Your search keyword '"Sphingosine kinase-1"' showing total 32 results

1. Feline mammary carcinoma-derived extracellular vesicle promotes liver metastasis via sphingosine kinase-1-mediated premetastatic niche formation.

Author

Chang, Yi-Chih, Liu, Hao-Ping, Chuang, Hsiao-Li, Liao, Jiunn-Wang, Kao, Pei-Ling, Chan, Hsun-Lung, Chen, Ter-Hsin, and Wang, Yu-Chih

Subjects

*LIVER metastasis, *EXTRACELLULAR vesicles, *SPHINGOSINE, *SPHINGOSINE kinase, *LIVER cells

Abstract

Background: Feline mammary carcinoma (FMC) is one of the most prevalent malignancies of female cats. FMC is highly metastatic and thus leads to poor disease outcomes. Among all metastases, liver metastasis occurs in about 25% of FMC patients. However, the mechanism underlying hepatic metastasis of FMC remains largely uncharacterized. Results: Herein, we demonstrate that FMC-derived extracellular vesicles (FMC-EVs) promotes the liver metastasis of FMC by activating hepatic stellate cells (HSCs) to prime a hepatic premetastatic niche (PMN). Moreover, we provide evidence that sphingosine kinase 1 (SK1) delivered by FMC-EV was pivotal for the activation of HSC and the formation of hepatic PMN. Depletion of SK1 impaired cargo sorting in FMC-EV and the EV-potentiated HSC activation, and abolished hepatic colonization of FMC cells. Conclusions: Taken together, our findings uncover a previously uncharacterized mechanism underlying liver-metastasis of FMC and provide new insights into prognosis and treatment of this feline malignancy. [ABSTRACT FROM AUTHOR]

Published

2023

2. Advancements on the Multifaceted Roles of Sphingolipids in Hematological Malignancies.

Author

Raza, Yasharah, Atallah, Jane, and Luberto, Chiara

Subjects

*HEMATOLOGIC malignancies, *SPHINGOLIPIDS, *SPHINGOSINE kinase, *ACUTE myeloid leukemia, *AMIDASES, *LEUKEMIA

Abstract

Dysregulation of sphingolipid metabolism plays a complex role in hematological malignancies, beginning with the first historical link between sphingolipids and apoptosis discovered in HL-60 leukemic cells. Numerous manuscripts have reviewed the field including the early discoveries that jumpstarted the studies. Many studies discussed here support a role for sphingolipids, such as ceramide, in combinatorial therapeutic regimens to enhance anti-leukemic effects and reduce resistance to standard therapies. Additionally, inhibitors of specific nodes of the sphingolipid pathway, such as sphingosine kinase inhibitors, significantly reduce leukemic cell survival in various types of leukemias. Acid ceramidase inhibitors have also shown promising results in acute myeloid leukemia. As the field moves rapidly, here we aim to expand the body of literature discussed in previously published reviews by focusing on advances reported in the latter part of the last decade. [ABSTRACT FROM AUTHOR]

Published

2022

3. 鞘鞍醇激酶-1抑制剂 PF-543 改善1型糖尿病心肌纤维化的实验研究.

Author

史承勇, 刁繁荣, 蒋颖人, 宋晓伟, 唐文栋, 郭显, and 赵仙先

Abstract

Objective: This study was aimed to explore the effects of PF-543, a specific inhibitor of sphingosine kinase-1(SphK1),on cardiac fibrosis in type 1 diabetes mice. Methods: Sixty eight-week-old C57 BL6 J mice were randomly divided into control group(n=15), control+PF-543 group(n=15), type 1 diabetes mellitus(T1 DM)group(n=15), and T1 DM+PF-543 group(n=15). T1 DM were induced by intraperitoneally injected with streptozocin(STZ, 150 mg/kg). These control and diabetic mice were randomly received with vehicle or PF-543(10 mg/kg/d) treatment for 16 weeks. By the end of the study, cardiac sphingosine 1 phosphate(S1 P) levels were analyzed by enzyme linked immunosorbent assay(ELISA). Cardiac function was evaluated by echocardiography. Myocardial fibrosis was evaluated by masson trichrome staining. The cardiac expression levels of transforming growth factor-β1(TGF-β1), Collagen I(Col I)and Collagen III(Col III) were determined by Western blot. Results: Compared with T1 DM group, cardiac S1 P levels were significantly reduced in T1 DM+PF-543 group(P<0.05). PF-543 significantly increased the left ventricular ejection fractions(LVEF) in diabetic mice(65.7 ±3.3% vs 54.4 ±3.4%, P<0.05). PF-543 alsodecreased the left ventricular end-diastolic diameters(LVEDD) in diabetic mice(3.81±0.21 mm vs 4.52±0.20 mm P<0.05). Moreover, PF-543 treatment reduced interstitial fibrosis in diabetic mice(7.13±0.32% vs10.21±0.41%, P<0.05). the cardiac expression of TGF-β1, Col I and Col III were significantly reduced by PF-543 treatment in type 1 diabetic mice(all P<0.05). Conclusion: PF-543 treatment significantly reduces cardiac S1 P levels and ameliorates myocardial fibrosis by decreasing TGF-β1 and collagen expression in type 1 diabetic mice. [ABSTRACT FROM AUTHOR]

Published

2019

4. Sphingosine kinase 1 protects renal tubular epithelial cells from renal fibrosis via induction of autophagy.

Author

Du, Chunyang, Ren, Yunzhuo, Yao, Fang, Duan, Jialiang, Zhao, Hui’er, Du, Yunxia, Xiao, Xia, Duan, Huijun, and Shi, Yonghong

Subjects

*SPHINGOSINE kinase, *EPITHELIAL cells, *RENAL fibrosis, *AUTOPHAGY, *HOMEOSTASIS, *PROTEOLYSIS

Abstract

Autophagy is an important homoeostatic mechanism for the lysosomal degradation of protein aggregates and damaged cytoplasmic components. Recent studies suggest that autophagy which is induced by TGF-β1 suppresses kidney fibrosis in renal tubular epithelial cells (RTECs) of obstructed kidneys. Sphingosine kinase 1(SK1), converting sphingosine into endogenous sphingosine-1-phosphate (S1P), was shown to modulate autophagy and involved in the processes of fibrotic diseases. Since SK1 activity is also up-regulated by TGF-β1, we explored its effect on the induction of autophagy and development of renal fibrosis in this study. In vitro, SK1 expression and activity were markedly increased by TGF-β1 stimulation in a time and concentration dependent manner, and concomitant changes in autophagic response were observed in HK-2 cells. Further, knockdown of SK-1 led to a decrease of autophagy whereas overexpression of SK1 caused a greater induction of autophagy. In addition, overexpression of SK1 resulted in decreased of mature TGF-β levels through autophagic degradation. In vivo, SK1 enzymatic activity and autophagic response were both up-regulated in a mouse model of kidney fibrosis induced by unilateral ureteral obstruction (UUO); meanwhile, increased of mature TGF-β1 and deposition of extracellular matrix (ECM) were observed in tubulointerstitial areas compared with sham-operated mice. However, aggravation of renal fibrosis was detected when SK1 inhibitor PF-543 was applied to suppress SK1 enzymatic activity in UUO mice. At the same time, autophagy was also inhibited by PF-543. Thus, our findings suggest that SK1 activation is renoprotective via induction of autophagy in the fibrotic process. [ABSTRACT FROM AUTHOR]

Published

2017

5. The effects of berberine on a murine model of multiple sclerosis and the SPHK1/S1P signaling pathway.

Author

Qin, Xinyue, Luo, Jiaming, Zeng, Siyu, Yu, Juming, Jiang, Guohui, Wang, Li, and Chen, Rong

Subjects

*MULTIPLE sclerosis, *BERBERINE, *ENCEPHALOMYELITIS, *ASTROCYTES, *SPHINGOSINE-1-phosphate, *SPHINGOSINE kinase

Abstract

Berberine (BBR) has shown neuroprotective properties. The present study aims to investigate the effects of BBR on experimental autoimmune encephalomyelitis (EAE), a murine model of multiple sclerosis (MS), and SphK1/S1P signaling, which plays a key role in MS. EAE was induced in mice, followed by treatment with BBR at 50, 100, or 300 mg/kg/d. Neurophysiological function was evaluated daily; inflammation, cell infiltration, and the severity of demyelination were also examined. The SphK1, SphK2, and S1P levels in the animals and primary astrocyte culture were measured. We found that treatment with BBR reduced the loss of neurophysiological function and the degree of demyelination. Moreover, BBR was associated with a decrease in SphK1 and S1P levels both in the animals and in culture. These results indicated that BBR suppresses demyelination and loss of neurophysiological function by inhibiting the SphK1/S1P signaling pathway. The use of BBR as a treatment of MS warrant further exploration. [ABSTRACT FROM AUTHOR]

Published

2017

6. Sphingosine Kinase-1 Involves the Inhibitory Action of HIF-1α by Chlorogenic Acid in Hypoxic DU145 Cells.

Author

Myoung-Sun Lee, Seon-Ok Lee, Kyu-Ri Kim, and Hyo-Jeong Lee

Subjects

*SPHINGOSINE kinase, *SPHINGOSINE, *CHLOROGENIC acid, *TRANSCRIPTION factors, *PATHOPHYSIOLOGY of anoxemia, *CANCER diagnosis, *PHYSIOLOGY

Abstract

Hypoxia enhances cancer development in a solid tumor. Hypoxia-inducible factor-1 α (HIF-1α) is a transcription factor that is dominantly expressed under hypoxia in solid tumor cells and is a key factor that regulates tumor. HIF-1α regulates several target genes involved in many aspects of cancer progression, including angiogenesis, metastasis, anti-apoptosis and cell proliferation as well as imparts resistance to cancer treatment. In this study, we assessed Crataegus Pinnatifida Bunge var. typical Schneider ethanol extract (CPE) for its anti-cancer effects in hypoxia-induced DU145 human prostate cancer cell line. CPE decreased the abundance of HIF-1α and sphingosine kinase-1 (SPHK-1) in hypoxia-induced prostate cancer DU145 cells. CPE decreased HIF-1α and SPHK-1 as well as SPHK-1 activity. Chlorogenic acid (CA) is one of four major compounds of CPE. Compared to CPE, CA significantly decreased the expression of HIF-1α and SPHK-1 as well as SPHK-1 activity in hypoxia-induced DU145 cells. Furthermore, CA decreased phosphorylation AKT and GSK-3β, which are associated with HIF-1α stabilization and affected SPHK-1 in a concentration-dependent manner. We confirmed the mechanism of CA-induced inhibition of HIF-1α by SPHK-1 signaling pathway using SPHK-1 siRNA and SPHK inhibitor (SKI). CA decreased the secretion and cellular expression of VEGF, thus inhibiting hypoxia-induced angiogenesis. Treatment of DU145cells with SPHK1 siRNA and CA for 48 h decreased cancer cell growth, and the inhibitory action of SPHK siRNA and CA on cell growth was confirmed by decrease in the abundance of Proliferating cell nuclear antigen (PCNA). [ABSTRACT FROM AUTHOR]

Published

2017

7. Selective inhibition of sphingosine kinase-1 protects adipose tissue against LPS-induced inflammatory response in Zucker diabetic fatty rats.

Author

Tous, Monica, Ferrer-Lorente, Raquel, and Badimon, Lina

Subjects

*SPHINGOSINE kinase, *SELECTIVE inhibition (Chemistry), *TREATMENT of diabetes, *ADIPOSE tissues, *CHEMOKINES, *ZUCKER rats

Abstract

Obesity is associated with a state of chronic inflammation. The chemokine (C-C motif) ligand 5 (CCL5) has been proposed to modulate the inflammatory response in adipose tissue (AT). However, the mechanisms underlying CCL5 upregulation in AT remain undefined. The objective of the present study was to evaluate whether the enzyme sphingosine kinase-1 (SK1) would modulate the expression of CCL5 and other inflammatory biomarkers in primary adipocytes and its potential role in lipopolysaccharide (LPS)-induced AT inflammation in a rat model of diabetes. To address this, LPS-stimulated primary adipocytes and 3T3-L1 cells were treated with a SK inhibitor, and the expression of Ccl5 and other CC chemokines were studied. Moreover, the effect of SK1 knockdown on cytokine production was analyzed in 3T3-L1 cells by transfection of SK1-specific smallinterfering RNA (siRNA). The anti-inflammatory effects of SK inhibitor in AT were also investigated in vivo using the Zucker lean normoglycemic control (ZLC) rats. LPS treatment stimulated Ccl5, IL-6, pentraxin 3 (Ptx3), and Tnfα mRNA expression in primary adipocytes and 3T3-L1 cells, whereas pharmacologically and siRNA-mediated SK1 inhibition strongly reduced mRNA levels of proinflammatory cytokines in these cells. Similarly, administration of SK inhibitor to ZLC rats prevented the LPS-induced inflammatory response in AT. Our data demonstrate a role for SK1 in endotoxin-induced cytokine expression in adipocytes and suggest that inhibition of SK1 may be a potential therapeutic tool in the prevention and treatment of chronic and common metabolic disorders, including obesity, insulin-resistance, and type 2 diabetes. [ABSTRACT FROM AUTHOR]

Published

2014

8. Sphingosine Kinase-1 Protects Differentiated N2a Cells Against Beta-Amyloid25-35-Induced Neurotoxicity Via the Mitochondrial Pathway.

Author

Yang, Yang, Wang, Min, Lv, Bingjie, Ma, Rong, Hu, Jing, Dun, Yaoyan, Sun, Shenggang, and Li, Gang

Subjects

*SPHINGOSINE kinase, *AMYLOID beta-protein, *MITOCHONDRIA, *NEUROTOXICOLOGY, *ALZHEIMER'S disease, *DISEASE progression, *SPHINGOMYELIN

Abstract

Although the etiology of Alzheimer's disease (AD) is not fully understood, multiple lines of evidence suggests the importance of amyloid-β (Aβ) in the initiation/progression of the disease. Aβ has been shown to induce neuronal apoptosis via the sphingomyelin/ceramide pathway. This study was designed to elucidate whether the sphingosine kinase-1 (SPK1), a critical regulator of the ceramide/sphingosine 1-phosphate rheostat, plays a pivotal role in the regulation of death and survival of differentiated neuro-2a cells in response to beta-amyloid peptide fragment 25-35 (Aβ25-35). These results show that the expression of SPK1 was markedly decreased in Aβ25-35-induced neurotoxicity, as evidenced by the decreased cell viability and the increased apoptotic rate. Overexpression of SPK1 significantly attenuated Aβ25-35-induced neurotoxicity, whereas silencing the expression of SPK1 exacerbated it. Moreover, overexpression of SPK1 can significantly attenuate Aβ25-35-induced upregulation of Bax and rehabilitate the level of Bcl-2; concomitantly, it can ameliorate mitochondrial ultrastructure. These studies demonstrate that overexpression of SPK1 may moderate Aβ25-35-induced neurotoxicity by regulating the Bcl-2/Bax ratio and improving mitochondrial ultrastructure. Based on these findings, SPK1 is a potential therapeutic target for AD. [ABSTRACT FROM AUTHOR]

Published

2014

9. Factor-Xa-induced mitogenesis and migration require sphingosine kinase activity and S1P formation in human vascular smooth muscle cells.

Author

Böhm, Andreas, Flößer, Anja, Ermler, Swen, Fender, Anke C., Lüth, Anja, Kleuser, Burkhard, Schrör, Karsten, and Rauch, Bernhard H.

Subjects

*SPHINGOSINE kinase, *BLOOD coagulation factors, *VASCULAR smooth muscle, *MUSCLE cells, *SPHINGOSINE-1-phosphate, *CELLULAR signal transduction, *GENETIC transcription

Abstract

Aims Sphingosine-1-phosphate (S1P) is a cellular signalling lipid generated by sphingosine kinase-1 (SPHK1). The aim of the study was to investigate whether the activated coagulation factor-X (FXa) regulates SPHK1 transcription and the formation of S1P and subsequent mitogenesis and migration of human vascular smooth muscle cells (SMC). Methods and results FXa induced a time- (3–6 h) and concentration-dependent (3–30 nmol/L) increase of SPHK1 mRNA and protein expression in human aortic SMC, resulting in an increased synthesis of S1P. FXa-stimulated transcription of SPHK1 was mediated by the protease-activated receptor-1 (PAR-1) and PAR-2. In human carotid artery plaques, expression of SPHK1 was observed at SMC-rich sites and was co-localized with intraplaque FX/FXa content. FXa-induced SPHK1 transcription was attenuated by inhibitors of Rho kinase (Y27632) and by protein kinase C (PKC) isoforms (GF109203X). In addition, FXa rapidly induced the activation of the small GTPase Rho A. Inhibition of signalling pathways which regulate SPHK1 expression, inhibition of its activity or siRNA-mediated SPHK1 knockdown attenuated the mitogenic and chemotactic response of human SMC to FXa. Conclusion These data suggest that FXa induces SPHK1 expression and increases S1P formation independent of thrombin and that this involves the activation of Rho A and PKC signalling. In addition to its key function in coagulation, this direct effect of FXa on human SMC may increase cell proliferation and migration at sites of vessel injury and thereby contribute to the progression of vascular lesions. [ABSTRACT FROM PUBLISHER]

Published

2013

10. Sphingosine-1-phosphate: A Janus-faced mediator of fibrotic diseases

Author

Schwalm, Stephanie, Pfeilschifter, Josef, and Huwiler, Andrea

Subjects

*SPHINGOSINE-1-phosphate, *FIBROSIS, *G protein coupled receptors, *CELL membranes, *NEOVASCULARIZATION, *CARCINOGENESIS, *IMMUNITY

Abstract

Abstract: Sphingosine-1-phosphate (S1P) is a pleiotropic lipid mediator that acts either on G protein-coupled S1P receptors on the cell surface or via intracellular target sites. In addition to the well established effects of S1P in angiogenesis, carcinogenesis and immunity, evidence is now continuously accumulating which demonstrates that S1P is an important regulator of fibrosis. The contribution of S1P to fibrosis is of a Janus-faced nature as S1P exhibits both pro- and anti-fibrotic effects depending on its site of action. Extracellular S1P promotes fibrotic processes in a S1P receptor-dependent manner, whereas intracellular S1P has an opposite effect and dampens a fibrotic reaction by yet unidentified mechanisms. Fibrosis is a result of chronic irritation by various factors and is defined by an excess production of extracellular matrix leading to tissue scarring and organ dysfunction. In this review, we highlight the general effects of extracellular and intracellular S1P on the multistep cascade of pathological fibrogenesis including tissue injury, inflammation and the action of pro-fibrotic cytokines that stimulate ECM production and deposition. In a second part we summarize the current knowledge about the involvement of S1P signaling in the development of organ fibrosis of the lung, kidney, liver, heart and skin. Altogether, it is becoming clear that targeting the sphingosine kinase-1/S1P signaling pathway offers therapeutic potential in the treatment of various fibrotic processes. This article is part of a Special Issue entitled Advances in Lysophospholipid Research. [Copyright &y& Elsevier]

Published

2013

11. Sphingosine kinase-1/sphingosine-1-phosphate receptor type 1 signalling axis is induced by transforming growth factor-β1 and stimulates cell migration in RAW264.7 macrophages

Author

Li, Changyong, Yang, Guohua, and Ruan, Jie

Subjects

*SPHINGOSINE kinase, *SPHINGOSINE-1-phosphate, *MACROPHAGES, *SMALL interfering RNA, *TRANSFORMING growth factors-beta, *RNA interference, *CELLULAR signal transduction, *CELL migration

Abstract

Abstract: Macrophage recruitment to sites of inflammation is an essential step in host defense. However, the signals regulating the mobilization of these cells are still not fully understood. Sphingosine-1-phosphate (S1P), a pleiotropic bioactive lipid mediator, is known to regulate an array of biological activities in various cell types. Here, we investigated the roles of S1P and S1P receptors (S1PRs) in macrophage migration in vitro. Furthermore, we explored the cross-talk between transforming growth factor-β1 (TGF-β1) and S1P signalling pathways in this process. We found that S1P exerted a powerful migratory action on RAW264.7 macrophages, as determined in Boyden chambers. Moreover, by employing RNA interference technology and pharmacological tools, we have demonstrated that S1PR1, but not S1PR2 and S1PR3, is required for S1P-induced macrophage migration. Importantly, we observed a pronounced increase in sphingosine kinase-1 (SphK1) mRNA expression and subsequently increase in S1P production, following transforming growth factor-β1 (TGF-β1) stimulation in RAW264.7 macrophages. The expression of S1PR1, but not S1PR2 and S1PR3, was also significantly up-regulated after TGF-β1 stimulation. Interestingly, exogenously added S1P-induced up-regulation of SphK1 and the synthesis of additional S1P, suggesting a self-amplifying loop of S1P to enhance macrophage migration. In conclusion, our results reveal that SphK1/S1PR1 signalling axis is induced by TGF-β1 and stimulates cell migration in RAW 264.7 macrophages. This study provides new clues for the molecular mechanisms of macrophage recruitment during inflammation. [Copyright &y& Elsevier]

Published

2012

12. Co-administration phenoxodiol with doxorubicin synergistically inhibit the activity of sphingosine kinase-1 (SphK1), a potential oncogene of osteosarcoma, to suppress osteosarcoma cell growth both in vivo and in vitro

Author

Yao, Chen, Wu, Sujia, Li, Dong, Ding, Huimin, Wang, Zuyu, Yang, Yongjiang, Yan, Shichang, and Gu, Zhangping

Subjects

*OSTEOSARCOMA, *ADENOSINE diphosphate, *SPHINGOSINE kinase, *PHOSPHOPROTEIN phosphatases, *APOPTOSIS, *SPHINGOSINE, *DOXORUBICIN, *CANCER cell growth

Abstract

Abstract: Elucidation of the mechanisms of chemo-resistance and implementation of strategies to overcome it will be pivotal to improve the survival for osteosarcoma (OS) patients. We here suggest that sphingosine kinase-1 (SphK1) might be the key factor contributing to chemo-resistance in OS. Our Western-blots and immunohistochemistry results showed that SphK1 is over-expressed in multiple clinical OS tissues. Over-expression of SphK1 in OS cell line U2OS promoted its growth and endorsed its resistance against doxorubicin, while knocking-down of SphK1 by shRNA inhibited U2OS cell growth and increased its sensitivity to doxorubicin. Co-administration phenoxodiol with doxorubicin synergistically inhibited SphK1 activity to trigger cellular ceramide accumulation, and achieved synergistic anti-OS growth effect, accompanied with a significant increased of apoptosis and cytotoxicity. Increased cellular level of ceramide by the co-administration induced the association between Akt and Protein Phosphatase 1 (PP1) to dephosphorylate Akt, and to introduce a constitutively active Akt (CA-Akt) restored Akt activation and diminished cell growth inhibition. Further, phenoxodiol and doxorubicin synergistically activated apoptosis signal-regulating kinase 1(ASK1)/c-jun-NH2-kinase (JNK) signaling, which also contributed to cell growth inhibition. Significantly, the role of SphK1 in OS cell growth and the synergistic anti-OS effect of phenoxodiol and doxorubicin were also seen in a mice OS xenograft model. In conclusion, our data suggest that SphK1 might be a critical oncogene of OS and co-administration phenoxodiol with doxorubicin synergistically inhibited the activity of SphK1 to suppress osteosarcoma cell growth both in vivo and in vitro. [Copyright &y& Elsevier]

Published

2012

13. Isoflurane delays the development of early brain injury after subarachnoid hemorrhage through sphingosine-related pathway activation in mice.

Author

Altay, Orhan, Hasegawa, Yu, Sherchan, Prativa, Suzuki, Hidenori, Khatibi, Nikan H., Tang, Jiping, and Zhan, John H.

Subjects

*ISOFLURANE, *BRAIN injuries, *SUBARACHNOID hemorrhage, *LABORATORY mice, *SPHINGOSINE

Abstract

The article discusses a study which examined whether isoflurane posttreat-ment is protective against early brain injury after subarachnoid hemorrhage in mice. It also determined whether this effect needs sphingosine-related pathway activation. The study concluded that soflurane posttreatment would result in the delay of the development of postsubarachnoid hemorrhage early brain injury through antiapoptotic mechanisms including sphingosine-related pathway activation.

Published

2012

14. Sphingosine kinase-1 activity and expression in human prostate cancer resection specimens

Author

Malavaud, Bernard, Pchejetski, Dimitri, Mazerolles, Catherine, de Paiva, Geisilène Russano, Calvet, Cyril, Doumerc, Nicolas, Pitson, Stuart, Rischmann, Pascal, and Cuvillier, Olivier

Subjects

*SPHINGOSINE, *PROTEIN kinases, *GENE expression, *PROSTATE cancer, *SURGICAL excision, *PROSTATECTOMY, *STATISTICAL correlation, *PROSTATE surgery, *CONFIDENCE intervals, *EPIDEMIOLOGY, *FISHER exact test, *IMMUNOHISTOCHEMISTRY, *LONGITUDINAL method, *PHOSPHOTRANSFERASES, *PROBABILITY theory, *PROSTATE tumors, *RESEARCH funding, *STATISTICS, *T-test (Statistics), *TUMOR classification, *PROSTATE-specific antigen, *DATA analysis, *TREATMENT effectiveness, *SURGICAL site, *TISSUE arrays

Abstract

Purpose: Sphingosine kinase-1 (SphK1) was shown in preclinical models and non-genitourinary cancers to be instrumental in cancer progression, adaptation to hypoxia and in tumour angiogenesis. No data were available in human prostate cancer. The present study was designed to assess SphK1 expression and activity in radical prostatectomy specimens and to research correlations with clinical features. Materials and methods: Transverse section of fresh tissue was obtained from 30 consecutive patients undergoing laparoscopic prostatectomy. SphK1 enzymatic activities of tumour and normal counterpart were determined. Relationships with PSA, Gleason sum, pathological stage, resection margin status and treatment failure were researched. SphK1 pattern of expression was then assessed on tissue microarray. Results: A significant 2-fold increase in SphK1 enzymatic activity(11.1±8.4 versus 5.9±3.2 (P <0.04)) was observed in cancer. The upper quartile of SphK1 activity was associated with higher PSA (16.7 versus 6.4ng/ml, P =0.04), higher tumor volumes (20.7 versus 9.8, P =0.002), higher rates of positive margins (85.7% versus 28.6%, P =0.01) and surgical failure (71.4% versus 9.5%, P =0.003) than the lower three quartiles. Odds ratios (OR) for treatment failure showed a strong relationship with SphK1 activity (OR: 23.7, P =0.001), positive resection margins (OR: 15.0, P =0.007) and Gleason sum (⩾4+3, OR: 8.0, P =0.003). Tissue microarrays showed discrete epithelial expression that varied with Gleason sum with significant relationship between SphK1 expression and higher Gleason sum. Conclusion: In complement to preclinical literature, the demonstrated relationships between SphK1-increased activity in cancer and relevant clinical features confirm a central role for SphK1 in prostate cancer that herald promising avenues in risk-assessment and treatment. [Copyright &y& Elsevier]

Published

2010

15. Sphingosine kinase-1/S1P1 signalling axis negatively regulates mitogenic response elicited by PDGF in mouse myoblasts

Author

Nincheri, Paola, Bernacchioni, Caterina, Cencetti, Francesca, Donati, Chiara, and Bruni, Paola

Subjects

*PLATELET-derived growth factor, *SPHINGOSINE, *CELLULAR signal transduction, *GENETIC regulation, *MITOGENS, *MYOBLASTS, *LABORATORY mice, *MOLECULAR biology

Abstract

Abstract: PDGF is known to be critically implicated in skeletal muscle repair; however its molecular mechanism of action has been only marginally investigated. In this study we show that in mouse myoblasts PDGF transactivates S1P1 receptor via sphingosine kinase (SK)-1 activation and that this molecular event exerts a negative regulation of the mitogenic effect elicited by this growth factor. Indeed, pharmacological inhibition of S1P1, or its specific silencing increased PDGF-dependent cell proliferation, whereas S1P1 overexpression diminished the biological effect. Moreover, the mitogenic response to PDGF was enhanced by pharmacological inhibition of SK activity as well as specific silencing of SK1 but not SK2. Furthermore, ERK1/2 signalling pathway was found to be upstream of the observed attenuation of PDGF-induced cell proliferation. Interestingly, PDGF-directed engagement of S1P1 exerted also a positive modulatory action of the growth factor-dependent cell motility. The here highlighted dual role of S1P1-mediated signalling in response to myoblast challenge with PDGF is likely important to guarantee the fine control of the biological response to this growth factor, finalized to efficient repopulation of skeletal muscle after damage, where a tight balance between proliferation and migration of tissue progenitor cells is required. [ABSTRACT FROM AUTHOR]

Published

2010

16. Spred2 is involved in imatinib-induced cytotoxicity in chronic myeloid leukemia cells

Author

Liu, Xiao-Yun, Yang, Yue-Feng, Wu, Chu-Tse, Xiao, Feng-Jun, Zhang, Qun-Wei, Ma, Xiao-Ni, Li, Qing-Fang, Yan, Jun, Wang, Hua, and Wang, Li-Sheng

Subjects

*RAS proteins, *CELLULAR signal transduction, *MYELOID leukemia, *IMATINIB, *HEMATOLOGIC malignancies, *ADENOVIRUSES, *SPHINGOSINE, *CELL-mediated cytotoxicity

Abstract

Abstract: Spreds, a recently established class of negative regulators of the Ras–ERK (extracellular signal-regulated kinase) pathway, are involved in hematogenesises, allergic disorders and tumourigenesis. However, their role in hematologic neoplasms is largely unknown. Possible effects of Spreds on other signal pathways closely related to Ras–ERK have been poorly investigated. In this study, we investigated the in vitro effects of Spred2 on chronic myeloid leukemia (CML) cells. In addition to inhibiting the well-established Ras–ERK cascade, adenovirus-mediated Spred2 over-expression inhibits constitutive and stem cell factor (SCF)-stimulated sphingosine kinase-1 (SPHK1) and Mcl-1 expression, as well as inhibiting proliferation and inducing apoptosis in CML cells. In K562 cells and primary CML cells, imatinib induces endogenous Spred2 expression. Spred2 silencing by stable RNA interference partly protects K562 cells against imatinib-induced apoptosis. Together, these data implicate Spred2 in imatinib-induced cytotoxicity in CML cells, possibly by inhibiting the Ras–ERK cascade and the pro-survival signaling molecules SPHK1 and Mcl-1. These findings reveal potential targets for selective therapy of CML. [Copyright &y& Elsevier]

Published

2010

17. Sphingosine kinase-1 mediates androgen-induced osteoblast cell growth

Author

Martin, Claire, Lafosse, Jean-Michel, Malavaud, Bernard, and Cuvillier, Olivier

Subjects

*PROTEIN kinases, *SPHINGOSINE, *ANDROGENS, *CELL growth, *LIPIDS, *CELL proliferation, *CELLULAR signal transduction

Abstract

Abstract: Herein we report that the lipid kinase sphingosine kinase-1 (SphK1) is instrumental in mediating androgen-induced cell proliferation in osteoblasts. Dihydrotestosterone (DHT) triggered cell growth in steroid-deprived MC3T3 cells, which was associated with a rapid stimulation of SphK1 and activation of both Akt and ERK signaling pathways. This mechanism relied on functional androgen receptor/PI3K/Akt nongenotropic signaling as pharmacological antagonists could block SphK1 stimulation by DHT and its consequences. Finally, SphK1 inhibition not only abrogated DHT-induced ERK activation but also blocked cell proliferation, while ERK inhibition had no impact, suggesting that SphK1 was critical for DHT signaling yet independently of the ERK. [Copyright &y& Elsevier]

Published

2010

18. Transforming growth factor-β2 upregulates sphingosine kinase-1 activity, which in turn attenuates the fibrotic response to TGF-β2 by impeding CTGF expression.

Author

Shuyu Ren, Babelova, Andrea, Moreth, Kristin, Cuiyan Xin, Eberhardt, Wolfgang, Doller, Anke, Pavenstädt, Hermann, Schaefer, Liliana, Pfeilschifter, Josef, and Huwiler, Andrea

Subjects

*TRANSFORMING growth factors-beta, *SPHINGOSINE, *FOCAL adhesion kinase, *CONNECTIVE tissue development, *FIBROSIS, *KIDNEY diseases, *GENE expression, *MESSENGER RNA

Abstract

Transforming growth factor-β2 (TGF-β2) stimulates the expression of pro-fibrotic connective tissue growth factor (CTGF) during the course of renal disease. Because sphingosine kinase-1 (SK-1) activity is also upregulated by TGF-β, we studied its effect on CTGF expression and on the development of renal fibrosis. When TGF-β2 was added to an immortalized human podocyte cell line we found that it activated the promoter of SK-1, resulting in upregulation of its mRNA and protein expression. Further, depletion of SK-1 by small interfering RNA or its pharmacological inhibition led to accelerated CTGF expression in the podocytes. Over-expression of SK-1 reduced CTGF induction, an effect mediated by intracellular sphingosine-1-phosphate. In vivo, SK-1 expression was also increased in the podocytes of kidney sections of patients with diabetic nephropathy when compared to normal sections of kidney obtained from patients with renal cancer. Similarly, in a mouse model of streptozotocin-induced diabetic nephropathy, SK-1 and CTGF were upregulated in podocytes. In SK-1 deficient mice, exacerbation of disease was detected by increased albuminuria and CTGF expression when compared to wild-type mice. Thus, SK-1 activity has a protective role in the fibrotic process and its deletion or inhibition aggravates fibrotic disease. [ABSTRACT FROM AUTHOR]

Published

2009

19. Sphingosine kinase-1 is a hypoxia-regulated gene that stimulates migration of human endothelial cells

Author

Schwalm, Stephanie, Döll, Frauke, Römer, Isolde, Bubnova, Svetlana, Pfeilschifter, Josef, and Huwiler, Andrea

Subjects

*AMINO alcohols, *CELL lines, *HYPOXEMIA, *CELL culture

Abstract

Abstract: Sphingosine kinases (SK) catalyze the production of sphingosine-1-phosphate which in turn regulates cell responses such as proliferation and migration. Here, we show that exposure of the human endothelial cell line EA.hy 926 to hypoxia stimulates a increased SK-1, but not SK-2, mRNA, protein expression, and activity. This effect was due to stimulated SK-1 promoter activity which contains two putative hypoxia-inducible factor-responsive-elements (HRE). By deletion of one of the two HREs, hypoxia-induced promoter activation was abrogated. Furthermore, hypoxia upregulated the expression of HIF-1α and HIF-2α, and both contributed to SK-1 gene transcription as shown by selective depletion of HIF-1α or HIF-2α by siRNA. The hypoxia-stimulated SK-1 upregulation was functionally coupled to increased migration since the selective depletion of SK-1, but not of SK-2, by siRNAs abolished the migratory response. In summary, these data show that hypoxia upregulates SK-1 activity and results in an accelerated migratory capacity of endothelial cells. SK-1 may thus serve as an attractive therapeutic target to treat diseases associated with increased endothelial migration and angiogenesis such as cancer growth and progression. [Copyright &y& Elsevier]

Published

2008

20. Cyclooxygenase-2 induction by adiponectin is regulated by a sphingosine kinase-1 dependent mechanism in cardiac myocytes

Author

Ikeda, Yasumasa, Ohashi, Koji, Shibata, Rei, Pimentel, David R., Kihara, Shinji, Ouchi, Noriyuki, and Walsh, Kenneth

Subjects

*HEART diseases, *THERAPEUTICS, *CYCLOOXYGENASE 2, *GROWTH factors, *PROTEIN kinases

Abstract

Abstract: The adipose-derived plasma protein, adiponectin (APN), has various protective effects on cardiovascular diseases. In this study, we show that endogenous APN is required for full cyclooxygenase-2 (COX-2) induction by ischemia-reperfusion injury in the heart in vivo. In rat neonatal cardiac myocytes, APN-induced COX-2 expression was reduced by treatment with a sphingosine kinase-1 (SphK-1) inhibitor or siRNA targeting SphK-1. Treatment with a sphingosine-1-phosphate (S1P) receptor antagonist also diminished COX-2 expression in response to APN stimulation. These findings suggest that APN is a physiological regulator of COX-2 signaling in the heart and that this regulation occurs in part via a SphK-1–S1P receptor dependent mechanism in cardiac myocytes. [Copyright &y& Elsevier]

Published

2008

21. Sphingosine kinase-1 mediates BCR/ABL-induced upregulation of Mcl-1 in chronic myeloid leukemia cells.

Author

Li, Q.-F., Huang, W.-R., Duan, H.-F., Wang, H., Wu, C.-T., and Wang, L.-S.

Subjects

*SPHINGOSINE, *BIOGENIC amines, *MYELOID leukemia, *BONE marrow diseases, *CANCER cells, *MITOGEN-activated protein kinases

Abstract

The signaling mechanisms responsible for BCR/ABL-induced regulation of Mcl-1 expression in chronic myelogenous leukemia (CML) cells remain unclear. In this study, we show that BCR/ABL could upregulate sphingosine kinase-1 (SPK1) expression via multiple signal pathways, including mitogen-activated protein kinase (MAPK), phosphoinositide 3-kinase (PI3K) and Janus kinase 2 (JAK2), leading to increase cellular SPK1 activity in CML cells. Retrovirus-mediated overexpression of bcr-abl gene in NIH-3T3, Ba/F3 and HL-60 cells results in upregulation and increased cellular activity of SPK1, whereas treatment of CML cells with specific inhibitors of the BCR/ABL, PI3K, MAPK and JAK2 pathways decreases BCR/ABL-induced SPK1 expression and cellular activity. BCR/ABL also induces upregulation of Mcl-1 expression in CML cells. Inhibition of SPK1 by adenovirus-mediated transfer of small interfering RNA or N,N-dimethylsphingosine reduced expression of Mcl-1 in CML cells. Our data indicated that BCR/ABL induces SPK1 expression and increases its cellular activity, leading to upregulation of Mcl-1 in CML cells. SPK1 silencing enhances the STI571-induced apoptosis of CML cell lines. It is suggested that SPK1 may be a potential therapeutic target in CML.Oncogene (2007) 26, 7904–7908; doi:10.1038/sj.onc.1210587; published online 18 June 2007 [ABSTRACT FROM AUTHOR]

Published

2007

22. Adult cardiac fibroblasts null for sphingosine kinase-1 exhibit growth dysregulation and an enhanced proinflammatory response

Author

Kacimi, Rachid, Vessey, Donald A., Honbo, Norman, and Karliner, Joel S.

Subjects

*CELLS, *FIBROBLASTS, *HYPOXEMIA, *CULTURES (Biology)

Abstract

Abstract: Cardiac fibroblasts are critical for the maintenance of extracellular matrix deposition and turnover in the normal heart and are key mediators of inflammatory and fibrotic myocardial remodeling in the injured and failing heart. Sphingosine kinase (SphK) activation is a well-recognized determinant of cell fate in cardiac myocytes and other cells, but SphK responses have not previously been studied in cardiac fibroblasts. Initially we found that total SphK activity is over 10-fold higher in cardiac fibroblasts than in adult mouse cardiac myocytes. SphK is composed of two major isoforms, SphK-1 and SphK-2. In fibroblasts isolated from SphK-1 knockout mice, SphK activity was greatly reduced indicating that SphK-1 is the major isoform expressed in these cells. To determine whether SphK regulates cell proliferation and the proinflammatory protein inducible nitric oxide synthase (iNOS), we exposed cultured cardiac fibroblasts to the cytokine interleukin-1β (IL-1β) and/or hypoxia. Both hypoxia and IL-1β alone and in combination enhanced fibroblast SphK activity. In wild-type fibroblasts, hypoxia induced proliferation, but in SphK-1 null fibroblasts this response was blunted even in the presence of serum. In contrast, we found that iNOS expression and NO production were enhanced in SphK-1 null fibroblasts during hypoxia. In wild-type fibroblasts, IL-1β was only a weak inducer of iNOS and of NO accumulation and hypoxia alone had no significant effect on iNOS activation. However, IL-1β in combination with hypoxia extensively stimulated iNOS and NO production, and this stimulation was enhanced in SphK-1 null fibroblasts. We conclude that activation of endogenous SphK-1 serves a dual regulatory function: it is required for optimal cardiac fibroblast proliferation but is a negative modulator of proinflammatory responses during hypoxia. [Copyright &y& Elsevier]

Published

2007

23. Extracellular nucleotides induce migration of renal mesangial cells by upregulating sphingosine kinase-1 expression and activity.

Author

Klawitter, S., Hofmann, L. P., Pfeilschifter, J., and Huwiler, A.

Subjects

*NUCLEOTIDES, *SPHINGOSINE, *CELL proliferation, *CELLS, *RNA

Abstract

Background and purpose:Extracellular nucleotides act as potent mitogens for renal mesangial cells (MC). In this study we determined whether extracellular nucleotides trigger additional responses in MCs and the mechanisms involved.Experimental approach:MC migration was measured after nucleotide stimulation in an adapted Boyden-chamber. Sphingosine kinase-1 (SK-1) protein expression was detected by Western blot analysis and mRNA expression quantified by real-time PCR. SK activity was measured by an in vitro kinase assay using sphingosine as substrate.Key results:Nucleotide stimulation caused biphasic activation of SK-1, but not SK-2. The first peak occurred after minutes of stimulation and was followed by a second delayed peak after 4–24 h of stimulation. The delayed activation of SK-1 is due to increased SK-1 mRNA steady-state levels and de novo synthesis of SK-1 protein, and depends on PKC and the classical MAPK cascade. To see whether nucleotide-stimulated cell responses require SK-1, we selectively depleted SK-1 from cells by using small-interference RNA (siRNA). MC migration is highly stimulated by ATP and UTP; this is mimicked by exogenously added S1P. Depletion of SK-1 by siRNA drastically reduced the effect of ATP and UTP on cell migration but not on cell proliferation. Furthermore, MCs isolated from SK-1-deficient mice were completely devoid of nucleotide-induced migration.Conclusions and implications:These data show that extracellular nucleotides besides being mitogenic also trigger MC migration and this cell response critically requires SK-1 activity. Thus, pharmacological intervention of SK-1 may have impacts on situations where MC migration is important such as during inflammatory kidney diseases.British Journal of Pharmacology (2007) 150, 271–280. doi:10.1038/sj.bjp.0706983; published online 2 January 2007 [ABSTRACT FROM AUTHOR]

Published

2007

24. Platelet-derived microvesicles induce differential gene expression in monocytic cells: A DNA microarray study*.

Author

Setzer, Florian, Oberle, Volker, Bläss, Markus, Möller, Eva, Russwurm, Stefan, Deigner, Hans-Peter, Claus, Ralf A., Bauer, Michael, Reinhart, Konrad, and Lösche, Wolfgang

Subjects

*GENE expression, *DNA microarrays, *CELL membranes, *BLOOD platelets, *CELL lines, *LIPID metabolism

Abstract

Platelet-derived microvesicles (PMV) that are shed from the plasma membrane of activated platelets, expose various platelet-type antigens on their surface and are able to adhere to other blood cells and endothelial cells. There are several clinical conditions with markedly increased numbers of PMV, e.g. acute coronary syndrome, thrombotic microangiopathy and sepsis. To prove whether PMV may contribute to an inflammatory response we used DNA microarray technology to study the effect of PMV on gene expression in the prototypic monocytic cell line MonoMac 6 (MM6). PMV were generated by activating human platelets in plasma with collagen and subsequent removal of platelets and plasma by repeated centrifugation. MM6 were incubated for 2 h with PMV in a ratio corresponding to 75 platelets/cell, or saline as control. After RNA isolation, reverse transcription and fluorescence labelling, cDNA was hybridized on a medium density microarray comprising 5308 probes addressing 4868 transcripts of 4730 human genes relevant to inflammation, immune response and related processes. The formation of PMV-MM6 conjugates was associated with significant variations in gene expression, i.e. 93 genes were found to be differentially expressed (P < 0.001; q < 0.087). Among them, 47 genes with annotated transcripts and proteins were identified. Using Ingenuity Pathway Analysis, 37 of the differentially expressed genes were identified as parts of networks associated with functional pathways including cell-to-cell signalling, cellular growth and proliferation, regulation of gene expression and lipid metabolism. For sphingosine kinase-1 the increased expression could be confirmed exemplarily not only by RT-PCR but also on the enzyme activity level. The data indicate that PMV signal differential expression of inflammation-relevant genes in monocytic cells and may represent a novel link between hemostasis and inflammation. *F.S. and V.O. contributed equally to this article. [ABSTRACT FROM AUTHOR]

Published

2006

25. Histamine increases sphingosine kinase-1 expression and activity in the human arterial endothelial cell line EA.hy 926 by a PKC-α-dependent mechanism

Author

Huwiler, Andrea, Döll, Frauke, Ren, Shuyu, Klawitter, Sabine, Greening, Anna, Römer, Isolde, Bubnova, Svetlana, Reinsberg, Luise, and Pfeilschifter, Josef

Subjects

*HISTAMINE, *SPHINGOSINE, *CELL lines, *PROTEIN kinases

Abstract

Abstract: Sphingosine 1-phosphate (S1P) is a potent mitogenic signal generated from sphingosine by the action of sphingosine kinases (SKs). In this study, we show that in the human arterial endothelial cell line EA.hy 926 histamine induces a time-dependent upregulation of the SK-1 mRNA and protein expression which is followed by increased SK-1 activity. A similar upregulation of SK-1 is also observed with the direct protein kinase C activator 12-O-tetradecanoylphorbol-13-acetate (TPA). In contrast, SK-2 activity is not affected by neither histamine nor TPA. The increased SK-1 protein expression is due to stimulated de novo synthesis since cycloheximide inhibited the delayed SK-1 protein upregulation. Moreover, the increased SK-1 mRNA expression results from an increased promoter activation by histamine and TPA. In mechanistic terms, the transcriptional upregulation of SK-1 is dependent on PKC and the extracellular signal-regulated protein kinase (ERK) cascade since staurosporine and the MEK inhibitor U0126 abolish the TPA-induced SK-1 induction. Furthermore, the histamine effect is abolished by the H1-receptor antagonist diphenhydramine, but not by the H2-receptor antagonist cimetidine. Parallel to the induction of SK-1, histamine and TPA stimulate an increased migration of endothelial cells, which is prevented by depletion of the SK-1 by small interfering RNA (siRNA). To appoint this specific cell response to a specific PKC isoenzyme, siRNA of PKC-α, -δ, and -ε were used to selectively downregulate the respective isoforms. Interestingly, only depletion of PKC-α leads to a complete loss of TPA- and histamine-triggered SK-1 induction and cell migration. In summary, these data show that PKC-α activation in endothelial cells by histamine-activated H1-receptors, or by direct PKC activators leads to a sustained upregulation of the SK-1 protein expression and activity which, in turn, is critically involved in the mechanism of endothelial cell migration. [Copyright &y& Elsevier]

Published

2006

26. The epidermal growth factor stimulates sphingosine kinase-1 expression and activity in the human mammary carcinoma cell line MCF7

Author

Döll, Frauke, Pfeilschifter, Josef, and Huwiler, Andrea

Subjects

*SPHINGOSINE, *BREAST cancer, *EPIDERMAL growth factor, *MESSENGER RNA, *PROTEIN kinase C, *PHOSPHOINOSITIDES, *CELL proliferation, *CELL migration

Abstract

Abstract: Sphingosine 1-phosphate (S1P) the product of sphingosine kinase (SK) action plays an important role in various pathological conditions like inflammation and cancer. In this study, we show that in the human breast cancer cell line MCF7, epidermal growth factor (EGF) stimulates SK-1 activity in a biphasic manner with a first peak after 15 min and a second delayed activation occurring after 1 h up to 18 h and thereafter declining again. This delayed activation is accompanied by increased mRNA and protein expression of SK-1, but not SK-2. Mechanistically, the transcriptional upregulation is dependent on the classical mitogen-activated protein kinase, protein kinase C (PKC) and the phosphoinositide 3-kinase, since specific inhibitors of these enzymes all abolish the EGF-induced mRNA upregulation and activity of SK-1. Moreover, dexamethasone also suppressed EGF-induced SK-1 mRNA expression and activity which is reversed by the glucocorticoid receptor antagonist RU486. To see whether EGF-induced upregulation of SK-1 is of relevance for tumor progression, we investigated two hallmarks of carcinogenesis, i.e., cell proliferation and migration. Stimulation of cells with EGF leads to enhanced [3H]thymidine incorporation into DNA and also to stimulated migration in a modified Boyden chamber assay. When cells are depleted of SK-1, but not SK-2, by siRNA transfection or by dexamethasone treatment, EGF-induced proliferation and migration are drastically reduced. In summary, these data show that EGF causes an acute stimulation of SK-1 activity and, moreover, triggers a delayed SK activation which is due to increased gene transcription and de novo synthesis of SK-1, which in turn directs cells towards growth and increased motility. Thus, the sphingosine kinase-1 may represent a novel attractive target for cancer therapy. [Copyright &y& Elsevier]

Published

2005

27. Silencing of Sphingosine kinase 1 Affects Maturation Pathways in Mouse Neonatal Cardiomyocytes.

Author

Jozefczuk, Ewelina, Szczepaniak, Piotr, Guzik, Tomasz Jan, Siedlinski, Mateusz, and Giussani, Paola

Subjects

*SPHINGOSINE kinase, *GLYCOGEN synthase kinase, *GLYCOGEN synthase kinase-3, *ANGIOTENSIN II, *CARDIAC hypertrophy

Abstract

Sphingosine kinase-1 (Sphk1) and its product, sphingosine-1-phosphate (S1P) are important regulators of cardiac growth and function. Numerous studies have reported that Sphk1/S1P signaling is essential for embryonic cardiac development and promotes pathological cardiac hypertrophy in adulthood. However, no studies have addressed the role of Sphk1 in postnatal cardiomyocyte (CM) development so far. The present study aimed to assess the molecular mechanism(s) by which Sphk1 silencing might influence CMs development and hypertrophy in vitro. Neonatal mouse CMs were transfected with siRNA against Sphk1 or negative control, and subsequently treated with 1 µM angiotensin II (AngII) or a control buffer for 24 h. The results of RNASeq analysis revealed that diminished expression of Sphk1 significantly accelerated neonatal CM maturation by inhibiting cell proliferation and inducing developmental pathways in the stress (AngII-induced) conditions. Importantly, similar effects were observed in the control conditions. Enhanced maturation of Sphk1-lacking CMs was further confirmed by the upregulation of the physiological hypertrophy-related signaling pathway involving Akt and downstream glycogen synthase kinase 3 beta (Gsk3β) downregulation. In summary, we demonstrated that the Sphk1 silencing in neonatal mouse CMs facilitated their postnatal maturation in both physiological and stress conditions. [ABSTRACT FROM AUTHOR]

Published

2021

28. Quail (Coturnix japonica) egg attenuated 2-butoxyethanol-induced enzymatic dysregulation, disseminated thrombosis and hemolytic impairment in female wistar rats.

Author

Oladipo, G.O., Oladipo, M.C., Ibukun, E.O., and Salawu, S.O.

Subjects

*EGGS, *ALBUMINURIA, *ANIMAL experimentation, *BIRDS, *ANALYTICAL chemistry, *ENZYMES, *HEMOLYSIS & hemolysins, *RATS, *THROMBOSIS, *ALBUMINS, *CASPASES

Abstract

Influence of quail egg on pathologies has increased research interests and series of investigations are currently being done on its influence against these pathologies. The influence of quail egg against 2-butoxyethanol induced hemolysis and disseminated thrombosis was investigated to determine the enzymatic regulations that ensue in the amelioration of deleterious hemolytic and disseminated thrombosis displayed in female Wistar rats. Quail egg was separated into three (3) components (extracts)-quail egg yolk water soluble (QYWS) and fat soluble (QYFS), and albumen extract (QA) and the inorganic and organic compositions were characterized. Depranocytotic assaults was achieved by 250 mg/kg of 2-Butoxyethanol administered for 4 days, the clinical observation revealed a dark purple-red discoloration on the distal tails of the rats and therapeutic applications followed with 1000 mg/kg BWT of QYWS, QYFS and QA, and 15 mg/kg BWT of hydroxyurea. Morphological evaluation, haematological estimations and biochemical evaluations of the influence on the activities of sphingosine kinase-1, RNase, red cell carbonic anhydrase, lactate dehydrogenase, glutathione peroxidase and caspase-3, vis a vis the concentrations of sphingosine-1 phosphate, selenium and zinc (plasma and urine). In vitro anti-inflammatory influence of quail egg components were investigated against hemolysis and key enzymes of inflammation-cycloxygenase, lipoxygenase and β-glucuronidase. The in vitro anti-inflammatory effects of QYWS, QYFS and QA were concentration dependent from 200 to 800 μg/ml against hemolysis and the key enzymes of inflammation. The characterization of inorganic and organic bioactive composition of the yolk and albumen revealed the presence of folic acid, cobalamin, pyridine, riboflavin, ascorbic acid as well as vitamins D and E, selenium, zinc, iron and calcium. These had reflected in the attenuation of the induced hemolytic and disseminated thrombosis by regulations of enzymes linked to the infarction, apoptosis and oxidative stress characterized in sickle cell index. [ABSTRACT FROM AUTHOR]

Published

2021

29. Isoflurane versus sevoflurane for early brain injury and expression of sphingosine kinase 1 after experimental subarachnoid hemorrhage.

Author

Altay, Orhan, Suzuki, Hidenori, Altay, Bilge Nur, Calisir, Vahit, Tang, Jiping, and Zhang, John H.

Subjects

*ISOFLURANE, *SPHINGOSINE kinase, *SUBARACHNOID hemorrhage, *BRAIN injuries, *CEREBRAL edema, *ENCEPHALITIS

Abstract

• 2% Isoflurane and 3% sevoflurane are neuroprotective equally. • Isoflurane and sevoflurane are effective against early brain injury after SAH. • Isoflurane and sevoflurane suppress post-SAH apoptosis and brain inflammation. • Effect of isoflurane and sevoflurane is mediated by sphingosine-related pathway. • Isoflurane and sevoflurane are good candidates for neuroanesthesia after SAH. The first step to treat aneurysmal subarachnoid hemorrhage (SAH) is aneurysmal obliteration under general anesthesia but not treat the SAH itself and the secondary effects. However, the identification of anesthetics with properties that help to attenuate post-SAH brain injury can be useful for improving outcomes of SAH patients. We examined whether 2% isoflurane and 3% sevoflurane posttreatment are protective against early brain injury (EBI) after SAH. This study used 87 8-week-old male CD-1 mice. We induced SAH by endovascular perforation in mice. Animals were randomly divided into 4 groups: sham-operated (n = 16), SAH + vehicle-medical air (n = 26), SAH + 2% isoflurane (n = 22), and SAH + 3% sevoflurane (n = 23). Neurobehavioral function, brain water content and Western blotting were evaluated at 24 h. The expression of sphingosine kinase (SphK), cleaved caspase-3 and cyclooxygenase-2 (COX2) was determined by Western blotting. Cell death was examined by terminal deoxynucleotidyl transferase-mediated uridine 5′-triphosphate-biotin nick end-labeling staining. Both 2% isoflurane and 3% sevoflurane significantly improved neurobehavioral function, and brain edema at 24 h after SAH and attenuated cell death, associated with an increase in SphK1, a decrease in cleaved caspase-3 and COX2. The neuroprotective effects were similar between 2% isoflurane and 3% sevoflurane. These findings suggest that both 2% isoflurane and 3% sevoflurane significantly inhibited EBI by suppressing post-SAH apoptosis and brain inflammation possibly via the SphK1-related pathway. [ABSTRACT FROM AUTHOR]

Published

2020

30. Design and Development of Novel Urea, Sulfonyltriurea, and Sulfonamide Derivatives as Potential Inhibitors of Sphingosine Kinase 1.

Author

Roy, Sonam, Mahapatra, Amarjyoti Das, Mohammad, Taj, Gupta, Preeti, Alajmi, Mohamed F., Hussain, Afzal, Rehman, Md. Tabish, Datta, Bhaskar, and Hassan, Md. Imtaiyaz

Subjects

*SPHINGOSINE kinase, *UREA derivatives, *SMALL molecules, *ISOTHERMAL titration calorimetry, *KINASE inhibitors, *SULFONAMIDES, *UREA

Abstract

Sphingosine kinase 1 (SphK1) is one of the well-studied drug targets for cancer and inflammatory diseases. Recently discovered small-molecule inhibitors of SphK1 have been recommended in cancer therapeutics; however, selectivity and potency of first-generation inhibitors are great challenge. In search of effective SphK1 inhibitors, a set of small molecules have been designed and synthesized bearing urea, sulfonylurea, sulfonamide, and sulfonyltriurea groups. The binding affinity of these inhibitors was measured by fluorescence-binding assay and isothermal titration calorimetry. Compounds 1, 5, 6, and 7 showed an admirable binding affinity to the SphK1 in the sub-micromolar range and significantly inhibited SphK1 activity with admirable IC50 values. Molecular docking studies revealed that these compounds fit well into the sphingosine binding pocket of SphK1 and formed significant number of hydrogen bonds and van der Waals interactions. These molecules may be exploited as potent and selective inhibitors of SphK1 that could be implicated in cancer therapeutics after the required in vivo validation. [ABSTRACT FROM AUTHOR]

Published

2020

31. Sphingosine-1-Phosphate Facilitates Skin Wound Healing by Increasing Angiogenesis and Inflammatory Cell Recruitment with Less Scar Formation.

Author

Aoki, Masayo, Aoki, Hiroaki, Mukhopadhyay, Partha, Tsuge, Takuya, Yamamoto, Hirofumi, Matsumoto, Noriko M., Toyohara, Eri, Okubo, Yuri, Ogawa, Rei, and Takabe, Kazuaki

Subjects

*WOUND healing, *SPHINGOSINE-1-phosphate, *NEOVASCULARIZATION, *TRANSFORMING growth factors, *CHRONIC wounds & injuries, *SCARS

Abstract

Wound healing starts with the recruitment of inflammatory cells that secrete wound-related factors. This step is followed by fibroblast activation and tissue construction. Sphingosine-1-phosphate (S1P) is a lipid mediator that promotes angiogenesis, cell proliferation, and attracts immune cells. We investigated the roles of S1P in skin wound healing by altering the expression of its biogenic enzyme, sphingosine kinase-1 (SphK1). The murine excisional wound splinting model was used. Sphingosine kinase-1 (SphK1) was highly expressed in murine wounds and that SphK1−/− mice exhibit delayed wound closure along with less angiogenesis and inflammatory cell recruitment. Nanoparticle-mediated topical SphK1 overexpression accelerated wound closure, which associated with increased angiogenesis, inflammatory cell recruitment, and various wound-related factors. The SphK1 overexpression also led to less scarring, and the interaction between transforming growth factor (TGF)-β1 and S1P receptor-2 (S1PR2) signaling is likely to play a key role. In summary, SphK1 play important roles to strengthen immunity, and contributes early wound healing with suppressed scarring. S1P can be a novel therapeutic molecule with anti-scarring effect in surgical, trauma, and chronic wound management. [ABSTRACT FROM AUTHOR]

Published

2019

32. Building a better sphingosine kinase-1 inhibitor.

Author

LYNCH, Kevin R.

Subjects

*SPHINGOSINE kinase, *PHOSPHOTRANSFERASES, *LYMPHOCYTES, *LEUCOCYTES, *MONONUCLEAR leukocytes

Abstract

Sphingosine 1-phosphate (S1P) is currently one of the most intensely studied lipid mediators. Interest in S1P has been propelled by the development of fingolimod, an S1P receptor agonist prodrug, which revealed both a theretofore unsuspected role of S1P in lymphocyte trafficking and that such modulation of the immune system achieves therapeutic benefit in multiple sclerosis patients. S1P is synthesized from sphingosine by two SphKs (sphingosine kinases) (SphK1 and SphK2). Manipulation of SphK levels using molecular biology and mouse genetic tools has implicated these enzymes, particularly SphK1, in a variety of pathological processes such as fibrosis, inflammation and cancer progression. The results of such studies have spurred interest in SphK1 as a drug target. In this issue of the Biochemical Journal, Schnute et al. describe a small molecule inhibitor of SphK1 that is both potent and selective. Such chemical tools are essential to learn whether targeting S1P signalling at the level of synthesis is a viable therapeutic strategy. [ABSTRACT FROM AUTHOR]

Published

2012