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血浆抗α-半乳糖苷抗体与脂蛋白(a)(Lp(a))中载脂蛋白(a)亚基富含丝氨酸和苏氨酸的肽序列结合。

Plasma anti-α-galactoside antibody binds to serine- and threonine-rich peptide sequence of apo(a) subunit in Lp(a).

作者信息

Geetha M, Kalaivani V, Sabarinath P S, Appukuttan P S

机构信息

Department of Biochemistry, Sree Chitra Tirunal Institute for Medical Sciences and Technology, Thiruvananthapuram, 695011, India.

出版信息

Glycoconj J. 2014 May;31(4):289-98. doi: 10.1007/s10719-014-9521-2. Epub 2014 Apr 11.

Abstract

Lipoprotein(a) immune complexes [Lp(a) IC] of varying particle density obtained by ultracentrifugation of plasma from normal healthy donors were markedly dominated by IgG. Lp(a) and immunoglobulins were liberated from plasma Lp(a) IC by treatment with melibiose, a sugar specific for circulating anti-α-galactoside antibody (anti-Gal). Upon incubation with plasma lipoprotein fraction anti-Gal but not the α-glucoside-specific antibody from human plasma formed de novo IC with Lp(a). Binding of Lp(a) sugar-reversibly enhanced the fluorescence of FITC-labeled anti-Gal as did binding of α-galactoside-containing glycoproteins. This effect apparently due to conformational shift in the Fc region of the antibody was also produced by apo(a) subunit separated from Lp(a) and de-O-glycosylated apo(a) but not by any other plasma lipoproteins or by Lp(a) pre-incubated with the O-glycan-specific lectin jacalin. O-Glycans and their terminal sialic acid moieties in apo(a) of circulating Lp(a)-anti-Gal IC, in contrast to those in pure Lp(a), were inaccessible to jacalin and anion exchange resin, respectively. Unlike other plasma lipoproteins, Lp(a) inhibited Griffonia simplicifolia isolectin B4 which also accommodates serine- and threonine-rich peptide sequence (STPS) as surrogate ligand to α-galactosides at its binding site. Results suggest that anti-Gal recognizes STPS in the O-glycan-rich regions of apo(a) subunit in Lp(a) which contains no α-linked galactose.

摘要

通过超速离心从正常健康供体血浆中获得的不同颗粒密度的脂蛋白(a)免疫复合物[Lp(a) IC]中,IgG占主导地位。通过用蜜二糖(一种循环抗α-半乳糖苷抗体(抗Gal)特异性的糖)处理,可从血浆Lp(a) IC中释放出Lp(a)和免疫球蛋白。与血浆脂蛋白部分一起孵育时,抗Gal而非人血浆中的α-葡萄糖苷特异性抗体与Lp(a)形成了新生IC。Lp(a)糖的结合可逆地增强了FITC标记的抗Gal的荧光,含α-半乳糖苷的糖蛋白的结合也有此效果。这种显然由抗体Fc区域构象变化引起的效应,也由从Lp(a)分离的载脂蛋白(a)亚基和去O-糖基化的载脂蛋白(a)产生,但其他血浆脂蛋白或预先与O-聚糖特异性凝集素红豆蔻凝集素孵育的Lp(a)则不会产生。与纯Lp(a)中的O-聚糖及其末端唾液酸部分相比,循环Lp(a)-抗Gal IC的载脂蛋白(a)中的O-聚糖及其末端唾液酸部分分别无法与红豆蔻凝集素和阴离子交换树脂结合。与其他血浆脂蛋白不同,Lp(a)抑制了简单型非洲豆蔻凝集素B4,该凝集素在其结合位点也容纳富含丝氨酸和苏氨酸的肽序列(STPS)作为α-半乳糖苷的替代配体。结果表明,抗Gal识别Lp(a)中载脂蛋白(a)亚基富含O-聚糖区域中的STPS,该区域不含α-连接的半乳糖。

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