florian, Andrea, Vlach, Logan, Lorey, Shelly, Grieb, Brian, Smith, Brianna, Slota, Macey, Reynolds, Elizabeth, Goswami, Soumita, Savona, Michael, Mason, Frank, Lee, Taekyu, Fesik, Stephen, Liu, Qi, and Tansey, William

Subjects

WDR5, cancer biology, cancer therapy, chromosomes, gene expression, human, p53, ribosomes, Humans, Antineoplastic Agents, Cell Cycle Proteins, Cell Line, Tumor, Histone-Lysine N-Methyltransferase, Intracellular Signaling Peptides and Proteins, Myeloid-Lymphoid Leukemia Protein, Nuclear Proteins, Proto-Oncogene Proteins, Ribosomes, Tumor Suppressor Protein p53, Peptidomimetics

Abstract

The chromatin-associated protein WD Repeat Domain 5 (WDR5) is a promising target for cancer drug discovery, with most efforts blocking an arginine-binding cavity on the protein called the WIN site that tethers WDR5 to chromatin. WIN site inhibitors (WINi) are active against multiple cancer cell types in vitro, the most notable of which are those derived from MLL-rearranged (MLLr) leukemias. Peptidomimetic WINi were originally proposed to inhibit MLLr cells via dysregulation of genes connected to hematopoietic stem cell expansion. Our discovery and interrogation of small-molecule WINi, however, revealed that they act in MLLr cell lines to suppress ribosome protein gene (RPG) transcription, induce nucleolar stress, and activate p53. Because there is no precedent for an anticancer strategy that specifically targets RPG expression, we took an integrated multi-omics approach to further interrogate the mechanism of action of WINi in human MLLr cancer cells. We show that WINi induce depletion of the stock of ribosomes, accompanied by a broad yet modest translational choke and changes in alternative mRNA splicing that inactivate the p53 antagonist MDM4. We also show that WINi are synergistic with agents including venetoclax and BET-bromodomain inhibitors. Together, these studies reinforce the concept that WINi are a novel type of ribosome-directed anticancer therapy and provide a resource to support their clinical implementation in MLLr leukemias and other malignancies.

Published

2024

9. Gastrulation-stage gene expression in Nipbl+/− mouse embryos foreshadows the development of syndromic birth defects

Author

Chea, Stephenson, Kreger, Jesse, Lopez-Burks, Martha E, MacLean, Adam L, Lander, Arthur D, and Calof, Anne L

Subjects

Reproductive Medicine, Biomedical and Clinical Sciences, Cardiovascular, Congenital Structural Anomalies, Rare Diseases, Intellectual and Developmental Disabilities (IDD), Genetics, Pediatric, Brain Disorders, Animals, Mice, Cell Cycle Proteins, De Lange Syndrome, Gastrulation, Gene Expression, Mutation, Phenotype

Abstract

In animal models, Nipbl deficiency phenocopies gene expression changes and birth defects seen in Cornelia de Lange syndrome, the most common cause of which is Nipbl haploinsufficiency. Previous studies in Nipbl+/- mice suggested that heart development is abnormal as soon as cardiogenic tissue is formed. To investigate this, we performed single-cell RNA sequencing on wild-type and Nipbl+/- mouse embryos at gastrulation and early cardiac crescent stages. Nipbl+/- embryos had fewer mesoderm cells than wild-type and altered proportions of mesodermal cell subpopulations. These findings were associated with underexpression of genes implicated in driving specific mesodermal lineages. In addition, Nanog was found to be overexpressed in all germ layers, and many gene expression changes observed in Nipbl+/- embryos could be attributed to Nanog overexpression. These findings establish a link between Nipbl deficiency, Nanog overexpression, and gene expression dysregulation/lineage misallocation, which ultimately manifest as birth defects in Nipbl+/- animals and Cornelia de Lange syndrome.

Published

2024

10. The Arabidopsis BUB1/MAD3 family protein BMF3 requires BUB3.3 to recruit CDC20 to kinetochores in spindle assembly checkpoint signaling.

Author

Deng, Xingguang, Peng, Felicia Lei, Tang, Xiaoya, Lee, Yuh-Ru Julie, Lin, Hong-Hui, and Liu, Bo

Subjects

Biochemistry and Cell Biology, Biological Sciences, Genetics, 1.1 Normal biological development and functioning, Underpinning research, Generic health relevance, Animals, Kinetochores, Arabidopsis, M Phase Cell Cycle Checkpoints, Cell Cycle Proteins, Cell Cycle Checkpoints, Spindle Apparatus, BUB3, CDC20, kinetochore, spindle assembly checkpoint

Abstract

The spindle assembly checkpoint (SAC) ensures faithful chromosome segregation during cell division by monitoring kinetochore-microtubule attachment. Plants produce both sequence-conserved and diverged SAC components, and it has been largely unknown how SAC activation leads to the assembly of these proteins at unattached kinetochores to prevent cells from entering anaphase. In Arabidopsis thaliana, the noncanonical BUB3.3 protein was detected at kinetochores throughout mitosis, unlike MAD1 and the plant-specific BUB1/MAD3 family protein BMF3 that associated with unattached chromosomes only. When BUB3.3 was lost by a genetic mutation, mitotic cells often entered anaphase with misaligned chromosomes and presented lagging chromosomes after they were challenged by low doses of the microtubule depolymerizing agent oryzalin, resulting in the formation of micronuclei. Surprisingly, BUB3.3 was not required for the kinetochore localization of other SAC proteins or vice versa. Instead, BUB3.3 specifically bound to BMF3 through two internal repeat motifs that were not required for BMF3 kinetochore localization. This interaction enabled BMF3 to recruit CDC20, a downstream SAC target, to unattached kinetochores. Taken together, our findings demonstrate that plant SAC utilizes unconventional protein interactions for arresting mitosis, with BUB3.3 directing BMF3's role in CDC20 recruitment, rather than the recruitment of BUB1/MAD3 proteins observed in fungi and animals. This distinct mechanism highlights how plants adapted divergent versions of conserved cell cycle machinery to achieve specialized SAC control.

Published

2024

11. Molecular and clinicopathologic characteristics of CNS embryonal tumors with BRD4::LEUTX fusion.

Author

Andreiuolo, Felipe, Ferrone, Christina, Rajan, Sharika, Guney, Ekin, Cham, Elaine, Giannini, Caterina, Toland, Angus, Willard, Nicholas, de Souza, Andrea, Dazelle, Karen, Chung, Hye-Jung, Singh, Omkar, Conway, Kyle, Coley, Nicholas, Dampier, Christopher, Abdullaev, Zied, Pratt, Drew, Cimino, Patrick, Quezado, Martha, Aldape, Kenneth, and Perry, Arie

Subjects

BRD4::LEUTX, Embryonal tumor, Methylation, Humans, Brain Neoplasms, Nuclear Proteins, Transcription Factors, Central Nervous System Neoplasms, Neoplasms, Germ Cell and Embryonal, Bromodomain Containing Proteins, Cell Cycle Proteins, Forkhead Transcription Factors, Homeodomain Proteins

Abstract

Central nervous system (CNS) embryonal tumors are a heterogeneous group of high-grade malignancies, and the increasing clinical use of methylation profiling and next-generation sequencing has led to the identification of molecularly distinct subtypes. One proposed tumor type, CNS tumor with BRD4::LEUTX fusion, has been described. As only a few CNS tumors with BRD4::LEUTX fusions have been described, we herein characterize a cohort of 9 such cases (4 new, 5 previously published) to further describe their clinicopathologic and molecular features. We demonstrate that CNS embryonal tumor with BRD4::LEUTX fusion comprises a well-defined methylation class/cluster. We find that patients are young (4 years or younger), with large tumors at variable locations, and frequently with evidence of leptomeningeal/cerebrospinal fluid (CSF) dissemination. Histologically, tumors were highly cellular with high-grade embryonal features. Immunohistochemically, 5/5 cases showed synaptophysin and 4/5 showed OLIG2 expression, thus overlapping with CNS neuroblastoma, FOXR2-activated. DNA copy number profiles were generally flat; however, two tumors had chromosome 1q gains. No recurring genomic changes, besides the presence of the fusion, were found. The LEUTX portion of the fusion transcript was constant in all cases assessed, while the BRD4 portion varied but included a domain with proto-oncogenic activity in all cases. Two patients with clinical follow up available had tumors with excellent response to chemotherapy. Two of our patients were alive without evidence of recurrence or progression after gross total resection and chemotherapy at 16 and 33 months. One patient relapsed, and the last of our four patients died of disease one month after diagnosis. Overall, this case series provides additional evidence for this as a distinct tumor type defined by the presence of a specific fusion as well as a distinct DNA methylation signature. Studies on larger series are required to further characterize these tumors.

Published

2024

12. Bone scan findings of Pagets disease of bone in patients with VCP Multisystem Proteinopathy 1.

Author

Columbres, Rod, Din, Sarosh, Gibbs, Liliane, and Kimonis, Virginia

Subjects

Male, Female, Humans, Frontotemporal Dementia, Valosin Containing Protein, Cell Cycle Proteins, Osteitis Deformans, Merozoite Surface Protein 1, Tomography, X-Ray Computed, Mutation, Myositis, Inclusion Body, Muscular Dystrophies, Limb-Girdle

Abstract

Multisystem Proteinopathy 1 (MSP1) disease is a rare genetic disorder caused by mutations in the Valosin-Containing Protein (VCP) gene with clinical features of inclusion body myopathy (IBM), frontotemporal dementia (FTD), and Pagets disease of bone (PDB). We performed bone scan imaging in twelve patients (6 females, 6 males) with confirmed VCP gene mutation six (50%) of which has myopathy alone, four (33%) with both PDB and myopathy, and two (15%) were presymptomatic carriers. We aim to characterize the PDB in diagnosed individuals, and potentially identify PDB in the myopathy and presymptomatic groups. Interestingly, two patients with previously undiagnosed PDB had positive diagnostic findings on the bone scan and subsequent radiograph imaging. Among the individuals with PDB, increased radiotracer uptake of the affected bones were of typical distribution as seen in conventional PDB and those reported in other MSP1 cohorts which are the thoracic spine and ribs (75%), pelvis (75%), shoulder (75%) and calvarium (15%). Overall, we show that technetium-99m bone scans done at regular intervals are a sensitive screening tool in patients with MSP1 associated VCP variants at risk for PDB. However, diagnostic confirmation should be coupled with clinical history, biochemical analysis, and skeletal radiographs to facilitate early treatment and prevention complications, acknowledging its limited specificity.

Published

2024

13. Nuclear morphology is shaped by loop-extrusion programs

Author

Patta, Indumathi, Zand, Maryam, Lee, Lindsay, Mishra, Shreya, Bortnick, Alexandra, Lu, Hanbin, Prusty, Arpita, McArdle, Sara, Mikulski, Zbigniew, Wang, Huan-You, Cheng, Christine S, Fisch, Kathleen M, Hu, Ming, and Murre, Cornelis

Subjects

Biochemistry and Cell Biology, Biological Sciences, Genetics, Cell Cycle Checkpoints, Cell Cycle Proteins, Cell Movement, Chromatin, Chromosomes, Neutrophils, Cell Nucleus Shape, Nucleic Acid Conformation, Cell Differentiation, Inflammation, Enhancer Elements, Genetic, Cell Lineage, General Science & Technology

Abstract

It is well established that neutrophils adopt malleable polymorphonuclear shapes to migrate through narrow interstitial tissue spaces1-3. However, how polymorphonuclear structures are assembled remains unknown4. Here we show that in neutrophil progenitors, halting loop extrusion-a motor-powered process that generates DNA loops by pulling in chromatin5-leads to the assembly of polymorphonuclear genomes. Specifically, we found that in mononuclear neutrophil progenitors, acute depletion of the loop-extrusion loading factor nipped-B-like protein (NIPBL) induced the assembly of horseshoe, banded, ringed and hypersegmented nuclear structures and led to a reduction in nuclear volume, mirroring what is observed during the differentiation of neutrophils. Depletion of NIPBL also induced cell-cycle arrest, activated a neutrophil-specific gene program and conditioned a loss of interactions across topologically associating domains to generate a chromatin architecture that resembled that of differentiated neutrophils. Removing NIPBL resulted in enrichment for mega-loops and interchromosomal hubs that contain genes associated with neutrophil-specific enhancer repertoires and an inflammatory gene program. On the basis of these observations, we propose that in neutrophil progenitors, loop-extrusion programs produce lineage-specific chromatin architectures that permit the packing of chromosomes into geometrically confined lobular structures. Our data also provide a blueprint for the assembly of polymorphonuclear structures, and point to the possibility of engineering de novo nuclear shapes to facilitate the migration of effector cells in densely populated tumorigenic environments.

Published

2024

14. The FBXW7-binding sites on FAM83D are potential targets for cancer therapy.

Author

Jiang, Xiaoyu, Wang, Yuli, Guo, Lulu, Wang, Yige, Miao, Tianshu, Ma, Lijuan, Wei, Qin, Lin, Xiaoyan, Mao, Jian-Hua, and Zhang, Pengju

Subjects

Breast cancer, Chemotherapy, FAM83D, FBXW7, Metastasis, Ubiquitination and degradation, Humans, Female, F-Box-WD Repeat-Containing Protein 7, Cell Cycle Proteins, Cell Line, Tumor, Breast Neoplasms, Prognosis, Cell Proliferation, Gene Expression Regulation, Neoplastic, Microtubule-Associated Proteins

Abstract

Increasing evidence shows the oncogenic function of FAM83D in human cancer, but how FAM83D exerts its oncogenic function remains largely unclear. Here, we investigated the importance of FAM83D/FBXW7 interaction in breast cancer (BC). We systematically mapped the FBXW7-binding sites on FAM83D through a comprehensive mutational analysis together with co-immunoprecipitation assay. Mutations at the FBXW7-binding sites on FAM83D led to that FAM83D lost its capability to promote the ubiquitination and proteasomal degradation of FBXW7; cell proliferation, migration, and invasion in vitro; and tumor growth and metastasis in vivo, indicating that the FBXW7-binding sites on FAM83D are essential for its oncogenic functions. A meta-evaluation of FAM83D revealed that the prognostic impact of FAM83D was independent on molecular subtypes. The higher expression of FAM83D has poorer prognosis. Moreover, high expression of FAM83D confers resistance to chemotherapy in BCs, which is experimentally validated in vitro. We conclude that identification of FBXW7-binding sites on FAM83D not only reveals the importance for FAM83D oncogenic function, but also provides valuable insights for drug target.

Published

2024

15. Structural dynamics of RAF1-HSP90-CDC37 and HSP90 complexes reveal asymmetric client interactions and key structural elements.

Author

Finci, Lorenzo, Chakrabarti, Mayukh, Gulten, Gulcin, Finney, Joseph, Grose, Carissa, Fox, Tara, Yang, Renbin, Nissley, Dwight, Esposito, Dominic, Balius, Trent, Simanshu, Dhirendra, and Mccormick, Frank

Subjects

Humans, Cell Cycle Proteins, Protein Binding, Chaperonins, Molecular Chaperones, HSP90 Heat-Shock Proteins

Abstract

RAF kinases are integral to the RAS-MAPK signaling pathway, and proper RAF1 folding relies on its interaction with the chaperone HSP90 and the cochaperone CDC37. Understanding the intricate molecular interactions governing RAF1 folding is crucial for comprehending this process. Here, we present a cryo-EM structure of the closed-state RAF1-HSP90-CDC37 complex, where the C-lobe of the RAF1 kinase domain binds to one side of the HSP90 dimer, and an unfolded N-lobe segment of the RAF1 kinase domain threads through the center of the HSP90 dimer. CDC37 binds to the kinase C-lobe, mimicking the N-lobe with its HxNI motif. We also describe structures of HSP90 dimers without RAF1 and CDC37, displaying only N-terminal and middle domains, which we term the semi-open state. Employing 1 μs atomistic simulations, energetic decomposition, and comparative structural analysis, we elucidate the dynamics and interactions within these complexes. Our quantitative analysis reveals that CDC37 bridges the HSP90-RAF1 interaction, RAF1 binds HSP90 asymmetrically, and that HSP90 structural elements engage RAF1s unfolded region. Additionally, N- and C-terminal interactions stabilize HSP90 dimers, and molecular interactions in HSP90 dimers rearrange between the closed and semi-open states. Our findings provide valuable insight into the contributions of HSP90 and CDC37 in mediating client folding.

Published

2024

16. A genome-wide CRISPR screen identifies BRD4 as a regulator of cardiomyocyte differentiation.

Author

Padmanabhan, Arun, de Soysa, T, Pelonero, Angelo, Sapp, Valerie, Shah, Parisha, Wang, Qiaohong, Li, Li, Lee, Clara, Sadagopan, Nandhini, Nishino, Tomohiro, Ye, Lin, Yang, Rachel, Karnay, Ashley, Poleshko, Andrey, Bolar, Nikhita, Linares-Saldana, Ricardo, Ranade, Sanjeev, Alexanian, Michael, Morton, Sarah, Jain, Mohit, Haldar, Saptarsi, Srivastava, Deepak, and Jain, Rajan

Subjects

Myocytes, Cardiac, Transcription Factors, Animals, Cell Differentiation, Induced Pluripotent Stem Cells, Humans, CRISPR-Cas Systems, Cell Cycle Proteins, Mice, Mouse Embryonic Stem Cells, Nuclear Proteins, Gene Expression Regulation, Developmental, Cell Lineage, Cells, Cultured, Single-Cell Analysis, Bromodomain Containing Proteins

Abstract

Human induced pluripotent stem cell (hiPSC) to cardiomyocyte (CM) differentiation has reshaped approaches to studying cardiac development and disease. In this study, we employed a genome-wide CRISPR screen in a hiPSC to CM differentiation system and reveal here that BRD4, a member of the bromodomain and extraterminal (BET) family, regulates CM differentiation. Chemical inhibition of BET proteins in mouse embryonic stem cell (mESC)-derived or hiPSC-derived cardiac progenitor cells (CPCs) results in decreased CM differentiation and persistence of cells expressing progenitor markers. In vivo, BRD4 deletion in second heart field (SHF) CPCs results in embryonic or early postnatal lethality, with mutants demonstrating myocardial hypoplasia and an increase in CPCs. Single-cell transcriptomics identified a subpopulation of SHF CPCs that is sensitive to BRD4 loss and associated with attenuated CM lineage-specific gene programs. These results highlight a previously unrecognized role for BRD4 in CM fate determination during development and a heterogenous requirement for BRD4 among SHF CPCs.

Published

2024

17. NCAPH drives breast cancer progression and identifies a gene signature that predicts luminal a tumour recurrence.

Author

Mendiburu-Eliçabe, Marina, García-Sancha, Natalia, Corchado-Cobos, Roberto, Martínez-López, Angélica, Chang, Hang, Hua Mao, Jian, Blanco-Gómez, Adrián, García-Casas, Ana, Castellanos-Martín, Andrés, Salvador, Nélida, Jiménez-Navas, Alejandro, Pérez-Baena, Manuel, Sánchez-Martín, Manuel, Abad-Hernández, María, Carmen, Sofía, Claros-Ampuero, Juncal, Cruz-Hernández, Juan, Rodríguez-Sánchez, César, García-Cenador, María, García-Criado, Francisco, Vicente, Rodrigo, Castillo-Lluva, Sonia, and Pérez-Losada, Jesús

Subjects

LASSO, NCAPH, breast cancer, genetic signature, luminal A subtype, prognosis, relapse-free survival, Humans, Mice, Animals, Female, Breast Neoplasms, Neoplasm Recurrence, Local, Gene Expression Profiling, Prognosis, Mice, Transgenic, Nuclear Proteins, Cell Cycle Proteins

Abstract

BACKGROUND: Luminal A tumours generally have a favourable prognosis but possess the highest 10-year recurrence risk among breast cancers. Additionally, a quarter of the recurrence cases occur within 5 years post-diagnosis. Identifying such patients is crucial as long-term relapsers could benefit from extended hormone therapy, while early relapsers might require more aggressive treatment. METHODS: We conducted a study to explore non-structural chromosome maintenance condensin I complex subunit Hs (NCAPH) role in luminal A breast cancer pathogenesis, both in vitro and in vivo, aiming to identify an intratumoural gene expression signature, with a focus on elevated NCAPH levels, as a potential marker for unfavourable progression. Our analysis included transgenic mouse models overexpressing NCAPH and a genetically diverse mouse cohort generated by backcrossing. A least absolute shrinkage and selection operator (LASSO) multivariate regression analysis was performed on transcripts associated with elevated intratumoural NCAPH levels. RESULTS: We found that NCAPH contributes to adverse luminal A breast cancer progression. The intratumoural gene expression signature associated with elevated NCAPH levels emerged as a potential risk identifier. Transgenic mice overexpressing NCAPH developed breast tumours with extended latency, and in Mouse Mammary Tumor Virus (MMTV)-NCAPHErbB2 double-transgenic mice, luminal tumours showed increased aggressiveness. High intratumoural Ncaph levels correlated with worse breast cancer outcome and subpar chemotherapy response. A 10-gene risk score, termed Gene Signature for Luminal A 10 (GSLA10), was derived from the LASSO analysis, correlating with adverse luminal A breast cancer progression. CONCLUSIONS: The GSLA10 signature outperformed the Oncotype DX signature in discerning tumours with unfavourable outcomes, previously categorised as luminal A by Prediction Analysis of Microarray 50 (PAM50) across three independent human cohorts. This new signature holds promise for identifying luminal A tumour patients with adverse prognosis, aiding in the development of personalised treatment strategies to significantly improve patient outcomes.

Published

2024

18. A coadapted KNL1 and spindle assembly checkpoint axis orchestrates precise mitosis in Arabidopsis

Author

Deng, Xingguang, He, Ying, Tang, Xiaoya, Liu, Xianghong, Lee, Yuh-Ru Julie, Liu, Bo, and Lin, Honghui

Subjects

Plant Biology, Biochemistry and Cell Biology, Bioinformatics and Computational Biology, Biological Sciences, Genetics, 1.1 Normal biological development and functioning, Underpinning research, Generic health relevance, Arabidopsis, M Phase Cell Cycle Checkpoints, Microtubule-Associated Proteins, Protein Binding, Cell Cycle Proteins, Mitosis, Kinetochores, Spindle Apparatus, Chromosome Segregation, KNL1, SAC |, kinetochore, SAC

Abstract

The kinetochore scaffold 1 (KNL1) protein recruits spindle assembly checkpoint (SAC) proteins to ensure accurate chromosome segregation during mitosis. Despite such a conserved function among eukaryotic organisms, its molecular architectures have rapidly evolved so that the functional mode of plant KNL1 is largely unknown. To understand how SAC signaling is regulated at kinetochores, we characterized the function of the KNL1 gene in Arabidopsis thaliana. The KNL1 protein was detected at kinetochores throughout the mitotic cell cycle, and null knl1 mutants were viable and fertile but exhibited severe vegetative and reproductive defects. The mutant cells showed serious impairments of chromosome congression and segregation, that resulted in the formation of micronuclei. In the absence of KNL1, core SAC proteins were no longer detected at the kinetochores, and the SAC was not activated by unattached or misaligned chromosomes. Arabidopsis KNL1 interacted with SAC essential proteins BUB3.3 and BMF3 through specific regions that were not found in known KNL1 proteins of other species, and recruited them independently to kinetochores. Furthermore, we demonstrated that upon ectopic expression, the KNL1 homolog from the dicot tomato was able to functionally substitute KNL1 in A. thaliana, while others from the monocot rice or moss associated with kinetochores but were not functional, as reflected by sequence variations of the kinetochore proteins in different plant lineages. Our results brought insights into understanding the rapid evolution and lineage-specific connection between KNL1 and the SAC signaling molecules.

Published

2024

19. Evolved histone tail regulates 53BP1 recruitment at damaged chromatin

Author

Kelliher, Jessica L, Folkerts, Melissa L, Shen, Kaiyuan V, Song, Wan, Tengler, Kyle, Stiefel, Clara M, Lee, Seong-Ok, Dray, Eloise, Zhao, Weixing, Koss, Brian, Pannunzio, Nicholas R, and Leung, Justin W

Subjects

Biochemistry and Cell Biology, Biological Sciences, Genetics, 1.1 Normal biological development and functioning, Generic health relevance, Humans, Adaptor Proteins, Signal Transducing, BRCA1 Protein, Camptothecin, Cell Cycle Proteins, Chromatin, DNA Damage, DNA Repair, HEK293 Cells, Histones, Phosphorylation, Tumor Suppressor p53-Binding Protein 1, Ubiquitin-Protein Ligases, Ubiquitination

Abstract

The master DNA damage repair histone protein, H2AX, is essential for orchestrating the recruitment of downstream mediator and effector proteins at damaged chromatin. The phosphorylation of H2AX at S139, γH2AX, is well-studied for its DNA repair function. However, the extended C-terminal tail is not characterized. Here, we define the minimal motif on H2AX for the canonical function in activating the MDC1-RNF8-RNF168 phosphorylation-ubiquitination pathway that is important for recruiting repair proteins, such as 53BP1 and BRCA1. Interestingly, H2AX recruits 53BP1 independently from the MDC1-RNF8-RNF168 pathway through its evolved C-terminal linker region with S139 phosphorylation. Mechanistically, 53BP1 recruitment to damaged chromatin is mediated by the interaction between the H2AX C-terminal tail and the 53BP1 Oligomerization-Tudor domains. Moreover, γH2AX-linker mediated 53BP1 recruitment leads to camptothecin resistance in H2AX knockout cells. Overall, our study uncovers an evolved mechanism within the H2AX C-terminal tail for regulating DNA repair proteins at damaged chromatin.

Published

2024

20. Spindle checkpoint activation by fungal orthologs of the S. cerevisiae Mps1 kinase

Author

Fabritius, Amy, Alonso, Anabel, Wood, Andrew, Sulthana, Shaheen, and Winey, Mark

Subjects

Microbiology, Biochemistry and Cell Biology, Biological Sciences, Genetics, Biotechnology, Infection, Humans, Antifungal Agents, Cell Cycle Proteins, M Phase Cell Cycle Checkpoints, Prospective Studies, Protein Serine-Threonine Kinases, Protein-Tyrosine Kinases, Saccharomyces cerevisiae, Saccharomyces cerevisiae Proteins, Spindle Apparatus, General Science & Technology

Abstract

There is an ongoing need for antifungal agents to treat humans. Identification of new antifungal agents can be based on screening compounds using whole cell assays. Screening compounds that target a particular molecule is possible in budding yeast wherein sophisticated strain engineering allows for controlled expression of endogenous or heterologous genes. We have considered the yeast Mps1 protein kinase as a reasonable target for antifungal agents because mutant or druggable forms of the protein, upon inactivation, cause rapid loss of cell viability. Furthermore, extensive analysis of the Mps1 in budding yeast has offered potential tactics for identifying inhibitors of its enzymatic activity. One such tactic is based on the finding that overexpression of Mps1 leads to cell cycle arrest via activation of the spindle assembly checkpoint. We have endeavored to adapt this assay to be based on the overexpression of Mps1 orthologs from pathogenic yeast in hopes of having a whole-cell assay system to test the activity of these orthologs. Mps1 orthologous genes from seven pathogenic yeast or other pathogenic fungal species were isolated and expressed in budding yeast. Two orthologs clearly produced phenotypes similar to those produced by the overexpression of budding yeast Mps1, indicating that this system for heterologous Mps1 expression has potential as a platform for identifying prospective antifungal agents.

Published

2024

21. The small GTPase Cdc42 regulates shell field morphogenesis in a gastropod mollusk.

Author

Liu, Xinyu, Huan, Pin, and Liu, Baozhong

Subjects

*CELL cycle proteins, *SMALL molecules, *CELL morphology, *F-actin, *ACTOMYOSIN

Abstract

In most mollusks (conchiferans), the early tissue responsible for shell development, namely, the shell field, shows a common process of invagination during morphogenesis. Moreover, lines of evidence indicated that shell field invagination is not an independent event, but an integrated output reflecting the overall state of shell field morphogenesis. Nevertheless, the underlying mechanisms of this conserved process remain largely unknown. We previously found that actomyosin networks (regularly organized filamentous actin (F-actin) and myosin) may play essential roles in this process by revealing the evident aggregation of F-actin in the invaginated region and demonstrating that nonmuscle myosin II (NM II) is required for invagination in the gastropod Lottia peitaihoensis (= Lottia goshimai). Here, we investigated the roles of the Rho family of small GTPases (RhoA, Rac1, and Cdc42) to explore the upstream regulators of actomyosin networks. Functional assays using small molecule inhibitors suggested that Cdc42 modulates key events of shell field morphogenesis, including invagination and cell rearrangements, while the roles of RhoA and Rac1 may be nonspecific or negligible. Further investigations revealed that the Cdc42 protein was concentrated on the apical side of shell field cells and colocalized with F-actin aggregation. The aggregation of these two molecules could be prevented by treatment with Cdc42 inhibitors. These findings suggest a possible regulatory cascade of shell field morphogenesis in which Cdc42 recruits F-actin (actomyosin networks) on the apical side of shell field cells, which then generates resultant mechanical forces that mediate correct shell field morphogenesis (cell shape changes, invagination and cell rearrangement). Our results emphasize the roles of the cytoskeleton in early shell development and provide new insights into molluscan shell evolution. [Display omitted] • Cdc42 and F-actin were aggregated in the shell field of a gastropod mollusk Lottia. • Inhibiting Cdc42 impaired shell field invagination and prevented shell formation. • Inhibition of Cdc42 eliminated F-actin aggregation from the shell field. • Cdc42 regulated cell rearrangement during shell field morphogenesis. • A cascade of Cdc42-actomyosin networks-shell field invagination was proposed. [ABSTRACT FROM AUTHOR]

Published

2024

22. A comparative study of the cryo-EM structures of Saccharomyces cerevisiae and human anaphase-promoting complex/cyclosome (APC/C).

Author

Vazquez Fernandez, Ester, Yang, Jing, Zhang, Ziguo, Andreeva, Antonina E., Emsley, Paul, and Barford, David

Subjects

*CELL cycle proteins, *SACCHAROMYCES cerevisiae, *UBIQUITIN ligases, *BINDING sites, *CELL cycle, *CYCLINS

Abstract

The anaphase-promoting complex/cyclosome (APC/C) is a large multi-subunit E3 ubiquitin ligase that controls progression through the cell cycle by orchestrating the timely proteolysis of mitotic cyclins and other cell cycle regulatory proteins. Although structures of multiple human APC/C complexes have been extensively studied over the past decade, the Saccharomyces cerevisiae APC/C has been less extensively investigated. Here, we describe medium resolution structures of three S. cerevisiae APC/C complexes: unphosphorylated apo-APC/C and the ternary APC/CCDH1-substrate complex, and phosphorylated apo-APC/C. Whereas the overall architectures of human and S. cerevisiae APC/C are conserved, as well as the mechanism of CDH1 inhibition by CDK-phosphorylation, specific variations exist, including striking differences in the mechanism of coactivator-mediated stimulation of E2 binding, and the activation of APC/CCDC20 by phosphorylation. In contrast to human APC/C in which coactivator induces a conformational change of the catalytic module APC2:APC11 to allow E2 binding, in S. cerevisiae apo-APC/C the catalytic module is already positioned to bind E2. Furthermore, we find no evidence of a phospho-regulatable autoinhibitory segment of APC1, that in the unphosphorylated human APC/C, sterically blocks the CDC20C-box binding site of APC8. Thus, although the functions of APC/C are conserved from S. cerevisiae to humans, molecular details relating to their regulatory mechanisms differ. [ABSTRACT FROM AUTHOR]

Published

2024

23. Arp2/3-dependent endocytosis ensures Cdc42 oscillations by removing Pak1-mediated negative feedback.

Author

Harrell, Marcus A., Ziyi Liu, Campbell, Bethany F., Chinsen, Olivia, Tian Hong, and Das, Maitreyi

Subjects

*SCHIZOSACCHAROMYCES pombe, *CELL cycle proteins, *CELL polarity, *GUANOSINE triphosphatase, *ENDOCYTOSIS, *OSCILLATIONS

Abstract

The GTPase Cdc42 regulates polarized growth in most eukaryotes. In the bipolar yeast Schizosaccharomyces pombe, Cdc42 activation cycles periodically at sites of polarized growth. These periodic cycles are caused by alternating positive feedback and time-delayed negative feedback loops. At each polarized end, negative feedback is established when active Cdc42 recruits the Pak1 kinase to prevent further Cdc42 activation. It is unclear how Cdc42 activation returns to each end after Pak1- dependent negative feedback. We find that disrupting branched actin-mediated endocytosis disables Cdc42 reactivation at the cell ends. Using experimental and mathematical approaches, we show that endocytosis-dependent Pak1 removal from the cell ends allows the Cdc42 activator Scd1 to return to that end to enable reactivation of Cdc42. Moreover, we show that Pak1 elicits its own removal via activation of endocytosis. These findings provide a deeper insight into the self-organization of Cdc42 regulation and reveal previously unknown feedback with endocytosis in the establishment of cell polarity. [ABSTRACT FROM AUTHOR]

Published

2024

24. Importance of Nectin2, NUF2, and Nectin4 Gene Expression in the Pathogenesis of Different Subtypes of Breast Cancer.

Author

Roshanizadeh, Zahra, Haghshenas, Mohammad Reza, Ramezani, Amin, Shajari, Neda, Tahmasebi, Sedigheh, Akrami, Majid, and Ghaderi, Abbas

Subjects

*CELL cycle proteins, *RESEARCH funding, *T-test (Statistics), *HORMONE receptor positive breast cancer, *PROGESTERONE receptors, *BREAST tumors, *CELL adhesion molecules, *POLYMERASE chain reaction, *TUMOR markers, *DESCRIPTIVE statistics, *GENE expression, *ESTROGEN receptors, *CASE-control method, *ONE-way analysis of variance, *ONCOGENES, *DATA analysis software, *EPIDERMAL growth factor receptors

Abstract

Background: The targeted therapy using breast cancer (BC)-associated biomarkers has significantly minimized the side-effects of BC treatment. This study aims to elucidate the role of Nectin2, NUF2, and Nectin4 gene expression in the pathogenesis of BC. Method: In this case-control study, the expression of Nectin2, Nectin4, and NUF2 genes was investigated through real-time polymerase chain reaction assay in 46 tumor tissues from BC patients and 46 adjacent non-tumorous tissues as a control group. Data were analyzed using SPSS-21 software, employing independent t-tests and oneway ANOVA. A P-value of <0.05 was considered statistically significant. Results: The results demonstrated a significant increase in the expression of the NUF2 gene in tumor tissues compared with adjacent normal tissues (P = 0.005, fold change = 3.7). No statistically significant difference was observed in the expression of Nectin2 and Nectin4 between the tumor and adjacent tissues. However, higher expression of Nectin2 was noted in the early stages of the disease, particularly in subtypes with estrogen receptor-positive (ER+), progesterone receptor positive (PR+), and human epidermal growth factor receptor 2 negative (HER2-). Furthermore, the expression of NUF2 and Nectin4 was elevated in advanced stages and triple-negative BC subtypes. Notably, the expression of these three genes was higher in patients aged ≤ 45 years. Conclusion: The findings suggest that the expression levels of NUF2, Nectin2, and Nectin4 genes may influence the initiation, progression, and pathogenesis of BC subtypes. [ABSTRACT FROM AUTHOR]

Published

2024

25. Bayesian mapping of protein kinases to vasopressin-regulated phosphorylation sites in renal collecting duct.

Author

Deshpande, Venkatesh, Park, Euijung, Jayatissa, Nipun U., Khan, Shaza, Mejia, Raymond, Yang, Chin-Rang, Chou, Chung-Lin, Raghuram, Viswanathan, and Knepper, Mark A.

Subjects

*EXTRACELLULAR signal-regulated kinases, *CYCLIC-AMP-dependent protein kinase, *CARRIER proteins, *MITOGEN-activated protein kinases, *CELL cycle proteins, *AQUAPORINS, *PROTEIN kinases

Abstract

Vasopressin controls water permeability in the renal collecting duct by regulating the water channel protein, aquaporin-2 (AQP2). Phosphoproteomic studies have identified multiple proteins that undergo phosphorylation changes in response to vasopressin. The kinases responsible for the phosphorylation of most of these sites have not been identified. Here, we use large-scale Bayesian data integration to predict the responsible kinases for 51 phosphoproteomically identified vasopressin-regulated phosphorylation sites in the renal collecting duct. To do this, we applied Bayes' rule to rank the 515 known mammalian protein kinases for each site. Bayes' rule was applied recursively to integrate each of the seven independent datasets, each time using the posterior probability vector of a given step as the prior probability vector of the next step. In total, 30 of the 33 phosphorylation sites that increase with vasopressin were predicted to be phosphorylated by protein kinase A (PKA) catalytic subunit-α, consistent with prior studies implicating PKA in vasopressin signaling. Eighteen of the vasopressin-regulated phosphorylation sites were decreased in response to vasopressin and all but three of these sites were predicted to be targets of extracellular signal-regulated kinases, ERK1 and ERK2. This result implies that ERK1 and ERK2 are inhibited in response to vasopressin V2 receptor occupation, secondary to PKA activation. The six phosphorylation sites not predicted to be phosphorylated by PKA or ERK1/2 are potential targets of other protein kinases previously implicated in aquaporin-2 regulation, including cyclin-dependent kinase 18 (CDK18), calmodulin-dependent kinase 2δ (CAMK2D), AMP-activated kinase catalytic subunit-α-1 (PRKAA1) and CDC42 binding protein kinase β (CDC42BPB). NEW & NOTEWORTHY: Vasopressin regulates water transport in the renal collecting duct in part through phosphorylation or dephosphorylation of proteins that regulate aquaporin-2. Prior studies have identified 51 vasopressin-regulated phosphorylation sites in 45 proteins. This study uses Bayesian data integration techniques to combine information from multiple prior proteomics and transcriptomics studies to predict the protein kinases that phosphorylate the 51 sites. Most of the regulated sites were predicted to be phosphorylated by protein kinase A or ERK1/ERK2. [ABSTRACT FROM AUTHOR]

Published

2024

26. Increased activity of epithelial Cdc42 Rho GTPase and tight junction permeability in the Cftr knockout intestine.

Author

Woode, Rowena A., Strubberg, Ashlee M., Liu, Jinghua, Walker, Nancy M., and Clarke, Lane L.

Subjects

*INTESTINAL barrier function, *CELL cycle proteins, *TIGHT junctions, *CYSTIC fibrosis transmembrane conductance regulator, *WNT signal transduction

Abstract

Increased intestinal permeability is a manifestation of cystic fibrosis (CF) in people with CF (pwCF) and in CF mouse models. CF transmembrane conductance regulator knockout (Cftr KO) mouse intestine exhibits increased proliferation and Wnt/β-catenin signaling relative to wild-type mice (WT). Since the Rho GTPase Cdc42 plays a central role in intestinal epithelial proliferation and tight junction remodeling, we hypothesized that Cdc42 may be altered in the Cftr KO crypts. Immunofluorescence showed distinct tight junction localization of Cdc42 in Cftr KO fresh crypts and enteroids, the latter indicating an epithelial-autonomous feature. Quantitative PCR and immunoblots revealed similar expression of Cdc42 in the Cftr KO crypts/enteroids relative to WT, whereas pulldown assays showed increased GTP-bound (active) Cdc42 in proportion to total Cdc42 in Cftr KO enteroids. Cdc42 activity in the Cftr KO and WT enteroids could be reduced by inhibition of the Wnt transducer Disheveled. With the use of a dye permeability assay, Cftr KO enteroids exhibited increased paracellular permeability to 3 kDa dextran relative to WT. Leak permeability and Cdc42 tight junction localization were reduced to a greater extent by inhibition of Wnt/β-catenin signaling with endo-IWR1 in Cftr KO relative to WT enteroids. Increased proliferation or inhibition of Cdc42 activity with ML141 in WT enteroids had no effect on permeability. In contrast, inhibition of Cdc42 with ML141 increased permeability to both 3 kDa dextran and tight junction impermeant 500 kDa dextran in Cftr KO enteroids. These data suggest that increased constitutive Cdc42 activity may alter the stability of paracellular permeability in Cftr KO crypt epithelium. NEW & NOTEWORTHY: Increased tight junction localization and GTP-bound activity of the Rho GTPase Cdc42 was identified in small intestinal crypts and enteroids of cystic fibrosis (CF) transmembrane conductance regulator knockout (Cftr KO) mice. The increase in epithelial Cdc42 activity was associated with increased Wnt signaling. Paracellular flux of an uncharged solute (3 kDa dextran) in Cftr KO enteroids indicated a moderate leak permeability under basal conditions that was strongly exacerbated by Cdc42 inhibition. These findings suggest increased activity of Cdc42 in the Cftr KO intestine underlies alterations in intestinal permeability. [ABSTRACT FROM AUTHOR]

Published

2024

27. Fdo1, Fkh1, Fkh2, and the Swi6–Mbp1 MBF complex regulate Mcd1 levels to impact eco1 rad61 cell growth in Saccharomyces cerevisiae.

Author

Singh, Gurvir and Skibbens, Robert V

Subjects

*PROTEIN metabolism, *NUCLEAR proteins, *FLOW cytometry, *CELL cycle proteins, *GENOMICS, *CHALONES, *TRANSCRIPTION factors, *CELL cycle, *GENES, *GENE expression, *WESTERN immunoblotting, *DNA-binding proteins, *YEAST, *SACCHAROMYCES, *SEQUENCE analysis, *DISEASE progression

Abstract

Cohesins promote proper chromosome segregation, gene transcription, genomic architecture, DNA condensation, and DNA damage repair. Mutations in either cohesin subunits or regulatory genes can give rise to severe developmental abnormalities (such as Robert Syndrome and Cornelia de Lange Syndrome) and also are highly correlated with cancer. Despite this, little is known about cohesin regulation. Eco1 (ESCO2/EFO2 in humans) and Rad61 (WAPL in humans) represent two such regulators but perform opposing roles. Eco1 acetylation of cohesin during S phase, for instance, stabilizes cohesin-DNA binding to promote sister chromatid cohesion. On the other hand, Rad61 promotes the dissociation of cohesin from DNA. While Eco1 is essential, ECO1 and RAD61 co-deletion results in yeast cell viability, but only within a limited temperature range. Here, we report that eco1 rad61 cell lethality is due to reduced levels of the cohesin subunit Mcd1. Results from a suppressor screen further reveals that FDO1 deletion rescues the temperature-sensitive (ts) growth defects exhibited by eco1 rad61 double mutant cells by increasing Mcd1 levels. Regulation of MCD1 expression, however, appears more complex. Elevated expression of MBP1 , which encodes a subunit of the MBF transcription complex, also rescues eco1 rad61 cell growth defects. Elevated expression of SWI6 , however, which encodes the Mbp1 -binding partner of MBF, exacerbates eco1 rad61 cell growth and also abrogates the Mpb1-dependent rescue. Finally, we identify two additional transcription factors, Fkh1 and Fkh2 , that impact MCD1 expression. In combination, these findings provide new insights into the nuanced and multi-faceted transcriptional pathways that impact MCD1 expression. [ABSTRACT FROM AUTHOR]

Published

2024

28. KNSTRN Is a Prognostic Biomarker That Is Correlated with Immune Infiltration in Breast Cancer and Promotes Cell Cycle and Proliferation.

Author

Zhang, Wenwu, Xiao, Yuhan, Zhou, Quan, Zhu, Xin, Zhang, Yanxia, Xiang, Qin, Wu, Shunhong, Song, Xiaoyu, Zhao, Junxiu, Yuan, Ruanfei, Xiao, Bin, and Li, Linhai

Subjects

*CELL cycle proteins, *REGULATORY T cells, *KILLER cells, *GENE expression, *CANCER cell proliferation

Abstract

Kinetochore-localized astrin/SPAG5-binding protein (KNSTRN) promotes the progression of bladder cancer and lung adenocarcinoma. However, its expression and biological function in breast cancer remain largely unknown. Therefore, this study aimed to analyze KNSTRN expression, prognoses, correlation with immune infiltration, expression-associated genes, and regulated signaling pathways to characterize its role in regulating the cell cycle using both bioinformatics and in vitro functional experiments. Analyses of The Cancer Genome Atlas, Gene Expression Omnibus, TIMER, and The Human Protein Atlas databases revealed a significant upregulation of KNSTRN transcript and protein levels in breast cancer. Kaplan–Meier survival analyses demonstrated a significant association between high expression of KNSTRN and poor overall survival, relapse-free survival, post-progression survival, and distant metastases-free survival in patients with breast cancer. Furthermore, multivariate Cox regression analyses confirmed that KNSTRN is an independent prognostic factor for breast cancer. Immune infiltration analysis indicated a positive correlation between KNSTRN expression and T regulatory cell infiltration while showing a negative correlation with Tgd and natural killer cell infiltration. Gene set enrichment analysis along with single-cell transcriptome data analysis suggested that KNSTRN promoted cell cycle progression by regulating the expression of key cell cycle proteins. The overexpression and silencing of KNSTRN in vitro, respectively, promoted and inhibited the proliferation of breast cancer cells. The overexpression of KNSTRN enhanced the expression of key cell cycle regulators, including CDK4, CDK6, and cyclin D3, thereby accelerating the G1/S phase transition and leading to aberrant proliferation of breast cancer cells. In conclusion, our study demonstrates that KNSTRN functions as an oncogene in breast cancer by regulating immune response, promoting G1/S transition, and facilitating breast cancer cell proliferation. Moreover, KNSTRN has potential as a molecular biomarker for diagnostic and prognostic prediction in breast cancer. [ABSTRACT FROM AUTHOR]

Published

2024

29. cIAP-2 protein is upregulated by human papillomavirus in oropharyngeal cancers: role in radioresistance in vitro.

Author

Oliva, Carolina, Carrillo-Beltrán, Diego, Osorio, Julio C., Gallegos, Iván, Carvajal, Felipe, Mancilla-Miranda, Claudio, Boettiger, Paul, Boccardo, Enrique, and Aguayo, Francisco

Subjects

*IN vitro studies, *CELL cycle proteins, *RESEARCH funding, *OROPHARYNGEAL cancer, *APOPTOSIS, *PAPILLOMAVIRUSES, *DESCRIPTIVE statistics, *RETROSPECTIVE studies, *REVERSE transcriptase polymerase chain reaction, *GENE expression, *IMMUNOHISTOCHEMISTRY, *RESEARCH methodology, *RESEARCH, *RADIATION-protective agents, *DATA analysis software

Abstract

Background: High-risk human papillomaviruses are the causal agents of a subset of head and neck cancers. A previous transcriptomic analysis showed that cIAP2 protein, involved in cell survival and apoptosis, is upregulated in OKF6 oral cells that express HPV16 E6/E7. In addition, cIAP2 promotes radioresistance, a very important concern in HNC treatment. However, cIAP2 increase has not yet been evaluated in oropharyngeal carcinomas (OPCs), nor has been the role of cIAP2 in HNC radioresistance. Methods: We carried out a descriptive-analytical retrospective study in 49 OPCs from Chilean patients. We determined the expression of cIAP2 at transcript and proteins levels using reverse-transcriptase -polymerase chain reaction and immunohistochemistry, respectively. HPV and p16 expression were previously analyzed in these specimens. In addition, SCC-143 HNC cells ectopically expressing HPV16 E6/E7 were analyzed for cIAP2 expression and after transfection with a siRNA for HPV16 E6/E7 knocking down. Results: We found a statistically significant association between HPV presence and cIAP2 expression (p = 0.0032 and p = 0.0061, respectively). An association between p16 and cIAP2 levels was also found (p = 0.038). When SCC-143 cells were transfected with a construct expressing HPV16 E6/E7, the levels of cIAP2 were significantly increased (p = 0.0383 and p = 0.0115, respectively). Conversely, HPV16 E6 and E7 knocking down resulted in a decrease of cIAP2 levels (p = 0.0161 and p = 0.006, respectively). Finally, cIAP2 knocking down in HPV16 E6/E7 cells resulted in increased apoptosis after exposure to radiation at 4 and 8 Gy (p = 0.0187 and p = 0.0061, respectively). Conclusion: This study demonstrated for the first time a positive relationship between HPV presence and cIAP2 levels in OPCs. Additionally, cIAP2 knocking down sensitizes HNC cells to apoptosis promoted by radiation. Therefore, cIAP2 is a potential therapeutic target for radiation in HPV-driven HNC. [ABSTRACT FROM AUTHOR]

Published

2024

30. CCDC68 Maintains Mitotic Checkpoint Activation by Promoting CDC20 Integration into the MCC.

Author

Li, Qi, Chen, Qingzhou, Zheng, Tao, Wang, Fulin, Teng, Junlin, Zhou, Haining, and Chen, Jianguo

Subjects

*CHROMOSOME segregation, *CELL cycle proteins, *KINETOCHORE, *ANAPHASE, *CHROMOSOMES

Abstract

The spindle assembly checkpoint (SAC) ensures chromosome segregation fidelity by manipulating unattached kinetochore‐dependent assembly of the mitotic checkpoint complex (MCC). The MCC binds to and inhibits the anaphase promoting complex/cyclosome (APC/C) to postpone mitotic exit. However, the mechanism by which unattached kinetochores mediate MCC formation is not yet fully understood. Here, it is shown that CCDC68 is an outer kinetochore protein that preferentially localizes to unattached kinetochores. Furthermore, CCDC68 interacts with the SAC factor CDC20 to inhibit its autoubiquitination and MCC disassembly. Therefore, CCDC68 restrains APC/C activation to ensure a robust SAC and allow sufficient time for chromosome alignment, thus ensuring chromosomal stability. Hence, the study reveals that CCDC68 is required for CDC20‐dependent MCC stabilization to maintain mitotic checkpoint activation. [ABSTRACT FROM AUTHOR]

Published

2024

31. Ailanthone suppresses cell proliferation of renal cell carcinoma partially via inhibition of EZH2.

Author

Zhu, Jianbing, Dai, Guangcheng, Chen, Ting, Zhou, Yibin, Zang, Yachen, Xu, Lijun, Jin, Lu, and Zhu, Jin

Subjects

RENAL cell carcinoma, CELL survival, PROTEOMICS, CELL cycle proteins, MOLECULAR docking

Abstract

Background: Ailanthone (Ail) extracted from medicinal plants has played an anticancer role in multiple cancers, while there is no research about Ail in renal cell carcinoma (RCC). Methods: In the present study, we performed CCK-8 and flow cytometry to assess the effect of Ail on cell viability, apoptosis and cycle. We also performed tandem mass tags (TMT)-labeled quantitative proteomic technology and bioinformatic analysis to identify the functional pathway and proteins of Ail in RCC. Results: The results showed Ail could inhibit cell viability and induce cell apoptosis. Proteomic profiling identified 1732 differentially expressed proteins in cells treated with Ail, compared to the negative control group. Gene ontology function annotation and Gene Set Enrichment Analysis (GSEA) were performed to identified the involved biological processes, molecular function and pathway. Results of GSEA proved the enrichment of Deps in EZH2 targets. The comparison between Deps and EZH2 co-expressed genes revealed 44 overlapped genes and we identified 4 hub genes (CDC20, CEP55, TOP2A, and UBE2C) associated with RCC progression. The molecular docking study revealed a moderate to tight binding potential of Ail and EZH2, and western blotting showed EZH2 was suppressed after cells treated with Ail. Conclusion: Altogether, we identified the anticancer role of Ail in RCC, including inhibition of cell proliferation and induction of apoptosis. The results also screened the key proteins mediate the function of Ail, which have laid a theoretical foundation for elucidating the applications of Ail in clinical research. [ABSTRACT FROM AUTHOR]

Published

2024

32. Cell cycle regulated expression of the <italic>WHI7</italic> Start repressor gene.

Author

Ros-Carrero, Cristina, Gomar-Alba, Mercè, and Igual, J. Carlos

Subjects

*CELL cycle proteins, *GENE expression, *CELL cycle, *GENETIC transcription regulation, *GENETIC transcription

Abstract

Periodic transcriptional waves along the cell cycle ensure the accurate progression of the different cell cycle phases through the timely regulated expression of cell cycle proteins. The G1/S transition (Start) consists in the activation of a transcriptional program by G1 CDKs through the inactivation of Start transcriptional repressors, Whi5 and Whi7 in yeast or Rb in mammals. Here, we provide a comprehensive characterization of the transcriptional regulation of the Start repressor Whi7 in budding yeast. We found that WHI7 is a cell cycle regulated gene that shows periodic expression peaking in G1. Our results demonstrate that the three cell cycle transcriptional programs related to G1 and their corresponding transcription factors are involved in the transcriptional control of WHI7. Specifically, we identified that the transcriptional regulators Swi5 and Mcm1-Yox1, which are involved in late M and early G1 expression, and the transcription factors MBF and SBF, which are responsible for G1/S expression, are able to associate and regulate the WHI7 gene. In summary, in this work, we provide new mechanisms for the regulation of the Start repressor Whi7, which highlights the precise and complex control of the cell cycle machinery governing the G1/S transition. [ABSTRACT FROM AUTHOR]

Published

2024

33. CASIN exerts anti‐aging effects through RPL4 on the skin of naturally aging mice.

Author

Zhang, Yijia, Wang, Xueer, Huang, Jianyuan, Zhang, Xinyue, Bu, Lingwei, Zhang, Yarui, Liang, Fengting, Wu, Shenhua, Zhang, Min, Zhang, Lu, and Zhang, Lin

Subjects

*TOPICAL drug administration, *RIBOSOMAL proteins, *SUBCUTANEOUS injections, *CELL cycle proteins, *LABORATORY mice, *SKIN aging, KERATINOCYTE differentiation

Abstract

Skin aging has been associated with the onset of various skin issues, and recent studies have identified an increase in Cdc42 activity in naturally aging mice. While previous literature has suggested that CASIN, a specific inhibitor of Cdc42 activity, may possess anti‐aging properties, its specific effects on the epidermis and dermis, as well as the underlying mechanisms in naturally aging mice, remain unclear. Our study revealed that CASIN demonstrated the ability to increase epidermal and dermal thickness, enhance dermal‐epidermal junction, and stimulate collagen and elastic fiber synthesis in 9‐, 15‐, and 24‐month‐old C57BL/6 mice in vivo. Moreover, CASIN was found to enhance the proliferation, differentiation, and colony formation and restore the cytoskeletal morphology of primary keratinocytes in naturally aging skin in vitro. Furthermore, the anti‐aging properties of CASIN on primary fibroblasts in aging mice were mediated by the ribosomal protein RPL4 using proteomic sequencing, influencing collagen synthesis and cytoskeletal morphology both in vitro and in vivo. Meanwhile, both subcutaneous injection and topical application exhibited anti‐aging effects for a duration of 21 days. Additionally, CASIN exhibited anti‐inflammatory properties, while reduced expression of RPL4 was associated with increased inflammation in the skin of naturally aging mice. Taken together, our results unveil a novel function of RPL4 in skin aging, providing a foundational basis for future investigations into ribosomal proteins. And CASIN shows promise as a potential anti‐aging agent for naturally aging mouse skin, suggesting potential applications in the field. [ABSTRACT FROM AUTHOR]

Published

2024

34. The Mitotic Checkpoint Complex controls the association of Cdc20 regulatory protein with the ubiquitin ligase APC/C in mitosis.

Author

Sitry-Shevah, Danielle, Miniowitz-Shemtov, Shirly, Dan, Tanya Liburkin, and Hershko, Avram

Subjects

*SPINDLE apparatus, *CELL cycle proteins, *CELL cycle, *PROTEIN kinases, *ANAPHASE

Abstract

The ubiquitin ligase Anaphase-Promoting Complex/Cyclosome (APC/C) and its regulatory protein Cdc20 play important roles in the control of different stages of mitosis. APC/C associated with Cdc20 is active and promotes metaphase-anaphase transition by targeting for degradation inhibitors of anaphase initiation. Earlier in mitosis, premature action of APC/C is prevented by the mitotic checkpoint (or spindle assembly checkpoint) system, which ensures that anaphase is not initiated until all chromosomes are properly attached to the mitotic spindle. The active mitotic checkpoint system promotes the assembly of a Mitotic Checkpoint Complex (MCC), which binds to APC/C and inhibits its activity. The interaction of MCC with APC/C is strongly enhanced by Cdc20 bound to APC/C. While the association of Cdc20 with APC/C was known to be essential for both these stages of mitosis, it was not known how Cdc20 remains bound in spite of ongoing processes, phosphorylation and ubiquitylation, that stimulate its release from APC/C. We find that MCC strongly inhibits the release of Cdc20 from APC/C by the action of mitotic protein kinase Cdk1-cyclin B. This is not due to protection from phosphorylation of specific sites in Cdc20 that affect its interaction with APC/C. Rather, MCC stabilizes the binding to APC/C of partially phosphorylated forms of Cdc20. MCC also inhibits the autoubiquitylation of APC/C-bound Cdc20 and its ubiquitylation-promoted release from APC/C. We propose that these actions of MCC to maintain Cdc20 bound to APC/C in mitosis are essential for the control of mitosis during active mitotic checkpoint and in subsequent anaphase initiation. [ABSTRACT FROM AUTHOR]

Published

2024

35. Proteome-scale characterisation of motif-based interactome rewiring by disease mutations.

Author

Kliche, Johanna, Simonetti, Leandro, Krystkowiak, Izabella, Kuss, Hanna, Diallo, Marcel, Rask, Emma, Nilsson, Jakob, Davey, Norman E, and Ivarsson, Ylva

Subjects

*SINGLE nucleotide polymorphisms, *WHOLE genome sequencing, *GENETIC variation, *CELL cycle proteins, *REPORTING of diseases

Abstract

Whole genome and exome sequencing are reporting on hundreds of thousands of missense mutations. Taking a pan-disease approach, we explored how mutations in intrinsically disordered regions (IDRs) break or generate protein interactions mediated by short linear motifs. We created a peptide-phage display library tiling ~57,000 peptides from the IDRs of the human proteome overlapping 12,301 single nucleotide variants associated with diverse phenotypes including cancer, metabolic diseases and neurological diseases. By screening 80 human proteins, we identified 366 mutation-modulated interactions, with half of the mutations diminishing binding, and half enhancing binding or creating novel interaction interfaces. The effects of the mutations were confirmed by affinity measurements. In cellular assays, the effects of motif-disruptive mutations were validated, including loss of a nuclear localisation signal in the cell division control protein CDC45 by a mutation associated with Meier-Gorlin syndrome. The study provides insights into how disease-associated mutations may perturb and rewire the motif-based interactome. Synopsis: Hundreds of mutations in the intrinsically disordered regions of the human proteome that break, diminish, enhance or create motif-based interactions are uncovered by mutational proteomic peptide-phage display. A novel peptide-phage display library that combines disease-associated amino acid changing mutations with the intrinsically disordered regions of the human proteome is described. 275 mutations associated with various diseases are reported to affect 279 motif-based protein-protein interactions. About 50% of the mutations enhance or create binding motifs, and the rest disrupt or diminish interactions. The study provides novel insights into how disease-associated mutations perturb and rewire the motif-based interactome. Hundreds of mutations in the intrinsically disordered regions of the human proteome that break, diminish, enhance or create motif-based interactions are uncovered by mutational proteomic peptide-phage display. [ABSTRACT FROM AUTHOR]

Published

2024

36. Chios gum mastic enhance the proliferation and odontogenic differentiation of human dental pulp stem cells.

Author

Hyun-Su Baek, Se-Jin Park, Eun-Gyung Lee, Yong-Il Kim, and In-Ryoung Kim

Subjects

*DENTAL pulp, *CELL cycle proteins, *CELL cycle, *MESENCHYMAL stem cells, *EXTRACELLULAR matrix proteins

Abstract

Dental pulp stem cells (DPSCs) are a type of adult stem cell present in the dental pulp tissue. They possess a higher proliferative capacity than bone marrow mesenchymal stem cells. Their ease of collection from patients makes them well-suited for tissue engineering applications, such as tooth and nerve regeneration. Chios gum mastic (CGM), a resin extracted from the stems and leaves of Pistacia lentiscus var. Chia, has garnered attention for its potential in tissue regeneration. This study aims to confirm alterations in cell proliferation rates and induce differentiation in human DPSCs (hDPSCs) through CGM treatment, a substance known for effectively promoting odontogenic differentiation. Administration of CGM to hDPSC cells was followed by an assessment of cell survival, proliferation, and odontogenic differentiation through protein and gene analysis. The study revealed that hDPSCs exhibited low sensitivity to CGM toxicity. CGM treatment induced cell proliferation by activating cell-cycle proteins through the Wnt/β-catenin pathway. Additionally, the study demonstrated that CGM enhances alkaline phosphatase activation by upregulating the expression of collagen type I, a representative matrix protein of dentin. This activation of markers associated with odontogenic and bone differentiation ultimately facilitated the mineralization of hDPSCs. This study concludes that CGM, as a natural substance, fosters the cell cycle and cell proliferation in hDPSCs. Furthermore, it triggers the transcription of odontogenic and osteogenic markers, thereby facilitating odontogenic differentiation. [ABSTRACT FROM AUTHOR]

Published

2024

37. Molecular Insights into the Anticancer Activity of Withaferin-A: The Inhibition of Survivin Signaling.

Author

Wadhwa, Renu, Wang, Jia, Shefrin, Seyad, Zhang, Huayue, Sundar, Durai, and Kaul, Sunil C.

Subjects

*COMPUTER-assisted molecular modeling, *IN vitro studies, *CELL cycle proteins, *EPITHELIAL-mesenchymal transition, *RESEARCH funding, *ANTINEOPLASTIC agents, *APOPTOSIS, *CELLULAR signal transduction, *CELL cycle, *CELL motility, *DESCRIPTIVE statistics, *PLANT extracts, *CELL lines, *MESSENGER RNA, *BIOINFORMATICS, *CELL survival, *DIMERIZATION, *PHENOTYPES, *CYCLIN-dependent kinases, *PHARMACODYNAMICS, CERVIX uteri tumors

Abstract

Simple Summary: The inactivation of apoptotic signaling by inhibitors of apoptosis proteins (IAPs) is one of the important hallmarks of cancer cells. Survivin, a 16.5 kDa member of the IAP family, is commonly enriched in many cancers and is a potential therapeutic target. We investigated the Survivin-targeting potential of Withaferin-A (Wi-A) and Withanone (Wi-N), two major withanolides from Withania somnifera (Ashwagandha), using computational assays. The results were validated in various in vitro experimental assays using Wi-A-rich extracts from Ashwagandha leaves, suggesting their use as an important bioresource for cancer drug development. Survivin, a member of the IAP family, functions as a homodimer and inhibits caspases, the key enzymes involved in apoptosis. Several Survivin inhibitors, including YM-155, Debio1143, EM1421, LQZ-7I, and TL32711, have emerged as potential anticancer drugs awaiting validation in clinical trials. Due to the high cost and adverse side effects of synthetic drugs, natural compounds with similar activity have also been in demand. In this study, we conducted molecular docking assays to evaluate the ability of Wi-A and Wi-N to block Survivin dimerization. We found that Wi-A, but not Wi-N, can bind to and prevent the homodimerization of Survivin, similar to YM-155. Therefore, we prepared a Wi-A-rich extract from Ashwagandha leaves (Wi-AREAL). Experimental analyses of human cervical carcinoma cells (HeLa and ME-180) treated with Wi-AREAL (0.05–0.1%) included assessments of viability, apoptosis, cell cycle, migration, invasion, and the expression levels (mRNA and protein) of molecular markers associated with these phenotypes. We found that Wi-AREAL led to growth arrest mediated by the upregulation of p21WAF1 and the downregulation of several proteins (CDK1, Cyclin B, pRb) involved in cell cycle progression. Furthermore, Wi-AREAL treatment activated apoptosis signaling, as evidenced by reduced PARP-1 and Bcl-2 levels, increased procaspase-3, and elevated Cytochrome C. Additionally, treating cells with a nontoxic low concentration (0.01%) of Wi-AREAL inhibited migration and invasion, as well as EMT (epithelial–mesenchymal transition) signaling. By combining computational and experimental approaches, we demonstrate the potential of Wi-A and Wi-AREAL as natural inhibitors of Survivin, which may be helpful in cancer treatment. [ABSTRACT FROM AUTHOR]

Published

2024

38. Chk2 homolog Mek1 limits exonuclease 1–dependent DNA end resection during meiotic recombination in Saccharomyces cerevisiae.

Author

Krystosek, Jennifer T and Bishop, Douglas K

Subjects

*DNA metabolism, *PHOSPHORYLATION, *CELL cycle proteins, *RESEARCH funding, *CELL physiology, *DNA, *ESTERASES, *PROTEIN-tyrosine kinases, *MASS spectrometry, *YEAST

Abstract

The conserved Rad2/XPG family 5′–3′ exonuclease, exonuclease 1 (Exo1), plays many roles in DNA metabolism including during resolution of DNA double-strand breaks via homologous recombination. Prior studies provided evidence that the end resection activity of Exo1 is downregulated in yeast and mammals by Cdk1/2 family cyclin-dependent and checkpoint kinases, including budding yeast kinase Rad53 which functions in mitotic cells. Here, we provide evidence that the master meiotic kinase Mek1 , a paralog of Rad53 , limits 5′–3′ single-strand resection at the sites of programmed meiotic DNA breaks. Mutational analysis suggests that the mechanism of Exo1 suppression by Mek1 differs from that of Rad53. [ABSTRACT FROM AUTHOR]

Published

2024

39. Selection of Reference Genes in Siraitia siamensis and Expression Patterns of Genes Involved in Mogrosides Biosynthesis.

Author

Chen, Wenqiang, Lin, Xiaodong, Wang, Yan, Mu, Detian, Mo, Changming, Huang, Huaxue, Zhao, Huan, Luo, Zuliang, Liu, Dai, Wilson, Iain W., Qiu, Deyou, and Tang, Qi

Subjects

GENE expression, GENE expression profiling, HERBAL medicine, BIOSYNTHESIS, CELL cycle proteins

Abstract

Siraitia siamensis is a traditional Chinese medicinal herb. In this study, using S. siamensis cultivated in vitro, twelve candidate reference genes under various treatments were analyzed for their expression stability by using algorithms such as GeNorm, NormFinder, BestKeeper, Delta CT, and RefFinder. The selected reference genes were then used to characterize the gene expression of cucurbitadienol synthase, which is a rate-limiting enzyme for mogroside biosynthesis. The results showed that CDC6 and NCBP2 expression was the most stable across all treatments and are the best reference genes under the tested conditions. Utilizing the validated reference genes, we analyzed the expression profiles of genes related to the synthesis pathway of mogroside in S. siamensis in response to a range of abiotic stresses. The findings of this study provide clear standards for gene expression normalization in Siraitia plants and exploring the rationale behind differential gene expression related to mogroside synthesis pathways. [ABSTRACT FROM AUTHOR]

Published

2024

40. The p97/VCP adaptor UBXD1 drives AAA+ remodeling and ring opening through multi-domain tethered interactions

Author

Braxton, Julian R, Altobelli, Chad R, Tucker, Maxwell R, Tse, Eric, Thwin, Aye C, Arkin, Michelle R, and Southworth, Daniel R

Subjects

Biochemistry and Cell Biology, Biological Sciences, Underpinning research, 1.1 Normal biological development and functioning, Humans, Valosin Containing Protein, Protein Binding, Protein Structure, Tertiary, Cell Cycle Proteins, Chemical Sciences, Medical and Health Sciences, Biophysics, Developmental Biology, Biological sciences, Biomedical and clinical sciences, Chemical sciences

Abstract

p97, also known as valosin-containing protein, is an essential cytosolic AAA+ (ATPases associated with diverse cellular activities) hexamer that unfolds substrate polypeptides to support protein homeostasis and macromolecular disassembly. Distinct sets of p97 adaptors guide cellular functions but their roles in direct control of the hexamer are unclear. The UBXD1 adaptor localizes with p97 in critical mitochondria and lysosome clearance pathways and contains multiple p97-interacting domains. Here we identify UBXD1 as a potent p97 ATPase inhibitor and report structures of intact human p97-UBXD1 complexes that reveal extensive UBXD1 contacts across p97 and an asymmetric remodeling of the hexamer. Conserved VIM, UBX and PUB domains tether adjacent protomers while a connecting strand forms an N-terminal domain lariat with a helix wedged at the interprotomer interface. An additional VIM-connecting helix binds along the second (D2) AAA+ domain. Together, these contacts split the hexamer into a ring-open conformation. Structures, mutagenesis and comparisons to other adaptors further reveal how adaptors containing conserved p97-remodeling motifs regulate p97 ATPase activity and structure.

Published

2023

41. Mutate and Conjugate: A Method to Enable Rapid In-Cell Target Validation

Author

Thomas, Adam M, Serafini, Marta, Grant, Emma K, Coombs, Edward AJ, Bluck, Joseph P, Schiedel, Matthias, McDonough, Michael A, Reynolds, Jessica K, Lee, Bernadette, Platt, Michael, Sharlandjieva, Vassilena, Biggin, Philip C, Duarte, Fernanda, Milne, Thomas A, Bush, Jacob T, and Conway, Stuart J

Subjects

Medicinal and Biomolecular Chemistry, Chemical Sciences, Rare Diseases, Genetics, 5.1 Pharmaceuticals, Development of treatments and therapeutic interventions, Generic health relevance, Humans, Nuclear Proteins, Ligands, HEK293 Cells, Transcription Factors, Mutant Proteins, Cell Cycle Proteins, Biological Sciences, Organic Chemistry, Biological sciences, Chemical sciences

Abstract

Target validation remains a challenge in drug discovery, which leads to a high attrition rate in the drug discovery process, particularly in Phase II clinical trials. Consequently, new approaches to enhance target validation are valuable tools to improve the drug discovery process. Here, we report the combination of site-directed mutagenesis and electrophilic fragments to enable the rapid identification of small molecules that selectively inhibit the mutant protein. Using the bromodomain-containing protein BRD4 as an example, we employed a structure-based approach to identify the L94C mutation in the first bromodomain of BRD4 [BRD4(1)] as having a minimal effect on BRD4(1) function. We then screened a focused, KAc mimic-containing fragment set and a diverse fragment library against the mutant and wild-type proteins and identified a series of fragments that showed high selectivity for the mutant protein. These compounds were elaborated to include an alkyne click tag to enable the attachment of a fluorescent dye. These clickable compounds were then assessed in HEK293T cells, transiently expressing BRD4(1)WT or BRD4(1)L94C, to determine their selectivity for BRD4(1)L94C over other possible cellular targets. One compound was identified that shows very high selectivity for BRD4(1)L94C over all other proteins. This work provides a proof-of-concept that the combination of site-directed mutagenesis and electrophilic fragments, in a mutate and conjugate approach, can enable rapid identification of small molecule inhibitors for an appropriately mutated protein of interest. This technology can be used to assess the cellular phenotype of inhibiting the protein of interest, and the electrophilic ligand provides a starting point for noncovalent ligand development.

Published

2023

42. The Chlamydia pneumoniae effector SemD exploits its host's endocytic machinery by structural and functional mimicry.

Author

Kocher, Fabienne, Applegate, Violetta, Reiners, Jens, Port, Astrid, Spona, Dominik, Hänsch, Sebastian, Mirzaiebadizi, Amin, Ahmadian, Mohammad Reza, Smits, Sander H. J., Hegemann, Johannes H., and Mölleken, Katja

Subjects

CELL cycle proteins, CYTOSKELETON, CELL membranes, INTRACELLULAR pathogens, EPITHELIAL cells

Abstract

To enter epithelial cells, the obligate intracellular pathogen Chlamydia pneumoniae secretes early effector proteins, which bind to and modulate the host-cell's plasma membrane and recruit several pivotal endocytic host proteins. Here, we present the high-resolution structure of an entry-related chlamydial effector protein, SemD. Co-crystallisation of SemD with its host binding partners demonstrates that SemD co-opts the Cdc42 binding site to activate the actin cytoskeleton regulator N-WASP, making active, GTP-bound Cdc42 superfluous. While SemD binds N-WASP much more strongly than Cdc42 does, it does not bind the Cdc42 effector protein FMNL2, indicating effector protein specificity. Furthermore, by identifying flexible and structured domains, we show that SemD can simultaneously interact with the membrane, the endocytic protein SNX9, and N-WASP. Here, we show at the structural level how a single effector protein can hijack central components of the host's endocytic system for efficient internalization. The Chlamydia pneumoniae effector SemD binds and activates the actin regulator N-WASP, structurally and functionally mimicking the endogenous N-WASP activator and small GTPase Cdc42GTP, hijacking the host cell endocytic machinery via this interaction. [ABSTRACT FROM AUTHOR]

Published

2024

43. Cryo-EM structure of the CDK2-cyclin A-CDC25A complex.

Author

Rowland, Rhianna J., Korolchuk, Svitlana, Salamina, Marco, Tatum, Natalie J., Ault, James R., Hart, Sam, Turkenburg, Johan P., Blaza, James N., Noble, Martin E. M., and Endicott, Jane A.

Subjects

PROTEIN-protein interactions, CELL cycle proteins, CELL division, CELL cycle, PHOSPHATASES

Abstract

The cell division cycle 25 phosphatases CDC25A, B and C regulate cell cycle transitions by dephosphorylating residues in the conserved glycine-rich loop of CDKs to activate their activity. Here, we present the cryo-EM structure of CDK2-cyclin A in complex with CDC25A at 2.7 Å resolution, providing a detailed structural analysis of the overall complex architecture and key protein-protein interactions that underpin this 86 kDa complex. We further identify a CDC25A C-terminal helix that is critical for complex formation. Sequence conservation analysis suggests CDK1/2-cyclin A, CDK1-cyclin B and CDK2/3-cyclin E are suitable binding partners for CDC25A, whilst CDK4/6-cyclin D complexes appear unlikely substrates. A comparative structural analysis of CDK-containing complexes also confirms the functional importance of the conserved CDK1/2 GDSEID motif. This structure improves our understanding of the roles of CDC25 phosphatases in CDK regulation and may inform the development of CDC25-targeting anticancer strategies. CDC25 phosphatases are attractive anticancer drug targets that regulate CDK activity. Here, the authors present the cryo-EM structure of the CDK2-cyclin A-CDC25A complex at 2.7 Å resolution, detailing key protein-protein interactions. [ABSTRACT FROM AUTHOR]

Published

2024

44. Based on machine learning, CDC20 has been identified as a biomarker for postoperative recurrence and progression in stage I & II lung adenocarcinoma patients.

Author

Rui Miao, Zhi Xu, Tao Han, Yafeng Liu, Jiawei Zhou, Jianqiang Guo, Yingru Xing, Ying Bai, Zhonglei He, Jing Wu, Wenxin Wang, and Dong Hu

Subjects

RANDOM forest algorithms, CANCER cell migration, GENE regulatory networks, GENE expression, CELL cycle proteins

Abstract

Objective: By utilizing machine learning, we can identify genes that are associated with recurrence, invasion, and tumor stemness, thus uncovering new therapeutic targets. Methods: To begin, we obtained a gene set related to recurrence and invasion from the GEO database, a comprehensive gene expression database. We then employed the Weighted Gene Co-expression Network Analysis (WGCNA) to identify core gene modules and perform functional enrichment analysis on them. Next, we utilized the random forest and random survival forest algorithms to calculate the genes within the key modules, resulting in the identification of three crucial genes. Subsequently, one of these key genes was selected for prognosis analysis and potential drug screening using the Kaplan-Meier tool. Finally, in order to examine the role of CDC20 in lung adenocarcinoma (LUAD), we conducted a variety of in vitro and in vivo experiments, including wound healing assay, colony formation assays, Transwell migration assays, flow cytometric cell cycle analysis, western blotting, and a mouse tumor model experiment. Results: First, we collected a total of 279 samples from two datasets, GSE166722 and GSE31210, to identify 91 differentially expressed genes associated with recurrence, invasion, and stemness in lung adenocarcinoma. Functional enrichment analysis revealed that these key gene clusters were primarily involved in microtubule binding, spindle, chromosomal region, organelle fission, and nuclear division. Next, using machine learning, we identified and validated three hub genes (CDC45, CDC20, TPX2), with CDC20 showing the highest correlation with tumor stemness and limited previous research. Furthermore, we found a close association between CDC20 and clinical pathological features, poor overall survival (OS), progression-free interval (PFI), progression-free survival (PFS), and adverse prognosis in lung adenocarcinoma patients. Lastly, our functional research demonstrated that knocking down CDC20 could inhibit cancer cell migration, invasion, proliferation, cell cycle progression, and tumor growth possibly through the MAPK signaling pathway. Conclusion: CDC20 has emerged as a novel biomarker for monitoring treatment response, recurrence, and disease progression in patients with lung adenocarcinoma. Due to its significance, further research studying CDC20 as a potential therapeutic target is warranted. Investigating the role of CDC20 could lead to valuable insights for developing new treatments and improving patient outcomes. [ABSTRACT FROM AUTHOR]

Published

2024

45. Differential miRNA and Protein Expression Reveals miR-1285, Its Targets TGM2 and CDH-1, as Well as CD166 and S100A13 as Potential New Biomarkers in Patients with Diabetes Mellitus and Pancreatic Adenocarcinoma.

Author

Kolokotronis, Theodoros, Majchrzak-Stiller, Britta, Buchholz, Marie, Mense, Vanessa, Strotmann, Johanna, Peters, Ilka, Skrzypczyk, Lea, Liffers, Sven-Thorsten, Menkene, Louise Massia, Wagner, Mathias, Glanemann, Matthias, Betsou, Fay, Ammerlaan, Wim, Schmidt, Ronny, Schröder, Christoph, Uhl, Waldemar, Braumann, Chris, and Höhn, Philipp

Subjects

*DIABETES complications, *CELL cycle proteins, *RESEARCH funding, *DATA analysis, *T-test (Statistics), *MICRORNA, *POLYMERASE chain reaction, *TRANSGLUTAMINASES, *ENZYMES, *TUMOR markers, *CANCER patients, *PROTEIN microarrays, *DESCRIPTIVE statistics, *PANCREATIC tumors, *ANTIGENS, *GENE expression, *DUCTAL carcinoma, *PROTEOMICS, *WESTERN immunoblotting, *ONE-way analysis of variance, *STATISTICS, *COMPARATIVE studies, *DISEASE risk factors

Abstract

Simple Summary: Pancreatic ductal adenocarcinoma is a very lethal tumor entity with the late appearance of clinical signs and the absence of biomarkers for early diagnosis. Diabetes mellitus can increase the risk of pancreatic cancer, as well as the effect of treatment modalities, so patients with PDAC and DM represent a special study group. We validated miRNA1285-3p, TGM2, CDH-1, CD166, and S100A13 as potential meaningful biomarkers to characterize patients with PDAC + DM. The present study represents a pilot approach to address this question. The potential biomarkers presented in the current study could contribute to the search for biomarkers for the diagnosis of PDAC, enabling early detection of PDAC in DM patients in the future. Early detection of PDAC remains challenging due to the lack of early symptoms and the absence of reliable biomarkers. The aim of the present project was to identify miRNA and proteomics signatures discriminating PDAC patients with DM from nondiabetic PDAC patients. Proteomics analysis and miRNA array were used for protein and miRNA screening. We used Western blotting and Real-Time Quantitative Reverse Transcription polymerase chain reaction (qRT-PCR) for protein and miRNA validation. Comparisons between experimental groups with normal distributions were performed using one-way ANOVA followed by Tukey's post hoc test, and pairwise tests were performed using t-tests. p ≤ 0.05 was considered statistically significant. Protein clusters of differentiation 166 (CD166), glycoprotein CD63 (CD63), S100 calcium-binding protein A13 (S100A13), and tumor necrosis factor-β (TNF-β) were detected in the proteomics screening. The miRNA assay revealed a differential miRNA 1285 regulation. Previously described target proteins of miR-1285 cadherin-1 (CDH-1), cellular Jun (c-Jun), p53, mothers against decapentaplegic homolog 4 (Smad4), human transglutaminase 2 (TGM2) and yes-associated protein (YAP), were validated via Western blotting. miR-1285-3p was successfully validated as differentially regulated in PDAC + DM via qRT-PCR. Overall, our data suggest miRNA1285-3p, TGM2, CDH-1, CD166, and S100A13 as potential meaningful biomarker candidates to characterize patients with PDAC + DM. Data are available via ProteomeXchange with the identifier PXD053169. [ABSTRACT FROM AUTHOR]

Published

2024

46. CDC20 Holds Novel Regulation Mechanism in RPA1 during Different Stages of DNA Damage to Induce Radio-Chemoresistance.

Author

Gao, Yang, Wen, Pengbo, Shao, Chenran, Ye, Cheng, Chen, Yuji, You, Junyu, and Su, Zhongjing

Subjects

*HOMOLOGOUS recombination, *CELL cycle proteins, *CELL nuclei, *DNA repair, *DNA damage, *REPORTER genes

Abstract

Targeting CDC20 can enhance the radiosensitivity of tumor cells, but the function and mechanism of CDC20 on DNA damage repair response remains vague. To examine that issue, tumor cell lines, including KYSE200, KYSE450, and HCT116, were utilized to detect the expression, function, and underlying mechanism of CDC20 in radio-chemoresistance. Western blot and immunofluorescence staining were employed to confirm CDC20 expression and location, and radiation could upregulate the expression of CDC20 in the cell nucleus. The homologous recombination (HR) and non-homologous end joining (NHEJ) reporter gene systems were utilized to explore the impact of CDC20 on DNA damage repair, indicating that CDC20 could promote HR repair and radio/chemo-resistance. In the early stages of DNA damage, CDC20 stabilizes the RPA1 protein through protein-protein interactions, activating the ATR-mediated signaling cascade, thereby aiding in genomic repair. In the later stages, CDC20 assists in the subsequent steps of damage repair by the ubiquitin-mediated degradation of RPA1. CCK-8 and colony formation assay were used to detect the function of CDC20 in cell vitality and proliferation, and targeting CDC20 can exacerbate the increase in DNA damage levels caused by cisplatin or etoposide. A tumor xenograft model was conducted in BALB/c-nu/nu mice to confirm the function of CDC20 in vivo, confirming the in vitro results. In conclusion, this study provides further validation of the potential clinical significance of CDC20 as a strategy to overcome radio-chemoresistance via uncovering a novel role of CDC20 in regulating RPA1 during DNA damage repair. [ABSTRACT FROM AUTHOR]

Published

2024

47. PLEKHG1 : New Potential Candidate Gene for Periventricular White Matter Abnormalities.

Author

Calì, Francesco, Vinci, Mirella, Treccarichi, Simone, Papa, Carla, Gloria, Angelo, Musumeci, Antonino, Federico, Concetta, Vitello, Girolamo Aurelio, Nicotera, Antonio Gennaro, Di Rosa, Gabriella, Vetri, Luigi, Saccone, Salvatore, and Elia, Maurizio

Subjects

*GUANINE nucleotide exchange factors, *CELL physiology, *PERIVENTRICULAR leukomalacia, *CELL cycle proteins, *WHITE matter (Nerve tissue)

Abstract

Hypoxic-ischemic brain damage presents a significant neurological challenge, often manifesting during the perinatal period. Specifically, periventricular leukomalacia (PVL) is emerging as a notable contributor to cerebral palsy and intellectual disabilities. It compromises cerebral microcirculation, resulting in insufficient oxygen or blood flow to the periventricular region of the brain. As widely documented, these pathological conditions can be caused by several factors encompassing preterm birth (4–5% of the total cases), as well single cotwin abortion and genetic variants such as those associated with GTPase pathways. Whole exome sequencing (WES) analysis identified a de novo causative variant within the pleckstrin homology domain-containing family G member 1 (PLEKHG1) gene in a patient presenting with PVL. The PLEKHG1 gene is ubiquitously expressed, showing high expression patterns in brain tissues. PLEKHG1 is part of a family of Rho guanine nucleotide exchange factors, and the protein is essential for cell division control protein 42 (CDC42) activation in the GTPase pathway. CDC42 is a key small GTPase of the Rho-subfamily, regulating various cellular functions such as cell morphology, migration, endocytosis, and cell cycle progression. The molecular mechanism involving PLEKHG1 and CDC42 has an intriguing role in the reorientation of cells in the vascular endothelium, thus suggesting that disruption responses to mechanical stress in endothelial cells may be involved in the formation of white matter lesions. Significantly, CDC42 association with white matter abnormalities is underscored by its MIM phenotype number. In contrast, although PLEKHG1 has been recently associated with patients showing white matter hyperintensities, it currently lacks a MIM phenotype number. Additionally, in silico analyses classified the identified variant as pathogenic. Although the patient was born prematurely and subsequently to dichorionic gestation, during which its cotwin died, we suggest that the variant described can strongly contribute to PVL. The aim of the current study is to establish a plausible association between the PLEKHG1 gene and PVL. [ABSTRACT FROM AUTHOR]

Published

2024

48. Acylhydrazone Derivative A5 Promotes Neurogenesis by Up-Regulating Neurogenesis-Related Genes and Inhibiting Cell-Cycle Progression in Neural Stem/Progenitor Cells.

Author

Xiang, Xiaoliang, Jiang, Xia, Lin, Hongwei, Yu, Meixing, Wu, Liming, and Zhou, Rong

Subjects

*CELL cycle proteins, *NEURAL stem cells, *DEVELOPMENTAL neurobiology, *DRUG discovery, *NEURAL circuitry, *PROGENITOR cells

Abstract

Adult neurogenesis involves the generation of functional neurons from neural progenitor cells, which have the potential to complement and restore damaged neurons and neural circuits. Therefore, the development of drugs that stimulate neurogenesis represents a promising strategy in stem cell therapy and neural regeneration, greatly facilitating the reconstruction of neural circuits in cases of neurodegeneration and brain injury. Our study reveals that compound A5, previously designed and synthesized by our team, exhibits remarkable neuritogenic activities, effectively inducing neurogenesis in neural stem/progenitor cells (NSPCs). Subsequently, transcriptome analysis using high-throughput Illumina RNA-seq technology was performed to further elucidate the underlying molecular mechanisms by which Compound A5 promotes neurogenesis. Notably, comparative transcriptome analysis showed that the up-regulated genes were mainly associated with neurogenesis, and the down-regulated genes were mainly concerned with cell cycle progression. Furthermore, we confirmed that Compound A5 significantly affected the expression of transcription factors related to neurogenesis and cell cycle regulatory proteins. Collectively, these findings identify a new compound with neurogenic activity and may provide insights into drug discovery for neural repair and regeneration. [ABSTRACT FROM AUTHOR]

Published

2024

49. Proteomic profiling improves prognostic risk stratification of the Sarculator nomogram in soft tissue sarcomas of the extremities and trunk wall.

Author

Chadha, Madhumeeta, Iadecola, Sara, Jenks, Andrew, Pankova, Valeriya, Tam, Yuen Bun, Burns, Jessica, Arthur, Amani, Wilding, Christopher P., Chen, Liang, Chudasama, Priya, Callegaro, Dario, Strauss, Dirk C., Thway, Khin, Gronchi, Alessandro, Jones, Robin L., Miceli, Rosalba, Pasquali, Sandro, and Huang, Paul H.

Subjects

*CELL cycle proteins, *SARCOMA, *DNA replication, *OVERALL survival, *DRUG target

Abstract

Background: High‐risk soft tissue sarcomas of the extremities and trunk wall (eSTS), as defined by the Sarculator nomogram, are more likely to benefit from (neo)adjuvant anthracycline‐based therapy compared to low/intermediate‐risk patients. The biology underpinning these differential treatment outcomes remain unknown. Methods: We analysed proteomic profiles and clinical outcomes of 123 eSTS patients. A Cox model for overall survival including the Sarculator was fitted to individual data to define four risk groups. A DNA replication protein signature‐Sarcoma Proteomic Module 6 (SPM6) was evaluated for association with clinicopathological factors and risk groups. SPM6 was added as a covariate together with Sarculator in a multivariable Cox model to assess improvement in prognostic risk stratification. Results: DNA replication and cell cycle proteins were upregulated in high‐risk versus very low‐risk patients. Evaluation of the functional effects of CRISPR‐Cas9 gene knockdown of proteins enriched in high‐risk patients using the cancer cell line encyclopaedia database identified candidate drug targets. SPM6 was significantly associated with tumour malignancy grade (p = 1.6e‐06), histology (p = 1.4e‐05) and risk groups (p = 2.6e‐06). Cox model analysis showed that SPM6 substantially contributed to a better calibration of the Sarculator nomogram (Index of Prediction Accuracy = 0.109 for Sarculator alone versus 0.165 for Sarculator + SPM6). Conclusions: Risk stratification of patient with STS is defined by distinct biological pathways across a range of cancer hallmarks. Incorporation of SPM6 protein signature improves prognostic risk stratification of the Sarculator nomogram. This study highlights the utility of integrating protein signatures for the development of next‐generation nomograms. [ABSTRACT FROM AUTHOR]

Published

2024

50. TUSC3, p53 and p21 genetic association with development of oral submucous fibrosis and oral squamous cell carcinoma among addictive tobacco chewers of Pakistan.

Author

Zaidi, Syed Aqib Ali, Chughtai, Nadia, Abbassi, Zubair Ahmed, Alam, Jehan, Malick, Tuba Shakil, Salim, Asmat, and Saleem, Saima

Subjects

SUBSTANCE abuse, SQUAMOUS cell carcinoma, MOUTH tumors, RESEARCH funding, CELL cycle proteins, HEAD & neck cancer, PRECANCEROUS conditions, SEX distribution, GENETIC markers, DESCRIPTIVE statistics, FIBROSIS, TUMOR suppressor genes, GENETIC polymorphisms, GENETIC variation, GENE expression profiling, SMOKELESS tobacco, GENETIC mutation, COMPARATIVE studies, GENOTYPES, DNA-binding proteins, DISEASE complications

Abstract

Background: This study delves into the intricate landscape of oral cancer, a global concern with a high incidence in Asian countries. We focus on oral squamous cell carcinoma (OSCC), primarily driven by the consumption of betel nut and its derivatives. OSCC often arises from premalignant lesions like oral submucous fibrosis (OSF). In Pakistan, OSCC is prevalent among men due to various addictive substances, including smokeless tobacco and chewing materials. Mutations in tumor suppressor genes, such as TP53 and p21, play crucial roles in this malignancy's development. We also explore the involvement of TUSC3 gene deletion in OSCC and OSF. Methods: In this study we investigated demographics, TUSC3 gene expression, deletion analysis, and TP53 and p21 genetic alterations in OSCC and OSF patients (blood and tissue of 50 samples in each condition) who had tobacco derivates usage history. The association analysis was carried out mainly through PCR based genotyping. Results: The study's patient cohort (OSCC and OSF) displayed a wide age range from 13 to 65 years (Mean = 32.96 years). Both conditions were more prevalent in males, with a male-female ratio of approximately 2.5:1. Chewing habits analysis revealed high frequencies of gutka use in both OSF and OSCC patients. TUSC3 expression analysis in OSCC cell lines indicated significant downregulation. Genotyping showed no TUSC3 deletion in OSF cases, but a deletion rate of over 22% in OSCC tissue samples. Analysis supported a significant association of TUSC3 deletion with OSCC development but not with OSF. Polymorphism in p53 exon 4 and p21 (rs1801270) were significantly associated with both OSCC and OSF, adding to their pathogenesis. Our findings further revealed a strong correlation between TUSC3 deletion and the excessive use of tobacco and related products, shedding light on the genetic underpinnings of OSCC development. Conclusions: Notably, our study provides a crucial insight into genetic aspects underlying OSCC and OSF in response of addictive consumption of areca nut, betel quid, and tobacco derivatives. A significant association between TUSC3 deletion and OSCC development, along with polymorphisms in TP53 and p21, underscores the importance of further research into the molecular mechanisms driving oral cancer progression for improved diagnosis and treatment outcomes. [ABSTRACT FROM AUTHOR]

Published

2024