AACR 2021:抗CD47抗体AO-176治疗实体瘤和多发性骨髓瘤,临床前试验取得积极结果

2021-03-11 Allan MedSci原创

生物技术公司Arch Oncology今天宣布,在美国癌症研究协会(AACR)年会上介绍了AO-176的最新临床前数据。

生物技术公司Arch Oncology今天宣布,在美国癌症研究协会(AACR)年会上介绍了AO-176的最新临床前数据。AO-176是一种抗CD47抗体,可通过阻断“don't eat me”信号并直接杀死肿瘤细胞而发挥作用,并优先与肿瘤细胞结合。目前,AO-176正在I/II期临床试验中进行评估,以单一疗法或与标准疗法相结合的方式治疗部分实体瘤和多发性骨髓瘤。

AO-176是一种人源化的抗CD47 IgG2抗体。AO-176通过阻止“don't eat me”信号(抗CD47抗体的标准机制)起作用。除阻断该信号外,AO-176还具有其他机制,包括直接杀死肿瘤细胞和诱导DAMP(损伤相关分子模式),从而导致免疫原性细胞死亡。重要的是,AO-176优先与肿瘤细胞结合,而不与正常细胞结合,并且在酸性微环境(低pH)中更有效地与肿瘤结合。

Arch Oncology首席科学官Daniel Pereira博士说:“我们将在今年的AACR上展示两个新的非临床数据集,以证明AO-176在淋巴瘤和儿科T-ALL中具有强大的治疗潜力。在淋巴瘤中,AO-176在淋巴瘤异种移植物中表现出很强的活性。在酸性pH下,AO-176能够与淋巴瘤细胞的结合。AO-176或与利妥昔单抗联合使用。最后,还将介绍AO-176独特的诱导膜联蛋白V和DAMPs的独特能力,这些蛋白最终可能有助于诱导淋巴瘤细胞的免疫原性细胞死亡”。

 

原始出处:

https://www.firstwordpharma.com/node/1808442?tsid=4

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    2021-03-28 病毒猎手

    #CD47抗体#作为#巨噬细胞#信号,在巨噬细胞抗癌中发挥主要作用,与PD-1类药物联合使用,充分将巨噬细胞+T细胞双重激活,应该具有一定的协同作用。未来与#NK细胞#活化分子再结合,可能真正能解决大部分实体瘤的问题,未来远景可能也就10年时间,应该又是一个划时代进步。到2030年以后,会针对肿瘤的蛋白和基因,出现#mRNA疫苗#,针对肿瘤蛋白靶向降解#PROTAC#,以及更针对性的肿瘤基因治疗出现,肿瘤届时真正成为慢病了。

    0

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    2021-03-11 356947897

    学习了,受教

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