Your search keyword '"PROTEIN phosphatase inhibitors"' showing total 247 results

51. The therapeutic effects of SET/I2PP2A inhibitors on canine melanoma.

Author

Shuhei ENJOJI, Ryotaro YABE, Nobuyuki FUJIWARA, Shunya TSUJI, VITEK, Michael P., Takuya MIZUNO, Takayuki NAKAGAWA, Tatsuya USUI, Takashi OHAMA, and Koichi SATO

Subjects

MELANOMA treatment, PROTEIN phosphatase inhibitors, CANCER in dogs

Abstract

Canine melanoma is one of the most important diseases in small animal medicine. Protein phosphatase 2A (PP2A), a well conserved serine/threonine phosphatase, plays a critical role as a tumor suppressor. SET/I2PP2A is an endogenous inhibitor for PP2A, which directly binds to PP2A and suppresses its phosphatase activity. Elevated SET protein levels have been reported to exacerbate human tumor progression. The role of SET in canine melanoma, however, has not been understood. Here, we investigated the potential therapeutic role for SET inhibitors in canine melanoma. The expression of SET protein was observed in 6 canine melanoma cell lines. We used CMeC-1 cells (primary origin) and CMeC-2 cells (metastatic origin) to generate cell lines stably expressing SET-targeting shRNAs. Knockdown of SET expression in CMeC-2, but not in CMeC-1, leads to decreased cell proliferation, invasion and colony formation. Phosphorylation level of p70 S6 kinase was decreased by SET knockdown in CMeC-2, suggesting the involvement of mTOR (mammalian target of rapamycin)/p70 S6 kinase signaling. The SET inhibitors, OP449 and FTY720, more effectively killed CMeC-2 than CMeC-1. We observed PP2A activation in CMeC-2 treated with OP449 and FTY720. These results demonstrated the potential therapeutic application of SET inhibitors for canine melanoma. [ABSTRACT FROM AUTHOR]

Published

2015

52. Protective Effect of Tat PTD-Hsp27 Fusion Protein on Tau Hyperphosphorylation Induced by Okadaic Acid in the Human Neuroblastoma Cell Line SH-SY5Y.

Author

Choi, Sunghyun, Oh, Jae, Kim, Hyeseon, Nam, So, Shin, Jeehae, and Park, Jong-Sang

Subjects

*ALZHEIMER'S disease treatment, *TAU proteins, *HEAT shock proteins, *PROTEIN phosphatase inhibitors, *PHOSPHORYLATION, *NEUROBLASTOMA, *CHIMERIC proteins, *CELL lines

Abstract

Alzheimer's disease (AD) is an age-related disorder that causes a loss of brain function. Hyperphosphorylation of tau and the subsequent formation of intracellular neurofibrillary tangles (NFTs) are implicated in the pathogenesis of AD. Hyperphosphorylated tau accumulates into insoluble paired helical filaments that aggregate into NFTs; therefore, regulation of tau phosphorylation represents an important treatment approach for AD. Heat shock protein 27 (Hsp27) plays a specific role in human neurodegenerative diseases; however, few studies have examined its therapeutic effect. In this study, we induced tau hyperphosphorylation using okadaic acid, which is a protein phosphatase inhibitor, and generated a fusion protein of Hsp27 and the protein transduction domain of the HIV Tat protein (Tat-Hsp27) to enhance the delivery of Hsp27. We treated Tat-Hsp27 to SH-SY5Y neuroblastoma cells for 2 h; the transduction level was proportional to the Tat-hsp27 concentration. Additionally, Tat-Hsp27 reduced the level of hyperphosphorylated tau and protected cells from apoptotic cell death caused by abnormal tau aggregates. These results reveal that Hsp27 represents a valuable protein therapeutic for AD. [ABSTRACT FROM AUTHOR]

Published

2015

53. Concise synthesis of the C15–C38 fragment of okadaic acid, a specific inhibitor of protein phosphatases 1 and 2A.

Author

Fuwa, Haruhiko, Sakamoto, Keita, Muto, Takashi, and Sasaki, Makoto

Subjects

*CHEMICAL synthesis, *CHEMICAL inhibitors, *PROTEIN phosphatase inhibitors, *NATURAL products, *POLYETHERS

Abstract

A marine polyether natural product okadaic acid is known to be a potent and specific inhibitor of protein phosphatases 1 and 2A. Herein, concise synthesis of the C15–C38 fragment of okadaic acid is reported. We investigated two different strategies for the construction of two spiroacetal substructures found in the target compound. The first strategy involved Suzuki–Miyaura coupling for the synthesis of endocyclic enol ethers and subsequent spiroacetalization. The second strategy exploited Suzuki–Miyaura coupling for the synthesis of exo -olefins as the precursor of spiroacetals. An alkynylaluminum–anomeric sulfone coupling effectively assembled the key spiroacetal substructures and completed the target compound. [ABSTRACT FROM AUTHOR]

Published

2015

54. Characterization and Functional Analysis of Pyrabactin Resistance-Like Abscisic Acid Receptor Family in Rice.

Author

Tian, Xiaojie, Wang, Zhenyu, Li, Xiufeng, Lv, Tianxiao, Liu, Huazhao, Wang, Lizhi, Niu, Hongbin, and Bu, Qingyun

Subjects

*RICE, *PLANTING, *ABSCISIC acid, *GRAIN growth, *REVERSE transcriptase polymerase chain reaction, *PROTEIN phosphatase inhibitors, *GERMINATION

Abstract

Background: Abscisic acid (ABA) plays crucial roles in regulating plant growth and development, especially in responding to abiotic stress. The pyrabactin resistance-like (PYL) abscisic acid receptor family has been identified and widely characterized in Arabidopsis. However, PYL families in rice were largely unknown. In the present study, 10 out of 13 PYL orthologs in rice ( OsPYL) were isolated and investigated. Results: Quantitative reverse transcription-polymerase chain reaction (qRT-PCR) analysis showed that expression of OsPYL genes is tissue-specific and display differential response to ABA treatment, implying their functional diversity. The interaction between 10 OsPYL members and 5 protein phosphatase 2C in rice (OsPP2C) members was investigated in yeast two-hybrid and tobacco transient expression assays, and an overall interaction map was generated, which was suggestive of the diversity and complexity of ABA-sensing signaling in rice. To study the biological function of OsPYLs, two OsPYL genes ( OsPYL3 and OsPYL9) were overexpressed in rice. Phenotypic analysis of OsPYL3 and OsPYL9 transgenic rice showed that OsPYLs positively regulated the ABA response during the seed germination. More importantly, the overexpression of OsPYL3 and OsPYL9 substantially improved drought and cold stress tolerance in rice. Conclusion: Taken together, we comprehensively uncovered the properties of OsPYLs, which may be good candidates for the improvement of abiotic stress tolerance in rice. [ABSTRACT FROM AUTHOR]

Published

2015

55. Inhibition of protein phosphatase 5 (PP5) suppresses survival and growth of colorectal cancer cells.

Author

Wang, Jianwei, Zhu, Jinhui, Dong, Mingjun, Yu, Hua, Dai, Xiaoyu, and Li, Keqiang

Subjects

*COLON cancer treatment, *TUMOR suppressor genes, *CANCER cell growth, *PROTEIN phosphatase inhibitors, *CELLULAR signal transduction, *DNA damage

Abstract

Protein phosphatase 5 (PP5) is a unique member of the protein phosphatases family that functions in multiple signaling pathways involved in DNA damage, cell cycle control, cell growth, and apoptosis. Recent evidence indicated that PP5 may play a role in cancer progression. In this study, we aimed to examine the biological effect of PP5 on cell growth and apoptosis in human colorectal cancer (CRC). We first knocked down PP5 expression in RKO cells via a short hairpin RNA containing lentivirus system. Then, methylthiazoletetrazolium assay, colony formation assay, and flow cytometry analysis were performed. The proliferation and colony formation ability of RKO cells were remarkably suppressed in PP5-silenced groups, as compared with control groups. Moreover, downregulation of PP5 resulted in a significant G0/G1 phase cell cycle arrest and an induction of apoptosis. In all, these results demonstrated the importance of PP5 in CRC cell growth, and it might be used as a potential therapeutic target for the treatment of CRC. [ABSTRACT FROM AUTHOR]

Published

2015

56. Up-regulation of micro- RNA765 in human failing hearts is associated with post-transcriptional regulation of protein phosphatase inhibitor-1 and depressed contractility.

Author

Cai, Wen ‐ Feng, Liu, Guan ‐ Sheng, Lam, Chi Keung, Florea, Stela, Qian, Jiang, Zhao, Wen, Pritchard, Tracy, Haghighi, Kobra, Lebeche, Djamel, Lu, Long Jason, Deng, Jingyuan, Fan, Guo ‐ Chang, Hajjar, Roger J., and Kranias, Evangelia G.

Subjects

*HEART failure patients, *HEART failure treatment, *GENETIC regulation, *MICRORNA, *PROTEIN phosphatase inhibitors, *MESSENGER RNA, *CONTRACTILITY (Biology)

Abstract

Aims Impaired sarcoplasmic reticulum ( SR) Ca2+ cycling and depressed contractility, a hallmark of human and experimental heart failure, has been partially attributed to increased protein phosphatase 1 ( PP-1) activity, associated with down-regulation of its endogenous inhibitor-1. The levels and activity of inhibitor-1 are reduced in failing hearts, contributing to dephosphorylation and inactivation of key calcium cycling proteins. Therefore, we investigated the mechanisms that mediate decreases in inhibitor-1 by post-transcriptional modification. Methods and Results Bioinformatics revealed that 17 human microRNAs may serve as modulators of inhibitor-1. However, real-time PCR analysis identified only one of these microRNAs, miR-765, as being increased in human failing hearts concomitant with decreased inhibitor-1 levels. Expression of miR-765 in HEK293 cells or mouse ventricular myocytes confirmed suppression of inhibitor-1 levels through binding of this miR-765 to the 3'-untranslated region of inhibitor-1 mRNA. To determine the functional significance of miR-765 in Ca2+ cycling, pri- miR-765 as well as a non-translated nucleotide sequence ( miR-Ctrl) were expressed in adult mouse ventricular myocytes. The inhibitor-1 expression levels were decreased, accompanied by enhanced PP-1 activity in the miR-765 cardiomyocytes, and these reflected depressed contractile mechanics and Ca2+ transients, compared with the miR-Ctrl group. The depressive effects were associated with decreases in the phosphorylation of phospholamban and SR Ca2+ load. These miR-765 negative inotropic effects were abrogated in inhibitor-1-deficient cardiomyocytes, suggesting its apparent specificity for inhibitor-1. Conclusions miR-765 levels are increased in human failing hearts. Such increases may contribute to depressed cardiac function through reduced inhibitor-1 expression and enhanced PP-1 activity, associated with reduced SR Ca2+ load. [ABSTRACT FROM AUTHOR]

Published

2015

57. Integrative Transcriptome Profiling of Cognitive Aging and Its Preservation through Ser/Thr Protein Phosphatase Regulation.

Author

Park, C. Sehwan, Valomon, Amandine, and Welzl, Hans

Subjects

*AGING, *MESSENGER RNA, *COGNITION disorders, *PROTEIN phosphatase inhibitors, *SERINE/THREONINE kinase regulation

Abstract

Environmental enrichment has been reported to delay or restore age-related cognitive deficits, however, a mechanism to account for the cause and progression of normal cognitive decline and its preservation by environmental enrichment is lacking. Using genome-wide SAGE-Seq, we provide a global assessment of differentially expressed genes altered with age and environmental enrichment in the hippocampus. Qualitative and quantitative proteomics in naïve young and aged mice was used to further identify phosphorylated proteins differentially expressed with age. We found that increased expression of endogenous protein phosphatase-1 inhibitors in aged mice may be characteristic of long-term environmental enrichment and improved cognitive status. As such, hippocampus-dependent performances in spatial, recognition, and associative memories, which are sensitive to aging, were preserved by environmental enrichment and accompanied by decreased protein phosphatase activity. Age-associated phosphorylated proteins were also found to correspond to the functional categories of age-associated genes identified through transcriptome analysis. Together, this study provides a comprehensive map of the transcriptome and proteome in the aging brain, and elucidates endogenous protein phosphatase-1 inhibition as a potential means through which environmental enrichment may ameliorate age-related cognitive deficits. [ABSTRACT FROM AUTHOR]

Published

2015

58. Cellular localization of CIP2A determines its prognostic impact in superficial spreading and nodular melanoma.

Author

Flørenes, Vivi Ann, Emilsen, Elisabeth, Dong, Hiep Phuc, Førsund, Mette, Holm, Ruth, and Slipicevic, Ana

Subjects

*PROTEIN phosphatase inhibitors, *MELANOMA prognosis, *APOPTOSIS, *NODULAR disease, *CELL lines, *ONCOGENES

Abstract

Cancerous inhibitor of protein phosphatase 2A (CIP2A) is an important oncogene contributing to cancer progression partially by regulating cMYC and AKT. We examined CIP2A expression in cutaneous melanomas, its association with clinicopathological parameters and mapped molecular mechanisms regulated by CIP2A in vitro. CIP2A expression was analyzed by immunohistochemistry in 17 nevi, 132 primary melanomas and 49 metastases. Effects of siRNA-mediated down-regulation on proliferation, apoptosis and signaling pathways were assessed in melanoma cell lines. In superficial spreading melanomas (SSM), high nuclear CIP2A expression was associated with poor overall survival (OS) (P = 0.0018). Surprisingly, high cytoplasmic expression was related to improved relapse-free (P = 0.031) and OS (P = 0.014) in nodular melanomas (NM). In vitro experiments revealed that CIP2A can regulate proliferation and/or apoptosis partially through the PI3K/AKT pathway but also independently. In summary, CIP2A could represent a potential therapeutic target in SSM. However, in NM cytoplasmic CIP2A is associated with improved prognosis indicating that CIP2A has distinct, complex functions dependent on the molecular context and histological subtype. As seen in other cancer types, CIP2A can influence cMYC and AKT, but our data also suggest that in melanoma it has additional targets which need to be identified. [ABSTRACT FROM AUTHOR]

Published

2015

59. DUSP3 Genetic Deletion Confers M2-like Macrophage-Dependent Tolerance to Septic Shock.

Author

Singh, Pratibha, Dejager, Lien, Amand, Mathieu, Theatre, Emilie, Vandereyken, Maud, Zurashvili, Tinatin, Singh, Maneesh, Mack, Matthias, Timmermans, Steven, Musumeci, Lucia, Dejardin, Emmanuel, Mustelin, Tomas, Van Ginderachter, Jo A., Moutschen, Michel, Oury, Cécile, Libert, Claude, and Rahmouni, Souad

Subjects

*DUAL specificity phosphatase 1, *PROTEIN phosphatase inhibitors, *IMMUNOLOGICAL tolerance, *ANIMAL models in research, *SEPTIC shock, *MONOCYTES, *GENE delivery techniques, *LABORATORY mice

Abstract

DUSP3 is a small dual-specificitv protein phosphatase with an unknown physiological function. We report that DUSP3 is strongly expressed in human and mouse monocytes and macrophages, and that its deficiency in mice promotes tolerance to LPS-induced endotoxin shock and to polymicrobial septic shock after cecal ligation and puncture. By using adoptive transfer experiments, we demonstrate that resistance to endotoxin is macrophage dependent and transferable, and that this protection is associated with a striking increase of M2-like macrophages in DUSP3-/- mice in both the LPS and cecal ligation and puncture models. We show that the altered response of DUSP3-/- mice to sepsis is reflected in decreased TNF production and impaired ERK1/2 activation. Our results demonstrate that DUSP3 plays a key and nonredundant role as a regulator of innate immune responses by mechanisms involving the control of ERK1/2 activation, TNF secretion, and macrophage polarization. [ABSTRACT FROM AUTHOR]

Published

2015

60. Protein tyrosine phosphatase 1B (PTP1B) is involved in the defective erythropoietic function of carbamylated erythropoietin.

Author

Chamorro, María Eugenia, Maltaneri, Romina Eugenia, Vittori, Daniela Cecilia, and Nesse, Alcira Beatriz

Subjects

*PROTEIN-tyrosine kinases, *PROTEIN phosphatase inhibitors, *ERYTHROPOIETIC failure, *ERYTHROPOIETIN, *CELL proliferation, *JANUS kinases

Published

2015

61. Inhibition of protein phosphatase-1 and -2A decreases the chemosensitivity of leukemic cells to chemotherapeutic drugs.

Author

Dedinszki, Dóra, Kiss, Andrea, Márkász, László, Márton, Adrienn, Tóth, Emese, Székely, László, and Erdődi, Ferenc

Subjects

*PROTEIN phosphatase inhibitors, *CANCER chemotherapy, *PHOSPHORYLATION, *CANCER cell culture, *DAUNOMYCIN, *PROTEIN kinase B, *SMALL interfering RNA

Abstract

The phosphorylation of key proteins balanced by protein kinases and phosphatases are implicated in the regulation of cell cycle and apoptosis of malignant cells and influences anticancer drug actions. The efficacy of daunorubicin (DNR) in suppression of leukemic cell survival was investigated in the presence of tautomycin (TM) and calyculin A (CLA), specific membrane permeable inhibitors of protein phosphatase-1 (PP1) and -2A (PP2A), respectively. CLA (50 nM) or TM (1 μM) suppressed viability of THP-1 and KG-1 myeloid leukemia cell lines to moderate extents; however, they significantly increased survival upon DNR-induced cell death. CLA increased the phosphorylation level of Erk1/2 and PKB/Akt kinases, the retinoblastoma protein (pRb), decreased caspase-3 activation by DNR and increased the phosphorylation level of the inhibitory sites (Thr696 and Thr853) in the myosin phosphatase (MP) target subunit (MYPT1) as well as in a 25 kDa kinase-enhanced phosphatase inhibitor (KEPI)-like protein. TM induced enhanced phosphorylation of pRb only, suggesting that this event may be a common factor upon CLA-induced PP2A and TM-induced PP1 inhibitory influences on cell survival. Silencing PP1 by siRNA in HeLa cells, or overexpression of Flag-KEPI in MCF-7 cells coupled with inducing its phosphorylation by PMA or CLA, resulted in increased phosphorylation of pRb. Our results indicate that PP1 directly dephosphorylates pRb, while PP2A might have an indirect influence via mediating the phosphorylation level of PP1 inhibitory proteins. These data imply the importance of PP1 inhibitory proteins in controlling the phosphorylation state of key proteins and regulating drug sensitivity and apoptosis in leukemic cells. [ABSTRACT FROM AUTHOR]

Published

2015

62. Enhanced anticancer activity of a protein phosphatase 2A inhibitor on chemotherapy and radiation in head and neck squamous cell carcinoma.

Author

Zhu, Dong-wang, Yuan, Yong-xiang, Qiao, Jin-ke, Yu, Cong, Yang, Xi, Wang, Li-zhen, Zhang, Zhi-yuan, and Zhong, Lai-ping

Subjects

*HEAD & neck cancer treatment, *ANTINEOPLASTIC agents, *PROTEIN phosphatase inhibitors, *CANCER chemotherapy, *CANCER radiotherapy, *SQUAMOUS cell carcinoma

Abstract

The aim of this study is to eliminate more cancer cells by promoting them from quiescence into cell cycle or by changing their molecular events, leading them to be sensitive to radiation or chemotherapy. Protein phosphatase 2A plays an important role in many cellular functions and regulates various biological processes. It is unclear that LB1, which is an inhibitor of protein phosphatase 2A, has enhanced anticancer activity on chemotherapy (cisplatin and 5-fluorourcil) and radiation in head and neck squamous cell carcinoma (HNSCC). Herein, we performed both in vitro and in vivo studies to determine the anticancer activity of LB1 on chemotherapy and radiation in HNSCC, with detection of p53 expression, AKT and MDM2 phosphorylation. In vitro studies indicated that, LB1 could significantly enhance the cytotoxicity of cisplatin, 5-fluorourcil, and radiation; LB1 could also significantly enhance the treatment effect of cisplatin in nude mice. The anticancer activity of LB1 was mediated by increased AKT phosphorylation and decreased p53 expression with increased MDM2 phosphorylation, especially when combined with cisplatin. Our data suggest a strategy of improving treatment effect through the enhanced anticancer activity of LB1 on cisplatin-based chemotherapy and radiation in HNSCC. [ABSTRACT FROM AUTHOR]

Published

2015

63. CIP2A cooperates with H-Ras to promote epithelial–mesenchymal transition in cervical-cancer progression.

Author

Wu, Yi, Gu, Ting-Ting, and Zheng, Peng-Sheng

Subjects

*PROTEIN phosphatase inhibitors, *PROMOTERS (Genetics), *CERVICAL cancer, *CANCER invasiveness, *PHOSPHOPROTEIN phosphatases, *GENETICS

Abstract

The oncoprotein Cancerous Inhibitor of PP2A (CIP2A) has been reported to interact with Protein phosphatase 2 (PP2A) to stabilize c-Myc and prevent its degradation, and high expression levels of CIP2A have been proved to be related to poor clinical outcomes in multiple cancers. Here, we not only proved that the expression of CIP2A is positively correlated with lymph-node metastasis and cervical-cancer progression, but also revealed a close correlation between the protein's expression and the expression levels of two core epithelial-to-mesenchymal transition (EMT) markers, Vimentin and Snail. In addition, we manipulated CIP2A expression to regulate EMT conversion and employed a pull-down assay, mass-spectrometric (MS) peptide sequencing, as well as bilateral co-immunoprecipitation to identify potentially interacting proteins in cervical-cancer cells. In this study, we proposed and successfully proved, for the first time, that CIP2A physically associates with H-Ras, which leads to the activation of the MEK/ERK signaling pathway and promotes EMT and cervical-cancer progression. Based on our observations and prior findings that CIP2A participates in c-Myc regulation, we conjecture that CIP2A may be a potentially promising molecular target for the adoptive therapy of human cancer. [ABSTRACT FROM AUTHOR]

Published

2015

64. Synthesis and biological evaluation of norcantharidin derivatives as protein phosphatase-1 inhibitors.

Author

Zhao, Jie, Guan, Xiao-Wen, Chen, Shi-Wu, and Hui, Ling

Subjects

*DRUG synthesis, *DRUG derivatives, *PROTEIN phosphatase inhibitors, *ANTINEOPLASTIC agents, *CANCER cell culture, *HELA cells

Abstract

Cantharidin and norcantharidin display anticancer activity against a broad range of tumor cell lines. In this study, we have synthesized a series of norcantharidin derivatives and evaluated their cytotoxic effects on four human tumor cell lines together with the genetically normal human diploid fibroblast line WI-38. One of our compounds (1 S ,4 R )-3-((4-(4-(4-fluorophenyl)piperazin-1-ylsulfonyl) phenyl)carbamoyl)-7-oxa-bicyclo[2.2.1]heptane-2-carboxylic acid ( 12 ) exhibited potent cytotoxic effects on the tumor cell lines A-549, HepG2, HeLa, and HCT-8, whereas it was less toxic to WI-38 cells than its parent compound, norcantharidin. In addition, this compound inhibited protein phosphatase-1 activity and microtubule formation in HeLa cells, and it also interacts with calf thymus DNA. [ABSTRACT FROM AUTHOR]

Published

2015

65. Cantharidin, a protein phosphatase inhibitor, strongly upregulates detoxification enzymes in the Arabidopsis proteome.

Author

Bajsa, Joanna, Pan, Zhiqiang, and Duke, Stephen O.

Subjects

*TERPENES, *PROTEIN phosphatase inhibitors, *ARABIDOPSIS, *PROTEOMICS, *PHYTOTOXICITY, *PHOTOSYNTHESIS, *GEL electrophoresis

Abstract

Cantharidin, a potent inhibitor of plant serine/threonine protein phosphatases (PPPs), is highly phytotoxic and dramatically affects the transcriptome in Arabidopsis . To investigate the effect of cantharidin on the Arabidopsis proteome, a combination of two-dimensional difference gel electrophoresis (2-D DIGE) and matrix-assisted laser desorption ionization time-of-flight (MALDI/TOF) mass spectrometry was employed for protein profiling. Multivariate statistical analysis identified 75 significant differential spots corresponding to 59 distinct cantharidin-responsive proteins, which were representative of different biological processes, cellular components, and molecular functions categories. The majority of identified proteins localized in the chloroplast had a significantly decreased presence, especially proteins involved in photosynthesis. Detoxification enzymes, especially glutathione- S -transferases (GSTs), were the most upregulated group (ca. 1.5- to 3.3-fold). Given that the primary role of GSTs is involved in the process of detoxification of both xenobiotic and endobiotic compounds, the induction of GSTs suggests that cantharidin promoted inhibition of PPPs may lead to defense-like responses through regulation of GST enzymes as well as other metabolic pathways. [ABSTRACT FROM AUTHOR]

Published

2015

66. Inhibition of protein phosphatase 2A sensitizes pancreatic cancer to chemotherapy by increasing drug perfusion via HIF-1α-VEGF mediated angiogenesis.

Author

Bai, Xueli, Zhi, Xiao, Zhang, Qi, Liang, Feng, Chen, Wei, Liang, Chao, Hu, Qida, Sun, Xu, Zhuang, Zhengping, and Liang, Tingbo

Subjects

*PROTEIN phosphatase inhibitors, *PANCREATIC cancer, *CANCER chemotherapy, *ANTINEOPLASTIC agents, *VASCULAR endothelial growth factors, *NEOVASCULARIZATION, *HYPOXIA-inducible factor 1

Abstract

Pancreatic cancer is a malignant disease without efficient treatment. Improved treatments are urgently needed to enhance or replace chemotherapy. Here we used a small molecular compound LB-100 to assess the effect of pharmacological inhibition of protein phosphatase 2A (PP2A) in combination with doxorubicin on the proliferation of pancreatic cancer in cell lines and a xenograft model. LB-100 moderately reduced PP2A activity and the growth of the cell lines but did not show chemosensitization in vitro. In vivo , however, LB-100 synergistically enhanced the activity of doxorubicin. This effect was associated with increased microvessel density, blood perfusion, and doxorubicin concentrations within the xenografts. Mechanically, LB-100 induced expression of hypoxia-induced factor-1α (HIF-1α) and vascular endothelial growth factor (VEGF). In an umbilical vein endothelial cell monolayer model for measuring changes in vascular permeability, increased VEGF secretion following exposure to LB-100 and doxorubicin was accompanied by increased amounts of doxorubicin penetrating the endothelial barrier. In conclusion, PP2A inhibition by LB-100 enhanced the cytotoxicity of doxorubicin in vivo but not in vitro potentially via HIF-1α-VEGF mediated angiogenesis. Combining inhibition of PP2A with chemotherapeutic regimens may enhance their effectiveness against pancreatic cancer. [ABSTRACT FROM AUTHOR]

Published

2014

67. H2O2 Inhibits ABA-Signaling Protein Phosphatase HAB1.

Author

Sridharamurthy, Madhuri, Kovach, Amanda, Zhao, Yang, Zhu, Jian-Kang, Xu, H. Eric, Swaminathan, Kunchithapadam, and Melcher, Karsten

Subjects

*CELLULAR signal transduction, *PROTEIN phosphatase inhibitors, *ABIOTIC stress, *PLANT genetics, *ABSCISIC acid

Abstract

Due to its ability to be rapidly generated and propagated over long distances, H2O2 is an important second messenger for biotic and abiotic stress signaling in plants. In response to low water potential and high salt concentrations sensed in the roots of plants, the stress hormone abscisic acid (ABA) activates NADPH oxidase to generate H2O2, which is propagated in guard cells in leaves to induce stomatal closure and prevent water loss from transpiration. Using a reconstituted system, we demonstrate that H2O2 reversibly prevents the protein phosphatase HAB1, a key component of the core ABA-signaling pathway, from inhibiting its main target in guard cells, SnRK2.6/OST1 kinase. We have identified HAB1 C186 and C274 as H2O2-sensitive thiols and demonstrate that their oxidation inhibits both HAB1 catalytic activity and its ability to physically associate with SnRK2.6 by formation of intermolecular dimers. [ABSTRACT FROM AUTHOR]

Published

2014

68. 1E7-03, a low MW compound targeting host protein phosphatase-1, inhibits HIV-1 transcription.

Author

Ammosova, Tatyana, Platonov, Maxim, Ivanov, Andrei, Kont, Yasemin Saygideğer, Kumari, Namita, Kehn ‐ Hall, Kylene, Jerebtsova, Marina, Kulkarni, Amol A, Üren, Aykut, Kovalskyy, Dmytro, and Nekhai, Sergei

Subjects

*PROTEIN phosphatase inhibitors, *MOLECULAR weights, *HIV protease inhibitors, *TARGETED drug delivery, *GENETIC transcription, *CELL-mediated cytotoxicity

Abstract

Background and Purpose HIV-1 transcription is activated by the Tat protein which recruits the cyclin-dependent kinase CDK9/cyclin T1 to TAR RNA. Tat binds to protein phosphatase-1 ( PP1) through the Q35 VCF38 sequence and translocates PP1 to the nucleus. PP1 dephosphorylates CDK9 and activates HIV-1 transcription. We have synthesized a low MW compound 1H4, that targets PP1 and prevents HIV-1 Tat interaction with PP1 and inhibits HIV-1 gene transcription. Here, we report our further work with the 1H4-derived compounds and analysis of their mechanism of action. Experimental Approach Using the 1H4- PP1 complex as a model, we iteratively designed and synthesized follow-up libraries that were analysed for the inhibition of HIV-1 transcription and toxicity. We also confirmed the mechanism of action of the PP1-targeting molecules by determining the affinity of binding of these molecules to PP1, by analysing their effects on PP1 activity, disruption of PP1 binding to Tat and shuttling of PP1 to the nucleus. Key Results We identified a tetrahydroquinoline derivative, compound 7, which disrupted the interaction of Tat with PP1. We further optimized compound 7 and obtained compound 7c, renamed 1 E7-03, which inhibited HIV-1 with low IC50 (fivefold lower than the previously reported compound, 1H4), showed no cytotoxicity and displayed a plasma half-life greater than 8 h in mice. 1E7-03 bound to PP1 in vitro and prevented shuttling of PP1 into the nucleus. Conclusions and Implications Our study shows that low MW compounds that functionally mimic the PP1-binding RVxF peptide can inhibit HIV-1 transcription by deregulating PP1. [ABSTRACT FROM AUTHOR]

Published

2014

69. Immune Minimization Strategies in Renal Transplantation.

Author

Brar, Jyoti Eknoor and Nader, Nader D.

Subjects

*KIDNEY transplantation, *GRAFT rejection, *HOMOGRAFTS, *HEALTH outcome assessment, *IMMUNOSUPPRESSION, *PROTEIN phosphatase inhibitors, *NEPHROTOXICOLOGY, *IMMUNOREGULATION

Abstract

Very low early rejection rates and excellent short-term kidney allograft outcomes have been the mainstay of forwarding the field of Kidney Transplantation in the last few decades. This progress is mainly achieved by using the current armamentarium of maintenance immunosuppression in different combinations and dosages of calcineurin inhibitors (CNI), corticosteroids and antiproliferative drugs. Metabolic risks and nephrotoxicity of CNIs has led to a search for strategies to minimize their use. Similarly, metabolic risks, mood abnormalities and Cushing-like side effects of steroids have forced physicians and patients alike to try to minimize their use in transplantation. Here, we review the most recent randomized controlled trials of minimization of CNI/steroids in a manner (with incident immunologic risks, state of net immunosuppression and side- effects) that may be helpful to choose the best strategy for the individual patient. New trials testing minimization strategies should include in their design, an assessment of the impact of minimization on development of donor specific antibodies and antibody-mediated rejection as well as long-term outcomes. [ABSTRACT FROM AUTHOR]

Published

2014

70. Stable SET knockdown in breast cell carcinoma inhibits cell migration and invasion.

Author

Li, Jie, Yang, Xi-fei, Ren, Xiao-hu, Meng, Xiao-jing, Huang, Hai-yan, Zhao, Qiong-hui, Yuan, Jian-hui, Hong, Wen-xu, Xia, Bo, Huang, Xin-feng, Zhou, Li, Liu, Jian-jun, and Zou, Fei

Subjects

*BREAST cancer treatment, *PROTEIN phosphatase inhibitors, *CANCER cell migration, *CANCER invasiveness, *RNA interference, *GENE expression, *MATRIX metalloproteinases

Abstract

Breast cancer is the most malignant tumor for women, however, the mechanisms underlying this devastating disease remain unclear. SET is an endogenous inhibitor of protein phosphatase 2A (PP2A) and involved in many physiological and pathological processes. SET could promote the occurrence of tumor through inhibiting PP2A. In this study, we explore the role of SET in the migration and invasion of breast cancer cells MDA-MB-231 and ZR-75-30. The stable suppression of SET expression through lentivirus-mediated RNA interference (RNAi) was shown to inhibit the growth, migration and invasion of breast cancer cells. Knockdown of SET increases the activity and expression of PP2Ac and decrease the expression of matrix metalloproteinase 9 (MMP-9). These data demonstrate that SET may be involved in the pathogenic processes of breast cancer, indicating that SET can serve as a potential therapeutic target for the treatment of breast cancer. [ABSTRACT FROM AUTHOR]

Published

2014

71. Identification of a Plasmodium falciparum inhibitor-2 motif involved in the binding and regulation activity of protein phosphatase type.

Author

Fréville, Aline, Tellier, Géraldine, Vandomme, Audrey, Pierrot, Christine, Vicogne, Jérôme, Cantrelle, François ‐ Xavier, Martoriati, Alain, Cailliau ‐ Maggio, Katia, Khalife, Jamal, and Landrieu, Isabelle

Subjects

*PLASMODIUM falciparum, *PHOSPHOPROTEIN phosphatases, *NUCLEAR magnetic resonance spectroscopy, *PROTEIN-protein interactions, *GENETIC mutation, *PROTEIN phosphatase inhibitors, *XENOPUS eggs

Abstract

The regulation of Plasmodium falciparum protein phosphatase type 1 (PfPP1) activity remains to be deciphered. Data from homologous eukaryotic type 1 protein phosphatases (PP1) suggest that several protein regulators should be involved in this essential process. One such regulator, named PfI2 based on its primary sequence homology with eukaryotic inhibitor 2 (I2), was recently shown to be able to interact with PfPP1 and to inhibit its phosphatase activity, mainly through the canonical 'RVxF' binding motif. The details of the structural and functional characteristics of this interaction are investigated here. Using NMR spectroscopy, a second site of interaction is suggested to reside between residues D94 and T117 and contains the 'FxxR/KxR/K' binding motif present in other I2 proteins. This site seems to play in concert/synergy with the 'RVxF' motif to bind PP1, because only mutations in both motifs were able to abolish this interaction completely. However, regarding the structure/function relationship, mutation of either the 'RVxF' or 'FxxR/KxR/K' motif is more drastic, because each mutation prevents the capacity of PfI2 to trigger germinal vesicle breakdown in microinjected Xenopus oocytes. This indicates that the tight association of the PfI2 regulator to PP1, mediated by a two-site interaction, is necessary to exert its function. Based on these results, the use of a peptide derived from the 'FxxR/KxR/K' PfI2 motif was investigated for its potential effect on Plasmodium growth. This peptide, fused at its N-terminus to a penetrating sequence, was shown to accumulate specifically in infected erythrocytes and to have an antiplasmodial effect. [ABSTRACT FROM AUTHOR]

Published

2014

72. Interaction of protein phosphatase inhibitors with membrane lipids assessed by surface plasmon resonance based binding technique.

Author

Bécsi, Bálint, Kiss, Andrea, and Erdődi, Ferenc

Subjects

*PROTEIN phosphatase inhibitors, *MOLECULAR interactions, *MEMBRANE lipids, *SURFACE plasmon resonance, *BINDING agents, *LIPOSOMES

Abstract

The interaction of okadaic acid (OA), tautomycin (TM), microcystin-LR (MC-LR), cantharidin (CA), epigallocatechin-gallate (EGCG) and cyclosporin A (CsA), inhibitors of protein phosphatases, with liposome covered surfaces prepared from the lipid extracts of bovine brain, heart and liver was investigated by surface plasmon resonance (SPR) based binding technique. The SPR sensorgrams indicated reversible association or partial intercalation of the inhibitors with liposomes at 20 °C or 37 °C, respectively. Distinct lipid composition specificities were reflected in different saturation values of inhibitor binding in a decreasing order of liver > heart >> brain lipids. Assaying the effect of OA, TM, MC-LR, CA and EGCG on the activity of protein phosphatases in neuroblastoma B50, cardiomyoblast H9C2 and hepatocarcinoma HepG2 cells implied that the cell type specific association of phosphatase inhibitors with membrane lipids may influence their inhibitory potencies exerted on intact cells. [ABSTRACT FROM AUTHOR]

Published

2014

73. TIMAP promotes angiogenesis by suppressing PTEN-mediated Akt inhibition in human glomerular endothelial cells.

Author

Obeidat, Marya, Laiji Li, and Ballermann, Barbara J.

Subjects

*NEOVASCULARIZATION, *ENDOTHELIAL cells, *PROTEIN phosphatase inhibitors, *KIDNEY glomerulus, *PHOSPHORYLATION, *CELL proliferation

Abstract

The function of TIMAP, an endothelial cell (EC)-predominant protein phosphatase 1-regulatory subunit, is poorly understood. We explored the potential role of TIMAP in the Akt-dependent regulation of glomerular EC proliferation, survival, and in vitro angiogenesis. To deplete TIMAP, the EC were transfected with TIMAP-specific or nonspecific small interfering (si) RNA. The rate of electrical impedance development across subconfluent EC monolayers, a measure of the time-dependent increase in EC number, was 93 ± 2% lower in TIMAP-depleted than in control EC. This effect on cell proliferation was associated with reduced DNA synthesis and increased apoptosis: TIMAP silencing reduced 5-ethynyl-2'-deoxyuridine incorporation by 38 ± 2% during the exponential phase of EC proliferation, and cleaved caspase 3 as well as caspase 3 activity increased in TIMAPdepleted relative to control cells. Furthermore, TIMAP depletion inhibited the formation of angiogenic sprouts by glomerular EC in three-dimensional culture. TIMAP depletion strongly diminished growth factor-stimulated Akt phosphorylation without altering ERK1/2 phosphorylation, suggesting a specific effect on the PI3K/ Akt/PTEN pathway. Endogenous TIMAP and PTEN colocalized in EC and coimmunoprecipitated from EC lysates. The inhibitory PTEN phosphorylation on S370 was significantly reduced in TIMAP-depleted compared with control EC, while phosphorylation of PTEN on the S380/T382/T383 cluster remained unchanged. Finally, the PTEN inhibitor bpV(phen) fully reversed the suppressive effect of TIMAP depletion on Akt phosphorylation. The data indicate that in growing EC, TIMAP is necessary for Akt-dependent EC proliferation, survival, and angiogenic sprout formation and that this effect of TIMAP is mediated by inhibition of the tumor suppressor PTEN. [ABSTRACT FROM AUTHOR]

Published

2014

74. Sudden flamingo deaths in Kenyan Rift Valley lakes.

Author

Straubinger-Gansberger, Nadja, Gruber, Martin, Kaggwa, Mary N., Lawton, Linda, Oduor, Steve Omondi, and Schagerl, Michael

Subjects

*LESSER flamingo, *DIE-off (Zoology), *CYANOBACTERIAL toxins, *BIRD diseases, *PROTEIN phosphatase inhibitors

Abstract

The East African Rift Valley Lakes Bogoria and Nakuru sometimes host around 75% of the world population of lesser flamingos Phoeniconaias minor. In this area, mysterious flamingo die-offs have occupied researchers for four decades. Recently, cyanobacterial toxins came into the fore as a possible explanation for mass mortalities because the main food source of lesser flamingos is the cyanobacterium Arthrospira fusiformis. We took weekly samples from July 2008 to November 2009 from Lakes Nakuru and Bogoria and analyzed them by high performance liquid chromatography for microcystins. Monthly, samples were cross-checked using protein phosphatase inhibition assays with lower detection limits and additionally screened for polar toxins. During our study period, three flamingo die-offs occurred at L. Bogoria and we were able to analyze tissues of 20 carcasses collected at the shoreline. No cyanotoxins were detected either in plankton samples or in flamingo tissues. Accordingly, other reasons such as food composition or bird diseases played a key role in the observed flamingo die-offs. [ABSTRACT FROM AUTHOR]

Published

2014

75. CIP2A mediates erlotinib-induced apoptosis in non-small cell lung cancer cells without EGFR mutation.

Author

Cheng-Yi Wang, Ting-Ting Chao, Fang-Yu Chang, Yen-Lin Chen, Yi-Ting Tsai, Hen-I Lin, Yuh-Chin T. Huang, Chung-Wai Shiau, Chong-Jen Yu, and Kuen-Feng Chen

Subjects

*SMALL cell lung cancer, *CANCER treatment, *PROTEIN phosphatase inhibitors, *EPIDERMAL growth factor receptors, *ERLOTINIB, *APOPTOSIS, *CANCER cells, *PATIENTS, *THERAPEUTICS

Abstract

Background Epidermal growth factor receptor (EGFR) inhibitors show favorable clinical response in some patients with non-small cell lung cancer (NSCLC) who have no EGFR mutation, indicating alternative mechanisms for their tumoricidal effects. We previously showed erlotinib, a selective EGFR antagonist, inhibited the growth of sensitive hepatocellular carcinoma cells by inhibiting the cancerous inhibitor of protein phosphatase 2A (CIP2A) pathway. The aim of this study was to determine if erlotinib can also inhibit the growth of NSCLC cells by inactivating the CIP2A-dependent signaling pathway. Methods Four NSCLC cell lines (H358 H441 H460 and A549) were treated with erlotinib to determine their sensitivity to erlotinib-induced cell death and apoptosis. Expression of CIP2A and the downstream AKT were analyzed. The effects of CIP2A on erlotinib-induced apoptosis were confirmed by overexpression of CIP2A and knockdown of CIP2A gene expression in the sensitive cells and resistant cells, respectively. In vivo efficacy of erlotinib against H358 xenograft tumor was also determined in nude mice. Results Erlotinib induced significant cell death and apoptosis in H358 and H441 cells, as evidenced by increased caspase 3 activity and cleavage of pro-caspase 9 and PARP, but not in H460 or A549 cells. The apoptotic effect of erlotinib in the sensitive H358 cells was associated with downregulation of CIP2A, increase in PP2A activity and decrease in AKT phosphorylation. Overexpression of CIP2A and AKT protected the sensitive H358 cells from erlotinib-induced apoptosis. Knockdown of CIP2A gene expression by siRNA enhanced the erlotinib-induced apoptotic in the resistant H460 cells that resembled the sensitive H358 cells. Erlotinib also inhibited the growth of H358 tumors in nude mice. Conclusions The CIP2A-dependent pathway mediates the tumoricidal effects of erlotinib on NSCLC cells without EGFR mutations in vitro and in vivo. CIP2A may be a novel molecular target against NSCLC for future drug development. [ABSTRACT FROM AUTHOR]

Published

2014

76. Activation of the receptor for advanced glycation end products induces nuclear inhibitor of protein phosphatase-1 suppression.

Author

Liebisch, Marita, Bondeva, Tzvetanka, Franke, Sybille, Daniel, Christoph, Amann, Kerstin, and Wolf, Gunter

Subjects

*PROTEIN phosphatase inhibitors, *DIABETIC nephropathies, *CELL cycle, *NF-kappa B, *LABORATORY mice

Abstract

The activation of the receptor for advanced glycation end products (RAGE) is involved in the development of diabetic nephropathy. Analysis of protein phosphatase-1 indicated that advanced glycation end products did not affect its expression, but increased its phosphatase activity. Using differential display analysis we previously demonstrated that stimulation of RAGE in podocytes modulates the expression of numerous genes, among others nuclear inhibitor of protein phosphatase-1 (NIPP1). Here we found that silencing of NIPP1 induced podocyte hypertrophy, cell cycle arrest, and significantly increased protein phosphatase-1 activity. NIPP1 downregulation was associated with increased p27Kip1 protein expression. Reporter assays revealed a transcriptional activation of nuclear factor-κB in podocytes after suppression of NIPP1. The protein level of NIPP1 was also significantly reduced in podocytes of diabetic mice. Blocking the RAGE in vivo by a soluble analog elevated the NIPP1 protein in podocytes of diabetic mice. Thus, activation of the RAGE by advanced glycation end products or other ligands suppresses NIPP1 expression in diabetic nephropathy, contributes to podocyte hypertrophy, and glomerular inflammation. [ABSTRACT FROM AUTHOR]

Published

2014

77. PP2A-Mediated Regulation of Ras Signaling in G2 Is Essential for Stable Quiescence and Normal G1 Length.

Author

Naetar, Nana, Soundarapandian, Velmurugan, Litovchick, Larisa, Goguen, Kelsey?L., Sablina, Anna?A., Bowman-Colin, Christian, Sicinski, Piotr, Hahn, William?C., DeCaprio, James?A., and Livingston, David?M.

Subjects

*GENETIC regulation, *RAS proteins, *CELLULAR signal transduction, *CELL proliferation, *PROTEIN phosphatase inhibitors, *CYCLIN E, *MITOSIS

Abstract

Summary: Quiescence (G0) allows cycling cells to reversibly cease proliferation. A decision to enter quiescence is suspected of occurring early in G1, before the restriction point (R). Surprisingly, we have identified G2 as an interval during which inhibition of the protein phosphatase PP2A results in failure to exhibit stable quiescence. This effect is accompanied by shortening of the ensuing G1. The PP2A subcomplex required for stable G0 contains the B56γ B subunit. After PP2A inhibition in G2, aberrant overexpression of cyclin E occurs during mitosis and is responsible for overriding quiescence. Strikingly, suppression of Ras signaling re-establishes normal cyclin E levels during M and restores G0. These data point to PP2A-B56γ-driven Ras signaling modulation in G2 as essential for suppressing aberrant cyclin E expression during mitosis and thereby achieving normal G0 control. Thus, G2 is an interval during which the length and growth factor dependence of the next G1 interval are established. [ABSTRACT FROM AUTHOR]

Published

2014

78. Overexpression of CIP2A is an independent prognostic indicator in nasopharyngeal carcinoma and its depletion suppresses cell proliferation and tumor growth.

Author

Na Liu, Qing-Mei He, Jie-Wei Chen, Ying-Qin Li, Ya-Fei Xu, Xian-Yue Ren, Ying Sun, Hai-Qiang Mai, Jian-Yong Shao, Wei-Hua Jia, Tie-Bang Kang, Mu-Sheng Zeng, and Jun Ma

Subjects

*PROTEIN phosphatase inhibitors, *CELL proliferation, *TUMOR growth, *CELL growth, *WESTERN immunoblotting, *IMMUNOHISTOCHEMISTRY, *CELL lines, *MESSENGER RNA

Abstract

Background Cancerous inhibitor of protein phosphatase 2A (CIP2A) is an oncoprotein that acts as a prognostic marker for several human malignancies. In this study, we investigated the clinical significance of CIP2A and its function in nasopharyngeal carcinoma (NPC). Methods Quantitative RT-PCR, western blot, and immunohistochemistry analyses were used to quantify CIP2A expression in NPC cell lines and clinical samples. Kaplan-Meier curves were used to estimate the association between CIP2A expression and patient survival. The functional role of CIP2A in NPC cell lines was evaluated by small interfering RNA-mediated depletion of the protein followed by analyses of cell proliferation and xenograft growth. Results CIP2A levels were upregulated in NPC cell lines and clinical samples at both the mRNA and protein levels (P < 0.01). Patients with high CIP2A expression had poorer overall survival (HR, 1.98; 95% CI, 1.16-3.34; P = 0.01) and poorer disease-free survival (HR, 1.68; 95% CI, 1.07-2.62; P = 0.02) rates than patients with low CIP2A expression. In addition, CIP2A expression status was an independent prognostic indicator for NPC patients. The depletion of CIP2A expression inhibited c-Myc protein expression in NPC cell lines, suppressed cell viability, colony formation, and anchorage-independent growth in vitro, and inhibited xenograft tumor growth in vivo. Conclusions Our data demonstrate that high CIP2A expression in patients was associated with poor survival in NPC, and depletion of CIP2A expression inhibited NPC cell proliferation and tumor growth. Thus, these results warrant further investigation of CIP2A as a novel therapeutic target for the treatment of NPC. [ABSTRACT FROM AUTHOR]

Published

2014

79. Silencing I2PP2A rescues tau pathologies and memory deficits through rescuing PP2A and inhibiting GSK-3β signaling in human tau transgenic mice.

Author

Yao Zhang, Rong-Hong Ma, Xia-Chun Li, Jia-Yu Zhang, Hai-Rong Shi, Wei Wei, Dan-Ju Luo, Qun Wang, Jian-Zhi Wang, and Gong-Ping Liu

Subjects

PROTEIN phosphatase inhibitors, MEMORY disorders, ALZHEIMER'S disease, AMYLOID beta-protein precursor, PHOSPHORYLATION, LABORATORY mice

Abstract

Increase of inhibitor-2 of protein phosphatase-2A I2PP2A is associated with protein phosphatase-2A (PP2A) inhibition and tau hyperphosphorylation in Alzheimer's disease (AD). Down-regulating I2PP2A attenuated amyloidogenesis and improved the cognitive functions in transgenic mice expressing amyloid precursor protein (tg2576). Here, we found that silencing I2PP2A by hippocampal infusion of Lenti - siI2PP2A down-regulated I2PP2A (噟45%) with reduction of tau phosphorylation/accumulation, improvement of memory deficits, and dendritic plasticity in 12-month-old human tau transgenic mice. Silencing I2PP2A not only restored PP2A activity but also inhibited glycogen synthase kinase-3ß (GSK-3ß) with a significant activation of protein kinase A (PKA) and Akt. In HEK293/tau and N2a/tau cells, silencing I2PP2A by pSUPER - siI2PP2A also significantly reduced tau hyperphosphorylation with restoration of PP2A activity and inhibition of GSK-3ß, demonstrated by the decreased GSK-3ß total protein and mRNA levels, and the increased inhibitory phosphorylation of GSK-3ß at serine-9. Furthermore, activation of PKA but not Akt mediated the inhibition of GSK-3ß by I2PP2A silencing. We conclude that targeting I2PP2A can improve tau pathologies and memory deficits in human tau transgenic mice, and activation of PKA contributes to GSK-3ß inhibition induced by silencing I2PP2A in vitro, suggesting that I2PP2A is a promising multiple target of AD. [ABSTRACT FROM AUTHOR]

Published

2014

80. Knockdown of cancerous inhibitor of protein phosphatase 2A may sensitize NSCLC cells to cisplatin.

Author

Wei, L, Qu, W, Sun, J, Wang, X, Lv, L, Xie, L, and Song, X

Subjects

*PROTEIN phosphatase inhibitors, *SMALL interfering RNA, *PROTEOLYSIS, *SMALL cell lung cancer, *CISPLATIN, *CANCER invasiveness, *CANCER cell proliferation

Abstract

Cancerous inhibitor of protein phosphatase 2A (CIP2A) is a recently identified human oncoprotein that can stabilize some proteins by inhibiting degradation mediated by protein phosphatase 2A (PP2A) and it increases the proliferation of several cancer cells. Recent studies have highlighted a potential role for CIP2A in promoting tumor progression and metastasis. However, whether CIP2A could increase chemoresistance of cancer cells to chemotherapeutic agent cisplatin remains unclear. To determine whether CIP2A serves as a potential therapeutic target of human non-small-cell lung cancer (NSCLC), we utilized small interference RNA (siRNA) to knock down CIP2A expression in human NSCLC cells and analyzed their phenotypic changes. The data demonstrated that CIP2A silencing led to decreased proliferation, impaired clonogenicity and enhanced chemosensitivity and apoptosis to cisplatin in human NSCLC cells, as well as reduced Akt phosphorylation. In addition, overexpression of CIP2A diminished NSCLC cell chemosensitivity to cisplatin by inducing activation of Akt pathway, suggesting critical roles of CIP2A in NSCLC cell chemoresistance to cisplatin and rasing the possibility of CIP2A inhibition as a promising approach for lung cancer therapy. [ABSTRACT FROM AUTHOR]

Published

2014

81. Synergistic Role of Protein Phosphatase Inhibitor 1 and Sarco/Endoplasmic Reticulum Ca2+-ATPase in the Acquisition of the Contractile Phenotype of Arterial Smooth Muscle Cells.

Author

Lipskaia, Larissa, Bobe, Regis, Jiqiu Chen, Turnbull, Irene C., Lopez, Jose J., Merlet, Elise, Dongtaq Jeong, Karakikes, Ioannis, Ross, Alexandra S., Lifan Liang, Mougenot, Nathalie, Atassi, Fabrice, Lompré, Anne-Marie, Tarzami, Sima T., Kovacic, Jason C., Kranias, Evangelia, Hajjar, Roger J., and Hadri, Lahouaria

Subjects

*PROTEIN phosphatase inhibitors, *MUSCLE cells, *VASCULAR smooth muscle contraction, *ADENOSINE triphosphatase, *CYCLIC guanylic acid, *PHOSPHORYLATION, *ACETYLCHOLINE, *GENETIC transformation

Abstract

Background--Phenotypic modulation or switching of vascular smooth muscle cells from a contractile/quiescent to a proliferative/synthetic phenotype plays a key role in vascular proliferative disorders such as atherosclerosis and restenosis. Although several calcium handling proteins that control differentiation of smooth muscle cells have been identified, the role of protein phosphatase inhibitor 1 (I-1) in the acquisition or maintenance of the contractile phenotype modulation remains unknown. Methods and Results--In human coronary arteries, I-1 and sarco/endoplasmic reticulum Ca2+-ATPase expression is specific to contractile vascular smooth muscle cells. In synthetic cultured human coronary artery smooth muscle cells, protein phosphatase inhibitor 1 (I-1 target) is highly expressed, leading to a decrease in phospholamban phosphorylation, sarco/endoplasmic reticulum Ca2+-ATPase, and cAMP-responsive element binding activity. I-1 knockout mice lack phospholamban phosphorylation and exhibit vascular smooth muscle cell arrest in the synthetic state with excessive neointimal proliferation after carotid injury, as well as significant modifications of contractile properties and relaxant response to acetylcholine of femoral artery in vivo. Constitutively active I-1 gene transfer decreased neointimal formation in an angioplasty rat model by preventing vascular smooth muscle cell contractile to synthetic phenotype change. Conclusions--I-1 and sarco/endoplasmic reticulum Ca2+-ATPase synergistically induce the vascular smooth muscle cell contractile phenotype. Gene transfer of constitutively active I-1 is a promising therapeutic strategy for preventing vascular proliferative disorders. [ABSTRACT FROM AUTHOR]

Published

2014

82. Regulation of α-endosulfine, an inhibitor of protein phosphatase 2 A, by multisite phosphorylation.

Author

Mochida, Satoru

Subjects

*PROTEIN phosphatase inhibitors, *PHOSPHORYLATION, *CYCLIN-dependent kinases, *ADENOSINE monophosphate, *CELL cycle, *CELLULAR signal transduction, *XENOPUS laevis

Abstract

Progression into M phase requires inhibition of heterotrimeric PP2 A containing the regulatory B55 subunit ( PP2A- B55) as well as the activation of cyclin-dependent kinase 1 ( Cdk1). α-endosulfine ( ENSA)/cyclic AMP-regulated 19 kDa phosphoprotein ( ARPP-19) family proteins phosphorylated at S67 by Greatwall kinase bind and inhibit PP2 A- B55. This study shows that endogenous kinases phosphorylate not only S67 but also two additional sites in ENSA ( T28 and S109) with different kinetics at different cell-cycle stages in Xenopus laevis intact cells and cell-free egg extracts. When assayed in vitro, these phosphorylations had qualitatively and/or quantitatively different effects on inhibition of PP2 A- B55 by ENSA. Structural analyses revealed that the most-conserved middle region of ENSA containing S67 physically interacts with PP2 A- B55 at the interface of the B55 and C subunits, where the catalytic centre of PP2 A is located. As non-phosphorylated ENSA has an intrinsic potential for PP2 A- B55 inhibition, these three phosphorylations differentially affect physical interaction of the middle region of ENSA with PP2 A- B55. These results suggest that the two additional phosphorylation sites together with S67 allow ENSA to function as a 'stepwise tuner' for PP2 A- B55, which may be regulated by multiple cellular signals, rather than a simple 'on/off' switch. [ABSTRACT FROM AUTHOR]

Published

2014

83. Feedback regulation mediated by Bcl-2 and DARPP-32 regulates inositol 1,4,5-trisphosphate receptor phosphorylation and promotes cell survival.

Author

Ming-Jin Chang, Fei Zhong, Lavik, Andrew R., Parys, Jan B., Berridge, Michael J., and Distelhorst, Clark W.

Subjects

*CALCIUM, *LYMPHOCYTE transformation, *T cells, *PROTEIN phosphatase inhibitors, *PHOSPHORYLATION, *CELLULAR signal transduction, *CHRONIC lymphocytic leukemia, *APOPTOSIS

Abstract

Bcl-2 interacts with the inositol 1,4,5-trisphosphate receptor (InsP3R) and thus prevents InsP3-induced Ca2+ elevation that induces apoptosis. Here we report that Bcl-2 binds dopamine- and cAMP-regulated phosphoprotein of 32 kDa (DARPP-32), a protein kinase A (PKA)-activated and calcineurin (CaN)-deactivated inhibitor of protein phosphatase 1 (PP1). Bcl-2 docks DARPP-32 and CaN in a complex on the InsP3R, creating a negative feedback loop that prevents exaggerated Ca2+ release by decreasing PKA-mediated InsP3R phosphorylation. T-cell activation increases PKA activity, phosphorylating both the InsP3R and DARPP-32. Phosphorylated DARPP-32 inhibits PP1, enhancing InsP3R phosphorylation and Ca2+ release. Elevated Ca2+ activates CaN, which dephosphorylates DARPP-32 to dampen Ca2+ release by eliminating PP1 inhibition to enable it to dephosphorylate the InsP3R. Knocking down either Bcl-2 or DARPP-32 abrogates this feedback mechanism, resulting in increased Ca2+ elevation and apoptosis. This feedback mechanism appears to be exploited by high levels of Bcl-2 in chronic lymphocytic leukemia cells, repressing B-cell receptor-induced Ca2+ elevation and apoptosis. [ABSTRACT FROM AUTHOR]

Published

2014

84. Does the calcineurin inhibitor have influence on cytomegalovirus infection in heart transplantation?

Author

Rodríguez‐Serrano, María, Sánchez‐Lázaro, Ignacio, Almenar‐Bonet, Luis, Martínez‐Dolz, Luis, Portolés‐Sanz, Manuel, Rivera‐Otero, Miguel, and Salvador‐Sanz, Antonio

Subjects

*CYTOMEGALOVIRUS diseases, *CALCINEURIN, *PROTEIN phosphatase inhibitors, *HEART transplantation, *HEART disease related mortality, *CYCLOSPORINE

Abstract

Cytomegalovirus ( CMV) infection is a major cause of morbidity and mortality in heart transplant ( HTx). Our aim was to analyze the rate of CMV infection in HTx patients receiving treatment with cyclosporine ( Cs A) or tacrolimus (Tac). Ninety-five patients were randomized to receive either Cs A (53.7%) or Tac (46.3%). We performed prophylaxis with valganciclovir in patients with the highest risk of CMV infection. We considered CMV infection as an increased viral load or the presence of CMV in histological samples. We analyzed baseline characteristics, CMV infection, and other complications. Event-free rates were calculated using the Kaplan-Meier method. There were no significant differences in baseline characteristics between both groups. CMV infection was detected in 31.6% of patients (in 66.7% due to asymptomatic replication). The group treated with Tac had a lower rate of CMV infection (15.9% vs. 45.1%, p = 0.002) and longer CMV infection-free survival time (1440 vs. 899 d, p = 0.001). No differences were observed in the complications analyzed in both groups. The independent risk factors for infection identified in the multivariate analysis were treatment with Cs A and bacterial infections. This was the first study to demonstrate a lower rate of CMV infection in patients treated with Tac vs. those treated with Cs A after HTx. [ABSTRACT FROM AUTHOR]

Published

2014

85. Conversion of stable ABO-incompatible kidney transplant recipients from mycophenolate mofetil with standard exposure calcineurin inhibitors (CNIs) to everolimus with very low exposure CNIs-a short-term pilot study.

Author

Uchida, Junji, Machida, Yuichi, Iwai, Tomoaki, Kuwabara, Nobuyuki, Kabei, Kazuya, Naganuma, Toshihide, Kumada, Norihiko, Kawashima, Hidenori, and Nakatani, Tatsuya

Subjects

*MYCOPHENOLIC acid, *ABO blood group system, *KIDNEY transplantation, *CALCINEURIN, *PROTEIN phosphatase inhibitors, *EVEROLIMUS, *B cells, *CELL proliferation

Abstract

Background A recent report has demonstrated that as with mycophenolate mofetil ( MMF), everolimus is capable of inhibiting human B-lymphocyte function and activation including B-lymphocyte proliferation, apoptosis, and immunoglobulin production in vitro. Everolimus may therefore be used as an immunosuppressant in ABO-incompatible kidney transplantation. Methods A three-month pilot study was performed to examine the efficacy and safety of conversion of stable ABO-incompatible kidney transplant recipients from MMF with standard exposure calcineurin inhibitors ( CNIs) to everolimus with very low exposure CNIs. Sixteen recipients were enrolled in the study. The patients without acute rejection by graft biopsy were switched from MMF to everolimus with CNI minimization. At three months after conversion, graft biopsies were performed to check for acute rejection and C4d deposition. Results Conversion to everolimus with CNI minimization for three months did not induce acute rejection and C4d deposition in all of the ABO-incompatible kidney transplant recipients. A slight elevation of anti-A/B antibody titer occurred in our present study. Everolimus was associated with hyperlipidemia and edema. Conclusions These results demonstrated that short-term conversion from MMF to everolimus after one yr post-transplant may be a safe and effective alternate for ABO-incompatible kidney transplant recipients requiring temporary discontinuation of MMF. [ABSTRACT FROM AUTHOR]

Published

2014

86. Cancerous Inhibitor of Protein Phosphatase 2A (CIP2A) Protein Is Involved in Centrosome Separation through the Regulation of NIMA (Never In Mitosis Gene A)-related Kinase 2 (NEK2) Protein Activity.

Author

Ae Lee Jeong, Sunyi Lee, Jeong Su Park, Sora Han, Chang-Young Jang, Jong-Seok Lim, Myung Sok Lee, and Young Yang

Subjects

*CENTROSOMES, *MITOSIS, *PROTEIN phosphatase inhibitors, *SPINDLE apparatus, *BIOLOGICAL rhythms, *CELL proliferation

Abstract

Cancerous inhibitor of protein phosphatase 2A (CIP2A) is overexpressed in most human cancers and has been described as being involved in the progression of several human malignancies via the inhibition of protein phosphatase 2A (PP2A) activity toward c-Myc. However, with the exception of this role, the cellular function of CIP2A remains poorly understood. On the basis of yeast two-hybrid and coimmunoprecipitation assays, we demonstrate here that NIMA (never in mitosis gene A)-related kinase 2 (NEK2) is a binding partner for CIP2A. CIP2A exhibited dynamic changes in distribution, including the cytoplasm and centrosome, depending on the cell cycle stage. When CIP2A was depleted, centrosome separation and the mitotic spindle dynamics were impaired, resulting in the activation of spindle assembly checkpoint signaling and, ultimately, extension of the cell division time. Our data imply that CIP2A strongly interacts with NEK2 during G2/M phase, thereby enhancingNEK2kinase activity to facilitate centrosome separation in a PP1- and PP2A-independent manner. In conclusion, CIP2A is involved in cell cycle progression through centrosome separation and mitotic spindle dynamics. [ABSTRACT FROM AUTHOR]

Published

2014

87. Silencing PP2A Inhibitor by Lenti-shRNA Interference Ameliorates Neuropathologies and Memory Deficits in tg2576 Mice.

Author

Liu, Gong-Ping, Wei, Wei, Zhou, Xin, Shi, Hai-Rong, Liu, Xing-Hua, Chai, Gao-Shang, Yao, Xiu-Qing, Zhang, Jia-Yu, Peng, Cai-Xia, Hu, Juan, Li, Xia-Chun, Wang, Qun, and Wang, Jian-Zhi

Subjects

*PHOSPHOPROTEIN phosphatases, *PROTEIN phosphatase inhibitors, *ALZHEIMER'S disease, *MESSENGER RNA, *LABORATORY mice

Abstract

Deficits of protein phosphatase-2A (PP2A) play a crucial role in tau hyperphosphorylation, amyloid overproduction, and synaptic suppression of Alzheimer's disease (AD), in which PP2A is inactivated by the endogenously increased inhibitory protein, namely inhibitor-2 of PP2A (I2PP2A). Therefore, in vivo silencing I2PP2A may rescue PP2A and mitigate AD neurodegeneration. By infusion of lentivirus-shRNA targeting I2PP2A (LV-siI2PP2A) into hippocampus and frontal cortex of 11-month-old tg2576 mice, we demonstrated that expression of LV-siI2PP2A decreased remarkably the elevated I2PP2A in both mRNA and protein levels. Simultaneously, the PP2A activity was restored with the mechanisms involving reduction of the inhibitory binding of I2PP2A to PP2A catalytic subunit (PP2AC), repression of the inhibitory Leu309-demethylation and elevation of PP2AC. Silencing I2PP2A induced a long-lasting attenuation of amyloidogenesis in tg2576 mice with inhibition of amyloid precursor protein hyperphosphorylation and β-secretase activity, whereas simultaneous inhibition of PP2A abolished the antiamyloidogenic effects of I2PP2A silencing. Finally, silencing I2PP2A could improve learning and memory of tg2576 mice with preservation of several memory-associated components. Our data reveal that targeting I2PP2A can efficiently rescue Aβ toxicities and improve the memory deficits in tg2576 mice, suggesting that I2PP2A could be a promising target for potential AD therapies.Molecular Therapy (2013); 21 12, 2247-2257. doi:10.1038/mt.2013.189 [ABSTRACT FROM AUTHOR]

Published

2013

88. CIP2A facilitates apoptotic resistance of fibroblast-like synoviocytes in rheumatoid arthritis independent of c-Myc expression.

Author

Lee, Jaejoon, Jeong, Hyemin, Park, Eun-Jung, Hwang, Ji, Huang, Bo, Bae, Eun-Kyung, Ahn, Joong, Cha, Hoon-Suk, and Koh, Eun-Mi

Subjects

*PROTEIN phosphatase inhibitors, *APOPTOSIS inhibition, *FIBROBLASTS, *SYNOVIAL fluid, *RHEUMATOID arthritis, *MYC oncogenes, *GENE expression, *SMALL interfering RNA

Abstract

The aim of this study is to investigate the effects of CIP2A (Cancerous inhibitor of protein phosphatase 2A) on the apoptosis of RA FLS. Proliferation and apoptotic activity of RA FLS following treatment with CIP2A siRNA or control siRNA were analyzed using MTT assays and Cell Death Detection kit. RA FLS was treated with CIP2A siRNA or control siRNA in 3-, 6-, and 9-day intervals for a Western blot analysis to determine C-Myc expression. To evaluate the signal transduction pathways engaged in apoptosis, caspase-3 activity, caspase-9 activity, PARP, and phosphorylation of the Akt kinase were analyzed by Western blot. Cell viability of RA FLS was significantly lower in the CIP2A siRNA-treated group compared with the control after 7 days ( p = 0.022). Apoptosis of RA FLS was significantly higher in the CIP2A siRNA-treated group compared with the control when incubated for 3, 6, and 9 days ( p = 0.029, p = 0.021, p = 0.043, respectively). C-Myc expression did not change with the different incubation periods. CIP2A siRNA-treated FLS expressed higher level of activated caspase-3, caspase-9, and PARP ( p = 0.014, p = 0.020, p = 0.021, respectively) and lower level of phosphorylated Akt ( p = 0.001) compared with those treated with the control siRNA. Our data show that CIP2A expression in RA FLS is an important mediator of dysfunctional apoptosis independent of c-Myc stabilization. Expression of CIP2A may contribute to apoptotic resistance of RA FLS through the activation of Akt and deactivation of caspase-3, caspase-9, and PARP. Inhibition of CIP2A may therefore constitute a novel, promising therapeutic target in RA. [ABSTRACT FROM AUTHOR]

Published

2013

89. Spermidine promotes adipogenesis of 3T3-L1 cells by preventing interaction of ANP32 with HuR and PP2A.

Author

HYVÖNEN, Mervi T., KOPONEN, Taina, WEISELL, Janne, PIETILÄ, Marko, KHOMUTOV, Alex R., VEPSÄLÄINEN, Jouko, ALHONEN, Leena, and KEINÄNEN, Tuomo A.

Subjects

*SPERMIDINE, *BIOSYNTHESIS, *POLYAMINES, *PHOSPHOPROTEINS, *PROTEIN phosphatase inhibitors, *ADIPOGENESIS, *TRANSCRIPTION factors

Abstract

We have shown previously that the polyamine spermidine is indispensable for differentiation of 3T3-L1 preadipocytes. In the present study, we examined the mechanism of spermidine function by using the polyamine biosynthesis inhibitor a- difluoromethylornithine in combination with the metabolically stable polyamine analogues ? -methylspermidine or (R,R)- a,?-bismethylspermine. At the early phase of differentiation, spermidine-depleted 3T3-L1 cells showed decreased translation of the transcription factor C/EBPß (CCAAT/enhancer-binding protein ß), decreased PP2A (protein phosphatase 2A) activity and increased cytoplasmic localization of the RNA-binding protein HuR (human antigen R). The amount of HuR bound to C/EBPß mRNA was reduced, whereas the amount of bound CUGBP2, an inhibitor of C/EBPß translation, was increased. ANP32 (acidic nuclear phosphoprotein 32) proteins, which are known PP2A inhibitors and HuR ligands, bound more PP2A and HuR in spermidine-depleted than in control cells, whereas immunodepletion of ANP32 proteins from the lysate of spermidine-depleted cells restored PP2A activity. Taken together, our data shows that spermidine promotes C/EBPß translation in differentiating 3T3-L1 cells, and that this process is controlled by the interaction of ANP32 with HuR and PP2A. [ABSTRACT FROM AUTHOR]

Published

2013

90. Suppression of Antifolate Resistance by Targeting the Myosin Va Trafficking Pathway in Melanoma.

Author

Fernández-Pérez, María Piedad, Montenegro, María F., Sáez-Ayala, Magalí, Sánchez-del-Campo, Luis, Piñero-Madrona, Antonio, Cabezas-Herrera, Juan, and Rodríguez-López, José Neptuno

Subjects

*MELANOMA, *ANTINEOPLASTIC agents, *MULTIDRUG resistance, *METHOTREXATE, *PROTEIN phosphatase inhibitors, *MORTALITY, *DRUG resistance

Abstract

Human melanoma is a significant clinical problem. As most melanoma patients relapse with lethal drug-resistant disease, understanding and preventing mechanism(s) of resistance is one of the highest priorities to improve melanoma therapy. Melanosomal sequestration and the cellular exportation of cytotoxic drugs have been proposed to be important melanoma-specific mechanisms that contribute to multidrug resistance in melanoma. Concretely, we found that treatment of melanoma with methotrexate (MTX) altered melanogenesis and accelerated the exportation of melanosomes; however, the cellular and molecular processes by which MTX is trapped into melanosomes and exported out of cells have not been elucidated. In this study, we identified myosin Va (MyoVa) as a possible mediator of these cellular processes. The results demonstrated that melanoma treatment with MTX leads to Akt2-dependent MyoVa phosphorylation, which enhances its ability to interact with melanosomes and accelerates their exportation. To understand the mechanism(s) by which MTX activates Akt2, we examined the effects of this drug on the activity of protein phosphatase 2A, an Akt inhibitor activated by the methylation of its catalytic subunit. Taken together, this study identified a novel trafficking pathway in melanoma that promotes tumor resistance through Akt2/MyoVa activation. Because of these findings, we explored several MTX combination therapies to increase the susceptibility of melanoma to this drug. By avoiding MTX exportation, we observed that the E2F1 apoptotic pathway is functional in melanoma, and its induction activates p73 and apoptosis protease-activating factor 1 following a p53-autonomous proapoptotic signaling event. [ABSTRACT FROM AUTHOR]

Published

2013

91. Ser9 phosphorylation causes cytoplasmic detention of I2 PP2A/SET in Alzheimer disease

Author

Yu, Guang, Yan, Tonghai, Feng, Ye, Liu, Xinghua, Xia, Yiyuan, Luo, Hongbin, Wang, Jian-Zhi, and Wang, Xiaochuan

Subjects

*ALZHEIMER'S disease, *PROTEIN phosphatase inhibitors, *CYTOPLASM, *PHOSPHORYLATION, *CASEIN kinase, *AMINO acid analysis

Abstract

Abstract: The nuclear protein I2 PP2A/SET, an endogenous inhibitor of protein phosphatase-2A (PP2A), is increased and translocated to the cytoplasm in the neurons of Alzheimer''s disease (AD) brains, and PP2A activity in cytoplasm is compromised. However, it is not fully understood how SET is retained in the cytoplasm. By generating a phosphorylation site-specific antibody, we found in the present study that SET is phosphorylated at Ser9, by which it is accumulated in the cytoplasm of the AD brains. Further studies demonstrate that both the phosphor-mimic and casein kinase (CK)II-mediated phosphorylation at Ser9 interferes with the formation of the SET/importin-α/importin-β complex, and thus inhibits SET nuclear import and induces the cytoplasmic detention of SET. Interestingly, Ser9 is nested in the center of the sequence 6AKVSKK11 of SET, which is consistent with a classical nuclear localization signal (NLS). To test whether 6AKVSKK11 is a new NLS of SET, we mutated SET lysine 7, lysine 10, and lysine 11 to alanine acid (K7A, K10A, K11A) respectively, and expressed these mutants in HEK293/tau cells. We found that expression of SET (K11A) led to a nuclear import defect of SET, and application of a synthesized peptide Tat-AAKVSKKE that can competitively bind to importin α/β resulted in cytoplasmic detention of SET. Finally, phosphorylation of SET aggravates PP2A inhibition and leads to tau hyperphosphorylation. In conclusion, the current study has identified a novel mechanism that causes cytoplasmic detention of SET with a new NLS-dependent CKII-associated phosphorylation of Ser9, suggesting that inhibition of CKII arrests cytoplasmic accumulation of SET and thus preserves PP2A activity in AD brains. [Copyright &y& Elsevier]

Published

2013

92. Impaired expression of protein phosphatase 2A subunits enhances metastatic potential of human prostate cancer cells through activation of AKT pathway.

Author

Pandey, P, Seshacharyulu, P, Das, S, Rachagani, S, Ponnusamy, M P, Yan, Y, Johansson, S L, Datta, K, Fong Lin, M, and Batra, S K

Subjects

*PROSTATE cancer treatment, *GENE expression, *PROTEIN phosphatase inhibitors, *METASTASIS, *CANCER cells, *GENETIC regulation, *CELLULAR signal transduction, *TRANSCRIPTION factors

Abstract

Background:Protein phosphatase 2A (PP2A) is a dephosphorylating enzyme, loss of which can contribute to prostate cancer (PCa) pathogenesis. The aim of this study was to analyse the transcriptional and translational expression patterns of individual subunits of the PP2A holoenzyme during PCa progression.Methods:Immunohistochemistry (IHC), western blot, and real-time PCR was performed on androgen-dependent (AD) and androgen-independent (AI) PCa cells, and benign and malignant prostate tissues for all the three PP2A (scaffold, regulatory, and catalytic) subunits. Mechanistic and functional studies were performed using various biochemical and cellular techniques.Results:Through immunohistochemical analysis we observed significantly reduced levels of PP2A-A and -B′γ subunits (P<0.001 and P=0.0002) in PCa specimens compared with benign prostate. Contemporarily, there was no significant difference in PP2A-C subunit expression between benign and malignant tissues. Similar to the expression pattern observed in tissues, the endogenous levels of PP2A-A and B′γ subunits were abrogated from the low metastatic to high metastatic and AD to AI cell line models, without any change in the catalytic subunit expression. Furthermore, using in vitro studies we demonstrated that PP2A-Aα scaffold subunit has a role in dampening AKT, β-catenin, and FAK (focal adhesion kinase) signalling.Conclusion:We conclude that loss of expression of scaffold and regulatory subunits of PP2A is responsible for its altered function during PCa pathogenesis. [ABSTRACT FROM AUTHOR]

Published

2013

93. Contractile protein phosphorylation predicts human heart disease phenotypes.

Author

Walker, Lori A., Fullerton, David A., and Buttrick, Peter M.

Subjects

*HEART failure, *CONTRACTILITY (Biology), *PHOSPHORYLATION, *AORTIC stenosis, *PROTEIN phosphatase inhibitors, *WESTERN immunoblotting

Abstract

Human heart failure has been associated with a low level of thin-filament protein phosphorylation and an increase in calcium sensitivity of contraction relative to both "control" human heart tissue and tissue from small animal models. However, diverse strategies of human tissue procurement and the reliance on tissue obtained from subjects with end-stage heart failure suggest this may be an incomplete characterization. Therefore, we evaluated cardiac left ventricular (LV) biopsy samples from patients with aortic stenosis undergoing valve replacement who presented either with LV hypertrophy and preserved systolic function (Hyp) or with LV dilation and reduced ejection fraction (Dil). In Hyp, total troponin I (TnI) phosphorylation was markedly increased and myosin light chain 2 (MLC2) phosphorylation was unchanged relative to a control group of patients with normal LV function. Conversely, in Dil, total TnI phosphorylation was significantly reduced compared with control subjects and MLC2 phosphorylation was increased. Site-specific analysis of TnI phosphorylation revealed phenotypespecific differences such that Hyp samples demonstrated significant increases in phosphorylation at serine 22/23 and Dil samples had significant decreases at serine 43. The ratio of phosphorylation at the two sites was biased toward serine 22/23 in Hyp and toward serine 43/45 in Dil. Western blot analysis showed that protein phosphatase-1 was reduced in Hyp and protein phosphatase-2 was reduced in Dil. These data suggest that posttranslational modifications of sarcomeric proteins, both singly and in combination, are stage specific. Defining these changes in progressive heart disease may provide important diagnostic and treatment information. [ABSTRACT FROM AUTHOR]

Published

2013

94. Comparative Toxicological Study of the Novel Protein Phosphatase Inhibitor 19-Epi-Okadaic Acid in Primary Cultures of Rat Cerebellar Cells.

Author

Fernández-Sánchez, Maria-Teresa, Cabrera-García, David, Ferrero-Gutierrez, Amaia, Pérez-Gómez, Anabel, Cruz, Patricia G., Daranas, Antonio H., Fernández, José J., Norte, Manuel, and Novelli, Antonello

Subjects

*NEUROTOXICOLOGY, *POISONOUS shellfish, *COMPARATIVE studies, *LABORATORY rats, *CEREBELLAR cortex, *PROTEIN phosphatase inhibitors, *CASPASES

Abstract

Okadaic acid (OKA) and analogues are frequent contaminants of coastal waters and seafood. Structure analysis of the isolated OKA analogue 19-epi-OKA showed important conformation differences expected to result in lower protein phosphatase (PP) inhibitory potencies than OKA. However, 19-epi-OKA and OKA inhibitory activities versus PP2A were unexpectedly found to be virtually equipotent. To investigate the toxicological relevance of these findings, we tested the effects of 19-epi-OKA on cultured cerebellar cells and compared them with those of OKA and its isomer dinophysistoxin-2. 19-epi-OKA caused degeneration of neurites and neuronal death with much lower potency than its congeners. The concentration of 19-epi-OKA that reduced after 24h the maximum neuronal survival (EC5024) by 50% was ~300nM compared with ~2nM and ~8nM for OKA and dinophysistoxin-2, respectively. Exposure to 19-epi-OKA resulted also in less toxicity for cultured glial cells (EC5024,19-epi-OKA ~ 600nM; EC5024,OKA ~ 20nM). 19-epi-OKA induced apoptotic condensation and fragmentation of chromatin, activation of caspases, and activation of ERK1/2 MAP kinases, features previously reported for OKA and dinophysistoxin-2. Also, differential sensitivity to 19-epi-OKA was observed between neuronal and glial cells, a specific characteristic shared by OKA and dinophysistoxin-2 but not by other toxins. Our results are consistent with 19-epi-OKA being included among the group of toxins of OKA and derivatives and support the suitability of cellular bioassays for the detection of these compounds. [ABSTRACT FROM PUBLISHER]

Published

2013

95. Protein phosphatase 1 inhibits p53 signaling by dephosphorylating and stabilizing Mdmx

Author

Lu, Zengxin, Wan, Guohui, Guo, Huarong, Zhang, Xinna, and Lu, Xiongbin

Subjects

*PROTEIN phosphatase inhibitors, *P53 protein, *CELLULAR signal transduction, *DEPHOSPHORYLATION, *STABILIZING agents, *DNA damage

Abstract

Abstract: The activation and stabilization of the p53 protein play a major role in the DNA damage response. Protein levels of p53 are tightly controlled by transcriptional regulation and a number of positive and negative posttranslational modifiers, including kinases, phosphatases, E3 ubiquitin ligases, deubiquitinases, acetylases and deacetylases. One of the primary p53 regulators is Mdmx. Despite its RING domain and structural similarity with Mdm2, Mdmx does not have an intrinsic ligase activity, but inhibits the transcriptional activity of p53. Previous studies reported that Mdmx is phosphorylated and destabilized in response to DNA damage stress. Three phosphorylation sites identified are Ser342, Ser367, and Ser403. In the present study, we identify protein phosphatase 1 (PP1) as a negative regulator in the p53 signaling pathway. PP1 directly interacts with Mdmx and specifically dephosphorylates Mdmx at Ser367. The dephosphorylation of Mdmx increases its stability and thereby inhibits p53 activity. Our results suggest that PP1 is a crucial component in the ATM-Chk2-p53 signaling pathway. [Copyright &y& Elsevier]

Published

2013

96. Schizophrenia susceptibility and NMDA-receptor mediated signalling: an association study involving 32 tagSNPs of DAO, DAOA, PPP3CC, and DTNBP1 genes.

Author

Sacchetti, Emilio, Scassellati, Catia, Minelli, Alessandra, Valsecchi, Paolo, Bonvicini, Cristian, Pasqualetti, Patrizio, Galluzzo, Alessandro, Pioli, Rosaria, and Gennarell, Massimo

Subjects

*SCHIZOPHRENIA, *METHYL aspartate receptors, *CELLULAR signal transduction, *AMINO acid oxidase, *ESTIMATION theory, *PROTEIN phosphatase inhibitors

Abstract

Background: Recent studies supported associations between four NMDA-receptor-mediated signalling genes (D-amino acid oxidase, DAO; D-amino acid oxidase activator, DAOA; protein phosphatase 3 catalytic subunit gamma isoform, PPP3CC; dystrobrevin-binding protein 1, DTNBP1) and schizophrenia susceptibility, even though with contrasting results. Methods: In an attempt to replicate these findings for the first time in an Italian population, a panel of 32 tagSNPs was analysed in a representative case-control sample involving 879 subjects. Results: An association in the allele frequency was observed for the estimated PPP3CC CAG triplotype in the SNP window rs4872499 T/C-rs11780915 A/G-rs13271367 G/A (pcorrect = 0.001). Similarly, the clustered genotype frequencies of the estimated/phased CAG triplotype differed between cases and controls (p = 0.004), with the carriers having a higher frequency in the control population (p = 0.002, odd ratio OR = 0.59, 95% confident interval CI: 0.43-0.82). Following the phenotypic dissection strategy, the analysis of single SNPs evidenced a protective effect in males of rs11780915 and rs13271367 in PPP3CC gene (pcorrect = 0.02, pcorrect = 0.04 respectively). Moreover the estimated/ phased GT diplotype (rs2070586A/G-rs3741775G/T) carriers of the DAO gene were more highly represented in female controls (p = 0.017, OR = 0.58, 95% CI: 0.37-0.90), as were the estimated/phased CAG triplotype carriers of the PPP3CC gene in females (p = 0.01, OR = 0.53, 95% CI: 0.32-0.87). In addition, we performed an interaction analysis, and a 66% (p = 0.003, OR = 0.34, 95% CI: 0.17-0.70) lower risk of developing schizophrenia for female (CAG + GT) carriers versus non-CAG or -GT carriers was observed. For DTNBP1, we found a protective effect in males for the rs6459409 (pcorrect = 0.02) and the estimated/phased CT diplotype (rs6459409-rs9476886) carriers (p = 3x10-4, OR = 0.46, 95% CI: 0.30-0.70). In relation to diagnostic subtypes, the estimated/phased DAO GT diplotype and PPP3CC CAG triplotype female carriers were found to show relative risk ratio (RRR) values of 0.52 and 0.54 lower risk for a paranoid phenotype respectively. Conclusions: Although the results are preliminary and needed replication in a larger sample, this study suggests that NMDA receptor-mediated signalling genes (DAO, PPP3CC, DTNBP1) might be involved in schizophrenia pathogenic mechanisms related to gender. [ABSTRACT FROM AUTHOR]

Published

2013

97. The PP2A Inhibitor I2PP2A Is Essential for Sister Chromatid Segregation in Oocyte Meiosis II

Author

Chambon, Jean-Philippe, Touati, Sandra A., Berneau, Stéphane, Cladière, Damien, Hebras, Céline, Groeme, Rachel, McDougall, Alex, and Wassmann, Katja

Subjects

*PROTEIN phosphatase inhibitors, *SISTER chromatid exchange, *CHROMOSOME segregation, *OVUM, *MEIOSIS, *CELL division, *SEPARASE

Abstract

Summary: Haploid gametes are generated through two consecutive meiotic divisions, with the segregation of chromosome pairs in meiosis I and sister chromatids in meiosis II. Separase-mediated stepwise removal of cohesion, first from chromosome arms and later from the centromere region, is a prerequisite for maintaining sister chromatids together until their separation in meiosis II [1]. In all model organisms, centromeric cohesin is protected from separase-dependent removal in meiosis I through the activity of PP2A-B56 phosphatase, which is recruited to centromeres by shugoshin/MEI-S332 (Sgo) [2–5]. How this protection of centromeric cohesin is removed in meiosis II is not entirely clear; we find that all the PP2A subunits remain colocalized with the cohesin subunit Rec8 at the centromere of metaphase II chromosomes. Here, we show that sister chromatid separation in oocytes depends on a PP2A inhibitor, namely I2PP2A. I2PP2A colocalizes with the PP2A enzyme at centromeres at metaphase II, independently of bipolar attachment. When I2PP2A is depleted, sister chromatids fail to segregate during meiosis II. Our findings demonstrate that in oocytes I2PP2A is essential for faithful sister chromatid segregation by mediating deprotection of centromeric cohesin in meiosis II. [Copyright &y& Elsevier]

Published

2013

98. Involvement of GSK3 and PP2A in ginsenoside Rb1's attenuation of aluminum-induced tau hyperphosphorylation

Author

Zhao, Hai-hua, Di, Jing, Liu, Wen-su, Liu, Hui-li, Lai, Hong, and Lü, Yong-li

Subjects

*GLYCOGEN synthase kinase-3, *GINSENOSIDES, *ALUMINUM in the body, *PHOSPHORYLATION, *ALZHEIMER'S disease, *PROTEIN phosphatase inhibitors

Abstract

Abstract: Environmental agent aluminum, a well-known neurotoxin, has been proposed to play a role in the development of Alzheimer''s disease (AD), and produced clinical and pathological features which were strikingly similar to those seen in AD brain, such as neurofibrillary tangles. Ginsenoside Rb1, highly abundant active component of ginseng, has been demonstrated to be neuroprotective against various neurotoxins. In this study we investigated the effect of Rb1 on aluminum-induced tau hyperphosphorylation in ICR mice. Mice were exposed to aluminum chloride (200mg/kg/day) for 6 months followed by a post treatment of Rb1 (20mg/kg/day) for another 4 months. Aluminum exposure induced the cognitive ability by Morris water maze, and upregulated the tau phosphorylation level at Ser396 accompanied by increasing p-GSK and decreasing PP2A level in motor, sensory cortex and hippocampal formation. Post treatment of Rb1 significantly improved the learning and memory and reduced the tau phosphorylation by reversing the p-GSK3 and PP2A level. Our results indicate that ginsenoside Rb1 protected mice against Al-induced toxicity. The possible mechanism may be its role in preventing tau hyperphosphorylation by regulating p-GSK3 and PP2A level, which implicate Rb1 as the potential preventive drug candidate for AD and other tau pathology-related neuronal degenerative diseases. [Copyright &y& Elsevier]

Published

2013

99. Decoy peptides targeted to protein phosphatase 1 inhibit dephosphorylation of phospholamban in cardiomyocytes

Author

Oh, Jae Gyun, Kim, Jihwa, Jang, Seung Pil, Nguen, Mai, Yang, Dong Kwon, Jeong, Dongtak, Park, Zee Yong, Park, Sung-Gyoo, Hajjar, Roger J., and Park, Woo Jin

Subjects

*PROTEIN phosphatase inhibitors, *HEART cells, *PEPTIDES, *DEPHOSPHORYLATION, *PHOSPHOLAMBAN, *PHOSPHOPROTEIN phosphatases, *SARCOPLASMIC reticulum, *PHOSPHORYLATION

Abstract

Abstract: Cardiac sarcoplasmic reticulum Ca2+-ATPase (SERCA2a) plays a crucial role in Ca2+ handling in cardiomyocytes. Phospholamban (PLB) is an endogenous inhibitor of SERCA2a and its inhibitory activity is enhanced via dephosphorylation by protein phosphatase 1 (PP1). Therefore, the inhibition of PP1-mediated dephosphorylation of PLB might be an efficient strategy for the restoration of reduced SERCA2a activity in failing hearts. We sought to develop decoy peptides that would mimic phosphorylated PLB and thus competitively inhibit the PP1-mediated dephosphorylation of endogenous PLB. The phosphorylation sites Ser16 and Thr17 are located within the flexible loop region (amino acids 14–22) of PLB. We therefore synthesized a 9-mer peptide derived from this region (ΨPLB-wt) and two pseudo-phosphorylated peptides where Ser16 was replaced with Glu (ΨPLB-SE) or Thr17 was replaced with Glu (ΨPLB-TE). These peptides were coupled to the cell-permeable peptide TAT to facilitate cellular uptake. Treatment of adult rat cardiomyocytes with ΨPLB-SE or ΨPLB-TE, but not with ΨPLB-wt, significantly elevated the phosphorylation levels of PLB at Ser16 and Thr17. This increased phosphorylation of PLB correlated with an increase in contractile parameters in vitro. Furthermore, the perfusion of isolated rat hearts with ΨPLB-SE or ΨPLB-TE, but not with ΨPLB-wt, significantly improved left ventricular developed pressure that had been previously impaired by ischemia. These data indicate that ΨPLB-SE and ΨPLB-TE efficiently prevented dephosphorylation of PLB by serving as decoys for PP1. Therefore, these peptides may provide an effective modality to regulate SERCA2a activity in failing hearts. [Copyright &y& Elsevier]

Published

2013

100. Sucrose transport is inhibited by okadaic acid during regeneration of sugar-starved Vicia faba root meristem cells

Author

Polit, Justyna T. and Nazarski, Ryszard B.

Subjects

*SUCROSE, *REGENERATION (Botany), *FATTY acids, *PROTEIN phosphatase inhibitors, *INVERTASE, *GLUCOKINASE, *SUCROSE synthase, *FAVA bean, *MERISTEMS

Abstract

Abstract: The sucrose-induced resumption of cell cycle in the Vicia faba root meristem cells, blocked in two principal control points PCP1/2 by carbohydrate starvation, occurs after 12h of metabolic regeneration comprising increased activity of sucrose synthase (SuSy) and hexokinase (HK) as well as starch grain and cell wall matrix polysaccharide biosynthesis. Okadaic acid (OA), the specific protein phosphatase 1/2A inhibitor, supplied at the beginning of the recovery period (0–3h) completely blocks these processes, making cell cycle resumption impossible. On the other hand, when added at the end (9–12h), OA has a weak inhibitory effect. The aim of these studies was: (1) to establish how sucrose is transported into the cells and whether the above-mentioned effects are correlated with the intensity of its uptake at the beginning and at the end of the metabolic regeneration; and (2) to determine whether OA, blocking sucrose metabolism, also interferes with the process of sucrose uptake and distribution. The level of [3H]sucrose uptake was measured by liquid scintillation counting while sugar distribution was analyzed using microautoradiography and electron microscopy. The results showed that sucrose entered the meristematic cells along symplastic or apoplastic pathways and, to a lesser extent, through endocytosis. The cytoplasmic compartments (endoplasmic reticulum, vacuoles, plastids) and the nucleus were labeled. The intensity of [3H]sucrose uptake was nearly 2-fold lower during the initial than during the final period of metabolic regeneration. OA inhibited the apoplastic pathway of radioactive molecule uptake and its distribution between cell compartments, implicating PP1/2A involvement in the regulation of this transport. [Copyright &y& Elsevier]

Published

2013