Your search keyword '"PP2A"' showing total 2,638 results

1. A combination of protein phosphatase 2A inhibition and checkpoint immunotherapy: a perfect storm.

Author

Clark, Mary, Lu, Rongze, Ho, Winson, Dias, Matheus, Bernards, René, and Forman, Stephen

Subjects

PP2A, TIL therapy, checkpoint inhibitor, Humans, Protein Phosphatase 2, Immunotherapy, Immune Checkpoint Inhibitors, Neoplasms, Animals

Abstract

Immune checkpoint blockade has emerged as a potent new tool in the war on cancer. However, only a subset of cancer patients benefit from this therapeutic modality, sparking a search for combination therapies to increase the fraction of responding patients. We argue here that inhibition of protein phosphatase 2A (PP2A) is a promising approach to increase responses to immune checkpoint blockade and other therapies that rely on the presence of tumor-reactive T cells. Inhibition of PP2A increases neoantigen expression on tumor cells, activates the cGAS/STING pathway, suppresses regulatory T cells, and increases cytotoxic T cell activation. In preclinical models, inhibition of PP2A synergizes with immune checkpoint blockade and emerging evidence indicates that patients who have tumors with mutations in PP2A respond better to immune checkpoint blockade. Therefore, inhibition of PP2A activity may be an effective way to sensitize cancer cells to immune checkpoint blockade and cell-based therapies using tumor-reactive T cells.

Published

2024

2. Impacts of exposure to and subsequent discontinuation of clozapine on tripartite synaptic transmission.

Author

Okada, Motohiro, Fukuyama, Kouji, and Motomura, Eishi

Subjects

*AMP-activated protein kinases, *FRONTAL lobe, *NEURAL transmission, *CONNEXIN 43, *CLOZAPINE, *HYDROXYTYROSOL

Abstract

Background and Purpose: Clozapine is an effective antipsychotic for treatment‐resistant schizophrenia, but its discontinuation leads to discontinuation syndrome/catatonia complicated by benzodiazepine‐resistance and rhabdomyolysis. Experimental Approach: This study determined time‐dependent effects of exposure and subsequent discontinuation of clozapine on expression of connexin43, 5‐HT receptors, intracellular L‐β‐aminoisobutyrate (L‐BAIBA) and 2nd‐messengers and signalling of AMPK, PP2A and Akt in cultured astrocytes and rat frontal cortex. Key Results: Intracellular L‐BAIBA levels increased during clozapine exposure but immediately recovered after discontinuation. Both exposure to clozapine and L‐BAIBA increased connexin43 and signalling of AMPK/Akt time‐dependently, but reduced PP2A signalling, 5‐HT receptor expression and IP3 level. These changes recovered within 2 weeks after discontinuation, while 5‐HT receptors and IP3 transiently increased during the recovery process. L‐BAIBA activated AMPK signalling, leading to attenuated PP2A signalling. Astroglial D‐serine release was increased by clozapine exposure but continued to increase within 1 week after discontinuation via activation of IP3 receptor function. Conclusion and Implications: Clozapine discontinuation restored PP2A signalling due to decreased L‐BAIBA, increased 5‐HT receptor expression via probably enhanced 5‐HT receptor recycling, but increased astroglial D‐serine release persisted by transiently activated IP3 receptors via transiently increased IP3 level. Decreased L‐BAIBA caused by clozapine discontinuation is, at least partially, involved in the transiently increased 5‐HT receptor and astroglial D‐serine release. [ABSTRACT FROM AUTHOR]

Published

2024

3. Down-regulation of miR-138-5p in PP2A KO mice promoted apoptosis of spermatocytes.

Author

Wang, Danni, Liu, Xing, Chen, Bingyan, Shang, Yuwei, Wan, Ting, Zhang, Shu, Liu, Huijun, Shi, Yichao, Chen, Xia, and Sun, Huiting

Abstract

Background: Protein phosphatase 2 A (PP2A) is known to have a pivotal and diverse functions in various physiological processes. In the previous study, we utilized the cre-loxp system to generate germ cell-specific knockout mice for the PP2A catalytic subunit alpha subunit (Ppp2cacKO). Methods and results: Using high-throughput miRNA sequencing of testis tissues and real‑time PCR, we have identified a notable decrease in the expression of miR-138-5p in the testes of Ppp2cacKO mice. Our findings indicate that miR-138-5p plays a role in the regulation of apoptosis and proliferation of GC2 cells. Furthermore, bioinformatics analyses suggested that miR-138- 5p may target the transcriptional repressor Trps1. Consistent with these predictions, we observed a significant upregulation of Trps1 in the testes of Ppp2cacKO mice. Through transfection experiments, we have validated the negative regulation of Trps1 expression by miR-138-5p in GC2 cells. Conclusion: Our study indicates that the down-regulation of miR-138-5p in PP2A KO mice, which targets Trps1 to promote spermatocyte apoptosis. [ABSTRACT FROM AUTHOR]

Published

2024

4. Development of luminescent probes for real‐time detection of the CDK/PP2A balance during the cell cycle.

Author

Hino, Hirotsugu, Takaki, Kaori, Kobe, Mika, and Mochida, Satoru

Subjects

*LUMINESCENT probes, *XENOPUS eggs, *PHOSPHOPROTEIN phosphatases, *PEPTIDES, *CELL cycle

Abstract

From a biochemical viewpoint, the cell cycle is controlled by the phosphorylation of cyclin‐dependent kinase (CDK) substrates, and the phosphorylation level is determined by the enzymatic balance between CDK and protein phosphatase 2A (PP2A). However, the conventional techniques for analyzing protein phosphorylation using radioisotopes and antibodies involve many operational steps and take days before obtaining results, making them difficult to apply to high‐throughput screening and real‐time observations. In this study, we developed luminescent probes with a light intensity that changes depending on its phosphorylation state. We modified the Nano‐lantern probe (Renilla luciferase‐based Ca2+ probe) by introducing a CDK‐substrate peptide and a phosphopeptide‐binding domain into the luciferase. Our initial trial resulted in new probes that could report the CDK/PP2A balance in a purified system. Further modifications of these probes (replacing the phospho‐Ser with phospho‐Thr and randomly replacing its surrounding amino acids) improved the dynamic range by up to four‐fold, making them practical for use in the Xenopus egg extracts system, where many physiological events can be reproduced. Taken together, our new probes enabled the monitoring of the CDK/PP2A balance in real time, and are applicable to high‐throughput systems; the new probes thus appear promising for use in substrate and drug screening. [ABSTRACT FROM AUTHOR]

Published

2024

5. A disease-associated PPP2R3C-MAP3K1 phospho-regulatory module controls centrosome function.

Author

Ganga, Anil Kumar, Sweeney, Lauren K., Rubio Ramos, Armando, Wrinn, Caitlin M., Bishop, Cassandra S., Hamel, Virginie, Guichard, Paul, and Breslow, David K.

Subjects

*GONADAL dysgenesis, *FUNCTIONAL genomics, *CENTRIOLES, *CARRIER proteins, GONADAL diseases

Abstract

Centrosomes have critical roles in microtubule organization, ciliogenesis, and cell signaling. 1,2,3,4,5,6,7,8 Centrosomal alterations also contribute to diseases, including microcephaly, cancer, and ciliopathies. 9,10,11,12,13 To date, over 150 centrosomal proteins have been identified, including several kinases and phosphatases that control centrosome biogenesis, function, and maintenance. 2,3,4,5,14,15,16,17,18,19,20,21 However, the regulatory mechanisms that govern centrosome function are not fully defined, and thus how defects in centrosomal regulation contribute to disease is incompletely understood. Using a systems genetics approach, we find here that PPP2R3C, a poorly characterized PP2A phosphatase subunit, is a distal centriole protein and functional partner of centriolar proteins CEP350 and FOP. We further show that a key function of PPP2R3C is to counteract the kinase activity of MAP3K1. In support of this model, MAP3K1 knockout suppresses growth defects caused by PPP2R3C inactivation, and MAP3K1 and PPP2R3C have opposing effects on basal and microtubule stress-induced JNK signaling. Illustrating the importance of balanced MAP3K1 and PPP2R3C activities, acute overexpression of MAP3K1 severely inhibits centrosome function and triggers rapid centriole disintegration. Additionally, inactivating PPP2R3C mutations and activating MAP3K1 mutations both cause congenital syndromes characterized by gonadal dysgenesis. 22,23,24,25,26,27,28 As a syndromic PPP2R3C variant is defective in centriolar localization and binding to centriolar protein FOP, we propose that imbalanced activity of this centrosomal kinase-phosphatase pair is the shared cause of these disorders. Thus, our findings reveal a new centrosomal phospho-regulatory module, shed light on disorders of gonadal development, and illustrate the power of systems genetics to identify previously unrecognized gene functions. • PP2A phosphatase subunit PPP2R3C localizes to the distal end of centrioles • PPP2R3C acts with FOP and CEP350 to oppose centrosomal kinase MAP3K1 • Imbalance of PPP2R3C/MAP3K1 activity impairs centrosome function and cell fitness • Impaired phospho-regulation at centrioles may underlie gonadal dysgenesis disorders Ganga et al. show that the PP2A phosphatase subunit PPP2R3C and the kinase MAP3K1 are centriolar proteins that functionally oppose each other. Imbalance of their activities impairs centrosome function and cell fitness and is further revealed as a shared basis of gonadal dysgenesis disorders caused by mutations in MAP3K1 and PPP2R3C. [ABSTRACT FROM AUTHOR]

Published

2024

6. Protein phosphatase 2A regulates blood cell proliferation and differentiation in Drosophila larval lymph glands.

Author

Zhang, Fang, Luo, Wang, Liu, Sumin, Zhao, Long, and Su, Ying

Subjects

*HEMATOPOIETIC system, *DROSOPHILA melanogaster, *HEDGEHOG signaling proteins, *PHOSPHOPROTEIN phosphatases, *CELL differentiation

Abstract

Protein phosphatase 2A (PP2A), one of the most abundant protein phosphatases, has divergent functions in multiple types of cells. Its inactivation has been closely associated with leukemia diseases. However, the physiological function of PP2A for hematopoiesis has been poorly understood in organisms. Drosophila hematopoiesis parallels the vertebrate counterpart in developmental and functional features but involves a much simpler hematopoietic system. Here, utilizing the Drosophila major larval hematopoietic organ lymph gland, we studied the function of PP2A for hematopoiesis in vivo. By knocking down the expression of Pp2A‐29B that encodes the scaffold subunit of the PP2A holoenzyme complex, we found that PP2A silencing in the differentiating hemocytes resulted in their excessive proliferation. Furthermore, this PP2A inhibition downregulated the expression of Smoothened (Smo), a crucial component in the Hedgehog pathway, and smo overexpression was able to rescue the phenotypes of PP2A depletion, indicating that Smo functions as a downstream effector of PP2A to restrict the hemocyte proliferation. PDGF/VEGF‐receptor (Pvr) overexpression also restored the Smo expression and lymph gland morphology of PP2A silencing, suggesting a PP2A‐Pvr‐Smo axis to regulate lymph gland growth and hemocyte proliferation. Moreover, inhibiting PP2A activity in the blood progenitor cells promoted their differentiation, but which was independent with Smo. Together, our data suggested that PP2A plays a dual role in the Drosophila lymph gland by preserving the progenitor population and restraining the hemocyte proliferation, to properly regulate the hematopoietic process. [ABSTRACT FROM AUTHOR]

Published

2024

7. PP2A catalytic subunit alpha is critically required for CD8+ T‐cell homeostasis and antibacterial responses.

Author

Zhou, Xian, Li, Meilu, Ai, Minji, Li, Yanfeng, Zhu, Xingxing, Hansen, Michael J., Zhong, Jun, Johnson, Kenneth L., Zenka, Roman, Pandey, Akhilesh, Pease, Larry R., and Zeng, Hu

Subjects

MUCOUS membranes, PHOSPHOPROTEIN phosphatases, T cells, CD8 antigen, IMMUNE response

Abstract

Although the functions of tyrosine phosphatases in T‐cell biology have been extensively studied, our knowledge on the contribution of serine/threonine phosphatases in T cells remains poor. Protein phosphatase 2A (PP2A) is one of the most abundantly expressed serine/threonine phosphatases. It is important in thymocyte development and CD4+ T‐cell differentiation. Utilizing a genetic model in which its catalytic subunit alpha isoform (PP2A Cα) is deleted in T cells, we investigated its contribution to CD8+ T‐cell homeostasis and effector functions. Our results demonstrate that T‐cell intrinsic PP2A Cα is critically required for CD8+ T‐cell homeostasis in secondary lymphoid organs and intestinal mucosal site. Importantly, PP2A Cα–deficient CD8+ T cells exhibit reduced proliferation and survival. CD8+ T‐cell antibacterial response is strictly dependent on PP2A Cα. Expression of Bcl2 transgene rescues CD8+ T‐cell homeostasis in spleens, but not in intestinal mucosal site, nor does it restore defective antibacterial responses. Finally, proteomics and phosphoproteomics analyses reveal potential targets dependent on PP2A Cα, including mTORC1 and AKT. Thus, PP2A Cα is a key modulator of CD8+ T‐cell homeostasis and effector functions. [ABSTRACT FROM AUTHOR]

Published

2024

8. ETS1 Expression in Diabetic Foot Ulcers: Implications for Fibroblast Phenotype and Wound Healing Through the PP2A/YAP Pathway

Author

Yi W, Bao Q, Xu D, Long C, Fang R, Cheng W, Song J, and Feng H

Subjects

diabetic wound, diabetic foot ulcer, ets1, pp2a, yap., Pathology, RB1-214, Therapeutics. Pharmacology, RM1-950

Abstract

Wenjuan Yi,1 Qionglin Bao,2 Dingkun Xu,3 Chenyu Long,1 Ruixin Fang,1 Wenlin Cheng,4 Jiquan Song,1 Huiting Feng1 1Department of Dermatology, Zhongnan Hospital of Wuhan University, Wuhan, People’s Republic of China; 2Wound Repair Center, Chronic Wound and Diabetic Foot Clinical Medical Research Center, Liyuan Hospital Affiliated to Tongji Medical College, Huazhong University of Science and Technology, Wuhan, People’s Republic of China; 3Hubei Key Laboratory of Cell Homeostasis, College of Life Sciences, TaiKang Center for Life and Medical Sciences, Wuhan University, Wuhan, People’s Republic of China; 4Department of Cardiology, Zhongnan Hospital, Wuhan University, Wuhan, People’s Republic of ChinaCorrespondence: Huiting Feng; Jiquan Song, Email feng_huiting@126.com; songjiq@126.comObjective: Diabetic foot ulcers (DFUs) are a serious complication of diabetes, characterized by impaired wound healing and high morbidity and mortality risks. While ETS1 is known to influence fibroblast pathological remodeling, its specific role in DFU and fibroblast wound healing remains unclear.Methods: Skin tissue samples from DFU patients were categorized by Wagner grades to analyze ETS1 expression. Primary fibroblasts derived from diabetes mellitus wound (DMFBs) were collected from wound margins to test migration ability and analyze cell phenotype by immunofluorescence; they were further treated with siETS1 and the ETS1 inhibitor YK-4-279. Techniques including Western blotting, quantitative Real-Time PCR (qRT-PCR), and immunofluorescence were used to assess the expressionof ETS1, Collagen I, and phenotype in DMFBs. Additionally, the binding sites between human ETS1 and the PP2A promoter were predicted by the UCSC and JASPAR databases. It intended to explore the negative transcriptional regulation of PP2A by ETS1 and its implications in fibroblast function and wound healing.Results: Fibroblasts derived from Wagner Grades II–IV exhibit differences in cell morphology, migratory ability, and phenotype. Our findings indicate a significant upregulation of ETS1 in Wagner III and IV. The downregulation of ETS1 was observed to enhance DMFB migration and increase the expression of Collagen I and α-SMA. These changes suggest a potential mechanism by which PP2A regulates the YAP/Hippo pathway in diabetic wound healing.Conclusion: ETS1 appears to impede the repair processes in DFUs, likely through the negative regulation of PP2A, affecting fibroblast function and wound healing.Keywords: diabetic wound, diabetic foot ulcer, ETS1, PP2A, YAP

Published

2024

9. A combination of protein phosphatase 2A inhibition and checkpoint immunotherapy: a perfect storm

Author

Mary C. Clark, Rongze Olivia Lu, Winson S. Ho, Matheus Henrique Dias, René Bernards, and Stephen J. Forman

Subjects

checkpoint inhibitor, PP2A, TIL therapy, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Immune checkpoint blockade has emerged as a potent new tool in the war on cancer. However, only a subset of cancer patients benefit from this therapeutic modality, sparking a search for combination therapies to increase the fraction of responding patients. We argue here that inhibition of protein phosphatase 2A (PP2A) is a promising approach to increase responses to immune checkpoint blockade and other therapies that rely on the presence of tumor‐reactive T cells. Inhibition of PP2A increases neoantigen expression on tumor cells, activates the cGAS/STING pathway, suppresses regulatory T cells, and increases cytotoxic T cell activation. In preclinical models, inhibition of PP2A synergizes with immune checkpoint blockade and emerging evidence indicates that patients who have tumors with mutations in PP2A respond better to immune checkpoint blockade. Therefore, inhibition of PP2A activity may be an effective way to sensitize cancer cells to immune checkpoint blockade and cell‐based therapies using tumor‐reactive T cells.

Published

2024

10. ATM Kinase Small Molecule Inhibitors Prevent Radiation-Induced Apoptosis of Mouse Neurons In Vivo.

Author

Aydar, Yüksel, Rambukkanage, Sanara S., Brown, Lauryn, Wang, Juan, Seo, Ji Sung, Li, Keming, Cheng, Yong, Biddlestone-Thorpe, Laura, Boyd, Caila, Sule, Amrita, and Valerie, Kristoffer

Subjects

*DNA repair, *CENTRAL nervous system, *KNOCKOUT mice, *SMALL molecules, *NEURONS

Abstract

ATM kinase is becoming an important therapeutic target for tumor radiosensitization. Radiation is known to cause neuro-inflammation and neurodegeneration; however, the effects of small molecule ATM inhibitors (ATMi's) and radiation on normal tissue, including healthy brain, are largely unexplored. Therefore, we examined the mouse CNS after ATMi radiosensitization with a focus on the fate of neurons. We used several approaches to assess the effects on the DNA damage response (DDR) and apoptosis of neurons using immunostaining. In vivo, a significant decrease in viable neurons and increase in degenerating neurons and apoptosis was observed in mice treated with radiation alone. On the other hand, an ATMi alone had little to no effect on neuron viability and did not induce apoptosis. Importantly, the ATMi's did not further increase radiation toxicity. In fact, multiplex immunostaining showed that a clinical candidate ATMi (AZD1390) protected mouse neurons from apoptosis by 90% at 4 h after radiation. We speculate that the lack of toxicity to neurons is due to a normal ATM–p53 response that, if blocked transiently with an ATMi, is protective. Altogether, in line with previous work using ATM knockout mice, we provide evidence that ATM kinase inhibition using small molecules does not add to neuronal radiation toxicity, and might, in fact, protect them from radiation-induced apoptosis at least in the short term. [ABSTRACT FROM AUTHOR]

Published

2024

11. Inducible degradation-coupled phosphoproteomics identifies PP2ARts1 as a novel eisosome regulator.

Author

DeMarco, Andrew G., Dibble, Marcella G., and Hall, Mark C.

Subjects

PHOSPHOPROTEIN phosphatases, POST-translational modification, PROTEOLYSIS, CELL division, BIOCHEMICAL substrates

Abstract

Introduction: Reversible protein phosphorylation is an abundant posttranslational modification dynamically regulated by opposing kinases and phosphatases. Protein phosphorylation has been extensively studied in cell division, where waves of cyclin-dependent kinase activity, peaking in mitosis, drive the sequential stages of the cell cycle. Here we developed and employed a strategy to specifically probe kinase or phosphatase substrates at desired times or experimental conditions in the model organism Saccharomyces cerevisiae. Methods: We combined auxin-inducible degradation (AID) with mass spectrometry-based phosphoproteomics, which allowed us to arrest physiologically normal cultures in mitosis prior to rapid phosphatase degradation and phosphoproteome analysis. Results and discussion: Our results revealed that protein phosphatase 2A coupled with its B56 regulatory subunit, Rts1 (PP2ARts1), is involved in dephosphorylation of numerous proteins in mitosis, highlighting the need for phosphatases to selectively maintain certain proteins in a hypophosphorylated state in the face of high mitotic kinase activity. Unexpectedly, we observed elevated phosphorylation at many sites on several subunits of the fungal eisosome complex following rapid Rts1 degradation. Eisosomes are dynamic polymeric assemblies that create furrows in the plasma membrane important in regulating nutrient import, lipid metabolism, and stress responses, among other things. We found that PP2ARts1-mediated dephosphorylation of eisosomes promotes their plasma membrane association and we provide evidence that this regulation impacts eisosome roles in metabolic homeostasis. The combination of rapid, inducible protein degradation with proteomic profiling offers several advantages over common protein disruption methods for characterizing substrates of regulatory enzymes involved in dynamic biological processes. [ABSTRACT FROM AUTHOR]

Published

2024

12. TIPRL, a Potential Double-edge Molecule to be Targeted and Re-targeted Toward Cancer.

Author

Gao, Jie, You, Tiantian, Liu, Jiao, Yang, Lili, Liu, Yan, and Wang, Yanyan

Abstract

The target of rapamycin (TOR) proteins exhibits phylogenetic conservation across various species, ranging from yeast to humans, and are classified as members of the phosphatidylinositol kinase (PIK)-related kinase family. Multiple serine/threonine (Ser/Thr) protein phosphatases (PP)2A, PP4, and PP6, have been recognized as constituents of the TOR signaling pathway in mammalian cells. The protein known as TOR signaling pathway regulator-like (TIPRL) functions as a regulatory agent by impeding the activity of the catalytic subunits of PP2A. Various cellular contexts have been postulated for TIPRL, encompassing the regulation of mechanistic target of rapamycin (mTOR) signaling, inhibition of apoptosis and biogenesis, and recycling of PP2A. According to reports, there has been an observed increase in TIPRL levels in several types of carcinomas, such as non-small-cell lung carcinoma (NSCLC) and hepatocellular carcinomas (HCC). This review aims to comprehensively examine the significance of the Tor pathway in regulating apoptosis and proliferation of cancer cells, with a specific focus on the role of TOR signaling and TIPRL in cancer. [ABSTRACT FROM AUTHOR]

Published

2024

13. Palmitic Acid Induces Posttranslational Modifications of Tau Protein in Alzheimer's Disease–Related Epitopes and Increases Intraneuronal Tau Levels.

Author

García-Cruz, Valeria Melissa and Arias, Clorinda

Abstract

Metabolic diseases derived from an unhealthy lifestyle have been linked with an increased risk for developing cognitive impairment and even Alzheimer's disease (AD). Although high consumption of saturated fatty acids such as palmitic acid (PA) has been associated with the development of obesity and type II diabetes, the mechanisms connecting elevated neuronal PA levels and increased AD marker expression remain unclear. Among other effects, PA induces insulin resistance, increases intracellular calcium and reactive oxygen species (ROS) production, and reduces the NAD+/NADH ratio, resulting in decreased activity of the deacetylase Sirtuin1 (SIRT1) in neurons. These mechanisms may affect signaling pathways that impact the posttranslational modifications (PTMs) of the tau protein. To analyze the role played by PA in inducing the phosphorylation and acetylation of tau, we examined PTM changes in human tau in differentiated neurons from human neuroblastoma cells. We found changes in the phosphorylation state of several AD-related sites, namely, S199/202 and S214, that were mediated by a mechanism associated with the dysregulated activity of the kinases GSK3β and mTOR. PA also increased the acetylation of residue K280 and elevated total tau level after long exposure time. These findings provide information about the mechanisms by which saturated fatty acids cause tau PTMs that are similar to those observed in association with AD biochemical changes. [ABSTRACT FROM AUTHOR]

Published

2024

14. Further investigations on the influence of protein phosphatases on the signaling of muscarinic receptors in the atria of mouse hearts.

Author

Gergs, Ulrich, Wackerhagen, Silke, Fuhrmann, Tobias, Schäfer, Inka, and Neumann, Joachim

Subjects

PHOSPHOPROTEIN phosphatases, MUSCARINIC receptors, CALCIUM ions, TRANSGENIC mice, ADENYLATE cyclase

Abstract

The vagal regulation of cardiac function involves acetylcholine (ACh) receptor activation followed by negative chronotropic and negative as well as positive inotropic effects. The resulting signaling pathways may include Gi/o protein-coupled reduction in adenylyl cyclase (AC) activity, direct Gi/o protein-coupled activation of ACh-activated potassium current (IKACh), inhibition of L-type calcium ion channels, and/or the activation of protein phosphatases. Here, we studied the role of the protein phosphatases 1 (PP1) and 2A (PP2A) for muscarinic receptor signaling in isolated atrial preparations of transgenic mice with cardiomyocyte-specific overexpression of either the catalytic subunit of PP2A (PP2A-TG) or the inhibitor-2 (I2) of PP1 (I2-TG) or in double transgenic mice overexpressing both PP2A and I2 (DT). In mouse left atrial preparations, carbachol (CCh), cumulatively applied (1 nM–10 µM), exerted at low concentrations a negative inotropic effect followed by a positive inotropic effect at higher concentrations. This biphasic effect was noted with CCh alone as well as when CCh was added after β-adrenergic pre-stimulation with isoprenaline (1 µM). Whereas the response to stimulation of β-adrenoceptors or adenosine receptors (used as controls) was changed in PP2A-TG, the response to CCh was unaffected in atrial preparations from all transgenic models studied here. Therefore, the present data tentatively indicate that neither PP2A nor PP1, but possibly other protein phosphatases, is involved in the muscarinic receptor-induced inotropic and chronotropic effects in the mouse heart. [ABSTRACT FROM AUTHOR]

Published

2024

15. Treatments with Diquat Reveal the Relationship between Protein Phosphatases (PP2A) and Oxidative Stress during Mitosis in Arabidopsis thaliana Root Meristems.

Author

Kelemen, Adrienn, Garda, Tamás, Kónya, Zoltán, Erdődi, Ferenc, Ujlaky-Nagy, László, Juhász, Gabriella Petra, Freytag, Csongor, M-Hamvas, Márta, and Máthé, Csaba

Subjects

PHOSPHOPROTEIN phosphatases, REACTIVE oxygen species, ARABIDOPSIS thaliana, POST-translational modification, CELL division

Abstract

Reversible protein phosphorylation regulates various cellular mechanisms in eukaryotes by altering the conformation, activity, localization, and stability of substrate proteins. In Arabidopsis thaliana root meristems, histone post-translational modifications are crucial for proper cell division, and they are also involved in oxidative stress signaling. To investigate the link between reactive oxygen species (ROS) and mitosis, we treated various Arabidopsis genotypes, including wild-types and mutants showing dysfunctional PP2A, with the ROS-inducing herbicide diquat (DQ). Studying the c3c4 double catalytic subunit mutant and fass regulatory subunit mutants of PP2A provided insights into phosphorylation-dependent mitotic processes. DQ treatment reduced mitotic activity in all genotypes and caused early mitotic arrest in PP2A mutants, likely due to oxidative stress-induced damage to essential mitotic processes. DQ had a minimal effect on reversible histone H3 phosphorylation in wild-type plants but significantly decreased phospho-histone H3 levels in PP2A mutants. Following drug treatment, the phosphatase activity decreased only in the stronger phenotype mutant plants (fass-5 and c3c4). Our findings demonstrate that (i) the studied PP2A loss-of-function mutants are more sensitive to increased intracellular ROS and (ii) DQ has indirect altering effects of mitotic activities and histone H3 phosphorylation. All these findings underscore the importance of PP2A in stress responses. [ABSTRACT FROM AUTHOR]

Published

2024

16. Structural basis for PP2A-mediated regulation of accurate chromosome segregation

Author

Sotelo Parrilla, Paula, Arulanandam, Jeyaprakash, and Cheerambathur, Dhanya Kolozhy

Subjects

PP2A-mediated regulation, accurate chromosome segregation, kinases, phosphatases, mitosis, Protein phosphatases, Chromosomal Passenger Complex (CPC), Aurora B kinase, PP2A, Shugoshin1 (Sgo1), Aurora B, Spindle Assembly Checkpoint, mitotic exit, Spindle and Kinetochoreassociated (Ska) complex

Abstract

The dynamic crosstalk between kinases and phosphatases is essential to ensure faithful mitosis. Protein phosphatases PP2A(B55) and PP2A(B56), and the Chromosomal Passenger Complex -CPC, containing Aurora B kinase-, establish a signalling network that controls sister chromatid cohesion, kinetochore-microtubule attachments, and timely chromosome segregation. PP2A(B56), together with Shugoshin1 (Sgo1), opposes Aurora B during early mitosis to protect cohesin from being disassembled at the inner centromere. PP2A(B56) and Aurora B also act antagonistically in controlling the processes of error correction and activation of the Spindle Assembly Checkpoint, both of which are essential to achieve chromosome biorientation. PP2A(B55) is the master regulator of mitotic exit, as it triggers late mitotic events by counteracting Cdk1 activity. Combining biochemistry, structural biology and biophysics, my work sheds light into the mechanistic basis of how PP2A regulates these key mitotic events through its interaction with Shugoshin1, the Chromosomal Passenger Complex and the Ska complex. Recent studies have shown that individual PP2A(B56) isoforms might have differential roles during mitosis. Nevertheless, the structural and functional basis of this isoform specificity and how it affects Sgo1 function remain unclear. In my thesis, I have explored the intricacies of PP2A(B56)-Sgo1 interactions and have discovered that Sgo1 binds PP2A(B56) in a B56- isoform-dependent manner. Our ongoing work hints that this specificity is mediated by dynamic interactions between Sgo1 and the B56 subunits, and aims to decipher the functional contribution of these interactions in achieving faithful chromosome segregation My work also unveils a novel interaction between PP2A(B56) and the CPC. Structural analysis of this complex shows that Borealin - one of the components of the CPC - contains a short linear motif that binds PP2A(B56) via the LxxIxE-binding pocket of B56. This highly conserved pocket is key for the recognition of PP2A(B56) interactors, and it is heavily involved in the regulation of PP2A activity and localisation during mitosis. The importance of this interaction in PP2A(B56) and/or CPC localisation and function in vivo is an outstanding question that our ongoing research aims to resolve. Recent studies suggested that PP2A(B55) might interact with the Spindle and Kinetochoreassociated (Ska) complex. The Ska complex is a key protein assembly -consisting of Ska1, Ska2 and Ska3- essential for stabilising load-bearing end-on kinetochore-microtubule attachments, and it is also found in the central spindle and midbody at the end of mitosis. Our research shows that the interaction between PP2A(B55) and the Ska complex is mediated by a short unstructured region of Ska3. This region binds the B55 subunit of PP2A and, according to our predicted models, it might involve its substrate-binding groove. Ongoing efforts in human cell lines aim to explain how this interaction controls the localisation and function of the Ska complex during late mitotic events.

Published

2023

17. The protein phosphatase-2A subunit PR130 is involved in the formation of cytotoxic protein aggregates in pancreatic ductal adenocarcinoma cells

Author

Alexandra Nguyen, Al-Hassan M. Mustafa, Alessa K. Leydecker, Melisa Halilovic, Janine Murr, Falk Butter, and Oliver H. Krämer

Subjects

Apoptosis, PDAC cells, Phendione, PP2A, PR130, Protein aggregates, Medicine, Cytology, QH573-671

Abstract

Abstract As a major source of cellular serine and threonine phosphatase activity, protein phosphatase-2A (PP2A) modulates signaling pathways in health and disease. PP2A complexes consist of catalytic, scaffolding, and B-type subunits. Seventeen PP2A B-type subunits direct PP2A complexes to selected substrates. It is ill-defined how PP2A B-type subunits determine the growth and drug responsiveness of tumor cells. Pancreatic ductal adenocarcinoma (PDAC) is a disease with poor prognosis. We analyzed the responses of murine and human mesenchymal and epithelial PDAC cells to the specific PP2A inhibitor phendione. We assessed protein levels by immunoblot and proteomics and cell fate by flow cytometry, confocal microscopy, and genetic manipulation. We show that murine mesenchymal PDAC cells express significantly higher levels of the PP2A B-type subunit PR130 than epithelial PDAC cells. This overexpression of PR130 is associated with a dependency of such metastasis-prone cells on the catalytic activity of PP2A. Phendione induces apoptosis and an accumulation of cytotoxic protein aggregates in murine mesenchymal and human PDAC cells. These processes occur independently of the frequently mutated tumor suppressor p53. Proteomic analyses reveal that phendione upregulates the chaperone HSP70 in mesenchymal PDAC cells. Inhibition of HSP70 promotes phendione-induced apoptosis and phendione promotes a proteasomal degradation of PR130. Genetic elimination of PR130 sensitizes murine and human PDAC cells to phendione-induced apoptosis and protein aggregate formation. These data suggest that the PP2A-PR130 complex dephosphorylates and thereby prevents the aggregation of proteins in tumor cells. Graphical Abstract

Published

2024

18. Resveratrol Induces Myotube Development by Altering Circadian Metabolism via the SIRT1-AMPK-PP2A Axis.

Author

Avital-Cohen, Natalie, Chapnik, Nava, and Froy, Oren

Subjects

*RESVERATROL, *CIRCADIAN rhythms, *AMP-activated protein kinases, *MUSCLE growth, *MUSCLE cells, *CELLULAR signal transduction, *METABOLISM

Abstract

Resveratrol is a polyphenol known to have metabolic as well as circadian effects. However, there is little information regarding the metabolic and circadian effect of resveratrol on muscle cells. We sought to investigate the metabolic impact of resveratrol throughout the circadian cycle to clarify the associated signaling pathways. C2C12 myotubes were incubated with resveratrol in the presence of increasing concentrations of glucose, and metabolic and clock proteins were measured for 24 h. Resveratrol led to SIRT1, AMPK and PP2A activation. Myotubes treated with increasing glucose concentrations showed higher activation of the mTOR signaling pathway. However, resveratrol did not activate the mTOR signaling pathway, except for P70S6K and S6. In accordance with the reduced mTOR activity, resveratrol led to advanced circadian rhythms and reduced levels of pBMAL1 and CRY1. Resveratrol increased myogenin expression and advanced its rhythms. In conclusion, resveratrol activates the SIRT1-AMPK-PP2A axis, advances circadian rhythms and induces muscle development. [ABSTRACT FROM AUTHOR]

Published

2024

19. TIPRL1 and its ATM-dependent phosphorylation promote radiotherapy resistance in head and neck cancer.

Author

Cokelaere, Célie, Dok, Rüveyda, Cortesi, Emanuela E., Zhao, Peihua, Sablina, Anna, Nuyts, Sandra, Derua, Rita, and Janssens, Veerle

Subjects

*HEAD & neck cancer, *DNA repair, *PHOSPHORYLATION, *PHOSPHOPROTEIN phosphatases, *MTOR protein, *CELL cycle, *REVERSE transcriptase

Abstract

Purpose: TIPRL1 (target of rapamycin signaling pathway regulator-like 1) is a known interactor and inhibitor of protein phosphatases PP2A, PP4 and PP6 – all pleiotropic modulators of the DNA Damage Response (DDR). Here, we investigated the role of TIPRL1 in the radiotherapy (RT) response of Head and Neck Squamous Cell Carcinoma (HNSCC). Methods: TIPRL1 mRNA (cBioportal) and protein expression (immunohistochemistry) in HNSCC samples were linked with clinical patient data. TIPRL1-depleted HNSCC cells were generated by CRISPR/Cas9 editing, and effects on colony growth, micronuclei formation (microscopy), cell cycle (flow cytometry), DDR signaling (immunoblots) and proteome (mass spectrometry) following RT were assessed. Mass spectrometry was used for TIPRL1 phosphorylation and interactomics analysis in irradiated cells. Results: TIPRL1 expression was increased in tumor versus non-tumor tissue, with high tumoral TIPRL1 expression associating with lower locoregional control and decreased survival of RT-treated patients. TIPRL1 deletion in HNSCC cells resulted in increased RT sensitivity, a faster but prolonged cell cycle arrest, increased micronuclei formation and an altered proteome-wide DDR. Upon irradiation, ATM phosphorylates TIPRL1 at Ser265. A non-phospho Ser265Ala mutant could not rescue the increased radiosensitivity phenotype of TIPRL1-depleted cells. While binding to PP2A-like phosphatases was confirmed, DNA-dependent protein kinase (DNA-PKcs), RAD51 recombinase and nucleosomal histones were identified as novel TIPRL1 interactors. Histone binding, although stimulated by RT, was adversely affected by TIPRL1 Ser265 phosphorylation. Conclusions: Our findings underscore a clinically relevant role for TIPRL1 and its ATM-dependent phosphorylation in RT resistance through modulation of the DDR, highlighting its potential as a new HNSCC predictive marker and therapeutic target. [ABSTRACT FROM AUTHOR]

Published

2024

20. LncRNA ENST00000440246.1 Promotes Alzheimer's Disease Progression by Targeting PP2A.

Author

Gao, Shang, Fan, Chang, Wang, Yongzhong, Yang, Wenming, and Jiang, Hui

Subjects

*ALZHEIMER'S disease, *LINCRNA, *PEARSON correlation (Statistics), *DISEASE progression, *MONTREAL Cognitive Assessment, *GENE expression

Abstract

Alzheimer's disease (AD) is an extremely prevalent neurodegenerative disease. Long noncoding RNAs (lncRNAs) play pivotal roles in the regulation of AD. However, the function of most lncRNAs in AD remains to be elucidated. In this study, the effects of lncRNA ENST00000440246.1 on the biological characteristics of AD were explored. Differentially expressed lncRNAs in AD were identified through bioinformatics analysis and peripheral blood from thirty AD patients was collected to verify the expression of these lncRNAs by quantitative real-time polymerase chain reaction (RT-qPCR). The correlations between lncRNAs and the Mini-Mental State Examination (MMSE) or the Montreal Cognitive Assessment (MoCA) were assessed by Pearson's correlation analysis. Immunofluorescence (IF), Cell Counting Kit-8 (CCK-8) and flow cytometry assays were conducted to evaluate the biological effect of ENST00000440246.1 and protein phosphatase 2 A (PP2A) in SK-N-SH cells. Gene expression at the protein and mRNA levels was analyzed by Western blotting and RT-qPCR. The interaction between PP2A and ENST00000440246.1 was confirmed by IntaRNA and RNA pulldown assays. ENST00000440246.1 was upregulated and significantly negatively correlated with the MMSE and MoCA scores and the overexpression of ENST00000440246.1 inhibited cell proliferation and facilitated apoptosis and Aβ expression in SK-N-SH cells. Mechanistically, ENST00000440246.1 targeted PP2A and regulated AD-related gene expression. The silencing of ENST00000440246.1 had the opposite effect. Furthermore, PP2A overexpression reversed the influence of ENST00000440246.1 overexpression in SK-N-SH cells. In conclusion, ENST00000440246.1 could promote AD progression by targeting PP2A, which indicates that ENST00000440246.1 has the potential to be a diagnostic target in AD. [ABSTRACT FROM AUTHOR]

Published

2024

21. Protein phosphatase 2A modulation and connection with miRNAs and natural products.

Author

Chuang, Ya‐Ting, Yen, Ching‐Yu, Tang, Jen‐Yang, Chang, Fang‐Rong, Tsai, Yi‐Hong, Wu, Kuo‐Chuan, Chien, Tsu‐Ming, and Chang, Hsueh‐Wei

Subjects

PHOSPHOPROTEIN phosphatases, NATURAL products, MICRORNA, CELL physiology, DATABASES

Abstract

Protein phosphatase 2A (PP2A), a heterotrimeric holoenzyme (scaffolding, catalytic, and regulatory subunits), regulates dephosphorylation for more than half of serine/threonine phosphosites and exhibits diverse cellular functions. Although several studies on natural products and miRNAs have emphasized their impacts on PP2A regulation, their connections lack systemic organization. Moreover, only part of the PP2A family has been investigated. This review focuses on the PP2A‐modulating effects of natural products and miRNAs' interactions with potential PP2A targets in cancer and non‐cancer cells. PP2A‐modulating natural products and miRNAs were retrieved through a literature search. Utilizing the miRDB database, potential PP2A targets of these PP2A‐modulating miRNAs for the whole set (17 members) of the PP2A family were retrieved. Finally, PP2A‐modulating natural products and miRNAs were linked via a literature search. This review provides systemic directions for assessing natural products and miRNAs relating to the PP2A‐modulating functions in cancer and disease treatments. [ABSTRACT FROM AUTHOR]

Published

2024

22. The protein phosphatase-2A subunit PR130 is involved in the formation of cytotoxic protein aggregates in pancreatic ductal adenocarcinoma cells.

Author

Nguyen, Alexandra, Mustafa, Al-Hassan M., Leydecker, Alessa K., Halilovic, Melisa, Murr, Janine, Butter, Falk, and Krämer, Oliver H.

Subjects

*PANCREATIC duct, *TUMOR proteins, *EPITHELIAL cells, *PROTEINS, *ADENOCARCINOMA, *TUMOR suppressor genes, *SERINE/THREONINE kinases

Abstract

As a major source of cellular serine and threonine phosphatase activity, protein phosphatase-2A (PP2A) modulates signaling pathways in health and disease. PP2A complexes consist of catalytic, scaffolding, and B-type subunits. Seventeen PP2A B-type subunits direct PP2A complexes to selected substrates. It is ill-defined how PP2A B-type subunits determine the growth and drug responsiveness of tumor cells. Pancreatic ductal adenocarcinoma (PDAC) is a disease with poor prognosis. We analyzed the responses of murine and human mesenchymal and epithelial PDAC cells to the specific PP2A inhibitor phendione. We assessed protein levels by immunoblot and proteomics and cell fate by flow cytometry, confocal microscopy, and genetic manipulation. We show that murine mesenchymal PDAC cells express significantly higher levels of the PP2A B-type subunit PR130 than epithelial PDAC cells. This overexpression of PR130 is associated with a dependency of such metastasis-prone cells on the catalytic activity of PP2A. Phendione induces apoptosis and an accumulation of cytotoxic protein aggregates in murine mesenchymal and human PDAC cells. These processes occur independently of the frequently mutated tumor suppressor p53. Proteomic analyses reveal that phendione upregulates the chaperone HSP70 in mesenchymal PDAC cells. Inhibition of HSP70 promotes phendione-induced apoptosis and phendione promotes a proteasomal degradation of PR130. Genetic elimination of PR130 sensitizes murine and human PDAC cells to phendione-induced apoptosis and protein aggregate formation. These data suggest that the PP2A-PR130 complex dephosphorylates and thereby prevents the aggregation of proteins in tumor cells. [ABSTRACT FROM AUTHOR]

Published

2024

23. Inducible degradation-coupled phosphoproteomics identifies PP2ARts1 as a novel eisosome regulator

Author

Andrew G. DeMarco, Marcella G. Dibble, and Mark C. Hall

Subjects

eisosome, PP2A, Rts1, B56, phosphatase, phosphoproteomics, Biology (General), QH301-705.5

Abstract

IntroductionReversible protein phosphorylation is an abundant post-translational modification dynamically regulated by opposing kinases and phosphatases. Protein phosphorylation has been extensively studied in cell division, where waves of cyclin-dependent kinase activity, peaking in mitosis, drive the sequential stages of the cell cycle. Here we developed and employed a strategy to specifically probe kinase or phosphatase substrates at desired times or experimental conditions in the model organism Saccharomyces cerevisiae.MethodsWe combined auxin-inducible degradation (AID) with mass spectrometry-based phosphoproteomics, which allowed us to arrest physiologically normal cultures in mitosis prior to rapid phosphatase degradation and phosphoproteome analysis.Results and discussionOur results revealed that protein phosphatase 2A coupled with its B56 regulatory subunit, Rts1 (PP2ARts1), is involved in dephosphorylation of numerous proteins in mitosis, highlighting the need for phosphatases to selectively maintain certain proteins in a hypophosphorylated state in the face of high mitotic kinase activity. Unexpectedly, we observed elevated phosphorylation at many sites on several subunits of the fungal eisosome complex following rapid Rts1 degradation. Eisosomes are dynamic polymeric assemblies that create furrows in the plasma membrane important in regulating nutrient import, lipid metabolism, and stress responses, among other things. We found that PP2ARts1-mediated dephosphorylation of eisosomes promotes their plasma membrane association and we provide evidence that this regulation impacts eisosome roles in metabolic homeostasis. The combination of rapid, inducible protein degradation with proteomic profiling offers several advantages over common protein disruption methods for characterizing substrates of regulatory enzymes involved in dynamic biological processes.

Published

2024

24. PP2A-B55 phosphatase counteracts Ki-67-dependent chromosome individualization during mitosis

Author

María Sanz-Flores, Miguel Ruiz-Torres, Cristina Aguirre-Portolés, Aicha El Bakkali, Beatriz Salvador-Barberó, Carolina Villarroya-Beltri, Sagrario Ortega, Diego Megías, Daniel W. Gerlich, Mónica Álvarez-Fernández, and Marcos Malumbres

Subjects

PP2A, PPP2R2A, PPP2R2D, B55, Ki-67, mitosis, Biology (General), QH301-705.5

Abstract

Summary: Cell cycle progression is regulated by the orderly balance between kinase and phosphatase activities. PP2A phosphatase holoenzymes containing the B55 family of regulatory B subunits function as major CDK1-counteracting phosphatases during mitotic exit in mammals. However, the identification of the specific mitotic roles of these PP2A-B55 complexes has been hindered by the existence of multiple B55 isoforms. Here, through the generation of loss-of-function genetic mouse models for the two ubiquitous B55 isoforms (B55α and B55δ), we report that PP2A-B55α and PP2A-B55δ complexes display overlapping roles in controlling the dynamics of proper chromosome individualization and clustering during mitosis. In the absence of PP2A-B55 activity, mitotic cells display increased chromosome individualization in the presence of enhanced phosphorylation and perichromosomal loading of Ki-67. These data provide experimental evidence for a regulatory mechanism by which the balance between kinase and PP2A-B55 phosphatase activity controls the Ki-67-mediated spatial organization of the mass of chromosomes during mitosis.

Published

2024

25. Altering phosphorylation in cancer through PP2A modifiers

Author

Hannah Johnson, Satya Narayan, and Arun K. Sharma

Subjects

PP2A, Activators, Inhibitors, Cancer, Therapeutics, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282, Cytology, QH573-671

Abstract

Abstract Protein phosphatase 2A (PP2A) is a serine/threonine phosphatase integral to the regulation of many cellular processes. Due to the deregulation of PP2A in cancer, many of these processes are turned toward promoting tumor progression. Considerable research has been undertaken to discover molecules capable of modulating PP2A activity in cancer. Because PP2A is capable of immense substrate specificity across many cellular processes, the therapeutic targeting of PP2A in cancer can be completed through either enzyme inhibitors or activators. PP2A modulators likewise tend to be effective in drug-resistant cancers and work synergistically with other known cancer therapeutics. In this review, we will discuss the patterns of PP2A deregulation in cancer, and its known downstream signaling pathways important for cancer regulation, along with many activators and inhibitors of PP2A known to inhibit cancer progression.

Published

2024

26. Altering phosphorylation in cancer through PP2A modifiers

Author

Johnson, Hannah, Narayan, Satya, and Sharma, Arun K.

Published

2024

27. Astrocyte‐derived lactoferrin reduces β‐amyloid burden by promoting the interaction between p38 kinase and PP2A phosphatase in male APP/PS1 transgenic mice.

Author

Fan, Yong‐Gang, Guo, Chuang, Zhao, Ling‐Xiao, Ge, Ri‐Le, Pang, Zhong‐Qiu, He, Da‐Long, Ren, Hang, Wu, Ting‐Yao, Zhang, Yan‐Hui, and Wang, Zhan‐You

Subjects

*TRANSGENIC mice, *AMYLOID beta-protein precursor, *PRESENILINS, *ALZHEIMER'S disease, *MITOGEN-activated protein kinase phosphatases, *LACTOFERRIN, *PROTEIN overexpression, *PHOSPHOPROTEIN phosphatases

Abstract

Background and Purpose: Overexpression of astrocytic lactoferrin (Lf) was observed in the brain of Alzheimer's disease (AD) patients, whereas the role of astrocytic Lf in AD progression remains unexplored. In this study, we aimed to evaluate the effects of astrocytic Lf on AD progression. Experimental Approach: Male APP/PS1 mice with astrocytes overexpressing human Lf were developed to evaluate the effects of astrocytic Lf on AD progression. N2a‐sw cells also were employed to further uncover the mechanism of astrocytic Lf on β‐amyloid (Aβ) production. Key Results: Astrocytic Lf overexpression increased protein phosphatase 2A (PP2A) activity and reduced amyloid precursor protein (APP) phosphorylation, Aβ burden and tau hyperphosphorylation in APP/PS1 mice. Mechanistically, astrocytic Lf overexpression promoted the uptake of astrocytic Lf into neurons in APP/PS1 mice, and conditional medium from astrocytes overexpressing Lf inhibited p‐APP (Thr668) expression in N2a‐sw cells. Furthermore, recombinant human Lf (hLf) significantly enhanced PP2A activity and inhibited p‐APP expression, whereas inhibition of p38 or PP2A activities abrogated the hLf‐induced p‐APP down‐regulation in N2a‐sw cells. Additionally, hLf promoted the interaction of p38 and PP2A via p38 activation, thereby enhancing PP2A activity, and low‐density lipoprotein receptor‐related protein 1 (LRP1) knockdown significantly reversed the hLf‐induced p38 activation and p‐APP down‐regulation. Conclusions and Implications: Our data suggested that astrocytic Lf promoted neuronal p38 activation, via targeting to LRP1, subsequently promoting p38 binding to PP2A to enhance PP2A enzyme activity, which finally inhibited Aβ production via APP dephosphorylation. In conclusion, promoting astrocytic Lf expression may be a potential strategy against AD. LINKED ARTICLES: This article is part of a themed issue From Alzheimer's Disease to Vascular Dementia: Different Roads Leading to Cognitive Decline. To view the other articles in this section visit http://onlinelibrary.wiley.com/doi/10.1111/bph.v181.6/issuetoc [ABSTRACT FROM AUTHOR]

Published

2024

28. Mutations at Two Key Sites in PP2A Safeguard Caenorhabditis elegans Neurons from Microcystin-LR Toxicity.

Author

Zhan, Chunhua and Gong, Jianke

Subjects

*CAENORHABDITIS elegans, *GENOME editing, *BODIES of water, *AMINO acids, *NEMATODES

Abstract

Microcystin-LR (MC-LR) is a secondary metabolite produced by cyanobacteria, globally renowned for its potent hepatotoxicity. However, an increasing body of research suggests that it also exhibits pronounced neurotoxicity. PP2A is a fundamental intracellular phosphatase that plays a pivotal role in cell development and survival. Although extensive research has focused on the binding of MC-LR to the C subunit of PP2A, few studies have explored the key amino acid sites that can prevent the binding of MC-LR to PP2A-C. Due to the advantages of Caenorhabditis elegans (C. elegans), such as ease of genetic editing and a short lifespan, we exposed nematodes to MC-LR in a manner that simulated natural exposure conditions based on MC-LR concentrations in natural water bodies (immersion exposure). Our findings demonstrate that MC-LR exerts comprehensive toxicity on nematodes, including reducing lifespan, impairing reproductive capabilities, and diminishing sensory functions. Notably, and for the first time, we observed that MC-LR neurotoxic effects can persist up to the F3 generation, highlighting the significant threat that MC-LR poses to biological populations in natural environments. Furthermore, we identified two amino acid sites (L252 and C278) in PP2A-C through mutations that prevented MC-LR binding without affecting PP2A activity. This discovery was robustly validated through behavioral studies and neuronal calcium imaging using nematodes. In conclusion, we identified two crucial amino acid sites that could prevent MC-LR from binding to PP2A-C, which holds great significance for the future development of MC-LR detoxification drugs. [ABSTRACT FROM AUTHOR]

Published

2024

29. PP2A and GSK3 act as modifiers of FUS-ALS by modulating mitochondrial transport.

Author

Tziortzouda, Paraskevi, Steyaert, Jolien, Scheveneels, Wendy, Sicart, Adria, Stoklund Dittlau, Katarina, Barbosa Correia, Adriana Margarida, Burg, Thibaut, Pal, Arun, Hermann, Andreas, Van Damme, Philip, Moens, Thomas G., and Van Den Bosch, Ludo

Abstract

Amyotrophic lateral sclerosis (ALS) is a fatal neurodegenerative disease which currently lacks effective treatments. Mutations in the RNA-binding protein FUS are a common cause of familial ALS, accounting for around 4% of the cases. Understanding the mechanisms by which mutant FUS becomes toxic to neurons can provide insight into the pathogenesis of both familial and sporadic ALS. We have previously observed that overexpression of wild-type or ALS-mutant FUS in Drosophila motor neurons is toxic, which allowed us to screen for novel genetic modifiers of the disease. Using a genome-wide screening approach, we identified Protein Phosphatase 2A (PP2A) and Glycogen Synthase Kinase 3 (GSK3) as novel modifiers of FUS-ALS. Loss of function or pharmacological inhibition of either protein rescued FUS-associated lethality in Drosophila. Consistent with a conserved role in disease pathogenesis, pharmacological inhibition of both proteins rescued disease-relevant phenotypes, including mitochondrial trafficking defects and neuromuscular junction failure, in patient iPSC-derived spinal motor neurons (iPSC-sMNs). In FUS-ALS flies, mice, and human iPSC-sMNs, we observed reduced GSK3 inhibitory phosphorylation, suggesting that FUS dysfunction results in GSK3 hyperactivity. Furthermore, we found that PP2A acts upstream of GSK3, affecting its inhibitory phosphorylation. GSK3 has previously been linked to kinesin-1 hyperphosphorylation. We observed this in both flies and iPSC-sMNs, and we rescued this hyperphosphorylation by inhibiting GSK3 or PP2A. Moreover, increasing the level of kinesin-1 expression in our Drosophila model strongly rescued toxicity, confirming the relevance of kinesin-1 hyperphosphorylation. Our data provide in vivo evidence that PP2A and GSK3 are disease modifiers, and reveal an unexplored mechanistic link between PP2A, GSK3, and kinesin-1, that may be central to the pathogenesis of FUS-ALS and sporadic forms of the disease. [ABSTRACT FROM AUTHOR]

Published

2024

30. Regulation of DNA replication by PP2A family phosphatases

Author

Jenkinson, Fiona and Zegerman, Philip

Subjects

PP2A, DNA replication, phosphatases, replication initiation, dephosphorylation, Sld3, cell cycle

Abstract

In eukaryotes, DNA is replicated once and only once per cell cycle from hundreds of replication initiation sites (origins) across the genome. This process is strictly controlled as mis-regulation can cause replication stress and genome instability, characteristics of cancer. S phase Cyclin-dependent kinase (S-CDK) plays a dual role in this regulation both by restricting helicase loading (licensing) to G1 phase, and by activating origin firing in S phase. The essential S-CDK phosphorylation of the limiting initiation proteins, Sld2 and Sld3, is sufficient for CDK's role in replisome activation in Saccharomyces cerevisiae. This modification permits a cascade of protein recruitment to origins that completes replisome assembly, however, Sld2 and Sld3 do not travel with the replisome during replication elongation. It is not known whether the release of these factors from origins is phospho-dependent or whether this dissociation is important for replication control. In this thesis I investigate the observation that Sld2 and Sld3 are specifically, actively dephosphorylated in S phase. I identify PP2A-Rts1 and PP2A-Cdc55, alongside PP4, as the phosphatases responsible for Sld3 dephosphorylation and partially of Sld2. To overcome the pleiotropy of these phosphatases hindering S phase analysis, I identify the Sld3-PP2A-RTS1 interaction site and mutation of this site affects Sld3 dephosphorylation in S phase and at mitotic exit. Conditionally disrupting the S phase dephosphorylation of Sld3 results in impaired genome duplication and is lethal. Replication profiling and helicase chromatin immunoprecipitation (ChIP) show that this is due to a global defect in replication initiation. Adding recombinant PP2A-Rts1 to a reconstituted yeast replication system is sufficient to enhance DNA replication. Finally, I use ChIP-seq and genetics to test models for the mechanisms by which PP2A acts as a novel positive regulator of DNA replication initiation. This work has revealed that the dynamic turnover of Sld2 and Sld3 phosphorylation in S phase is essential. It appears that, like CDK, PP2A plays a critical dual role in preventing inappropriate replication initiation outside of S phase and stimulating it in S phase. With the conservation of this phenomenon to metazoa showing promise, this work should incentivise further studies to uncover the potential of PP2A phosphatases in differential S phase length control and as targets for cancer therapy.

Published

2022

31. I2PP2A (SET) and Cancerous Inhibitor of Protein Phosphatase 2A (CIP2A) as novel therapeutic targets for Mixed Lineage Leukaemia(MLL)

Author

Di Mambro, Antonella, Calle-Patino, Yolanda, Esposito, Maria, and Wrench, Bela

Subjects

MLL, Leukaemia, FTY720, Carfilzomib, SETBP1, SET, CIP2A, PP2A

Abstract

Mixed Lineage Leukaemia (MLL) is an aggressive form of blood cancer which predominantly affects children as results of rearrangements of the MLL (KMT2A) gene at 11q23. MLL accounts for more than 70% of infant Acute Lymphoblastic Leukaemia (ALL) and between 35-50% of infant Acute Myeloid Leukaemia (AML) and, presents a very poor survival. Indeed, only 40% of the MLL patients approaches 5-years survival rate. Although new treatments have been devised to target the activity of KMT2A fusion proteins, none of these have been translated into new therapies for patients and MLL is a leukaemia of unmet clinical need. Several recent papers have identified protein kinases as hyperactivated in MLL leukaemia and potential target for treatment. Our group is investigating the contribution of Protein Phosphatase 2A (PP2A), one of the upstream regulators of protein kinases, in MLL. Our results showed that the downstream targets of this phosphatase were constitutively deregulated and hyperactivated in MLL, suggesting a potential inactivation of PP2A in this disease. SET and CIP2A are the best well-known endogenous inhibitors of PP2A. SET directly interacts with the catalytic subunit of PP2A and impairs its activity towards the phosphorylation of AKT, ERK and GSK3-ß, whereas CIP2A modulates the activity of the phosphatase by direct interaction with the structural and regulatory subunit PP2A/B56 and by preventing the dephosphorylation of a PP2A downstream target and potent oncoprotein known as c-Myc. Published studies showed that therapeutic targeting of SET and CIP2A, rescued PP2A activity and blocked malignant proliferation in solid tumours and haematological malignancies. In this study I investigated for the first time the molecular profile of SET and CIP2A in MLL. Importantly, my findings showed that SET and CIP2A are essential proteins involved in MLL self renewal of MLL and that their pharmacological inhibition blocks MLL proliferation. The impact of these data open new avenues of research into promising and treatments for this disease, with the aim of sparing the MLL patients from toxic chemotherapy treatment and improving their survival chances.

Published

2022

32. Mitf, with Yki and STRIPAK-PP2A, is a key determinant of form and fate in the progenitor epithelium of the Drosophila eye.

Author

Tianyi Zhang, Qingxiang Zhou, Nisveta Jusić, Wenwen Lu, Francesca Pignoni, and Scott J. Neal

Subjects

Striatin, YAP, PP2A, Retina, Fate, Epithelial morphology, Cytology, QH573-671

Abstract

The Microphthalmia-associated Transcription Factor (MITF) governs numerous cellular and developmental processes. In mice, it promotes specification and differentiation of the retinal pigmented epithelium (RPE), and in humans, some mutations in MITF induce congenital eye malformations. Herein, we explore the function and regulation of Mitf in Drosophila eye development and uncover two roles. We find that knockdown of Mitf results in retinal displacement (RDis), a phenotype associated with abnormal eye formation. Mitf functions in the peripodial epithelium (PE), a retinal support tissue akin to the RPE, to suppress RDis, via the Hippo pathway effector Yorkie (Yki). Yki physically interacts with Mitf and can modify its transcriptional activity in vitro. Severe loss of Mitf, instead, results in the de-repression of retinogenesis in the PE, precluding its development. This activity of Mitf requires the protein phosphatase 2 A holoenzyme STRIPAK-PP2A, but not Yki; Mitf transcriptional activity is potentiated by STRIPAK-PP2A in vitro and in vivo. Knockdown of STRIPAK-PP2A results in cytoplasmic retention of Mitf in vivo and in its decreased stability in vitro, highlighting two potential mechanisms for the control of Mitf function by STRIPAK-PP2A. Thus, Mitf functions in a context-dependent manner as a key determinant of form and fate in the Drosophila eye progenitor epithelium.

Published

2024

33. Protein phosphatase 2A anchoring disruptor gene therapy for familial dilated cardiomyopathy

Author

Xueyi Li, Jinliang Li, Anne-Maj Samuelsson, Hrishikesh Thakur, and Michael S. Kapiloff

Subjects

dilated cardiomyopathy, PP2A, adeno-associated virus, gene therapy, Genetics, QH426-470, Cytology, QH573-671

Abstract

Familial dilated cardiomyopathy is a prevalent cause of heart failure that results from the mutation of genes encoding proteins of diverse function. Despite modern therapy, dilated cardiomyopathy typically has a poor outcome and is the leading cause of cardiac transplantation. The phosphatase PP2A at cardiomyocyte perinuclear mAKAPβ signalosomes promotes pathological eccentric cardiac remodeling, as is characteristic of dilated cardiomyopathy. Displacement of PP2A from mAKAPβ, inhibiting PP2A function in that intracellular compartment, can be achieved by expression of a mAKAPβ-derived PP2A binding domain-derived peptide. To test whether PP2A anchoring disruption would be effective at preventing dilated cardiomyopathy-associated cardiac dysfunction, the adeno-associated virus gene therapy vector AAV9sc.PBD was devised to express the disrupting peptide in cardiomyocytes in vivo. Proof-of-concept is now provided that AAV9sc.PBD improves the cardiac structure and function of a cardiomyopathy mouse model involving transgenic expression of a mutant α-tropomyosin E54K Tpm1 allele, while AAV9sc.PBD has no effect on normal non-transgenic mice. At the cellular level, AAV9sc.PBD restores cardiomyocyte morphology and gene expression in the mutant Tpm1 mouse. As the mechanism of AAV9sc.PBD action suggests potential efficacy in dilated cardiomyopathy regardless of the underlying etiology, these data support the further testing of AAV9sc.PBD as a broad-based treatment for dilated cardiomyopathy.

Published

2024

34. Global post-translational modification profiling of HIV-1-infected cells reveals mechanisms of host cellular pathway remodeling

Author

Johnson, Jeffrey R, Crosby, David C, Hultquist, Judd F, Kurland, Andrew P, Adhikary, Prithy, Li, Donna, Marlett, John, Swann, Justine, Hüttenhain, Ruth, Verschueren, Erik, Johnson, Tasha L, Newton, Billy W, Shales, Michael, Simon, Viviana A, Beltrao, Pedro, Frankel, Alan D, Marson, Alexander, Cox, Jeffery S, Fregoso, Oliver I, Young, John AT, and Krogan, Nevan J

Subjects

HIV/AIDS, Infectious Diseases, Biotechnology, Genetics, Aetiology, 2.1 Biological and endogenous factors, Infection, HIV Infections, HIV Seropositivity, HIV-1, Humans, Protein Processing, Post-Translational, Proteomics, Ubiquitination, CP: Microbiology, CP: Molecular biology, b56, histone h1, phosphorylation, pp2a, proteomics, systems biology, ubiquitination, vif, vpr, Biochemistry and Cell Biology, Medical Physiology

Abstract

Viruses must effectively remodel host cellular pathways to replicate and evade immune defenses, and they must do so with limited genomic coding capacity. Targeting post-translational modification (PTM) pathways provides a mechanism by which viruses can broadly and rapidly transform a hostile host environment into a hospitable one. We use mass spectrometry-based proteomics to quantify changes in protein abundance and two PTM types-phosphorylation and ubiquitination-in response to HIV-1 infection with viruses harboring targeted deletions of a subset of HIV-1 genes. PTM analysis reveals a requirement for Aurora kinase activity in HIV-1 infection and identified putative substrates of a phosphatase that is degraded during infection. Finally, we demonstrate that the HIV-1 Vpr protein inhibits histone H1 ubiquitination, leading to defects in DNA repair.

Published

2022

35. Circular RNA CCT3 is a unique molecular marker in bladder cancer

Author

Lin Luo, Qingzhi Xie, Yunchou Wu, Ping Li, FuQiang Qin, Dunming Liao, and KangNing Wang

Subjects

Circular RNA CCT3, Bladder cancer, Diagnosis, Prognosis, PP2A, miR-135a-5p, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract This study surveyed circular RNA CCT3 in bladder cancer (BCa). We recruited 85 BCa patients and 40 normal controls (Normal) and collected clinical specimens for analysis. circRNA CCT3 expression was analyzed by RT-qPCR, diagnostic accuracy was calculated by ROC curves, and survival outcomes were evaluated by survival curves. CircRNA CCT3 was overexpressed or knocked down in cells, thereafter to observe the changes in cell malignant phenotypes. The downstream molecules of circRNA CCT3 were detected. Our data suggest that circRNA CCT3 was upregulated in human BCa and was associated with poor survival outcomes of BCa patients. In cell experiments, overexpressing circRNA CCT3 promoted BCa cell malignancy, whereas silencing circRNA CCT3 did the opposite. In addition, circRNA CCT3 modulated PP2A expression by miR-135a-5p. This study demonstrates that circRNA CCT3 is a diagnostic and prognostic biomarker in BCa patients and is a tumor promoter in BCa.

Published

2023

36. Unraveling pathogen deceptive disguise: from modules to mimicry.

Author

Thakur, Kanika, Shree, Ankita, and Verma, Praveen Kumar

Subjects

*HOST plants, *PHYTOPHTHORA, *PATHOGENIC microorganisms

Abstract

Pathogens rely on their effector proteins to colonize host plants. These effectors have diverse functions. A recent study by Li et al. highlights the significance of protein modularity in generating functional diversity among Phytophthora effectors. It underscores the sophisticated tactics that phytopathogens adopt to alter host cellular processes. [ABSTRACT FROM AUTHOR]

Published

2024

37. Treatments with Diquat Reveal the Relationship between Protein Phosphatases (PP2A) and Oxidative Stress during Mitosis in Arabidopsis thaliana Root Meristems

Author

Adrienn Kelemen, Tamás Garda, Zoltán Kónya, Ferenc Erdődi, László Ujlaky-Nagy, Gabriella Petra Juhász, Csongor Freytag, Márta M-Hamvas, and Csaba Máthé

Subjects

protein phosphatases, PP2A, FASS, C3-C4, histone H3 phosphorylation, mitosis, Botany, QK1-989

Abstract

Reversible protein phosphorylation regulates various cellular mechanisms in eukaryotes by altering the conformation, activity, localization, and stability of substrate proteins. In Arabidopsis thaliana root meristems, histone post-translational modifications are crucial for proper cell division, and they are also involved in oxidative stress signaling. To investigate the link between reactive oxygen species (ROS) and mitosis, we treated various Arabidopsis genotypes, including wild-types and mutants showing dysfunctional PP2A, with the ROS-inducing herbicide diquat (DQ). Studying the c3c4 double catalytic subunit mutant and fass regulatory subunit mutants of PP2A provided insights into phosphorylation-dependent mitotic processes. DQ treatment reduced mitotic activity in all genotypes and caused early mitotic arrest in PP2A mutants, likely due to oxidative stress-induced damage to essential mitotic processes. DQ had a minimal effect on reversible histone H3 phosphorylation in wild-type plants but significantly decreased phospho-histone H3 levels in PP2A mutants. Following drug treatment, the phosphatase activity decreased only in the stronger phenotype mutant plants (fass-5 and c3c4). Our findings demonstrate that (i) the studied PP2A loss-of-function mutants are more sensitive to increased intracellular ROS and (ii) DQ has indirect altering effects of mitotic activities and histone H3 phosphorylation. All these findings underscore the importance of PP2A in stress responses.

Published

2024

38. PP2A‐based triple‐strike therapy overcomes mitochondrial apoptosis resistance in brain cancer cells

Author

Oxana V. Denisova, Joni Merisaari, Riikka Huhtaniemi, Xi Qiao, Laxman Yetukuri, Mikael Jumppanen, Amanpreet Kaur, Mirva Pääkkönen, Сarina vonSchantz‐Fant, Michael Ohlmeyer, Krister Wennerberg, Otto Kauko, Raphael Koch, Tero Aittokallio, Mikko Taipale, and Jukka Westermarck

Subjects

AKT, apoptosis, glioblastoma, mitochondria, PDK, PP2A, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Mitochondrial glycolysis and hyperactivity of the phosphatidylinositol 3‐kinase–protein kinase B (AKT) pathway are hallmarks of malignant brain tumors. However, kinase inhibitors targeting AKT (AKTi) or the glycolysis master regulator pyruvate dehydrogenase kinase (PDKi) have failed to provide clinical benefits for brain tumor patients. Here, we demonstrate that heterogeneous glioblastoma (GB) and medulloblastoma (MB) cell lines display only cytostatic responses to combined AKT and PDK targeting. Biochemically, the combined AKT and PDK inhibition resulted in the shutdown of both target pathways and priming to mitochondrial apoptosis but failed to induce apoptosis. In contrast, all tested brain tumor cell models were sensitive to a triplet therapy, in which AKT and PDK inhibition was combined with the pharmacological reactivation of protein phosphatase 2A (PP2A) by NZ‐8‐061 (also known as DT‐061), DBK‐1154, and DBK‐1160. We also provide proof‐of‐principle evidence for in vivo efficacy in the intracranial GB and MB models by the brain‐penetrant triplet therapy (AKTi + PDKi + PP2A reactivator). Mechanistically, PP2A reactivation converted the cytostatic AKTi + PDKi response to cytotoxic apoptosis, through PP2A‐elicited shutdown of compensatory mitochondrial oxidative phosphorylation and by increased proton leakage. These results encourage the development of triple‐strike strategies targeting mitochondrial metabolism to overcome therapy tolerance in brain tumors.

Published

2023

39. A pigmentary manifestation associated with PPP2R5D-related neurodevelopmental disorder: a case report and review of literature

Author

Philippe Pierre Robichaud, Nadia Bouhamdani, Eugénie Girouard, Emily Biden, and Mouna Ben Amor

Subjects

PPP2R5D, Neurodevelopmental disorder, PP2A, Intellectual disability, Café-au-lait macules, MRD35, Science

Abstract

Abstract Background The protein phosphatase 2 (PP2A) is one of the major serine/threonine phosphatases in humans. The most frequently reported pathogenic PP2A variants have been identified in PPP2R5D, encoding the regulatory subunit B’ delta, and are known to cause intellectual developmental disorder autosomal dominant 35 (MRD35). Case presentation Herein, we describe a unique case of a patient with a heterozygous pathogenic variant, c.592G>A/p.(Glu198Lys) in the PPP2R5D gene which was associated with hyperpigmented skin lesions arising from increased melanin production, known as Café-au-lait macules (CALMs). To our knowledge, this is the first reported case of a PPP2R5D-related neurodevelopmental disorder associated with CALMs. Conclusions Our findings suggest that the documentation and reporting of CALMs when associated with one or more physical and/or neurodevelopmental findings are of utmost importance as they could be indicative of an underreported phenotype and may extend the phenotypic spectrum of MRD35.

Published

2023

40. The B56γ3-containing protein phosphatase 2A attenuates p70S6K-mediated negative feedback loop to enhance AKT-facilitated epithelial-mesenchymal transition in colorectal cancer

Author

Kai-Ching Hsiao, Siou-Ying Ruan, Shih-Min Chen, Tai-Yu Lai, Ren-Hao Chan, Yan-Ming Zhang, Chien-An Chu, Hung-Chi Cheng, Hung-Wen Tsai, Yi-Fang Tu, Brian K. Law, Ting-Tsung Chang, Nan-Haw Chow, and Chi-Wu Chiang

Subjects

AKT, B56γ3, Colorectal cancer, EMT, PP2A, p70S6K, Medicine, Cytology, QH573-671

Abstract

Abstract Background Protein phosphatase 2A (PP2A) is one of the major protein phosphatases in eukaryotic cells and is essential for cellular homeostasis. PP2A is a heterotrimer comprising the dimeric AC core enzyme and a highly variable regulatory B subunit. Distinct B subunits help the core enzyme gain full activity toward specific substrates and contribute to diverse cellular roles of PP2A. PP2A has been thought to play a tumor suppressor and the B56γ3 regulatory subunit was shown to play a key tumor suppressor regulatory subunit of PP2A. Nevertheless, we uncovered a molecular mechanism of how B56γ3 may act as an oncogene in colorectal cancer (CRC). Methods Polyclonal pools of CRC cells with stable B56γ3 overexpression or knockdown were generated by retroviral or lentiviral infection and subsequent drug selection. Co-immunoprecipitation(co-IP) and in vitro pull-down analysis were applied to analyze the protein–protein interaction. Transwell migration and invasion assays were applied to investigate the role of B56γ3 in affecting motility and invasive capability of CRC cells. The sensitivity of CRC cells to 5-fluorouracil (5-FU) was analyzed using the PrestoBlue reagent assay for cell viability. Immunohistochemistry (IHC) was applied to investigate the expression levels of phospho-AKT and B56γ3 in paired tumor and normal tissue specimens of CRC. DataSets of TCGA and GEO were analyzed to investigate the correlation of B56γ3 expression with overall survival rates of CRC patients. Results We showed that B56γ3 promoted epithelial-mesenchymal transition (EMT) and reduced the sensitivity of CRC cells to 5-FU through upregulating AKT activity. Mechanistically, B56γ3 upregulates AKT activity by targeting PP2A to attenuate the p70S6K-mediated negative feedback loop regulation on PI3K/AKT activation. B56γ3 was highly expressed and positively correlated with the level of phospho-AKT in tumor tissues of CRC. Moreover, high B56γ3 expression is associated with poor prognosis of a subset of patients with CRC. Conclusions Our finding reveals that the B56γ3 regulatory subunit-containing PP2A plays an oncogenic role in CRC cells by sustaining AKT activation through suppressing p70S6K activity and suggests that the interaction between B56γ3 and p70S6K may serve as a therapeutic target for CRC. Video Abstract

Published

2023

41. Genetic manipulation of protein phosphatase 2A affects multiple agronomic traits and physiological parameters in potato (Solanum tuberosum).

Author

Muñiz García, María N., Baroli, Irene, Cortelezzi, Juan I., Zubillaga, Martina, and Capiati, Daniela A.

Subjects

*POTATOES, *PHOSPHOPROTEIN phosphatases, *ABSCISIC acid, *TUBERS, *FOLIAGE plants

Abstract

In this study, agronomic and functional characteristics of potato (Solanum tuberosum) plants constitutively overexpressing the protein phosphatase 2A (PP2A) catalytic subunit StPP2Ac2b (StPP2Ac2b-OE) were evaluated. StPP2Ac2b-OE plants display reduced vegetative growth, tuber yield and tuber weight under well-watered and drought conditions. Leaves of StPP2Ac2b-OE plants show an increased rate of water loss, associated with an impaired ability to close stomata in response to abscisic acid. StPP2Ac2b-OE lines exhibit larger stomatal size and reduced stomatal density. These altered stomatal characteristics might be responsible for the impaired stomatal closure and the elevated transpiration rates, ultimately leading to increased sensitivity to water-deficit stress and greater yield loss under drought conditions. Overexpression of StPP2Ac2b accelerates senescence in response to water-deficit stress, which could also contribute to the increased sensitivity to drought. Actively photosynthesising leaves of StPP2Ac2b-OE plants exhibit elevated levels of carbohydrates and a down-regulation of the sucrose transporter StSWEET11 , suggesting a reduced sucrose export from leaves to developing tubers. This effect, combined with the hindered vegetative development, may contribute to the reduced tuber weight and yield in StPP2Ac2b-OE plants. These findings offer novel insights into the physiological functions of PP2A in potato plants and provide valuable information for enhancing potato productivity by modulating the expression of StPP2Ac2b. This study provides novel insights into the physiological functions of protein phosphatase 2A in potato (Solanum tuberosum) plants. The results obtained reveal that the catalytic subunit StPP2Ac2b is involved in stomatal development, senescence induced by water-deficit stress and sucrose export from leaves. Manipulating the expression of StPP2Ac2b has significant effects on these physiological processes, ultimately impacting on important agronomic traits. This work presents valuable information for improving potato productivity by modulating the expression of StPP2Ac2b. [ABSTRACT FROM AUTHOR]

Published

2023

42. Circular RNA CCT3 is a unique molecular marker in bladder cancer.

Author

Luo, Lin, Xie, Qingzhi, Wu, Yunchou, Li, Ping, Qin, FuQiang, Liao, Dunming, and Wang, KangNing

Subjects

*CIRCULAR RNA, *BLADDER cancer, *TUMOR markers, *CARCINOGENS, *SURVIVAL rate

Abstract

This study surveyed circular RNA CCT3 in bladder cancer (BCa). We recruited 85 BCa patients and 40 normal controls (Normal) and collected clinical specimens for analysis. circRNA CCT3 expression was analyzed by RT-qPCR, diagnostic accuracy was calculated by ROC curves, and survival outcomes were evaluated by survival curves. CircRNA CCT3 was overexpressed or knocked down in cells, thereafter to observe the changes in cell malignant phenotypes. The downstream molecules of circRNA CCT3 were detected. Our data suggest that circRNA CCT3 was upregulated in human BCa and was associated with poor survival outcomes of BCa patients. In cell experiments, overexpressing circRNA CCT3 promoted BCa cell malignancy, whereas silencing circRNA CCT3 did the opposite. In addition, circRNA CCT3 modulated PP2A expression by miR-135a-5p. This study demonstrates that circRNA CCT3 is a diagnostic and prognostic biomarker in BCa patients and is a tumor promoter in BCa. [ABSTRACT FROM AUTHOR]

Published

2023

43. Invivo anti-cancer activity of 10-methyl-aplog-1, a simplified analog of aplysiatoxin, and its possible signaling pathway associated with G1 arrest.

Author

Hanaki, Yusuke, Shikata, Yuki, Kikumori, Masayuki, Okamura, Mutsumi, Dan, Shingo, Imoto, Masaya, and Irie, Kazuhiro

Subjects

*ANTINEOPLASTIC agents, *CELLULAR signal transduction, *PHORBOL esters, *CELL cycle, *PROTEIN kinase C, *CELL lines

Abstract

Naturally occurring protein kinase C (PKC) activators such as phorbol esters, teleocidins, and aplysiatoxins, have the potential to become anti-cancer agents, since they are anti-proliferative against specific cancer cell lines in vitro. However, their potent tumor-promoting and proinflammatory activities have hampered their clinical uses. Recently, we developed 10-methyl-aplog-1 (1), a simplified analog of tumor-promoting debromoaplysiatoxin (DAT), which retained anti-proliferative activity comparable to DAT, but induced neither tumorigenesis nor inflammation on mouse skin. Our previous study suggested that PKCα and δ were involved in the cell line-selective anti-proliferative activity of 1 , but the downstream signaling of PKC isozymes remained unknown. In this study, we confirmed that 1 inhibited the growth of three aplog-sensitive cancer cell lines (NCI–H460, HCC-2998, and HBC-4) without severe side effects in mice xenograft models. In addition, in vitro analysis using A549, one of the aplog-sensitive cell lines in vitro , revealed that PKCα induced PP2A-mediated attenuation of the Akt/S6 signaling axis. Since S6 inhibition in A549 was reported to result in G1 arrest, this pathway could be involved in the PKCα-dependent anti-proliferative activity of 1. • 10-Methyl-aplog-1 showed anti-cancer activity in vivo against NCI–H460, HCC2988, and HBC-4 cancer cell lines. • 10-Methyl-aplog-1 induced cell cycle arrest in G1 phase via PKCα activation in A549 cells. • PKCα induced PP2A-mediated attenuation of Akt/S6 signaling axis in A549 cells. • The crosstalk between PKC and Akt could be a factor that determines sensitivity to PKC ligands. [ABSTRACT FROM AUTHOR]

Published

2023

44. The B56α subunit of PP2A is necessary for mesenchymal stem cell commitment to adipocyte

Author

Hanse, Eric A, Pan, Min, Liu, Wenzhu, Yang, Ying, Gabra, Mari B Ishak, Tran, Thai Q, Lowman, Xazmin H, Ruiz, Bryan, Wang, Qiong A, and Kong, Mei

Subjects

Stem Cell Research, Regenerative Medicine, Stem Cell Research - Nonembryonic - Non-Human, 2.1 Biological and endogenous factors, Underpinning research, Aetiology, 1.1 Normal biological development and functioning, Generic health relevance, Adipocytes, Adipogenesis, Animals, Cell Differentiation, Mesenchymal Stem Cells, Mice, Phosphorylation, Protein Phosphatase 2, adipocyte, B56 alpha, PP2A, PPAR gamma, Wnt, B56α, PPARγ, Biochemistry and Cell Biology, Developmental Biology

Abstract

Adipose tissue plays a major role in maintaining organismal metabolic equilibrium. Control over the fate decision from mesenchymal stem cells (MSCs) to adipocyte differentiation involves coordinated command of phosphorylation. Protein phosphatase 2A plays an important role in Wnt pathway and adipocyte development, yet how PP2A complexes actively respond to adipocyte differentiation signals and acquire specificity in the face of the promiscuous activity of its catalytic subunit remains unknown. Here, we report the PP2A phosphatase B subunit B56α is specifically induced during adipocyte differentiation and mediates PP2A to dephosphorylate GSK3β, thereby blocking Wnt activity and driving adipocyte differentiation. Using an inducible B56α knock-out mouse, we further demonstrate that B56α is essential for gonadal adipose tissue development in vivo and required for the fate decision of adipocytes over osteoblasts. Moreover, we show B56α expression is driven by the adipocyte transcription factor PPARγ thereby establishing a novel link between PPARγ signaling and Wnt blockade. Overall, our results reveal B56α is a necessary part of the machinery dictating the transition from pre-adipocyte to mature adipocyte and provide fundamental insights into how PP2A complex specifically and actively regulates unique signaling pathway in biology.

Published

2021

45. PAK6-mediated phosphorylation of PPP2R2C regulates LRRK2-PP2A complex formation

Author

Lucia Iannotta, Marco Emanuele, Giulia Favetta, Giulia Tombesi, Laurine Vandewynckel, Antonio Jesús Lara Ordóñez, Jean-Michel Saliou, Matthieu Drouyer, William Sibran, Laura Civiero, R. Jeremy Nichols, Panagiotis S. Athanasopoulos, Arjan Kortholt, Marie-Christine Chartier-Harlin, Elisa Greggio, and Jean-Marc Taymans

Subjects

LRRK2, Parkinson’s disease, dephosphorylation, PP2A, PPP2R2C, Pak6, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Mutations in leucine-rich repeat kinase 2 (LRRK2) are a common cause of inherited and sporadic Parkinson’s disease (PD) and previous work suggests that dephosphorylation of LRRK2 at a cluster of heterologous phosphosites is associated to disease. We have previously reported subunits of the PP1 and PP2A classes of phosphatases as well as the PAK6 kinase as regulators of LRRK2 dephosphorylation. We therefore hypothesized that PAK6 may have a functional link with LRRK2’s phosphatases. To investigate this, we used PhosTag gel electrophoresis with purified proteins and found that PAK6 phosphorylates the PP2A regulatory subunit PPP2R2C at position S381. While S381 phosphorylation did not affect PP2A holoenzyme formation, a S381A phosphodead PPP2R2C showed impaired binding to LRRK2. Also, PAK6 kinase activity changed PPP2R2C subcellular localization in a S381 phosphorylation-dependent manner. Finally, PAK6-mediated dephosphorylation of LRRK2 was unaffected by phosphorylation of PPP2R2C at S381, suggesting that the previously reported mechanism whereby PAK6-mediated phosphorylation of 14-3-3 proteins promotes 14-3-3-LRRK2 complex dissociation and consequent exposure of LRRK2 phosphosites for dephosphorylation is dominant. Taken together, we conclude that PAK6-mediated phosphorylation of PPP2R2C influences the recruitment of PPP2R2C to the LRRK2 complex and PPP2R2C subcellular localization, pointing to an additional mechanism in the fine-tuning of LRRK2 phosphorylation.

Published

2023

46. The impact of SETBP1 mutations in neurological diseases and cancer.

Author

Kohyanagi, Naoki and Ohama, Takashi

Subjects

*NEUROLOGICAL disorders, *GENETIC mutation, *MYELODYSPLASTIC syndromes, *DISABILITIES, *CANCER prognosis

Abstract

SE translocation (SET) is a cancer‐promoting factor whose expression is upregulated in many cancers. High SET expression positively correlates with a poor cancer prognosis. SETBP1 (SET‐binding protein 1/SEB/MRD29), identified as SET‐binding protein, is the causative gene of Schinzel–Giedion syndrome, which is characterized by severe intellectual disability and a distorted facial appearance. Mutations in these genetic regions are also observed in some blood cancers, such as myelodysplastic syndromes, and are associated with a poor prognosis. However, the physiological role of SETBP1 and the molecular mechanisms by which the mutations lead to disease progression have not yet been fully elucidated. In this review, we will describe the current epidemiological data on SETBP1 mutations and shed light on the current knowledge about the SET‐dependent and ‐independent functions of SETBP1. [ABSTRACT FROM AUTHOR]

Published

2023

47. TaTIP41 and TaTAP46 positively regulate drought tolerance in wheat by inhibiting PP2A activity.

Author

Ma, Jianhui, Geng, Yuke, Liu, Hong, Zhang, Mengqi, Liu, Shujuan, Hao, Chenyang, Hou, Jian, Zhang, Youfu, Zhang, Daijing, Zhang, Weijun, Zhang, Xueyong, and Li, Tian

Subjects

*DROUGHT tolerance, *RNA interference, *ABSCISIC acid, *WHEAT, *PHOSPHOPROTEIN phosphatases, *MOLECULAR cloning

Abstract

Drought is a major environmental stress limiting global wheat (Triticum aestivum) production. Exploring drought tolerance genes is important for improving drought adaptation in this crop. Here, we cloned and characterized TaTIP41, a novel drought tolerance gene in wheat. TaTIP41 is a putative conserved component of target of rapamycin (TOR) signaling, and the TaTIP41 homoeologs were expressed in response to drought stress and abscisic acid (ABA). The overexpression of TaTIP41 enhanced drought tolerance and the ABA response, including ABA‐induced stomatal closure, while its downregulation using RNA interference (RNAi) had the opposite effect. Furthermore, TaTIP41 physically interacted with TaTAP46, another conserved component of TOR signaling. Like TaTIP41, TaTAP46 positively regulated drought tolerance. Furthermore, TaTIP41 and TaTAP46 interacted with type‐2A protein phosphatase (PP2A) catalytic subunits, such as TaPP2A‐2, and inhibited their enzymatic activities. Silencing TaPP2A‐2 improved drought tolerance in wheat. Together, our findings provide new insights into the roles of TaTIP41 and TaTAP46 in the drought tolerance and ABA response in wheat, and their potential application in improving wheat environmental adaptability. [ABSTRACT FROM AUTHOR]

Published

2023

48. Cancer progression by the okadaic acid class of tumor promoters and endogenous protein inhibitors of PP2A, SET and CIP2A.

Author

Fujiki, Hirota, Sueoka, Eisaburo, Watanabe, Tatsuro, Komori, Atsumasa, and Suganuma, Masami

Subjects

*ERLOTINIB, *CARCINOGENS, *PROSTATE cancer, *CANCER invasiveness, *EPIDERMAL growth factor receptors, *CHRONIC myeloid leukemia

Abstract

Purpose: Okadaic acid class of tumor promoters are transformed into endogenous protein inhibitors of PP2A, SET, and CIP2A in human cancers. This indicates that inhibition of PP2A activity is a common mechanism of cancer progression in humans. It is important to study the roles of SET and CIP2A vis-à-vis their clinical significance on the basis of new information gathered from a search of PubMed. Results and discussion: The first part of this review introduces the carcinogenic roles of TNF-α and IL-1, which are induced by the okadaic acid class of compounds. The second part describes unique features of SET and CIP2A in cancer progression for several types of human cancer: (1) SET-expressing circulating tumor cells (SET-CTCs) in breast cancer, (2) knockdown of CIP2A and increased PP2A activity in chronic myeloid leukemia, (3) CIP2A and epidermal growth factor receptor (EGFR) activity in erlotinib sensitive- and resistant-non-small cell lung cancer, (4) SET antagonist EMQA plus radiation therapy against hepatocellular carcinoma, (5) PP2A inactivation as a common event in colorectal cancer, (6) prostate cancer susceptibility variants, homeobox transcription factor (HOXB13 T) and CIP2A T, and (7) SET inhibitor OP449 for pre-clinical investigation of pancreatic cancer. In the Discussion, the binding complex of SET is briefly introduced, and overexpression of SET and CIP2A proteins is discussed in relation to age-associated chronic inflammation (inflammaging). Conclusion: This review establishes the concept that inhibition of PP2A activity is a common mechanism of human cancer progression and activation of PP2A activity leads to effective anticancer therapy. [ABSTRACT FROM AUTHOR]

Published

2023

49. Lithium inhibits GSK-3 through disruption of Striatal β-Arrestin, PP2A, and Akt Signaling.

Author

Oladipo, G. O., Oladipo, M. C., Olusanya, T., Ibukun, O. E., and Akinola, O. A.

Subjects

*LITHIUM, *ARRESTINS, *NEURODEGENERATION, *DISEASE progression, *DISEASE remission

Abstract

β-Arrestin, PP2A, and Akt form a signaling complex that affects the activation of GSK-3. GSK-3 affects the pathway leading to neurodegenerative diseases. Lithium is a known mood stabilizer which exhibits a direct or indirect inhibition of GSK-3. GSK-3 is the link between neurodegeneration and the mitigating potential of lithium via the direct and indirect inhibition of this enzyme. This review reveals the mechanisms associated with lithium neuroprotection and the synergies between β-arrestin, PP2A, AKT, and GSK-3, the limiting effects on the progression of neurodegeneration. [ABSTRACT FROM AUTHOR]

Published

2023

50. PP2A‐based triple‐strike therapy overcomes mitochondrial apoptosis resistance in brain cancer cells.

Author

Denisova, Oxana V., Merisaari, Joni, Huhtaniemi, Riikka, Qiao, Xi, Yetukuri, Laxman, Jumppanen, Mikael, Kaur, Amanpreet, Pääkkönen, Mirva, von Schantz‐Fant, Сarina, Ohlmeyer, Michael, Wennerberg, Krister, Kauko, Otto, Koch, Raphael, Aittokallio, Tero, Taipale, Mikko, and Westermarck, Jukka

Abstract

Mitochondrial glycolysis and hyperactivity of the phosphatidylinositol 3‐kinase–protein kinase B (AKT) pathway are hallmarks of malignant brain tumors. However, kinase inhibitors targeting AKT (AKTi) or the glycolysis master regulator pyruvate dehydrogenase kinase (PDKi) have failed to provide clinical benefits for brain tumor patients. Here, we demonstrate that heterogeneous glioblastoma (GB) and medulloblastoma (MB) cell lines display only cytostatic responses to combined AKT and PDK targeting. Biochemically, the combined AKT and PDK inhibition resulted in the shutdown of both target pathways and priming to mitochondrial apoptosis but failed to induce apoptosis. In contrast, all tested brain tumor cell models were sensitive to a triplet therapy, in which AKT and PDK inhibition was combined with the pharmacological reactivation of protein phosphatase 2A (PP2A) by NZ‐8‐061 (also known as DT‐061), DBK‐1154, and DBK‐1160. We also provide proof‐of‐principle evidence for in vivo efficacy in the intracranial GB and MB models by the brain‐penetrant triplet therapy (AKTi + PDKi + PP2A reactivator). Mechanistically, PP2A reactivation converted the cytostatic AKTi + PDKi response to cytotoxic apoptosis, through PP2A‐elicited shutdown of compensatory mitochondrial oxidative phosphorylation and by increased proton leakage. These results encourage the development of triple‐strike strategies targeting mitochondrial metabolism to overcome therapy tolerance in brain tumors. [ABSTRACT FROM AUTHOR]

Published

2023