OATD - 02验证了药理学抑制精氨酸酶1和2在癌症中的益处。
OATD-02 Validates the Benefits of Pharmacological Inhibition of Arginase 1 and 2 in Cancer.
作者信息
Grzybowski Marcin Mikołaj, Stańczak Paulina Seweryna, Pomper Paulina, Błaszczyk Roman, Borek Bartłomiej, Gzik Anna, Nowicka Julita, Jędrzejczak Karol, Brzezińska Joanna, Rejczak Tomasz, Güner-Chalimoniuk Nazan Cemre, Kikulska Agnieszka, Mlącki Michał, Pęczkowicz-Szyszka Jolanta, Olczak Jacek, Gołębiowski Adam, Dzwonek Karolina, Dobrzański Paweł, Zasłona Zbigniew
机构信息
Molecure SA, 02-089 Warsaw, Poland.
出版信息
Cancers (Basel). 2022 Aug 17;14(16):3967. doi: 10.3390/cancers14163967.
BACKGROUND
Arginases play essential roles in metabolic pathways, determining the fitness of both immune and tumour cells. Along with the previously validated role of ARG1 in cancer, the particular significance of ARG2 as a therapeutic target has emerged as its levels correlate with malignant phenotype and poor prognosis. These observations unveil arginases, and specifically ARG2, as well-validated and promising therapeutic targets. OATD-02, a new boronic acid derivative, is the only dual inhibitor, which can address the benefits of pharmacological inhibition of arginase 1 and 2 in cancer.
METHODS
The inhibitory activity of OATD-02 was determined using recombinant ARG1 and ARG2, as well as in a cellular system using primary hepatocytes and macrophages. In vivo antitumor activity was determined in syngeneic models of colorectal and kidney carcinomas (CT26 and Renca, respectively), as well as in an ARG2-dependent xenograft model of leukaemia (K562).
RESULTS
OATD-02 was shown to be a potent dual (ARG1/ARG2) arginase inhibitor with a cellular activity necessary for targeting ARG2. Compared to a reference inhibitor with predominant extracellular activity towards ARG1, we have shown improved and statistically significant antitumor efficacy in the CT26 model and an immunomodulatory effect reflected by Treg inhibition in the Renca model. Importantly, OATD-02 had a superior activity when combined with other immunotherapeutics. Finally, OATD-02 effectively inhibited the proliferation of human K562 leukemic cells both in vitro and in vivo.
CONCLUSIONS
OATD-02 is a potent small-molecule arginase inhibitor with optimal drug-like properties, including PK/PD profile. Excellent activity against intracellular ARG2 significantly distinguishes OATD-02 from other arginase inhibitors. OATD-02 represents a very promising drug candidate for the combined treatment of tumours, and is the only pharmacological tool that can effectively address the benefits of ARG1/ARG2 inhibition. OATD-02 will enter clinical trials in cancer patients in 2022.
背景
精氨酸酶在代谢途径中发挥着重要作用,决定着免疫细胞和肿瘤细胞的适应性。随着ARG1在癌症中的作用得到先前验证,ARG2作为治疗靶点的特殊意义也已显现,因为其水平与恶性表型和不良预后相关。这些观察结果揭示了精氨酸酶,特别是ARG2,是经过充分验证且有前景的治疗靶点。新型硼酸衍生物OATD-02是唯一的双重抑制剂,它能发挥药理学抑制精氨酸酶1和2在癌症治疗中的益处。
方法
使用重组ARG1和ARG2测定OATD-02的抑制活性,并在使用原代肝细胞和巨噬细胞的细胞系统中进行测定。在结直肠癌和肾癌的同基因模型(分别为CT26和Renca)以及白血病的ARG2依赖性异种移植模型(K562)中测定体内抗肿瘤活性。
结果
OATD-02被证明是一种有效的双重(ARG1/ARG2)精氨酸酶抑制剂,具有靶向ARG2所需的细胞活性。与对ARG1具有主要细胞外活性的参考抑制剂相比,我们已证明在CT26模型中抗肿瘤疗效有所改善且具有统计学意义,在Renca模型中表现为对调节性T细胞的抑制所反映的免疫调节作用。重要的是,OATD-02与其他免疫疗法联合使用时具有更强的活性。最后,OATD-02在体外和体内均有效抑制人K562白血病细胞的增殖。
结论
OATD-02是一种有效的小分子精氨酸酶抑制剂,具有包括药代动力学/药效学特征在内的最佳类药性质。对细胞内ARG2的优异活性使OATD-02与其他精氨酸酶抑制剂显著区分开来。OATD-02是联合治疗肿瘤非常有前景的候选药物,并且是唯一能有效发挥抑制ARG1/ARG2益处的药理学工具。OATD-02将于2022年进入癌症患者的临床试验。
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