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维基百科

载脂蛋白A1

載脂蛋白A1(英語:Apolipoprotein A1,簡稱ApoA1)為附著於高密度脂蛋白(HDL)及乳靡小球上的載脂蛋白,基因編碼為「APOA1[1][2]。載脂蛋白A1可以活化卵磷脂-胆固醇酰基转移酶英语Lecithin—cholesterol acyltransferase(Lecithin Cholesterol Acyltransferase,LCAT);當高密度脂蛋白運送組織中多餘的膽固醇回到肝臟細胞中時,載脂蛋白A1同時也可作為高密度脂蛋白的配體,在脂質代謝英语lipid metabolism中扮演重要角色。研究指出,APOA1的mRNA是由反義RNA轉譯出的內源性蛋白質所調控[3]

Apolipoprotein A-I
载脂蛋白A1
PDB rendering based on 1av1.
有效结构
PDB 直系同源检索:PDBe, RCSB
标识
代号 APOA1; MGC117399
扩展标识 遗传学:107680 鼠基因:88049 同源基因:47900 ChEMBL: 5984 GeneCards: APOA1 Gene
RNA表达模式
更多表达数据
直系同源体
物种 人类 小鼠
Entrez 335 11806
Ensembl ENSG00000118137 ENSMUSG00000032083
UniProt P02647 Q00623
mRNA序列 NM_000039 NM_009692
蛋白序列 NP_000030 NP_033822
基因位置 Chr 11:
116.71 – 116.71 Mb
Chr 9:
46.23 – 46.23 Mb
PubMed查询 [1] [2]

結構 编辑

APOA1基因位於第11對染色體上(11q23-q24),該基因包含4個外顯子[4]。载脂蛋白A1的質量為45.4 kDa ,含有 396 個胺基酸;質譜分析可觀察到蛋白質由21個胜肽片段組成[5][6]

功能 编辑

載脂蛋白A1(ApoA1)為構成血漿中高密度脂蛋白(HDL)蛋白質部分的主要成分。小腸腸道細胞所分泌的乳糜微粒中雖然也含有載脂蛋白A1,但在血流中很快就會被轉為HDL[7]。ApoA1可促進將周邊組織脂質及膽固醇回收至肝臟,並藉由膽管分泌至小腸。另外該蛋白也是卵磷脂-胆固醇酰基转移酶英语Lecithin—cholesterol acyltransferase(LCAT)的輔因子,製造了血漿中大多數的膽固醇脂英语cholesteryl esters。ApoA1同時也是前列环素(PGI2)的穩定因子,因此也具有抗凝血的作用[8]。如果編碼該蛋白的基因有缺陷,會導致個體體內缺乏HDL,導致包含Tangier disease英语Tangier disease在內的症狀,以及非神經性全身類澱粉變性[4]

由於ApoA1在體內脂質代謝的角色相當重要,因此常被視為預測個體冠心病風險的生物標記。有研究發現「apoB-100/apoA1」的比值預測心肌梗塞的效果比任何其他脂質標記更有效果[9]。ApoA1可利用ELISAnephelometry英语nephelometry檢驗。

臨床意義 编辑

交互作用途徑 编辑

点击基因、蛋白质和代谢产物的链接访问对应的介绍条目。 [§ 1]

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  1. ^ 这个相互作用途径可以在WikiPathways上编辑: Statin_Pathway_WP430. 

參見 编辑

參考文獻 编辑

  1. ^ Breslow, JL; Ross, D; McPherson, J; Williams, H; Kurnit, D; Nussbaum, AL; et al. Isolation and characterization of cDNA clones for human apolipoprotein A-I. Proc. Natl. Acad. Sci. U.S.A. November 1982, 79 (22): 6861–5. PMC 347233 . PMID 6294659. doi:10.1073/pnas.79.22.6861.  已忽略未知参数|author-name-separator= (帮助); 已忽略未知参数|author-separator= (帮助)
  2. ^ Arinami, T; Hirano, T; Kobayashi, K; Yamanouchi, Y; Hamaguchi, H. Assignment of the apolipoprotein A-I gene to 11q23 based on RFLP in a case with a partial deletion of chromosome 11, del(11)(q23.3----qter). Hum. Genet. June 1990, 85 (1): 39–40. PMID 1972696. doi:10.1007/BF00276323.  已忽略未知参数|author-name-separator= (帮助); 已忽略未知参数|author-separator= (帮助)
  3. ^ Halley, P; Kadakkuzha, BM; Faghihi, MA; Magistri, M; Zeier, Z; Khorkova, O; et al. Regulation of the Apolipoprotein Gene Cluster by a Long Noncoding RNA. Cell Reports. 16 January 2014, 6 (1): 222–230. PMID 24388749. doi:10.1016/j.celrep.2013.12.015.  已忽略未知参数|author-name-separator= (帮助); 已忽略未知参数|author-separator= (帮助)
  4. ^ 4.0 4.1 Entrez Gene: APOA1 apolipoprotein A1. (原始内容于2019-10-16). 
  5. ^ ]Zong NC, Li H, Li H, Lam MP, Jimenez RC, Kim CS, Deng N, Kim AK, Choi JH, Zelaya I, Liem D, Meyer D, Odeberg J, Fang C, Lu HJ, Xu T, Weiss J, Duan H, Uhlen M, Yates JR, Apweiler R, Ge J, Hermjakob H, Ping P. Integration of cardiac proteome biology and medicine by a specialized knowledgebase. Circulation Research. Oct 2013, 113 (9): 1043–53. PMC 4076475 . PMID 23965338. doi:10.1161/CIRCRESAHA.113.301151. 
  6. ^ . Cardiac Organellar Protein Atlas Knowledgebase (COPaKB). [2016-08-13]. (原始内容存档于2016-03-05). 
  7. ^ Wasan KM, Brocks DR, Lee SD, Sachs-Barrable K, Thornton SJ. Impact of lipoproteins on the biological activity and disposition of hydrophobic drugs: implications for drug discovery. Nature Reviews Drug Discovery. January 2008, 7 (1): 84–99. PMID 18079757. doi:10.1038/nrd2353. 
  8. ^ Yui Y, Aoyama T, Morishita H, Takahashi M, Takatsu Y, Kawai C. Serum prostacyclin stabilizing factor is identical to apolipoprotein A1 (apo A1). A novel function of apo A1. J. Clin. Invest. 1988, 82 (3): 803–7. PMC 303586 . PMID 3047170. doi:10.1172/JCI113682. 
  9. ^ McQueen MJ, Hawken S, Wang X, Ounpuu S, Sniderman A, Probstfield J, Steyn K, Sanderson JE, Hasani M, Volkova E, Kazmi K, Yusuf S. Lipids, lipoproteins, and apolipoproteins as risk markers of myocardial infarction in 52 countries (the INTERHEART study): a case-control study. Lancet. 2008, 372 (9634): 224–33. PMID 18640459. doi:10.1016/S0140-6736(08)61076-4. 
  10. ^ Dastani Z, Dangoisse C, Boucher B, Desbiens K, Krimbou L, Dufour R, Hegele RA, Pajukanta P, Engert JC, Genest J, Marcil M. A novel nonsense apolipoprotein A-I mutation (apoA-I(E136X)) causes low HDL cholesterol in French Canadians. Atherosclerosis. March 2006, 185 (1): 127–36. PMID 16023124. doi:10.1016/j.atherosclerosis.2005.05.028. 
  11. ^ Franceschini G, Sirtori M, Gianfranceschi G, Sirtori CR. Relation between the HDL apoproteins and A-I isoproteins in subjects with the AIMilano abnormality. Metab. Clin. Exp. May 1981, 30 (5): 502–9. PMID 6785551. doi:10.1016/0026-0495(81)90188-8. 
  12. ^ Zhu X, Wu G, Zeng W, Xue H, Chen B. Cysteine mutants of human apolipoprotein A-I: a study of secondary structural and functional properties. J. Lipid Res. 2005, 46 (6): 1303–11. PMID 15805548. doi:10.1194/jlr.M400401-JLR200. 
  13. ^ Chiesa G, Sirtori CR. Apolipoprotein A-I(Milano): current perspectives. Curr. Opin. Lipidol. 2003, 14 (2): 159–63. PMID 12642784. doi:10.1097/00041433-200304000-00007. 
  14. ^ 14.0 14.1 Apo A-I-Milano Trial: Where are we now?. Cleveland Clinic. [2008-07-26]. (原始内容于2007-12-21). 
  15. ^ Nissen SE, Tsunoda T, Tuzcu EM, Schoenhagen P, Cooper CJ, Yasin M, Eaton GM, Lauer MA, Sheldon WS, Grines CL, Halpern S, Crowe T, Blankenship JC, Kerensky R. Effect of recombinant ApoA-I Milano on coronary atherosclerosis in patients with acute coronary syndromes: a randomized controlled trial. JAMA. November 2003, 290 (17): 2292–300. PMID 14600188. doi:10.1001/jama.290.17.2292. 
  16. ^ . Cedars-Sinai Heart Institute. [2008-07-26]. (原始内容存档于2007-12-21). 
  17. ^ Singh P, Singh M, Kaur TP, Grewal SS. A novel haplotype in ApoAI-CIII-AIV gene region is detrimental to Northwest Indians with coronary heart disease. Int. J. Cardiol. September 2007, 130 (3): e93–5. PMID 17825930. doi:10.1016/j.ijcard.2007.07.029. 
  18. ^ Singh P, Singh M, Gaur S, Kaur T. The ApoAI-CIII-AIV gene cluster and its relation to lipid levels in type 2 diabetes mellitus and coronary heart disease: determination of a novel susceptible haplotype. Diab Vasc Dis Res. June 2007, 4 (2): 124–9. PMID 17654446. doi:10.3132/dvdr.2007.030. 
  19. ^ Vollbach H, Heun R, Morris CM, Edwardson JA, McKeith IG, Jessen F, Schulz A, Maier W, Kölsch H. APOA1 polymorphism influences risk for early-onset non-familial AD. Ann. Neurol. 2005, 58 (3): 436–41. PMID 16130094. doi:10.1002/ana.20593. 
  20. ^ Maezawa I, Jin LW, Woltjer RL, Maeda N, Martin GM, Montine TJ, Montine KS. Apolipoprotein E isoforms and apolipoprotein A-I protect from amyloid precursor protein carboxy terminal fragment-associated cytotoxicity. J. Neurochem. 2004, 91 (6): 1312–21. PMID 15584908. doi:10.1111/j.1471-4159.2004.02818.x. 
  21. ^ Solomon A, Murphy CL, Kestler D, Coriu D, Weiss DT, Makovitzky J, Westermark P. Amyloid contained in the knee joint meniscus is formed from apolipoprotein A-I. Arthritis Rheum. 2006, 54 (11): 3545–50. PMID 17075859. doi:10.1002/art.22201. 
  22. ^ Ma J, Liao XL, Lou B, Wu MP. Role of apolipoprotein A-I in protecting against endotoxin toxicity. Acta Biochim. Biophys. Sin. (Shanghai). 2004, 36 (6): 419–24. PMID 15188057. doi:10.1093/abbs/36.6.419. 
  23. ^ Huang JT, Wang L, Prabakaran S, Wengenroth M, Lockstone HE, Koethe D, Gerth CW, Gross S, Schreiber D, Lilley K, Wayland M, Oxley D, Leweke FM, Bahn S. Independent protein-profiling studies show a decrease in apolipoprotein A1 levels in schizophrenia CSF, brain and peripheral tissues. Mol Psychiatry. 2007, 13 (12): 1118–28. PMID 17938634. doi:10.1038/sj.mp.4002108. 
  24. ^ Singh P, Singh M, Kaur T. Role of apolipoproteins E and A-I: Epistatic villains of triglyceride mediation in coronary heart disease. Int J Cardiol. 2008, 134 (3): 410–2. PMID 18378026. doi:10.1016/j.ijcard.2007.12.102. 
  25. ^ Wehmeier K, Beers A, Haas MJ, Wong NC, Steinmeyer A, Zugel U, Mooradian AD. Inhibition of apolipoprotein AI gene expression by 1, 25-dihydroxyvitamin D3. Biochim. Biophys. Acta. 2005, 1737 (1): 16–26. PMID 16236546. doi:10.1016/j.bbalip.2005.09.004. 
  26. ^ Lahoz C, Peña R, Mostaza JM, Jiménez J, Subirats E, Pintó X, Taboada M, López-Pastor A. Apo A-I promoter polymorphism influences basal HDL-cholesterol and its response to pravastatin therapy. Atherosclerosis. 2003, 168 (2): 289–95. PMID 12801612. doi:10.1016/S0021-9150(03)00094-7. 
  27. ^ Fitzgerald ML, Morris AL, Rhee JS, Andersson LP, Mendez AJ, Freeman MW. Naturally occurring mutations in the largest extracellular loops of ABCA1 can disrupt its direct interaction with apolipoprotein A-I. J. Biol. Chem. September 2002, 277 (36): 33178–87. PMID 12084722. doi:10.1074/jbc.M204996200. 
  28. ^ Deeg MA, Bierman EL, Cheung MC. GPI-specific phospholipase D associates with an apoA-I- and apoA-IV-containing complex. J. Lipid Res. March 2001, 42 (3): 442–51. PMID 11254757. 
  29. ^ Pussinen PJ, Jauhiainen M, Metso J, Pyle LE, Marcel YL, Fidge NH, Ehnholm C. Binding of phospholipid transfer protein (PLTP) to apolipoproteins A-I and A-II: location of a PLTP binding domain in the amino terminal region of apoA-I. J. Lipid Res. January 1998, 39 (1): 152–61. PMID 9469594. 
  30. ^ . (原始内容存档于2011-07-18). 

外部連結 编辑

载脂蛋白a1, 載脂蛋白a1, 英語, apolipoprotein, 簡稱apoa1, 為附著於高密度脂蛋白, 及乳靡小球上的載脂蛋白, 基因編碼為, apoa1, 載脂蛋白a1可以活化卵磷脂, 胆固醇酰基转移酶, 英语, lecithin, cholesterol, acyltransferase, lecithin, cholesterol, acyltransferase, lcat, 當高密度脂蛋白運送組織中多餘的膽固醇回到肝臟細胞中時, 載脂蛋白a1同時也可作為高密度脂蛋白的配體, 在脂質代謝, 英语,. 載脂蛋白A1 英語 Apolipoprotein A1 簡稱ApoA1 為附著於高密度脂蛋白 HDL 及乳靡小球上的載脂蛋白 基因編碼為 APOA1 1 2 載脂蛋白A1可以活化卵磷脂 胆固醇酰基转移酶 英语 Lecithin cholesterol acyltransferase Lecithin Cholesterol Acyltransferase LCAT 當高密度脂蛋白運送組織中多餘的膽固醇回到肝臟細胞中時 載脂蛋白A1同時也可作為高密度脂蛋白的配體 在脂質代謝 英语 lipid metabolism 中扮演重要角色 研究指出 APOA1的mRNA是由反義RNA轉譯出的內源性蛋白質所調控 3 Apolipoprotein A I载脂蛋白A1PDB rendering based on 1av1 有效结构PDB 直系同源检索 PDBe RCSBPDB查询代码列表1AV1 1GW3 1GW4 1ODP 1ODQ 1ODR 2A01 3J00 3K2S 3R2P标识代号APOA1 MGC117399扩展标识遗传学 107680 鼠基因 88049 同源基因 47900 ChEMBL 5984 GeneCards APOA1 Gene基因本体论描述分子功能 beta amyloid binding protein binding phospholipid binding phospholipid transporter activity high density lipoprotein particle binding cholesterol binding cholesterol transporter activity enzyme binding apolipoprotein receptor binding apolipoprotein A I receptor binding identical protein binding lipase inhibitor activity phosphatidylcholine sterol O acyltransferase activator activity high density lipoprotein particle receptor binding细胞成分 extracellular region extracellular space nucleus early endosome endoplasmic reticulum lumen cytosol plasma membrane endocytic vesicle cytoplasmic vesicle very low density lipoprotein particle high density lipoprotein particle spherical high density lipoprotein particle secretory granule lumen生物过程 retinoid metabolic process regulation of protein phosphorylation endothelial cell proliferation platelet degranulation negative regulation of cytokine secretion involved in immune response lipid metabolic process phosphatidylcholine biosynthetic process cholesterol biosynthetic process G protein coupled receptor signaling pathway response to nutrient blood coagulation phototransduction visible light cholesterol metabolic process glucocorticoid metabolic process negative regulation of tumor necrosis factor mediated signaling pathway positive regulation of cholesterol esterification negative regulation of very low density lipoprotein particle remodeling peripheral nervous system axon regeneration protein oxidation peptidyl methionine modification lipid storage platelet activation regulation of intestinal cholesterol absorption cholesterol transport adrenal gland development organ regeneration regulation of Cdc42 protein signal transduction cholesterol efflux phospholipid efflux negative regulation of heterotypic cell cell adhesion high density lipoprotein particle remodeling high density lipoprotein particle assembly high density lipoprotein particle clearance lipoprotein metabolic process lipoprotein biosynthetic process response to drug cholesterol homeostasis blood vessel endothelial cell migration response to estrogen stimulus reverse cholesterol transport cellular lipid metabolic process small molecule metabolic process negative regulation of interleukin 1 beta secretion negative regulation of inflammatory response protein stabilization positive regulation of hydrolase activity positive regulation of transferase activity transmembrane transport phospholipid homeostasis negative regulation of lipase activity negative regulation of cell adhesion molecule production negative regulation of response to cytokine stimulus triglyceride homeostasis cholesterol importSources Amigo QuickGORNA表达模式更多表达数据直系同源体物种人类小鼠Entrez33511806EnsemblENSG00000118137ENSMUSG00000032083UniProtP02647Q00623mRNA序列NM 000039NM 009692蛋白序列NP 000030NP 033822基因位置Chr 11 116 71 116 71 MbChr 9 46 23 46 23 MbPubMed查询 1 2 查论编 目录 1 結構 2 功能 3 臨床意義 3 1 Activity associated with high HDL C and protection from heart disease 3 2 Novel Haplotypes within apolipoprotein AI CIII AIV gene cluster 3 3 Role in other diseases 3 4 Epistatic impact of apo A1 3 5 Factors affecting apo A1 activity 4 交互作用 4 1 Potential binding partners 4 2 交互作用途徑 5 參見 6 參考文獻 7 外部連結結構 编辑APOA1基因位於第11對染色體上 11q23 q24 該基因包含4個外顯子 4 载脂蛋白A1的質量為45 4 kDa 含有 396 個胺基酸 質譜分析可觀察到蛋白質由21個胜肽片段組成 5 6 功能 编辑載脂蛋白A1 ApoA1 為構成血漿中高密度脂蛋白 HDL 蛋白質部分的主要成分 小腸腸道細胞所分泌的乳糜微粒中雖然也含有載脂蛋白A1 但在血流中很快就會被轉為HDL 7 ApoA1可促進將周邊組織脂質及膽固醇回收至肝臟 並藉由膽管分泌至小腸 另外該蛋白也是卵磷脂 胆固醇酰基转移酶 英语 Lecithin cholesterol acyltransferase LCAT 的輔因子 製造了血漿中大多數的膽固醇脂 英语 cholesteryl esters ApoA1同時也是前列环素 PGI2 的穩定因子 因此也具有抗凝血的作用 8 如果編碼該蛋白的基因有缺陷 會導致個體體內缺乏HDL 導致包含Tangier disease 英语 Tangier disease 在內的症狀 以及非神經性全身類澱粉變性 4 由於ApoA1在體內脂質代謝的角色相當重要 因此常被視為預測個體冠心病風險的生物標記 有研究發現 apoB 100 apoA1 的比值預測心肌梗塞的效果比任何其他脂質標記更有效果 9 ApoA1可利用ELISA或nephelometry 英语 nephelometry 檢驗 臨床意義 编辑已隱藏部分未翻譯内容 歡迎參與翻譯 Activity associated with high HDL C and protection from heart disease 编辑 As a major component of the high density lipoprotein complex protective fat removal particles apo A1 helps to clear fats including cholesterol from white blood cells within artery walls making the WBCs less likely to become fat overloaded transform into foam cells die and contribute to progressive atheroma 英语 atheroma Five of nine men found to carry a mutation E164X who were at least 35 years of age had developed premature coronary artery disease 10 One of four mutants of apo A1 is present in roughly 0 3 of the Japanese population but is found in 6 of those with low HDL cholesterol levels ApoA 1 Milano 英语 ApoA 1 Milano is a naturally occurring mutant of apo A1 found in a few families in Limone sul Garda Italy and by genetic church record family tree detective work traced to a single individual in the 14th century Described in 1980 it was the first known molecular abnormality of apolipoproteins 11 Paradoxically carriers of this mutation have very low HDL C HDL Cholesterol levels but no increase in the risk of heart disease often living to age 100 or older This unusual observation was what lead Italian investigators to track down what was going on and lead to the discovery of apo A1 Milano the city Milano 160 km away in which the researcher s lab was located Biochemically apo A1 contains an extra cysteine bridge causing it to exist as a homodimer or as a heterodimer with apo A II However the enhanced cardioprotective activity of this mutant which likely depends on fat amp cholesterol efflux cannot easily be replicated by other cysteine mutants 12 Recombinant apo A1 Milano dimers formulated into liposomes can reduce atheroma 英语 atheroma s in animal models by up to 30 13 Apo A1 Milano has also been shown in small clinical trials to have a statistically significant effect in reducing reversing plaque build up on arterial walls 14 15 In human trials the reversal of plaque build up was measured over the course of five weeks 14 16 Novel Haplotypes within apolipoprotein AI CIII AIV gene cluster 编辑 Lately two novel susceptibility haplotypes i e P2 S2 X1 and P1 S2 X1 have been discovered in ApoAI CIII AIV gene cluster on chromosome 11q23 which confer approximately threefold higher risk of coronary heart disease in normal 17 as well as in the patients having non insulin diabetes mellitus 18 Role in other diseases 编辑 A G A polymorphism in the promoter of the apo A1 gene has been associated with the age at which patients presented with Alzheimer disease 19 Protection from Alzheimer s disease by apo A1 may rely on a synergistic interaction with alpha tocopherol 英语 alpha tocopherol 20 Amyloid deposited in the knee following surgery consists largely of apo A1 secreted from chondrocytes cartilage cells 21 A wide variety of amyloidosis symptoms are associated with rare Apo A1 mutants Apo A I binds to lipopolysaccharide or endotoxin and has a major role in the anti endotoxin function of HDL 22 In one study a decrease in apo A1 levels was detected in schizophrenia patients CSF brain and peripheral tissues 23 Epistatic impact of apo A1 编辑 Apolipoprotein A1 and APOE interact epistatically to modulate triglyceride levels in coronary heart disease patients Individually neither apo A1 nor apo E was found to be associated with triglyceride TG levels but pairwise epistasis additive x additive model explored their significant synergistic contributions with raised TG levels P lt 0 01 24 Factors affecting apo A1 activity 编辑 Apo A1 production is decreased by calcitriol and increased by a drug that antagonizes it 25 Exercise or statin treatment may cause an increase in HDL C levels by inducing apo A1 production but this depends on the G A promoter polymorphism 26 交互作用 编辑 載脂蛋白A1可與下列蛋白產生交互作用 ABCA1 英语 ABCA1 27 GPLD1 英语 GPLD1 28 and PLTP 英语 PLTP 29 Potential binding partners 编辑 Apolipoprotein A1 binding precursor a relative of APOA 1 abbreviated APOA1BP 英语 APOA1BP has a predicted biochemical interaction with Carbohydrate Kinase Domain Containing Protein 英语 CARKD The relationship between these two proteins is substantiated by cooccurance across genomes and coexpression 30 The ortholog of CARKD in E coli contains a domain not present in any eukaryotic ortholog This domain has a high sequence identity to APOA1BP CARKD is a protein of unknown function and the biochemical basis for this interaction is unknown 交互作用途徑 编辑 点击基因 蛋白质和代谢产物的链接访问对应的介绍条目 1 File nbsp nbsp bSize px alt 他汀类药物途径 编辑 他汀类药物途径 编辑 这个相互作用途径可以在WikiPathways上编辑 Statin Pathway WP430 參見 编辑载脂蛋白B 心血管疾病 ApoA 1 Milano 英语 ApoA 1 Milano 參考文獻 编辑 Breslow JL Ross D McPherson J Williams H Kurnit D Nussbaum AL et al Isolation and characterization of cDNA clones for human apolipoprotein A I Proc Natl Acad Sci U S A November 1982 79 22 6861 5 PMC 347233 nbsp PMID 6294659 doi 10 1073 pnas 79 22 6861 已忽略未知参数 author name separator 帮助 已忽略未知参数 author separator 帮助 Arinami T Hirano T Kobayashi K Yamanouchi Y Hamaguchi H Assignment of the apolipoprotein A I gene to 11q23 based on RFLP in a case with a partial deletion of chromosome 11 del 11 q23 3 qter Hum Genet June 1990 85 1 39 40 PMID 1972696 doi 10 1007 BF00276323 已忽略未知参数 author name separator 帮助 已忽略未知参数 author separator 帮助 Halley P Kadakkuzha BM Faghihi MA Magistri M Zeier Z Khorkova O et al Regulation of the Apolipoprotein Gene Cluster by a Long Noncoding RNA Cell Reports 16 January 2014 6 1 222 230 PMID 24388749 doi 10 1016 j celrep 2013 12 015 已忽略未知参数 author name separator 帮助 已忽略未知参数 author separator 帮助 4 0 4 1 Entrez Gene APOA1 apolipoprotein A1 原始内容存档于2019 10 16 Zong NC Li H Li H Lam MP Jimenez RC Kim CS Deng N Kim AK Choi JH Zelaya I Liem D Meyer D Odeberg J Fang C Lu HJ Xu T Weiss J Duan H Uhlen M Yates JR Apweiler R Ge J Hermjakob H Ping P Integration of cardiac proteome biology and medicine by a specialized knowledgebase Circulation Research Oct 2013 113 9 1043 53 PMC 4076475 nbsp PMID 23965338 doi 10 1161 CIRCRESAHA 113 301151 Apolipoprotein A IV Cardiac Organellar Protein Atlas Knowledgebase COPaKB 2016 08 13 原始内容存档于2016 03 05 Wasan KM Brocks DR Lee SD Sachs Barrable K Thornton SJ Impact of lipoproteins on the biological activity and disposition of hydrophobic drugs implications for drug discovery Nature Reviews Drug Discovery January 2008 7 1 84 99 PMID 18079757 doi 10 1038 nrd2353 Yui Y Aoyama T Morishita H Takahashi M Takatsu Y Kawai C Serum prostacyclin stabilizing factor is identical to apolipoprotein A1 apo A1 A novel function of apo A1 J Clin Invest 1988 82 3 803 7 PMC 303586 nbsp PMID 3047170 doi 10 1172 JCI113682 McQueen MJ Hawken S Wang X Ounpuu S Sniderman A Probstfield J Steyn K Sanderson JE Hasani M Volkova E Kazmi K Yusuf S Lipids lipoproteins and apolipoproteins as risk markers of myocardial infarction in 52 countries the INTERHEART study a case control study Lancet 2008 372 9634 224 33 PMID 18640459 doi 10 1016 S0140 6736 08 61076 4 Dastani Z Dangoisse C Boucher B Desbiens K Krimbou L Dufour R Hegele RA Pajukanta P Engert JC Genest J Marcil M A novel nonsense apolipoprotein A I mutation apoA I E136X causes low HDL cholesterol in French Canadians Atherosclerosis March 2006 185 1 127 36 PMID 16023124 doi 10 1016 j atherosclerosis 2005 05 028 Franceschini G Sirtori M Gianfranceschi G Sirtori CR Relation between the HDL apoproteins and A I isoproteins in subjects with the AIMilano abnormality Metab Clin Exp May 1981 30 5 502 9 PMID 6785551 doi 10 1016 0026 0495 81 90188 8 Zhu X Wu G Zeng W Xue H Chen B Cysteine mutants of human apolipoprotein A I a study of secondary structural and functional properties J Lipid Res 2005 46 6 1303 11 PMID 15805548 doi 10 1194 jlr M400401 JLR200 Chiesa G Sirtori CR Apolipoprotein A I Milano current perspectives Curr Opin Lipidol 2003 14 2 159 63 PMID 12642784 doi 10 1097 00041433 200304000 00007 14 0 14 1 Apo A I Milano Trial Where are we now Cleveland Clinic 2008 07 26 原始内容存档于2007 12 21 Nissen SE Tsunoda T Tuzcu EM Schoenhagen P Cooper CJ Yasin M Eaton GM Lauer MA Sheldon WS Grines CL Halpern S Crowe T Blankenship JC Kerensky R Effect of recombinant ApoA I Milano on coronary atherosclerosis in patients with acute coronary syndromes a randomized controlled trial JAMA November 2003 290 17 2292 300 PMID 14600188 doi 10 1001 jama 290 17 2292 Apo A I Milano Cedars Sinai Heart Institute 2008 07 26 原始内容存档于2007 12 21 Singh P Singh M Kaur TP Grewal SS A novel haplotype in ApoAI CIII AIV gene region is detrimental to Northwest Indians with coronary heart disease Int J Cardiol September 2007 130 3 e93 5 PMID 17825930 doi 10 1016 j ijcard 2007 07 029 Singh P Singh M Gaur S Kaur T The ApoAI CIII AIV gene cluster and its relation to lipid levels in type 2 diabetes mellitus and coronary heart disease determination of a novel susceptible haplotype Diab Vasc Dis Res June 2007 4 2 124 9 PMID 17654446 doi 10 3132 dvdr 2007 030 Vollbach H Heun R Morris CM Edwardson JA McKeith IG Jessen F Schulz A Maier W Kolsch H APOA1 polymorphism influences risk for early onset non familial AD Ann Neurol 2005 58 3 436 41 PMID 16130094 doi 10 1002 ana 20593 Maezawa I Jin LW Woltjer RL Maeda N Martin GM Montine TJ Montine KS Apolipoprotein E isoforms and apolipoprotein A I protect from amyloid precursor protein carboxy terminal fragment associated cytotoxicity J Neurochem 2004 91 6 1312 21 PMID 15584908 doi 10 1111 j 1471 4159 2004 02818 x Solomon A Murphy CL Kestler D Coriu D Weiss DT Makovitzky J Westermark P Amyloid contained in the knee joint meniscus is formed from apolipoprotein A I Arthritis Rheum 2006 54 11 3545 50 PMID 17075859 doi 10 1002 art 22201 Ma J Liao XL Lou B Wu MP Role of apolipoprotein A I in protecting against endotoxin toxicity Acta Biochim Biophys Sin Shanghai 2004 36 6 419 24 PMID 15188057 doi 10 1093 abbs 36 6 419 Huang JT Wang L Prabakaran S Wengenroth M Lockstone HE Koethe D Gerth CW Gross S Schreiber D Lilley K Wayland M Oxley D Leweke FM Bahn S Independent protein profiling studies show a decrease in apolipoprotein A1 levels in schizophrenia CSF brain and peripheral tissues Mol Psychiatry 2007 13 12 1118 28 PMID 17938634 doi 10 1038 sj mp 4002108 Singh P Singh M Kaur T Role of apolipoproteins E and A I Epistatic villains of triglyceride mediation in coronary heart disease Int J Cardiol 2008 134 3 410 2 PMID 18378026 doi 10 1016 j ijcard 2007 12 102 Wehmeier K Beers A Haas MJ Wong NC Steinmeyer A Zugel U Mooradian AD Inhibition of apolipoprotein AI gene expression by 1 25 dihydroxyvitamin D3 Biochim Biophys Acta 2005 1737 1 16 26 PMID 16236546 doi 10 1016 j bbalip 2005 09 004 Lahoz C Pena R Mostaza JM Jimenez J Subirats E Pinto X Taboada M Lopez Pastor A Apo A I promoter polymorphism influences basal HDL cholesterol and its response to pravastatin therapy Atherosclerosis 2003 168 2 289 95 PMID 12801612 doi 10 1016 S0021 9150 03 00094 7 Fitzgerald ML Morris AL Rhee JS Andersson LP Mendez AJ Freeman MW Naturally occurring mutations in the largest extracellular loops of ABCA1 can disrupt its direct interaction with apolipoprotein A I J Biol Chem September 2002 277 36 33178 87 PMID 12084722 doi 10 1074 jbc M204996200 Deeg MA Bierman EL Cheung MC GPI specific phospholipase D associates with an apoA I and apoA IV containing complex J Lipid Res March 2001 42 3 442 51 PMID 11254757 Pussinen PJ Jauhiainen M Metso J Pyle LE Marcel YL Fidge NH Ehnholm C Binding of phospholipid transfer protein PLTP to apolipoproteins A I and A II location of a PLTP binding domain in the amino terminal region of apoA I J Lipid Res January 1998 39 1 152 61 PMID 9469594 STRING Known and Predicted Protein Protein Interactions 原始内容存档于2011 07 18 外部連結 编辑醫學主題詞表 MeSH Apolipoprotein A I Applied Research on Apolipoprotein A1 页面存档备份 存于互联网档案馆 取自 https zh wikipedia org w index php title 载脂蛋白A1 amp oldid 70868705, 维基百科,wiki,书籍,书籍,图书馆,

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