Your search keyword '"Jang, Hyunduk"' showing total 2 results

1. Effect of Long-Term Treatment with Fimasartan on Transient Focal Ischemia in Rat Brain.

Author

Kim, Chi Kyung, Yang, Xiu-Li, Kim, Young-Ju, Choi, In-Young, Jeong, Han-Gil, Park, Hong-Kyun, Kim, Dohoung, Kim, Tae Jung, Jang, Hyunduk, Ko, Sang-Bae, and Yoon, Byung-Woo

Subjects

ANGIOTENSIN-receptor blockers, ISCHEMIA, BRAIN, LABORATORY rats, MYOCARDIAL infarction, ATHEROSCLEROSIS, PHOSPHATES, INFLAMMATION treatment

Abstract

Fimasartan is a newly developed angiotensin receptor blocker, which may have protective effects during myocardial infarction or atherosclerosis. In this context, we investigated the effects of long-term treatment with low-dose fimasartan on focal ischemia in rat brain. We induced focal ischemia in brain by transient intraluminal occlusion of middle cerebral artery (MCA) and administered low-dose (0.5 mg/kg) or regular doses (1 or 3 mg/kg) of fimasartan via intravenous routes. After the administration of low-dose (0.5 mg/kg) fimasartan, blood pressure did not decrease compared to the phosphate-buffered saline- (PBS-) control with MCA occlusion (MCAO) group. The infarct volume and ischemic cell death were reduced in the low-dose fimasartan-treated group (46 ± 41 mm(3) for 0.5 mg/kg and 153 ± 47 mm(3) for PBS-control with MCAO; P < 0.01) but not in the regular-dose groups. Low-dose fimasartan treatment improved functional recovery after ischemia and significantly decreased mortality. In our study, fimasartan reduced the degradation of IκB and the formation of an inflammatory end-product, COX-2. As a result, the recruitment of inflammatory cells in the peri-infarct area decreased in fimasartan-treated group. We have demonstrated that long-term, low-dose fimasartan treatment improved outcomes after focal ischemia in the brain via a reduction of inflammation. [ABSTRACT FROM AUTHOR]

Published

2015

2. Decrease of GSK3β phosphorylation in the rat nucleus accumbens core enhances cocaine-induced hyper-locomotor activity.

Author

Kim, Wha Y., Jang, Ju K., Lee, Jung W., Jang, Hyunduk, and Kim, Jeong ‐ Hoon

Subjects

TREATMENT of musculoskeletal system diseases, PHOSPHORYLATION, NUCLEUS accumbens, COCAINE, TARGETED drug delivery, NEURAL stimulation, LABORATORY rats

Abstract

Glycogen synthase kinase 3β ( GSK3β), which is abundantly present in the brain, is known to contribute to psychomotor stimulant-induced locomotor behaviors. However, most studies have been focused in showing that GSK3β is able to attenuate psychomotor stimulants-induced hyperactivity by increasing its phosphorylation levels in the nucleus accumbens ( NAcc). So, here we examined in the opposite direction about the effects of decreased phosphorylation of GSK3β in the NAcc core on both basal and cocaine-induced locomotor activity by a bilateral microinjection into this site of an artificially synthesized peptide, S9 (0.5 or 5.0 μg/μL), which contains sequences around N-terminal serine 9 residue of GSK3β. We found that decreased levels of GSK3β phosphorylation in the NAcc core enhance cocaine-induced hyper-locomotor activity, while leaving basal locomotor activity unchanged. This is the first demonstration, to our knowledge, that the selective decrease of GSK3β phosphorylation levels in the NAcc core may contribute positively to cocaine-induced locomotor activity, while this is not sufficient for the generation of locomotor behavior by itself without cocaine. Taken together, these findings importantly suggest that GSK3β may need other molecular targets which are co-activated (or deactivated) by psychomotor stimulants like cocaine to contribute to generation of locomotor behaviors. [ABSTRACT FROM AUTHOR]

Published

2013