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无药物大分子治疗学:结构对 Raji B 细胞凋亡诱导的影响。

Drug-free macromolecular therapeutics: Impact of structure on induction of apoptosis in Raji B cells.

机构信息

Department of Pharmaceutics and Pharmaceutical Chemistry, CCCD, University of Utah, Salt Lake City, UT 84112, USA.

Department of Pharmaceutics and Pharmaceutical Chemistry, CCCD, University of Utah, Salt Lake City, UT 84112, USA; Department of Bioengineering, University of Utah, Salt Lake City, UT 84112, USA.

出版信息

J Control Release. 2017 Oct 10;263:139-150. doi: 10.1016/j.jconrel.2016.12.025. Epub 2016 Dec 24.

Abstract

Recently, we developed a new paradigm in macromolecular therapeutics that avoids the use of low molecular weight drugs. The activity of the "drug-free macromolecular therapeutics" is based on the biorecognition of complementary motifs at cell surface resulting in receptor crosslinking and apoptosis induction. The system is composed of two nanoconjugates: (1) a single-stranded morpholino oligonucleotide (MORF1) attached to an anti-CD20 Fab' fragment (Fab'-MORF1); (2) multiple copies of complementary oligonucleotide MORF2 grafted to a linear polymer of N-(2-hydroxypropyl)methacrylamide (HPMA) - P-(MORF2). The two conjugates crosslink CD20 antigens via MORF1-MORF2 hybridization at the surface of CD20 malignant B-cells and induce apoptosis. Preclinical studies in a murine model of human non-Hodgkin's lymphoma showed cancer cells eradication and long-term survivors. The aim of this study was to determine the relationship between the detailed structure of the nanoconjugates and apoptosis induction in Raji cells to allow system optimization. The factors studied include the length of the MORF sequence, the valence of P-(MORF2) (varying x), molecular weight of P-(MORF2), incorporation of a miniPEG spacer between Fab' and MORF1 and between polymer backbone and pendant MORF2, and comparison of two Fab' fragments, one from 1F5 antibody (Fab'), the other from Rituximab (Fab'). The results of apoptosis induction in human Burkitt's B-cell non-Hodgkin's lymphoma (NHL) Raji cells as determined using three apoptotic assays (Annexin V, Caspase 3, and TUNEL) indicated that: a) An improvement of apoptotic activity was observed for a 28 base pair MORF sequence when compared to MORFs composed of 20 and 25 base pairs. The differences depended on type of assay, concentration and exposure schedule (consecutive vs. premixed). b) The higher the valence of P-(MORF2) the higher the levels of apoptosis. c) Higher molecular weight of P-(MORF2) induced higher levels of apoptosis. d) A miniPEG spacer was effective in enhancing apoptotic levels in contrast to a miniPEG spacer. e) There was not a statistically significant difference when comparing Fab'-MORF1 with Fab'-MORF1.

摘要

最近,我们在大分子治疗学中开发了一种新的范例,避免使用低分子量药物。“无药物大分子治疗学”的活性基于细胞表面互补基序的生物识别,导致受体交联和凋亡诱导。该系统由两种纳米缀合物组成:(1)附着在抗 CD20 Fab'片段(Fab'-MORF1)上的单链吗啉代寡核苷酸(MORF1); (2)多个互补寡核苷酸 MORF2 接枝到 N-(2-羟丙基)甲基丙烯酰胺(HPMA)-P-(MORF2)的线性聚合物上。两种缀合物通过 MORF1-MORF2 杂交在 CD20 恶性 B 细胞表面交联 CD20 抗原,并诱导细胞凋亡。在人类非霍奇金淋巴瘤的鼠模型中的临床前研究显示出癌细胞的消除和长期存活。本研究的目的是确定纳米缀合物的详细结构与 Raji 细胞凋亡诱导之间的关系,以允许系统优化。研究的因素包括 MORF 序列的长度、P-(MORF2)的价数(变化 x)、P-(MORF2)的分子量、Fab'和 MORF1 之间以及聚合物主链和悬挂的 MORF2 之间的迷你 PEG 间隔物的掺入,以及两种 Fab'片段的比较,一种来自 1F5 抗体(Fab'),另一种来自利妥昔单抗(Fab')。使用三种凋亡测定法(Annexin V、Caspase 3 和 TUNEL)在人 Burkitt 的 B 细胞非霍奇金淋巴瘤(NHL)Raji 细胞中测定的凋亡诱导结果表明:a)与由 20 和 25 个碱基对组成的 MORF 相比,28 个碱基对 MORF 序列的凋亡活性得到改善。差异取决于测定法、浓度和暴露方案(连续与预混合)的类型。b)P-(MORF2)的价数越高,凋亡水平越高。c)P-(MORF2)的分子量越高,诱导的凋亡水平越高。d)与迷你 PEG 间隔物相比,迷你 PEG 间隔物有效提高了凋亡水平。e)当比较 Fab'-MORF1 与 Fab'-MORF1 时,没有统计学上的显着差异。

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