• 한국수정란이식학회지
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• 제19권2호
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• pp.89-99
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• 2004

음압에 의한 세포막 신전으로 열리는 Stretch-activated channel(SAC)은 세포의 부피조적, 세포의 분화, 혈관 긴장도의 조절, 호르몬 분비 조절에서 SAC 존재 유무를 확인하기 위하여 patch clamp기법을 시행하여 SAC의 조절기전과 전기생리학적인 성질을 조사하였다. 음압이 주어지기 전에는 관찰되지 않던 단일통로 전류가 -20 cm$H_2O$이하의 음압이 주어졌을 때 관찰되었다. 음압에 의해 열리는 단일통로 전류는 $Na^+$이나 $K^+$과 같은 일가 양이온이 존재할 때 관찰되었으나 대신 비투과성인 tetramethylamonium이나 meglumine과 같은 양이온으로 교환해 주면 나타나지 않았다. 이는 이 단일 통로 전류가 양이온만을 투과시키는 nonselective cationic channel(NSC)을 통하여 이동하는 stretch-activated NSC(SA-NSC)임을 시사하였다. 이 SA-NSC 전류는 적혈구나 양서류 난자에서 관찰된 SAC의 전류-전압 관계와 유사한 inward rectification 양상을 나타내었으며 PKA에 의하여 통로활성이 증가하였다. 햄스터 난자에서 관찰되는 SA-NSC는 수정 전부터 2-세포 배아기까지 관찰되었으며 통로전류의 크기는 수정란과 1-세포기 배아에서 가장 크게 관찰되었으며 2-세포기 배아에서는 그 크기가 현저하게 감소하였다. 이와 같이 본 연구에서는 햄스터 난자의 발생 초기 단계에서 전기생리학적 기법을 사용하여 처음으로 SA-NSC존재를 직접 확인하였다. 세포 항상성 유지에 필수적인 이 통로의 일반적인 속성으로 미루어 보아, 햄스터 난자의 수정 전후 난자의 활성과 초기 배아 분화 및 발달에 필수적인 역할을 할 것으로 생각된다.}$1.50개였다. 또한 배란된 성숙난자의 채란 율은 각각 70.2, 74.7 및 54.3%로서 41~50시간째에 회수하였을 때가 가장 낮았다. 두당 회수율에 있어서도 8.25${\pm}$1.34, 8.87${\pm}$1.10 및 5.00${\pm}$1.30개로서 회수시간에 따른 유의적인 차이는 없었다. 회수한 난포내 미성숙 난자의 등급에 있어서 회수시간대별 1등급은 각각 24.2, 19.5 및 12.0%였으며, 2등급의 경우는 41~50시간이 4.0%로서 29~34시간과 35~40시간의 14.4% 및 16.2%보다 유의적(P<0.05)으로 낮았다. 난자의 pH 조절과 용적조절과 같은 생리적 환경 조성에 관여할 것으로 추정된다.았으며, 난포내 난자의 회수율은 투여 호르몬 및 반복사용 여부에 따른 차이는 없었다.떤 특정한 질환의 환자가 상대적으로 많을 가능성이 있으므로 국내에서의 소아 신질환의 발병형태를 보다 체계적으로 조사하고 이를 자료화하기 위해서는 개별 기관들의 연구결과만으로는 미흡하다고 생각되며, 이를 위해서는 전국적인 협동조사가 필요하다고 사료된다.9%$, 좌측 $22.2{\pm}3.9%$, 전체 $44.2{\pm}7.8%$보다 유의하게 감소되었다(p<0.01). 4) 양측성 미만성 결손을 보인 급성 신우신염시 상대적 신섭취율은 우측 $48.9{\pm}1.9%$, 좌측 $51.0{\pm}1.9%$로 대조군의 우측 $49.4{\pm}2.6%$, 좌측 $50.2{\pm}2.5%$에 비해 유의한 차이가 없었으나 절대적 신섭취율은 우측 $18.1{\pm}3.9%$,

• 대한화학회지
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• 제27권2호
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• pp.127-132
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• 1983

톨루엔의 동종간 주고 받기 반응에 대한 ZSM-5 촉매의 활성은 양이온의 종류, 이온교환을 그리고 반응온도에 좌우된다. 활성은 알카리금속, 알카리토금속, 수소, 희토류 금속 이온이 교환되는 순서로 증가하며 이온 교환도가 증가함에 따라 감소한다. 이온 교환된 ZSM-5 촉매중에서 Cs-ZSM-5만이 p-크실렌에 대해 우세한 선택성을 나타내는데 p-크실렌에 대한 선택성은 세슘이온 교환율이 증가할 수록 반응온도가 감소 할수록 증가한다. 이러한 현상은 ZSM-5의 세공 교차점에 있는 세슘이온이 부분적으로 세공을 막아주는 형상 선택성으로 해석된다.

• Nuclear Engineering and Technology
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• 제55권2호
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• pp.640-647
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• 2023

Material corrosion in nuclear power plant (NPP) is not controlled only by amine injection but also by ion exchange (IX) which is the best option to remove trace Na⁺. This study was conducted to understand the Na⁺ leakage characteristics of IX beds packed with ethanolamine-form (ETAH-form) and hydrogen-form (H-form) resins in the simulated water-steam cycle in terms of intrinsic behaviors of four kinds of cation-exchange resins through ASTM test and Vanselow mass action modeling. Na⁺ was inappreciably escaped throughout the channel created in resin layer. Na⁺ leakage from IX bed was non-linearly raised because of its decreasing selectivity with increasing Na⁺ capture and with increasing the fraction of ETAH-form resin. Na⁺ did not reach the breakthrough earlier than ETAH⁺ and NH₄⁺ due to the increased selectivity of Na⁺ to the cation-exchange resin (H⁺ < ETAH⁺ < NH₄⁺ ≪ Na⁺) at the feed composition. Na⁺ leakage from the resin bed filled with small particles was decreased due to the enhanced dynamic IX processes, regardless of its low selectivity. Thus, the particle size is a predominant factor among intrinsic properties of IX resin to reduce Na⁺ leakage from the condensate polishing plant (CPP) in NPPs.

• Animal cells and systems
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• 제15권2호
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• pp.95-106
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• 2011

The transient receptor potential vanilloid 4 (TRPV4) cation channel, a member of the TRP vanilloid subfamily, is expressed in a broad range of tissues. Nitric oxide (NO) as a gaseous signal mediator shows a variety of important biological effects. In many instances, NO has been shown to exhibit its activities via a protein S-nitrosylation mechanism in order to regulate its protein functions. With functional assays via site-directed mutagenesis, we demonstrate herein that NO induces the S-nitrosylation of TRPV4 $Ca^{2+}$ channel on the $Cys^{853}$ residue, and the S-nitrosylation of $Cys^{853}$ reduced its channel sensitivity to 4-${\alpha}$ phorbol 12,13-didecanoate and the interaction between TRPV4 and calmodulin. A patch clamp experiment and $Ca^{2+}$ image analysis show that the S-nitrosylation of $Cys^{853}$ modulates the TRPV4 channel as an inhibitor. Thus, our data suggest a novel regulatory mechanism of TRPV4 via NO-mediated S-nitrosylation on its $Cys^{853}$ residue.

• 한국생물물리학회:학술대회논문집
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• 한국생물물리학회 2001년도 학술 발표회 진행표 및 논문초록
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• pp.37-37
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• 2001

Cyclic nucleotide-gated (CNG) channels are composed of homo or hetero tetramer of ${\alpha}$ and ${\beta}$ subunits. The a subunits of these channels have a conserved glutamate residue within the pore-forming region. This residue determines the selectivity as well as the affinity for the extracellular divalent cations. Using the high affinity mutant (E363D) of bovine retinal CNG channel in which the Glu was replaced to Asp at position 363, we constructed tandem dimers and investigated the binding symmetry of divalent cation to the site.(omitted)

• 한국생물물리학회:학술대회논문집
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• 한국생물물리학회 1997년도 학술발표회
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• pp.26-26
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• 1997

In the present study, we recorded CCh-activated nonselective cation (NSC) current in guinea-pig gastric smooth muscle cells and investigated the characteristics of the current. In whole-cell voltage-clamp mode, CCh activated NSC current. The same NSC current could be activated by internal dialysis of GTP${\gamma}$S.(omitted)

• Molecules and Cells
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• 제27권2호
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• pp.167-173
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• 2009

The classical type of transient receptor potential (TRPC) channel is a molecular candidate for $Ca^{2+}$-permeable cation channels in mammalian cells. Because TRPC4 and TRPC5 belong to the same subfamily of TRPC, they have been assumed to have the same physiological properties. However, we found that TRPC4 had its own functional characteristics different from those of TRPC5. TRPC4 channels had no constitutive activity and were activated by muscarinic stimulation only when a muscarinic receptor was co-expressed with TRPC4 in human embryonic kidney (HEK) cells. Endogenous muscarinic receptor appeared not to interact with TRPC4. TPRC4 activation by $GTP{\gamma}S$ was not desensitized. TPRC4 activation by $GTP{\gamma}S$ was not inhibited by either Rho kinase inhibitor or MLCK inhibitor. TRPC4 was sensitive to external pH with $pK_a$ of 7.3. Finally, TPRC4 activation by $GTP{\gamma}S$ was inhibited by the calmodulin inhibitor W-7. We conclude that TRPC4 and TRPC5 have different properties and their own physiological roles.

• International Journal of Oral Biology
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• 제43권1호
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• pp.23-27
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• 2018

Increased intracellular levels of $Ca^{2+}$ are generally thought to negatively regulate lipolysis in mature adipocytes, whereas store-operated $Ca^{2+}$ entry was recently reported to facilitate lipolysis and attenuate lipotoxicity by inducing lipophagy. Transient receptor potential mucolipin1 (TRPML1), a $Ca^{2+}$-permeable non-selective cation channel, is mainly expressed on the lysosomal membrane and plays key roles in lysosomal homeostasis and membrane trafficking. However, the roles of TRPML1 in lipolysis remains unclear. In this study, we examined whether the channel function of TRPML1 induces lipolysis in mature adipocytes. We found that treatment of mature adipocytes with ML-SA1, a specific agonist of TRPML1, solely upregulated extracellular glycerol release, but not to the same extent as isoproterenol. In addition, knockdown of TRPML1 in mature adipocytes significantly reduced autophagic flux, regardless of ML-SA1 treatment. Our findings demonstrate that the channel function of TRPML1 partially contributes to lipid metabolism and autophagic membrane trafficking, suggesting that TRPML1, particularly the channel function of TRPML1, is as therapeutic target molecule for treating obesity.

• The Korean Journal of Physiology and Pharmacology
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• 제16권1호
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• pp.25-30
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• 2012

Under some pathological conditions as bile flow obstruction or liver diseases with the enterohepatic circulation being disrupted, regurgitation of bile acids into the systemic circulation occurs and the plasma level of bile acids increases. Bile acids in circulation may affect the nervous system. We examined this possibility by studying the effects of bile acids on gating of neuronal (N)-type $Ca^{2+}$ channel that is essential for neurotransmitter release at synapses of the peripheral and central nervous system. N-type $Ca^{2+}$ channel currents were recorded from bullfrog sympathetic neuron under a cell-attached mode using 100 mM $Ba^{2+}$ as a charge carrier. Cholic acid (CA, $10^{-6}M$) that is relatively hydrophilic thus less cytotoxic was included in the pipette solution. CA suppressed the open probability of N-type $Ca^{2+}$ channel, which appeared to be due to an increase in (no activity) sweeps. For example, the proportion of sweep in the presence of CA was ~40% at +40 mV as compared with ~8% in the control recorded without CA. Other single channel properties including slope conductance, single channel current amplitude, open and shut times were not significantly affected by CA being present. The results suggest that CA could modulate N-type $Ca^{2+}$ channel gating at a concentration as low as $10^{-6}M$. Bile acids have been shown to activate nonselective cation conductance and depolarize the cell membrane. Under pathological conditions with increased circulating bile acids, CA suppression of N-type $Ca^{2+}$ channel function may be beneficial against overexcitation of the synapses.

• The Korean Journal of Physiology and Pharmacology
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• 제27권2호
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• pp.187-196
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• 2023

Transient receptor potential canonical (TRPC) channels are non-selective calcium-permeable cation channels. It is suggested that TRPC4β is regulated by phospholipase C (PLC) signaling and is especially maintained by phosphatidylinositol 4,5-bisphosphate (PIP₂). In this study, we present the regulation mechanism of the TRPC4 channel with PIP₂ hydrolysis which is mediated by a channel-bound PLCδ1 but not by the G_qPCR signaling pathway. Our electrophysiological recordings demonstrate that the Ca²⁺ via an open TRPC4 channel activates PLCδ1 in the physiological range, and it causes the decrease of current amplitude. The existence of PLCδ1 accelerated PIP₂ depletion when the channel was activated by an agonist. Interestingly, PLCδ1 mutants which have lost the ability to regulate PIP₂ level failed to reduce the TRPC4 current amplitude. Our results demonstrate that TRPC4 self-regulates its activity by allowing Ca²⁺ ions into the cell and promoting the PIP₂ hydrolyzing activity of PLCδ1.