• Molecules and Cells
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• 제38권6호
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• pp.573-579
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• 2015

Apolipoprotein A-I and A-IV are protein constituents of high-density lipoproteins although their functional difference in lipoprotein metabolism is still unclear. To compare anti-atherogenic properties between apoA-I and apoA-4, we characterized both proteins in lipid-free and lipidbound state. In lipid-free state, apoA4 showed two distinct bands, around 78 and $67{\AA}$ on native gel electrophoresis, while apoA-I showed scattered band pattern less than $71{\AA}$. In reconstituted HDL (rHDL) state, apoA-4 showed three major bands around $101{\AA}$ and $113{\AA}$, while apoA-I-rHDL showed almost single band around $98{\AA}$ size. Lipid-free apoA-I showed 2.9-fold higher phospholipid binding ability than apoA-4. In lipid-free state, $BS_3$-crosslinking revealed that apoA-4 showed less multimerization tendency upto dimer, while apoA-I showed pentamerization. In rHDL state (95:1), apoA-4 was existed as dimer as like as apoA-I. With higher phospholipid content (255:1), five apoA-I and three apoA-4 were required to the bigger rHDL formation. Regardless of particle size, apoA-I-rHDL showed superior LCAT activation ability than apoA-4-rHDL. Uptake of acetylated LDL was inhibited by apoA-I in both lipid-free and lipid-bound state, while apoA-4 inhibited it only lipid-free state. ApoA-4 showed less anti-atherogenic activity with more sensitivity to glycation. In conclusion, apoA-4 showed inferior physiological functions in lipid-bound state, compared with those of apoA-I, to induce more pro-atherosclerotic properties.

• Molecules and Cells
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• 제27권3호
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• pp.291-297
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• 2009

Apolipoprotein (apo) C-III is a marker protein of triacylglycerol (TG)-rich lipoproteins and high-density lipoproteins (HDL), and has been proposed as a risk factor of coronary heart disease. To compare the physiologic role of reconstituted HDL (rHDL) with or without apoC-III, we synthesized rHDL with molar ratios of apoA-I:apoC-III of 1:0, 1:0.5, 1:1, and 1:2. Increasing the apoC-III content in rHDL produced smaller rHDL particles with a lower number of apoA-I molecules. Furthermore, increasing the molar ratio of apoC-III in rHDL enhanced the surfactant-like properties and the ability to lyse dimyristoyl phosphatidylcholine. Furthermore, rHDL containing apoC-III was found to be more resistant to particle rearrangement in the presence of low-density lipoprotein (LDL) than rHDL that contained apoA-I alone. In addition, the lecithin:cholesterol acyltransferase (LCAT) activation ability was reduced as the apoC-III content of the rHDL increased; however, the CE transfer ability was not decreased by the increase of apoC-III. Finally, rHDL containing apoC-III aggravated the production of MDA in cell culture media, which led to increased cellular uptake of LDL. Thus, the addition of apoC-III to rHDL induced changes in the structural and functional properties of the rHDL, especially in particle size and rearrangement and LCAT activation. These alterations may lead to beneficial functions of HDL, which is involved in anti-atherogenic properties in the circulation.

• Clinical and Experimental Pediatrics
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• 제51권1호
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• pp.42-46
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• 2008

대 상 : Apolipoprotein E (Apo E)는 지단백 대사와 지질의 수송에 중요한 역할을 하는 물질이며 많은 연구들에 의해 Apo E의 다형성이 심혈관계 질환의 중요한 유전 인자임이 알려져 있다. 이에 저자들은 Apo E 의 다형성이 비만 청소년에서 이상 지혈증의 위험도를 증가시키는지를 알아보고자 하였으며 Apo E가 비만 청소년 중에서도 심혈관계 합병증의 위험성이 높은 군을 선별하여 적극적인 치료를 하는 기준이 될 수 있는지를 확인하기 위해 본 연구를 시행하였다. 방 법 : 14-18세의 86명의 비만아(각 연령 및 성별에 따른 체질량 지수[body mass index; BMI] 95백분위수 이상)를 대상으로 하였으며 8시간 금식 후 시행한 혈액검사를 통해 혈당, apolipoprotein (Apo) A1, Apo B, 총콜레스테롤(total cholesterol; TC), 중성지방(triglyceride; TG), 저밀도 콜레스테롤(LDL), 고밀도 콜레스테롤(HDL)을 측정하였고 polymerase chain reaction-restriction fragment length polymorphism (PCR-RFLP)를 통해 Apo E의 다형성을 검사하였다. 결 과 : 남아와 여아의 비는 1.7이었으며 86명의 평균 나이는 $16.2{\pm}1.8$세이었고 평균 BMI는 $27.4{\pm}2.5kg/m^2$이었다. 유전자 분석에 따른 아형의 빈도(allele frequency)는 ${\varepsilon}2$형이 8.1%, ${\varepsilon}3$형이 87.2%, ${\varepsilon}4$형이 4.7%이었다. Apo E의 유전자형에 따라 ${\varepsilon}2/{\varepsilon}3$와 ${\varepsilon}2/{\varepsilon}3$는 E2군으로 ${\varepsilon}3/{\varepsilon}3$는 E3군, ${\varepsilon}3/{\varepsilon}4$와 ${\varepsilon}4/{\varepsilon}4$는 E4군으로 분류하였고 E2군은 13명(15.1%), E3군은 65명(75.6%), E4군은 8명(9.3%)이었다. 세 군 사이에 나이, 성별, 체중, 키와 BMI는 차이가 없었다. 고지혈증에 대한 검사에서 혈당, Apo A1, TC, TG, HDL은 각 군간 차이를 보이지 않았으며 Apo B와 LDL만이 E4형에서 유의하게 높은 수치를 보였다(P<0.05). 결 론 : 저자들은 본 연구를 통해 비만아에서 Apo E의 유전자형의 빈도를 알 수 있었으며 Apo B와 LDL 농도가 Apo E의 유전자형에 따라 차이가 있음을 확인할 수 있었고 따라서 비만아 중에서도 특정 Apo E4의 유전형을 가진 경우 이상 지혈증의 위험성이 더 높은 것으로 사료된다.

• 생명과학회지
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• 제21권1호
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• pp.22-30
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• 2011

아포지방단백 A-I (apoA-I)은 항염증 및 항산화 작용을 가지고 있는 것으로 알려져 있다. 본 논문에서는 인간 혈액의 호중구를 이용하여 in vitro 상태에서 세포사멸과 시토카인의 분비 과정에 미치는 apoA-I의 영향을 조사하였다. 인간 호중구에 apoA-I을 처리한 결과 세포사멸의 정도가 감소되었다. 또한, apoA-I을 함유하는 고밀도 지방단백(HDL)에 의하여도 세포사멸은 현저히 감소되었다. HDL이 결합하는 수용체인 scavenger 수용체 B-1에 대한 항체에 의하여도 세포사멸은 억제되었다. ApoA-I을 20 시간 처리한 세포의 배양액내 인터루킨-8, 인터페론-유도단백질 10(IP-10) 및 종양괴사인자-α의 분비가 현저히 증가하였다. 호중구에 인터페론 감마와 apoA-I을 동시 처리하였을 때 시토카인 중에서 IP-10과 종양괴사인자-$\alpha$의 분비가 단독으로 처리한 경우에 비해 현저히 증가되었다. 이러한 결과들은 인간 혈액 호중구에 apoA-I을 처리한 경우 호중구가 활성화되고 호중구의 세포사멸이 지연된다는 것을 제시하는 것으로 apoA-I이 호중구에 대하여 염증성 인자로 작용할 것으로 추정된다.

• 한국산학기술학회논문지
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• 제17권10호
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• pp.199-203
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• 2016

아포리포포린-III (apoLp-III)를 꿀벌부채명나방 종령 유충 혈림프로부터 KBr 농도구배 초원심분리와 겔크로마토그래피(Sephadex G-100)를 이용하여 분리, 정제하였다. KBr 농도구배 초원심분리가 끝난 후, 리포포린을 제외한 분획 (lipophorin-free fractions)을 겔크로마토그래피 시료로 사용하였으며, 겔크로마토그래피를 행한후 sodium dodecyl sulfate (SDS)-전기영동으로 apoLp-III의 정제를 확인하였다. 또한, 본 연구에서는 유충 혈림프로부터 정제된 apoLp-III가 꿀벌부채명나방의 성충 정소에 의해 흡수되는 지를 조사하였다. 우화한 지 1일 또는 2일된 성충으로부터 성충 정소를 차가운 링거액에서 분리한 후 조직 배양의 시료로 사용하였다. 순수 정제한 apoLp-III를 dimethyl sulfoxide (DMSO)에 녹인 형광물질 fluorescein isothiocyanate (FITC)와 상온에서 계속 저어가면서 1시간 동안 배양하였다. FITC로 표지된 apoLp-III (FITC-labeled apoLp-III)를 Sephadex G-25 PD-10 column을 이용하여 정제하고 확인하였다. 정제된 FITC-labeled apoLp-III와 성충 정소 조직을 상온에서 30분간 배양하였다. 배양 후 형광현미경 (fluorescence Axioskop microscope)과 SDS-전기영동을 이용하여 FITC-labeled apoLp-III가 정소 조직으로 들어가는 지의 여부를 확인하였다. 그 결과 FITC-labeled apoLp-III가 성충 정소로 흡수된다는 사실을 알 수 있었다.

• Journal of Genetic Medicine
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• 제3권1호
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• pp.29-32
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• 1999

The Apolipoprotein E type 4 allele (ApoE ${\varepsilon}4$) is genetically associated with the common late onset familial and sporadic forms of Alzheimer's disease. The BchE-k variant, which is the common variant of the BchE gene, has been reported to show allelic association with AD in subjects who are also carriers of the ${\varepsilon}4$ allele of the ApoE, especially in subjects over the age of 75. This study was performed to evaluate the distribution of the ApoE and the BchE genotypes in the healthy and AD groups and to evaluate the synergy between the BchE-k variant and the ApoE ${\varepsilon}4$ in AD. The ApoE and the BchE genotypes were determined in DNA samples from 610 healthy people and 60 LOAD patients by using ARMS by standard agarose gel electrophoresis. The effect of the ApoE ${\varepsilon}4$ was closely related to AD(p<0.05). A comparison between the AD patients and the healthy individuals, both with the ${\varepsilon}4$ allele, indicated an interaction between the BchE-k and the ApoE ${\varepsilon}4$(p<0.05). The association of the BchE-k with AD was limited to carriers of the ApoE ${\varepsilon}4$ allele, among whom the presence of the BchE-k gave an odds ratio of AD 3.48 (95% C.I. 1.3-9.2). Therefore, these results suggested that further evidence of an association between the ApoE ${\varepsilon}4$ and LOAD, and the BchE-k acts in synergy with the ApoE ${\varepsilon}4$ as a susceptibility gene for AD.

• IMMUNE NETWORK
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• 제3권2호
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• pp.145-149
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• 2003

Background: Apoptosis has been implicated in pathogenesis of various disease. Apo-1/Fas (CD95) is one of the main pathway of apoptosis. To examine the possible relationship between Apo-1/Fas (CD95) and primary knee osteoarthritis, MvaI restriction length polymorphism (RFLP) in human Apo-1/Fas (CD95) gene was assessed. Methods: Genotype and allele frequencies in promoter region in the Apo-1/Fas (CD95) gene were studied by PCR-RFLP in 226 Korean controls and 148 Korean patients with primary knee osteoarthritis. Results: No statistically significant difference in the genotypic distribution and allelic frequencies was found between the control and the knee oateoarthritis patients. But in the severe grade (grade 3, 4) Kellgren-Lawrence score patients, the frequency of $MvaI^*1$ (G) allele was significantly decreased (P=0.0392) and the of $MvaI^*2$ (A) allele frequency was significantly increased (P=0.0473) compared to the normal controls. Conclusion: Apo-1/Fas (CD95) gene polymorphism is a part a determinant factor of severity in knee osteoarthritis, the patients with $MvaI^*2$ (A) allele is more severe radiologic progression. Further substantiation studies are needed in larger patient samples and various other apoptosis related genes to elucidate the mechanism of osteoarthritis, including the Fas ligand gene analysis.

• Preventive Nutrition and Food Science
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• 제7권4호
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• pp.353-357
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• 2002

We have previously demonstrated that kudzu root extracts have a hypocholesterolemic effect on rats fed diets high in fat and cholesterol. To further elucidate the mechanism involved, in this study we investigated the effect of water extracts of kudzu root, Pueraria radix, on the production of apolipoprotein B$_{100}$ (APo B$_{100}$) in HepG$_2$ liver cells and secretion of apolipoprotein B$_{48}$ (Apo B$_{48}$) in Caco$_2$ cells. Human cell lines, HepG$_2$ liver cells and Caco$_2$ intestinal epithelial cells, were grown with various concentrations (0%, 0.5%, 1.0%, 1.5%, 2.0%) of water extracts of kudzu root in the media. The kudzu root extract decreased Apo B$_{100}$ production and secretion. Treatment of HeP G$_2$ cells with the kudzu root extract also significantly decreased the intracellular total and free cholesterol concentration, and also decreased esterified cholesterol but was only significant at the highest dose of 2%. Apo B$_{48}$ production, but not secretion, from enterocytes was lowered by the kudzu root extracts. This research provided evidence that the hypocholesterolemic properties of kudzu root may be a consequence of decreased production and secretion of Apo B$_{100}$ in the liver and Apo B$_{48}$ in the intestine.

• Molecules and Cells
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• 제37권11호
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• pp.767-776
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• 2014

Alzheimer's disease (AD) is clinically characterized with progressive memory loss and cognitive decline. Synaptic dysfunction is an early pathological feature that occurs prior to neurodegeneration and memory dysfunction. Mounting evidence suggests that aggregation of amyloid-${\alpha}$ ($A{\alpha}$) and hyperphosphorylated tau leads to synaptic deficits and neurodegeneration, thereby to memory loss. Among the established genetic risk factors for AD, the ${\varepsilon}4$ allele of apolipoprotein E (APOE) is the strongest genetic risk factor. We and others previously demonstrated that apoE regulates $A{\alpha}$ aggregation and clearance in an isoform-dependent manner. While the effect of apoE on $A{\alpha}$ may explain how apoE isoforms differentially affect AD pathogenesis, there are also other underexplored pathogenic mechanisms. They include differential effects of apoE on cerebral energy metabolism, neuroinflammation, neurovascular function, neurogenesis, and synaptic plasticity. ApoE is a major carrier of cholesterols that are required for neuronal activity and injury repair in the brain. Although there are a few conflicting findings and the underlying mechanism is still unclear, several lines of studies demonstrated that apoE4 leads to synaptic deficits and impairment in long-term potentiation, memory and cognition. In this review, we summarize current understanding of apoE function in the brain, with a particular emphasis on its role in synaptic plasticity and the underlying cellular and molecular mechanisms, involving low-density lipoprotein receptor-related protein 1 (LRP1), syndecan, and LRP8/ApoER2.

• 생물정신의학
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• 제10권2호
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• pp.121-125
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• 2003

Objective:Recently, many experimental evidences have been reported that psychiatric diseases are closely related with neurodevelopmental abnormalities and this can be properly explained by apoptosis. It is known that Apo-1/Fas is one of the genes in charge of apoptosis related with neurodevelopmental abnormalities. In this study, the association between bipolar disorder and functional polymorphism in Apo-1/Fas promoter gene has been investigated. Method:For 81 bipolar disorder patients and 217 healthy control subjects, MvaI restriction fragment length polymorphism(RFLP) of Apo-1/Fas promoter gene was analyzed after polymerase chain reaction(PCR) amplification. Result:There was a statistical significant difference in genotypic distribution(${\chi}^2$=16.656, df=2, p=0.0002) and allelic frequencies(${\chi}^2$=14.225, df=1, p=0.0002) between bipolar disorder patients and healthy control subjects. Conclusion:Our results suggest an association between functional polymorphism in Apo-1/Fas promoter gene and bipolar disorder and provide the important genetic information related with the pathogenesis of the disease. Further studies employing larger samples are required to clarify the present results.