Immunoliposomes for Neuroblastoma: Review of the Past Experience and Design of a Novel Nanoparticle.

IF 1.6 4区 医学 Q4 ONCOLOGY
William S Panosyan, Daniel E Panosyan
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引用次数: 0

Abstract

Background/aim: High-risk/refractory neuro-blastoma (NBL) treatments include anti-GD2-monoclonal antibodies (mAbs). Several immunoliposomes (ILs) covered with anti-GD2-mAbs (GD2-ILs) have been tested pre-clinically. We aimed to review literature on GD2-IL for characteristics of nanoparticles/payloads, conjugation of mAb/fragments and preclinical data, as well as to explore the feasibility of a recently proposed GD2-IL loaded with the antimetabolite oxamate.

Materials and methods: Initial PubMed search was generalized for immunoliposomes in cancer. Further search was focused on papers for GD2-IL [keywords: "Immunoliposomes and cancer (or neuroblastoma)"].

Results: There were 811 results on "immunoliposomes"; >50% were on "immunoliposomes, cancer" (n=439, June 2024). Seventeen items resulted from "immunoliposomes, neuroblastoma" (one was "publishers' correction"). Sixteen GD2-IL references were reviewed (1993-current). The mean±SD GD2-ILs size was 124.8±31 nm (range=86-171). Six papers described GD2-ILs with DNA-damaging agents [doxorubicin (n=4), etoposide (n=1), irinotecan+HDAC inhibitor (n=1)]. Other payloads included: fenretinide (n=4 papers), C-myb antisense (n=2), survivin inhibitor (n=1), tyrosine kinase inhibitor (n=1), IL15 (n=1), and oxamate (n=1). These 9 drug-loads included both hydrophilic and hydrophobic molecules. Except for IL15 and C-myb antisense with high molecular weights (MWs), and oxamate with low MW, the remaining compounds had comparable MWs (496±100 g/mol, range=349-588.6). The overall encapsulation efficiency was 66.2±25.6%. There were 17-30 mAb molecules attached to an IL with PEGylation. Experiments with GD2-positive/GD2-negative cells demonstrated selective efficacy/tropism of GD2-ILs. Mouse models confirmed efficacy, GD2-specific tumor accumulation, decreased toxicity, and improved pharmacokinetic-pharmacodynamics.

Conclusion: PEGylated anti-GD2-IL may allow NBL tropism. A size of approximately 100 nm could allow vascular permeability and packaging of oxamate in amounts needed for profound/selective lactate dehydrogenase-A inhibition. Thus, oxamate-loaded GD2-ILs may allow exploring the great translational potential of Warburg effect inhibition in GD2-positive cancers.

治疗神经母细胞瘤的免疫脂质体:回顾过去的经验,设计新型纳米粒子。
背景/目的:高危/难治性神经母细胞瘤(NBL)的治疗方法包括抗 GD2-单克隆抗体(mAbs)。临床前已对几种包覆有抗 GD2-mAbs(GD2-ILs)的免疫脂质体(ILs)进行了测试。我们旨在回顾有关GD2-IL的文献,以了解纳米颗粒/载荷的特点、mAb/碎片的共轭情况和临床前数据,并探讨最近提出的一种负载有抗代谢物草酸盐的GD2-IL的可行性:最初在 PubMed 上搜索癌症免疫脂质体。进一步搜索的重点是有关 GD2-IL 的论文[关键词:"免疫脂质体和癌症(或神经母细胞瘤)"]:结果:共有 811 条关于 "免疫脂质体 "的结果;超过 50% 的结果涉及 "免疫脂质体、癌症"(n=439,2024 年 6 月)。17项结果来自 "免疫脂质体、神经母细胞瘤"(1项为 "出版商更正")。查阅了 16 篇 GD2-IL 参考文献(1993 年至今)。GD2-IL的平均±SD大小为124.8±31 nm(范围=86-171)。六篇论文描述了含有DNA损伤剂[多柔比星(n=4)、依托泊苷(n=1)、伊立替康+HDAC抑制剂(n=1)]的GD2-ILs。其他载药包括:非瑞替尼(n=4)、C-myb 反义(n=2)、存活素抑制剂(n=1)、酪氨酸激酶抑制剂(n=1)、IL15(n=1)和草酸盐(n=1)。这 9 种药物负载包括亲水性和疏水性分子。除了 IL15 和 C-myb antisense 的分子量较高,草氨酸的分子量较低外,其余化合物的分子量相当(496±100 g/mol,范围=349-588.6)。总体封装效率为 66.2±25.6%。有 17-30 个 mAb 分子附着在 PEG 化的 IL 上。用 GD2 阳性/GD2 阴性细胞进行的实验表明,GD2-ILs 具有选择性功效/倾向性。小鼠模型证实了药效、GD2 特异性肿瘤蓄积、毒性降低以及药代动力学-药效学的改善:结论:PEG化的抗GD2-IL可能具有NBL趋向性。约 100 nm 的尺寸可实现血管通透性,并将草酸盐包装成深度/选择性乳酸脱氢酶-A 抑制所需的量。因此,含有草氨酸的 GD2-IL可能有助于探索抑制 GD2 阳性癌症的沃伯格效应的巨大转化潜力。
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来源期刊
Anticancer research
Anticancer research 医学-肿瘤学
CiteScore
3.70
自引率
10.00%
发文量
566
审稿时长
2 months
期刊介绍: ANTICANCER RESEARCH is an independent international peer-reviewed journal devoted to the rapid publication of high quality original articles and reviews on all aspects of experimental and clinical oncology. Prompt evaluation of all submitted articles in confidence and rapid publication within 1-2 months of acceptance are guaranteed. ANTICANCER RESEARCH was established in 1981 and is published monthly (bimonthly until the end of 2008). Each annual volume contains twelve issues and index. Each issue may be divided into three parts (A: Reviews, B: Experimental studies, and C: Clinical and Epidemiological studies). Special issues, presenting the proceedings of meetings or groups of papers on topics of significant progress, will also be included in each volume. There is no limitation to the number of pages per issue.
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