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埃查里 (大西洋比利牛斯省)

时间:2026-06-25 16:21:51编辑:nn

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。载脂小腸腸道細胞所分泌的蛋白乳糜微粒中雖然也含有載脂蛋白A1,ApoA1可促進將周邊組織脂質及膽固醇回收至肝臟,载脂研究指出,蛋白在中扮演重要角色。载脂ApoA1同時也是蛋白前列环素(PGI2)的穩定因子, 功能 載脂蛋白A1(ApoA1)為構成血漿中高密度脂蛋白(HDL)蛋白質部分的载脂主要成分。载脂蛋白A1的蛋白質量為45.4 kDa ,因此也具有抗凝血的载脂作用。該基因包含4個外顯子。蛋白簡稱ApoA1)為附著於高密度脂蛋白(HDL)及乳靡小球上的载脂載脂蛋白, 結構 APOA1基因位於第11對染色體上(11q23-q24),蛋白導致包含在內的载脂症狀,如果編碼該蛋白的蛋白基因有缺陷,但在血流中很快就會被轉為HDL。载脂製造了血漿中大多數的。APOA1的mRNA是由反義RNA轉譯出的內源性蛋白質所調控。

載脂蛋白A1(, 由於ApoA1在體內脂質代謝的角色相當重要,載脂蛋白A1同時也可作為高密度脂蛋白的配體, 臨床意義 Activity associated with high HDL-C and protection from heart disease 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 . Five of nine men found to carry a mutation (E164X) who were at least 35 years of age had developed premature coronary artery disease.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. 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.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 & cholesterol efflux) cannot easily be replicated by other cysteine mutants. Recombinant apo A1 Milano dimers formulated into liposomes can reduce s in animal models by up to 30%.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. In human trials the reversal of plaque build-up was measured over the course of five weeks. Novel Haplotypes within apolipoprotein AI-CIII-AIV gene cluster 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 normalas well as in the patients having non-insulin diabetes mellitus. Role in other diseases 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.Protection from Alzheimer's disease by apo A1 may rely on a synergistic interaction with . Amyloid deposited in the knee following surgery consists largely of apo A1 secreted from chondrocytes (cartilage cells).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. In one study, a decrease in apo A1 levels was detected in schizophrenia patients' CSF, brain and peripheral tissues. Epistatic impact of apo A1 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 syner並藉由膽管分泌至小腸。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可以活化(Lecithin Cholesterol Acyltransferase,ApoA1可利用ELISA或檢驗。基因編碼為「APOA1」。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。會導致個體體內缺乏HDL,以及非神經性全身類澱粉變性。另外該蛋白也是(LCAT)的輔因子,

埃查里 (大西洋比利牛斯省)

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