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Proteomic identification of galectin-3 binding ligands and characterization of galectin-3 proteolytic cleavage in human prostasomes

机译:galectin-3结合配体的蛋白质组学鉴定和人类prosomesome中galectin-3蛋白水解切割的表征

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摘要

Galectin-3 is a multifunctional carbohydrate-binding protein that was previously characterized as a proteolytic substrate for prostate-specific antigen (PSA) and was shown to be associated with prostasomes in human semen. Prostasomes are exosome-like vesicles that are secreted by the prostatic epithelium and have multiple proposed functions in normal reproduction and prostate cancer. In the current study, galectin-3 binding ligands in human prostasomes were identified and characterized with the goal to investigate galectin-3 function in prostasomes. Galectin-3 binding proteins were isolated by affinity column chromatography. Candidate ligands identified by MS/MS were PSA, prostatic acid phosphatase (PAP), zinc alpha-2-glycoprotein (ZAG), dipeptidyl peptidase-4 (CD26), aminopeptidase N (CD13), neprilysin, clusterin, antibacterial protein (FALL-39) and alpha-1-acid glycoprotein (ORM1). Biochemical methods were used to characterize the ability of galectin-3 to bind to selected ligands, and galectin-3 cleavage assays were utilized to investigate the protease(s) in prostasomes that cleaves galectin-3. CD26, CD13, PSA, PAP and ZAG immunoreactivity were detected in extracts of purified prostasomes. One-dimensional electroblot analysis of prostasomes demonstrated that CD26, PAP and CD13 immunoreactivity co-migrated with galectin-3-reactive protein bands. PSA and ZAG were found to be associated with the surface of prostasomes. Both intact and cleaved galectin-3 were detected in prostate and prostasome extracts. Cleavage and inhibition assays indicated that PSA in prostasomes proteolytically cleaves galectin-3. The identification of these glycoproteins as galectin-3 ligands lays the groundwork for future studies of galectin-3 and prostasome function in reproduction and prostate cancer.
机译:Galectin-3是一种多功能的碳水化合物结合蛋白,以前被表征为前列腺特异抗原(PSA)的蛋白水解底物,并被证明与人精液中的前体相关。前体是由前列腺上皮分泌的外泌体样囊泡,在正常生殖和前列腺癌中具有多种提议的功能。在当前的研究中,鉴定和表征了人类前列腺中的galectin-3结合配体,目的是研究galectin-3在前列腺中的功能。通过亲和柱色谱法分离Galectin-3结合蛋白。通过MS / MS鉴定的候选配体为PSA,前列腺酸磷酸酶(PAP),α-2-糖蛋白锌(ZAG),二肽基肽酶-4(CD26),氨基肽酶N(CD13),中性溶酶,簇蛋白,抗菌蛋白(FALL- 39)和α-1-酸糖蛋白(ORM1)。生化方法用于表征半乳凝素3与选定配体结合的能力,半乳凝素3裂解分析用于研究裂解半乳凝素3的前体中的蛋白酶。在纯化的前体提取物中检测到CD26,CD13,PSA,PAP和ZAG免疫反应性。一维蛋白质体印迹分析表明,CD26,PAP和CD13免疫反应性与半乳糖凝集素3反应性蛋白带共同迁移。发现PSA和ZAG与前体表面有关。在前列腺和前体提取物中均检测到完整和切割的半乳凝素3。切割和抑制测定表明,前体中的PSA蛋白水解切割galectin-3。将这些糖蛋白鉴定为galectin-3配体,为将来研究galectin-3和前列腺素在生殖和前列腺癌中的功能奠定了基础。

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