AB005. Development of tumour specific therapy for treatment of diffuse intrinsic pontine glioma (DIPG).

IF 2.1 4区医学 Q3 ONCOLOGY

Chinese clinical oncology Pub Date : 2024-08-01 DOI:10.21037/cco-24-ab005

Jiney Jose, Peter Choi, Maria Tsoli, Anjana Gopalakrishnan, Carina Lee, Thomas I I Park, David Ziegler, William Denny

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引用次数: 0

Abstract

Background: Diffuse intrinsic pontine glioma (DIPG), is an aggressive form of paediatric high-grade glioma (pHGG) that affects children below the age of 10 months. The survival period for a child suffering from DIPG has not changed in decades (approximately 10 months). This pattern is similar for most pHGG; even though the survival period is more extended, tumour recurrence and death are almost inevitable. This is primarily due to the presence of the blood-brain barrier (BBB), which blocks the entry of most therapeutics into the brain, and also due to tumour heterogeneity associated with central nervous system (CNS) tumours that blunt the efficacy of targeted therapy. The development of a meaningful cure for paediatric brain cancer hinges on discovering chemotherapy agents that (I) can cross the BBB; (II) accumulates explicitly in tumour tissues; and (III) can block pathways leading to the escape of cancer stem cells, promoting recurrence.

Methods: This project aims to develop therapeutics that can cross the BBB, a significant hindrance to delivering medicines across the brain, and specifically target cancer cells without affecting normal brain cells. We will accomplish this by attaching novel dyes possessing tumour specificity to various classes of chemotherapy agents. The compounds will be tested on patient-derived paediatric brain cancer cell lines and the most potent compounds will be progressed to an animal model of DIPG.

Results: Several drug-dye conjugates were designed and synthesized to target various aberrant pathways involved in disease initiation and progression of DIPG. These were tested first in patient-derived DIPG cell lines. Several of these drug-dye conjugates showed potent antiproliferative effect in various DIPG cell lines. One of these conjugates is currently undergoing maximum tolerated dose study in an animal model of DIPG.

Conclusions: The present work details an effort to develop BBB crossing tumour specific therapeutic agents for the treatment of DIPG. The work has resulted in several promising drug-dye conjugates showing antiproliferative activity in various patient-derived DIPG cell lines, enabling the progression of such conjugates into animal models of DIPG. Such studies will inform the utility of such drug-dye conjugates for application in difficult to treat pHGGs such as DIPG.

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AB005.开发治疗弥漫性内生性桥脑胶质瘤（DIPG）的肿瘤特异性疗法。

背景：弥漫性桥脑胶质瘤（DIPG）是儿科高级别胶质瘤（pHGG）的一种侵袭性形式，多发于10个月以下的儿童。几十年来，DIPG患儿的存活期（约10个月）从未改变。这种模式与大多数 pHGG 相似；尽管存活期更长，但肿瘤复发和死亡几乎不可避免。这主要是由于血脑屏障（BBB）的存在阻碍了大多数治疗药物进入大脑，同时中枢神经系统（CNS）肿瘤的异质性也削弱了靶向治疗的疗效。要想真正治愈小儿脑癌，关键在于发现以下化疗药物：（1）能穿过 BBB；（2）能在肿瘤组织中明确蓄积；（3）能阻断导致癌症干细胞逃逸的途径，从而促进复发：本项目旨在开发能够穿过 BBB（这是药物在大脑中输送的一大障碍）的治疗药物，并在不影响正常脑细胞的情况下专门针对癌细胞。为此，我们将在各类化疗药物上添加具有肿瘤特异性的新型染料。这些化合物将在源自患者的儿科脑癌细胞系上进行测试，最有效的化合物将用于 DIPG 动物模型：结果：设计并合成了几种药物-染料共轭物，以靶向参与 DIPG 疾病发生和发展的各种异常途径。这些药物首先在源自患者的 DIPG 细胞系中进行了测试。其中几种药物-染料共轭物在各种 DIPG 细胞系中显示出了强效的抗增殖作用。其中一种共轭物目前正在 DIPG 动物模型中进行最大耐受剂量研究：目前的工作详细介绍了为治疗 DIPG 而开发穿越 BBB 的肿瘤特异性治疗药物所做的努力。这项工作产生了几种很有前景的药物-染料共轭物，它们在各种源自患者的 DIPG 细胞系中显示出抗增殖活性，从而使这些共轭物能够进入 DIPG 动物模型。这些研究将为此类药物-染料共轭物在 DIPG 等难以治疗的 pHGG 中的应用提供信息。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Chinese clinical oncology ONCOLOGY-

CiteScore

3.90

自引率

0.00%

发文量

期刊介绍： The Chinese Clinical Oncology (Print ISSN 2304-3865; Online ISSN 2304-3873; Chin Clin Oncol; CCO) publishes articles that describe new findings in the field of oncology, and provides current and practical information on diagnosis, prevention and clinical investigations of cancer. Specific areas of interest include, but are not limited to: multimodality therapy, biomarkers, imaging, tumor biology, pathology, chemoprevention, and technical advances related to cancer. The aim of the Journal is to provide a forum for the dissemination of original research articles as well as review articles in all areas related to cancer. It is an international, peer-reviewed journal with a focus on cutting-edge findings in this rapidly changing field. To that end, Chin Clin Oncol is dedicated to translating the latest research developments into best multimodality practice. The journal features a distinguished editorial board, which brings together a team of highly experienced specialists in cancer treatment and research. The diverse experience of the board members allows our editorial panel to lend their expertise to a broad spectrum of cancer subjects.