• 동의생리병리학회지
• /
• 제17권6호
• /
• pp.1463-1467
• /
• 2003

In the present study, the effects of Ginseng radix and Ophiopogonis tuber on field potentials in rat hippocampal slices and cardiac muscle slices were investigated by multi-channel extracellular recording using MED64 system. The field potentials in the brain slices represent synaptic transmission and nerve excitability, and the field potentials in heart muscles represent muscle contractility. The present results show that the aqueous extract of Ginseng radix enhanced field potentials in the both hippocampal slices and cardiac muscle slices. In contrast, the aqueous extract Ophiopogonis tuber exerted no significant effect on the field potentials in the hippocampal slices and cardiac muscle slices. These results suggest the possibility that Yin-Yang theory could be studied in relation with excitability in neurons and muscles.

• The Korean Journal of Physiology and Pharmacology
• /
• 제10권3호
• /
• pp.123-129
• /
• 2006

In several experimental models, estrogens protect neurons against ischemic insults. However, the recent clinical studies of hormone replacement showed negative results to prevent stroke. Therefore, optimal models to study estrogen replacement for neuroprotection are needed before its clinical ap-plication. Organotypic hippocampal slice under oxygen-glucose deprivation (OGD) has been established as a model of cerebral ischemia and has advantages to study drug effects. We investigated whether estrogen protected CAI neurons and affected activation of Akt (pAkt) in CAI region under OGD. Thus, rat hippocampal slices on day 7 of culture were treated with $17-{\beta}$ estradiol (E, 1 nM) for 7 days before 30 min OGD, and cell death of CAI neurons was quantified by propidium iodide (PI) staining and expression of pAkt was studied by Western blot and immunofluorescence. PI intensity in slices treated with E was significantly reduced 72 hour after OGD compared to that of non-treated slices (p < 0.05). E pretreatment also increased the expression of pAkt 72 hour after OGD compared to that of no treatment (p<0.01). These data suggest that estrogen pretreatment may rescue neurons from ischemic insults through the activation of Akt and also indicate that our model would be a useful alternative method to study the mechanisms and effects of estrogen replacement treatment for neuroprotection.

• The Korean Journal of Physiology and Pharmacology
• /
• 제8권6호
• /
• pp.301-305
• /
• 2004

This study examined the effects of N-methyl-D-aspartate (NMDA), ${\alpha}-amino$-3-hydroxy-5-methyl-4-isoxazole propionic acid (AMPA) and kainate on basal and electrically-evoked release of acetylcholine (ACh) from the rat hippocampal and striatal slices which were preincubated with $[^3H]choline$. Unexpectedly, the basal and evoked ACh release were not affected at all by the treatment with NMDA $(3{\sim}100{\mu}M)$, AMPA $(1{\sim}100{\mu}M)$ or kainate $(1{\sim}100{\mu}M)$ in hippocampal slices. However, in striatal slices, under the $Mg^{2+}-free$ medium, $30{\mu}M$ NMDA increased the basal ACh release with significant decrease of the electrically-evoked releases. The treatment with $1{\mu}M MK-801 not only reversed the $30{\mu}M$ NMDA-induced decrease of the evoked ACh release, but also attenuated the facilitatory effect of $30\;{\mu}M$ NMDA on the basal ACh release. The treatment with either $30\;{\mu}M$ AMPA or $100\;{\mu}M$ kainate increased the basal ACh release without any effects on the evoked release. The treatment with $10{\mu}M$ NBQX abolished the AMPA- or kainate-induced increase of the basal ACh release. Interestingly, NBQX significantly attenuated the evoked release when it was treated with AMPA, although it did not affect the evoked release alone without AMPA. These observations demonstrate that in hippocampal slices, ionotropic glutamate receptors do not modulate the ACh release in cholinergic terminals, whereas in striatal slices, activations of ionotropic glutamate receptors increase the basal ACh release though NMDA may decrease the electrically-evoked ACh release.

• Toxicological Research
• /
• 제13권4호
• /
• pp.359-365
• /
• 1997

Many factors are known to be responsible for cerebral ischemic injury, such as excitatory neurotransmitters, increased intraneuronal calcium, or disturbance of cellular energy metabolism. Recently, oxygen free radicals, formed during ischemia/reperfusion, have been proposed as one of the main causes of ischemia/reperfusion injury. Therefore, to investigate the role of oxygen free radical during ischemia/reperfusion, in the present study the effect of endogenous oxygen free radical scavenger, superoxide dismutase / catalase(SOD / catalase) on the release of [$^3$H]-5-hydroxytryptamine([$^3$H]-5-HT) during hypoxia/reoxygenation in rat hippocampal slices was measured. The hippocampus was obtained from the rat brain and sliced 400 gm thickness with manual chopper. After 30 min's preincubation in the normal buffer, the slices were incubated for 20 min in a buffer containing [$^3$H]-5-HT(0.1 $\mu$M, 74 $\mu$Ci) for uptake, and washed. To measure the release of [$^3$H]-5-HT into the buffer, the incubation medium was drained off and refilled every ten minutes through a sequence of 14 tubes. Induction of hypoxia for 20 min (gassing it with 95% N$_2$/5% CO$_2$) was done in the 6th and 7th tube, and oxygen free radical scavenger, SOD / catalase was added 10 minutes prior to induction of hypoxia. The radioactivity in each buffer and the tissue were counted using liquid scintillation counter and the results were expressed as a percentage of the total activity. When slices were exposed to hypoxia for 20 min, [$^3$H]-5-HT release was markedly decreased and a rebound release of [$^3$H]-5-HT was observed on the post-hypoxic reoxygenation period. SOD / catalase did not changed the release of [$^3$H]-5-HT in control group, but inhibited the decrease of [$^3$H]-5-HT release in hypoxic period and rebound increase of [$^3$H]-5-HT in reoxygenation period. This result suggest that superoxide anion may play a role in the hypoxic-, and reoxygenation-induced change of [$^3$H]-5-HT release in rat hippocampal slices.

• Toxicological Research
• /
• 제14권4호
• /
• pp.483-488
• /
• 1998

During cerebral ischemia two important factors such as hypoxia and reduction of glucose can act as modulating stressor affecting the release of amine neurotransmitters including 5-hydroxytryptamine (5-HT). This study was performed to investigate the effect of glucose deprivation on the oxygen deprivation-induced changes of [3H]-5-HT release in the rat hippocampal slices. Experimental groups were divided into 4 groups for this study: normoxic/normoglycemic group, oxygen-deprived group, glucose-deprived group, and oxygen/glucose-deprived group. The hippocampus of rat brain was sliced by 400 $\mu\textrm{m}$ thickness with manual chopper. After 30 minutes preincubation in the normal buffer, the slices were incubated for 20 min in buffer containing [3H]-5-HT (0.1 M, 74 $\mu\textrm$Ci) for uptake. To measure the release of [3H]-5-HT into the buffer, the incubation medium was drained of and refilled with fresh buffer every ten minutes through a sequence of 14 tubes. Oxygen deprivation by gassing with 95% $N_2$/5% $CO_2$ and/or glucose deprivation was done in the 6th and 7th tube. The radioactivities in each buffer and the tissue were counted using scintillation counter. The results were expressed as fractional release. When slices were exposed to oxygen-deprived media for 20 min, the diminution followed by the rebound release of [3H]-5-HT was observed during the post-oxygen deprived period. However, glucose deprivation or oxygen/glucose deprivation markedly increased the release of [3H]-5-HT. which was opposite to the pattern observed in oxygen-deprived group. These results suggested that oxygen deprivation itself inhibits [3H]-5-HT release in rat hippocampal slices during oxygen-deprived period, but additional glucose deprivation convert the inhibitory response to increase of [3H]-5-HT release.

• The Korean Journal of Physiology and Pharmacology
• /
• 제4권5호
• /
• pp.347-353
• /
• 2000

It has been well documented that a massive release of not only glutamate but also other neurotransmitters may modulate the final responses of nerve cells to the ischemic neuronal injury. But there is no information regarding whether the release of monoamines is directly associated with synaptic vesicular proteins under ischemia. In the present study, it was investigated whether synapsin 1, syntaxin and SNAP-25 are involved in the release of 5-hydroxytryptamine $([^3H]5-HT)$ in glucose/oxygen deprived (GOD) rat hippocampal slices. And, the effect of NMDA receptor using DL-2-amino-5-phosphonovaleric acid (APV) on ischemia- induced release of 5-HT and the changes of the above proteins were also investigated. GOD for 20 minutes enhanced release of $[^3H]5-HT,$ which was in part blocked by the NMDA receptor antagonist, APV. The augmented expression of synapsin 1 during GOD for 20 minutes, which was also in part prevented by APV. In contrast, the expression of syntaxin and SNAP-25 were not altered during GOD. These results suggest that ischemic insult induces release of $[^3H]5-HT$ associated with synapsin 1, synaptic vesicular protein, via activation of NMDA receptor in part.

• Clinical and Experimental Pediatrics
• /
• 제52권5호
• /
• pp.588-593
• /
• 2009

목 적 : 산소-포도당 박탈(oxygen-glucose deprivation, OGD)에 노출된 신생 흰쥐 해마 절편에서 성장호르몬이 신경 세포 보호 효과가 있는지를 연구하고자 하였다. 방 법 : 배양된 생후 7일된 신생 흰쥐의 해마 절편을 OGD에 60분간 노출 시켰다. 이후 각기 다른 세 용량의 성장 호르몬(5, 50, $500{\mu}M$)을 배양액에 투여하고 OGD 노출 후 12 와 24시간에 해마 절편의 상대적 propidium iodide (PI) uptake와 배양액의 상대적 lactate dehydrogenase (LDH) 활성도를 측정하여 성장 호르몬 처치군과 성장 호르몬 처치하지 않은 대조군 사이에 비교하였다. 신경 세포의 세포 사멸에 대한 성장호르몬의 효과를 관찰하고자 caspase-3의 면역 형광 염색과 TUNEL 염색을 시행하였다. 결 과 : 1) 각기 다른 세 용량의 성장호르몬을 처치한 해마 절편의 CA1과 DG에서 상대적 PI uptake는 처치하지 않은 대조군에 비해 OGD 노출 후 12시간과 24시간에 의미 있는 차이를 보이지 않았다(P>0.05). 2) 상대적 LDH 활성도는 OGD 노출 후 12시간에만 성장 호르몬을 투여한 군의 배양액에서 대조군에 비해 통계적으로 의미 있게 감소하였다(P<0.05). 3) 성장 호르몬($50{\mu}M$)으로 처치한 해마 절편의 CA1과 DG에서 caspase-3 발현과 TUNEL 양성의 발현은 OGD 노출 후 12와 24시간에 대조군과 차이를 보이지 않았다. 결 론 : OGD에 노출된 해마 절편에서 성장호르몬 처치는 확실한 신경세포 보호 효과를 보이지 않았으나 OGD 노출 후 12시간에 배양액으로 LDH 유출을 감소시킬 수 있었다.

• 동의신경정신과학회지
• /
• 제21권1호
• /
• pp.43-57
• /
• 2010

Objectives: This study was designed to assess neuroprotective effects of herb medicine against Alzhheimer's disease related brain damage in organotypic hippocampal slice culture. Methods: We induced dementia related brain damage in organotypic hippocampal slices by $\beta$-amyloid. Those slices were treated with herb medicines - Hwangryeonhaedoktang, Sopungsoongiwon. Using by PI staining, the extents of cell death were assessed. After that, we selected the best effective one among those herb medicines and the major components of that medicine were studied to reveal neuroprotective effects and related proteins by using PI stating. Results: In PI staining, Sopungsoongiwon is the best effective herb medicine between Hwangryeonhaedoktang and Sopungsoongiwon. Notopterygii Rhizoma, Corni Fructus, Areca Catechu, Aurantii Fructus Immaturus, Plantaginis Semen is the best effective one among the components of Sopungsoongiwon. Conclusions: We suggested that purgative effect would be the best effetive medicine on dementia related brain damage between clearing heat and toxic materials.

• The Korean Journal of Physiology and Pharmacology
• /
• 제1권6호
• /
• pp.657-664
• /
• 1997

The effects of adenosine, adenosine A1 receptor antagonist (DPCPX), or NMDA receptor antagonist (APV) on the spontaneous release of $[^3H]-5-hydroxytryptamine$ ($[^3H]-5-HT$) during normoxic/normoglycemic or hypoxic/hypoglycemic period were studied in the rat hippocampal slices. The hippocampus was obtained from the rat brain and sliced $400\;{\mu}m$ thickness with the tissue slicer. After 30 min's preincubation in the normal buffer, the slices were incubated for 30 min in a buffer containing $[^3H]-5-HT$ ($0.1\;{\mu}M,\;74{\mu}Ci/8\;ml$) for uptake, and washed. To measure the release of $[^3H]-5-HT$ into the buffer, the incubation medium was drained off and refilled every ten minutes through sequence of 14 tubes. Induction of glucose/oxygen deprivation (GOD; medium depleting glucose and gassed with 95% $N_2/5%\;CO_2$) was done in 6th and 7th tube. The radioactivities in each buffer and the tissue were counted using liquid scintillation counter and the results were expressed as a percentage of the total radioactivities. When slices were exposed to GOD for 20 mins, the spontaneous release of $[^3H]-5-HT$ was markedly increased and this increase of $[^3H]-5-HT$ release was blocked by adenosine ($10\;{\mu}M$) or DL-2-amino-5-phosphonovaleric acid (APV; $30\;{\mu}M$). Adenosine $A_1$ receptor specific antagonist, 8-cyclopentyl-1,3-dipropylxanthine (DPCPX) exacerbate GOD-induced increase of spontaneous release of $[^3H]-5-HT$. These results suggest that Adenosine may play a role in the GOD-induced spontaneous release of $[^3H]-5-HT$ through adenosine $A_1$ receptor activity.

• Clinical and Experimental Pediatrics
• /
• 제49권5호
• /
• pp.558-564
• /
• 2006

목 적 : 경뇌 전자기 자극법은 변조 자기장을 이용하여 뇌세포에 대한 직접적인 영향을 주지 않으면서 중추 신경계를 자극할 수 있는 비침습적인 방법이다. 이전의 연구들은 대부분 생체 동물을 대상으로 수행되어져 왔으며 배양 조직에서의 연구는 별로 이루어진 바 없다. 이에 본 연구에서는 배양된 해마 절편에서 다른 주파수의 전자기 자극이 신경원에 미치는 영향과 약물에 의한 세포 손상 후 전자기 자극의 세포보호효과 여부에 대해 알아보고자 하였다. 방 법 : 생후 8일된 실험쥐의 대뇌를 적출하여 dissection microscope 하에서 양쪽 해마 부위를 분리하고 tissue chopper를 이용하여 $450{\mu}M$ 두께로 절편을 만든 후 Stoppini가 고안한 방법대로 배양을 시행하였다. 각각 5개의 건강한 해마 절편이 포함된 inserts를 선택하고, 전자기 자극군에 대해 0.67 Hz와 50 Hz의 주파수로 각각 배양 5일부터 3일 간격으로 6차례 전자기 자극을 가하였다. 또한, 배양 제 14일에 inserts 2개에 $100{\mu}M$ NMDA에 노출시키고 3일 후부터 3일 간격으로 insert 1개에 전자기 자극을 3차례 시행하였고 다른 1개의 insert와 대조군에는 자극을 가하지 않았다. 결 과 : 전자기 자극 후 신경원의 활성도를 알아보기 위해 NeuN 단백 발현을 western blotting을 이용하여 측정한 후 ${\beta}$-actin 단백 발현과의 비를 얻어 각 군에서 비교 분석하였다. 대조군($1.01{\pm}0.27$)에 비해 전자기 자극군에서 NeuN의 발현이 증가되어 있었으며, 특히 저주파 자극군($1.12{\pm}0.14$)에서보다 고주파 자극군($1.27{\pm}0.17$)에서 현저하였고 고주파 자극군에서는 대조군에 비해 통계적으로 유의한 증가를 보였다(P<0.05). 또한, NMDA 노출 후 실험군(전자기 자극군 : $1.15{\pm}0.27$, 전자기 비자극군 : $0.92{\pm}0.09$)에서 대조군($1.26{\pm}0.04$)에 비해 NeuN 발현이 감소되었으나 전자기 비자극군에서 더 많이 감소한 것을 알 수 있었다. 결 론 : 배양된 해마조직의 신경세포에 대한 전자기 자극은 저주파 자극군에 비해 고주파 자극군에서 대조군보다 통계적으로 유의한 수준의 NeuN 발현의 증가를 관찰할 수 있었고, NMDA 노출 후 전자기 자극을 가한 군에서 대조군보다 NeuN 발현 감소가 관찰되기는 하였으나 고주파 자극군에서는 통계적으로 유의하지 않은 정도였던 것으로 보아 전자기 자극이 신경원 활성을 증가시켜 신경세포의 발생 및 증식을 유도하며 세포 손상에 대한 신경보호효과도 보인다는 것을 알 수 있었다. 따라서 전자기 자극은 여러 신경 질환에 있어서 치료적 역할을 할 수 있는 가능성이 있다고 사료된다.