AIM: To study the effects of aminoguanidine (AG) and two L-arginine analogues N(omega)-nitro-L-arginine methyl ester (L-NAME) and N(omega)-nitro-L-arginine (L-NNA) on nitric oxide (NO) production induced by cytokines ...AIM: To study the effects of aminoguanidine (AG) and two L-arginine analogues N(omega)-nitro-L-arginine methyl ester (L-NAME) and N(omega)-nitro-L-arginine (L-NNA) on nitric oxide (NO) production induced by cytokines (TNF-alpha, IL-1 beta, and IFN-gamma) and bacterial lipopolysaccharide (LPS) mixture (CM) in the cultured rat hepatocytes, and examine their mechanisms action. METHODS: Rat hepatocytes were incubated with AG, L-NAME, L-NNA, Actinomycin D (ActD) and dexamethasone in a medium containing CM (LPS plus TNF-alpha, IL-1 beta, and IFN-gamma) for 24h. NO production in the cultured supernatant was measured with the Griess reaction. Intracellular cGMP level was detected with radioimmunoassy. RESULTS: NO production was markedly blocked by AG and L-NAME in a dose-dependent manner under inflammatory stimuli condition triggered by CM in vitro. The rate of the maximum inhibitory effects of L-NAME (38.9%) was less potent than that obtained with AG(53.7%, P 【 0.05). There was no significant difference between the inhibitory effects of AG and two L-arginine analogues on intracellular cGMP accumulation in rat cultured hepatocytes. Non-specific NOS expression inhibitor dexamethasone (DEX)and iNOS mRNA transcriptional inhibitor ActD also significantly inhibited CM-induced NO production. AG(0.1 mmol x L(-1)) and ActD (0.2 ng x L(-1)) were equipotent in decreasing NO production induced by inflammatory stimuli in vitro, and both effects were more potent than that induced by non-selectivity NOS activity inhibitor L-NAME (0.1 mmol x L(-1)) under similar stimuli conditions (P【0.01). CONCLUSION: AG is a potent selective inhibitor of inducible isoform of NOS,and the mechanism of action may be not only competitive inhibition in the substrate level, but also the gene expression level in rat hepatocytes.展开更多
To study whether the diacylglycerol (Dia) signaling pathway is stimulated by advanced glycosylation end products (AGEP) and to test the effect of vitamin E and aminoguanidine (AG) on the elevation of Dia induced by AG...To study whether the diacylglycerol (Dia) signaling pathway is stimulated by advanced glycosylation end products (AGEP) and to test the effect of vitamin E and aminoguanidine (AG) on the elevation of Dia induced by AGEP in cultured human umbilical vein endothelial cells (HUVECs) Methods The effects of AGEP on Dia levels in cultured HUVEC were studied with radio enzymatic assay Quantitative measurements of 32 P phosphatidic acid were achieved by thin layer chromatography and autoradiography Results The Dia levels in HUVECs were increased by AGEP modified bovine serum albumin (AGEP BSA) in a dose dependent, biphasic manner The early phase was rapid and transient, peaking at 15?s; the late phase reached the maximal level at 10?min and then decayed slowly Dia levels in HUVEC exposed to different concentrations (50, 100 and 200?mg/L) of AGEP BSA (341±14, 678±16, and 873±18?pmol/L, respectively vs control 225±10?pmol/L) and AGEP BSA samples with various glycosylation times (4, 8 and 12 weeks) were significantly increased (270±12, 394±16, and 556±19?pmol/L) as compared with the controls 50 and 100?mmol/L of vitamin E can reduce AGEP BSA induced Dia levels from 873±18?pmol/L to 764±29 and 441±21?pmol/L in HUVEC, respectively In AG treated (100?mmol/L) groups, the same concentration (100 and 200?mg/L) of AGEP BSA induced elevation of Dia was decreased to 312±8 and 351±13?pmol/L, respectively Glycosylated low density lipoprotein (LDL) did not affect Dia levels Conclusion AGEP causes a robust stimulation of the Dia/protein kinase C pathway in HUVEC Vitamin E can attenuate the AGEP BSA induced elevation of Dia levels AG can suppress the ability of AGEP BSA to increase Dia levels in HUVEC展开更多
Chiral organobases occupy a significant position in asymmetric organocatalysis. The general types of chiral organobases include tertiary amines, amidines, guanidines, cyclopropenimines, and iminophosphoranes, etc. The...Chiral organobases occupy a significant position in asymmetric organocatalysis. The general types of chiral organobases include tertiary amines, amidines, guanidines, cyclopropenimines, and iminophosphoranes, etc. These organobases are demonstrated to be effective organocatalysts to promote divers kinds of base-initiated reactions in excellent yields and stereoselectivities. In previous reports, several groups have summarized each kind of chiral organobases in different reviews. To the aim of understanding the whole of them in one review, herein, we provide a brief introduction of these chiral organobases in asymmetric catalysis.展开更多
基金Project supported by the National Natural Science Foundation of China,No.39770861.and JANSSEN Science Research Foundation.
文摘AIM: To study the effects of aminoguanidine (AG) and two L-arginine analogues N(omega)-nitro-L-arginine methyl ester (L-NAME) and N(omega)-nitro-L-arginine (L-NNA) on nitric oxide (NO) production induced by cytokines (TNF-alpha, IL-1 beta, and IFN-gamma) and bacterial lipopolysaccharide (LPS) mixture (CM) in the cultured rat hepatocytes, and examine their mechanisms action. METHODS: Rat hepatocytes were incubated with AG, L-NAME, L-NNA, Actinomycin D (ActD) and dexamethasone in a medium containing CM (LPS plus TNF-alpha, IL-1 beta, and IFN-gamma) for 24h. NO production in the cultured supernatant was measured with the Griess reaction. Intracellular cGMP level was detected with radioimmunoassy. RESULTS: NO production was markedly blocked by AG and L-NAME in a dose-dependent manner under inflammatory stimuli condition triggered by CM in vitro. The rate of the maximum inhibitory effects of L-NAME (38.9%) was less potent than that obtained with AG(53.7%, P 【 0.05). There was no significant difference between the inhibitory effects of AG and two L-arginine analogues on intracellular cGMP accumulation in rat cultured hepatocytes. Non-specific NOS expression inhibitor dexamethasone (DEX)and iNOS mRNA transcriptional inhibitor ActD also significantly inhibited CM-induced NO production. AG(0.1 mmol x L(-1)) and ActD (0.2 ng x L(-1)) were equipotent in decreasing NO production induced by inflammatory stimuli in vitro, and both effects were more potent than that induced by non-selectivity NOS activity inhibitor L-NAME (0.1 mmol x L(-1)) under similar stimuli conditions (P【0.01). CONCLUSION: AG is a potent selective inhibitor of inducible isoform of NOS,and the mechanism of action may be not only competitive inhibition in the substrate level, but also the gene expression level in rat hepatocytes.
文摘To study whether the diacylglycerol (Dia) signaling pathway is stimulated by advanced glycosylation end products (AGEP) and to test the effect of vitamin E and aminoguanidine (AG) on the elevation of Dia induced by AGEP in cultured human umbilical vein endothelial cells (HUVECs) Methods The effects of AGEP on Dia levels in cultured HUVEC were studied with radio enzymatic assay Quantitative measurements of 32 P phosphatidic acid were achieved by thin layer chromatography and autoradiography Results The Dia levels in HUVECs were increased by AGEP modified bovine serum albumin (AGEP BSA) in a dose dependent, biphasic manner The early phase was rapid and transient, peaking at 15?s; the late phase reached the maximal level at 10?min and then decayed slowly Dia levels in HUVEC exposed to different concentrations (50, 100 and 200?mg/L) of AGEP BSA (341±14, 678±16, and 873±18?pmol/L, respectively vs control 225±10?pmol/L) and AGEP BSA samples with various glycosylation times (4, 8 and 12 weeks) were significantly increased (270±12, 394±16, and 556±19?pmol/L) as compared with the controls 50 and 100?mmol/L of vitamin E can reduce AGEP BSA induced Dia levels from 873±18?pmol/L to 764±29 and 441±21?pmol/L in HUVEC, respectively In AG treated (100?mmol/L) groups, the same concentration (100 and 200?mg/L) of AGEP BSA induced elevation of Dia was decreased to 312±8 and 351±13?pmol/L, respectively Glycosylated low density lipoprotein (LDL) did not affect Dia levels Conclusion AGEP causes a robust stimulation of the Dia/protein kinase C pathway in HUVEC Vitamin E can attenuate the AGEP BSA induced elevation of Dia levels AG can suppress the ability of AGEP BSA to increase Dia levels in HUVEC
基金the National Natural Science Foundation of China (Nos. 21625205 and 21332003)the National Program for Support of Top-Notch Young Professionals for financial support
文摘Chiral organobases occupy a significant position in asymmetric organocatalysis. The general types of chiral organobases include tertiary amines, amidines, guanidines, cyclopropenimines, and iminophosphoranes, etc. These organobases are demonstrated to be effective organocatalysts to promote divers kinds of base-initiated reactions in excellent yields and stereoselectivities. In previous reports, several groups have summarized each kind of chiral organobases in different reviews. To the aim of understanding the whole of them in one review, herein, we provide a brief introduction of these chiral organobases in asymmetric catalysis.
