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从Gla结构域到一种新型的细胞凋亡小分子检测剂。

From the Gla domain to a novel small-molecule detector of apoptosis.

作者信息

Cohen Avi, Shirvan Anat, Levin Galit, Grimberg Hagit, Reshef Ayelet, Ziv Ilan

机构信息

Aposense Ltd, 5-7 Ha'Odem St, Kiryat Matalon, PO Box 7119, Petach Tikva, Israel.

出版信息

Cell Res. 2009 May;19(5):625-37. doi: 10.1038/cr.2009.17.

Abstract

Apoptosis plays a pivotal role in the etiology or pathogenesis of numerous medical disorders, and thus, targeting of apoptotic cells may substantially advance patient care. In our quest for novel low-molecular-weight probes for apoptosis, we focused on the uncommon amino acid gamma-carboxyglutamic acid (Gla), which plays a vital role in the binding of clotting factors to negatively charged phospholipid surfaces. Based on the alkyl-malonic acid motif of Gla, we have developed and now present ML-10 (2-(5-fluoro-pentyl)-2-methyl-malonic acid, MW=206 Da), the prototypical member of a novel family of small-molecule detectors of apoptosis. ML-10 was found to perform selective uptake and accumulation in apoptotic cells, while being excluded from either viable or necrotic cells. ML-10 uptake correlates with the apoptotic hallmarks of caspase activation, Annexin-V binding and disruption of mitochondrial membrane potential. The malonate moiety was found to be crucial for ML-10 function in apoptosis detection. ML-10 responds to a unique complex of features of the cell in early apoptosis, comprising irreversible loss of membrane potential, permanent acidification of cell membrane and cytoplasm, and preservation of membrane integrity. ML-10 is therefore the most compact apoptosis probe known to date. Due to its fluorine atom, ML-10 is amenable to radio-labeling with the (18)F isotope, towards its potential future use for clinical positron emission tomography imaging of apoptosis.

摘要

细胞凋亡在众多医学病症的病因学或发病机制中起着关键作用,因此,针对凋亡细胞可能会极大地改善患者护理。在我们寻找新型低分子量细胞凋亡探针的过程中,我们聚焦于不常见的氨基酸γ-羧基谷氨酸(Gla),它在凝血因子与带负电荷的磷脂表面结合中起着至关重要的作用。基于Gla的烷基丙二酸基序,我们开发并展示了ML-10(2-(5-氟戊基)-2-甲基丙二酸,分子量=206 Da),这是一种新型小分子细胞凋亡探测器家族的原型成员。发现ML-10在凋亡细胞中进行选择性摄取和积累,而活细胞或坏死细胞则将其排除。ML-10的摄取与半胱天冬酶激活、膜联蛋白-V结合以及线粒体膜电位破坏等细胞凋亡标志相关。发现丙二酸部分对于ML-10在细胞凋亡检测中的功能至关重要。ML-10对早期凋亡细胞的独特特征复合体做出反应,包括膜电位的不可逆丧失、细胞膜和细胞质的永久性酸化以及膜完整性的保留。因此,ML-10是迄今为止已知的最紧凑的细胞凋亡探针。由于其氟原子,ML-10适合用(18)F同位素进行放射性标记,有望未来用于细胞凋亡的临床正电子发射断层扫描成像。

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