Your search keyword '"CELL cycle proteins"' showing total 71,774 results

101. Survivin as a Therapeutic Target for the Treatment of Human Cancer.

Author

Wang, Qiang and Greene, Mark I.

Subjects

*CELL cycle proteins, *MITOCHONDRIA, *AUTOPHAGY, *CANCER relapse, *CELL physiology, *APOPTOSIS, *TREATMENT effectiveness, *CANCER chemotherapy, *CHROMOSOMES, *TUMORS, *DRUG resistance, *CHEMICAL inhibitors

Abstract

Simple Summary: Survivin is overexpressed in a wide variety of human cancers and is associated with increased chemotherapy resistance, recurrence, and shorter patient survival. Although survivin was first identified as an inhibitor of apoptosis based on its sequence homology, recent studies show that survivin primarily plays a role in the regulation of cell division, as a component of the chromosome passenger complex, which can be localized to the centromere, the spindle midzone, or midbody in a cell cycle-dependent manner. Disruption of survivin function generally leads to mitotic catastrophe and is associated with elevated levels of aneuploidy. In contrast, ectopic expression of survivin can promote cell survival under certain conditions and is implicated in mediating resistance to various cancer drugs, possibly by interactions with molecules that modulate apoptotic pathways. A potential role of survivin in the regulation of mitochondrial functions and processes of autophagy has emerged. Because of its prevalent overexpression in cancer and very limited expression in normal tissues, survivin has been proposed as an ideal therapeutic target, and various approaches have been investigated for survivin inhibition. Here we provide a critical review of our current understanding of the role of survivin in promoting malignancy and strategies for the development of survivin-targeted therapy for cancer. Survivin was initially identified as a member of the inhibitor apoptosis (IAP) protein family and has been shown to play a critical role in the regulation of apoptosis. More recent studies showed that survivin is a component of the chromosome passenger complex and acts as an essential mediator of mitotic progression. Other potential functions of survivin, such as mitochondrial function and autophagy, have also been proposed. Survivin has emerged as an attractive target for cancer therapy because its overexpression has been found in most human cancers and is frequently associated with chemotherapy resistance, recurrence, and poor survival rates in cancer patients. In this review, we discuss our current understanding of how survivin mediates various aspects of malignant transformation and drug resistance, as well as the efforts that have been made to develop therapeutics targeting survivin for the treatment of cancer. [ABSTRACT FROM AUTHOR]

Published

2024

102. Idebenone Exerts anti-Triple Negative Breast Cancer Effects via Dual Signaling Pathways of GADD45 and AMPK.

Author

Zhang, Yidan, Yang, Fan, Wu, Jiahao, Huang, Jianhong, Li, Peiqing, and Huang, Guanqun

Subjects

*MITOCHONDRIAL physiology, *BIOLOGICAL models, *IN vitro studies, *XENOGRAFTS, *IN vivo studies, *STAINS & staining (Microscopy), *SEQUENCE analysis, *AUTOPHAGY, *CELL cycle proteins, *APOPTOSIS, *CELLULAR signal transduction, *UBIQUINONES, *CELL survival, *CELL cycle, *CELL motility, *TRANSFERASES, *GENE expression profiling, *CELL proliferation, *CELL lines, *BIOLOGICAL assay, *BREAST tumors, *MEMBRANE potential

Abstract

Idebenone, a mitochondrial regulator, has exhibited anti-cancer activity in neurogenic and prostate tumor cells; however, its efficacy and specific targets in the treatment of triple-negative breast cancer (TNBC) remain unclear. This study aims to evaluate the potential of Idebenone as a therapeutic agent for TNBC. TNBC cell lines and Xenograft mouse models were used to assess the effect of Idebenone on TNBC both in vitro and in vivo. To investigate the underlying mechanism of Idebenone's effect on TNBC, cell viability assay, transwell invasion assay, cell cycle analysis, apoptosis assay, mitochondrial membrane potential assay, immunofluorescence staining, and transcriptome sequencing were utilized. The results showed that Idebenone impeded the proliferation, colony formation, migration, and invasion of TNBC cells, suppressed apoptosis, and halted the cell cycle in the G2/M phase. The inhibitory effect of Idebenone on TNBC was associated with the GADD45/CyclinB/CDK1 signaling pathway. By disrupting the mitochondrial membrane potential (MMP) and promoting mitophagy, Idebenone promoted cell autophagy through the AMPK/mTOR pathway, thus further suppressing the proliferation of TNBC cells. Furthermore, we found that Idebenone inhibited the development of TNBC in vivo. In conclusion, Idebenone may be a promising therapeutic option for TNBC as it is capable of inducing autophagy and apoptosis. [ABSTRACT FROM AUTHOR]

Published

2024

103. The Role of Speedy/RINGO Protein in Breast Cancer as a Future Biomarker.

Author

TANRIVERDI, OZGUR and YILDIZ, AYSEGUL

Subjects

BREAST cancer, CYCLIN-dependent kinase inhibitors, CELL cycle proteins, CYCLIN-dependent kinases, AMINO acid sequence, BIOMARKERS, PROTEINS

Abstract

Background/Aim: Cyclin-dependent kinases (CDKs) are proteins that require the binding of regulatory subunits called cyclins and play a key role in cell cycle progression and activation. CDKs play a key role in carcinogenesis of many solid malignancies, and inhibition of these proteins has produced anti-cancer effects demonstrated in preclinical studies. This narrative review was conducted to develop a hypothetical approach to determine whether Speedy/RINGO, a protein associated with CDK2, could be a possible predictive factor in breast cancer patients treated with a CDK4/6 inhibitor. Materials and Methods: A literature search was conducted in PubMed, Web of Science, Medline, and Google Scholars search engines to match the following words: "Speedy/RINGO" or "Spy1" and "CDKs" or "Cyclindependent kinases (CDKs)" and "CDK4/6 inhibitors" and "Regulation" and "Molecular" and "Breast cancer" and "Carcinogenesis". Only articles investigating the relationship between the Speedy/RINGO protein and CDKs at the molecular level were included. Literature information was compiled by trying to establish a relationship with our hypothesis question. Results: Speedy/RINGO is a tightly regulated proto-oncogenic mammalian protein playing important roles in the somatic cell cycle. Studies have emphasized that although it does not have amino acid sequence homology with cyclins, it can activate CDK2. In addition, results showing molecular compensation of CDK4/6 inhibition through CDK2 activation, also showed that CDK2 can predict drug resistance. Another important finding was that overexpressed Speedy/RINGO, during CDK4/6 inhibitor treatment, could strongly activate CDK2, resulting in a negative response to treatment. Conclusion: Although many predictive factors have been investigated to indicate response to CDK4/6 inhibitors or determine drug resistance, a consensus biomarker has yet to be established. In light of the information obtained from our review, it can be concluded that the Speedy/RINGO protein may have an important role as a predictive biomarker in terms of response to treatment, continuity of treatment and drug resistance in patients treated with CDK4/6 inhibitors. [ABSTRACT FROM AUTHOR]

Published

2024

104. The TP53-activated E3 ligase RNF144B is a tumour suppressor that prevents genomic instability.

Author

Abad, Etna, Sandoz, Jérémy, Romero, Gerard, Zadra, Ivan, Urgel-Solas, Julia, Borredat, Pablo, Kourtis, Savvas, Ortet, Laura, Martínez, Carlos M., Weghorn, Donate, Sdelci, Sara, and Janic, Ana

Subjects

*UBIQUITIN ligases, *DNA repair, *CELL transformation, *CELL proliferation, *CELL cycle, *CELL cycle proteins

Abstract

Background: TP53, the most frequently mutated gene in human cancers, orchestrates a complex transcriptional program crucial for cancer prevention. While certain TP53-dependent genes have been extensively studied, others, like the recently identified RNF144B, remained poorly understood. This E3 ubiquitin ligase has shown potent tumor suppressor activity in murine Eμ Myc-driven lymphoma, emphasizing its significance in the TP53 network. However, little is known about its targets and its role in cancer development, requiring further exploration. In this work, we investigate RNF144B's impact on tumor suppression beyond the hematopoietic compartment in human cancers. Methods: Employing TP53 wild-type cells, we generated models lacking RNF144B in both non-transformed and cancerous cells of human and mouse origin. By using proteomics, transcriptomics, and functional analysis, we assessed RNF144B's impact in cellular proliferation and transformation. Through in vitro and in vivo experiments, we explored proliferation, DNA repair, cell cycle control, mitotic progression, and treatment resistance. Findings were contrasted with clinical datasets and bioinformatics analysis. Results: Our research underscores RNF144B's pivotal role as a tumor suppressor, particularly in lung adenocarcinoma. In both human and mouse oncogene-expressing cells, RNF144B deficiency heightened cellular proliferation and transformation. Proteomic and transcriptomic analysis revealed RNF144B's novel function in mediating protein degradation associated with cell cycle progression, DNA damage response and genomic stability. RNF144B deficiency induced chromosomal instability, mitotic defects, and correlated with elevated aneuploidy and worse prognosis in human tumors. Furthermore, RNF144B-deficient lung adenocarcinoma cells exhibited resistance to cell cycle inhibitors that induce chromosomal instability. Conclusions: Supported by clinical data, our study suggests that RNF144B plays a pivotal role in maintaining genomic stability during tumor suppression. [ABSTRACT FROM AUTHOR]

Published

2024

105. Deubiquitination of CDC6 by OTUD6A promotes tumour progression and chemoresistance.

Author

Cui, Jianfeng, Liu, Xiaochen, Shang, Qinghong, Sun, Shuna, Chen, Shouzhen, Dong, Jianping, Zhu, Yaofeng, Liu, Lei, Xia, Yangyang, Wang, Yong, Xiang, Lu, Fan, Bowen, Zhan, Jiafeng, Zhou, Yadi, Chen, Pengxiang, Zhao, Renchang, Liu, Xiaofei, Xing, Nianzeng, Wu, Dalei, and Shi, Benkang

Subjects

*CELL cycle proteins, *ONCOGENIC proteins, *CELL cycle regulation, *UBIQUITIN ligases, *DRUG resistance in cancer cells

Abstract

Background: CDC6 is an oncogenic protein whose expression level fluctuates during the cell cycle. Although several E3 ubiquitin ligases responsible for the ubiquitin-mediated proteolysis of CDC6 have been identified, the deubiquitination pathway for CDC6 has not been investigated. Methods: The proteome-wide deubiquitinase (DUB) screening was used to identify the potential regulator of CDC6. Immunofluorescence, protein half-life and deubiquitination assays were performed to determine the protein stability of CDC6. Gain- and loss-of-function experiments were implemented to analyse the impacts of OUTD6A-CDC6 axis on tumour growth and chemosensitivity in vitro. N-butyl-N-(4-hydroxybutyl) nitrosamine (BBN)-induced conditional Otud6a knockout (CKO) mouse model and tumour xenograft model were performed to analyse the role of OTUD6A-CDC6 axis in vivo. Tissue specimens were used to determine the association between OTUD6A and CDC6. Results: OTUD6A interacts with, depolyubiquitinates and stabilizes CDC6 by removing K6-, K33-, and K48-linked polyubiquitination. Moreover, OTUD6A promotes cell proliferation and decreases sensitivity to chemotherapy by upregulating CDC6. CKO mice are less prone to BCa tumorigenesis induced by BBN, and knockdown of OTUD6A inhibits tumour progression in vivo. Furthermore, OTUD6A protein level has a positive correlation with CDC6 protein level, and high protein levels of OTUD6A and CDC6 are associated with poor prognosis in patients with bladder cancer. Conclusions: We reveal an important yet missing piece of novel DUB governing CDC6 stability. In addition, our findings propose a model for the OTUD6A-CDC6 axis that provides novel insights into cell cycle and chemosensitivity regulation, which may become a potential biomarker and promising drug target for cancer treatment. [ABSTRACT FROM AUTHOR]

Published

2024

106. Short-chain fatty acids induced lung tumor cell death and increased peripheral blood CD4+ T cells in NSCLC and control patients ex vivo.

Author

Thome, Carolin D., Tausche, Patrick, Hohenberger, Katja, Zuqin Yang, Krammer, Susanne, Trufa, Denis I., Sirbu, Horia, Schmidt, Joachim, and Finotto, Susetta

Subjects

SHORT-chain fatty acids, CELL death, CELL cycle proteins, NON-small-cell lung carcinoma, T cells

Abstract

Background: Despite therapy advances, one of the leading causes of cancer deaths still remains lung cancer. To improve current treatments or prevent nonsmall cell lung cancer (NSCLC), the role of the nutrition in cancer onset and progression needs to be understood in more detail. While in colorectal cancer, the influence of local microbiota derived SCFAs have been well investigated, the influence of SCFA on lung cancer cells via peripheral blood immune system should be investigated more deeply. In this respect, nutrients absorbed via the gut might affect the tumor microenvironment (TME) and thus play an important role in tumor cell growth. Objective: This study focuses on the impact of the short-chain fatty acid (SCFA) Sodium Butyrate (SB), on lung cancer cell survival. We previously described a protumoral role of glucose on A549 lung adenocarcinoma cell line. In this study, we wanted to know if SB would counteract the effect of glucose and thus cultured A549 and H520 in vitro with and without SB in the presence or absence of glucose and investigated how the treatment with SB affects the survival of lung cancer cells and its influence on immune cells fighting against lung cancer. Methods: In this study, we performed cell culture experiments with A549, H520 and NSCLC-patient-derived epithelial cells under different SB levels. To investigate the influence on the immune system, we performed in vitro culture of peripheral mononuclear blood cells (PBMC) from control, smoker and lung cancer patients with increasing SB concentrations. Results: To investigate the effect of SB on lung tumor cells, we first analyzed the effect of 6 different concentrations of SB on A549 cells at 48 and 72 hours cell culture. Here we found that, SB treatment reduced lung cancer cell survival in a concentration dependent manner. We next focused our deeper analysis on the two concentrations, which caused the maximal reduction in cell survival. Here, we observed that SB led to cell cycle arrest and induced early apoptosis in A549 lung cancer cells. The expression of cell cycle regulatory proteins and A549 lung cancer stem cell markers (CD90) was induced. Additionally, this study explored the role of interferon-gamma (IFN-g) and its receptor (IFN-g-R1) in combination with SB treatment, revealing that, although IFN-g-R1 expression was increased, IFN-g did not affect the efficacy of SB in reducing tumor cell viability. Furthermore, we examined the effects of SB on immune cells, specifically CD8 + T cells and natural killer (NK) cells from healthy individuals, smokers, and NSCLC patients. SB treatment resulted in a decreased production of IFN-g and granzyme B in CD8+ T cells and NK cells. Moreover, SB induced IFN-g-R1 in NK cells and CD4+ T cells in the absence of glucose both in PBMCs from controls and NSCLC subjects. Conclusion: Overall, this study highlights the potential of SB in inhibiting lung cancer cell growth, triggering apoptosis, inducing cell cycle arrest, and modulating immune responses by activating peripheral blood CD4+ T cells while selectively inducing IFN-g-R1 in NK cells in peripheral blood and inhibiting peripheral blood CD8+ T cells and NK cells. Thus, understanding the mechanisms of action of SB in the TME and its influence on the immune system provide valuable insights of potentially considering SB as a candidate for adjunctive therapies in NSCLC. [ABSTRACT FROM AUTHOR]

Published

2024

107. 发育性颈椎管狭窄与脊髓型颈椎病血清差异蛋白组学分析.

Author

卜献忠, 卜保献, 许 伟, 李智斐, 杨汉立, 王微微, 周劲衍, and 钟远鸣

Subjects

*LIQUID chromatography-mass spectrometry, *CERVICAL spondylotic myelopathy, *SPINAL stenosis, *ADHERENS junctions, *CELL cycle proteins, *MICROFILAMENT proteins, *FIBRONECTINS, *CLAUDINS

Abstract

BACKGROUND: Previous studies have found that qi deficiency and blood stasis syndrome is the main syndrome among various TCM syndromes of cervical spondylotic myelopathy. However, there is no report on proteomic markers as early diagnosis indicators for the transformation of developmental cervical spinal stenosis with qi deficiency and blood stasis syndrome to cervical spondylotic myelopathy. OBJECTIVE: To explore serum proteomics difference between developmental cervical spinal stenosis and cervical spondylotic myelopathy and to find and identify the potential serum biomarkers between them. METHODS: Serum samples of nine patients with cervical spondylotic myelopathy of qi deficiency and blood stasis syndrome (experimental group) and nine patients with developmental cervical spinal stenosis of qi deficiency and blood stasis syndrome (control group) were collected. The proteomic analysis was carried out by Tandem Mass Tag combined with liquid chromatography tandem mass spectrometry, so as to find and identify differentially expressed proteins. RESULTS AND CONCLUSION: A total of 1027 significantly differential proteins were initially screened by TMT technology and 89 significantly differential proteins were finally identified (P < 0.05). Compared with the control group, there were 45 up-regulated proteins in the experimental group, such as α-actinin-4, α-actinin-1, cell division control protein 42 homolog, integrin-linked protein kinase and B-actin. Conversely, there were 44 down-regulated proteins in the experimental group compared with the control group, such as fibronectin, fibrinogen γ chain, fibrinogen α chain, fibrinogen β chain. Gene ontology enrichment analysis indicated that these differential proteins were involved in signal receptor binding, kinase binding, protein kinase activity, integrin binding, actin filament binding and other molecular functions. Based on the Kyoto Encyclopedia of Genes and Genomes pathway analysis, 20 common differential signal/metabolic pathways were identified, including Rap1 signaling pathway, adherens junction, tight junction, platelet activation, and regulation of actin cytoskeleton. Proteinprotein interaction analysis showed that ILK, FGA, FGB, FGG, FN1, Cdc42, ACTN1, ACTN4 and ACTB were located at the nodes of protein-protein interaction network and were closely related to bone formation and destruction system, nervous system, coagulation system, cellular inflammation and other systems. To conclude, the serum differentially expressed proteins between developmental cervical spinal stenosis and cervical spondylotic myelopathy can be successfully screened by Tandem Mass Tag combined with liquid chromatography tandem mass spectrometry. ILK, FN1, CDC42 and ACTN 4 are identified as specific markers for the transformation of developmental cervical spinal stenosis with qi deficiency and blood stasis syndrome into cervical spondylotic myelopathy. These findings provide a basis for further clarifying the transformation mechanism. [ABSTRACT FROM AUTHOR]

Published

2024

108. Synergistic Activity of DNA Damage Response Inhibitors in Combination with Radium-223 in Prostate Cancer.

Author

Dunne, Victoria L., Wright, Timothy C., Liberal, Francisco D. C. Guerra, O'Sullivan, Joe M., and Prise, Kevin M.

Subjects

*RADIUMTHERAPY, *CASTRATION-resistant prostate cancer, *IN vitro studies, *FLOW cytometry, *CELL cycle proteins, *T-test (Statistics), *RADIOTHERAPY, *RESEARCH funding, *ENZYME inhibitors, *ANTINEOPLASTIC agents, *APOPTOSIS, *TREATMENT effectiveness, *CELL culture, *CELL lines, *DNA damage, *COMBINED modality therapy, *X-rays, *WESTERN immunoblotting, *ONE-way analysis of variance, *CELL survival, *DRUG synergism, *PHARMACODYNAMICS, *EVALUATION

Abstract

Simple Summary: Radium-223 is used for the management of metastatic castration-resistant prostate cancer. However, the response to this treatment is poor. Targeting the DNA damage response pathway through pharmacological inhibition has the ability to enhance the radiation response. In this study, we investigated the radiosensitising effects of three different DNA damage response inhibitors targeting ATM, ATR, and PARP in combination with X-rays and radium-223 on human prostate cancer cell lines. Their effects on cell survival, DNA double-strand break repair, cell cycle distribution, and apoptosis were evaluated. We determined that these inhibitors increase the ability of X-rays and radium-223 to kill prostate cells to varying degrees. Moreover, inhibition of the DNA damage response pathways impeded the repair of radiation-induced DNA double-strand breaks and induced changes in cell cycle distribution. Altogether, our study determined DDR inhibition as a promising strategy to increase the effectiveness of treatments utilising X-rays and/or 223Ra for localised and metastatic castration-resistant prostate cancer. Radium-223 (223Ra) and Lutetium-177-labelled-PSMA-617 (177Lu-PSMA) are currently the only radiopharmaceutical treatments to prolong survival for patients with metastatic-castration-resistant prostate cancer (mCRPC); however, mCRPC remains an aggressive disease. Recent clinical evidence suggests patients with mutations in DNA repair genes associated with homologous recombination have a greater clinical benefit from 223Ra. In this study, we aimed to determine the utility of combining DNA damage response (DDR) inhibitors to increase the therapeutic efficacy of X-rays, or 223Ra. Radiobiological responses were characterised by in vitro assessment of clonogenic survival, repair of double strand breaks, cell cycle distribution, and apoptosis via PARP-1 cleavage. Here, we show that DDR inhibitors increase the therapeutic efficacy of both radiation qualities examined, which is associated with greater levels of residual DNA damage. Co-treatment of ATM or PARP inhibition with 223Ra increased cell cycle arrest in the G2/M phase. In comparison, combined ATR inhibition and radiation qualities caused G2/M checkpoint abrogation. Additionally, greater levels of apoptosis were observed after the combination of DDR inhibitors with 223Ra. This study identified the ATR inhibitor as the most synergistic inhibitor for both radiation qualities, supporting further pre-clinical evaluation of DDR inhibitors in combination with 223Ra for the treatment of prostate cancer. [ABSTRACT FROM AUTHOR]

Published

2024

109. NEDD4L is a promoter for angiogenesis and cell proliferation in human umbilical vein endothelial cells.

Author

Liu, Binghong, Song, Fei, Zhou, Xiaoxia, Wu, Chan, Huang, Huizhu, Wu, Weiyin, Li, Gang, and Wang, Yan

Subjects

UMBILICAL veins, ENDOTHELIAL cells, CELL proliferation, NEOVASCULARIZATION, CELL migration, CELL cycle proteins

Abstract

Dysregulated angiogenesis leads to neovascularization, which can promote or exacerbate various diseases. Previous studies have proved that NEDD4L plays an important role in hypertension and atherosclerosis. Hence, we hypothesized that NEDD4L may be a critical regulator of endothelial cell (EC) function. This study aimed to define the role of NEDD4L in regulating EC angiogenesis and elucidate their underlying mechanisms. Loss‐ and gain‐of‐function of NEDD4L detected the angiogenesis and mobility role in human umbilical vein endothelial cells (HUVECs) using Matrigel tube formation assay, cell proliferation and migration. Pharmacological pathway inhibitors and western blot were used to determine the underlying mechanism of NEDD4L‐regulated endothelial functions. Knockdown of NEDD4L suppressed tube formation, cell proliferation and cell migration in HUVECs, whereas NEDD4L overexpression promoted these functions. Moreover, NEDD4L‐regulated angiogenesis and cell progression are associated with the phosphorylation of Akt, Erk1/2 and eNOS and the expression of VEGFR2 and cyclin D1 and D3. Mechanically, further evidence was confirmed by using Akt blocker MK‐2206, Erk1/2 blocker U0126 and eNOS blocker L‐NAME. Overexpression NEDD4L‐promoted angiogenesis, cell migration and cell proliferation were restrained by these inhibitors. In addition, overexpression NEDD4L‐promoted cell cycle‐related proteins cyclin D1 and D3 were also suppressed by Akt blocker MK‐2206, Erk1/2 blocker U0126 and eNOS blocker L‐NAME. Our results demonstrated a novel finding that NEDD4L promotes angiogenesis and cell progression by regulating the Akt/Erk/eNOS pathways. [ABSTRACT FROM AUTHOR]

Published

2024

110. CDC45 promotes the stemness and metastasis in lung adenocarcinoma by affecting the cell cycle.

Author

Liu, Yafeng, Han, Tao, Xu, Zhi, Wu, Jing, Zhou, Jiawei, Guo, Jianqiang, Miao, Rui, Xing, Yingru, Ge, Deyong, Bai, Ying, and Hu, Dong

Subjects

*CELL cycle proteins, *CELL cycle, *CELL cycle regulation, *NON-small-cell lung carcinoma, *CANCER cell proliferation

Abstract

Objective: This study aimed to assess the functions of cell division cycle protein 45 (CDC45) in Non-small cell lung cancer (NSCLC) cancer and its effects on stemness and metastasis. Methods: Firstly, differentially expressed genes related to lung cancer metastasis and stemness were screened by differential analysis and lasso regression. Then, in vitro, experiments such as colony formation assay, scratch assay, and transwell assay were conducted to evaluate the impact of CDC45 knockdown on the proliferation and migration abilities of lung cancer cells. Western blotting was used to measure the expression levels of related proteins and investigate the regulation of CDC45 on the cell cycle. Finally, in vivo model with subcutaneous injection of lung cancer cells was performed to verify the effect of CDC45 on tumor growth. Results: This study identified CDC45 as a key gene potentially influencing tumor stemness and lymph node metastasis. Knockdown of CDC45 not only suppressed the proliferation and migration abilities of lung cancer cells but also caused cell cycle arrest at the G2/M phase. Further analysis revealed a negative correlation between CDC45 and cell cycle-related proteins, stemness-related markers, and tumor mutations. Mouse experiments confirmed that CDC45 knockdown inhibited tumor growth. Conclusion: As a novel regulator of stemness, CDC45 plays a role in regulating lung cancer cell proliferation, migration, and cell cycle. Therefore, CDC45 may serve as a potential target for lung cancer treatment and provide a reference for further mechanistic research and therapeutic development. [ABSTRACT FROM AUTHOR]

Published

2024

111. Significance of RCC2, Rac1 and p53 Expression in Breast Infiltrating Ductal Carcinoma; An Immunohistochemical Study.

Author

Hemida, Aiat Shaban, Abdelaziz, Reham Ahmed, Abd El-Wahed, Moshira Mohammed, Asaad, Nancy Yousef, Serag El-Dien, Marwa Mohammed, and Elshahat Ali, Hend Ali

Subjects

*TUMOR suppressor proteins, *CELL cycle proteins, *G proteins, *P53 protein, *CANCER cell proliferation, *BREAST

Abstract

Background & Objective: The regulator of chromosome condensation 2 (RCC2) and RAS-related C3 botulinum toxin substrate 1 (Rac1) have been implicated in the promotion of breast cancer cell proliferation and migration. The signaling pathway involving p53/RCC2/Rac1 has been proposed to contribute to the regulation of colon cancer metastasis. However, until now, this pathway has not been thoroughly investigated in breast cancer. This study seeks to explore the influence of immunohistochemical expression and the correlation among RCC2, Rac1, and p53 in breast infiltrating ductal carcinoma (IDC). Methods: Immunostaining was performed on 120 breast IDC specimens using RCC2, Rac1, and p53 antibodies. Statistical analyses were conducted to examine the correlations between these antibodies. Results: A Positive expression of RCC2, Rac1, and p53 was observed in 116 (96.7%), 120 (100%), and 33 (27.5%) of the breast cancer cases, respectively. RCC2, Rac1, and p53 demonstrated association with poor prognostic parameters such as frequent mitoses, high Ki-67 status, positive lymphovascular invasion (LVI), and advanced tumor stage. A highly significant direct correlation was found between each immunohistochemical marker and the other two markers. Shorter overall survival was linked to multifocal tumors (P=0.017), advanced tumor stage (T3) (P=0.010), Luminal B subtype (P=0.015), progressive disease (P=0.003), positive Her2neu status (P=0.008), and metastasis to distant organs (P<0.001). However, RCC2, Rac1, and p53 did not exhibit a significant association with overall survival. Conclusion: The high expression levels of RCC2, Rac1, and p53 in breast IDC suggest their potential role in tumor behavior. The association of RCC2 and Rac1 with poor prognostic parameters may serve as predictive indicators for aggressive tumors, thus implying that targeted therapy could be beneficial in the treatment of breast cancer. [ABSTRACT FROM AUTHOR]

Published

2024

112. Alterations in gene expression and microbiome composition upon calcium-sensing receptor deletion in the mouse esophagus.

Author

Abdulnour-Nakhoul, Solange M., Kolls, Jay K., Flemington, Erik K., Ungerleider, Nathan A., Nakhoul, Hani N., Song, Kejing, and Nakhoul, Nazih L.

Subjects

*CALCIUM-sensing receptors, *GENE expression, *KNOCKOUT mice, *G protein coupled receptors, *TIGHT junctions, *GENE expression profiling, *CELL cycle proteins

Abstract

The calcium-sensing receptor (CaSR), a G protein-coupled receptor, regulates Ca2+ concentration in plasma by regulating parathyroid hormone secretion. In other tissues, it is reported to play roles in cellular differentiation and migration and in secretion and absorption. We reported previously that CaSR can be conditionally deleted in the mouse esophagus. This conditional knockout (KO) (EsoCaSR-/-) model showed a significant reduction in the levels of adherens and tight junction proteins and had a marked buildup of bacteria on the luminal esophageal surface. To further examine the role of CaSR, we used RNA sequencing to determine gene expression profiles in esophageal epithelia of control and EsoCaSR-/- mice RNA Seq data indicated upregulation of gene sets involved in DNA replication and cell cycle in EsoCaSR-/-. This is accompanied by the downregulation of gene sets involved in the innate immune response and protein homeostasis including peptide elongation and protein trafficking. Ingenuity pathway analysis (IPA) demonstrated that these genes are mapped to important biological networks including calcium and Ras homologus A (RhoA) signaling pathways. To further explore the bacterial buildup in EsoCaSR-/- esophageal tissue, 16S sequencing of the mucosal-associated bacterial microbiome was performed. Three bacterial species, g_Rodentibacter, s_Rodentibacter_unclassified, and s_Lactobacillus_hilgardi were significantly increased in EsoCaSR-/-. Furthermore, metagenomic analysis of 16S sequences indicated that pathways related to oxidative phosphorylation and metabolism were downregulated in EsoCaSR-/- tissues. These data demonstrate that CaSR impacts major pathways of cell proliferation, differentiation, cell cycle, and innate immune response in esophageal epithelium. The disruption of these pathways causes inflammation and significant modifications of the microbiome. [ABSTRACT FROM AUTHOR]

Published

2024

113. Premature endocycling of Drosophila follicle cells causes pleiotropic defects in oogenesis.

Author

Herriage, Hunter C and Calvi, Brian R

Subjects

*OVUM physiology, *OVARIAN follicle, *CELL cycle proteins, *RESEARCH funding, *CELL physiology, *DESCRIPTIVE statistics, *CELL cycle, *GENES, *HUMAN reproduction, *ANIMAL experimentation, *INSECTS, *OVARIAN diseases, *GENE amplification, *GRANULOSA cells, *GENOMES, *DISEASE risk factors

Abstract

Endocycling cells grow and repeatedly duplicate their genome without dividing. Cells switch from mitotic cycles to endocycles in response to developmental signals during the growth of specific tissues in a wide range of organisms. The purpose of switching to endocycles, however, remains unclear in many tissues. Additionally, cells can switch to endocycles in response to conditional signals, which can have beneficial or pathological effects on tissues. However, the impact of these unscheduled endocycles on development is underexplored. Here, we use Drosophila ovarian somatic follicle cells as a model to examine the impact of unscheduled endocycles on tissue growth and function. Follicle cells normally switch to endocycles at mid-oogenesis. Inducing follicle cells to prematurely switch to endocycles resulted in the lethality of the resulting embryos. Analysis of ovaries with premature follicle cell endocycles revealed aberrant follicular epithelial structure and pleiotropic defects in oocyte growth, developmental gene amplification, and the migration of a special set of follicle cells known as border cells. Overall, these findings reveal how unscheduled endocycles can disrupt tissue growth and function to cause aberrant development. [ABSTRACT FROM AUTHOR]

Published

2024

114. Effect of CDK4/6 Inhibitors on Tumor Immune Microenvironment.

Author

Liu, Jie, Cheng, Min, Xu, Jiamei, Liang, Yue, Yin, Beibei, and Liang, Jing

Subjects

*CYCLIN-dependent kinase inhibitors, *CELL cycle regulation, *TUMOR microenvironment, *REGULATORY T cells, *NEUROBLASTOMA, *CYCLIN-dependent kinases, *T cell receptors, *CELL cycle proteins

Abstract

Cancer is an abnormal proliferation of cells that is stimulated by cyclin-dependent kinases (CDKs) and defective cell cycle regulation. The essential agent that drive the cell cycle, CDK4/6, would be activated by proliferative signals. Activated CDK4/6 results in the phosphorylation of the neuroblastoma protein (RB) and the release of the transcription factor E2F, which promotes the cell cycle progression. CDK4/6 inhibitor (CDK4/6i) has been currently a research focus, which inhibits the CDK4/6-RB-E2F axis, thereby reducing the cell cycle transition from G1 to S phase and mediating the cell cycle arrest. This action helps achieve an anti-tumor effect. Recent research has demonstrated that CDK4/6i, in addition to contributing to cell cycle arrest, is also essential for the interaction between the tumor cells and the host immune system, i.e., activating the immune system, strengthening the tumor antigen presentation, and reducing the number of regulatory T cells (Treg). Additionally, CDK4/6i would elevate the level of PD-L1, an immunosuppressive factor, in tumor cells, and CDK4/6i in combination with anti-PD-L1 therapy would more effectively reduce the tumor growth. Our results showed that CDK4/6i caused autophagy and senescence in tumor cells. Herein, the impact of CDK4/6i on the immune microenvironment of malignant tumors was mainly focused, as well as their interaction with immune checkpoint inhibitors in affecting anti-tumor immunity. [ABSTRACT FROM AUTHOR]

Published

2024

115. ETS1 regulates NDRG1 to promote the proliferation, migration, and invasion of OSCC.

Author

Sheng, Xun, Li, Xudong, Qian, Yemei, Wang, Shuhui, and Xiao, Chunjie

Subjects

*SQUAMOUS cell carcinoma, *IN vitro studies, *RNA-binding proteins, *CELL cycle proteins, *MOUTH tumors, *CANCER invasiveness, *RESEARCH funding, *CELL proliferation, *APOPTOSIS, *TRANSCRIPTION factors, *CELL motility, *QUANTITATIVE research, *REVERSE transcriptase polymerase chain reaction, *IN vivo studies, *MICE, *IMMUNOHISTOCHEMISTRY, *GENE expression, *ANIMAL experimentation, *PRECIPITIN tests

Abstract

Objective: The aim of this study was to investigate the molecular mechanism by which the transcription factor ETS1 regulates N‐myc downstream regulatory gene 1 (NDRG1) to provide a new theoretical basis for the study of oral squamous cell carcinoma (OSCC). Methods: In this study, eight human OSCC and paraneoplastic samples were collected. The expressions of NDRG1, ETS1, and Ki67 were detected by immunohistochemistry; apoptosis was detected by tdt‐mediated dUTP notched end labeling; cell migration and invasion were detected by Transwell; quantitative real‐time PCR was performed to detect the expression of NDRG1; RNA‐binding protein immunoprecipitation (RIP) assays detected NDRG1 expression; immunofluorescence assays detected ETS1 expression. Results: NDRG1 and ETS1 expression was significantly upregulated in cancer tissues and CAL‐27 and SCC‐6 cells. Knockdown of NDRG1 and ETS1 inhibited cell proliferation, migration, invasion, cloning, and EMT while promoting apoptosis and inhibited tumor development; ETS1 positively regulated NDRG1 expression; Finally, overexpression of NDRG1 in vivo and in vitro reversed the effect of ETS1 knockdown on CAL‐27 and SCC‐6 cells. Conclusions: ETS1 positively regulates the expression of NDRG1 and promotes OSCC. Therefore, ETS1 may serve as a new target for the clinical diagnosis and treatment of OSCC. [ABSTRACT FROM AUTHOR]

Published

2024

116. CIP/KIP and INK4 families as hostages of oncogenic signaling.

Author

Csergeová, Lucia, Krbušek, David, and Janoštiak, Radoslav

Subjects

*CELL cycle proteins, *CYCLIN-dependent kinase inhibitors, *TUMOR suppressor genes, *POST-translational modification, *CANONICAL correlation (Statistics), *MOLECULAR oncology

Abstract

CIP/KIP and INK4 families of Cyclin-dependent kinase inhibitors (CKIs) are well-established cell cycle regulatory proteins whose canonical function is binding to Cyclin-CDK complexes and altering their function. Initial experiments showed that these proteins negatively regulate cell cycle progression and thus are tumor suppressors in the context of molecular oncology. However, expanded research into the functions of these proteins showed that most of them have non-canonical functions, both cell cycle-dependent and independent, and can even act as tumor enhancers depending on their posttranslational modifications, subcellular localization, and cell state context. This review aims to provide an overview of canonical as well as non-canonical functions of CIP/KIP and INK4 families of CKIs, discuss the potential avenues to promote their tumor suppressor functions instead of tumor enhancing ones, and how they could be utilized to design improved treatment regimens for cancer patients. [ABSTRACT FROM AUTHOR]

Published

2024

117. BRCA1 deficiency enhances the aggressiveness of breast cancer cells expressing HPV16 oncoproteins.

Author

Sangthong, Jariya, Thuwajit, Chanitra, Jensen, Laran T., Komyod, Waraporn, Yuvaniyama, Jirundon, and Ponglikitmongkol, Mathurose

Subjects

*BREAST, *BRCA genes, *BREAST cancer, *CELL cycle proteins, *CANCER cells, *GENE expression

Abstract

Background Information: The precise etiology of breast cancer is not completely understood, although women with BRCA1 gene mutations have a significantly increased risk of developing the disease. In addition, sporadic breast cancer is frequently associated with decreased BRCA1 gene expression. Growing evidence of Human papillomaviruses (HPVs) infections in breast tumors has raised the possibility of the involvement of HPVs in the pathogenesis of breast cancer. We investigated whether the effects of HPV oncoproteins E6 and E7 were influenced by the expression levels of BRCA1. HPV16E6E7 (prototype or E6D25E/E7N29S Asian variant type) were stably expressed in MDA‐MB231 breast cancer cells, wild type for BRCA1, or with BRCA1 knocked down. Results: Expression of HPV16E6E7 oncogenes did not affect BRCA1 levels and the abundance of HPV16E6E7 was not altered by BRCA1 knockdown. BRCA1 levels did not alter HPV16E6E7‐dependent degradation of G1‐S cell cycle proteins p53 and pRb. However, we found that the expression of G2‐M cell cycle protein cyclin B1 enhanced by HPV16E6E7 was impacted by BRCA1 levels. Especially, we found the correlation between BRCA1 and cyclin B1 expression and this was also confirmed in breast cancer samples from a Thai cohort. We further demonstrated that the combination of HPV oncoproteins and low levels of BRCA1 protein appears to enhance proliferation and invasion. Transactivation activities of HPV16E6E7 on genes regulating cell proliferation and invasion (TGF‐β and vimentin) were significantly increased in BRCA1‐deficient cells. Conclusions: Our results indicate that a deficiency of BRCA1 promotes the transactivation activity of HPV16E6E7 leading to increase of cell proliferation and invasion. Significance: HPV infection appears to have the potential to enhance the aggressiveness of breast cancers, especially those deficient in BRCA1. [ABSTRACT FROM AUTHOR]

Published

2024

118. A Natural Small Molecule Mitigates Kidney Fibrosis by Targeting Cdc42‐mediated GSK‐3β/β‐catenin Signaling.

Author

Hu, Xinrong, Gan, Lu, Tang, Ziwen, Lin, Ruoni, Liang, Zhou, Li, Feng, Zhu, Changjian, Han, Xu, Zheng, Ruilin, Shen, Jiani, Yu, Jing, Luo, Ning, Peng, Wenxing, Tan, Jiaqing, Li, Xiaoyan, Fan, Jinjin, Wen, Qiong, Wang, Xin, Li, Jianbo, and Zheng, Xunhua

Subjects

*RENAL fibrosis, *CATENINS, *SMALL molecules, *CHRONIC kidney failure, *KIDNEY diseases, *CELL cycle proteins

Abstract

Kidney fibrosis is a common fate of chronic kidney diseases (CKDs), eventually leading to renal dysfunction. Yet, no effective treatment for this pathological process has been achieved. During the bioassay‐guided chemical investigation of the medicinal plant Wikstroemia chamaedaphne, a daphne diterpenoid, daphnepedunin A (DA), is characterized as a promising anti‐renal fibrotic lead. DA shows significant anti‐kidney fibrosis effects in cultured renal fibroblasts and unilateral ureteral obstructed mice, being more potent than the clinical trial drug pirfenidone. Leveraging the thermal proteome profiling strategy, cell division cycle 42 (Cdc42) is identified as the direct target of DA. Mechanistically, DA targets to reduce Cdc42 activity and down‐regulates its downstream phospho‐protein kinase Cζ(p‐PKCζ)/phospho‐glycogen synthase kinase‐3β (p‐GSK‐3β), thereby promoting β‐catenin Ser33/37/Thr41 phosphorylation and ubiquitin‐dependent proteolysis to block classical pro‐fibrotic β‐catenin signaling. These findings suggest that Cdc42 is a promising therapeutic target for kidney fibrosis, and highlight DA as a potent Cdc42 inhibitor for combating CKDs. [ABSTRACT FROM AUTHOR]

Published

2024

119. A scenario of unhealthy life cycle: The role of circadian rhythms in health.

Author

Chandramouli, Manasa, Basavanna, Vrushabendra, and Ningaiah, Srikantamurthy

Subjects

CELL cycle proteins, CELL proliferation, CELL physiology, TRANSCRIPTION factors, CELL cycle, OXIDATIVE stress, GENE expression, CIRCADIAN rhythms, AGING, DNA repair, MAMMALS, CARCINOGENESIS, HUMAN genome, SIGNAL peptides

Abstract

Circadian rhythms are oscillations in physiology and behavior caused by the circadian regulator. Cryptochromes, Periods, and Bmal1 are circadian clock genes that have been linked to aging and cancer. Human pathologies alter circadian clock gene expression, and transgenic rats with clock gene defects progress to cancer and age prematurely. In the growth of age‐linked pathologies and carcinogenesis, cell proliferation and genome integrity play critical roles. The relationship concerning the cell cycle regulation and circadian clock is discussed in this article. The circadian clock controls the behavior and countenance of many main cell cycle and cell cycle check‐point proteins, and cell cycle‐associated proteins, in turn, control the activity and expression of circadian clock proteins. The circadian clock can be reset by DNA disruption, providing a molecular mechanism for mutual control amid the cell cycle and the clock. This circadian clock‐dependent regulation of cell proliferation, composed with other circadian clock‐dependent physiological functions including metabolism control, genotoxic and oxidative stress response, and DNA repair, unlocks new avenues for studying the processes of aging and carcinogenesis. [ABSTRACT FROM AUTHOR]

Published

2024

120. Collective dynamics of actin and microtubule and its crosstalk mediated by FHDC1.

Author

Chee San Tong, Maohan Su, He Sun, Xiang Le Chua, Ding Xiong, Su Guo, Raj, Ravin, Wen Pei Ong, Nicole, Ann Gie Lee, Yansong Miao, and Min Wu

Subjects

ACTIN, MICROTUBULES, TUBULINS, MAST cells, CELL cycle proteins, CELL migration

Abstract

The coordination between actin and microtubule network is crucial, yet this remains a challenging problem to dissect and our understanding of the underlying mechanisms remains limited. In this study, we used travelling waves in the cell cortex to characterize the collective dynamics of cytoskeletal networks. Our findings show that Cdc42 and F-BAR-dependent actin waves in mast cells are mainly driven by formin-mediated actin polymerization, with the microtubule-binding formin FH2 domain-containing protein 1 (FHDC1) as an early regulator. Knocking down FHDC1 inhibits actin wave formation, and this inhibition require FHDC1's interaction with both microtubule and actin. The phase of microtubule depolymerization coincides with the nucleation of actin waves and microtubule stabilization inhibit actin waves, leading us to propose that microtubule shrinking and the concurrent release of FHDC1 locally regulate actin nucleation. Lastly, we show that FHDC1 is crucial for multiple cellular processes such as cell division and migration. Our data provided molecular insights into the nucleation mechanisms of actin waves and uncover an antagonistic interplay between microtubule and actin polymerization in their collective dynamics. [ABSTRACT FROM AUTHOR]

Published

2024

121. Screening and verification of hub genes in esophageal squamous cell carcinoma by integrated analysis.

Author

Wu, Hongqiang, Zhu, Peiyao, Shu, Peng, and Zhang, Shuguang

Subjects

*GENE expression profiling, *SQUAMOUS cell carcinoma, *GENE expression, *GENES, *DNA replication, *CELL cycle proteins, *BIOINFORMATICS software

Abstract

Esophageal squamous cell carcinoma (ESCC) is one of the most common malignant tumors. However, the mechanisms underlying ESCC tumorigenesis have not been fully elucidated. Thus, we aimed to determine the key genes involved in ESCC tumorigenesis. The following bioinformatics analyses were performed: identification of differentially expressed genes (DEGs); gene ontology and Kyoto Encyclopedia of Genes and Genomes pathway enrichment analysis; integrated analysis of the protein–protein interaction network and Gene Expression Profiling Interactive Analysis database for validation of hub genes. Finally, western blotting and qPCR were used to explore the expression of cell division cycle 6 (CDC6) in ESCC cell lines. Immunohistochemistry analysis of ESCC samples from patients and matched clinical characteristics was used to determine the effects of CDC6. A total of 494 DEGs were identified, and functional enrichment was mainly focused on cell cycle and DNA replication. Biological pathway analysis of the hub genes was closely related to the cell cycle. We found that CDC6 was upregulated in ESCC cell lines and patient tissues and was related to the clinicopathological characteristics of ESCC. In conclusion, this study identified hub genes and crucial biological pathways related to ESCC tumorigenesis and integrated analyses indicated that CDC6 may be a novel diagnostic and therapeutic target for ESCC. [ABSTRACT FROM AUTHOR]

Published

2024

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

Author

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

Subjects

*CELL cycle proteins, *CHROMOSOME segregation, *CELL cycle, *CELL division, *ARABIDOPSIS, PLANNING techniques

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. [ABSTRACT FROM AUTHOR]

Published

2024

123. Long non-coding RNA Loc105611671 promotes the proliferation of ovarian granulosa cells and steroid hormone production upregulation of CDC42.

Author

Jinglei Wang, Hanying Chen, Yongsheng Zhang, Hong Shen, and Xiancun Zeng

Subjects

GRANULOSA cells, LINCRNA, CELL cycle proteins, STEROID hormones, SYNCRIP protein, HORMONE synthesis, ESTROGEN

Abstract

Granulosa cells (GCs) are essential for follicular development, and long noncoding RNAs (LncRNAs) are known to support the maintenance of this process and hormone synthesis in mammals. Nevertheless, the regulatory roles of these lncRNAs within sheep follicular GCs remain largely unexplored. This study delved into the influence of a Loc105611671, on the proliferation and steroid hormone synthesis of sheep ovarian GCs and the associated target genes in vitro. Cell Counting Kit-8 (CCK-8) gain-of-function experiments indicated that overexpression of Loc105611671 significantly boosted GCs proliferation, along with estrogen (E2) and progesterone (P4) levels. Further mechanistic scrutiny revealed that Loc105611671 is primarily localized within the cytoplasm of ovarian granulosa cells and engages in molecular interplay with CDC42. This interaction results in the upregulation of CDC42 protein expression. Moreover, it was discerned that increased CDC42 levels contribute to augmented proliferation of follicular granulosa cells and the secretion of E2 and P4. Experiments involving co-transfection elucidated that the concurrent overexpression of CDC42 and Loc105611671 acted synergistically to potentiate these effects. These findings provide insights into the molecular underpinnings of fecundity in ovine species and may inform future strategies for enhancing reproductive outcomes. [ABSTRACT FROM AUTHOR]

Published

2024

124. Filopodial protrusion driven by density-dependent Ena-TOCA-1 interactions.

Author

Blake, Thomas C. A., Fox, Helen M., Urbančič, Vasja, Ravishankar, Roshan, Wolowczyk, Adam, Allgeyer, Edward S., Mason, Julia, Danuser, Gaudenz, and Gallop, Jennifer L.

Subjects

*RETINAL ganglion cells, *FORMINS, *CELL cycle proteins, *ADAPTOR proteins, *FILOPODIA, *PROTEIN binding

Abstract

Filopodia are narrow actin-rich protrusions with important roles in neuronal development where membrane-binding adaptor proteins, such as I-BAR- and F-BAR-domain-containing proteins, have emerged as upstream regulators that link membrane interactions to actin regulators such as formins and proteins of the Ena/VASP family. Both the adaptors and their binding partners are part of diverse and redundant protein networks that can functionally compensate for each other. To explore the significance of the F-BAR domain-containing neuronal membrane adaptor TOCA-1 (also known as FNBP1L) in filopodia we performed a quantitative analysis of TOCA-1 and filopodial dynamics in Xenopus retinal ganglion cells, where Ena/VASP proteins have a native role in filopodial extension. Increasing the density of TOCA-1 enhances Ena/VASP protein binding in vitro, and an accumulation of TOCA-1, as well as its coincidence with Ena, correlates with filopodial protrusion in vivo. Two-colour single-molecule localisation microscopy of TOCA-1 and Ena supports their nanoscale association. TOCA-1 clusters promote filopodial protrusion and this depends on a functional TOCA-1 SH3 domain and activation of Cdc42, which we perturbed using the small-molecule inhibitor CASIN. We propose that TOCA-1 clusters act independently of membrane curvature to recruit and promote Ena activity for filopodial protrusion. [ABSTRACT FROM AUTHOR]

Published

2024

125. The distinct localization of CDC42 isoforms is responsible for their specific functions during migration.

Author

Ravichandran, Yamini, Hänisch, Jan, Murray, Kerren, Roca, Vanessa, Dingli, Florent, Loew, Damarys, Sabatet, Valentin, Boëda, Batiste, Stradal, Theresia E., and Etienne-Manneville, Sandrine

Subjects

*CELL cycle proteins, *ALTERNATIVE RNA splicing, *CELL membranes, *CELL migration, *CELL physiology, *RNA splicing, *G protein coupled receptors

Abstract

The small G-protein CDC42 is an evolutionary conserved polarity protein and a key regulator of polarized cell functions, including directed cell migration. In vertebrates, alternative splicing gives rise to two CDC42 proteins: the ubiquitously expressed isoform (CDC42u) and the brain isoform (CDC42b), which only differ in their carboxy-terminal sequence, including the CAAX motif essential for their association with membranes. We show that these divergent sequences do not directly affect the range of CDC42's potential binding partners but indirectly influence CDC42-driven signaling by controlling the subcellular localization of the two isoforms. In astrocytes and neural precursors, which naturally express both variants, CDC42u associates with the leading-edge plasma membrane of migrating cells, where it recruits the Par6-PKCζ complex to fulfill its polarity function. In contrast, CDC42b mainly localizes to intracellular membrane compartments, where it regulates N-WASP-mediated endocytosis. Both CDC42 isoforms contribute their specific functions to promote the chemotaxis of neural precursors, demonstrating that their expression pattern is decisive for tissue-specific cell behavior. [ABSTRACT FROM AUTHOR]

Published

2024

126. Chromatin Remodeling-Related PRDM1 Increases Stomach Cancer Proliferation and Is Counteracted by Bromodomain Inhibitor.

Author

Hung, Yu-Hsuan, Wang, Hui-Ching, Pan, Mei-Ren, and Chen, Li-Tzong

Subjects

*STOMACH cancer, *CHROMATIN, *GASTROINTESTINAL cancer, *CELL cycle, *PROGNOSIS, *CELL cycle proteins

Abstract

Gastrointestinal (GI) cancers are some of the main public health threats to the world. Even though surgery, chemotherapy, and targeted therapy are available for their treatments, these approaches provide limited success in reducing mortality, making the identification of additional therapeutic targets mandatory. Chromatin remodeling in cancer has long been studied and related therapeutics are widely used, although less is known about factors with prognostic and therapeutic potential in such areas as gastrointestinal cancers. Through applying systematic bioinformatic analysis, we determined that out of 31 chromatin remodeling factors in six gastrointestinal cancers, only PR/SET domain 1 (PRDM1) showed both expression alteration and prognosis prediction. Analyses on pathways, therapies, and mediators showed that cell cycle, bromodomain inhibitor IBET151, and BET protein BRD4 were, respectively involved in PRDM1-high stomach cancer, while cell line experiments validated that PRDM1 knockdown in human stomach cancer cell line SNU-1 decreased its proliferation, BRD4 expression, and responsiveness to IBET151; accordingly, these results indicate the contribution by PRDM1 in stomach cancer formation and its association with BRD4 modulation as well as BET inhibitor treatment. [ABSTRACT FROM AUTHOR]

Published

2024

127. Cdc42 couples septin recruitment to the axial landmark assembly via Axl2 in budding yeast.

Author

Jung Kang, Pil, Mullner, Rachel, Lian, Kendra, and Hay-Oak Park

Subjects

*CELL cycle proteins, *SACCHAROMYCES cerevisiae, *G proteins, *YEAST, *CELL division, *SEPTINS, *GUANOSINE triphosphate

Abstract

Cell polarization generally occurs along a single axis that is directed by a spatial cue. Cells of the budding yeast Saccharomyces cerevisiae undergo polarized growth and oriented cell division in a spatial pattern by selecting a specific bud site. Haploid a or a cells bud in the axial pattern in response to a transient landmark that includes Bud3, Bud4, Axl1 and Axl2. Septins, a family of filament-forming GTP-binding proteins, are also involved in axial budding and are recruited to an incipient bud site, but the mechanism of recruitment remains unclear. Here, we show that Axl2 interacts with Bud3 and the Cdc42 GTPase in its GTP-bound state. Axl2 also interacts with Cdc10, a septin subunit, promoting efficient recruitment of septins near the cell division site. Furthermore, a cdc42 mutant defective in the axial budding pattern at a semi-permissive temperature had a reduced interaction with Axl2 and compromised septin recruitment in the G1 phase. We thus propose that active Cdc42 brings Axl2 to the Bud3-Bud4 complex and that Axl2 then interacts with Cdc10, linking septin recruitment to the axial landmark. [ABSTRACT FROM AUTHOR]

Published

2024

128. Copper Chaperone Atox1 Protected the Cochlea From Cisplatin by Regulating the Copper Transport Family and Cell Cycle.

Author

Chen, Xubo, Xiang, Weiren, Li, Lihua, and Xu, Kai

Subjects

*CELL cycle, *CELL cycle proteins, *COCHLEA, *CISPLATIN, *COPPER, *MOLECULAR chaperones, *CONTRACTILE proteins

Abstract

Antioxidant 1 copper chaperone (Atox1) may contribute to preventing DDP cochlear damage by regulating copper transport family and cell cycle proteins. A rat model of cochlear damage was developed by placing gelatin sponges treated with DDP in the cochlea. HEI-OC1 cells were treated with 133 μM DDP as a cell model. DDP-induced ototoxicity in rats was confirmed by immunofluorescence (IF) imaging. The damage of DDP to HEI-OC1 cells was assessed by using CCK-8, TUNEL, and flow cytometry. The relationship between Atox1, a member of the copper transport protein family, and the damage to in vivo / vitro models was explored by qRT-PCR, western blot, CCK-8, TUNEL, and flow cytometry. DDP had toxic and other side effects causing cochlear damage and promoted HEI-OC1 cell apoptosis and cell cycle arrest. The over-expression of Atox1 (oe-Atox1) was accomplished by transfecting lentiviral vectors into in vitro / vivo models. We found that oe-Atox1 increased the levels of Atox1, copper transporter 1 (CTR1), and SOD3 in HEI-OC1 cells and decreased the expression levels of ATPase copper transporting α (ATP7A) and ATPase copper transporting β (ATP7B). In addition, the transfection of oe-Atox1 decreased cell apoptosis rate and the number of G2/M stage cells. Similarly, the expression of myosin VI and phalloidin of cochlea cells in vivo decreased. Atox1 ameliorated DDP-induced damage to HEI-OC1 cells or rats' cochlea by regulating the levels of members of the copper transport family. [ABSTRACT FROM AUTHOR]

Published

2024

129. Upregulation of miR-519d-3p Inhibits Viability, Proliferation, and G1/S Cell Cycle Transition of Oral Squamous Cell Carcinoma Cells Through Targeting CCND1.

Author

Zhang, Wenjie and Hong, Wei

Subjects

*SQUAMOUS cell carcinoma, *IN vitro studies, *FLOW cytometry, *PEARSON correlation (Statistics), *MOUTH tumors, *CELL cycle proteins, *MICRORNA, *CELL proliferation, *CHOLECYSTOKININ, *CELL cycle, *REVERSE transcriptase polymerase chain reaction, *WESTERN immunoblotting, *CELL survival

Abstract

Background: MicroRNA (miR)-519d-3p suppresses tumor development, however, its role in oral squamous cell carcinoma (OSCC) has yet to be determined. Materials and Methods: OSCC and adjacent tissues were collected (n = 45 for adjacent; n = 21 for Stage I–II OSCC; n = 24 for Stage III–IV OSCC). The cell viability, proliferation, and cell cycle of OSCC were, respectively, assessed by the Cell Counting Kit-8 (CCK-8), colony formation assay, and flow cytometry. Relative expressions of cell cycle-regulated proteins (Cyclin D1 [CCND1], CDK4, and CDK6) and miR-519d-3p were measured with Western blot and quantitative real-time polymerase chain reaction as needed. Dual-luciferase reporter assay was performed to verify the prediction of TargetScan that miR-519d-3p and CCND1 shared potential binding sites. Correlation analysis between miR-519d-3p and CCND1 was performed with Pearson's correlation test. Results: In OSCC tissues, downregulating miR-519d-3p expression correlated with a higher tumor grade. Upregulating miR-519d-3p expression inhibited OSCC cell viability and proliferation, increased cells in G0/G1 phase and reduced those in S/G2 phase, and downregulated the expressions of cell cycle-related protein (CDK4, CDK6). CCND1 was the target gene of miR-519d-3p, and overexpressed CCND1 reversed the effects of upregulation of miR-519d-3p on suppressing the viability, proliferation, and cell cycle of OSCC cells. Conclusions: miR-519d-3p upregulation suppressed the cell viability, proliferation, and G1/S cell cycle transition of OSCC through targeting CCND1. The current findings provide a possible clinical option for OSCC treatment. [ABSTRACT FROM AUTHOR]

Published

2024

130. Genome-Wide Identification and Analysis of APC E3 Ubiquitin Ligase Genes Family in Triticum aestivum.

Author

Wang, Jinnan, Zhang, Tianye, Tu, Aizhu, Xie, Haoxin, Hu, Haichao, Chen, Jianping, and Yang, Jian

Subjects

*UBIQUITIN ligases, *GENE families, *PLANT defenses, *POST-translational modification, *CELL cycle proteins, *PLANT proteins

Abstract

E3 ubiquitin ligases play a pivotal role in ubiquitination, a crucial post-translational modification process. Anaphase-promoting complex (APC), a large cullin-RING E3 ubiquitin ligase, regulates the unidirectional progression of the cell cycle by ubiquitinating specific target proteins and triggering plant immune responses. Several E3 ubiquitin ligases have been identified owing to advancements in sequencing and annotation of the wheat genome. However, the types and functions of APC E3 ubiquitin ligases in wheat have not been reported. This study identified 14 members of the APC gene family in the wheat genome and divided them into three subgroups (CCS52B, CCS52A, and CDC20) to better understand their functions. Promoter sequence analysis revealed the presence of several cis-acting elements related to hormone and stress responses in the APC E3 ubiquitin ligases in wheat. All identified APC E3 ubiquitin ligase family members were highly expressed in the leaves, and the expression of most genes was induced by the application of methyl jasmonate (MeJA). In addition, the APC gene family in wheat may play a role in plant defense mechanisms. This study comprehensively analyzes APC genes in wheat, laying the groundwork for future research on the function of APC genes in response to viral infections and expanding our understanding of wheat immunity mechanisms. [ABSTRACT FROM AUTHOR]

Published

2024

131. Newcastle disease virus activates diverse signaling pathways via Src to facilitate virus entry into host macrophages.

Author

Qiankai Shi, Ran Zhao, Linna Chen, Tianyi Liu, Tao Di, Chunwei Zhang, Zhiying Zhang, Fangfang Wang, Zongxi Han, Junfeng Sun, and Shengwang Liu

Subjects

*NEWCASTLE disease virus, *CELLULAR signal transduction, *RHO GTPases, *CELL cycle proteins, *PROTEIN-tyrosine kinases, *MYOSIN, *CYTOSKELETAL proteins, *COATED vesicles

Abstract

As an intrinsic cellular mechanism responsible for the internalization of extracellular ligands and membrane components, caveolae-mediated endocytosis (CavME) is also exploited by certain pathogens for endocytic entry [e.g., Newcastle disease virus (NDV) of paramyxovirus]. However, the molecular mechanisms of NDVinduced CavME remain poorly understood. Herein, we demonstrate that sialic acid-containing gangliosides, rather than glycoproteins, were utilized by NDV as receptors to initiate the endocytic entry of NDV into HD11 cells. The binding of NDV to gangliosides induced the activation of a non-receptor tyrosine kinase, Src, leading to the phosphorylation of caveolin-1 (Cav1) and dynamin-2 (Dyn2), which contributed to the endocytic entry of NDV. Moreover, an inoculation of cells with NDV-induced actin cytoskeletal rearrangement through Src to facilitate NDV entry via endocytosis and direct fusion with the plasma membrane. Subsequently, unique members of the Rho GTPases family, RhoA and Cdc42, were activated by NDV in a Src-dependent manner. Further analyses revealed that RhoA and Cdc42 regulated the activities of specific effectors, cofilin and myosin regulatory light chain 2, responsible for actin cytoskeleton rearrangement, through diverse intracellular signaling cascades. Taken together, our results suggest that an inoculation of NDV-induced Src-mediated cellular activation by binding to ganglioside receptors. This process orchestrated NDV endocytic entry by modulating the activities of caveolae-associated Cav1 and Dyn2, as well as specific Rho GTPases and downstream effectors. [ABSTRACT FROM AUTHOR]

Published

2024

132. SETDB2 interacts with BUBR1 to induce accurate chromosome segregation independently of its histone methyltransferase activity.

Author

Tu, Yanhong, Zhang, Haomiao, Xia, Jialin, Zhao, Yu, Yang, Ruifang, Feng, Jing, Ma, Xueyun, and Li, Jing

Subjects

CHROMOSOME segregation, METHYLTRANSFERASES, CENTROMERE, CELL cycle proteins, MITOSIS, CYCLINS

Abstract

SETDB2 is a H3K9 histone methyltransferase required for accurate chromosome segregation. Its H3K9 histone methyltransferase activity was reported to be associated with chromosomes during metaphase. Here, we confirm that SETDB2 is required for mitosis and accurate chromosome segregation. However, these functions are independent of its histone methyltransferase activity. Further analysis showed that SETDB2 can interact with BUBR1, and is required for CDC20 binding to BUBR1 and APC/C complex and CYCLIN B1 degradation. The ability of SETDB2 to regulate the binding of CDC20 to BUBR1 or APC/C complex, and stabilization of CYCLIN B1 are also independent of its histone methyltransferase activity. These results suggest that SETDB2 interacts with BUBR1 to promote binding of CDC20 to BUBR1 and APC3, then degrades CYCLIN B1 to ensure accurate chromosome segregation and mitosis, independently of its histone methyltransferase activity. [ABSTRACT FROM AUTHOR]

Published

2024

133. Validation of CDC45 as a novel biomarker for diagnosis and prognosis of gastric cancer.

Author

Lihua Wu, Gan Gao, Hui Mi, Zhou Luo, Zheng Wang, Yongdong Liu, Liangyan Wu, Haihua Long, and Yongqi Shen

Subjects

G protein coupled receptors, CELL cycle proteins, STOMACH cancer, BIOMARKERS, RECEIVER operating characteristic curves, CANCER prognosis

Abstract

Background: Cell division cycle protein 45 (CDC45) has been demonstrated to play vital roles in the progression of various malignancies. However, the clinical significance of CDC45 in gastric cancer (GC) remains unreported. Method: In this study, we employed the TCGA database and the TCGA & GTEx dataset to compare the mRNA expression levels of CDC45 between gastric cancer tissues and adjacent or normal tissues (p < 0.05 was considered statistically significant), which was further validated in multiple datasets including GSE13911, GSE29272, GSE118916, GSE66229, as well as RT-qPCR. Furthermore, we harnessed the Human Protein Atlas (HPA) to evaluate the protein expression of CDC45, which was subsequently verified through immunohistochemistry (IHC). To ascertain the diagnostic utility of CDC45, receiver operating characteristic (ROC) curves and the area under the ROC curve (AUC) were calculated in TCGA database, and further validated it in TCGA & GTEx and GSE66229 datasets. The Kaplan-Meier method was used to reveal the prognostic importance of CDC45 in The Cancer Genome Atlas (TCGA) database and authenticated through the GSE66229, GSE84433, and GSE84437 datasets. Through cBioPortal, we identified co-expressed genes of CDC45, and pursued enrichment analysis. Additionally, we availed gene set enrichment analysis (GSEA) to annotate the biological functions of CDC45. Results: Differential expression analysis revealed that CDC45 was significantly upregulated at both the mRNA and protein levels in GC (all p < 0.05). Remarkably, CDC45 emerged as a promising prognostic indicator and a novel diagnostic biomarker for GC. In a comprehensive the drug susceptibility analysis, we found that patients with high expression of CDC45 had high sensitivity to various chemotherapeutic agents, among which 5-fluorouracil, docetaxel, cisplatin, and elesclomol were most evident. Furthermore, our findings suggested a plausible association between CDC45 and immune cell infiltration. Enrichment analysis revealed that CDC45 and its associated genes may play crucial roles in muscle biofunction, whereas GSEA demonstrated significant enrichment of gene sets pertaining to G protein-coupled receptor ligand binding and G alpha (i) signaling events. Conclusion: Our study elucidates that upregulation of CDC45 is intricately associated with immune cell infiltration and holds promising potential as a favorable prognostic marker and a novel diagnostic biomarker for GC. [ABSTRACT FROM AUTHOR]

Published

2024

134. UHRF2 accumulates in early G1-phase after serum stimulation or mitotic exit to extend G1 and total cell cycle length.

Author

Wang, Xiaohong, Lu, Huarui, Sprangers, Grace, and Hallstrom, Timothy C.

Subjects

CELL cycle, CELL cycle regulation, GENE expression, PROTEIN stability, DNA replication, SERUM, CYCLIN-dependent kinases, CELL cycle proteins

Abstract

Ubiquitin like with PHD and ring finger domains 2 (UHRF2) regulates the cell cycle and epigenetics as a multi-domain protein sharing homology with UHRF1. UHRF1 functions with DNMT1 to coordinate daughter strand methylation during DNA replication, but UHRF2 can't perform this function, and its roles during cell cycle progression are not well defined. UHRF2 role as an oncogene vs. tumor suppressor differs in distinct cell types. UHRF2 interacts with E2F1 to control Cyclin E1 (CCNE1) transcription. UHRF2 also functions in a reciprocal loop with Cyclin E/CDK2 during G1, first as a direct target of CDK2 phosphorylation, but also as an E3-ligase with direct activity toward both Cyclin E and Cyclin D. In this study, we demonstrate that UHRF2 is expressed in early G1 following either serum stimulation out of quiescence or in cells transiting directly out of M-phase, where UHRF2 protein is lost. Further, UHRF2 depletion in G2/M is reversed with a CDK1 specific inhibitor. UHRF2 controls expression levels of cyclins and CDK inhibitors and controls its own transcription in a negative-feedback loop. Deletion of UHRF2 using CRISPR/Cas9 caused a delay in passage through each cell cycle phase. UHRF2 loss culminated in elevated levels of cyclins but also the CDK inhibitor p27KIP1, which regulates G1 passage, to reduce retinoblastoma phosphorylation and increase the amount of time required to reach G1/S passage. Our data indicate that UHRF2 is a central regulator of cell-cycle pacing through its complex regulation of cell cycle gene expression and protein stability. [ABSTRACT FROM AUTHOR]

Published

2024

135. The Nse5/6-like SIMC1-SLF2 complex localizes SMC5/6 to viral replication centers.

Author

Oravcová, Martina, Nie, Minghua, Zilio, Nicola, Maeda, Shintaro, Jami-Alahmadi, Yasaman, Lazzerini-Denchi, Eros, Wohlschlegel, James, Ulrich, Helle, Otomo, Takanori, and Boddy, Michael

Subjects

C5orf25, Nse5, SIMC1, SMC5/6, cell biology, human, molecular biophysics, nsmce5, polyomavirus, structural biology, Humans, Cell Cycle Proteins, Chromosomal Proteins, Non-Histone, Proteomics, Viral Replication Compartments

Abstract

The human SMC5/6 complex is a conserved guardian of genome stability and an emerging component of antiviral responses. These disparate functions likely require distinct mechanisms of SMC5/6 regulation. In yeast, Smc5/6 is regulated by its Nse5/6 subunits, but such regulatory subunits for human SMC5/6 are poorly defined. Here, we identify a novel SMC5/6 subunit called SIMC1 that contains SUMO interacting motifs (SIMs) and an Nse5-like domain. We isolated SIMC1 from the proteomic environment of SMC5/6 within polyomavirus large T antigen (LT)-induced subnuclear compartments. SIMC1 uses its SIMs and Nse5-like domain to localize SMC5/6 to polyomavirus replication centers (PyVRCs) at SUMO-rich PML nuclear bodies. SIMC1s Nse5-like domain binds to the putative Nse6 orthologue SLF2 to form an anti-parallel helical dimer resembling the yeast Nse5/6 structure. SIMC1-SLF2 structure-based mutagenesis defines a conserved surface region containing the N-terminus of SIMC1s helical domain that regulates SMC5/6 localization to PyVRCs. Furthermore, SLF1, which recruits SMC5/6 to DNA lesions via its BRCT and ARD motifs, binds SLF2 analogously to SIMC1 and forms a separate Nse5/6-like complex. Thus, two Nse5/6-like complexes with distinct recruitment domains control human SMC5/6 localization.

Published

2022

136. 1,4-Dihydropyridinebutyrolactone-derived ring-opened ester and amide analogs targeting BET bromodomains.

Author

Jiang, Jiewei, Zhao, Pei-Liang, Sigua, Logan, Chan, Alice, Schönbrunn, Ernst, Qi, Jun, and Georg, Gunda

Subjects

AlphaScreen, BET selectivity, BROMOscan, X-ray, bromodomain and extra-terminal (BET) proteins, Humans, Male, Amides, Cell Cycle Proteins, Esters, Nuclear Proteins, Structure-Activity Relationship, Transcription Factors, Lactones

Abstract

Based on a previously reported 1,4-dihydropyridinebutyrolactone virtual screening hit, nine lactone ring-opened ester and seven amide analogs were prepared. The analogs were designed to provide interactions with residues at the entrance of the ZA loop of the testis-specific bromodomain (ZA) channel to enhance the affinity and selectivity for the bromodomain and extra-terminal (BET) subfamily of bromodomains. Compound testing by AlphaScreen showed that neither the affinity nor the selectivity of the ester and lactam analogs was improved for BRD4-1 and the first bromodomain of the testis-specific bromodomain (BRDT-1). The esters retained affinity comparable to the parent compound, whereas the affinity for the amide analogs was reduced 10-fold. A representative benzyl ester analog was found to retain high selectivity for BET bromodomains as shown by a BROMOscan. X-ray analysis of the allyl ester analog in complex with BRD4-1 and BRDT-1 revealed that the ester side chain is located next to the ZA loop and solvent exposed.

Published

2022

137. Genetic and immunohistochemical profiling of small cell and large cell neuroendocrine carcinomas of the breast.

Author

Bean, Gregory R, Najjar, Saleh, Shin, Sandra J, Hosfield, Elizabeth M, Caswell-Jin, Jennifer L, Urisman, Anatoly, Jones, Kirk D, Chen, Yunn-Yi, and Krings, Gregor

Subjects

Humans, Neuroendocrine Tumors, Carcinoma, Neuroendocrine, Carcinoma, Intraductal, Noninfiltrating, Carcinoma, Large Cell, Breast Neoplasms, Carrier Proteins, Cell Cycle Proteins, Proto-Oncogene Proteins, Female, Tumor Suppressor Protein p53, Class I Phosphatidylinositol 3-Kinases, Clinical Trials and Supportive Activities, Cancer, Clinical Research, Breast Cancer, Medical and Health Sciences, Pathology

Abstract

Neuroendocrine carcinomas (NEC) of the breast are exceedingly rare tumors, which are classified in the WHO system as small cell (SCNEC) and large cell (LCNEC) carcinoma based on indistinguishable features from their lung counterparts. In contrast to lung and enteropancreatic NEC, the genomics of breast NEC have not been well-characterized. In this study, we examined the clinicopathologic, immunohistochemical, and genetic features of 13 breast NEC (7 SCNEC, 4 LCNEC, 2 NEC with ambiguous small versus large cell morphology [ANEC]). Co-alterations of TP53 and RB1 were identified in 86% (6/7) SCNEC, 100% (2/2) ANEC, and 50% (2/4) LCNEC. The one SCNEC without TP53/RB1 alteration had other p53 pathway aberrations (MDM2 and MDM4 amplification) and was immunohistochemically RB negative. PIK3CA/PTEN pathway alterations and ZNF703 amplifications were each identified in 46% (6/13) NEC. Two tumors (1 SCNEC, 1 LCNEC) were CDH1 mutated. By immunohistochemistry, 100% SCNEC (6/6) and ANEC (2/2) and 50% (2/4) LCNEC (83% NEC) showed RB loss, compared to 0% (0/8) grade 3 neuroendocrine tumors (NET) (p

Published

2022

138. Zika virus alters centrosome organization to suppress the innate immune response

Author

Kodani, Andrew, Knopp, Kristeene A, Di Lullo, Elizabeth, Retallack, Hanna, Kriegstein, Arnold R, DeRisi, Joseph L, and Reiter, Jeremy F

Subjects

Biochemistry and Cell Biology, Biological Sciences, Infectious Diseases, 2.1 Biological and endogenous factors, Aetiology, Good Health and Well Being, Animals, Cell Cycle Proteins, Centrosome, Humans, Immunity, Innate, Microcephaly, Zika Virus, Zika Virus Infection, centrosome, innate immunity, microcephaly, Zika virus, Developmental Biology, Biochemistry and cell biology

Abstract

Zika virus (ZIKV) is a flavivirus transmitted via mosquitoes and sex to cause congenital neurodevelopmental defects, including microcephaly. Inherited forms of microcephaly (MCPH) are associated with disrupted centrosome organization. Similarly, we found that ZIKV infection disrupted centrosome organization. ZIKV infection disrupted the organization of centrosomal proteins including CEP63, a MCPH-associated protein. The ZIKV nonstructural protein NS3 bound CEP63, and expression of NS3 was sufficient to alter centrosome architecture and CEP63 localization. Loss of CEP63 suppressed ZIKV-induced centrosome disorganization, indicating that ZIKV requires CEP63 to disrupt centrosome organization. ZIKV infection or CEP63 loss decreased the centrosomal localization and stability of TANK-binding kinase 1 (TBK1), a regulator of the innate immune response. ZIKV infection also increased the centrosomal accumulation of the CEP63 interactor DTX4, a ubiquitin ligase that degrades TBK1. Therefore, we propose that ZIKV disrupts CEP63 function to increase centrosomal DTX4 localization and destabilization of TBK1, thereby tempering the innate immune response.

Published

2022

139. Cyclin-dependent kinase-mediated phosphorylation and the negative regulatory domain of transcription factor B-Myb modulate its DNA binding

Author

Wijeratne, Tilini U, Guiley, Keelan Z, Lee, Hsiau-Wei, Müller, Gerd A, and Rubin, Seth M

Subjects

Genetics, 1.1 Normal biological development and functioning, Underpinning research, Generic health relevance, Cell Cycle Proteins, Cyclin A, Cyclin-Dependent Kinase 2, DNA, Humans, Phosphorylation, Protein Domains, Trans-Activators, Transcriptional Activation, CHR genes, Cdk, autoregulation, cell cycle, gene regulation, intrinsically disordered protein, Chemical Sciences, Biological Sciences, Medical and Health Sciences, Biochemistry & Molecular Biology

Abstract

B-Myb is a highly conserved member of the vertebrate Myb family of transcription factors that plays a critical role in cell-cycle progression and proliferation. Myb proteins activate Myb-dependent promoters by interacting specifically with Myb-binding site (MBS) sequences using their DNA-binding domain (DBD). Transactivation of MBS promoters by B-Myb is repressed by its negative regulatory domain (NRD), and phosphorylation of the NRD by Cdk2-CyclinA relieves the repression to activate B-Myb-dependent promoters. However, the structural mechanisms underlying autoinhibition and activation of B-Myb-mediated transcription have been poorly characterized. Here, we determined that a region in the B-Myb NRD (residues 510-600) directly associates with the DBD and inhibits binding of the DBD to the MBS DNA sequence. We demonstrate using biophysical assays that phosphorylation of the NRD at T515, T518, and T520 is sufficient to disrupt the interaction between the NRD and the DBD, which results in increased affinity for MBS DNA and increased B-Myb-dependent promoter activation in cell assays. Our biochemical characterization of B-Myb autoregulation and the activating effects of phosphorylation provide insight into how B-Myb functions as a site-specific transcription factor.

Published

2022

140. Understanding Cellular, Molecular, and Functional Specificity, Heterogeneity, and Diversity of the Endocannabinoid System.

Author

Aoki, Jun and Isokawa, Masako

Subjects

*CANNABINOID receptors, *CELL cycle proteins, *FATTY acid synthases, *FATTY acid-binding proteins, *LIFE sciences, *B cell receptors

Abstract

The article discusses the endocannabinoid system (ECS), which is involved in various aspects of health and disease. It reviews recent research on the pharmacology of the ECS, its role in development and synaptic function, and its signaling in pathological conditions. The article also highlights the cellular, molecular, and functional specificity, heterogeneity, and diversity of (endo)cannabinoid action. It provides examples of how data mining strategies and data profiling can help identify critical molecules in the ECS. The article concludes by discussing methodological tools for data generation and analysis, such as single-cell RNA sequencing and dimensionality reduction techniques. It encourages further applications of these techniques in the study of the ECS. [Extracted from the article]

Published

2024

141. In vitro reconstitution of calcium-dependent recruitment of the human ESCRT machinery in lysosomal membrane repair

Author

Shukla, Sankalp, Larsen, Kevin P, Ou, Chenxi, Rose, Kevin, and Hurley, James H

Subjects

Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Biological Sciences, Rare Diseases, 1.1 Normal biological development and functioning, Underpinning research, Generic health relevance, ATPases Associated with Diverse Cellular Activities, Apoptosis Regulatory Proteins, Biological Transport, Calcium, Calcium-Binding Proteins, Cell Cycle Proteins, Endosomal Sorting Complexes Required for Transport, Humans, In Vitro Techniques, Intracellular Membranes, Lysosomes, membrane biology, membrane remodeling, membrane repair, in vitro reconstitution, neurodegeneration, in vitro reconstitution

Abstract

The endosomal sorting complex required for transport (ESCRT) machinery is centrally involved in the repair of damage to both the plasma and lysosome membranes. ESCRT recruitment to sites of damage occurs on a fast time scale, and Ca2+ has been proposed to play a key signaling role in the process. Here, we show that the Ca2+-binding regulatory protein ALG-2 binds directly to negatively charged membranes in a Ca2+-dependent manner. Next, by monitoring the colocalization of ALIX with ALG-2 on negatively charged membranes, we show that ALG-2 recruits ALIX to the membrane. Furthermore, we show that ALIX recruitment to the membrane orchestrates the downstream assembly of late-acting CHMP4B, CHMP3, and CHMP2A subunits along with the AAA+ ATPase VPS4B. Finally, we show that ALG-2 can also recruit the ESCRT-III machinery to the membrane via the canonical ESCRT-I/II pathway. Our reconstitution experiments delineate the minimal sets of components needed to assemble the entire membrane repair machinery and open an avenue for the mechanistic understanding of endolysosomal membrane repair.

Published

2022

142. Pathogenic variants of Valosin-containing protein induce lysosomal damage and transcriptional activation of autophagy regulators in neuronal cells.

Author

Ferrari, Veronica, Cristofani, Riccardo, Cicardi, Maria, Tedesco, Barbara, Crippa, Valeria, Chierichetti, Marta, Casarotto, Elena, Cozzi, Marta, Mina, Francesco, Galbiati, Mariarita, Piccolella, Margherita, Carra, Serena, Vaccari, Thomas, Nalbandian, Angele, Fortuna, Tyler, Pandey, Udai, Gagliani, Maria, Cortese, Katia, Rusmini, Paola, Poletti, Angelo, and Kimonis, Virginia

Subjects

ALS, PQC, TFE3, lysosome, neurodegeneration, p97, Adenosine Triphosphatases, Animals, Autophagy, Cell Cycle Proteins, Lysosomes, Motor Neurons, Transcriptional Activation, Valosin Containing Protein

Abstract

AIM: Mutations in the valosin-containing protein (VCP) gene cause various lethal proteinopathies that mainly include inclusion body myopathy with Pagets disease of bone and frontotemporal dementia (IBMPFD) and amyotrophic lateral sclerosis (ALS). Different pathological mechanisms have been proposed. Here, we define the impact of VCP mutants on lysosomes and how cellular homeostasis is restored by inducing autophagy in the presence of lysosomal damage. METHODS: By electron microscopy, we studied lysosomal morphology in VCP animal and motoneuronal models. With the use of western blotting, real-time quantitative polymerase chain reaction (RT-qPCR), immunofluorescence and filter trap assay, we evaluated the effect of selected VCP mutants in neuronal cells on lysosome size and activity, lysosomal membrane permeabilization and their impact on autophagy. RESULTS: We found that VCP mutants induce the formation of aberrant multilamellar organelles in VCP animal and cell models similar to those found in patients with VCP mutations or with lysosomal storage disorders. In neuronal cells, we found altered lysosomal activity characterised by membrane permeabilization with galectin-3 redistribution and activation of PPP3CB. This selectively activated the autophagy/lysosomal transcriptional regulator TFE3, but not TFEB, and enhanced both SQSTM1/p62 and lipidated MAP1LC3B levels inducing autophagy. Moreover, we found that wild type VCP, but not the mutants, counteracted lysosomal damage induced either by trehalose or by a mutant form of SOD1 (G93A), also blocking the formation of its insoluble intracellular aggregates. Thus, chronic activation of autophagy might fuel the formation of multilamellar bodies. CONCLUSION: Together, our findings provide insights into the pathogenesis of VCP-related diseases, by proposing a novel mechanism of multilamellar body formation induced by VCP mutants that involves lysosomal damage and induction of lysophagy.

Published

2022

143. Adaptor-Specific Antibody Fragment Inhibitors for the Intracellular Modulation of p97 (VCP) Protein–Protein Interactions

Author

Jiang, Ziwen, Kuo, Yu-Hsuan, Zhong, Mengqi, Zhang, Jianchao, Zhou, Xin X, Xing, Lijuan, Wells, James A, Wang, Yanzhuang, and Arkin, Michelle R

Subjects

Engineering, Chemical Sciences, 2.1 Biological and endogenous factors, Aetiology, Generic health relevance, Adaptor Proteins, Signal Transducing, Adenosine Triphosphatases, Cell Cycle Proteins, Immunoglobulin Fragments, Protein Binding, Valosin Containing Protein, General Chemistry, Chemical sciences

Abstract

Protein-protein interactions (PPIs) form complex networks to drive cellular signaling and cellular functions. Precise modulation of a target PPI helps explain the role of the PPI in cellular events and possesses therapeutic potential. For example, valosin-containing protein (VCP/p97) is a hub protein that interacts with more than 30 adaptor proteins involved in various cellular functions. However, the role of each p97 PPI during the relevant cellular event is underexplored. The development of small-molecule PPI modulators remains challenging due to a lack of grooves and pockets in the relatively large PPI interface and the fact that a common binding groove in p97 binds to multiple adaptors. Here, we report an antibody fragment-based modulator for the PPI between p97 and its adaptor protein NSFL1C (p47). We engineered these antibody modulators by phage display against the p97-interacting domain of p47 and minimizing binding to other p97 adaptors. The selected antibody fragment modulators specifically disrupt the intracellular p97/p47 interaction. The potential of this antibody platform to develop PPI inhibitors in therapeutic applications was demonstrated through the inhibition of Golgi reassembly, which requires the p97/p47 interaction. This study presents a unique approach to modulate specific intracellular PPIs using engineered antibody fragments, demonstrating a method to dissect the function of a PPI within a convoluted PPI network.

Published

2022

144. PLK4 is upregulated in prostate cancer and its inhibition reduces centrosome amplification and causes senescence.

Author

Singh, Chandra, Denu, Ryan, Nihal, Minakshi, Shabbir, Maria, Garvey, Debra, Huang, Wei, Iczkowski, Kenneth, and Ahmad, Nihal

Subjects

CFI-400945, PLK4, centriole overduplication, centrosome, prostate cancer, Androgens, Cell Cycle Proteins, Centrioles, Centrosome, Humans, Male, Prostatic Neoplasms, Protein Serine-Threonine Kinases

Abstract

BACKGROUND: Identification of novel molecular target(s) is important for designing newer mechanistically driven approaches for the treatment of prostate cancer (PCa), which is one of the main causes of morbidity and mortality in men. In this study, we determined the role of polo-like kinase 4 (PLK4), which regulates centriole duplication and centrosome amplification (CA), in PCa. MATERIALS AND METHODS: Employing human PCa tissue microarrays, we assessed the prevalence of CA, correlated with Gleason score, and estimated major causes of CA in PCa (cell doubling vs. centriole overduplication) by staining for mother/mature centrioles. We also assessed PLK4 expression and correlated it with CA in human PCa tissues and cell lines. Further, we determined the effects of PLK4 inhibition in human PCa cells. RESULTS: Compared to benign prostate, human PCa demonstrated significantly higher CA, which was also positively correlated with the Gleason score. Further, most cases of CA were found to arise by centriole overduplication rather than cell doubling events (e.g., cytokinesis failure) in PCa. In addition, PLK4 was overexpressed in human PCa cell lines and tumors. Moreover, PLK4 inhibitors CFI-400945 and centrinone-B inhibited cell growth, viability, and colony formation of both androgen-responsive and androgen-independent PCa cell lines. PLK4 inhibition also induced cell cycle arrest and senescence in human PCa cells. CONCLUSIONS: CA is prevalent in PCa and arises predominantly by centriole overduplication as opposed to cell doubling events. Loss of centrioles is cellular stress that can promote senescence and suggests that PLK4 inhibition may be a viable therapeutic strategy in PCa.

Published

2022

145. The Astrin-SKAP complex reduces friction at the kinetochore-microtubule interface

Author

Rosas-Salvans, Miquel, Sutanto, Renaldo, Suresh, Pooja, and Dumont, Sophie

Subjects

Biochemistry and Cell Biology, Biological Sciences, 1.1 Normal biological development and functioning, Underpinning research, Generic health relevance, Alcian Blue, Animals, Cell Cycle Proteins, Chromosome Segregation, Friction, Kinetochores, Mammals, Microtubule-Associated Proteins, Microtubules, Mitosis, Phenazines, Phenothiazines, Resorcinols, Spindle Apparatus, Astrin-SKAP, dynamics, force, friction, grip, kinetochore, mammal, mechanics, microtubule, spindle, Medical and Health Sciences, Psychology and Cognitive Sciences, Developmental Biology, Biological sciences, Biomedical and clinical sciences, Psychology

Abstract

The kinetochore links chromosomes to spindle microtubules to drive chromosome segregation at cell division. While we know nearly all mammalian kinetochore proteins, how these give rise to the strong yet dynamic microtubule attachments required for function remains poorly understood. Here, we focus on the Astrin-SKAP complex, which localizes to bioriented kinetochores and is essential for chromosome segregation but whose mechanical role is unclear. Live imaging reveals that SKAP depletion dampens the movement and decreases the coordination of metaphase sister kinetochores and increases the tension between them. Using laser ablation to isolate kinetochores bound to polymerizing versus depolymerizing microtubules, we show that without SKAP, kinetochores move slower on both polymerizing and depolymerizing microtubules and that more force is needed to rescue microtubules to polymerize. Thus, in contrast to the previously described kinetochore proteins that increase the grip on microtubules under force, Astrin-SKAP reduces the grip, increasing attachment dynamics and force responsiveness and reducing friction. Together, our findings suggest a model where the Astrin-SKAP complex effectively "lubricates" correct, bioriented attachments to help preserve them.

Published

2022

146. Severe cardiomyopathy associated with the VCP p.R155C and c.177_187del MYBPC3 gene variants

Author

Choy, Nicole, Wang, Stephani, Abbona, Pablo, Leffler, Dale, and Kimonis, Virginia

Subjects

Biological Sciences, Biomedical and Clinical Sciences, Genetics, Rare Diseases, Cardiovascular, Neurodegenerative, Heart Disease, Aetiology, 2.1 Biological and endogenous factors, Cardiomyopathies, Cell Cycle Proteins, Frontotemporal Dementia, Humans, Mutation, Myositis, Inclusion Body, Osteitis Deformans, Valosin Containing Protein, Hereditary inclusion body myopathy, Paget's disease of bone, Frontotemporal dementia, Cardiomyopathy, Clinical Sciences, Genetics & Heredity, Clinical sciences

Abstract

Inclusion Body Myopathy, Paget's Disease of Bone, with Frontotemporal Dementia is a progressive autosomal dominant disease that affects the ubiquitin-proteasome complex, that is caused by variants in the Valosin Containing Protein (VCP) gene. We report the first case of concurrent pathogenic variants in both MYBPC3 and VCP that led to earlier onset of congestive heart failure with features of dilated cardiomyopathy. Cardiomyopathy has previously been associated with VCP inclusion body myopathy mostly at an advanced stage of the disease. Due to acute onset of cardiomyopathy in a previous asymptomatic individual, a cardiomyopathy gene panel was obtained which revealed an additional c.177_187del variant of the MYBPC3 gene. We report a first case of concurrent pathogenic variants in both c.177_187del gene of MYBPC3 and p.R155C VCP that led to earlier onset and a more severe form of the cardiomyopathy.

Published

2022

147. TopBP1 utilises a bipartite GINS binding mode to support genome replication.

Author

Day, Matthew, Tetik, Bilal, Parlak, Milena, Almeida-Hernández, Yasser, Räschle, Markus, Kaschani, Farnusch, Siegert, Heike, Marko, Anika, Sanchez-Garcia, Elsa, Kaiser, Markus, Barker, Isabel A., Pearl, Laurence H., Oliver, Antony W., and Boos, Dominik

Subjects

XENOPUS eggs, GIN, HEREDITY, CELL cycle proteins, AMINO acids, DNA polymerases, DNA replication

Abstract

Activation of the replicative Mcm2-7 helicase by loading GINS and Cdc45 is crucial for replication origin firing, and as such for faithful genetic inheritance. Our biochemical and structural studies demonstrate that the helicase activator GINS interacts with TopBP1 through two separate binding surfaces, the first involving a stretch of highly conserved amino acids in the TopBP1-GINI region, the second a surface on TopBP1-BRCT4. The two surfaces bind to opposite ends of the A domain of the GINS subunit Psf1. Mutation analysis reveals that either surface is individually able to support TopBP1-GINS interaction, albeit with reduced affinity. Consistently, either surface is sufficient for replication origin firing in Xenopus egg extracts and becomes essential in the absence of the other. The TopBP1-GINS interaction appears sterically incompatible with simultaneous binding of DNA polymerase epsilon (Polε) to GINS when bound to Mcm2-7-Cdc45, although TopBP1-BRCT4 and the Polε subunit PolE2 show only partial competitivity in binding to Psf1. Our TopBP1-GINS model improves the understanding of the recently characterised metazoan pre-loading complex. It further predicts the coordination of three molecular origin firing processes, DNA polymerase epsilon arrival, TopBP1 ejection and GINS integration into Mcm2-7-Cdc45. Effective and regulated activation of the Mcm2-7 helicase underlies faithful genome replication. Here the authors reveal mechanistic detail how the pre-loading complex proteins TopBP1 and GINS interact and, thus, how the helicase activator GINS loads on Mcm2-7 during replication origin firing. [ABSTRACT FROM AUTHOR]

Published

2024

148. Functional analysis of Cdc20 reveals a critical role of CRY box in mitotic checkpoint signaling.

Author

Zhang, Yuqing, Young, Rose, Garvanska, Dimitriya H., Song, Chunlin, Zhai, Yujing, Wang, Ying, Jiang, Hongfei, Fang, Jing, Nilsson, Jakob, Alfieri, Claudio, and Zhang, Gang

Subjects

*CHROMOSOME segregation, *CELL cycle proteins, *FUNCTIONAL analysis, *RNA interference, *SMALL interfering RNA, *CELL lines

Abstract

Accurate mitosis is coordinated by the spindle assembly checkpoint (SAC) through the mitotic checkpoint complex (MCC), which inhibits the anaphase-promoting complex or cyclosome (APC/C). As an essential regulator, Cdc20 promotes mitotic exit through activating APC/C and monitors kinetochore-microtubule attachment through activating SAC. Cdc20 requires multiple interactions with APC/C and MCC subunits to elicit these functions. Functionally assessing these interactions within cells requires efficient depletion of endogenous Cdc20, which is highly difficult to achieve by RNA interference (RNAi). Here we generated Cdc20 RNAi-sensitive cell lines which display a penetrant metaphase arrest by a single RNAi treatment. In this null background, we accurately measured the contribution of each known motif of Cdc20 on APC/C and SAC activation. The CRY box, a previously identified degron, was found critical for SAC by promoting MCC formation and its interaction with APC/C. These data reveal additional regulation within the SAC and establish a novel method to interrogate Cdc20. Functional analysis of Cdc20 motifs in a clean background generated by combining CRISPR/Cas9 and RNAi reveals a critical role of the CRY box in the mitotic checkpoint signaling. [ABSTRACT FROM AUTHOR]

Published

2024

149. New record of reusing brewing by-product for biosynthesis of prodigiosin and its novel anti-pathogen fungi via in vitro tests and molecular docking study.

Author

Nguyen, Thi Hanh, Wang, San-Lang, Phan, Tu Quy, Nguyen, Thi Huyen, Tran, Thi Ha Trang, Doan, Manh Dung, Ngo, Van Anh, Nguyen, Anh Dzung, and Nguyen, Van Bon

Subjects

*PRODIGIOSIN, *MOLECULAR docking, *COLLETOTRICHUM gloeosporioides, *SWEET potatoes, *BIOSYNTHESIS, *BEER brewing, *CELL cycle proteins

Abstract

Prodigiosin (PG)—a molecule with promising applications in many fields—was effectively biosynthesized in this study using a novel and eco-friendly fermentation substrate—i.e., beer brewing by-product (BBB). It was confirmed as a nutrient-rich substrate source of protein (22.18%), ash (10.1%), carbohydrate (1.98%), sugar, and abundant mineral elements. The cultural medium with a newly designed formula on a small flask containing 1.25% BBB/Casein (9/1), 0.025% FeSO4, and 0.125% Na2HPO4 for a notable PG yield achieved 6230 mg/L after 48 h. PG production on a bioreactor system also enhanced yield by 1.16 folds (reaching 7220 mg/L) and shortened fermentation time (only taking 10 h). This pure pigment was isolated and identified by analyzing UV/vis absorption, MALDI-TOF MS, and HPLC. The obtained PG was used for antifungal tests. Notably, in this work, most of PG's pathogen fungal inhibition activity are new findings. Of those, PG showed the most positive effect on Colletotrichum gloeosporioides F05 strain (causing on sweet potato roots) with inhibition rates of mycelial growth and spore germination achieved at 47 and 57%, respectively. In particular, PG also reduced resistance and wholly inhibited mycelium growth germinating from spores. Furthermore, PG showed the good interaction ability with multiple target proteins (CDC42, CYP51, CAS2, Pectate lyase B, and Beta tubulin) inhibiting C. gloeosporioides via docking simulation. The results of this study revealed useful scientific information related to the novel application of BBB in PG production and the new PG's effects in the management of fungal pathogens in crops. [ABSTRACT FROM AUTHOR]

Published

2024

150. TET1 Regulates Proliferation of Mouse Skin-Derived Stem Cells In Vitro.

Author

Qiao, Tian, Li, Li, Zang, Ming-Xin, Jiang, Yi-Nuo, Wang, Sha-Sha, Li, Chun-Xiao, Xie, Xin-Xiang, Zhang, Geng, Zhang, Ying, Ge, Wei, Shen, Wei, and Cheng, Shun-Feng

Subjects

*STEM cells, *MOLECULAR biology, *MULTIPOTENT stem cells, *CELL cycle proteins, *CELL cycle regulation

Abstract

This article, published in Stem Cell Reviews & Reports, explores the role of the TET1 protein in the proliferation of mouse skin-derived stem cells (SDSCs) in vitro. The study found that TET1 is crucial for maintaining the self-renewal and proliferation abilities of SDSCs. Knockdown of TET1 resulted in decreased cell proliferation and altered cell cycle distribution. The study suggests that TET1 regulates SDSC proliferation through the DNA replication pathway. This research provides valuable insights into the mechanisms underlying the maintenance of stem cell characteristics and may have implications for regenerative medicine. [Extracted from the article]

Published

2024