Preclinical toxicological assessment of amido-bridged nucleic acid-modified antisense oligonucleotides targeting synaptotagmin XIII for intra-abdominal treatment of peritoneal metastasis of gastric cancer.

IF 6 1区 医学 Q1 GASTROENTEROLOGY & HEPATOLOGY Gastric Cancer Pub Date : 2024-11-01 Epub Date: 2024-08-27 DOI:10.1007/s10120-024-01548-9
Mitsuro Kanda, Nao Takano, Hiroshi Miyauchi, Kohei Ueda, Masaaki Mizuno, Yuuya Kasahara, Yasuhiro Kodera, Satoshi Obika
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Abstract

Background: Peritoneal metastasis of gastric cancer is closely associated with dismal prognosis. In previous preclinical proof-of-concept studies, an amido-bridged nucleic acid (AmNA)-modified antisense oligonucleotide (ASO), designated ASO-4733 that targets the gene encoding synaptotagmin XIII (SYT13), inhibited cellular functions required for the formation of peritoneal metastasis of gastric cancer cells. ASO-4733 achieved therapeutic effects when intra-abdominally administered to mouse xenograft models. Here, we conducted an analysis of Syt13-deficient mice to determine the pharmacokinetics and toxicity of intra-abdominal administration of ASO-4733.

Methods: The effects of Syt13-deficiency in mice were determined. Good Laboratory Practice toxicity tests and the toxicokinetics of intra-abdominal administration of ASO-4733 were conducted in cynomolgus monkeys and rats. The pharmacokinetics of ASO-4733 administered intravenously or intra-abdominally to rats were investigated.

Results: Syt13-deficient mice exhibited normal reproduction, organ functions, and motor functions. Weekly intra-abdominal administration of ASO-4733 (125 mg/kg), corresponding to a 50-fold increase of the estimated clinical dose for 4 weeks, was well tolerated by cynomolgus monkeys. In rats, off-target toxicity (not attributable to hybridization) was observed after weekly intra-abdominal administration of ASO-4733. Blood concentrations of ASO-4733 were lower and rose more slowly after intra-abdominal administration compared with intravenous administration.

Conclusions: The preclinical profile of intra-abdominal administration of ASO-4733 demonstrated its suitability for entry into clinical trials of patients with peritoneal metastasis of gastric cancer.

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针对突触素敏 XIII 的氨基桥接核酸修饰反义寡核苷酸用于腹腔内治疗胃癌腹膜转移的临床前毒理学评估。
背景:胃癌腹膜转移与预后不良密切相关:胃癌腹膜转移与预后不良密切相关。在之前的临床前概念验证研究中,一种氨基桥接核酸(AmNA)修饰的反义寡核苷酸(ASO)(ASO-4733)靶向编码突触诱导素 XIII(SYT13)的基因,抑制了胃癌细胞形成腹膜转移所需的细胞功能。ASO-4733 在小鼠异种移植模型中腹腔给药后取得了治疗效果。在此,我们对Syt13缺陷小鼠进行了分析,以确定腹腔给药ASO-4733的药代动力学和毒性:方法:确定 Syt13 缺陷对小鼠的影响。在猴和大鼠体内进行了良好实验室规范毒性试验和腹腔注射 ASO-4733 的毒代动力学试验。研究了大鼠静脉注射或腹腔注射 ASO-4733 的药代动力学:结果:Syt13缺陷小鼠的生殖、器官功能和运动功能正常。腹腔注射 ASO-4733(125 毫克/千克)每周一次,相当于估计临床剂量的 50 倍,连续注射 4 周,猴的耐受性良好。对大鼠每周腹腔注射 ASO-4733 后,观察到了脱靶毒性(与杂交无关)。与静脉给药相比,腹腔给药后 ASO-4733 的血药浓度更低,且上升速度更慢:ASO-4733腹腔内给药的临床前特征表明,它适合用于胃癌腹膜转移患者的临床试验。
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来源期刊
Gastric Cancer
Gastric Cancer 医学-胃肠肝病学
CiteScore
14.70
自引率
2.70%
发文量
80
审稿时长
6-12 weeks
期刊介绍: Gastric Cancer is an esteemed global forum that focuses on various aspects of gastric cancer research, treatment, and biology worldwide. The journal promotes a diverse range of content, including original articles, case reports, short communications, and technical notes. It also welcomes Letters to the Editor discussing published articles or sharing viewpoints on gastric cancer topics. Review articles are predominantly sought after by the Editor, ensuring comprehensive coverage of the field. With a dedicated and knowledgeable editorial team, the journal is committed to providing exceptional support and ensuring high levels of author satisfaction. In fact, over 90% of published authors have expressed their intent to publish again in our esteemed journal.
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