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Query: UMLS:C0393754 (
HSA
)
2,996
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Advanced glycation end-products (AGEs) inhibit
ischemia
-induced angiogenesis but are potential triggers of neoangiogenesis that occurs in peritoneal dialysis (PD) patients. We investigated whether the effect of glucose and AGEs on human peritoneal mesothelial cells (HPMCs) might alter the release of vascular endothelial growth factor (VEGF) and subsequently the formation of capillary tubes by human umbilical vein endothelial cells (HUVECs). HPMCs were exposed to glucose and the glycated protein Nvarepsilon-(carboxymethyl)lysine-human serum albumin (CML-
HSA
) and VEGF production was measured by reverse transcription-polymerase chain reaction and enzyme-linked immunosorbent assay. Capillary tube formation by HUVECs in presence of HPMC supernatant or co-cultured with HPMC was investigated. AGE and VEGF levels in PD effluents from 11 patients were measured. CML-
HSA
stimulated VEGF production by HPMCs, P<0.001. Glucose and AGE inhibited capillary tube formation by HUVECs, P<0.001. HPMC supernatant potentiated capillary tube formation, P<0.001. In co-culture with HPMC capillary tube formation was increased, especially by HPMCs stimulated by CML-
HSA
, P<0.001. Anti-VEGF antibody limited this effect, P<0.001. Preincubation of HPMCs with anti-receptor for AGEs (RAGE) antibody reduced capillary tube formation, P<0.001. AGE and VEGF levels in PD effluents were increased during long dwell time, P<0.05 and P<0.001, respectively. In a co-culture system, we showed that VEGF production by HPMC favors capillary tube formation through mesothelial RAGE activation and could explain neoangiogenesis in PD patient.
...
PMID:Mesothelial RAGE activation by AGEs enhances VEGF release and potentiates capillary tube formation. 1714 74
Binding of oleate to S-nitrosylated human serum albumin (SNO-HSA) enhances its cytoprotective effect on liver cells in a rat
ischemia
/reperfusion model. It enhances the antiapoptotic effect of SNO-
HSA
on HepG2 cells exposed to anti-Fas antibody. To identify some of the reasons for the increased cytoprotective effects, additional experiments were performed with glutathione and HepG2 cells. As indicated by 5,5'-dithiobis-2-nitrobenzoic acid binding, the addition of oleate increased the accessibility of the single thiol group of albumin. Binding of increasing amounts of oleate resulted in increasing and more rapid S-transnitrosation of glutathione. Likewise, binding of oleate, or of a mixture of endogenous fatty acids, improved S-denitrosation of SNO-
HSA
by HepG2 cells. Oleate also enhanced S-transnitrosation by HepG2 cells, as detected by intracellular fluorescence of diaminofluorescein-FM. All of the S-transnitrosation caused by oleate binding was blocked by filipin III. Oleate also increased, in a dose-dependent manner, the binding of SNO-
HSA
labeled with fluorescein isothiocyanate to the surface of the hepatocytes. A model in two parts was worked out for S-transnitrosation, which does not involve low molecular weight thiols. Fatty acid binding facilitates S-denitrosation of SNO-
HSA
, increases its binding to HepG2 cells and greatly increases S-transnitrosation by hepatocytes in a way that is sensitive to filipin III. A small nitric oxide transfer takes place in a slow system, which is unaffected by fatty acid binding to SNO-
HSA
and not influenced by filipin III. Thus, fatty acids could be a novel type of mediator for S-transnitrosation.
...
PMID:S-nitrosylated human serum albumin-mediated cytoprotective activity is enhanced by fatty acid binding. 1894 Aug 10
S-Nitrosated human serum albumin (SNO-HSA) is a large molecular weight nitric oxide carrier in human plasma, and because of its many beneficial effects in different tests, it is currently under investigation as a cytoprotective agent. However, making SNO-
HSA
preparations is a complicated and time-consuming process. We found that binding of caprylic acid (CA) and N-acetyl-l-tryptophan (N-AcTrp) to defatted mercaptalbumin increased S-nitrosation by S-nitrosoglutathione (GS-NO) by making Cys-34 of
HSA
more accessible and by protecting it against oxidation, respectively. Fortunately,
HSA
solutions for clinical use contain high concentrations of CA and N-AcTrp as stabilizers. By making use of that fact it was possible to work-out a fast and simple procedure for producing SNO-
HSA
: incubation of a commercial
HSA
formulation with GS-NO for only 1 min results in S-nitrosation of
HSA
. The biological usefulness of such a preparation was tested in a rat
ischemia
-reperfusion liver injury model. Although our procedure for making SNO-
HSA
is fast and straightforward, the cytoprotective effect of the preparation was similar to, or better than, that of a preparation made in a more traditional way. The clinical development of SNO-
HSA
as a strong cytoprotective agent is under way using this method in collaboration with clinicians and industrial developers.
...
PMID:One-step preparation of S-nitrosated human serum albumin with high biological activities. 2045 47
S-Nitrosated human serum albumin (SNO-HSA) is useful in preventing liver
ischemia
/reperfusion injury, and SNO-
HSA
should thus be able to prevent cell injury during liver transplantation. However, the potential protective effect of SNO-
HSA
on a combination of cold and warm
ischemia
, which is obligatory when performing liver transplantation, has not been examined. Therefore, we evaluated the protective effect of SNO-
HSA
added to University of Wisconsin (UW) solution during cold or/and warm
ischemia
in situ and in vitro. First, we observed that apoptotic and necrotic cell death were increased during cold and warm
ischemia
, respectively. SNO-
HSA
, which possesses anti-apoptosis activity at low NO concentrations, can inhibit cold
ischemia
injury both in situ and in vitro. In contrast, SNO-
HSA
had no significant effect on warm liver
ischemia
injury which, however, can be reduced by UW solution. We also demonstrated that the cellular uptake of NO from SNO-
HSA
can occur during cold
ischemia
resulting in induction of heme oxygenase-1 within 3h of cold
ischemia
. Our results indicate that treatment with SNO-
HSA
or UW solution alone is not sufficient to inhibit liver injury during a period of both cold and warm
ischemia
. However, a combination of SNO-
HSA
and UW solution can be used to prevent the two types of
ischemia
. SNO-
HSA
-added UW solution could be very useful in transplantation, because the previously imposed constraints on preservation time can be removed. This is a great advantage in a situation as the present one with increased utilization of scarce donor organs for more recipients.
...
PMID:UW solution improved with high anti-apoptotic activity by S-nitrosated human serum albumin. 2340 24
Zinc (Zn) is a co-factor for a vast number of enzymes, and functions as a regulator for immune mechanism and protein synthesis. However, excessive Zn release induced in pathological situations such as stroke or transient global
ischemia
is toxic. Previously, we demonstrated that the interaction of Zn and copper (Cu) is involved in the pathogenesis of Alzheimer's disease and vascular dementia. Furthermore, oxidative stress has been shown to play a significant role in the pathogenesis of various metal ions induced neuronal death. Thioredoxin-Albumin fusion (
HSA
-Trx) is a derivative of thioredoxin (Trx), an antioxidative protein, with improved plasma retention and stability of Trx. In this study, we examined the effect of
HSA
-Trx on Cu
2+
/Zn
2+
-induced neurotoxicity. Firstly,
HSA
-Trx was found to clearly suppress Cu
2+
/Zn
2+
-induced neuronal cell death in mouse hypothalamic neuronal cells (GT1-7 cells). Moreover,
HSA
-Trx markedly suppressed Cu
2+
/Zn
2+
-induced ROS production and the expression of oxidative stress related genes, such as heme oxygenase-1. In contrast,
HSA
-Trx did not affect the intracellular levels of both Cu
2+
and Zn
2+
after Cu
2+
/Zn
2+
treatment. Finally,
HSA
-Trx was found to significantly suppress endoplasmic reticulum (ER) stress response induced by Cu
2+
/Zn
2+
treatment in a dose dependent manner. These results suggest that
HSA
-Trx counteracted Cu
2+
/Zn
2+
-induced neurotoxicity by suppressing the production of ROS via interfering the related gene expressions, in addition to the highly possible radical scavenging activity of the fusion protein. Based on these findings,
HSA
-Trx has great potential as a promising therapeutic agent for the treatment of refractory neurological diseases.
...
PMID:Thioredoxin-albumin fusion protein prevents copper enhanced zinc-induced neurotoxicity via its antioxidative activity. 2912 8
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