Your search keyword '"SPHINGOSINE"' showing total 16,461 results

151. Potential role of autophagy induced by FLT3-ITD and acid ceramidase in acute myeloid leukemia chemo-resistance: new insights.

Author

Zalpoor, Hamidreza, Bakhtiyari, Maryam, Akbari, Abdullatif, Aziziyan, Fatemeh, Shapourian, Hooriyeh, Liaghat, Mahsa, Zare-Badie, Zahra, Yahyazadeh, Sheida, Tarhriz, Vahideh, and Ganjalikhani-Hakemi, Mazdak

Subjects

*AMIDASES, *ACUTE myeloid leukemia, *AUTOPHAGY, *OLDER patients, *CELL differentiation

Abstract

Acute myeloid leukemia (AML) is a type of leukemia with a poor prognosis and survival characterized by abnormal cell proliferation and differentiation. Despite advances in treatment, AML still has a low complete remission rate, particularly in elderly patients, and recurrences are frequently seen even after complete remissions. The major challenge in treating AML is the resistance of leukemia cells to chemotherapy drugs. Thus, to overcome this issue, it can be crucial to conduct new investigations to explore the mechanisms of chemo-resistance in AML and target them. In this review, the potential role of autophagy induced by FLT3-ITD and acid ceramidase in chemo-resistance in AML patients are analyzed. With regard to the high prevalence of FLT3-ITD mutation (about 25% of AML cases) and high level of acid ceramidase in these patients, we hypothesized that both of these factors could lead to chemo-resistance by inducing autophagy. Therefore, pharmacological targeting of autophagy, FLT3-ITD, and acid ceramidase production could be a promising therapeutic approach for such AML patients to overcome chemo-resistance. 1YfY7H3U7P_Lh2F17h5Z3d Video abstract [ABSTRACT FROM AUTHOR]

Published

2022

152. Clonorchis sinensis infection induces hepatobiliary injury via disturbing sphingolipid metabolism and activating sphingosine 1-phosphate receptor 2.

Author

Ji-Xin Liu, Man Liu, Guo-Zhi Yu, Qian-Qian Zhao, Jian-Ling Wang, Yan-Hong Sun, Koda, Stephane, Beibei Zhang, Qian Yu, Chao Yan, Ren-Xian Tang, Zhi-Hua Jiang, and Kui-Yang Zheng

Subjects

CLONORCHIS sinensis, SPHINGOSINE, WOUNDS & injuries, BILE ducts, METABOLISM

Abstract

Clonorchis sinensis (C. sinensis) infection induces severe hepatobiliary injuries, which can cause inflammation, periductal fibrosis, and even cholangiocarcinoma. Sphingolipid metabolic pathways responsible for the generation of sphingosine-1-phosphate (S1P) and its receptor S1P receptors (S1PRs) have been implicated in many liver-related diseases. However, the role of S1PRs in C. sinensis-mediated biliary epithelial cells (BECs) proliferation and hepatobiliary injury has not been elucidated. In the present study, we found that C. sinensis infection resulted in alteration of bioactive lipids and sphingolipid metabolic pathways in mice liver. Furthermore, S1PR2 was predominantly activated among these S1PRs in BECs both in vivo and in vitro. Using JTE- 013, a specific antagonist of S1PR2, we found that the hepatobiliary pathological injuries, inflammation, bile duct hyperplasia, and periductal fibrosis can be significantly inhibited in C. sinensis-infected mice. In addition, both C. sinensis excretory-secretory products (CsESPs)- and S1P-induced activation of AKT and ERK1/2 were inhibited by JTE-013 in BECs. Therefore, the sphingolipid metabolism pathway and S1PR2 play an important role, and may serve as potential therapeutic targets in hepatobiliary injury caused by C. sinensis-infection. [ABSTRACT FROM AUTHOR]

Published

2022

153. Disease Reactivation in Secondary Progressive Multiple Sclerosis Patients Switching from Fingolimod to Siponimod: A Case Series.

Author

Abbadessa, Gianmarco, Maida, Elisabetta, Miele, Giuseppina, Bile, Floriana, Lavorgna, Luigi, and Bonavita, Simona

Subjects

*MULTIPLE sclerosis, *FINGOLIMOD, *SECONDARY markets, *SPHINGOSINE, *TREATMENT effectiveness

Abstract

Siponimod, a selective modulator of sphingosine 1-phosphate receptors 1 (S1P1) and 5 (S1P5), has recently been marketed for patients with Secondary Progressive Multiple Sclerosis (SPMS). Herein, we report three SPMS patients presenting disease reactivation in the first three months after switching from fingolimod to siponimod. Fingolimod binds to S1P1, S1P3, S1P4 and S1P5 receptors. S1P3 holds a central role in eliciting central proinflammatory responses, thus it has been hypothesized that upregulation of S1P3 may be the mechanism behind relapses after switching from fingolimod to siponimod. Further studies are needed to investigate the safety and efficacy of this treatment sequencing. [ABSTRACT FROM AUTHOR]

Published

2022

154. Sphingosine 1-Phoshpate Receptors are Located in Synapses and Control Spontaneous Activity of Mouse Neurons in Culture.

Author

Skoug, Cecilia, Martinsson, Isak, Gouras, Gunnar K., Meissner, Anja, and Duarte, João M. N.

Subjects

*NERVE endings, *SYNAPSES, *NEURONS, *CENTRAL nervous system, *SPHINGOSINE, *SUBCELLULAR fractionation

Abstract

Sphingosine-1-phosphate (S1P) is best known for its roles as vascular and immune regulator. Besides, it is also present in the central nervous system (CNS) where it can act as neuromodulator via five S1P receptors (S1PRs), and thus control neurotransmitter release. The distribution of S1PRs in the active zone and postsynaptic density of CNS synapses remains unknown. In the current study, we investigated the localization of S1PR1-5 in synapses of the mouse cortex. Cortical nerve terminals purified in a sucrose gradient were endowed with all five S1PRs. Further subcellular fractionation of cortical nerve terminals revealed S1PR2 and S1PR4 immunoreactivity in the active zone of presynaptic nerve terminals. Interestingly, only S1PR2 and S1PR3 immunoreactivity was found in the postsynaptic density. All receptors were present outside the active zone of nerve terminals. Neurons in the mouse cortex and primary neurons in culture showed immunoreactivity against all five S1PRs, and Ca2+ imaging revealed that S1P inhibits spontaneous neuronal activity in a dose-dependent fashion. When testing selective agonists for each of the receptors, we found that only S1PR1, S1PR2 and S1PR4 control spontaneous neuronal activity. We conclude that S1PR2 and S1PR4 are located in the active zone of nerve terminals and inhibit neuronal activity. Future studies need to test whether these receptors modulate stimulation-induced neurotransmitter release. [ABSTRACT FROM AUTHOR]

Published

2022

155. The TRPV1 Receptor Is Up-Regulated by Sphingosine 1-Phosphate and Is Implicated in the Anandamide-Dependent Regulation of Mitochondrial Activity in C2C12 Myoblasts.

Author

Standoli, Sara, Pecchioli, Sara, Tortolani, Daniel, Di Meo, Camilla, Fanti, Federico, Sergi, Manuel, Bacci, Marina, Seidita, Isabelle, Bernacchioni, Caterina, Donati, Chiara, Bruni, Paola, Maccarrone, Mauro, Rapino, Cinzia, and Cencetti, Francesca

Subjects

*CANNABINOID receptors, *TRPV cation channels, *MYOBLASTS, *MEMBRANE potential, *SPHINGOSINE, *MITOCHONDRIAL membranes

Abstract

The sphingosine 1-phosphate (S1P) and endocannabinoid (ECS) systems comprehend bioactive lipids widely involved in the regulation of similar biological processes. Interactions between S1P and ECS have not been so far investigated in skeletal muscle, where both systems are active. Here, we used murine C2C12 myoblasts to investigate the effects of S1P on ECS elements by qRT-PCR, Western blotting and UHPLC-MS. In addition, the modulation of the mitochondrial membrane potential (ΔΨm), by JC-1 and Mitotracker Red CMX-Ros fluorescent dyes, as well as levels of protein controlling mitochondrial function, along with the oxygen consumption were assessed, by Western blotting and respirometry, respectively, after cell treatment with methanandamide (mAEA) and in the presence of S1P or antagonists to endocannabinoid-binding receptors. S1P induced a significant increase in TRPV1 expression both at mRNA and protein level, while it reduced the protein content of CB2. A dose-dependent effect of mAEA on ΔΨm, mediated by TRPV1, was evidenced; in particular, low doses were responsible for increased ΔΨm, whereas a high dose negatively modulated ΔΨm and cell survival. Moreover, mAEA-induced hyperpolarization was counteracted by S1P. These findings open new dimension to S1P and endocannabinoids cross-talk in skeletal muscle, identifying TRPV1 as a pivotal target. [ABSTRACT FROM AUTHOR]

Published

2022

156. S1P (Sphingosine-1-Phosphate)-Induced Vasodilation in Human Resistance Arterioles During Health and Disease.

Author

Katunaric, Boran, SenthilKumar, Gopika, Schulz, Mary E., De Oliveira, Nilto, and Freed, Julie K.

Abstract

Background: Preclinical studies suggest that S1P (sphingosine-1-phosphate) influences blood pressure regulation primarily through NO-induced vasodilation. Because microvascular tone significantly contributes to mean arterial pressure, the mechanism of S1P on human resistance arterioles was investigated. We hypothesized that S1P induces NO-mediated vasodilation in human arterioles from adults without coronary artery disease (non-coronary artery disease) through activation of 2 receptors, S1PR1 (S1P receptor 1) and S1PR3 (S1P receptor 3). Furthermore, we tested whether this mechanism is altered in vessels from patients diagnosed with coronary artery disease.Methods: Human arterioles (50-200 µm in luminal diameter) were dissected from otherwise discarded surgical adipose tissue, cannulated, and pressurized. Following equilibration, resistance vessels were preconstricted with ET-1 (endothelin-1) and changes in internal diameter to increasing concentrations of S1P (10-12 to 10-7 M) in the presence or absence of various inhibitors were measured.Results: S1P resulted in significant dilation that was abolished in vessels treated with S1PR1 and S1PR3 inhibitors and in vessels with reduced expression of each receptor. Dilation to S1P was significantly reduced in the presence of the NOS (NO synthase) inhibitor Nω-nitro-L-arginine methyl ester and the NO scavenger 2-4-(carboxyphenyl)-4,4,5,5-tetramethylimidazoline-1-oxyl-3-oxide. Interestingly, dilation was also significantly impaired in the presence of PEG-catalase (polyethylene glycol-catalase), apocynin, and specific inhibitors of NOX (NADPH oxidases) 2 and 4. Dilation in vessels from patients diagnosed with coronary artery disease was dependent on H2O2 alone which was only dependent on S1PR3 activation.Conclusions: These translational studies highlight the inter-species variation observed in vascular signaling and provide insight into the mechanism by which S1P regulates microvascular resistance and ultimately blood pressure in humans. [ABSTRACT FROM AUTHOR]

Published

2022

157. The atypical sphingosine 1‐phosphate variant, d16:1 S1P, mediates CTGF induction via S1P2 activation in renal cell carcinoma.

Author

Glueck, Melanie, Koch, Alexander, Brunkhorst, Robert, Ferreiros Bouzas, Nerea, Trautmann, Sandra, Schaefer, Liliana, Pfeilschifter, Waltraud, Pfeilschifter, Josef, and Vutukuri, Rajkumar

Subjects

*RENAL cell carcinoma, *CONNECTIVE tissue growth factor, *SPHINGOSINE

Abstract

Sphingosine 1‐phosphate (S1P) is a lipid mediator with numerous biological functions. The term 'S1P' mainly refers to the sphingolipid molecule with a long‐chain sphingoid base of 18 carbon atoms, d18:1 S1P. The enzyme serine palmitoyltransferase catalyses the first step of the sphingolipid de novo synthesis using palmitoyl‐CoA as the main substrate. After further reaction steps, d18:1 S1P is generated. However, also stearyl‐CoA or myristoyl‐CoA can be utilised by the serine palmitoyltransferase, which at the end of the S1P synthesis pathway, results in the production of d20:1 S1P and d16:1 S1P respectively. We measured these S1P homologues in mice and renal tissue of patients suffering from renal cell carcinoma (RCC). Our experiments highlight the relevance of d16:1 S1P for the induction of connective tissue growth factor (CTGF) in the human renal clear cell carcinoma cell line A498 and human RCC tissue. We show that d16:1 S1P versus d18:1 and d20:1 S1P leads to the highest CTGF induction in A498 cells via S1P2 signalling and that both d16:1 S1P and CTGF levels are elevated in RCC compared to adjacent healthy tissue. Our data indicate that d16:1 S1P modulates conventional S1P signalling by acting as a more potent agonist at the S1P2 receptor than d18:1 S1P. We suggest that elevated plasma levels of d16:1 S1P might play a pro‐carcinogenic role in the development of RCC via CTGF induction. [ABSTRACT FROM AUTHOR]

Published

2022

158. Sphingosine 1‐phosphate lyase facilitates cancer progression through converting sphingolipids to glycerophospholipids.

Author

Uranbileg, Baasanjav, Kurano, Makoto, Kano, Kuniyuki, Sakai, Eri, Arita, Junichi, Hasegawa, Kiyoshi, Nishikawa, Takeshi, Ishihara, Soichiro, Yamashita, Hiroharu, Seto, Yasuyuki, Ikeda, Hitoshi, Aoki, Junken, and Yatomi, Yutaka

Subjects

*CANCER invasiveness, *LIQUID chromatography-mass spectrometry, *SPHINGOLIPIDS, *GLYCEROPHOSPHOLIPIDS, *SPHINGOSINE

Abstract

Background: In addition to potent agonist properties for sphingosine 1‐phosphate (S1P) receptors, intracellularly, S1P is an intermediate in metabolic conversion pathway from sphingolipids to glycerolysophospholipids (glyceroLPLs). We hypothesized that this S1P metabolism and its products might possess some novel roles in the pathogenesis of cancer, where S1P lyase (SPL) is a key enzyme. Methods: The mRNA levels of sphingolipid‐related and other cancer‐related factors were measured in human hepatocellular carcinoma (HCC), colorectal cancer, and esophageal cancer patients' tumours and in their adjacent non‐tumour tissues. Phospholipids (PL) and glyceroLPLs were measured by using liquid chromatography‐tandem mass spectrometry (LC‐MS/MS). In‐vitro experiments were performed in Colon 26 cell line with modulation of the SPL and GPR55 expressions. Xenograft model was used for determination of the cancer progression and for pharmacological influence. Results: Besides high SPL levels in human HCC and colon cancer, SPL levels were specifically and positively linked with levels of glyceroLPLs, including lysophosphatidylinositol (LPI). Overexpression of SPL in Colon 26 cells resulted in elevated levels of LPI and lysophosphatidylglycerol (LPG), which are agonists of GPR55. SPL overexpression‐enhanced cell proliferation was inhibited by GPR55 silencing. Conversely, inhibition of SPL led to the opposite outcome and reversed by adding LPI, LPG, and metabolites generated during S1P degradation, which is regulated by SPL. The xenograft model results suggested the contribution of SPL and glyceroLPLs to tumour progression depending on levels of SPL and GPR55. Moreover, the pharmacological inhibition of SPL prevented the progression of cancer. The underlying mechanisms for the SPL‐mediated cancer progression are the activation of p38 and mitochondrial function through the LPI, LPG‐GPR55 axis and the suppression of autophagy in a GPR55‐independent manner. Conclusion: A new metabolic pathway has been proposed here in HCC and colon cancer, SPL converts S1P to glyceroLPLs, mainly to LPI and LPG, and facilitates cancer development. [ABSTRACT FROM AUTHOR]

Published

2022

159. Differential interaction modes of As(III)/As(V) with microbial cell membrane induces opposite effects on organic contaminant biodegradation in groundwater.

Author

Guo W, Li D, Zhai Y, Xu X, Qiu H, Miao A, Cao X, and Zhao L

Abstract

Arsenic, a widespread toxic metalloid in groundwater, derives both from natural geological environment and industrial discharge, is extensively detected to be coexisting with organic contaminants, such as 2,4,6-trichlorophenol (TCP), a prior concerned pollutant. During biological remediation of groundwater, arsenic potentially intervenes microbial behaviors. This study found an opposite interference of arsenic in its two different valences (III and V) on the degradation of TCP by the functional bacteria, Sphingomonas fennica K101. As(III) inhibited TCP degradation in a concentration-dependent manner (from 0.1-10 mg/L), with a maximum inhibition rate of 35.5%, whereas As(V) exhibited promoting effects by 13.8% and 33.2% at 1 mg/L and 10 mg/L, respectively. Employing field emission transmission electron microscopy, quantum chemical calculations, fourier-transform ion cyclotron resonance mass spectrometry and metabolomic analysis, we unveil distinct interactions between cell membranes and arsenic in two valence states. Exposure to As(III) led to significant accumulation of As(III) in the cytoplasm, followed by interaction with intracellular ferritin (ferritin heavy chain 1), releasing iron ions and generating ROS. Subsequently, it induced ferroptosis and disrupted bacterial basal metabolism, thereby inhibiting TCP biodegradation. Oppositely, As(V) bound to a critical component sphingosine and triggered sphingosine polymerization, increasing membrane permeability, which was evidenced by measuring lactate dehydrogenase release. This process facilitated TCP transmembrane permeation by reducing membrane or extracellular secretion resistance. As(V) concurrently upregulated energy metabolism and accelerated TCP degradation. Our study elucidates the influence of prevalent arsenic on biodegradation efficacy, particularly amidst changing redox conditions associated with varying arsenic valences., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024. Published by Elsevier Ltd.)

Published

2024

160. Targeting SNAI1-Mediated Colorectal Cancer Chemoresistance and Stemness by Sphingosine Kinase 2 Inhibition.

Author

Janakiraman H, Gao Z, Zhu Y, Dong J, Becker SA, Janneh A, Ogretmen B, and Camp ER

Abstract

Background: Epithelial-to-mesenchymal transition (EMT), cancer stem cells (CSCs), and colorectal cancer (CRC) therapy resistance are closely associated. Prior reports have demonstrated that sphingosine-1-phosphate (S1P) supports stem cells and maintains the CSC phenotype. We hypothesized that the EMT inducer SNAI1 drives S1P signaling to amplify CSC self-renewal capacity and chemoresistance., Methods: CRC cell lines with or without ectopic expression of SNAI1 were used to study the role of S1P signaling as mediators of cancer stemness and 5-fluorouracil (5FU) chemoresistance. The therapeutic ability of sphingosine kinase 2 (SPHK2) was assessed using siRNA and ABC294640, a SPHK2 inhibitor. CSCs were isolated from patient-derived xenografts (PDXs) and assessed for SPHK2 and SNAI1 expression., Results: Ectopic SNAI1 expressing cell lines demonstrated elevated SPHK2 expression and increased SPHK2 promoter activity. SPHK2 inhibition with siRNA or ABC294640 ablated in vitro self-renewal and sensitized cells to 5FU. CSCs isolated from CRC PDXs express increased SPHK2 relative to the non-CSC population. Combination ABC294640/5FU therapy significantly inhibited tumor growth in mice and enhanced 5FU response in therapy-resistant CRC patient-derived tumor organoids (PDTOs)., Conclusions: SNAI1/SPHK2 signaling mediates cancer stemness and 5FU resistance, implicating S1P as a therapeutic target for CRC. The S1P inhibitor ABC294640 holds potential as a therapeutic agent to target CSCs in therapy refractory CRC., Competing Interests: The authors declare no conflict of interest., (Copyright 2024, Janakiraman et al.)

Published

2024

161. Metabolomics study of serum from patients with type 2 diabetes: Peripheral neuropathy could be associated with sphingosine and phospholipid molecules.

Author

Zhong J, Li X, Yuan M, Chen D, Li Y, Lian X, and Wang M

Abstract

Abnormal lipid metabolism is one of the risk factors for type 2 diabetes mellitus peripheral neuropathy (DPN). This study aimed to determine the differences in lipid metabolism in patients with type 2 diabetes and DPN and the possible pathogenesis caused by this difference. The participants comprised type 2 diabetes mellitus patients with DPN (N = 60) and healthy controls (N = 20). Blood samples were drawn from the participants in the morning in the fasting state, and then changes in serum lipids were explored using targeted metabolomics on the liquid chromatography-electrospray ionization-tandem mass spectrometry platform. Among the 1768 differentially abundant lipid metabolites, the results of orthogonal partial least squares-discriminant analysis combined with random forest analysis showed that the levels of sphingosine (SPH) (d18:0), carnitine 22:1, lysophosphatidylethanolamine (LPE) (18:0/0:0), LPC (16:0/0:0), lysophosphatidylcholine (LPC) (18:1/0:0), LPC (0:0/18:0) and LPE (0:0/18:1) were significantly different between the two groups. Spearman correlation analysis showed that SPH (d18:0), carnitine 22:1, LPE (18:0/0:0), and LPC (0:0/18:0) levels correlated highly with the patients' electromyography results. Kyoto Encyclopedia of Genes and Genomes pathway annotation and enrichment analysis of 538 differentially abundant lipid metabolites revealed that type 2 diabetes mellitus DPN was related to glycerophospholipid metabolism and glycerol metabolism. Our results further identified the dangerous lipid metabolites associated with DPN and abnormal lipid metabolism. The influence of lipid metabolites such as SPH and phospholipid molecules on DPN development in patients with type 2 diabetes mellitus were suggested and the possible pathogenic pathways were clarified, providing new insights into the clinical risk of DPN in patients with type 2 diabetes mellitus., (© 2024 AOCS.)

Published

2024

162. The Pseudomonas aeruginosa sphBC genes are important for growth in the presence of sphingosine by promoting sphingosine metabolism.

Author

DiGianivittorio P, Hinkel LA, Mackinder JR, Schutz K, Klein EA, and Wargo MJ

Abstract

Sphingoid bases, including sphingosine, are important components of the antimicrobial barrier at epithelial surfaces where they can cause growth inhibition and killing of susceptible bacteria. Pseudomonas aeruginosa is a common opportunistic pathogen that is less susceptible to sphingosine than many Gram-negative bacteria. Here, we determined that deletion of the sphBCD operon reduced growth in the presence of sphingosine. Using deletion mutants, complementation, and growth assays in P. aeruginosa PAO1, we determined that the sphC and sphB genes, encoding a periplasmic oxidase and periplasmic cytochrome c, respectively, were important for growth on sphingosine, while sphD was dispensable under these conditions. Deletion of sphBCD in P. aeruginosa PA14, P. protegens Pf-5, and P. fluorescens Pf01 also showed reduced growth in the presence of sphingosine. The P. aeruginosa sphBC genes were also important for growth in the presence of two other sphingoid bases, phytosphingosine and sphinganine. In wild-type P. aeruginosa , sphingosine is metabolized to an unknown non-inhibitory product, as sphingosine concentrations drop in the culture. However, in the absence of sphBC , sphingosine accumulates, pointing to SphC and SphB as having a role in sphingosine metabolism. Finally, metabolism of sphingosine by wild-type P. aeruginosa protected susceptible cells from full growth inhibition by sphingosine, pointing to a role for sphingosine metabolism as a public good. This work shows that metabolism of sphingosine by P. aeruginosa presents a novel pathway by which bacteria can alter host-derived sphingolipids, but it remains an open question whether SphB and SphC act directly on sphingosine.

Published

2024

163. The molecular mechanism of phytosphingosine binding to FFAR4/GPR120 differs from that of other fatty acids

Author

Tomotaka Nagasawa, Masaki Horitani, Shin‐ichi Kawaguchi, Shigeki Higashiyama, Yoichiro Hama, and Susumu Mitsutake

Subjects

FFAR4, GPCR, GPR120, phytosphingosine, sphingolipid, sphingosine, Biology (General), QH301-705.5

Abstract

Free fatty acid receptor 4 (FFAR4)/GPR120 comprises a receptor for medium‐ and long‐chain fatty acids. We previously identified phytosphingosine (PHS) as a novel ligand of FFAR4. Although many natural FFAR4 ligands have carboxyl groups, PHS does not, thus suggesting that binding to FFAR4 is driven by a completely different mechanism than other natural ligands such as α‐linolenic acid (ALA). To test this hypothesis, we performed docking simulation analysis using a FFAR4 homology model based on a protein model derived from the crystal structure of activated turkey beta‐1 adrenoceptor. The docking simulation revealed that the probable hydrogen bonds to FFAR4 differ between various ligands. In particular, binding was predicted between R264 of the FFAR4 and the oxygen of the carboxylate group in ALA, as well as between E249 of the FFAR4 and the oxygen of the hydroxy group at the C4‐position in PHS. Alanine substitution at E249 (E249A) dramatically reduced PHS‐induced FFAR4 activation but demonstrated a weaker effect on ALA‐induced FFAR4 activation. Kinetic analysis and Km values clearly demonstrated that the E249A substitution resulted in reduced affinity for PHS but not for ALA. Additionally, we observed that sphingosine, lacking a hydroxyl group at C4‐position, could not activate FFAR4. Our data show that E249 of the FFAR4 receptor is crucial for binding to the hydroxy group at the C4‐position in PHS, and this is a completely different molecular mechanism of binding from ALA. Because GPR120 agonists have attracted attention as treatments for type 2 diabetes, our findings may provide new insights into their development.

Published

2021

164. Research in the Area of Immunology Reported from National Institute of Allergy and Infectious Diseases (NIAID) (Sphingosine-1-Phosphate Receptor 4 links neutrophils and early local inflammation to lymphocyte recruitment into the draining lymph ...)

Subjects

United States. National Institute of Allergy and Infectious Diseases, Communicable diseases, Sphingosine, Lymphocytes, Phosphates, Health

Abstract

2024 AUG 30 (NewsRx) -- By a News Reporter-Staff News Editor at Health & Medicine Week -- New research on immunology is the subject of a new report. According to [...]

Published

2024

165. Research from Universita degli Studi di Milano Broadens Understanding of Gliomas (Sphingosine 1-Phosphate Stimulates ER to Golgi Ceramide Traffic to Promote Survival in T98G Glioma Cells)

Subjects

Sphingosine, Gliomas -- Development and progression, Immunotherapy, Brain tumors -- Development and progression, Phosphates, Health

Abstract

2024 AUG 28 (NewsRx) -- By a News Reporter-Staff News Editor at Immunotherapy Weekly -- New research on gliomas is the subject of a new report. According to news reporting [...]

Published

2024

166. Sphingosine-1-phosphate receptor 3 activation promotes sociability and regulates the expression of genes associated with anxiolytic-like behavior

Subjects

Genes -- Genetic aspects, Sphingosine, Antianxiety agents, Stress management, Phosphates, Health

Abstract

2024 AUG 23 (NewsRx) -- By a News Reporter-Staff News Editor at Health & Medicine Week -- According to news reporting based on a preprint abstract, our journalists obtained the [...]

Published

2024

167. RedHill Biopharma reports promising results for opaganib in obesity and diabetes studies

Subjects

Biological products industry, Sphingosine, Diabetes -- Research, Chemistry

Abstract

M2 PHARMA-August 19, 2024-RedHill Biopharma reports promising results for opaganib in obesity and diabetes studies (C)2024 M2 COMMUNICATIONS Biopharmaceutical company RedHill Biopharma Ltd (Nasdaq: RDHL) on Monday announced positive outcomes [...]

Published

2024

168. RedHill Biopharma reports promising results for opaganib in obesity and diabetes studies

Subjects

Biological products industry, Sphingosine, Diabetes -- Research, Business

Abstract

M2 EQUITYBITES-August 19, 2024-RedHill Biopharma reports promising results for opaganib in obesity and diabetes studies (C)2024 M2 COMMUNICATIONS http://www.m2.co.uk Biopharmaceutical company RedHill Biopharma Ltd (Nasdaq: RDHL) on Monday announced positive [...]

Published

2024

169. Is FAM19A5 an adipokine? Peripheral FAM19A5 in wild-type, FAM19A5 knock-out, and LacZ knock-in mice

Subjects

Sphingosine, Biological sciences, Health

Abstract

2024 AUG 13 (NewsRx) -- By a News Reporter-Staff News Editor at Life Science Weekly -- According to news reporting based on a preprint abstract, our journalists obtained the following [...]

Published

2024

170. 'Compositions For Binding Sphingosine-1-Phosphate Receptor 1 (S1p1), Imaging Of S1p1, And Processes For Preparation Thereof' in Patent Application Approval Process (USPTO 20240228448)

Subjects

Sphingosine, Phosphates -- Intellectual property, Health

Abstract

2024 AUG 2 (NewsRx) -- By a News Reporter-Staff News Editor at Health & Medicine Week -- A patent application by the inventors Gropler, Robert (St. Louis, MO, US); Gu, [...]

Published

2024

171. New Vasculitis Study Findings Have Been Reported by Researchers at Peking University First Hospital (Fty720 Ameliorates Experimental Mpo-anca-associated Vasculitis By Regulating Fatty Acid Oxidation Via the Neutrophil Ppara-cpt1a Pathway)

Subjects

Medical research, Medicine, Experimental, Vasculitis, Sphingosine, Fatty acids, Health

Abstract

2024 AUG 2 (NewsRx) -- By a News Reporter-Staff News Editor at Health & Medicine Week -- Current study results on Cardiovascular Diseases and Conditions - Vasculitis have been published. [...]

Published

2024

172. Sphingosine-1-phosphate signaling inhibition suppresses Th1-like Treg generation by reversing mitochondrial uncoupling

Subjects

Multiple sclerosis, Sphingosine, Phosphates, Health

Abstract

2024 JUN 7 (NewsRx) -- By a News Reporter-Staff News Editor at Health & Medicine Week -- According to news reporting based on a preprint abstract, our journalists obtained the [...]

Published

2024

173. Editorial: Bioactive sphingolipids in health and disease

Author

Mutay Aslan, Yesim Oztas, and Liana C. Silva

Subjects

sphingolipid, sphingosine, glycosphingolipid, ceramide, ganglioside, Biology (General), QH301-705.5

Published

2022

174. Perturbations of Glutathione and Sphingosine Metabolites in Port Wine Birthmark Patient-Derived Induced Pluripotent Stem Cells

Author

Vi Nguyen, Jacob Kravitz, Chao Gao, Marcelo L. Hochman, Dehao Meng, Dongbao Chen, Yunguan Wang, Anil G. Jegga, J Stuart Nelson, and Wenbin Tan

Subjects

Port Wine Birthmark, induced pluripotent stem cells, metabolome, glutathione, sphingolipid, sphingosine, Microbiology, QR1-502

Abstract

Port Wine Birthmarks (PWBs) are a congenital vascular malformation on the skin, occurring in 1–3 per 1000 live births. We have recently generated PWB-derived induced pluripotent stem cells (iPSCs) as clinically relevant disease models. The metabolites associated with the pathological phenotypes of PWB-derived iPSCs are unknown, and so we aim to explore them in this study. Metabolites were separated by ultra-performance liquid chromatography and screened with electrospray ionization mass spectrometry. Orthogonal partial least-squares discriminant, multivariate, and univariate analyses were used to identify differential metabolites (DMs). KEGG analysis was used to determine the enrichment of metabolic pathways. A total of 339 metabolites was identified. There were 22 DMs, among which nine were downregulated—including sphingosine—and 13 were upregulated, including glutathione in PWB iPSCs, as compared to controls. Pathway enrichment analysis confirmed the upregulation of glutathione and the downregulation of sphingolipid metabolism in PWB-derived iPSCs as compared to normal ones. We next examined the expression patterns of the key molecules associated with glutathione metabolism in PWB lesions. We found that hypoxia-inducible factor 1α (HIF1α), glutathione S-transferase Pi 1 (GSTP1), γ-glutamyl transferase 7 (GGT7), and glutamate cysteine ligase modulatory subunit (GCLM) were upregulated in PWB vasculatures as compared to blood vessels in normal skin. Other significantly affected metabolic pathways in PWB iPSCs included pentose and glucuronate interconversions; amino sugar and nucleotide sugars; alanine, aspartate, and glutamate; arginine, purine, D-glutamine, and D-glutamate; arachidonic acid, glyoxylate, and dicarboxylate; nitrogen, aminoacyl-tRNA biosynthesis, pyrimidine, galactose, ascorbate, and aldarate; and starch and sucrose. Our data demonstrated that there were perturbations in sphingolipid and cellular redox homeostasis in PWB vasculatures, which could facilitate cell survival and pathological progression. Our data implied that the upregulation of glutathione could contribute to laser-resistant phenotypes in some PWB vasculatures.

Published

2023

175. The Interplay between Bioactive Sphingolipids in the Psoriatic Skin and the Severity of the Disease

Author

Mateusz Matwiejuk, Hanna Mysliwiec, Bartłomiej Lukaszuk, Marta Lewoc, Hend Malla, Piotr Mysliwiec, Jacek Dadan, Adrian Chabowski, and Iwona Flisiak

Subjects

psoriasis, ceramide, sphingosine-1-phosphate, sphinganine-1-phosphate, sphinganine, sphingosine, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Psoriasis is a complex chronic immunologically mediated disease that may involve skin, nails, and joints. It is characterized by hyperproliferation, deregulated differentiation, and impaired apoptosis of keratinocytes. Sphingolipids, namely ceramide, sphingosine-1-phosphate, sphingosine, sphingomyelin, and sphinganine-1-phosphate, are signal molecules that may regulate cell growth, immune reactions, and apoptosis. Fifteen patients with psoriasis and seventeen healthy persons were enrolled in the study. Skin samples were taken from psoriatic lesions and non-lesional areas. Tissue concentration of ceramides, sphingosine-1-phosphate, sphingosine, sphingomyelin, and sphinganine-1-phosphate was measured by liquid chromatography. We assessed that all levels of ceramides, sphingosine-1-phosphate, sphingosine, sphingomyelin, and sphinganine-1-phosphate were higher in lesioned psoriatic skin than in non-affected skin. The profile of bioactive lipids in the lesional skin of patients with psoriasis differed significantly from non-involved psoriatic skin and skin in healthy subjects.

Published

2023

176. Sphingosine 1-phosphate signaling in perivascular cells enhances inflammation and fibrosis in the kidney.

Author

Tanaka, Shinji, Zheng, Shuqiu, Kharel, Yugesh, Fritzemeier, Russell G., Huang, Tao, Foster, Daniel, Poudel, Nabin, Goggins, Eibhlin, Yamaoka, Yusuke, Rudnicka, Kinga P., Lipsey, Jonathan E., Radel, Hope V., Ryuh, Sophia M., Inoue, Tsuyoshi, Yao, Junlan, Rosin, Diane L., Schwab, Susan R., Santos, Webster L., Lynch, Kevin R., and Okusa, Mark D.

Subjects

RENAL fibrosis, SPHINGOSINE, CHRONIC kidney failure, CELL communication, SPHINGOSINE kinase, CHEMOKINES

Abstract

Chronic kidney disease (CKD), characterized by sustained inflammation and progressive fibrosis, is highly prevalent and can eventually progress to end-stage kidney disease. However, current treatments to slow CKD progression are limited. Sphingosine 1-phosphate (S1P), a product of sphingolipid catabolism, is a pleiotropic mediator involved in many cellular functions, and drugs targeting S1P signaling have previously been studied particularly for autoimmune diseases. The primary mechanism of most of these drugs is functional antagonism of S1P receptor-1 (S1P1) expressed on lymphocytes and the resultant immunosuppressive effect. Here, we documented the role of local S1P signaling in perivascular cells in the progression of kidney fibrosis using primary kidney perivascular cells and several conditional mouse models. S1P was predominantly produced by sphingosine kinase 2 in kidney perivascular cells and exported via spinster homolog 2 (Spns2). It bound to S1P1 expressed in perivascular cells to enhance production of proinflammatory cytokines/chemokines upon injury, leading to immune cell infiltration and subsequent fibrosis. A small-molecule Spns2 inhibitor blocked S1P transport, resulting in suppression of inflammatory signaling in human and mouse kidney perivascular cells in vitro and amelioration of kidney fibrosis in mice. Our study provides insight into the regulation of inflammation and fibrosis by S1P and demonstrates the potential of Spns2 inhibition as a treatment for CKD and potentially other inflammatory and fibrotic diseases that avoids the adverse events associated with systemic modulation of S1P receptors. Cell type–specific sphingosine signaling: Current treatment options to slow chronic kidney disease are limited, in part due to a lack of understanding of the precise mechanisms involved with disease. Here, Tanaka et al. demonstrated that a signaling axis involving sphingosine 1-phosphate (S1P) in kidney perivascular cells resulted in increased proinflammatory cytokine production after injury in vitro and in mouse models of kidney disease. This pathway has known anti-inflammatory effects in kidney endothelial cells, highlighting cell type–specific responses to the same signaling pathway. Spinster homolog 2 inhibition to prevent perivascular cell export of S1P suppressed proinflammatory signaling in vitro and ameliorated kidney injury and fibrosis in a mouse model of kidney disease, suggesting that targeted inhibition of this pathway might serve as a potential treatment for chronic kidney diseases. [ABSTRACT FROM AUTHOR]

Published

2022

177. Chemoenzymatic Synthesis of Globo‐series Glycosphingolipids and Evaluation of Their Immunosuppressive Activities.

Author

Chiang, Pei‐Yun, Adak, Avijit K., Liang, Wei‐Lun, Tsai, Chen‐Yen, Tseng, Hsin‐Kai, Cheng, Jing‐Yan, Hwu, Jih Ru, Yu, Alice L., Hung, Jung‐Tung, and Lin, Chun‐Cheng

Subjects

*GLYCOSPHINGOLIPIDS, *CERAMIDES, *IMMUNOSUPPRESSIVE agents, *GLYCOSYLTRANSFERASES, *SPHINGOSINE

Abstract

Glycosphingolipids (GSLs) play essential roles in many important biological processes, making them attractive synthetic targets. In this paper, a viable chemoenzymatic method is described for the synthesis of globo‐series GSLs, namely, Gb4, Gb5, SSEA‐4, and Globo H. The strategy uses a chemically synthesized lactoside acceptor equipped with a partial ceramide structure that is uniquely extended by glycosyltransferases in a highly efficient one‐pot multiple enzyme (OPME) procedure. A direct and quantitative conversion of Gb4 sphingosine to Globo H sphingosine is achieved by performing two‐sequential OPME glycosylations. A reduction and N‐acylation protocol allows facile incorporation of various fatty acids into the lipid portions of the GSLs. The chemically well‐defined lipid‐modified Globo H‐GSLs displayed some differences in their immunosuppressive activities, which may benefit the structural modifications of Globo H ceramides in finding new types of immunosuppressive agents. The strategy outlined in this work should be applicable to the rapid access to other complex GSLs. [ABSTRACT FROM AUTHOR]

Published

2022

178. Ceramide/Sphingosine 1-Phosphate Axis as a Key Target for Diagnosis and Treatment in Alzheimer's Disease and Other Neurodegenerative Diseases.

Author

Custodia, Antía, Romaus-Sanjurjo, Daniel, Aramburu-Núñez, Marta, Álvarez-Rafael, Diego, Vázquez-Vázquez, Laura, Camino-Castiñeiras, Javier, Leira, Yago, Pías-Peleteiro, Juan Manuel, Aldrey, José Manuel, Sobrino, Tomás, and Ouro, Alberto

Subjects

*ALZHEIMER'S disease, *NEURODEGENERATION, *CERAMIDES, *SPHINGOSINE, *SPHINGOLIPIDS, *APOLIPOPROTEIN E4

Abstract

Alzheimer's disease (AD) is considered the most prevalent neurodegenerative disease and the leading cause of dementia worldwide. Sphingolipids, such as ceramide or sphingosine 1-phosphate, are bioactive molecules implicated in structural and signaling functions. Metabolic dysfunction in the highly conserved pathways to produce sphingolipids may lead to or be a consequence of an underlying disease. Recent studies on transcriptomics and sphingolipidomics have observed alterations in sphingolipid metabolism of both enzymes and metabolites involved in their synthesis in several neurodegenerative diseases, including AD. In this review, we highlight the most relevant findings related to ceramide and neurodegeneration, with a special focus on AD. [ABSTRACT FROM AUTHOR]

Published

2022

179. Antimicrobial effects of inhaled sphingosine against Pseudomonas aeruginosa in isolated ventilated and perfused pig lungs.

Author

Carstens, Henning, Kalka, Katharina, Verhaegh, Rabea, Schumacher, Fabian, Soddemann, Matthias, Wilker, Barbara, Keitsch, Simone, Sehl, Carolin, Kleuser, Burkhard, Hübler, Michael, Rauen, Ursula, Becker, Anne Katrin, Koch, Achim, Gulbins, Erich, and Kamler, Markus

Subjects

*LUNGS, *SPHINGOSINE, *PSEUDOMONAS aeruginosa, *PSEUDOMONAS aeruginosa infections, *LUNG transplantation, *BACTERIAL cultures

Abstract

Background: Ex-vivo lung perfusion (EVLP) is a save way to verify performance of donor lungs prior to implantation. A major problem of lung transplantation is a donor-to-recipient-transmission of bacterial cultures. Thus, a broadspectrum anti-infective treatment with sphingosine in EVLP might be a novel way to prevent such infections. Sphingosine inhalation might provide a reliable anti-infective treatment option in EVLP. Here, antimicrobial potency of inhalative sphingosine in an infection EVLP model was tested. Methods: A 3-hour EVLP run using pig lungs was performed. Bacterial infection was initiated 1-hour before sphingosine inhalation. Biopsies were obtained 60 and 120 min after infection with Pseudomonas aeruginosa. Aliquots of broncho-alveolar lavage (BAL) before and after inhalation of sphingosine were plated and counted, tissue samples were fixed in paraformaldehyde, embedded in paraffin and sectioned. Immunostainings were performed. Results: Sphingosine inhalation in the setting of EVLP rapidly resulted in a 6-fold decrease of P. aeruginosa CFU in the lung (p = 0.016). We did not observe any negative side effects of sphingosine. Conclusion: Inhalation of sphingosine induced a significant decrease of Pseudomonas aeruginosa at the epithelial layer of tracheal and bronchial cells. The inhalation has no local side effects in ex-vivo perfused and ventilated pig lungs. [ABSTRACT FROM AUTHOR]

Published

2022

180. Sphingolipid Catabolism and Glycerophospholipid Levels Are Altered in Erythrocytes and Plasma from Multiple Sclerosis Patients.

Author

Momchilova, Albena, Pankov, Roumen, Alexandrov, Alexander, Markovska, Tania, Pankov, Stefan, Krastev, Plamen, Staneva, Galya, Vassileva, Evgenia, Krastev, Nikolai, and Pinkas, Adriana

Subjects

*ERYTHROCYTES, *MULTIPLE sclerosis, *UNSATURATED fatty acids, *CENTRAL nervous system diseases, *WESTERN immunoblotting, *BLOOD lipids

Abstract

Multiple sclerosis (MS) is an autoimmune, inflammatory, degenerative disease of the central nervous system. Changes in lipid metabolism have been suggested to play important roles in MS pathophysiology and progression. In this work we analyzed the lipid composition and sphingolipid-catabolizing enzymes in erythrocytes and plasma from MS patients and healthy controls. We observed reduction of sphingomyelin (SM) and elevation of its products—ceramide (CER) and shingosine (SPH). These changes were supported by the detected up-regulation of the activity of acid sphingomyelinase (ASM) in MS plasma and alkaline ceramidase (ALCER) in erythrocytes from MS patients. In addition, Western blot analysis showed elevated expression of ASM, but not of ALCER. We also compared the ratios between saturated (SAT), unsaturated (UNSAT) and polyunsaturated fatty acids and suggest, based on the significant differences observed for this ratio, that the UNSAT/SAT values could serve as a marker distinguishing erythrocytes and plasma of MS from controls. In conclusion, the application of lipid analysis in the medical practice would contribute to definition of more precise diagnosis, analysis of disease progression, and evaluation of therapeutic strategies. Based on the molecular changes of blood lipids in neurodegenerative pathologies, including MS, clinical lipidomic analytical approaches could become a promising contemporary tool for personalized medicine. [ABSTRACT FROM AUTHOR]

Published

2022

181. Sphingosine 1-phosphate pathway is dysregulated in adenomyosis.

Author

Vannuzzi, Valentina, Bernacchioni, Caterina, Muccilli, Angela, Castiglione, Francesca, Nozzoli, Filippo, Vannuccini, Silvia, Capezzuoli, Tommaso, Ceccaroni, Marcello, Bruni, Paola, Donati, Chiara, and Petraglia, Felice

Subjects

*ENDOMETRIOSIS, *SPHINGOSINE, *SPHINGOSINE kinase, *POLYMERASE chain reaction, *ENDOMETRIUM, *PROTEIN kinases

Abstract

• S1P is a key molecule in fibrosis, proliferation, and inflammation. • S1P axis is involved in adenomyosis and could be an innovative biomarker. • mRNA levels of S1P pathway molecules are dysregulated in adenomyosis. Is sphingosine 1-phosphate (S1P) pathway involved in the process of fibrosis in adenomyosis? RNA was extracted from paraffin-embedded slices collected from the ectopic endometrium of patients with nodular adenomyosis (n = 27) and eutopic endometrium of healthy controls women (n = 29). Expression of genes involved in the metabolism and signalling of S1P, and actin-alpha-2 smooth muscle, encoded by ACTA2 gene, a gene involved in fibrogenesis, was evaluated by real-time polymerase chain reaction analysis. In adenomyotic samples, the expression of sphingosine kinase 1 (SPHK1), the enzyme responsible for the synthesis of S1P, and of S1P phosphatase 2 (SGPP2), the enzyme responsible for the conversion of S1P back to sphingosine, was lower (P = 0.0006; P = 0.0015), whereas that of calcium and integrin-binding protein 1, responsible for membrane translocation of SPHK1, was higher (P = 0.0001) compared with healthy controls. In S1P signalling, a higher expression of S1P receptor S1P 3 (P = 0.001), and a lower expression of S1P 2 (P = 0.0019) mRNA levels, were found compared with healthy endometrium. In adenomyotic nodules, a higher expression of ACTA2 mRNA levels were observed (P = 0.0001), which correlated with S1P 3 levels (P = 0.0138). Present data show a profound dysregulation of the S1P signalling axis in adenomyosis. This study also highlights that the bioactive sphingolipid might be involved in the fibrotic tract of the disease, correlated with the expression of ACTA2, suggesting its role as novel potential biomarker of adenomyosis. [ABSTRACT FROM AUTHOR]

Published

2022

182. Sphingosine 1‐Phosphate Prevents Human Embryonic Stem Cell Death Following Ischemic Injury.

Author

Assis, Juliane L. de, Fernandes, Aline M., Aniceto, Bárbara S., Pompeu, Pedro, Banchio, Claudia, Girardini, Javier, Vieyra, Adalberto, Valverde, Rafael H. F., and Einicker‐Lamas, Marcelo

Subjects

*HUMAN embryonic stem cells, *G protein coupled receptors, *CELL communication, *SPHINGOSINE, *CELL death, *SPHINGOSINE kinase

Abstract

Cell therapy based on humanembryonic stem cells (hESCs) is a potential treatment for several human diseases caused by ischemic processes. Efficiency and feasibility of these therapies rely on understanding stem cell biology and the interaction and survival of these cells within the injured tissue. hESCs are an important source of diffusible bioactive paracrine modulators and the targets for different signaling molecules that prime cellular tissue repair. Notably, sphingosine 1‐phosphate (S1P) is an emerging bioactive lipid that activates G protein‐coupled receptors, known as S1P receptors (S1PR1–5), promoting cell survival, differentiation, and migration. It is shown that S1P increases cell viability and prevents death in about 50% after the ischemic insult. S1P‐mediated protectiveeffect is attributed to the modulation of S1PR3 and S1PR4 expression, which have been associated with the reperfusion injury salvage kinase/survivoractivating factor enhancement (RISK/SAFE) pathway. Involvement of the SAFE pathway is further verified by applying Janus Kinase (JAK2) and signal transducer and activation of transcription 3 pathway inhibitors, which prevents the S1P protective effect. An increase in sphingosine kinase (SphK) activity is also observed after S1P pretreatment. These results provide evidence for an S1P‐dependent, SphK positive feedback that stimulates hESCs to deliver large amounts of S1P. Thus, S1P protects hESC under ischemic conditions through the different receptors. Practical Applications: It is considered that S1P can be used as an adjuvant to pretreat hESCs prior to the administration in cell therapy‐based protocols for different diseases. [ABSTRACT FROM AUTHOR]

Published

2022

183. Effects of Sphingosine 1-Phosphate/Sphingosine-1-Phosphate Receptor on Pro-Angiogenesis in HT-29 Human Colon Cancer Cells.

Author

YI ZHI DENG, WEI CHEN, and HUI XU

Subjects

*COLON cancer, *MESSENGER RNA, *CANCER cells, *SPHINGOSINE, *GENE expression

Abstract

To investigate the effects and mechanism of sphingosine-1-phosphate/sphingosine-1-phosphate receptor on pro-angiogenesis in human colon cancer cells is the main objective. The effects of sphingosine-1-phosphate on the pro-angiogenesis in human colon cancer cells HT-29 and SW480 were assessed by tube formation assay. Quantitative real-time polymerase chain reaction was used to detect the expression of interleukin-8, interleukin-6 and vascular endothelial growth factor in HT29 and SW480 cells after sphingosine-1-phosphate treatment. Small interfering ribonucleic acid was designed to silence the expression of sphingosine-1- phosphate receptor 1, sphingosine-1-phosphate receptor 2 and sphingosine-1-phosphate receptor 3 in HT-29 and SW480 cells. Western blot and quantitative real-time polymerase chain reaction were used to assess the down-regulation efficiency of sphingosine-1-phosphate receptor in HT-29 and SW480 cells. Later, the effects of sphingosine-1-phosphate receptor were detected by quantitative real-time polymerase chain reaction. Tube formation assay showed that the number of formed tubes in human umbilical vein endothelial cell-fused cells (EA.hy926) resuspended in the culture supernatant from HT-29 and SW480 cells treated with sphingosine-1-phosphate was significantly more than that of the control group (t=3.667 and 4.881, p=0.021 and 0.013), indicating that sphingosine-1-phosphate promoted the pro-angiogenic ability of colon cancer cells. Moreover, the messenger ribonucleic acid expression of interleukin-8, interleukin-6 and vascular endothelial growth factor were significantly increased after sphingosine-1-phosphate treatment compared to the control group (p<0.05) where sphingosine-1-phosphate receptor 1 gene silence could significantly decrease the messenger ribonucleic acid expression in HT-29 and SW480 cells (p<0.05), while sphingosine-1-phosphate receptor 2 and sphingosine-1-phosphate receptor 3 gene silence did not lead to significant messenger ribonucleic acid changes. Sphingosine-1-phosphate up-regulated the expression of interleukin-8, interleukin-6 and vascular endothelial growth factor in human colon cancer cells through sphingosine-1-phosphate receptor 1 and thereby enhancing the proangiogenic effect of colon cancer cells. The sphingosine-1-phosphate/sphingosine-1-phosphate receptor pathway is a promising novel therapeutic target for inhibiting colon cancer growth. [ABSTRACT FROM AUTHOR]

Published

2022

184. Sphingosine 1-Phosphate Modulation in Inflammatory Bowel Diseases: Keeping Lymphocytes Out of the Intestine.

Author

Dal Buono, Arianna, Gabbiadini, Roberto, Alfarone, Ludovico, Solitano, Virginia, Repici, Alessandro, Vetrano, Stefania, Spinelli, Antonino, and Armuzzi, Alessandro

Subjects

INFLAMMATORY bowel diseases, SPHINGOSINE, G protein coupled receptors, LYMPHOCYTES, SMALL molecules, HYPERPHOSPHATEMIA, DISEASE remission

Abstract

Inflammatory bowel diseases (IBDs) are chronic and disabling conditions that, uncontrolled, lead to irreversible bowel damage and associated comorbidities. Despite the new era of biological therapies, IBDs remain not curative. The treatment purpose is to induce endoscopic remission, reduce the progression of the disease and improve the quality of life. Optimal and early treatment could enable the prevention of their complications. Small molecules, administrated as oral agents, have the capacity of overcoming the limitations of biologic agents (i.e., parenteral administration, rapidity of action and primary and secondary non-responsiveness). Of special interest are results from the use of oral sphingosine 1-phosphate (S1P) receptor modulators (ozanimod, etrasimod, fingolimod and laquinimod), based on S1P activities to target lymphocyte recirculation in the mucosa, acting as immunosuppressive agents. Most S1P modulators are reported to be safe and effective in the treatment of both UC and CD. High and satisfactory rates of clinical remission as well as endoscopic improvement and remission can be achieved with these molecules. Safety alarms remain rather low, although the S1P binding to two of its G protein-coupled receptors, 2 and 3 (S1PR2 and S1PR3), may be associated with cardiovascular risks. Cost-effectiveness studies and head-to-head trials are needed to better define their place in therapy. This review summarizes these emerging data published by PubMed and EMBASE databases and from ongoing clinical trials on the safety and efficacy of selectivity of S1P modulators in the treatment of IBD. [ABSTRACT FROM AUTHOR]

Published

2022

185. Competitive Binding of Ozanimod and Other Sphingosine 1-Phosphate Receptor Modulators at Receptor Subtypes 1 and 5.

Author

Selkirk, Julie V., Bortolato, Andrea, Yan, Yingzhuo Grace, Ching, Nathan, and Hargreaves, Richard

Subjects

SPHINGOSINE, RADIOLIGAND assay, BINDING sites, MOLECULAR docking, ULCERATIVE colitis, GLATIRAMER acetate, ARRESTINS

Abstract

Ozanimod, a sphingosine 1-phosphate (S1P) receptor modulator, binds with high affinity selectively to S1P receptor subtypes 1 (S1P1) and 5 (S1P5), and is approved in multiple countries for treating adults with relapsing forms of multiple sclerosis (MS) or moderately to severely active ulcerative colitis (UC). Other S1P receptor modulators have been approved for the treatment of MS or are in clinical development for MS or UC, but it is unknown whether these compounds bind competitively with each other to S1P1 or S1P5. We developed a competitive radioligand binding assay using tritiated ozanimod and demonstrate full displacement of ozanimod by S1P (endogenous ligand), suggesting that ozanimod binds to the S1P1 and S1P5 orthosteric binding sites. S1P receptor modulators FTY720-p, siponimod, etrasimod, ponesimod, KRP-203-p, and amiselimod-p also completely displacing radiolabeled ozanimod; thus, on a macroscopic level, all bind to the same site. Molecular docking studies support these results and predict the binding of each molecule to the orthosteric site of the receptors, creating similar interactions within S1P1 and S1P5. The absolute free energy perturbation method further validated key proposed binding modes. Functional potency tightly aligned with binding affinities across S1P1 and S1P5 and all compounds elicited S1P1-mediated β-arrestin recruitment. Since all the S1P modulators included in this study display similar receptor pharmacology and compete for binding at the same site, they can be considered interchangeable with one another. The choice of any one particular agent should therefore be made on the basis of overall therapeutic profile, and patients can be offered the opportunity to switch S1P medications without the potential concern of additive S1P pharmacology. [ABSTRACT FROM AUTHOR]

Published

2022

186. Sphingosine 1-Phosphate Signaling at the Skin Barrier Interface.

Author

Masuda-Kuroki, Kana and Di Nardo, Anna

Subjects

*G protein coupled receptors, *SPHINGOSINE, *CELL physiology, *CELL migration, *INHIBITION of cellular proliferation, *MAST cells, KERATINOCYTE differentiation

Abstract

Simple Summary: Sphingosine 1-phosphate is a bioactive phospholipid derived from cell membranes. It is biosynthesized and metabolized within the cell and released extracellularly to trigger various cellular responses via sphingosine 1-phosphate receptors. Keratinocyte and mast cell functions are responsible for skin barrier acquired and innate immunity, and express sphingosine 1-phosphate receptors. These receptors regulate not only cell differentiation and proliferation, but also immune responses such as cell migration and cytokine secretion, through G-protein-mediated signaling pathways. Sphingosine 1-phosphate and its receptor signaling pathways are also involved in several skin diseases along with various receptor agonists and are being investigated as potential therapeutic agents. Here, we focus on the association of sphingosine 1-phosphate and its receptors within the skin barrier interface. Sphingosine 1-phosphate (S1P) is a product of membrane sphingolipid metabolism. S1P is secreted and acts via G-protein-coupled receptors, S1PR1-5, and is involved in diverse cellular functions, including cell proliferation, immune suppression, and cardiovascular functions. Recent studies have shown that the effects of S1P signaling are extended further by coupling the different S1P receptors and their respective downstream signaling pathways. Our group has recently reported that S1P inhibits cell proliferation and induces differentiation in human keratinocytes. There is a growing understanding of the connection between S1P signaling, skin barrier function, and skin diseases. For example, the activation of S1PR1 and S1PR2 during bacterial invasion regulates the synthesis of inflammatory cytokines in human keratinocytes. Moreover, S1P-S1PR2 signaling is involved in the production of inflammatory cytokines and can be triggered by epidermal mechanical stress and bacterial invasion. This review highlights how S1P affects human keratinocyte proliferation, differentiation, immunoreaction, and mast cell immune response, in addition to its effects on the skin barrier interface. Finally, studies targeting S1P-S1PR signaling involved in inflammatory skin diseases are also presented. [ABSTRACT FROM AUTHOR]

Published

2022

187. Sphk1 and Sphk2 Differentially Regulate Erythropoietin Synthesis in Mouse Renal Interstitial Fibroblast-like Cells.

Author

Hafizi, Redona, Imeri, Faik, Stepanovska Tanturovska, Bisera, Manaila, Roxana, Schwalm, Stephanie, Trautmann, Sandra, Wenger, Roland H., Pfeilschifter, Josef, and Huwiler, Andrea

Abstract

Erythropoietin (Epo) is a crucial hormone regulating red blood cell number and consequently the hematocrit. Epo is mainly produced in the kidney by interstitial fibroblast-like cells. Previously, we have shown that in cultures of the immortalized mouse renal fibroblast-like cell line FAIK F3-5, sphingosine 1-phosphate (S1P), by activating S1P1 and S1P3 receptors, can stabilize hypoxia-inducible factor (HIF)-2α and upregulate Epo mRNA and protein synthesis. In this study, we have addressed the role of intracellular iS1P derived from sphingosine kinases (Sphk) 1 and 2 on Epo synthesis in F3-5 cells and in mouse primary cultures of renal fibroblasts. We show that stable knockdown of Sphk2 in F3-5 cells increases HIF-2α protein and Epo mRNA and protein levels, while Sphk1 knockdown leads to a reduction of hypoxia-stimulated HIF-2α and Epo protein. A similar effect was obtained using primary cultures of renal fibroblasts isolated from wildtype mice, Sphk1−/−, or Sphk2−/− mice. Furthermore, selective Sphk2 inhibitors mimicked the effect of genetic Sphk2 depletion and also upregulated HIF-2α and Epo protein levels. The combined blockade of Sphk1 and Sphk2, using Sphk2−/− renal fibroblasts treated with the Sphk1 inhibitor PF543, resulted in reduced HIF-2α and Epo compared to the untreated Sphk2−/− cells. Exogenous sphingosine (Sph) enhanced HIF-2α and Epo, and this was abolished by the combined treatment with the selective S1P1 and S1P3 antagonists NIBR-0213 and TY52156, suggesting that Sph was taken up by cells and converted to iS1P and exported to then act in an autocrine manner through S1P1 and S1P3. The upregulation of HIF-2α and Epo synthesis by Sphk2 knockdown was confirmed in the human hepatoma cell line Hep3B, which is well-established to upregulate Epo production under hypoxia. In summary, these data show that sphingolipids have diverse effects on Epo synthesis. While accumulation of intracellular Sph reduces Epo synthesis, iS1P will be exported to act through S1P1+3 to enhance Epo synthesis. Furthermore, these data suggest that selective inhibition of Sphk2 is an attractive new option to enhance Epo synthesis and thereby to reduce anemia development in chronic kidney disease. [ABSTRACT FROM AUTHOR]

Published

2022

188. Studies from University of California Further Understanding of Gene Therapy (Factors influencing survival in sphingosine phosphate lyase insufficiency syndrome: a retrospective cross-sectional natural history study of 76 patients).

Abstract

A recent study conducted at the University of California focused on sphingosine-1-phosphate lyase insufficiency syndrome (SPLIS), a metabolic disorder associated with various symptoms including nephrotic syndrome, adrenal insufficiency, and neurological and skin manifestations. The study aimed to identify factors that influence survival in SPLIS patients. The research found that overall survival was 50%, with age and organ involvement at first presentation, kidney transplantation, and SGPL1 genotype being major influences on survival. The study also revealed that patients diagnosed with SPLIS nephropathy in the first year of life and those with the R222Q SGPL1 variant had higher risks, while kidney transplantation significantly extended survival outcomes. [Extracted from the article]

Published

2024

189. Researchers from Fukuoka Dental College Publish Research in Dental Science (Sphingosine-1-phosphate receptor 1-mediated odontogenic differentiation of mouse apical papilla-derived stem cells).

Abstract

Researchers from Fukuoka Dental College in Japan have published a study on the effect of sphingosine-1-phosphate (S1P) on the odontogenic differentiation of mouse stem cells derived from dental apical papilla. The study found that S1P, along with bone morphogenetic protein-9 (BMP-9), increased the expression of odontogenic differentiation markers and facilitated mineralization in the stem cells. S1P receptor 1 (S1PR1) was found to be expressed in the apical papilla and dentin-pulp interface of immature rat molars. The findings suggest that S1P and S1PR1 play a role in the odontogenic differentiation of dental stem cells. [Extracted from the article]

Published

2024

190. The Pseudomonas aeruginosa sphBC genes are important for growth in the presence of sphingosine by promoting sphingosine metabolism.

Abstract

According to a preprint abstract, researchers have found that the sphBC genes in Pseudomonas aeruginosa are important for growth in the presence of sphingosine, a component of the antimicrobial barrier at epithelial surfaces. The deletion of the sphBCD operon reduced growth in the presence of sphingosine, and the sphC and sphB genes were found to be important for growth on sphingosine. The metabolism of sphingosine by P. aeruginosa protected susceptible cells from full growth inhibition by sphingosine. However, it is still unclear whether SphB and SphC act directly on sphingosine. This research provides insights into how bacteria can alter host-derived sphingolipids. [Extracted from the article]

Published

2024

191. Researchers from University of Paris Discuss Findings in Cardiovascular Research (Zonation and Ligand and Dose Dependence of Sphingosine 1-phosphate Receptor-1 Signalling In Blood and Lymphatic Vasculature).

Subjects

AMINO alcohols, SPHINGOSINE kinase, DIGESTIVE system diseases, PHOSPHORIC acid, SPHINGOSINE

Abstract

Researchers from the University of Paris have conducted a study on sphingosine 1-phosphate receptor-1 (S1PR1) signaling in blood and lymphatic vasculature. The study aimed to determine the zonation and ligand and dose dependence of S1PR1 engagement in different vascular subsets. The researchers found that S1PR1 engagement was restricted to specific blood vessels and lymphatic vessels, and that reductions in plasma S1P levels had a significant impact on S1PR1 signaling and endothelial function. The study highlights the importance of S1P as a circulating biomarker for endothelial function. [Extracted from the article]

Published

2024

192. Aga Khan University Researcher Adds New Data to Research in Ulcerative Colitis (Efficacy and Safety of Sphingosine 1-Phosphate Receptor Modulators for Ulcerative Colitis).

Subjects

ULCERATIVE colitis, SPHINGOSINE, INFLAMMATORY bowel diseases, RESEARCH personnel, DIGESTIVE system diseases

Abstract

The article presents new research from Aga Khan University on the effectiveness and safety of Sphingosine 1-phosphate receptor modulators (S1PRMs) for treating moderate to severe ulcerative colitis. Topics discussed include the efficacy of S1PRMs in achieving clinical and endoscopic remission, their comparative safety with placebo, and the overall impact on patient outcomes.

Published

2024

193. Researchers at Michigan Medicine Release New Data on Ulcerative Colitis (Efficacy and Safety of Sphingosine 1-phosphate Receptor Modulators for Ulcerative Colitis a Systematic Review and Meta-analysis of Randomized Controlled Trials).

Subjects

ULCERATIVE colitis, RANDOMIZED controlled trials, SPHINGOSINE, INFLAMMATORY bowel diseases, RESEARCH personnel, HYPERPHOSPHATEMIA

Abstract

The article reports on new findings from Michigan Medicine regarding the use of Sphingosine 1-phosphate receptor modulators (S1PRMs) for treating ulcerative colitis. Topics discussed include the efficacy and safety of S1PRM therapy, its impact on various clinical and endoscopic outcomes, and the overall quality of evidence from randomized controlled trials.

Published

2024

194. Researchers at Division of Immunology Publish New Data on Pharmacology (The functional antagonist of sphingosine-1-phosphate, FTY720, impairs gut barrier function).

Abstract

Researchers at the Division of Immunology have published new data on the pharmacology of FTY720, a functional antagonist of sphingosine-1-phosphate (S1P). FTY720 is known to be effective in treating multiple sclerosis and preventing inflammatory bowel disease (IBD). However, the researchers found that FTY720 can increase susceptibility to mucosal infections and impair gut barrier function. The study showed that FTY720 therapy in mice led to increased inflammation, immune cell infiltration, and production of inflammatory markers. The researchers concluded that vigilance of gut pathology should be maintained when using FTY720 as a treatment option. [Extracted from the article]

Published

2024

195. Study Findings on Medical Science Published by Researchers at Shahroud University of Medical Sciences (Injectable multifunctional hydrogel containing Sphingosine 1-phosphate and human acellular amniotic membrane for skin wound healing).

Abstract

A recent study conducted by researchers at Shahroud University of Medical Sciences focused on the development of a novel hydrogel scaffold for skin wound healing. The scaffold, made of carboxymethyl cellulose (CMC) and gelatin (Gel) hydrogels cross-linked with 1-(3-dimethylaminopropyl)-3-ethylcarbodiimide hydrochloride (EDC) containing Sphingosine 1-phosphate (S1P), was applied topically to treat acute wounds and covered with a human acellular amniotic membrane (hAAM) as a secondary dressing. The study found that the scaffold was biocompatible, exhibited excellent hemocompatibility, and led to faster wound healing in treated rats compared to the control group. The researchers concluded that the CMC/Gel/EDC hydrogel with S1P and hAAM showed promise as an effective wound dressing. [Extracted from the article]

Published

2024

196. Findings from McGovern Medical School University of Texas Provides New Data about Ubiquitins (Sphingosine Kinase 2 Regulates Protein Ubiquitination Networks In Neurons).

Abstract

A recent study conducted at McGovern Medical School University of Texas has found that sphingosine kinase 2 (SPHK2) regulates protein ubiquitination networks in neurons. The researchers discovered that inhibiting SPHK2 decreases protein ubiquitination, and mass spectrometry revealed that this inhibition affects lipid and synaptic protein networks as well as a ubiquitin-dependent protein network. The study also found that SPHK2 and HUWE1 were upregulated in the striatum of a mouse model of Huntington's disease, suggesting that these findings may be relevant to neurodegenerative diseases. This research provides new insights into the role of SPHK2 in protein ubiquitination and offers a potential target for developing therapies for neurodegenerative diseases. [Extracted from the article]

Published

2024

197. Complete Acid Ceramidase ablation prevents cancer-initiating cell formation in melanoma cells.

Author

Lai, Michele, Realini, Natalia, La Ferla, Marco, Passalacqua, Ilaria, Matteoli, Giulia, Ganesan, Anand, Pistello, Mauro, Mazzanti, Chiara Maria, and Piomelli, Daniele

Subjects

Cell Line, Tumor, Melanocytes, Humans, Sphingosine, Ceramides, Lysophospholipids, Cell Proliferation, Acid Ceramidase, Gene Knockout Techniques, Clustered Regularly Interspaced Short Palindromic Repeats, Cellular Senescence, CRISPR-Associated Protein 9, Cancer, Rare Diseases, Prevention

Abstract

Acid ceramidase (AC) is a lysosomal cysteine hydrolase that catalyzes the conversion of ceramide into fatty acid and sphingosine. This reaction lowers intracellular ceramide levels and concomitantly generates sphingosine used for sphingosine-1-phosphate (S1P) production. Since increases in ceramide and consequent decreases of S1P reduce proliferation of various cancers, AC might offer a new target for anti-tumor therapy. Here we used CrispR-Cas9-mediated gene editing to delete the gene encoding for AC, ASAH1, in human A375 melanoma cells. ASAH1-null clones show significantly greater accumulation of long-chain saturated ceramides that are substrate for AC. As seen with administration of exogenous ceramide, AC ablation blocks cell cycle progression and accelerates senescence. Importantly, ASAH1-null cells also lose the ability to form cancer-initiating cells and to undergo self-renewal, which is suggestive of a key role for AC in maintaining malignancy and self-renewal of invasive melanoma cells. The results suggest that AC inhibitors might find therapeutic use as adjuvant therapy for advanced melanoma.

Published

2017

198. SGPL1 (sphingosine phosphate lyase 1) modulates neuronal autophagy via phosphatidylethanolamine production.

Author

Mitroi, Daniel, Karunakaran, Indulekha, Gräler, Markus, Saba, Julie, Ehninger, Dan, Ledesma, María, and van Echten-Deckert, Gerhild

Subjects

amyloid precursor protein, autophagy, lysosomes, neuropathology, phosphatidylethanolamine, sphingosine-1-phosphate lyase, α-synuclein/SNCA, Aldehyde-Lyases, Amyloid beta-Peptides, Animals, Autophagy, Brain, Lysophospholipids, Lysosomes, Mice, Neurons, Phosphatidylethanolamines, Sphingosine

Abstract

Macroautophagy/autophagy defects have been identified as critical factors underlying the pathogenesis of neurodegenerative diseases. The roles of the bioactive signaling lipid sphingosine-1-phosphate (S1P) and its catabolic enzyme SGPL1/SPL (sphingosine phosphate lyase 1) in autophagy are increasingly recognized. Here we provide in vitro and in vivo evidence for a previously unidentified route through which SGPL1 modulates autophagy in neurons. SGPL1 cleaves S1P into ethanolamine phosphate, which is directed toward the synthesis of phosphatidylethanolamine (PE) that anchors LC3-I to phagophore membranes in the form of LC3-II. In the brains of SGPL1fl/fl/Nes mice with developmental neural specific SGPL1 ablation, we observed significantly reduced PE levels. Accordingly, alterations in basal and stimulated autophagy involving decreased conversion of LC3-I to LC3-II and increased BECN1/Beclin-1 and SQSTM1/p62 levels were apparent. Alterations were also noticed in downstream events of the autophagic-lysosomal pathway such as increased levels of lysosomal markers and aggregate-prone proteins such as APP (amyloid β [A4] precursor protein) and SNCA/α-synuclein. In vivo profound deficits in cognitive skills were observed. Genetic and pharmacological inhibition of SGPL1 in cultured neurons promoted these alterations, whereas addition of PE was sufficient to restore LC3-I to LC3-II conversion, and control levels of SQSTM1, APP and SNCA. Electron and immunofluorescence microscopy showed accumulation of unclosed phagophore-like structures, reduction of autolysosomes and altered distribution of LC3 in SGPL1fl/fl/Nes brains. Experiments using EGFP-mRFP-LC3 provided further support for blockage of the autophagic flux at initiation stages upon SGPL1 deficiency due to PE paucity. These results emphasize a formerly overlooked direct role of SGPL1 in neuronal autophagy and assume significance in the context that autophagy modulators hold an enormous therapeutic potential in the treatment of neurodegenerative diseases.

Published

2017

199. Cutting Edge: Targeting Epithelial ORMDL3 Increases, Rather than Reduces, Airway Responsiveness and Is Associated with Increased Sphingosine-1-Phosphate

Author

Miller, Marina, Tam, Arvin B, Mueller, James L, Rosenthal, Peter, Beppu, Andrew, Gordillo, Ruth, McGeough, Matthew D, Vuong, Christine, Doherty, Taylor A, Hoffman, Hal M, Niwa, Maho, and Broide, David H

Subjects

Asthma, Lung, 2.1 Biological and endogenous factors, Aetiology, Respiratory, Animals, Disease Models, Animal, Lysophospholipids, Membrane Proteins, Mice, Mice, Inbred C57BL, Mice, Knockout, Polymerase Chain Reaction, Respiratory Hypersensitivity, Sphingosine, Immunology

Abstract

In this study, we used cre-lox techniques to generate mice selectively deficient in ORMDL3 in airway epithelium (Ormdl3Δ2-3/Δ2-3/CC10) to simulate an inhaled therapy that effectively inhibited ORMDL3 expression in the airway. In contrast to the anticipated reduction in airway hyperresponsiveness (AHR), OVA allergen-challenged Ormdl3Δ2-3/Δ2-3/CC10 mice had a significant increase in AHR compared with wild-type mice. Levels of airway inflammation, mucus, fibrosis, and airway smooth muscle were no different in Ormdl3Δ2-3/Δ2-3/CC10 and wild-type mice. However, levels of sphingosine-1-phosphate (S1P) were significantly increased in Ormdl3Δ2-3/Δ2-3/CC10 mice as well as in airway epithelial cells in which ORMDL3 was inhibited with small interfering RNA. Incubation of S1P with airway smooth muscle cells significantly increased contractility. Overall, Ormdl3Δ2-3/Δ2-3/CC10 mice exhibit increased allergen-induced AHR independent of inflammation and associated with increased S1P generation. These studies raise concerns for inhaled therapies that selectively and effectively inhibit ORMDL3 in airway epithelium in asthma.

Published

2017

200. Sphingosine-1-phosphate improves endothelialization with reduction of thrombosis in recellularized human umbilical vein graft by inhibiting syndecan-1 shedding in vitro

Author

Hsia, Kai, Yang, Ming-Jie, Chen, Wei-Min, Yao, Chao-Ling, Lin, Chih-Hsun, Loong, Che-Chuan, Huang, Yi-Long, Lin, Ya-Ting, Lander, Arthur D, Lee, Hsinyu, and Lu, Jen-Her

Subjects

Engineering, Biomedical and Clinical Sciences, Biomedical Engineering, Regenerative Medicine, Stem Cell Research - Umbilical Cord Blood/ Placenta, Stem Cell Research, Hematology, Cardiovascular, Stem Cell Research - Umbilical Cord Blood/ Placenta - Human, Stem Cell Research - Nonembryonic - Human, 5.1 Pharmaceuticals, 2.1 Biological and endogenous factors, Blood Coagulation, Blood Vessel Prosthesis, Cell Adhesion, Endothelial Progenitor Cells, Endothelium, Vascular, Fluorescent Antibody Technique, Glycocalyx, Human Umbilical Vein Endothelial Cells, Humans, Kinetics, Lysophospholipids, Matrix Metalloproteinase 7, Models, Biological, Platelet Adhesiveness, Sphingosine, Syndecan-1, Thrombosis, Tissue Scaffolds, Umbilical Veins, Sphingosine-l-phosphate, Endothelial cell, Endothelial progenitor, Platelet adhesion, Sphingosine-1-phosphate

Abstract

Sphingosine-1-phosphate (S1P) has been known to promote endothelial cell (EC) proliferation and protect Syndecan-1 (SDC1) from shedding, thereby maintaining this antithrombotic signal. In the present study, we investigated the effect of S1P in the construction of a functional tissue-engineered blood vessel by using human endothelial cells and decellularized human umbilical vein (DHUV) scaffolds. Both human umbilical vein endothelial cells (HUVEC) and human cord blood derived endothelial progenitor cells (EPC) were seeded onto the scaffold with or without the S1P treatment. The efficacy of re-cellularization was determined by using the fluorescent marker CellTracker CMFDA and anti-CD31 immunostaining. The antithrombotic effect of S1P was examined by the anti-aggregation tests measuring platelet adherence and clotting time. Finally, we altered the expression of SDC1, a major glycocalyx protein on the endothelial cell surface, using MMP-7 digestion to explore its role using platelet adhesion tests in vitro. The result showed that S1P enhanced the attachment of HUVEC and EPC. Based on the anti-aggregation tests, S1P-treated HUVEC recellularized vessels when grafted showed reduced thrombus formation compared to controls. Our results also identified reduced SDC1 shedding from HUVEC responsible for inhibition of platelet adherence. However, no significant antithrombogenic effect of S1P was observed on EPC. In conclusion, S1P is an effective agent capable of decreasing thrombotic risk in engineered blood vessel grafts.Statement of significanceSphingosine-1phosphate (S1P) is a low molecular-weight phospholipid mediator that regulates diverse biological activities of endothelial cell, including survival, proliferation, cell barrier integrity, and also influences the development of the vascular system. Based on these characters, we the first time to use it as an additive during the process of a small caliber blood vessel construction by decellularized human umbilical vein and endothelial cell/endothelial progenitor. We further explored the function and mechanism of S1P in promoting revascularization and protection against thrombosis in this tissue engineered vascular grafts. The results showed that S1P could not only accelerate the generation but also reduce thrombus formation of small caliber blood vessel.

Published

2017